**1. Introduction**

Type 2 diabetes mellitus (T2DM) is among the most prevalent chronic disease [1], affecting approximately 463 million people in 2019, and more than 690 million are expected to be diagnosed by 2045 [2]. People diagnosed with T2DM have a 2–4-fold higher risk of developing cardiovascular disease (CVD) [3]. Despite significant advantages in the prevention strategies that lessen related risk factors, CVD remains the leading cause of morbidity and mortality in patients with T2DM [4].

T2DM and CVD both have multi-factorial etiology, and disorders of lipid metabolism is one of the coexistence features sharing by them. For the development of CVD, the cumulation of ApoB-containing lipoproteins in the arterial wall would lead to lipid deposition and an atheroma initiation, resulting in the progression of atherosclerotic plaques, and eventually atherosclerotic vascular disease [5]. Therefore, lipid-lowering drugs, such as statins, have been recommended as front-line therapy for primary prevention of atherosclerotic CVD [6], and the stateof-the-art therapy in dyslipidemia in diabetic patients [3, 7, 8]. For the potential mechanism between lipid metabolism and diabetes, one meta-analysis reported that lipid parameters, such as triglyceride (TG), and low-density lipoprotein (LDL), can reflect the risk of T2DM [9]. Other lipid subfractions, such as high-density lipoprotein cholesterol (HDL) and lipid-free ApoA-I, could also benefit glycemic control by increasing glucose uptake in skeletal muscle, improving beta-cell function, and decreasing insulin resistance through inhibiting the proinflammatory signal transduction pathways [10].

#### *Management of Dyslipidemia*

Considering the rather complex components of lipid and different directions for the associations between different lipid components and diabetes [11], more efforts are needed to elucidate the relationships between lipid profile and diabetes.

### **2. Lipid abnormality and incident type 2 diabetes mellitus**

There are six major lipoproteins exist in blood: chylomicrons, very-low-density lipoprotein (VLDL), intermediate-density lipoprotein (IDL), low-density lipoprotein (LDL); lipoprotein(a) (Lp(a)), and high-density lipoprotein (HDL) [12]. Dyslipidemia represents a cluster of lipid and lipoprotein abnormalities, including elevation of both fasting and postprandial TG, apolipoprotein (Apo)A, or ApoB. The prevalence of dyslipidemia is getting severer worldwide. According to the 2015 Global Burden of Disease Study, the prevalence of elevated total cholesterol (TC) (≥200 mg/dL) was highest in the WHO European Region (54% for both sexes), followed by the WHO Region of the Americas (48% for both sexes). The WHO African Region and the WHO South-East Asia Region showed the lowest percentages (23% and 30%, respectively) [13]. In China, the prevalence of dyslipidemia was 42.8% overall [14], with 4.3%, 2.4%, 14.7%, and 17.4% for the age-standardized prevalence of high TC, LDL, TG, and HDL, respectively [15].

Evidence suggests that the development of T2DM was closely associated with lipid abnormality [16–26]. A study based on the 2010–2012 China National Nutrition and Health Survey (CNNHS) reported that the prevalence of dyslipidemia was 39.9%, 46.8%, and 59.3% in participants with normal glucose, prediabetes, and T2DM [16]. Zhu et al. 's meta-analysis reported that there were positive associations between different lipid parameters and T2DM. Moreover, the standardized mean difference for the Atherogenic index of plasma (AIP, lg(TG/ HDL)) is 1.78 (95% confidence interval (CI): 1.04–2.52), which is higher than for other parameters (TG: 0.93, 95% CI: 0.78–1.09; TC: 0.46, 95% CI: 0.21–0.71; HDL-C: −0.89, 95%CI: −1.18 to −0.60; and LDL-C: 0.44, 95% CI: 0.11–0.77), suggesting AIP may be more closely associated with the risk of T2DM [9]. Results from the prospective cohort study (Multi-Ethnic Study of Atherosclerosis) found that elevated total ApoC-III concentrations were associated with a higher rate of diabetes, while ApoC-III-defined HDL subspecies displayed opposing associations: HDL lacking ApoC-III was inversely associated with incident diabetes, while no association was found for HDL containing ApoC-III. Further adjustment for plasma TG as a potential intermediate attenuated these associations [17]. Besides, not only baseline cross-sectional estimated or abnormal lipid level is related, Zheng et al. found that time-dependent TG/HDL ratios were also positively associated with future incident T2DM, which supports the change patterns for these parameters during the follow-up could intricate the development of diabetes [18]. Beshars et al. evaluated the relationship between diabetes and the increment in triglyceride levels within the normal range. Their results suggest that sustained increments in rising triglyceride levels, even within the accepted normal range, might pose a cumulative risk for the development of diabetes and impaired fasting glucose [19].

