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肿瘤坏死因子相关凋亡诱导配体 1(TRAIL1)增强了非洲爪蟾变态过程中从幼体到成体类型的红细胞转化。

Tumor necrosis factor-related apoptosis-inducing ligand 1 (TRAIL1) enhances the transition of red blood cells from the larval to adult type during metamorphosis in Xenopus.

机构信息

Department of Biosciences, School of Science, Kitasato University, Sagamihara, Japan.

出版信息

Blood. 2010 Jan 28;115(4):850-9. doi: 10.1182/blood-2009-04-218966. Epub 2009 Nov 25.

DOI:10.1182/blood-2009-04-218966
PMID:19965624
Abstract

The transition of red blood cells (RBCs) from primitive to definitive erythropoiesis is conserved across vertebrates. In anuran amphibians, the larval RBCs from primitive erythropoiesis are replaced by adult RBCs from definitive erythropoiesis during metamorphosis. The molecular mechanisms by which the primitive (larval) blood cells are specifically removed from circulation are not yet understood. In this study, we identified Xenopus tumor necrosis factor-related apoptosis-inducing ligand 1 (xTRAIL1) and xTRAIL2 as ligands of Xenopus death receptor-Ms (xDR-Ms) and investigated whether TRAIL signaling could be involved in this transition. The Trail and xDR-M genes were highly expressed in the liver and RBCs, respectively, during metamorphosis. Interestingly, xTRAIL1 enhanced the transition of the RBCs, and a dominant-negative form of the xTRAIL1 receptor attenuated it, when injected into tadpoles. Moreover, xTRAIL1 induced apoptosis in larval RBCs, but had little effect on adult RBCs in vitro. We also found that adult RBCs treated with staurosporine, a protein kinase C (PKC) inhibitor, were sensitized to xTRAIL1. The mRNAs for PKC isoforms were up-regulated in RBCs during metamorphosis. These results suggest that xTRAIL1 can cause apoptosis, probably mediated through xDR-Ms, in larval RBCs, but may not kill adult RBCs, presumably owing to PKC activation, as part of the mechanism for RBC switching.

摘要

红细胞(RBC)从原始到定型的转变在脊椎动物中是保守的。在无尾两栖类动物中,在变态过程中,来自原始红细胞生成的幼虫 RBC 被来自定型红细胞生成的成年 RBC 取代。原始(幼虫)血细胞从循环中被特异性清除的分子机制尚不清楚。在这项研究中,我们鉴定出 Xenopus 肿瘤坏死因子相关凋亡诱导配体 1(xTRAIL1)和 xTRAIL2 是 Xenopus 死亡受体-Ms(xDR-Ms)的配体,并研究了 TRAIL 信号是否参与了这一转变。在变态过程中,Trail 和 xDR-M 基因在肝脏和 RBC 中分别高度表达。有趣的是,xTRAIL1 在注射到蝌蚪中时增强了 RBC 的转变,而 xTRAIL1 受体的显性负形式则减弱了这种转变。此外,xTRAIL1 在体外诱导幼虫 RBC 凋亡,但对成年 RBC 几乎没有影响。我们还发现,用蛋白激酶 C(PKC)抑制剂 staurosporine 处理的成年 RBC 对 xTRAIL1 敏感。在变态过程中,RBC 中 PKC 同工型的 mRNA 上调。这些结果表明,xTRAIL1 可以在幼虫 RBC 中引起凋亡,可能是通过 xDR-Ms 介导的,但可能不会杀死成年 RBC,可能是由于 PKC 激活,作为 RBC 转换的机制之一。

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