*Helicobacter pylori***—Associated Dyspepsia in Paediatrics**

Mónica Roxo-Rosa, Mónica Oleastro and Ana Isabel Lopes

Additional information is available at the end of the chapter

http://dx.doi.org/10.5772/56551

### **1. Introduction**

[40] Watanabe K, Tanaka A, Imase K, et al. Amoxicillin resistance in Helicobacter pylori: studies from Tokyo, Japan from 1985 to 2003*. Helicobacter* 2005; 10(1):4–11.

[41] Mahachai V, Sirimontaporn N, Tumwasorn S, et al. Sequential Therapy in Clarithro‐ mycin Sensitive and Resistant *H. pylori* Based on PCR Molecular Test. *J Gastroenterol*

[42] van Zanten SJ, Goldie J, Hollingsworth J, et al. Secretion of intravenously adminis‐ tered antibiotics in gastric juice: implications for management of *Helicobacter pylori*. *J*

[43] Tytgat GN. Treatments that impact favorably upon the eradication of Helicobacter

[44] Segura AM, Gutierrez O, OteroW, et al. Furazolidone, amoxycillin, bismuth triple therapy for Helicobacter pylori infection. *Aliment Pharmacol Ther* 1997;11(3):529–32.

[45] Mahachai V, Treeprasertsuk S, Chaithongrat S, Vilaichone RK. Seven day Bismuthbased quadruple therapy as an initial therapy for *Helicobacter pylori* infection in a

[46] Kongchayanun C,Vilaichone RK, Pornthisarn B, et al. Pilot studies to identify the op‐ timum duration of concomitant *Helicobacter pylori* eradication therapy in Thailand.

pylori and ulcer recurrence. *Aliment Pharmacol Ther* 1994;8(4):359–68.

high Metroninazole resistant area. *Helicobacter* 2007; 12(4) (A).

*Hepatol* 2011; 26(5):825-8.

68 Dyspepsia - Advances in Understanding and Management

*Clin Pathol* 1992; 45(3):225–7.

*Helicobacter* 2012; 17(4):282-5.

*Helicobacter pylori* ubiquitously infects the human gastric mucosa since time immemorial, predictably before the man's diaspora out of East Africa around 58,000 years ago [1]. Colonization may have been somehow beneficial for human carriers, allowing the coevolution of this gram-negative bacterium and its host over the centuries. Yet, at least nowadays [2], this may not be a peaceful association, with infection almost invariably causing an acute host immune response. However, in a fully adapted manner, *H. pylori* avoids recognition and, thus, clearance, by the host immune system, with both infection and the consequent gastritis persisting throughout the patients' life. The clinical outcome of this persistence is dependent on a sophisticated crosstalk between the host and the pathogen. If often asymptomatic, the *H. pylori*-associated non-ulcer dyspepsia is clearly the strongest aetiological factor for severe gastric diseases that will develop late in adult life in a minority of infected patients, *i.e.*, peptic ulcer disease, both gastric and duodenal ulcers, and gastric cancer, namely, adenocarcinoma and mucosa associated lymphoid tissue (MALT) lymphom*a (reviewed in [3])*. Peptic ulcer disease rarely occurs soon after *H. pylori* infection [4-8] that generally starts in childhood; this presumably reflects marked differen‐ ces in the virulence [9-16] and/or in the susceptibility of young patients [17-19].

This chapter, focussing on the paediatric population, seeks to explore: the prevalence of *H. pylori* infection; the molecular mechanism used by *H. pylori* during colonization and infection; the role of this bacterium in the development of peptic ulcer-related organic dyspepsia; and the genetic/proteome profile of the *H. pylori*-strains associated with peptic ulcer disease.

© 2013 Roxo-Rosa et al.; licensee InTech. This is a paper distributed under the terms of the Creative Commons Attribution License (http://creativecommons.org/licenses/by/3.0), which permits unrestricted use, distribution, and reproduction in any medium, provided the original work is properly cited.

#### **1.1. Prevalence of infection**

*H. pylori* is one of the most common gastrointestinal bacterial infections among humans, affecting more than 50% of the world's population [1,20]. *Infection is usually acquired during the first years of life in both developing and industrialized countries, with* intra-familial spread playing a central role in transmission of the infection [21,22]. The prevalence of *H. pylori* is markedly variable between developing and developed countries, and even among individuals living in the same country, varying according to ethnicity, place of birth and socioeconomic factors. Besides geographic area, age is also significantly and independently associated with an increase in *H. pylori* prevalence, a phenomenon known as birth cohort effect, which is a progressive reduction of the infection rate in successive birth cohorts, due to the improvements in general living conditions (reviewed in [23]). In less developed countries the infection rate reaches almost 50% in very young children and more than 90% in adults, whereas in indus‐ trialized countries *H. pylori* infects 20-50% of adults and less than 10% of children, and has been declining over time [23,24]. Indeed, the prevalence of *H. pylori* infection is *showing a decreased trend* worldwide that *is directly associated with an improvement in the socioeconomic status and hygienic conditions of the populations.*

associated molecular mechanisms as a top priority to define disease-risk and to target *H. pylori* eradication in high-risk individuals. Ultimately, it may provide novel bacterial and/or

*Helicobacter pylori*—Associated Dyspepsia in Paediatrics

http://dx.doi.org/10.5772/56551

71

In a fully adapted manner, during colonization and persistence, this neutralophile bacterium resists gastric acidity mainly through its urease activity. Its urease enzyme, a Ni2+-containing dodecameric protein of approximately 1100 kDa, composed of 12 small subunits, UreA (27 kDa), and 12 large subunits, UreB (62 kDa), catalyzes the hydrolysis of urea into ammonia and carbon dioxide, buffering both the bacteria cytoplasm and periplasm [39]. Accounting for 5-10% of the total protein content, urease is one of the most abundant proteins in the *H. pylori* proteome [16,30]. Probably due to the toxicity of ammonia, urease activity is known to be dependent on low pH and/or Ni2+ concentration conditions [39,40], being essential for bacteria survival only under acidic conditions. In the early stages of colonization, *H. pylori* seeks parts of the stomach with higher pH, such as the antrum (the distal part of the stomach). Indeed, this bacterium uses the pH gradient as chemotactic signal to achieve regions of neutral pH, since its spatial orientation is lost in the absence of the mucus pH gradient [41]. Thus, the

acid-producing parietal cells may protect the corpus region from initial invasion.

epithelial cells [48]. Invasion beyond the epithelial layer is, however, is a rare event.

Efficient colonization of the gastric niche by *H. pylori* is also dependent on how fast it escapes from the lumen of the stomach and reaches the mucus layer, avoiding elimination by gastric peristalsis [42]. Its helical shape and the two to six polar, sheathed flagella provide swimming abilities. According to a longstanding theory [43], the helical shape allows *H. pylori* to have a corkscrew motion which, although not being essential for motility, enhances its ability to swim through the viscous mucus layer. The machinery that gives rise to the spiral shape of this bacterium remains largely unknown, but seems dependent on the coordinated action of multiple proteins in a shape-generating pathway that leads to the relaxation of the peptido‐ glycan crosslinking [44]. Flagella are, however, essential for *H. pylori* motility. Indeed, aflagel‐ lated strains (obtained by elimination of both *flaA* and *flaB*, genes encoding the two major components of flagellar filament, flagellins A and B) [45], as well as strains presenting nonfunctional flagella (in knockout *motB* models lacking the gene that encodes the MotB flagellar motor protein), are non-motile [42]. Such mutants are able to establish only transient coloni‐ zation in animal models [42,46]. Moreover, lower-motility strains are long known to induce *in vitro* reduced inflammation levels, when compared to higher motility strains [47]. Once in the mucus layer of the stomach, *H. pylori* resides here thereafter, either freely swimming [43] or attached to host's extracellular mucins [41], getting closer to the host's gastric epithelial surface whenever necessary. Occasionally *H. pylori* also can be internalized, entering the gastric

**1.2. Molecular mechanisms of** *H. pylori* **colonization and infection**

host's therapeutic or vaccine targets.

*1.2.1. Acid resistance and motility*

Accordingly, *in Europe and North America, the epidemiology of H. pylori infection in children has changed in recent decades. Nowadays, low incidence rates are found in the northern and western European countries, resulting in prevalence far below 10% in children and adolescents. In contrast, the infection is still common in certain geographic areas such as southern or eastern Europe, Mexico, and certain immigrant populations from South America, Africa, most Asian countries, and first-nation (aboriginal) people in North America* [25-27]. In Portugal with the worst scenario of Europe, the prevalence of H. pylori infection is closer to the situation observed in developing countries, reaching 80% among the adult population in their early nineties, and, more recently, varying from approximately 20% in young children (less than 5 years old) to 50% in children 10 to 15 years old [28,29].

The absence of effective vaccines [30] and of efficient alternatives to antibiotics [31-34] renders difficult the worldwide prevention of *H. pylori* infection-associated diseases through massive eradication of the bacterium. The current antibiotic therapy against *H. pylori* infection fails in about 20% of the patients; depending on the therapeutic schema and strain resistance pattern, the failure rate may reach 70%. Antibiotic resistance, mainly to clarithromycin, is the major factor affecting the efficacy of standard triple therapy of *H. pylori* infection (co-administration of two antibiotics and a proton pump inhibitor or ranitidine bismuth for seven to ten days). In fact, the resistance rates to this and other second line antibiotics, such as the fluoroquinolones, are increasing in many geographical areas [34-36].

Several studies reveal a similar or higher resistance rate to clarithromycin among paediatric isolates as compared to those obtained from adults, especially in southern European countries, reflecting the recognized overuse of macrolides in children in these countries [31,34,37,38]. As an example, Portugal displays one of the highest rates of *H. pylori* primary resistance to clarithromycin in Europe, similarly high in children as among adults (≈33%) [34]. Moreover, resistance to second line antibiotics has rapidly increased over the last decade and is a matter of concern [31-34]. This places the research on disease-specific bacterial biomarkers and their associated molecular mechanisms as a top priority to define disease-risk and to target *H. pylori* eradication in high-risk individuals. Ultimately, it may provide novel bacterial and/or host's therapeutic or vaccine targets.

#### **1.2. Molecular mechanisms of** *H. pylori* **colonization and infection**

#### *1.2.1. Acid resistance and motility*

**1.1. Prevalence of infection**

70 Dyspepsia - Advances in Understanding and Management

*hygienic conditions of the populations.*

are increasing in many geographical areas [34-36].

years old [28,29].

