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Published October 19, 2021 | Published + Supplemental Material
Journal Article Open

Dynamic changes in tRNA modifications and abundance during T cell activation

Abstract

The tRNA pool determines the efficiency, throughput, and accuracy of translation. Previous studies have identified dynamic changes in the tRNA (transfer RNA) supply and mRNA (messenger RNA) demand during cancerous proliferation. Yet dynamic changes may also occur during physiologically normal proliferation, and these are less well characterized. We examined the tRNA and mRNA pools of T cells during their vigorous proliferation and differentiation upon triggering their antigen receptor. We observed a global signature of switch in demand for codons at the early proliferation phase of the response, accompanied by corresponding changes in tRNA expression levels. In the later phase, upon differentiation, the response of the tRNA pool relaxed back to the basal level, potentially restraining excessive proliferation. Sequencing of tRNAs allowed us to evaluate their diverse base-modifications. We found that two types of tRNA modifications, wybutosine and ms2t6A, are reduced dramatically during T cell activation. These modifications occur in the anticodon loops of two tRNAs that decode "slippery codons," which are prone to ribosomal frameshifting. Attenuation of these frameshift-protective modifications is expected to increase the potential for proteome-wide frameshifting during T cell proliferation. Indeed, human cell lines deleted of a wybutosine writer showed increased ribosomal frameshifting, as detected with an HIV gag-pol frameshifting site reporter. These results may explain HIV's specific tropism toward proliferating T cells since it requires ribosomal frameshift exactly on the corresponding codon for infection. The changes in tRNA expression and modifications uncover a layer of translation regulation during T cell proliferation and expose a potential tradeoff between cellular growth and translation fidelity.

Additional Information

© 2021 National Academy of Sciences. Published under the PNAS license. Edited by Nahum Sonenberg, McGill University, Montreal, QC, Canada, and approved July 28, 2021 (received for review April 14, 2021). We thank the Y.P. and N.F. laboratory members Noa Hefetz-Aharon, Martin Mikl, Schraga Schwartz, and Daniel Douek for stimulating discussions. We also thank the European Research Council, the Israel Science Foundation, and the Israel Cancer Research Fund for grant support. Data Availability: The data reported in this paper have been deposited in the Gene Expression Omnibus (GEO) database (accession no. GSE165622) (66). Data sources are as follows: The coding sequences of Mus musculus were downloaded from the Consensus CDS (CCDS) project (https://www.ncbi.nlm.nih.gov/projects/CCDS/CcdsBrowse.cgi). For classification of gene categories, defined gene categories by biological process were downloaded from the GO project (http://geneontology.org/); to avoid too-small gene sets, we considered only those with at least 40 genes. Pathway lists were downloaded from mouseMine. For tRNA modifications, annotation of tRNA modifications were downloaded from the MODOMICS (9) database (http://genesilico.pl/modomics/). Author contributions: R.R., M.P., O.D., N.F., and Y.P. designed research; R.R., M.P., I.E.-M., Y.M., Y.S., O.M., and S.R.-Z., performed research; R.R. contributed new reagents/analytic tools; R.R., A.N., N.S.-G., and Y.P. analyzed data; and R.R., O.D., T.S., N.F., and Y.P. wrote the paper. The authors declare no competing interest. This article is a PNAS Direct Submission. This article contains supporting information online at https://www.pnas.org/lookup/suppl/doi:10.1073/pnas.2106556118/-/DCSupplemental.

Attached Files

Published - e2106556118.full.pdf

Supplemental Material - pnas.2106556118.sapp.pdf

Supplemental Material - pnas.2106556118.sd01.csv

Supplemental Material - pnas.2106556118.sd02.csv

Supplemental Material - pnas.2106556118.sd03.csv

Supplemental Material - pnas.2106556118.sd04.xlsx

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Created:
August 22, 2023
Modified:
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