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  • Abnormal regulation of glucagon secretion by human islet alpha cells in the absence of beta cells.

Abnormal regulation of glucagon secretion by human islet alpha cells in the absence of beta cells.

EBioMedicine (2019-11-30)
Wei Liu, Tatsuya Kin, Siuhong Ho, Craig Dorrell, Sean R Campbell, Ping Luo, Xiaojuan Chen
ZUSAMMENFASSUNG

The understanding of the regulation of glucagon secretion by pancreatic islet α-cells remains elusive. We aimed to develop an in vitro model for investigating the function of human α-cells under direct influence of glucose and other potential regulators. Highly purified human α-cells from islets of deceased donors were re-aggregated in the presence or absence of β-cells in culture, evaluated for glucagon secretion under various treatment conditions, and compared to that of intact human islets and non-sorted islet cell aggregates. The pure human α-cell aggregates maintained proper glucagon secretion capability at low concentrations of glucose, but failed to respond to changes in ambient glucose concentration. Addition of purified β-cells, but not the secreted factors from β-cells at low or high concentrations of glucose, partly restored the responsiveness of α-cells to glucose with regulated glucagon secretion. The EphA stimulator ephrinA5-fc failed to mimic the inhibitory effect of β-cells on glucagon secretion. Glibenclamide inhibited glucagon secretion from islets and the α- and β-mixed cell-aggregates, but not from the α-cell-only aggregates, at 2.0 mM glucose. This study validated the use of isolated and then re-aggregated human islet cells for investigating α-cell function and paracrine regulation, and demonstrated the importance of cell-to-cell contact between α- and β-cells on glucagon secretion. Loss of proper β- and α-cell physical interaction in islets likely contributes to the dysregulated glucagon secretion in diabetic patients. Re-aggregated select combinations of human islet cells provide unique platforms for studying islet cell function and regulation.

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Sigma-Aldrich
Propidiumjodid, ≥94.0% (HPLC)
Sigma-Aldrich
Low Trypsin-High EDTA, PBS Based, 0.025% Trypsin and 0.75mM EDTA (1X), without Ca2+ and Mg2+, The Low Trypsin-High EDTA, PBS Based, 0.025% Trypsin & 0.75mM EDTA (1X), without Ca 2+ & Mg 2+ is available in a 100 mL format.
Sigma-Aldrich
Fluoreszeindiacetat, used as cell viability stain
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Monoklonales ANTI-Glucagon in Maus hergestellte Antikörper, clone K79bB10, ascites fluid
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Glybenclamid, ≥99% (HPLC)
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Somatostatin, powder, BioReagent, suitable for cell culture