Pancreatic islet-autonomous insulin and smoothened-mediated signalling modulate identity changes of glucagon+ α-cells

Cigliola, Valentina; Ghila, Luiza; Thorel, Fabrizio; Gurp, Léon van; Baronnier, Delphine; Oropeza, Daniel; Gupta, Saloni; Miyatsuka, Takeshi; Kaneto, Hideaki; Magnuson, Mark A.; Osipovich, Anna B.; Sander, Maike; Wright, Christopher E V; Thomas, Melissa K.; Furuyama, Kenichiro; Chera, Simona; Herrera, Pedro Luis

doi:10.1038/s41556-018-0216-y

Cited by 51 publications

(66 citation statements)

References 50 publications

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“…In these mice, the DTR is specifically overexpressed on the surface of the β‐cells, under the control of the RIP. As previously described, upon diphtheria toxin (DT) administration, the β‐cell compartment is specifically ablated with extremely high and reproducible efficiency (97.88% in NSG RIP‐DTR, Figure B,C), similar to the one reported for SCID RIP‐DTR (97.8%) . Ablated animals developed hyperglycaemia and displayed lower weight compared to their normoglycaemic counterparts (Figure D,E).…”

Section: Resultssupporting

confidence: 71%

“…The mice were given ad libitum access to water and standard diet RM1A (SDS). First group received three intraperitoneally (ip) DT (Sigma, cat.# D0564‐1MG) injections to induce diabetes as previously described . Blood glucose was monitored twice a week at 4‐5 pm with a Contour XT glucometer (Bayer) to confirm diabetes (blood glucose >300 mg/dL on 2 consecutive measurements).…”

Section: Methodsmentioning

confidence: 99%

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In vivo hyperglycaemia exposure elicits distinct period‐dependent effects on human pancreatic progenitor differentiation, conveyed by oxidative stress

et al. 2020

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Aim The loss of insulin‐secreting β‐cells, ultimately characterizing most diabetes forms, demands the development of cell replacement therapies. The common endpoint for all ex vivo strategies is transplantation into diabetic patients. However, the effects of hyperglycaemia environment on the transplanted cells were not yet properly assessed. Thus, the main goal of this study was to characterize global effect of brief and prolonged in vivo hyperglycaemia exposure on the cell fate acquisition and maintenance of transplanted human pancreatic progenitors. Methods To rigorously study the effect of hyperglycaemia, in vitro differentiated human‐induced pluripotent stem cells (hiPSC)‐derived pancreatic progenitors were xenotransplanted in normoglycaemic and diabetic NSG rat insulin promoter (RIP)‐diphtheria toxin receptor (DTR) mice. The transplants were retrieved after 1‐week or 1‐month exposure to overt hyperglycaemia and analysed by large‐scale microscopy or global proteomics. For this study we pioneer the use of the NSG RIP‐DTR system in the transplantation of hiPSC, making use of its highly reproducible specific and absolute β‐cell ablation property in the absence of inflammation or other organ toxicity. Results Here we show for the first time that besides the presence of an induced oxidative stress signature, the cell fate and proteome landscape response to hyperglycaemia was different, involving largely different mechanisms, according to the period spent in the hyperglycaemic environment. Surprisingly, brief hyperglycaemia exposure increased the bihormonal cell number by impeding the activity of specific islet lineage determinants. Moreover, it activated antioxidant and inflammation protection mechanisms signatures in the transplanted cells. In contrast, the prolonged exposure was characterized by decreased numbers of hormone + cells, low/absent detoxification signature, augmented production of oxygen reactive species and increased apoptosis. Conclusion Hyperglycaemia exposure induced distinct, period‐dependent, negative effects on xenotransplanted human pancreatic progenitor, affecting their energy homeostasis, cell fate acquisition and survival.

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Section: Resultssupporting

confidence: 71%

Section: Methodsmentioning

confidence: 99%

In vivo hyperglycaemia exposure elicits distinct period‐dependent effects on human pancreatic progenitor differentiation, conveyed by oxidative stress

et al. 2020

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“…Their identification as regeneration modulators through gene profiling analyses will be cumbersome. As mentioned above, we have found, for instance, that insulin and hedgehog signaling in pancreatic islets are such players …”

Section: Resultsmentioning

confidence: 63%

“…Hence, Hedgehog and Insulin signaling are, together with other pathways not yet identified, natural brakes making α-cells to preserve their identity. 102 By using a wide range of genetic tools, recent studies have revealed that α-to-β transdifferentiation can be artificially potentiated by the concomitant inhibition of the key α-cell-specific transcription factor Arx and the epigenetic modifier DNMT1. 103 This suggests that α-cells are epigenetically locked, and that these brakes can be released.…”

Section: Pancreasmentioning

confidence: 99%

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Tissue repair brakes: A common paradigm in the biology of regeneration

et al. 2019

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To date, most attention on tissue regeneration has focused on the exploration of positive cues promoting or allowing the engagement of natural cellular restoration upon injury. In contrast, the signals fostering cell identity maintenance in the vertebrate body have been poorly investigated; yet they are crucial, for their counteraction could become a powerful method to induce and modulate regeneration. Here we review the mechanisms inhibiting pro‐regenerative spontaneous adaptive cell responses in different model organisms and organs. The pharmacological or genetic/epigenetic modulation of such regenerative brakes could release a dormant but innate adaptive competence of certain cell types and therefore boost tissue regeneration in different situations.

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Pancreatic Endocrine–Exocrine Relationship

Furuyama

Kawaguchi

2023

The Pancreas

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Pancreatic islet-autonomous insulin and smoothened-mediated signalling modulate identity changes of glucagon+ α-cells

Cited by 51 publications

References 50 publications

In vivo hyperglycaemia exposure elicits distinct period‐dependent effects on human pancreatic progenitor differentiation, conveyed by oxidative stress

In vivo hyperglycaemia exposure elicits distinct period‐dependent effects on human pancreatic progenitor differentiation, conveyed by oxidative stress

Tissue repair brakes: A common paradigm in the biology of regeneration

Pancreatic Endocrine–Exocrine Relationship

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