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HCPro 两个氨基酸的适应性替换分别修饰了其功能特性,从而提高了马铃薯 Y 病毒嵌合体的毒力。

Adaptive substitutions at two amino acids of HCPro modify its functional properties to separately increase the virulence of a potyviral chimera.

机构信息

Department of Microbial and Plant Biotechnology, Margarita Salas Center for Biological Research (CIB), Spanish National Research Council, CSIC, Madrid, Spain.

Laboratory of Molecular Genetics, Immunology and Biotechnology, Faculty of Sciences, University of Tunis El Manar, Tunis, Tunisia.

出版信息

Mol Plant Pathol. 2024 Jun;25(6):e13487. doi: 10.1111/mpp.13487.

Abstract

We had previously reported that a plum pox virus (PPV)-based chimera that had its P1-HCPro bi-cistron replaced by a modified one from potato virus Y (PVY) increased its virulence in some Nicotiana benthamiana plants, after mechanical passages. This correlated with the natural acquisition of amino acid substitutions in several proteins, including in HCPro at either position 352 (Ile→Thr) or 454 (Leu→Arg), or of mutations in non-coding regions. Thr in position 352 is not found among natural potyviruses, while Arg in 454 is a reversion to the native PVY HCPro amino acid. We show here that both mutations separately contributed to the increased virulence observed in the passaged chimeras that acquired them, and that Thr in position 352 is no intragenic suppressor to a Leu in position 454, because their combined effects were cumulative. We demonstrate that Arg in position 454 improved HCPro autocatalytic cleavage, while Thr in position 352 increased its accumulation and the silencing suppression of a reporter in agropatch assays. We assessed infection by four cloned chimera variants expressing HCPro with none of the two substitutions, one of them or both, in wild-type versus DCL2/4-silenced transgenic plants. We found that during infection, the transgenic context of altered small RNAs affected the accumulation of the four HCPro variants differently and hence, also infection virulence.

摘要

我们之前曾报道过,一种基于李痘病毒(PPV)的嵌合体,其 P1-HCPro 双顺反子被来自马铃薯 Y 病毒(PVY)的修饰序列所取代,在机械传递后,其在一些本氏烟植株中的毒力增加。这与包括 HCPro 第 352 位(Ile→Thr)或 454 位(Leu→Arg)氨基酸取代在内的几种蛋白的自然获得以及非编码区突变有关。第 352 位的 Thr 不在天然的 potyviruses 中发现,而 454 位的 Arg 是对天然 PVY HCPro 氨基酸的回复。我们在这里表明,这两个突变分别导致了获得它们的传代嵌合体中观察到的毒力增加,并且 454 位的 Thr 不是 454 位 Leu 的基因内抑制物,因为它们的共同作用是累积的。我们证明 454 位的 Arg 提高了 HCPro 的自我切割,而 352 位的 Thr 增加了其积累和在 agro-patch 测定中报告基因的沉默抑制。我们评估了四个表达 HCPro 的克隆嵌合体变体在野生型和 DCL2/4 沉默的转基因植物中的感染情况,这些变体均不表达这两个突变、其中一个突变或两个突变。我们发现,在感染过程中,改变的小 RNA 的转基因背景对四种 HCPro 变体的积累产生了不同的影响,因此也影响了感染的毒力。

https://cdn.ncbi.nlm.nih.gov/pmc/blobs/ec15/11178974/2bea5d0808cd/MPP-25-e13487-g005.jpg

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