Multidrug Efflux Pumps at the Crossroad between Antibiotic Resistance and Bacterial Virulence

Alcalde-Rico, Manuel; Hernando-Amado, Sara; Blanco, Paula; Martínez, José Luis

doi:10.3389/fmicb.2016.01483

Cited by 186 publications

(169 citation statements)

References 135 publications

(179 reference statements)

Supporting

Mentioning

160

Contrasting

Unclassified

Order By: Relevance

“…Overexpression of transmembrane multidrug efflux pumps as well as reduced uptake results in sub-toxic levels of drugs within the microbial cells. 20 In P. aeruginosa, mutation in regulatory protein that normally dampens the gene encoding efflux proteins results in enhanced outpour. E. coli uses transmembrane proton gradient to expel multiple antibiotics through its numerous efflux pumps.…”

mentioning

confidence: 99%

Nanomaterials for alternative antibacterial therapy

Hemeg

2017

IJN

441

262

View full text Add to dashboard Cite

Despite an array of cogent antibiotics, bacterial infections, notably those produced by nosocomial pathogens, still remain a leading factor of morbidity and mortality around the globe. They target the severely ill, hospitalized and immunocompromised patients with incapacitated immune system, who are prone to infections. The choice of antimicrobial therapy is largely empirical and not devoid of toxicity, hypersensitivity, teratogenicity and/or mutagenicity. The emergence of multidrug-resistant bacteria further intensifies the clinical predicament as it directly impacts public health due to diminished potency of current antibiotics. In addition, there is an escalating concern with respect to biofilm-associated infections that are refractory to the presently available antimicrobial armory, leaving almost no therapeutic option. Hence, there is a dire need to develop alternate antibacterial agents. The past decade has witnessed a substantial upsurge in the global use of nanomedicines as innovative tools for combating the high rates of antimicrobial resistance. Antibacterial activity of metal and metal oxide nanoparticles (NPs) has been extensively reported. The microbes are eliminated either by microbicidal effects of the NPs, such as release of free metal ions culminating in cell membrane damage, DNA interactions or free radical generation, or by microbiostatic effects coupled with killing potentiated by the host’s immune system. This review encompasses the magnitude of multidrug resistance in nosocomial infections, bacterial evasion of the host immune system, mechanisms used by bacteria to develop drug resistance and the use of nanomaterials based on metals to overcome these challenges. The diverse annihilative effects of conventional and biogenic metal NPs for antibacterial activity are also discussed. The use of polymer-based nanomaterials and nanocomposites, alone or functionalized with ligands, antibodies or antibiotics, as alternative antimicrobial agents for treating severe bacterial infections is also discussed. Combinatorial therapy with metallic NPs, as adjunct to the existing antibiotics, may aid to restrain the mounting menace of bacterial resistance and nosocomial threat.

show abstract

mentioning

confidence: 99%

Nanomaterials for alternative antibacterial therapy

Hemeg

2017

IJN

441

262

View full text Add to dashboard Cite

show abstract

“…One of the ways for achieving such modulation is by interfering with the available concentrations of the signals that trigger the regulatory networks. For this purpose, multidrug efflux pumps can be particularly well suited, because the activity of these antibiotic resistance determinants can affect the bacterial physiology through the extrusion of endogenous/exogenous molecular compounds with relevance for bacterial physiology [3, 7]. As a consequence of this extrusion, the expression of a large number of genes, including those encoding virulence determinants, may be altered, which has been usually considered as the fitness cost associated to the acquisition of antibiotic resistance.…”

Section: Discussionmentioning

confidence: 99%

“…It is worth noticing that genes that contribute to P. aeruginosa intrinsic antibiotic resistance are, in several occasions, key components of bacterial physiology [3, 4]. This is the case of the Resistance, Nodulation and cell-Division (RND) family of efflux pumps, which, besides being important mechanisms of antibiotic resistance in P. aeruginosa [5, 6], also may play a key role in its pathogenesis and adaption to host environment [3, 7]. In this work, we address the role of the MexAB-OprM efflux system, one of the most relevant RND systems for intrinsic and acquired antibiotic resistance of P. aeruginosa [8, 9], on the modulation of quorum sensing (QS) responses in this bacterium.…”

