Resistance of mRNAs with AUG-proximal nonsense mutations to nonsense-mediated decay reflects variables of mRNA structure and translational activity

Francisco J.C. Pereira(National Institute of Health Dr. Ricardo Jorge), Alexandre Teixeira(Universidade Nova de Lisboa), Jian Kong(University of Pennsylvania), Cristina Barbosa(University of Lisbon), Ana Luísa Silva(National Institute of Health Dr. Ricardo Jorge), Ana Marques-Ramos(National Institute of Health Dr. Ricardo Jorge), Stephen A. Liebhaber(University of Pennsylvania), Luı́sa Romão(University of Lisbon)
Nucleic Acids Research
June 11, 2015
Cited by 41Open Access
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Abstract

Nonsense-mediated mRNA decay (NMD) is a surveillance pathway that recognizes and selectively degrades mRNAs carrying premature termination codons (PTCs). The level of sensitivity of a PTC-containing mRNA to NMD is multifactorial. We have previously shown that human β-globin mRNAs carrying PTCs in close proximity to the translation initiation AUG codon escape NMD. This was called the 'AUG-proximity effect'. The present analysis of nonsense codons in the human α-globin mRNA illustrates that the determinants of the AUG-proximity effect are in fact quite complex, reflecting the ability of the ribosome to re-initiate translation 3' to the PTC and the specific sequence and secondary structure of the translated ORF. These data support a model in which the time taken to translate the short ORF, impacted by distance, sequence, and structure, not only modulates translation re-initiation, but also impacts on the exact boundary of AUG-proximity protection from NMD.


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