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Protease-activated receptor (Par)1 alters bioelectric properties of distal lung epithelia without compromising barrier function.

作者信息

Moraes Theo J, Rafii Bijan, Niessen Frank, Suzuki Tomoko, Martin Raiza, Vachon Eric, Vogel Wolfgang, Ruf Wolfram, O'Brodovich Hugh, Downey Gregory P

机构信息

Department of Medicine, The University of Toronto, Toronto, Ontario, Canada.

出版信息

Exp Lung Res. 2009 Mar;35(2):136-54. doi: 10.1080/01902140802490723.

Abstract

Proteinases contribute to the pathogenesis of various lung diseases, partly through activating cell surface receptors by limited proteolytic cleavage. The authors provide evidence that in primary cultures of distal lung epithelia, basolateral protease-activated receptor 1 activation rapidly reduces transepithelial resistance but does not alter paracellular permeability to small uncharged solutes. Changes in transepithelial resistance were partially blocked by ion transport inhibitors and were completely blocked by placing cells in low chloride buffer. In vivo studies did not reveal enhanced lung permeability in response to pulmonary or intravenous administration of protease-activated receptor 1 activators. This information is relevant as strategies to inhibit protease-activated receptor 1 signaling are considered in order to preserve lung epithelial barrier function.

摘要

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