New Multidrug Efflux Inhibitors for Gram-Negative Bacteria

Marshall, Robert L.; Lloyd, Georgina S.; Lawler, Amelia J.; Element, Sarah J; Kaur, Jaswant; Ciusa, Maria Laura; Ricci, Vito; Tschumi, Andreas; Kühne, Holger; Alderwick, Luke J.; Piddock, Laura J. V.

doi:10.1128/mbio.01340-20

Cited by 32 publications

(23 citation statements)

References 55 publications

(83 reference statements)

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“…Examples of non-essential target inhibitors are represented by: Inhibitors of virulence-conferring factors or pathways (also known as anti-virulence compounds or pathoblockers 86 that target, for example, quorum sensing mechanisms 87 , biofilm formation 88 , bacterial secretion systems 89 , 90 , enzymes for tissue penetration 91 or intracellular survival 92 ). Efflux pump inhibitors 93 . Suicide substrates such as β-lactamase inhibitors 94 , 95 .…”

Section: Synthetic Hit Compoundsmentioning

confidence: 99%

“…These factors can be addressed by suitable compound design, which generally remains rather empirical and challenging 254 – 257 . Other possibilities to address this key area would be to use these compounds in combination with outer membrane permeabilizing agents 258 , 259 or efflux inhibitors 93 , 260 . Alternative approaches targeting extracellular virulence factors, for example, extracellular lectins required for attachment and biofilm formation or secreted proteolytic enzymes, do not suffer from a possible lack of bacterial uptake 261 .…”

Section: Advancing Hits To (Pre)clinical Statusmentioning

confidence: 99%

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Towards the sustainable discovery and development of new antibiotics

et al. 2021

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An ever-increasing demand for novel antimicrobials to treat life-threatening infections caused by the global spread of multidrug-resistant bacterial pathogens stands in stark contrast to the current level of investment in their development, particularly in the fields of natural-product-derived and synthetic small molecules. New agents displaying innovative chemistry and modes of action are desperately needed worldwide to tackle the public health menace posed by antimicrobial resistance. Here, our consortium presents a strategic blueprint to substantially improve our ability to discover and develop new antibiotics. We propose both short-term and long-term solutions to overcome the most urgent limitations in the various sectors of research and funding, aiming to bridge the gap between academic, industrial and political stakeholders, and to unite interdisciplinary expertise in order to efficiently fuel the translational pipeline for the benefit of future generations.

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Section: Synthetic Hit Compoundsmentioning

confidence: 99%

Section: Advancing Hits To (Pre)clinical Statusmentioning

confidence: 99%

Towards the sustainable discovery and development of new antibiotics

et al. 2021

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“…Of the EIs identified, auranofin ( 8 , Figure 56 ), an antirheumatic agent, increased ethidium bromide accumulation and potentiated antibiotic activity in checkerboard assays. 898 While most drug screening efforts have focused on looking at inhibitors of RND inner membrane transporters, a recent study identified an inhibitor of the ABC type efflux pump MacAB in S. Typhimurium. Compound 9 ( Figure 56 ) was identified from screening a drug library for compounds that inhibited the growth of a macAB -overexpressing strain in the presence of erythromycin.…”

Section: Targeting Tripartite Assemblies—pump Inhibitors and Disruptorsmentioning

confidence: 99%

Structure, Assembly, and Function of Tripartite Efflux and Type 1 Secretion Systems in Gram-Negative Bacteria

et al. 2021

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Tripartite efflux pumps and the related type 1 secretion systems (T1SSs) in Gram-negative organisms are diverse in function, energization, and structural organization. They form continuous conduits spanning both the inner and the outer membrane and are composed of three principal components—the energized inner membrane transporters (belonging to ABC, RND, and MFS families), the outer membrane factor channel-like proteins, and linking the two, the periplasmic adaptor proteins (PAPs), also known as the membrane fusion proteins (MFPs). In this review we summarize the recent advances in understanding of structural biology, function, and regulation of these systems, highlighting the previously undescribed role of PAPs in providing a common architectural scaffold across diverse families of transporters. Despite being built from a limited number of basic structural domains, these complexes present a staggering variety of architectures. While key insights have been derived from the RND transporter systems, a closer inspection of the operation and structural organization of different tripartite systems reveals unexpected analogies between them, including those formed around MFS- and ATP-driven transporters, suggesting that they operate around basic common principles. Based on that we are proposing a new integrated model of PAP-mediated communication within the conformational cycling of tripartite systems, which could be expanded to other types of assemblies.

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“…So when a substance activates ramA, the fluorescent protein is produced and the researchers can see the glow using high-throughput screening machinery. The team has now screened nearly 50,000 compounds, identifying 43 efflux-pump inhibitors, 11 of which have been shown to increase the efficacy of antibiotics in lab tests 2 .…”

Section: Top Targetsmentioning

confidence: 99%