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A Novel Mutant Gene Involved in T-Lymphocyte-Specific Homing Into Peripheral Lymphoid Organs on Mouse Chromosome 4 

Hideki Nakano, Shigeyuki Mori, Hiromichi Yonekawa, Hideo Nariuchi, Akio Matsuzawa, and Terutaka Kakiuchi

From the Department of Immunology, Toho University School of Medicine, Tokyo, Japan; the Laboratory Animal Research Center and Department of Allergology, Institute of Medical Science, University of Tokyo, Tokyo, Japan; and the Department of Laboratory Animal Science, The Tokyo Metropolitan Institute of Medical Science, Tokyo, Japan.

Previously, we have shown a mutant mouse DDD/1 with T-cell-specific homing defect that is regulated by an autosomal recessive gene, plt (paucity of lymph node T cells), and seems to be caused by lymph node (LN) stromal cells. In the present study, immunohistochemical analysis showed unusual distribution of T cells in LN, Peyer's patches (PP), and spleen from plt/plt, probably due to the failure of T cells to migrate from blood into the T-cell zone in LN or PP, or into the spleen white pulp across high endothelial venule or marginal zone, respectively, based on the experiments in which labelled T cells were injected intravenously and detected in the tissues. Analysis of surface L-selectin and CD44 suggested that T cells with memory phenotype, probably from afferent lymphatics, recruit into plt/plt LN. Linkage mapping by simple-sequence length polymorphism of genomic DNA from 190 backcross progenies produced by intercrossing with MSM/Ms, linked plt most closely with D4Mit237, and localized at 24.7 cM from cetromere on chromosome 4. We discuss the possibility that a wild-type gene on plt locus encodes a chemokine inducing T-cell-specific homing into peripheral lymphoid tissues.

Blood, Vol. 91 No. 8 (April 15), 1998: pp. 2886-2895
© 1998 by The American Society of Hematology.


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