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An N-Terminal Fragment of Yeast Ribosomal Protein L3 Inhibits the Cytotoxicity of Pokeweed Antiviral Protein in Saccharomyces cerevisiae

机译:酵母核糖体蛋白L3的N末端片段抑制酿酒酵母抗病毒蛋白在啤酒酵母中的细胞毒性。

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We have previously shown that ribosomal protein L3 is required for pokeweed antiviral protein (PAP), a type I ribosome inactivating protein, to bind to ribosomes and depurinate the α-sarcin/ricin loop (SRL) in yeast. Co-expression of the N-terminal 99 amino acids of yeast L3 (L3Δ99) with PAP in transgenic tobacco plants completely abolished the toxicity of PAP. In this study, we investigated the interaction between PAP and L3Δ99 in Saccharomyces cerevisiae. Yeast cells co-transformed with PAP and L3Δ99 showed markedly reduced growth inhibition and reduced rRNA depurination by PAP, compared to cells transformed with PAP alone. Co-transformation of yeast with PAP and L3Δ21 corresponding to the highly conserved N-terminal 21 amino acids of L3Δ99, reduced the cytotoxicity of PAP. PAP mRNA and protein levels were elevated and L3Δ99 or L3Δ21 mRNA and protein levels were reduced in yeast co-transformed with PAP and L3Δ99 or with PAP and L3Δ21, respectively. PAP interacted with L3Δ21 in yeast cells in vivo and by Biacore analysis in vitro, suggesting that the interaction between L3Δ21 and PAP may inhibit PAP-mediated depurination of the SRL, leading to a reduction in the cytotoxicity of PAP.
机译:先前我们已经证明,商陆抗病毒蛋白(PAP)是I型核糖体失活蛋白,需要核糖体蛋白L3才能与核糖体结合并使酵母中的α-sarcin/ ricin环(SRL)脱嘌呤化。酵母L3(L3Δ99)的N末端99个氨基酸与PAP在转基因烟草植物中的共表达完全消除了PAP的毒性。在这项研究中,我们调查了酿酒酵母中PAP和L3Δ99之间的相互作用。与仅用PAP转化的细胞相比,用PAP和L3Δ99共转化的酵母细胞显示出生长抑制显着降低,并且rAP对rRNA的净化作用降低。酵母与PAP和L3Δ21的共转化(对应于L3Δ99的高度保守的N端21个氨基酸)降低了PAP的细胞毒性。在分别用PAP和L3Δ99或用PAP和L3Δ21共转化的酵母中,PAP mRNA和蛋白水平升高,而L3Δ99或L3Δ21mRNA和蛋白水平降低。 PAP在体内和体外通过Biacore分析与酵母细胞中的L3Δ21相互作用,这表明L3Δ21与PAP之间的相互作用可能抑制PAP介导的SRL的脱嘌呤,从而降低PAP的细胞毒性。

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