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R/vc_score.R
In dearseq: Differential Expression Analysis for RNA-seq data through a robust variance component test
Defines functions
vc_score
Documented in
vc_score
#'Computes variance component test statistic for longitudinal
#'
#'This function computes an approximation of the Variance Component test for a
#'mixture of \eqn{\chi^{2}}s using Davies method from
#'\code{\link[CompQuadForm]{davies}}
#'
#'@keywords internal
#'
#'@param y a numeric matrix of dim \code{g x n} containing the raw RNA-seq
#'counts for g genes from \code{n} samples
#'
#'@param x a numeric design matrix of dim \code{n x p} containing the \code{p}
#'covariates to be adjusted for
#'
#'@param indiv a vector of length \code{n} containing the information for
#'attributing each sample to one of the studied individuals. Coerced
#'to be a \code{factor}
#'
#'@param phi a numeric design matrix of size \code{n x K} containing the
#'\code{K} variables to be tested
#'
#'@param w a vector of length \code{n} containing the weights for the \code{n}
#'samples.
#'
#'@param Sigma_xi a matrix of size \code{K x K} containing the covariance matrix
#'of the \code{K} random effects on \code{phi}
#'
#'@param na_rm logical: should missing values (including \code{NA} and
#'\code{NaN}) be omitted from the calculations? Default is \code{FALSE}.
#'
#'@return A list with the following elements:\itemize{
#' \item \code{score}: approximation of the set observed score
#' \item \code{q}: observation-level contributions to the score
#' \item \code{q_ext}: pseudo-observations used to compute the covariance,
#' taking into account the contributions of OLS estimates
#' \item \code{gene_scores_unscaled}: a vector of the approximations of the
#' individual gene scores
#' }
#'
#'@seealso \code{\link[CompQuadForm]{davies}}
#'
#'@examples
#'set.seed(123)
#'
#'##generate some fake data
#'########################
#'n <- 100
#'r <- 12
#'t <- matrix(rep(1:3), r/3, ncol=1, nrow=r)
#'sigma <- 0.4
#'b0 <- 1
#'
#'#under the null:
#'b1 <- 0
#'#under the alternative:
#'b1 <- 0.7
#'y.tilde <- b0 + b1*t + rnorm(r, sd = sigma)
#'y <- t(matrix(rnorm(n*r, sd = sqrt(sigma*abs(y.tilde))), ncol=n, nrow=r) +
#' matrix(rep(y.tilde, n), ncol=n, nrow=r))
#'x <- matrix(1, ncol=1, nrow=r)
#'
#'#run test
#'scoreTest <- vc_score(y, x, phi=t, w=matrix(1, ncol=ncol(y), nrow=nrow(y)),
#' Sigma_xi=matrix(1), indiv=rep(1:(r/3), each=3))
#'scoreTest$score
#'
#'@importFrom CompQuadForm davies
#'@importFrom stats model.matrix
#'
#'@export
vc_score <- function(y, x, indiv, phi, w, Sigma_xi = diag(ncol(phi)),
na_rm = FALSE) {
## validity checks
if (sum(!is.finite(w)) > 0) {
stop("At least 1 non-finite weight in 'w'")
}
## dimensions check------
stopifnot(is.matrix(y))
stopifnot(is.matrix(x))
stopifnot(is.matrix(phi))
g <- nrow(y) # the number of genes measured
n <- ncol(y) # the number of samples measured
p <- ncol(x) # the number of covariates
