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胶原蛋白的吞噬作用及细胞内消化,其在周转和重塑中的作用。

Phagocytosis and intracellular digestion of collagen, its role in turnover and remodelling.

作者信息

Everts V, van der Zee E, Creemers L, Beertsen W

机构信息

Department of Periodontology, Academic Centre for Dentistry Amsterdam (ACTA), The Netherlands.

出版信息

Histochem J. 1996 Apr;28(4):229-45. doi: 10.1007/BF02409011.

DOI:10.1007/BF02409011
PMID:8762055
Abstract

Collagens of most connective tissues are subject to continuous remodelling and turnover, a phenomenon which occurs under both physiological and pathological conditions. Degradation of these proteins involves participation of a variety of proteolytic enzymes including members of the following proteinase classes: matrix metalloproteinases (e.g. collagenase, gelatinase and stromelysin), cysteine proteinases (e.g. cathepsin B and L) and serine proteinases (e.g. plasmin and plasminogen activator). Convincing evidence is available indicating a pivotal role for matrix metalloproteinases, in particular collagenase, in the degradation of collagen under conditions of rapid remodelling, e.g. inflammation and involution of the uterus. Under steady state conditions, such as during turnover of soft connective tissues, involvement of collagenase has yet to be demonstrated. Under these circumstances collagen degradation is likely to take place particularly within the lysosomal apparatus after phagocytosis of the fibrils. We propose that this process involves the following steps: (i) recognition of the fibril by membrane-bound receptors (integrins?), (ii) segregation of the fibril, (iii) partial digestion of the fibril and/or its surrounding non-collagenous proteins by matrix metalloproteinases (possibly gelatinase), and finally (iv) lysosomal digestion by cysteine proteinases, such as cathepsin B and/or L. Modulation of this pathway is carried out under the influence of growth factors and cytokines, including transforming growth factor beta and interleukin 1 alpha.

摘要

大多数结缔组织中的胶原蛋白会持续重塑和更新,这一现象在生理和病理条件下均会发生。这些蛋白质的降解涉及多种蛋白水解酶的参与,包括以下蛋白酶类别的成员:基质金属蛋白酶(如胶原酶、明胶酶和基质溶解素)、半胱氨酸蛋白酶(如组织蛋白酶B和L)和丝氨酸蛋白酶(如纤溶酶和纤溶酶原激活剂)。有确凿证据表明,在快速重塑的条件下,如炎症和子宫 involution 期间,基质金属蛋白酶,特别是胶原酶,在胶原蛋白降解中起关键作用。在稳态条件下,如在软结缔组织更新期间,胶原酶的参与尚未得到证实。在这种情况下,胶原蛋白降解可能特别是在原纤维被吞噬后在溶酶体装置内发生。我们提出这个过程涉及以下步骤:(i)膜结合受体(整合素?)识别原纤维,(ii)原纤维的分离,(iii)基质金属蛋白酶(可能是明胶酶)对原纤维和/或其周围非胶原蛋白的部分消化,最后(iv)半胱氨酸蛋白酶,如组织蛋白酶B和/或L进行溶酶体消化。该途径受生长因子和细胞因子的影响进行调节,包括转化生长因子β和白细胞介素1α。

注

文中“involution”未找到准确对应中文释义,保留英文。

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