Your search keyword '"Ayyub SA"' showing total 11 results

1. Interferon-Stimulated Genes that Target Retrovirus Translation.

Author

Jäger N, Pöhlmann S, Rodnina MV, and Ayyub SA

Subjects

Humans, Immunity, Innate, Animals, Signal Transduction, Retroviridae Infections virology, Retroviridae Infections immunology, Retroviridae Infections genetics, Interferons immunology, Interferons metabolism, Interferons genetics, Retroviridae genetics, Retroviridae physiology, Protein Biosynthesis

Abstract

The innate immune system, particularly the interferon (IFN) system, constitutes the initial line of defense against viral infections. IFN signaling induces the expression of interferon-stimulated genes (ISGs), and their products frequently restrict viral infection. Retroviruses like the human immunodeficiency viruses and the human T-lymphotropic viruses cause severe human diseases and are targeted by ISG-encoded proteins. Here, we discuss ISGs that inhibit the translation of retroviral mRNAs and thereby retrovirus propagation. The Schlafen proteins degrade cellular tRNAs and rRNAs needed for translation. Zinc Finger Antiviral Protein and RNA-activated protein kinase inhibit translation initiation factors, and Shiftless suppresses translation recoding essential for the expression of retroviral enzymes. We outline common mechanisms that underlie the antiviral activity of multifunctional ISGs and discuss potential antiretroviral therapeutic approaches based on the mode of action of these ISGs.

Published

2024

2. The Inhibition of Gag-Pol Expression by the Restriction Factor Shiftless Is Dispensable for the Restriction of HIV-1 Infection.

Author

Jäger N, Ayyub SA, Peske F, Liedtke D, Bohne J, Hoffmann M, Rodnina MV, and Pöhlmann S

Subjects

Humans, Frameshifting, Ribosomal, Gene Expression Regulation, Viral, HEK293 Cells, Leukemia Virus, Murine genetics, Leukemia Virus, Murine physiology, Virus Replication, Fusion Proteins, gag-pol genetics, Fusion Proteins, gag-pol metabolism, HIV Infections virology, HIV Infections genetics, HIV Infections metabolism, HIV-1 genetics, HIV-1 physiology, RNA-Binding Proteins metabolism

Abstract

The interferon-induced host cell protein Shiftless (SFL) inhibits -1 programmed ribosomal frameshifting (-1PRF) required for the expression of HIV-1 Gal-Pol and the formation of infectious HIV-1 particles. However, the specific regions in SFL required for antiviral activity and the mechanism by which SFL inhibits -1PRF remain unclear. Employing alanine scanning mutagenesis, we found that basic amino acids in the predicted zinc ribbon motif of SFL are essential for the suppression of Gag-Pol expression but dispensable for anti-HIV-1 activity. We have shown that SFL inhibits the expression of the murine leukemia virus (MLV) Gag-Pol polyprotein and the formation of infectious MLV particles, although Gag-Pol expression of MLV is independent of -1PRF but requires readthrough of a stop codon. These findings indicate that SFL might inhibit HIV-1 infection by more than one mechanism and that SFL might target programmed translational readthrough as well as -1PRF signals, both of which are regulated by mRNA secondary structure elements.

Published

2024

3. The initiation factor 3 (IF3) residues interacting with initiator tRNA elbow modulate the fidelity of translation initiation and growth fitness in Escherichia coli.

