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首页> 外文期刊>Journal of cellular biochemistry. >Carboxy-terminal fragment of osteogenic growth peptide regulates myeloid differentiation through RhoA.
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Carboxy-terminal fragment of osteogenic growth peptide regulates myeloid differentiation through RhoA.

机译:成骨生长肽的羧基末端片段通过RhoA调节骨髓分化。

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摘要

The carboxy-terminal fragment of osteogenic growth peptide, OGP(10-14), is a pentapeptide with bone anabolic effects and hematopoietic activity. The latter activity appears to be largely enhanced by specific growth factors. To study the direct activity of OGP(10-14) on myeloid cells, we tested the pentapeptide proliferating/differentiating effects in HL60 cell line. In this cell line, OGP(10-14) significantly inhibited cell proliferation, and enhanced myeloperoxidase (MPO) activity and nitroblue tetrazolium reducing ability. Moreover, it induced cytoskeleton remodeling and small GTP-binding protein RhoA activation. RhoA, which is known to be involved in HL60 differentiation, mediated these effects as shown by using its specific inhibitor, C3. Treatment with GM-CSF had a comparable OGP(10-14) activity on proliferation, MPO expression, and RhoA activation. Further studies on cell proliferation and RhoA activation proved enhanced activity by association of the two factors. These results strongly suggest that OGP(10-14) acts directly on HL60 cells by activating RhoA signaling although other possibilities cannot be ruled out.
机译:成骨生长肽OGP(10-14)的羧基末端片段是具有骨合成代谢作用和造血活性的五肽。后者的活性似乎被特定的生长因子大大增强。为了研究OGP(10-14)对髓样细胞的直接活性,我们测试了五肽在HL60细胞系中的增殖/分化作用。在此细胞系中,OGP(10-14)显着抑制细胞增殖,并增强了髓过氧化物酶(MPO)活性和硝基蓝四唑还原能力。此外,它诱导细胞骨架重塑和小的GTP结合蛋白RhoA激活。已知与HL60分化有关的RhoA通过使用其特异性抑制剂C3介导了这些作用。 GM-CSF治疗对增殖,MPO表达和RhoA激活具有类似的OGP(10-14)活性。关于细胞增殖和RhoA活化的进一步研究证明,通过这两个因素的结合增强了活性。这些结果强烈暗示OGP(10-14)通过激活RhoA信号传导直接作用于HL60细胞,尽管不能排除其他可能性。

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