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1                                              M. ulcerans causes Buruli ulcer, a severe human skin les
2                                              M. ulcerans is an opportunistic environmental pathogen;
3                                              M. ulcerans pathogenesis may not only be an individual a
4                                              M. ulcerans produces the polyketide-derived macrolide my
5                                              M. ulcerans was s.c. inoculated in three consanguine mou
6 rocess and did not confer protection against M. ulcerans.
7 ze the relationship between M. liflandii and M. ulcerans, strains were analyzed for the presence of t
8 se soils were Mycobacterium tuberculosis and M. ulcerans, M. tuberculosis (macrolide-lincosamide-stre
9 s revealed a significant association between M. ulcerans and Aedes notoscriptus.
10 ulation of responses such as effects between M. ulcerans, mycolactone, and S. aureus virulence that w
11                     The relationship between M. ulcerans, mycolactone, and Ae. aegypti further sugges
12 non-random, co-correlated clustering of both M. ulcerans positive possum excreta and human BU cases.
13 colactone, a lipid-like exotoxin secreted by M. ulcerans, inhibits the Sec61 translocon, driving tiss
14 rtance of innate immune responses to control M. ulcerans infection.
15 culture-positive samples were able to detect M. ulcerans DNA in all 21 culture-confirmed patients.
16  We evaluated the IS2404-based PCR to detect M. ulcerans DNA in tissue specimens from 143 BUD patient
17 ment membranes were disrupted in vivo during M. ulcerans infection in the mouse model.
18 stological diagnosis, a positive culture for M. ulcerans, or a smear positive for acid-fast bacilli (
19 specimens of which 11% were PCR positive for M. ulcerans-specific DNA.
20  single-nucleotide-polymorphism profiles for M. ulcerans detected in mosquitoes, possum excreta and h
21   Possums are a local wildlife reservoir for M. ulcerans and, although mosquitoes have been implicate
22 ective, simple, cheap and safe treatment for M. ulcerans disease.
23 terized a macrolide toxin, mycolactone, from M. ulcerans.
24                     One member of the genus, M. ulcerans, causes a necrotizing skin disease called Bu
25 rveys show that locales where possums harbor M. ulcerans overlap with human cases of BU, raising the
26                                     However, M. ulcerans infections are not limited to skin, and oste
27  was to assess using statistical modeling if M. ulcerans surveillance of possum excreta provided usef
28  Our data suggest that additional factors in M. ulcerans may be involved in Buruli ulcer pathogenesis
29                      At the molecular level, M. ulcerans is distinguished from M. marinum by the pres
30 rs of M. ulcerans-positive Ae. notoscriptus, M. ulcerans-positive possum excreta and Buruli ulcer cas
31 conducted extensive field survey analyses of M. ulcerans prevalence among mosquitoes in the Morningto
32         For 70 clinically diagnosed cases of M. ulcerans disease, the modified PCR was 98% sensitive
33 tistics revealed overlap between clusters of M. ulcerans-positive Ae. notoscriptus, M. ulcerans-posit
34  and histopathology in making a diagnosis of M. ulcerans disease in a field setting.
35 he difficulties associated with diagnosis of M. ulcerans osteomyelitis, with one-fourth of patients h
36 s important to understand the interaction of M. ulcerans with other bacteria encountered during skin
37                        This in vivo model of M. ulcerans infection now paves the way for new avenues
38 tter understanding of the pathophysiology of M. ulcerans infection, and the development of new therap
39 bstacle to understand the pathophysiology of M. ulcerans infection.
40  interval, 68 to 82%) showed the presence of M. ulcerans DNA by PCR.
41  Australian native possums are reservoirs of M. ulcerans and that they shed the bacteria in their fec
42 ationship between possum excreta shedding of M. ulcerans and humans developing BU.
43 nce of a toxin in the culture supernatant of M. ulcerans which causes a cytopathic effect on the mous
44  lipid toxin from the culture supernatant of M. ulcerans which is capable of causing the cytopathic e
45 ure of mycolactone F is identical to that of M. ulcerans mycolactones, but a unique side chain struct
46 s, but the specific route of transmission of M. ulcerans to humans remains unclear.
47 ost detailed field data in space and time on M. ulcerans and Buruli ulcer available today, we assess
48 ycolactone congeners from the human pathogen M. ulcerans, the frog pathogen Mycobacterium liflandii,
49 tients with polymerase chain reaction-proved M. ulcerans infections.
50  of combination antibiotic therapy for small M. ulcerans lesions.
51                           For selected small M. ulcerans lesions, 6 weeks may be as effective as 8 we
52 is on cultured cells but is less potent than M. ulcerans mycolactones.
53        Together, these data demonstrate that M. ulcerans infection causes systemic perturbations in t
54                                          The M. ulcerans genome strain has a deletion in RD1 and lack
55                                          The M. ulcerans toxin does not cause cell death but instead
56                               In contrast to M. ulcerans and conventional M. marinum, mycolactone F-p
57 cobacterium liflandii, is closely related to M. ulcerans and Mycobacterium marinum, and as further ev
58 e as all other mouse strains with respect to M. ulcerans infection, presented a spontaneous healing a
59 ts suggest that the human immune response to M. ulcerans is similar to that seen with some other myco
60  molecule appears so far to be restricted to M. ulcerans.
61                     Mycolactone is unique to M. ulcerans and an immunological Ag capture assay would
62  indicate Ae. notoscriptus probably transmit M. ulcerans in southeastern Australia and highlight mosq
63 cterial species isolated from areas in which M. ulcerans infection is endemic.
64                               Infection with M. ulcerans results in persistent severe necrosis withou
65 d radiological features in all patients with M. ulcerans infections with bone involvement, identified