Q Fever Clinical Trial
Official title:
Cost-effectiveness of a Screening Strategy for Q Fever Among Pregnant Women in Risk Areas: a Clustered Randomized Controlled Trial
Q fever in the Netherlands is becoming more common. A Q fever infection is a serious threat
to certain risk groups,including pregnant women. Pregnant women are more often than the
general population asymptomatic. Studies from France show that an infection with Coxiella
burnetii may cause obstetric complications including spontaneous abortion, intrauterine
fetal death, intrauterine growth retardation and oligohydramnios.
The aim of this study is to assess the effectiveness and cost effectiveness of a
multidisciplinary screening program, whereby pregnant women in first line healthcare in
high-risk areas for Q fever are screened with a single blood sample during pregnancy. If
found positive for Q fever, advise for antibiotic treatment will follow as part of regular
healthcare. Treatment is therefore not part of the study protocol.
The results of this study will give more insights in the risks of asymptomatic Q fever in
pregnancy and the benefits and harms of a screening strategy during pregnancy. This study
will be used to give an evidence based advice to the Dutch minister of health on screening
for Q fever in pregnancy.
We will conduct a clustered randomized controlled trial among pregnant women within an area
of high transmission. The study participants will be recruited by the midwives in high risk
areas, defined by postal code from the RIVM. To inform the public in this area about the
study we will publish an article in local newspapers. The midwife centers will be randomized
to recruit pregnant women for either the control group or the intervention group. The
pregnant women will receive study information by mail using the midwives patients file. It
is estimated that approximately 10,000 eligible women live in the areas of transmission.
After written informed consent, they will start with the strategy for which the midwife
center is randomized.
Participants will be asked for a blood sample in their second trimester of pregnancy,
possibly combined with the routine structural ultrasound around 20 weeks of pregnancy to
minimize hospital visit. If participants are enrolled in their third trimester, they will
have their blood sampling as soon as possible after inclusion.
When taking part in the intervention group the sample will be tested immediately for Q
fever. If found positive for acute or chronic Q fever, patients have to be referred,
according to local protocol, to a hospital for further pregnancy monitoring and long-term
bacteriostatic treatment. Follow-up blood samples are required at 14 days, 3, 6 and 12
months after the first blood sampling as part of the standardized control of Q fever disease
to diagnose possible chronicity of infection. Furthermore, current routine for pregnant
women being treated with antibiotics against Q fever is to perform monthly blood analyses to
monitor treatment, and if the serological parameters descend, these controls are brought
back to once every two months. According to local protocol patients with Q fever have to
deliver in hospital. After pregnancy serology should be continued with check-ups at 3, 6 and
12 months following the current protocol. Furthermore, after delivery a bacteriocide
treatment with doxycycline or an alternative will be started by the specialist as part of
regular health care.
In the control arm the blood samples will be stored, and analyzed for Q fever after
delivery. If tested positive for Q fever after pregnancy antibiotics could be started if
needed as part of regular health care.
At baseline, a questionnaire will be administered to all participants asking about the
current pregnancy , pregnancy outcome of any previous pregnancies and demographics. Further
risk factors for pregnancy outcome will also be obtained such as smoking and drinking
behavior, risk-elevating comorbidities and medication use.
After delivery all relevant outcome data will be collected by questionnaires filled out by
the midwife, GP or specialist after delivery, notably the presence of obstetric
complications. One month after delivery or end of pregnancy, a last questionnaire will be
administered to the participant to verify potential long-term consequences of Q fever,
potential loss of income, health-related quality-of-life, fatigue and depressive symptoms.
Furthermore questions will be asked about the condition of the newborn and risk-accessing
questions for Q fever infection will be asked.
In the context of the secondary research questions an extra blood sample will be required,
and placentas as well as amniotic fluid will be collected after delivery. The latter will
only take place in a limited number of women and only if they gave birth in a hospital.
All participants will receive usual care and will be asked to visit the general practitioner
if symptoms of Q fever occur. He/she will start diagnostic research and treatment or will
refer the patient to the hospital. Furthermore, both arms have access to an expert team for
support.
;
Allocation: Randomized, Endpoint Classification: Efficacy Study, Intervention Model: Parallel Assignment, Masking: Open Label, Primary Purpose: Screening
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