R/examples/RGWAS.twostep.epi_example.R
In KosukeHamazaki/RAINBOWR: Genome-Wide Association Study with SNP-Set Methods
\dontshow{
### Import RAINBOWR
require(RAINBOWR)
### Load example datasets
data("Rice_Zhao_etal")
Rice_geno_score <- Rice_Zhao_etal$genoScore
Rice_geno_map <- Rice_Zhao_etal$genoMap
Rice_pheno <- Rice_Zhao_etal$pheno
### Select one trait for example
trait.name <- "Flowering.time.at.Arkansas"
y <- Rice_pheno[1:50, trait.name, drop = FALSE]
# use first 50 accessions
### Remove SNPs whose MAF <= 0.05
x.0 <- t(Rice_geno_score)
MAF.cut.res <- MAF.cut(x.0 = x.0, map.0 = Rice_geno_map)
x <- MAF.cut.res$x
map <- MAF.cut.res$map
### Estimate genomic relationship matrix (GRM)
K.A <- calcGRM(genoMat = x)
### Modify data
modify.data.res <- modify.data(pheno.mat = y, geno.mat = x, map = map,
return.ZETA = TRUE, return.GWAS.format = TRUE)
pheno.GWAS <- modify.data.res$pheno.GWAS
geno.GWAS <- modify.data.res$geno.GWAS
ZETA <- modify.data.res$ZETA
### Perform two-step epistasis GWAS (single-snp GWAS -> Check epistasis for significant markers)
twostep.epi.res <- RGWAS.twostep.epi(pheno = pheno.GWAS, geno = geno.GWAS, ZETA = ZETA,
n.PC = 4, test.method = "LR", gene.set = NULL,
window.size.half = 10, window.slide = 21,
plot.Manhattan.1 = FALSE, plot.qq.1 = FALSE,
plot.epi.3d = FALSE, plot.epi.2d = FALSE,
verbose = FALSE, count = FALSE, time = FALSE,
package.MM = "gaston", parallel.method = "mclapply",
skip.check = TRUE, n.core = 1)
}
\donttest{
### Import RAINBOWR
require(RAINBOWR)
### Load example datasets
data("Rice_Zhao_etal")
Rice_geno_score <- Rice_Zhao_etal$genoScore
Rice_geno_map <- Rice_Zhao_etal$genoMap
Rice_pheno <- Rice_Zhao_etal$pheno
### View each dataset
See(Rice_geno_score)
See(Rice_geno_map)
See(Rice_pheno)
### Select one trait for example
trait.name <- "Flowering.time.at.Arkansas"
y <- Rice_pheno[, trait.name, drop = FALSE]
### Remove SNPs whose MAF <= 0.05
x.0 <- t(Rice_geno_score)
MAF.cut.res <- MAF.cut(x.0 = x.0, map.0 = Rice_geno_map)
x <- MAF.cut.res$x
map <- MAF.cut.res$map
### Estimate genomic relationship matrix (GRM)
K.A <- calcGRM(genoMat = x)
### Modify data
modify.data.res <- modify.data(pheno.mat = y, geno.mat = x, map = map,
return.ZETA = TRUE, return.GWAS.format = TRUE)
pheno.GWAS <- modify.data.res$pheno.GWAS
geno.GWAS <- modify.data.res$geno.GWAS
ZETA <- modify.data.res$ZETA
### View each data for RAINBOWR
See(pheno.GWAS)
See(geno.GWAS)
str(ZETA)
### Perform two-step epistasis GWAS (single-snp GWAS -> Check epistasis for significant markers)
twostep.epi.res <- RGWAS.twostep.epi(pheno = pheno.GWAS, geno = geno.GWAS, ZETA = ZETA,
n.PC = 4, test.method = "LR", gene.set = NULL,
window.size.half = 10, window.slide = 21,
package.MM = "gaston", parallel.method = "mclapply",
skip.check = TRUE, n.core = 2)
See(twostep.epi.res$epistasis$scores)
}
KosukeHamazaki/RAINBOWR documentation built on Dec. 9, 2024, 12:06 a.m.