Despite the aforementioned epidemiologic evidence, the precise mechanisms of the associations are complex and remain unclear. Since the hallmark of T2DM is the inability of pancreatic beta-cells to produce adequate amounts of insulin, accompanied by reduced tissue responsiveness to insulin, also known as insulin resistance. Lipotoxicity caused by dyslipidemia plays an important role in the development and progression of insulin resistance [10]. It can disturb the utilization of insulin in peripheral target tissues (such as the liver), thus affecting the amount of lipids synthesis in the liver. So, elevated blood lipid can lead to insulin resistance,

**41**

*Lipids Abnormality and Type 2 Diabetes Mellitus: Causes and Consequences*

muscle LRP2 causes insulin resistance and glucose intolerance [30].

**3. Lipid-lowering medication and incident type 2 diabetes mellitus**

Lipid-lowering medication plays an essential role in the current healthcare system, not only for the optimization of the lipid profile but also to reduce cardiovascular risk [6, 12]. Recently, there is increased awareness of the possibility that lipid-lowering medications may affect glucose control and insulin resistance [31–33]. This phenomenon is reported in all classes of lipid-modifying agents, with

Some insights into this question emerged from some recent studies. Barak et al. systematically reviewed the related evidence and reported that both statins and niacin are associated with increased risk of impaired glucose control and development of new-onset diabetes, as opposed to bile-acid sequestrants which display concomitant moderate lipid and glucose-lowering effects, and fibrates (particularly the pan-PPAR agonist bezafibrate) which may produce beneficial effects on glucose metabolism and insulin sensitivity [34]. Another recently published meta-analysis, which included 163,688 nondiabetic patients from thirty-three randomized controlled trials, reported no significant association between 1-mmol/L reduction in LDL cholesterol and incident diabetes for statins or PCSK9 inhibitors. More intensive lipid-lowering therapy (defined as the more potent pharmacological strategy, such as PCSK9 inhibitors, higher intensity statins, or statins) was associated with a higher risk of incident diabetes compared with less intensive therapy (active control group or placebo/usual care of the trial). Meta-regression analysis suggested that these results were mainly driven by a higher risk of incident diabetes with statins, whereas PCSK9 inhibitors were not associated with incident diabetes (P = 0.02 for interaction). Thus, among intensive lipid-lowering therapies, there was no independent association between reduction in LDL cholesterol and incident diabetes [32]. The precise mechanisms for statin-induced diabetes remain unclear. However, several mechanisms have been proposed, including impaired insulin sensitivity, impaired insulin secretion, and compromised beta-cell function via enhanced intracellular cholesterol uptake due to inhibition of intracellular cholesterol synthesis by statins [34]. Recently, genetic studies have added more evidence to this. LDL-lowering alleles in *HMGCR*, which encodes the statins' molecular target, were associated with a higher risk of T2DM and higher body mass index [35]. A further larger-scale individual meta-analysis concluded that other LDL-lowering alleles, such as *NPC1L1*, *PCSK9*, *ABCG5/G8*, were also associated with a higher risk T2DM [31]. Nevertheless, it has to be stressed here that the cardiovascular benefits of

