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白细胞介素6和促红细胞生成素在体内的促红细胞生成作用。

The erythropoietic effects of interleukin 6 and erythropoietin in vivo.

作者信息

Ulich T R, del Castillo J, Yin S M, Egrie J C

机构信息

Department of Pathology, University of California, Irvine School of Medicine 92717.

出版信息

Exp Hematol. 1991 Jan;19(1):29-34.

PMID:1989892
Abstract

The purpose of this investigation was to compare the erythropoietic effects of recombinant interleukin 6 (IL-6) and recombinant erythropoietin (EPO) on the marrow and peripheral blood in vivo. IL-6 administered to rats as a single i.v. injection induces a selective erythroid hyperplasia of the marrow's late normoblasts at 12 and 24 h with a return to preinjection numbers of normoblasts at 48 and 72 h. The hyperplasia of late normoblasts in the marrow is accompanied by a left-shifted peripheral reticulocytosis. Daily injection of IL-6 does not induce any effects on the erythroid population of the marrow or circulation beyond those of a single injection. After daily administration of IL-6 for 4 or 7 days, the erythroid differential in the marrow and the peripheral reticulocyte count are equal to negative control values, indicating a rapid tachyphylaxis to the erythropoietic effect of IL-6. In contrast to IL-6, EPO administered as a single i.v. injection induces a panerythroid marrow hyperplasia with sequential peak increases in pronormoblasts and early normoblasts at 24 h, intermediate normoblasts at 24-48 h, and late normoblasts at 72 h. The peripheral reticulocyte count mirrors the development of erythroid precursors in the marrow by demonstrating an increasing left-shifted reticulocytosis between 24 and 72 h. Daily injection of EPO for 7 days induces a striking erythroid hyperplasia and a myeloid hypoplasia in the marrow. In summary, IL-6 in vivo is a differentiation factor that rapidly induces tolerance to its own effect, whereas EPO in vivo affects all stages of erythropoiesis and sustains erythropoiesis indefinitely. IL-6 may be one of the non-EPO factors in pokeweed mitogen spleen cell-conditioned medium that has been reported by previous investigators to enhance erythropoiesis, although many of those factors were thought to act upon an earlier stage of erythropoiesis. IL-6 is unlikely to exert an indirect erythropoietic effect in vivo via the induction of EPO because the sera of IL-6-treated rats did not contain elevated levels of EPO and because the effects of exogenously administered IL-6 and EPO are so different.

摘要

本研究的目的是比较重组白细胞介素6(IL-6)和重组促红细胞生成素(EPO)对体内骨髓和外周血的促红细胞生成作用。以单次静脉注射方式给予大鼠IL-6后,在12小时和24小时时可诱导骨髓晚期正成红细胞选择性增生,而在48小时和72小时时正成红细胞数量恢复到注射前水平。骨髓中晚期正成红细胞的增生伴随着外周网织红细胞增多且向左移。每日注射IL-6对骨髓或循环中红细胞群体的影响不会超过单次注射的效果。在每日给予IL-6 4天或7天后,骨髓中的红细胞分化情况和外周网织红细胞计数与阴性对照值相当,表明对IL-6的促红细胞生成作用迅速产生快速耐受性。与IL-6不同,单次静脉注射EPO可诱导全红细胞系骨髓增生,原成红细胞和早期正成红细胞在24小时时依次达到峰值增加,中间正成红细胞在24至48小时时达到峰值,晚期正成红细胞在72小时时达到峰值。外周网织红细胞计数通过显示在24至72小时之间向左移的网织红细胞增多情况反映了骨髓中红细胞前体的发育过程。每日注射EPO 7天可诱导骨髓中显著的红细胞增生和髓细胞发育不全。总之,体内的IL-6是一种分化因子,可迅速诱导对其自身作用的耐受性,而体内的EPO会影响红细胞生成的所有阶段并无限期维持红细胞生成。IL-6可能是商陆丝裂原脾细胞条件培养基中的非EPO因子之一,先前的研究人员已报道该培养基可增强红细胞生成,尽管其中许多因子被认为作用于红细胞生成的较早阶段。IL-6不太可能通过诱导EPO在体内发挥间接促红细胞生成作用,因为经IL-6处理的大鼠血清中EPO水平并未升高,而且外源性给予IL-6和EPO的作用差异很大。

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