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多瘤病毒中T抗原:一种肿瘤进展因子。

Polyoma virus middle t antigen: a tumor progression factor.

作者信息

Seif R

出版信息

J Virol. 1980 Aug;35(2):479-87. doi: 10.1128/JVI.35.2.479-487.1980.

Abstract

Polyoma virus (PyV) deletion mutant dl23 (affecting both large T and middle t but not small t antigens) was used to study transformation of 3T3 rat cells. This mutant generated stable transformants in the agar assay at a frequency similar to that of wild-type virus (WT). However, WT-induced transformants were detected 3 weeks after infection, whereas those induced by the mutant could not be detected until 6 to 8 weeks after infection. In this respect, dl23 PyV behaved like WT simian virus 40 (SV40). Cells transformed by WT SV40 or by dl23 PyV were similar in all their transformed properties. Those transformed by WT PyV were different from the others on the basis of morphology, cell adhesion to the substrate, release of protease activity, efficiency of doubling in agar, growth rate, and time required for tumor formation. Saturation density, the ability to grow in agar, the serum requirement for cloning, and the ability to grow on a cell monolayer were similar for all transformants. Middle t antigen enhanced membrane alterations and growth rate of the transformed cells, shortening the time required for tumor formation in rats.

摘要

多瘤病毒(PyV)缺失突变体dl23(影响大T抗原和中T抗原,但不影响小T抗原)被用于研究3T3大鼠细胞的转化。该突变体在琼脂试验中产生稳定转化体的频率与野生型病毒(WT)相似。然而,WT诱导的转化体在感染后3周即可检测到,而突变体诱导的转化体直到感染后6至8周才能检测到。在这方面,dl23 PyV的表现与WT猴病毒40(SV40)相似。WT SV40或dl23 PyV转化的细胞在所有转化特性上都相似。WT PyV转化的细胞在形态、细胞与底物的粘附、蛋白酶活性的释放、琼脂中倍增效率、生长速率以及肿瘤形成所需时间等方面与其他细胞不同。所有转化体的饱和密度、在琼脂中生长的能力、克隆所需的血清以及在细胞单层上生长的能力相似。中T抗原增强了转化细胞的膜改变和生长速率,缩短了大鼠肿瘤形成所需的时间。

https://cdn.ncbi.nlm.nih.gov/pmc/blobs/1336/288833/911963466857/jvirol00176-0214-a.jpg

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