论文标题

抗体在疫苗接种中的影响的调解分析

Mediation Analyses for the Effect of Antibodies in Vaccination

论文作者

Fay, Michael P., Follmann, Dean A.

论文摘要

我们回顾了标准的中介假设,因为它们适用于在随机疫苗试验中识别抗体效应,并提出了新的研究设计,以识别以前无法识别的估计值。对于这些中介分析,我们将随机疫苗试验的总比率效应(一种减去疫苗效应)分为间接(通过抗体作用)和直接效应(其他效应)。识别$λ$,由于间接效应而引起的总效应的比例取决于跨世界的数量,即抗体水平的接种疫苗的个体的潜在结果,好像给定安慰剂一样,反之亦然。我们审查了识别$λ$的假设,并表明有两个版本的$λ$,除非在安慰剂组中添加抗体的效果与从疫苗臂中减去抗体的效果相等。我们专注于安慰剂组中的个人不太可能具有所需抗体的情况。在这种情况下,如果标准假设(给定的混杂因素,潜在的调解人和潜在结果是独立的)是正确的,则只有一个版本的$λ$可识别,如果不能识别。我们建议使用实验设计来识别以前的跨世界数量,以识别其他版本的$λ$。两种替代实验设计使用三个ARM试验,多余的手臂是被动免疫(给予单克隆抗体),有或没有近距离疫苗接种。另一种选择是将安慰剂对照疫苗试验中的信息与安慰剂对照的被动免疫试验相结合。

We review standard mediation assumptions as they apply to identifying antibody effects in a randomized vaccine trial and propose new study designs to allow identification of an estimand that was previously unidentifiable. For these mediation analyses, we partition the total ratio effect (one minus the vaccine effect) from a randomized vaccine trial into indirect (effects through antibodies) and direct effects (other effects). Identifying $λ$, the proportion of the total effect due to an indirect effect, depends on a cross-world quantity, the potential outcome among vaccinated individuals with antibody levels as if given placebo, or vice versa. We review assumptions for identifying $λ$ and show that there are two versions of $λ$, unless the effect of adding antibodies to the placebo arm is equal in magnitude to the effect of subtracting antibodies from the vaccine arm. We focus on the case when individuals in the placebo arm are unlikely to have the needed antibodies. In that case, if a standard assumption (given confounders, potential mediators and potential outcomes are independent) is true, only one version of $λ$ is identifiable, and if not neither is identifiable. We propose alternatives for identifying the other version of $λ$, using experimental design to identify a formerly cross-world quantity. Two alternative experimental designs use a three arm trial with the extra arm being passive immunization (administering monoclonal antibodies), with or without closeout vaccination. Another alternative is to combine information from a placebo-controlled vaccine trial with a placebo-controlled passive immunization trial.

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