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First published online November 1, 2007
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2006-0262v1
26/2/381    most recent
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Submitted on April 28, 2006
Accepted on October 19, 2007

EMBRYONIC STEM CELLS

Hematopoietic Mixed Chimerism Derived From Allogeneic Embryonic Stem Cells Prevents Autoimmune Diabetes Mellitus In Nod Mice

Larissa Verda 1, Duck An Kim 1, Susumu Ikehara 2, Laisvyde Statkute 1, Delphine Bronesky 1, Yevgeniya Petrenko 1, Yu Oyama 1, Xiang He 3, Charles Link 4, Nicholas N. Vahanian 4, Richard K. Burt 1*

1 Division of Immunotherapy, Department of Medicine, Northwestern University Feinberg School of Medicine, Chicago, IL 60611
2 First Department of Pathology, Transplantation Center, Kansai Medical University, Osaka, Japan
3 Pathology Core Facility, Northwestern University Cancer Center, Chicago, IL 60611
4 NewLink Genetics Corporation, Iowa State University Research Park, Ames, IA 50010

* To whom correspondence should be addressed. E-mail: rburt{at}northwestern.edu.


  Abstract

Embryonic stem cell (ESC)-derived hematopoietic stem cells (HSC), unlike HSC harvested from the blood or marrow, are not contaminated by lymphocytes. We therefore evaluated whether ESC-derived HSC could produce islet cell tolerance, a phenomenon termed graft versus autoimmune (GVA) without causing the usual allogeneic hematopoietic stem cell transplant (HSCT) complication - graft versus host disease (GVHD). Herein, we demonstrate that ESC-derived HSC may be used to prevent autoimmune diabetes mellitus in NOD mice without GVHD or other adverse side effects. ESC were cultured in vitro to induce differentiation toward HSC, selected for c-kit expression, and injected either intravenous (IV) or intra bone marrow (IBM) into sublethally irradiated NOD/LtJ mice. Nine out of 10 mice from the IBM group and 5 out of 8 from the IV group did not become hyperglycemic, in contrast to the control group, in which 8 of 9 mice developed end-stage diabetes. All mice with > 5% donor chimerism remained free of diabetes and insulitis that was confirmed by histology. Splenocytes from transplanted mice were unresponsive to GAD65, a diabetic specific auto-antigen, but responded normally to 3rd party antigens. ESC-derived HSC can induce an islet cell tolerizing GVA effect without GVHD. This study represents the first instance, in our knowledge, of ESC-derived HSC cells treating disease in an animal model.

Key Words. embryonic stem cells, diabetes mellitus, immune tolerance, hematopoiesis




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R. K. Burt, Y. Loh, W. Pearce, N. Beohar, W. G. Barr, R. Craig, Y. Wen, J. A. Rapp, and J. Kessler
Clinical Applications of Blood-Derived and Marrow-Derived Stem Cells for Nonmalignant Diseases
JAMA, February 27, 2008; 299(8): 925 - 936.
[Abstract] [Full Text] [PDF]


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