*H. pylori* is one of the most common gastrointestinal bacterial infections among humans, affecting more than 50% of the world's population [1,20]. *Infection is usually acquired during the first years of life in both developing and industrialized countries, with* intra-familial spread playing a central role in transmission of the infection [21,22]. The prevalence of *H. pylori* is markedly variable between developing and developed countries, and even among individuals living in the same country, varying according to ethnicity, place of birth and socioeconomic factors. Besides geographic area, age is also significantly and independently associated with an increase in *H. pylori* prevalence, a phenomenon known as birth cohort effect, which is a progressive reduction of the infection rate in successive birth cohorts, due to the improvements in general living conditions (reviewed in [23]). In less developed countries the infection rate reaches almost 50% in very young children and more than 90% in adults, whereas in indus‐ trialized countries *H. pylori* infects 20-50% of adults and less than 10% of children, and has been declining over time [23,24]. Indeed, the prevalence of *H. pylori* infection is *showing a decreased trend* worldwide that *is directly associated with an improvement in the socioeconomic status and*

Accordingly, *in Europe and North America, the epidemiology of H. pylori infection in children has changed in recent decades. Nowadays, low incidence rates are found in the northern and western European countries, resulting in prevalence far below 10% in children and adolescents. In contrast, the infection is still common in certain geographic areas such as southern or eastern Europe, Mexico, and certain immigrant populations from South America, Africa, most Asian countries, and first-nation (aboriginal) people in North America* [25-27]. In Portugal with the worst scenario of Europe, the prevalence of H. pylori infection is closer to the situation observed in developing countries, reaching 80% among the adult population in their early nineties, and, more recently, varying from approximately 20% in young children (less than 5 years old) to 50% in children 10 to 15

The absence of effective vaccines [30] and of efficient alternatives to antibiotics [31-34] renders difficult the worldwide prevention of *H. pylori* infection-associated diseases through massive eradication of the bacterium. The current antibiotic therapy against *H. pylori* infection fails in about 20% of the patients; depending on the therapeutic schema and strain resistance pattern, the failure rate may reach 70%. Antibiotic resistance, mainly to clarithromycin, is the major factor affecting the efficacy of standard triple therapy of *H. pylori* infection (co-administration of two antibiotics and a proton pump inhibitor or ranitidine bismuth for seven to ten days). In fact, the resistance rates to this and other second line antibiotics, such as the fluoroquinolones,

Several studies reveal a similar or higher resistance rate to clarithromycin among paediatric isolates as compared to those obtained from adults, especially in southern European countries, reflecting the recognized overuse of macrolides in children in these countries [31,34,37,38]. As an example, Portugal displays one of the highest rates of *H. pylori* primary resistance to clarithromycin in Europe, similarly high in children as among adults (≈33%) [34]. Moreover, resistance to second line antibiotics has rapidly increased over the last decade and is a matter of concern [31-34]. This places the research on disease-specific bacterial biomarkers and their In a fully adapted manner, during colonization and persistence, this neutralophile bacterium resists gastric acidity mainly through its urease activity. Its urease enzyme, a Ni2+-containing dodecameric protein of approximately 1100 kDa, composed of 12 small subunits, UreA (27 kDa), and 12 large subunits, UreB (62 kDa), catalyzes the hydrolysis of urea into ammonia and carbon dioxide, buffering both the bacteria cytoplasm and periplasm [39]. Accounting for 5-10% of the total protein content, urease is one of the most abundant proteins in the *H. pylori* proteome [16,30]. Probably due to the toxicity of ammonia, urease activity is known to be dependent on low pH and/or Ni2+ concentration conditions [39,40], being essential for bacteria survival only under acidic conditions. In the early stages of colonization, *H. pylori* seeks parts of the stomach with higher pH, such as the antrum (the distal part of the stomach). Indeed, this bacterium uses the pH gradient as chemotactic signal to achieve regions of neutral pH, since its spatial orientation is lost in the absence of the mucus pH gradient [41]. Thus, the acid-producing parietal cells may protect the corpus region from initial invasion.

Efficient colonization of the gastric niche by *H. pylori* is also dependent on how fast it escapes from the lumen of the stomach and reaches the mucus layer, avoiding elimination by gastric peristalsis [42]. Its helical shape and the two to six polar, sheathed flagella provide swimming abilities. According to a longstanding theory [43], the helical shape allows *H. pylori* to have a corkscrew motion which, although not being essential for motility, enhances its ability to swim through the viscous mucus layer. The machinery that gives rise to the spiral shape of this bacterium remains largely unknown, but seems dependent on the coordinated action of multiple proteins in a shape-generating pathway that leads to the relaxation of the peptido‐ glycan crosslinking [44]. Flagella are, however, essential for *H. pylori* motility. Indeed, aflagel‐ lated strains (obtained by elimination of both *flaA* and *flaB*, genes encoding the two major components of flagellar filament, flagellins A and B) [45], as well as strains presenting nonfunctional flagella (in knockout *motB* models lacking the gene that encodes the MotB flagellar motor protein), are non-motile [42]. Such mutants are able to establish only transient coloni‐ zation in animal models [42,46]. Moreover, lower-motility strains are long known to induce *in vitro* reduced inflammation levels, when compared to higher motility strains [47]. Once in the mucus layer of the stomach, *H. pylori* resides here thereafter, either freely swimming [43] or attached to host's extracellular mucins [41], getting closer to the host's gastric epithelial surface whenever necessary. Occasionally *H. pylori* also can be internalized, entering the gastric epithelial cells [48]. Invasion beyond the epithelial layer is, however, is a rare event.

#### *1.2.2. Bacterial Adherence*

In the human stomach, the vast majority of *H. pylori* cells exist in their motile form within the mucus layer lining; only a small portion (≈30%) are adherent to the surfaces of epithelial cells [41]. Nevertheless, adherence to the gastric epithelium is important for the ability of *H. pylori* to cause disease because this intimate attachment facilitates: 1) persistence, by preventing the bacteria from being eliminated from the stomach through mucus turnover and gastric peristalsis, and also by enabling the bacteria to replicate; 2) evasion from the human immune system; 3) efficient delivery of the bacterial toxic proteins; and 4) acquiring nutrients released from the damaged host cells.

neutrophil infiltration and, ultimately, with peptic ulceration and gastric cancer [58,59]. Supporting the later association, the inactivation of *oipA* results in a reduced nuclear translo‐ cation of β-catenin, a known factor involved in the transcriptional up-regulation of genes

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73

After adherence, *H. pylori* delivers its virulence factors into the cytoplasm of the host's cells by using a type IV secretion system (T4SS) and/or outer membrane vesicles. The genes encoding the components of the T4SS, which is a syringe-like pilus protruding from the bacterial surface used to inject virulence factors in host target cells' cytoplasm, are located in the *cag* pathoge‐ nicity island (PAI) [60]. This is an approximately 40 kpb chromosomal insertion that is thought to have been incorporated into the *H. pylori* genome by horizontal transfer from an unknown source [61]. As a result, strains are heterogenic regarding the presence of this chromosomal region, varying between those that contain the intact *cag* PAI to those that completely lack it. For those lacking an intact T4SS, the delivery of their virulence factors is totally dependent on the secretion of outer membrane vesicles with a still poorly known content; these are endocy‐

Encoded by *cytotoxin associated gene A*, one of the 32 genes of the *cag* PAI region, CagA is perhaps the most extensively studied translocated protein, the only known effector protein injected by the T4SS. Once injected into cytoplasm of target cells, CagA interferes with several host cell signalling cascades, ultimately inducing abnormal proliferation, cytoskeleton rearrangements and inflammation through the release of cytokines, such as interleukin-1β (IL-1β), IL-8 and tumour necrosis factor-α (TNF-α) (reviewed in [63]). There are two types of clinical isolates regarding CagA: those producing this protein (*cagA*-positive *H. pylori* strains), and the CagA-nonproducing strains (*cagA*-negative *H. pylori* strains). The *cagA*-positive strains are considerably more virulent [60]. In Western countries, individuals carriers of *cagA*-positive strains are thus at higher risk of peptic ulcer disease and/or gastric cancer [64,65], leading to the classification of CagA as a bacterium-derived oncogenic protein [66]. In a not fully undisclosed manner, the virulence of the *cagA*-positive strains is associated with the number and the type of the phosphorylation motifs of the C-terminal variable region of the protein. Of these motifs, defined as EPIYA (Glu-Pro-Ile-Tyr-Ala) A, B, C and D according to different flanking amino acids, CagA protein nearly always possesses EIPYA-A and B segments, followed by none, one, two or three C segments in Western-strains or a D segment in strains of East Asian countries. The East Asian-type of CagA (ABD) is known to be more carcinogenic than the Western-type; within the latter, the variants possessing multiple EPIYA-C motifs (ABCC or ABCCC) are more virulent compared with those with a single segment (ABC) (reviewed in [63]). Moreover, the association of CagA expression levels with polymorphisms in the *cagA* promoter region may further contribute to differences in virulence among *cagA*positive strains and different disease-associated risks [67]. The virulence of the strain must also be dependent on additional bacterial factors, since in East Asia most strains are *cagA*-positive

implicated in carcinogenesis [59].

*1.2.3. Delivery and virulence factors*

irrespective of the patient disease.

tosed by the host epithelial cells (reviewed in [62]).

*H. pylori* expresses a multitude of different adhesins. Best characterized is the blood group antigen-binding adhesin (BabA), a ligand of ABO (of the blood group system) Lewis b (Leb ) antigens [49]. Sequence analyses reveals the existence of two allelic variants of *babA*, the *babA1* and *babA2* alleles, which are identical except for a 10 base pair insertion that results in a translational initiation codon present in *babA2* but absent in *babA1*, and of a highly homologous gene, *babB*. Of these, only *babA2* allele encodes a functional Leb adhesin [49]. BabA is not likely to be essential for the colonization; BabA-expressing strains are no different in this step compared to BabA-non-expressing strains [50]. BabA, being an adhesin, however likely plays an important role in the induction of host inflammatory response. Indeed, *babA2* allele is clinically important, namely in a *vacA*/*cagA*-positive genetic background (two additional important virulence factors discussed in section 1.2.3. of this chapter), which is associated with peptic ulcer disease and gastric cancer [51]. BabA-expressing strains induces change in the glycosylation pattern of the gastric mucosa of humans and animal models [50].

