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Cell type-selective expression of circular RNAs in human pancreatic islets

Simranjeet Kaur, Aashiq H. Mirza, Flemming Pociot*

*Corresponding author for this work
32 Citations (Scopus)

Abstract

Understanding distinct cell-type specific gene expression in human pancreatic islets is important for developing islet regeneration strategies and therapies to improve β-cell function in type 1 diabetes (T1D). While numerous transcriptome-wide studies on human islet cell-types have focused on protein-coding genes, the non-coding repertoire, such as long non-coding RNA, including circular RNAs, remains mostly unexplored. Here, we explored transcriptional landscape of human α-, β-, and exocrine cells from published total RNA sequencing (RNA-seq) datasets to identify circular RNAs (circRNAs). Our analysis revealed that circRNAs are highly abundant in both α- and β-cells. We identified 10,830 high-confidence circRNAs expressed in human α-, β-, and exocrine cells. The most highly expressed candidates were MAN1A2, RMST, and HIPK3 across the three cell-types. Alternate circular isoforms were observed for circRNAs in the three cell-types, indicative of potential distinct functions. Highly selective α- and β-cell circRNAs were identified, which is suggestive of their potential role in regulating β-cell function.

Original languageEnglish
Article number38
JournalNon-Coding RNA
Volume4
Issue number4
ISSN2311-553X
DOIs
Publication statusPublished - 27 Nov 2018

Keywords

  • CircRNA
  • Circular RNAs
  • Human islets
  • RNA-seq
  • Type 1 diabetes
  • β-cell

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