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Preprint Article Version 1 Preserved in Portico This version is not peer-reviewed

Uncovering Pathogenic Variants in Cancer Susceptibility Genes through Genetic Testing for Pancreatic Cancer Patients

Kevisa Potska
,
Anastasia Katseli
,
Konstantinos Agiannitopoulos
,
Christina Ntogka
,
Georgios N. Tsaousis
ORCID logo ,
Nikolaos Tsoulos
,
Adina Emilia Croitoru
ORCID logo ,
Dimitrios Ziogas
ORCID logo ,
Maria Theochari
,
Christos Christodoulou
,
Epaminondas Samantas
,
Dimitrios Janninis
,
Ilias Athanasiadis
,
Angelos Koutras
ORCID logo ,
Eirini Papadopoulou
,
Onder Kirca
,
Muharrem Okan Cakir
,
Gholam Hossein Ashrafi
ORCID logo ,
George Nasioulas
,
Mustafa Ozdogan
*
Version 1 : Received: 23 March 2024 / Approved: 25 March 2024 / Online: 25 March 2024 (09:58:18 CET)

How to cite: Potska, K.; Katseli, A.; Agiannitopoulos, K.; Ntogka, C.; Tsaousis, G. N.; Tsoulos, N.; Croitoru, A. E.; Ziogas, D.; Theochari, M.; Christodoulou, C.; Samantas, E.; Janninis, D.; Athanasiadis, I.; Koutras, A.; Papadopoulou, E.; Kirca, O.; Cakir, M. O.; Ashrafi, G. H.; Nasioulas, G.; Ozdogan, M. Uncovering Pathogenic Variants in Cancer Susceptibility Genes through Genetic Testing for Pancreatic Cancer Patients. Preprints 2024, 2024031473. https://doi.org/10.20944/preprints202403.1473.v1 Potska, K.; Katseli, A.; Agiannitopoulos, K.; Ntogka, C.; Tsaousis, G. N.; Tsoulos, N.; Croitoru, A. E.; Ziogas, D.; Theochari, M.; Christodoulou, C.; Samantas, E.; Janninis, D.; Athanasiadis, I.; Koutras, A.; Papadopoulou, E.; Kirca, O.; Cakir, M. O.; Ashrafi, G. H.; Nasioulas, G.; Ozdogan, M. Uncovering Pathogenic Variants in Cancer Susceptibility Genes through Genetic Testing for Pancreatic Cancer Patients. Preprints 2024, 2024031473. https://doi.org/10.20944/preprints202403.1473.v1

Abstract

Pancreatic cancer stands out as one of the most lethal forms of malignancies, representing 2% of all cancer cases and contributing to 5% of cancer-related fatalities. Therefore, early detection of pancreatic cancer is crucial for enhancing treatment outcomes. Various hereditary cancer syndromes have been linked to an elevated risk of developing pancreatic cancer, suggesting potential benefits from surveillance strategies for individuals at risk. Presently, precision medicine employs PARP inhibitor therapy for pancreatic cancer patients carrying germline variants in Homologous Recombination Repair (HRR) genes. Our objective was to ascertain the occurrence of germline pathogenic/likely pathogenic variants in genes predisposing to cancer among pancreatic cancer patients. Methodologically, we analyzed 184 pancreatic cancer patients referred to our laboratory for genetic examination. Utilizing a Next-Generation Sequencing (NGS) approach, we scrutinized 52 genes implicated in hereditary cancer predisposition. Our findings revealed that 21% of the patients analyzed harbored germline pathogenic/likely pathogenic variants. Within this subset, 48% exhibited positive results in pancreatic cancer susceptibility genes, namely ATM (17%), BRCA1 (12%), BRCA2 (7%), CDKN2A (7%), and PALB2. Significantly, 64.3% of the pathogenic variants were associated with genes involved in the HRR pathway (ATM, BRCA1, BRCA2, BRIP1, CHEK2, FANCL, MRE11, PALB2, RAD50, RAD51B and RAD51C). In conclusion, our study underscores the significance of multigene genetic testing for pancreatic cancer patients, with 21% of individuals yielding findings linked to pancreatic or other cancer predisposition. Moreover, patients carried pathogenic/likely pathogenic variants in HRR genes, potentially benefiting from targeted therapies such as PARP inhibitors or platinum-based treatments.

Keywords

Hereditary; Pancreatic cancer; Next Generation Sequencing (NGS)

Subject

Medicine and Pharmacology, Oncology and Oncogenics

Copyright: This is an open access article distributed under the Creative Commons Attribution License which permits unrestricted use, distribution, and reproduction in any medium, provided the original work is properly cited.

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