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从疫苗相关麻痹型脊髓灰质炎病例中分离出的具有天然重组基因组的脊髓灰质炎病毒。

Polioviruses with natural recombinant genomes isolated from vaccine-associated paralytic poliomyelitis.

作者信息

Furione M, Guillot S, Otelea D, Balanant J, Candrea A, Crainic R

机构信息

Unité de Virologie Médicale, Institut Pasteur, Paris, France.

出版信息

Virology. 1993 Sep;196(1):199-208. doi: 10.1006/viro.1993.1468.

Abstract

To determine how oral poliovirus vaccine (Sabin) strains evolve during replication in humans and to confirm the etiology of vaccine-associated paralytic poliomyelitis (VAPP), we examined 70 vaccine-derived strains isolated from VAPP cases. Two distant sequences of the poliovirus genome were targeted for a double restriction fragment length polymorphism assay (RFLP) of reverse-transcribed genomic segments amplified by PCR, an extension of the method that we described previously (Balanant et al., 1991). One (RFLP-1) was a 480-long nucleotide sequence coding for the N-terminal part of the VP1 capsid polypeptide, situated in the 5' third of the viral genome (nucleotides 2401-2880). The other (RFLP-3D1) was a 291-long nucleotide sequence coding for a part of the viral polymerase, situated near the 3' end of the genome (nucleotides 6086-6376). Strain-specific restriction profiles could be generated for different field isolates by using three restriction enzymes in each case: HaeIII, DdeI, and HpaII for RFLP-1 and HaeIII, DdeI and RsaI for RFLP-3D1. With few exceptions, the vaccine-specific RFLP profiles were found to be conserved in both regions during replication of these viruses in humans. Thus, RFLP could be used as a marker so as to identify the origin of viral isolates at both ends of their genome. Whether viral isolates were vaccine-derived was determined by using strain-specific monoclonal antibodies and RFLP-1. Among the 70 isolates, 21 of the 43 type 2 strains and 15 of the 22 type 3 strains had a recombinant genome. None of the 5 type 1 Sabin-derived isolates was found to be recombinant. Both intertypic vaccine/vaccine and vaccine/non-vaccine recombinants were detected. Partial nucleotide sequencing confirmed the RFLP results in all cases that were investigated. In one case, it was possible to predict the recombination junction site from the restriction profiles. This site was more precisely localized by sequencing. The C6203 > U nucleotide substitution, which is suspected to contribute to the reversion toward neurovirulence of the attenuated Sabin 1 strain, was detected in almost all the recombinant genomes containing Sabin 1-specific sequences at the 3' extremity. This mutation was detected by identification of the modified RsaI profile in the RFLP-3D1. The results presented in this paper suggest that recombination, alone or together with mutation, might be one of the mechanisms of the reversion toward neurovirulence of attenuated vaccine strains and of the natural evolution of poliovirus.

摘要

为了确定口服脊髓灰质炎疫苗(萨宾株)毒株在人体复制过程中的演变情况,并证实疫苗相关麻痹型脊髓灰质炎(VAPP)的病因,我们检测了从VAPP病例中分离出的70株疫苗衍生毒株。针对脊髓灰质炎病毒基因组的两个远距离序列,进行了逆转录基因组片段的双重限制性片段长度多态性分析(RFLP),该片段通过PCR扩增,是我们之前描述方法的扩展(Balanant等人,1991年)。一个(RFLP - 1)是一个480个核苷酸长的序列,编码VP1衣壳多肽的N端部分,位于病毒基因组的5'三分之一处(核苷酸2401 - 2880)。另一个(RFLP - 3D1)是一个291个核苷酸长的序列,编码病毒聚合酶的一部分,位于基因组的3'端附近(核苷酸6086 - 6376)。通过在每种情况下使用三种限制性内切酶,可为不同的现场分离株生成菌株特异性的限制性图谱:对于RFLP - 1使用HaeIII、DdeI和HpaII,对于RFLP - 3D1使用HaeIII、DdeI和RsaI。除少数例外,发现这些病毒在人体复制过程中,这两个区域的疫苗特异性RFLP图谱都是保守的。因此,RFLP可作为一种标记,用于识别病毒分离株基因组两端的起源。通过使用菌株特异性单克隆抗体和RFLP - 1来确定病毒分离株是否源自疫苗。在这70株分离株中,43株2型毒株中的21株和22株3型毒株中的15株具有重组基因组。5株源自萨宾1型的分离株均未发现是重组的。检测到了型间疫苗/疫苗和疫苗/非疫苗重组体。部分核苷酸测序在所有研究的病例中都证实了RFLP结果。在一个病例中,有可能从限制性图谱预测重组连接位点。通过测序更精确地定位了该位点。C6203>U核苷酸替换,被怀疑有助于减毒的萨宾1型毒株向神经毒力逆转,在几乎所有在3'末端含有萨宾1型特异性序列的重组基因组中都被检测到。通过在RFLP - 3D1中鉴定修饰的RsaI图谱检测到了这种突变。本文给出的结果表明,重组单独或与突变一起,可能是减毒疫苗毒株向神经毒力逆转以及脊髓灰质炎病毒自然进化的机制之一。

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