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Native-State Stability Determines the Extent of Degradation Relative to Secretion of Protein Variants from Pichia pastoris

机译:原始状态的稳定性确定相对于巴斯德毕赤酵母蛋白质变体分泌的降解程度

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摘要

We have investigated the relationship between the stability and secreted yield of a series of mutational variants of human lysozyme (HuL) in Pichia pastoris. We show that genes directly involved in the unfolded protein response (UPR), ER-associated degradation (ERAD) and ER-phagy are transcriptionally up-regulated more quickly and to higher levels in response to expression of more highly-destabilised HuL variants and those variants are secreted to lower yield. We also show that the less stable variants are retained within the cell and may also be targeted for degradation. To explore the relationship between stability and secretion further, two different single-chain-variable-fragment (scFv) antibodies were also expressed in P. pastoris, but only one of the scFvs gave rise to secreted protein. The non-secreted scFv was detected within the cell and the UPR indicators were pronounced, as they were for the poorly-secreted HuL variants. The non-secreted scFv was modified by changing either the framework regions or the linker to improve the predicted stability of the scFv and secretion was then achieved and the levels of UPR indicators were lowered Our data support the hypothesis that less stable proteins are targeted for degradation over secretion and that this accounts for the decrease in the yields observed. We discuss the secretion of proteins in relation to lysozyme amyloidosis, in particular, and optimised protein secretion, in general.
机译:我们研究了人类溶菌酶(HuL)在毕赤酵母中的一系列突变变体的稳定性与分泌产量之间的关系。我们显示直接参与未折叠的蛋白应答(UPR),ER相关降解(ERAD)和ER噬菌体的基因在转录上的上调速度更快,响应于高度不稳定的HuL变体和那些表达异常的表达水平也更高变体被分泌以降低产量。我们还表明,稳定性较差的变体保留在细胞内,也可能靶向降解。为了进一步探讨稳定性与分泌之间的关系,在巴斯德毕赤酵母中还表达了两种不同的单链可变片段(scFv)抗体,但只有一种scFv产生了分泌的蛋白质。在细胞内检测到非分泌的scFv,并且显着说明了UPR指标,因为它们是针对分泌较弱的HuL变体。通过改变构架区或接头来修饰非分泌的scFv,以提高scFv的预测稳定性,然后实现分泌,降低UPR指标的水平。我们的数据支持以下假设:稳定性较弱的蛋白质可用于降解分泌过多,这说明观察到的产量下降。我们讨论与溶菌酶淀粉样变性有关的蛋白质的分泌,尤其是与优化的蛋白质分泌有关。

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