Diabetic dyslipidemia is a cluster of plasma lipid and lipoprotein abnormalities that are metabolically interrelated among diabetic patients. It is mainly

which in turn aggravates the generation of lipid metabolism disorder [27–29]. More recently, Seo et al. found that ApoJ is a novel hepatokine targeting muscle glucose metabolism and insulin sensitivity through low-density lipoprotein receptor-related protein-2 (LRP2)-dependent mechanism, coupled with the insulin receptor signaling cascade. In muscle, LRP2 is necessary for insulin receptor internalization, an initial trigger for insulin signaling, that is crucial in regulating downstream signaling and glucose uptake. Of physiologic significance, deletion of hepatic ApoJ or

*DOI: http://dx.doi.org/10.5772/intechopen.96592*

differential effects of distinct drugs.

statins far outweigh diabetes risk [3].

**4. Type 2 diabetic dyslipidemia**

*Lipids Abnormality and Type 2 Diabetes Mellitus: Causes and Consequences DOI: http://dx.doi.org/10.5772/intechopen.96592*

*Management of Dyslipidemia*

Considering the rather complex components of lipid and different directions for the associations between different lipid components and diabetes [11], more efforts

There are six major lipoproteins exist in blood: chylomicrons, very-low-density lipoprotein (VLDL), intermediate-density lipoprotein (IDL), low-density lipoprotein (LDL); lipoprotein(a) (Lp(a)), and high-density lipoprotein (HDL) [12]. Dyslipidemia represents a cluster of lipid and lipoprotein abnormalities, including elevation of both fasting and postprandial TG, apolipoprotein (Apo)A, or ApoB. The prevalence of dyslipidemia is getting severer worldwide. According to the 2015 Global Burden of Disease Study, the prevalence of elevated total cholesterol (TC) (≥200 mg/dL) was highest in the WHO European Region (54% for both sexes), followed by the WHO Region of the Americas (48% for both sexes). The WHO African Region and the WHO South-East Asia Region showed the lowest percentages (23% and 30%, respectively) [13]. In China, the prevalence of dyslipidemia was 42.8% overall [14], with 4.3%, 2.4%, 14.7%, and 17.4% for the age-standardized

are needed to elucidate the relationships between lipid profile and diabetes.

**2. Lipid abnormality and incident type 2 diabetes mellitus**

prevalence of high TC, LDL, TG, and HDL, respectively [15].

Evidence suggests that the development of T2DM was closely associated with lipid abnormality [16–26]. A study based on the 2010–2012 China National Nutrition and Health Survey (CNNHS) reported that the prevalence of dyslipidemia was 39.9%, 46.8%, and 59.3% in participants with normal glucose, prediabetes, and T2DM [16]. Zhu et al. 's meta-analysis reported that there were positive associations between different lipid parameters and T2DM. Moreover, the standardized mean difference for the Atherogenic index of plasma (AIP, lg(TG/ HDL)) is 1.78 (95% confidence interval (CI): 1.04–2.52), which is higher than for other parameters (TG: 0.93, 95% CI: 0.78–1.09; TC: 0.46, 95% CI: 0.21–0.71; HDL-C: −0.89, 95%CI: −1.18 to −0.60; and LDL-C: 0.44, 95% CI: 0.11–0.77), suggesting AIP may be more closely associated with the risk of T2DM [9]. Results from the prospective cohort study (Multi-Ethnic Study of Atherosclerosis) found that elevated total ApoC-III concentrations were associated with a higher rate of diabetes, while ApoC-III-defined HDL subspecies displayed opposing associations: HDL lacking ApoC-III was inversely associated with incident diabetes, while no association was found for HDL containing ApoC-III. Further adjustment for plasma TG as a potential intermediate attenuated these associations [17]. Besides, not only baseline cross-sectional estimated or abnormal lipid level is related, Zheng et al. found that time-dependent TG/HDL ratios were also positively associated with future incident T2DM, which supports the change patterns for these parameters during the follow-up could intricate the development of diabetes [18]. Beshars et al. evaluated the relationship between diabetes and the increment in triglyceride levels within the normal range. Their results suggest that sustained increments in rising triglyceride levels, even within the accepted normal range, might pose a cumulative

risk for the development of diabetes and impaired fasting glucose [19].

