Alginate–Poly[2-(methacryloyloxy)ethyl]trimethylammonium Chloride (PMETAC) Immunoisolating Capsules Prolong the Viability of Pancreatic Islets In Vivo

Polina Ermakova(Privolzhsky Research Medical University), Ekaterina Vasilchikova(Privolzhsky Research Medical University), Arseniy L. Potapov(Privolzhsky Research Medical University), М. А. Батенькин(G.A. Razuvaev Institute of Organometallic Chemistry), L. A. Lugovaya(Privolzhsky Research Medical University), Alexandra Bogomolova(Privolzhsky Research Medical University), Julia Tselousova(Privolzhsky Research Medical University), А. Н. Конев(G.A. Razuvaev Institute of Organometallic Chemistry), Н. В. Анисимова(G.A. Razuvaev Institute of Organometallic Chemistry), Alena Egoshina(G.A. Razuvaev Institute of Organometallic Chemistry), Mariya Zakharina(G.A. Razuvaev Institute of Organometallic Chemistry), Nasipbek Naraliev(Privolzhsky Research Medical University), Denis Kuchin(Privolzhsky Research Medical University), В. Е. Загайнов(Privolzhsky Research Medical University), С. A. Чесноков(G.A. Razuvaev Institute of Organometallic Chemistry), Aleksandra Kashina(Privolzhsky Research Medical University), Elena V. Zagaynova(Privolzhsky Research Medical University)
Biomedicines
November 10, 2024
Cited by 2Open Access
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Abstract

BACKGROUND/OBJECTIVES: This study focuses on the development and evaluation of novel alginate-poly[2-(methacryloyloxy)ethyl]trimethylammonium chloride (PMETAC) microcapsules for encapsulating pancreatic islets to address insulin deficiency in diabetes. METHODS: In previous research, we fabricated and characterized PMETAC microcapsules, evaluating their stability and permeability in vitro. This study further probes the capsules in vivo, focusing on the functional activity of the encapsulated islets post-transplantation, their viability extension, and the assessment of the immunoprotective, antifibrotic properties, and biostability of the capsules. RESULTS: Rabbit-derived islets were encapsulated and transplanted into diabetic rats. The encapsulated islets maintained insulin secretion for up to 90 days, significantly longer than non-encapsulated ones, which ceased functioning after 7 days. Histological analysis demonstrated high biocompatibility of the PMETAC coating, resulting in minimal fibrotic overgrowth around the capsules. CONCLUSIONS: The study highlights the critical role of immunoprotection and the tendency to reduce fibrosis in prolonging islet function. These findings suggest that PMETAC-coated capsules offer a promising solution for cell-based therapies in diabetes by improving graft longevity and reducing fibrotic overgrowth.


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