Identification of Cell-Penetrating Peptides That Are Bactericidal to Neisseria meningitidis and Prevent Inflammatory Responses upon Infection

Eriksson, Olaspers Sara; Geörg, Miriam; Sjölinder, Hong; Sillard, Rannar; Lindberg, Staffan; Langel, Ülo; Jonsson, Ann‐Beth

doi:10.1128/aac.00624-13

Cited by 24 publications

(18 citation statements)

References 66 publications

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“…aureus and Neisseria meningitides ( N . meningitides ) . However, its potential use against multi‐drug resistant bacteria with high separation rates when isolated from clinics has not been reported.…”

Section: Introductionmentioning

confidence: 99%

“…Transportan 10 (TP10) is a deletion analogue of the CPP transportan, a 21-residue chimeric construct consisting of the N-terminal part of the neuropeptide galanin linked to the full-length wasp venom peptide mastoparan that lacks the toxic side effects of its parent peptide. TP10 can transport cargo across cell membranes [10,11] and it has been reported that TP10 can enter both mammalian and microbial cells, preferentially permeabilising and killing microbes such as S. aureus and Neisseria meningitides (N. meningitides) [6,9]. However, its potential use against multi-drug resistant bacteria with high separation rates when isolated from clinics has not been reported.…”

Section: Introductionmentioning

confidence: 99%

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Antimicrobial activities and action mechanism studies of transportan 10 and its analogues against multidrug‐resistant bacteria

Xie

Gou

Zhao

et al. 2015

Journal of Peptide Science

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The increased emergence of multidrug-resistant bacteria is perceived as a critical public health threat, creating an urgent need for the development of novel classes of antimicrobials. Cell-penetrating peptides that share common features with antimicrobial peptides have been found to have antimicrobial activity and are currently being considered as potential alternatives to antibiotics. Transportan 10 is a chimeric cell-penetrating peptide that has been reported to transport biologically relevant cargoes into mammalian cells and cause damage to microbial membranes. In this study, we designed a series of TP10 analogues and studied their structure-activity relationships. We first evaluated the antimicrobial activities of these compounds against multidrug-resistant bacteria, which are responsible for most nosocomial infections. Our results showed that several of these compounds had potent antimicrobial and biofilm-inhibiting activities. We also measured the toxicity of these compounds, finding that Lys substitution could increase the antimicrobial activity but significantly enhanced the cytotoxicity. Pro introduction could reduce the cytotoxicity but disrupted the helical structure, resulting in a loss of activity. In the mechanistic studies, TP10 killed bacteria by membrane-active and DNA-binding activities. In conclusion, TP10 and its analogues could be developed into promising antibiotic candidates for the treatment of infections caused by multidrug-resistant bacteria.

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Section: Introductionmentioning

confidence: 99%

Section: Introductionmentioning

confidence: 99%

Antimicrobial activities and action mechanism studies of transportan 10 and its analogues against multidrug‐resistant bacteria

Xie

Gou

Zhao

et al. 2015

Journal of Peptide Science

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“…1B), thus, rendering the bacteria resistant to physiologically relevant concentrations of LL-37 (Schaller-Bals et al, 2002). The abrogation of selective host-cell Oehlke et al (1998); Palm et al (2006); Eriksson et al (2013). b.…”

Section: Discussionmentioning

confidence: 99%

Meningococcal resistance to antimicrobial peptides is mediated by bacterial adhesion and host cell RhoA and Cdc42 signalling

et al. 2013

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SummaryAntimicrobial peptides (AMPs) constitute an essential part of the innate immune defence. Pathogenic bacteria have evolved numerous strategies to withstand AMP-mediated killing. The influence of host epithelia on bacterial AMP resistance is, however, still largely unknown. We found that adhesion to pharyngeal epithelial cells protected Neisseria meningitidis, a leading cause of meningitis and sepsis, from the human cathelicidin LL-37, the cationic model amphipathic peptide (MAP) and the peptaibol alamethicin, but not from polymyxin B. Adhesion to primary airway epithelia resulted in a similar increase in LL-37 resistance. The inhibition of selective host cell signalling mediated by RhoA and Cdc42 was found to abolish the adhesion-induced LL-37 resistance by a mechanism unrelated to the actin cytoskeleton. Moreover, N. meningitidis triggered the formation of cholesterol-rich membrane microdomains in pharyngeal epithelial cells, and host cell cholesterol proved to be essential for adhesion-induced resistance. Our data highlight the importance of Rho GTPasedependent host cell signalling for meningococcal AMP resistance. These results indicate that N. meningitidis selectively exploits the epithelial microenvironment in order to protect itself from LL-37.

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“…The ability of CPF-C1 and several of its analogs to decrease bacterial quantities was approximated in an in vivo infection example in mice using a prior established method. [30,31] In summary, female Kunming mice (18-22 g; Medical Experimental Animal Center, Lanzhou University, China) were maintained in a 12-hr light-dark cycle with an unlimited supply of water and food. The mice were challenged intraperitoneally with 1.2 × 10 8 CFU of E. coli ATCC 25922 or E. coli 780 cells in 100 μl of 0.9% NaCl (normal saline or NS).…”

Section: In Vivo Antimicrobial Activitymentioning

confidence: 99%

Novel antimicrobial peptide CPF‐C1 analogs with superior stabilities and activities against multidrug‐resistant bacteria

Xie

Zhao

et al. 2017

Chem Biol Drug Des

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As numerous clinical isolates are resistant to most conventional antibiotics, infections caused by multidrug-resistant bacteria are associated with a higher death rate. Antimicrobial peptides show great potential as new antibiotics. However, a major obstacle to the development of these peptides as useful drugs is their low stability. To overcome the problem of the natural antimicrobial peptide CPF-C1, we designed and synthesized a series of analogs. Our results indicated that by introducing lysine, which could increase the number of positive charges, and by introducing tryptophan, which could increase the hydrophobicity, we could improve the antimicrobial activity of the peptides against multidrug-resistant strains. The introduction of d-amino acids significantly improved stability. Certain analogs demonstrated antibiofilm activities. In mechanistic studies, the analogs eradicated bacteria not just by interrupting the bacterial membranes, but also by linking to DNA, which was not impacted by known mechanisms of resistance. In a mouse model, certain analogs were able to significantly reduce the bacterial load. Among the analogs, CPF-9 was notable due to its greater antimicrobial potency in vitro and in vivo and its superior stability, lower hemolytic activity, and higher antibiofilm activity. This analog is a potential antibiotic candidate for treating infections induced by multidrug-resistant bacteria.

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Identification of Cell-Penetrating Peptides That Are Bactericidal to Neisseria meningitidis and Prevent Inflammatory Responses upon Infection

Cited by 24 publications

References 66 publications

Antimicrobial activities and action mechanism studies of transportan 10 and its analogues against multidrug‐resistant bacteria

Antimicrobial activities and action mechanism studies of transportan 10 and its analogues against multidrug‐resistant bacteria

Meningococcal resistance to antimicrobial peptides is mediated by bacterial adhesion and host cell RhoA and Cdc42 signalling

Novel antimicrobial peptide CPF‐C1 analogs with superior stabilities and activities against multidrug‐resistant bacteria

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