tests/testthat/test_calcNhoodExpression.R
In MikeDMorgan/miloR: Differential neighbourhood abundance testing on a graph
context("Testing calcNhoodExpression function")
library(miloR)
### Set up a mock data set using simulated data
library(SingleCellExperiment)
library(scran)
library(scater)
library(irlba)
library(MASS)
library(mvtnorm)
library(miloR)
set.seed(42)
r.n <- 1000
n.dim <- 50
block1.cells <- 500
# select a set of eigen values for the covariance matrix of each block, say 50 eigenvalues?
block1.eigens <- sapply(1:n.dim, FUN=function(X) rexp(n=1, rate=abs(runif(n=1, min=0, max=50))))
block1.eigens <- block1.eigens[order(block1.eigens)]
block1.p <- qr.Q(qr(matrix(rnorm(block1.cells^2, mean=4, sd=0.01), block1.cells)))
block1.sigma <- crossprod(block1.p, block1.p*block1.eigens)
block1.gex <- abs(rmvnorm(n=r.n, mean=rnorm(n=block1.cells, mean=2, sd=0.01), sigma=block1.sigma))
block2.cells <- 400
# select a set of eigen values for the covariance matrix of each block, say 50 eigenvalues?
block2.eigens <- sapply(1:n.dim, FUN=function(X) rexp(n=1, rate=abs(runif(n=1, min=0, max=50))))
block2.eigens <- block2.eigens[order(block2.eigens)]
block2.p <- qr.Q(qr(matrix(rnorm(block2.cells^2, mean=4, sd=0.01), block2.cells)))
block2.sigma <- crossprod(block2.p, block2.p*block2.eigens)
block2.gex <- abs(rmvnorm(n=r.n, mean=rnorm(n=block2.cells, mean=4, sd=0.01), sigma=block2.sigma))
block3.cells <- 200
# select a set of eigen values for the covariance matrix of each block, say 50 eigenvalues?
block3.eigens <- sapply(1:n.dim, FUN=function(X) rexp(n=1, rate=abs(runif(n=1, min=0, max=50))))
block3.eigens <- block3.eigens[order(block3.eigens)]
block3.p <- qr.Q(qr(matrix(rnorm(block3.cells^2, mean=4, sd=0.01), block3.cells)))
block3.sigma <- crossprod(block3.p, block3.p*block3.eigens)
block3.gex <- abs(rmvnorm(n=r.n, mean=rnorm(n=block3.cells, mean=5, sd=0.01), sigma=block3.sigma))
sim1.gex <- do.call(cbind, list("b1"=block1.gex, "b2"=block2.gex, "b3"=block3.gex))
colnames(sim1.gex) <- paste0("Cell", 1:ncol(sim1.gex))
rownames(sim1.gex) <- paste0("Gene", 1:nrow(sim1.gex))
sim1.pca <- prcomp_irlba(t(sim1.gex), n=50+1, scale.=TRUE, center=TRUE)
set.seed(42)
block1.cond <- rep("A", block1.cells)
block1.a <- sample(1:block1.cells, size=floor(block1.cells*0.9))
block1.b <- setdiff(1:block1.cells, block1.a)
block1.cond[block1.b] <- "B"
block2.cond <- rep("A", block2.cells)
block2.a <- sample(1:block2.cells, size=floor(block2.cells*0.05))
block2.b <- setdiff(1:block2.cells, block2.a)
block2.cond[block2.b] <- "B"
block3.cond <- rep("A", block3.cells)
block3.a <- sample(1:block3.cells, size=floor(block3.cells*0.5))
block3.b <- setdiff(1:block3.cells, block3.a)
block3.cond[block3.b] <- "B"
meta.df <- data.frame("Block"=c(rep("B1", block1.cells), rep("B2", block2.cells), rep("B3", block3.cells)),
"Condition"=c(block1.cond, block2.cond, block3.cond),
"Replicate"=c(rep("R1", floor(block1.cells*0.33)), rep("R2", floor(block1.cells*0.33)),
rep("R3", block1.cells-(2*floor(block1.cells*0.33))),
rep("R1", floor(block2.cells*0.33)), rep("R2", floor(block2.cells*0.33)),
rep("R3", block2.cells-(2*floor(block2.cells*0.33))),
