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1 ellular bacterium and the causative agent of Q fever.
2 f developing a peptide mimic vaccine against Q fever.
3 eloping a safe and effective vaccine against Q fever.
4 differently modulated in men and women with Q fever.
5 ver but are lacking in patients with chronic Q fever.
6 a lions may be a risk factor for contracting Q fever.
7 l pathogen responsible for acute and chronic Q fever.
8 ich is associated with a case of human acute Q fever.
9 oonotic bacterial pathogen that causes human Q fever.
10 r bacterium and the causative agent of human Q fever.
11 d by or nonreactive in subjects with chronic Q fever.
12 he design of new generation vaccines against Q fever.
13 d the etiological agent of the human disease Q fever.
14 iella burnetii, the causative agent of human Q fever.
15 the clinical illness seen in human cases of Q fever.
16 he etiological agent of the zoonotic disease Q fever.
17 differential diagnosis of acute and chronic Q fever.
18 lular bacterium and the etiological agent of Q fever.
19 rnetii, the rickettsial organism that causes Q fever.
20 in the absence of additional data of chronic Q fever.
21 ck and humans with an acute disease known as Q fever.
22 iella burnetii, the causative agent of human Q fever.
23 g dynamic during early stages of human acute Q fever.
24 logical evolution and progression to chronic Q fever.
25 oms and/or serological confirmation of acute Q fever.
26 e etiological agent of the emerging zoonosis Q fever.
27 r Gram-negative bacterium which causes human Q fever.
28 iphospholipid dosages in patients with acute Q fever.
29 sorders have been described in patients with Q fever.
30 4 at the French National Referral Center for Q fever.
31 ith predisposition to development of chronic Q fever.
32 iella burnetii can lead to acute and chronic Q fever.
33 n an increased likelihood to develop chronic Q fever.
34 e bacterium that causes the zoonotic disease Q fever.
35 MYD88 (-938C>A) were associated with chronic Q fever.
36 contribute to the increased risk of chronic Q fever.
37 et need for a safe and effective vaccine for Q-fever.
38 tracellular parasite and the cause of query (Q) fever.
39 ntracellular bacterium that causes query, or Q fever, a disease that typically manifests as a severe
41 ar Gram-negative bacterium that causes human Q fever, a flu-like disease that can progress to chronic
43 Coxiella burnetii is the causative agent of Q fever, a zoonotic disease that threatens both human an
45 as used to investigate local inflammation in Q fever AAAs compared to atherosclerotic AAAs in aorta t
51 suspected patient-to-patient transmission of Q fever among pregnant women in a high-risk pregnancy un
52 ellular bacterial pathogen that causes human Q fever, an acute debilitating flu-like illness that can
53 lla burnetii is the bacterial agent of human Q fever, an acute, flu-like illness that can present as
59 ver vaccine in treated patients with chronic Q fever and demonstrated that they successfully mounted
61 We determined the interval between acute Q fever and diagnosis of chronic infection, assessed wha
62 a valuable technique in diagnosis of chronic Q fever and during follow-up, often leading to a change
63 nt aortic vegetation in a patient with acute Q fever and high levels of IgG anticardiolipin antibodie
64 were genotyped in 139 patients with chronic Q fever and in 220 controls with cardiovascular risk-fac
65 ligate intracellular bacterium, causes human Q fever and is considered a potential agent of bioterror
69 ntibiotic prophylaxis in patients with acute Q fever and valvulopathy has never been validated in a c
70 important in the pathophysiology of clinical Q fever and/or the induction of protective immunity.
72 ma, were up-regulated in patients with acute Q fever, and the expression levels of the late genes ALO
75 burnetii, the biothreat pathogen that causes Q fever, as in vitro propagation of this organism leads
79 omas are present in patients with resolutive Q fever but are lacking in patients with chronic Q fever
80 th Coxiella burnetii, the causative agent of Q fever, can result in life-threatening persistent infec
85 Linking a single dairy-goat farm to a human Q-fever cluster, we show widespread transmission, massiv
88 e, we sought to determine how commonly acute Q fever could cause valvular vegetations associated with
89 igate intracellular bacterial agent of human Q fever, Coxiella burnetii, has a remarkable ability to
93 -5% of all acute Q fever infections, chronic Q fever develops, mostly manifesting as endocarditis, in
95 lop classic serological criteria for chronic Q fever diagnosis in the absence of additional data of c
97 ith classic serological criteria for chronic Q fever diagnosis remained asymptomatic despite no speci
98 ria: (1) patients aged >=18 years; (2) acute Q fever diagnosis, defined as suggestive symptoms in the
103 tes of Coxiella burnetii, the cause of human Q fever, display different phenotypes with respect to in
105 lla burnetii is the causative agent of human Q fever, eliciting symptoms that range from acute fever
106 U]) were independently associated with acute Q fever endocarditis (odds ratio [OR], 2.7 [95% confiden
108 que opportunity for early diagnosis of acute Q fever endocarditis and for the prevention of persisten
109 fevers for 14 months who was diagnosed with Q fever endocarditis based on an extremely high antibody
110 of clinical and epidemiological features of Q fever endocarditis collected through passive surveilla
117 (TTE) identified a valvular lesion of acute Q fever endocarditis without underlying valvulopathy.
