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骨关节炎软骨中组织蛋白酶D的组织学评估

Histologic assessment of cathepsin D in osteoarthritic cartilage.

作者信息

Vittorio N, Crissman J D, Hopson C N, Herman J H

出版信息

Clin Exp Rheumatol. 1986 Jul-Sep;4(3):221-30.

PMID:3769240
Abstract

The lysosomal endopeptidase cathepsin D is the most abundant proteinase in chondrocytes. Its significance in the pathogenesis of cartilage matrix proteoglycan (PG) degradation in osteoarthritis (OA) is unclear. The extracellular localization of cathepsin D and its potential spatial relationship to areas of PG depletion has been studied in human femoral head OA cartilage. Enzyme was identified by indirect immunofluorescence using rabbit antisera developed against a highly purified cathepsin D preparation. PG distribution was assessed in parallel sections by safranin O staining. Specimens were selected to include regions of cartilage having minimal structural and cellular alterations, severe reduction in thickness, hypocellularity, multicellular chondrocyte clusters and varying degrees of PG loss. Cathepsin D was identified in chondrocytes. When overlying fibrous connective tissue pannus was present, extracellular enzyme was predominantly localized to the cartilage-pannus interface. Cathepsin D could not be demonstrated extracellularly in areas of cartilage that were partially or totally devoid of PG. Chondrocytes in damaged regions, particularly in the superficial and upper transitional zones showing diffuse hypercellularity and/or "brood" clusters, contained increased enzyme staining. Results fail to support a role for cathepsin D in extracellular matrix PG degradation. The potential significance of this enzyme in the pathogenesis of OA would appear relegated to intracellular catabolism. Its intracellular increase at pathologic sites is consistent with enhanced catabolic activity in such regions.

摘要

溶酶体组织蛋白酶D是软骨细胞中含量最丰富的蛋白酶。其在骨关节炎(OA)软骨基质蛋白聚糖(PG)降解发病机制中的意义尚不清楚。本研究在人股骨头OA软骨中,对组织蛋白酶D的细胞外定位及其与PG耗竭区域的潜在空间关系进行了研究。使用针对高度纯化的组织蛋白酶D制剂制备的兔抗血清,通过间接免疫荧光鉴定该酶。通过番红O染色在平行切片中评估PG分布。选择的标本包括软骨结构和细胞改变最小、厚度严重减少、细胞减少、多细胞软骨细胞簇以及不同程度PG丢失的区域。在软骨细胞中鉴定出组织蛋白酶D。当存在覆盖的纤维结缔组织血管翳时,细胞外酶主要定位于软骨-血管翳界面。在部分或完全缺乏PG的软骨区域,未在细胞外检测到组织蛋白酶D。受损区域的软骨细胞,特别是在浅层和上过渡区表现出弥漫性细胞增多和/或“巢”状簇,其酶染色增加。结果不支持组织蛋白酶D在细胞外基质PG降解中起作用。该酶在OA发病机制中的潜在意义似乎局限于细胞内分解代谢。其在病理部位的细胞内增加与这些区域增强的分解代谢活性一致。

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