正常及早期骨关节炎软骨中骨形态发生蛋白拮抗剂卵泡抑素和gremlin的免疫组化研究

The BMP antagonists follistatin and gremlin in normal and early osteoarthritic cartilage: an immunohistochemical study.

作者信息

Tardif G, Pelletier J-P, Boileau C, Martel-Pelletier J

机构信息

Osteoarthritis Research Unit, University of Montreal Hospital Centre, Notre-Dame Hospital, Montreal, Quebec, Canada.

出版信息

Osteoarthritis Cartilage. 2009 Feb;17(2):263-70. doi: 10.1016/j.joca.2008.06.022. Epub 2008 Aug 8.

DOI:10.1016/j.joca.2008.06.022

PMID:18691909

Abstract

OBJECTIVE

Bone morphogenic protein (BMP) activities are controlled in part by antagonists. In human osteoarthritic (OA) cartilage, the BMP antagonists follistatin and gremlin are increased but differentially regulated. Using the OA dog model, we determined if these BMP antagonists were produced at different stages during the disease process by comparing their in situ temporal and spatial distribution.

METHODS

Dogs were sacrificed at 4, 8, 10 and 12 weeks after surgery; normal dogs served as control. Cartilage was removed, differentiating fibrillated and non-fibrillated areas. Immunohistochemistry and morphometric analyses were performed for follistatin, gremlin, BMP-2/4 and IL-1beta. Growth factor-induced gremlin expression was assessed in dog chondrocytes.

RESULTS

Follistatin and gremlin production were very low in normal cartilage. Gremlin was significantly up-regulated in both non-fibrillated and fibrillated areas at 4 weeks, and only slightly increased with disease progression. Follistatin showed a time-dependent increased level in the non-fibrillated areas with significance reached at 8-12 weeks; in the fibrillated areas significant high levels were seen as early as 4 weeks. In the whole cartilage, follistatin and IL-1beta temporal production showed similar patterns; this was also true for gremlin and BMP-2/4, though BMP-2/4 production was already high in the normal dogs. Interestingly, data revealed that basic fibroblast growth factor (bFGF) could be another factor increasing gremlin expression early in the disease process. Comparison between superficial and deep zones revealed similar patterns for follistatin and IL-1beta in the superficial zone only; gremlin and BMP-2/4 had similar patterns in both zones.

CONCLUSION

Data show, for the first time, different spatial and temporal production of gremlin and follistatin in cartilage during OA progression. These findings may reflect different roles for each antagonist in this disease.

摘要

目的

骨形态发生蛋白（BMP）的活性部分受拮抗剂调控。在人类骨关节炎（OA）软骨中，BMP拮抗剂卵泡抑素和gremlin表达增加，但调控方式不同。利用OA犬模型，通过比较它们在疾病过程中的原位时空分布，我们确定了这些BMP拮抗剂是否在疾病进程的不同阶段产生。

方法

术后4、8、10和12周处死犬；正常犬作为对照。取出软骨，区分纤维化和未纤维化区域。对卵泡抑素、gremlin、BMP-2/4和IL-1β进行免疫组织化学和形态计量分析。在犬软骨细胞中评估生长因子诱导的gremlin表达。

结果

正常软骨中卵泡抑素和gremlin的产生量非常低。Gremlin在4周时在未纤维化和纤维化区域均显著上调，且随疾病进展仅略有增加。卵泡抑素在未纤维化区域呈时间依赖性升高，8 - 12周时达到显著水平；在纤维化区域，早在4周时就可见到显著高水平。在整个软骨中，卵泡抑素和IL-1β的时间产生模式相似；gremlin和BMP-2/4也是如此，尽管正常犬中BMP-2/4的产生量已经很高。有趣的是，数据显示碱性成纤维细胞生长因子（bFGF）可能是疾病早期增加gremlin表达的另一个因素。浅层和深层区域的比较显示，仅在浅层区域卵泡抑素和IL-1β有相似模式；gremlin和BMP-2/4在两个区域都有相似模式。