Rebecca O'Mahony
University College Dublin
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Publication
Featured researches published by Rebecca O'Mahony.
Letters in Applied Microbiology | 2007
Ciara Walsh; Geraldine Duffy; Nally P; Rebecca O'Mahony; D.A. McDowell; Séamus Fanning
Aims: To investigate the transfer of antibiotic resistance from a donor Salmonella Typhimurium DT104 strain to a recipient Escherichia coli K12 strain.
Letters in Applied Microbiology | 2010
O'Connor L; O'Leary M; Nola Leonard; Godinho M; O'Reilly C; Coffey L; John Egan; Rebecca O'Mahony
Aim: To enhance the information pertaining to the epidemiology of a collection of 378 Listeria spp. isolates obtained from several food‐processing plants in Ireland over a 3‐ year period (2004–2007).
Current Drug Targets | 2006
Teresa Quinn; Rebecca O'Mahony; Alan W. Baird; Denise Drudy; Paul Whyte; Séamus Fanning
Bacterial drug resistance represents one of the most crucial problems in present day antibacterial chemotherapy. Of particular concern to public health is the continuing worldwide epidemic spread of Salmonella enterica serovar Typhimurium phage type DT104 harbouring a genomic island called Salmonella genomic island I (SGI-1). This island contains an antibiotic gene cluster conferring resistance to ampicillin, chloramphenicol, florfenicol, streptomycin, sulfonamides and tetracyclines. These resistance genes are assembled in a mosaic pattern, indicative of several independent recombinational events. The mobility of SGI-1 coupled with the ability of various antibiotic resistance genes to be integrated and lost from the chromosomal resistance locus allows for the transfer of stable antibiotic resistance to most of the commonly used antibiotics and adaptation to new antibiotic challenges. This, coupled with the incidence of increasing fluoroquinolone resistance in these strains increases the risk of therapeutic failure in cases of life-threatening salmonellosis. Fluoroquinolone resistance has largely been attributed to mutations occurring in the genes coding for intracellular targets of these drugs. However, efflux by the AcrAB-TolC multi-drug efflux pump has recently been shown to directly contribute to fluoroquinolone resistance. Furthermore, the resistance to chloramphenicol-florfenicol and tetracyclines in DT104 isolates, is due to interaction between specific transporters for these antibiotics encoded by genes mapping to the SGI-1 and the AcrAB-TolC tripartite efflux pump. The potential for the use of efflux pump inhibitors to restore therapeutic efficacy to fluoroquinolones and other antibiotics offers an exciting developmental area for drug discovery.
International Journal of Food Microbiology | 2006
Denise Drudy; Michele O'Rourke; Mary Murphy; Niall Mullane; Rebecca O'Mahony; Lorraine Kelly; Matthias Fischer; Suhad Sanjaq; Pauline Shannon; Patrick G. Wall; M. O'Mahony; Paul Whyte; Séamus Fanning
Journal of Antimicrobial Chemotherapy | 2006
Denise Drudy; Teresa Quinn; Rebecca O'Mahony; Lorraine Kyne; Peadar O'Gaora; Séamus Fanning
Clinical Microbiology and Infection | 2007
Denise Drudy; N. Harnedy; Séamus Fanning; Rebecca O'Mahony; Lorraine Kyne
International Journal of Food Microbiology | 2006
C. Walsh; Geraldine Duffy; Rebecca O'Mahony; Séamus Fanning; I.S. Blair; D.A. McDowell
Microbial Drug Resistance | 2006
Rebecca O'Mahony; Teresa Quinn; Denise Drudy; Ciara Walsh; Paul Whyte; Salim Mattar; Séamus Fanning
Journal of Antimicrobial Chemotherapy | 2005
Y. Abbott; Rebecca O'Mahony; Nola Leonard; P. Joseph Quinn; Tanny van der Reijden; Lenie Dijkshoorn; Séamus Fanning
Fems Microbiology Letters | 2007
Brenda P. Murphy; Rebecca O'Mahony; James F. Buckley; Priscilla Shine; E. Fidelma Boyd; Deirdre Gilroy; Séamus Fanning