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Moving from Q fever to C. burnetii infection

Published online by Cambridge University Press:  26 November 2015

C. ELDIN  and
D. RAOULT
C. ELDIN
Affiliation:
Unité de Recherche sur les Maladies Infectieuses et Tropicales Emergentes, Faculté de Médecine, Aix-Marseille Université, Marseille, France
D. RAOULT*
Affiliation:
Unité de Recherche sur les Maladies Infectieuses et Tropicales Emergentes, Faculté de Médecine, Aix-Marseille Université, Marseille, France
*
*Author for correspondence: D. Raoult (Email: [email protected])
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Abstract

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Type
Correspondence
Information
Epidemiology & Infection , Volume 144 , Issue 6 , April 2016 , pp. 1163 - 1164
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Copyright
Copyright © Cambridge University Press 2015 

To the Editor

This paper by Van Loenhout et al. [Reference Van Loenhout1] gives us the opportunity to discuss the accuracy of the EU case definition for notification of Q fever, and more generally the current nomenclature of this infection.

In the EU definition, cases of ‘acute Q fever’ are defined by the combination of clinical symptoms (fever, pneumonia, hepatitis) and laboratory criteria. As stated by the authors, the major limitation of this classification is that it probably significantly underestimated the number of cases of Coxiella burnetii primary infection during The Netherlands epidemic. Interestingly, the use of this definition can be used to compare symptomatic (notified as ‘acute Q fever’) and asymptomatic or poorly symptomatic (non-notified) C. burnetii primary infections. The main significant differences between these two groups are age and sex, with symptomatic patients being significantly older and more often men than asymptomatic or poorly symptomatic patients. This result confirms what has already been described in previous studies: age and sex are the two major determinants of clinical manifestations of C. burnetii primary infection, with older men being more frequently symptomatic than young women, pregnant women and children [Reference Tissot-Dupont2Reference Leone4]. Moreover, the results of Van Loenhout et al. confirm that there is no correlation between clinical manifestations of C. burnetii primary infection and the long-term consequences of the infection, with no significant difference in long-term health status between notified and non-notified patients [Reference Million and Raoult5].

These elements bring new arguments for an updated nosography of C. burnetii infection. We consider that the natural history of C. burnetii infection is quite close to what is observed in Mycobacterium tuberculosis infection (TB), so that the old simplistic classification of ‘acute’ and ‘chronic Q fever’ is no longer accurate. In TB, the primary infection can be symptomatic or not. If left untreated, and in the presence of host factors like immunosuppression or age, long-term complications of the infection can occur and affect different organs (Pott's disease, meningitis, miliary, lymphadenitis). Localization of the focus of infection is necessary to determine treatment duration and prognosis. In the case of C. burnetii, the primary infection can be symptomatic (currently described as ‘acute Q fever’) or not, depending on two major determinants: the strain involved [Reference D'Amato6] and the patient's susceptibilities (age, sex, pregnancy, immunosuppression) [Reference Raoult7]. Then, long-term complications can be classified into two main entities: persistent focalized infections and fatigue syndrome (without an identified focus of infection). These complications are not linked to the severity of the primary infection but mainly to host factors. There is no ‘chronic Q fever’ with multiplying C. burnetii without a focus of infection and different focalized persistent infections have different risk factors, prognoses and treatments. C. burnetii endocarditis occurs in subjects with pre-existing valvulopathy, and is associated with high IgG anticardiolipin antibody titres during primary infection [Reference Million8]. Its prognosis has improved thanks to prophylaxis, early diagnosis and treatment [Reference Million9]. Vascular infections occur in patients with pre-existing aneurysm or vascular grafts, requires surgical treatment and still has a very poor prognosis [Reference Botelho-Nevers10]. Conversely, no death has been reported to date in patients with C. burnetii osteoarticular infections [Reference Million11, Reference Angelakis12]. C.burnetii infection during pregnancy is frequently asymptomatic but can lead to severe obstetrical complications like fetal death and malformations [Reference Million13]. Finally, we recently demonstrated that C. burnetii persistent lymphadenitis can lead to lymphoma [Reference Melenotte14].

Regarding fatigue syndrome, a disease without evidence of C. burnetii multiplication and not treatable with antibiotics, this paper demonstrates that it is equally frequent after C. burnetii symptomatic and asymptomatic primary infections. Recently, another study from The Netherlands on ‘Q fever fatigue syndrome’ used the definition of the National Dutch consensus guidelines, which is cited as follows: ‘a sudden onset of fatigue related to a symptomatic acute Q fever infection’ [Reference Keijmel15]. Given the data from Van Loenhout et al. [Reference Van Loenhout1], this definition is obviously misleading. Further studies using a definition allowing detection of fatigue syndrome after C. burnetii asymptomatic primary infections are necessary to reach a conclusion on the actual occurrence and risk factors of this syndrome.

In conclusion, the work of Van Loenhout et al. stresses the need for moving from the old unspecific ‘Q fever’ nomenclature to more precise definitions of the different forms of C. burnetii infection in order to establish efficient public health strategies. In epidemic situations like the one experienced in The Netherlands, detection and follow-up of asymptomatic C. burnetii primary infections should be a priority, especially in high-risk patients (valvulopathy, vascular aneurysms or prosthesis, osteoarticular prosthesis, pregnant women) to detect and prevent the development of both focalized persistent infections and fatigue syndrome.

Declaration of Interest

None.

References

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