Despite the aforementioned epidemiologic evidence, the precise mechanisms of the associations are complex and remain unclear. Since the hallmark of T2DM is the inability of pancreatic beta-cells to produce adequate amounts of insulin, accompanied by reduced tissue responsiveness to insulin, also known as insulin resistance. Lipotoxicity caused by dyslipidemia plays an important role in the development and progression of insulin resistance [10]. It can disturb the utilization of insulin in peripheral target tissues (such as the liver), thus affecting the amount of lipids synthesis in the liver. So, elevated blood lipid can lead to insulin resistance,

**40**

which in turn aggravates the generation of lipid metabolism disorder [27–29]. More recently, Seo et al. found that ApoJ is a novel hepatokine targeting muscle glucose metabolism and insulin sensitivity through low-density lipoprotein receptor-related protein-2 (LRP2)-dependent mechanism, coupled with the insulin receptor signaling cascade. In muscle, LRP2 is necessary for insulin receptor internalization, an initial trigger for insulin signaling, that is crucial in regulating downstream signaling and glucose uptake. Of physiologic significance, deletion of hepatic ApoJ or muscle LRP2 causes insulin resistance and glucose intolerance [30].

#### **3. Lipid-lowering medication and incident type 2 diabetes mellitus**

Lipid-lowering medication plays an essential role in the current healthcare system, not only for the optimization of the lipid profile but also to reduce cardiovascular risk [6, 12]. Recently, there is increased awareness of the possibility that lipid-lowering medications may affect glucose control and insulin resistance [31–33]. This phenomenon is reported in all classes of lipid-modifying agents, with differential effects of distinct drugs.

Some insights into this question emerged from some recent studies. Barak et al. systematically reviewed the related evidence and reported that both statins and niacin are associated with increased risk of impaired glucose control and development of new-onset diabetes, as opposed to bile-acid sequestrants which display concomitant moderate lipid and glucose-lowering effects, and fibrates (particularly the pan-PPAR agonist bezafibrate) which may produce beneficial effects on glucose metabolism and insulin sensitivity [34]. Another recently published meta-analysis, which included 163,688 nondiabetic patients from thirty-three randomized controlled trials, reported no significant association between 1-mmol/L reduction in LDL cholesterol and incident diabetes for statins or PCSK9 inhibitors. More intensive lipid-lowering therapy (defined as the more potent pharmacological strategy, such as PCSK9 inhibitors, higher intensity statins, or statins) was associated with a higher risk of incident diabetes compared with less intensive therapy (active control group or placebo/usual care of the trial). Meta-regression analysis suggested that these results were mainly driven by a higher risk of incident diabetes with statins, whereas PCSK9 inhibitors were not associated with incident diabetes (P = 0.02 for interaction). Thus, among intensive lipid-lowering therapies, there was no independent association between reduction in LDL cholesterol and incident diabetes [32].

The precise mechanisms for statin-induced diabetes remain unclear. However, several mechanisms have been proposed, including impaired insulin sensitivity, impaired insulin secretion, and compromised beta-cell function via enhanced intracellular cholesterol uptake due to inhibition of intracellular cholesterol synthesis by statins [34]. Recently, genetic studies have added more evidence to this. LDL-lowering alleles in *HMGCR*, which encodes the statins' molecular target, were associated with a higher risk of T2DM and higher body mass index [35]. A further larger-scale individual meta-analysis concluded that other LDL-lowering alleles, such as *NPC1L1*, *PCSK9*, *ABCG5/G8*, were also associated with a higher risk T2DM [31]. Nevertheless, it has to be stressed here that the cardiovascular benefits of statins far outweigh diabetes risk [3].