Author

Singh J, Mishra RK, Ayyub SA, Hussain T, and Varshney U

Subjects

Elbow, Peptide Initiation Factors metabolism, Prokaryotic Initiation Factor-3 metabolism, Escherichia coli metabolism, RNA, Transfer, Met genetics, RNA, Transfer, Met metabolism, Escherichia coli Proteins

Abstract

Initiation factor 3 (IF3) regulates the fidelity of bacterial translation initiation by debarring the use of non-canonical start codons or non-initiator tRNAs and prevents premature docking of the 50S ribosomal subunit to the 30S pre-initiation complex (PIC). The C-terminal domain (CTD) of IF3 can carry out most of the known functions of IF3 and sustain Escherichia coli growth. However, the roles of the N-terminal domain (NTD) have remained unclear. We hypothesized that the interaction between NTD and initiator tRNAfMet (i-tRNA) is essential to coordinate the movement of the two domains during the initiation pathway to ensure fidelity of the process. Here, using atomistic molecular dynamics (MD) simulation, we show that R25A/Q33A/R66A mutations do not impact NTD structure but disrupt its interaction with i-tRNA. These NTD residues modulate the fidelity of translation initiation and are crucial for bacterial growth. Our observations also implicate the role of these interactions in the subunit dissociation activity of CTD of IF3. Overall, the study shows that the interactions between NTD of IF3 and i-tRNA are crucial for coupling the movements of NTD and CTD of IF3 during the initiation pathway and in imparting growth fitness to E. coli., (© The Author(s) 2022. Published by Oxford University Press on behalf of Nucleic Acids Research.)

Published

2022

4. Mutagenic Analysis of the HIV Restriction Factor Shiftless.

Author

Jäger N, Ayyub SA, Korniy N, Peske F, Hoffmann M, Rodnina MV, and Pöhlmann S

Subjects

Amino Acids, Antiviral Agents, Humans, Mutagens, RNA, HIV Infections

Abstract

The interferon-induced host cell protein shiftless (SFL) was reported to inhibit human immunodeficiency virus (HIV) infection by blocking the -1 programmed ribosomal frameshifting (-1PRF) required for expression of the Gag-Pol polyprotein. However, it is not clear how SFL inhibits -1PRF. To address this question, we focused on a 36 amino acids comprising region (termed required for antiviral activity (RAA)) that is essential for suppression of -1PRF and HIV infection and is missing from SFL short (SFLS), a splice variant of SFL with unknown function. Here, we confirm that SFL, but not SFLS, inhibits HIV -1PRF and show that inhibition is cell-type-independent. Mutagenic and biochemical analyses demonstrated that the RAA region is required for SFL self-interactions and confirmed that it is necessary for ribosome association and binding to the HIV RNA. Analysis of SFL mutants with six consecutive amino-acids-comprising deletions in the RAA region suggests effects on binding to the HIV RNA, complete inhibition of -1PRF, inhibition of Gag-Pol expression, and antiviral activity. In contrast, these amino acids did not affect SFL expression and were partially dispensable for SFL self-interactions and binding to the ribosome. Collectively, our results support the notion that SFL binds to the ribosome and the HIV RNA in order to block -1PRF and HIV infection, and suggest that the multimerization of SFL may be functionally important.

Published

2022

5. Translation initiation in mammalian mitochondria- a prokaryotic perspective.

Author

Ayyub SA and Varshney U

Subjects

Animals, Disease Susceptibility, Humans, Mammals metabolism, Mitochondria metabolism, Mitochondrial Diseases genetics, Mitochondrial Diseases metabolism, Mitochondrial Ribosomes chemistry, Mitochondrial Ribosomes metabolism, Models, Molecular, Prokaryotic Cells metabolism, Protein Biosynthesis, RNA, Messenger genetics, RNA, Transfer genetics, Ribosomes chemistry, Ribosomes metabolism, Structure-Activity Relationship, Mammals genetics, Mitochondria genetics, Peptide Chain Initiation, Translational

Abstract

ATP is generated in mitochondria of eukaryotic cells by oxidative phosphorylation (OXPHOS). The OXPHOS complex, which is crucial for cellular metabolism, comprises of both nuclear and mitochondrially encoded subunits. Also, the occurrence of several pathologies because of mutations in the mitochondrial translation apparatus indicates the importance of mitochondrial translation and its regulation. The mitochondrial translation apparatus is similar to its prokaryotic counterpart due to a common origin of evolution. However, mitochondrial translation has diverged from prokaryotic translation in many ways by reductive evolution. In this review, we focus on mammalian mitochondrial translation initiation, a highly regulated step of translation, and present a comparison with prokaryotic translation.

