金属蛋白酶和TIMP在正常和病理组织中的免疫定位。

J J Reynolds, R M Hembry
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引用次数: 0

摘要

分子和生物化学研究对了解金属蛋白酶(MPs)及其天然抑制剂TIMP(金属蛋白酶组织抑制剂)做出了重大贡献,但对它们在体内组织分解中的具体作用的了解仍然很少。一个主要的问题是,很少有技术可以在吸收部位检测到少量的这些实体。解决这一问题的一种方法是制备特异性多克隆抗血清,用于体外细胞和组织的免疫定位研究。另一个是开发快速破坏矩阵的模型系统。这些技术的例子被提出并讨论与其他研究的关系。在许多情况下,已经观察到独特的合成模式,与个别MPs和生化数据的特定作用一致。活性胶原酶可定位于快速破坏的组织中的细胞外成分。因此,这两种方法在确定MPs和TIMP在正常和病理情况下的作用方面被证明是无价的。
本文章由计算机程序翻译,如有差异,请以英文原文为准。
Immunolocalization of metalloproteinases and TIMP in normal and pathological tissues.

Molecular and biochemical studies have made substantial contributions to the understanding of metalloproteinases (MPs) and their natural inhibitor TIMP (tissue inhibitor of metalloproteinases) but knowledge of their specific roles in tissue breakdown in vivo is still meagre. A major problem is that there are few techniques available that can detect small amounts of these entities at the sites of resorption. One approach to this problem is to prepare specific polyclonal antisera for use in immunolocalization studies on cells and tissues ex vivo. Another is to develop model systems of rapid matrix destruction. Examples of these techniques are presented and discussed in relation to other studies. In many situations unique patterns of synthesis have been observed, consistent with specific roles for the individual MPs and biochemical data. Active collagenase can be localized to extracellular components in tissues where rapid destruction is taking place. Thus both approaches are proving invaluable in defining the roles of MPs and TIMP in normal and pathological situations.

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