Pan-cancer analysis of the spectrum of homologous recombination DNA repair (HRR) pathway genes in the Indian population: A retrospective observational study
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Published:2023
Issue:4
Volume:6
Page:512-525
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ISSN:2590-3233
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Container-title:Cancer Research, Statistics, and Treatment
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language:en
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Short-container-title:
Author:
Parween Nasreen1, Gupta Trisha Dutta1, Subramanyam Paridhy Vanniya1, Tanwar Nishtha Ajit Singh1, Narayana Archana S1, Hussain Shabnam1, Fathima Nusrath1, Rangan Saranya1, Prakash Ashwini1, Jayaraman Sharanya1, Javle Vyomesh1, Gowda Pooja1, Anju K1, Varghese Linu1, Sreekanthreddy Peddagangannagari1, Nagarkar Raj2, Chithrathara G3, Vinusarathy 4, Ranade Rohit Raghunath5, Kolluru Saikrishna6, Srinivasan Sankar7, Shrestha Sudip8, Patil Tushar9, Maniar Vashisht10, Joshi Ashish10, Biswas Sutapa11, Subuddhi Ganesh Chandra11, Biswas Ghanashyam11, Thirumalairaj Raja7, Joshi Amit12, Rishi Kshitij D1, Goswami Hitesh M1, Veldore Vidya H1
Affiliation:
1. 4baseCare Onco Solutions Pvt. Ltd., Bengaluru, India 2. HCG Manavata Cancer Centre, Nashik, India 3. VPS Lakeshore Hospital, Kochi, India 4. Bangalore Baptist Hospital, Bangalore, India 5. Narayana Health, Bangalore, India 6. American Oncology Institute (Cancer Hospital) - Kanuru, Vijayawada, India 7. Apollo Hospital, Chennai, India 8. Nepal Cancer Hospital and Research Center, Lalitpur, Nepal 9. Jupiter Hospital, Pune, India 10. Mumbai Oncocare Center, Mumbai, India 11. Sparsh Hospitals and Critical Care Pvt Ltd, Bhubaneswar, India 12. Tata Memorial Hospital, Mumbai, India, India
Abstract
Background:
Homologous recombinant repair (HRR) deficit and the associated sensitivity to poly (ADP-ribose) polymerase inhibitors (PARPi) has been well studied in breast, ovarian, prostate, and pancreatic cancers, but very little is known about it in other cancer types.
Objectives:
We sought to understand the spectrum of HRR mutations in various cancer types, with the goal of identifying therapeutic targets in lesser-explored cancers.
Materials and Methods:
In this retrospective study conducted between January 2021 and December 2022, we analyzed a cohort of 659 patients with various cancer types with mutations in 15 HRR genes using next generation sequencing, at 4baseCare Onco Solutions Pvt. Ltd., Bengaluru, Karnataka, India.
Results:
We identified a total of 825 gene variants, including 366 likely pathogenic/pathogenic mutations (44.4%), with BRCA1 (196 variants; 22.8%), BRCA2 (183 variants; 21.3%), and ATM (157 variants; 18.3%) being prevalent. Germline and somatic mutations were prevalent in BRCA1 (114 variants; 60.3%) and BRCA2 (46 variants; 24%), respectively. Recurrent mutations were identified in 8 genes, including BRCA1,
BRCA2, BRIP1, BARD1, CDK12, CHEK2, PALB2 and RAD54L. BRCA1 and BRCA2 mutations were observed in breast, gynecologic, and musculoskeletal cancers; ATM and BRCA2 in gastrointestinal and biliary tract cancers, respiratory, and head-and-neck cancers; BRCA2 and CDK12 in genitourinary cancers. Additionally, co-occurring mutations (in genes such as BRCA1-BRIP1, ATM-BRCA2, ATM-BRIP1) and known therapeutically significant mutations were identified.
Conclusions:
The presence of therapeutically significant HRR mutations across a broad spectrum of cancer types in our study suggests that these mutations can possibly be targeted, especially in cancers where there is a paucity of therapeutic targets. Further, non-BRCA HRR genes, such as ATM and CDK12, could play a more prominent role than previously recognized.
Subject
Cancer Research,Oncology (nursing),Drug Guides,Oncology
Cited by
2 articles.
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1. Homologous recombinant repair gene mutations across tumors;Cancer Research, Statistics, and Treatment;2024-01 2. Authors’ reply to Weiner et al.;Cancer Research, Statistics, and Treatment;2024-01
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