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  #1   ^
Old Tue, May-16-17, 06:28
teaser's Avatar
teaser teaser is offline
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Default Beta cell implant in a human

https://www.sciencedaily.com/releas...70511083806.htm

Quote:
Novel tissue-engineered islet transplant achieves insulin independence in type 1 diabetes

Scientists from the Diabetes Research Institute (DRI) at the University of Miami Miller School of Medicine have produced the first clinical results demonstrating that pancreatic islet cells transplanted within a tissue-engineered platform can successfully engraft and achieve insulin independence in type 1 diabetes. The findings, published in the May 11 issue of the New England Journal of Medicine, are part of an ongoing clinical study to test this novel strategy as an important step toward offering this life-changing cell replacement therapy to millions living with the disease.

Islet transplantation has demonstrated the ability to restore natural insulin production and eliminate severe hypoglycemia in people with type 1 diabetes. The insulin-producing cells have traditionally been implanted within the liver, but this transplant site poses some limitations for emerging applications, leading researchers to investigate other options. DRI scientists have focused on the omentum, an apron-like tissue covering abdominal organs, which is easily accessed with minimally invasive surgery and has the same blood supply and physiological drainage characteristics as the pancreas.

"The objective of testing this novel tissue-engineered platform is to initially determine that insulin-producing cells can function in this new site, and subsequently introduce additional technologies towards our ultimate goal to replace the pancreatic endocrine function lost in type 1 diabetes without the need for anti-rejection drugs, what we call the DRI BioHub," explains Camillo Ricordi, M.D., director of the DRI and the Stacy Joy Goodman Professor of Surgery, Distinguished Professor of Medicine, Professor of Biomedical Engineering, Microbiology and Immunology at the University of Miami Miller School. Dr. Ricordi also serves as director of the DRI's Cell Transplant Center.

This was the first successful tissue-engineered "mini pancreas" that has achieved long-term insulin independence in a patient with type 1 diabetes. The biological platform was made by combining donor islets with the patient's own (autologous) blood plasma, which was laparoscopically layered onto the omentum. Clinical-grade thrombin was then layered over the islet/plasma mixture. Together, these substances create a gel-like material that sticks to the omentum and holds the islets in place. Over time, the body will absorb the gel, leaving the islets intact. The technique has been designed to minimize the inflammatory reaction that is normally observed when islets are implanted in the liver or in other sites with immediate contact to blood. The DRI's clinical trial, an important first step toward developing the BioHub mini organ, includes the immunosuppressive regimen currently used for clinical islet transplantation studies.

"The results thus far have shown that the omentum appears to be a viable site for islet implantation using this new platform technique," said lead author David Baidal, M.D., Assistant Professor of Medicine and member of the DRI's Clinical Cell Transplant team. "Data from our study and long-term follow up of additional omental islet transplants will determine the safety and feasibility of this strategy of islet transplantation, but we are quite excited about what we are seeing now."

In type 1 diabetes, the insulin-producing cells of the pancreas have been mistakenly destroyed by the immune system, requiring patients to manage their blood sugar levels through a daily regimen of insulin therapy. Islet transplantation has allowed many patients to live without the need for insulin injections after receiving a transplant of donor cells. Some patients who have received islet transplants at the DRI have been insulin independent for more than a decade, as DRI researchers have published.



The omentum drains into the portal vein, so I think you'd be missing some of the first pass insulin signalling within the pancreas itself that decreases glucagon, but this does give the liver the opportunity to do the lion's share of the insulin and glucose uptake that it's supposed to do.

Not much glucose uptake, in this case;

http://www.nejm.org/doi/suppl/10.10...59_appendix.pdf

That's a supplement to the article;

Quote:
Following islet transplantation, a gradual weight loss of 8.2 Kg was observed by 6
months post-transplant. Her weight stabilized and plateaued at 45.5 Kg after a
nutritional evaluation and resumption of a balanced diet. Weight loss post islet
transplantation is not unexpected and has been previously reported.
2 Possible
contributing factors include optimization of insulin requirements (i.e., elimination of
exogenous insulin administration and physiologic endogenous insulin delivery) and a
reduction in carbohydrate intake, in part due to the resolution of hypoglycemia.




Quote:
The patient has continued to exercise regularly doing
mostly aerobic exercises and follows a healthy low carbohydrate diet. We speculate that
these factors likely contribute to her stable glycemic control.
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  #2   ^
Old Tue, May-16-17, 10:17
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GRB5111 GRB5111 is offline
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Very exciting potential option for Type 1s. Funny how a healthy low carb diet is in the midst of all the recovery protocol. Some day, we'll just call it a healthy diet, as the low carb part will be assumed.
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