Adult Duct-Lining Cells Can Reprogram into β-like Cells Able to Counter Repeated Cycles of Toxin-Induced Diabetes

Al-Hasani, Keith; Pfeifer, Anja; Courtney, Monica; Ben-Othman, Nouha; Gjernes, Elisabet; Vieira, Andhira; Druelle, Noémie; Avolio, Fabio; Ravassard, Philippe; Leuckx, Gunter; Lacas‐Gervais, Sandra; Ambrosetti, Damien; Benizri, Emmanuel; Hecksher‐Sørensen, Jacob; Gounon, Pierre; Ferrer, Jorge; Gradwohl, Gérard; Heimberg, Harry; Mansouri, Ahmed; Collombat, Patrick

doi:10.1016/j.devcel.2013.05.018

Cited by 177 publications

(203 citation statements)

References 35 publications

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“…Al-Hasani et al [65] recently reported that upon Pax4 misexpression, adult alpha cells are converted into insulinproducing cells, independent of their age, mutation state or microenvironment. They also report a duct cell to beta-like cell regeneration pathway that could be repeatedly activated by streptozotocin injury in an age-dependent manner.…”

Section: Adulthoodmentioning

confidence: 99%

The regulation of pre- and post-maturational plasticity of mammalian islet cell mass

Mezza

Kulkarni

2014

Diabetologia

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Regeneration of mature cells that produce functional insulin represents a major focus and a challenge of current diabetes research aimed at restoring beta cell mass in patients with most forms of diabetes, as well as in ageing. The capacity to adapt to diverse physiological states during life and the consequent ability to cope with increased metabolic demands in the normal regulation of glucose homeostasis is a distinctive feature of the endocrine pancreas in mammals. Both beta and alpha cells, and presumably other islet cells, are dynamically regulated via nutrient, neural and/or hormonal activation of growth factor signalling and the post-transcriptional modification of a variety of genes or via the microbiome to continually maintain a balance between regeneration (e.g. proliferation, neogenesis) and apoptosis. Here we review key regulators that determine islet cell mass at different ages in mammals. Understanding the chronobiology and the dynamics and agedependent processes that regulate the relationship between the different cell types in the overall maintenance of an optimally functional islet cell mass could provide important insights into planning therapeutic approaches to counter and/or prevent the development of diabetes.

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Section: Adulthoodmentioning

confidence: 99%

The regulation of pre- and post-maturational plasticity of mammalian islet cell mass

Mezza

Kulkarni

2014

Diabetologia

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“…Néanmoins, les relations de lignage entre précurseurs canalaires, cellules exprimant Neurog3 et cellules endocrines restent floues et controversées [15,24] (➜). Après avoir confirmé par immunomarquage la réex-pression de Neurog3 dans les cellules canalaires des animaux transgé-niques exprimant Pax4 dans les cellules , nous avons croisé ces souris avec un autre modèle transgénique, ce qui nous a permis d'observer le devenir de ces cellules canalaires [26]. Nos résultats démontrent que les cellules qui réactivent Neurog3 adoptent un destin endocrine, et SYNTHÈSE REVUES rentes combinaisons de facteurs de transcription (Neurog3, Pdx1 et MafA [musculoaponeurotic fibrosarcoma oncogene homolog A)]) permet la conversion des cellules acinaires infectées en cellules -like chez la souris adulte.…”

Section: Les Canaux Pancréatiques : Une Source Potentielle De Précursunclassified

Reprogrammation des cellules pancréatiques en cellules β

et al. 2013

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“…We therefore generated animals allowing the forced expression of Pax4 in a-cells and animals permitting the specific loss of Arx expression in a-cells. [3][4][5] In both instances, a conversion of a-cells into b-like cells was indeed observed. Surprisingly, we also outlined continued processes of compensatory a-cell neogenesis, such cells being again turned into b-like cells upon Pax4 misexpression/Arx inactivation.…”

mentioning

confidence: 74%

“…Importantly, the b-like cells thereby generated were found to be functional and able to replace their endogenous counterparts in vivo. [3][4][5] Lastly, further worked provided evidences that the main trigger of the conversion of a-cells into b-like cells (and the ensuing cycle of b-like cell neogenesis) was the downregulation of Arx activity, Pax4 misexpression mainly acting to decrease Arx expression. 5 Even though promising, these results remained far from a putative medical application.…”

mentioning

confidence: 99%