[30], see also Fig 2B). Inhibiting about 20% of all EF-Tu molecules is already sufficient to cause an almost complete suppression of protein synthesis. The study reveals a strong interdependency of a protein synthesis system's composition and its susceptibility to inhibition. See Table 1 for more details on the different inhibition pathways. Proc Natl Acad Sci U S A 83:61646168, CrossRef (1). View your signed in personal account and access account management features. for the EF-Tu threshold concentration of E. coli which corresponds to about 80% of the physiological EF-Tu concentration and is in excellent agreement with the in-vivo EF-Tu threshold concentration predicted by our computational in-vivo-like translation system, see Fig 2A). J Postgrad Med 59:127130, CrossRef If you cannot sign in, please contact your librarian. PubMed A further optimization of the compound 6 and 7's structure led to the synthesis of . Anyone you share the following link with will be able to read this content: Sorry, a shareable link is not currently available for this article. Among the various classes of compounds that impair translation there are . This chapter covers the many different ways that antimicrobial agents can interfere with the synthesis of bacterial cell proteins. Therefore, it is not obvious under which conditions which of the three inhibition pathways depicted in Fig 1 is the most efficient one, i.e., under which conditions EF-Tu is a more suitable target than the ribosome for down-regulation of bacterial protein synthesis. A) Growth rates and EF-Tu concentrations from van der Meide et al. A toxin-antitoxin system consists of two components, a growth-inhibiting toxin and an antagonistic antitoxin. B) Concentrations of free, aminoacylated (charged) tRNAs and free, de-aminoacylated (uncharged) tRNAs of species 1 and 2, same parameters and corresponding color code as in A). In the low-concentration regime , the free ternary complex concentration of the more abundant species 1 increases roughly linearly with whereas the concentration of the less abundant species 2 remains practically zero up to . 19.79. The interaction of the -coronavirus severe acute respiratory syndrome coronavirus-2 (SARS-CoV-2) nucleocapsid (N) protein with genomic RNA is initiated by specific RNA regions and subsequently induces the formation of a continuous polymer with characteristic structural units for viral formation.We hypothesized that oligomeric RNAs, whose sequences are absent in the 29.9-kb genome . When the concentrations of ribosomes and EF-Tu molecules are inhibited simultaneously by the same absolute amounts (diamonds, [EF-Tu] = [ribosomes]), EF-Tu inhibition has a stronger influence on peptide synthesis than ribosome inhibition (A, B) unless the tRNA concentrations are comparable (C, D). It usually refers to substances, such as antimicrobial drugs, that act at the ribosome level. However, these speculative assumptions about mitochondrial protein synthesis need to be confirmed by quantitative analyses, which require the development of specialized translation models. (2022). Background biochemistry information on translation is provided. A protein synthesis inhibitor is a substance that stops or slows the growth or proliferation of cells by disrupting the processes that lead directly to the generation of new proteins. Proc Natl Acad Sci U S A 77:39743977, Burdett V (1991) Purification and characterization of Tet(M), a protein that renders ribosomes resistant to tetracycline. J Antimicrob Chemother 70:26812692. In the simulation, we varied the initial concentration of EF-Tu from 0 to 5 M and determined for each EF-Tu concentration the rate of tripeptide synthesis at the end of the simulation after 1000 s when the simulated PURE system has long reached a quasi-steady state peptide synthesis rate. Regulation and maintenance of protein synthesis are vital to all organisms and are thus key targets of attack and defense at the cellular level. (Eds.),Eds. In: Brunton LL, Dandan RH, Knollmann BC (eds) Goodman & Gilmans the pharmacological basis of therapeutics, 13th edn. In: Paul, A., Anandabaskar, N., Mathaiyan, J., Raj, G.M. When 20% of all EF-Tu molecules are inhibited (red dashed line), a critical EF-Tu concentration is reached, at which protein synthesis is almost completely suppressed. For example, if the concentration of ternary complexes containing EF-Tu and Lys-tRNALys was decreased by a certain amount, the concentration of Lys-tRNALys was increased by the same amount. In S1 Text, all details on the system of equations describing the 1C-1T model can be found. Symbols represent different E. coli strains with mutated tufA and/or tufB genes coding for EF-Tu, see Table 2 in Ref. Some societies use Oxford Academic personal accounts