Department of Microbiology and Immunology, Indiana University School of Medicine, Indianapolis, Indiana, USA.
J Exp Med. 2013 Feb 11;210(2):205-8. doi: 10.1084/jem.20122760.
Erythropoietin (EPO), a humoral regulator of erythropoiesis and replacement therapy for selected red blood cell disorders in EPO-deficient patients, has been implicated in a wide range of activities on diverse cell, tissue, and organ types. EPO signals via two receptors, one comprising EPO receptor (EPOR) homodimers and the other a heterodimer of EPOR and CD131-the common β chain component of the GM-CSF, interleukin (IL)-3, and IL-5 receptors. Ligation of EPORs triggers various signaling pathways, including the JAK2-STAT5 and MAPK-NF-κB pathways, depending both on the receptor and the target cell type. A new study in this issue reveals a novel EPO-triggered pathway involving a Spi2A serpin-lysosome-cathepsin cascade that is initiated through the homodimeric EPOR complex and is required for the survival of erythroid progenitors. A full understanding of EPO's effects on various cell types and their potential clinical relevance requires more work on the signaling events initiated through both EPORs, the effects of other cytokines and growth factors that modulate EPO's actions, and a comparison of the effects of full-length versus truncated forms of EPO.
促红细胞生成素(EPO)是一种红细胞生成的体液调节剂,也是 EPO 缺乏患者某些红细胞疾病的替代治疗药物,它被涉及到各种细胞、组织和器官类型的广泛活动中。EPO 通过两种受体发挥作用,一种受体由 EPO 受体(EPOR)同二聚体组成,另一种受体由 EPOR 和 CD131(GM-CSF、白细胞介素[IL]-3 和 IL-5 受体的共同β链成分)组成的异二聚体组成。EPOR 的配体结合会触发各种信号通路,包括 JAK2-STAT5 和 MAPK-NF-κB 通路,这取决于受体和靶细胞类型。本期中的一项新研究揭示了一种新的 EPO 触发途径,涉及 Spi2A 丝氨酸蛋白酶抑制剂-溶酶体-组织蛋白酶级联反应,该途径通过同源二聚体 EPOR 复合物启动,是红系祖细胞存活所必需的。要充分了解 EPO 对各种细胞类型的影响及其潜在的临床相关性,需要更多地研究通过两种 EPOR 启动的信号事件、调节 EPO 作用的其他细胞因子和生长因子的影响,以及全长与截短形式的 EPO 的作用比较。
