BIOSYNTHESIS OF HUMAN ACUTE-PHASE SERUM AMYLOID A-PROTEIN (A-SAA) INVITRO - THE ROLES OF MESSENGER-RNA ACCUMULATION, POLY(A) TAIL SHORTENING AND TRANSLATIONAL EFFICIENCY

被引：43

作者：

STEEL, DM

ROGERS, JT

DEBEER, MC

DEBEER, FC

WHITEHEAD, AS

机构：

[1] UNIV DUBLIN TRINITY COLL,DEPT GENET,DUBLIN 2,IRELAND

[2] HARVARD UNIV,BRIGHAM & WOMENS HOSP,SCH MED,DEPT HEMATOL,BOSTON,MA 02115

[3] UNIV KENTUCKY,MED CTR,DEPT MED,LEXINGTON,KY 40536

[4] DEPT VET AFFAIRS MED CTR,LEXINGTON,KY 40536

来源：

BIOCHEMICAL JOURNAL | 1993年 / 291卷

基金：

英国惠康基金;

关键词：

D O I：

10.1042/bj2910701

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：

Human 'acute-phase' serum amyloid A protein (A-SAA) is a major acute-phase reactant (APR) and an apolipoprotein of high density lipoprotein 3 (HDL3). We have examined several parameters of A-SAA biosynthesis in PLC/PRF/5 hepatoma cells in response to monocyte conditioned medium (MoCM) and dual treatment with interleukin-1beta and interleukin-6 (IL-1beta+IL-6). Treatment of PLC/PRF/5 cells with MoCM or IL-1beta+IL-6 caused a dramatic and rapid increase in A-SAA mRNA and protein synthesis; A-SAA mRNA was first detectable at 3 h, with peak levels reached by 24 h. A-SAA mRNA accumulation is accompanied by a gradual and homogeneous decrease in the length of the A-SAA poly(A) tail; the poly(A) tail shortening does not apparently affect the intrinsic stability of A-SAA mRNA. Analysis of RNA isolated from the ribonucleoprotein, monosome and polysome fractions of cytokine-treated PLC/PRF/5 cells showed that most A-SAA mRNA was associated with small polyribosomes, regardless of time post-stimulus, suggesting that the translational efficiency of A-SAA mRNA is constant throughout cytokine-driven induction. Moreover, the transit time of A-SAA protein out of the cell is also constant throughout the time course of induction. These data provide evidence of a paradox with regard to the transcriptional up-regulation of A-SAA by IL-1beta+IL-6 and the relative synthesis of A-SAA protein and suggest a role for post-transcriptional control of A-SAA biosynthesis during the acute phase.

引用

页码：701 / 707

页数：7

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