Human SMG-1, a Novel Phosphatidylinositol 3-kinase-related Protein Kinase, Associates with Components of the MRNA Surveillance Complex and is Involved in the Regulation of Nonsense-mediated MRNA Decay

Overview

Journal Genes Dev

Specialty Molecular Biology

Date 2001 Sep 7

PMID 11544179

Citations 197

Authors

A Yamashita

T Ohnishi

I Kashima

Y Taya

S Ohno

Affiliations

Soon will be listed here.

Abstract

Nonsense-mediated mRNA decay (NMD) is a conserved surveillance mechanism that eliminates imperfect mRNAs that contain premature translation termination codons (PTCs) and code for nonfunctional or potentially harmful polypeptides. We show that a novel phosphatidylinositol 3-kinase-related protein kinase, hSMG-1, is a human ortholog of a product of Caenorhabditis elegans smg-1, one of seven smg genes involved in NMD. hSMG-1 phosphorylates hUPF1/SMG-2 in vivo and in vitro at specific serine residues in SQ motifs. hSMG-1 can associate with hUPF1/SMG-2 and other components of the surveillance complex. In particular, overexpression of a kinase-deficient point mutant of hSMG-1, hSMG-1-DA, results in a marked suppression of the PTC-dependent beta-globin mRNA degradation; whereas that of wild-type hSMG-1 enhances it. We also show that inhibitors of hSMG-1 induce the accumulation of truncated p53 proteins in human cancer cell lines with p53 PTC mutation. Taken together, we conclude that hSMG-1 plays a critical role in NMD through the direct phosphorylation of hUPF1/SMG-2 in the evolutionally conserved mRNA surveillance complex.

Citing Articles

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Identification of nonsense-mediated decay inhibitors that alter the tumor immune landscape.

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Misincorporations of amino acids in p53 in human cells at artificially constructed termination codons in the presence of the aminoglycoside Gentamicin.

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Effect of nonsense-mediated mRNA decay factor SMG9 deficiency on premature aging in zebrafish.

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