THOC5/FMIP，一种 mRNA 输出 TREX 复合物蛋白，对于体内造血原始细胞的存活是必需的。

THOC5/FMIP, an mRNA export TREX complex protein, is essential for hematopoietic primitive cell survival in vivo.

机构信息

Institut fuer Biochemie, OE4310, Medizinische Hochschule Hannover, Carl-Neuberg-Str, 1, D-30623 Hannover, Germany.

出版信息

BMC Biol. 2010 Jan 5;8:1. doi: 10.1186/1741-7007-8-1.

DOI:10.1186/1741-7007-8-1

PMID:20051105

原文链接:https://pmc.ncbi.nlm.nih.gov/articles/PMC2806247/

Abstract

BACKGROUND

The transcription/export complex is evolutionarily conserved from yeast to man and is required for coupled transcription elongation and nuclear export of mRNAs. FMIP(Fms interacting protein) is a member of the THO (suppressors of the transcriptional defects of hpr1delta by overexpression) complex which is a subcomplex of the transcription/export complex. THO complex (THOC) components are not essential for bulk poly (A)+ RNA export in higher eukaryotes, but for the nuclear export of subset of mRNAs, however, their exact role is still unclear.

RESULTS

To study the role of THOC5/Fms interacting protein in vivo, we generated THOC5/Fms interacting protein knockout mice. Since these mice are embryonic lethal, we then generated interferon inducible conditional THOC5/Fms interacting protein knockout mice. After three poly injections all of the mice died within 14 days. No pathological alterations, however, were observed in liver, kidney or heart. Thus we considered the hematopoietic system and found that seven days after poly injection, the number of blood cells in peripheral blood decreased drastically. Investigation of bone marrow cells showed that these became apoptotic within seven days after poly injection. Committed myeloid progenitor cells and cells with long term reconstituting potential were lost from bone marrow within four days after poly injection. Furthermore, infusion of normal bone marrow cells rescued mice from death induced by loss of THOC5/Fms interacting protein.

CONCLUSION

THOC5/Fms interacting protein is an essential element in the maintenance of hematopoiesis. Furthermore, mechanistically depletion of THOC5/Fms interacting protein causes the down-regulation of its direct interacting partner, THOC1 which may contribute to altered THO complex function and cell death.

摘要

背景

从酵母到人，转录/输出复合物在进化上是保守的，对于 mRNA 的偶联转录延伸和核输出是必需的。FMIP（Fms 相互作用蛋白）是 THO（通过过度表达抑制 hpr1delta 的转录缺陷）复合物的成员，THO 复合物是转录/输出复合物的亚基。THO 复合物（THOC）的成分对于高等真核生物的大量多聚 A+RNA 输出不是必需的，但对于一组 mRNA 的核输出是必需的，然而，它们的确切作用仍不清楚。

结果

为了研究 THOC5/Fms 相互作用蛋白在体内的作用，我们生成了 THOC5/Fms 相互作用蛋白敲除小鼠。由于这些小鼠是胚胎致死的，我们随后生成了干扰素诱导的条件性 THOC5/Fms 相互作用蛋白敲除小鼠。在三次多聚注射后，所有小鼠在 14 天内死亡。然而，在肝、肾或心脏中没有观察到任何病理改变。因此，我们考虑造血系统，并发现多聚注射后 7 天，外周血中的血细胞数量急剧减少。对骨髓细胞的研究表明，这些细胞在多聚注射后 7 天内凋亡。多聚注射后 4 天，骨髓中具有长期重建潜能的髓系祖细胞和细胞消失。此外，输注正常骨髓细胞可挽救 THOC5/Fms 相互作用蛋白缺失引起的小鼠死亡。

结论

THOC5/Fms 相互作用蛋白是维持造血的必需因素。此外，THOC5/Fms 相互作用蛋白的耗竭会导致其直接相互作用伙伴 THOC1 的下调，这可能导致 THO 复合物功能改变和细胞死亡。

https://cdn.ncbi.nlm.nih.gov/pmc/blobs/a6af/2806247/1d395bdba9d7/1741-7007-8-1-1.jpg

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THOC5/FMIP，一种 mRNA 输出 TREX 复合物蛋白，对于体内造血原始细胞的存活是必需的。

THOC5/FMIP, an mRNA export TREX complex protein, is essential for hematopoietic primitive cell survival in vivo.

机构信息

Institut fuer Biochemie, OE4310, Medizinische Hochschule Hannover, Carl-Neuberg-Str, 1, D-30623 Hannover, Germany.