scholarly journals Enzyme Histochemistry in Experimental Diabetes Mellitus. The findings of several enzymez activities in pancreatic islet cells

1964 ◽  
Vol 1964 (5) ◽  
pp. 98-98
Author(s):  
Nobuo IHARA
1980 ◽  
Vol 89 (1) ◽  
pp. 63-65 ◽  
Author(s):  
V. I. Shumakov ◽  
B. I. Shal'nev ◽  
V. N. Blyumkin ◽  
N. N. Shaletskii ◽  
R. A. Babikova ◽  
...  

2019 ◽  
Author(s):  
Anna Gooch ◽  
Ping Zhang ◽  
Zhuma Hu ◽  
Natasha Loy Son ◽  
Nicole Avila ◽  
...  

AbstractWe previously reported that allogeneic, intraperitoneally administered “Neo-Islets,” composed of cultured pancreatic islet cells co-aggregated with high numbers of immunoprotective and cytoprotective Adipose-derived Stem Cells, reestablished, through omental engraftment, redifferentiation and splenic and omental up-regulation of Regulatory T-cells, normoglycemia in autoimmune Type-1 Diabetic Non-Obese Diabetic (NOD) mice without the use of immunosuppressive agents or encapsulation devices. Based on these observations, we are currently testing this Neo-Islet technology in an FDA guided Pilot Study (INAD 012-776) in insulin-dependent, spontaneously diabetic pet dogs by the intraperitoneal administration of 2×10e5 Neo-Islets/kilogram body weight to metabolically controlled (blood glucose, triglycerides, thyroid and adrenal functions) animals under sedation and local anesthesia and ultrasound guidance. We report here initial observations on the first 4 Neo-Islet-treated, insulin dependent pet dogs that are now in the intermediate-term follow-up phase of the study (> 6 months post treatment). Current results indicate that in dogs, Neo-Islets appear to engraft, redifferentiate and physiologically produce insulin, and are neither rejected by auto- or allo-immune attacks, as evidenced by (a) an absent IgG response to the allogeneic cells contained in the administered Neo-Islets, and (b) progressively improved glycemic control that achieves up to a 50% reduction in daily insulin needs paralleled by a significant fall in serum glucose levels. This is accomplished without the use of anti-rejection drugs or encapsulation devices. No adverse or serious adverse events related to the Neo-Islet administration have been observed to date. We conclude that this minimally invasive therapy has significant translational relevance to veterinary and clinical Type 1 Diabetes Mellitus by achieving complete and at this point partial glycemic control in two species, i.e., diabetic mice and dogs, respectively.


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