Alterations in ribosomal protein L19 that decrease the fidelity of translation

VanNice, John; Gregory, Steven T.; Kamath, Divya; O’Connor, Michael B.

doi:10.1016/j.biochi.2016.07.015

“…The phosphorylation of ribosomal proteins can reduce up to 50% of their activity ( Mikulík et al, 2001 ), although it seems that phosphorylated L19 is the active form of the protein that contribute to the assembly and decoding processes ( Soung et al, 2009 ). Moreover, a mutagenic study of the rplS gene in E. coli revealed that, despite the restraint in translation, the defective mutants did not exhibit problems in 30S–50S association or cell growth ( VanNice et al, 2016 ). There is no record of L19 protein as a drug target in the DrugBank database.…”

Section: Resultsmentioning

confidence: 99%

In silico Prediction of New Drug Candidates Against the Multidrug-Resistant and Potentially Zoonotic Fish Pathogen Serotype III Streptococcus agalactiae

Favero

¹

,

Chideroli

²

,

Ferrari

³

et al. 2020

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Streptococcus agalactiae is an invasive multi-host pathogen that causes invasive diseases mainly in newborns, elderly, and individuals with underlying health complications. In fish, S. agalactiae causes streptococcosis, which is characterized by septicemia and neurological signs, and leads to great economic losses to the fish farming industry worldwide. These bacteria can be classified into different serotypes based on capsular antigens, and into different sequence types (ST) based on multilocus sequence typing (MLST). In 2015, serotype III ST283 was identified to be associated with a foodborne invasive disease in non-pregnant immunocompetent humans in Singapore, and the infection was related to raw fish consumption. In addition, a serotype III strain isolated from tilapia in Brazil has been reported to be resistant to five antibiotic classes. This specific serotype can serve as a reservoir of resistance genes and pose a serious threat to public health. Thus, new approaches for the control and treatment of S. agalactiae infections are needed. In the present study, 24 S. agalactiae serotype III complete genomes, isolated from human and fish hosts, were compared. The core genome was identified, and, using bioinformatics tools and subtractive criteria, five proteins were identified as potential drug targets. Furthermore, 5,008 drug-like natural compounds were virtually screened against the identified targets. The ligands with the best binding properties are suggested for further in vitro and in vivo analysis.

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“…Examples of genes that formed GIs with ITT1 and RPS1A are large ribosomal subunit protein 19A ( RPL19A ) and general control non-derepressible ( GCN3 ), respectively. Rpl19p is a conserved large ribosomal subunit protein involved in ribosomal intersubunit bridging and its alteration is connected to the fidelity of translation [ 54 ], [ 55 ]. On the other hand, GCN3 is the alpha subunit of translation initiation factor 2B (eIF2B), which is involved in guanine-nucleotide exchange for eIF2.…”

Section: Resultsmentioning

confidence: 99%

Heavy metal sensitivities of gene deletion strains for ITT1 and RPS1A connect their activities to the expression of URE2, a key gene involved in metal detoxification in yeast

Moteshareie

¹

,

Hajikarimlou

²

,

Indrayanti

³

et al. 2018

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Heavy metal and metalloid contaminations are among the most concerning types of pollutant in the environment. Consequently, it is important to investigate the molecular mechanisms of cellular responses and detoxification pathways for these compounds in living organisms. To date, a number of genes have been linked to the detoxification process. The expression of these genes can be controlled at both transcriptional and translational levels. In baker’s yeast, Saccharomyces cerevisiae, resistance to a wide range of toxic metals is regulated by glutathione S-transferases. Yeast URE2 encodes for a protein that has glutathione peroxidase activity and is homologous to mammalian glutathione S-transferases. The URE2 expression is critical to cell survival under heavy metal stress. Here, we report on the finding of two genes, ITT1, an inhibitor of translation termination, and RPS1A, a small ribosomal protein, that when deleted yeast cells exhibit similar metal sensitivity phenotypes to gene deletion strain for URE2. Neither of these genes were previously linked to metal toxicity. Our gene expression analysis illustrates that these two genes affect URE2 mRNA expression at the level of translation.

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“…Examples of genes that formed GIs with ITT1 and RPS1A are large ribosomal subunit protein 19A (RPL19A) and general control non-derepressible (GCN3), respectively. Rpl19p is a conserved large ribosomal subunit protein involved in ribosomal intersubunit bridging and its alteration is connected to the fidelity of translation [54], [55]. On the .…”

Section: Genetic Interaction Analysis Further Connects the Activity Omentioning

confidence: 99%

Heavy metal sensitivities of gene deletion strains forITT1andRPS1Aconnect their activities to the expression ofURE2, a key gene involved in metal detoxification in yeast

Moteshareie

¹

,

Hajikarimlou

²

,

Indrayanti

³

et al. 2018

Preprint

2

0

View full text Add to dashboard Cite

Heavy metal and metalloid contaminations are among the most concerning types of pollutant in the environment. Consequently, it is important to investigate the molecular mechanisms of cellular responses and detoxification pathways for these compounds in living organisms. To date, a number of genes have been linked to the detoxification process. The expression of these genes can be controlled at both transcriptional and translational levels. In baker’s yeast, Saccharomyces cerevisiae, resistance to a wide range of toxic metals is regulated by glutathione S-transferases. Yeast URE2 encodes for a protein that has glutathione peroxidase activity and is homologous to mammalian glutathione S-transferases. The URE2 expression is critical to cell survival under heavy metal stress. Here, we report on the finding of two genes, ITT1, an inhibitor of translation termination, and RPS1A, a small ribosomal protein, that when deleted yeast cells exhibit similar metal sensitivity phenotypes to gene deletion strain for URE2. Neither of these genes were previously linked to metal toxicity. Our gene expression analysis illustrates that these two genes affect URE2 mRNA expression at the level of translation.Summary statementWe identified two yeast genes, ITT1 and RPS1A, that when deleted, results in yeast cells sensitivity to heavy metals and metalloids. Further investigation indicated that they influence the expression of URE2 gene, a key player in metal detoxification, by upregulating its translation. Our findings suggest that ITT1 and RPS1A play an indirect role in responding to toxic metal stress.

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Alterations in ribosomal protein L19 that decrease the fidelity of translation

Cited by 8 publications

References 28 publications

In silico Prediction of New Drug Candidates Against the Multidrug-Resistant and Potentially Zoonotic Fish Pathogen Serotype III Streptococcus agalactiae

In silico Prediction of New Drug Candidates Against the Multidrug-Resistant and Potentially Zoonotic Fish Pathogen Serotype III Streptococcus agalactiae

Heavy metal sensitivities of gene deletion strains for ITT1 and RPS1A connect their activities to the expression of URE2, a key gene involved in metal detoxification in yeast

Heavy metal sensitivities of gene deletion strains forITT1andRPS1Aconnect their activities to the expression ofURE2, a key gene involved in metal detoxification in yeast

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