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关于骨胶原酶的潜在前体——前胶原酶激活的进一步研究。溶酶体组织蛋白酶B、纤溶酶和激肽释放酶的作用以及自发激活。

Further studies on the activation of procollagenase, the latent precursor of bone collagenase. Effects of lysosomal cathepsin B, plasmin and kallikrein, and spontaneous activation.

作者信息

Eeckhout Y, Vaes G

出版信息

Biochem J. 1977 Jul 15;166(1):21-31. doi: 10.1042/bj1660021.

Abstract
  1. Cathepsin B, a tissue (lysosomal) proteinase, and two humoral proteinases, plasmin and kallikrein, activate the latent collagenase ('procollagenase') which is released by mouse bone explants in culture. Other lysosomal proteinases (carboxypeptidase B, cathepsin C and D) and thrombin did not activate the procollagenase. Dialysis of the culture fluids against 3M-NaSCN at 4 degrees C and, for some culture fluids, prolonged preincubation at 25 degrees C also caused the activation of procollagenase. 2. In all these cases, activation of procollagenase involved at least two successive steps: the activation of an endogenous latent activator present in the culture fluids and the activation of procollagenase itself. 3. An assay method was developed for the endogenous activator. Human serum, bovine serum albumin, casein and cysteine inhibited the endogenous activator at concentrations that did not influence the collagenase activity. N-Ethylmaleimide and 4-hydroxy-mercuribenzoate stimulated the endogenous activator, but iodoacetate had no effect. 4. It is proposed that cathepsin B, kallikrein and plasmin may play a role in the physiological activation of latent collagenase and thus initiate degradation of collagen in vivo. This may occur whatever the molecular nature of procollagenase (zymogen or enzyme-inhibitor complex) might be.
摘要
  1. 组织(溶酶体)蛋白酶组织蛋白酶B以及两种体液蛋白酶,即纤溶酶和激肽释放酶,可激活潜在的胶原酶(“前胶原酶”),这种酶由培养的小鼠骨外植体释放。其他溶酶体蛋白酶(羧肽酶B、组织蛋白酶C和D)以及凝血酶均不能激活前胶原酶。将培养液在4℃下用3M硫氰酸钠进行透析,并且对于某些培养液,在25℃下长时间预孵育也会导致前胶原酶的激活。2. 在所有这些情况下,前胶原酶的激活至少涉及两个连续步骤:激活培养液中存在的内源性潜在激活剂以及前胶原酶本身的激活。3. 开发了一种针对内源性激活剂的检测方法。人血清、牛血清白蛋白、酪蛋白和半胱氨酸在不影响胶原酶活性的浓度下可抑制内源性激活剂。N-乙基马来酰亚胺和4-羟基汞苯甲酸刺激内源性激活剂,但碘乙酸没有作用。4. 有人提出,组织蛋白酶B、激肽释放酶和纤溶酶可能在潜在胶原酶的生理激活中起作用,从而启动体内胶原蛋白的降解。无论前胶原酶的分子性质(酶原或酶-抑制剂复合物)如何,这种情况都可能发生。

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