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重组胰岛素样生长因子结合蛋白-4对小鼠骨形成参数的影响。

Effects of recombinant insulin-like growth factor-binding protein-4 on bone formation parameters in mice.

作者信息

Miyakoshi N, Richman C, Qin X, Baylink D J, Mohan S

机构信息

Musculoskeletal Disease Center, J. L. Pettis Veterans Administration Medical Center, Loma Linda, California 92357, USA.

出版信息

Endocrinology. 1999 Dec;140(12):5719-28. doi: 10.1210/endo.140.12.7175.

DOI:10.1210/endo.140.12.7175
PMID:10579337
Abstract

Insulin-like growth factor (IGF)-binding protein-4 (IGFBP-4), one of the most abundant IGFBPs produced by bone cells, is a potent inhibitor of IGF actions in vitro. To evaluate the modulation of IGF actions on bone formation in vivo by IGFBP-4, we produced intact and fragment (50- to 100-fold reduced IGF affinity) forms of BP-4 and examined their local and systemic effects using biochemical markers. Local administration of IGF-I over the right parietal bone significantly increased bone extract alkaline phosphatase activity; this was completely blocked by an equimolar dose of intact IGFBP-4, but not IGFBP-4 fragment. A single sc administration of IGF-I (2 microg/g BW) significantly increased bone formation markers in both serum and skeletal extracts; surprisingly, so did intact IGFBP-4, but not fragment IGFBP-4. Subcutaneous administration of an equimolar dose of IGFBP-4 along with IGF-I did not significantly block the IGF-I effect. Administration of intact IGFBP-4 significantly increased the serum 50-kDa IGF pool and decreased the 150-kDa IGF pool without significantly changing total IGF-I. We postulate that the increase in the 50-kDa IGF pool might enhance IGFs bioavailability via a mechanism involving IGFBP-4-specific protease. This study demonstrates for the first time that a single local administration of IGFBP-4 inhibits IGF-I-induced increases in bone formation, whereas systemic administration of IGFBP-4 alone increases serum levels of bone formation markers.

摘要

胰岛素样生长因子(IGF)结合蛋白-4(IGFBP-4)是骨细胞产生的最为丰富的IGF结合蛋白之一,在体外是IGF作用的有效抑制剂。为了评估IGFBP-4对体内IGF作用于骨形成的调节作用,我们制备了完整形式和片段形式(IGF亲和力降低50至100倍)的BP-4,并使用生化标志物检测了它们的局部和全身效应。在右顶骨局部给予IGF-I可显著增加骨提取物碱性磷酸酶活性;这被等摩尔剂量的完整IGFBP-4完全阻断,但未被IGFBP-4片段阻断。单次皮下注射IGF-I(2微克/克体重)可显著增加血清和骨骼提取物中的骨形成标志物;令人惊讶的是,完整的IGFBP-4也有此作用,但片段IGFBP-4则不然。皮下给予等摩尔剂量的IGFBP-4与IGF-I一起并未显著阻断IGF-I的作用。给予完整的IGFBP-4可显著增加血清50 kDa IGF池并降低150 kDa IGF池,而总IGF-I没有显著变化。我们推测50 kDa IGF池的增加可能通过涉及IGFBP-4特异性蛋白酶的机制增强IGF的生物利用度。本研究首次证明,单次局部给予IGFBP-4可抑制IGF-I诱导的骨形成增加,而单独全身给予IGFBP-4可增加血清骨形成标志物水平。

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