The second best characterized *H. pylori* adhesin is the sialic acid binding adhesin (SabA) which mediates attachment to the inflammation-associated (sialylated Lewisx and Lewisa ) antigens [52]. In fact, gastric tissue inflammation and malignant transformation promote synthesis of sialylated glycoconjugates, which are rare in healthy human stomachs [52, 53]. Accordingly, high levels of sialylated glycoconjugates are found in *H. pylori* infected persons; these decrease after eradication of the infection and resolution of the gastritis [54]. *H. pylori* can agglutinate erythrocytes and neutrophils *in vitro*. The SabA adhesin is the hemagglutinin of *H. pylori* and allows bacterial adherence to blood cells; this may result in systemic dissemination of the pathogen [55]. Moreover, the binding of SabA to sialic acid carries neutrophil receptors, essential for the nonopsonic activation of human neutrophils [56]. Neutrophils play a major role in the epithelium injury, since these cells have direct toxic effects on the epithelial cells, through the induction of an oxidative burst, with the release of reactive oxygen and nitrogen species. Thus, the neutrophil activating capacity of SabA makes this protein an additional virulence factor that is important in the pathogenesis of *H. pylori* infection.

The outer membrane inflammatory protein (OipA), a member of the Hop family of proteins, is another *H. pylori* membrane protein with an active role in bacterial adherence, for which no host receptors are known. Its encoding gene (*oipA*) is present in all *H. pylori* strains but it is only expressed in those presenting the *oipA* "on" (*i.e.*, functional) genotype. This is regulated by slipped-strand mispairing, depending on the number of CT repeats in the 5' region of the gene [57]. OipA expression by *H. pylori* is associated with high bacterial densities, severe neutrophil infiltration and, ultimately, with peptic ulceration and gastric cancer [58,59]. Supporting the later association, the inactivation of *oipA* results in a reduced nuclear translo‐ cation of β-catenin, a known factor involved in the transcriptional up-regulation of genes implicated in carcinogenesis [59].

#### *1.2.3. Delivery and virulence factors*

*1.2.2. Bacterial Adherence*

72 Dyspepsia - Advances in Understanding and Management

from the damaged host cells.

In the human stomach, the vast majority of *H. pylori* cells exist in their motile form within the mucus layer lining; only a small portion (≈30%) are adherent to the surfaces of epithelial cells [41]. Nevertheless, adherence to the gastric epithelium is important for the ability of *H. pylori* to cause disease because this intimate attachment facilitates: 1) persistence, by preventing the bacteria from being eliminated from the stomach through mucus turnover and gastric peristalsis, and also by enabling the bacteria to replicate; 2) evasion from the human immune system; 3) efficient delivery of the bacterial toxic proteins; and 4) acquiring nutrients released

*H. pylori* expresses a multitude of different adhesins. Best characterized is the blood group antigen-binding adhesin (BabA), a ligand of ABO (of the blood group system) Lewis b (Leb

antigens [49]. Sequence analyses reveals the existence of two allelic variants of *babA*, the *babA1* and *babA2* alleles, which are identical except for a 10 base pair insertion that results in a translational initiation codon present in *babA2* but absent in *babA1*, and of a highly homologous

to be essential for the colonization; BabA-expressing strains are no different in this step compared to BabA-non-expressing strains [50]. BabA, being an adhesin, however likely plays an important role in the induction of host inflammatory response. Indeed, *babA2* allele is clinically important, namely in a *vacA*/*cagA*-positive genetic background (two additional important virulence factors discussed in section 1.2.3. of this chapter), which is associated with peptic ulcer disease and gastric cancer [51]. BabA-expressing strains induces change in the

The second best characterized *H. pylori* adhesin is the sialic acid binding adhesin (SabA) which

[52]. In fact, gastric tissue inflammation and malignant transformation promote synthesis of sialylated glycoconjugates, which are rare in healthy human stomachs [52, 53]. Accordingly, high levels of sialylated glycoconjugates are found in *H. pylori* infected persons; these decrease after eradication of the infection and resolution of the gastritis [54]. *H. pylori* can agglutinate erythrocytes and neutrophils *in vitro*. The SabA adhesin is the hemagglutinin of *H. pylori* and allows bacterial adherence to blood cells; this may result in systemic dissemination of the pathogen [55]. Moreover, the binding of SabA to sialic acid carries neutrophil receptors, essential for the nonopsonic activation of human neutrophils [56]. Neutrophils play a major role in the epithelium injury, since these cells have direct toxic effects on the epithelial cells, through the induction of an oxidative burst, with the release of reactive oxygen and nitrogen species. Thus, the neutrophil activating capacity of SabA makes this protein an additional

The outer membrane inflammatory protein (OipA), a member of the Hop family of proteins, is another *H. pylori* membrane protein with an active role in bacterial adherence, for which no host receptors are known. Its encoding gene (*oipA*) is present in all *H. pylori* strains but it is only expressed in those presenting the *oipA* "on" (*i.e.*, functional) genotype. This is regulated by slipped-strand mispairing, depending on the number of CT repeats in the 5' region of the gene [57]. OipA expression by *H. pylori* is associated with high bacterial densities, severe

glycosylation pattern of the gastric mucosa of humans and animal models [50].

mediates attachment to the inflammation-associated (sialylated Lewisx

virulence factor that is important in the pathogenesis of *H. pylori* infection.

gene, *babB*. Of these, only *babA2* allele encodes a functional Leb

)

adhesin [49]. BabA is not likely

and Lewisa

) antigens

After adherence, *H. pylori* delivers its virulence factors into the cytoplasm of the host's cells by using a type IV secretion system (T4SS) and/or outer membrane vesicles. The genes encoding the components of the T4SS, which is a syringe-like pilus protruding from the bacterial surface used to inject virulence factors in host target cells' cytoplasm, are located in the *cag* pathoge‐ nicity island (PAI) [60]. This is an approximately 40 kpb chromosomal insertion that is thought to have been incorporated into the *H. pylori* genome by horizontal transfer from an unknown source [61]. As a result, strains are heterogenic regarding the presence of this chromosomal region, varying between those that contain the intact *cag* PAI to those that completely lack it. For those lacking an intact T4SS, the delivery of their virulence factors is totally dependent on the secretion of outer membrane vesicles with a still poorly known content; these are endocy‐ tosed by the host epithelial cells (reviewed in [62]).

Encoded by *cytotoxin associated gene A*, one of the 32 genes of the *cag* PAI region, CagA is perhaps the most extensively studied translocated protein, the only known effector protein injected by the T4SS. Once injected into cytoplasm of target cells, CagA interferes with several host cell signalling cascades, ultimately inducing abnormal proliferation, cytoskeleton rearrangements and inflammation through the release of cytokines, such as interleukin-1β (IL-1β), IL-8 and tumour necrosis factor-α (TNF-α) (reviewed in [63]). There are two types of clinical isolates regarding CagA: those producing this protein (*cagA*-positive *H. pylori* strains), and the CagA-nonproducing strains (*cagA*-negative *H. pylori* strains). The *cagA*-positive strains are considerably more virulent [60]. In Western countries, individuals carriers of *cagA*-positive strains are thus at higher risk of peptic ulcer disease and/or gastric cancer [64,65], leading to the classification of CagA as a bacterium-derived oncogenic protein [66]. In a not fully undisclosed manner, the virulence of the *cagA*-positive strains is associated with the number and the type of the phosphorylation motifs of the C-terminal variable region of the protein. Of these motifs, defined as EPIYA (Glu-Pro-Ile-Tyr-Ala) A, B, C and D according to different flanking amino acids, CagA protein nearly always possesses EIPYA-A and B segments, followed by none, one, two or three C segments in Western-strains or a D segment in strains of East Asian countries. The East Asian-type of CagA (ABD) is known to be more carcinogenic than the Western-type; within the latter, the variants possessing multiple EPIYA-C motifs (ABCC or ABCCC) are more virulent compared with those with a single segment (ABC) (reviewed in [63]). Moreover, the association of CagA expression levels with polymorphisms in the *cagA* promoter region may further contribute to differences in virulence among *cagA*positive strains and different disease-associated risks [67]. The virulence of the strain must also be dependent on additional bacterial factors, since in East Asia most strains are *cagA*-positive irrespective of the patient disease.

The vacuolating toxin (VacA), another important virulence factor (reviewed in [68]), is synthesized as a pro-toxin of ≈140 kDa, which contains a *N*-terminal signal sequence, a passenger domain and *C*-terminal autotransporter domain. The passenger toxin domain (≈88 kDa) is cleaved and processed at some point during its secretion into the extracellular milieu through the autotransporter that functions as a type V secretion system. This 88 kDa toxin is further proteolytically cleaved, creating a *N*-terminal fragment of ≈33 kDa (p33) and a *C*terminal fragment of ≈55 kDa (p55) that remain non-covalently associated. Required for the cytotoxic activity, the p33 subunit is postulated to be involved in the formation of anionic membrane channels, while p55 subunit seems to mediate VacA binding to host cells (reviewed in [68]). These functions are, however, highly dependent of the tridimensional structure of both subunits [69,70]. Once secreted by the bacterial cells, VacA triggers various responses in the host, resulting in the cellular vacuolation, pore formation in the cell membrane, disruption of endosomal ⁄ lysosomal structure and function, apoptosis by toxin trafficking to mitochon‐ dria, and immunomodulation [71-73]. Virtually all *H. pylori* strains have a functional VacA. However, the amount of toxin produced is related to the allelic variation of the encoding gene, especially in its signal and middle regions (reviewed in [74]). Therefore, an association between particular *vacA* allele types and peptic ulcer disease has been reported worldwide..

used by *H. pylori* is the expression of proteins at its surface, which specifically bind to hostsecreted proteins, *e.g.,* bacterial plasminogen-binding proteins (PgbA and PgbB). This allows the bacterium to be coated with host proteins [78]. *H. pylori* also avoids immune recognition through the *in vitro* and *in vivo* impairment of the expression of host's specific heat shock

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75

Allelic diversification of its virulence factors encoding genes allows *H. pylori* to occupy different microenvironments within the human stomach and to adapt to the varying conditions in the niche over time. This is even more efficient, considering that the expression of different variants of those genes may switch through mechanisms of phase variation. Indeed, several *in vitro* studies have demonstrated that *H. pylori* Lewis-like antigens can undergo phase variation (reviewed in [76]). Moreover, in animal models, persistent infection leads to the loss of expression of *babA*. This occurs either by phase variation switching between an "on" and an "off" status in a manner similar to that described for *oipA* (see section 1.2.2 of this chapter),

The existence of a small subpopulation of *H. pylori* within gastric epithelial cells (as briefly discussed in section 1.2.1 of this chapter) may represent a sanctuary site that protects bacteria

