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多瘤病毒中间肿瘤抗原的一个亚类与DNA纤维素结合。

A subclass of polyomavirus middle tumor antigen binds to DNA cellulose.

作者信息

Bolen J B, Cary K, Scheller A, Basilico C, Israel M A, Prives C

出版信息

J Virol. 1986 Apr;58(1):157-64. doi: 10.1128/JVI.58.1.157-164.1986.

Abstract

We examined the binding of polyomavirus large (L-T)-, middle (M-T)-, and small-tumor antigens to DNA cellulose. At pH 6.0, the majority of L-T bound to calf thymus DNA cellulose, while little or no small tumor antigen was retained under these conditions. Unexpectedly, a small but reproducible proportion of M-T bound to both native and denatured DNA cellulose. M-T encoded by polyomavirus mutant dl 8, which expressed shortened L-T and M-T, bound to DNA, indicating that the deleted sequences are not required for DNA binding. Also, M-T from transformed BMT-1 rat cells, which synthesize exclusively this polyomavirus tumor antigen, bound to DNA, indicating that its binding is not due to association with other polyomavirus-encoded proteins. Using the DNA fragment immunoassay, we found that, under conditions in which L-T bound specifically to DNA fragments containing viral regulatory sequences, no viral DNA fragments were bound by M-T. The existence of distinct subpopulations of M-T that differ in their DNA-binding properties was indicated by rebinding experiments in which M-T that had bound to DNA cellulose rebound very efficiently, while that which had not been originally retained by DNA cellulose rebound poorly. Furthermore, the M-T-pp60 c-src complex did not bind to DNA cellulose. These data suggest that polyomavirus M-T is heterogeneous, consisting of populations of molecules that differ in their interactions with DNA cellulose.

摘要

我们检测了多瘤病毒大(L-T)、中(M-T)和小肿瘤抗原与DNA纤维素的结合情况。在pH 6.0时,大多数L-T与小牛胸腺DNA纤维素结合,而在此条件下小肿瘤抗原很少或没有被保留。出乎意料的是,一小部分但可重复比例的M-T与天然和变性的DNA纤维素都结合。由多瘤病毒突变体dl 8编码的M-T,其表达缩短的L-T和M-T,能与DNA结合,这表明缺失的序列对于DNA结合并非必需。此外,来自转化的BMT-1大鼠细胞的M-T,其仅合成这种多瘤病毒肿瘤抗原,也能与DNA结合,这表明其结合并非由于与其他多瘤病毒编码蛋白的关联。使用DNA片段免疫测定法,我们发现,在L-T特异性结合含有病毒调控序列的DNA片段的条件下,没有病毒DNA片段能被M-T结合。重新结合实验表明存在DNA结合特性不同的M-T不同亚群,其中已与DNA纤维素结合的M-T能非常有效地重新结合,而最初未被DNA纤维素保留的M-T则重新结合较差。此外,M-T-pp60 c-src复合物不与DNA纤维素结合。这些数据表明多瘤病毒M-T是异质的,由与DNA纤维素相互作用不同的分子群体组成。

https://cdn.ncbi.nlm.nih.gov/pmc/blobs/08aa/252888/b2cd5ea35a52/jvirol00109-0167-a.jpg

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