Literature DB >> 30221068

Clinical implication of tumor mutational burden in patients with HER2-positive refractory metastatic breast cancer.

Song Ee Park1, Kyunghee Park2, Eunjin Lee2, Ji-Yeon Kim1, Jin Seok Ahn1, Young-Hyuck Im1, Choonghoon Lee3, Hun Jung4, Soo Youn Cho5, Woong-Yang Park2, Razvan Cristescu6, Yeon Hee Park1.   

Abstract

This study explored the clinical implications of tumor mutational burden (TMB) in a well-defined HER2-positive metastatic breast cancer (MBC) patient population who had been previously treated but had subsequent disease progression. Whole exome sequencing was performed on formalin-fixed paraffin-embedded tumor samples and matched normal tissue. Among the 46 patients, 13 (28.3%) were estrogen receptor-positive and nine (19.6%) were progesterone receptor-positive by immunohistochemistry analysis. Twenty patients (43.5%) had recurrent MBC compared with de novo MBC (n = 26, 56.5%). Sixteen patients (34.6%) demonstrated more than 100 somatic non-synonymous SNV mutations, which was predefined as a high TMB. The median follow-up duration was 57.5 months. The median overall survival (mOS) differed significantly between low and high TMB status (44.9 months vs. 85.8 months, respectively, p = 0.016). In a multivariate Cox regression analysis, TMB was the only independent prognostic factor for good metastatic overall survival after adjusting for age and recurrence (Hazard ratio [HR] = 0.32, 95% confidence interval [CI], 0.103-0.998, p = 0.049). These data suggest that high TMB may be a prognostic marker for predicting good overall survival for patients undergoing conventional HER2-directed treatments and chemotherapy. Further, future clinical trials harnessing TMB may benefit by identifying an appropriate population who may have a favorable response to immunotherapy after recurrence following HER2-directed treatments.

Entities:  

Keywords:  Human epidermal growth factor receptor 2 (HER2); Long survival outcomes; Metastatic breast cancer (MBC); Tumor mutational burden (TMB); whole exome sequencing (WES)

Year:  2018        PMID: 30221068      PMCID: PMC6136852          DOI: 10.1080/2162402X.2018.1466768

Source DB:  PubMed          Journal:  Oncoimmunology        ISSN: 2162-4011            Impact factor:   8.110


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