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Targeted DNA sequencing of high-grade serous ovarian carcinoma reveals association of TP53 mutations with platinum resistance when combined with gene expression

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Autor
Holý, PetrORCiD Profile - 0000-0002-6950-5563WoS Profile - O-2307-2018Scopus Profile - 36917339500
Hlaváč, ViktorORCiD Profile - 0000-0003-0695-0552WoS Profile - AGB-4024-2022Scopus Profile - 55620668700
Šeborová, KarolínaORCiD Profile - 0000-0002-8925-2321WoS Profile - S-2866-2017Scopus Profile - 57206729991
Šůsová, Simona
Tesařová, TerezaORCiD Profile - 0000-0002-1035-7375
Rob, LukášORCiD Profile - 0000-0003-3770-651XWoS Profile - AFQ-9215-2022Scopus Profile - 16538536400
Hruda, MartinORCiD Profile - 0000-0002-7606-5164WoS Profile - J-5202-2017Scopus Profile - 55130589200
Bouda, JiříORCiD Profile - 0000-0003-2954-9817WoS Profile - L-5553-2017Scopus Profile - 8536254700
Bartáková, AlenaScopus Profile - 57196299241
Mrhalová, MarcelaScopus Profile - 6602309568
Kopečková, KateřinaScopus Profile - 57191164590
Al Obeed Allah, Mohammad Moufaq Khatar
Špaček, Jiří
Sedláková, Iva
Souček, PavelORCiD Profile - 0000-0002-4294-6799WoS Profile - H-8018-2019Scopus Profile - 55503473000
Václavíková, Radka

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Datum vydání
2024
Publikováno v
International Journal of Cancer
Ročník / Číslo vydání
155 (1)
ISBN / ISSN
ISSN: 0020-7136
ISBN / ISSN
eISSN: 1097-0215
Metadata
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Kolekce
  • 2. lékařská fakulta
  • 3. lékařská fakulta
  • Lékařská fakulta v Plzni

Tato publikace má vydavatelskou verzi s DOI 10.1002/ijc.34908

Abstrakt
High-grade serous ovarian carcinoma (HGSC) is the most common subtype of ovarian cancer and is among the most fatal gynecological malignancies worldwide, due to late diagnosis at advanced stages and frequent therapy resistance. In 47 HGSC patients, we assessed somatic and germline genetic variability of a custom panel of 144 known or suspected HGSC-related genes by high-coverage targeted DNA sequencing to identify the genetic determinants associated with resistance to platinum-based therapy. In the germline, the most mutated genes were DNAH14 (17%), RAD51B (17%), CFTR (13%), BRCA1 (11%), and RAD51 (11%). Somatically, the most mutated gene was TP53 (98%), followed by CSMD1/2/3 (19/19/36%), and CFTR (23%). Results were compared with those from whole exome sequencing of a similar set of 35 HGSC patients. Somatic variants in TP53 were also validated using GENIE data of 1287 HGSC samples. Our approach showed increased prevalence of high impact somatic and germline mutations, especially those affecting splice sites of TP53, compared to validation datasets. Furthermore, nonsense TP53 somatic mutations were negatively associated with patient survival. Elevated TP53 transcript levels were associated with platinum resistance and presence of TP53 missense mutations, while decreased TP53 levels were found in tumors carrying mutations with predicted high impact, which was confirmed in The Cancer Genome Atlas data (n = 260). Targeted DNA sequencing of TP53 combined with transcript quantification may contribute to the concept of precision oncology of HGSC. Future studies should explore targeting the p53 pathway based on specific mutation types and co-analyze the expression and mutational profiles of other key cancer genes.
Klíčová slova
biomarkers, ovarian carcinoma, platinum resistance, TP53, treatment response
Trvalý odkaz
https://hdl.handle.net/20.500.14178/2401
Zobraz publikaci v dalších systémech
WOS:001180449400001
SCOPUS:2-s2.0-85187176229
PUBMED:38447012
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