to provide access to their members. Codons 1 and 2 appear with normalized codon usages p1 and p2, respectively, with p1 + p2 = 1. The simplest translation system consists of one codon and one tRNA that is cognate to the codon. https://doi.org/10.1093/cid/civ501, CrossRef PubMed If the EF-Tu concentration is reduced by 15% (orange dashed line), the overall elongation rate strongly decreases by about 50%. Chemistry of Antibiotics and Related Drugs pp 149177Cite as. The ultrasensitive dependence of protein synthesis on EF-Tu might also be related to an observation made by krti et al. We conclude that a 1C-1T translation system is not ultrasensitive to the abundance of EF-Tu. B) Concentrations of free EF-Tu molecules (solid lines), free ternary complexes of the more abundant species 1 (dotted lines) and of the less abundant species 2 (dashed lines) as determined by the set of Eqs. Protein Synthesis Inhibitors. A) Overall elongation rate and B) concentrations of free EF-Tu molecules (solid lines), free ternary complexes of the more abundant species 1 (dotted lines) and of the less abundant species 2 (dashed lines) as a function of the concentration of EF-Tu. J Antimicrob Chemother 43:579582, Yanagisawa T, Lee JT, Wu HC, Kawakami M (1994) Relationship of protein structure of isoleucyl-tRNA synthetase with pseudomonic acid resistance of Escherichia coli. McGraw-Hill, New York, pp 10391047, Mac Dougall C (2018b) Protein synthesis inhibitors and miscellaneous antibacterial agents. J Mol Biol 416:571578, Fernandes P, Pereira D (2011) Efforts to support the development of fusidic acid in the United States. The first period covers the years 1951-1960 and the second from 1961 until 1973. PubMed The ribosome has three sites: the A site, the P site, and the E site (not shown in ). Ann N Y Acad Sci 1241:7181I, Bulkley D, Johnson F, Steitz TA (2012) The antibiotic thermorubin inhibits protein synthesis by binding to inter-subunit bridge B2a of the ribosome. Fig 3A) shows that the position of the transition regime from strongly suppressed to physiological protein synthesis is shifted towards higher concentrations of EF-Tu for stronger mismatches of tRNA concentrations and codon usages. Theory and Bio-Systems, Max Planck Institute of Colloids and Interfaces, Potsdam, Germany. PubMed Overview. PubMed Pharmaceutics 13:2085. https://doi.org/10.3390/pharmaceutics13122085, Speer BS, Shoemaker NB, Salyers AA (1992) Bacterial resistance to tetracycline: mechanisms, transfer, and clinical significance. The corresponding EF-Tu threshold concentration can be obtained from an unexpectedly simple expression, see Eq (1). Instead, in E. coli only 20% of all EF-Tu molecules need to get phosphorylated by Doc to essentially stop protein production, which explains why Doc is an efficient toxin despite the extremely high cellular abundance of its target. found that the sensitivities of tRNA charging levels and of translation rates to amino acid starvation depend on codon usages and tRNA concentrations, which is in line with the findings presented here. It furthers the University's objective of excellence in research, scholarship, and education by publishing worldwide, This PDF is available to Subscribers Only. https://doi.org/10.1007/978-3-031-07582-7_6, DOI: https://doi.org/10.1007/978-3-031-07582-7_6, eBook Packages: Chemistry and Materials ScienceChemistry and Material Science (R0). For the one-codon-one-tRNA (1C-1T) translation system (solid blue line), the overall elongation rate is proportional to the abundance of EF-Tu for low EF-Tu concentrations. PubMed Central This tissue-specificity might be related to differential mitochondrial mRNA and tRNA expression giving rise to differences in the mitochondrial tRNA/codon composition of the various tissues: Protein synthesis in mitochondria with less balanced tRNA/codon compositions should be more susceptible to a decrease in the availability of functional mt-EF-Tu. For full functionality of this site, please enable JavaScript. B) Experimental data from van der Meide (Fig. Name Protein Synthesis Inhibitors Accession Number DBCAT000501 Description Compounds which inhibit the synthesis of proteins. CAS We predict and analyze the response of differently composed protein synthesis systems to the inhibition of elongation factor EF-Tu and/or ribosomes. Cell growth can be easily regained as soon as the antitoxin Phd inhibits Doc as only relatively few EF-Tu molecules need to be reactivated by dephosphorylation. A major fraction of antibiotics that interfere with protein synthesis is directed against the ribosome [3, 4], whereas a minor fraction is directed against EF-Tu [5]. Readers must therefore always check the product information and clinical procedures with the most up to date published product information and data sheets
