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Second generation antitumour human RNase: significance of its structural and functional features for the mechanism of antitumour action

机译:第二代抗肿瘤人类核糖核酸酶:其结构和功能特征对抗肿瘤作用机制的意义

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pA second generation mutant of dimeric human pancreas RNase (HHP2-RNase), was obtained by a single residue mutation (Glusup111/sup → Gly) of the previously described dimeric human pancreas RNase variant (HHP-RNase). HHP2-RNase was found to be a highly specific antitumour agent, with an enhanced cytotoxic activity compared with HHP-RNase. The structural and functional requisites of the antitumour action of HHP2-RNase were investigated and compared with those of other dimeric antitumour RNases. The stability of the dimeric structure, i.e. the resistance of human dimeric RNase variants to reductive cleavage of the two intersubunit disulphide bonds that bridge the subunits, was determined to be an essential feature of antitumour dimeric RNases. The stability of the dimeric structure is in turn responsible for the resistance to inhibition by the cytosolic RNase inhibitor (cRI). Both the stability of the dimeric structure and the resistance to cRI inhibition appeared to be highly enhanced by an RNase substrate. This suggests a possible role for RNA in the amplification of the antitumour potential of dimeric RNases./p
机译:>二聚人胰腺RNase(HHP2-RNase)的第二代突变体是通过先前描述的二聚人胰腺RNase变异体(HHP--)的单残基突变(Glu 111 →Gly)获得的RNase)。发现HHP2-RNase是高度特异性的抗肿瘤剂,与HHP-RNase相比具有增强的细胞毒性活性。研究了HHP2-RNase抗肿瘤作用的结构和功能要求,并将其与其他二聚体抗肿瘤RNase进行了比较。二聚体结构的稳定性,即人二聚体RNase变体对桥接该亚基的两个亚基间二硫键的还原裂解的抗性被确定为抗肿瘤二聚体RNase的基本特征。二聚体结构的稳定性继而引起对胞质RNase抑制剂(cRI)抑制的抗性。二聚体结构的稳定性和对cRI抑制的抵抗力似乎都被RNase底物大大增强了。这表明RNA可能在二聚RNase的抗肿瘤潜力的扩增中发挥作用。

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