The Evolutionarily Conserved Eukaryotic Arginine Attenuator Peptide Regulates the Movement of Ribosomes That Have Translated It

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Molecular and Cellular Biology, December 1998, p. 7528-7536, Vol. 18, No. 12
0270-7306/98/$04.00+0
Copyright © 1998, American Society for Microbiology. All rights reserved.

The Evolutionarily Conserved Eukaryotic Arginine Attenuator Peptide Regulates the Movement of Ribosomes That Have Translated It

Zhong Wang,¹ Peng Fang,¹ and Matthew S. Sachs¹^,²^,^*

Department of Biochemistry and Molecular Biology, Oregon Graduate Institute of Science & Technology, Portland, Oregon 97291-1000,¹ and Department of Molecular Microbiology and Immunology, Oregon Health Sciences University, Portland, Oregon 97201-3098²

Received 17 July 1998/Returned for modification 21 August 1998/Accepted 28 August 1998

Translation of the upstream open reading frame (uORF) in the 5' leader segment of the Neurospora crassa arg-2 mRNA causesreduced initiation at a downstream start codon when arginine isplentiful. Previous examination of this translational attenuationmechanism using a primer-extension inhibition (toeprint) assayin a homologous N. crassa cell-free translation system showedthat arginine causes ribosomes to stall at the uORF terminationcodon. This stalling apparently regulates translation by preventingtrailing scanning ribosomes from reaching the downstream startcodon. Here we provide evidence that neither the distance betweenthe uORF stop codon and the downstream initiation codon nor thenature of the stop codon used to terminate translation of theuORF-encoded arginine attenuator peptide (AAP) is important forregulation. Furthermore, translation of the AAP coding regionregulates synthesis of the firefly luciferase polypeptide whenit is fused directly at the N terminus of that polypeptide. Inthis case, the elongating ribosome stalls in response to Arg soonafter it translates the AAP coding region. Regulation by thiseukaryotic leader peptide thus appears to be exerted through anovel mechanism of cis-acting translationalcontrol.

^* Corresponding author. Mailing address: Department of Biochemistry and Molecular Biology, Oregon Graduate Institute of Science& Technology, P.O. Box 91000, Portland, OR 97291-1000. Phone:(503) 748-1487. Fax: (748) 690-1464. E-mail: msachs{at}bmb.ogi.edu.

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