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用甘露醇来操纵血迷路屏障,以预防顺铂所致的听力损失。

Manipulating the blood labyrinth barrier with mannitol to prevent cisplatin-induced hearing loss.

机构信息

Institute of Medical Science, Faculty of Medicine, University of Toronto, Toronto, Canada; Sunnybrook Research Institute, Sunnybrook Health Sciences Centre, Toronto, Canada.

Sunnybrook Research Institute, Sunnybrook Health Sciences Centre, Toronto, Canada.

出版信息

Hear Res. 2022 Dec;426:108646. doi: 10.1016/j.heares.2022.108646. Epub 2022 Nov 6.

Abstract

Cisplatin, a chemotherapeutic medication, remains in the cochlea indefinitely, causing permanent hearing loss. Mannitol, a diuretic medication, has been shown to increase the permeability of the blood labyrinth barrier (BLB). We hypothesize that mannitol increases the permeability of the BLB and therefore increases the rate of entry and egression of cisplatin and entry of otoprotective agents. Rats treated with cisplatin (t = 0) were given mannitol at either t = 0, t = 6 or t = 0,6 h. Another group of rats were treated with cisplatin with mannitol at 0 h and NAC/STS with and without mannitol at 6 h. Concurrent mannitol (t = 0) transiently increased cisplatin entry into the inner ear and exacerbated cisplatin-induced hearing loss. Delayed mannitol (t = 6) did not significantly increase cisplatin entry into the inner ear and preserved inner ear functionality and structure. Additional-delayed mannitol (t = 0,6) showed that the 2nd dose of mannitol prevented exacerbation of cisplatin with mannitol-induced hearing loss. A combination of delayed NAC/STS with mannitol (t = 6) was better than NAC/STS (t = 6) alone at providing partial to full protection against cisplatin with mannitol-induced hearing loss. In conclusion, mannitol injections at t = 6 h reduced cisplatin ototoxicity (instead of exacerbating cisplatin ototoxicity at t = 0 h), and it enhanced the otoprotective efficacy of antioxidants. This may provide an important therapeutic strategy to prevent cisplatin-induced hearing loss, a direct implication in protection against hearing loss in cisplatin chemotherapy.

摘要

顺铂是一种化疗药物,会在耳蜗中无限期存在,导致永久性听力损失。甘露醇是一种利尿剂药物,已被证明可增加血迷路屏障 (BLB) 的通透性。我们假设甘露醇增加 BLB 的通透性,从而增加顺铂的进入和流出率以及耳保护剂的进入率。用顺铂治疗的大鼠(t=0)在 t=0、t=6 或 t=0、6 h 时给予甘露醇。另一组大鼠用顺铂(t=0)治疗,同时在 6 h 时用 NAC/STS 和甘露醇治疗,以及不用甘露醇治疗。同时给予甘露醇(t=0)短暂增加顺铂进入内耳,并加重顺铂引起的听力损失。延迟给予甘露醇(t=6)不会显著增加顺铂进入内耳,并保留内耳功能和结构。额外延迟给予甘露醇(t=0、6)表明第二剂甘露醇可预防甘露醇加重顺铂引起的听力损失。延迟给予 NAC/STS 和甘露醇(t=6)的组合在提供部分至完全保护免受顺铂和甘露醇引起的听力损失方面优于单独给予 NAC/STS(t=6)。总之,在 t=6 h 时给予甘露醇可降低顺铂耳毒性(而不是在 t=0 h 时加重顺铂耳毒性),并增强抗氧化剂的耳保护作用。这可能为预防顺铂引起的听力损失提供重要的治疗策略,这对顺铂化疗引起的听力损失保护具有直接意义。

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