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\dontshow{
### Import RAINBOWR
require(RAINBOWR)
### Load example datasets
data("Rice_Zhao_etal")
Rice_geno_score <- Rice_Zhao_etal$genoScore
Rice_geno_map <- Rice_Zhao_etal$genoMap
Rice_pheno <- Rice_Zhao_etal$pheno
### Select one trait for example
trait.name <- "Flowering.time.at.Arkansas"
y <- Rice_pheno[1:50, trait.name, drop = FALSE]
# use first 50 accessions
### Remove SNPs whose MAF <= 0.05
x.0 <- t(Rice_geno_score)
MAF.cut.res <- MAF.cut(x.0 = x.0, map.0 = Rice_geno_map)
x <- MAF.cut.res$x
map <- MAF.cut.res$map
### Estimate genomic relationship matrix (GRM)
K.A <- calcGRM(genoMat = x)
### Modify data
modify.data.res <- modify.data(pheno.mat = y, geno.mat = x, map = map,
return.ZETA = TRUE, return.GWAS.format = TRUE)
pheno.GWAS <- modify.data.res$pheno.GWAS
geno.GWAS <- modify.data.res$geno.GWAS
ZETA <- modify.data.res$ZETA
### Perform two-step epistasis GWAS (single-snp GWAS -> Check epistasis for significant markers)
twostep.epi.res <- RGWAS.twostep.epi(pheno = pheno.GWAS, geno = geno.GWAS, ZETA = ZETA,
n.PC = 4, test.method = "LR", gene.set = NULL,
window.size.half = 10, window.slide = 21,
plot.Manhattan.1 = FALSE, plot.qq.1 = FALSE,
plot.epi.3d = FALSE, plot.epi.2d = FALSE,
verbose = FALSE, count = FALSE, time = FALSE,
package.MM = "gaston", parallel.method = "mclapply",
skip.check = TRUE, n.core = 1)
}
\donttest{
### Import RAINBOWR
require(RAINBOWR)
### Load example datasets
data("Rice_Zhao_etal")
Rice_geno_score <- Rice_Zhao_etal$genoScore
Rice_geno_map <- Rice_Zhao_etal$genoMap
Rice_pheno <- Rice_Zhao_etal$pheno
### View each dataset
See(Rice_geno_score)
See(Rice_geno_map)
See(Rice_pheno)
### Select one trait for example
trait.name <- "Flowering.time.at.Arkansas"
y <- Rice_pheno[, trait.name, drop = FALSE]
### Remove SNPs whose MAF <= 0.05
x.0 <- t(Rice_geno_score)
MAF.cut.res <- MAF.cut(x.0 = x.0, map.0 = Rice_geno_map)
x <- MAF.cut.res$x
map <- MAF.cut.res$map
### Estimate genomic relationship matrix (GRM)
K.A <- calcGRM(genoMat = x)
### Modify data
modify.data.res <- modify.data(pheno.mat = y, geno.mat = x, map = map,
return.ZETA = TRUE, return.GWAS.format = TRUE)
pheno.GWAS <- modify.data.res$pheno.GWAS
geno.GWAS <- modify.data.res$geno.GWAS
ZETA <- modify.data.res$ZETA
### View each data for RAINBOWR
See(pheno.GWAS)
See(geno.GWAS)
str(ZETA)
### Perform two-step epistasis GWAS (single-snp GWAS -> Check epistasis for significant markers)
twostep.epi.res <- RGWAS.twostep.epi(pheno = pheno.GWAS, geno = geno.GWAS, ZETA = ZETA,
n.PC = 4, test.method = "LR", gene.set = NULL,
window.size.half = 10, window.slide = 21,
package.MM = "gaston", parallel.method = "mclapply",
skip.check = TRUE, n.core = 2)
See(twostep.epi.res$epistasis$scores)
}
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We want your feedback!
Note that we can't provide technical support on individual packages. You should contact the package authors for that.
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