Insulin mutations impair beta-cell development in a patient-derived iPSC model of neonatal diabetes

Diego Balboa; Jonna Saarimäki-Vire; Daniel Borshagovski; Mantas Survila; Päivi Lindholm; Emilia Galli; Solja Eurola; Jarkko Ustinov; Heli Grym; Hanna Huopio; Juha Partanen; Kirmo Wartiovaara; Timo Otonkoski

doi:10.7554/eLife.38519

Insulin mutations impair beta-cell development in a patient-derived iPSC model of neonatal diabetes

Elife. 2018 Nov 9:7:e38519. doi: 10.7554/eLife.38519.

Authors

Affiliations

¹ Research Programs Unit, Molecular Neurology and Biomedicum Stem Cell Centre, Faculty of Medicine, University of Helsinki, Helsinki, Finland.
² Department of Biosciences, University of Helsinki, Helsinki, Finland.
³ Institute of Biotechnology, Helsinki Institute of Life Science, University of Helsinki, Helsinki, Finland.
⁴ University of Eastern Finland and Kuopio University Hospital, Kuopio, Finland.
⁵ Clinical Genetics, HUSLAB, Helsinki University Central Hospital, Helsinki, Finland.
⁶ Children's Hospital, University of Helsinki and Helsinki University Hospital, Helsinki, Finland.

Abstract

Insulin gene mutations are a leading cause of neonatal diabetes. They can lead to proinsulin misfolding and its retention in endoplasmic reticulum (ER). This results in increased ER-stress suggested to trigger beta-cell apoptosis. In humans, the mechanisms underlying beta-cell failure remain unclear. Here we show that misfolded proinsulin impairs developing beta-cell proliferation without increasing apoptosis. We generated induced pluripotent stem cells (iPSCs) from people carrying insulin (INS) mutations, engineered isogenic CRISPR-Cas9 mutation-corrected lines and differentiated them to beta-like cells. Single-cell RNA-sequencing analysis showed increased ER-stress and reduced proliferation in INS-mutant beta-like cells compared with corrected controls. Upon transplantation into mice, INS-mutant grafts presented reduced insulin secretion and aggravated ER-stress. Cell size, mTORC1 signaling, and respiratory chain subunits expression were all reduced in INS-mutant beta-like cells, yet apoptosis was not increased at any stage. Our results demonstrate that neonatal diabetes-associated INS-mutations lead to defective beta-cell mass expansion, contributing to diabetes development.

Keywords: CRISPR-Cas9; Insulin gene mutations; beta-cell development; endoplasmic reticulum stress; human; induced pluripotent stem cells; mTORC1; regenerative medicine; stem cells.

Publication types

Research Support, Non-U.S. Gov't

MeSH terms

Animals
Apoptosis / genetics
CRISPR-Cas Systems / genetics
Cell Differentiation / genetics
Cell Proliferation / genetics
Diabetes Mellitus / genetics*
Diabetes Mellitus / pathology
Endoplasmic Reticulum / genetics
Endoplasmic Reticulum Stress / genetics*
Female
Humans
Induced Pluripotent Stem Cells / chemistry*
Induced Pluripotent Stem Cells / metabolism
Infant, Newborn
Insulin-Secreting Cells / chemistry
Insulin-Secreting Cells / metabolism
Male
Mice
Mutation
Proinsulin / chemistry
Proinsulin / genetics*
Protein Folding
Sequence Analysis, RNA
Signal Transduction
Single-Cell Analysis

Substances

Proinsulin

Supplementary concepts

Diabetes Mellitus, Permanent Neonatal

Grants and funding

The funders had no role in study design, data collection and interpretation, or the decision to submit the work for publication.