Transcriptional analysis of islets of Langerhans from organ donors of different ages

Author:

Seiron Peter,Stenwall Anton,Hedin Anders,Granlund Louise,Esguerra Jonathan Lou S.,Volkov Petr,Renström Erik,Korsgren Olle,Lundberg MarcusORCID,Skog Oskar

Abstract

Insulin secretion is impaired with increasing age. In this study, we aimed to determine whether aging induces specific transcriptional changes in human islets. Laser capture microdissection was used to extract pancreatic islet tissue from 37 deceased organ donors aged 1–81 years. The transcriptomes of the extracted islets were analysed using Ion AmpliSeq sequencing. 346 genes that co-vary significantly with age were found. There was an increased transcription of genes linked to senescence, and several aspects of the cell cycle machinery were downregulated with increasing age. We detected numerous genes not linked to aging in previous studies likely because earlier studies analysed islet cells isolated by enzymatic digestion which might affect the islet transcriptome. Among the novel genes demonstrated to correlate with age, we found an upregulation of SPP1 encoding osteopontin. In beta cells, osteopontin has been seen to be protective against both cytotoxicity and hyperglycaemia. In summary, we present a transcriptional profile of aging in human islets and identify genes that could affect disease course in diabetes.

Funder

Novo Nordisk Foundation

Diabetes Wellness Foundation Sweden Junior Grants

Juvenile Diabetes Foundation International

Magnus Bergvall foundation

Vetenskapsrådet

Åke Wiberg Stiftelse

Tore Nilsons Stiftelse för Medicinsk Forskning

The Ernfors Family Fund

Barndiabetesfonden

Åke Wiberg foundation

Swedish Diabetes Association

Sten A Olsson foundation

EFSD/Novo Nordisk Grant

Helmsley Charitable Trust

Diabetesfonden

Tore Nilsson foundation

Publisher

Public Library of Science (PLoS)

Subject

Multidisciplinary

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