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Science 14 February 1986:
Vol. 231. no. 4739, pp. 733 - 735
DOI: 10.1126/science.3003909
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Articles

Science, Vol 231, Issue 4739, 733-735
Copyright © 1986 by American Association for the Advancement of Science

articles

The NOD mouse: recessive diabetogenic gene in the major histocompatibility complex

M Hattori, JB Buse, RA Jackson, L Glimcher, ME Dorf, M Minami, S Makino, K Moriwaki, H Kuzuya, H Imura, and al. et

Examination of the histocompatibility region of the nonobese diabetic (NOD) mouse with antibodies against class II glycoproteins (products of immune response genes of the major histocompatibility complex I-A and I-E), hybrid T-cell clones, and mixed-lymphocyte cultures and analysis of restriction fragment length polymorphisms indicate that the NOD mouse has a unique class II major histocompatibility complex with no expression of surface I-E, no messenger RNA for I-E alpha, and an I-A not recognized by any monoclonal antibodies or hybrid T-cell clones studied. In crosses of NOD mice with control C3H mice, the development of diabetes was dependent on homozygosity for the NOD mouse's unique major histocompatibility region.


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Evidence for the Presence of Insulin-Dependent Diabetes-Associated Alleles on the Distal Part of Mouse Chromosome 6.
E. Melanitou, F. Joly, M. Lathrop, C. Boitard, and P. Avner (1998)
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   Abstract »    Full Text »
Autoreactivity of T cells from nonobese diabetic mice: An I-Ag7-dependent reaction.
O. Kanagawa, S. M. Martin, B. A. Vaupel, E. Carrasco-Marin, and E. R. Unanue (1998)
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   Abstract »    Full Text »    PDF »
Major Histocompatibility Complex Class II Molecules Can Protect from Diabetes by Positively Selecting T Cells with Additional Specificities.
F. Luhder, J. Katz, C. Benoist, and D. Mathis (1998)
J. Exp. Med. 187, 379-387
   Abstract »    Full Text »    PDF »
A Mechanism for the Major Histocompatibility Complex-linked Resistance to Autoimmunity.
D. Schmidt, J. Verdaguer, N. Averill, and P. Santamaria (1997)
J. Exp. Med. 186, 1059-1075
   Abstract »    Full Text »    PDF »
Requirement of Fas for the Development of Autoimmune Diabetes in Nonobese Diabetic Mice.
N. Itoh, A. Imagawa, T. Hanafusa, M. Waguri, K. Yamamoto, H. Iwahashi, M. Moriwaki, H. Nakajima, J. Miyagawa, M. Namba, et al. (1997)
J. Exp. Med. 186, 613-618
   Abstract »    Full Text »    PDF »
Abnormal T cell selection on nod thymic epithelium is sufficient to induce autoimmune manifestations in C57BL/6 athymic nude mice.
V. Thomas-Vaslin, D. Damotte, M. Coltey, N. M. Le Douarin, A. Coutinho, and J. Salaun (1997)
PNAS 94, 4598-4603
   Abstract »    Full Text »    PDF »
Prevention of Type I Diabetes and Recurrent {beta}-Cell Destruction of Transplanted Islets.
R. H. Slover and G. S. Eisenbarth (1997)
Endocr. Rev. 18, 241-258
   Abstract »    Full Text »
T cell receptor restriction of diabetogenic autoimmune NOD T cells.
E. Simone, D. Daniel, N. Schloot, P. Gottlieb, S. Babu, E. Kawasaki, D. Wegmann, and G. S. Eisenbarth (1997)
PNAS 94, 2518-2521
   Abstract »    Full Text »    PDF »
T helper cell subsets in insulin-dependent diabetes.
J. Katz, C Benoist, and D Mathis (1995)
Science 268, 1185-1188
   Abstract »    PDF »
Linkage on chromosome 3 of autoimmune diabetes and defective Fc receptor for IgG in NOD mice.
J. Prins, J. Todd, N. Rodrigues, S Ghosh, P. Hogarth, L. Wicker, E Gaffney, P. Podolin, P. Fischer, A Sirotina, et al. (1993)
Science 260, 695-698
   Abstract »    PDF »
Linkage of faulty major histocompatibility complex class I to autoimmune diabetes.
D Faustman, X. Li, H. Lin, Y. Fu, G Eisenbarth, J Avruch, and J Guo (1991)
Science 254, 1756-1761
   Abstract »    PDF »
MHC-linked protection from diabetes dissociated from clonal deletion of T cells.
J Bohme, B Schuhbaur, O Kanagawa, C Benoist, and D Mathis (1990)
Science 249, 293-295
   Abstract »    PDF »
A molecular basis for MHC class II--associated autoimmunity.
J. Todd, H Acha-Orbea, J. Bell, N Chao, Z Fronek, C. Jacob, M McDermott, A. Sinha, L Timmerman, L Steinman, et al. (1988)
Science 240, 1003-1009
   Abstract »    PDF »
Immunotherapy of the nonobese diabetic mouse: treatment with an antibody to T-helper lymphocytes.
J. Shizuru, C Taylor-Edwards, B. Banks, A. Gregory, and C. Fathman (1988)
Science 240, 659-662
   Abstract »    PDF »
Three recessive loci required for insulin-dependent diabetes in nonobese diabetic mice.
M Prochazka, E. Leiter, D. Serreze, and D. Coleman (1987)
Science 237, 286-289
   Abstract »    PDF »


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