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全身给药后外周前庭细胞对荧光庆大霉素的摄取。

Uptake of fluorescent gentamicin by peripheral vestibular cells after systemic administration.

作者信息

Liu Jianping, Kachelmeier Allan, Dai Chunfu, Li Hongzhe, Steyger Peter S

机构信息

Oregon Hearing Research Center, Oregon Health & Science University, Portland, Oregon, United States of America; Department of Otology and Skull Base Surgery, Eye Ear Nose and Throat Hospital,Fudan University, Shanghai, China.

Oregon Hearing Research Center, Oregon Health & Science University, Portland, Oregon, United States of America.

出版信息

PLoS One. 2015 Mar 20;10(3):e0120612. doi: 10.1371/journal.pone.0120612. eCollection 2015.

Abstract

OBJECTIVE

In addition to cochleotoxicity, systemic aminoglycoside pharmacotherapy causes vestibulotoxicity resulting in imbalance and visual dysfunction. The underlying trafficking routes of systemically-administered aminoglycosides from the vasculature to the vestibular sensory hair cells are largely unknown. We investigated the trafficking of systemically-administered gentamicin into the peripheral vestibular system in C56Bl/6 mice using fluorescence-tagged gentamicin (gentamicin-Texas-Red, GTTR) imaged by scanning laser confocal microscopy to determine the cellular distribution and intensity of GTTR fluorescence in the three semicircular canal cristae, utricular, and saccular maculae at 5 time points over 4 hours.

RESULTS

Low intensity GTTR fluorescence was detected at 0.5 hours as both discrete puncta and diffuse cytoplasmic fluorescence. The intensity of cytoplasmic fluorescence peaked at 3 hours, while punctate fluorescence was plateaued after 3 hours. At 0.5 and 1 hour, higher levels of diffuse GTTR fluorescence were present in transitional cells compared to hair cells and supporting cells. Sensory hair cells typically exhibited only diffuse cytoplasmic fluorescence at all time-points up to 4 hours in this study. In contrast, non-sensory cells rapidly exhibited both intense fluorescent puncta and weaker, diffuse fluorescence throughout the cytosol. The numbers and size of fluorescent puncta in dark cells and transitional cells increased over time. There is no preferential GTTR uptake by the five peripheral vestibular organs' sensory cells. Control vestibular tissues exposed to Dulbecco's phosphate-buffered saline or hydrolyzed Texas Red had negligible fluorescence.

CONCLUSIONS

All peripheral vestibular cells rapidly take up systemically-administered GTTR, reaching peak intensity 3 hours after injection. Sensory hair cells exhibited only diffuse fluorescence, while non-sensory cells displayed both diffuse and punctate fluorescence. Transitional cells may act as a primary pathway for trafficking of systemic GTTR from the vasculature to endolymph prior to entering hair cells.

摘要

目的

除了具有耳蜗毒性外,全身应用氨基糖苷类药物进行药物治疗还会导致前庭毒性,进而引起平衡失调和视觉功能障碍。全身给药的氨基糖苷类药物从血管系统进入前庭感觉毛细胞的潜在运输途径在很大程度上尚不清楚。我们使用扫描激光共聚焦显微镜成像的荧光标记庆大霉素(庆大霉素-德克萨斯红,GTTR),研究了全身给药的庆大霉素在C56Bl/6小鼠外周前庭系统中的运输情况,以确定在4小时内的5个时间点,GTTR荧光在三个半规管嵴、椭圆囊和球囊斑中的细胞分布和强度。

结果

在0.5小时时检测到低强度的GTTR荧光,表现为离散的点状荧光和弥漫的细胞质荧光。细胞质荧光强度在3小时达到峰值,而点状荧光在3小时后趋于平稳。在0.5小时和1小时时,与毛细胞和支持细胞相比,过渡细胞中弥漫性GTTR荧光水平更高。在本研究中,直至4小时的所有时间点,感觉毛细胞通常仅表现出弥漫的细胞质荧光。相比之下,非感觉细胞在整个细胞质中迅速表现出强烈的荧光点状和较弱的弥漫性荧光。暗细胞和过渡细胞中荧光点状的数量和大小随时间增加。五个外周前庭器官的感觉细胞对GTTR没有优先摄取。暴露于杜氏磷酸盐缓冲盐水或水解德克萨斯红的对照前庭组织荧光可忽略不计。

结论

所有外周前庭细胞都迅速摄取全身给药的GTTR,注射后3小时达到峰值强度。感觉毛细胞仅表现出弥漫性荧光,而非感觉细胞则同时表现出弥漫性和点状荧光。过渡细胞可能是全身GTTR从血管系统运输到内淋巴然后进入毛细胞的主要途径。

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