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A Novel Truncated env Gene Isolated from a Feline Leukemia Virus-Induced Thymic Lymphosarcoma

机译:从猫白血病病毒诱导的胸腺淋巴肉瘤中分离出一种新型截短的env基因。

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摘要

We PCR amplified the exogenous feline leukemia virus (FeLV)-related env gene species from lymphosarcomas induced by intradermally administered plasmid DNA of either the prototype FeLV, subgroup A molecular clone, F6A, or a new molecular clone, FeLV-A, Rickard strain (FRA). Of the nine tumors examined, six showed the presence of deleted env species of variable sizes in the tumor DNA. One env mutant, which was detected in a FRA-induced thymic lymphosarcoma, had a large internal deletion beginning from almost the N-terminal surface glycoprotein (SU) up to the middle region of the transmembrane (TM) protein of the env gene. The deduced polypeptide of this truncated env (tenv) retained the complete signal peptide and seven amino acids of the N-terminal mature SU of FRA env gene, followed by eight amino acids from the frameshift in the TM region. To study the biological function of tenv, we used a murine retrovirus vector to produce amphotropic virions. Infection of feline fibroblasts (H927), human fibrosarcoma cells (HT1080), or human B-lymphoma cells (Raji) led to pronounced cytotoxicity, while the tenv virus did not induce significant cytotoxicity to feline T-lymphoma cells (3201B) or human T-lymphoma cells (CEM). Together, these results convincingly demonstrated that the genetic events that led to truncation in the env gene occurred de novo in FeLV lymphomagenesis and that such a product, tenv could induce cytotoxicity to fibroblastic and B-lymphoid cells but not to T-lymphoid tumor cells. This type of selective toxicity might be potentially important in the development of the neoplastic disease.
机译:我们通过PCR扩增了由原型FeLV,亚组A分子克隆F6A或新的分子克隆FeLV-A,Rickard菌株(皮内注射)诱导的淋巴肉瘤中外源性猫白血病病毒(FeLV)相关的env基因种FRA)。在检查的9种肿瘤中,有6种显示肿瘤DNA中存在大小可变的缺失env物种。在FRA诱导的胸腺淋巴肉瘤中检测到的一个env突变体,从几乎N端表面糖蛋白(SU)到env基因的跨膜(TM)蛋白的中部开始都有较大的内部缺失。该截短的env(tenv)的推导多肽保留了完整的信号肽和FRA env基因的N端成熟SU的七个氨基酸,其后是TM区中移码的八个氨基酸。为了研究tenv的生物学功能,我们使用了鼠逆转录病毒载体生产两性病毒粒子。猫成纤维细胞(H927),人纤维肉瘤细胞(HT1080)或人B淋巴瘤细胞(Raji)的感染导致明显的细胞毒性,而tenv病毒对猫T淋巴瘤细胞(3201B)或人T并没有明显的细胞毒性。 -淋巴瘤细胞(CEM)。在一起,这些结果令人信服地证明,导致env基因被截断的遗传事件在FeLV淋巴瘤的发生中重新发生,并且这种产物tenv可以诱导对成纤维细胞和B淋巴样细胞的细胞毒性,而不是对T淋巴样肿瘤细胞的毒性。这种类型的选择性毒性可能在肿瘤疾病的发展中具有潜在的重要性。

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