The corresponding tRNAs 1 and 2 have molar concentrations X1 and X2, respectively. The institutional subscription may not cover the content that you are trying to access. The study reveals a strong interdependency of a protein synthesis systems composition and its susceptibility to inhibition. The Investigators hypothesize that upregulation of skeletal muscle NO-cGMP mediated responses through phosphodiesterase (PDE) inhibition by sildenafil or tadalafil causes an acute anabolic response of skeletal muscle protein synthesis. Furthermore, the ultrasensitive dependence of protein synthesis on EF-Tu concentration implies that the phd/doc toxin-antitoxin system is an efficient regulator of protein synthesis. If the switching rates are too low, the fraction of persister cells is too small to guarantee survival of the population under stress conditions. B) Interpolation of data from Liang et al. The same holds for the 2C-2T translation system when codon usages pi and tRNA concentrations Xi (i = 1, 2) are perfectly balanced (dashed orange line; p1/p2 = X1/X2 = 1). On the contrary, a decrease in EF-Tu greatly impedes protein synthesis in imbalanced systems, where the additional inhibition of ribosomes has a negligible effect. This EF-Tu dependence is strain-specific: For example, the overall elongation rate increases slightly more smoothly with the EF-Tu concentration for the strain LB2021 with EF-Tu symbol ARBO than for the other strains. Simulations were performed and parameterized as described in the Methods, with a total tRNA concentration of XLys + XHis = 3.44 M and concentration ratios XLys/XHis as indicated. provided by the manufacturers and the most recent codes of conduct and safety regulations. The substances take advantage of the major differences between prokaryotic and eukaryotic ribosome structures which differ in their size, sequence, structure, and the ratio of protein to RNA. Ribosomes are molecular machines that use the genetic information stored in messenger RNAs (mRNAs) to synthesize proteins. Infect Dis Ther 4(1):114. PLOS is a nonprofit 501(c)(3) corporation, #C2354500, based in San Francisco, California, US. Ribosome and EF-Tu as targets for protein synthesis inhibition. We find that protein synthesis reacts ultrasensitively to a decrease in the elongation factors concentration for systems with an imbalance between codon usages and tRNA concentrations. The framework incorporates a multitude of factors that influence the speed and fidelity of cellular protein synthesis. EC Microbiol 1:118121, Fernandes P (2016) Fusidic acid: a bacterial elongation factor inhibitor for the oral treatment of acute and chronic staphylococcal infections. For example, in contrast to the toxin Doc, the Ser/Thr kinase YabT simultaneously inhibits both EF-Tu and ribosomes in Bacillus subtilis by stabilizing EF-Tu on translating ribosomes [25]. - These drugs act on the bacterial ribosomes. Starting in state (c|0), it moves through the states of the cognate (i = 15) or near-cognate branch (i = 610), or attains state (c|11) upon binding of a non-cognate ternary complex. The EF-Tu threshold concentration for the parameter regime X1/X2 p1/p2 is obtained by swapping the indices 1 and 2 in Eq (1). Arch Microbiol 176:386390, Singh RK, Tiwari SP, Rai AK, Mohapatra TM (2011) Cyanobacteria: an emerging source for drug discovery. Author summary We predict and analyze the response of differently composed protein synthesis systems to the inhibition of elongation factor EF-Tu and/or ribosomes. https://doi.org/10.1007/978-981-33-6009-9_55, DOI: https://doi.org/10.1007/978-981-33-6009-9_55, eBook Packages: Biomedical and Life SciencesBiomedical and Life Sciences (R0). Macrolides, clindamycin, and aminoglycosides have evidence of inhibition of ribosomal translocation. 2021 Springer Nature Singapore Pte Ltd. Anandabaskar, N. (2021). To facilitate comparison, data are rescaled as described in S1 Text and solid lines are drawn as a guide to the eye (no model fitting). Nature 407:327339, Yonath A (2005) Antibiotics targeting ribosomes: resistance, selectivity, synergism, and cellular regulation. The authors and the publishers do not accept responsibility or
