vibriocidal

杀弧菌
  • 文章类型: Journal Article
    在霍乱缺席多年之后,2022年10月在海地爆发了霍乱弧菌O1。在2021年血清调查的样本中,我们在<5岁的儿童中发现了较低的循环抗霍乱弧菌脂多糖抗体,并且没有抗弧菌抗体。表明对霍乱的高度易感性,尤其是在年幼的孩子中。
    A Vibrio cholerae O1 outbreak emerged in Haiti in October 2022 after years of cholera absence. In samples from a 2021 serosurvey, we found lower circulating antibodies against V. cholerae lipopolysaccharide in children <5 years of age and no vibriocidal antibodies, suggesting high susceptibility to cholera, especially among young children.
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  • 文章类型: Preprint
    在海地没有确诊霍乱病例三年后,2022年10月爆发霍乱弧菌O1。预先存在的抗体水平提供了对先前免疫暴露的估计,揭示潜在相关的免疫反应,并为未来的血清监测设定基线。我们分析了2021年从海地Ouest省两个社区的人口加权代表性横断面血清调查中收集的干血点。我们发现针对霍乱弧菌脂多糖的循环IgG和IgA抗体水平较低(LPS,与5岁及以上的人群相比,5岁以下的人群中的IgG和IgAp<0.0001)。在抗体滴度较高的患者中,我们无法检测到任何功能性(杀弧菌)抗体。总之,缺乏可检测的功能性抗体,和年龄不一致的霍乱弧菌LPSIgG水平,表明海地的人口可能高度易患霍乱病,尤其是在年幼的孩子中。
    After three years with no confirmed cholera cases in Haiti, an outbreak of Vibrio cholerae O1 emerged in October 2022. Levels of pre-existing antibodies provide an estimate of prior immunologic exposure, reveal potentially relevant immune responses, and set a baseline for future serosurveillance. We analyzed dried blood spots collected in 2021 from a population-weighted representative cross-sectional serosurvey in two communes in the Ouest Department of Haiti. We found lower levels of circulating IgG and IgA antibodies against V. cholerae lipopolysaccharide (LPS, IgG and IgA p<0.0001) in those below 5 years of age compared to those five years and older. Among a subset of patients with higher titers of antibodies, we were unable to detect any functional (vibriocidal) antibodies. In conclusion, the lack of detectable functional antibodies, and age-discordant levels of V. cholerae LPS IgG, suggest that populations in Haiti may be highly susceptible to cholera disease, especially among young children.
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  • 文章类型: Journal Article
    全世界每年约有290万人患有霍乱。他们中的许多人是贫困的。然而,对霍乱免疫力的了解仍然有限。一些研究报道了霍乱后抗体的持续时间;然而,缺乏包括定量综合在内的系统评价。
    对评估了杀弧菌的队列研究进行荟萃分析,霍乱毒素B亚基(CTB),和临床霍乱病例后的脂多糖(LPS)抗体水平。
    设计:系统评价和荟萃分析。我们搜索了PubMed和Webofscience,以评估临床霍乱患者队列中抗霍乱弧菌抗体的研究。两位作者独立提取数据并评估纳入研究的质量。随机效应模型用于汇集成人和年龄较大的儿童(年龄≥6岁)的抗体滴度。在敏感性分析中,纳入了报告幼儿(2~5岁)数据的研究.
