Repository Akfar Bumi Siliwangi
Construction and Transfer of PEI-miRNA-126/210 Polyplex into Human Umbilical Vein Endothelial Cells with Investigation of Its Effect on Islets Survival and Function
Description:
Background: Type 1 diabetes is an autoimmune disorder characterized by the loss of pancreatic
islets. Islet allotransplantation is a potentially beneficial therapeutic approach for diabetes. Islets
suffer a variety of cellular insults including ischemia and partial vascular loss during isolation,
resulting in a significant reduction in viability prior to transplantation. The present study aimed
to investigate the effect of angiogenic microRNA (miRNA)-126 and -210 on islet function and
viability in an indirect way.
Methods: Poly Ethylenimine (PEI)-miRNA-126 and -210 polyplexes were constructed at various
Nitrogen/Phosphate (N/P) ratios. After confirmation by gel retardation and ethidium bromide
dye exclusion assay, its cytotoxicity and transfection efficiency were analyzed by MTT and
fluorescent assays, respectively. After that, the selected polyplexes were used to transfect Human
Umbilical Vein Endothelial Cells (HUVECs) in vitro and were indirectly co-cultured with islet
cells for three days. Real-time polymerase chain reaction and enzyme-linked immunoassay were
conducted to verify the regulation of target genes and the functionality of the islets.
Results: The findings showed that PEI could condense miRNAs at N/P=5. The viability of the
HUVECs was decreased by increasing the amount of PEI. Additionally, ployplex-126 and -210
led to a decrease in the expressions of target genes, phosphoinositol-3 kinase regulatory subunit
2, sprouty-related EVH1 domain-containing protein 1, and ephrin-A3 in the islets. Moreover,
the expressions of Bax and Bcl2 and their ratio in the treated groups by polyplex-126 and -210
led to better survival and function of the islets, with a higher expression of insulin and response
to glucose stimulations. Furthermore, polyplex-210 could downregulate the anti-angiogenic
protein, thrombospondin 1, compared to the other groups. Finally, the secretion of C-peptide
was higher in polyplex-210 than in the other groups, adjusted for insulin secretion.
Conclusion: The results indicated that angiogenic miRNAs could promote the survival and
function of islet cells by interacting with their targets
URL:
http://103.158.96.210:88/web_repository/uploads/ps-29-90.pdf
Type:
Journal
Document:
Diploma III Farmasi
Date:
23-06-2024
Author:
Fatemeh Sabet Sarvestani