HUMAN CD4 RESTORES NORMAL T-CELL DEVELOPMENT AND FUNCTION IN MICE DEFICIENT IN MURINE CD4

被引:34
作者
LAW, YM
YEUNG, RSM
MAMALAKI, C
KIOUSSIS, D
MAK, TW
FLAVELL, RA
机构
[1] YALE UNIV, SCH MED,HOWARD HUGHES MED INST,IMMUNOBIOL SECT, FMB 410,310 CEDAR ST, NEW HAVEN, CT 06510 USA
[2] UNIV TORONTO, DEPT IMMUNOL, TORONTO M4X 1K9, ONTARIO, CANADA
[3] UNIV TORONTO, DEPT MED BIOPHYS, TORONTO M4X 1K9, ONTARIO, CANADA
[4] NATL INST MED RES, LONDON NW7 1AA, ENGLAND
来源
JOURNAL OF EXPERIMENTAL MEDICINE | 1994年 / 179卷 / 04期
关键词
D O I
10.1084/jem.179.4.1233
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 ability of a human coreceptor to function in mice was investigated by generating human CD4 (hCD4)-expressing transgenic mice on a mouse CD4-deficient (mCD4-/-) background. From developing thymocyte to matured T lymphocyte functions, hCD4 was shown to be physiologically active. By examining the expansion and deletion of specific Vbeta T cell families in mutated mice with and without hCD4, it was found that hCD4 can participate in positive and negative selection. Mature hCD4 single positive cells also were found in the periphery and they were shown to restore MHC class II-restricted alloreactive and antigen-specific T cell responses that were deficient in the mCD4 (-/-) mice. In addition, these hCD4 reconstituted mice can generate a secondary immunoglobulin G humoral response matching that of mCD4 wild-type mice. The fact that human CD4 is functional in mice and can be studied in the absence of murine CD4 should facilitate studies of human CD4 activity in general and human immunodeficiency virus 1 gp120-mediated pathogenesis in acquired immune deficiency syndrome specifically.
引用
收藏
页码:1233 / 1242
页数:10
相关论文
共 46 条
[1]   EXOGENOUS AND ENDOGENOUS MOUSE MAMMARY-TUMOR VIRUS SUPERANTIGENS [J].
ACHAORBEA, H ;
HELD, W ;
WAANDERS, GA ;
SHAKHOV, AN ;
SCARPELLINO, L ;
LEES, RK ;
MACDONALD, HR .
IMMUNOLOGICAL REVIEWS, 1993, 131 :5-25
[2]   CROSS-LINKING CD4 BY HUMAN IMMUNODEFICIENCY VIRUS-GP120 PRIMES T-CELLS FOR ACTIVATION-INDUCED APOPTOSIS [J].
BANDA, NK ;
BERNIER, J ;
KURAHARA, DK ;
KURRLE, R ;
HAIGWOOD, N ;
SEKALY, RP ;
FINKEL, TH .
JOURNAL OF EXPERIMENTAL MEDICINE, 1992, 176 (04) :1099-1106
[3]   THE CD4 AND CD8 ANTIGENS ARE COUPLED TO A PROTEIN-TYROSINE KINASE (P56LCK) THAT PHOSPHORYLATES THE CD3 COMPLEX [J].
BARBER, EK ;
DASGUPTA, JD ;
SCHLOSSMAN, SF ;
TREVILLYAN, JM ;
RUDD, CE .
PROCEEDINGS OF THE NATIONAL ACADEMY OF SCIENCES OF THE UNITED STATES OF AMERICA, 1989, 86 (09) :3277-3281
[4]   SPECIES SPECIFICITY AND AUGMENTATION OF RESPONSES TO CLASS-II MAJOR HISTOCOMPATIBILITY COMPLEX-MOLECULES IN HUMAN CD4 TRANSGENIC MICE [J].
BARZAGAGILBERT, E ;
GRASS, D ;
LAWRANCE, SK ;
PETERSON, PA ;
LACY, E ;
ENGELHARD, VH .
JOURNAL OF EXPERIMENTAL MEDICINE, 1992, 175 (06) :1707-1715
[5]   THE MHC MOLECULE I-E IS NECESSARY BUT NOT SUFFICIENT FOR THE CLONAL DELETION OF V-BETA-11-BEARING T-CELLS [J].
BILL, J ;
KANAGAWA, O ;
WOODLAND, DL ;
PALMER, E .
JOURNAL OF EXPERIMENTAL MEDICINE, 1989, 169 (04) :1405-1419
[6]   DEVELOPMENT OF THE CD4 AND CD8 LINEAGE OF T-CELLS - INSTRUCTION VERSUS SELECTION [J].
BORGULYA, P ;
KISHI, H ;
MULLER, U ;
KIRBERG, J ;
VONBOEHMER, H .
EMBO JOURNAL, 1991, 10 (04) :913-918
[7]   ANOTHER VIEW OF THE SELECTIVE MODEL OF THYMOCYTE SELECTION [J].
CHAN, SH ;
COSGROVE, D ;
WALTZINGER, C ;
BENOIST, C ;
MATHIS, D .
CELL, 1993, 73 (02) :225-236
[8]   IDENTIFICATION OF HUMAN CD4 RESIDUES AFFECTING CLASS-II MHC VERSUS HIV-1 GP120 BINDING [J].
CLAYTON, LK ;
SIEH, M ;
PIOUS, DA ;
REINHERZ, EL .
NATURE, 1989, 339 (6225) :548-551
[9]   EVIDENCE FOR A STOCHASTIC MECHANISM IN THE DIFFERENTIATION OF MATURE SUBSETS OF T-LYMPHOCYTES [J].
DAVIS, CB ;
KILLEEN, N ;
CROOKS, MEC ;
RAULET, D ;
LITTMAN, DR .
CELL, 1993, 73 (02) :237-247
[10]   DELETION OF SELF-REACTIVE THYMOCYTES OCCURS AT A CD4+8+ PRECURSOR STAGE [J].
FOWLKES, BJ ;
SCHWARTZ, RH ;
PARDOLL, DM .
NATURE, 1988, 334 (6183) :620-623
12345