Islet cell engraftment and control of diabetes in rats after transplantation of pig pancreatic anlagen

Rogers, Sharon A.; Chen, Feng; Talcott, Mike; Hammerman, Marc R.

doi:10.1152/ajpendo.00445.2003

Cited by 31 publications

(111 citation statements)

References 24 publications

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“…However, the immune suppression required to maintain the implants was either too toxic or included anti-CD40L, which cannot be used in human patients due to its thrombotic properties. Other studies suggested that E28 pancreatic tissue might be accepted in nonimmunosuppressed rats (33) and monkeys (34). In contrast, our mouse (9) and rat (35) data has revealed fierce rejection of pig embryonic tissue of any gestational time point in the absence of immune suppression, while demonstrating that the immunogenicity of E42 tissue was relatively lower compared to tissues harvested at E56 or beyond (9).…”

Section: Discussioncontrasting

confidence: 63%

Embryonic pig pancreatic tissue for the treatment of diabetes in a nonhuman primate model

Hecht

Eventov‐Friedman

Rosen

et al. 2009

Proc. Natl. Acad. Sci. U.S.A.

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Xenotransplantation of pig tissues has great potential to overcome the shortage of organ donors. One approach to address the vigorous immune rejection associated with xenotransplants is the use of embryonic precursor tissue, which induces and utilizes host vasculature upon its growth and development. Recently, we showed in mice that embryonic pig pancreatic tissue from embryonic day 42 (E42) exhibits optimal properties as a ␤ cell replacement therapy. We now demonstrate the proof of concept in 2 diabetic Cynomolgus monkeys, followed for 393 and 280 days, respectively. A marked reduction of exogenous insulin requirement was noted by the fourth month after transplantation, reaching complete independence from exogenous insulin during the fifth month after transplantation, with full physiological control of blood glucose levels. The porcine origin of insulin was documented by a radioimmunoassay specific for porcine C-peptide. Furthermore, the growing tissue was found to be predominantly vascularized with host blood vessels, thereby evading hyperacute or acute rejection, which could potentially be mediated by preexisting anti-pig antibodies. Durable graft protection was achieved, and most of the late complications could be attributed to the immunosuppressive protocol. While fine tuning of immune suppression, tissue dose, and implantation techniques are still required, our results demonstrate that porcine E-42 embryonic pancreatic tissue can normalize blood glucose levels in primates. Its long-term proliferative capacity, its revascularization by host endothelium, and its reduced immunogenicity, strongly suggest that this approach could offer an attractive replacement therapy for diabetes.immune-suppression ͉ rejection ͉ xeno-transplantation

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Section: Discussioncontrasting

confidence: 63%

Embryonic pig pancreatic tissue for the treatment of diabetes in a nonhuman primate model

Hecht

Eventov‐Friedman

Rosen

et al. 2009

Proc. Natl. Acad. Sci. U.S.A.

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“…Among them are such widespread diseases as diabetes, end-stage renal disease, Parkinson's disease, acute and chronic liver failure, and inherited metabolic disorders. The efficacy of committed embryonic pig or human kidney (13,28), pancreas (29)(30)(31)(32)(33)(34), lung (35), heart, or intestine (35,36) as well as hepatocytes (37)(38)(39)(40) or neuronal precursors (41)(42)(43), which grew and differentiated upon implantation into SCID or nude mice or rats, has been extensively Embryonic pig pancreas tissues obtained at various gestational ages were implanted under the kidney capsule. Tissue growth and serum levels of pig insulin were evaluated 6 weeks after implantation as described in Methods.…”

Section: Discussionmentioning

confidence: 99%

Embryonic pig liver, pancreas, and lung as a source for transplantation: Optimal organogenesis without teratoma depends on distinct time windows

Eventov‐Friedman

Katchman

Shezen

et al. 2005

Proc. Natl. Acad. Sci. U.S.A.

