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在携带t(14; 18)的转基因小鼠中从淋巴样增生发展为高级别恶性淋巴瘤。

Progression from lymphoid hyperplasia to high-grade malignant lymphoma in mice transgenic for the t(14; 18).

作者信息

McDonnell T J, Korsmeyer S J

机构信息

Howard Hughes Medical Institute, Washington University School of Medicine, St Louis, Missouri 63110.

出版信息

Nature. 1991 Jan 17;349(6306):254-6. doi: 10.1038/349254a0.

Abstract

Follicular lymphoma, the most common human lymphoma, characteristically has a t(14; 18) interchromosomal translocation. It is typically an indolent disease comprised of small resting B cells, but frequently develops into a high-grade lymphoma. The t(14; 18) translocates the Bcl-2 gene, generating a deregulated Bcl-2-immunoglobulin fusion gene. Bcl-2 is a novel inner mitochondrial membrane protein that extends the survival of certain cells by blocking programmed cell death. To determine the oncogenic potential of the t(14; 18) translocation, we produced transgenic mice bearing a Bcl-2-immunoglobulin minigene that structurally mimicked the t(14; 18). An indolent follicular hyperplasia in these transgenic mice progressed to a malignant diffuse large-cell lymphoma. The long latency, progression from polyclonal to monoclonal disease, and histological conversion, are all suggestive of secondary changes. Half of the immunoblastic high-grade lymphomas had a rearranged c-myc gene. Our transgenic mice provide an animal model for tumour progression in t(14; 18) lymphoma and show that prolonged B-cell life increases tumour incidence.

摘要

滤泡性淋巴瘤是最常见的人类淋巴瘤,其特征是存在14号和18号染色体间的易位[t(14; 18)]。它通常是一种由静止的小B细胞组成的惰性疾病,但常发展为高级别淋巴瘤。t(14; 18)易位使Bcl-二基因移位,产生一个失调的Bcl-二免疫球蛋白融合基因。Bcl-二是一种新型线粒体内膜蛋白,通过阻断程序性细胞死亡来延长某些细胞的存活时间。为了确定t(14; 18)易位的致癌潜力,我们培育了携带结构上模拟t(14; 18)的Bcl-二免疫球蛋白小基因的转基因小鼠。这些转基因小鼠中出现的惰性滤泡性增生发展为恶性弥漫性大细胞淋巴瘤。较长的潜伏期、从多克隆疾病进展为单克隆疾病以及组织学转变,都提示了继发性改变。一半的免疫母细胞性高级别淋巴瘤有c-myc基因重排。我们的转基因小鼠为t(14; 18)淋巴瘤的肿瘤进展提供了一个动物模型,并表明B细胞寿命延长会增加肿瘤发生率。

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