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Identification of binding sites on the regulatory A subunit of protein phosphatase 2A for the catalytic C subunit and for tumor antigens of simian virus 40 and polyomavirus.

机译:确定蛋白磷酸酶2A的调节性A亚基上催化C亚基以及猿猴病毒40和多瘤病毒的肿瘤抗原的结合位点。

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摘要

Protein phosphatase 2A is composed of three subunits: the catalytic subunit C and two regulatory subunits, A and B. The A subunit consists of 15 nonidentical repeats and has a rodlike shape. It is associated with the B and C subunits as well as with the simian virus 40 small T, polyomavirus small T, and polyomavirus medium T tumor antigens. We determined the binding sites on subunit A for subunit C and tumor antigens by site-directed mutagenesis of A. Twenty-four N- and C-terminal truncations and internal deletions of A were assayed by coimmunoprecipitation for their ability to bind C and tumor antigens. It was found that C binds to repeats 11 to 15 at the C terminus of A, whereas T antigens bind to overlapping but distinct regions of the N terminus. Simian virus 40 small T binds to repeats 3 to 6, and polyomavirus small T and medium T bind to repeats 2 to 8. The data suggest cooperativity between C and T antigens in binding to A. This is most apparent for medium T antigen, which can only bind to those A subunit molecules that provide the entire binding region for the C subunit. We infer from our results that B also binds to N-terminal repeats. A model of the small T/medium T/B-A-C complexes is presented.
机译:蛋白磷酸酶2A由三个亚基组成:催化亚基C和两个调节亚基A和B。A亚基由15个不同的重复序列组成,呈棒状。它与B和C亚基以及猿猴病毒40小T,多瘤病毒小T和多瘤病毒中等T肿瘤抗原相关。我们通过定点诱变A确定了亚基C与肿瘤抗原的亚基A的结合位点。通过免疫共沉淀法测定了A的24个N和C端截短以及A的内部缺失,以分析它们结合C和肿瘤抗原的能力。 。发现C结合在A的C末端的重复11至15,而T抗原结合在N末端的重叠但不同的区域。猿猴病毒40小T结合重复序列3至6,多瘤病毒小T和中等T结合重复序列2至8。数据表明C和T抗原在结合A方面具有协同作用。这对于中等T抗原最为明显,只能结合那些为C亚基提供整个结合区的A亚基分子。从我们的结果推断,B也结合到N-末端重复序列。提出了小型T / T / B-A-C复合物的模型。

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