Although rarely associated with severe forms of organic dyspepsia (namely peptic ulcer disease) in the paediatric age group, *H. pylori* is clearly linked with acute gastric inflammation in childhood and occurs frequently in children with dyspepsia [81]. This important association gains relevance when considering that: a) gastric colonization by *H. pylori* occurring in childhood and the consequent inflammation continues for life if left untreated; and b) *this* lifelong persistence of inflammation after decades of infection is the main etiology for peptic ulceration and/or cancer in adulthood. Moreover, some studies suggest a possible impact of *H. pylori*-associated dyspepsia on anthropometry, as children with dyspepsia and *H. pylori* infection are shorter and lighter than children with similar symptoms but no infection [82,83]. Evidence for the importance of *H. pylori* infection as a factor for dyspepsia in childhood comes from *H. pylori* eradication resulting in a significant long-term improvement of dyspeptic symptoms [84]. The symptoms of *H. pylori*-associated paediatric dyspepsia however do not differ from those of non-infected dyspeptic children [85], raising questions about which approach should be adopted in children with dyspepsia, in terms of *H. pylori* testing. According to current guidelines for the management of *H. pylori* infection at pediatric age [86,87], the primary goal of diagnostic interventions should be to determine the cause of the presenting gastrointestinal symptoms ("scope and treat" strategy) and not just the presence of *H. pylori* infection ("test and treat" strategy). Indeed, recurrent abdominal pain is not an indication for a "test and treat" strategy concerning *H. pylori* infection in children, as evidence regarding the association with *H. pylori* infection has been so far inconclusive (even in the presence of peptic ulcer). Indeed, several studies using different noninvasive tests for *H pylori* infection compared the prevalence of positive results in children with recurrent abdominal pain and controls and found no significant difference in infection rates between cases and controls [88,89]. On the

**1.3. Peptic Ulcer — Related organic dyspepsia in paediatrics, a rare event**

proteins, thus, inactivating both the innate and adaptive immune response [79].

or by nonreciprocal gene conversion of *babA* to *babB* [80].

against immune clearance [48].

The ancient association between *H. pylori* and the modern humans [1,20] has determined the abnormal high diversity in both their genetic background and the virulence observed among strains. This generates complex scenario that creates difficulty in understanding the contribu‐ tion of each individual factor. Nevertheless, *H. pylori* strains presenting the association of these two virulence factors, *i.e.*, *cagA*-positive and *vacA*-toxigenic alleles, are considered to be more virulent and thus more associated with severe organic dyspepsia inducers of a high production of proinflammatory cytokines in the gastric mucosa and thus more severe non-ulcer dyspepsia. Even so, these virulence factors do not appear to determine the overall pattern of gastroduodenal disease and a complex interplay between host bacterial factors and environment seems to be involved in the development of gastric pathology [75].

#### *1.2.4. Evasion*

Upon colonization, *H. pylori*-infected patients experience a strong and complex immune response in the gastric mucosa, both at the humoral and cellular levels; despite this response, nevertheless the infection fails to clear. Therefore, in the absence of effective treatment, infection becomes chronic, persists, and contributes to the immunopathology. The persistence of infection throughout the life of its host is guaranteed by a set of molecular mechanisms used by *H. pylori* to constantly evade the host immune response (reviewed in [76]). Bacterial mimicry and genetic diversity play a central role in such successful strategies.

Mimicking the cell surfaces of the host, the lipopolysaccharide of the *H. pylori* cell wall is relatively anergic compared to other gram-negative bacteria. In fact, the variable part of the *O*-antigen chain of *H. pylori* lipopolysaccharide is composed of host-related Lewis antigens, making it unrecognizable to the host immune system [77]. Therefore, this pathogen not only binds to human Lewis antigens through BabA and SabA, but it also expresses Lewis-like antigens facilitating the escape from the host immune system. Another ingenious camouflage used by *H. pylori* is the expression of proteins at its surface, which specifically bind to hostsecreted proteins, *e.g.,* bacterial plasminogen-binding proteins (PgbA and PgbB). This allows the bacterium to be coated with host proteins [78]. *H. pylori* also avoids immune recognition through the *in vitro* and *in vivo* impairment of the expression of host's specific heat shock proteins, thus, inactivating both the innate and adaptive immune response [79].

The vacuolating toxin (VacA), another important virulence factor (reviewed in [68]), is synthesized as a pro-toxin of ≈140 kDa, which contains a *N*-terminal signal sequence, a passenger domain and *C*-terminal autotransporter domain. The passenger toxin domain (≈88 kDa) is cleaved and processed at some point during its secretion into the extracellular milieu through the autotransporter that functions as a type V secretion system. This 88 kDa toxin is further proteolytically cleaved, creating a *N*-terminal fragment of ≈33 kDa (p33) and a *C*terminal fragment of ≈55 kDa (p55) that remain non-covalently associated. Required for the cytotoxic activity, the p33 subunit is postulated to be involved in the formation of anionic membrane channels, while p55 subunit seems to mediate VacA binding to host cells (reviewed in [68]). These functions are, however, highly dependent of the tridimensional structure of both subunits [69,70]. Once secreted by the bacterial cells, VacA triggers various responses in the host, resulting in the cellular vacuolation, pore formation in the cell membrane, disruption of endosomal ⁄ lysosomal structure and function, apoptosis by toxin trafficking to mitochon‐ dria, and immunomodulation [71-73]. Virtually all *H. pylori* strains have a functional VacA. However, the amount of toxin produced is related to the allelic variation of the encoding gene, especially in its signal and middle regions (reviewed in [74]). Therefore, an association between

74 Dyspepsia - Advances in Understanding and Management

particular *vacA* allele types and peptic ulcer disease has been reported worldwide..

seems to be involved in the development of gastric pathology [75].

and genetic diversity play a central role in such successful strategies.

*1.2.4. Evasion*

The ancient association between *H. pylori* and the modern humans [1,20] has determined the abnormal high diversity in both their genetic background and the virulence observed among strains. This generates complex scenario that creates difficulty in understanding the contribu‐ tion of each individual factor. Nevertheless, *H. pylori* strains presenting the association of these two virulence factors, *i.e.*, *cagA*-positive and *vacA*-toxigenic alleles, are considered to be more virulent and thus more associated with severe organic dyspepsia inducers of a high production of proinflammatory cytokines in the gastric mucosa and thus more severe non-ulcer dyspepsia. Even so, these virulence factors do not appear to determine the overall pattern of gastroduodenal disease and a complex interplay between host bacterial factors and environment

Upon colonization, *H. pylori*-infected patients experience a strong and complex immune response in the gastric mucosa, both at the humoral and cellular levels; despite this response, nevertheless the infection fails to clear. Therefore, in the absence of effective treatment, infection becomes chronic, persists, and contributes to the immunopathology. The persistence of infection throughout the life of its host is guaranteed by a set of molecular mechanisms used by *H. pylori* to constantly evade the host immune response (reviewed in [76]). Bacterial mimicry

Mimicking the cell surfaces of the host, the lipopolysaccharide of the *H. pylori* cell wall is relatively anergic compared to other gram-negative bacteria. In fact, the variable part of the *O*-antigen chain of *H. pylori* lipopolysaccharide is composed of host-related Lewis antigens, making it unrecognizable to the host immune system [77]. Therefore, this pathogen not only binds to human Lewis antigens through BabA and SabA, but it also expresses Lewis-like antigens facilitating the escape from the host immune system. Another ingenious camouflage

Allelic diversification of its virulence factors encoding genes allows *H. pylori* to occupy different microenvironments within the human stomach and to adapt to the varying conditions in the niche over time. This is even more efficient, considering that the expression of different variants of those genes may switch through mechanisms of phase variation. Indeed, several *in vitro* studies have demonstrated that *H. pylori* Lewis-like antigens can undergo phase variation (reviewed in [76]). Moreover, in animal models, persistent infection leads to the loss of expression of *babA*. This occurs either by phase variation switching between an "on" and an "off" status in a manner similar to that described for *oipA* (see section 1.2.2 of this chapter), or by nonreciprocal gene conversion of *babA* to *babB* [80].

The existence of a small subpopulation of *H. pylori* within gastric epithelial cells (as briefly discussed in section 1.2.1 of this chapter) may represent a sanctuary site that protects bacteria against immune clearance [48].

#### **1.3. Peptic Ulcer — Related organic dyspepsia in paediatrics, a rare event**

Although rarely associated with severe forms of organic dyspepsia (namely peptic ulcer disease) in the paediatric age group, *H. pylori* is clearly linked with acute gastric inflammation in childhood and occurs frequently in children with dyspepsia [81]. This important association gains relevance when considering that: a) gastric colonization by *H. pylori* occurring in childhood and the consequent inflammation continues for life if left untreated; and b) *this* lifelong persistence of inflammation after decades of infection is the main etiology for peptic ulceration and/or cancer in adulthood. Moreover, some studies suggest a possible impact of *H. pylori*-associated dyspepsia on anthropometry, as children with dyspepsia and *H. pylori* infection are shorter and lighter than children with similar symptoms but no infection [82,83].

Evidence for the importance of *H. pylori* infection as a factor for dyspepsia in childhood comes from *H. pylori* eradication resulting in a significant long-term improvement of dyspeptic symptoms [84]. The symptoms of *H. pylori*-associated paediatric dyspepsia however do not differ from those of non-infected dyspeptic children [85], raising questions about which approach should be adopted in children with dyspepsia, in terms of *H. pylori* testing. According to current guidelines for the management of *H. pylori* infection at pediatric age [86,87], the primary goal of diagnostic interventions should be to determine the cause of the presenting gastrointestinal symptoms ("scope and treat" strategy) and not just the presence of *H. pylori* infection ("test and treat" strategy). Indeed, recurrent abdominal pain is not an indication for a "test and treat" strategy concerning *H. pylori* infection in children, as evidence regarding the association with *H. pylori* infection has been so far inconclusive (even in the presence of peptic ulcer). Indeed, several studies using different noninvasive tests for *H pylori* infection compared the prevalence of positive results in children with recurrent abdominal pain and controls and found no significant difference in infection rates between cases and controls [88,89]. On the other hand, pediatric studies are limited by the lack of a clear definition for recurrent abdomi‐ nal pain or by the use of nonspecific criteria for the diagnosis of chronic abdominal pain [90]. Nevertheless, in patients with persistent abdominal pain (after exclusion of other causes, such as lactose intolerance, giardiasis, celiac disease, *inflammatory bowel disease*, among others) and/ or severe upper abdominal symptoms (namely suggesting peptic ulcer disease, such as nocturnal pain), upper endoscopy with biopsy should be performed (diagnostic investigation of choice). Furthermore, testing for *H. pylori* in children/adolescents should be considered if there is a family history of gastric cancer and in children/adolescents with refractory iron deficiency anemia, when no other cause is found. In these settings, when upper endoscopy is performed, the presence of *H. pylori* should be systematically sought through histological examination and, whenever feasible, culture and antibiotic susceptibility testing; treatment should be offered in the presence of *H. pylori* positivity. Population screening for *H. pylori* in asymptomatic children to prevent gastric cancer is not warranted. Although 13C-urea breath testing is a validated noninvasive diagnostic test for *H. pylori* infection in children, a "test and treat" strategy including this tool should not be indiscriminately adopted in clinical practice at this age group, considering the fact that this test merely identifies *H. pylori* presence but not necessarily the causality of symptoms. Noninvasive tests for *H.pylori* include different methods for the detection of bacterial antigens in stool, detection of antibodies (IgG, IgA) against *H. pylori* in serum, urine, and oral samples, and the 13C-UBT. In the paediatric group, both fecal antigens determination and respiratory test are reliable to determine whether *H pylori* has been eradicated or not after antibiotic treatment, while tests based on the detection of antibodies against *H pylori* are considered not reliable for use in the clinical setting, but may be useful in epidemiological studies [91].

