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系统回顾和荟萃分析流行病学数据,研究疫苗反应与接触五种主要全氟烷基物质的关系。

Systematic review and meta-analysis of epidemiologic data on vaccine response in relation to exposure to five principal perfluoroalkyl substances.

机构信息

Ramboll U.S. Consulting, Inc., 28 Amity St., Suite 2A, Amherst, MA 01002, USA.

Canadian Center for Vaccinology, Dalhousie University and the IWK Health Centre and Nova Scotia Health Authority, Halifax, Canada; Department of Pediatrics, Dalhousie University, Halifax, Canada; Department of Microbiology and Immunology, Dalhousie University , Halifax, Canada.

出版信息

Environ Int. 2023 Feb;172:107734. doi: 10.1016/j.envint.2023.107734. Epub 2023 Jan 7.

Abstract

BACKGROUND

Epidemiologic studies of serum per- and polyfluoroalkyl substances (PFAS) and antibody response to vaccines have suggested an adverse association, but the consistency and magnitude of this association remain unclear.

OBJECTIVE

The goal of this systematic review was to determine the size of the association between a doubling in perfluoroalkyl substances (PFAS) serum concentration and difference in log antibody concentration following a vaccine, with a focus on five PFAS: perfluorooctanoic acid (PFOA), perfluorooctane sulfonate (PFOS), perfluorohexane sulfonate (PFHxS), perfluorononanoic acid (PFNA), and perfluorodecanoic acid (PFDA).

DATA SOURCE

We conducted online searches of PubMed and Web of Science through May 17, 2022 and identified 14 eligible reports published from 2012 to 2022.

STUDY ELIGIBILITY CRITERIA, PARTICIPANTS, AND INTERVENTIONS: We included studies conducted in humans, including mother-child pairs, which examined serum PFAS concentration in relation to serum concentration of antibody to a specific antigen following a vaccine.

STUDY APPRAISAL AND SYNTHESIS METHODS

We used the risk of bias assessment for non-randomized studies of exposure and certainty assessment method proposed by Morgan et al. (2019). Using a multilevel meta-regression model, we quantitatively synthesized the data.

RESULTS

The 14 reports represented 13 unique groups of subjects; the frequency of studies of a given antibody was Tetanus (n = 7); followed by Diphtheria (6); Measles (4); Rubella (3); Haemophilus influenzae type b and Influenza A H1N1 (2 each); and Hepatitis A, Hepatitis B, Influenza A H2N3, Influenza B, and Mumps (1 each). There were approximately 4,830 unique participants included in the analyses across the 14 reports. The models of coefficients between antibody concentration and the five principal PFAS showed homogeneity of associations across antibody types for each principal PFAS. In the models with all antibodies treated as one type, evidence of effect modification by life stage was present for PFOA and PFOS, and for consistency, all associations were evaluated for all ages and for children. The summary associations (coefficients for difference in log[antibody concentration] per doubling of serum PFAS) with 95% confidence intervals that excluded zero ("statistical support"), and certainty of evidence ratings were as follows: for PFOA and all antibodies treated as one type in all ages, -0.06 (-0.10, -0.01; moderate) and in children, -0.10 (-0.16, -0.03; moderate); for Diphtheria in children, -0.12 (-0.23, -0.00; high); for Rubella in all ages, -0.09 (-0.17, -0.01; moderate), and for Tetanus in children, -0.12 (-0.24, -0.00; moderate). For PFOS the summary associations were, for all antibodies treated as one type in all ages, -0.06 (-0.11, -0.01; moderate) and in children, -0.10 (-0.18, -0.03; moderate); for Rubella in all ages, -0.09 (-0.15, -0.03; high) and in children, -0.12 (-0.20, -0.04; high). For PFHxS the summary associations were, for all antibodies treated as one type in all ages, -0.03 (-0.06, -0.00; moderate) and in children, -0.05 (-0.09, -0.00; low); and for Rubella in children, -0.07 (-0.11, -0.02; high). Summary associations for PFNA and PFDA did not have statistical support, but all PFAS studied tended to have an inverse association with antibody concentrations.

