An RNasin-resistant Ribonuclease Selective for Interleukin 2 MRNA

Overview

Journal Nucleic Acids Res

Publisher Oxford University Press

Specialty Biochemistry

Date 1993 Jan 11

PMID 8441610

Citations 3

Authors

J Hua

R Garner

V Paetkau

Affiliations

Soon will be listed here.

Abstract

Interleukin 2 (IL2) mRNA has a short half-life in the cytoplasm of T lymphocytes, relative to most mRNA. We have discovered a candidate ribonuclease to account for the rapid turnover of IL2 mRNA in the cytosol of the human T lymphocyte cell line Jurkat. In partially purified form, this RNase is about 7 times as active on IL2 as on beta-globin mRNA. Pancreatic RNase, by contrast, does not show a significant preference for IL2 mRNA. Neither 5' capping, nor polyadenylation of the substrate mRNAs affects their degradation by the IL2-selective mRNase, whose activity is optimal in 0.5 mM Mg++ and 100 mM potassium acetate. The mRNase behaves like a protein of molecular weight 60-70,000 on gel chromatography, and is unusual in that it is insensitive to placental RNase inhibitor (RNasin). The mRNase cleaves IL2 mRNA at a small number of sites in the coding region, and IL2 mRNA containing only the coding region and 36 nucleotides of the 3'-noncoding region competes efficiently with full-length IL2 mRNA for the mRNase, whereas beta-globin mRNA does not.

Citing Articles

Characterization of nuclear RNases that cleave hepatitis B virus RNA near the La protein binding site.

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PMID: 11435567 PMC: 114415. DOI: 10.1128/JVI.75.15.6874-6883.2001.

A binding factor for interleukin 2 mRNA.

Hua J, Paetkau V Nucleic Acids Res. 1996; 24(5):970-6.

PMID: 8600467 PMC: 145722. DOI: 10.1093/nar/24.5.970.

mRNA stability in mammalian cells.

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PMID: 7565413 PMC: 239368. DOI: 10.1128/mr.59.3.423-450.1995.

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