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首页> 外文期刊>Applied biochemistry and biotechnology, Part A. enzyme engineering and biotechnology >Enhanced Anti-Tumor (Anti-Proliferation) Activity of Recombinant Human Interleukin-29 (IL-29) Mutants Using Site-Directed Mutagenesis Method
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Enhanced Anti-Tumor (Anti-Proliferation) Activity of Recombinant Human Interleukin-29 (IL-29) Mutants Using Site-Directed Mutagenesis Method

机译:使用定点诱变方法增强重组人白介素29(IL-29)突变体的抗肿瘤(抗增殖)活性

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摘要

Interferon (IFN)-lambda, also known as IL-28A, IL-28B, or IL-29, is a new type III IFN, which shares many functional characteristics with type I IFN (alpha/beta). Currently, IFN-alpha is used in the treatment of certain forms of cancer with severe adverse effects. Some researches had stated that IFN-lambda s induced a similar but restricted growth inhibition of tumor cells relative to IFN-alpha; moreover, mutations of IFN-lambda s could strongly impact its biological properties. In this study, three hIL-29 mutants (K33R, R35K, and K33R/R35K) were generated by site-directed mutagenesis and efficiently expressed in Pichia pastoris GS115, which have considerable abilities to inhibit the growth of BEL-7402, HCT-8, and SGC-7901 tumor cells in vitro. The results showed that these mutants (K33R, R35K, and K33R/R35K) exhibited a significantly enhanced anti-proliferation activity against these tumor cells, compared with native hIL-29 in vitro. Further assay in vitro indicated that superior to K33R and R35K, K33R/R35K had a significant increase in anti-tumor activity compared with IFN-alpha 2b, which suggested that the K33R/R35K could make improvement for the effectiveness of native hIL-29 in clinic and could be used as a potentially powerful candidate for cancer immunotherapy.
机译:干扰素(IFN)-λ,也称为IL-28A,IL-28B或IL-29,是一种新型的III型IFN,与I型IFN(alpha / beta)具有许多功能特征。目前,IFN-α用于治疗某些形式的具有严重不良反应的癌症。一些研究表明,相对于IFN-α,IFN-λ诱导了类似但受限的肿瘤细胞生长抑制。此外,IFN-λ的突变可能强烈影响其生物学特性。在这项研究中,通过定点诱变产生了三个hIL-29突变体(K33R,R35K和K33R / R35K)并在毕赤酵母GS115中有效表达,它们具有相当大的抑制BEL-7402,HCT-8生长的能力。和SGC-7901体外肿瘤细胞。结果表明,与体外hIL-29相比,这些突变体(K33R,R35K和K33R / R35K)对这些肿瘤细胞表现出显着增强的抗增殖活性。进一步的体外试验表明,与IFN-alpha 2b相比,K33R / R35K优于K33R和R35K,其抗肿瘤活性显着提高,这表明K33R / R35K可以改善天然hIL-29的抗肿瘤活性。可以用作癌症免疫疗法的潜在强大候选药物。

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