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通过非放射性同位素分子分析定量基因组变化来评估脊髓灰质炎病毒的神经毒力。

Estimation of the neurovirulence of poliovirus by non-radioisotope molecular analysis to quantify genomic changes.

作者信息

Horie H, Tano Y, Doi Y, Hashizume S

机构信息

Japan Poliomyelitis Research Institute, Tokyo, Japan.

出版信息

Biologicals. 1998 Dec;26(4):289-97. doi: 10.1006/biol.1998.0159.

Abstract

Mutant analysis by polymerase chain reaction and restriction enzyme cleavage (MAPREC) has been developed for poliovirus to determine quantitatively for the presence of genomic changes in particular nucleotide sequences correlate with the characteristic of neurovirulence for monkeys. Currently the MAPREC is scheduled to be used as a routine safety test for oral poliomyelitis vaccine (OPV). Radioisotopes (RI) are used in MAPREC for quantitative determinations, a circumstance likely to limit its use. We investigated the possibility of developing a modified MAPREC, which did not require the use of radioisotopes, and developed a procedure designated NON-RI MAPREC. Conventional MAPREC and NON-RI MAPREC were then used in a series of studies in which analyses were performed on Sabin type 1 and Sabin type 3 attenuated vaccine polioviruses prepared under various conditions. Under the experimental conditions used, the stability of the genome of type 1 virus was shown to be markedly greater than that of the type 3 virus, and the frequency of mutants was observed to vary in relation to both the virus strain and the virus inoculum used. The results of the studies relating to the two analytical procedures used indicated that the reproducibility of both methods was of a similarly high order, but that MAPREC had a somewhat broader range of sensitivity than NON-RI MAPREC. As the quantity of genomic changes in OPV relating to neurovirulent properties are within the range of detection by NON-RI MAPREC, this procedure can be used as a quality control test for OPV.

摘要

聚合酶链反应和限制性内切酶切割突变分析(MAPREC)已被开发用于脊髓灰质炎病毒,以定量确定特定核苷酸序列中的基因组变化,这些变化与猴子的神经毒力特征相关。目前,MAPREC计划用作口服脊髓灰质炎疫苗(OPV)的常规安全性测试。MAPREC中使用放射性同位素(RI)进行定量测定,这种情况可能会限制其使用。我们研究了开发一种改良的MAPREC的可能性,这种方法不需要使用放射性同位素,并开发了一种称为非放射性同位素MAPREC的程序。然后,在一系列研究中使用传统的MAPREC和非放射性同位素MAPREC,对在各种条件下制备的1型和3型减毒疫苗脊髓灰质炎病毒进行分析。在所使用的实验条件下,1型病毒基因组的稳定性明显高于3型病毒,并且观察到突变体的频率因病毒株和所用病毒接种物而异。与所使用的两种分析程序相关的研究结果表明,两种方法的重现性都处于相似的高水平,但MAPREC的灵敏度范围比非放射性同位素MAPREC略宽。由于OPV中与神经毒力特性相关的基因组变化量在非放射性同位素MAPREC的检测范围内,因此该程序可作为OPV的质量控制测试。

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