n_t <- ncol(phi) # the number of time bases
stopifnot(nrow(x) == n)
stopifnot(nrow(w) == g)
stopifnot(ncol(w) == n)
stopifnot(nrow(phi) == n)
stopifnot(length(indiv) == n)
# the number of random effects
if (length(Sigma_xi) == 1) {
K <- 1
Sigma_xi <- matrix(Sigma_xi, K, K)
} else {
K <- nrow(Sigma_xi)
stopifnot(ncol(Sigma_xi) == K)
}
stopifnot(n_t == K)
## data formating ------
indiv <- as.factor(indiv)
nb_indiv <- length(levels(indiv))
## OLS for conditional mean -----
y_T <- t(y)
if (na_rm & sum(is.na(y_T)) > 0) {
y_T0 <- y_T
y_T0[is.na(y_T0)] <- 0
yt_mu <- y_T - x %*% solve(crossprod(x)) %*% t(x) %*% y_T0
} else {
yt_mu <- y_T - x %*% solve(crossprod(x)) %*% t(x) %*% y_T
}
## x_tilde_list <- y_tilde_list <- Phi_list <- list()
## for (i in 1:nb_indiv) {
## select <- indiv==levels(indiv)[i]
## n_i <- length(which(select))
## x_i <- x[select,]
## y_i <- y[,select]
## phi_i <- phi[select,]
## Phi_list[[i]] <- kronecker(diag(g), phi_i)
## x_tilde_list[[i]] <- kronecker(diag(g), x_i)
## y_tilde_list[[i]] <- matrix(t(y_i), ncol=1)
## }
## x_tilde <- do.call(rbind, x_tilde_list)
## y_tilde <- do.call(rbind, y_tilde_list)
## Phi <- do.call(rbind, Phi_list)
## alpha <- solve(t(x_tilde)%*%x_tilde)%*%t(x_tilde)%*%y_tilde
## mu_new <- x_tilde %*% alpha
## y_mu <- y_tilde - mu_new
## test statistic computation ------
## q <- matrix(NA, nrow=nb_indiv, ncol=g*K)
## XT_i <- array(NA, c(nb_indiv, g*p, g*K))
## U <- matrix(NA, nrow = nb_indiv, ncol = p*g)
## long_indiv <- rep(indiv, each = g)
## xtx_inv <- solve(t(x_tilde) %*% x_tilde)
## Sigma_xi_new_sqrt <- kronecker(diag(g), (Sigma_xi*diag(K))%^% (-0.5))
## for (i in 1:nb_indiv){ #for all the genes at once
## select <- indiv==levels(indiv)[i]
## long_select <- long_indiv==levels(indiv)[i]
## y_mu_i <- as.vector(y_mu[long_select,])
## y_tilde_i <- c(t(y_ij))
## x_tilde_i <- x_tilde[long_select,]
## sigma_eps_inv_diag <- as.vector(t(w)[select,])#/sigma
## T_i <- sigma_eps_inv_diag*(Phi[long_select,] %*% Sigma_xi_new_sqrt)
## q[i,] <- c(y_mu_i %*% T_i)
## XT_i[i,,] <- t(x_tilde_i) %*% T_i
## U[i,] <- xtx_inv %*% t(x_tilde_i) %*% y_mu_i }
## XT <- colMeans(XT_i) q_ext <- q - U %*% XT
## sig_eps_inv <- w/sigma #no need as this just scales the test statistics
sig_xi_sqrt <- (Sigma_xi * diag(K)) %^% (-0.5)
sig_eps_inv_T <- t(w)
phi_sig_xi_sqrt <- phi %*% sig_xi_sqrt
T_fast <- do.call(cbind, replicate(K, sig_eps_inv_T, simplify = FALSE)) *
matrix(apply(phi_sig_xi_sqrt, 2, rep, g), ncol = g * K)
##---------------------
## the structure of T_fast is time_basis_1*gene_1, time_basis_1*gene_2, ...,
## time_basis_1*gene_p, ..., time_basis_K*gene_1, ..., time_basis_K*gene_p
##----------------------------
q_fast <- matrix(yt_mu, ncol = g * n_t, nrow = n) * T_fast
