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内源性逆转录病毒env在原发性小鼠白血病中的表达:缺乏嗜异性抗原,但存在与嗜亲性病毒接种及小鼠品系相关的不同的貂细胞灶形成env亚型。

Endogenous retroviral env expression in primary murine leukemias: lack of xenotropic antigens but presence of distinct mink cell focus-forming env subtypes correlating with ecotropic virus inoculated and mouse strain.

作者信息

Cloyd M W, Evans L H

出版信息

J Natl Cancer Inst. 1987 Jan;78(1):181-9. doi: 10.1093/jnci/78.1.181.

Abstract

The expression of endogenous retroviral env products on primary leukemia cells of mice was studied with the use of a panel of monoclonal antibodies that discriminate between the various classes of murine leukemia viruses [MuLVs; ecotropic, xenotropic, and mink cell focus-forming (MCF)], as well as between various subtypes within each class. Most spontaneous AKR or Friend MuLV (F-MuLV)- or Moloney MuLV (M-MuLV)-induced AKR or NFS mouse leukemia cells expressed no xenotropic viral envelope antigens but always expressed MCF proteins. Spontaneous C58 lymphomas, on the other hand, often expressed xenotropic proteins in addition to MCF proteins. The subtype of MCF envelope antigens present on leukemia cells, as well as on isolated MCF viruses, varied in a reproducible manner, depending on the mouse strain inoculated and the ecotropic virus used (F-MuLV or M-MuLV). Specifically, F-MuLV consistently induced certain type(s) of MCF envelope antigens on leukemia cells of NFS mice, whereas M-MuLV induced different ones. Similar antigenic patterns were found on the MCF viruses isolated from these mice. Furthermore, MCF envelope antigens (on viruses or leukemia cells) induced in NFS mice by M-MuLV differed from those induced in AKR mice. This finding demonstrated a mouse strain influence on the endogenous MCF env sequences expressed following infection by a given ecotropic virus. The endogenous MCF env sequences in mice thus appear to be a set of genes highly expressed during leukemogenesis, with particular ones specifically expressed in a given mouse strain infected with a given ecotropic virus.

摘要

利用一组单克隆抗体研究了小鼠原发性白血病细胞上内源性逆转录病毒env产物的表达,这些抗体可区分不同类别的鼠白血病病毒[MuLVs;嗜亲性、异嗜性和貂细胞集落形成(MCF)],以及每一类中的各种亚型。大多数自发的AKR或Friend MuLV(F-MuLV)或莫洛尼MuLV(M-MuLV)诱导的AKR或NFS小鼠白血病细胞不表达异嗜性病毒包膜抗原,但总是表达MCF蛋白。另一方面,自发的C58淋巴瘤除了表达MCF蛋白外,还经常表达异嗜性蛋白。白血病细胞以及分离出的MCF病毒上存在的MCF包膜抗原亚型,根据接种的小鼠品系和使用的嗜亲性病毒(F-MuLV或M-MuLV)以可重复的方式变化。具体而言,F-MuLV始终在NFS小鼠的白血病细胞上诱导某些类型的MCF包膜抗原,而M-MuLV诱导的则不同。从这些小鼠分离出的MCF病毒上也发现了类似的抗原模式。此外,M-MuLV在NFS小鼠中诱导的MCF包膜抗原(在病毒或白血病细胞上)与在AKR小鼠中诱导的不同。这一发现表明小鼠品系对给定嗜亲性病毒感染后表达的内源性MCF env序列有影响。因此,小鼠中的内源性MCF env序列似乎是一组在白血病发生过程中高度表达的基因,特定的基因在感染给定嗜亲性病毒的给定小鼠品系中特异性表达。

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