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丙烯酰胺和其他巯基化合物在体内和体外对碘化锌锇技术染色运动神经末梢的影响。

Effects of acrylamide and other sulfhydryl compounds in vivo and in vitro on staining of motor nerve terminals by the zinc iodide-osmium technique.

作者信息

Kemplay S, Cavanagh J B

出版信息

Muscle Nerve. 1984 Feb;7(2):94-100. doi: 10.1002/mus.880070203.

Abstract

The zinc iodide-osmium technique blackens motor nerve terminals by selectively staining synaptic vesicles. Intraperitoneal injections of acrylamide (30 mg/kg/day, 5 times each week) cause inhibition of staining by this technique so that approximately one third of the end-plates in rat sternocostalis muscle are unstained after 24 hours, and by 17 days more than 70% are unstained. This is not associated with nerve fiber degeneration. A similar inhibition of staining can also be shown after prior incubation of the sternocostalis muscle in 4 mM acrylamide in oxygenated Ringer's solution. Intraperitoneal injection of the thiol group blocker N-ethylmaleimide also causes marked inhibition of staining of motor end-plates by this method. Dithiothreitol, which prevents the oxidation of thiol groups, will partly prevent the inhibition of staining by both acrylamide and N-ethylmaleimide, when given in vivo.

摘要

碘化锌-锇技术通过选择性地对突触小泡染色,使运动神经末梢变黑。腹腔注射丙烯酰胺(30毫克/千克/天,每周5次)会导致该技术的染色受到抑制,以至于大鼠胸肋肌中约三分之一的终板在24小时后未被染色,到17天时超过70%未被染色。这与神经纤维变性无关。在含氧的林格氏液中用4毫摩尔丙烯酰胺预先孵育胸肋肌后,也可显示出类似的染色抑制。腹腔注射巯基阻断剂N-乙基马来酰亚胺也会导致该方法对运动终板的染色明显受到抑制。在体内给予二硫苏糖醇(可防止巯基氧化),将部分防止丙烯酰胺和N-乙基马来酰亚胺对染色的抑制。

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