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Nascent chains can form co-translational folding intermediates that promote post-translational folding outcomes in a disease-causing protein

Author

Listed:
  • Elena Plessa

    (University College London)

  • Lien P. Chu

    (University College London)

  • Sammy H. S. Chan

    (University College London)

  • Oliver L. Thomas

    (University College London)

  • Anaïs M. E. Cassaignau

    (University College London)

  • Christopher A. Waudby

    (University College London)

  • John Christodoulou

    (University College London
    School of Crystallography, Birkbeck College, University of London)

  • Lisa D. Cabrita

    (University College London)

Abstract

During biosynthesis, proteins can begin folding co-translationally to acquire their biologically-active structures. Folding, however, is an imperfect process and in many cases misfolding results in disease. Less is understood of how misfolding begins during biosynthesis. The human protein, alpha-1-antitrypsin (AAT) folds under kinetic control via a folding intermediate; its pathological variants readily form self-associated polymers at the site of synthesis, leading to alpha-1-antitrypsin deficiency. We observe that AAT nascent polypeptides stall during their biosynthesis, resulting in full-length nascent chains that remain bound to ribosome, forming a persistent ribosome-nascent chain complex (RNC) prior to release. We analyse the structure of these RNCs, which reveals compacted, partially-folded co-translational folding intermediates possessing molten-globule characteristics. We find that the highly-polymerogenic mutant, Z AAT, forms a distinct co-translational folding intermediate relative to wild-type. Its very modest structural differences suggests that the ribosome uniquely tempers the impact of deleterious mutations during nascent chain emergence. Following nascent chain release however, these co-translational folding intermediates guide post-translational folding outcomes thus suggesting that Z’s misfolding is initiated from co-translational structure. Our findings demonstrate that co-translational folding intermediates drive how some proteins fold under kinetic control, and may thus also serve as tractable therapeutic targets for human disease.

Suggested Citation

  • Elena Plessa & Lien P. Chu & Sammy H. S. Chan & Oliver L. Thomas & Anaïs M. E. Cassaignau & Christopher A. Waudby & John Christodoulou & Lisa D. Cabrita, 2021. "Nascent chains can form co-translational folding intermediates that promote post-translational folding outcomes in a disease-causing protein," Nature Communications, Nature, vol. 12(1), pages 1-13, December.
    • Handle: RePEc:nat:natcom:v:12:y:2021:i:1:d:10.1038_s41467-021-26531-1
    DOI: 10.1038/s41467-021-26531-1
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    References listed on IDEAS

    as
    1. Alistair M. Jagger & Christopher A. Waudby & James A. Irving & John Christodoulou & David A. Lomas, 2020. "High-resolution ex vivo NMR spectroscopy of human Z α1-antitrypsin," Nature Communications, Nature, vol. 11(1), pages 1-13, December.
    2. Hideki Shishido & Jae Seok Yoon & Zhongying Yang & William R. Skach, 2020. "CFTR trafficking mutations disrupt cotranslational protein folding by targeting biosynthetic intermediates," Nature Communications, Nature, vol. 11(1), pages 1-11, December.
    3. Mehdi Eshraghi & Pabalu P. Karunadharma & Juliana Blin & Neelam Shahani & Emiliano P. Ricci & Audrey Michel & Nicolai T. Urban & Nicole Galli & Manish Sharma & Uri Nimrod Ramírez-Jarquín & Katie Flore, 2021. "Mutant Huntingtin stalls ribosomes and represses protein synthesis in a cellular model of Huntington disease," Nature Communications, Nature, vol. 12(1), pages 1-20, December.
    4. Lisa M. Alexander & Daniel H. Goldman & Liang M. Wee & Carlos Bustamante, 2019. "Non-equilibrium dynamics of a nascent polypeptide during translation suppress its misfolding," Nature Communications, Nature, vol. 10(1), pages 1-11, December.
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    Cited by:

    1. Minkoo Ahn & Tomasz Włodarski & Alkistis Mitropoulou & Sammy H. S. Chan & Haneesh Sidhu & Elena Plessa & Thomas A. Becker & Nediljko Budisa & Christopher A. Waudby & Roland Beckmann & Anaïs M. E. Cass, 2022. "Modulating co-translational protein folding by rational design and ribosome engineering," Nature Communications, Nature, vol. 13(1), pages 1-14, December.
    2. Naoto Soya & Haijin Xu & Ariel Roldan & Zhengrong Yang & Haoxin Ye & Fan Jiang & Aiswarya Premchandar & Guido Veit & Susan P. C. Cole & John Kappes & Tamás Hegedüs & Gergely L. Lukacs, 2023. "Folding correctors can restore CFTR posttranslational folding landscape by allosteric domain–domain coupling," Nature Communications, Nature, vol. 14(1), pages 1-21, December.

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