*prevalence trends, H. pylori*-induced gastritis causing mucosal ulceration either in the stomach (gastric ulcer) or the proximal duodenum (duodenal ulcer) is a relatively uncommon event in children, compared with adults [4-8]. In fact, during childhood, H. pylori is associated with predominant antral gastritis or with pangastritis [96]. *In children, few studies have yet investigated the actual trend of H. pylori prevalence in peptic ulcer disease* [5-8] and the available data are more difficult to interpret, considering that the rates of peptic ulcer diagnosis depend also on the clinical setting (endoscopy versus outpatient clinic or hospital admissions) [97,98]. For example, in Italy the detection rate of ulcer disease was 7.8% out of an average of 180 paediatric gastrointestinal endoscopies performed each year [99]. Similarly, a retrospective review (from 1998 to 2006) showed that 43 (6.9%) out of 619 Chinese children who underwent upper endoscopy for investigation of upper gastrointestinal symptoms had peptic ulcer [7]; and another retrospective study (from 2003 to 2006) have also reported a high incidence of peptic ulcer (6.8%) in Israeli children submitted to upper endoscopy [100]. In Canada, however, the approximate incidence of peptic ulcer was 1 case per 2,500 hospital admissions [92]. In a recent large European multicenter study, including 1233 symptomatic children with H. pylori infection, peptic ulcer disease was diagnosed in less than 5% of children younger than 12 years of age and in ≈10% of teenagers [8]. Interestingly, other studies indicate a higher association of H. pylori with peptic ulcer in adolescents than in younger children [100,101]. But, the prevalence of H. pylori-positive ulcers in children also differs between countries and this is not completely explained by the prevalence of the infection in the population studied. This is easily demonstrated from data collected from January 2001 to December 2002 on 518 children from the paediatric European register for treatment of H. pylori [5]. At endoscopy, 454 of those patients had H. pylori-associated gastritis and 64 had a peptic ulcer (12.3%). This series also included children from Russia, who had a significantly higher prevalence of peptic ulcer (35%) compared to that of the remainder of European children (6.7%) [6]. In another report, schoolaged children with chronic abdominal complaints living in the rural area of Russia had a high prevalence rate of H. pylori infection (80%) and also of peptic ulcer disease (24%) [102].

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In adults, the prevalence of *H. pylori* infection is higher than 95% in duodenal ulcer cases and around 60% to 80% in gastric ulcer cases [103]. This scenario is similar in children i.e. when *H. pylori*-associated ulcers occur in children, duodenal ulceration is much more frequently identified than gastric ulcers [104]. In fact, pooled analysis of early reports (from 1983 to 1994) has demonstrated that the prevalence of *H. pylori* in children with duodenal ulcer was relatively higher (ranging from 33% to 100%, with a median value of 92%), compared with children with gastric ulcer (ranging from 11% to 75%, with a median value of 25%) [104]. A more recent retrospective study (from 1995 to 2001) from Japan confirmed a very high prevalence of *H. pylori* in antral gastritis and duodenal ulcer (98.5% and 83%, respectively), also identifying *H. pylori* as a risk factor for the development of gastric ulcer although with a lower prevalence of infection (less than 50%) [101]. Finally, in a Chinese study, it was reported that among 43 Chinese children suffering with peptic ulcer disease, 37 had duodenal ulcer, of which 21 were *H. pylori* positive, while only six had gastric ulcer, of which only two were positive for the infection [7]. In summary, *H. pylori* infection is much more associated to

duodenal ulcer than to gastric ulcer, in both children and adults.

Therefore, *H. pylori infection in childhood differs from adults not only in terms of the prevalence of the infection and a higher rate of antibiotic resistance, but also with respect to the complication rate, agespecific problems with diagnostic tests and drugs, and the near-absence of gastric malignancies* [92]. Nevertheless, H. pylori-associated peptic ulcer disease may also occur shortly after infection in childhood [4-8]. This rare event may be due to more virulent strains [9-16], and/or more predisposed subjects [17-19]. The two forms of H. pylori-associated peptic ulcers, i.e., gastric ulcer and duodenal ulcers, are divergent in prevalence and physiopathology, but both cause considerable patients' morbidity entailing high annual costs of treatment [93].

#### *1.3.1. Prevalence of H. pylori-associated gastric and duodenal ulcers in childhood*

*In general, about 10-15% of the H. pylori infected patients suffer from duodenal ulcer disease and 2-5% with gastric ulcer and/or gastric cancer late in the adulthood [3]. Population-based studies in patients with organic dyspepsia suggest that peptic ulcer disease related to H. pylori infection is decreasing in prevalence in Western countries, along with a decrease in the prevalence of infection [94]. The former should be a direct consequence of the second; with improved living standards, cohorts of children became progressively less likely to acquire the organism and thus suffer from H. pylori-associated diseases. Nevertheless, specific populations such as immigrants and rural communities may have a high prevalence of infection and peptic ulcer disease; these individuals should be separately reviewed even in areas where the general prevalence of H. pylori infection has declined below 15% [95]. Despite changing* *prevalence trends, H. pylori*-induced gastritis causing mucosal ulceration either in the stomach (gastric ulcer) or the proximal duodenum (duodenal ulcer) is a relatively uncommon event in children, compared with adults [4-8]. In fact, during childhood, H. pylori is associated with predominant antral gastritis or with pangastritis [96]. *In children, few studies have yet investigated the actual trend of H. pylori prevalence in peptic ulcer disease* [5-8] and the available data are more difficult to interpret, considering that the rates of peptic ulcer diagnosis depend also on the clinical setting (endoscopy versus outpatient clinic or hospital admissions) [97,98]. For example, in Italy the detection rate of ulcer disease was 7.8% out of an average of 180 paediatric gastrointestinal endoscopies performed each year [99]. Similarly, a retrospective review (from 1998 to 2006) showed that 43 (6.9%) out of 619 Chinese children who underwent upper endoscopy for investigation of upper gastrointestinal symptoms had peptic ulcer [7]; and another retrospective study (from 2003 to 2006) have also reported a high incidence of peptic ulcer (6.8%) in Israeli children submitted to upper endoscopy [100]. In Canada, however, the approximate incidence of peptic ulcer was 1 case per 2,500 hospital admissions [92]. In a recent large European multicenter study, including 1233 symptomatic children with H. pylori infection, peptic ulcer disease was diagnosed in less than 5% of children younger than 12 years of age and in ≈10% of teenagers [8]. Interestingly, other studies indicate a higher association of H. pylori with peptic ulcer in adolescents than in younger children [100,101]. But, the prevalence of H. pylori-positive ulcers in children also differs between countries and this is not completely explained by the prevalence of the infection in the population studied. This is easily demonstrated from data collected from January 2001 to December 2002 on 518 children from the paediatric European register for treatment of H. pylori [5]. At endoscopy, 454 of those patients had H. pylori-associated gastritis and 64 had a peptic ulcer (12.3%). This series also included children from Russia, who had a significantly higher prevalence of peptic ulcer (35%) compared to that of the remainder of European children (6.7%) [6]. In another report, schoolaged children with chronic abdominal complaints living in the rural area of Russia had a high prevalence rate of H. pylori infection (80%) and also of peptic ulcer disease (24%) [102].

other hand, pediatric studies are limited by the lack of a clear definition for recurrent abdomi‐ nal pain or by the use of nonspecific criteria for the diagnosis of chronic abdominal pain [90]. Nevertheless, in patients with persistent abdominal pain (after exclusion of other causes, such as lactose intolerance, giardiasis, celiac disease, *inflammatory bowel disease*, among others) and/ or severe upper abdominal symptoms (namely suggesting peptic ulcer disease, such as nocturnal pain), upper endoscopy with biopsy should be performed (diagnostic investigation of choice). Furthermore, testing for *H. pylori* in children/adolescents should be considered if there is a family history of gastric cancer and in children/adolescents with refractory iron deficiency anemia, when no other cause is found. In these settings, when upper endoscopy is performed, the presence of *H. pylori* should be systematically sought through histological examination and, whenever feasible, culture and antibiotic susceptibility testing; treatment should be offered in the presence of *H. pylori* positivity. Population screening for *H. pylori* in

asymptomatic children to prevent gastric cancer is not warranted. Although 13

*pylori* in serum, urine, and oral samples, and the 13

76 Dyspepsia - Advances in Understanding and Management

epidemiological studies [91].

testing is a validated noninvasive diagnostic test for *H. pylori* infection in children, a "test and treat" strategy including this tool should not be indiscriminately adopted in clinical practice at this age group, considering the fact that this test merely identifies *H. pylori* presence but not necessarily the causality of symptoms. Noninvasive tests for *H.pylori* include different methods for the detection of bacterial antigens in stool, detection of antibodies (IgG, IgA) against *H.*

antigens determination and respiratory test are reliable to determine whether *H pylori* has been eradicated or not after antibiotic treatment, while tests based on the detection of antibodies against *H pylori* are considered not reliable for use in the clinical setting, but may be useful in

Therefore, *H. pylori infection in childhood differs from adults not only in terms of the prevalence of the infection and a higher rate of antibiotic resistance, but also with respect to the complication rate, agespecific problems with diagnostic tests and drugs, and the near-absence of gastric malignancies* [92]. Nevertheless, H. pylori-associated peptic ulcer disease may also occur shortly after infection in childhood [4-8]. This rare event may be due to more virulent strains [9-16], and/or more predisposed subjects [17-19]. The two forms of H. pylori-associated peptic ulcers, i.e., gastric ulcer and duodenal ulcers, are divergent in prevalence and physiopathology, but both cause

*In general, about 10-15% of the H. pylori infected patients suffer from duodenal ulcer disease and 2-5% with gastric ulcer and/or gastric cancer late in the adulthood [3]. Population-based studies in patients with organic dyspepsia suggest that peptic ulcer disease related to H. pylori infection is decreasing in prevalence in Western countries, along with a decrease in the prevalence of infection [94]. The former should be a direct consequence of the second; with improved living standards, cohorts of children became progressively less likely to acquire the organism and thus suffer from H. pylori-associated diseases. Nevertheless, specific populations such as immigrants and rural communities may have a high prevalence of infection and peptic ulcer disease; these individuals should be separately reviewed even in areas where the general prevalence of H. pylori infection has declined below 15% [95]. Despite changing*

considerable patients' morbidity entailing high annual costs of treatment [93].