Published

2020

6. Rescuing stalled mammalian mitoribosomes - what can we learn from bacteria?

Author

Ayyub SA, Gao F, Lightowlers RN, and Chrzanowska-Lightowlers ZM

Subjects

Animals, Bacteria metabolism, Mitochondrial Ribosomes metabolism

Abstract

In the canonical process of translation, newly completed proteins escape from the ribosome following cleavage of the ester bond that anchors the polypeptide to the P-site tRNA, after which the ribosome can be recycled to initiate a new round of translation. Not all protein synthesis runs to completion as various factors can impede the progression of ribosomes. Rescuing of stalled ribosomes in mammalian mitochondria, however, does not share the same mechanisms that many bacteria use. The classic method for rescuing bacterial ribosomes is trans -translation. The key components of this system are absent from mammalian mitochondria; however, four members of a translation termination factor family are present, with some evidence of homology to members of a bacterial back-up rescue system. To date, there is no definitive demonstration of any other member of this family functioning in mitoribosome rescue. Here, we provide an overview of the processes and key players of canonical translation termination in both bacteria and mammalian mitochondria, followed by a perspective of the bacterial systems used to rescue stalled ribosomes. We highlight any similarities or differences with the mitochondrial translation release factors, and suggest potential roles for these proteins in ribosome rescue in mammalian mitochondria., Competing Interests: Competing interestsThe authors declare no competing or financial interests., (© 2020. Published by The Company of Biologists Ltd.)

Published

2020

7. Sustenance of Escherichia coli on a single tRNAMet.

Author

Govindan A, Ayyub SA, and Varshney U

Subjects

Base Pairing, Escherichia coli growth & development, Escherichia coli Proteins genetics, Peptide Chain Initiation, Translational, Peptide Elongation Factor Tu genetics, Prokaryotic Initiation Factor-2 genetics, Escherichia coli genetics, Mutation, RNA, Transfer, Met

Abstract

Living organisms possess two types of tRNAs for methionine. Initiator tRNAs bind directly into the ribosomal P-site to initiate protein synthesis, and the elongators bind to the A-site during the elongation step. Eubacterial initiators (tRNAfMet) are unique in that the methionine attached to them is formylated to facilitate their binding to initiation factor 2 (IF2), and to preclude them from binding to elongation factor Tu (EFTu). However, in mammalian mitochondria, protein synthesis proceeds with a single dual function tRNAMet. Escherichia coli possesses four tRNAfMet (initiator) and two tRNAMet (elongator) genes. Free-living organisms possessing the mitochondrion like system of single tRNAMet are unknown. We characterized mutants of E. coli tRNAfMet that function both as initiators and elongators. We show that some of the tRNAfMet mutants sustain E. coli lacking all four tRNAfMet and both tRNAMet genes, providing a basis for natural occurrence of mitochondria like situation in free living organisms. The tRNA mutants show in vivo binding to both IF2 and EFTu, indicating how they carry out these otherwise mutually exclusive functions by precise regulation of their in vivo formylation. Our results provide insights into how distinct initiator and elongator methionine tRNAs might have evolved from a single 'dual function' tRNA.

Published

2018

8. Antimicrobial activity of fusidic acid in Escherichia coli is dependent on the relative levels of ribosome recycling factor and elongation factor G.

