作者
Gillian M Beattie, Anthony MP Montgomery, Ana D Lopez, Ergeng Hao, Brandon Perez, Margaret L Just, Jonathan RT Lakey, Marquis E Hart, Alberto Hayek
发表日期
2002/12/1
期刊
Diabetes
卷号
51
期号
12
页码范围
3435-3439
出版商
American Diabetes Association
简介
Human islet expansion in monolayer culture leads to loss of function and senescence. By maintaining the 3-D configuration of islets in fibrin gels, it is feasible to expand β-cells in response to hepatocyte growth factor (HGF) while preserving physiologic glucose responsiveness both in vitro and in vivo after transplantation into nude mice. Islets were cultured free floating with or without growth factors and nicotinamide and in fibrin gels with the same conditions. Proliferation was observed only in islets cultured in fibrin gels and the cocktail; total insulin increased by threefold, with a concomitant increase in β-cell mass by morphometry. Insulin release after glucose challenge was also preserved. Islets in fibrin gels gave rise in vivo to large grafts rich in insulin and glucagon, and grafts from free-floating islets were smaller with fewer endocrine cells. Circulating human C-peptide levels were higher than in the mice receiving …
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