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Hsp90 伴侣蛋白在红细胞和非红细胞中辅助血红蛋白成熟。

Hsp90 chaperones hemoglobin maturation in erythroid and nonerythroid cells.

机构信息

Department of Pathobiology, Lerner Research Institute, The Cleveland Clinic, Cleveland, OH 44195;

Department of Pathobiology, Lerner Research Institute, The Cleveland Clinic, Cleveland, OH 44195.

出版信息

Proc Natl Acad Sci U S A. 2018 Feb 6;115(6):E1117-E1126. doi: 10.1073/pnas.1717993115. Epub 2018 Jan 22.

Abstract

Maturation of adult (α2β2) and fetal hemoglobin (α2γ2) tetramers requires that heme be incorporated into each globin. While hemoglobin alpha (Hb-α) relies on a specific erythroid chaperone (alpha Hb-stabilizing protein, AHSP), the other chaperones that may help mature the partner globins (Hb-γ or Hb-β) in erythroid cells, or may enable nonerythroid cells to express mature Hb, are unknown. We investigated a role for heat-shock protein 90 (hsp90) in Hb maturation in erythroid precursor cells that naturally express Hb-α with either Hb-γ (K562 and HiDEP-1 cells) or Hb-β (HUDEP-2) and in nonerythroid cell lines that either endogenously express Hb-αβ (RAW and A549) or that we transfected to express the globins. We found the following: () AHSP and hsp90 associate with distinct globin partners in their immature heme-free states (AHSP with apo-Hbα, and hsp90 with apo-Hbβ or Hb-γ) and that hsp90 does not associate with mature Hb. () Hsp90 stabilizes the apo-globins and helps to drive their heme insertion reactions, as judged by pharmacologic hsp90 inhibition or by coexpression of an ATP-ase defective hsp90. () In nonerythroid cells, heme insertion into all globins became hsp90-dependent, which may explain how mixed Hb tetramers can mature in cells that do not express AHSP. Together, our findings uncover a process in which hsp90 first binds to immature, heme-free Hb-γ or Hb-β, drives their heme insertion process, and then dissociates to allow their heterotetramer formation with Hb-α. Thus, in driving heme insertion, hsp90 works in concert with AHSP to generate functional Hb tetramers during erythropoiesis.

摘要

成人(α2β2)和胎儿血红蛋白(α2γ2)四聚体的成熟需要将血红素掺入每个球蛋白中。虽然血红蛋白α(Hb-α)依赖于特定的红细胞伴侣(α血红蛋白稳定蛋白,AHSP),但在红细胞中帮助成熟伴侣球蛋白(Hb-γ 或 Hb-β)的其他伴侣,或者可能使非红细胞表达成熟 Hb 的伴侣,尚不清楚。我们研究了热休克蛋白 90(hsp90)在红细胞前体细胞中血红蛋白成熟中的作用,这些细胞天然表达 Hb-α 与 Hb-γ(K562 和 HiDEP-1 细胞)或 Hb-β(HUDEP-2),以及非红细胞细胞系,这些细胞系要么内源性表达 Hb-αβ(RAW 和 A549),要么我们转染以表达球蛋白。我们发现:()AHSP 和 hsp90 在其未成熟的无血红素状态下与不同的球蛋白伴侣结合(AHSP 与 apo-Hbα 结合,hsp90 与 apo-Hbβ 或 Hb-γ 结合),并且 hsp90 不与成熟 Hb 结合。()hsp90 稳定 apo-球蛋白并有助于驱动其血红素插入反应,这可以通过药理学 hsp90 抑制或共表达 ATP 酶缺陷的 hsp90 来判断。()在非红细胞细胞中,所有球蛋白的血红素插入都变得依赖于 hsp90,这可能解释了为什么在不表达 AHSP 的细胞中可以成熟混合 Hb 四聚体。总之,我们的发现揭示了一个过程,其中 hsp90 首先与未成熟的、无血红素的 Hb-γ 或 Hb-β 结合,驱动它们的血红素插入过程,然后解离以允许它们与 Hb-α 形成异四聚体。因此,在驱动血红素插入过程中,hsp90 与 AHSP 协同作用,在红细胞生成过程中产生功能性 Hb 四聚体。

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