Your search keyword '"Raoult, D"' showing total 11 results

1. Q fever and pregnancy: disease, prevention, and strain specificity.

Author

Angelakis, E., Million, M., D'Amato, F., Rouli, L., Richet, H., Stein, A., Rolain, J.-M., and Raoult, D.

Subjects

Q fever, FETAL diseases, ANTIBIOTICS, COXIELLA burnetii, MISCARRIAGE, PREVENTION

Abstract

The link between fetal morbidity and Q fever and the necessity of long-term antibiotics for Coxiella burnetii infection during pregnancy have been recently questioned in the Netherlands, where the clone responsible for the Q fever outbreak harbors the QpH1 plasmid. In this context, we assessed pregnancy outcomes according to antibiotic administration in a new series and compared the plasmid type between isolates associated with abortion and other clinical isolates to determine if there is a link between genotype and abortion in humans. All French patients who received a diagnosis of Q fever during pregnancy at the French National Referral Centre for Q Fever from 2006 through July 2011 were included. On the other hand, the plasmid types of 160 clinical isolates, including seven isolates from patients who experienced an abortion, were compared. The differences between the QpDV and QpH1 plasmid sequences were analyzed. Acute Q fever was a cause of fetal morbidity, and the absence of long-term cotrimoxazole therapy was associated with fetal death ( p < 0.0001). Genotypic analysis showed that the QpDV plasmid was more frequent in isolates associated with abortion ( p = 0.03). A comparison of the plasmid sequences revealed that four QpDV proteins had no direct counterparts in QpH1, with two whose functions were not present in QpH1. The different obstetrical morbidity of C. burnetii relative to different geographical areas could be related to strain specificity, possibly based on differences in plasmid sequences, or to a failure of public health authorities to detect early miscarriages. [ABSTRACT FROM AUTHOR]

Published

2013

2. The hypervirulent Coxiella burnetii Guiana strain compared in silico, in vitro and in vivo to the Nine Mile and the German strain.

Author

Melenotte, C., Caputo, A., Bechah, Y., Lepidi, H., Terras, J., Kowalczewska, M., Di Pinto, F., Nappez, C., Raoult, D., and Brégeon, F.

Subjects

*COXIELLA burnetii, *Q fever, *WEIGHT loss

Abstract

Q fever epidemic outbreaks have been reported in French Guiana and in The Netherlands. To determine whether the C. burnetii strains involved in these epidemics had a peculiar virulence pattern, we compared the pathogenicity of the Guiana and the German strain (a clone of The Netherlands strain), in silico , in vitro , and in vivo versus the Nine Mile strain. The pan-genomes of the Guiana (Cb175), German (Z3055), and the referent Nine Mile (RSA 493) C. burnetii strains were compared. In vitro, the growth rate and the morphological presentation were compared. In vivo (SCID and Balb/c mice), weight loss, histological lesions, C. burnetii bacterial load in deep organs, and serological response were reported according to each C. burnetii strain studied. The Guiana strain had 77 times more missing genes and 12 times more unique genes than the German strain. The Guiana strain presented as large cell variants (LCVs) and led to the most pronounced fatality rate in SCID mice (100% at 4 weeks). The German strain presented as small cell variants (SCVs), and had an intermediate fatality rate (75% at 4 weeks). Both the Guiana and the German strains led to a significant higher serological response at 2 and 4 weeks post infection (p <0.05). The Guiana strain was the most virulent strain, followed by the German strain and the referent Nine Mile strain. Unique and missing genes could be implicated but further investigations are necessary to specify their role. [ABSTRACT FROM AUTHOR]

Published

2019

3. The genome of Coxiella burnetii Z3055, a clone linked to the Netherlands Q fever outbreaks, provides evidence for the role of drift in the emergence of epidemic clones.

Author

D'Amato F, Rouli L, Edouard S, Tyczka J, Million M, Robert C, Nguyen TT, and Raoult D

Subjects

Ankyrin Repeat genetics, Bacterial Proteins metabolism, Clone Cells, Coxiella burnetii classification, Coxiella burnetii pathogenicity, Genotype, Humans, INDEL Mutation, Membrane Proteins genetics, Membrane Proteins metabolism, Netherlands epidemiology, Phylogeny, Point Mutation, Q Fever microbiology, Q Fever pathology, Transcription Factors genetics, Transcription Factors metabolism, Bacterial Proteins genetics, Coxiella burnetii genetics, Disease Outbreaks, Genetic Drift, Genome, Bacterial, Q Fever epidemiology

