Germline Mutations in Cancer Predisposition Genes are Frequent in Sporadic Sarcomas

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作者
Sock Hoai Chan
Weng Khong Lim
Nur Diana Binte Ishak
Shao-Tzu Li
Wei Lin Goh
Gek San Tan
Kiat Hon Lim
Melissa Teo
Cedric Ng Chuan Young
Simeen Malik
Mann Hong Tan
Jonathan Yi Hui Teh
Francis Kuok Choon Chin
Sittampalam Kesavan
Sathiyamoorthy Selvarajan
Patrick Tan
Bin Tean Teh
Khee Chee Soo
Mohamad Farid
Richard Quek
Joanne Ngeow
机构
[1] Cancer Genetics Service,
[2] Division of Medical Oncology,undefined
[3] National Cancer Centre,undefined
[4] Centre for Computational Biology,undefined
[5] Duke-NUS Medical School,undefined
[6] Singhealth Duke-NUS Institute of Precision Medicine (PRISM),undefined
[7] Division of Medical Oncology,undefined
[8] National Cancer Centre,undefined
[9] Department of Molecular Pathology,undefined
[10] Singapore General Hospital,undefined
[11] Department of Anatomical Pathology,undefined
[12] Singapore General Hospital,undefined
[13] Division of Surgical Oncology,undefined
[14] National Cancer Centre,undefined
[15] Laboratory of Cancer Epigenome,undefined
[16] Division of Medical Sciences,undefined
[17] National Cancer Centre,undefined
[18] Cancer & Stem Cell Biology Program,undefined
[19] Duke-NUS Medical School,undefined
[20] Department of Orthopaedic Surgery,undefined
[21] Singapore General Hospital,undefined
[22] Division of Radiation Oncology,undefined
[23] National Cancer Centre,undefined
[24] Cancer Science Institute of Singapore,undefined
[25] National University Singapore,undefined
[26] Division of Molecular and Cellular Research,undefined
[27] National Cancer Centre,undefined
[28] Institute of Molecular and Cellular Biology,undefined
[29] A*STAR,undefined
[30] Oncology Academic Clinical Program,undefined
[31] Duke-NUS Medical School,undefined
[32] Lee Kong Chian School of Medicine,undefined
[33] Nanyang Technological University,undefined
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摘要
Associations of sarcoma with inherited cancer syndromes implicate genetic predisposition in sarcoma development. However, due to the apparently sporadic nature of sarcomas, little attention has been paid to the role genetic susceptibility in sporadic sarcoma. To address this, we performed targeted-genomic sequencing to investigate the prevalence of germline mutations in known cancer-associated genes within an Asian cohort of sporadic sarcoma patients younger than 50 years old. We observed 13.6% (n = 9) amongst 66 patients harbour at least one predicted pathogenic germline mutation in 10 cancer-associated genes including ATM, BRCA2, ERCC4, FANCC, FANCE, FANCI, MSH6, POLE, SDHA and TP53. The most frequently affected genes are involved in the DNA damage repair pathway, with a germline mutation prevalence of 10.6%. Our findings suggests that genetic predisposition plays a larger role than expected in our Asian cohort of sporadic sarcoma, therefore clinicians should be aware of the possibility that young sarcoma patients may be carriers of inherited mutations in cancer genes and should be considered for genetic testing, regardless of family history. The prevalence of germline mutations in DNA damage repair genes imply that therapeutic strategies exploiting the vulnerabilities resulting from impaired DNA repair may be promising areas for translational research.
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