118 We identified a new clinical entity, acute Q fever endocarditis, defined as valvular lesion potenti
119 ults, 9 (1.2%) were considered to have acute Q fever endocarditis, none of whom had a previously know
126 onsidered in the management of patients with Q fever, especially those with persistent focalized infe
127 Coxiella burnetii, the causative agent of Q fever, establishes a unique lysosome-derived intracell
128 perform microbiological testing for chronic Q fever even many years after an outbreak or acute Q fev
131 uman cases and occurred in a region that was Q-fever free before 2009, providing a unique quasi-exper
132 d in the French National Referral Center for Q fever from January 2007 to December 2011 were included
133 iella burnetii, the causative agent of human Q fever, has been considered a prototypical obligate int
137 the Gram-negative bacterium responsible for Q fever in humans and coxiellosis in domesticated agricu
139 haride (LPS), is highly virulent, and causes Q fever in humans and pathology in experimental animals.
140 rRNA gene of Coxiella burnetii, the agent of Q fever in humans, contains an unusually high number of
141 , the etiological agent of acute and chronic Q fever in humans, is a naturally intracellular pathogen
142 Coxiella burnetii, the etiological agent of Q fever in humans, is an intracellular pathogen that rep
145 ides new insights into the seroprevalence of Q fever in large ruminants across seven studied district
147 s is considered to be a late complication of Q fever in patients with preexisting valvular heart dise
150 was to describe the natural history of acute Q fever, including its clinical and serological evolutio
152 ignificant disabilities, related to an acute Q fever infection, without other somatic or psychiatric
154 a, Coxiella burnetii, the etiologic agent of Q fever, inhabits a spacious acidified intracellular vac
165 istent focalized infection forms after acute Q fever is extremely low and does not justify the use of
172 Coxiella burnetii, the etiological agent of Q fever, is a Gram-negative bacterium transmitted to hum
173 Coxiella burnetii, the etiological agent of Q fever, is a gram-negative obligate intracellular bacte
174 Coxiella burnetii, the causative agent of Q fever, is a human intracellular pathogen that utilizes
175 Coxiella burnetii, the etiological agent of Q fever, is a small, Gram-negative, obligate intracellul
177 Coxiella burnetii, the causative agent of Q fever, is a zoonotic disease with potentially life-thr
179 Coxiella burnetii, the causative agent of Q fever, is an emerging pathogen that has the potential
180 Coxiella burnetii, the etiological agent of Q fever, is an obligate intracellular bacterium prolifer
182 Growth of Coxiella burnetii, the agent of Q fever, is strictly limited to colonization of a viable
183 were comparable to those seen in human acute Q fever, making this an accurate and valuable animal mod
185 strated that individuals treated for chronic Q fever mount a broader ex vivo response to class II epi
186 lla burnetii, the etiological agent of human Q fever, occupies a unique niche inside the host cell, w
187 lar survival are poorly defined and a recent Q fever outbreak in the Netherlands emphasizes the need
188 Successful host cell colonization by the Q fever pathogen, Coxiella burnetii, requires translocat
189 g the LPA delivery system to study pulmonary Q fever pathogenesis as well as designing vaccine counte
190 ected biomarkers were assessed in blood from Q fever patients by real-time reverse transcription poly
191 An excess risk of DLBCL and FL was found in Q fever patients compared with the general population (S
200 urately identifies patients with low risk of Q fever pneumonia and may help physicians to make more r
201 bjectives were to estimate the prevalence of Q fever pneumonia and to build a prediction rule to iden
202 a prediction rule to identify patients with Q fever pneumonia for empirical antibiotic guidance.
203 -one patients with CAP were included and the Q fever pneumonia prevalence was 24.4% (95% confidence i
204 th a predictive score </=3 had a low risk of Q fever pneumonia with a negative predictive value of 0.
209 ellular bacterial pathogen Coxiella burnetii Q fever presents with acute flu-like and pulmonary sympt
210 ogenesis and genetics and aid development of Q fever preventatives such as an effective subunit vacci
216 Coxiella burnetii, the etiologic agent of Q fever, replicates in an intracellular phagolysosome wi
217 xiella burnetii (Cb), the causative agent of Q fever, replicates within host macrophages by modulatin
219 unity against a murine model of experimental Q fever requires MHC-II-restricted, CD4(+) T cell-depend
220 ion by Coxiella burnetii, the cause of human Q fever, requires pathogen-directed biogenesis of a larg
222 human patients who had recovered from acute Q fever, respectively, revealed both unique SCV/LCV anti
224 llular pathogens that cause diseases such as Q fever, rickettsioses, brucelloses, tularemia, and othe
225 Coxiella burnetii, the causative agent of Q fever, secretes bacterial effector proteins via its Ty
226 The incidence of seroconversion to a chronic Q fever serological pattern, defined as phase I IgG tite
227 is, with directed serological testing (i.e., Q fever serology, Bartonella serology) in culture-negati
229 t (ELISpot) assays, individuals with chronic Q fever showed strong class II epitope-specific response
231 We observed a lymphoma in a patient with Q fever that prompted us to investigate the association
237 epitopes for a novel T-cell targeted subunit Q fever vaccine in treated patients with chronic Q fever
240 ular complications, we aimed to detect acute Q fever valvular injury to improve therapeutic managemen
243 In the French national reference center for Q fever, we prospectively collected data from patients w
244 single-nucleotide polymorphisms and chronic Q fever were assessed by means of univariate logistic re
245 ological follow-up was performed after acute Q fever were diagnosed less often after this 2-year inte
250 ls treated for persistent infection (chronic Q fever) whether they recognize the same set of epitopes
251 ll adult Dutch patients suspected of chronic Q fever who were diagnosed since 2007 were retrospective
252 Approximately 20% of patients with acute Q fever will develop chronic fatigue, referred to as Q f