Abstract

Coxiella burnetii is a pathogen causing Q fever. The aim of our work was to study Z3055, a strain that is genotypically related to the strain causing the Netherlands outbreak. We compared Z3055 to 5 other completed genomes available in GenBank. We calculated the blast score ratio (BSR) to analyze genetic differences among the strains. The ratio core genome/pangenome was 98% likely other bacteria with closed pangenomes. Differences between Z3055 and the reference NMI consisted only of point mutations and insertion/deletion (INDELs). Non-synonymous mutations significantly increased in genes coding for membrane proteins (16/156 vs 103/1757, bilateral Chi(2) test, p<0.05), ankyrin repeat domains containing proteins (2/9 vs 117/1904, bilateral Chi(2) test, p<0.05), transcription factors (7/53 vs 112/1860, bilateral Chi(2) test, p<0.05) and translation proteins (15/144 vs 109/1655, bilateral Chi(2) test, p<0.05). The evolution of this strain may have been driven by mutations in critical genes., (Copyright © 2014 Elsevier Ltd. All rights reserved.)

Published

2014

4. Comparison of the performance of IFA, CFA, and ELISA assays for the serodiagnosis of acute Q fever by quality assessment.

Author

Herremans T, Hogema BM, Nabuurs M, Peeters M, Wegdam-Blans M, Schneeberger P, Nijhuis C, Notermans DW, Galama J, Horrevorts A, van Loo IH, Vlaminckx B, Zaaijer HL, Koopmans MP, Berkhout H, Socolovschi C, Raoult D, Stenos J, Nicholson W, and Bijlmer H

Subjects

Australia, Complement Fixation Tests methods, Enzyme-Linked Immunosorbent Assay methods, Fluorescent Antibody Technique methods, France, Humans, International Cooperation, Netherlands, Serologic Tests methods, United States, Bacteriological Techniques methods, Q Fever diagnosis

Abstract

The indirect immunofluorescence assay (IFA) is considered the reference method for diagnosing Q fever, but serology is also performed by complement fixation assay (CFA) or enzyme-linked immunosorbent assay (ELISA). However, comparability between these assays is not clear, and therefore a quality assessment was performed. A total of 25 serum samples from negative controls, Q fever patients, and a serial diluted high-positive sample were analyzed in 10 Dutch laboratories. Six laboratories performed CFA, 5 performed IFA, and 5 performed ELISAs. Three international reference laboratories from Australia, France, and the USA also participated in this study. Qualitative values between laboratories using the same methods were within close range, and all 3 methods correctly identified acute Q fever patients. The IFA, ELISA, and CFA are all suitable serodiagnostic assays to diagnose acute Q fever, but the IFA remains an important tool in the follow-up of patients and in identifying patients at risk for developing chronic Q fever., (Copyright © 2013 Elsevier Inc. All rights reserved.)

Published

2013

5. Chronic Q fever: expert opinion versus literature analysis and consensus.

Author

Raoult D

Subjects

Communicable Disease Control methods, Consensus, Disease Outbreaks, Endocarditis pathology, Endocarditis virology, Histocytochemistry, Humans, Netherlands epidemiology, Q Fever epidemiology, Q Fever prevention & control, Radiography, Thoracic, Vasculitis pathology, Vasculitis virology, Endocarditis diagnosis, Expert Testimony, Q Fever diagnosis, Q Fever pathology, Vasculitis diagnosis

Abstract

Q fever has long been considered a rare disease. The extensive outbreak in the Netherlands generated a body of literature based solely on the consensus in the Netherlands. As a long-standing expert on Q fever, I offer my experience and recommendations to the E-CDC and the Dutch Q fever Consensus Group. My (biased) opinion is that experts deeply involved in the field continue to be useful in the management of outbreaks and can avoid decisions that produce an unfavorable progression in patients. Here, I propose that the definition of "chronic Q fever" be avoided and suggest a new score-based diagnosis for Q fever endocarditis and vascular infection., (Copyright © 2012 The British Infection Association. Published by Elsevier Ltd. All rights reserved.)

Published

2012

6. Epidemic genotype of Coxiella burnetii among goats, sheep, and humans in the Netherlands.

Author

Tilburg JJ, Roest HJ, Buffet S, Nabuurs-Franssen MH, Horrevorts AM, Raoult D, and Klaassen CH

Subjects

Animals, Goat Diseases epidemiology, Goat Diseases microbiology, Goats, Humans, Multilocus Sequence Typing, Netherlands epidemiology, Q Fever microbiology, Q Fever veterinary, Sheep, Sheep Diseases epidemiology, Sheep Diseases microbiology, Coxiella burnetii genetics, Genotype, Q Fever epidemiology

Published

2012

7. A case of rickettsialpox in Northern Europe.

Author

Renvoisé A, van't Wout JW, van der Schroeff JG, Beersma MF, and Raoult D

Subjects

Animals, Arthropod Vectors, Communicable Diseases, Emerging diagnosis, Communicable Diseases, Emerging microbiology, Humans, Male, Middle Aged, Mites microbiology, Netherlands, Rickettsia akari pathogenicity, Rickettsiaceae Infections diagnosis, Rickettsiaceae Infections microbiology

Abstract

We report the first case of rickettsialpox caused by Rickettsia akari in the Netherlands. The diagnosis was suspected based on clinical grounds and was confirmed by Western blot analysis with cross-adsorption. Because the arthropod vector (Liponyssoides sanguineus) is ubiquitous, we suspect that the disease is under-diagnosed in non-endemic areas., (Copyright © 2011 International Society for Infectious Diseases. All rights reserved.)

