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肝素与碱性成纤维细胞生长因子对21日龄胎鼠颅骨胶原合成的相互作用

The interaction of heparin and basic fibroblast growth factor on collagen synthesis in 21-day fetal rat calvariae.

作者信息

Hurley M M, Kessler M, Gronowicz G, Raisz L G

机构信息

Department of Medicine, University of Connecticut Health Center, Farmington 06030-1850.

出版信息

Endocrinology. 1992 May;130(5):2675-82. doi: 10.1210/endo.130.5.1374012.

Abstract

We examined the interactions of the glycosaminoglycan, heparin, and recombinant human basic fibroblast growth factor (bFGF) on collagen synthesis in 21-day fetal rat calvariae. In calvariae treated for 96 h, heparin (25 micrograms/ml) and bFGF (10(-9) M) inhibited collagenase-digestible protein (CDP) labeling by 52 and 60% of control, respectively, and the combination further inhibited CDP labeling. Inhibition of CDP labeling by heparin (25 micrograms/ml) or bFGF (10(-9), 10(-8) M) was similar in the presence or absence of aphidicolin (30 microM) an inhibitor of cell replication. Heparin selectively inhibited CDP labeling in the osteoblast rich central bone but bFGF alone or in combination with heparin inhibited CDP labeling both in the periosteum and central bone. Heparin and bFGF alone decreased steady state levels of alpha 1(I)procollagen messenger RNA (mRNA) at 24 h and the combination further decreased mRNA levels. A high concentration of insulin-like growth factor-1 (IGF-1, 3 x 10(-8) M) reversed the inhibitory effect of heparin on DNA synthesis and CDP labeling. In contrast, IGF-1 could not reverse the inhibitory effects of bFGF on CDP labeling but enhanced the stimulatory effects of bFGF on thymidine incorporation into DNA. We conclude that the inhibitory effects of heparin and bFGF on CDP are independent of effects on cell replication. We further conclude that both heparin and bFGF inhibit collagen synthesis at a pretranslational site since they decreased procollagen mRNA levels in osteoblasts. However, the inhibition of collagen synthesis by heparin and bFGF appears to involve divergent pathways since exogenous IGF-1 could overcome the effect of heparin but not bFGF on collagen synthesis.

摘要

我们研究了糖胺聚糖、肝素和重组人碱性成纤维细胞生长因子(bFGF)对21日龄胎鼠颅骨胶原合成的相互作用。在处理96小时的颅骨中,肝素(25微克/毫升)和bFGF(10^(-9) M)分别使胶原酶可消化蛋白(CDP)标记抑制了对照的52%和60%,二者联合使用进一步抑制了CDP标记。在存在或不存在细胞复制抑制剂阿非科林(30微摩尔)的情况下,肝素(25微克/毫升)或bFGF(10^(-9)、10^(-8) M)对CDP标记的抑制作用相似。肝素选择性抑制富含成骨细胞的中央骨中的CDP标记,但单独的bFGF或与肝素联合使用时,在骨膜和中央骨中均抑制CDP标记。单独的肝素和bFGF在24小时时降低了α1(I)前胶原信使核糖核酸(mRNA)的稳态水平,二者联合使用进一步降低了mRNA水平。高浓度的胰岛素样生长因子-1(IGF-1,3×10^(-8) M)逆转了肝素对DNA合成和CDP标记的抑制作用。相比之下,IGF-1不能逆转bFGF对CDP标记的抑制作用,但增强了bFGF对胸苷掺入DNA的刺激作用。我们得出结论,肝素和bFGF对CDP的抑制作用与对细胞复制的影响无关。我们进一步得出结论,肝素和bFGF均在翻译前位点抑制胶原合成,因为它们降低了成骨细胞中前胶原mRNA的水平。然而,肝素和bFGF对胶原合成的抑制作用似乎涉及不同的途径,因为外源性IGF-1可以克服肝素对胶原合成的影响,但不能克服bFGF的影响。

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