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在Rbtn-2转基因小鼠中具有不同表型的T细胞肿瘤。

T cell tumours of disparate phenotype in mice transgenic for Rbtn-2.

作者信息

Larson R C, Fisch P, Larson T A, Lavenir I, Langford T, King G, Rabbitts T H

机构信息

MRC Laboratory of Molecular Biology, Cambridge, UK.

出版信息

Oncogene. 1994 Dec;9(12):3675-81.

PMID:7970726
Abstract

RBTN2 is a LIM domain protein which can be activated by the translocation t(11;14)(p13;q11) in childhood T cell acute leukaemia. Transgenic mice were examined in which rbtn2 protein is expressed in the T cell lineage. An average of 72% of these mice developed T cell tumours before 18 months of age, compared with 9% in transgenic mice expressing the related gene Rbtn-1. Rbtn2-induced tumours first appeared at 5 months of age and were clonal. They displayed a range of phenotypes, the most notable being CD3/CD45R double-positive cells. Tumours expressing either T cell receptor alpha/beta or gamma/delta heterodimers were found. Thus rbtn2 can promote tumours within a range of T cell types and maturities. The latency period before tumour development indicates that secondary events must occur before the onset of overt malignancy.

摘要

RBTN2是一种LIM结构域蛋白,在儿童T细胞急性白血病中可因t(11;14)(p13;q11)易位而被激活。对在T细胞谱系中表达rbtn2蛋白的转基因小鼠进行了检测。这些小鼠平均有72%在18个月龄前发生T细胞肿瘤,而表达相关基因Rbtn - 1的转基因小鼠这一比例为9%。Rbtn2诱导的肿瘤最早在5个月龄时出现,且为克隆性肿瘤。它们表现出一系列表型,最显著的是CD3/CD45R双阳性细胞。发现了表达T细胞受体α/β或γ/δ异二聚体的肿瘤。因此,rbtn2可促进多种T细胞类型和成熟阶段的肿瘤发生。肿瘤发生前的潜伏期表明,在明显的恶性肿瘤发生之前必须发生二次事件。

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