软骨中间层蛋白/核苷酸焦磷酸水解酶的表达与细胞外无机焦磷酸因生长因子及衰老作用的产生情况平行。

Expression of cartilage intermediate layer protein/nucleotide pyrophosphohydrolase parallels the production of extracellular inorganic pyrophosphate in response to growth factors and with aging.

作者信息

Hirose J, Masuda I, Ryan L M

机构信息

Department of Medicine, Medical College of Wisconsin, Milwaukee 53226, USA.

出版信息

Arthritis Rheum. 2000 Dec;43(12):2703-11. doi: 10.1002/1529-0131(200012)43:12<2703::AID-ANR10>3.0.CO;2-Y.

DOI:10.1002/1529-0131(200012)43:12<2703::AID-ANR10>3.0.CO;2-Y

PMID:11145028

Abstract

OBJECTIVE

To evaluate the role of the extracellular inorganic pyrophosphate (ePPi)-generating ectoenzyme cartilage intermediate layer protein/nucleotide pyrophosphohydrolase (CILP/NTPPH) in chondrocyte PPi elaboration, we studied CILP/NTPPH expression in response to growth factors during aging.

METHODS

Porcine chondrocytes from adult (3-4-year-old) and young (2-week-old) animals were stimulated with transforming growth factor beta1 (TGFbeta1), which enhances ePPi elaboration, and/or insulin-like growth factor 1 (IGF-1), which diminishes ePPi elaboration. Measurements of ePPi, NTPPH enzyme activity, Western blot analysis, reverse transcriptase-polymerase chain reaction (RT-PCR), and Northern blot analysis were performed.

RESULTS

Elaboration of ePPi into conditioned media from adult chondrocytes was significantly increased by TGFbeta1 and significantly inhibited by IGF-1, but no significant differences were observed in young chondrocytes. The protein levels of CILP/NTPPH by Western analysis in the media from adult and young porcine chondrocytes were increased by TGFbeta1. RT-PCR and Northern analysis showed that CILP/NTPPH messenger RNA (mRNA) expression in both adult and young chondrocytes was increased by TGFbeta1 and decreased by IGF-1, but these changes were less significant in the young chondrocytes. Basal and TGFbeta1-up-regulated levels of CILP/NTPPH expression were higher in adult chondrocytes than in young chondrocytes.

CONCLUSION

These results provide evidence that CILP/NTPPH expression and ePPi elaboration are concomitantly stimulated by TGFbeta1 and down-regulated by IGF-1, especially in adult chondrocytes, implicating CILP/NTPPH as a functional participant in ePPi elaboration. Increased CILP/NTPPH mRNA expression in chondrocytes derived from aged animals compared with young animals might promote the formation of calcium pyrophosphate dihydrate crystals in aged cartilage.

摘要

目的

为了评估生成细胞外无机焦磷酸（ePPi）的外切酶软骨中间层蛋白/核苷酸焦磷酸水解酶（CILP/NTPPH）在软骨细胞PPi生成中的作用，我们研究了衰老过程中生长因子对CILP/NTPPH表达的影响。

方法

用增强ePPi生成的转化生长因子β1（TGFβ1）和减少ePPi生成的胰岛素样生长因子1（IGF-1）刺激成年（3 - 4岁）和幼年（2周龄）猪的软骨细胞。进行了ePPi、NTPPH酶活性的测定、蛋白质印迹分析、逆转录聚合酶链反应（RT-PCR）和Northern印迹分析。

结果

TGFβ1显著增加了成年软骨细胞条件培养基中ePPi的生成，IGF-1显著抑制了其生成，但幼年软骨细胞中未观察到显著差异。蛋白质印迹分析显示，TGFβ1增加了成年和幼年猪软骨细胞培养基中CILP/NTPPH的蛋白水平。RT-PCR和Northern分析表明，TGFβ1增加了成年和幼年软骨细胞中CILP/NTPPH信使核糖核酸（mRNA）的表达，IGF-1则降低了其表达，但这些变化在幼年软骨细胞中不太明显。成年软骨细胞中CILP/NTPPH表达的基础水平和TGFβ1上调水平均高于幼年软骨细胞。

结论

这些结果表明，TGFβ1可同时刺激CILP/NTPPH表达和ePPi生成，IGF-1则下调二者，尤其是在成年软骨细胞中，这表明CILP/NTPPH是ePPi生成的功能性参与者。与幼年动物来源的软骨细胞相比，老年动物来源的软骨细胞中CILP/NTPPH mRNA表达增加可能促进老年软骨中焦磷酸钙二水合物晶体的形成。