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Subtle Mutational Changes in the SU Protein of a Natural Feline Leukemia Virus Subgroup A Isolate Alter Disease Spectrum

机译:天然猫白血病病毒亚组A的SU蛋白的细微突变变化改变疾病谱

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摘要

FeLV-945 is a representative isolate of the natural feline leukemia virus (FeLV) variant predominant in non-T-cell malignant, proliferative, and degenerative diseases in a geographic cohort. The FeLV-945 surface glycoprotein (SU) is closely related to natural horizontally transmissible FeLV subgroup A (FeLV-A) but was found to differ from a prototype to a larger extent than the members of FeLV-A differ among themselves. The sequence differences included point mutations restricted largely to the functional domains of SU, i.e., VRA, VRB, and PRR. Despite the sequence differences in these critical domains, measurements of receptor utilization, including host range and superinfection interference, confirmed the assignment of FeLV-945 to subgroup A. Other proviruses isolated from the cohort contained similar sequence hallmarks and were assigned to FeLV subgroup A. A provirus from cat 1046 contained a histidine-to-proline change at SU residue 6 within an SPHQ motif that was previously identified as a critical mediator of fusion events during virus entry. The 1046 pseudotype virus entered cells only in the presence of the soluble cofactor FeLIX provided in trans, but it retained an ecotropic host range even in the presence of FeLIX. The mutational changes in FeLV-945 were shown to confer significant functional differences compared to prototype FeLV-A viruses. The substitution of FeLV-945 envelope gene sequences for FeLV-A/61E sequences conferred a small but statistically significant replicative advantage in some feline cells. Moreover, substitution of the unique FeLV-945 long terminal repeat and envelope gene for those of FeLV-A/61E altered the disease spectrum entirely, from a thymic lymphoma of a T-cell origin to an as yet uncharacterized multicentric lymphoma that did not contain T cells.
机译:FeLV-945是天然猫白血病病毒(FeLV)变体的代表性分离株,主要存在于地理区域的非T细胞恶性,增生和变性疾病中。 FeLV-945表面糖蛋白(SU)与天然水平可传播的FeLV亚组A(FeLV-A)密切相关,但发现与原型的差异比FeLV-A成员之间的差异更大。序列差异包括点突变,该点突变主要限于SU的功能域,即VRA,VRB和PRR。尽管在这些关键域中存在序列差异,但受体利用率的测量(包括宿主范围和超级感染干扰)仍确认FeLV-945属于亚组A.从队列中分离出的其他前病毒也具有相似的序列特征,并被分配给FeLV亚组。来自猫1046的原病毒在SPHQ基序内的SU残基6处含有一个组氨酸到脯氨酸的变化,该变化先前被确定为病毒进入期间融合事件的关键介体。 1046假型病毒仅在存在反式提供的可溶性辅因子FeLIX的情况下才进入细胞,但即使在FeLIX的存在下,它也保留了亲环境宿主范围。与原型FeLV-A病毒相比,FeLV-945中的突变变化显示出显着的功能差异。 FeLV-945包膜基因序列被FeLV-A / 61E序列取代后,在某些猫科动物细胞中具有较小但统计学上显着的复制优势。此外,用独特的FeLV-945长末端重复序列和包膜基因代替FeLV-A / 61E的疾病谱图,从T细胞起源的胸腺淋巴瘤到尚无特征的多中心淋巴瘤,彻底改变了疾病谱T细胞。

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