Awards Nomination 20+ Million Readerbase
PMC/PubMed Indexed Articles

The mPEG-PCL Copolymer for Selective Fermentation of Staphylococcus lugdunensis Against Candida parapsilosis in the Human Microbiome

Expression Profiling of LPS Responsive miRNA in Primary Human Macrophages

View More »

Google Scholar citation report
Citations : 9436

Journal of Microbial & Biochemical Technology received 9436 citations as per Google Scholar report

Flyer image
Journal of Microbial & Biochemical Technology peer review process verified at publons
Flyer image
Indexed In
  • Academic Journals Database
  • Genamics JournalSeek
  • Academic Keys
  • JournalTOCs
  • China National Knowledge Infrastructure (CNKI)
  • Scimago
  • Access to Global Online Research in Agriculture (AGORA)
  • Electronic Journals Library
  • RefSeek
  • Directory of Research Journal Indexing (DRJI)
  • Hamdard University
  • EBSCO A-Z
  • OCLC- WorldCat
  • SWB online catalog
  • Virtual Library of Biology (vifabio)
  • Publons
  • MIAR
  • University Grants Commission
  • Geneva Foundation for Medical Education and Research
  • Euro Pub
  • Google Scholar
View More
Useful Links
Share This Page
Journal Flyer
Flyer image
Open Access Journals
View More
Caenorhabditis elegans as a simple in vivo model for combinatorial therapy with thioridazine and dicloxacillin against infections with methicillin-resistant Staphylococcus aureus
12th World Congress on Biotechnology and Microbiology
June 28-29, 2018 | Amsterdam, Netherlands

Marianne O Poulsen, Lone Scholer, Anders Olsen, Hans Jorn Kolmos and Janne K Klitgaard

University of Southern Denmark, Denmark
Aalborg University, Denmark

Scientific Tracks Abstracts: J Microb Biochem Technol

Abstract:

The shortage of drugs active against methicillin-resistant Staphylococcus aureus (MRSA) is a growing clinical problem. In vitro studies indicate that the phenothiazine thioridazine (TZ) might enhance the activity of the β-lactam antibiotic dicloxacillin (DCX) to a level where MRSA is killed, but positive in vivo studies have yet to be performed. We have introduced Caenorhabditis elegans infected by MRSA as an in vivo model to test the effect of TZ as a helper drug in combination with DCX. Because TZ is an anthelmintic, initial experiments were carried out to define the thresholds of toxicity, determined by larval development, and induction of stress-response markers. No measurable stress effects were observed at the concentrations below 64 mg/L TZ. Of seven tested MRSA strains the most pathogenic strain (ATCC 33591) was chosen for treatment analysis. Full-grown C. elegans were exposed to the test strain for three days and subsequently treated with 8 mg/L DCX and 8 mg/L TZ for two days. This resulted in a 14-fold reduction in the intestinal MRSA load as compared with untreated controls. Each drug alone resulted in a two to threefold reduction in MRSA load. In conclusion, we have proved C. elegans as a simple model for testing synergy between TZ and DCX against MRSA. Moreover, we have shown that TZ enhances the activity of DCX in a simple in vivo host model as C. elegans leading to a decrease of bacterial load of MRSA in the nematode gut and intestine.

Biography :

Marianne O Poulsen is pursuing her PhD from Southern University of Denmark, Odense, Denmark. She is currently working at Odense University Hospital, Odense, Denmark and has published five papers.

E-mail: mpoulsen@health.sdu.dk

PDF HTML