A new graph-based clustering method with application to single-cell RNA-seq data from human pancreatic islets

Hao Wu; Disheng Mao; Yuping Zhang; Zhiyi Chi; Michael Stitzel; Zhengqing Ouyang

doi:10.1093/nargab/lqaa087

A new graph-based clustering method with application to single-cell RNA-seq data from human pancreatic islets

NAR Genom Bioinform. 2021 Jan 12;3(1):lqaa087. doi: 10.1093/nargab/lqaa087. eCollection 2021 Mar.

Authors

Hao Wu¹, Disheng Mao¹, Yuping Zhang¹, Zhiyi Chi¹, Michael Stitzel², Zhengqing Ouyang³

Affiliations

¹ Department of Statistics, University of Connecticut, 215 Glenbrook Rd., Storrs, CT 06269, USA.
² The Jackson Laboratory for Genomic Medicine, 10 Discovery Drive, Farmington, CT 06032, USA.
³ Department of Biostatistics and Epidemiology, School of Public Health and Health Sciences, University of Massachusetts, 715 North Pleasant Street, Amherst, MA 01003, USA.

Abstract

Traditional bulk RNA-sequencing of human pancreatic islets mainly reflects transcriptional response of major cell types. Single-cell RNA sequencing technology enables transcriptional characterization of individual cells, and thus makes it possible to detect cell types and subtypes. To tackle the heterogeneity of single-cell RNA-seq data, powerful and appropriate clustering is required to facilitate the discovery of cell types. In this paper, we propose a new clustering framework based on a graph-based model with various types of dissimilarity measures. We take the compositional nature of single-cell RNA-seq data into account and employ log-ratio transformations. The practical merit of the proposed method is demonstrated through the application to the centered log-ratio-transformed single-cell RNA-seq data for human pancreatic islets. The practical merit is also demonstrated through comparisons with existing single-cell clustering methods. The R-package for the proposed method can be found at https://github.com/Zhang-Data-Science-Research-Lab/LrSClust.