In vitro expansion of pancreatic islet clusters facilitated by hormones and chemicals

Jing Yu Lin, Jie Cheng, Ya Qin Du, Wei Pan, Zhong Zhang, Jin Wang, Jie An, Fan Yang, Yun Fei Xu, Hui Lin, Wen Tao An, Jia Wang, Zhao Yang, Ren Jie Chai, Xue Ying Sha, Hui Li Hu, Jin Peng Sun, Xiao Yu*

*Corresponding author for this work

Research output: Contribution to journalArticlepeer-review

9 Citations (Scopus)

Abstract

Tissue regeneration, such as pancreatic islet tissue propagation in vitro, could serve as a promising strategy for diabetes therapy and personalised drug testing. However, such a strategy has not been realised yet. Propagation could be divided into two steps, in vitro expansion and repeated passaging. Even the first step of the in vitro islet expansion has not been achieved to date. Here, we describe a method that enables the expansion of islet clusters isolated from pregnant mice or wild-type rats by employing a combination of specific regeneration factors and chemical compounds in vitro. The expanded islet clusters expressed insulin, glucagon and somatostatin, which are markers corresponding to pancreatic β cells, α cells and δ cells, respectively. These different types of cells grouped together, were spatially organised and functioned similarly to primary islets. Further mechanistic analysis revealed that forskolin in our recipe contributed to renewal and regeneration, whereas exendin-4 was essential for preserving islet cell identity. Our results provide a novel method for the in vitro expansion of islet clusters, which is an important step forward in developing future protocols and media used for islet tissue propagation in vitro. Such method is important for future regenerative diabetes therapies and personalised medicines using large amounts of pancreatic islets derived from the same person.

Original languageEnglish
Article number20
JournalCell Discovery
Volume6
Issue number1
DOIs
Publication statusPublished - 1 Dec 2020
Externally publishedYes

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