A Bayesian quantile joint modeling of multivariate longitudinal and time-to-event data

被引:0
|
作者
Kundu, Damitri [1 ]
Krishnan, Shekhar [2 ]
Gogoi, Manash Pratim [2 ]
Das, Kiranmoy [1 ,3 ]
机构
[1] Indian Stat Inst, Appl Stat Div, Kolkata, India
[2] Tata Med Ctr, Tata Translat Canc Res Ctr, Kolkata, India
[3] Beijing Inst Math Sci & Applicat, Beijing, Peoples R China
关键词
Acute lymphocytic leukemia (ALL); Asymmetric laplace distribution (ALD); Joint model; MCMC; Quantile regression; REGRESSION; CURE;
D O I
10.1007/s10985-024-09622-1
中图分类号
O1 [数学];
学科分类号
0701 ; 070101 ;
摘要
Linear mixed models are traditionally used for jointly modeling (multivariate) longitudinal outcomes and event-time(s). However, when the outcomes are non-Gaussian a quantile regression model is more appropriate. In addition, in the presence of some time-varying covariates, it might be of interest to see how the effects of different covariates vary from one quantile level (of outcomes) to the other, and consequently how the event-time changes across different quantiles. For such analyses linear quantile mixed models can be used, and an efficient computational algorithm can be developed. We analyze a dataset from the Acute Lymphocytic Leukemia (ALL) maintenance study conducted by Tata Medical Center, Kolkata. In this study, the patients suffering from ALL were treated with two standard drugs (6MP and MTx) for the first two years, and three biomarkers (e.g. lymphocyte count, neutrophil count and platelet count) were longitudinally measured. After treatment the patients were followed nearly for the next three years, and the relapse-time (if any) for each patient was recorded. For this dataset we develop a Bayesian quantile joint model for the three longitudinal biomarkers and time-to-relapse. We consider an Asymmetric Laplace Distribution (ALD) for each outcome, and exploit the mixture representation of the ALD for developing a Gibbs sampler algorithm to estimate the regression coefficients. Our proposed model allows different quantile levels for different biomarkers, but still simultaneously estimates the regression coefficients corresponding to a particular quantile combination. We infer that a higher lymphocyte count accelerates the chance of a relapse while a higher neutrophil count and a higher platelet count (jointly) reduce it. Also, we infer that across (almost) all quantiles 6MP reduces the lymphocyte count, while MTx increases the neutrophil count. Simulation studies are performed to assess the effectiveness of the proposed approach.
引用
收藏
页码:680 / 699
页数:20
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