Combined genetic polymorphisms of the GSTT1 and NRF2 genes increase susceptibility to cisplatin-induced ototoxicity: A preliminary study

IF 2.5 2区 医学 Q1 AUDIOLOGY & SPEECH-LANGUAGE PATHOLOGY
Taro Fujikawa , Taku Ito , Ryuhei Okada , Mitsutaka Sawada , Kaori Mohri , Yumiko Tateishi , Ryosuke Takahashi , Takahiro Asakage , Takeshi Tsutsumi
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Abstract

Objective

The genotype-phenotype relationship in cisplatin-induced ototoxicity remains unclear. By assessing early shifts in distortion product otoacoustic emission (DPOAE) levels after initial cisplatin administration, we aimed to discriminate patients’ susceptibility to cisplatin-induced ototoxicity and elucidate their genetic background.

Study Design

A prospective cross-sectional study.

Setting

Tertiary referral hospital in Japan.

Patients

Twenty-six patients with head and neck cancer were undergoing chemoradiotherapy with three cycles of 100 mg/m2 cisplatin.

Interventions

Repetitive pure-tone audiometry and DPOAE measurements, and blood sampling for DNA extraction were performed. Patients were grouped into early ototoxicity presence or absence based on whether DPOAE level shifts exceeded the corresponding reference limits of the 21-day test interval.

Main Outcome Measures

Hearing thresholds after each cisplatin cycle, severity of other adverse events, and polymorphisms in cisplatin-induced ototoxicity-associated genes were compared.

Results

Early ototoxicity was present in 14 and absent in 12 patients. Ototoxicity presence on DPOAEs was associated with greater progression of hearing loss in frequencies ≥2 kHz throughout therapy and with higher ototoxicity grades compared with ototoxicity absence. Ototoxicity was further associated with grade ≥2 nausea. Ototoxicity presence was genetically associated with the GSTT1 null genotype and G-allele of NFE2L2 rs6721961, whereas ototoxicity absence was associated with the GSTM1 null genotype. Dose-dependent progression of hearing loss was the greatest in the combined genotype pattern of GSTT1 null and the T/G or G/G variants of rs6721961.

Conclusion

Early DPOAE changes reflected genetic vulnerability to cisplatin-induced ototoxicity. Hereditary insufficiency of the antioxidant defense system causes severe cisplatin-induced hearing loss and nausea.

GSTT1 和 NRF2 基因的组合遗传多态性会增加顺铂诱发耳毒性的易感性:一项初步研究
目的 顺铂诱发耳毒性的基因型与表型关系尚不清楚。通过评估首次使用顺铂后失真产物耳声发射(DPOAE)水平的早期变化,我们旨在区分患者对顺铂诱导的耳毒性的易感性,并阐明其遗传背景。患者26名头颈部癌症患者正在接受化放疗,顺铂剂量为100 mg/m2,共三个周期。主要结果测量比较了每个顺铂周期后的听阈、其他不良事件的严重程度以及顺铂诱导的耳毒性相关基因的多态性。结果14例患者存在早期耳毒性,12例患者不存在。与无耳毒性相比,DPOAEs上出现耳毒性与整个治疗过程中听力损失频率≥2 kHz的恶化程度更大以及耳毒性等级更高有关。耳毒性还与≥2级的恶心有关。出现耳毒性与GSTT1无效基因型和NFE2L2 rs6721961的G-等位基因有关,而不出现耳毒性与GSTM1无效基因型有关。GSTT1无效基因型和rs6721961的T/G或G/G变体的组合基因型中,听力损失的剂量依赖性进展最大。抗氧化防御系统的遗传缺陷会导致严重的顺铂诱导性听力损失和恶心。
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来源期刊
Hearing Research
Hearing Research 医学-耳鼻喉科学
CiteScore
5.30
自引率
14.30%
发文量
163
审稿时长
75 days
期刊介绍: The aim of the journal is to provide a forum for papers concerned with basic peripheral and central auditory mechanisms. Emphasis is on experimental and clinical studies, but theoretical and methodological papers will also be considered. The journal publishes original research papers, review and mini- review articles, rapid communications, method/protocol and perspective articles. Papers submitted should deal with auditory anatomy, physiology, psychophysics, imaging, modeling and behavioural studies in animals and humans, as well as hearing aids and cochlear implants. Papers dealing with the vestibular system are also considered for publication. Papers on comparative aspects of hearing and on effects of drugs and environmental contaminants on hearing function will also be considered. Clinical papers will be accepted when they contribute to the understanding of normal and pathological hearing functions.
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