Your search keyword '"Parsons, Michael J"' showing total 2 results

1. Sox9b is a mediator of retinoic acid signaling restricting endocrine progenitor differentiation.

Author

Huang, Wei, Beer, Rebecca L., Delaspre, Fabien, Wang, Guangliang, Edelman, Hannah E., Park, Hyewon, Azuma, Mizuki, and Parsons, Michael J.

Subjects

*TRETINOIN, *PROGENITOR cells, *NOTCH signaling pathway, *SOX transcription factors, *CELL differentiation, *ALLELES, *REGENERATION (Biology), *PANCREATIC physiology

Abstract

Centroacinar cells (CACs) are ductal Notch-responsive progenitors that in the larval zebrafish pancreas differentiate to form new islets and ultimately contribute to the majority of the adult endocrine mass. Uncovering the mechanisms regulating CAC differentiation will facilitate understanding how insulin-producing β cells are formed. Previously we reported retinoic acid (RA) signaling and Notch signaling both regulate larval CAC differentiation, suggesting a shared downstream intermediate. Sox9b is a transcription factor important for islet formation whose expression is upregulated by Notch signaling in larval CACs. Here we report that sox9b expression in larval CACs is also regulated by RA signaling. Therefore, we hypothesized that Sox9b is an intermediate between both RA- and Notch-signaling pathways. In order to study the role of Sox9b in larval CACs, we generated two cre/lox based transgenic tools, which allowed us to express full-length or truncated Sox9b in larval CACs. In this way we were able to perform spatiotemporal-controlled Sox9b gain- and loss-of-function studies and observe the subsequent effect on progenitor differentiation. Our results are consistent with Sox9b regulating CAC differentiation by being a downstream intermediate of both RA- and Notch-signaling pathways. We also demonstrate that adult zebrafish with only one functional allele of sox9b undergo accelerated β-cell regeneration, an observation consistent with sox9b regulating CAC differentiation in adults. [ABSTRACT FROM AUTHOR]

Published

2016

2. Zebrafish sox9b is crucial for hepatopancreatic duct development and pancreatic endocrine cell regeneration

Author

Manfroid, Isabelle, Ghaye, Aurélie, Naye, François, Detry, Nathalie, Palm, Sarah, Pan, Luyuan, Ma, Taylur P., Huang, Wei, Rovira, Meritxell, Martial, Joseph A., Parsons, Michael J., Moens, Cecilia B., Voz, Marianne L., and Peers, Bernard

Subjects

*ZEBRA danio, *SOX transcription factors, *DEVELOPMENTAL biology, *PANCREATIC duct, *REGENERATION (Biology), *PANCREATIC beta cells, *EMBRYOLOGY, *MORPHOGENESIS, *BONE morphogenetic proteins

Abstract

Abstract: Recent zebrafish studies have shown that the late appearing pancreatic endocrine cells are derived from pancreatic ducts but the regulatory factors involved are still largely unknown. Here, we show that the zebrafish sox9b gene is expressed in pancreatic ducts where it labels the pancreatic Notch-responsive cells previously shown to be progenitors. Inactivation of sox9b disturbs duct formation and impairs regeneration of beta cells from these ducts in larvae. sox9b expression in the midtrunk endoderm appears at the junction of the hepatic and ventral pancreatic buds and, by the end of embryogenesis, labels the hepatopancreatic ductal system as well as the intrapancreatic and intrahepatic ducts. Ductal morphogenesis and differentiation are specifically disrupted in sox9b mutants, with the dysmorphic hepatopancreatic ducts containing misdifferentiated hepatocyte-like and pancreatic-like cells. We also show that maintenance of sox9b expression in the extrapancreatic and intrapancreatic ducts requires FGF and Notch activity, respectively, both pathways known to prevent excessive endocrine differentiation in these ducts. Furthermore, beta cell recovery after specific ablation is severely compromised in sox9b mutant larvae. Our data position sox9b as a key player in the generation of secondary endocrine cells deriving from pancreatic ducts in zebrafish. [Copyright &y& Elsevier]

Published

2012