首页> 外文期刊>The Journal of Experomental Medicine >Friend murine leukemia virus-induced leukemia is associated with the formation of mink cell focus-inducing viruses and is blocked in mice expressing endogenous mink cell focus-inducing xenotropic viral envelope genes.
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Friend murine leukemia virus-induced leukemia is associated with the formation of mink cell focus-inducing viruses and is blocked in mice expressing endogenous mink cell focus-inducing xenotropic viral envelope genes.

机译:朋友鼠白血病病毒诱发的白血病与貂细胞病原诱导病毒的形成有关,并在表达内源性貂细胞病原诱导异源性病毒包膜基因的小鼠中被阻断。

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In these studies, we have shown data that are consistent with the hypothesis that mink cell focus-inducing viruses (MCF) play an important role in the generation of an erythroproliferative disease developing after injection of certain strains of newborn mice with ecotropic Friend murine leukemia virus (F-MuLV). Resistance to this disease is correlated with the endogenous expression of an MCF/xenotropic virus-gp70-related protein that may interfere with the replication or spread of MCF viruses. These ideas are supported by the following observations: (a) after infection with F-MuLV, only 6/13 strains of mice-developed disease, and studies with crosses between susceptible and resistant strains indicated that resistance was dominant. Although F-MuLV was shown to replicate equally well in all strains tested, viruses coding for MCF-specific viral envelope proteins could be detected only in the spleens of mice from strains that were resistant to F-MuLV-induced disease and not in the spleens of mice from strains that were resistant to F-MuLV-induced disease; (b) a Friend MCF (Fr-MCF) virus isolated from the spleen of an F-MuLV-infected mouse from a susceptible strain induced the same erythroproliferative disease when injected as an appropriate pseudotype into mice from susceptible but not resistant strains of mice; and (c) resistant but not susceptible strains of mice endogenously express MCF/xenotropic virus-related envelope glycoproteins that may be responsible for resistance by blocking receptors for MCF viruses. These results not only indicate that Fr-MCF virus is a crucial intermediate in the induction of disease by F-MuLV, but also suggest that a novel gene, either an MCF/xenotropic virus-related envelope gene or a gene controlling its expression, is responsible for resistance to erythroleukemia induced by F-MuLV.
机译:在这些研究中,我们显示了与以下假设相符的数据:貂细胞聚焦诱导病毒(MCF)在向新生小鼠注射某些品系的嗜性Friend鼠白血病病毒后,在促红细胞生成性疾病的产生中起着重要作用(F-MuLV)。对这种疾病的抵抗力与MCF /异种病毒-gp70相关蛋白的内源表达有关,该蛋白可能会干扰MCF病毒的复制或传播。这些观点得到以下观察结果的支持:(a)在感染F-MuLV之后,只有6/13株小鼠发展为疾病,并且对易感株和抗性株之间的杂交进行的研究表明,抗性是主要的。尽管显示F-MuLV在所有测试菌株中均能很好地复制,但是编码MCF特异性病毒包膜蛋白的病毒只能在对F-MuLV诱导的疾病具有抗性的菌株的小鼠脾脏中检测到,而在脾脏中则无法检测到来自对F-MuLV诱导的疾病具有抗性的品系的小鼠; (b)从易感株的F-MuLV感染小鼠的脾脏中分离出来的Friend MCF(Fr-MCF)病毒,当作为合适的假型从易感但非抗性小鼠品系注射入小鼠时,会诱发相同的促红细胞生成性疾病; (c)抗性但不是易感小鼠品系内源性表达MCF /异种病毒相关的包膜糖蛋白,该蛋白可能通过阻断MCF病毒的受体而引起抗性。这些结果不仅表明Fr-MCF病毒是通过F-MuLV诱导疾病的关键中间体,而且还暗示了一个新的基因,即MCF /异种病毒相关的包膜基因或控制其表达的基因。负责抵抗由F-MuLV引起的红白血病。

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