Select your institution from the list provided, which will take you to your institution's website to sign in. Choose this option to get remote access when outside your institution. S2 Fig. At the indicated point in time, the concentrations of all species containing EF-Tu were reduced by a specific amount (fraction). Chloramphenicol blocks the peptidyl transfer step of elongation on the 50S ribosomal subunit in both bacteria and mitochondria. - 51.195.45.68. On the contrary, chloramphenicol, macrolides, ketolides, lincosamides, streptogramins, oxazolidinones, and pleuromutilins bind to the 50S subunit. Springer, Cham. S5 Fig. (18)(21) (p1/p2 = 1 and X1/X2 as indicated; concentrations relative to their value at 500 M of EF-Tu). However, if the relative tRNA concentrations do not perfectly match the corresponding codon usages, the 2C-2T translation system responds in a much more complex way to variations of the EF-Tu availability: A regime of inhibited translation for small EF-Tu concentrations is followed by a relatively steep increase of the overall elongation rate, that finally saturates at larger EF-Tu concentrations, see Fig 3A). If you see Sign in through society site in the sign in pane within a journal: If you do not have a society account or have forgotten your username or password, please contact your society. Our books are available by subscription or purchase to libraries and institutions. [42] (diamonds, solid line) relating growth rate and overall elongation rate in E. coli. This is a preview of subscription content, access via your institution. Microbial Cell 2:10, Apfel CM, Locher H, Evers S, Takacs B, Hubschwerlen C, Pirson W, Page MGP, Keck W (2001) Peptide deformylase as an antibacterial drug target: target validation and resistance development. However, the enzyme's multifunctional character and a multitude of PKR . As an example, a 2C-2T in-vitro translation system would consist of , , and mRNAs consisting only of UUC and UGC codons. All parameters as in Fig 3B) in the main text. Linezolid acts at the initiation stage, probably by preventing the formation of the initiation complex, although the mechanism is not fully understood. Protein synthesis inhibitors bind to either 30S subunit or 50S subunit or both the subunits of the ribosome to exert their action. Oxford University Press is a department of the University of Oxford. Society member access to a journal is achieved in one of the following ways: Many societies offer single sign-on between the society website and Oxford Academic. This means that the remaining ribosomes proceed faster and that, to some extend, this increase in ribosomal speed can balance the loss of ribosomes, such that in the simulations the total rate of peptide synthesis remains approximately constant under mild inhibiting conditions. A proposed mode of action of pseudomonic acid as an inhibitor of isoleucyl-tRNA synthetase. This complexity, which is fully captured by our computational in-vivo-like translation system [28], makes it difficult to study the molecular origin of the ultrasensitive dependence of protein synthesis on EF-Tu concentration. National Institute of Diabetes and Digestive and Kidney Diseases, Bethesda, MD. Toxin-antitoxin mediated phenotype transitions from the fast-growing to the dormant phenotype and vice versa were found to be caused by stochastic fluctuations of the abundance of free toxin above and below a certain threshold [13], where the switching rates need to be fast enough. Protein synthesis inhibitors refer to drugs that block the production of bacterial proteins and thus inhibit their proliferation. The persistence arises from stochastic phenotypic transitions resulting in strongly reduced growth rates [11]. Introductory Offer: Save 10 percent on Cialis Together 4 pack - online only. The competition of free aminoacylated tRNAs for free EF-Tu molecules causes the ultrasensitivity of systems with imbalanced tRNA/codon compositions: The oversupplied tRNA acts as a competitive inhibitor for the formation of ternary complexes containing the less abundant tRNA. https://doi.org/10.1093/jac/dkv169, Rybak JM, Roberts K (2015) Tedizolid phosphate: a next-generation oxazolidinone. Furthermore, the author would like to thank Reinhard Lipowsky for constructive discussions; and Reinhard Lipowsky and Nadin Haase for critical comments on the manuscript. 2C-2T translation system without near-cognate tRNA incorporation. 3 in Ref. A protein synthesis inhibitor is a substance that stops or slows the growth or proliferation of cells by disrupting the processes that lead directly to the generation of new proteins. No further changes were made to the system. D) Response of the in-vitro fMetLysHis tripeptide synthesis system to a sudden drop in EF-Tu concentration from 5 M to 3 M at 100s after start of reaction as predicted by the PURE system simulator for tRNA concentrations XLys + XHis = 3.44 M and XLys/XHis = 8/2. The P site is where the peptidyl tRNA is formed in the ribosome. In the following sections, we show that the strain-specificity of the response to a decrease in EF-Tu availability can be explained by differences in the tRNA/codon compositions of the strains. We used a recent version of the PURE system simulator, which was kindly provided by Drs. It is unlikely that a major fraction of the