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小檗胺类似物对氨基糖苷类药物诱导的毛细胞死亡具有不同的保护作用。

Berbamine Analogs Exhibit Differential Protective Effects From Aminoglycoside-Induced Hair Cell Death.

作者信息

Hudson Alexandria M, Lockard Gavin M, Namjoshi Ojas A, Wilson Joseph W, Kindt Katie S, Blough Bruce E, Coffin Allison B

机构信息

Integrative Physiology and Neuroscience, Washington State University, Vancouver, WA, United States.

College of Arts and Sciences, Washington State University, Vancouver, WA, United States.

出版信息

Front Cell Neurosci. 2020 Jul 29;14:234. doi: 10.3389/fncel.2020.00234. eCollection 2020.

Abstract

Hearing loss is the third most common chronic health condition in the United States and largely results from damage to sensory hair cells. Major causes of hair cell damage include aging, noise exposure, and medications such as aminoglycoside antibiotics. Due to their potent antibacterial properties and low cost, aminoglycosides are often used for the treatment of gram-negative bacterial infections, surpassing expensive antibiotics with fewer harmful side effects. However, their use is coupled with permanent hearing loss in over 20% of patients requiring these life-sustaining antibiotics. There are currently no FDA-approved drugs that prevent hearing loss from aminoglycosides. A previous study by our group identified the plant alkaloid berbamine as a strong protectant of zebrafish lateral line hair cells from aminoglycoside damage. This effect is likely due to a block of the mechanotransduction channel, thereby reducing aminoglycoside entry into hair cells. The present study builds on this previous work, investigating 16 synthetic berbamine analogs to determine the core structure underlying their protective mechanisms. We demonstrate that nearly all of these berbamine analogs robustly protect lateral line hair cells from ototoxic damage, with ED values nearing 20 nM for the most potent analogs. Of the 16 analogs tested, nine strongly protected hair cells from both neomycin and gentamicin damage, while one conferred strong protection only from gentamicin. These data are consistent with prior research demonstrating that different aminoglycosides activate somewhat distinct mechanisms of damage. Regardless of the mechanism, protection required the entire berbamine scaffold. Phenolic alkylation or acylation with lipophilic groups appeared to improve protection compared to berbamine, implying that these structures may be responsible for mitigating damage. While the majority of analogs confer protection by blocking aminoglycoside uptake, 18% of our analogs also confer protection an uptake-independent mechanism; these analogs exhibited protection when delivered after aminoglycoside removal. Based on our studies, berbamine analogs represent a promising tool to further understand the pathology of aminoglycoside-induced hearing loss and can serve as lead compounds to develop otoprotective drugs.

摘要

听力损失是美国第三常见的慢性健康问题,主要是由感觉毛细胞受损所致。毛细胞损伤的主要原因包括衰老、噪声暴露以及诸如氨基糖苷类抗生素等药物。由于其强大的抗菌特性和低成本,氨基糖苷类药物常被用于治疗革兰氏阴性菌感染,其使用频率超过了副作用较小但价格昂贵的抗生素。然而,在超过20% 需要使用这些维持生命的抗生素的患者中,使用氨基糖苷类药物会导致永久性听力损失。目前尚无美国食品药品监督管理局(FDA)批准的预防氨基糖苷类药物所致听力损失的药物。我们团队之前的一项研究确定,植物生物碱小檗胺是斑马鱼侧线毛细胞免受氨基糖苷类药物损伤的强大保护剂。这种作用可能是由于其阻断了机械转导通道,从而减少了氨基糖苷类药物进入毛细胞。本研究基于之前的工作,对16种合成小檗胺类似物进行研究,以确定其保护机制背后的核心结构。我们证明,几乎所有这些小檗胺类似物都能有力地保护侧线毛细胞免受耳毒性损伤,最有效的类似物的半数有效浓度(ED)值接近20纳摩尔。在测试的16种类似物中,9种能有力地保护毛细胞免受新霉素和庆大霉素损伤,而1种仅对庆大霉素有强大的保护作用。这些数据与之前的研究一致,表明不同的氨基糖苷类药物激活的损伤机制略有不同。无论机制如何,保护作用都需要完整的小檗胺骨架。与小檗胺相比,用亲脂性基团进行酚烷基化或酰化似乎能增强保护作用,这意味着这些结构可能是减轻损伤的原因。虽然大多数类似物通过阻断氨基糖苷类药物的摄取来提供保护,但18% 的类似物还通过一种不依赖摄取的机制提供保护;这些类似物在氨基糖苷类药物去除后给药时仍表现出保护作用。基于我们的研究,小檗胺类似物是进一步了解氨基糖苷类药物所致听力损失病理的有前途的工具,并且可作为开发耳保护药物的先导化合物。

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