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嗜淋巴细胞乳头多瘤病毒早期区域在转基因小鼠中受到特异性调控,并能有效诱导肿瘤形成。

Lymphotropic papovavirus early region is specifically regulated transgenic mice and efficiently induces neoplasia.

作者信息

Chen J D, Neilson K, Van Dyke T

机构信息

Department of Biological Sciences, University of Pittsburgh, Pennsylvania 15260.

出版信息

J Virol. 1989 May;63(5):2204-14. doi: 10.1128/JVI.63.5.2204-2214.1989.

Abstract

Transgenic mice have been generated which carry the early region of lymphotropic papovavirus (LPV). Eight of eleven founder animals died before 3 months of age after developing one or both of two distinct proliferative disorders. Of the three surviving animals, two are known to have rearranged or partial copies of the LPV genes. The majority of the founder animals (six) developed debilitating choroid plexus tumors by 26 to 42 days. Although this is the same tumor type induced by the simian virus 40 T-antigen gene, those induced by LPV appeared at a much younger age. The LPV early region was expressed in the brain tumors of these mice, as well as in the thymus and spleen. Expression in the latter two tissues reflects the cell-type specificity of the LPV enhancer demonstrated in cultured cells (i.e., lymphoid cells). Two founder animals (LP41 and LP50) gave rise to lines of mice that routinely develop lymphoproliferative disorders. LP50 and its LPV-positive offspring developed aggressive lymphomas and choroid plexus tumors. The transgenic offspring of LP41 also developed lymphomas. High levels of LPV RNA were expressed in the lymphomas of these mice as well as in the spleens and thymuses. The origin of the lymphomas from B- and T-cell lineages suggests that the LPV early genes are expressed in and can transform both of these cell types in vivo.

摘要

已培育出携带亲淋巴性乳头多瘤病毒(LPV)早期区域的转基因小鼠。11只奠基动物中有8只在出现一种或两种不同的增殖性疾病后,在3个月龄前死亡。在三只存活的动物中,已知有两只具有LPV基因的重排或部分拷贝。大多数奠基动物(6只)在26至42天时出现了使人衰弱的脉络丛肿瘤。尽管这与猿猴病毒40 T抗原基因诱导的肿瘤类型相同,但由LPV诱导的肿瘤出现的年龄要小得多。LPV早期区域在这些小鼠的脑肿瘤以及胸腺和脾脏中表达。在后两种组织中的表达反映了在培养细胞(即淋巴细胞)中所证明的LPV增强子的细胞类型特异性。两只奠基动物(LP41和LP50)产生了经常发生淋巴增殖性疾病的小鼠品系。LP50及其LPV阳性后代发生了侵袭性淋巴瘤和脉络丛肿瘤。LP41的转基因后代也发生了淋巴瘤。在这些小鼠的淋巴瘤以及脾脏和胸腺中表达了高水平的LPV RNA。淋巴瘤起源于B细胞和T细胞谱系,这表明LPV早期基因在体内可在这两种细胞类型中表达并使其发生转化。

https://cdn.ncbi.nlm.nih.gov/pmc/blobs/8b5c/250638/2dd9870d0d34/jvirol00072-0376-a.jpg

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