#### **4. Type 2 diabetic dyslipidemia**

Diabetic dyslipidemia is a cluster of plasma lipid and lipoprotein abnormalities that are metabolically interrelated among diabetic patients. It is mainly characterized by increased TG levels, low HDL levels, and postprandial lipemia and contributes to the development of vascular complications [36]. Results from the 2010–2012 China National Nutrition and Health Survey (CNNHS) shown that the prevalence of dyslipidemia was 39.9%, 46.8%, and 59.3% in participants with normal glucose, prediabetes, and T2DM [16]. Another study using data from the 2010–2014 Diabetes Mellitus/Hypertension (DM/HT) study, which included 140,557 Thai adults with diabetes, reported that the dyslipidemia prevalence of 88.9% [37]. Despite the heterogeneity between different studies, the prevalence of diabetic dyslipidemia has grown gradually worldwide [4].

The pathophysiology of diabetic dyslipidemia is intricate and has not been fully understood [38]. Briefly speaking, changes in plasma lipoproteins among diabetic patients are affected by insufficient insulin function and hyperglycemia [39]. During the postprandial state, dietary fatty acids (FA) and cholesterol absorbed by the intestinal cells are incorporated as TG and cholesteryl esters into chylomicrons. In the capillary beds of adipocytes (especially in the fed state) and muscle, chylomicrons are the substrate for lipoprotein lipase (LPL), promoting lipolysis of chylomicrons TG and the release of FA. Insulin regulates LPL activity at several levels, including gene expression, protein synthesis, and secretion, and LPL is reduced in insulin-resistant individuals with T2DM with a consequent increase in plasma TG and decrease in HDL [40].

#### **5. Type 2 diabetic dyslipidemia and cardiovascular disease**

Both diabetes and dyslipidemia are important risk factors for CVD development, powered by the dyslipidemia-insulin resistance-hyperinsulinemia cycle [41]. This makes patients with diabetes dyslipidemia much more vulnerable to CVD outcomes. Results from the Multiple Risk Factor Intervention Trial (MRFIT) reported that among men who had diabetes at baseline, the absolute risk of coronary mortality at each level of blood cholesterol (for 20 mg/dL increments in TC starting from 180 mg/dL to >280 mg/dL), was 3–5 times higher in the presence of diabetes [42]. The United Kingdom Prospective Diabetes Study (UKPDS) has provided further evidence of a similarly direct and continuous association of coronary disease risk with LDL concentration. Among newly diagnosed T2DM, one mmol/L increase in LDL was associated with a 57% increased risk of myocardial infarction [43].

Many former studies have widely reported the causal association between dyslipidemia and CVD. Due to the rather complex components of lipid profile, diagnosis of diabetic dyslipidemia is not always revealed by the lipid measures used in clinical practice, as LDL levels may remain within the normal range. Therefore, it is suggested to use non-HDL levels to reflect the whole lipid spectrum [12]. The 2019 ESC/EAS Guidelines stated that ApoB analysis is recommended for risk assessment, particularly in people with high TG, diabetes, obesity, or metabolic syndrome. ApoB can be used as an alternative to LDL-C, if available, as the primary measurement for screening, diagnosis, and management [6].

Since a higher risk of atherosclerotic vascular disease in diabetic patients, lipid management has been recommended by diabetes-related clinical guidelines [3, 7, 8, 44, 45]. Consistent data have demonstrated the efficacy of statins, the firstchoice lipid-lowering treatment, in preventing cardiovascular events and reducing cardiovascular mortality in patients with diabetes. A meta-analysis including 18,686 diabetic patients demonstrated that a statin-induced reduction of LDL by 1.0 mmol/L was associated with a 9% reduction in all-cause mortality and a 21% reduction in the incidence of major CV events [46]. The newly released ADA's Standards of Medical Care in Diabetes-2020 has stated that statins should be used

