IMMUNOGLOBULIN LIGHT CHAIN VARIABLE REGION GENE-SEQUENCES FOR HUMAN-ANTIBODIES TO HAEMOPHILUS-INFLUENZAE TYPE-B CAPSULAR POLYSACCHARIDE ARE DOMINATED BY A LIMITED NUMBER OF V-KAPPA AND V-LAMBDA SEGMENTS AND VJ COMBINATIONS

被引：66

作者：

ADDERSON, EE

SHACKELFORD, PG

INSEL, RA

QUINN, A

WILSON, PM

CARROLL, WL

机构：

[1] WASHINGTON UNIV,ST LOUIS CHILDRENS HOSP,SCH MED,DIV INFECT DIS,ST LOUIS,MO 63110

[2] WASHINGTON UNIV,ST LOUIS CHILDRENS HOSP,SCH MED,MALLINCKRODT DEPT PEDIAT,ST LOUIS,MO 63110

[3] UNIV ROCHESTER,SCH MED & DENT,DEPT PEDIAT,ROCHESTER,NY 14642

来源：

JOURNAL OF CLINICAL INVESTIGATION | 1992年 / 89卷 / 03期

关键词：

B-CELL REPERTOIRE; SOMATIC MUTATION; GENE REARRANGEMENT; CARBOHYDRATE ANTIGEN;

D O I：

10.1172/JCI115649

中图分类号：

R-3 [医学研究方法]; R3 [基础医学];

学科分类号：

1001 ;

摘要：

The immune repertoire to Haemophilus influenzae type b capsular polysaccharide (Hib PS) appears to be dominated by certain light chain variable region genes (IgV(L)). In order to examine the molecular basis underlying light chain bias, IgV(L) genes have been cloned from a panel of heterohybridomas secreting human anti-Hib PS (antibody) (anti-Hib PS Ab). One hybridoma, representative of the predominant serum clonotype of anti-Hib PS Ab in older children and adults following immunization or Hib infection, uses a V(kappa)II segment identical to the germline gene A2, and a JK3 segment. A second kappa hybridoma uses a member of the V(kappa)I family and a JK4 segment. Four lambda antibodies, all cross-reactive with the structurally related antigen Escherichia coli K100 PS, use V(lambda)VII segments which are 96-98% homologous to one another, and may originate from a single germline gene. Two additional lambda antibodies, not K100-cross-reactive, are encoded by members of the V(lambda)II family. All lambda antibodies use highly homologous J(lambda)2 or J(lambda)3 segments. The VJ joints of all lambda antibodies and the V(kappa)II-encoded antibody are notable for the presence of an arginine codon, suggesting an important role in antigen binding. Although more complex than heavy chain variable region gene usage, a significant portion of serum anti-Hib PS Ab is likely to be encoded by a limited number of V(kappa) and V(lambda) segments and VJ combinations, which may be selectively expressed during development, or following antigen exposure.

引用

页码：729 / 738

页数：10

共 54 条

[1] ADDERSON EE, 1991, J IMMUNOL, V147, P1667
[2] 2 PAIRS OF RECOMBINATION SIGNALS ARE SUFFICIENT TO CAUSE IMMUNOGLOBULIN-V-(D)-J JOINING
AKIRA, S
OKAZAKI, K
SAKANO, H
[J]. SCIENCE, 1987, 238 (4830) : 1134 - 1138
[3] DEVELOPMENT OF THE PRIMARY ANTIBODY REPERTOIRE
ALT, FW
BLACKWELL, TK
YANCOPOULOS, GD
[J]. SCIENCE, 1987, 238 (4830) : 1079 - 1087
[4] KAPPA-LIGHT CHAIN AND LAMBDA-LIGHT CHAIN COMPOSITION OF ANTIBODY TO THE CAPSULAR POLYSACCHARIDE OF HAEMOPHILUS-INFUENZAE TYPE-B
AMBROSINO, DM
GREIF, W
THOMPSON, C
SIBER, GR
[J]. JOURNAL OF INFECTIOUS DISEASES, 1990, 161 (05) : 922 - 925
[5] THE ISOLATION OF A HUMAN IG V-LAMBDA GENE FROM A RECOMBINANT LIBRARY OF CHROMOSOME 22 AND ESTIMATION OF ITS COPY NUMBER
ANDERSON, MLM
SZAJNERT, MF
KAPLAN, JC
MCCOLL, L
YOUNG, BD
[J]. NUCLEIC ACIDS RESEARCH, 1984, 12 (17) : 6647 - 6661
[6] CONTENT AND ORGANIZATION OF THE HUMAN IG VH LOCUS - DEFINITION OF 3 NEW VH FAMILIES AND LINKAGE TO THE IG CH LOCUS
BERMAN, JE
MELLIS, SJ
POLLOCK, R
SMITH, CL
SUH, H
HEINKE, B
KOWAL, C
SURTI, U
CHESS, L
CANTOR, CR
ALT, FW
[J]. EMBO JOURNAL, 1988, 7 (03) : 727 - 738
[7] BROCKLEY F, 1989, NUCLEIC ACIDS RES, V10, P3976
[8] ALTERNATIVE V-KAPPA GENE REARRANGEMENTS IN A MURINE B-CELL LYMPHOMA - AN EXPLANATION FOR IDIOTYPIC HETEROGENEITY
CARROLL, WL
STARNES, CO
LEVY, R
LEVY, S
[J]. JOURNAL OF EXPERIMENTAL MEDICINE, 1988, 168 (05) : 1607 - 1620
[9] A 16/6 IDIOTYPE POSITIVE ANTI-DNA ANTIBODY IS ENCODED BY A CONSERVED VH GENE WITH NO SOMATIC MUTATION
CHEN, PP
LIU, MF
SINHA, SM
CARSON, DA
[J]. ARTHRITIS AND RHEUMATISM, 1988, 31 (11): : 1429 - 1431
[10] 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

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