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接受抗逆转录病毒药物治疗的小鼠出现噪声性听力损失。

Noise-induced hearing loss in mice treated with antiretroviral drugs.

作者信息

Bektas Devrim, Martin Glen K, Stagner Barden B, Lonsbury-Martin Brenda L

机构信息

Department of Otorhinolaryngology, Head and Neck Surgery, Karadeniz Technical University Medical School, Trabzon, Turkey.

出版信息

Hear Res. 2008 May;239(1-2):69-78. doi: 10.1016/j.heares.2008.01.016. Epub 2008 Feb 8.

Abstract

The results reported here for CBA/CaJ mice describe the effects of regular dosing with a common antiretroviral drug combination on outer hair cell (OHC) function using measures of 2f1-f2 distortion product otoacoustic emissions (DPOAEs) and auditory brainstem responses (ABRs). Specifically, experimental mice were treated daily over a 3-mo period with the nucleoside reverse transcriptase inhibitors (NRTIs), zidovudine (ZDV) and lamivudine (3TC), dissolved in their drinking water, while their control counterparts received untreated water. DPOAE levels and ABR detection thresholds prior to and after 12 wk of NRTI treatment did not differ between experimental and control groups. To assess whether NRTI treatment potentiates the adverse effects of noise over-exposure on OHC function, both experimental and control mice were exposed 1 wk later, while still on the drug regimen, to a 10-kHz octave-band noise (OBN) at 105-dB SPL for 1h. A major outcome of the sound over-exposure episode was that the NRTI-pretreated mice showed significantly greater permanent OBN-induced reductions in DPOAE levels at 2 wk postexposure than were observed for the untreated control animals. These findings support the notion that a synergistic relationship exists between certain NRTIs and intense sounds in that such preexposure drug treatments produced greater noise-induced decreases in DPOAE activity than did noise exposure alone. This drug/noise interaction is consistent with the known harmful effects of NRTIs on cellular mitochondrial activity.

摘要

这里报告的关于CBA/CaJ小鼠的结果描述了使用2f1-f2畸变产物耳声发射(DPOAE)和听觉脑干反应(ABR)测量方法,常规给予常见抗逆转录病毒药物组合对外毛细胞(OHC)功能的影响。具体而言,实验小鼠在3个月的时间里每天饮用溶解有核苷类逆转录酶抑制剂(NRTIs)齐多夫定(ZDV)和拉米夫定(3TC)的水,而它们的对照小鼠饮用未处理的水。在接受NRTI治疗12周之前和之后,实验组和对照组的DPOAE水平和ABR检测阈值没有差异。为了评估NRTI治疗是否会增强噪声过度暴露对OHC功能的不利影响,在仍处于药物治疗方案期间,实验组和对照组小鼠在1周后都暴露于105分贝声压级的10千赫倍频程带噪声(OBN)中1小时。声音过度暴露事件的一个主要结果是,与未处理的对照动物相比,接受NRTI预处理的小鼠在暴露后2周时,DPOAE水平因OBN导致的永久性降低明显更大。这些发现支持了这样一种观点,即某些NRTIs与高强度声音之间存在协同关系,因为这种预先暴露于药物的治疗比单独的噪声暴露产生了更大的噪声诱导的DPOAE活性降低。这种药物/噪声相互作用与NRTIs对细胞线粒体活性的已知有害影响一致。

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