首页> 美国卫生研究院文献>Proceedings of the National Academy of Sciences of the United States of America >Mouse mammary tumor viruses with functional superantigen genes are selected during in vivo infection.
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Mouse mammary tumor viruses with functional superantigen genes are selected during in vivo infection.

机译:在体内感染期间选择具有功能性超抗原基因的小鼠乳腺肿瘤病毒。

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摘要

Mouse mammary tumor virus (MMTV) encodes a superantigen that is important for viral infectivity in vivo. To determine whether superantigen function was required for infection by milk-borne MMTV, we created HYB PRO/Cla transgenic mice. These mice produced a full-length, packaged viral RNA with a frameshift mutation that caused premature termination of the superantigen protein. Young HYB PRO/Cla mice showed no deletion of their cognate V beta 14+ T cells, although they shed virus in their milk. The nontransgenic offspring of the HYB PRO/Cla mice were infected with this virus, since transgene-specific viral transcripts were detected in their mammary glands. Surprisingly, these offspring demonstrated the progressive deletion of V beta 14+ T cells characteristic of exogenous MMTV (C3H) infection. Sequence analysis demonstrated that these newly acquired viruses had reconstituted superantigen open reading frames resulting from recombination between the HYB PRO/Cla and endogenous Mtv-1 proviral RNAs. Thus, there is selection during the infection process for MMTVs with functional superantigen genes.
机译:小鼠乳腺肿瘤病毒(MMTV)编码一种对体内病毒感染性很重要的超抗原。为了确定牛奶传播的MMTV感染是否需要超抗原功能,我们创建了HYB PRO / Cla转基因小鼠。这些小鼠产生全长包装的病毒RNA,并带有移码突变,导致超抗原蛋白过早终止。年轻的HYB PRO / Cla小鼠虽然在乳汁中感染了病毒,但并未显示其同源V beta 14+ T细胞的缺失。 HYB PRO / Cla小鼠的非转基因后代感染了该病毒,因为在其乳腺中检测到转基因特异性病毒转录本。令人惊讶的是,这些后代证明了外源性MMTV(C3H)感染特征性的V beta 14+ T细胞的逐步缺失。序列分析表明,这些新获得的病毒已经重组了HYB PRO / Cla与内源性Mtv-1前病毒RNA重组产生的超抗原开放阅读框。因此,在感染过程中对于具有功能性超抗原基因的MMTV有选择。

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