A novel resistance gene, named poxtA, encoding a protein of the antibiotic resistance (ARE) ABC-F lineage, was identified in the genome of an MRSA of clinical origin. PoxtA can confer decreased susceptibility to phenicols, oxazolidinones and tetracyclines and is associated with a putative mobile element that could contribute to its horizontal dissemination.
Candidemia and invasive candidiasis are the most common healthcare-associated invasive fungal infections, with a crude mortality rate of 25-50%. Candida albicans remains the most frequent etiology, followed by C. glabrata, C. parapsilosis and C. tropicalis. With the exception of a limited number of species (ie: C. krusei, C. glabrata and rare Candida species), resistance to fluconazole and other triazoles are quite uncommon. However, recently fluconazoleresistant C. parapsilosis, echinocandin-resistant C. glabrata and the multidrug resistant C. auris have emerged. Resistance to amphotericin B is even more rare due to the reduced fitness of resistant isolates. The mechanisms of antifungal resistance in Candida (altered drug-target interactions, reduced cellular drug concentrations, and physical barriers associated with biofilms) are analyzed.The choice of the antifungal therapy for candidemia must take into account several factors such as type of patient, presence of devices, severity of illness, recent exposure to antifungals, local epidemiology, organs involvement, and Candida species. The first-line therapy in nonneutropenic critical patient is an echinocandin switching to fluconazole in clinically stable patients with negative blood cultures and azole susceptible isolate. Similarly, an echinocandin is the drug of choice also in neutropenic patients. The treatment duration is 14 days after the first negative blood culture or longer in cases of organ involvement. An early removal of vascular catheter improves the outcome. The promising results of new antifungal molecules, such as the terpenoid derivative ibrexafungerp, the novel echinocandin with an enhanced half-life rezafungin, oteseconazole and fosmanogepix, representative of new classes of antifungals, are discussed.
Enterococcus faecium E35048, a bloodstream isolate from Italy, was
the first strain where the oxazolidinone resistance gene optrA was
detected outside China. The strain was also positive for the oxazolidinone resistance
gene cfr. WGS analysis revealed that the two genes were linked (23.1
kb apart), being co-carried by a 41,816-bp plasmid that was named pE35048-oc. This
plasmid also carried the macrolide resistance gene erm(B) and a
backbone related to that of the well-known Enterococcus faecalis
plasmid pRE25 (identity 96%, coverage 65%). The optrA gene context
was original, optrA being part of a composite transposon, named
Tn6628, which was integrated into the gene encoding for the
ζ toxin protein (orf19 of pRE25). The cfr
gene was flanked by two ISEnfa5 insertion sequences and the element
was inserted into an lnu(E) gene. Both optrA and
cfr contexts were excisable. pE35048-oc could not be transferred
to enterococcal recipients by conjugation or transformation. A plasmid-cured
derivative of E. faecium E35048 was obtained following growth at
42°C, and the complete loss of pE35048-oc was confirmed by WGS. pE35048-oc
exhibited some similarity but also notable differences from pEF12-0805, a recently
described enterococcal plasmid from human E. faecium also
co-carrying optrA and cfr; conversely it was
completely unrelated to other optrA- and
cfr-carrying plasmids from Staphylococcus sciuri.
The optrA-cfr linkage is a matter of concern since
it could herald the possibility of a co-spread of the two genes, both involved in
resistance to last resort agents such as the oxazolidinones.
scite is a Brooklyn-based organization that helps researchers better discover and understand research articles through Smart Citations–citations that display the context of the citation and describe whether the article provides supporting or contrasting evidence. scite is used by students and researchers from around the world and is funded in part by the National Science Foundation and the National Institute on Drug Abuse of the National Institutes of Health.