mr_mvinput: Inputting and formatting data for use in causal estimation
In MendelianRandomization: Mendelian Randomization Package
mr_mvinput R Documentation
Inputting and formatting data for use in causal estimation
Description
The mr_mvinput function is required for inputting and formatting data for use in the multivariable Mendelian randomization functions provided in this package.
Usage
mr_mvinput(
bx = matrix(),
bxse = matrix(),
by = 0,
byse = 0,
correlation = matrix(),
exposure = "exposure",
outcome = "outcome",
snps = "snp",
effect_allele = NA,
other_allele = NA,
eaf = NA
)
Arguments
bx
A matrix of beta-coefficient values for genetic associations with the risk factor variables. These should be arranged so that column 1 are the beta-coefficients for risk factor 1, and row 1 are the beta-coefficients for genetic variant 1.
bxse
The matrix of standard errors associated with the beta-coefficients bx.
by
A numeric vector of beta-coefficient values for genetic associations with the second variable (often referred to as the outcome). For a disease outcome, the beta coefficients are log odds estimates from logistic regression analyses.
byse
The vector standard errors associated with the beta-coefficients in by.
correlation
The matrix of correlations between genetic variants. If this variable is not provided, then we assume that genetic variants are uncorrelated.
exposure
The names of the exposure variables.
outcome
The name of the outcome variable.
snps
The names of the genetic variants (SNPs) included in the analysis. The inputs exposure, outcome, and snps are not required, but may be useful for keeping track of various MRInput objects. They are also used by the mr_plot function.
effect_allele
The name of the effect allele for each SNP. The beta-coefficients are the associations with the exposure and outcome per additional copy of the effect allele.
other_allele
The name of the non-effect allele.
eaf
The expected allele frequencies (numeric). The slots effect_allele, other_allele, and eaf are neither required, nor currently used in the MendelianRandomization package. They are included for future compatibility with the MR-Base suite of functions.
Details
The beta-coefficients are assumed to be estimated for uncorrelated (independent) genetic variants, although a correlation matrix can be specified if the variants are correlated in their distributions. We also assume that the beta-coefficients for associations with the exposure and with the outcome are uncorrelated (corresponding to a two-sample Mendelian randomization analysis), although correlation between associations with the exposure and with the outcome generally have little impact on causal estimates or standard errors.
If the variables are not all the same length, then an error message will be reported. The analyses will still try to run, but the output may be misleading. However, in some analyses (for example, the standard IVW and MR-Egger methods), the values of bxse are not used in the analysis, and can therefore safely be omitted (provided that the other variables are correctly labelled).
Value
An MRMVInput object containing:
betaX
The genetic associations with the exposures.
betaXse
The corresponding standard errors.
betaY
The genetic associations with the outcome.
betaYse
The corresponding standard errors.
correlation
The matrix of genetic correlations.
exposure
Character strings with the names given to the exposures.
outcome
A character string giving the name given to the outcome.
snps
A vector of character strings with the names of the genetic variants.
effect_allele
A vector of character strings with the names of the effect alleles.
other_allele
A vector of character strings with the names of the non-effect alleles.
eaf
A numeric vector with the effect allele frequencies.
MendelianRandomization documentation built on Aug. 9, 2023, 1:05 a.m.
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| mr_mvinput | R Documentation |
Inputting and formatting data for use in causal estimation
Description
The mr_mvinput function is required for inputting and formatting data for use in the multivariable Mendelian randomization functions provided in this package.
Usage
mr_mvinput(
bx = matrix(),
bxse = matrix(),
by = 0,
byse = 0,
correlation = matrix(),
exposure = "exposure",
outcome = "outcome",
snps = "snp",
effect_allele = NA,
other_allele = NA,
eaf = NA
)
Arguments
bx |
A matrix of beta-coefficient values for genetic associations with the risk factor variables. These should be arranged so that column 1 are the beta-coefficients for risk factor 1, and row 1 are the beta-coefficients for genetic variant 1. |
bxse |
The matrix of standard errors associated with the beta-coefficients |
by |
A numeric vector of beta-coefficient values for genetic associations with the second variable (often referred to as the outcome). For a disease outcome, the beta coefficients are log odds estimates from logistic regression analyses. |
byse |
The vector standard errors associated with the beta-coefficients in |
correlation |
The matrix of correlations between genetic variants. If this variable is not provided, then we assume that genetic variants are uncorrelated. |
exposure |
The names of the exposure variables. |
outcome |
The name of the outcome variable. |
snps |
The names of the genetic variants (SNPs) included in the analysis. The inputs |
effect_allele |
The name of the effect allele for each SNP. The beta-coefficients are the associations with the exposure and outcome per additional copy of the effect allele. |
other_allele |
The name of the non-effect allele. |
eaf |
The expected allele frequencies (numeric). The slots |
Details
The beta-coefficients are assumed to be estimated for uncorrelated (independent) genetic variants, although a correlation matrix can be specified if the variants are correlated in their distributions. We also assume that the beta-coefficients for associations with the exposure and with the outcome are uncorrelated (corresponding to a two-sample Mendelian randomization analysis), although correlation between associations with the exposure and with the outcome generally have little impact on causal estimates or standard errors.
If the variables are not all the same length, then an error message will be reported. The analyses will still try to run, but the output may be misleading. However, in some analyses (for example, the standard IVW and MR-Egger methods), the values of bxse are not used in the analysis, and can therefore safely be omitted (provided that the other variables are correctly labelled).
Value
An MRMVInput object containing:
betaX |
The genetic associations with the exposures. |
betaXse |
The corresponding standard errors. |
betaY |
The genetic associations with the outcome. |
betaYse |
The corresponding standard errors. |
correlation |
The matrix of genetic correlations. |
exposure |
Character strings with the names given to the exposures. |
outcome |
A character string giving the name given to the outcome. |
snps |
A vector of character strings with the names of the genetic variants. |
effect_allele |
A vector of character strings with the names of the effect alleles. |
other_allele |
A vector of character strings with the names of the non-effect alleles. |
eaf |
A numeric vector with the effect allele frequencies. |
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