首页> 外文期刊>Journal of child science. >Group A Rotavirus G1P[6] Associated Fatalities in Diarrheic Nigerian Infants, Possible Impact of Enterovirus Environmental Enteric Dysfunction, and Implications for Rota-Vaccinology
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Group A Rotavirus G1P[6] Associated Fatalities in Diarrheic Nigerian Infants, Possible Impact of Enterovirus Environmental Enteric Dysfunction, and Implications for Rota-Vaccinology

机译:组RotaVirus G1p [6]腹泻尼日利亚婴儿的病症,肠道病毒环境肠道功能障碍的可能影响,以及对罗拉疫苗学的影响

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Abstract Group A rotavirus (RVA) diarrhea disease and mortality are yet unabated, particularly in developing countries. As global knowledge of specific strains associated with infant mortality is crucial for successful vaccination efforts, candidate RVA strains detected in mortality and fatal cases of severely diarrheic hospitalized infants in Akure, Nigeria were investigated.Fecal samples from comatose patients were tested for RVAs, other diarrhea viruses, and enteric bacterial pathogens. Genomic dsRNA was extracted from 10% rotavirus positive stool suspension, the VP4 and VP7 genes were reverse transcribed and amplified by one-step reverse transcription polymerase chain reaction (PCR) and genotyped by seminested multiplex PCR. Amplicons were sequenced, aligned by ClustalW, and phylogenetic analyses were conducted in MEGA6. Sequences data were deposited to GenBank and DDBJ.Medical examination and microbiological analyses upheld viral diarrhea. EIA revealed RVA and enterovirus. PCR identified virulent RVA strain GIP[6] whose VP7 nucleotide sequences shared a common cluster with Cuban isolate G1P[6], while the VP4 P[6] sequences were related to Asian strains. Reassortant RVA G1P[6] was found in fatal diarrhea cases and mortality of a Nigerian child. RVA coinfection with enterovirus and associated biomarkers of environmental enteric dysfunction in infantile diarrhea should henceforth be evaluated. Current rotavirus vaccines may fare badly against the prevailing virulent strains. The disease severity and outcome necessitates a wider epidemiological study, a review and inclusion of the P[6] genotype in future rotavirus vaccines.
机译:摘要群体RotaVirus(RVA)腹泻病和死亡率尚未发达,特别是在发展中国家。随着与婴儿死亡相关的特定菌株的全球知识对于成功的疫苗接种努力至关重要,研究了在尼日利亚的严重疫苗接种效力中检测到患有严重腹泻住院婴儿的候选RVA菌株,尼日利亚的患者患有尼日利亚。昏迷患者的次数对户RVA进行了测试,其他腹泻病毒和肠道细菌病原体。从10%轮状病毒阳性粪便悬浮液中提取基因组dsRNA,通过一步逆转录聚合酶链反应(PCR)逆转录并扩增,并通过半精化多重PCR进行基因分型。通过CLUSTALW对齐进行扩增子,并在MEGA6中进行系统发育分析。序列数据被沉积在Genbank和DDBJ.Medical检查和微生物分析的软化性病毒腹泻。 EIA揭示了RVA和肠道病毒。 PCR鉴定的毒力RVA菌株GIP [6],其VP7核苷酸序列与古巴分离G1p [6]共享常见群,而VP4 P [6]序列与亚洲菌株有关。重新排列RVA G1P [6]在致命的腹泻病例和尼日利亚儿童的死亡率中发现。应评估与肠道病毒和婴儿腹泻的相关生物标志物的RVA杂交应得到评估。目前的轮状病毒疫苗可能对普遍的毒力菌株造成严重票价。疾病严重程度和结果需要更广泛的流行病学研究,综述和在未来轮状病毒疫苗中的P [6]基因型。

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