Acute Respiratory Distress Syndrome Clinical Trial
— GRAILOfficial title:
A Randomized Double-Blind Placebo-Controlled Trial of Ganciclovir/Valganciclovir for Prevention of Cytomegalovirus Reactivation in Acute Injury of the Lung and Respiratory Failure (The GRAIL Study)
Verified date | July 2018 |
Source | Fred Hutchinson Cancer Research Center |
Contact | n/a |
Is FDA regulated | No |
Health authority | |
Study type | Interventional |
To evaluate whether administration of ganciclovir reduces serum IL-6 levels (i.e. reduction
between baseline and 14 days post-randomization) in immunocompetent adults with severe sepsis
or trauma associated respiratory failure.
Primary Hypotheses:
- In CMV seropositive adults with severe sepsis or trauma , pulmonary and systemic CMV
reactivation amplifies and perpetuates both lung and systemic inflammation mediated through
specific cytokines, and contributes to pulmonary injury and multiorgan system failure,
AND
- Prevention of CMV reactivation with ganciclovir decreases pulmonary and systemic
inflammatory cytokines that are important in the pathogenesis of sepsis and trauma related
complications.
Status | Completed |
Enrollment | 160 |
Est. completion date | October 28, 2016 |
Est. primary completion date | June 17, 2016 |
Accepts healthy volunteers | No |
Gender | All |
Age group | 18 Years and older |
Eligibility |
Inclusion Criteria: 1. Subject/next of kin informed consent 2. Age >= 18 years 3. CMV IgG seropositive. The following tests are acceptable: - FDA licensed test in a local lab approved by the coordinating center (FHCRC, Seattle, WA). - Test in central study lab (ARUP, Salt Lake City, UT) - A report that patient has previously been tested and found to be CMV seropositive at any time (a credible next of kin report is acceptable; confirmatory test will be done but results are not required for randomization) 4. Intubated and requiring mechanical positive pressure ventilation (including Acute Lung Injury/ARDS (EA Consensus Definition)) 5. Meets criteria for either: 1. Severe sepsis criteria (as defined in appendix G) within a 24-hour time period within the 120 hour window OR 2. Trauma with respiratory failure and an ISS score > 15 within a 24 hour time period, and within the 120 hour window (where mechanical ventilation is not due solely to a head injury) 6. On the day of randomization (by local criteria): - Not eligible for SBT (use of sedation and/or vasopressor does not specifically contraindicate SBT),or - Failed SBT Exclusion Criteria: 1. BMI > 60 (1st weight during hospital admission) 2. Known or suspected immunosuppression, including: - HIV+ (i.e. prior positive test or clinical signs of suspicion of HIV/AIDS; a negative HIV test is not required for enrollment) - stem cell transplantation: - within 6 months after autologous transplantation or - within 1 years after allogeneic transplantation (regardless of immunosuppression) - greater than 1 year of allogeneic transplantation if still taking systemic immunosuppression or prophylactic antibiotics (e.g. for chronic graft versus host disease) Note: if details of stem cell transplantation are unknown, patients who do not take systemic immunosuppression and do not take anti-infective prophylaxis are acceptable for enrollment and randomization. - solid organ transplantation with receipt of systemic immunosuppression (any time). - cytotoxic anti-cancer chemotherapy within the past three months (Note: next-of-kin estimate is acceptable). - congenital immunodeficiency requiring antimicrobial prophylaxis (e.g. TMP-SMX, dapsone, antifungal drugs, intravenous immunoglobulin). - receipt of one or more of the following in the indicated time period: - within 6 months: alemtuzumab, antithymocyte/antilymphocyte antibodies - within 3 months: immunomodulator therapy (TNF-alpha antagonist, rituximab, tocilizumab, IL1 receptor antagonist and other biologics) - within 30 days: - corticosteroids > 10 mg/day (chronic administration, daily average over the time period) - topical steroids are permissible - use of hydrocortisone in "stress doses" up to 100 mg four times a day (400mg/daily) for up to 4 days prior to randomization is permissible - use of temporary short-term (up to 2 weeks) increased doses of systemic steroids (up tp 1 mg/kg) for exacerbation of chronic conditions are permissible. - methotrexate (> 10.0 mg/week) - azathioprine (> 75 mg/day) Note: if no information on these agents is available in the history and no direct or indirect evidence exists from the history that any condition exists that requires treatment with these agents (based on the investigator's assessment), the subject may be enrolled. For all drug information, next-of-kin estimates are acceptable. See Appendix D for commonly prescribed immunosuppressive agents. 3. Expected to survive < 72 hours (in the opinion of the investigator) 4. Has been hospitalized for > 120 hours (subjects who are transferred from a chronic care ward, such as a rehabilitation unit, with an acute event are acceptable). 5. Pregnant or breastfeeding (either currently or expected within one month). Note: for women of childbearing age (18-60 years, unless documentation of surgical sterilization [hysterectomy, tubal ligation, oophorectomy]), if a pregnancy test has not been done as part of initial ICU admission work-up, it will be ordered stat and documented to be negative before randomization. Both urine and blood tests are acceptable. 