Literature DB >> 33754015

Mutational spectrum and precision oncology for biliary tract carcinoma.

Jianzhen Lin1,2,3, Yinghao Cao4, Xu Yang1,3, Guangyu Li4, Yang Shi5, Dongxu Wang1,3, Junyu Long1,3, Yang Song1,3, Jinzhu Mao1,3, Fucun Xie1,3, Yi Bai1,3, Lei Zhang1,3, Xiaobo Yang1,3, Xueshuai Wan1,3, Anqiang Wang6, Mei Guan3, Lin Zhao3, Ke Hu3, Jie Pan3, Li Huo3, Xin Lu1,3, Yilei Mao1,3, Xinting Sang1,3, Henghui Zhang7, Kai Wang8, Xiaoyue Wang4, Haitao Zhao1,3.   

Abstract

Background: The genomic spectrum of biliary tract carcinoma (BTC) has been characterized and is associated with distinct anatomic and etiologic subtypes, yet limited studies have linked genomic alterations with personalized therapies in BTC patients.
Methods: This study analyzed 803 patients with BTC:164 with gallbladder cancer, 475 with intrahepatic cholangiocarcinoma (ICC) and 164 with extrahepatic cholangiocarcinoma. We determined genomic alterations, mutational signatures related to etiology and histopathology and prognostic biomarkers. Personalized targeted therapies for patients harboring potentially actionable targets (PATs) were investigated.
Results: The median tumor mutation burden (TMB) was 1.23 Mut/Mb, with 4.1% of patients having hypermutated BTCs. Unlike the results obtained from the Western population, the most frequently altered cancer-related genes in our cohort included TP53 (53%), KRAS (26%), ARID1A (18%), LRP1B (14%) and CDKN2A (14%). Germline mutations occurred mostly in DNA damage repair genes. Notably, 35.8% of the ICCs harbored aristolochic acid related signatures and an elevated TMB. TP53 and KRAS mutations and amplified 7q31.2 were demonstrated to negatively affect patient prognosis. Moreover, 19 genes were proposed to be PATs in BTCs, with 25.4% of patients harboring these PATs. Forty-six patients received PAT-matched targeted therapies, achieving a 26.1% objective response rate; the median progression-free survival (PFS) was 5.0 months, with 56.8% of patients obtaining PFS benefits. Conclusions: Extensive genomic diversity and heterogeneity were observed among BTC patients, with contributions according to potential etiology exposures, anatomical subtypes and clinicopathological characteristics. We also demonstrated that patients with refractory BTCs who have PATs can derive considerable benefit from receiving a matched therapy, initiating further prospective clinical trials guided by molecular profiling among this aggressive cancer. © The author(s).

Entities:  

Keywords:  biliary tract cancer; genomic alterations; molecular screening; precision medicine; targeted therapy

Year:  2021        PMID: 33754015      PMCID: PMC7978308          DOI: 10.7150/thno.56539

Source DB:  PubMed          Journal:  Theranostics        ISSN: 1838-7640            Impact factor:   11.556


  54 in total

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5.  Detection of Mismatch Repair Deficiency and Microsatellite Instability in Colorectal Adenocarcinoma by Targeted Next-Generation Sequencing.

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Review 2.  Aristolochic acid-associated cancers: a public health risk in need of global action.

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4.  Toripalimab in advanced biliary tract cancer.

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6.  Comprehensive germline and somatic genomic profiles of Chinese patients with biliary tract cancer.

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