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基质金属蛋白酶-13在软骨细胞肥大过程中被诱导产生。

MMP-13 is induced during chondrocyte hypertrophy.

作者信息

D'Angelo M, Yan Z, Nooreyazdan M, Pacifici M, Sarment D S, Billings P C, Leboy P S

机构信息

Department of Biochemistry, School of Dental Medicine, University of Pennsylvania, Philadelphia, Pennsylvania 19104, USA.

出版信息

J Cell Biochem. 2000 Apr;77(4):678-93.

Abstract

During development, mRNA for matrix metalloproteinase-13 (MMP-13) is found associated with cartilage undergoing hypertrophy, suggesting that this collagenase plays a role in cell enlargement and/or cartilage calcification. Using chondrocytes from prehypertrophic cartilage of chick embryo sternae, we have examined the relationship between MMP-13 expression and the transition to hypertrophy. When hypertrophy was induced by serum-free culture with ascorbate and bone morphogenetic protein-2 (BMP-2), MMP-13 mRNA levels paralleled those for type X collagen. Chondrocytes from the caudal, nonhypertrophying portion of chick sternae expressed neither type X collagen nor MMP-13, confirming that MMP-13 mRNA is a marker for hypertrophy. Zymography with conditioned medium yielded a proteinase band at 59 kDa, which was absent in nonhypertrophic chondrocytes. A polyclonal antibody raised against chick MMP-13 reacted with the 59-kDa protein, confirming that it is MMP-13. Although mRNA for MMP-13 peaked at days 4-5 of culture, only low levels of MMP-13 activity were present, and the activity increased gradually in parallel with later increases in MMP-2. These results suggest that MMP-13 is activated by MMP-2 during chondrocyte maturation, and that the combination of both proteinases is required to prepare cartilage matrix for subsequent calcification, before endochondral ossification.

摘要

在发育过程中,发现基质金属蛋白酶-13(MMP-13)的信使核糖核酸(mRNA)与正在经历肥大的软骨相关联,这表明这种胶原酶在细胞增大和/或软骨钙化中起作用。利用鸡胚胸骨前肥大软骨的软骨细胞,我们研究了MMP-13表达与向肥大转变之间的关系。当通过无血清培养并添加抗坏血酸和骨形态发生蛋白-2(BMP-2)诱导肥大时,MMP-13 mRNA水平与X型胶原的水平平行。来自鸡胸骨尾部非肥大部分的软骨细胞既不表达X型胶原也不表达MMP-13,证实MMP-13 mRNA是肥大的标志物。用条件培养基进行酶谱分析产生了一条59 kDa的蛋白酶带,在非肥大软骨细胞中不存在。针对鸡MMP-13产生的多克隆抗体与59 kDa的蛋白质发生反应,证实它就是MMP-13。虽然MMP-13的mRNA在培养的第4 - 5天达到峰值,但仅存在低水平的MMP-13活性,并且该活性随着MMP-2的后期增加而逐渐增加。这些结果表明,在软骨细胞成熟过程中MMP-13被MMP-2激活,并且两种蛋白酶的组合是在软骨内骨化之前为后续钙化准备软骨基质所必需的。

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