## dplyr seems to be less efficient here
## q_fast_tb <- tibble::as_tibble(cbind.data.frame(indiv, q_fast))
## q_dp <- q_fast_tb %>% group_by(indiv) %>% summarise_all(sum)
## aggregate is much slower also
## qtemp <- aggregate(. ~ indiv, cbind.data.frame(indiv, q_fast), sum)
## qtemp <- aggregate(. ~ indiv, cbind.data.frame(indiv, q_fast), sum)
## data.table hard to test, but seems to be at least 10 times slower on big
## datasets (weird)
## m_dt <- data.table('indiv'=factor(rep(c(1:20), each=5)), mbig)
## temp <- m_dt[, lapply(.SD, sum), by=indiv]
# the 2 'by' statements below used to represent the longest AND most memory
# intensive part of this for genewise analysis:
if (length(levels(indiv)) > 1) {
indiv_mat <- stats::model.matrix(~0 + factor(indiv))
} else {
indiv_mat <- matrix(as.numeric(indiv), ncol = 1)
}
if (na_rm & sum(is.na(q_fast)) > 0) {
q_fast[is.na(q_fast)] <- 0
}
q <- crossprod(indiv_mat, q_fast)
XT_fast <- crossprod(x, T_fast)/nb_indiv
avg_xtx_inv_tx <- nb_indiv * tcrossprod(solve(crossprod(x, x)), x)
U_XT <- matrix(yt_mu, ncol = g * n_t, nrow = n) *
crossprod(avg_xtx_inv_tx, XT_fast)
if (na_rm & sum(is.na(U_XT)) > 0) {
U_XT[is.na(U_XT)] <- 0
}
U_XT_indiv <- crossprod(indiv_mat, U_XT)
q_ext <- q - U_XT_indiv
# sapply(1:6, function(i){(q_ext[i,] - q_ext_fast_indiv[i,])})
qq <- colSums(q, na.rm = na_rm)^2/nb_indiv # genewise scores
##qq <- unlist(by(data=matrix(qq, ncol=1), INDICES=rep(1:g, K), FUN=sum,
## simplify = FALSE)) # veryslow
## gene_inds <- lapply(1:g, function(x){x + (g)*(0:(K-1))})
## gene_Q <- sapply(gene_inds, function(x) sum(qq[x])) # old computation
## gene_Q <- tcrossprod(qq, matrix(diag(g), nrow=g, ncol=g*K))[1, ] # faster
gene_Q <- rowSums(matrix(qq, ncol = K)) # even faster
QQ <- sum(qq) #nb_indiv=nrow(q) # set score
return(list(score = QQ, q = q, q_ext = q_ext,
gene_scores_unscaled = gene_Q))
}
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dearseq documentation built on Nov. 8, 2020, 5:49 p.m.
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Defines functions vc_score
Documented in vc_score
#'Computes variance component test statistic for longitudinal
#'
#'This function computes an approximation of the Variance Component test for a
#'mixture of \eqn{\chi^{2}}s using Davies method from
#'\code{\link[CompQuadForm]{davies}}
#'
#'@keywords internal
#'
#'@param y a numeric matrix of dim \code{g x n} containing the raw RNA-seq
#'counts for g genes from \code{n} samples
#'
#'@param x a numeric design matrix of dim \code{n x p} containing the \code{p}
#'covariates to be adjusted for
#'
#'@param indiv a vector of length \code{n} containing the information for
#'attributing each sample to one of the studied individuals. Coerced
#'to be a \code{factor}
#'
#'@param phi a numeric design matrix of size \code{n x K} containing the
#'\code{K} variables to be tested
#'
#'@param w a vector of length \code{n} containing the weights for the \code{n}
#'samples.
#'
#'@param Sigma_xi a matrix of size \code{K x K} containing the covariance matrix
#'of the \code{K} random effects on \code{phi}
#'
#'@param na_rm logical: should missing values (including \code{NA} and
#'\code{NaN}) be omitted from the calculations? Default is \code{FALSE}.