LIMITATIONS AND CONCLUSIONS

Epidemiologic data on immunosuppression and five principal PFAS suggest an association, with support across antibodies against multiple types of antigens. Data on Diphtheria, Rubella, and Tetanus were more supportive of an association than for other antibodies, and support was greater for associations with PFOA, PFOS, and PFHxS, than for PFNA or PFDA. The data on any specific antibody were scarce. Confounding factors that might account for the relation were not identified. Nearly all studies evaluated were judged to have a low or moderate risk of bias.

摘要

背景

血清中持久性有机污染物和多氟烷基物质(PFAS)的流行病学研究以及疫苗抗体反应的研究表明,两者之间存在负面关联,但这种关联的一致性和规模尚不清楚。

目的

本系统综述的目的是确定血清中 PFAS 浓度增加一倍与疫苗接种后抗体浓度对数差异之间的关联大小,重点关注五种 PFAS:全氟辛酸(PFOA)、全氟辛烷磺酸(PFOS)、全氟己烷磺酸(PFHxS)、全氟壬酸(PFNA)和全氟癸酸(PFDA)。

数据来源

我们通过 2022 年 5 月 17 日在 PubMed 和 Web of Science 上进行了在线搜索,确定了 2012 年至 2022 年期间发表的 14 份符合条件的报告。

研究入选标准、参与者和干预措施:我们纳入了在人类中进行的研究,包括母婴对,这些研究考察了疫苗接种后血清 PFAS 浓度与特定抗原抗体浓度之间的关系。

研究评估和综合方法

我们使用了用于暴露的非随机研究的风险评估和由 Morgan 等人提出的(2019 年)的确定性评估方法。我们使用多水平荟萃回归模型对数据进行了定量综合。

结果

14 份报告代表了 13 个独特的研究对象组;研究特定抗体的频率为破伤风(n=7);其次是白喉(6);麻疹(4);风疹(3);乙型流感嗜血杆菌和甲型 H1N1 流感(2 种);以及甲型肝炎、乙型肝炎、甲型 H2N3 流感、乙型流感和腮腺炎(1 种)。在 14 份报告中,共有约 4830 名独特的参与者纳入了分析。五种主要 PFAS 的抗体浓度与系数之间的模型显示,每种主要 PFAS 的抗体类型之间的关联具有同质性。在将所有抗体视为一种类型的模型中,对于 PFOA 和 PFOS,存在生命阶段对效应修饰的证据,为了一致性,所有关联都在所有年龄组和儿童中进行了评估。排除零值(“统计学支持”)的汇总关联(血清 PFAS 每增加一倍时的抗体浓度差异系数及其 95%置信区间)和证据确定性评级如下:对于 PFOA 和所有抗体视为一种类型的所有年龄组,-0.06(-0.10,-0.01;中度)和儿童,-0.10(-0.16,-0.03;中度);对于儿童中的白喉,-0.12(-0.23,-0.00;高);对于所有年龄组的风疹,-0.09(-0.17,-0.01;中度),以及儿童中的破伤风,-0.12(-0.24,-0.00;中度)。对于 PFOS,汇总关联为,所有抗体视为一种类型的所有年龄组,-0.06(-0.11,-0.01;中度)和儿童,-0.10(-0.18,-0.03;中度);对于所有年龄组的风疹,-0.09(-0.15,-0.03;高)和儿童,-0.12(-0.20,-0.04;高)。对于 PFHxS,汇总关联为,所有抗体视为一种类型的所有年龄组,-0.03(-0.06,-0.00;中度)和儿童,-0.05(-0.09,-0.00;低);以及儿童中的风疹,-0.07(-0.11,-0.02;高)。PFNA 和 PFDA 的汇总关联没有统计学支持,但研究的所有 PFAS 都倾向于与抗体浓度呈负相关。

局限性和结论

关于免疫抑制和五种主要 PFAS 的流行病学数据表明存在关联,对多种类型抗原的抗体具有支持作用。关于白喉、风疹和破伤风的证据比其他抗体更支持关联,而对于 PFOA、PFOS 和 PFHxS 的关联支持程度高于对 PFNA 或 PFDA 的关联支持程度。任何特定抗体的数据都很少。无法确定可能解释这种关系的混杂因素。几乎所有评估的研究都被认为具有低或中度偏倚风险。

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