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Titlebook: Current Trends in Histocompatibility; Volume 1 Immunogenet Ralph A. Reisfeld,Soldano Ferrone Book 1981 Springer Science+Business Media New

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s, we have made an effort to bring together the most current work on topics that have generated most of the re cent advances and discussions. We have asked each author to present and interpret his most current work, and we have judiciously refrained from imposing our own prejudices and viewpoints. A
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https://doi.org/10.1007/978-3-658-25823-8r histocompatibility system of the mouse, the . system, adjoins closely the . genetic complex in chromosome 17. The . complex occupies a region of the chromosome 20 times longer than that pertaining to the . system, and controls a variety of vital functions necessary for the development of the organism and survival of the species.
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https://doi.org/10.1007/978-3-658-25823-8es to the multiple functions associated (in physiology and pathology) with the MHS is still unclear. It is characteristic of the MHS that an extensive series of alleles (a high degree of polymorphism) occurs at the individual gene loci.
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https://doi.org/10.1007/978-3-658-25823-8tribution, and clinical importance of the .-region antigens are discussed (see also Thorsby ., 1978). The HLA-D determinants are recognized by cellular techniques, while the HLA-D-related (DR) antigens are detected by serological methods. The relationship between the HLA-D determinants and HLA-DR antigens is also discussed.
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ontents I. Serology and Genetics Chapter 1 Studies of HLA-DR Antigens by Complement Fixation Jacques M. Colombani, Laurent Degos, Virginia Lepage, Helene Dastot, Muriel Reboul, and Pierre Lethielleux 1. Introduction. . . . . . . . . . . . . . . . . . . . . . . . . . . . . . . . . . . . . . . . . . . . . . . .978-1-4684-3760-7978-1-4684-3758-4
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Serological and Cellular Recognition of Human Histocompatibility Antigensmolecular weights of 35,000 and 27,000 (Cress-well and Geier, 1975; Springer ., 1977). Which of these molecules is the true product of the . gene is not absolutely certain; conflicting evidence suggests that both the isolated 27,000-dalton and the 35,000-dalton molecule can bind alloantibodies to HL
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