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首页> 外文期刊>Journal of Virology >Nonidentity of Some Simian Virus 40-induced Enzymes with Tumor Antigen
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Nonidentity of Some Simian Virus 40-induced Enzymes with Tumor Antigen

机译:一些Simian病毒40诱导酶与肿瘤抗原的非鉴定性

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摘要

The complement-fixing tumor (T) antigen induced by simian virus 40 (SV40) has been prepared from SV40-infected cell cultures, from infected cell cultures treated at the time of infection with 1-β-d-arabinofuranosylcytosine (ara-C), and from SV40-transformed cells. Upon partial purification, the T antigen exhibited the following properties: it was tightly adsorbed by calcium phosphate gel, it was precipitated by acetic acid at pH 5 or by ammonium sulfate at about 20 to 32% saturation, and it had a molecular weight greater than 250,000, as estimated by Sephadex G-200 gel chromatography. In contrast, deoxycytidylate (dCMP) deaminase, thymidylate (dTMP) kinase, and thymidine (dT) kinase were less strongly bound to calcium phosphate and were not precipitated at pH 5; these enzymes also had much lower molecular weights than the T antigen, as did dihydrofolic (FH2) reductase. Furthermore, higher ammonium sulfate concentrations were required to precipitate dCMP deaminase, dTMP kinase, and FH2 reductase activities than to precipitate the T antigen. Another difference was that the T antigen was not stabilized, but dCMP deaminase, dTMP kinase, and dT kinase, were stabilized, respectively, by dCTP, dTMP, and dT or dTTP. Deoxyribonucleic acid (DNA) polymerase activity resembled the T antigen in adsorption to calcium phosphate, in precipitation by ammonium sulfate or at pH 5, and in the rate of inactivation when incubated at 38 C. However, the polymerase activity could be partly separated from the T antigen by Sephadex G-200 gel chromatography. The cell fraction containing partially purified T antigen also contained a soluble complement-fixing antigen (presumably a subunit of the viral capsid) which reacted with hyperimmune monkey sera. The latter antigen was present in very low titers or absent from cell extracts prepared from SV40-infected monkey kidney cell cultures which had been treated with ara-C at the time of infection, or from SV40-transformed mouse kidney (mKS) or hamster tumor (H-50) cells. The T antigen, however, was present in usual amounts in SV40-transformed cells or ara-C treated, infected cells.
机译:由Simian病毒40(SV40)诱导的补体固定肿瘤(T)抗原由SV40感染的细胞培养物制备,来自感染在感染时处理的感染细胞培养物与1-β-D-Arabinofuranylylylys(ARA-C)处理,来自SV40转化的细胞。在局部纯化后,T抗原表现出下列性质:它用磷酸钙凝胶紧密吸附,通过乙酸在 P H 5中沉淀,或通过硫酸铵在约20至32%的饱和度下沉淀,它的分子量大于250,000,如Sephadex G-200凝胶色谱估计。相比之下,脱氧胞苷(DCMP)脱氨酶,胸酰替酯(DTMP)激酶和胸苷(DT)激酶对磷酸钙的强烈结合,并且在 P H 5中沉淀出来;这些酶的分子量比T抗原也大得多,如二氢摩洛(FH 2 )还原酶。此外,需要较高的硫酸铵浓度来沉淀DCMP脱氨酶,DTMP激酶和FH 2 /亚>还原酶活性,而不是沉淀T抗原。另一个不同之处在于,T抗原未稳定,但DCMP脱氨酶,DTMP激酶和DT激酶分别通过DCTP,DTMP和DT或DTTP稳定。脱氧核糖核酸(DNA)聚合酶活性类似于吸附于磷酸钙的T抗原,硫酸铵沉淀或在 p H 5中,并在38℃温育时灭活的速率。然而,通过Sephadex G-200凝胶色谱法将聚合酶活性部分分离与T抗原分离。含有部分纯化的T抗原的细胞级分也含有可溶的补体固定抗原(大概是病毒衣壳的亚基),其与超免疫猴血清反应。后一种抗原存在于非常低的滴度中或不存在于由SV40感染的猴肾细胞培养物制备的细胞提取物,其在感染时用ARA-C处理,或来自SV40转化的小鼠肾(MKS)或仓鼠肿瘤(H-50)细胞。然而,T抗原在SV40转化的细胞或ARA-C处理的感染细胞中以通常的量存在。

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