2′-<i>O</i>-Methylation of the second transcribed nucleotide within the mRNA 5′ cap impacts the protein production level in a cell-specific manner and contributes to RNA immune evasion

Drążkowska, Karolina; Tomecki, Rafał; Warmiński, Marcin; Baran, Natalia; Cysewski, Dominik; Depaix, Anaïs; Kasprzyk, Renata; Kowalska, Joanna; Jemielity, Jacek; Sikorski, Pawel J.

doi:10.1093/nar/gkac722

Cited by 38 publications

(55 citation statements)

References 59 publications

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“…6D). Thus, the precursor ion m/z 305.086 can be predicted as a methylinosine analog with a ribosyl methylation, which commonly locates at the 2’-OH position of ribose (Ayadi et al, 2019; Drazkowska et al, 2022). The synthetic reference 1-methylinosine compound with methylation at the N1 position of the purine base was detected at a similar retention time to the predicted methylinosine analog (Fig.…”

Section: Resultsmentioning

confidence: 99%

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Metabolomics reveals nucleoside analogs for regulating mucosal-associated invariant T cell responses

Huang

Sharma

Sallans

et al. 2023

Preprint

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Although mucosal-associated invariant T (MAIT) cells recognize riboflavin-like metabolites from Gram-negative bacteria, MAIT cell stimulation by broad bacterial families and mammalian cells suggests the existence of novel ligands from different biological sources. Here we established a comparative platform of functional metabolomics and used Mycobacterium tuberculosis as a model to characterize novel metabolites for MAIT cell activation. We extracted and fractionated small metabolites of M. tuberculosis using high-performance liquid chromatography, showing a different MAIT cell stimulation pattern of M. tuberculosis metabolite fractions in comparison with Escherichia coli fractions. Mass profiling predicted multiple nucleoside analogs enriched in a biologically active fraction of M. tuberculosis. Whereas the synthetic forms of these predicted M. tuberculosis nucleosides were unavailable, structural-based autodocking of analogous nucleosides conserved in mammals supported potential binding with MR1 protein. Indeed, functional assays of these conserved nucleosides demonstrated guanosine as a stimulator and deoxyformyluridine as an inhibitor of MAIT cell activation. Identification of bioactive nucleoside metabolites broadly conserved in bacterial and mammalian systems will facilitate an understanding of the regulatory roles of MAIT cells in infectious and inflammatory conditions.

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Section: Resultsmentioning

confidence: 99%

“…6D). Thus, the precursor ion m/z 305.086 can be predicted as a methylinosine analog with a ribosyl Page11 methylation, which commonly locates at the 2'-OH position of ribose (Ayadi et al, 2019;Drazkowska et al, 2022).…”

Section: Prediction Of Methylinosine and Formyluridine Analogs Enrich...mentioning

confidence: 99%

Metabolomics reveals nucleoside analogs for regulating mucosal-associated invariant T cell responses

Huang

Sharma

Sallans

et al. 2023

Preprint

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“…32 Interestingly, the trinucleotide-based approach did not require methylation of the m 7 G ribose to prevent reverse incorporation thanks to an additional base pair between adenosine of the trinucleotide primer and thymidine at the −1 position of the template. 31 A few years ago, several trinucleotide cap analogs became commercially available as CleanCap reagents, 33 and a modified variant of a trinucleotide cap, m 2 7,3 ′ -O GpppA m pG (Figure 3B), has been used for the production of the Comirnaty vaccine. 5 Recently, we reevaluated the trinucleotide analogs of m 7 GpppA*pG and expanded this set with m 7 GpppNpG trinucleotides containing nucleobases other than adenosine (C, G, and U).…”

Section: How To Cap Rnamentioning

confidence: 99%

“…In a follow-up study, we showed that tetranucleotide cap analogs m 7 GpppA m pG m pG are also efficient IVT primers (ca. 90% capping using ϕ6.5 promoter) and provide direct access to mRNAs with cap-2 structures . We then applied a similar approach to incorporate noncanonical caps including NAD, FAD, and UDP-sugars …”

Section: How To Cap Rnamentioning

confidence: 99%

“…Although some GTP analogs are tolerated by the vaccinia enzyme as substrates for GMP transfer, the co-transcriptional capping with trinucleotides offers a more general platform for incorporating modifications. Those include natural methylations of 5′-terminal nucleotides (cap-1, cap-2, m 6 A m ), ,, noncanonical caps, synthetic modulators of translational properties, , and functional groups for molecular labeling. − …”

Section: How To Cap Rnamentioning

confidence: 99%

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Chemical Modifications of mRNA Ends for Therapeutic Applications

Warminski,

Mamot,

Depaix

et al. 2023

Acc. Chem. Res.