Author

Ayyub SA, Lahry K, Dobriyal D, Mondal S, and Varshney U

Subjects

Escherichia coli drug effects, Escherichia coli genetics, Escherichia coli Proteins genetics, Peptide Elongation Factor G genetics, Ribosomal Proteins genetics, Ribosomes genetics, Ribosomes metabolism, Anti-Bacterial Agents pharmacology, Escherichia coli metabolism, Escherichia coli Proteins metabolism, Fusidic Acid pharmacology, Peptide Elongation Factor G metabolism, Ribosomal Proteins metabolism, Ribosomes drug effects

Abstract

During protein synthesis, elongation factor G (EFG) participates at the steps of translocation and ribosome recycling. Fusidic acid (FA) is a bacteriostatic antibiotic, which traps EFG on ribosomes, stalling them on mRNAs. How the bacterial susceptibility to FA is determined, and which of the two functions of EFG (translocation or ribosome recycling) is more vulnerable, has remained debatable. The in vivo studies addressing these aspects of FA mediated inhibition of protein synthesis are lacking. Here, we used a system of Escherichia coli strains and their complementation/supplementation with the plasmid borne copies of the inducible versions of EFG and ribosome recycling factor (RRF) genes. Additionally, we investigated FA sensitivity in a strain with increased proportion of stalled ribosomes. We show that the cells with high EFG/RRF (or low RRF/EFG) ratios are more susceptible to FA than those with low EFG/RRF (or high RRF/EFG) ratios. Our in vivo observations are consistent with the recent in vitro reports of dependence of FA susceptibility on EFG/RRF ratios, and the notion that an overriding target of FA is the translocation function of EFG. An applied outcome of our in vivo study is that FA mediated growth inhibition could be facilitated by depletion or inactivation of cellular RRF.

Published

2018

9. Fidelity of translation in the presence of mammalian mitochondrial initiation factor 3.

Author

Ayyub SA, S L A, Dobriyal D, Aluri S, Spremulli LL, and Varshney U

Subjects

Codon, Initiator, Humans, Mitochondrial Proteins genetics, Prokaryotic Initiation Factor-3 genetics, RNA, Transfer metabolism, Recombinant Proteins genetics, Recombinant Proteins metabolism, Escherichia coli enzymology, Escherichia coli metabolism, Mitochondrial Proteins metabolism, Peptide Chain Initiation, Translational, Prokaryotic Initiation Factor-3 metabolism

Abstract

Initiation factor 3 (IF3) is a conserved translation factor. Mutations in mitochondrial IF3 (IF3 mt ) have been implicated in disease pathology. Escherichia coli infCΔ55, compromised for IF3 activity, has provided an excellent heterologous system for IF3 mt structure-function analysis. IF3 mt allowed promiscuous initiation from AUA, AUU and ACG codons but avoided initiation with initiator tRNAs lacking the conserved 3GC pairs in their anticodon stems. Expression of IF3 mt N-terminal domain, or IF3 mt devoid of its typical N-, and C-terminal extensions improved fidelity of initiation in E. coli. The observations suggest that the IF3 mt terminal extensions relax the fidelity of translational initiation in mitochondria., (Copyright © 2017 Elsevier B.V. and Mitochondria Research Society. All rights reserved.)

Published

2018

10. Coevolution of the translational machinery optimizes initiation with unusual initiator tRNAs and initiation codons in mycoplasmas.

Author

Ayyub SA, Dobriyal D, Shah RA, Lahry K, Bhattacharyya M, Bhattacharyya S, Chakrabarti S, and Varshney U

Subjects

Anticodon genetics, Codon, Initiator genetics, Escherichia coli genetics, Humans, Mycoplasma pathogenicity, Nucleic Acid Conformation, RNA, Ribosomal, 16S genetics, RNA, Transfer, Met genetics, Ribosomal Proteins genetics, Evolution, Molecular, Mycoplasma genetics, Protein Biosynthesis, RNA, Transfer genetics

