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线粒体和肌浆网作为神经毒性和肌毒性磷脂酶A2的模型靶点。

Mitochondria and sarcoplasmic reticulum as model targets for neurotoxic and myotoxic phospholipases A2.

作者信息

Ng R H, Howard B D

出版信息

Proc Natl Acad Sci U S A. 1980 Mar;77(3):1346-50. doi: 10.1073/pnas.77.3.1346.

Abstract

Certain neurotoxins and myotoxins from snake venoms have phospholipase A(2) activity (phosphatide 2-acylhydrolase, EC 3.1.1.4), which appears to be necessary for their toxicity. Several of these toxins inhibit the net uptake of Ca(2+) into sarcoplasmic reticulum vesicles and brain mitochondria. We have obtained evidence that the ability to inhibit this Ca(2+) uptake is a mechanistically relevant correlate of the toxicity of these proteins rather than being just a nonspecific consequence of their phospholipase A(2) activity. Two of the toxins, beta-bungarotoxin and notexin, had 5% and 50%, respectively, of the phospholipase A(2) activity of IVa phospholipase A(2)(a nontoxic enzyme), but beta-bungarotoxin was as effective as IVa in inhibiting Ca(2+) uptake into brain mitochondria and notexin was more effective. Each of the myotoxic enzymes substantially inhibited Ca(2+) uptake into sarcoplasmic reticulum, notexin being the most effective in this regard. This ability correlated better with their myotoxic potency than with their phospholipase A(2) activity. beta-Bungarotoxin lost its toxicity but not its measurable phospholipase A(2) activity after modification with ethoxyformic anhydride in the presence of dihexanoylphosphatidylcholine. The modified toxin also lost most of its ability to inhibit Ca(2+) uptake into sarcoplasmic reticulum and brain mitochondria. Sarcoplasmic reticulum vesicles reconstituted from solubilized sarcoplasmic reticulum retained their sensitivity to notexin.

摘要

某些来自蛇毒的神经毒素和肌毒素具有磷脂酶A(2)活性(磷脂2-酰基水解酶,EC 3.1.1.4),这似乎是它们毒性所必需的。其中几种毒素会抑制Ca(2+)向肌浆网囊泡和脑线粒体的净摄取。我们已经获得证据表明,抑制这种Ca(2+)摄取的能力是这些蛋白质毒性的一个与机制相关的关联因素,而不仅仅是其磷脂酶A(2)活性的非特异性结果。两种毒素,β-银环蛇毒素和诺维毒素,分别具有IVA磷脂酶A(2)(一种无毒酶)5%和50%的磷脂酶A(2)活性,但β-银环蛇毒素在抑制Ca(2+)摄取到脑线粒体方面与IVA一样有效,而诺维毒素更有效。每种肌毒性酶都能显著抑制Ca(2+)摄取到肌浆网中,诺维毒素在这方面最为有效。这种能力与其肌毒性效力的相关性比与其磷脂酶A(2)活性的相关性更好。在二己酰磷脂酰胆碱存在下用乙氧基甲酸酐修饰后,β-银环蛇毒素失去了毒性,但仍保留可测量的磷脂酶A(2)活性。修饰后的毒素也失去了大部分抑制Ca(2+)摄取到肌浆网和脑线粒体中的能力。由溶解的肌浆网重构的肌浆网囊泡对诺维毒素仍保持敏感性。

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