Publikation: NAC controls cotranslational N-terminal methionine excision in eukaryotes
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N-terminal methionine excision from newly synthesized proteins, catalyzed cotranslationally by methionine aminopeptidases (METAPs), is an essential and universally conserved process that plays a key role in cell homeostasis and protein biogenesis. However, how METAPs interact with ribosomes and how their cleavage specificity is ensured is unknown. We discovered that in eukaryotes the nascent polypeptide–associated complex (NAC) controls ribosome binding of METAP1. NAC recruits METAP1 using a long, flexible tail and provides a platform for the formation of an active methionine excision complex at the ribosomal tunnel exit. This mode of interaction ensures the efficient excision of methionine from cytosolic proteins, whereas proteins targeted to the endoplasmic reticulum are spared. Our results suggest a broader mechanism for how access of protein biogenesis factors to translating ribosomes is controlled.
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GAMERDINGER, Martin, Min JIA, Renate SCHLÖMER, Laurenz RABL, Katrin KHAKZAR, Zeynel ULUSOY, Annalena WALLISCH, Gundula HUNAEUS, Kay DIEDERICHS, Nenad BAN, Elke DEUERLING, 2023. NAC controls cotranslational N-terminal methionine excision in eukaryotes. In: Science. American Association for the Advancement of Science (AAAS). 2023, 380(6651), pp. 1238-1243. ISSN 0036-8075. eISSN 1095-9203. Available under: doi: 10.1126/science.adg3297BibTex
@article{Gamerdinger2023-06-23contr-67665, year={2023}, doi={10.1126/science.adg3297}, title={NAC controls cotranslational N-terminal methionine excision in eukaryotes}, number={6651}, volume={380}, issn={0036-8075}, journal={Science}, pages={1238--1243}, author={Gamerdinger, Martin and Jia, Min and Schlömer, Renate and Rabl, Laurenz and Khakzar, Katrin and Ulusoy, Zeynel and Wallisch, Annalena and Hunaeus, Gundula and Diederichs, Kay and Ban, Nenad and Deuerling, Elke} }
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