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Human interferon-inducible protein 10: expression and purification of recombinant protein demonstrate inhibition of early human hematopoietic progenitors

机译:人干扰素诱导蛋白10:重组蛋白的表达和纯化显示出对早期人类造血祖细胞的抑制作用

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摘要

Human interferon-inducible protein 10 (IP-10), a member of the family of the small secreted proteins called intercrine cytokines or chemokines, is secreted by interferon gamma-stimulated T cells, monocytes, endothelial cells, and keratinocytes. We have begun to explore the biological properties of IP-10 by cloning and overexpression in baculovirus and in bacterial protein expression systems. A 9.9-kD protein was secreted by infected insect cells, which on sodium dodecyl sulfate-polyacrilamide gel electrophoresis comigrated with keratinocyte IP-10 and with f(22-98), a bacterial recombinant fragment lacking the signal sequence but containing all other residues of IP-10. All three reacted with antibodies recognizing residues 10-98 (alpha IP-10) and 77-98 of IP-10 (alpha 22), demonstrating that it is secreted by keratinocytes and insect cells after removal of the signal sequence but without proteolysis of the COOH-terminal end. Purified rIP- 10 suppresses in vitro colony formation by early human bone marrow progenitor cells which need r-steel factor (rSLF) and rGM-CSF or rSLF and r-erythropoeitin (rEPO). The inhibition is dose dependent, is complete at concentrations > or = 50 ng/ml, is prevented by preincubation of rIP-10 with alpha IP-10, but not by alpha 22, and is seen with highly purified CD34+ cells, suggesting direct effect of rIP- 10 on the progenitors. Combination of rIP-10 and other chemokines at inactive concentrations inhibited colony formation in a synergistic manner. rIP-10 did not affect colony formation in the absence of any growth factors or in the presence of rEPO or rGM-CSF but in absence of rSLF. The effects of IP-10 may be relevant to normal marrow function and might be harnessed to protect human hematopoietic progenitors from the cytotoxic effects of chemotherapy.
机译:人干扰素诱导蛋白10(IP-10)是被称为间分泌细胞因子或趋化因子的小分泌蛋白家族的成员,由干扰素γ刺激的T细胞,单核细胞,内皮细胞和角质形成细胞分泌。我们已经开始通过杆状病毒和细菌蛋白表达系统的克隆和过度表达来探索IP-10的生物学特性。被感染的昆虫细胞分泌一种9.9 kD的蛋白质,该蛋白质在十二烷基硫酸钠-聚丙烯酰胺凝胶电泳上与角质形成细胞IP-10和f(22-98)结合使用,f(22-98)是一种细菌重组片段,缺乏信号序列,但包含所有其他残基。 IP-10。这三者均与识别IP-10残基10-98(alpha IP-10)和77-98(alpha 22)的抗体发生反应,表明去除信号序列后,它由角质形成细胞和昆虫细胞分泌,但没有蛋白水解。 COOH末端。纯化的rIP-10抑制了早期人类骨髓祖细胞的体外集落形成,这些早期人类骨髓祖细胞需要r-钢因子(rSLF)和rGM-CSF或rSLF和r-促红细胞生成素(rEPO)。抑制作用是剂量依赖性的,在浓度大于或等于50 ng / ml时完全抑制,可通过将rIP-10与alpha IP-10进行预温育来预防,而不受alpha 22的抑制,并在高度纯化的CD34 +细胞中观察到,表明具有直接作用祖细胞上的rIP-10片段。惰性浓度的rIP-10和其他趋化因子的组合以协同方式抑制菌落形成。在没有任何生长因子的情况下或在rEPO或rGM-CSF存在但rSLF不存在的情况下,rIP-10不会影响菌落形成。 IP-10的作用可能与正常的骨髓功能有关,可以用来保护人类造血祖细胞免受化学疗法的细胞毒作用。

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