Staphylococcus lugdunensis is a recently described coagulase-negative staphylococcus that has been associated with human infections, including nine reported cases of infective endocarditis. The present study describes 11 other cases of infective endocarditis caused by this organism. The infection occurred in patients whose mean age was 61 years and was community-acquired in most cases. A preexisting cardiac abnormality was present in eight patients. Three of the 11 infections involved prosthetic valves. Ten strains were susceptible to penicillin. The destructive course of the infection, the need for valve replacement, and the high mortality suggest that S. lugdunensis causes a virulent form of endocarditis.
The aim of the present study was to detect the
Staphylococcus aureus
delta-toxin using Whole-Cell (WC) Matrix Assisted Laser Desorption Ionization - Time-of-Flight (MALDI-TOF) mass spectrometry (MS), correlate delta-toxin expression with accessory gene regulator (
agr
) status, and assess the prevalence of
agr
deficiency in clinical isolates with and without resistance to methicillin and glycopeptides. The position of the delta-toxin peak in the mass spectrum was identified using purified delta-toxin and isogenic wild type and mutant strains for
agr-rna
III, which encodes delta-toxin. Correlation between delta-toxin production and
agr
RNAIII expression was assessed by northern blotting. A series of 168 consecutive clinical isolates and 23 unrelated glycopeptide-intermediate
S. aureus
strains (GISA/heterogeneous GISA) were then tested by WC-MALDI-TOF MS. The delta-toxin peak was detected at 3005±5 Thomson, as expected for the naturally formylated delta toxin, or at 3035±5 Thomson for its G10S variant. Multivariate analysis showed that chronicity of
S. aureus
infection and glycopeptide resistance were significantly associated with delta-toxin deficiency (
p
= 0.048; CI 95%: 1.01–10.24;
p
= 0.023; CI 95%: 1.20–12.76, respectively). In conclusion, the
S. aureus
delta-toxin was identified in the WC-MALDI-TOF MS spectrum generated during routine identification procedures. Consequently,
agr
status can potentially predict infectious complications and rationalise application of novel virulence factor-based therapies.
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