MafA and MafB regulate genes critical to beta-cells in a unique temporal manner

MafA 和 MafB 以独特的时间方式调控对 β 细胞至关重要的基因

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作者:Isabella Artner, Yan Hang, Magdalena Mazur, Tsunehiko Yamamoto, Min Guo, Jill Lindner, Mark A Magnuson, Roland Stein

Conclusions

Our results provide insight into the sequential manner by which MafA and MafB regulate islet β-cell formation and maturation.

Methods

The distribution of MafA and MafB in the β-cell population was determined immunohistochemically at various developmental and perinatal stages in mice. To identify genes regulated by MafB, microarray profiling was performed on wild-type and MafB(-/-) pancreata at embryonic day 18.5, with candidates evaluated by quantitative RT-PCR and in situ hybridization. The potential role of MafA in the expression of verified targets was next analyzed in adult islets of a pancreas-wide MafA mutant (termed MafA(ΔPanc)).

Objective

Several transcription factors are essential to pancreatic islet β-cell development, proliferation, and activity, including MafA and MafB. However, MafA and MafB are distinct from others in regard to temporal and islet cell expression pattern, with β-cells affected by MafB only during development and exclusively by MafA in the adult. Our aim was to define the functional relationship between these closely related activators to the β-cell. Research design and

Results

MafB was produced in a larger fraction of β-cells than MafA during development and found to regulate potential effectors of glucose sensing, hormone processing, vesicle formation, and insulin secretion. Notably, expression from many of these genes was compromised in MafA(ΔPanc) islets, suggesting that MafA is required to sustain expression in adults. Conclusions: Our results provide insight into the sequential manner by which MafA and MafB regulate islet β-cell formation and maturation.

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