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Variations in the cytoplasmic region account for the heterogeneity of the chicken MHC class I (B-F) molecules
Authors:Lisbeth B Møller  Jim Kaufman  Sten Verland  Jan Salomonsen  David Avila  John D Lambris  Karsten Skjødt
Affiliation:(1) Institute for Experimental Immunology, University of Copenhagen, Nørre Alle 71, DK-2100 Copenhagen Ø, Denmark;(2) Basel Institute for Immunology, Grenzacherstrabetae 487, CH-4058 Basel, Switzerland;(3) Present address: Institute for Microbiology, University of Copenhagen, DK-1535 Copenhagen K, Denmark;(4) Department of Medical Microbiology, J. B. Winsløws Vej 19, DK-5000 Odense C, Denmark
Abstract:Molecular variation among major histocompatibility complex (MHC) class I (B-F) proteins from B-homozygous chickens is apparently caused by C-terminal variation. Analysis of the total B-F protein pool revealed substantial heterogeneity with two or three molecular mass constituents, each being comprised by several isoelectric focusing variants. This heterogeneity could not be reduced by enzymatic deglycosylation. By contrast, proteolytic removal of a small (M r 1000–4000) fragment from the agr chain resulted in the generation of a M r 36 000 fragment, common to all the molecular mass variants. Unlike the parent proteins, the M r 36 000 fragment derived from isolated variants yielded identical, simple patterns in two-dimensional gel electrophoresis and identical finger prints in peptide mapping. This, together with N-terminal amino acid sequencing, as well as comparison of hydrophobicity properties of fragments obtained by gradual proteolytic digestion, indicated that the small peptide responsible for the major B-F heterogeneity was situated in the intracellular, C-terminal part.
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