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编码HPC-HPH/PRC1复合物的多梳蛋白家族基因在临床定义的原发性淋巴结和皮肤大B细胞淋巴瘤中的位点特异性表达。

Site-specific expression of polycomb-group genes encoding the HPC-HPH/PRC1 complex in clinically defined primary nodal and cutaneous large B-cell lymphomas.

作者信息

Raaphorst Frank M, Vermeer Maarten, Fieret Elly, Blokzijl Tjasso, Dukers Danny, Sewalt Richard G A B, Otte Arie P, Willemze Rein, Meijer Chris J L M

机构信息

Department of Pathology, Vrije Universiteit Medical Center, Amsterdam, The Netherlands.

出版信息

Am J Pathol. 2004 Feb;164(2):533-42. doi: 10.1016/S0002-9440(10)63143-4.

DOI:10.1016/S0002-9440(10)63143-4
PMID:14742259
原文链接:https://pmc.ncbi.nlm.nih.gov/articles/PMC1602277/
Abstract

Polycomb-group (PcG) genes preserve cell identity by gene silencing, and contribute to regulation of lymphopoiesis and malignant transformation. We show that primary nodal large B-cell lymphomas (LBCLs), and secondary cutaneous deposits from such lymphomas, abnormally express the BMI-1, RING1, and HPH1 PcG genes in cycling neoplastic cells. By contrast, tumor cells in primary cutaneous LBCLs lacked BMI-1 expression, whereas RING1 was variably detected. Lack of BMI-1 expression was characteristic for primary cutaneous LBCLs, because other primary extranodal LBCLs originating from brain, testes, and stomach were BMI-1-positive. Expression of HPH1 was rarely detected in primary cutaneous LBCLs of the head or trunk and abundant in primary cutaneous LBCLs of the legs, which fits well with its earlier recognition as a distinct clinical pathological entity with different clinical behavior. We conclude that clinically defined subclasses of primary LBCLs display site-specific abnormal expression patterns of PcG genes of the HPC-HPH/PRC1 PcG complex. Some of these patterns (such as the expression profile of BMI-1) may be diagnostically relevant. We propose that distinct expression profiles of PcG genes results in abnormal formation of HPC-HPH/PRC1 PcG complexes, and that this contributes to lymphomagenesis and different clinical behavior of clinically defined LBCLs.

摘要

多梳蛋白家族(PcG)基因通过基因沉默来维持细胞特性,并参与淋巴细胞生成和恶性转化的调控。我们发现,原发性淋巴结大B细胞淋巴瘤(LBCL)以及此类淋巴瘤的继发性皮肤沉积物,在增殖的肿瘤细胞中异常表达BMI-1、RING1和HPH1等PcG基因。相比之下,原发性皮肤LBCL中的肿瘤细胞缺乏BMI-1表达,而RING1的表达则存在差异。缺乏BMI-1表达是原发性皮肤LBCL的特征,因为源自脑、睾丸和胃的其他原发性结外LBCL为BMI-1阳性。HPH1在头颈部或躯干的原发性皮肤LBCL中很少被检测到,而在腿部的原发性皮肤LBCL中大量表达,这与其早期被认定为具有不同临床行为的独特临床病理实体相吻合。我们得出结论,临床上定义的原发性LBCL亚类显示出HPC-HPH/PRC1 PcG复合物的PcG基因的位点特异性异常表达模式。其中一些模式(如BMI-1的表达谱)可能具有诊断意义。我们提出,PcG基因的不同表达谱导致HPC-HPH/PRC1 PcG复合物异常形成,这有助于淋巴瘤的发生以及临床上定义的LBCL的不同临床行为。

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Site-specific expression of polycomb-group genes encoding the HPC-HPH/PRC1 complex in clinically defined primary nodal and cutaneous large B-cell lymphomas.编码HPC-HPH/PRC1复合物的多梳蛋白家族基因在临床定义的原发性淋巴结和皮肤大B细胞淋巴瘤中的位点特异性表达。
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Polycomb group genes as epigenetic regulators of normal and leukemic hemopoiesis.多梳蛋白家族基因作为正常和白血病造血的表观遗传调节因子。
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Drosophila enhancer of Zeste/ESC complexes have a histone H3 methyltransferase activity that marks chromosomal Polycomb sites.果蝇Zeste增强子/ESC复合物具有一种组蛋白H3甲基转移酶活性,可标记染色体上的多梳位点。
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Selective interactions between vertebrate polycomb homologs and the SUV39H1 histone lysine methyltransferase suggest that histone H3-K9 methylation contributes to chromosomal targeting of Polycomb group proteins.脊椎动物多梳蛋白同源物与SUV39H1组蛋白赖氨酸甲基转移酶之间的选择性相互作用表明,组蛋白H3-K9甲基化有助于多梳蛋白家族蛋白的染色体靶向定位。
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Polycomb group gene rae28 is required for sustaining activity of hematopoietic stem cells.多梳蛋白家族基因rae28是维持造血干细胞活性所必需的。
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Programming off and on states in chromatin: mechanisms of Polycomb and trithorax group complexes.染色质中开关状态的编程:多梳蛋白和三胸节复合物的机制
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