Published

2012

8. Chronic q Fever detection in the Netherlands.

Author

Raoult D, Million M, Thuny F, and Carrieri P

Subjects

Antibodies, Bacterial blood, Echocardiography methods, Humans, Immunoassay methods, Netherlands, Polymerase Chain Reaction methods, Predictive Value of Tests, Clinical Laboratory Techniques methods, Endocarditis, Bacterial diagnosis, Q Fever complications, Q Fever diagnosis

Published

2011

9. The Q fever epidemic in The Netherlands: history, onset, response and reflection.

Author

Roest HI, Tilburg JJ, van der Hoek W, Vellema P, van Zijderveld FG, Klaassen CH, and Raoult D

Subjects

Animals, Goat Diseases epidemiology, Goat Diseases prevention & control, Goats, History, 20th Century, History, 21st Century, Humans, Netherlands epidemiology, Q Fever history, Q Fever prevention & control, Sheep, Sheep Diseases epidemiology, Sheep Diseases prevention & control, Zoonoses epidemiology, Epidemics history, Epidemics prevention & control, Q Fever epidemiology

Abstract

The 2007-2009 human Q fever epidemic in The Netherlands attracted attention due to its magnitude and duration. The current epidemic and the historical background of Q fever in The Netherlands are reviewed according to national and international publications. Seroprevalence studies suggest that Q fever was endemic in The Netherlands several decades before the disease was diagnosed in dairy goats and dairy sheep. This was in 2005 and the increase in humans started in 2007. Q fever abortions were registered on 30 dairy goat and dairy sheep farms between 2005 and 2009. A total of 3523 human cases were notified between 2007 and 2009. Proximity to aborting small ruminants and high numbers of susceptible humans are probably the main causes of the human Q fever outbreak in The Netherlands. In general good monitoring and surveillance systems are necessary to assess the real magnitude of Q fever.

Published

2011

10. African tickbite fever in travelers, Swaziland.

Author

Oostvogel PM, van Doornum GJ, Ferreira R, Vink J, Fenollar F, and Raoult D

Subjects

Adolescent, Adult, Animals, Arachnid Vectors, Child, Child, Preschool, Eswatini epidemiology, Female, Humans, Male, Middle Aged, Netherlands epidemiology, Tick-Borne Diseases diagnosis, Bites and Stings microbiology, Rickettsiaceae Infections epidemiology, Tick-Borne Diseases epidemiology, Ticks microbiology, Travel

Published

2007

11. Q fever in children.

Author

Maltezou HC and Raoult D

Subjects

Animals, Animals, Domestic, Antibodies, Bacterial blood, Child, Disease Reservoirs, Endocarditis, Bacterial microbiology, Endocarditis, Bacterial pathology, Greece epidemiology, Humans, Immunochemistry, Netherlands epidemiology, Osteomyelitis pathology, Pneumonia microbiology, Pneumonia pathology, Q Fever blood, Q Fever epidemiology, Seroepidemiologic Studies, Spain epidemiology, Switzerland epidemiology, Zambia epidemiology, Coxiella burnetii immunology, Coxiella burnetii isolation & purification, Q Fever diagnosis

Abstract

Q fever is a zoonosis caused by Coxiella burnetii. Farm animals and pets are the main reservoirs of infection, and transmission to human beings is mainly accomplished through inhalation of contaminated aerosols. This illness is associated with a wide clinical spectrum, from asymptomatic or mildly symptomatic seroconversion to fatal disease. Q fever in children has been rarely reported. We reviewed published work on this topic. Seroepidemiological studies show that children are frequently exposed to C burnetii. However, children are less frequently symptomatic than adults following infection, and may have milder diseases. Using the standard diagnostic criteria, we identified 46 published paediatric cases only. Self-limited febrile illness and pneumonia were the most common manifestations of acute Q fever. Chronic disease manifested as endocarditis and osteomyelitis. A history of exposure to possible sources of infection with C burnetii in a child with a compatible infectious syndrome should prompt testing for Q fever. Studies are required to determine the spectrum of morbidity associated with Q fever during childhood.

Published

2002