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Autori principali: Deng, Yuhao, Wang, Rui, Zhang, Tao, Zhan, Xiang
Natura: Preprint
Pubblicazione: 2024
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Accesso online:https://arxiv.org/abs/2412.06114
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author Deng, Yuhao
Wang, Rui
Zhang, Tao
Zhan, Xiang
author_facet Deng, Yuhao
Wang, Rui
Zhang, Tao
Zhan, Xiang
contents In clinical studies, the risk of the primary (terminal) event may be modified by intermediate events, resulting in semicompeting risks. To study the treatment effect on the terminal event mediated by the intermediate event, researchers wish to decompose the total effect into direct and indirect effects. In this article, we extend the randomized interventional approach to time-to-event outcomes, where both intermediate and terminal events are subject to right censoring. We envision a random draw for the intermediate event process from a reference distribution, either marginally over time-varying confounders or conditionally given the observed history. We present the identification formula for interventional effects. We also discuss some variants of the identification assumptions. We estimate the treatment effects using nonparametric maximum likelihood estimation and propose a sensitivity analysis that incorporates a latent frailty. As an illustration, we study the effect of matched unrelated donor versus haploidentical donor on death mediated by relapse in a hematopoietic cell transplantation study with graft-versus-host disease (GVHD) as the time-varying confounder. We find that matched unrelated donor transplantation is preferable in terms of survival rates under the use of post-transplant PTCy GVHD prophylaxis for lymphoma patients.
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id arxiv_https___arxiv_org_abs_2412_06114
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publishDate 2024
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spellingShingle Randomized interventional effects in semicompeting risks, with application to a hematopoietic cell transplantation study
Deng, Yuhao
Wang, Rui
Zhang, Tao
Zhan, Xiang
Methodology
In clinical studies, the risk of the primary (terminal) event may be modified by intermediate events, resulting in semicompeting risks. To study the treatment effect on the terminal event mediated by the intermediate event, researchers wish to decompose the total effect into direct and indirect effects. In this article, we extend the randomized interventional approach to time-to-event outcomes, where both intermediate and terminal events are subject to right censoring. We envision a random draw for the intermediate event process from a reference distribution, either marginally over time-varying confounders or conditionally given the observed history. We present the identification formula for interventional effects. We also discuss some variants of the identification assumptions. We estimate the treatment effects using nonparametric maximum likelihood estimation and propose a sensitivity analysis that incorporates a latent frailty. As an illustration, we study the effect of matched unrelated donor versus haploidentical donor on death mediated by relapse in a hematopoietic cell transplantation study with graft-versus-host disease (GVHD) as the time-varying confounder. We find that matched unrelated donor transplantation is preferable in terms of survival rates under the use of post-transplant PTCy GVHD prophylaxis for lymphoma patients.
title Randomized interventional effects in semicompeting risks, with application to a hematopoietic cell transplantation study
topic Methodology
url https://arxiv.org/abs/2412.06114