Normal glucagon signaling and β-cell function after near-total α-cell ablation in adult mice.

Herrera, P.L.

doi:10.2337/db11-0876

Titre

Normal glucagon signaling and β-cell function after near-total α-cell ablation in adult mice.

Type

article

Institution

UNIL/CHUV/Unisanté + institutions partenaires

Périodique

Diabetes

Auteur(s)

Thorel, F.

Auteure/Auteur

Damond, N.

Auteure/Auteur

Chera, S.

Auteure/Auteur

Wiederkehr, A.

Auteure/Auteur

Thorens, B.

Auteure/Auteur

Meda, P.

Auteure/Auteur

Wollheim, C.B.

Auteure/Auteur

Herrera, P.L.

Auteure/Auteur

Liens vers les personnes

Thorens, Bernard

Liens vers les unités

CIG

Dép. des Sciences Biomédicales

Groupe Thorens

ISSN

1939-327X

Statut éditorial

Publié

Date de publication

2011

Volume

60

Numéro

11

Première page

2872

Dernière page/numéro d’article

2882

Langue

anglais

Résumé

OBJECTIVEEvaluate whether healthy or diabetic adult mice can tolerate an extreme loss of pancreatic α-cells and how this sudden massive depletion affects β-cell function and blood glucose homeostasis.RESEARCH DESIGN AND METHODSWe generated a new transgenic model allowing near-total α-cell removal specifically in adult mice. Massive α-cell ablation was triggered in normally grown and healthy adult animals upon diphtheria toxin (DT) administration. The metabolic status of these mice was assessed in 1) physiologic conditions, 2) a situation requiring glucagon action, and 3) after β-cell loss.RESULTSAdult transgenic mice enduring extreme (98%) α-cell removal remained healthy and did not display major defects in insulin counter-regulatory response. We observed that 2% of the normal α-cell mass produced enough glucagon to ensure near-normal glucagonemia. β-Cell function and blood glucose homeostasis remained unaltered after α-cell loss, indicating that direct local intraislet signaling between α- and β-cells is dispensable. Escaping α-cells increased their glucagon content during subsequent months, but there was no significant α-cell regeneration. Near-total α-cell ablation did not prevent hyperglycemia in mice having also undergone massive β-cell loss, indicating that a minimal amount of α-cells can still guarantee normal glucagon signaling in diabetic conditions.CONCLUSIONSAn extremely low amount of α-cells is sufficient to prevent a major counter-regulatory deregulation, both under physiologic and diabetic conditions. We previously reported that α-cells reprogram to insulin production after extreme β-cell loss and now conjecture that the low α-cell requirement could be exploited in future diabetic therapies aimed at regenerating β-cells by reprogramming adult α-cells.

PID Serval

serval:BIB_16B62B557AAA

DOI

10.2337/db11-0876

PMID

21926270

WOS

000296954600026

Permalien

https://iris.unil.ch/handle/iris/34543

Open Access

Oui

Date de création

2011-10-13T09:32:18.230Z

Date de création dans IRIS

2025-05-20T13:25:22Z

Fichier(s)

Nom

BIB_16B62B557AAA.P001.pdf

Version du manuscrit

preprint

Taille

2.14 MB

Format

Adobe PDF

PID Serval

serval:BIB_16B62B557AAA.P001

URN

urn:nbn:ch:serval-BIB_16B62B557AAA7

Somme de contrôle

(MD5):5440287d48af0aaea27add621ec5ef45