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组织压缩对软骨外植体中新合成蛋白聚糖的透明质酸结合特性的影响。

Effects of tissue compression on the hyaluronate-binding properties of newly synthesized proteoglycans in cartilage explants.

作者信息

Sah R L, Grodzinsky A J, Plaas A H, Sandy J D

机构信息

Department of Electrical Engineering and Computing Science, Massachusetts Institute of Technology, Cambridge 02139.

出版信息

Biochem J. 1990 May 1;267(3):803-8. doi: 10.1042/bj2670803.

Abstract

The effects of tissue compression on the hyaluronate-binding properties of newly synthesized proteoglycans in calf cartilage explants were examined. Pulse-chase experiments showed that conversion of low-affinity monomers to the high-affinity form (that is, to a form capable of forming aggregates with 1.6% hyaluronate on Sephacryl S-1000) occurred with a t1/2 of about 5.7 h in free-swelling discs at pH 7.45. Static compression during chase (in pH 7.45 medium) slowed the conversion, as did incubation in acidic medium (without compression). Both effects were dose-dependent. For example, the t1/2 for conversion was increased to about 11 h by either (1) compression from a thickness of 1.25 mm to 0.5 mm or (2) medium acidification from pH 7.45 to 6.99. Oscillatory compression of 2% amplitude at 0.001, 0.01, or 0.1 cycles/s during chase did not, however, affect the conversion. Changes in the hyaluronate-binding affinity of [35S]proteoglycans in these experiments were accompanied by no marked change in the high percentage (approximately 80%) of monomers which could form aggregates with excess hyaluronate and link protein. Since static tissue compression would result in an increased matrix proteoglycan concentration and thereby a lower intra-tissue pH [Gray, Pizzanelli, Grodzinsky & Lee (1988) J. Orthop. Res. 6, 777-792], it seems likely that matrix pH may influence proteoglycan aggregate assembly by an effect on the hyaluronate-binding affinity of proteoglycan monomer. Such a pH mechanism might have a physiological role, promoting proteoglycan deposition in regions of low proteoglycan concentration.

摘要

研究了组织压缩对小牛软骨外植体中新合成蛋白聚糖的透明质酸结合特性的影响。脉冲追踪实验表明,在pH 7.45的自由膨胀圆片中,低亲和力单体向高亲和力形式(即能够在Sephacryl S - 1000上与1.6%透明质酸形成聚集体的形式)的转化发生的半衰期约为5.7小时。追踪过程中的静态压缩(在pH 7.45培养基中)减缓了转化,酸性培养基(无压缩)中的孵育也有同样效果。两种效应均呈剂量依赖性。例如,通过以下两种方式之一,转化的半衰期增加到约11小时:(1)从1.25毫米厚度压缩到0.5毫米,或(2)培养基从pH 7.45酸化到6.99。然而,追踪过程中0.001、0.01或0.1次/秒的2%振幅的振荡压缩并未影响转化。在这些实验中,[35S]蛋白聚糖的透明质酸结合亲和力的变化伴随着能够与过量透明质酸和连接蛋白形成聚集体的单体的高比例(约80%)没有明显变化。由于静态组织压缩会导致基质蛋白聚糖浓度增加,从而使组织内pH降低[格雷、皮扎内利、格罗津斯基和李(1988年)《矫形外科研究杂志》6,777 - 792],基质pH似乎可能通过对蛋白聚糖单体的透明质酸结合亲和力的影响来影响蛋白聚糖聚集体的组装。这样的pH机制可能具有生理作用,促进蛋白聚糖在蛋白聚糖浓度低的区域沉积。

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