AI Article Synopsis

  • Neonatal porcine islet-like cell clusters (NPCCs) from piglets show promise in treating type 1 diabetes in humans, but rejection due to xenoantigens is a major issue.
  • Researchers developed a novel nano-encapsulation method using bifunctional polymersomes (PSomes), which effectively targets and binds NPCCs to enhance transplantation success.
  • By encapsulating triiodothyronine (T3) in PSomes, the study finds improved glucose sensitivity and insulin secretion from NPCCs, suggesting a significant advance in islet cell encapsulation techniques.

Article Abstract

There is growing evidence that neonatal porcine islet-like cell clusters (NPCCs) isolated from piglets can be used to treat type 1 diabetes in humans. However, graft rejection is a common complication in humans owing to the prevalence of xenoantigens in porcine. Therefore, researchers have investigated various islet encapsulation techniques that could protect against these antigens. To this end, this study presents a robust nano-encapsulation method based on bifunctional polymersomes (PSomes), in which N-hydroxysuccinimide (NHS) and maleimide (Mal) groups conjugated to the PSomes terminal interact with the amine and thiol groups on the surface of NPCCs to induce dual targeting via two covalent bonds. The findings indicate that the ratio of NHS to Mal on PSomes is optimal for dual targeting. Moreover, triiodothyronine (T3) is known to promotes pancreatic islet maturation and differentiation of endocrine cells into beta cells. T3 encapsulated in PSomes is shown to increase the glucose sensitivity of NPCCs and enhance insulin secretion from NPCCs. Furthermore, improvements in the nano-encapsulation efficiency and insulin-secreting capability of NPCCs through dual targeting via dual-Psomes are demonstrated. In conclusion, the proposed nano-encapsulation technique could pave the way for significant advances in islet nano-encapsulation and the imprevement of NPCC immaturity via T3 release.

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Source
http://www.ncbi.nlm.nih.gov/pmc/articles/PMC10844179PMC
http://dx.doi.org/10.1186/s11671-024-03964-3DOI Listing

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