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Comprehensive translational profiling and STE AI uncover rapid control of protein biosynthesis during cell stress

Attila Horvath 1
Yoshika Janapala 1
Katrina Woodward 1
Shafi Mahmud 1
Alice Cleynen 1, 2
Elizabeth E. Gardiner 3
Katherine Hannan 1, 4, 5, 6, 7
Eduardo Eyras 1, 8, 9
Thomas Preiss 1, 10
Nikolay E. Shirokikh 1
Тип публикацииJournal Article
Дата публикации2024-05-09
scimago Q1
wos Q1
БС1
SJR7.776
CiteScore31.7
Impact factor13.1
ISSN03051048, 13624962
Краткое описание

Translational control is important in all life, but it remains a challenge to accurately quantify. When ribosomes translate messenger (m)RNA into proteins, they attach to the mRNA in series, forming poly(ribo)somes, and can co-localize. Here, we computationally model new types of co-localized ribosomal complexes on mRNA and identify them using enhanced translation complex profile sequencing (eTCP-seq) based on rapid in vivo crosslinking. We detect long disome footprints outside regions of non-random elongation stalls and show these are linked to translation initiation and protein biosynthesis rates. We subject footprints of disomes and other translation complexes to artificial intelligence (AI) analysis and construct a new, accurate and self-normalized measure of translation, termed stochastic translation efficiency (STE). We then apply STE to investigate rapid changes to mRNA translation in yeast undergoing glucose depletion. Importantly, we show that, well beyond tagging elongation stalls, footprints of co-localized ribosomes provide rich insight into translational mechanisms, polysome dynamics and topology. STE AI ranks cellular mRNAs by absolute translation rates under given conditions, can assist in identifying its control elements and will facilitate the development of next-generation synthetic biology designs and mRNA-based therapeutics.

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Cancer Cell International
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Drug Discovery Today
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Cold Spring Harbor Laboratory
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Horvath A. et al. Comprehensive translational profiling and STE AI uncover rapid control of protein biosynthesis during cell stress // Nucleic Acids Research. 2024. Vol. 52. No. 13. pp. 7925-7946.
ГОСТ со всеми авторами (до 50) Скопировать
Horvath A., Janapala Y., Woodward K., Mahmud S., Cleynen A., Gardiner E. E., Hannan K., Eyras E., Preiss T., Shirokikh N. E. Comprehensive translational profiling and STE AI uncover rapid control of protein biosynthesis during cell stress // Nucleic Acids Research. 2024. Vol. 52. No. 13. pp. 7925-7946.
RIS |
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TY - JOUR
DO - 10.1093/nar/gkae365
UR - https://academic.oup.com/nar/article/52/13/7925/7667526
TI - Comprehensive translational profiling and STE AI uncover rapid control of protein biosynthesis during cell stress
T2 - Nucleic Acids Research
AU - Horvath, Attila
AU - Janapala, Yoshika
AU - Woodward, Katrina
AU - Mahmud, Shafi
AU - Cleynen, Alice
AU - Gardiner, Elizabeth E.
AU - Hannan, Katherine
AU - Eyras, Eduardo
AU - Preiss, Thomas
AU - Shirokikh, Nikolay E.
PY - 2024
DA - 2024/05/09
PB - Oxford University Press
SP - 7925-7946
IS - 13
VL - 52
PMID - 38721779
SN - 0305-1048
SN - 1362-4962
ER -
BibTex |
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@article{2024_Horvath,
author = {Attila Horvath and Yoshika Janapala and Katrina Woodward and Shafi Mahmud and Alice Cleynen and Elizabeth E. Gardiner and Katherine Hannan and Eduardo Eyras and Thomas Preiss and Nikolay E. Shirokikh},
title = {Comprehensive translational profiling and STE AI uncover rapid control of protein biosynthesis during cell stress},
journal = {Nucleic Acids Research},
year = {2024},
volume = {52},
publisher = {Oxford University Press},
month = {may},
url = {https://academic.oup.com/nar/article/52/13/7925/7667526},
number = {13},
pages = {7925--7946},
doi = {10.1093/nar/gkae365}
}
MLA
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Horvath, Attila, et al. “Comprehensive translational profiling and STE AI uncover rapid control of protein biosynthesis during cell stress.” Nucleic Acids Research, vol. 52, no. 13, May. 2024, pp. 7925-7946. https://academic.oup.com/nar/article/52/13/7925/7667526.