STAT1 is involved in signal transduction in the EPOinduced HEL cells

Erythropoietin (EPO) is the ma jor regulator of mammalian erythropoisis, which stimulates the growth and differentiation of hematopoietic cells through interaction with its receptor (EPO-R). Here we use HEL cells (a human erythro-leukemia cell line) as a model to elucidate the pathway of signal transduction in the EPO-induced HEL cells. our data show that the EPOR (EPO receptor) on the surface of HEL cells interacts with the Janus tyrosine protein kinase (Jak2) to transduce intracellular signals through phosphorylation of cytoplasmic proteins in EPO-treated HEL cells. Both STAT1 and STAT5 in this cell line are tyrosine-phosphorylated and translocated to nucleus following the binding of EPO to HEL cells.Furthermore, the binding of both STAT1 and STAT5 proteins to specific DNA elements (SIE and PIE elements) is revealed in an EPO-dependent manner. Our data demonstrate that the pathway of signal transduction following the binding of EPO to HEL cells is similar to immature erythroid cell from the spleen of mice infected with anemia strain of Friend virus.

促红细胞生成素对新生大鼠缺氧缺血性脑损伤的保护作用

目的:探讨外源性促红细胞生成素(EPO)对新生大鼠缺氧缺血性脑损伤后脑功能的改善作用。方法:将45只7日龄SD大鼠随机分成假手术对照组、EPO治疗组、缺氧缺血组(各组n=15),假手术组仅分离颈总动脉,不予缺氧缺血,EPO治疗组在造缺氧缺血性脑损伤(HIBD)模型后立即按质量分数5 000 IU/kg腹腔注射EPO1次,缺氧缺血组仅予生理盐水。通过组织学切片检查,脑干听觉诱发电位(BAEP)检查,判断各组脑功能差异,观察EPO的疗效。结果:相比假手术对照组大鼠,HIBD组大鼠脑组织病理变化明显,缺氧缺血侧大脑半球出现明显萎缩,神经元变性坏死,大量空泡形成。EPO治疗组则改变轻微。BAEP检查发现,EPO治疗组各日龄绝大部分的波峰潜伏期(PL)与假手术对照组相比无明显差异(除28、35日龄的Ⅴ波,21日龄的Ⅲ波外);从21日龄起EPO治疗组绝大部分的PL与HIBD组相比显著缩短(P<0.05,除21d的Ⅰ、Ⅴ波外);21日龄起,HIBD组大鼠各波峰间潜伏期(IPL)均明显长于假手术对照组(P<0.05),而EPO治疗组大鼠的大部分IPL相比HIBD组明显缩短(P<0.05,21、35日龄的Ⅱ-Ⅳ除外)。结论:外源性EPO的治疗可明显改善HIBD大鼠的脑功能及发育情况。

EPO激活HEL细胞内CREB转录因子

CREB(cAMPresponseelementbindingprotein)是一种细胞核内转录因子 ,激活的CREB能与特异调控元件CRE(cAMPresponseelement)结合 .研究结果显示 ,EPO(Erythropoietin)诱导HEL细胞 (Humanerythroleukemiacell) 2 0min后 ,HEL细胞核内CREB的 133位丝氨酸残基被磷酸化 ,并具有转录因子功能 .用 133位丝氨酸磷酸化的CREB特异抗体能抑制CREB转录因子与CREDNA序列的结合 ,揭示了CREB133位的丝氨酸残基磷酸化不仅与CREB转录因子活性相关 。