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Analysis of longitudinal binary data : an application to a disease process.

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Date

2008

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Abstract

The analysis of longitudinal binary data can be undertaken using any of the three families of models namely, marginal, random effects and conditional models. Each family of models has its own respective merits and demerits. The models are applied in the analysis of binary longitudinal data for childhood disease data namely the Respiratory Syncytial Virus (RSV) data collected from a study in Kilifi, coastal Kenya. The marginal model was fitted using generalized estimating equations (GEE). The random effects models were fitted using ‘Proc GLIMMIX’ and ‘NLMIXED’ in SAS and then again in Genstat. Because the data is a state transition type of data with the Markovian property the conditional model was used to capture the dependence of the current response to the previous response which is known as the history. The data set has two main complicating issues. Firstly, there is the question of developing a stochastically based probability model for the disease process. In the current work we use direct likelihood and generalized linear modelling (GLM) approaches to estimate important disease parameters. The force of infection and the recovery rate are the key parameters of interest. The findings of the current work are consistent and in agreement with those in White et al. (2003). The aspect of time dependence on the RSV disease is also highlighted in the thesis by fitting monthly piecewise models for both parameters. Secondly, there is the issue of incomplete data in the analysis of longitudinal data. Commonly used methods to analyze incomplete longitudinal data include the well known available case analysis (AC) and last observation carried forward (LOCF). However, these methods rely on strong assumptions such as missing completely at random (MCAR) for AC analysis and unchanging profile after dropout for LOCF analysis. Such assumptions are too strong to generally hold. In recent years, methods of analyzing incomplete longitudinal data have become available with weaker assumptions, such as missing at random (MAR). Thus we make use of multiple imputation via chained equations that require the MAR assumption and maximum likelihood methods that result in the missing data mechanism becoming ignorable as soon as it is MAR. Thus we are faced with the problem of incomplete repeated non–normal data suggesting the use of at least the Generalized Linear Mixed Model (GLMM) to account for natural individual heterogeneity. The comparison of the parameter estimates using the different methods to handle the dropout is strongly emphasized in order to evaluate the advantages of the different methods and approaches. The survival analysis approach was also utilized to model the data due to the presence of multiple events per subject and the time between these events.

Description

Thesis (Ph.D.)-University of KwaZulu-Natal, Pietermarizburg, 2008.

Keywords

Analysis of variance., Distribution (Probability theory), Linear models (Statistics), Medical statistics., Biometry.

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