Difference between revisions of "RAREMETALWORKER SPECIAL TOPICS"
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| + | [[Category:RAREMETALWORKER]] | ||
This page describes how [[RAREMETALWORKER]] handles some special cased during analyses. | This page describes how [[RAREMETALWORKER]] handles some special cased during analyses. | ||
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Here are some useful links to key pages: | Here are some useful links to key pages: | ||
| − | * [[RAREMETALWORKER | '''RAREMETALWORKER documentation''']] | + | * The [[RAREMETALWORKER | '''RAREMETALWORKER documentation''']] |
| − | * [[RAREMETALWORKER_METHOD | '''RAREMETALWORKER method''']] | + | * The [[RAREMETALWORKER_METHOD | '''RAREMETALWORKER method''']] |
| − | * [[RAREMETALWORKER_command_reference | '''RAREMETALWORKER command reference''']] | + | * The [[RAREMETALWORKER_command_reference | '''RAREMETALWORKER command reference''']] |
| − | * [[RAREMETAL_FAQ | '''FAQ''']] | + | * The [[Tutorial:_RAREMETAL| '''RAREMETALWORKER quick start tutorial''']] |
| + | * The [[RAREMETAL_FAQ | '''FAQ''']] | ||
== Unrelated Individuals == | == Unrelated Individuals == | ||
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== Analyzing Chromosome X== | == Analyzing Chromosome X== | ||
| + | * To make sure RAREMETALWORKER analyze chromosome X correctly, '''male must be code as 1 and female must be coded as 2''' in [[RAREMETALWORKER#PED_and_DAT_Files | '''PED''']] file. | ||
* --xStart and --xEnd options described the start and end position of nonPAR region on chromosome X. The default values are 2699520 and 154931044, according to Human Genome build 19. | * --xStart and --xEnd options described the start and end position of nonPAR region on chromosome X. The default values are 2699520 and 154931044, according to Human Genome build 19. | ||
* When samples are analyzed as unrelated (no any kind of kinship is used for linear mixed model approach), no special actions needed for analyzing markers on chromosome X. | * When samples are analyzed as unrelated (no any kind of kinship is used for linear mixed model approach), no special actions needed for analyzing markers on chromosome X. | ||
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* If a male is heterozygous in nonPAR region, then the genotype of that male sample is considered missing and will be imputed using mean genotype. | * If a male is heterozygous in nonPAR region, then the genotype of that male sample is considered missing and will be imputed using mean genotype. | ||
* If a male has genotype coded as ./x in nonPAR region, then the genotype of that male sample is considered missing and will be imputed using mean genotype. | * If a male has genotype coded as ./x in nonPAR region, then the genotype of that male sample is considered missing and will be imputed using mean genotype. | ||
| + | * For details of methods analyzing chromosomeX, please refer to [[RAREMETALWORKER_method | '''method''']]. | ||
Latest revision as of 17:50, 16 March 2018
This page describes how RAREMETALWORKER handles some special cased during analyses.
Useful Links
Here are some useful links to key pages:
- The RAREMETALWORKER documentation
- The RAREMETALWORKER method
- The RAREMETALWORKER command reference
- The RAREMETALWORKER quick start tutorial
- The FAQ
RAREMETALWORKER generates single variant association test statistics for a single study prior to meta-analysis. This page provides a brief description of the statistics that RAREMETALWORKER calculates, together with key formulae.
Missing Data
- Individuals with missing phenotypes will be excluded from analysis.
- If --makeResiduals is used for adjusting covariates, then individuals with missing covariates will also be excluded.
- Individuals that are not genotyped will also be excluded from analyses.
- Missing genotypes are imputed using mean genotype of a variant.
Analyzing Chromosome X
- To make sure RAREMETALWORKER analyze chromosome X correctly, male must be code as 1 and female must be coded as 2 in PED file.
- --xStart and --xEnd options described the start and end position of nonPAR region on chromosome X. The default values are 2699520 and 154931044, according to Human Genome build 19.
- When samples are analyzed as unrelated (no any kind of kinship is used for linear mixed model approach), no special actions needed for analyzing markers on chromosome X.
- If you want to use a linear mixed model approach to correct family structure, population structure, or cryptic relatedness, you should issue --vcX option in your command line. This approach will fit a separate linear mixed model using both autosomal kinship matrix and chromosomeX kinship matrix. This approach is believed to have larger power with type I error well controlled.
- On the other hand, if you want a fast association for chromosome X, another valid approach is to issue --vcX --separateX options. This will initiate fitting a separate linear mixed model using chromosomeX kinship only for analyzing markers on chromosomeX. This approach is expected to be faster than the above option, but with less power, although type I error is also expected to be under control.
- Male genotypes for variants in nonPAR region are coded to be 0 or 2.
- If a male is heterozygous in nonPAR region, then the genotype of that male sample is considered missing and will be imputed using mean genotype.
- If a male has genotype coded as ./x in nonPAR region, then the genotype of that male sample is considered missing and will be imputed using mean genotype.
- For details of methods analyzing chromosomeX, please refer to method.
