学术探索
学术期刊
新闻热点
数据分析
智能评审

DIRECT PHYSICAL INTERACTION INVOLVING CD40 LIGAND ON T-CELLS AND CD40 ON B-CELLS IS REQUIRED TO PROPAGATE MMTV

被引:43
作者
CHERVONSKY, AV [1 ]
XU, JC [1 ]
BARLOW, AK [1 ]
KHERY, M [1 ]
FLAVELL, RA [1 ]
JANEWAY, CA [1 ]
机构
[1] BOEHRINGER INGELHEIM PHARMACEUT INC,RIDGEFIELD,CT 06877
来源
IMMUNITY | 1995年 / 3卷 / 01期
关键词
D O I
10.1016/1074-7613(95)90166-3
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 propagation of mouse mammary tumor virus (MMTV) has been analyzed in mice defective for expression of CD40 ligand (CD40L). Mice with endogenous viral superantigen (SAG) delete T cells with cognate Vp independent of CD40L expression. Nevertheless, CD40L(-) mice do not show deletion of cognate T cells after being exposed to infectious MMTV and have greatly diminished viral replication. The response of CD40L(-) T cells to SAG in vitro is also impaired, but can be reconstituted by adding B cells activated by recombinant CD40L to express costimulatory molecules. Thus, direct CD40L-dependent B cell activation appears to be a critical step in the life cycle of MMTV. The initial step in SAG-dependent T cell activation, and hence the MMTV life cycle, may be mediated by non-B cells, because splenocytes from B cell-deficient SAG-transgenic mice are able to activate cognate T cells.
引用
收藏
页码:139 / 146
页数:8
相关论文
共 43 条
[1]   CLONAL DELETION OF V-BETA 14-BEARING T-CELLS IN MICE TRANSGENIC FOR MAMMARY-TUMOR VIRUS [J].
ACHAORBEA, H ;
SHAKHOV, AN ;
SCARPELLINO, L ;
KOLB, E ;
MULLER, V ;
VESSAZSHAW, A ;
FUCHS, R ;
BLOCHLINGER, K ;
ROLLINI, P ;
BILLOTTE, J ;
SARAFIDOU, M ;
MACDONALD, HR ;
DIGGELMANN, H .
NATURE, 1991, 350 (6315) :207-211
[2]   MOLECULAR AND BIOLOGICAL CHARACTERIZATION OF A MURINE LIGAND FOR CD40 [J].
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 .
NATURE, 1992, 357 (6373) :80-82
[3]   THE CD40 LIGAND, GP39, IS DEFECTIVE IN ACTIVATED T-CELLS FROM PATIENTS WITH X-LINKED HYPER-IGM SYNDROME [J].
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 .
CELL, 1993, 72 (02) :291-300
[4]   B-CELLS ARE ESSENTIAL FOR MURINE MAMMARY-TUMOR VIRUS TRANSMISSION, BUT NOT FOR PRESENTATION OF ENDOGENOUS SUPERANTIGENS [J].
BEUTNER, U ;
KRAUS, E ;
KITAMURA, D ;
RAJEWSKY, K ;
HUBER, BT .
JOURNAL OF EXPERIMENTAL MEDICINE, 1994, 179 (05) :1457-1466
[5]   A SUPERANTIGEN ENCODED IN THE OPEN READING FRAME OF THE 3' LONG TERMINAL REPEAT OF MOUSE MAMMARY-TUMOR VIRUS [J].
CHOI, YW ;
KAPPLER, JW ;
MARRACK, P .
NATURE, 1991, 350 (6315) :203-207
[6]   SURFACE-ANTIGEN EXPRESSION AND IMMUNOGLOBULIN GENE REARRANGEMENT DURING MOUSE PRE-B-CELL DEVELOPMENT [J].
COFFMAN, RL .
IMMUNOLOGICAL REVIEWS, 1983, 69 :5-23
[7]   CHARACTERIZATION OF THE MURINE ANTIGENIC DETERMINANT, DESIGNATED L3T4A, RECOGNIZED BY MONOCLONAL-ANTIBODY GK1.5 - EXPRESSION OF L3T4A BY FUNCTIONAL T-CELL CLONES APPEARS TO CORRELATE PRIMARILY WITH CLASS II MHC ANTIGEN-REACTIVITY [J].
DIALYNAS, DP ;
WILDE, DB ;
MARRACK, P ;
PIERRES, A ;
WALL, KA ;
HAVRAN, W ;
OTTEN, G ;
LOKEN, MR ;
PIERRES, M ;
KAPPLER, J ;
FITCH, FW .
IMMUNOLOGICAL REVIEWS, 1983, 74 :29-56
[8]   SMALL B-CELLS AS ANTIGEN-PRESENTING CELLS IN THE INDUCTION OF TOLERANCE TO SOLUBLE-PROTEIN ANTIGENS [J].
EYNON, EE ;
PARKER, DC .
JOURNAL OF EXPERIMENTAL MEDICINE, 1992, 175 (01) :131-138
[9]   B-CELLS TURN OFF VIRGIN BUT NOT MEMORY T-CELLS [J].
FUCHS, EJ ;
MATZINGER, P .
SCIENCE, 1992, 258 (5085) :1156-1159
[10]   HUMAN B-CELL CLONES CAN BE INDUCED TO PROLIFERATE AND TO SWITCH TO IGE AND IGG4 SYNTHESIS BY INTERLEUKIN-4 AND A SIGNAL PROVIDED BY ACTIVATED CD4+ T-CELL CLONES [J].
GASCAN, H ;
GAUCHAT, JF ;
RONCAROLO, MG ;
YSSEL, H ;
SPITS, H ;
DEVRIES, JE .
JOURNAL OF EXPERIMENTAL MEDICINE, 1991, 173 (03) :747-750
12345