首页> 外文期刊>Journal of cellular and molecular medicine. >Characterization of the expression of HTm4 (MS4A3), a cell cycle regulator, in human peripheral blood cells and normal and malignant tissues
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Characterization of the expression of HTm4 (MS4A3), a cell cycle regulator, in human peripheral blood cells and normal and malignant tissues

机译:HTm4(MS4A3)(一种细胞周期调节剂)在人外周血细胞以及正常和恶性组织中的表达特征

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HTm4 (MS4A3) is a member of a family of four-transmembrane proteins designated MS4A. MS4A proteins fulfil diverse functions, acting as cell surface signalling molecules and intracellular adapter proteins. Early reports demonstrated that HTm4 is largely restricted to the haematopoietic lineage, and is involved in cell cycle control, via a regulatory interaction with the kinase-associated phosphatase, cyclin A and cyclin-dependent kinase 2 (CDK2). Here we describe the expression pattern of HTm4 in peripheral blood cells using gene expression microarray technology, and in normal foetal and adult human tissues, as well as adult human cancers, using tissue microarray technology. Using oligonucleotide microarrays to evaluate HTm4 mRNA, all peripheral blood cell types demonstrated very low levels of HTm4 expression; however, HTm4 expression was greatest in basophils compared to eosinophils, which showed lower levels of HTm4 expression. Very weak HTm4 expression is found in monocytes, granulocytes and B cells, but not in T cells, by lineage specific haematopoietic cell flow cytometry analysis. Interestingly, phytohaemagglutinin stimulation increases HTm4 protein expression in peripheral blood CD4-T-lymphocytes over nearly undetectable baseline levels. Western blotting and immunohistochemical studies show strong HTm4 expression in the developing haematopoietic cells of human foetal liver. Immunohistochemical studies on normal tissue microarrays confirmed HTm4 expression in a subset of leucocytes in nodal, splenic tissues and thymic tissue, and weak staining in small numbers of cell types in non-haematopoietic tissues. Human foetal brain specimens from 19 to 31 gestational weeks showed that the strongest-staining cells are ventricular zone cells and the earliest-born, earliest-differentiating 'pioneer' neurons in the cortical plate, Cajal-Retzius and, to a lesser extent, subplate-like neurons. Malignant tissue microarray analysis showed HTm4 expression in a wide variety of adenocarcinomas, including breast, prostate and ovarian. These findings warrant the further study of the role of HTm4 in the cell cycle of both haematopoietic and tumour cells.
机译:HTm4(MS4A3)是称为MS4A的四跨膜蛋白家族的成员。 MS4A蛋白具有多种功能,可充当细胞表面信号分子和细胞内衔接子蛋白。早期报道表明,HTm4在很大程度上局限于造血谱系,并通过与激酶相关的磷酸酶,细胞周期蛋白A和细胞周期蛋白依赖性激酶2(CDK2)的调节相互作用而参与细胞周期控制。在这里,我们描述了使用基因表达微阵列技术在外周血细胞中HTm4的表达模式,以及使用组织微阵列技术在正常胎儿和成年人类组织以及成年人类癌症中的表达模式。使用寡核苷酸微阵列评估HTm4 mRNA,所有外周血细胞类型均显示出极低水平的HTm4表达。然而,与嗜酸性粒细胞相比,嗜碱性粒细胞中HTm4表达最大,后者表现出较低水平的HTm4表达。通过谱系特异性造血细胞流式细胞术分析,在单核细胞,粒细胞和B细胞中发现非常弱的HTm4表达,而在T细胞中则没有。有趣的是,植物血凝素刺激使外周血CD4-T淋巴细胞中的HTm4蛋白表达增加了几乎无法检测到的基线水平。蛋白质印迹和免疫组织化学研究表明,人胎儿肝脏发育中的造血细胞中有强烈的HTm4表达。正常组织微阵列的免疫组织化学研究证实,HTm4在淋巴结,脾组织和胸腺组织的白细胞亚群中表达,并且在非造血组织中少量细胞类型的染色较弱。从妊娠19到31周的人类胎儿脑标本显示,染色最强的细胞是心室区细胞,是皮质板,Cajal-Retzius以及在较小程度上亚板中最早,分化最早的“先锋”神经元。样神经元。恶性组织微阵列分析显示HTm4在多种腺癌中表达,包括乳腺癌,前列腺癌和卵巢癌。这些发现需要进一步研究HTm4在造血和肿瘤细胞的细胞周期中的作用。

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