SELECTION AGAINST N-REGION DIVERSITY IN IMMUNOGLOBULIN HEAVY-CHAIN VARIABLE REGIONS DURING THE DEVELOPMENT OF PREIMMUNE B-CELL REPERTOIRES

被引:33
作者
CARLSSON, L [1 ]
OVERMO, C [1 ]
HOLMBERG, D [1 ]
机构
[1] UMEA UNIV,APPL CELL & MOLEC BIOL UNIT,S-90187 UMEA,SWEDEN
来源
INTERNATIONAL IMMUNOLOGY | 1992年 / 4卷 / 05期
关键词
IMMUNOGLOBULIN REARRANGEMENTS; N-SEQUENCES; PRIMARY B-CELL REPERTOIRES;
D O I
10.1093/intimm/4.5.549
中图分类号
R392 [医学免疫学]; Q939.91 [免疫学];
学科分类号
100102 ;
摘要
The generation of Ig heavy chain chain diversity is dependent on the ordered rearrangement of three different, i.e. variable (V(H)), diversity (D(H)), and joining (J(H)), germline gene segments, exonuclease nibbling of the terminals of these gene segments, and the addition of template-independent nucleotide (N-sequences) in the junctions of these segments. The latter process has recently been reported to be limited within B cells formed during early ontogeny. In this study, we have analysed a large number of V(H)DJ(H) rearrangements isolated from genomic DNA of adult and neonatal C57Bl/6 mice using the polymerase chain reaction (PCR) technique. A comparison of functional versus non-functional V(H)DJ(H) rearrangements derived from these PCR libraries, or from a set of previously published clones of BALB/c origin, revealed a selection against N-region diversity both in neonatal and adult B cell repertoires. This selection process is most pronounced in the early development of the immune system but can still be observed in the adult. Furthermore, selection against N-sequence additions was evident amongst neonatal V(H)DJ(H) rearrangements utilizing both V(H) 7183 and V(H) J558 genes, but only in V(H) 7183 utilizing clones of adult origin. These results imply that in addition to a developmentally controlled onset of N-sequence additions, cellular selection against N-region diversity exist both in the neonatal and adult immune system.
引用
收藏
页码:549 / 553
页数:5
相关论文
共 28 条
[11]   VH-GENES ENCODING THE IMMUNE-RESPONSE TO BETA-(1,6)-GALACTAN - SOMATIC MUTATION IN IGM MOLECULES [J].
HARTMAN, AB ;
RUDIKOFF, S .
EMBO JOURNAL, 1984, 3 (12) :3023-3030
[12]   ESTABLISHMENT AND FUNCTIONAL IMPLICATIONS OF B-CELL CONNECTIVITY [J].
HOLMBERG, D ;
ANDERSSON, A ;
CARLSSON, L ;
FORSGREN, S .
IMMUNOLOGICAL REVIEWS, 1989, 110 :89-103
[13]   HIGH CONNECTIVITY, NATURAL ANTIBODIES PREFERENTIALLY USE 7183 AND QUPC52 VH FAMILIES [J].
HOLMBERG, D .
EUROPEAN JOURNAL OF IMMUNOLOGY, 1987, 17 (03) :399-403
[14]   COMPARISON OF THE FETAL AND ADULT FUNCTIONAL B-CELL REPERTOIRES BY ANALYSIS OF VH GENE FAMILY EXPRESSION [J].
JEONG, HD ;
TEALE, JM .
JOURNAL OF EXPERIMENTAL MEDICINE, 1988, 168 (02) :589-603
[15]   JUNCTIONAL SEQUENCES OF T-CELL RECEPTOR GAMMA-DELTA-GENES - IMPLICATIONS FOR GAMMA-DELTA-T-CELL LINEAGES AND FOR A NOVEL INTERMEDIATE OF V-(D)-J JOINING [J].
LAFAILLE, JJ ;
DECLOUX, A ;
BONNEVILLE, M ;
TAKAGAKI, Y ;
TONEGAWA, S .
CELL, 1989, 59 (05) :859-870
[16]   ADULT B-CELL REPERTOIRE IS BIASED TOWARD 2 HEAVY-CHAIN VARIABLE-REGION GENES THAT REARRANGE FREQUENTLY IN FETAL PRE-B CELLS [J].
LAWLER, AM ;
LIN, PS ;
GEARHART, PJ .
PROCEEDINGS OF THE NATIONAL ACADEMY OF SCIENCES OF THE UNITED STATES OF AMERICA, 1987, 84 (08) :2454-2458
[17]   BIASED EXPRESSION OF JH-PROXIMAL VH-GENES OCCURS IN THE NEWLY GENERATED REPERTOIRE OF NEONATAL AND ADULT MICE [J].
MALYNN, BA ;
YANCOPOULOS, GD ;
BARTH, JE ;
BONA, CA ;
ALT, FW .
JOURNAL OF EXPERIMENTAL MEDICINE, 1990, 171 (03) :843-859
[18]  
Maniatis T., 1982, MOL CLONING
[19]   ANALYSIS OF JUNCTIONAL DIVERSITY DURING LYMPHOCYTE-B DEVELOPMENT [J].
MEEK, K .
SCIENCE, 1990, 250 (4982) :820-823
[20]   STRUCTURAL RELATIONSHIPS AMONG MOUSE AND HUMAN-IMMUNOGLOBULIN VH-GENES IN THE SUBGROUP-III [J].
OLLO, R ;
SIKORAV, JL ;
ROUGEON, F .
NUCLEIC ACIDS RESEARCH, 1983, 11 (22) :7887-7897
123