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Chondroadherin Fragmentation Mediated by the Protease HTRA1 Distinguishes Human Intervertebral Disc Degeneration from Normal Aging

机译:由蛋白酶HTRa1介导的软骨粘合素片段化区分人类椎间盘退变与正常老化

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摘要

Chondroadherin, a member of the leucine-rich repeat family, has previously been demonstrated to be fragmented in some juveniles with idiopathic scoliosis. This observation led us to investigate adults with disc degeneration. Immunoblotting analysis demonstrated that non-degenerate discs from three different age groups show no chondroadherin fragmentation. Furthermore, the chondroadherin fragments in adult degenerate disc and the juvenile scoliotic disc were compared via immunoblot analysis and appeared to have a similar size. We then investigated whether or not chondroadherin fragmentation increases with the severity of disc degeneration. Three different samples with different severities were chosen from the same disc, and chondroadherin fragmentation was found to be more abundant with increasing severity of degeneration. This observation led us to the creation of a neoepitope antibody to the cleavage site observed. We then observed that the cleavage site in adult degenerate discs and juvenile scoliotic discs was identical as confirmed by the neoepitope antibody. Consequently, investigation of the protease capable of cleaving chondroadherin at this site was necessary. In vitro digests of disc tissue demonstrated that ADAMTS-4 and -5; cathepsins K, B, and L; and MMP-3, -7, -12, and -13 were incapable of cleavage of chondroadherin at this site and that HTRA1 was indeed the only protease capable. Furthermore, increased protein levels of the processed form of HTRA1 were demonstrated in degenerate disc tissues via immunoblotting. The results suggest that chondroadherin fragmentation can be used as a biomarker to distinguish the processes of disc degeneration from normal aging.
机译:软骨亮氨酸是富含亮氨酸的重复序列家族的成员,以前已被证明在患有特发性脊柱侧弯的一些少年中会破碎。这一观察结果促使我们调查了成年人椎间盘退变。免疫印迹分析表明,来自三个不同年龄组的未变性椎间盘均未显示软骨粘附素碎片。此外,通过免疫印迹分析比较了成人简并椎间盘和青少年脊柱侧凸椎间盘中的软骨粘附素片段,它们的大小相似。然后,我们调查了软骨黏着蛋白碎片是否随椎间盘退变的严重性增加。从同一张光盘中选择了三个具有不同严重度的样品,随着变性程度的增加,软骨粘附素的碎裂更为丰富。该观察导致我们产生了针对观察到的切割位点的新表位抗体。然后,我们观察到,如新表位抗体所证实的那样,成人简并椎间盘和青少年脊柱侧凸盘中的切割位点是相同的。因此,需要研究能够在该位点切割软骨粘合素的蛋白酶。椎间盘组织的体外消化证明,ADAMTS-4和-5;组织蛋白酶K,B和L; MMP-3,-7,-12和-13不能在该位点切割软骨粘附素,而HTRA1确实是唯一的蛋白酶。此外,通过免疫印迹在退化的椎间盘组织中证实了加工形式的HTRA1的蛋白质水平增加。结果表明,软骨粘附素片段化可以用作区分正常年龄的椎间盘退变过程的生物标记。

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