4.2 Review

Xenotransplantation of pancreatic and kidney primordia-Where do we stand?

Journal

TRANSPLANT IMMUNOLOGY
Volume 21, Issue 2, Pages 93-100

Publisher

ELSEVIER
DOI: 10.1016/j.trim.2008.10.007

Keywords

Cell therapy; Chronic kidney disease; Diabetes mellitus; Organogenesis; Stem cell

Funding

  1. JDRF [1-2008-37]
  2. NIDDK [P30 DK079333]

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Lack of donor availability limits the number of human donor organs. The need for host immunosuppression complicates transplantation procedures. It is possible to 'grow' new pancreatic tissue or kidneys in situ via xenotransplantation of organ primordia from animal embryos (organogenesis of the endocrine pancreas or kidney). The developing organ attracts its blood supply from the host, enabling the transplantation of pancreas or kidney in 'cellular' form obviating humoral rejection. In the case of pancreas, selective development of endocrine tissue takes place in post-transplantation. In the case of kidney, an anatomically-correct functional organ differentiates in situ. Glucose intolerance can be corrected in formerly diabetic rats and ameliorated in rhesus macaques on the basis of porcine insulin secreted in a glucose-dependent manner by beta cells originating from transplants. Primordia engraft and function after being stored in vitro prior to implantation. If obtained within a 'window' early during embryonic pancreas development, pig pancreatic primordia engraft in non immune suppressed diabetic rats or rhesus macaques. Engraftment of pig renal primordia transplanted directly into rats requires host immune suppression. However, embryonic rat kidneys into which human mesenchymal cells are incorporated into nephronic elements can be transplanted into non-immune suppressed rat hosts. Here we review recent findings germane to xenotransplantation of pancreatic or renal primordia as a novel organ replacement strategy. (C) 2008 Elsevier B.V. All rights reserved.

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