Section: Introductionmentioning

confidence: 99%

The analysis of the role of MexAB-OprM on quorum sensing homeostasis shows that the apparent redundancy of Pseudomonasaeruginosamultidrug efflux pumps allows keeping the robustness and the plasticity of this intercellular signaling network

Alcalde-Rico

Olivares-Pacheco

Halliday

et al. 2020

Preprint

Self Cite

View full text Add to dashboard Cite

The analysis of the role of MexAB-OprM on quorum sensing homeostasis shows 2 that the apparent redundancy of Pseudomonas aeruginosa multidrug efflux pumps 3 allows keeping the robustness and the plasticity of this intercellular signaling 4 network 5 6 Running: Efflux systems' redundancy on quorum sensing homeostasis 7 8 9 Abstract 22the resistance/virulence crosstalk since, besides contributing to antibiotic resistance, 47 they can also modulate the quorum sensing (QS) response. We show that mutants 48 overexpressing the MexAB-OprM efflux pump, present an impaired QS response due to 49 the reduced availability of the QS signal precursor octanoate, not because they extrude, 50 as previously stated, the QS signal 3-oxo-C12-HSL. Together with previous studies, this 51 indicates that, although the consequences of overexpressing efflux pumps are similar 52 (impaired QS response), the mechanisms are different. This 'apparent redundancy' of 53 RND efflux systems can be understood as a P. aeruginosa strategy to keep the 54 robustness of the QS regulatory network and modulate its output in response to different 55 signals. 57Pseudomonas aeruginosa is an opportunistic pathogen of special concern due to its 58 capability to produce a large variety of serious human infections and to its low 59 susceptibility to different antibiotics [1, 2]. It is worth noticing that genes that contribute 60 to P. aeruginosa intrinsic antibiotic resistance are, in several occasions, key components 61 of bacterial physiology [3, 4]. This is the case of the Resistance, Nodulation and cell-62 Division (RND) family of efflux pumps, which, besides being important mechanisms of 63 antibiotic resistance in P. aeruginosa [5, 6], also may play a key role in its pathogenesis 64 and adaption to host environment [3, 7]. In this work, we address the role of the 65MexAB-OprM efflux system, one of the most relevant RND systems for intrinsic and 66 acquired antibiotic resistance of P. aeruginosa [8, 9], on the modulation of quorum 67 sensing (QS) responses in this bacterium. 68The QS response consists in a population-scale cooperative behavior promoted by cell-69to-cell communication systems that control the expression of a large set of genes in a 70 cell-density way [10]. This intercellular communication system is based on the 71 synthesis, delivery and progressive accumulation of autoinducer compounds, known as 72 QS signal molecules (QSSMs), which are recognized by specific cell receptors. When 73QSSMs concentrations reach a threshold, the QS response is triggered in the population. 74This population-scale response regulates a wide number of diverse physiological 75 processes [11], including production of private and public goods [12], biofilm formation 76[13], host-bacteria interactions [14] and virulence factors production [15]. The QS 77 responses usually impose a fitness burden at single cell level but with social benefit at 78 population level [16, 17]. 79The QS regulatory network of P. aeruginosa is based on the production of two different 80 kinds...

show abstract

“…In Gram-negative bacteria Fe 3+ -siderophore complexes are recognized by selective outer-membrane TonB-dependent transporters [57] that bind the complex and translocate it into the periplasmic space. One of the mechanisms of bacterial resistance to antibiotics are the multidrug efflux pumps [58]. To overcome this aspect of bacterial resistance, a "Trojan horse" strategy has been conceived, consisting of attaching an antibiotic molecule to a siderophore [59].…”

Section: Highlighted By Stefano Manganimentioning

confidence: 99%