**43**

*Lipids Abnormality and Type 2 Diabetes Mellitus: Causes and Consequences*

*DOI: http://dx.doi.org/10.5772/intechopen.96592*

**Density (g/mL)**

Chylomicrons

VLDL

IDL LDL HDL Lp(a) *VLDL: very-low-density lipoprotein.*

*L, et al. Eur Heart J. 2020;41 [1]:111–88.*

**Table 1.**

*Physical and chemical characteristics of human plasma lipoproteins\**

*.*

<0.95 0.95–1.006 1.006–1.019 1.019–1.063 1.063–1.210 1.006–1.125

25–30

4–8

35–46 *Apo: apolipoprotein; HDL: high-density lipoprotein; IDL: intermediate-density lipoprotein; LDL: low-density lipoprotein; Lp(a): lipoprotein(a); PLs: phospholipids; TGs: triglycerides;* 

*\*Adapted from: "2019 ESC/EAS Guidelines for the management of dyslipidaemias: lipid modification to reduce cardiovascular risk." By Mach F, Baigent C, Catapano AL, Koskinas KC, Casula M, Badimon* 

17–24

6–9

Apo(a)

8–13

7

10–20

55

5

ApoA-I

ApoC-II, C-III, E, M

ApoB-100

20–25

4–6

34–35

22–26

6–15

ApoB-100

25–30

25–40

20–35

16–24

7–11

ApoB-100

30–80

50–65

8–14

12–16

4–7

ApoB-100

80–100

90–95

2–4

2–6

1

ApoB-48

**Diameter (nm)**

**TGs (%)**

**Cholesteryl esters (%)**

**PLs (%)**

**Cholesterol (%)**

**Major**

**Apolipoproteins**

**Others** ApoA-I, A-II, A-IV, A-V

ApoA-I, C-II, C-III, E, A-V

ApoC-II, C-III, E


**Table 1.**

*Physical and chemical characteristics of human plasma lipoproteins\**

*.*

*Lipids Abnormality and Type 2 Diabetes Mellitus: Causes and Consequences DOI: http://dx.doi.org/10.5772/intechopen.96592*

*Management of Dyslipidemia*

and decrease in HDL [40].

characterized by increased TG levels, low HDL levels, and postprandial lipemia and contributes to the development of vascular complications [36]. Results from the 2010–2012 China National Nutrition and Health Survey (CNNHS) shown that the prevalence of dyslipidemia was 39.9%, 46.8%, and 59.3% in participants with normal glucose, prediabetes, and T2DM [16]. Another study using data from the 2010–2014 Diabetes Mellitus/Hypertension (DM/HT) study, which included 140,557 Thai adults with diabetes, reported that the dyslipidemia prevalence of 88.9% [37]. Despite the heterogeneity between different studies, the prevalence of

The pathophysiology of diabetic dyslipidemia is intricate and has not been fully understood [38]. Briefly speaking, changes in plasma lipoproteins among diabetic patients are affected by insufficient insulin function and hyperglycemia [39]. During the postprandial state, dietary fatty acids (FA) and cholesterol absorbed by the intestinal cells are incorporated as TG and cholesteryl esters into chylomicrons. In the capillary beds of adipocytes (especially in the fed state) and muscle, chylomicrons are the substrate for lipoprotein lipase (LPL), promoting lipolysis of chylomicrons TG and the release of FA. Insulin regulates LPL activity at several levels, including gene expression, protein synthesis, and secretion, and LPL is reduced in insulin-resistant individuals with T2DM with a consequent increase in plasma TG

Both diabetes and dyslipidemia are important risk factors for CVD development, powered by the dyslipidemia-insulin resistance-hyperinsulinemia cycle [41]. This makes patients with diabetes dyslipidemia much more vulnerable to CVD outcomes. Results from the Multiple Risk Factor Intervention Trial (MRFIT) reported that among men who had diabetes at baseline, the absolute risk of coronary mortality at each level of blood cholesterol (for 20 mg/dL increments in TC starting from 180 mg/dL to >280 mg/dL), was 3–5 times higher in the presence of diabetes [42]. The United Kingdom Prospective Diabetes Study (UKPDS) has provided further evidence of a similarly direct and continuous association of coronary disease risk with LDL concentration. Among newly diagnosed T2DM, one mmol/L increase in LDL was associated with a 57% increased risk of myocardial infarction [43]. Many former studies have widely reported the causal association between dyslipidemia and CVD. Due to the rather complex components of lipid profile, diagnosis of diabetic dyslipidemia is not always revealed by the lipid measures used in clinical practice, as LDL levels may remain within the normal range. Therefore, it is suggested to use non-HDL levels to reflect the whole lipid spectrum [12]. The 2019 ESC/EAS Guidelines stated that ApoB analysis is recommended for risk assessment, particularly in people with high TG, diabetes, obesity, or metabolic syndrome. ApoB can be used as an alternative to LDL-C, if available, as the primary

