**2. Risk factors and pathogenesis**

Genetic mutations and the hereditary factors have been the key element for the aggressive behavior of this Cancer with the association of BARCA1 25% BARCA2 75% [5]. Germ line BRCA1 is the most frequently associated with the TNBC but still the debate is going on as there is the variation of the genetics and the ethnicity along with the caner presentation and the prognosis.

The other risk factors are:


*Management of the Triple Negative Locally Advanced Breast Cancer DOI: http://dx.doi.org/10.5772/intechopen.110149*


#### **3. Management**

TNBC presents with the restricted management options that leads it to the recurrence and metastasis with an unfortunate diagnosis. As it lack the hormone receptors status that target the disease and improves the survival. Chemotherapy looks to be the central approach towards the systemic management of TNBC with the surgery is to control the local disease.

#### **3.1 Chemotherapy**

It is the main treatment modality in the TNBC. It can be used as neo-adjuvant as well as the adjuvant setting depending upon the tumor staging.

After the local disease cure by the operative options followed by the adjuvant management by the chemotherapy, the disease free survival (DFS) will be observed. DFS is correlated with the pathological complete response (pCR). Neoadjuvant therapy have more chances to get a high pCR in patients with TNBC and reflected as substitute consequence of the outcome of the disease [12].

#### **3.2 Taxane**

Taxel act as the antitumor agent through the macrophages by initiating the apoptosis. The guidelines by national comprehensive cancer network endorse the sandwich of the regimens consists of taxane, anthracycline, cyclophosphamide, Cisplatin, & fluorouracil. Currently, Taxel/Docetaxel + Adriamycin + cyclophosphamide (TAC), Docetaxel + cyclophosphamide (TC), Adriamycin + cyclophosphamide (AC), cyclophosphamide + methotrexate + fluorouracil (CMF), cyclophosphamide + Adriamycin + fluorouracil (CAF), and cyclophosphamide + Epirubicin + fluorouracil + paclitaxel/ Docetaxel (CEF-T) are among favored adjuvant therapeutic regimens designed for TNBC. Suitable chemotherapy medications and its optimization for the patients with favorable outcome [1].

#### **3.3 Anthracycline**

Anthracycline and anthracycline antibiotics are a group of chemotherapy medications derived from *Streptomyces peucetius* var. *caesius*, having more power to treat the variety of the cancers in comparison to the other regimens. Ongoing clinical educations and studies proved the ideal plans of anthracycline adjuvant to treatment TNBC with dosage of doxorubicin is 60 mg/m2 and that of Epirubicin is 100 mg/m<sup>2</sup> . Anthracyclines that are FEC-100 (100 mg/m<sup>2</sup> Epirubicin), decreases 25–30% danger of relapse as well as mortality. Data currently suggesting that subsequently chemotherapy with anthracycline for the 6 months improves the mortality rate by 38% in

patients of 50 years and below age at the time of diagnosis, whereas the mortality rate in patients with 50 to 69years at the time of identification, reduced by 20%.

The CREATE-X experimental trial indicated that 6–8 cycles of adjuvant capecitabine (1250 mg/m2 from days 1 to 14, every 21 days) with better-quality DFS and OS in the TNBC cohort. The significance of aiming adjuvant capecitabine among patients had residual disease was presently emphasized with outcomes of the phase 3 GEICAM/CIBOMA trial. Phase 3 trial of 876 participants diagnosed with initial stage TNBC and accomplished average adjuvant or neoadjuvant chemotherapy was planned towards evaluation the impact of capecitabine (1000 mg/m2 from days 1 to 14, every 21 days) as an adjuvant therapy irrespective of their pCR status. Though the major transformation was not significant among 5-year DFS and OS between the treatment groups, emphasizing that still there is necessity to select a resistant groups. Outcome among CREATE-X trial currently strength the oncologist and surgeons for management of initial stage TNBC through neoadjuvant chemotherapy and comprehend the group, who ought to have capecitabine. Capecitabine must be considered, ongoing trials are assessing novel agents for the management of the TNBC with residual disease after neoadjuvant treatment [12].

Enhanced markers required to update improved-quality range and managing by the checkpoint inhibitors. Advanced prognosis is observed with checkpoint inhibitors when they are combined with chemotherapeutic agents as an initial therapy. The behavior of malignant tumor is categorizing the possible molecular targets and future researches are also valuing novel small molecule agents for the management of the TNBC with AKT inhibition and numerous others. The management model with chemotherapy agents as "one size fits all" methodology is fluctuating constructed on the behavior and have to be polished more to cover the multiple subtypes [14].

Studies showed that Anthracycline as a single drug up-to-date the pCR rates of 14 to 47%, however consecutive anthracycline and taxane combination therapies had reported pCR of 17 to 39%. Although the research studies are still in the way to express the peak rates of pCR with the chemotherapeutic regimens [12].

#### **3.4 Surgical management**

Multiple surgical options are available from the minimal invasive BCS to the MRM and the immediate reconstruction of the breast [5]. Breast and the axilla are the two different entities to treat. Axillary staging and the nodal involvement and the dissection will be done accordingly. As the presentation is usually in advanced stage and the BCS is not A primary treatment for aggressive and advance tumor, so the better option is to start the neo-adjuvant chemotherapy and assess the tumor response to the chemotherapy, again stage the disease and plan the surgery accordingly if possible then the BCS is the best option to the MRM.

