scholarly journals Are antibacterial effects of non-antibiotic drugs random or purposeful because of a common evolutionary origin of bacterial and mammalian targets?

Infection ◽  
2020 ◽  
Author(s):  
Axel Dalhoff
Keyword(s):  
Carbapenem Resistance ◽  
Antibacterial Activities ◽  
Bacterial Virulence ◽  
Evolutionary Origin ◽  
Carbonic Anhydrases ◽  
Aminoglycoside Resistance ◽  
Common Evolutionary Origin ◽  
Eukaryotic Genes ◽  
Antibiotic Drugs ◽  
Active Centres

Abstract Purpose Advances in structural biology, genetics, bioinformatics, etc. resulted in the availability of an enormous pool of information enabling the analysis of the ancestry of pro- and eukaryotic genes and proteins. Methods This review summarizes findings of structural and/or functional homologies of pro- and eukaryotic enzymes catalysing analogous biological reactions because of their highly conserved active centres so that non-antibiotics interacted with bacterial targets. Results Protease inhibitors such as staurosporine or camostat inhibited bacterial serine/threonine or serine/tyrosine protein kinases, serine/threonine phosphatases, and serine/threonine kinases, to which penicillin-binding-proteins are linked, so that these drugs synergized with β-lactams, reverted aminoglycoside-resistance and attenuated bacterial virulence. Calcium antagonists such as nitrendipine or verapamil blocked not only prokaryotic ion channels but interacted with negatively charged bacterial cell membranes thus disrupting membrane energetics and inducing membrane stress response resulting in inhibition of P-glycoprotein such as bacterial pumps thus improving anti-mycobacterial activities of rifampicin, tetracycline, fluoroquinolones, bedaquilin and imipenem-activity against Acinetobacter spp. Ciclosporine and tacrolimus attenuated bacterial virulence. ACE-inhibitors like captopril interacted with metallo-β-lactamases thus reverting carbapenem-resistance; prokaryotic carbonic anhydrases were inhibited as well resulting in growth impairment. In general, non-antibiotics exerted weak antibacterial activities on their own but synergized with antibiotics, and/or reverted resistance and/or attenuated virulence. Conclusions Data summarized in this review support the theory that prokaryotic proteins represent targets for non-antibiotics because of a common evolutionary origin of bacterial- and mammalian targets resulting in highly conserved active centres of both, pro- and eukaryotic proteins with which the non-antibiotics interact and exert antibacterial actions.

scholarly journals 1348. In vitro Activity of Plazomicin, a Next-Generation Aminoglycoside, Against Carbapenemase-Producing Klebsiella pneumoniae

2018 ◽  
Vol 5 (suppl_1) ◽  
pp. S412-S413
Author(s):  
Michael R Jacobs ◽  
Caryn E Good ◽  
Ayman M Abdelhamed ◽  
Daniel D Rhoads ◽  
Kristine M Hujer ◽  
...  
Keyword(s):  
Klebsiella Pneumoniae ◽  
Carbapenem Resistance ◽  
Vitro Activity ◽  
In Vitro Activity ◽  
Next Generation ◽  
Aminoglycoside Resistance ◽  
Carbapenem Resistant ◽  
Carbapenemase Gene ◽  
Research Grant

Abstract Background Plazomicin is a next-generation aminoglycoside with in vitro activity against multidrug-resistant Gram-negative species, including carbapenem-resistant isolates. The Consortium on Resistance Against Carbapenems in Klebsiella and other Enterobacteriaceae (CRACKLE) is a federally funded, prospective multicenter consortium of 20 hospitals from nine US healthcare systems to track carbapenem-resistant Enterobacteriaceae. Methods Minimum inhibitory concentrations (MICs) of plazomicin were determined by broth microdilution according to current CLSI guidelines against a collection of 697 carbapenem-resistant Klebsiella pneumoniae with defined carbapenem resistance mechanisms, including KPC and OXA carbapenemases. Isolates were submitted by participating CRACKLE centers. Results Carbapenemases present in study isolates included KPC-2 (n = 323), KPC-3 (n = 364), KPC-4 (n = 2), OXA-48 like (n = 7), and NDM (n = 1). Plazomicin MICs ranged from ≤0.12 to >32 mg/L, with MIC50 and MIC90 values of 0.25 and 1 mg/L, respectively (figure). MICs of 689 (98.8%) isolates were ≤4 mg/L, while MICs of the remaining eight isolates were >32 mg/L. Plazomicin MICs were related to specific carbapenemases present in isolates: of eight isolates with MICs >32 mg/L, seven contained OXA-48 like and one contained KPC-3, suggesting that these isolates possess an aminoglycoside-resistance mechanism on the same plasmid as their carbapenemase gene, such as a 16S ribosomal RNA methyltransferase, against which plazomicin is not active. Conclusion Plazomicin has good in vitro potency against a collection of carbapenemase-producing K. pneumoniae, with MIC90 value of 1 mg/L and MICs of ≤4 mg/L for 98.9% of isolates. Disclosures M. R. Jacobs, Achaogen: Investigator, Research grant. Shionogi: Investigator, Research grant. L. Connolly, Achaogen, Inc.: Consultant, Consulting fee. K. M. Krause, Achaogen: Employee, Salary. S. S. Richter, bioMerieux: Grant Investigator, Research grant. BD Diagnostics: Grant Investigator, Research grant. Roche: Grant Investigator, Research grant. Hologic: Grant Investigator, Research grant. Diasorin: Grant Investigator, Research grant. Accelerate: Grant Investigator, Research grant. Biofire: Grant Investigator, Research grant. D. Van Duin, achaogen: Scientific Advisor, Consulting fee. shionogi: Scientific Advisor, Consulting fee. Allergan: Scientific Advisor, Consulting fee. Astellas: Scientific Advisor, Consulting fee. Neumedicine: Scientific Advisor, Consulting fee. Roche: Scientific Advisor, Consulting fee. T2 Biosystems: Scientific Advisor, Consulting fee.

