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在体内经羟基脲处理后,巨噬细胞炎性蛋白-1α可提高造血脾集落形成细胞的自我更新能力。

MIP-1 alpha increases the self-renewal capacity of the hemopoietic spleen-colony-forming cells following hydroxyurea treatment in vivo.

作者信息

Lord B I

机构信息

CRC Department of Experimental Haematology, Paterson Institute for Cancer Research, Christie Hospital NHS Trust, Manchester, UK.

出版信息

Growth Factors. 1995;12(2):145-9. doi: 10.3109/08977199509028960.

Abstract

In this report, the effect of macrophage inflammatory protein (MIP-1alpha) on the self-renewal, in vivo, of haemopoietic spleen colony-forming units (CFU-S) following cytotoxic damage, has been investigated. CFU-S recovery following injection of hydroxyurea, HU (1 g/kg at 0 and 7 hers) with or without MIP-1alpha intervention was measured over the following 5 days. In addition to the initial protection conferred by MIP-1alpha, the CFU-S population recovered about 1.7 times faster than in the unprotected controls. Direct measurement of the self-renewal capacity of the CFU-S population was made at 2 days after HU + MIP-1alpha treatment by measuring the number of CFU-S/spleen colony in a secondary transplant assay. CFU-S following HU treatment alone generated 60 CFU-S/colony. Additional MIP-1alpha treatment increased this to 90 CFU-S/colony. It is concluded that MIP-1alpha modifies the generation age structure of a regenerating CFU-S population such that recovery is initiated from the more primitive cells of the population's age spectrum and that this observation should extend the range of cytotoxic agents from which MIP-1alpha can give protection.

摘要

在本报告中,研究了巨噬细胞炎性蛋白(MIP - 1α)对细胞毒性损伤后造血脾集落形成单位(CFU - S)体内自我更新的影响。在接下来的5天内,测量了注射羟基脲(HU,0小时和7小时时各1 g/kg)后,无论有无MIP - 1α干预的情况下CFU - S的恢复情况。除了MIP - 1α提供的初始保护外,CFU - S群体的恢复速度比未受保护的对照组快约1.7倍。在HU + MIP - 1α治疗后2天,通过在二次移植试验中测量每个脾脏集落中的CFU - S数量,直接测定CFU - S群体的自我更新能力。单独HU治疗后的CFU - S每个集落产生60个CFU - S。额外的MIP - 1α治疗使其增加到每个集落90个CFU - S。得出的结论是,MIP - 1α改变了再生CFU - S群体的生成年龄结构,使得恢复从该群体年龄谱中更原始的细胞开始,并且这一观察结果应扩大MIP - 1α能够提供保护的细胞毒性药物的范围。

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