rep("R1", floor(block3.cells*0.33)), rep("R2", floor(block3.cells*0.33)),
rep("R3", block3.cells-(2*floor(block3.cells*0.33)))))
colnames(meta.df) <- c("Block", "Condition", "Replicate")
# define a "sample" as teh combination of condition and replicate
meta.df$Sample <- paste(meta.df$Condition, meta.df$Replicate, sep="_")
meta.df$Vertex <- c(1:nrow(meta.df))
sim1.sce <- SingleCellExperiment(assays=list(logcounts=sim1.gex),
reducedDims=list("PCA"=sim1.pca$x))
sim1.mylo <- Milo(sim1.sce)
sim1.mylo <- buildGraph(sim1.mylo, k=21, d=30)
test_that("Incorrect/missing inputs produce proper errors", {
# test without running makeNhoods
expect_error(calcNhoodExpression(sim1.mylo),
"No neighbourhoods found - run makeNhoods first")
# pass a list but no expression
sim1.mylo <- makeNhoods(sim1.mylo, k=21, prop=0.1, refined=TRUE,
d=30,
reduced_dims="PCA")
expect_error(calcNhoodExpression(nhoods(sim1.mylo)),
"No expression data found. Please specific a gene expression matrix to exprs")
})
sim1.mylo <- makeNhoods(sim1.mylo, k=21, prop=0.1, refined=TRUE,
d=30,
reduced_dims="PCA")
test_that("Same output is generated by different input types", {
# do the Milo and list inputs generate the same result?
expect_equal(nhoodExpression(calcNhoodExpression(nhoods(sim1.mylo),
exprs=logcounts(sim1.mylo))),
nhoodExpression(calcNhoodExpression(sim1.mylo)))
})
test_that("Subsetting produces the expected output dimensionality", {
set.seed(42)
subset.genes <- sample(1:nrow(sim1.mylo), size=500)
# test with different inputs
expect_identical(nrow(nhoodExpression(calcNhoodExpression(sim1.mylo, subset.row=subset.genes))),
length(subset.genes))
expect_identical(nrow(nhoodExpression(calcNhoodExpression(nhoods(sim1.mylo),
exprs=logcounts(sim1.mylo),
subset.row=subset.genes))),
length(subset.genes))
})
MikeDMorgan/miloR documentation built on Feb. 29, 2024, 6:20 p.m.
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context("Testing calcNhoodExpression function")
library(miloR)
### Set up a mock data set using simulated data
library(SingleCellExperiment)
library(scran)
library(scater)
library(irlba)
library(MASS)
library(mvtnorm)
library(miloR)
set.seed(42)
r.n <- 1000
n.dim <- 50
block1.cells <- 500
# select a set of eigen values for the covariance matrix of each block, say 50 eigenvalues?
block1.eigens <- sapply(1:n.dim, FUN=function(X) rexp(n=1, rate=abs(runif(n=1, min=0, max=50))))
block1.eigens <- block1.eigens[order(block1.eigens)]
block1.p <- qr.Q(qr(matrix(rnorm(block1.cells^2, mean=4, sd=0.01), block1.cells)))
block1.sigma <- crossprod(block1.p, block1.p*block1.eigens)
block1.gex <- abs(rmvnorm(n=r.n, mean=rnorm(n=block1.cells, mean=2, sd=0.01), sigma=block1.sigma))
block2.cells <- 400
# select a set of eigen values for the covariance matrix of each block, say 50 eigenvalues?
block2.eigens <- sapply(1:n.dim, FUN=function(X) rexp(n=1, rate=abs(runif(n=1, min=0, max=50))))
block2.eigens <- block2.eigens[order(block2.eigens)]
block2.p <- qr.Q(qr(matrix(rnorm(block2.cells^2, mean=4, sd=0.01), block2.cells)))
block2.sigma <- crossprod(block2.p, block2.p*block2.eigens)
block2.gex <- abs(rmvnorm(n=r.n, mean=rnorm(n=block2.cells, mean=4, sd=0.01), sigma=block2.sigma))
