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Prostaglandin E2 regulates vertebrate haematopoietic stem cell homeostasis

机译:前列腺素E2调节脊椎动物造血干细胞稳态

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Haematopoietic stem cell (HSC) homeostasis is tightly controlled by growth factors, signalling molecules and transcription factors. Definitive HSCs derived during embryogenesis in the aorta-gonad-mesonephros region subsequently colonize fetal and adult haematopoietic organs. To identify new modulators of HSC formation and homeostasis, a panel of biologically active compounds was screened for effects on stem cell induction in the zebrafish aorta-gonad-mesonephros region. Here, we show that chemicals that enhance prostaglandin (PG) E2 synthesis increased HSC numbers, and those that block prostaglandin synthesis decreased stem cell numbers. The cyclooxygenases responsible for PGE2 synthesis were required for HSC formation. A stable derivative of PGE2 improved kidney marrow recovery following irradiation injury in the adult zebrafish. In murine embryonic stem cell differentiation assays, PGE2 caused amplification of multi-potent progenitors. Furthermore, ex vivo exposure to stabilized PGE2 enhanced spleen colony forming units at day 12 post transplant and increased the frequency of long-term repopulating HSCs present in murine bone marrow after limiting dilution competitive transplantation. The conserved role for PGE2 in the regulation of vertebrate HSC homeostasis indicates that modulation of the prostaglandin pathway may facilitate expansion of HSC number for therapeutic purposes.
机译:造血干细胞(HSC)的动态平衡受生长因子,信号分子和转录因子的严格控制。在胚胎形成过程中在主动脉-性腺-中肾区域产生的确定性造血干细胞随后定居于胎儿和成年造血器官。为了鉴定HSC形成和体内稳态的新调节剂,筛选了一组生物活性化合物对斑马鱼主动脉-性腺-中肾间质干细胞诱导干细胞的影响。在这里,我们表明增强前列腺素(PG)E2合成的化学物质增加了HSC的数量,而阻断前列腺素合成的化学物质减少了干细胞的数量。 HSC形成需要负责PGE2合成的环氧合酶。 PGE2的稳定衍生物改善了成年斑马鱼的放射损伤后的肾脏恢复。在鼠胚胎干细胞分化测定中,PGE2引起多能祖细胞的扩增。此外,在有限的稀释竞争性移植后,离体暴露于稳定化的PGE2会在移植后第12天增强脾脏集落形成单位,并增加长期存在于鼠骨髓中的HSC的长期繁殖频率。 PGE 2在调节脊椎动物HSC稳态中的保守作用表明,前列腺素途径的调节可以促进出于治疗目的的HSC数目的扩展。

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