NKX6.1 Promotes PDX-1-Induced Liver to Pancreatic β-Cells Reprogramming

Gefen-Halevi, Shiraz; Rachmut, Itzhak H.; Molakandov, Kfir; Berneman, Dana; Mor, Eytan; Meivar‐Levy, Irit; Ferber, Sarah

doi:10.1089/cell.2010.0030

Cited by 59 publications

(56 citation statements)

References 50 publications

Supporting

Mentioning

Contrasting

Order By: Relevance

“…Specifically, continuous expression of NKX6-1 in the entire pancreatic progenitor pool significantly represses Ptf1a expression, preventing acinar cell differentiation, and favours an endocrine over a ductal cell fate choice (Schaffer et al 2010). In the post-natal pancreas, nuclear NKX6-1 expression is restricted to endocrine b-cells (Sander et al 2000), and it has been shown that induction of NKX6-1 expression in PDX1-expressing liver cells promotes endocrine cell reprogramming (Gefen-Halevi et al 2010). The presence of NEUROG3 and NKX6-1 expression in a subpopulation of ductal cells indicates that these cells have an endocrine progenitor-like phenotype.…”

Section: Discussionmentioning

confidence: 99%

Gastrin induces ductal cell dedifferentiation and β-cell neogenesis after 90% pancreatectomy

Téllez¹,

Montanya²

2014

Journal of Endocrinology

View full text Add to dashboard Cite

Induction of b-cell mass regeneration is a potentially curative treatment for diabetes. We have recently found that long-term gastrin treatment results in improved metabolic control and b-cell mass expansion in 95% pancreatectomised (Px) rats. In this study, we investigated the underlying mechanisms of gastrin-induced b-cell mass expansion after Px. After 90%-Px, rats were treated with gastrin (PxCG) or vehicle (PxCV), pancreatic remnants were harvested on days 1, 3, 5, 7, and 14 and used for gene expression, protein immunolocalisation and morphometric analyses. Gastrin-and vehicle-treated Px rats showed similar blood glucose levels throughout the study. Initially, after Px, focal areas of regeneration, showing mesenchymal cells surrounding ductal structures that expressed the cholecystokinin B receptor, were identified. These focal areas of regeneration were similar in size and cell composition in the PxCG and PxCV groups. However, in the PxCG group, the ductal structures showed lower levels of keratin 20 and b-catenin (indicative of duct dedifferentiation) and higher levels of expression of neurogenin 3 and NKX6-1 (indicative of endocrine progenitor phenotype), as compared with PxCV rats. In PxCG rats, b-cell mass and the number of scattered b-cells were significantly increased compared with PxCV rats, whereas b-cell replication and apoptosis were similar in the two groups. These results indicate that gastrin treatment-enhanced dedifferentiation and reprogramming of regenerative ductal cells in Px rats, increased b-cell neogenesis and fostered b-cell mass expansion.

show abstract

Section: Discussionmentioning

confidence: 99%

Gastrin induces ductal cell dedifferentiation and β-cell neogenesis after 90% pancreatectomy

Téllez¹,

Montanya²

2014

Journal of Endocrinology

View full text Add to dashboard Cite

show abstract

“…In addition, recent studies have exploited the known islet transcriptional networks to transdifferentiate nonpancreatic or exocrine tissue into endocrine cells. Ectopic expression of different combinations of pancreatic transcription factors-including Pdx1, Ngn3, NeuroD, MafA, and Nkx6.1-promotes liver-to-pancreatic b-cell reprogramming Kojima et al 2003;Song et al 2007;Delisle et al 2009;Nagaya et al 2009;Gefen-Halevi et al 2010). Similarly, ectopic expression of a defined set of transcription factors in adult pancreatic acinar cells results in an acinar-to-b-cell conversion (Zhou et al 2008).…”

mentioning

confidence: 99%

Nkx2.2 repressor complex regulates islet β-cell specification and prevents β-to-α-cell reprogramming

Papizan¹,

Singer²,

Tschen³

et al. 2011

Genes Dev.

179

187

View full text Add to dashboard Cite

Regulation of cell differentiation programs requires complex interactions between transcriptional and epigenetic networks. Elucidating the principal molecular events responsible for the establishment and maintenance of cell fate identities will provide important insights into how cell lineages are specified and maintained and will improve our ability to recapitulate cell differentiation events in vitro. In this study, we demonstrate that Nkx2.2 is part of a large repression complex in pancreatic b cells that includes DNMT3a, Grg3, and HDAC1. Mutation of the endogenous Nkx2.2 tinman (TN) domain in mice abolishes the interaction between Nkx2.2 and Grg3 and disrupts b-cell specification. Furthermore, we demonstrate that Nkx2.2 preferentially recruits Grg3 and HDAC1 to the

show abstract

“…It has been demonstrated that ectopic expression of Nkx6.1 alone is not a strong inducer of upper-hierarchy β-cell transcription factor expression, and that only upon coexpression with Pdx-1 was it capable of substantial insulin expression and glucose-responsive secretion of insulin. 150 The lack of expression of the full hierarchy of β-cell transcription factors makes Nkx6.1 a mediocre choice for the generation of artificial β-cells for analysis in animal models of diabetes.…”

Section: 144mentioning

confidence: 99%

Diabetes reversal via gene transfer: building on successes in animal models

Gerace¹,

Martiniello‐Wilks²,

Simpson³

2015

RRED

View full text Add to dashboard Cite

Type 1 diabetes (T1D) is caused by the autoimmune destruction of the insulinproducing pancreatic β-cells. People with T1D manage their hyperglycemia using daily insulin injections; however, this does not prevent the development of long-term diabetic complications such as retinopathy, nephropathy, neuropathy, and various macrovascular disorders. Currently, the only "cure" for T1D is pancreas transplantation or islet-cell transplantation; however, this is hampered by the limited number of donors and the requirement for life-long immunosuppression. As a result, the need for alternative therapies is vital. One of the strategies employed to correct T1D is the use of gene transfer to generate the production of an "artificial" β-cell that is capable of secreting insulin in response to fluctuating glucose concentrations that normally occurs in people without T1D. The treatment of many diseases using cell and gene therapy is generating significant attention in the T1D research community; however, for a cell therapy to enter clinical trials, success and safety must first be shown in an appropriate animal model. Animal models have been used in diabetes research for over a century, have improved our understanding of the pathophysiology of diabetes, and have led to the discovery of useful drugs for the treatment of the disease. Currently, the nonobese diabetic mouse is the animal model of choice for the study of T1D as it most closely reflects disease development in humans. The aim of this review is to evaluate the success of cell and gene therapy to reverse T1D in animal models for future clinical application.

show abstract

NKX6.1 Promotes PDX-1-Induced Liver to Pancreatic β-Cells Reprogramming

Cited by 59 publications

References 50 publications

Gastrin induces ductal cell dedifferentiation and β-cell neogenesis after 90% pancreatectomy

Gastrin induces ductal cell dedifferentiation and β-cell neogenesis after 90% pancreatectomy

Nkx2.2 repressor complex regulates islet β-cell specification and prevents β-to-α-cell reprogramming

Diabetes reversal via gene transfer: building on successes in animal models

Contact Info

Product

Resources

About