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携带人嗜T淋巴细胞病毒I型长末端重复序列/原癌基因c-myc和免疫球蛋白/反式激活因子基因的转基因小鼠中的脑肿瘤和淋巴瘤

Brain tumours and lymphomas in transgenic mice that carry HTLV-I LTR/c-myc and Ig/tax genes.

作者信息

Benvenisty N, Ornitz D M, Bennett G L, Sahagan B G, Kuo A, Cardiff R D, Leder P

机构信息

Department of Genetics, Harvard Medical School, Howard Hughes Medical Institute, Boston, Massachusetts 02115.

出版信息

Oncogene. 1992 Dec;7(12):2399-405.

PMID:1461648
Abstract

The human T-cell leukemia virus type 1 (HTLV-I) is associated with adult CD4+ T-cell leukemia (ATL) and tropical spastic paraparesis (TSP). In as much as only a small percentage of individuals infected with HTLV-I develop either disease, we set out to model a genetic partner for this virus in an effort to understand and possibly reproduce its pathophysiology. To this end we have developed a binary set of transgenic mice, one bearing the relatively inactive HTLV-I long terminal repeat (LTR) positioned to drive the c-myc oncogene and another bearing a fusion transgene consisting of the immunoglobulin promoter/enhancer driving the gene for the HTLV-I transcription activator, tax. Alone, the tax construct, though expressed in the thymus, spleen, lung and brain, has no deleterious effect. Alone, the HTLV-I LTR/c-myc construct is expressed at very low levels in lymphoid cells and occasionally induces lymphomas in older animals. When these two transgenic lines are mated, bigenic offspring harboring both transgenes exhibit dramatic tumor formation. As in the human, these animals develop CD4+ T-cell lymphomas, but they also develop central nervous system tumors by 25-90 days of age. The syndrome, which is 100% penetrant and lethal, provides an animal model for adult T-cell lymphoma and a source of cultured cells of neurogenic origin.

摘要

人类1型T细胞白血病病毒(HTLV - I)与成人CD4 + T细胞白血病(ATL)和热带痉挛性截瘫(TSP)相关。由于感染HTLV - I的个体中只有一小部分会患上这两种疾病,我们着手构建该病毒的基因伴侣模型,以努力理解并可能重现其病理生理学过程。为此,我们培育了一组二元转基因小鼠,一组携带相对无活性的HTLV - I长末端重复序列(LTR),其位置被设定为驱动c - myc癌基因;另一组携带由免疫球蛋白启动子/增强子驱动HTLV - I转录激活因子tax基因的融合转基因。单独来看,tax构建体虽然在胸腺、脾脏、肺和脑中表达,但没有有害影响。单独来看,HTLV - I LTR/c - myc构建体在淋巴细胞中表达水平很低,偶尔会在老年动物中诱发淋巴瘤。当这两个转基因品系交配时,同时携带两个转基因的双基因后代会出现显著的肿瘤形成。与人类情况一样,这些动物会发展出CD4 + T细胞淋巴瘤,但它们在25 - 90日龄时也会发展出中枢神经系统肿瘤。这种综合征具有100%的外显率且是致命的,为成人T细胞淋巴瘤提供了一个动物模型,也是神经源性培养细胞的一个来源。

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