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急性乙醇暴露可刺激角质形成细胞中微囊泡颗粒的生成。

Acute ethanol exposure stimulates microvesicle particle generation in keratinocytes.

机构信息

Departments of Pharmacology and Toxicology, Boonshoft School of Medicine at Wright State University, Dayton, OH, 45435, United States.

Departments of Pharmacology and Toxicology, Boonshoft School of Medicine at Wright State University, Dayton, OH, 45435, United States; Departments of Dermatology, Boonshoft School of Medicine at Wright State University, Dayton, OH, 45435, United States; The Dayton V.A. Medical Center, Dayton, OH, 45428, United States.

出版信息

Toxicol Lett. 2022 Feb 1;355:100-105. doi: 10.1016/j.toxlet.2021.11.008. Epub 2021 Nov 18.

Abstract

Ethanol has been demonstrated to exert profound effects upon cells and tissues via multiple mechanisms. One recently appreciated means by which cells can communicate with other cells is via the production and release of extracellular vesicles. Though smaller exosomes have been demonstrated to be released in response to ethanol exposure, the ability of ethanol to modulate the generation and release of larger microvesicle particles (MVP) is lesser studied. The present studies examined the ability of exogenous ethanol to generate MVP with a focus on skin cells. Acute ethanol exposure resulted in augmented MVP release in keratinocytes and in the skin and blood of mice. Unlike other stimuli such as ultraviolet B radiation or thermal burn injury, ethanol-mediated MVP release was independent of the Platelet-activating Factor receptor (PAFR). However, ethanol pretreatment was found to augment thermal burn injury-induced MVP in a PAFR-dependent manner. These studies provide a novel mechanism for ethanol-mediated effects, that could be relevant in the significant toxicity associated with thermal burn injury in the setting of alcohol intoxication.

摘要

乙醇通过多种机制对细胞和组织产生深远影响。最近人们认识到,细胞间可以通过产生和释放细胞外囊泡进行通讯。虽然已经证明较小的外泌体可以响应乙醇暴露而释放,但乙醇调节较大的微泡颗粒(MVP)生成和释放的能力研究较少。本研究探讨了外源性乙醇生成 MVP 的能力,重点是皮肤细胞。急性乙醇暴露导致角质形成细胞以及小鼠皮肤和血液中 MVP 的释放增加。与其他刺激物(如紫外线 B 辐射或热烧伤损伤)不同,乙醇介导的 MVP 释放不依赖于血小板激活因子受体(PAFR)。然而,研究发现,乙醇预处理以 PAFR 依赖的方式增强了热烧伤诱导的 MVP。这些研究为乙醇介导的效应提供了一种新的机制,这可能与酒精中毒状态下热烧伤损伤相关的显著毒性有关。

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