Since a higher risk of atherosclerotic vascular disease in diabetic patients, lipid management has been recommended by diabetes-related clinical guidelines [3, 7, 8, 44, 45]. Consistent data have demonstrated the efficacy of statins, the firstchoice lipid-lowering treatment, in preventing cardiovascular events and reducing cardiovascular mortality in patients with diabetes. A meta-analysis including 18,686 diabetic patients demonstrated that a statin-induced reduction of LDL by 1.0 mmol/L was associated with a 9% reduction in all-cause mortality and a 21% reduction in the incidence of major CV events [46]. The newly released ADA's Standards of Medical Care in Diabetes-2020 has stated that statins should be used

diabetic dyslipidemia has grown gradually worldwide [4].

**5. Type 2 diabetic dyslipidemia and cardiovascular disease**

measurement for screening, diagnosis, and management [6].

**42**


#### **Table 2.**

*Guidelines for the management of diabetic dyslipidemia using statin.*

for both primary and secondary CVD prevention among diabetes. The detailed guideline are listed according to age groups: for 20–39 years-old diabetic patients with atherosclerotic cardiovascular disease risk factors, statin therapy is highly recommended in addition to lifestyle therapy; for patients with diabetes aged 40–75 years without atherosclerotic cardiovascular disease, use moderate-intensity statin therapy (lowers LDL by 30–49%) in addition to lifestyle therapy; while for patients aged 50–70 years with diabetes, high-intensity statin therapy (lowers LDL by ≥50%) is recommended [8]. The 2013 ACC/AHA guideline emphasized statin therapy recommended for all patients with diabetes 40 to 75 years of ageindependent of baseline cholesterol [47].

Despite the CVD protective effect among diabetic patients, statin therapy has been associated with new-onset T2DM [31, 32]. A former study reported that for every 40 mmol/L reduction of LDL by statins, conversion to T2DM is increased by 10% [48, 49]. Nevertheless, the benefits in terms of cardiovascular event reduction

**45**

**Author details**

The Netherlands

Kan Wang and Fariba Ahmadizar\*

provided the original work is properly cited.

Department of Epidemiology, Erasmus Medical Center, Rotterdam,

© 2021 The Author(s). Licensee IntechOpen. This chapter is 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,

\*Address all correspondence to: f.ahmadizar@erasmusmc.nl

*Lipids Abnormality and Type 2 Diabetes Mellitus: Causes and Consequences*

greatly exceed the risks of statin therapy, and this has been confirmed in patients at

Complex lipoprotein metabolism abnormalities could present both in the development and progression of type 2 diabetes, which indicates that lipid management can prevent cardiovascular complications among diabetic patients and involve in the prevention of diabetes. Epidemiological studies suggest that lipid components could be a marker for diabetes prediction, though it is still uncertain which lipid markers are of the most clinical value. Lipid control using a lipid-lowering medication, such as statins, could reduce CVD risk among the general population also diabetic people. However, it is necessary to consider statin diabetogenicity in

*DOI: http://dx.doi.org/10.5772/intechopen.96592*

**6. Conclusion**

**Conflict of interest**

low cardiovascular risk [46] (**Tables 1** and **2**).

clinical practice when the statin is indicated.

The authors declare no conflict of interest.

greatly exceed the risks of statin therapy, and this has been confirmed in patients at low cardiovascular risk [46] (**Tables 1** and **2**).
