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结缔组织激活。XXV. 人滑膜细胞中蛋白聚糖合成的调节。

Connective tissue activation. XXV. Regulation of proteoglycan synthesis in human synovial cells.

作者信息

Castor C W, Roberts D J, Hossler P A, Bignall M C

出版信息

Arthritis Rheum. 1983 Apr;26(4):522-7. doi: 10.1002/art.1780260411.

Abstract

In this study, virtually all sulfated glycosaminoglycan (GAG) synthesized and secreted by human synovial cells, both normal and rheumatoid, was detected in the form of proteoglycans of monomeric size. Enzyme hydrolysis studies that were performed demonstrated dermatan sulfate to be the dominant GAG in the proteoglycan, with lesser amounts of chondroitin 4/6 sulfate. Exposure to beta-xyloside, used as a false "core protein," resulted in marked enhancement of GAG chain formation, suggesting that the synthesis of the sulfated carbohydrate chain itself was not rate limiting. Proteoglycan synthesis and secretion were stimulated by several types of connective tissue activating peptides (CTAP); CTAP-III stimulation of incremental core protein and glycosaminoglycan was shown to be of a similar magnitude. Since chain synthesis was not rate limiting, it is suggested that stimulated proteoglycan formation caused by the CTAP peptides may be primarily modulated through increased formation of core protein.

摘要

在本研究中,无论是正常的还是类风湿性的人滑膜细胞合成并分泌的几乎所有硫酸化糖胺聚糖(GAG),均以单体大小的蛋白聚糖形式被检测到。所进行的酶水解研究表明,硫酸皮肤素是蛋白聚糖中主要的GAG,硫酸软骨素4/6的含量较少。暴露于用作假“核心蛋白”的β-木糖苷会导致GAG链形成显著增强,这表明硫酸化碳水化合物链本身的合成不是限速步骤。几种类型的结缔组织激活肽(CTAP)刺激了蛋白聚糖的合成和分泌;CTAP-III对核心蛋白和糖胺聚糖的增量刺激显示出相似的幅度。由于链合成不是限速步骤,因此提示CTAP肽引起的刺激蛋白聚糖形成可能主要通过增加核心蛋白的形成来调节。

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