*1.3.1. Prevalence of H. pylori-associated gastric and duodenal ulcers in childhood*

C-urea breath

C-UBT. In the paediatric group, both fecal

In adults, the prevalence of *H. pylori* infection is higher than 95% in duodenal ulcer cases and around 60% to 80% in gastric ulcer cases [103]. This scenario is similar in children i.e. when *H. pylori*-associated ulcers occur in children, duodenal ulceration is much more frequently identified than gastric ulcers [104]. In fact, pooled analysis of early reports (from 1983 to 1994) has demonstrated that the prevalence of *H. pylori* in children with duodenal ulcer was relatively higher (ranging from 33% to 100%, with a median value of 92%), compared with children with gastric ulcer (ranging from 11% to 75%, with a median value of 25%) [104]. A more recent retrospective study (from 1995 to 2001) from Japan confirmed a very high prevalence of *H. pylori* in antral gastritis and duodenal ulcer (98.5% and 83%, respectively), also identifying *H. pylori* as a risk factor for the development of gastric ulcer although with a lower prevalence of infection (less than 50%) [101]. Finally, in a Chinese study, it was reported that among 43 Chinese children suffering with peptic ulcer disease, 37 had duodenal ulcer, of which 21 were *H. pylori* positive, while only six had gastric ulcer, of which only two were positive for the infection [7]. In summary, *H. pylori* infection is much more associated to duodenal ulcer than to gastric ulcer, in both children and adults.

The causative role of *H. pylori* in gastric ulcers in children and adolescents is, therefore, less certain when compared to adults, possibly reflecting the fact that a large proportion of gastric ulcers are secondary in nature in children. Characteristically, in children younger than 10 years of age, peptic ulcers are usually due to noxious agents (such as corticosteroids and nonsteroidal anti-inflammatory drugs (NSAIDs)) or occur after major stresses (such as burns, trauma, and systemic illness). In these settings, upper gastrointestinal tract haemorrhage, vomiting and perforation are frequent presenting features. The ulcers tend not to recur after healing. In older children and adolescents, the clinical presentation and natural history of peptic ulcers are similar to that observed in adults, presenting as epigastric and nocturnal abdominal pain and being usually associated with *H. pylori* infection [8,100,101]. In this setting, even though the acute ulcer is likely to heal, the natural history is for ulcer recurrence. Moreover, the complication rate of peptic ulceration is important. The estimated incidence of peptic ulcer bleeding in the US paediatric population also has ranged from 0.5 to 4.4/100,000 individuals in 2008 [105].

*H. pylori* with consequent inflammation and ulceration [113]. Eradication of the *H. pylori* infection corrects the hypergastrinemia and decreases the basal acid secretory rate, heals any peptic ulcer and ameliorates any symptoms of gastroesophageal reflux [115]. Conversely, gastric ulcers are associated with *H. pylori*–induced pan- or corpus-predominant gastritis, resulting in multifocal atrophy of acid-secreting mucosa and reduced acid secretion. These ulcers usually arise at the junction of the antral and corpus mucosa, an area of intense inflam‐ mation [113]. Thus, the non-acidophilic nature of *H. pylori* (see section 1.2.1) explains how those with low acid secretory capacity are more susceptible to spread of infection through the corpus mucosa and to gastric ulceration. With their somewhat common pathobiology, gastric ulcer disease precedes the development of gastric cancer [93,116,117]. Gastric and duodenal ulcers have marked differences in their basis, placing them on opposite ends of disease spectrum. *H. pylori*-induced duodenal ulcer conveys a lower risk of developing a gastric cancer [117]. But, what makes it possible for *H. pylori* to be involved in both ends of disease spectrum? Although the mechanisms are unclear, the infecting strain itself may play a crucial role on the diverging point of this disease spectrum [16,93]. Moreover, the similarity between the phenotype of gastric ulcer and gastric cancer raises questions about the carcinogenic potential of the associated *H. pylori* strains [93]. Certainly the etiology for *H. pylori*-associated peptic ulcer in adults depends on the complex interplay of gastritis phenotype and of progressive physio‐ logical gastro-duodenal alterations through childhood until adulthood, a result of environ‐

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79

mental factors, bacterial virulence factors and host genetic background.

mucosal damage similar to an Arthus reaction [2].

Despite epidemiological evidence that infection during childhood is seldom associated with peptic ulceration or gastric atrophy, the mechanisms underlying differences in histopathology and clinical expression of *H. pylori* infection when compared to the adult, are still poorly identified. Theoretically, such differences might be explained by qualitative and/or quantita‐ tive differences in induced immune response, possibly age-related. Indeed, adults exhibit a predominantly neutrophil infiltrate, whereas *H. pylori*-associated gastritis in children is usually mild and superficial with a predominantly mononuclear infiltrate, a paucity of neutrophils and a higher degree of lymphoid follicular hyperplasia [118]. Therefore, different immunopathology and different patterns of cytokine expression would be anticipated for children when compared to adults [18]. There may be differences in adaptive component of gastric mucosa immune response in children compared to the adult host; a clear Th1 response has not always been demonstrated for young patients. The lower gastritis scores in children may also be a reflection of such a skewed Th1/Th2 balance, which may result in their lower risk for developing ulcer disease [18, 19]. These findings could indicate that the host humoral and cellular responses differ depending on the age at which the gastric infection is first acquired and might explain the varying rates of disease outcomes that are evident in different parts of the world. Nevertheless, higher anti-*H. pylori* IgG antibody titres occur in paediatric patients with duodenal ulcer compared to those without ulceration, suggesting that local humoral immune responses contribute to the development of peptic ulceration in these young patients [102,119,120]. This is not surprising, given the fact that the more severe inflammation, the greater the chance of ulcer formation [121] with increased IgG production leading to

These and other differences explain why some of the recommendations for adults may not apply in children [87,96]. Few randomized, placebo-controlled treatment trials are available in children for the different outcomes (gastritis or peptic ulcer), and often consist of only small numbers of cases [86,106]. Clearly in children as in adults, successful eradication of *H. pylori* markedly reduces the risk of ulcer recurrence [107-110]. Thus, there is general consensus worldwide to treat *H. pylori* infection when there is endoscopic evidence of peptic ulceration. Triple therapy is the treatment of choice in children for endoscopically proven duodenal ulcer and histologically proven *H. pylori* antral gastritis [91, 96, 111, 112].

#### *1.3.2. Differences in the physiopathology of H. pylori-associated gastric and duodenal ulcers*

Peptic ulceration is a multifactorial disease ultimately explained by disequilibrium between aggressive injurious factors and defensive gastroduodenal mucosa-protective factors, which raises the vulnerability of this mucosa to luminal secretions. *H. pylori* infection is considered the major causative factor for peptic ulceration. Nevertheless, there are other injurious mechanisms jeopardizing the mucosal integrity: some viral infections (*e.g.* cytomegalovirus and herpes simplex); drug-induced injury, particularly acetylsalicylic acid, NSAIDs and chemotherapy; vascular disorders interfering with perfusion; major stresses; and syndromes in which a marked overproduction of gastric acid occurs, as is the case of the Zollinger-Ellison syndrome and, more commonly in children, antral G cell hyperplasia (also referred to as pseudo-Zollinger Ellison syndrome) [113].

Although differing in their pathogenesis, both *H. pylori*-associated duodenal ulcers and gastric ulcers are intimately related to changes in the acid production by the gastric mucosa [113, 114]. Indeed, *H. pylori* infection can result in increased, decreased or no overall change in the level of gastric acid secretion. Duodenal ulcers arise on a background of *H. pylori*–induced antral-predominant gastritis with sparing of the oxyntic mucosa, resulting in hypergastrine‐ mia and consequent high levels of acid production from the healthy gastric corpus following meal or hormonal stimulation. In response to the excessive acid secretion, the duodenum develops gastric metaplasia. This, unlike the normal duodenal mucosa, can be colonized by

*H. pylori* with consequent inflammation and ulceration [113]. Eradication of the *H. pylori* infection corrects the hypergastrinemia and decreases the basal acid secretory rate, heals any peptic ulcer and ameliorates any symptoms of gastroesophageal reflux [115]. Conversely, gastric ulcers are associated with *H. pylori*–induced pan- or corpus-predominant gastritis, resulting in multifocal atrophy of acid-secreting mucosa and reduced acid secretion. These ulcers usually arise at the junction of the antral and corpus mucosa, an area of intense inflam‐ mation [113]. Thus, the non-acidophilic nature of *H. pylori* (see section 1.2.1) explains how those with low acid secretory capacity are more susceptible to spread of infection through the corpus mucosa and to gastric ulceration. With their somewhat common pathobiology, gastric ulcer disease precedes the development of gastric cancer [93,116,117]. Gastric and duodenal ulcers have marked differences in their basis, placing them on opposite ends of disease spectrum. *H. pylori*-induced duodenal ulcer conveys a lower risk of developing a gastric cancer [117]. But, what makes it possible for *H. pylori* to be involved in both ends of disease spectrum? Although the mechanisms are unclear, the infecting strain itself may play a crucial role on the diverging point of this disease spectrum [16,93]. Moreover, the similarity between the phenotype of gastric ulcer and gastric cancer raises questions about the carcinogenic potential of the associated *H. pylori* strains [93]. Certainly the etiology for *H. pylori*-associated peptic ulcer in adults depends on the complex interplay of gastritis phenotype and of progressive physio‐ logical gastro-duodenal alterations through childhood until adulthood, a result of environ‐ mental factors, bacterial virulence factors and host genetic background.