#'
#'@return A list with the following elements:\itemize{
#' \item \code{score}: approximation of the set observed score
#' \item \code{q}: observation-level contributions to the score
#' \item \code{q_ext}: pseudo-observations used to compute the covariance,
#' taking into account the contributions of OLS estimates
#' \item \code{gene_scores_unscaled}: a vector of the approximations of the
#' individual gene scores
#' }
#'
#'@seealso \code{\link[CompQuadForm]{davies}}
#'
#'@examples
#'set.seed(123)
#'
#'##generate some fake data
#'########################
#'n <- 100
#'r <- 12
#'t <- matrix(rep(1:3), r/3, ncol=1, nrow=r)
#'sigma <- 0.4
#'b0 <- 1
#'
#'#under the null:
#'b1 <- 0
#'#under the alternative:
#'b1 <- 0.7
#'y.tilde <- b0 + b1*t + rnorm(r, sd = sigma)
#'y <- t(matrix(rnorm(n*r, sd = sqrt(sigma*abs(y.tilde))), ncol=n, nrow=r) +
#' matrix(rep(y.tilde, n), ncol=n, nrow=r))
#'x <- matrix(1, ncol=1, nrow=r)
#'
#'#run test
#'scoreTest <- vc_score(y, x, phi=t, w=matrix(1, ncol=ncol(y), nrow=nrow(y)),
#' Sigma_xi=matrix(1), indiv=rep(1:(r/3), each=3))
#'scoreTest$score
#'
#'@importFrom CompQuadForm davies
#'@importFrom stats model.matrix
#'
#'@export
vc_score <- function(y, x, indiv, phi, w, Sigma_xi = diag(ncol(phi)),
na_rm = FALSE) {
## validity checks
if (sum(!is.finite(w)) > 0) {
stop("At least 1 non-finite weight in 'w'")
}
## dimensions check------
stopifnot(is.matrix(y))
stopifnot(is.matrix(x))
stopifnot(is.matrix(phi))
g <- nrow(y) # the number of genes measured
n <- ncol(y) # the number of samples measured
p <- ncol(x) # the number of covariates
n_t <- ncol(phi) # the number of time bases
stopifnot(nrow(x) == n)
stopifnot(nrow(w) == g)
stopifnot(ncol(w) == n)
stopifnot(nrow(phi) == n)
stopifnot(length(indiv) == n)
# the number of random effects
if (length(Sigma_xi) == 1) {
K <- 1
Sigma_xi <- matrix(Sigma_xi, K, K)
} else {
K <- nrow(Sigma_xi)
stopifnot(ncol(Sigma_xi) == K)
}
stopifnot(n_t == K)
## data formating ------
indiv <- as.factor(indiv)
nb_indiv <- length(levels(indiv))
## OLS for conditional mean -----
y_T <- t(y)
if (na_rm & sum(is.na(y_T)) > 0) {
y_T0 <- y_T
y_T0[is.na(y_T0)] <- 0
yt_mu <- y_T - x %*% solve(crossprod(x)) %*% t(x) %*% y_T0
} else {
yt_mu <- y_T - x %*% solve(crossprod(x)) %*% t(x) %*% y_T
}
## x_tilde_list <- y_tilde_list <- Phi_list <- list()
## for (i in 1:nb_indiv) {
## select <- indiv==levels(indiv)[i]
## n_i <- length(which(select))
## x_i <- x[select,]
## y_i <- y[,select]
## phi_i <- phi[select,]
## Phi_list[[i]] <- kronecker(diag(g), phi_i)
## x_tilde_list[[i]] <- kronecker(diag(g), x_i)
## y_tilde_list[[i]] <- matrix(t(y_i), ncol=1)
## }
## x_tilde <- do.call(rbind, x_tilde_list)
## y_tilde <- do.call(rbind, y_tilde_list)
## Phi <- do.call(rbind, Phi_list)
## alpha <- solve(t(x_tilde)%*%x_tilde)%*%t(x_tilde)%*%y_tilde
## mu_new <- x_tilde %*% alpha
## y_mu <- y_tilde - mu_new
## test statistic computation ------
## q <- matrix(NA, nrow=nb_indiv, ncol=g*K)
## XT_i <- array(NA, c(nb_indiv, g*p, g*K))
## U <- matrix(NA, nrow = nb_indiv, ncol = p*g)
## long_indiv <- rep(indiv, each = g)
## xtx_inv <- solve(t(x_tilde) %*% x_tilde)