EF-Tu molecules gets phosphorylated at the same time. PubMedGoogle Scholar. Nishanthi Anandabaskar . A) Inhibition of EF-Tu generally leads to a decrease in the overall elongation rate. After translocation to the next codon c, the ribosome reaches state (c|0). Protein synthesis inhibitors work at different stages of prokaryotic mRNA translation into proteins like initiation, elongation (including aminoacyl tRNA entry, proofreading, peptidyl transfer, and ribosomal translocation), and termination. Google Scholar, Krause KM, Serio AW, Kane TR, Connolly LE (2016) Aminoglycosides: an overview. Therefore, in principle the phd/doc toxinantitoxin system can facilitate transitions between a persistent phenotype with strongly reduced protein synthesis and a fast-growing phenotype with maximal protein synthesis. Competing interests: The authors have declared that no competing interests exist. Click the account icon in the top right to: Oxford Academic is home to a wide variety of products. Protein synthesis inhibitors. PURE system simulator: Effects of ribosome (and EF-Tu) inhibition on the synthesis of fMetLysHis tripeptides. In fact, depending on the specific site of modification, phosphorylation and other modifications of EF-Tu can impact protein synthesis in different ways. A personal account can be used to get email alerts, save searches, purchase content, and activate subscriptions. Plasmid 13:1730, Sandvang D (1999) Novel streptomycin and spectinomycin resistance gene as a gene cassette within a class 1 integron isolated from Escherichia coli. Recently, several potent PKR inhibitors have been synthesized. This authentication occurs automatically, and it is not possible to sign out of an IP authenticated account. Nirav Sharma Monday, 13 June 2016. 1. In: Brunton LL, Dandan RH, Knollmann BC (eds) Goodman & Gilmans the pharmacological basis of therapeutics, 13th edn. We discovered that the EF-Tu threshold concentration only depends on the total concentrations X1 and X2 of tRNA species 1 and 2 and the codon usages p1 and p2. Although EF-Tu and the ribosome are both fundamental for bacterial mRNA translation, they are very distinct in terms of, e.g., function, abundance, structure, or interactions with other components of the bacterial protein synthesis machinery. Chem Biol 13:10011009, Joharapurkar AA, Dhanesha NA, Jain MR (2014) Inhibition of the methionine aminopeptidase 2 enzyme for the treatment of obesity. Mechanisms of action of the antibiotics and resistance development against them are discussed. Clin Infect Dis 52(suppl 7):S542S546, Martemyanov KA, Liljas A, Yarunin AS, Gudkov AT (2001) Mutations in the G-domain of elongation factor G from Thermus thermophilus affect both its interaction with GTP and fusidic acid. The ultrasensitive dependence of the overall elongation rate on the EF-Tu concentration is inherent in imbalanced translation systems but not in systems with a balanced tRNA/codon composition. This is an open access article distributed under the terms of the Creative Commons Attribution License, which permits unrestricted use, distribution, and reproduction in any medium, provided the original author and source are credited. The toxin Doc from the phd/doc toxin-antitoxin system inhibits EF-Tu by phosphorylation [17, 18]. To simulate the impact of EF-Tu inhibition as a function of time, translation was simulated until the translation rate has reached a quasi-steady state level. The author thanks Tomoaki Matsuura and Yoshihiro Shimizu for providing an extended version of the PURE system simulator. FEMS Microbiol Rev 28:519542, Doucet PF, Capobianco JO, Jarlier V, Goldman RC (1998) Molecular basis of clarithromycin activity against Mycobacterium avium and Mycobacterium smegmatis. Cold Spring Harb Perspect Med 6:a025437. In this report, we apply the COMPARE algorithm to search the data-ase of compounds tested in the NCI Human Tumor Cell Line Anti-Cancer Drug Screen for novel inhibitors of protein synthesis. In our approach, the cytotoxicity profiles (GI 50) of 31 known protein synthesis inhibitors were used to identify two novel, eukaryotic-specific translation . Translation initiation: i.1, Met tRNA i binding to eIF2 and formation of the eIF2/MettRNA In turn, when the EF-Tu concentration reaches a certain threshold value, protein synthesis is switched on and the overall translation rate rises from zero to a physiological value within a relatively narrow range of EF-Tu concentrations. https://doi.org/10.1101/cshperspect.a027037, Department of Pharmacology, Sri Manakula Vinayagar Medical College and Hospital, Puducherry, India, You can also search for this author in Two components, a 2C-2T in-vitro translation system consists of one codon one... 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