Patients with stages I and II TNBC, will be benefited by BCS plus radiotherapy (BCS + RT), mastectomy only (MRM) or MRM plus radiotherapy (MRM + RT), still there is no single point surgical management has been concluded for the TNBC [15]. Disease free survival study revealed that BCS along with the simultaneous RT had considerable predictive effect than MRM and MRM + RT in the early management of the diagnosis. The axilla will be treated as a separate entity with the sentinel lymph node biopsy in case of clinically and radiological impalpable nodes was defined as removal of at least four lymph nodes and axillary node dissection was defined as removal of ≥10 nodes at least up to level-II clearance that is required for the specific staging of the disease [10].

*Management of the Triple Negative Locally Advanced Breast Cancer DOI: http://dx.doi.org/10.5772/intechopen.110149*

Recent National Comprehensive Cancer Network (NCCN) Guidelines recommend breast surgery (breast conservation surgery or mastectomy) and axillary staging for all TNBC patients diagnosed with the early disease. Study presented that the BCS + RT had better predictive effect than MRM and MRM with RT in the cohort of early staged diagnosed TNBC cases in terms of overall survival. Cox proportional model revealed MRM and MRM along with the RT remained to have unfavorable outcome to the prognosis as related with BCS + RT survival *P* value is 0.006 [15].

#### **3.5 Immunotherapy**

It acts on the immune check points.

#### *3.5.1 Immune check point monotherapy*

As the outcome results to ICIs are higher in cases with TNBC, but the monotherapy effectiveness is still low and under the research control.

PD-1 inhibitor pembrolizumab, avelumab and atezolizumab established a hopeful (ORR) of 18.5% among 32 cases among PD-L1 + ve TNBC. Though, successive bigger phase II KEYNOTE-086 study (NCT02447003) establish an ORR of 5.3% among 170 participants PD-L1 unselected pretreated cancers. Remarkably, 84 treatment-naïve participants included, ORR observed 21.4%, signifying ICIs had better efficiency with 1st line metastatic malignancy. By the favor of that impression, the phase III KEYNOTE-119 trial (NCT02555657) with cases had metastatic TNBC, not revealed any progress among ORR, PFS, or OS by monotherapy pembrolizumab vs. chemotherapy (monotherapy), while participants had peak PD-L1 impression experienced the tendency for better advantage by pembrolizumab [6].

Two research studies by chemotherapy with or without atezolizumab, presently increasing. The IMpassion131 trial (NCT03125902) have to explore the significances of first line atezolizumab along with paclitaxel compared with paclitaxel only in terms of overall improvement, while IMpassion132 study describe atezolizumab as first line joined by chemotherapeutic agents may progress consequences linked through chemotherapeutic only among participants presenting with recurrence of the disease within the year of adjuvant therapy. Several enduring early-stage disease trials will additional explain the effectiveness of ICIs in TNBC cases as neoadjuvant and adjuvant therapies.

Biomarkers assume advantage to immunotherapy in TNBC are required to sort out the cases with more advantage of ICIs monotherapy, progress blended treatments that overwhelmed the resistance of ICI. Individual with two authenticated biomarkers presently occur, mismatch repair deficiency and manifestation of PD-L1 on immune cells. Nonetheless, mismatch repair deficiency ensues hardly among carcinoma breast and usually among initial stage presentation, those with diagnosed as metastatic TNBC with PD-L1 -ve presently accepted SP-142 assay.

#### *3.5.2 Management of metastatic TNBC by immunotherapy*

The II KEYNOTE-086 Cohort A, had appraised Pembrolizumab (inhibitor of PD-1) as it was single arm research, among diagnosed cases of triple negative metastatic breast carcinoma. They had assessed pembrolizumab effectiveness among 170 patients who were kept in this research trial, irrespective of expression of PD-L1. 62% patients enrolled in study had expression of PD-L1 + ve cancers (*n* = 105).

The response rate 4.7%, seems to be not significant, only one case achieving a complete response and 7 cases with limited response. The overall survival was 8.9 months among all the participants and 8.3 vs. 10 months in the PD-L1 + ve and -ve cohorts separately.

Cohort B of KEYNOTE-086 appraised pembrolizumab as the first line treatment of patients diagnosed by PD-L1 + ve triple negative breast carcinoma. Around 84 participants included in the study, out of that 73 (87%), experienced traditional neoadjuvant or adjuvant chemotherapeutic medications. ORR were 23.1%, three patients achieving a CR and 16 had PR. 12 participants, presently were at data limit. Median PFS 2.1 months and median OS 16.1 months.

Pembrolizumab evaluated by phase III KEYNOTE-119 (NCT02555657) trial. 622 participant diagnosed as TNBC, randomized 1:1 to have pembrolizumab compared with monotherapy chemotherapy (capecitabine, eribulin, gemcitabine, or vinorelbine) as second- or third-line therapy. But the results are pending and expected to be presented at an future meeting [14].

Impassion130 (NCT02425891), phase III randomized research trial assessing nab-paclitaxel with PD-L1 inhibitor (atezolizumab) vs. nab-paclitaxel with placebo among diagnosed participants as first line management for metastatic or inoperable locally advanced triple –ve breast carcinoma. Neoadjuvant or adjuvant treatment may be permissible if more than 1 year from end of therapy. Participants with PD-L1 + ve when >1% staining is present within immune cells. Co-primary endpoints were PFS and OS in ITT and PD-L1+ participants [14].