scholarly journals Molecular Epidemiology of Emerging Carbapenem Resistance inAcinetobacter nosocomialisandAcinetobacter pittiiin Taiwan, 2010 to 2014

2019 ◽  
Vol 63 (4) ◽  
Author(s):  
Feng-Jui Chen ◽  
Wei-Cheng Huang ◽  
Yu-Chieh Liao ◽  
Hui-Ying Wang ◽  
Jui-Fen Lai ◽  
...  
Keyword(s):  
Molecular Epidemiology ◽  
Species Identification ◽  
Carbapenem Resistance ◽  
Close Monitoring ◽  
Aminoglycoside Resistance ◽  
Content Type ◽  
Carbapenem Resistant ◽  
Acinetobacter Pittii ◽  
Aminoglycoside Resistance Genes ◽  
Genetic Structures

ABSTRACTThis study investigated the molecular epidemiology of carbapenem-resistantAcinetobacter nosocomialisandAcinetobacter pittii(ANAP). Clinical isolates ofAcinetobacterspp. collected by the biennial nationwide Taiwan Surveillance of Antimicrobial Resistance program from 2010 to 2014 were subjected to species identification, antimicrobial susceptibility testing, and PCR for detection of carbapenemase genes. Whole-genome sequencing or PCR mapping was performed to study the genetic surroundings of the carbapenemase genes. Among 1,041Acinetobacterisolates, the proportion of ANAP increased from 11% in 2010 to 22% in 2014. The rate of carbapenem resistance in these isolates increased from 7.5% (3/40) to 22% (14/64), with a concomitant increase in their resistance to other antibiotics. TheblaOXA-72andblaOXA-58genes were highly prevalent in carbapenem-resistant ANAP. Various genetic structures were found upstream ofblaOXA-58in different plasmids. Among the plasmids found to containblaOXA-72flanked by XerC/XerD, pAB-NCGM253-like was identified in 8 of 10 isolates. Conjugations of plasmids carryingblaOXA-72orblaOXA-58toA. baumanniiwere successful. In addition, three isolates with chromosome-locatedblaOXA-23embedded in AbGRI1-type structure with disruption of genes other thancomMwere detected. Two highly similar plasmids carrying class I integron containingblaIMP-1and aminoglycoside resistance genes were also found. The universal presence ofblaOXA-272/213-likeonA. pittiichromosomes and their lack of contribution to carbapenem resistance indicate its potential to be a marker for species identification. The increase of ANAP, along with their diverse mechanisms of carbapenem resistance, may herald their further spread and warrants close monitoring.

scholarly journals A common evolutionary origin of two elementary enzyme folds

FEBS Letters ◽  
2001 ◽  
Vol 510 (3) ◽  
pp. 133-135 ◽  
Author(s):  
Birte Höcker ◽  
Steffen Schmidt ◽  
Reinhard Sterner
Keyword(s):  
Evolutionary Origin ◽  
Common Evolutionary Origin

scholarly journals Common evolutionary origin of alpha 2-macroglobulin and complement components C3 and C4.

1985 ◽  
Vol 82 (1) ◽  
pp. 9-13 ◽  
Author(s):  
L. Sottrup-Jensen ◽  
T. M. Stepanik ◽  
T. Kristensen ◽  
P. B. Lonblad ◽  
C. M. Jones ◽  
...  
Keyword(s):  
Evolutionary Origin ◽  
Complement Components ◽  
Common Evolutionary Origin
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