The SaeRS Two‐Component System of  Staphylococcus aureus

Liu, Qian; Yeo, Won Sik; Bae, Taeok

doi:10.3390/genes7100081

Cited by 173 publications

(211 citation statements)

References 139 publications

(235 reference statements)

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“…While Sae, CodY and Rot all interfered with SigB‐dependent promoter activity, only Sae additionally repressed activity of the SigA‐dependent promoter. This is in line with a predicted SaeR binding site located between the two promoters (Liu et al , ). We hypothesize that the repression of SigB‐dependent promoter activity occurs via steric interference, whereas the SigA‐dependent promoter activity might be repressed via a roadblock mechanism.…”

Section: Discussionsupporting

confidence: 88%

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Revisiting the regulation of the capsular polysaccharide biosynthesis gene cluster in Staphylococcus aureus

Keinhörster

Salzer

Duque‐Jaramillo

et al. 2019

Molecular Microbiology

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Summary Capsular polysaccharide (CP) biosynthesis in Staphylococcus aureus is tightly controlled resulting in a heterogeneous phenotype within a population and CP being mainly detectable in nongrowing cells. Expression of the corresponding biosynthesis gene cluster is driven by one promoter element (Pcap). Here, we demonstrate that Pcap contains a main SigB‐dependent promoter. The SigB consensus motif overlaps with a previously described inverted repeat (IR) that is crucial for cap expression. The essentiality of the IR is derived from this region acting as a SigB binding site rather than as an operator site for the proposed cap activators RbsR and MsaB. Furthermore, Pcap contains an extensive upstream region harboring a weak SigA‐dependent promoter and binding sites for cap repressors such as SaeR, CodY and Rot. Heterogeneous CP synthesis is determined by SigB activity and repressor binding to the upstream region. SigB dependency and regulation by the upstream repressors are also sufficient to explain the temporal gene expression pattern at the transcriptional level. However, CP synthesis remains growth phase‐dependent even when transcription is rendered constitutive, suggesting additional posttranscriptional regulatory circuits. Thus, the interference of multiple repressors with SigB‐dependent promoter activity as well as post‐transcriptional mechanisms ensure the appropriate regulation of CP synthesis.

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Section: Discussionsupporting

confidence: 88%

“…5B). Binding is consistent with a putative SaeR binding motif located between −79 bp and −94 bp upstreams of the capA start codon (Liu et al, 2016). Specific binding to the P cap upstream region was also found for Rot and CodY ( Fig.…”

Section: Sae Rot and Cody Repress P Cap By Direct Bindingsupporting

confidence: 79%

Revisiting the regulation of the capsular polysaccharide biosynthesis gene cluster in Staphylococcus aureus

Keinhörster

Salzer

Duque‐Jaramillo

et al. 2019

Molecular Microbiology

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“…8 For example, in the pathogenic bacterium Staphylococcus aureus , the SaeRS TCS affects the production of over 20 virulence factors. 9 The PhoPR system controls polyketide-derived lipid biosynthesis in Mycobacterium tuberculosis , and its absence causes dramatic changes to colonial and cording morphology of this highly dangerous microbe. 10 In Pseudomonas aeruginosa , many TCSs, including PPrBA, are responsible for activating virulence genes, cell motility, and quorum sensing signal production.…”

Section: Introductionmentioning

confidence: 99%

Rational Design of Selective Adenine-Based Scaffolds for Inactivation of Bacterial Histidine Kinases

2017

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Bacterial histidine kinases (HKs) are quintessential regulatory enzymes found ubiquitously in bacteria. Apart from their regulatory roles, they are also involved in the production of virulence factors and conferring resistance to various antibiotics in pathogenic microbes. We have previously reported compounds that inhibit multiple HKs by targeting the conserved catalytic and ATP-binding (CA) domain. Herein, we conduct a detailed structure–activity relationship assessment of adenine-based inhibitors using biochemical and docking methods. These studies have resulted in several observations. First, interaction of an inhibitor’s amine group with the conserved active-site Asp is essential for activity and likely dictates its orientation in the binding pocket. Second, a N-NH-N triad in the inhibitor scaffold is highly preferred for binding to conserved Gly:Asp:Asn residues. Lastly, hydrophobic electron-withdrawing groups at several positions in the adenine core enhance potency. The selectivity of these inhibitors was tested against heat shock protein 90 (HSP90), which possesses a similar ATP-binding fold. We found that groups that target the ATP-lid portion of the catalytic domain, such as a six-membered ring, confer selectivity for HKs.

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“…El Staphylococcus aureus es capaz de secretar entre 23 a 24 superantígenos diferentes serológicamente dentro de los que se encuentran más de 20 enterotoxinas estafi lococcicas (SEs del inglés) entre estas la TSST-1, las SEs con serotipos A, B n , C n , (N=múltiples variantes) D, E, F y G; y la SE -1 (serotipo H, I y J a la X). En función de muchos de estos superantígenos, especialmente el SEA, y con menos frecuencia el SEG, SEC, SEI, se ha explicado la patogénesis de los S.aureus y su evolución hacia la sepsis; así como la patogénesis de los S.aureus meticilina resistentes (MRSA en inglés) asociados a sepsis letal, endocarditis infecciosa y lesión renal en modelos animales debido específi camente a sus superantígenos SEA y SEC, así como al gen mecA que codifi ca la proteína de unión a la penicilina alterada (PBP2a) que es su principal mecanismo de resistencia a la meticilina lo que les hace unos de los microorganismos que más centran la atención en los últimos años de la comunidad científi ca y médica al ser responsables del aumento de la tasas de morbilidad y mortalidad de infecciones por estafi lococos a nivel hospitalario y comunitario dada la multirresistencia que exhiben y el estar asociados (19)(20)(21)(22)(23)(24)(25)(26)(27).…”

Section: Bacterias Gram Positivas: Estructura Molecular Antigénicaunclassified

Fisiopatología de la sepsis por gram positivos

Fandiño¹,

Barrera²

2016

rev cuarzo

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Las bacterias gram positivas vienen cobrando importancia como agentes etiológicos de la sepsis siendo algunos de principales representantes Staphylococcus aureus, las cepas de S.aureus meticilino resistentes (MRSA del inglés) y el Streptococcus pyogenes o también llamado Streptococcus del grupo A invasivo (GAS). Dado que en su estructura celular presentan diversas moléculas que pueden ser reconocidas como patrones moleculares asociados a patógenos (PAMPs) como son el peptidoglicano (PNG) el ácido teicoico (LTA), las lipoproteínas; y otras que activan directamente el sistema inmune adaptativo como son los Superantígenos; los pacientes infectados pueden exponerse de manera simultánea a una respuesta inmune amplifi cada de manera sinérgica entre todos estos tipos de antígenos, que a través de vías de señalización intracelular desencadenarán la transcripción de genes codifi cadores de citocinas pro infl amatorias como el TNFα, la IL-1β, la IL-6, el INFγ, IL-8, IL-18, IL-2, IL-12, IL-10 que darán lugar a muchas de las manifestaciones clínicas de la sepsis y se vienen asociando como predictores del pronóstico de esta junto a otros marcadores moleculares de la misma.

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The SaeRS Two‐Component System of Staphylococcus aureus

Cited by 173 publications

References 139 publications

Revisiting the regulation of the capsular polysaccharide biosynthesis gene cluster in Staphylococcus aureus

Revisiting the regulation of the capsular polysaccharide biosynthesis gene cluster in Staphylococcus aureus

Rational Design of Selective Adenine-Based Scaffolds for Inactivation of Bacterial Histidine Kinases

Fisiopatología de la sepsis por gram positivos

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