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D MDR Ref [62, 63] [64] [65, 66] [67, 68] [69] [70] [12] Implementation Java R Java R C��/CUDA C�� Java URL www.epistasis.org/software.html Accessible upon request, get in touch with authors sourceforge.net/projects/mdr/files/mdrpt/ cran.r-project.org/web/packages/MDR/index.html 369158 sourceforge.net/projects/mdr/files/mdrgpu/ ritchielab.psu.edu/software/mdr-download www.medicine.virginia.edu/clinical/departments/ psychiatry/sections/neurobiologicalstudies/ genomics/gmdr-software-request www.medicine.virginia.edu/clinical/departments/ psychiatry/sections/neurobiologicalstudies/ genomics/pgmdr-software-request Accessible upon request, make contact with authors www.epistasis.org/software.html Accessible upon request, speak to authors property.ustc.edu.cn/ zhanghan/ocp/ocp.html sourceforge.net/projects/sdrproject/ Obtainable upon request, contact authors www.epistasis.org/software.html Offered upon request, get in touch with authors ritchielab.psu.edu/software/mdr-download www.statgen.ulg.ac.be/software.html cran.r-project.org/web/packages/mbmdr/index.html www.statgen.ulg.ac.be/software.html Consist/Sig k-fold CV k-fold CV, bootstrapping k-fold CV, permutation k-fold CV, 3WS, permutation k-fold CV, permutation k-fold CV, permutation k-fold CV Cov Yes No No No No No YesGMDRPGMDR[34]Javak-fold CVYesSVM-GMDR RMDR OR-MDR Opt-MDR SDR Surv-MDR QMDR Ord-MDR MDR-PDT MB-MDR[35] [39] [41] [42] [46] [47] [48] [49] [50] [55, 71, 72] [73] [74]MATLAB Java R C�� Python R Java C�� C�� C�� R Rk-fold CV, permutation k-fold CV, permutation k-fold CV, bootstrapping GEVD k-fold CV, permutation k-fold CV, permutation k-fold CV, permutation k-fold CV, permutation k-fold CV, permutation Permutation Permutation PermutationYes Yes No No No Yes Yes No No No Yes YesRef ?Reference, Cov ?Covariate adjustment feasible, Consist/Sig ?Techniques applied to decide the consistency or significance of model.Figure 3. Overview of the original MDR algorithm as described in [2] around the left with categories of extensions or modifications on the suitable. The first stage is dar.12324 data input, and extensions for the original MDR technique dealing with other phenotypes or data structures are presented within the section `Different phenotypes or data structures’. The second stage comprises CV and permutation loops, and approaches addressing this stage are offered in section `Permutation and cross-validation strategies’. The following stages encompass the core algorithm (see Figure 4 for specifics), which classifies the multifactor combinations into danger groups, plus the evaluation of this classification (see Figure 5 for facts). Solutions, extensions and approaches mostly addressing these stages are described in sections `Classification of cells into risk groups’ and `Evaluation from the classification result’, respectively.A roadmap to multifactor dimensionality reduction strategies|Figure four. The MDR core algorithm as described in [2]. The following methods are executed for every number of elements (d). (1) In the exhaustive list of all possible d-factor combinations choose one particular. (2) Represent the selected Thonzonium (bromide) web things in d-dimensional space and estimate the instances to controls ratio within the instruction set. (three) A cell is labeled as higher danger (H) if the ratio exceeds some T0901317 chemical information threshold (T) or as low danger otherwise.Figure 5. Evaluation of cell classification as described in [2]. The accuracy of each d-model, i.e. d-factor combination, is assessed when it comes to classification error (CE), cross-validation consistency (CVC) and prediction error (PE). Amongst all d-models the single m.D MDR Ref [62, 63] [64] [65, 66] [67, 68] [69] [70] [12] Implementation Java R Java R C��/CUDA C�� Java URL www.epistasis.org/software.html Accessible upon request, speak to authors sourceforge.net/projects/mdr/files/mdrpt/ cran.r-project.org/web/packages/MDR/index.html 369158 sourceforge.net/projects/mdr/files/mdrgpu/ ritchielab.psu.edu/software/mdr-download www.medicine.virginia.edu/clinical/departments/ psychiatry/sections/neurobiologicalstudies/ genomics/gmdr-software-request www.medicine.virginia.edu/clinical/departments/ psychiatry/sections/neurobiologicalstudies/ genomics/pgmdr-software-request Available upon request, make contact with authors www.epistasis.org/software.html Obtainable upon request, contact authors home.ustc.edu.cn/ zhanghan/ocp/ocp.html sourceforge.net/projects/sdrproject/ Readily available upon request, contact authors www.epistasis.org/software.html Accessible upon request, get in touch with authors ritchielab.psu.edu/software/mdr-download www.statgen.ulg.ac.be/software.html cran.r-project.org/web/packages/mbmdr/index.html www.statgen.ulg.ac.be/software.html Consist/Sig k-fold CV k-fold CV, bootstrapping k-fold CV, permutation k-fold CV, 3WS, permutation k-fold CV, permutation k-fold CV, permutation k-fold CV Cov Yes No No No No No YesGMDRPGMDR[34]Javak-fold CVYesSVM-GMDR RMDR OR-MDR Opt-MDR SDR Surv-MDR QMDR Ord-MDR MDR-PDT MB-MDR[35] [39] [41] [42] [46] [47] [48] [49] [50] [55, 71, 72] [73] [74]MATLAB Java R C�� Python R Java C�� C�� C�� R Rk-fold CV, permutation k-fold CV, permutation k-fold CV, bootstrapping GEVD k-fold CV, permutation k-fold CV, permutation k-fold CV, permutation k-fold CV, permutation k-fold CV, permutation Permutation Permutation PermutationYes Yes No No No Yes Yes No No No Yes YesRef ?Reference, Cov ?Covariate adjustment feasible, Consist/Sig ?Approaches made use of to identify the consistency or significance of model.Figure three. Overview of the original MDR algorithm as described in [2] on the left with categories of extensions or modifications around the suitable. The first stage is dar.12324 information input, and extensions towards the original MDR process coping with other phenotypes or information structures are presented inside the section `Different phenotypes or data structures’. The second stage comprises CV and permutation loops, and approaches addressing this stage are offered in section `Permutation and cross-validation strategies’. The following stages encompass the core algorithm (see Figure 4 for details), which classifies the multifactor combinations into threat groups, plus the evaluation of this classification (see Figure 5 for facts). Solutions, extensions and approaches mainly addressing these stages are described in sections `Classification of cells into risk groups’ and `Evaluation with the classification result’, respectively.A roadmap to multifactor dimensionality reduction methods|Figure four. The MDR core algorithm as described in [2]. The following measures are executed for every number of aspects (d). (1) In the exhaustive list of all achievable d-factor combinations pick 1. (two) Represent the selected components in d-dimensional space and estimate the situations to controls ratio inside the training set. (three) A cell is labeled as high risk (H) if the ratio exceeds some threshold (T) or as low danger otherwise.Figure 5. Evaluation of cell classification as described in [2]. The accuracy of each and every d-model, i.e. d-factor mixture, is assessed in terms of classification error (CE), cross-validation consistency (CVC) and prediction error (PE). Among all d-models the single m.

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Author: Cholesterol Absorption Inhibitors