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E3 连接酶 axotrophin/MARCH-7:人类组织的蛋白质表达谱分析揭示了与成体干细胞的联系。

The E3 ligase axotrophin/MARCH-7: protein expression profiling of human tissues reveals links to adult stem cells.

机构信息

Human Proteome Resource, School of Biotechnology, Department of Proteomics, Royal Institute of Technology, Stockholm, Sweden.

出版信息

J Histochem Cytochem. 2010 Apr;58(4):301-8. doi: 10.1369/jhc.2009.954420. Epub 2009 Nov 9.

Abstract

Axotrophin/MARCH-7 was first identified in mouse embryonic stem cells as a neural stem cell gene. Using the axotrophin/MARCH-7 null mouse, we discovered profound effects on T lymphocyte responses, including 8-fold hyperproliferation and 5-fold excess release of the stem cell cytokine leukemia inhibitory factor (LIF). Our further discovery that axotrophin/MARCH-7 is required for targeted degradation of the LIF receptor subunit gp190 implies a direct role in the regulation of LIF signaling. Bioinformatics studies revealed a highly conserved RING-CH domain in common with the MARCH family of E3-ubiquitin ligases, and accordingly, axotrophin was renamed "MARCH-7." To probe protein expression of human axotrophin/MARCH-7, we prepared antibodies against different domains of the protein. Each antibody bound its specific target epitope with high affinity, and immunohistochemistry cross-validated target specificity. Forty-eight human tissue types were screened. Epithelial cells stained strongly, with trophoblasts having the greatest staining. In certain tissues, specific cell types were selectively positive, including neurons and neuronal progenitor cells in the hippocampus and cerebellum, endothelial sinusoids of the spleen, megakaryocytes in the bone marrow, crypt stem cells of the small intestine, and alveolar macrophages in the lung. Approximately 20% of central nervous system neuropils were positive. Notably, axotrophin/MARCH-7 has an expression profile that is distinct from that of other MARCH family members. This manuscript contains online supplemental material at http://www.jhc.org. Please visit this article online to view these materials.

摘要

Axotrophin/MARCH-7 最初在小鼠胚胎干细胞中被鉴定为一种神经干细胞基因。利用 axotrophin/MARCH-7 基因缺失小鼠,我们发现其对 T 淋巴细胞反应有深远影响,包括 8 倍的过度增殖和 5 倍的干细胞细胞因子白血病抑制因子(LIF)过量释放。我们进一步发现,axotrophin/MARCH-7 是 LIF 受体亚基 gp190 靶向降解所必需的,这意味着它在 LIF 信号转导的调节中起直接作用。生物信息学研究揭示了一个高度保守的 RING-CH 结构域,与 E3-泛素连接酶的 MARCH 家族具有共同性,因此,axotrophin 被重新命名为“MARCH-7”。为了研究人源 axotrophin/MARCH-7 的蛋白表达情况,我们制备了针对该蛋白不同结构域的抗体。每种抗体都与特定的靶标表位高亲和力结合,免疫组织化学交叉验证了靶标特异性。筛选了 48 种人类组织类型。上皮细胞染色强烈,滋养层染色最强。在某些组织中,特定的细胞类型呈阳性,包括海马体和小脑的神经元和神经元祖细胞、脾脏的内皮窦、骨髓中的巨核细胞、小肠的隐窝干细胞和肺中的肺泡巨噬细胞。约 20%的中枢神经系统神经原纤维呈阳性。值得注意的是,axotrophin/MARCH-7 的表达谱与其他 MARCH 家族成员明显不同。本文包含在线补充材料,可在 http://www.jhc.org 上查阅。请访问本文的在线版本以查看这些材料。

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