    9项研究符合我们系统评价的纳入标准,7项研究符合荟萃分析的纳入标准。在症状发作后第2天,成人和年龄较大的儿童(年龄≥6岁)的抗弧菌抗体滴度的合并平均值为123,在第7天急剧增加(合并平均值=6956),并在第30天逐渐减弱至2247,在第90天逐渐减弱至578,在第360天逐渐减弱至177。抗CTBIgA抗体也在第7天达到峰值(合并平均值=49),随后在第30天迅速下降(合并平均值=21),在第90天进一步下降(合并平均值=10),此后从第180天(合并平均值=8)稳定到360天(合并平均值=6)。同样,抗CTBIgG抗体在第7天(合并平均值=65)和第30天(合并平均值=69)之间的早期康复中达到峰值,然后在第90天(合并平均值=42)和第180天(合并平均值=30)逐渐减弱,并在第360天(合并平均值=24)恢复至基线.抗LPSIgA抗体在第7天达到峰值(合并平均值=124),在第30天逐渐下降(合并平均值=44),一直持续到第360天(合并平均值=10)。抗LPSIgG抗体在第7天达到峰值(合并平均值=94)。此后,它们在第30天下降(合并平均值=85),在第90天(合并平均值=51)和第180天(合并平均值=47)进一步下降,并在第360天返回基线(合并平均值=32)。包括来自幼儿(2-5岁)的数据在内的敏感性分析显示出与主要分析非常相似的发现。
    这项研究证实了血清学抗体(杀弧菌,CTB,和LPS)滴度在临床霍乱后1年内恢复到基线水平,即,在针对随后的霍乱的保护性免疫力减弱之前。然而,这种衰变不应被解释为免疫力下降,因为霍乱对随后疾病的免疫力持续3-10年。我们的研究为疫苗的监测策略和未来研究提供了证据,也表明需要进一步研究以提高我们对霍乱免疫的理解。
    Approximately 2.9 million people worldwide suffer from cholera each year, many of whom are destitute. However, understanding of immunity against cholera is still limited. Several studies have reported the duration of antibodies following cholera; however, systematic reviews including a quantitative synthesis are lacking.
    To meta-analyze cohort studies that have evaluated vibriocidal, cholera toxin B subunit (CTB), and lipopolysaccharide (LPS) antibody levels following a clinical cholera case.
    Design: Systematic review and meta-analysis. We searched PubMed and Web of science for studies assessing antibodies against Vibrio cholerae in cohorts of patients with clinical cholera. Two authors independently extracted data and assessed the quality of included studies. Random effects models were used to pool antibody titers in adults and older children (aged ≥ 6 years). In sensitivity analysis, studies reporting data on young children (2-5 years) were included.
    Nine studies met our inclusion criteria for systematic review and seven for meta-analysis. The pooled mean of vibriocidal antibody titers in adults and older children (aged ≥ 6 years) was 123 on day 2 post-symptom onset, which sharply increased on day 7 (pooled mean = 6956) and gradually waned to 2247 on day 30, 578 on day 90, and 177 on day 360. Anti-CTB IgA antibodies also peaked on day 7 (pooled mean = 49), followed by a rapid decrease on day 30 (pooled mean = 21), and further declined on day 90 (pooled mean = 10), after which it plateaued from day 180 (pooled mean = 8) to 360 (pooled mean = 6). Similarly, anti-CTB IgG antibodies peaked in early convalescence between days 7 (pooled mean = 65) and 30 (pooled mean = 69), then gradually waned on days 90 (pooled mean = 42) and 180 (pooled mean = 30) and returned to baseline on day 360 (pooled mean = 24). Anti-LPS IgA antibodies peaked on day 7 (pooled mean = 124), gradually declined on day 30 (pooled mean = 44), which persisted until day 360 (pooled mean = 10). Anti LPS IgG antibodies peaked on day 7 (pooled mean = 94). Thereafter, they decreased on day 30 (pooled mean = 85), and dropped further on days 90 (pooled mean = 51) and 180 (pooled mean = 47), and returned to baseline on day 360 (pooled mean = 32). Sensitivity analysis including data from young children (aged 2-5 years) showed very similar findings as in the primary analysis.
    This study confirms that serological antibody (vibriocidal, CTB, and LPS) titers return to baseline levels within 1 year following clinical cholera, i.e., before the protective immunity against subsequent cholera wanes. However, this decay should not be interpreted as waning immunity because immunity conferred by cholera against subsequent disease lasts 3-10 years. Our study provides evidence for surveillance strategies and future research on vaccines and also demonstrates the need for further studies to improve our understanding of immunity against cholera.
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  • 文章类型: Journal Article
    A glycoconjugate construct was based on attachment of V. cholerae O139 hydrazine-treated lipopolysaccharide (LPS) to carboxylated bovine serum albumin (CBSA) via its amino group. The immunological properties of the glycoconjugate were tested using BALB/c mice, injected subcutaneously without any adjuvant three times at 2 weeks interval. The immunogenicity of the conjugate was estimated by enzyme-linked immunosorbent assay, testing of anti-LPS IgG, IgM, and IgA antibodies. The conjugate elicited a statistically significant increase of LPS-specific IgG levels in mice (p < 0.001). The specific anti-LPS IgG and IgA response after the second booster dose was significantly higher compared with reference and unconjugated detoxified LPS response. Antibodies elicited by the dLPS-CBSA conjugate were vibriocidal.
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