Applied mixed models in medicine
著者
書誌事項
Applied mixed models in medicine
(Statistics in practice)
John Wiley & Sons, c2006
2nd ed
大学図書館所蔵 全8件
  青森
  岩手
  宮城
  秋田
  山形
  福島
  茨城
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  群馬
  埼玉
  千葉
  東京
  神奈川
  新潟
  富山
  石川
  福井
  山梨
  長野
  岐阜
  静岡
  愛知
  三重
  滋賀
  京都
  大阪
  兵庫
  奈良
  和歌山
  鳥取
  島根
  岡山
  広島
  山口
  徳島
  香川
  愛媛
  高知
  福岡
  佐賀
  長崎
  熊本
  大分
  宮崎
  鹿児島
  沖縄
  韓国
  中国
  タイ
  イギリス
  ドイツ
  スイス
  フランス
  ベルギー
  オランダ
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注記
Includes bibliographical references and index
内容説明・目次
内容説明
A mixed model allows the incorporation of both fixed and random variables within a statistical analysis. This enables efficient inferences and more information to be gained from the data. The application of mixed models is an increasingly popular way of analysing medical data, particularly in the pharmaceutical industry. There have been many recent advances in mixed modelling, particularly regarding the software and applications. This new edition of a groundbreaking text discusses the latest developments, from updated SAS techniques to the increasingly wide range of applications.
Presents an overview of the theory and applications of mixed models in medical research, including the latest developments and new sections on bioequivalence, cluster randomised trials and missing data.
Easily accessible to practitioners in any area where mixed models are used, including medical statisticians and economists.
Includes numerous examples using real data from medical and health research, and epidemiology, illustrated with SAS code and output.
Features new version of SAS, including the procedure PROC GLIMMIX and an introduction to other available software.
Supported by a website featuring computer code, data sets, and further material, available at: http://www.chs.med.ed.ac.uk/phs/mixed/.
This much-anticipated second edition is ideal for applied statisticians working in medical research and the pharmaceutical industry, as well as teachers and students of statistics courses in mixed models. The text will also be of great value to a broad range of scientists, particularly those working the medical and pharmaceutical areas.
目次
Preface to Second Edition. Mixed Model Notations.
1 Introduction.
1.1 The Use of Mixed Models.
1.2 Introductory Example.
1.3 A Multi-Centre Hypertension Trial.
1.4 Repeated Measures Data.
1.5 More aboutMixed Models.
1.6 Some Useful Definitions.
2 NormalMixed Models.
2.1 Model Definition.
2.2 Model Fitting Methods.
2.3 The Bayesian Approach.
2.4 Practical Application and Interpretation.
2.5 Example.
3 Generalised Linear MixedModels.
3.1 Generalised Linear Models.
3.2 Generalised Linear Mixed Models.
3.3 Practical Application and Interpretation.
3.4 Example.
4 Mixed Models for Categorical Data.
4.1 Ordinal Logistic Regression (Fixed Effects Model).
4.2 Mixed Ordinal Logistic Regression.
4.3 Mixed Models for Unordered Categorical Data.
4.4 Practical Application and Interpretation.
4.5 Example.
5 Multi-Centre Trials and Meta-Analyses.
5.1 Introduction to Multi-Centre Trials.
5.2 The Implications of using Different Analysis Models.
5.3 Example: A Multi-Centre Trial.
5.4 Practical Application and Interpretation.
5.5 Sample Size Estimation.
5.6 Meta-Analysis.
5.7 Example: Meta-analysis.
6 RepeatedMeasures Data.
6.1 Introduction.
6.2 Covariance Pattern Models.
6.3 Example: Covariance Pattern Models for Normal Data.
6.4 Example: Covariance Pattern Models for Count Data.
6.5 Random Coefficients Models.
6.6 Examples of Random Coefficients Models.
6.7 Sample Size Estimation.
7 Cross-Over Trials.
7.1 Introduction.
7.2 Advantages of Mixed Models in Cross-Over Trials.
7.3 The AB/BA Cross-Over Trial.
7.4 Higher Order Complete Block Designs.
7.5 Incomplete Block Designs.
7.6 Optimal Designs.
7.7 Covariance Pattern Models.
7.8 Analysis of Binary Data.
7.9 Analysis of Categorical Data.
7.10 Use of Results from Random Effects Models in Trial Design.
7.11 General Points.
8 Other Applications of MixedModels.
8.1 Trials with Repeated Measurements within Visits.
8.2 Multi-Centre Trials with Repeated Measurements.
8.3 Multi-Centre Cross-Over Trials.
8.4 Hierarchical Multi-Centre Trials and Meta-Analysis.
8.5 Matched Case-Control Studies.
8.6 Different Variances for Treatment Groups in a Simple Between-Patient Trial.
8.7 Estimating Variance Components in an Animal Physiology Trial.
8.8 Inter- and Intra-Observer Variation in Foetal Scan Measurements.
8.9 Components of Variation and Mean Estimates in a Cardiology Experiment.
8.10 Cluster Sample Surveys.
8.11 Small AreaMortality Estimates.
8.12 Estimating Surgeon Performance.
8.13 Event History Analysis.
8.14 A Laboratory Study Using aWithin-Subject 4 x 4 Factorial Design.
8.15 Bioequivalence Studies with Replicate Cross-Over Designs.
8.16 Cluster Randomised Trials.
9 Software for Fitting MixedModels.
9.1 Packages for Fitting Mixed Models.
9.2 Basic use of PROC MIXED.
9.3 Using SAS to Fit Mixed Models to Non-Normal Data.
Glossary.
References.
Index.
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