Critical Illness Clinical Trial
Official title:
Anti-viral Prophylaxis for Prevention of Cytomegalovirus (CMV) Reactivation in Immunocompetent Patients in Critical Care
The purpose of this study is to determine whether reactivation of latent cytomegalovirus
infection in critically ill patients looked after in the intensive care unit can be
successfully and safely prevented using antiviral agents. Comparison is made between
standard care, and treatment with one of two different antiviral regimens:
valaciclovir/aciclovir, which has a favourable side effect profile but requires high dosage
to be effective, and valganciclovir/ganciclovir, which has more side effects, but has been
demonstrated to be effective in low dosage.
The primary hypothesis is that cytomegalovirus reactivation can be effectively suppressed
with antiviral prophylaxis.
Background:
* Cytomegalovirus (CMV) is a common virus which infects around half the UK population.
Infection is usually mild, but after infection the virus is never completely eradicated, and
may reactivate in ill health. Reactivation is most commonly seen in those with compromised
immune systems, such as people with advanced HIV infection, or whilst on immunosuppression
following organ transplantation. CMV reactivation in these patients can be life threatening.
There is evidence to support the use of antiviral medication in these groups of
immunosuppressed patients to prevent CMV reactivation, and their use is part of standard
therapy. There is increasing evidence demonstrating that a third of critically ill patients
will reactivate CMV, and these patients have as much as a doubled mortality.
Aims:
* This study is a proof of concept study designed to assess whether antiviral prophylaxis
can effectively and safely suppress CMV reactivation in CMV seropositive high risk
critically ill patients. Antiviral prophylaxis is currently not standard practice in
critical care units, and no previous trials of prophylaxis have been undertaken in this
setting. All commonly used antiviral agents have side effects, and it is important to
demonstrate their efficacy and safety in the critical care setting before undertaking a
large multicentre trial powered to identify mortality or morbidity differences with
prophylaxis. Intravenous ganciclovir, and its oral prodrug valganciclovir have been
effectively used as prophylaxis at low doses in immunosuppressed patients. Intravenous
aciclovir and its oral prodrug valaciclovir in high dosage have also been demonstrated to be
effective as prophylaxis in immunosuppressed patients. This study sets out to determine
whether their use in critically ill patients are both effective and safe.
Plan of Investigation:
* This is a prospective, randomised, open-label single centre study. Patients admitted to
the Queen Elizabeth Hospital Birmingham critical care unit, and identified by study criteria
to be at high risk of CMV reactivation will be assessed for inclusion into the study. Blood
will be analysed for CMV antibodies to establish eligibility. Recruited patients will be
randomised to receive high dose aciclovir/valaciclovir, or low dose
ganciclovir/valganciclovir for the duration of their critical care stay, for a maximum of 28
days, or to enter the control group receiving standard care. CMV viral load by polymerase
chain reaction (PCR) will be measured in blood, throat swab, urine, and sputum via
non-directed bronchiolar lavage (NDBL) twice weekly.
Potential Impact:
* Latent CMV infection is common, affecting around half of all adults in the UK. Evidence
demonstrates that a third of these patients will reactivate leading to CMV viraemia when
critically ill. Epidemiological data from multiple independent groups have identified a
doubling in mortality in this group, although a causal link between CMV reactivation and
mortality without a trial of antiviral drugs can not be assumed. From these figures, it is
estimated that 16.5% of critically ill patients (current mortality rates of around 40%) may
benefit from antiviral prophylaxis. Almost no patients are receiving prophylaxis or
screening for reactivation worldwide in this group. Demonstration of mortality or morbidity
improvements could potentially change worldwide intensive care practice.
;
Allocation: Randomized, Endpoint Classification: Safety/Efficacy Study, Intervention Model: Parallel Assignment, Masking: Open Label, Primary Purpose: Prevention
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