首页> 外文期刊>Cell Proliferation >Exogenous bone marrow cells do not rescue non-irradiated mice from acute renal tubular damage caused by HgCl2, despite establishment of chimaerism and cell proliferation in bone marrow and spleen.
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Exogenous bone marrow cells do not rescue non-irradiated mice from acute renal tubular damage caused by HgCl2, despite establishment of chimaerism and cell proliferation in bone marrow and spleen.

机译:尽管在骨髓和脾脏中建立了趋化性和细胞增殖,但外源性骨髓细胞不能使非辐射小鼠免受HgCl2引起的急性肾小管损害。

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OBJECTIVE: Various studies have shown that bone marrow stem cells can rescue mice from acute renal tubular damage under a conditioning advantage (irradiation or cisplatin treatment) favouring donor cell engraftment and regeneration; however, it is not known whether bone marrow cells (BMCs) can contribute to repair of acute tubular damage in the absence of a selection pressure for the donor cells. The aim of this study was to examine this possibility. MATERIALS AND METHODS: Ten-week-old female mice were assigned into control non-irradiated animals having only vehicle treatment, HgCl(2)-treated non-irradiated mice, HgCl(2)-treated non-irradiated mice infused with male BMCs 1 day after HgCl(2), and vehicle-treated mice with male BMCs. Tritiated thymidine was given 1 h before animal killing. RESULTS: Donor BMCs could not alleviate non-irradiated mice from acute tubular damage caused by HgCl(2), deduced by no reduction in serum urea nitrogen combined with negligible cell engraftment. However, donor BMCs could home to the bone marrow and spleen and display proliferative activity. This is the first report to show that despite no preparative myeloablation of recipients, engrafted donor BMCs can synthesize DNA in the bone marrow and spleen. CONCLUSIONS: Exogenous BMCs do not rescue non-irradiated mice from acute renal tubular damage caused by HgCl(2), despite establishment of chimerism and cell proliferation in bone marrow and spleen.
机译:目的:各种研究表明,骨髓干细胞可以在有利于供体细胞植入和再生的条件调节条件下(辐射或顺铂治疗)使小鼠免受急性肾小管损害。然而,在没有供体细胞选择压力的情况下,骨髓细胞(BMC)是否能促进急性肾小管损伤的修复尚不明确。这项研究的目的是检验这种可能性。材料与方法:将十周大的雌性小鼠分为只接受媒介物处理的对照非辐照动物,HgCl(2)处理的非辐照小鼠,HgCl(2)处理的非辐照小鼠,其注入了雄性BMC 1 HgCl(2)后的第二天,以及雄性BMC的媒介物治疗小鼠。在杀死动物前1小时给予化的胸苷。结果:供体BMCs不能减轻未辐照的小鼠因HgCl(2)引起的急性肾小管损伤,这是由于血清尿素氮没有减少以及细胞移植可以忽略不计而引起的。但是,供体BMC可能归巢于骨髓和脾脏并表现出增殖活性。这是第一个表明接受者无准备性骨髓消融的报告,但植入的供体BMC可以在骨髓和脾脏中合成DNA。结论:尽管在骨髓和脾脏中建立了嵌合和细胞增殖,但外源BMC不能使非辐射小鼠免受HgCl(2)引起的急性肾小管损害。

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