Abstract

Initiator tRNAs (i-tRNAs) are characterized by the presence of three consecutive GC base pairs (GC/GC/GC) in their anticodon stems in all domains of life. However, many mycoplasmas possess unconventional i-tRNAs wherein the highly conserved sequence of GC/GC/GC is represented by AU/GC/GC, GC/GC/GU or AU/GC/GU. These mycoplasmas also tend to preferentially utilize non-AUG initiation codons. To investigate if initiation with the unconventional i-tRNAs and non-AUG codons in mycoplasmas correlated with the changes in the other components of the translation machinery, we carried out multiple sequence alignments of genes encoding initiation factors (IF), 16S rRNAs, and the ribosomal proteins such as uS9, uS12 and uS13. In addition, the occurrence of Shine-Dalgarno sequences in mRNAs was analyzed. We observed that in the mycoplasmas harboring AU/GC/GU i-tRNAs, a highly conserved position of R131 in IF3, is represented by P, F or Y and, the conserved C-terminal tail (SKR) of uS9 is represented by the TKR sequence. Using the Escherichia coli model, we show that the change of R131 in IF3 optimizes initiation with the AU/GC/GU i-tRNAs. Also, the SKR to TKR change in uS9 was compatible with the R131P variation in IF3 for initiation with the AU/GC/GU i-tRNA variant. Interestingly, the mycoplasmas harboring AU/GC/GU i-tRNAs are also human pathogens. We propose that these mycoplasmas might have evolved a relaxed translational apparatus to adapt to the environment they encounter in the host.

Published

2018

11. Contributions of the N- and C-Terminal Domains of Initiation Factor 3 to Its Functions in the Fidelity of Initiation and Antiassociation of the Ribosomal Subunits.

Author

Ayyub SA, Dobriyal D, and Varshney U

Subjects

Codon, Initiator genetics, Codon, Initiator metabolism, Escherichia coli chemistry, Escherichia coli genetics, Escherichia coli growth & development, Escherichia coli Proteins genetics, Protein Domains, Ribosome Subunits genetics, Escherichia coli metabolism, Escherichia coli Proteins chemistry, Escherichia coli Proteins metabolism, Peptide Chain Initiation, Translational, Prokaryotic Initiation Factor-3 chemistry, Prokaryotic Initiation Factor-3 metabolism, Ribosome Subunits metabolism

Abstract

Initiation factor 3 (IF3) is one of the three conserved prokaryotic translation initiation factors essential for protein synthesis and cellular survival. Bacterial IF3 is composed of a conserved architecture of globular N- and C-terminal domains (NTD and CTD) joined by a linker region. IF3 is a ribosome antiassociation factor which also modulates selection of start codon and initiator tRNA. All the functions of IF3 have been attributed to its CTD by in vitro studies. However, the in vivo relevance of these findings has not been investigated. By generating complete and partial IF3 ( infC ) knockouts in Escherichia coli and by complementation analyses using various deletion constructs, we show that while the CTD is essential for E. coli survival, the NTD is not. Polysome profiles reaffirm that CTD alone can bind to the 30S ribosomal subunit and carry out the ribosome antiassociation function. Importantly, in the absence of the NTD, bacterial growth is compromised, indicating a role for the NTD in the fitness of cellular growth. Using reporter assays for in vivo initiation, we show that the NTD plays a crucial role in the fidelity function of IF3 by avoiding (i) initiation from non-AUG codons and (ii) initiation by initiator tRNAs lacking the three highly conserved consecutive GC pairs (in the anticodon stem) known to function in concert with IF3. IMPORTANCE Initiation factor 3 regulates the fidelity of eubacterial translation initiation by ensuring the formation of an initiation complex with an mRNA bearing a canonical start codon and with an initiator tRNA at the ribosomal P site. Additionally, IF3 prevents premature association of the 50S ribosomal subunit with the 30S preinitiation complex. The significance of our work in Escherichia coli is in demonstrating that while the C-terminal domain alone sustains E. coli for its growth, the N-terminal domain adds to the fidelity of initiation of protein synthesis and to the fitness of the bacterial growth., (Copyright © 2017 American Society for Microbiology.)

Published

2017