Cancer Medicine (Mar 2023)

Genomic alteration profile and PD‐L1 expression among different breast cancer subtypes in Chinese population and their correlations

  • Kai Li,
  • Li Cao,
  • Cheukfai Li,
  • Jundong Wu,
  • Bo Chen,
  • Guochun Zhang,
  • Xueri Li,
  • Lingzhu Wen,
  • Minghan Jia,
  • Guangnan Wei,
  • Jiali Lin,
  • Yingzi Li,
  • Yuchen Zhang,
  • Hsiaopei Mok,
  • Chongyang Ren,
  • Yulei Wang,
  • Xiaofang Qi,
  • Lijie Guo,
  • Yue Che,
  • Ning Liao

DOI
https://doi.org/10.1002/cam4.5314
Journal volume & issue
Vol. 12, no. 5
pp. 5195 – 5208

Abstract

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Abstract Backgroud There were limitations existing in programmed cell‐death ligand 1 (PD‐L1) as predictive biomarkers for breast cancer (BC), hence exploring the correlation between PD‐L1 levels and other biomarkers in BC may become a very useful therapeutic clinical tool. Methods A total of 301 Chinese patients with different BC subtypes including 47 HR+/HER2+, 185 HR+/HER2−, 38 HR−/HER2+, and 31 triple‐negative breast cancer (TNBC) were enrolled in our study. Next‐generation sequencing based Yuansu450 gene panel was used for genomic alteration identification and PD‐L1 expression was tested using immunohistochemistry. Results The most prevalent BC‐related mutations were TP53 mutations, followed by mutations in PIK3CA, ERBB2, CDK12, and GATA3 in our Chinese cohort. We found that mutations DDR2 and MYCL were only mutated in HR−/HER2+ subtype, whereas H3‐3A and NRAS mutations were only occurred in HR−/HER2− subtype. The percentage of patients with PD‐L1‐positive expression was higher in patients with HR‐/HER2− mainly due to the percentage of PD‐L1‐high level. Mutational frequencies of TP53, MYC, FAT4, PBRM1, PREX2 were observed to have significant differences among patients with different BC subtypes based on PD‐L1 levels. Moreover, a positive correlation was observed between TMB and PD‐L1 level in HR+/HER2− subtype, and showed that the proportion of patients with high PD‐L1 expression was higher than that of patients with low PD‐L1 expression in the HR+/HER2− and HR+/HER2+ cohorts with high Ki67 expression. Conclusions The genomic alterations based on PD‐L1 and other biomarkers of different cohorts may provide more possibilities for the treatment of BC with different subtypes.

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