Case Report: Co-Existence of BRCA2 and PALB2 Germline Mutations in Familial Prostate Cancer With Solitary Lung Metastasis.

Tang Tang; Lin-Ang Wang; Peng Wang; Dali Tong; Gaolei Liu; Jun Zhang; Nan Dai; Yao Zhang; Gang Yuan; Kyla Geary; Dianzheng Zhang; Qiuli Liu; Jun Jiang

Case Report: Co-Existence of BRCA2 and PALB2 Germline Mutations in Familial Prostate Cancer With Solitary Lung Metastasis.

Tang Tang, Lin-Ang Wang, Peng Wang, Dali Tong, Gaolei Liu, Jun Zhang, Nan Dai, Yao Zhang, Gang Yuan, Kyla Geary, Dianzheng Zhang, Qiuli Liu, Jun Jiang

Department of Bio-Medical Sciences (PCOM)

Research output: Contribution to journal › Article › peer-review

Abstract

Background: Mutation-caused loss-of-function of factors involved in DNA damage response (DDR) is responsible for the development and progression of ~20% of prostate cancer (PCa). Some mutations can be used in cancer risk assessment and informed treatment decisions.

Methods: Target capture-based deep sequencing of 11 genes was conducted with total DNA purified from the proband's peripheral blood. Sanger sequencing was conducted to screen potential germline mutations in the proband's family members. Targeted sequencing of a panel of 1,021 genes was done with DNA purified from the tumor tissue.

Results: Two previously unreported germline mutations in the DDR pathway,

Conclusions: The newly identified germline mutations in DDR plays important role in PCa development. Since specific regimen worked well against this cancer, screening of DDR mutation could provide better management for patients with these mutation-mediated PCa.

Original language	American English
Journal	Frontiers in Oncology
Volume	10
State	Published - Jan 1 2020

Keywords

BRCA2
PALB2
case report
platinum-based chemotherapy
prostate cancer
radiotherapy

Disciplines

Medicine and Health Sciences
Oncology

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Case Report Co-Existence of BRCA2 and PALB2 Germline Mutations iFinal published version, 1.36 MBLicense: CC BY

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title = "Case Report: Co-Existence of BRCA2 and PALB2 Germline Mutations in Familial Prostate Cancer With Solitary Lung Metastasis.",

abstract = " Background: Mutation-caused loss-of-function of factors involved in DNA damage response (DDR) is responsible for the development and progression of ~20% of prostate cancer (PCa). Some mutations can be used in cancer risk assessment and informed treatment decisions. Methods: Target capture-based deep sequencing of 11 genes was conducted with total DNA purified from the proband's peripheral blood. Sanger sequencing was conducted to screen potential germline mutations in the proband's family members. Targeted sequencing of a panel of 1,021 genes was done with DNA purified from the tumor tissue. Results: Two previously unreported germline mutations in the DDR pathway, Conclusions: The newly identified germline mutations in DDR plays important role in PCa development. Since specific regimen worked well against this cancer, screening of DDR mutation could provide better management for patients with these mutation-mediated PCa.",

keywords = "BRCA2, PALB2, case report, platinum-based chemotherapy, prostate cancer, radiotherapy",

author = "Tang Tang and Lin-Ang Wang and Peng Wang and Dali Tong and Gaolei Liu and Jun Zhang and Nan Dai and Yao Zhang and Gang Yuan and Kyla Geary and Dianzheng Zhang and Qiuli Liu and Jun Jiang",

year = "2020",

month = jan,

day = "1",

language = "American English",

volume = "10",

journal = "Frontiers in Oncology",

}

TY - JOUR

T1 - Case Report: Co-Existence of BRCA2 and PALB2 Germline Mutations in Familial Prostate Cancer With Solitary Lung Metastasis.

AU - Tang, Tang

AU - Wang, Lin-Ang

AU - Wang, Peng

AU - Tong, Dali

AU - Liu, Gaolei

AU - Zhang, Jun

AU - Dai, Nan

AU - Zhang, Yao

AU - Yuan, Gang

AU - Geary, Kyla

AU - Zhang, Dianzheng

AU - Liu, Qiuli

AU - Jiang, Jun

PY - 2020/1/1

Y1 - 2020/1/1

N2 - Background: Mutation-caused loss-of-function of factors involved in DNA damage response (DDR) is responsible for the development and progression of ~20% of prostate cancer (PCa). Some mutations can be used in cancer risk assessment and informed treatment decisions. Methods: Target capture-based deep sequencing of 11 genes was conducted with total DNA purified from the proband's peripheral blood. Sanger sequencing was conducted to screen potential germline mutations in the proband's family members. Targeted sequencing of a panel of 1,021 genes was done with DNA purified from the tumor tissue. Results: Two previously unreported germline mutations in the DDR pathway, Conclusions: The newly identified germline mutations in DDR plays important role in PCa development. Since specific regimen worked well against this cancer, screening of DDR mutation could provide better management for patients with these mutation-mediated PCa.

AB - Background: Mutation-caused loss-of-function of factors involved in DNA damage response (DDR) is responsible for the development and progression of ~20% of prostate cancer (PCa). Some mutations can be used in cancer risk assessment and informed treatment decisions. Methods: Target capture-based deep sequencing of 11 genes was conducted with total DNA purified from the proband's peripheral blood. Sanger sequencing was conducted to screen potential germline mutations in the proband's family members. Targeted sequencing of a panel of 1,021 genes was done with DNA purified from the tumor tissue. Results: Two previously unreported germline mutations in the DDR pathway, Conclusions: The newly identified germline mutations in DDR plays important role in PCa development. Since specific regimen worked well against this cancer, screening of DDR mutation could provide better management for patients with these mutation-mediated PCa.

KW - BRCA2

KW - PALB2

KW - case report

KW - platinum-based chemotherapy

KW - prostate cancer

KW - radiotherapy

UR - https://digitalcommons.pcom.edu/scholarly_papers/2095

M3 - Article

VL - 10

JO - Frontiers in Oncology

JF - Frontiers in Oncology

ER -

Case Report: Co-Existence of BRCA2 and PALB2 Germline Mutations in Familial Prostate Cancer With Solitary Lung Metastasis.

Abstract

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