The causative role of *H. pylori* in gastric ulcers in children and adolescents is, therefore, less certain when compared to adults, possibly reflecting the fact that a large proportion of gastric ulcers are secondary in nature in children. Characteristically, in children younger than 10 years of age, peptic ulcers are usually due to noxious agents (such as corticosteroids and nonsteroidal anti-inflammatory drugs (NSAIDs)) or occur after major stresses (such as burns, trauma, and systemic illness). In these settings, upper gastrointestinal tract haemorrhage, vomiting and perforation are frequent presenting features. The ulcers tend not to recur after healing. In older children and adolescents, the clinical presentation and natural history of peptic ulcers are similar to that observed in adults, presenting as epigastric and nocturnal abdominal pain and being usually associated with *H. pylori* infection [8,100,101]. In this setting, even though the acute ulcer is likely to heal, the natural history is for ulcer recurrence. Moreover, the complication rate of peptic ulceration is important. The estimated incidence of peptic ulcer bleeding in the US paediatric population also has ranged from 0.5 to 4.4/100,000

These and other differences explain why some of the recommendations for adults may not apply in children [87,96]. Few randomized, placebo-controlled treatment trials are available in children for the different outcomes (gastritis or peptic ulcer), and often consist of only small numbers of cases [86,106]. Clearly in children as in adults, successful eradication of *H. pylori* markedly reduces the risk of ulcer recurrence [107-110]. Thus, there is general consensus worldwide to treat *H. pylori* infection when there is endoscopic evidence of peptic ulceration. Triple therapy is the treatment of choice in children for endoscopically proven duodenal ulcer

and histologically proven *H. pylori* antral gastritis [91, 96, 111, 112].

pseudo-Zollinger Ellison syndrome) [113].

*1.3.2. Differences in the physiopathology of H. pylori-associated gastric and duodenal ulcers*

Peptic ulceration is a multifactorial disease ultimately explained by disequilibrium between aggressive injurious factors and defensive gastroduodenal mucosa-protective factors, which raises the vulnerability of this mucosa to luminal secretions. *H. pylori* infection is considered the major causative factor for peptic ulceration. Nevertheless, there are other injurious mechanisms jeopardizing the mucosal integrity: some viral infections (*e.g.* cytomegalovirus and herpes simplex); drug-induced injury, particularly acetylsalicylic acid, NSAIDs and chemotherapy; vascular disorders interfering with perfusion; major stresses; and syndromes in which a marked overproduction of gastric acid occurs, as is the case of the Zollinger-Ellison syndrome and, more commonly in children, antral G cell hyperplasia (also referred to as

Although differing in their pathogenesis, both *H. pylori*-associated duodenal ulcers and gastric ulcers are intimately related to changes in the acid production by the gastric mucosa [113, 114]. Indeed, *H. pylori* infection can result in increased, decreased or no overall change in the level of gastric acid secretion. Duodenal ulcers arise on a background of *H. pylori*–induced antral-predominant gastritis with sparing of the oxyntic mucosa, resulting in hypergastrine‐ mia and consequent high levels of acid production from the healthy gastric corpus following meal or hormonal stimulation. In response to the excessive acid secretion, the duodenum develops gastric metaplasia. This, unlike the normal duodenal mucosa, can be colonized by

individuals in 2008 [105].

78 Dyspepsia - Advances in Understanding and Management

Despite epidemiological evidence that infection during childhood is seldom associated with peptic ulceration or gastric atrophy, the mechanisms underlying differences in histopathology and clinical expression of *H. pylori* infection when compared to the adult, are still poorly identified. Theoretically, such differences might be explained by qualitative and/or quantita‐ tive differences in induced immune response, possibly age-related. Indeed, adults exhibit a predominantly neutrophil infiltrate, whereas *H. pylori*-associated gastritis in children is usually mild and superficial with a predominantly mononuclear infiltrate, a paucity of neutrophils and a higher degree of lymphoid follicular hyperplasia [118]. Therefore, different immunopathology and different patterns of cytokine expression would be anticipated for children when compared to adults [18]. There may be differences in adaptive component of gastric mucosa immune response in children compared to the adult host; a clear Th1 response has not always been demonstrated for young patients. The lower gastritis scores in children may also be a reflection of such a skewed Th1/Th2 balance, which may result in their lower risk for developing ulcer disease [18, 19]. These findings could indicate that the host humoral and cellular responses differ depending on the age at which the gastric infection is first acquired and might explain the varying rates of disease outcomes that are evident in different parts of the world. Nevertheless, higher anti-*H. pylori* IgG antibody titres occur in paediatric patients with duodenal ulcer compared to those without ulceration, suggesting that local humoral immune responses contribute to the development of peptic ulceration in these young patients [102,119,120]. This is not surprising, given the fact that the more severe inflammation, the greater the chance of ulcer formation [121] with increased IgG production leading to mucosal damage similar to an Arthus reaction [2].

#### *1.3.3. Endoscopic features*

Endoscopy is the only method to accurately diagnose peptic ulceration in children [87,122]. A nodular mucosa in the gastric antrum or duodenal bulb and/or gastric or duodenal erosions or ulcerations are specific (but not sensitive) features, suggesting active *H. pylori* infection. For those with suspected infection, biopsies should be obtained for histopathology, as well as complementary tests for detection of *H. pylori* including rapid urease test, histopathology with Giemsa stain and, if available, culture. The rationale for the recommendation to perform more than one diagnostic test is based on their sensitivity results in children, which range from 66% to 100% for histology and from 75% to 100% for rapid urease tests [91]. In all paediatric age groups, for patients receiving therapy with a proton pump inhibitor, biopsies should be performed on the body and cardia (and, possibly, transition zones) of the stomach as well as from the antrum to reduce the chances of false-negative results. Follow-up endoscopy is rarely necessary, except in the setting of peptic ulceration associated with complications (such as haemorrhage or perforation).

IL-1 cluster, located on chromosome 2q12-22 region, includes the genes *IL-1A*, *IL-1B* and *IL-1RN* that code for the proinflammatory cytokines IL-1α, IL-1β and their endogenous receptor antagonist IL-1RA, respectively. The less common alleles of *IL-1B*, *i.e.*, *IL-1B-31C* and *IL-1B-511T* (representing, respectively, T-C and C-T transitions at positions 31 and 511 of the *IL-1B* promoter) are associated with a higher risk of hypochlorhydria [116]. This association can be explained considering that such polymorphisms lead to increased IL-1β expression/ secretion that, upon *H. pylori*-infection, amplifies the host inflammatory response. Also the less common allele of IL-1RA, *i.e.*, the IL-1RN\*2 (representing one of the five known 86 base pair tandem repeat polymorphisms in intron 2) is associated with a higher risk of gastric cancer in adults [116]. The risk is potentiated when in association with infection by *cagA*/*vacA*-positive *H. pylori* strains, highlighting the interplay between host and bacterial factors that seems to be involved in the development of gastric pathology [126]. Children presenting the IL1RN\*2 allele and infected by *cagA*-positive *H. pylori* strains are at higher risk of duodenal ulceration, emphasizing differences in the physiopathology of the disease between adult and paediatric patients [124]. Also at higher risk of developing duodenal ulcer are children presenting the transition G-A at position 238 of the TNF-α coding gene when infected by *iceA1*-positive *H.*

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Other putative host risk factors for *H. pylori*-severe gastroduodenal diseases are the polymorphisms in the genes coding for Toll-like receptors (TLRs) that might influence the innate and adaptive immune response to the infection. Indeed, the presence of the TLR4 allele in combination with infection by *cagA*-positive strains, leads to increased gastric levels

The co-evolution between *H. pylori* and the modern humans has determined the extremely high diversity of the bacterium in both its genetic background and virulence. Thus, it is likely that bacterial determinants may influence the clinical outcome, an association that is well established for *cagA*, *vacA* and *babA* genes (see sections 1.2.2 and 1.2.3 of this chapter). Never‐ theless, this topic is far from being fully clarified, and the identification of other factors responsible for the enhanced virulence of the bacteria leading to the development of more severe diseases remains pertinent. For that purpose, the study of *H. pylori* strains isolated in specific clinical situations, such as the paediatric peptic ulcer disease, can be useful. Indeed, *H. pylori* paediatric infection may be regarded as a privileged natural study model of the interaction of this bacterium with human host, as the child is usually not exposed to injurious factors as is the adult and represents a different stage of *H. pylori* infection in a immunologically maturing host. Comparative genomic studies of the rare paediatric ulcerogenic *H. pylori* strains and of the non-ulcerogenic strains show a distinctive genotype virulence pattern, suggesting a potential pathogenic role for new markers [9-15]. Two putative virulence determinants are associated with peptic ulceration, mostly duodenal ulcer, in children and with other *H. pylori*-virulence factors: j*hp0562*, involved in lipopolysaccharide biosynthesis and in the regulation of Lewis antigen expression [13]; and *homB*, a putative outer membrane protein, involved in bacterial adherence [9,11,12,14,15]. HomB contributes to the proinflammatory

**1.4. Molecular profile of ulcerogenic paediatric** *H. pylori* **strains**

*pylori* strains [127].

of IL-8 and IL-10 [128].

#### *1.3.4. Host susceptibility*

The multifactorial nature of peptic ulcer disease reflects its dependence on the patients' genetic susceptibility and habits (alcohol and/or non-steroid anti-inflammatory drug consumption, diet, smoking and stress) [20]. Paediatric peptic ulcer disease is significantly more frequent in boys than in girls (63.6% *versus* 36.4%, p<0.025) [32]. Although female hormones may have a protective role against developing peptic ulcerations [123], the true nature of this susceptibility of the male gender remains unclear.

Mucins, glycoproteins secreted by the gastric mucosa, form a gel layer that is essential to maintain a stable neutral pH adjacent to epithelium. This mucus barrier affords protection from attack by acid-pepsin and other luminal noxious agents [124]. *H. pylori* has a complex relationship with different gastric mucins' subtypes. Infected children for example have a decreased mucin in their gastric mucosa presumably weakening this important defense barrier [125]. The highly diverse carbohydrate structure of the gastric mucins, functioning as binding sites for *H. pylori*, should also play a role in the outcome of infection, with genetic and epigenetic changes in the mucin molecules influencing the susceptibility of the patient for *H. pylori*associated peptic ulcer disease. Recently, it was shown that *H. pylori*-infected children presented a normal pattern of expression and glycosylation of mucin 5AC (MUC5AC) in the surface mucous cells, and MUC6 in the gland mucous cells, contrasting with the aberrant expression of MUC6 and MUC2 found in infected adults. Additionally, it was shown that the pattern of Lewis blood group antigens in the surface epithelium of children was significantly correlated with *H. pylori* load, however no correlation with gastritis, nodularity, and gastric or duodenal ulcer was found [17].