block3.cells <- 200
# select a set of eigen values for the covariance matrix of each block, say 50 eigenvalues?
block3.eigens <- sapply(1:n.dim, FUN=function(X) rexp(n=1, rate=abs(runif(n=1, min=0, max=50))))
block3.eigens <- block3.eigens[order(block3.eigens)]
block3.p <- qr.Q(qr(matrix(rnorm(block3.cells^2, mean=4, sd=0.01), block3.cells)))
block3.sigma <- crossprod(block3.p, block3.p*block3.eigens)
block3.gex <- abs(rmvnorm(n=r.n, mean=rnorm(n=block3.cells, mean=5, sd=0.01), sigma=block3.sigma))
sim1.gex <- do.call(cbind, list("b1"=block1.gex, "b2"=block2.gex, "b3"=block3.gex))
colnames(sim1.gex) <- paste0("Cell", 1:ncol(sim1.gex))
rownames(sim1.gex) <- paste0("Gene", 1:nrow(sim1.gex))
sim1.pca <- prcomp_irlba(t(sim1.gex), n=50+1, scale.=TRUE, center=TRUE)
set.seed(42)
block1.cond <- rep("A", block1.cells)
block1.a <- sample(1:block1.cells, size=floor(block1.cells*0.9))
block1.b <- setdiff(1:block1.cells, block1.a)
block1.cond[block1.b] <- "B"
block2.cond <- rep("A", block2.cells)
block2.a <- sample(1:block2.cells, size=floor(block2.cells*0.05))
block2.b <- setdiff(1:block2.cells, block2.a)
block2.cond[block2.b] <- "B"
block3.cond <- rep("A", block3.cells)
block3.a <- sample(1:block3.cells, size=floor(block3.cells*0.5))
block3.b <- setdiff(1:block3.cells, block3.a)
block3.cond[block3.b] <- "B"
meta.df <- data.frame("Block"=c(rep("B1", block1.cells), rep("B2", block2.cells), rep("B3", block3.cells)),
"Condition"=c(block1.cond, block2.cond, block3.cond),
"Replicate"=c(rep("R1", floor(block1.cells*0.33)), rep("R2", floor(block1.cells*0.33)),
rep("R3", block1.cells-(2*floor(block1.cells*0.33))),
rep("R1", floor(block2.cells*0.33)), rep("R2", floor(block2.cells*0.33)),
rep("R3", block2.cells-(2*floor(block2.cells*0.33))),
rep("R1", floor(block3.cells*0.33)), rep("R2", floor(block3.cells*0.33)),
rep("R3", block3.cells-(2*floor(block3.cells*0.33)))))
colnames(meta.df) <- c("Block", "Condition", "Replicate")
# define a "sample" as teh combination of condition and replicate
meta.df$Sample <- paste(meta.df$Condition, meta.df$Replicate, sep="_")
meta.df$Vertex <- c(1:nrow(meta.df))
sim1.sce <- SingleCellExperiment(assays=list(logcounts=sim1.gex),
reducedDims=list("PCA"=sim1.pca$x))
sim1.mylo <- Milo(sim1.sce)
sim1.mylo <- buildGraph(sim1.mylo, k=21, d=30)
test_that("Incorrect/missing inputs produce proper errors", {
# test without running makeNhoods
expect_error(calcNhoodExpression(sim1.mylo),
"No neighbourhoods found - run makeNhoods first")
# pass a list but no expression
sim1.mylo <- makeNhoods(sim1.mylo, k=21, prop=0.1, refined=TRUE,
d=30,
reduced_dims="PCA")
expect_error(calcNhoodExpression(nhoods(sim1.mylo)),
"No expression data found. Please specific a gene expression matrix to exprs")
})
sim1.mylo <- makeNhoods(sim1.mylo, k=21, prop=0.1, refined=TRUE,
d=30,
reduced_dims="PCA")
test_that("Same output is generated by different input types", {
# do the Milo and list inputs generate the same result?
expect_equal(nhoodExpression(calcNhoodExpression(nhoods(sim1.mylo),
exprs=logcounts(sim1.mylo))),
nhoodExpression(calcNhoodExpression(sim1.mylo)))
})
test_that("Subsetting produces the expected output dimensionality", {
set.seed(42)
subset.genes <- sample(1:nrow(sim1.mylo), size=500)
# test with different inputs
expect_identical(nrow(nhoodExpression(calcNhoodExpression(sim1.mylo, subset.row=subset.genes))),
length(subset.genes))
expect_identical(nrow(nhoodExpression(calcNhoodExpression(nhoods(sim1.mylo),
exprs=logcounts(sim1.mylo),
subset.row=subset.genes))),
length(subset.genes))
})
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