AI Article Synopsis

  • This study focuses on the significance of beta cells in regulating blood sugar and addresses the need for new research tools to better understand pancreatic islet function for diabetes treatment.
  • The researchers developed a microporation technology that improves gene delivery into human pancreatic islets while maintaining their normal functions, such as secretion and cell viability.
  • The findings show that this method could effectively modify gene expression in both human and rodent islets, paving the way for further exploration of the mechanisms behind healthy islet function and potential diabetes therapies.

Article Abstract

Background: In view of the importance of beta cells in glucose homeostasis and the profound repercussions of beta cell pathology on human health, the acquisition of tools to study pancreatic islet function is essential for the design of alternative novel therapies for diabetes. One promising approach toward this goal involves the modification of gene expression profile of beta cells.

Results: This study describes a new method of gene and siRNA delivery into human pancreatic islets by microporation technology. We demonstrated that mild islet distention with accutase greatly enhanced the transfection efficiency without compromising in vitro function (secretion, apoptosis and viability). As an example, the recently identified gene involved in type 2 diabetes, ZnT8, can be over-expressed or silenced by RNA interference using this technology. Microporation can also be used on rodent islets.

Conclusions: Taken together, our results demonstrate that microporation technology can be used to modify gene expression in whole rodent and human islets without altering their in vitro function and will be key to the elucidation of the factors responsible for proper islet function.

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Source
http://www.ncbi.nlm.nih.gov/pmc/articles/PMC2853492PMC
http://dx.doi.org/10.1186/1472-6750-10-28DOI Listing

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