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半胱氨酸酯对化学诱导肺水肿的保护作用。

Protection by cysteine esters against chemically induced pulmonary oedema.

作者信息

Lailey A F, Hill L, Lawston I W, Stanton D, Upshall D G

机构信息

Biology Division, Chemical and Biological Defence Establishment, Porton Down, Salisbury, Wiltshire, U.K.

出版信息

Biochem Pharmacol. 1991 Dec 11;42 Suppl:S47-54. doi: 10.1016/0006-2952(91)90391-h.

Abstract

Perfluoroisobutene (PFIB) is a hydrophobic reactive gas produced by the pyrolysis of polytetrafluoroethane which induces pulmonary oedema similar to that induced by phosgene when inhaled. When a lethal dose is inhaled by Porton strain rats total non-protein thiol (NPSH) and glutathione (GSH) in the lung are reduced by between 30 and 49%, respectively. If the endogenous levels of thiols in the lung are reduced by pretreatment with buthionine sulfoximine (BSO) 16 hr before exposure to PFIB, the rats become more susceptible to the effects of the gas. The effect of BSO pretreatment on toxicity was prevented by pretreatment 30 min before exposure, with 5 mmol/kg N-acetylcysteine (NAc). NAc increased the levels of cysteine (CySH) in the lung by 150% and GSH was unaffected. Similarly pretreatment with 3 mmol/kg CySH also protected against toxicity and raised CySH levels by 100%. A series of cysteine esters and cystine dimethyl ester (CDME) have been synthesised which selectively raise lung levels of CySH in the rat lungs after intraperitoneal (i.p.) injection. The methyl ester and CDME raised lung levels of CySH by 4000 and 2000%, respectively, 10 min after i.p. injection whilst GSH levels remained unchanged. Cysteine isopropyl ester raised lung levels of CySH by 10,600% but liver levels by only 1400%. All esters except the t-butyl ester (CTBE) also raised maximal plasma levels of NPSH by up to 500%; however, when NAc was injected plasma levels increased by over 1500%. Rats treated with these esters at 3 mmol/kg and with NAc at 5 mmol/kg were protected against lethal doses of PFIB in all cases except when CTBE was used. It appears that these cysteine esters may distribute preferentially into the lung, unlike NAc. The selective enhancement of pulmonary CySH levels may provide a method for the protection of lungs against inhaled reactive toxicants by increasing intracellular CySH. Levels of CySH may also be raised in epithelial lining fluid thus reducing access of gaseous toxicants to pulmonary tissue.

摘要

全氟异丁烯(PFIB)是一种由聚四氟乙烷热解产生的疏水性反应气体,吸入后会引发类似于光气所致的肺水肿。当Porton品系大鼠吸入致死剂量的PFIB时,肺中的总非蛋白硫醇(NPSH)和谷胱甘肽(GSH)分别减少30%至49%。如果在暴露于PFIB前16小时用丁硫氨酸亚砜胺(BSO)预处理使肺中硫醇的内源性水平降低,大鼠会对该气体的影响更敏感。在暴露前30分钟用5 mmol/kg N - 乙酰半胱氨酸(NAc)预处理可防止BSO预处理对毒性的影响。NAc使肺中半胱氨酸(CySH)水平提高了150%,而GSH水平未受影响。同样,用3 mmol/kg CySH预处理也能预防毒性并使CySH水平提高100%。已经合成了一系列半胱氨酸酯和胱氨酸二甲酯(CDME),腹腔注射(i.p.)后它们能选择性提高大鼠肺中CySH的水平。腹腔注射10分钟后,甲酯和CDME分别使肺中CySH水平提高了4000%和2000%,而GSH水平保持不变。半胱氨酸异丙酯使肺中CySH水平提高了10600%,但肝脏中仅提高了1400%。除叔丁酯(CTBE)外,所有酯还使NPSH的最大血浆水平提高了500%;然而,注射NAc时血浆水平提高超过1500%。在所有情况下,除了使用CTBE时,用3 mmol/kg这些酯和5 mmol/kg NAc处理的大鼠都能免受致死剂量PFIB的影响。与NAc不同,这些半胱氨酸酯似乎可能优先分布到肺中。通过增加细胞内CySH选择性提高肺中CySH水平可能为保护肺免受吸入性反应性毒物侵害提供一种方法。上皮衬液中的CySH水平也可能升高,从而减少气态毒物进入肺组织。

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