TRANSCRIPTIONAL AND POSTTRANSCRIPTIONAL REGULATION OF TCR, CD4 AND CD8 GENE-EXPRESSION DURING ACTIVATION OF NORMAL HUMAN LYMPHOCYTES-T

被引：89

作者：

PAILLARD, F ^{[1
]}

STERKERS, G ^{[1
]}

VAQUERO, C ^{[1
]}

机构：

[1] HOP COCHIN,IMMUNOL & ONCOL MALADIES RETROVIRALES LAB,CNRS,URA 628,INSERM,F-75674 PARIS 14,FRANCE

来源：

EMBO JOURNAL | 1990年 / 9卷 / 06期

关键词：

mRNA expression; normal human T lymphocytes; post-transcriptional regulation; T cell receptor; transcriptional regulation;

D O I：

10.1002/j.1460-2075.1990.tb08312.x

中图分类号：

Q5 [生物化学]; Q7 [分子生物学];

学科分类号：

071010 ; 081704 ;

摘要：

We previously showed that the turnover rates of the messengers coding for the T cell receptor (TcR) α, β and γ, CD4 and CD8 molecules composing the multireceptor complex vary in normal human mature T lymphocytes according to their state of activation. Activation by soluble anti-CD3 which does not induce proliferation, promotes a weak up-modulation of the corresponding five mRNAs. In contrast, activation signals such as anti-CD3 + PMA, which lead to lymphokine mRNA expression and T cell proliferation, promote a decrease of the TcR, CD4 and CD8 mRNA levels within 4 h post-activation, followed by their gradual re-expression. Here we show that the down-modulation of these mRNAs results from early regulation controls at transcriptional and post-transcriptional levels, i.e. through a concomitant inhibition of transcription and destabilization of the mRNA. Moreover, later re-expression of the mRNA results from recovery of transcription and marked increase of the mRNA stability. Finally, down-modulation is specific for TcR, CD4 and CD8 mRNAs, all submitted to similar regulation processes. These results strongly suggest a direct correlation between down-modulation of the multireceptor complex mRNAs, and lymphokine mRNA expression, and cellular proliferation.

引用

页码：1867 / 1872

页数：6

共 43 条

[1] KINASES AND PHOSPHATASES IN T-CELL ACTIVATION [J].

ALEXANDER, DR ;

CANTRELL, DA .

IMMUNOLOGY TODAY, 1989, 10 (06) :200-205

[2] A CONSERVED SEQUENCE IN THE T-CELL RECEPTOR BETA-CHAIN PROMOTER REGION [J].

ANDERSON, SJ ;

CHOU, HS ;

LOH, DY .

PROCEEDINGS OF THE NATIONAL ACADEMY OF SCIENCES OF THE UNITED STATES OF AMERICA, 1988, 85 (10) :3551-3554

[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] NORTHERN BLOT NORMALIZATION WITH A 28S RIBOSOMAL-RNA OLIGONUCLEOTIDE PROBE [J].

BARBU, V ;

DAUTRY, F .

NUCLEIC ACIDS RESEARCH, 1989, 17 (17) :7115-7115

[5]

BLUE ML, 1987, J IMMUNOL, V139, P3949

[6] A T-CELL RECEPTOR GAMMA-CD3 COMPLEX FOUND ON CLONED FUNCTIONAL LYMPHOCYTES [J].

BORST, J ;

VANDEGRIEND, RJ ;

VANOOSTVEEN, JW ;

ANG, SL ;

MELIEF, CJ ;

SEIDMAN, JG ;

BOLHUIS, RLH .

NATURE, 1987, 325 (6106) :683-688

[7] CROSS-LINKING OF HUMAN T-CELL RECEPTOR PROTEINS - ASSOCIATION BETWEEN THE T-CELL IDIOTYPE BETA-SUBUNIT AND THE T3 GLYCOPROTEIN HEAVY SUBUNIT [J].

BRENNER, MB ;

TROWBRIDGE, IS ;

STROMINGER, JL .

CELL, 1985, 40 (01) :183-190

[8] REGULATION OF C-MYC MESSENGER-RNA STABILITY INVITRO BY A LABILE DESTABILIZER WITH AN ESSENTIAL NUCLEIC-ACID COMPONENT [J].

BREWER, G ;

ROSS, J .

MOLECULAR AND CELLULAR BIOLOGY, 1989, 9 (05) :1996-2006

[9] ASSOCIATION OF PHOSPHORYLATION OF THE T3 ANTIGEN WITH IMMUNE ACTIVATION OF LYMPHOCYTES-T [J].

CANTRELL, D ;

DAVIES, AA ;

LONDEI, M ;

FELDMAN, M ;

CRUMPTON, MJ .

NATURE, 1987, 325 (6104) :540-542

[10] STIMULATION AND PROLIFERATION OF CD4+ PERIPHERAL-BLOOD LYMPHOCYTES-T INDUCED BY AN ANTI-CD4 MONOCLONAL-ANTIBODY [J].

CARREL, S ;

MORETTA, A ;

PANTALEO, G ;

TAMBUSSI, G ;

ISLER, P ;

PERUSSIA, B ;

CEROTTINI, JC .

EUROPEAN JOURNAL OF IMMUNOLOGY, 1988, 18 (03) :333-339

← 1 2 3 4 5 →