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Metrics & MoreArticle Recommendations CONSPECTUS: Messenger ribonucleic acid (mRNA) is the universal cellular instruction for ribosomes to produce proteins. Proteins are responsible for most of the functions of living organisms, and their abnormal structure or activity is the cause of many diseases. mRNA, which is expressed in the cytoplasm and, unlike DNA, does not need to be delivered into the nucleus, appears to be an ideal vehicle for pursuing the idea of gene therapy in which genetic information about proteins is introduced into an organism to exert a therapeutic effect. mRNA molecules of any sequence can be synthesized using the same set of reagents in a cell-free system via a process called in vitro transcription (IVT), which is very convenient for therapeutic applications. However, this does not mean that the path from the idea to the first mRNA-based therapeutic was short and easy. It took 30 years of trial and error in the search for solutions that eventually led to the first mRNA vaccines created in record time during the SARS-CoV-2 pandemic. One of the fundamental problems in the development of RNA-based therapeutics is the legendary instability of mRNA, due to the transient nature of this macromolecule. From the chemical point of view, mRNA is a linear biopolymer composed of four types of ribonucleic subunits ranging in length from a few hundred to hundreds of thousands of nucleotides, with unique structures at its ends: a 5′-cap at the 5′-end and a poly(A) tail at the 3′-end. Both are extremely important for the regulation of translation and mRNA durability. These elements are also convenient sites for sequence-independent labeling of mRNA to create probes for enzymatic assays and tracking of the fate of mRNA in cells and living organisms. Synthetic 5′-cap analogs have played an important role in the studies of mRNA metabolism, and some of them have also been shown to significantly improve the translational properties of mRNA or affect mRNA stability and reactogenicity. The most effective of these is used in clinical trials of mRNA-based anticancer vaccines. Interestingly, thanks to the knowledge gained from the biophysical studies of cap-related processes, even relatively large modifications such as fluorescent tags can be attached to the cap structure without significant effects on the biological properties of the mRNA, if properly designed cap analogs are used. This has been exploited in the development of molecular tools (fluorescently labeled mRNAs) to track these macromolecules in complex biological systems, including organisms. These tools are extremely valuable for better understanding of the cellular mechanisms involved in mRNA metabolism but also for designing therapeutic mRNAs with superior properties. Much less is known about the usefulness/utility of poly(A) tail modifications in the therapeutic context, but it is clear that chemical modifications of poly(A) can also affect biochemical properties of mRNA. This Account is devoted to chemical modifications of both the 5′-and 3′-ends of mR...

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ACE mRNA (Additional Chimeric Element incorporated IVT mRNA) for Enhancing Protein Expression by Modulating Immunogenicity

Son,

Park,

Kim

et al. 2024

Advanced Science

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The development of in vitro transcribed mRNA (IVT mRNA)‐based therapeutics/vaccines depends on the management of IVT mRNA immunogenicity. IVT mRNA, which is used for intracellular protein translation, often triggers unwanted immune responses, interfering with protein expression and leading to reduced therapeutic efficacy. Currently, the predominant approach for mitigating immune responses involves the incorporation of costly chemically modified nucleotides like pseudouridine (Ψ) or N1‐methylpseudouridine (m1Ψ) into IVT mRNA, raising concerns about expense and the potential misincorporation of amino acids into chemically modified codon sequences. Here, an Additional Chimeric Element incorporated mRNA (ACE mRNA), a novel approach incorporating two segments within a single IVT mRNA structure, is introduced. The first segment retains conventional IVT mRNA components prepared with unmodified nucleotides, while the second, comprised of RNA/DNA chimeric elements, aims to modulate immunogenicity. Notably, ACE mRNA demonstrates a noteworthy reduction in immunogenicity of unmodified IVT mRNA, concurrently demonstrating enhanced protein expression efficiency. The reduced immune responses are based on the ability of RNA/DNA chimeric elements to restrict retinoic acid‐inducible gene I (RIG‐I) and stimulator of interferon genes (STING)‐mediated immune activation. The developed ACE mRNA shows great potential in modulating the immunogenicity of IVT mRNA without the need for chemically modified nucleotides, thereby advancing the safety and efficacy of mRNA‐based therapeutics/vaccines.

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2′-O-Methylation of the second transcribed nucleotide within the mRNA 5′ cap impacts the protein production level in a cell-specific manner and contributes to RNA immune evasion

Cited by 38 publications

References 59 publications

Metabolomics reveals nucleoside analogs for regulating mucosal-associated invariant T cell responses

Metabolomics reveals nucleoside analogs for regulating mucosal-associated invariant T cell responses

Chemical Modifications of mRNA Ends for Therapeutic Applications

ACE mRNA (Additional Chimeric Element incorporated IVT mRNA) for Enhancing Protein Expression by Modulating Immunogenicity

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