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RNA 噬菌体Qβ蛋白在医学体外进化中的作用

Function of the RNA Coliphage Qβ Proteins in Medical In Vitro Evolution.

作者信息

Singleton Rana L, Sanders Carrie A, Jones Kevin, Thorington Bobby, Egbo Timothy, Coats Mamie T, Waffo Alain Bopda

机构信息

Department of Biological Sciences, College STEM, 1627 Hall Street, Montgomery, AL 36101, USA.

Center for NanoBiotechnology Research, 1627 Harris Way, Montgomery, AL 36104, USA.

出版信息

Methods Protoc. 2018 May 31;1(2):18. doi: 10.3390/mps1020018.

Abstract

Qβ is a positive (+) single-stranded RNA bacteriophage covered by a 25 nm icosahedral shell. Qβ belongs to the family of Leviviridae and is found throughout the world (bacterial isolates and sewage). The genome of Qβ is about 4.2 kb, coding for four proteins. This genome is surrounded by 180 copies of coat proteins (capsomers) each comprised of 132 residues of amino acids. The other proteins, the subunit II (β) of a replicase, the maturation protein (A) and the read-through or minor coat protein (A), play a key role in phage infection. With the replicase protein, which lacks proofreading activity, as well as its short replication time, and high population size, Qβ phage has attractive features for in vitro evolution. The A protein gene shares the same initiation codon with the coat protein gene and is produced during translation when the coat protein's UGA stop codon triplet (about 400 nucleotides from the initiation) is suppressed by a low level of ribosome misincorporation of tryptophan. Thus, A is termed the read-through protein. This RNA phage platform technology not only serves to display foreign peptides but is also exceptionally suited to address questions about in vitro evolution. The C-terminus of A protein confers to this RNA phage platform an exceptional feature of not only a linker for foreign peptide to be displayed also a model for evolution. This platform was used to present a peptide library of the G-H loop of the capsid region P1 of the foot-and-mouth disease virus (FMDV) called VP1 protein. The library was exposed on the exterior surface of Qβ phages, evolved and selected with the monoclonal antibodies (mAbs) SD6 of the FMDV. These hybrid phages could principally be good candidates for FMDV vaccine development. Separately, the membrane proximal external region (MPER) of human immunodeficiency virus type 1 (HIV-1) epitopes was fused with the A proteins and exposed on the Qβ phage exterior surface. The engineered phages with MPER epitopes were recognized by anti-MPER specific antibodies. This system could be used to overcome the challenge of effective presentation of MPER to the immune system. A key portion of this linear epitope could be randomized and evolved with the Qβ system. Overall, antigens and epitopes of RNA viruses relevant to public health can be randomized, evolved and selected in pools using the proposed Qβ model to overcome their plasticity and the challenge of vaccine development. Major epitopes of a particular virus can be engineered or displayed on the Qβ phage surface and used for vaccine efficacy evaluation, thus avoiding the use of live viruses.

摘要

Qβ是一种正(+)单链RNA噬菌体,被一个25纳米的二十面体外壳所包裹。Qβ属于轻小噬菌体科,在世界各地均有发现(细菌分离株和污水中)。Qβ的基因组约为4.2千碱基对,编码四种蛋白质。该基因组被180个衣壳蛋白(壳粒)拷贝所包围,每个壳粒由132个氨基酸残基组成。其他蛋白质,即复制酶的亚基II(β)、成熟蛋白(A)和通读或次要衣壳蛋白(A),在噬菌体感染中起关键作用。由于缺乏校对活性的复制酶蛋白、其较短的复制时间以及高群体数量,Qβ噬菌体具有适合体外进化的吸引人的特性。A蛋白基因与衣壳蛋白基因共享相同的起始密码子,并且在翻译过程中,当衣壳蛋白的UGA终止密码子三联体(距起始约400个核苷酸)因色氨酸的低水平核糖体错掺入而被抑制时产生。因此,A被称为通读蛋白。这种RNA噬菌体平台技术不仅用于展示外源肽,还特别适合解决有关体外进化的问题。A蛋白的C末端赋予这个RNA噬菌体平台一个特殊的特性,即它不仅是用于展示外源肽的连接子,也是一个进化模型。这个平台被用于展示口蹄疫病毒(FMDV)衣壳区域P1的G-H环的肽库,该肽库被称为VP1蛋白。该库暴露在Qβ噬菌体的外表面,用FMDV的单克隆抗体(mAb)SD6进行进化和筛选。这些杂交噬菌体原则上可能是FMDV疫苗开发的良好候选者。另外,人类免疫缺陷病毒1型(HIV-1)表位的膜近端外部区域(MPER)与A蛋白融合,并暴露在Qβ噬菌体的外表面。带有MPER表位的工程噬菌体被抗MPER特异性抗体识别。这个系统可用于克服将MPER有效呈递给免疫系统的挑战。这个线性表位的一个关键部分可以随机化,并通过Qβ系统进行进化。总体而言,与公共卫生相关的RNA病毒的抗原和表位可以使用所提出的Qβ模型在群体中进行随机化、进化和筛选,以克服它们的可塑性和疫苗开发的挑战。特定病毒的主要表位可以在Qβ噬菌体表面进行工程改造或展示,并用于疫苗效力评估,从而避免使用活病毒。

https://cdn.ncbi.nlm.nih.gov/pmc/blobs/f8d5/6526423/964214b81bbe/mps-01-00018-g001.jpg

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