EXPRESSION CLONING OF AN EQUINE T-LYMPHOCYTE GLYCOPROTEIN CD2 CDNA STRUCTURE-BASED ANALYSIS OF CONSERVED SEQUENCE ELEMENTS

被引：22

作者：

TAVERNOR, AS

KYDD, JH

BODIAN, DL

JONES, EY

STUART, DI

DAVIS, SJ

BUTCHER, GW

机构：

[1] AFRC,BABRAHAM INST,DEPT IMMUNOL,CAMBRIDGE CB2 4AT,CAMBS,ENGLAND

[2] ANIM HLTH TRUST,DEPT INFECT DIS,NEWMARKET,SUFFOLK,ENGLAND

[3] LAB MOLEC BIOPHYS,OXFORD,ENGLAND

[4] UNIV OXFORD,OXFORD CTR MOLEC SCI,OXFORD,ENGLAND

[5] UNIV OXFORD,SIR WILLIAM DUNN SCH PATHOL,MRC,CELLULAR IMMUNOL UNIT,OXFORD OX1 3RE,ENGLAND

来源：

EUROPEAN JOURNAL OF BIOCHEMISTRY | 1994年 / 219卷 / 03期

关键词：

D O I：

10.1111/j.1432-1033.1994.tb18579.x

中图分类号：

Q5 [生物化学]; Q7 [分子生物学];

学科分类号：

071010 ; 081704 ;

摘要：

An equine CD2 cDNA has been isolated by monoclonal antibody screening of a T-lymphocyte cDNA library. The cDNA contained an open reading frame of 1041 bp encoding a translated product of 347 amino acids. Northern blotting analysis revealed a single mRNA species expressed in spleen, thymus and activated peripheral lymphocytes. The predicted amino acid sequence has 50-65% identity with the human, rat and mouse CD2 sequences with greatest similarity shared with the human homologue. Evolutionarily conserved structural and functional domains in CD2 were identified by comparing the sequences of the equine, human, mouse and rat CD2 homologues in the context of the recently derived crystal structure of rat soluble CD2 [Jones, E. Y., Davis, S. J., Williams, A, E, Harlos, K. and Stuart, D. I. (1992) Nature 360, 232-239]. The key conserved features of the extracellular region included core residues necessary to preserve the structural integrity of the molecule, residues in the linker region likely to maintain the unique domain organization of CD2, an array of highly charged residues in the putative ligand-binding face of the molecule and glycosylation-signal distributions that render the putative ligand-binding GFCC'C'' face of domain 1 relatively unhindered by glycosylation.

引用

页码：969 / 976

页数：8

共 49 条

[1] INTERDEPENDENCE OF CD3-TI AND CD2 ACTIVATION PATHWAYS IN HUMAN LYMPHOCYTES-T
ALCOVER, A
ALBERINI, C
ACUTO, O
CLAYTON, LK
TRANSY, C
SPAGNOLI, GC
MOINGEON, P
LOPEZ, P
REINHERZ, EL
[J]. EMBO JOURNAL, 1988, 7 (07) : 1973 - 1977
[2] A SOLUBLE MULTIMERIC RECOMBINANT CD2 PROTEIN IDENTIFIES CD48 AS A LOW AFFINITY LIGAND FOR HUMAN CD2 - DIVERGENCE OF CD2 LIGANDS DURING THE EVOLUTION OF HUMANS AND MICE
ARULANANDAM, ARN
MOINGEON, P
CONCINO, MF
RECNY, MA
KATO, K
YAGITA, H
KOYASU, S
REINHERZ, EL
[J]. JOURNAL OF EXPERIMENTAL MEDICINE, 1993, 177 (05) : 1439 - 1450
[3] ALSCRIPT - A TOOL TO FORMAT MULTIPLE SEQUENCE ALIGNMENTS
BARTON, GJ
[J]. PROTEIN ENGINEERING, 1993, 6 (01): : 37 - 40
[4] ACTIVATION OF LYMPHOCYTES-T VIA MONOCLONAL-ANTIBODIES AGAINST RAT-CELL SURFACE-ANTIGENS WITH PARTICULAR REFERENCE TO CD2 ANTIGEN
BEYERS, AD
BARCLAY, AN
LAW, DA
HE, Q
WILLIAMS, AF
[J]. IMMUNOLOGICAL REVIEWS, 1989, 111 : 59 - 77
[5] BIERER BE, 1990, J IMMUNOL, V144, P785
[6] CRYSTALLOGRAPHIC R-FACTOR REFINEMENT BY MOLECULAR-DYNAMICS
BRUNGER, AT
KURIYAN, J
KARPLUS, M
[J]. SCIENCE, 1987, 235 (4787) : 458 - 460
[7] INVOLVEMENT OF THE PPPGHR MOTIF IN T-CELL ACTIVATION VIA CD2
CHANG, HC
MOINGEON, P
PEDERSEN, R
LUCICH, J
STEBBINS, C
REINHERZ, EL
[J]. JOURNAL OF EXPERIMENTAL MEDICINE, 1990, 172 (01) : 351 - 355
[8] ISOLATION OF BIOLOGICALLY-ACTIVE RIBONUCLEIC-ACID FROM SOURCES ENRICHED IN RIBONUCLEASE
CHIRGWIN, JM
PRZYBYLA, AE
MACDONALD, RJ
RUTTER, WJ
[J]. BIOCHEMISTRY, 1979, 18 (24) : 5294 - 5299
[9] NATURE OF ACCESSIBLE AND BURIED SURFACES IN PROTEINS
CHOTHIA, C
[J]. JOURNAL OF MOLECULAR BIOLOGY, 1976, 105 (01) : 1 - 14
[10] ACTIVATION OF RAT LYMPHOCYTES-T BY ANTI-CD2 MONOCLONAL-ANTIBODIES
CLARK, SJ
LAW, DA
PATERSON, DJ
PUKLAVEC, M
WILLIAMS, AF
[J]. JOURNAL OF EXPERIMENTAL MEDICINE, 1988, 167 (06) : 1861 - 1872

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