In children and teenagers, as in adults, the severity of antral inflammation strongly correlates with the risk of duodenal ulcer disease. Among the host factors, polymorphisms in cytokines encoding genes, or in their promoters, that affect cytokine transcription, are good risk candi‐ dates. Indeed, polymorphisms in the IL-1 gene cluster play an important role in modulating the risk for *H. pylori*-induced hypochlorhydria and, thus, for gastric ulceration and cancer. The IL-1 cluster, located on chromosome 2q12-22 region, includes the genes *IL-1A*, *IL-1B* and *IL-1RN* that code for the proinflammatory cytokines IL-1α, IL-1β and their endogenous receptor antagonist IL-1RA, respectively. The less common alleles of *IL-1B*, *i.e.*, *IL-1B-31C* and *IL-1B-511T* (representing, respectively, T-C and C-T transitions at positions 31 and 511 of the *IL-1B* promoter) are associated with a higher risk of hypochlorhydria [116]. This association can be explained considering that such polymorphisms lead to increased IL-1β expression/ secretion that, upon *H. pylori*-infection, amplifies the host inflammatory response. Also the less common allele of IL-1RA, *i.e.*, the IL-1RN\*2 (representing one of the five known 86 base pair tandem repeat polymorphisms in intron 2) is associated with a higher risk of gastric cancer in adults [116]. The risk is potentiated when in association with infection by *cagA*/*vacA*-positive *H. pylori* strains, highlighting the interplay between host and bacterial factors that seems to be involved in the development of gastric pathology [126]. Children presenting the IL1RN\*2 allele and infected by *cagA*-positive *H. pylori* strains are at higher risk of duodenal ulceration, emphasizing differences in the physiopathology of the disease between adult and paediatric patients [124]. Also at higher risk of developing duodenal ulcer are children presenting the transition G-A at position 238 of the TNF-α coding gene when infected by *iceA1*-positive *H. pylori* strains [127].

Other putative host risk factors for *H. pylori*-severe gastroduodenal diseases are the polymorphisms in the genes coding for Toll-like receptors (TLRs) that might influence the innate and adaptive immune response to the infection. Indeed, the presence of the TLR4 allele in combination with infection by *cagA*-positive strains, leads to increased gastric levels of IL-8 and IL-10 [128].

#### **1.4. Molecular profile of ulcerogenic paediatric** *H. pylori* **strains**

*1.3.3. Endoscopic features*

80 Dyspepsia - Advances in Understanding and Management

haemorrhage or perforation).

of the male gender remains unclear.

duodenal ulcer was found [17].

*1.3.4. Host susceptibility*

Endoscopy is the only method to accurately diagnose peptic ulceration in children [87,122]. A nodular mucosa in the gastric antrum or duodenal bulb and/or gastric or duodenal erosions or ulcerations are specific (but not sensitive) features, suggesting active *H. pylori* infection. For those with suspected infection, biopsies should be obtained for histopathology, as well as complementary tests for detection of *H. pylori* including rapid urease test, histopathology with Giemsa stain and, if available, culture. The rationale for the recommendation to perform more than one diagnostic test is based on their sensitivity results in children, which range from 66% to 100% for histology and from 75% to 100% for rapid urease tests [91]. In all paediatric age groups, for patients receiving therapy with a proton pump inhibitor, biopsies should be performed on the body and cardia (and, possibly, transition zones) of the stomach as well as from the antrum to reduce the chances of false-negative results. Follow-up endoscopy is rarely necessary, except in the setting of peptic ulceration associated with complications (such as

The multifactorial nature of peptic ulcer disease reflects its dependence on the patients' genetic susceptibility and habits (alcohol and/or non-steroid anti-inflammatory drug consumption, diet, smoking and stress) [20]. Paediatric peptic ulcer disease is significantly more frequent in boys than in girls (63.6% *versus* 36.4%, p<0.025) [32]. Although female hormones may have a protective role against developing peptic ulcerations [123], the true nature of this susceptibility

Mucins, glycoproteins secreted by the gastric mucosa, form a gel layer that is essential to maintain a stable neutral pH adjacent to epithelium. This mucus barrier affords protection from attack by acid-pepsin and other luminal noxious agents [124]. *H. pylori* has a complex relationship with different gastric mucins' subtypes. Infected children for example have a decreased mucin in their gastric mucosa presumably weakening this important defense barrier [125]. The highly diverse carbohydrate structure of the gastric mucins, functioning as binding sites for *H. pylori*, should also play a role in the outcome of infection, with genetic and epigenetic changes in the mucin molecules influencing the susceptibility of the patient for *H. pylori*associated peptic ulcer disease. Recently, it was shown that *H. pylori*-infected children presented a normal pattern of expression and glycosylation of mucin 5AC (MUC5AC) in the surface mucous cells, and MUC6 in the gland mucous cells, contrasting with the aberrant expression of MUC6 and MUC2 found in infected adults. Additionally, it was shown that the pattern of Lewis blood group antigens in the surface epithelium of children was significantly correlated with *H. pylori* load, however no correlation with gastritis, nodularity, and gastric or

In children and teenagers, as in adults, the severity of antral inflammation strongly correlates with the risk of duodenal ulcer disease. Among the host factors, polymorphisms in cytokines encoding genes, or in their promoters, that affect cytokine transcription, are good risk candi‐ dates. Indeed, polymorphisms in the IL-1 gene cluster play an important role in modulating the risk for *H. pylori*-induced hypochlorhydria and, thus, for gastric ulceration and cancer. The The co-evolution between *H. pylori* and the modern humans has determined the extremely high diversity of the bacterium in both its genetic background and virulence. Thus, it is likely that bacterial determinants may influence the clinical outcome, an association that is well established for *cagA*, *vacA* and *babA* genes (see sections 1.2.2 and 1.2.3 of this chapter). Never‐ theless, this topic is far from being fully clarified, and the identification of other factors responsible for the enhanced virulence of the bacteria leading to the development of more severe diseases remains pertinent. For that purpose, the study of *H. pylori* strains isolated in specific clinical situations, such as the paediatric peptic ulcer disease, can be useful. Indeed, *H. pylori* paediatric infection may be regarded as a privileged natural study model of the interaction of this bacterium with human host, as the child is usually not exposed to injurious factors as is the adult and represents a different stage of *H. pylori* infection in a immunologically maturing host. Comparative genomic studies of the rare paediatric ulcerogenic *H. pylori* strains and of the non-ulcerogenic strains show a distinctive genotype virulence pattern, suggesting a potential pathogenic role for new markers [9-15]. Two putative virulence determinants are associated with peptic ulceration, mostly duodenal ulcer, in children and with other *H. pylori*-virulence factors: j*hp0562*, involved in lipopolysaccharide biosynthesis and in the regulation of Lewis antigen expression [13]; and *homB*, a putative outer membrane protein, involved in bacterial adherence [9,11,12,14,15]. HomB contributes to the proinflammatory characteristics of *H. pylori*. Strains that are also positive for both *homB* and *jhp562* are related to a higher risk of paediatric peptic ulcer disease. Thus, it is likely that these new markers acting together with the well-established virulence markers will promote a more severe antral inflammation, a phenomenon strongly associated with duodenal ulceration.

*pylori* strains and more susceptible young patients. *H. pylori*-associated paediatric peptic ulcer disease is, therefore, a privileged natural study model to search for ulcerogenic-specific bacterial biomarkers and implicated molecular mechanisms, a required step to better address this important public health problem. This includes enhanced virulence of the paediatric ulcerogenic *H. pylori* strains that also may have a natural ability to better adapt to the hostility

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This work was supported by BNP Paribas patronage and a research Grant from the Sociedade

and Ana Isabel Lopes3

1 Center for Biodiversity, Functional & Integrative Genomics, Faculty of Sciences, University of Lisbon, Lisbon, Portugal and Department of Genetics, National Institute of Health Dr. Ri‐

2 Department of Infectious Diseases, National Institute of Health Dr. Ricardo Jorge, Lisbon,

3 Gastroenterology Unit, Department of Paediatrics, University Hospital Santa Maria, Medi‐

[1] Linz B, Balloux F, Moodley Y, Manica A, Liu H, Roumagnac P et al. An African ori‐ gin for the intimate association between humans and Helicobacter pylori. Nature

[2] Blaser MJ. Helicobacters are indigenous to the human stomach: duodenal ulceration is due to changes in gastric microecology in the modern era. Gut 1998; 43(5):721-727.

[3] Konturek PC, Konturek SJ, Brzozowski T. Helicobacter pylori infection in gastric can‐

of their niche.

**Acknowledgements**

**Author details**

Mónica Roxo-Rosa1

Portugal

**References**

cardo Jorge, Lisbon, Portugal

cal Faculty of Lisbon, Lisbon, Portugal

2007; 445(7130):915-918.

cerogenesis. J Physiol Pharmacol 2009; 60(3):3-21.

Portuguesa de Gastrenterologia.

, Mónica Oleastro2

\*Address all correspondence to: roxorosa@hotmail.com

Other pathogenic genes interact synergistically to induce peptic ulcer in young patients. There is no gene or protein that acts alone to establish the virulence of *H. pylori* [74]. Accordingly, we investigated further virulence-associated genes by comparing the proteome of a group of genetically/epidemiologically-unlinked *H. pylori* strains, all isolated from Portuguese children, half suffering with peptic ulcer disease, and the other presenting only active gastritis [16]. Despite the typical proteome profile of all the *H. pylori* strains grown under the same labora‐ torial conditions [129], the ulcerogenic paediatric *H. pylori* strains presented differences suggestive of higher motility, better antioxidant defences and a metabolism favouring the biosynthesis of aromatic amino acids. As already mentioned in this chapter (see section 1.2.1 of this chapter) motility is a long known virulence-related trait [46], with lower-motility associated reduced inflammation levels [47] and with non-motile strains unable to establish a robust infection [42,45,46]. Moreover, it was more recently shown that higher motility enhances *H. pylori* density and inflammatory response in dyspeptic patients [130].

The differences in the abundance of antioxidant proteins observed between paediatric ulcerogenic and non-ulcerogenic strains may be important in conferring resistance to inflam‐ mation; the enzymes involved in key steps in the metabolism of glucose, amino acids and urea may be advantageous to respond to fluctuations of nutrients [16].

Additionally, by comparing the duodenal ulcer-associated paediatric strains with the one studied strain associated with gastric ulcer, we observed differences on the abundance of proteins associated with acid resistance and motility. These suggest that the former are better prepared to survive to the abnormal low levels of pH observed in duodenal ulceration, in contrast to the gastric ulcer strain which is a better swimmer, supporting the proximal spread of infection characteristic of this disease [16]. Overall, our data supports the idea that the infecting strain may be determinant in the divergence between duodenal and gastric ulcer [93].