## Sigma_xi_new_sqrt <- kronecker(diag(g), (Sigma_xi*diag(K))%^% (-0.5))
## for (i in 1:nb_indiv){ #for all the genes at once
## select <- indiv==levels(indiv)[i]
## long_select <- long_indiv==levels(indiv)[i]
## y_mu_i <- as.vector(y_mu[long_select,])
## y_tilde_i <- c(t(y_ij))
## x_tilde_i <- x_tilde[long_select,]
## sigma_eps_inv_diag <- as.vector(t(w)[select,])#/sigma
## T_i <- sigma_eps_inv_diag*(Phi[long_select,] %*% Sigma_xi_new_sqrt)
## q[i,] <- c(y_mu_i %*% T_i)
## XT_i[i,,] <- t(x_tilde_i) %*% T_i
## U[i,] <- xtx_inv %*% t(x_tilde_i) %*% y_mu_i }
## XT <- colMeans(XT_i) q_ext <- q - U %*% XT
## sig_eps_inv <- w/sigma #no need as this just scales the test statistics
sig_xi_sqrt <- (Sigma_xi * diag(K)) %^% (-0.5)
sig_eps_inv_T <- t(w)
phi_sig_xi_sqrt <- phi %*% sig_xi_sqrt
T_fast <- do.call(cbind, replicate(K, sig_eps_inv_T, simplify = FALSE)) *
matrix(apply(phi_sig_xi_sqrt, 2, rep, g), ncol = g * K)
##---------------------
## the structure of T_fast is time_basis_1*gene_1, time_basis_1*gene_2, ...,
## time_basis_1*gene_p, ..., time_basis_K*gene_1, ..., time_basis_K*gene_p
##----------------------------
q_fast <- matrix(yt_mu, ncol = g * n_t, nrow = n) * T_fast
## dplyr seems to be less efficient here
## q_fast_tb <- tibble::as_tibble(cbind.data.frame(indiv, q_fast))
## q_dp <- q_fast_tb %>% group_by(indiv) %>% summarise_all(sum)
## aggregate is much slower also
## qtemp <- aggregate(. ~ indiv, cbind.data.frame(indiv, q_fast), sum)
## qtemp <- aggregate(. ~ indiv, cbind.data.frame(indiv, q_fast), sum)
## data.table hard to test, but seems to be at least 10 times slower on big
## datasets (weird)
## m_dt <- data.table('indiv'=factor(rep(c(1:20), each=5)), mbig)
## temp <- m_dt[, lapply(.SD, sum), by=indiv]
# the 2 'by' statements below used to represent the longest AND most memory
# intensive part of this for genewise analysis:
if (length(levels(indiv)) > 1) {
indiv_mat <- stats::model.matrix(~0 + factor(indiv))
} else {
indiv_mat <- matrix(as.numeric(indiv), ncol = 1)
}
if (na_rm & sum(is.na(q_fast)) > 0) {
q_fast[is.na(q_fast)] <- 0
}
q <- crossprod(indiv_mat, q_fast)
XT_fast <- crossprod(x, T_fast)/nb_indiv
avg_xtx_inv_tx <- nb_indiv * tcrossprod(solve(crossprod(x, x)), x)
U_XT <- matrix(yt_mu, ncol = g * n_t, nrow = n) *
crossprod(avg_xtx_inv_tx, XT_fast)
if (na_rm & sum(is.na(U_XT)) > 0) {
U_XT[is.na(U_XT)] <- 0
}
U_XT_indiv <- crossprod(indiv_mat, U_XT)
q_ext <- q - U_XT_indiv
# sapply(1:6, function(i){(q_ext[i,] - q_ext_fast_indiv[i,])})
qq <- colSums(q, na.rm = na_rm)^2/nb_indiv # genewise scores
##qq <- unlist(by(data=matrix(qq, ncol=1), INDICES=rep(1:g, K), FUN=sum,
## simplify = FALSE)) # veryslow
## gene_inds <- lapply(1:g, function(x){x + (g)*(0:(K-1))})
## gene_Q <- sapply(gene_inds, function(x) sum(qq[x])) # old computation
## gene_Q <- tcrossprod(qq, matrix(diag(g), nrow=g, ncol=g*K))[1, ] # faster
gene_Q <- rowSums(matrix(qq, ncol = K)) # even faster
QQ <- sum(qq) #nb_indiv=nrow(q) # set score
return(list(score = QQ, q = q, q_ext = q_ext,
gene_scores_unscaled = gene_Q))
}
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