IN-VIVO CD40-GP39 INTERACTIONS ARE ESSENTIAL FOR THYMUS-DEPENDENT HUMORAL IMMUNITY .2. PROLONGED SUPPRESSION OF THE HUMORAL IMMUNE-RESPONSE BY AN ANTIBODY TO THE LIGAND FOR CD40, GP39

被引：340

作者：

FOY, TM

SHEPHERD, DM

DURIE, FH

ARUFFO, A

LEDBETTER, JA

NOELLE, RJ

机构：

[1] DARTMOUTH COLL SCH MED, DEPT MICROBIOL, 1 MED CTR DR, LEBANON, NH 03756 USA

[2] BRISTOL MYERS SQUIBB PHARMACEUT RES INST, SEATTLE, WA 98121 USA

来源：

JOURNAL OF EXPERIMENTAL MEDICINE | 1993年 / 178卷 / 05期

关键词：

D O I：

10.1084/jem.178.5.1567

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 ligand for CD40 has been recently identified as a 39-kd protein, gp39, expressed on the surface of activated CD4+ T helper cells (Th). In vitro, soluble CD40 and anti-gp39 have been shown to block the ability of Th to activate B cells, suggesting that gp39-CD40 interactions are important to T cell-dependent B cell activation. Here it is shown that in vivo administration of anti-gp39 dramatically reduced both primary and secondary humoral immune responses to erythrocytes and soluble protein antigens without altering responses to the T-independent type 11 antigen, trinitrophenyl-Ficoll. Treatment of mice for 4 d with anti-gp39 inhibited the anti-sheep red blood cell (SRBC) response for at least 3 wk and inhibited the expression of all immunoglobulin isotypes in secondary responses to the protein antigen, keyhole limpet hemocyanin. To examine the direct effect of anti-gp39 on Th function, SRBC-immune Th cells from anti-gp39-treated mice were adoptively transferred and shown to be fully capable of providing help. These results suggest that anti-gp39 treatment does not cause Th deletion or anergy. Anti-gp39 may mediate its profound immunosuppressive effects on humoral immunity by blocking gp39-CD40 interactions. Moreover, these studies establish gp39-CD40 as an important receptor-ligand pair for the targeting of therapeutic antibodies to control thymus-dependent humoral responses.

引用

页码：1567 / 1575

页数：9

共 32 条

[1] CD40 LIGAND GENE DEFECTS RESPONSIBLE FOR X-LINKED HYPER-IGM SYNDROME
ALLEN, RC
ARMITAGE, RJ
CONLEY, ME
ROSENBLATT, H
JENKINS, NA
COPELAND, NG
BEDELL, MA
EDELHOFF, S
DISTECHE, CM
SIMONEAUX, DK
FANSLOW, WC
BELMONT, J
SPRIGGS, MK
[J]. SCIENCE, 1993, 259 (5097) : 990 - 993
[2] IDENTIFICATION OF A SOURCE OF BIOLOGICALLY-ACTIVE CD40 LIGAND
ARMITAGE, RJ
SATO, TA
MACDUFF, BM
CLIFFORD, KN
ALPERT, AR
SMITH, CA
FANSLOW, WC
[J]. EUROPEAN JOURNAL OF IMMUNOLOGY, 1992, 22 (08) : 2071 - 2076
[3] MOLECULAR AND BIOLOGICAL CHARACTERIZATION OF A MURINE LIGAND FOR CD40
ARMITAGE, RJ
FANSLOW, WC
STROCKBINE, L
SATO, TA
CLIFFORD, KN
MACDUFF, BM
ANDERSON, DM
GIMPEL, SD
DAVISSMITH, T
MALISZEWSKI, CR
CLARK, EA
SMITH, CA
GRABSTEIN, KH
COSMAN, D
SPRIGGS, MK
[J]. NATURE, 1992, 357 (6373) : 80 - 82
[4] THE CD40 LIGAND, GP39, IS DEFECTIVE IN ACTIVATED T-CELLS FROM PATIENTS WITH X-LINKED HYPER-IGM SYNDROME
ARUFFO, A
FARRINGTON, M
HOLLENBAUGH, D
LI, X
MILATOVICH, A
NONOYAMA, S
BAJORATH, J
GROSMAIRE, LS
STENKAMP, R
NEUBAUER, M
ROBERTS, RL
NOELLE, RJ
LEDBETTER, JA
FRANCKE, U
OCHS, HD
[J]. CELL, 1993, 72 (02) : 291 - 300
[5] GROWING HUMAN LYMPHOCYTES-B IN THE CD40 SYSTEM
BANCHEREAU, J
ROUSSET, F
[J]. NATURE, 1991, 353 (6345) : 678 - 679
[6] ACTIVATION OF HUMAN B-CELLS MEDIATED THROUGH 2 DISTINCT CELL-SURFACE DIFFERENTIATION ANTIGENS, BP35 AND BP50
CLARK, EA
LEDBETTER, JA
[J]. PROCEEDINGS OF THE NATIONAL ACADEMY OF SCIENCES OF THE UNITED STATES OF AMERICA, 1986, 83 (12) : 4494 - 4498
[7] CD40 LIGAND MUTATIONS IN X-LINKED IMMUNODEFICIENCY WITH HYPER-IGM
DISANTO, JP
BONNEFOY, JY
GAUCHAT, JF
FISCHER, A
DESAINTBASILE, G
[J]. NATURE, 1993, 361 (6412) : 541 - 543
[8] SYNERGISTIC INTERACTION BETWEEN INTERLEUKIN-4 AND ANTI-BP50 (CDW40) REVEALED IN A NOVEL B-CELL RESTIMULATION ASSAY
GORDON, J
MILLSUM, MJ
GUY, GR
LEDBETTER, JA
[J]. EUROPEAN JOURNAL OF IMMUNOLOGY, 1987, 17 (10) : 1535 - 1538
[9] GORDON J, 1989, IMMUNOLOGY, V68, P526
[10] HELLSTROM I, 1986, CANCER RES, V46, P3917

← 1 2 3 4 →