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新合成的软骨蛋白聚糖在体内获得透明质酸结合亲和力。

Acquisition of hyaluronate-binding affinity in vivo by newly synthesized cartilage proteoglycans.

作者信息

Sandy J D, O'Neill J R, Ratzlaff L C

机构信息

Department of Orthopedics, Brown University, Rhode Island Hospital, Providence 02902.

出版信息

Biochem J. 1989 Mar 15;258(3):875-80. doi: 10.1042/bj2580875.

Abstract

We have studied the hyaluronate-binding properties of aggregating cartilage proteoglycans synthesized in vivo by immature (6-week), mature (25-week) and aged (75-week) rabbits. Precursor isotope (35SO4) was given by intra-articular injection and articular cartilage was removed from rabbits after periods ranging from 1.5 h to 168 h. Proteoglycans were extracted with 4 M-guanidinium/HCl and monomers were isolated by CsCl gradient centrifugation under dissociative conditions. The percentages of both radiolabelled and total tissue monomers with a high affinity for hyaluronate [that is, capable of forming aggregates on Sepharose CL-2B in the presence of 0.8% (w/w) hyaluronate] were then determined. For all samples about 30% of the tissue monomers were high-affinity; however, less than 5% of the radiolabelled monomers were high-affinity at 1.5 h after injection, and this figure increased gradually with time in vivo. The increase was rapid in immature rabbits, such that after 24 h, about 30% of the radiolabelled monomers were high-affinity; on the other hand for mature and aged rabbits the increase was markedly slower such that 30% high-affinity was attained only after about 72 h. The results show that aggregating cartilage proteoglycans are secreted in vivo in a 'precursor' form with a low affinity for hyaluronate, and suggest that conversion of these monomers to a form with a higher binding affinity occurs with a half-time of about 12 h in immature cartilages but greater than 24 h in mature cartilages. The possible relationship of these findings to the process of proteoglycan aggregation in vivo is discussed.

摘要

我们研究了未成熟(6周龄)、成熟(25周龄)和老龄(75周龄)兔体内合成的聚集性软骨蛋白聚糖的透明质酸结合特性。通过关节内注射给予前体同位素(35SO4),在1.5小时至168小时的不同时间段后从兔身上取出关节软骨。用4M-胍盐酸盐提取蛋白聚糖,并在解离条件下通过CsCl梯度离心分离单体。然后测定对透明质酸具有高亲和力的放射性标记单体和总组织单体的百分比[即,在存在0.8%(w/w)透明质酸的情况下能够在琼脂糖CL-2B上形成聚集体]。对于所有样品,约30%的组织单体具有高亲和力;然而,注射后1.5小时时,放射性标记单体中高亲和力的不到5%,且该数值在体内随时间逐渐增加。在未成熟兔中增加迅速,以至于24小时后,约30%的放射性标记单体具有高亲和力;另一方面,对于成熟和老龄兔,增加明显较慢,以至于仅在约72小时后才达到30%的高亲和力。结果表明,聚集性软骨蛋白聚糖在体内以对透明质酸亲和力低的“前体”形式分泌,并表明这些单体向具有更高结合亲和力形式的转化在未成熟软骨中的半衰期约为12小时,而在成熟软骨中大于24小时。讨论了这些发现与体内蛋白聚糖聚集过程的可能关系。

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