ID

45994

Descrizione

Principal Investigator: Arul Chinnaiyan, University of Michigan, MI, USA MeSH: Prostatic Neoplasms https://www.ncbi.nlm.nih.gov/projects/gap/cgi-bin/study.cgi?study_id=phs000915 Most prostate cancer deaths are caused by metastatic, castration resistant disease (mCRPC). To develop a precision medicine framework for mCRPC, we established a multi-institutional, international clinical sequencing infrastructure to enroll and carry out prospective whole exome and transcriptome sequencing of tumors from a cohort of mCRPC patients. We obtained high quality DNA and RNA sequence data from 150 bone or soft tissue biopsies. Central pathology revealed high-grade adenocarcinoma with only four cases (3.6%) showing neuroendocrine differentiation. Aberrations of AR, ETS genes, TP53 and PTEN were frequent (40-60% of cases), with TP53 and AR alterations being the most enriched in mCRPC compared to primary prostate cancer. We identified novel genomic alterations in PIK3CA/B (fusions and mutations); R-spondin, BRAF and RAF1 (fusions); APC (inactivating mutations); delta-catenin (missense mutations); and ZBTB16/PLZF (homozygous deletions). Aberrations of BRCA2, BRCA1 and ATM were observed at substantially higher frequencies (19.3% overall) than seen in primary prostate cancers, with 56% of these being exclusively somatic. Putative driver gene alterations were identified in nearly all patients, and over half also harbored driver gene fusions, homozygous deletions and/or amplifications. Moreover, 89% of patients harbored a clinically actionable aberration including 62.7% with aberrations in AR, 65% in other cancer-related genes, and 8% with actionable pathogenic germline alterations. Overall, integrative clinical sequencing analysis can be safely and efficiently performed in mCRPC, yields findings that may be actionable for enrolling patients in clinical trials of targeted therapies, and may inform the basis of individual clinical responses.

collegamento

dbGaP study=phs000915

Keywords

  1. 14/04/24 14/04/24 - Madita Rudolph
Titolare del copyright

Arul Chinnaiyan, University of Michigan, MI, USA

Caricato su

14 aprile 2024

DOI

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Licenza

Creative Commons BY 4.0

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dbGaP phs000915 Integrative Clinical Sequencing Analysis of Metastatic Castration Resistant Prostate Cancer Reveals a High Frequency of Clinical Actionability

Sample ID, sample type [tumor or normal tissue], and analyte type of sample obtained from participants with prostate cancer and involved in the "Stand Up To Cancer East Coast Prostate Cancer Research Group" project.

pht004947
Descrizione

pht004947

Alias
UMLS CUI [1,1]
C3846158
De-identified sample ID
Descrizione

SAMPLE_ID

Tipo di dati

string

Alias
UMLS CUI [1,1]
C4684638
UMLS CUI [1,2]
C1299222
Indicates the tumor / normal status of a sample [Normal, Tumor}
Descrizione

SAMPLE_TYPE

Tipo di dati

string

Alias
UMLS CUI [1,1]
C5237802
Molecular analyte [DNA, RNA, (DNA, RNA)]
Descrizione

ANALYTE_TYPE

Tipo di dati

string

Alias
UMLS CUI [1,1]
C1521991
UMLS CUI [1,2]
C0443354
UMLS CUI [1,3]
C0012854
UMLS CUI [1,4]
C0035668

Similar models

Sample ID, sample type [tumor or normal tissue], and analyte type of sample obtained from participants with prostate cancer and involved in the "Stand Up To Cancer East Coast Prostate Cancer Research Group" project.

Name
genere
Description | Question | Decode (Coded Value)
Tipo di dati
Alias
Item Group
pht004947
C3846158 (UMLS CUI [1,1])
SAMPLE_ID
Item
De-identified sample ID
string
C4684638 (UMLS CUI [1,1])
C1299222 (UMLS CUI [1,2])
SAMPLE_TYPE
Item
Indicates the tumor / normal status of a sample [Normal, Tumor}
string
C5237802 (UMLS CUI [1,1])
ANALYTE_TYPE
Item
Molecular analyte [DNA, RNA, (DNA, RNA)]
string
C1521991 (UMLS CUI [1,1])
C0443354 (UMLS CUI [1,2])
C0012854 (UMLS CUI [1,3])
C0035668 (UMLS CUI [1,4])

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