PDX1LOW MAFALOW β-cells contribute to islet function and insulin release

Nasteska, Daniela; Fine, Nicholas H F; Ashford, Fiona B; Cuozzo, Federica; Viloria, Katrina; Smith, Gabrielle; Dahir, Aisha; Dawson, Peter W J; Lai, Yu-Chiang; Bastidas-Ponce, Aimée; Bakhti, Mostafa; Rutter, Guy A; Fiancette, Remi; Nano, Rita; Piemonti, Lorenzo; Lickert, Heiko; Zhou, Qiao; Akerman, Ildem; Hodson, David J

doi:10.1038/s41467-020-20632-z

Transcriptionally mature and immature β-cells co-exist within the adult islet. How such diversity contributes to insulin release remains poorly understood. Here we show that subtle differences in β-cell maturity, defined using PDX1 and MAFA expression, contribute to islet operation. Functional mapping of rodent and human islets containing proportionally more PDX1HIGH and MAFAHIGH β-cells reveals defects in metabolism, ionic fluxes and insulin secretion. At the transcriptomic level, the presence of increased numbers of PDX1HIGH and MAFAHIGH β-cells leads to dysregulation of gene pathways involved in metabolic processes. Using a chemogenetic disruption strategy, differences in PDX1 and MAFA expression are shown to depend on islet Ca2+ signaling patterns. During metabolic stress, islet function can be restored by redressing the balance between PDX1 and MAFA levels across the β-cell population. Thus, preserving heterogeneity in PDX1 and MAFA expression, and more widely in β-cell maturity, might be important for the maintenance of islet function.

PDX1LOW MAFALOW β-cells contribute to islet function and insulin release / Nasteska, Daniela; Fine, Nicholas H F; Ashford, Fiona B; Cuozzo, Federica; Viloria, Katrina; Smith, Gabrielle; Dahir, Aisha; Dawson, Peter W J; Lai, Yu-Chiang; Bastidas-Ponce, Aimée; Bakhti, Mostafa; Rutter, Guy A; Fiancette, Remi; Nano, Rita; Piemonti, Lorenzo; Lickert, Heiko; Zhou, Qiao; Akerman, Ildem; Hodson, David J. - In: NATURE COMMUNICATIONS. - ISSN 2041-1723. - 12:1(2021), p. 674. [10.1038/s41467-020-20632-z]