IMMUNOGLOBULIN-E-BINDING SITE IN FC-EPSILON RECEPTOR (FC-EPSILON-RII CD23) IDENTIFIED BY HOMOLOG-SCANNING MUTAGENESIS

被引：0

作者：

BETTLER, B

TEXIDO, G

RAGGINI, S

RUEGG, D

HOFSTETTER, H

机构：

[1] SALK INST BIOL STUDIES, MOLEC NEUROBIOL LAB, SAN DIEGO, CA 92186 USA

[2] CIBA GEIGY LTD, TAKARAZUKA 665, JAPAN

来源：

JOURNAL OF BIOLOGICAL CHEMISTRY | 1992年 / 267卷 / 01期

关键词：

D O I：

暂无

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：

The IgE-binding site of the human low-affinity receptor for IgE (Fc(epsilon)RII/CD23) has previously been mapped to the extracellular domain between amino acid residues 160 and 287. We now have investigated which conformational epitope within this domain specifies the receptor-ligand interaction. The analysis of homolog-scanning mutants expressed in mammalian cells demonstrates that amino acid side chains that affect IgE binding are located in two discontinuous segments, between residues 165-190 and 224-256. The overall structure of the chimeric binding domains, as probed with 11 conformation-sensitive monoclonal antibodies, is generally not distorted, except by replacement of residues 165-183. In this region, disruption of binding function appears to be caused by global conformational constraints on the binding site. Substitution and deletion mutants demonstrate that six out of eight extracellular cysteines, Cys163, Cys174, Cys191, cys259, Cys273, and Cys282, are necessary for IgE binding and are most likely involved in intramolecular disulfide bridges. We show that the Fc(epsilon)RII domain delineated by Cys163 and Cys282 encodes all the structural information required to form the IgE-binding site.

引用

页码：185 / 191

页数：7

共 50 条

[1] FC-EPSILON-RII/CD23 - THE LOW AFFINITY RECEPTOR FOR IGE
CONRAD, DH
ANNUAL REVIEW OF IMMUNOLOGY, 1990, 8 : 623 - 645
[2] MODELING OF THE LECTIN-HOMOLOGY DOMAINS OF THE HUMAN AND MURINE LOW-AFFINITY FC-EPSILON RECEPTOR (FC-EPSILON-RII/CD23)
PADLAN, EA
HELM, BA
RECEPTOR, 1993, 3 (04) : 325 - 341
[3] MOLECULAR MECHANISMS OF MURINE FC-EPSILON-RII/CD23 REGULATION
DIERKS, SE
CAMPBELL, KA
STUDER, EJ
CONRAD, DH
MOLECULAR IMMUNOLOGY, 1994, 31 (15) : 1181 - 1189
[4] BIOLOGY AND CHEMISTRY OF THE LOW AFFINITY IGE RECEPTOR (FC-EPSILON-RII CD23)
RICHARDS, ML
KATZ, DH
CRITICAL REVIEWS IN IMMUNOLOGY, 1991, 11 (02) : 65 - 86
[5] CHROMOSOMAL LOCATION AND ISOFORM ANALYSIS OF MOUSE FC-EPSILON-RII/CD23
CONRAD, DH
KOZAK, CA
VERNACHIO, J
SQUIRE, CM
RAO, M
EICHER, EM
MOLECULAR IMMUNOLOGY, 1993, 30 (01) : 27 - 33
[6] EXPRESSION, REGULATION AND FUNCTION OF HUMAN FC-EPSILON-RII (CD23) ANTIGEN
SARFATI, M
FOURNIER, S
WU, CY
DELESPESSE, G
IMMUNOLOGIC RESEARCH, 1992, 11 (3-4) : 260 - 272
[7] THE OLIGOMERIC NATURE OF THE MURINE FC-EPSILON-RII/CD23 - IMPLICATIONS FOR FUNCTION
DIERKS, SE
BARTLETT, WC
EDMEADES, RL
GOULD, HJ
RAO, M
CONRAD, DH
JOURNAL OF IMMUNOLOGY, 1993, 150 (06): : 2372 - 2382
[8] STRUCTURE AND FUNCTION OF FC-EPSILON RECEPTOR-II (FC-EPSILON-RII CD23) - A POINT OF CONTACT BETWEEN THE EFFECTOR PHASE OF ALLERGY AND B-CELL DIFFERENTIATION
KIKUTANI, H
YOKOTA, A
UCHIBAYASHI, N
YUKAWA, K
TANAKA, T
SUGIYAMA, K
BARSUMIAN, EL
SUEMURA, M
KISHIMOTO, T
IGE, MAST CELLS AND THE ALLERGIC RESPONSE, 1989, 147 : 23 - 35
[9] RECOMBINANT SOLUBLE FC-EPSILON RECEPTOR-II (FC-EPSILON-RII/CD23) HAS IGE BINDING-ACTIVITY BUT NO B-CELL GROWTH-PROMOTING ACTIVITY
UCHIBAYASHI, N
KIKUTANI, H
BARSUMIAN, EL
HAUPTMANN, R
SCHNEIDER, FJ
SCHWENDENWEIN, R
SOMMERGRUBER, W
SPEVAK, W
MAURERFOGY, I
SUEMURA, M
KISHIMOTO, T
JOURNAL OF IMMUNOLOGY, 1989, 142 (11): : 3901 - 3908
[10] STRUCTURE AND FUNCTION OF FC-EPSILON RECEPTOR-II (FC-EPSILON-RII CD23) - A POINT OF CONTACT BETWEEN THE EFFECTOR PHASE OF ALLERGY AND B-CELL DIFFERENTIATION
KIKUTANI, H
YOKOTA, A
UCHIBAYASHI, N
YUKAWA, K
TANAKA, T
SUGIYAMA, K
BARSUMIAN, EL
SUEMURA, M
KISHIMOTO, T
CIBA FOUNDATION SYMPOSIA, 1989, 147 : 23 - 35

← 1 2 3 4 5 →