ICM.EM_structure: ICM-EM algorithm implementation with organized paramters
In PRECAST: Embedding and Clustering with Alignment for Spatial Datasets
ICM.EM_structure R Documentation
ICM-EM algorithm implementation with organized paramters
Description
Efficient data integration as well as spatial clustering for multiple spatial transcriptomics data
Usage
ICM.EM_structure(XList, K, AdjList, q=15,parameterList=NULL)
Arguments
XList
an M-length list consisting of multiple matrices with class dgCMatrix or matrix that specify the log-normalization gene expression matrix for each data sample used for PRECAST model.
K
a positive integer allowing scalar or vector, specify the number of clusters in model fitting.
AdjList
an M-length list of sparse matrices with class dgCMatrix, specify the adjacency matrix used for Potts model and Intrisic CAR model in PRECAST model. We provide this interface for those users who would like to define the adjacency matrix by their own.
q
a positive integer, specify the number of latent features to be extracted, default as 15.
parameterList
Other arguments in PRECAST model, it can be set by model_set.
Details
Nothing
Value
ICM.EM_structure returns a list with class "SeqK_PRECAST_Object" with the number of components equal to the length of K, where each component includes the model fitting results for one number of cluster and is a list consisting of following components:
cluster
an M-length list that includes the inferred class labels for each data sample.
hZ
an M-length list that includes the batch corrected low-dimensional embeddings for each data sample.
hV
an M-length list that includes the estimate the ICAR component for each sample.
Rf
an M-length list that includes the posterior probability of domain clusters for each sample.
beta
an M-length vector that includes the estimated smoothing parameters for each sample.
Mu
mean vectors of mixtures components.
Sigma
covariance matrix of mixtures components.
W
estimated loading matrix
Lam
estimated variance of errors in probabilistic PCA model
loglik
pseudo observed log-likelihood.
Note
nothing
Author(s)
Wei Liu
References
See Also
None
Examples
## we generate the spatial transcriptomics data with lattice neighborhood, i.e. ST platform.
library(Matrix)
q <- 10; K <- 4
data(PRECASTObj)
posList <- lapply(PRECASTObj@seulist, function(x) cbind(x$row, x$col))
AdjList <- lapply(posList, getAdj_reg, platform='ST')
XList <- lapply(PRECASTObj@seulist, function(x) t(x[['RNA']]@data))
XList <- lapply(XList, scale, scale=FALSE)
parList <- model_set(maxIter=4)
resList <- ICM.EM_structure(XList, AdjList = AdjList,
q=q, K=K, parameterList=parList)
PRECAST documentation built on May 29, 2024, 3 a.m.
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| ICM.EM_structure | R Documentation |
ICM-EM algorithm implementation with organized paramters
Description
Efficient data integration as well as spatial clustering for multiple spatial transcriptomics data
Usage
ICM.EM_structure(XList, K, AdjList, q=15,parameterList=NULL)
Arguments
XList |
an M-length list consisting of multiple matrices with class |
K |
a positive integer allowing scalar or vector, specify the number of clusters in model fitting. |
AdjList |
an M-length list of sparse matrices with class |
q |
a positive integer, specify the number of latent features to be extracted, default as 15. |
parameterList |
Other arguments in PRECAST model, it can be set by model_set. |
Details
Nothing
Value
ICM.EM_structure returns a list with class "SeqK_PRECAST_Object" with the number of components equal to the length of K, where each component includes the model fitting results for one number of cluster and is a list consisting of following components:
cluster |
an M-length list that includes the inferred class labels for each data sample. |
hZ |
an M-length list that includes the batch corrected low-dimensional embeddings for each data sample. |
hV |
an M-length list that includes the estimate the ICAR component for each sample. |
Rf |
an M-length list that includes the posterior probability of domain clusters for each sample. |
beta |
an M-length vector that includes the estimated smoothing parameters for each sample. |
Mu |
mean vectors of mixtures components. |
Sigma |
covariance matrix of mixtures components. |
W |
estimated loading matrix |
Lam |
estimated variance of errors in probabilistic PCA model |
loglik |
pseudo observed log-likelihood. |
Note
nothing
Author(s)
Wei Liu
References
See Also
None
Examples
## we generate the spatial transcriptomics data with lattice neighborhood, i.e. ST platform.
library(Matrix)
q <- 10; K <- 4
data(PRECASTObj)
posList <- lapply(PRECASTObj@seulist, function(x) cbind(x$row, x$col))
AdjList <- lapply(posList, getAdj_reg, platform='ST')
XList <- lapply(PRECASTObj@seulist, function(x) t(x[['RNA']]@data))
XList <- lapply(XList, scale, scale=FALSE)
parList <- model_set(maxIter=4)
resList <- ICM.EM_structure(XList, AdjList = AdjList,
q=q, K=K, parameterList=parList)
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