Stress, Physiological Clinical Trial
— RECYSTRESSOfficial title:
Observational Study of CMV Reactivation in Immunocompetent Children and Adult ICU Patients
Background. Human herpes viruses establish lifelong latency after primary infection and may
reactivate in immunosuppressed patients causing significant morbidity and mortality. In
immunocompetent patients, although reactivation may occur disease development is deterred by
the competent host immune response. Recent studies indicate that approximately one third of
CMV seropositive immunocompetent ICU patients present with CMV reactivation associated with
poor outcome, potentially secondary to the stress incurred. CMV reactivation among
immunocompetent critically ill children has not been assessed.
Study Hypothesis: Identifiable risk factors associated with CMV reactivation exist and may be
used for future assessment of antiviral prophylaxis administration.
Aim: Primary aim is to identify risk factors associated with CMV reactivation and poor
outcome in immunocompetent children and adults under severe stress. Whether CMV reactivation
occurs in critically ill children and its clinical implications remains to be determined.
Secondary aim is to study the role of cellular signaling pathways of inflammation and
specific adaptive immunity during this process.
Work packages: A multicenter observational prospective study will be conducted among CMV
seropositive pediatric and adult ICU patients. Patient clinical progress, laboratory
findings, management, and complications will be recorded during the 28 days following ICU
admission. Salivary free cortisol levels, plasma catecholamines, and serum cytokines levels
will be measured to assess stress. CMV reactivation will be evaluated weekly by detecting
CMV-DNA in peripheral blood and bronchial wash samples with real-time PCR. In a patient
subsample, the nuclear factor κB and intracellular GC receptor will be measured in peripheral
blood monocytes to study cellular signaling pathways of inflammation. The adaptive immune
response to CMV infection following in vitro viral polypeptide stimulation will be
prospectively examined in a subset of patients.
Expected Results: The study will provide original data on critically ill children. Further
knowledge regarding risk factors associated with CMV reactivation and poor outcome will be
accumulated. Novel information regarding the role of cellular inflammation and specific
adaptive immune responses during CMV reactivation will be gathered.
Status | Unknown status |
Enrollment | 275 |
Est. completion date | June 2015 |
Est. primary completion date | May 2015 |
Accepts healthy volunteers | No |
Gender | All |
Age group | 2 Years and older |
Eligibility |
Inclusion Criteria: - previously healthy children 5-16 years old (group A) and adults (group B) - no known immunosuppression (secondary to underlying disease or medications), - residence near the ICU (ability to return for follow up on day 28 post admission) - availability of patient guardian or first degree relative willing to provide written informed consent Exclusion Criteria: - imminent death - expected ICU stay <48 hours - intubation prior to admission (in a different center) for >48 hours |
Country | Name | City | State |
---|---|---|---|
Greece | University of Athens | Athens |
Lead Sponsor | Collaborator |
---|---|
University of Athens |
Greece,
Limaye AP, Kirby KA, Rubenfeld GD, Leisenring WM, Bulger EM, Neff MJ, Gibran NS, Huang ML, Santo Hayes TK, Corey L, Boeckh M. Cytomegalovirus reactivation in critically ill immunocompetent patients. JAMA. 2008 Jul 23;300(4):413-22. doi: 10.1001/jama.300.4.413. — View Citation
Type | Measure | Description | Time frame | Safety issue |
---|---|---|---|---|
Primary | Risk factors associated with CMV reactivation in critically ill children and adults | 28 days | ||
Secondary | Role of cellular signaling and adaptive immunity | 7 days |
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