Pharmacogenomic predictor of long-term residual chemotherapy-induced peripheral neuropathy in ovarian cancer survivors: A substudy of the GINECO Vivrovaire study

被引:0
|
作者
Zenatri, M. [1 ]
Perennec, T. [2 ]
Michon, C. [3 ]
Gernier, F. [4 ]
Grellard, J. -M. [4 ]
Piloquet, F. -X. [1 ]
Dubot-Poitelon, C. [5 ]
Kalbacher, E. [6 ]
Tredan, O. [7 ]
Augereau, P. [8 ]
Pautier, P. [9 ]
Fey, L. [3 ]
Joly, F. [5 ]
Frenel, J. -S [10 ,11 ]
机构
[1] Inst Cancerol Ouest, Ctr Rene Gauducheau, Dept Med Oncol, St Herblain, France
[2] Inst Cancerol Ouest, Ctr Rene Gauducheau, Radiat Oncol Dept, St Herblain, France
[3] Inst Cancerol Ouest, Ctr Paul Papin, Dept Biopathol, Angers, France
[4] Ctr Francois Baclesse, Clin Res Dept, Caen, France
[5] Unicaen Univ, Ctr Francois Baclesse, Med Oncol Dept, Caen, France
[6] CHRU Besancon Hop Jean Minjoz, Oncol Dept, Besancon, France
[7] Ctr Leon Berard, Med Oncol, Lyon, France
[8] Inst Cancerol Ouest, Ctr Paul Papin, Med Oncol Dept, Angers, France
[9] Inst Gustave Roussy, Med Dept, Villejuif, France
[10] Inst Cancerol Ouest, Ctr Rene Gauducheau, Med Oncol Dept, GINECO Grp, St Herblain, France
[11] GINEGEPS, St Herblain, France
关键词
Ovarian cancer; Long term survivors; Chemotherapy-induced peripheral neuropathy; Single nucleotide polymorphism; Pharmacogenomic; Patient-reported outcome; QUALITY-OF-LIFE; BREAST-CANCER; NEUROTOXICITY; TOXICITY; CISPLATIN; RISK;
D O I
10.1016/j.ygyno.2024.04.021
中图分类号
R73 [肿瘤学];
学科分类号
100214 ;
摘要
Background. Chemotherapy (CT) remains a backbone treatment of epithelial ovarian cancer (EOC) inducing persistent peripheral neuropathy (CIPN). Using a dedicated patient-reported outcome tool, this study investigated persistent CIPN and its pharmacogenetic predictors in a cohort of long-term EOC survivors. Methods. Vivrovaire was a French multicenter cohort of patients with EOC free of disease 3 years after CT completion. Persistent CIPN was assessed using the FACT/GOG-Ntx4 self-questionnaire. The association of homozygous (hom) or heterozygous (het) single nucleotide polymorphisms (SNPs) in selected genes was evaluated. Results. 130 patients were included with a median time from CT completion of 63 [35-180] months. The median CIPN score was 37 [18-44], with 35 (26.9%) patients reporting severe CIPN (<33). SNPs were identified as follows: CYP2C8 [hom, n = 32 (24.6%)/het, n = 99, (76.2%)]; CYP3A4 [hom, n = 0 (0%)/het, n = 8 (6.2%)], ERCC1 [hom, n = 21 (16.2%)/het, n = 57 (43.8%)], and XPC [hom, n = 45 (34.6%)/het, n = 66 (50.8%)]. In univariate analysis, the identification of >= 1 hom SNP was associated with a lower CIPN score (continuous variable; p = 0.045). Patients harboring hom or het CYP2C8_rs1934951 SNP reported more likely severe CIPN (threshold <33) score (OR 2.482; 95% CI [1.126-5.47], p = 0.024). In the multivariate analyses, age, interval from CT completion, type and number of CT courses were not significantly associated with CIPN score (OR 5.165, 95% CI [0.478-55.83], p = 0.176). Conclusions. Persistent CIPN is common among ovarian cancer long-term survivors. CYP2C8_rs1934951 SNP may be associated with severe residual CIPN in EOC survivors. More studies are warranted to identify predictive factors of CIPN.
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收藏
页码:139 / 144
页数:6
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