Rizkalla G, Reiner A, Bogoch E, Poole A R
Joint Diseases Laboratory, Shriners Hospital for Crippled Children, Montreal, Quebec, Canada.
J Clin Invest. 1992 Dec;90(6):2268-77. doi: 10.1172/JCI116113.
Changes in the structure of the proteoglycan aggrecan (PG) of articular cartilage were determined immunochemically by RIA and gel chromatography and related to cartilage degeneration documented histologically by the Mankin grading system. Monoclonal antibodies to glycosaminoglycan epitopes were used. In all cartilages, three chondroitin sulfate (CS)-rich populations of large size were observed in addition to a smaller keratan sulfate (KS)-rich population. In grades 7-13 OA cartilages (phase II), molecules were significantly larger than the equivalent molecules of grades 2-6 (phase I). CS chain lengths remained unchanged. In most OA cartilages, a CS epitope 846 was elevated in content, this being most marked in phase II (mean: fivefold). Loss of uronic acid, KS, and hyaluronic acid were only pronounced in phase II OA because of variations in normal contents. Aggregation of PG was unchanged (50-60%) or reduced in OA cartilages, but molecules bearing epitope 846 exhibited almost complete aggregation in normal cartilages. This study provides evidence for the capacity of OA cartilage to synthesize new aggrecan molecules to replace those damaged and lost by disease-related changes. It also defines two phases of PG change in OA: an early predominantly degenerate phase I followed by a net reparative phase II accompanied by net loss of these molecules.
通过放射免疫分析(RIA)和凝胶色谱法对关节软骨蛋白聚糖聚集蛋白聚糖(PG)的结构变化进行了免疫化学测定,并将其与通过曼金分级系统进行组织学记录的软骨退变情况相关联。使用了针对糖胺聚糖表位的单克隆抗体。在所有软骨中,除了一个较小的富含硫酸角质素(KS)的群体外,还观察到三个较大的富含硫酸软骨素(CS)的群体。在7 - 13级骨关节炎(OA)软骨(II期)中,分子明显大于2 - 6级(I期)的相应分子。CS链长度保持不变。在大多数OA软骨中,CS表位846的含量升高,在II期最为明显(平均:五倍)。由于正常含量的变化,糖醛酸、KS和透明质酸的损失仅在II期OA中明显。PG的聚集在OA软骨中未改变(50 - 60%)或减少,但带有表位846的分子在正常软骨中表现出几乎完全聚集。本研究为OA软骨合成新的聚集蛋白聚糖分子以替代因疾病相关变化而受损和丢失的分子的能力提供了证据。它还定义了OA中PG变化的两个阶段:早期主要是退变的I期,随后是伴有这些分子净损失的净修复II期。