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Pig embryonic tissues represent an attractive option for organ transplantation. However, the achievement of optimal organogenesis after transplantation, namely, maximal organ growth and function without teratoma development, represents a major challenge. In this study, we determined distinct gestational time windows for the growth of pig embryonic liver, pancreas, and lung precursors. Transplantation of embryonic-tissue precursors at various gestational ages [from E (embryonic day) 21 to E100] revealed a unique pattern of growth and differentiation for each embryonic organ. Maximal liver growth and function were achieved at the earliest teratoma-free gestational age (E28), whereas the growth and functional potential of the pancreas gradually increased toward E42 and E56 followed by a marked decline in insulin-secreting capacity at E80 and E100. Development of mature lung tissue containing essential respiratory system elements was observed at a relatively late gestational age (E56). These findings, showing distinct, optimal gestational time windows for transplantation of embryonic pig liver, pancreas, and lung, might explain, in part, the disappointing results in previous transplantation trials and could help enhance the chances for successful implementation of embryonic pig tissue in the treatment of a wide spectrum of human diseases.fetal ͉ porcine ͉ gestational age ͉ growth potential

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“…[29][30][31][32][33][34][35][36][37][38] No matter whether dispersed or intact developing pancreas is transplanted, there is a selective survival of the endocrine portion (islets) of pancreatic anlagen grafts. In studies that compared directly, host beta cell mass post-transplantation of whole versus digested pancreas, it was found that mass was larger if whole pancreas were transplanted.…”

Section: Organogenesis Of the Endocrine Pancreasmentioning

confidence: 99%

“…30 We have transplanted pancreatic anlagen from embryos into the peritoneal membranes of rodents using techniques developed for the transplantation of metanephroi. 35,36 Rat to Rat Isotransplantation. Shown in Figure 7A is a photograph of a section of duodenum (duo) from an E12.5 Lewis rat embryo.…”

Section: Organogenesis Of the Endocrine Pancreasmentioning

confidence: 99%

“…10 To determine whether induction of normoglycemia in diabetic hosts can be accelerated if pancreatic anlagen are incubated with two of them prior to implantation, we added vascular endothelial growth factor (VEGF) and hepatocyte growth factor (HGF) in the media in which anlagen are stored prior to placement into hosts. 36 Rats in transplant, diabetic and control groups had levels of glucose measured during the next 40 weeks.…”

Section: Organogenesis Of the Endocrine Pancreasmentioning

confidence: 99%

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Pancreas and Kidney Transplantation Using Embryonic Donor Organs

Hammerman¹

2004

Organogenesis

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One novel solution to the shortage of human organs available for transplantation envisions 'growing' new organs in situ. This can be accomplished by transplantation of developing organ anlagen/primordia. We and others have shown that renal anlagen (metanephroi) transplanted into animal hosts undergo differentiation and growth, become vascularized by blood vessels of host origin and exhibit excretory function. Metanephroi can be stored for up to 3 days in vitro prior to transplantation with no impairment in growth or function post-implantation. Metanephroi can be transplanted across both concordant (rat to mouse) and highly disparate (pig to rodent) xenogeneic barriers. Similarly, pancreatic anlagen can be transplanted across concordant and highly disparate barriers, and undergo growth, differentiation and secrete insulin in a physiological manner following intra-peritoneal placement. Implantation of the embryonic pancreas, is followed by selective differentiation of islet components. Here we review studies exploring the potential therapeutic applicability for organogenesis of the kidney or endocrine pancreas.

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Islet cell engraftment and control of diabetes in rats after transplantation of pig pancreatic anlagen

Cited by 31 publications

References 24 publications

Embryonic pig pancreatic tissue for the treatment of diabetes in a nonhuman primate model

Embryonic pig pancreatic tissue for the treatment of diabetes in a nonhuman primate model

Embryonic pig liver, pancreas, and lung as a source for transplantation: Optimal organogenesis without teratoma depends on distinct time windows

Pancreas and Kidney Transplantation Using Embryonic Donor Organs

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