Human umbilical cord perivascular cells improve human pancreatic islet transplant function by increasing vascularization

脐带 小岛 医学 病理 移植 解剖 糖尿病 内科学 内分泌学
作者
Shareen Forbes,Andrew Bond,Kayleigh Thirlwell,Paul S. Burgoyne,Kay Samuel,June Noble,Gary Borthwick,David Colligan,Neil McGowan,Philip Starkey Lewis,Alasdair R. Fraser,Joanne C. Mountford,Roderick N. Carter,Nicholas M. Morton,Marc L. Turner,Gerard J. Graham,John Campbell
出处
期刊:Science Translational Medicine [American Association for the Advancement of Science]
卷期号:12 (526) 被引量:48
标识
DOI:10.1126/scitranslmed.aan5907
摘要

Islet transplantation is an efficacious therapy for type 1 diabetes; however, islets from multiple donor pancreata are required, and a gradual attrition in transplant function is seen. Here, we manufactured human umbilical cord perivascular mesenchymal stromal cells (HUCPVCs) to Good Manufacturing Practice (GMP) standards. HUCPVCs showed a stable phenotype while undergoing rapid ex vivo expansion at passage 2 (p2) to passage 4 (p4) and produced proregenerative factors, strongly suppressing T cell responses in the resting state and in response to inflammation. Transplanting an islet equivalent (IEQ):HUCPVC ratio of 1:30 under the kidney capsule in diabetic NSG mice demonstrated the fastest return to normoglycemia by 3 days after transplant: Superior glycemic control was seen at both early (2.7 weeks) and later stages (7, 12, and 16 weeks) versus ratios of 1:0, 1:10, and 1:50, respectively. Syngeneic islet transplantation in immunocompetent mice using the clinically relevant hepatic portal route with a marginal islet mass showed that mice transplanted with an IEQ:HUCPVC ratio of 1:150 had superior glycemic control versus ratios of 1:0, 1:90, and 1:210 up to 6 weeks after transplant. Immunodeficient mice transplanted with human islets (IEQ:HUCPVC ratio of 1:150) exhibited better glycemic control for 7 weeks after transplant versus islet transplant alone, and islets transplanted via the hepatic portal vein in an allogeneic mouse model using a curative islet mass demonstrated delayed rejection of islets when cotransplanted with HUCPVCs (IEQ:HUCPVC ratio of 1:150). The immunosuppressive and proregenerative properties of HUCPVCs demonstrated long-term positive effects on graft function in vivo, indicating that they may improve long-term human islet allotransplantation outcomes.
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