Role of genetic variation in cytochromes P450 in breast cancer prognosis and therapy response

Hlaváč, Viktor; Václavíková, Radka; Brynychová, Veronika; Ostašov, Pavel; Koževnikovová, Renata; Kopečková, Katerina; Vrána, David; Gatěk, Jiří; Souček, Pavel

dc.title	Role of genetic variation in cytochromes P450 in breast cancer prognosis and therapy response	en
dc.contributor.author	Hlaváč, Viktor
dc.contributor.author	Václavíková, Radka
dc.contributor.author	Brynychová, Veronika
dc.contributor.author	Ostašov, Pavel
dc.contributor.author	Koževnikovová, Renata
dc.contributor.author	Kopečková, Katerina
dc.contributor.author	Vrána, David
dc.contributor.author	Gatěk, Jiří
dc.contributor.author	Souček, Pavel
dc.relation.ispartof	International journal of molecular sciences
dc.identifier.issn	1661-6596 Scopus Sources, Sherpa/RoMEO, JCR
dc.identifier.issn	1422-0067 Scopus Sources, Sherpa/RoMEO, JCR
dc.date.issued	2021
utb.relation.volume	22
utb.relation.issue	6
dc.type	article
dc.language.iso	en
dc.publisher	Multidisciplinary Digital Publishing Institute (MDPI AG)
dc.identifier.doi	10.3390/ijms22062826
dc.relation.uri	https://www.mdpi.com/1422-0067/22/6/2826
dc.subject	breast cancer	en
dc.subject	cytochrome P450	en
dc.subject	therapy	en
dc.subject	response	en
dc.subject	survival	en
dc.subject	prognosis	en
dc.subject	next-generation sequencing	en
dc.description.abstract	Breast cancer is the most frequent cancer in the female population worldwide. The role of germline genetic variability in cytochromes P450 (CYP) in breast cancer prognosis and individualized therapy awaits detailed elucidation. In the present study, we used the next-generation sequencing to assess associations of germline variants in the coding and regulatory sequences of all human CYP genes with response of the patients to the neoadjuvant cytotoxic chemotherapy and disease-free survival (n = 105). A total of 22 prioritized variants associating with a response or survival in the above evaluation phase were then analyzed by allelic discrimination in the large confirmation set (n = 802). Associations of variants in CYP1B1, CYP4F12, CYP4X1, and TBXAS1 with the response to the neoadjuvant cytotoxic chemotherapy were replicated by the confirmation phase. However, just association of variant rs17102977 in CYP4X1 passed the correction for multiple testing and can be considered clinically and statistically validated. Replicated associations for variants in CYP4X1, CYP24A1, and CYP26B1 with disease-free survival of all patients or patients stratified to subgroups according to therapy type have not passed a false discovery rate test. Although statistically not confirmed by the present study, the role of CYP genes in breast cancer prognosis should not be ruled out. In conclusion, the present study brings replicated association of variant rs17102977 in CYP4X1 with the response of patients to the neoadjuvant cytotoxic chemotherapy and warrants further research of genetic variation CYPs in breast cancer.	en
utb.faculty	Faculty of Humanities
dc.identifier.uri	http://hdl.handle.net/10563/1010294
utb.identifier.obdid	43882436
utb.identifier.scopus	2-s2.0-85103862222
utb.identifier.wok	000645818700001
utb.identifier.pubmed	33802237
utb.source	j-scopus
dc.date.accessioned	2021-04-30T19:22:35Z
dc.date.available	2021-04-30T19:22:35Z
dc.description.sponsorship	Czech Medical Council [NV19-08-00113]; Czech Ministry of Education, Youth and Sports, INTER-EXCELLENCE LTA-USA grant [19032]; Charles University Research Fund [Q39]
dc.description.sponsorship	NV19-08-00113; Univerzita Karlova v Praze, UK; Ministerstvo Školství, Mládeže a Tělovýchovy, MŠMT: 19032
dc.rights	Attribution 4.0 International
dc.rights.uri	https://creativecommons.org/licenses/by/4.0/
dc.rights.access	openAccess
utb.contributor.internalauthor	Gatěk, Jiří
utb.fulltext.sponsorship	This research was funded by the Czech Medical Council, grant number NV19-08-00113 to P.S., the Czech Ministry of Education, Youth and Sports, INTER-EXCELLENCE LTA-USA grant number 19032 to R.V., and the Charles University Research Fund, project number Q39 to P.O.
utb.wos.affiliation	[Hlavac, Viktor; Vaclavikova, Radka; Brynychova, Veronika; Soucek, Pavel] Natl Inst Publ Hlth, Toxicogen Unit, Prague 10000, Czech Republic; [Hlavac, Viktor; Vaclavikova, Radka; Brynychova, Veronika; Ostasov, Pavel; Soucek, Pavel] Charles Univ Prague, Fac Med Pilsen, Biomed Ctr, Plzen 30100, Czech Republic; [Kozevnikovova, Renata] MEDICON, Dept Oncosurg, Prague 14000, Czech Republic; [Kopeckova, Katerina] Charles Univ Prague, Fac Med 2, Dept Oncol, Prague 15000, Czech Republic; [Kopeckova, Katerina] Motol Univ Hosp, Prague 15000, Czech Republic; [Vrana, David] Hosp Novy Jicin, Comprehens Canc Ctr Novy Jicin, Novy Jicin 74101, Czech Republic; [Gatek, Jiri] EUC Hosp Zlin, Dept Surg, Zlin 76302, Czech Republic; [Gatek, Jiri] Tomas Bata Univ Zlin, Zlin 76302, Czech Republic
utb.scopus.affiliation	Toxicogenomics Unit, National Institute of Public Health, Prague, 100 00, Czech Republic; Biomedical Center, Faculty of Medicine in Pilsen, Charles University, Pilsen, 301 00, Czech Republic; Department of Oncosurgery, MEDICON, Prague, 140 00, Czech Republic; Department of Oncology, Second Faculty of Medicine, Charles University and Motol University Hospital, Prague, 150 00, Czech Republic; Comprehensive Cancer Center Novy Jicin, Hospital Novy Jicin, Novy Jicin, 741 01, Czech Republic; Department of Surgery, EUC Hospital Zlin and Tomas Bata University in ZlinZlin 763 02, Czech Republic
utb.fulltext.projects	NV19-08-00113
utb.fulltext.projects	19032
utb.fulltext.projects	Q39