6. Absolute neutrophil count < 1,000/mm3 (if no ANC value is available, the WBC must be > 2500/mm3) 7. Use of cidofovir within seven (7) days of patient randomization. The use of the following antivirals is permitted under the following conditions: - Ganciclovir, foscarnet, high-dose acyclovir, or valacyclovir until the day of randomization - Acyclovir as empiric therapy for central nervous system HSV or VZV infection until the diagnosis can be excluded - For enrolled patients during the active study drug phase, acyclovir, famciclovir, valacyclovir for treatment of HSV or VZV infection as clinically indicated. 8. Currently enrolled in an interventional trial of an investigational therapeutic agent known or suspected to have anti-CMV activity, or to be associated with significant known hematologic toxicity (Note: confirm eligibility with one of the study medical directors at the coordinating site). 9. At baseline patients who have both a tracheostomy, and have been on continuous 24-hour chronic mechanical ventilation. 10. Patients with Child Class C Cirrhosis. 11. Patients with pre-existing interstitial lung disease. |
Country | Name | City | State |
---|---|---|---|
United States | University of Michigan | Ann Arbor | Michigan |
United States | University of Vermont College of Medicine | Burlington | Vermont |
United States | University of Virginia | Charlottesville | Virginia |
United States | Northwestern University | Chicago | Illinois |
United States | The Cleveland Clinic Foundation | Cleveland | Ohio |
United States | Ohio State University Medical Center | Columbus | Ohio |
United States | University of Colorado / National Jewish Health / Swedish Medical Center | Denver | Colorado |
United States | University of Pennsylvania Medical Center | Philadelphia | Pennsylvania |
United States | University of Pittsburgh Medical Center | Pittsburgh | Pennsylvania |
United States | The Oregon Clinic | Portland | Oregon |
United States | Harborview Medical Center | Seattle | Washington |
United States | University of Washington Medical Center / Harborview Medical Center | Seattle | Washington |
United States | Baystate Critical Care Medicine / Tufts University School of Medicine | Springfield | Massachusetts |
United States | Wakeforest University, School of Medicine | Winston-Salem | North Carolina |
Lead Sponsor | Collaborator |
---|---|
Fred Hutchinson Cancer Research Center | Genentech, Inc., National Heart, Lung, and Blood Institute (NHLBI) |
United States,
Limaye AP, Stapleton RD, Peng L, Gunn SR, Kimball LE, Hyzy R, Exline MC, Files DC, Morris PE, Frankel SK, Mikkelsen ME, Hite D, Enfield KB, Steingrub J, O'Brien J, Parsons PE, Cuschieri J, Wunderink RG, Hotchkin DL, Chen YQ, Rubenfeld GD, Boeckh M. Effect — View Citation
Type | Measure | Description | Time frame | Safety issue |
---|---|---|---|---|
Primary | Serum IL-6 Level | Change between baseline and 14 days post-randomization between placebo & ganciclovir groups | Baseline and Day 14 | |
Secondary | Number of Participants With CMV Reactivation at 28 Days in Plasma | Number of participants in baseline negatives with CMV reactivation at any level at day 28 | at 28 days post-randomization | |
Secondary | BAL Levels of IL-6 | Levels of IL-6 from BALs at 7 days post-randomization | at 7 days post-randomization | |
Secondary | Number of Participants With Organ System Failure at 14 Days | Number of participants experiencing organ system failure at 14 days | at 14 days post-randomization | |
Secondary | Number of Days Alive and Not in the ICU | Number of ICU days alive and not in the ICU by day 28 | by 28 days post-randomization | |
Secondary | CMV Disease | Need to be biopsy-proven | by 180 days post-randomization | |
Secondary | Grade 3 AEs or Higher | Number of patients with greater than one AE of grade 3 or more | by 35 days post-randomization | |
Secondary | SF-36 Health Survey | Physical Component Summary of SF-36. The SF-36 consists of eight scaled scores, which are the weighted sums of the questions in their section. Each scale is directly transformed into a 0-100 scale on the assumption that each question carries equal weight. The lower the score the more disability. The higher the score the less disability. | at 1 day post-randomization | |
Secondary | Incidence of CMV Reactivation >1,000 IU Per mL at Day 28 in Plasma | Number of participants with CMV reactivation >1,000 IU per mL at day 28 in plasma | at 28 days post-randomization | |
Secondary | Incidence of CMV Reactivation at Any Level at 28 Days in Throat | CMV reactivation in baseline negatives at any level at day 28 in throat | at 28 days post-randomization | |
Secondary | Incidence of CMV Reactivation >1,000 IU Per mL at 28 Days in Throat | Number of participants with CMV reactivation >1,000 IU per mL at day 28 in throat | at 28 days post-randomization | |
Secondary | CMV AUC in Blood | CMV AUC in blood from day 0 to day 28 | Day 0 to 28 days post-randomization | |
Secondary | CMV AUC in Throat | CMV AUC in Throat from day 0 to day 28 | Day 0 to 28 days post-randomization | |
Secondary | CMV Peak Viral Load in Blood | CMV Peak Viremia in blood at day 28 | at 28 days post-randomization | |
Secondary | BAL Levels of IL-8 | Levels of IL-8 in BALs at day 7 | at 7 days post-randomization | |
Secondary | BAL Levels of TNFa | Levels of TNFa in BALs at day 7 | at 7 days post-randomization | |
Secondary | Plasma Levels of IL-6 | Plasma levels of IL-6. | at 7 days post-randomization | |
Secondary | Plasma Levels of IL-8 | Levels of IL-8 in plasma at day 7 | at 7 days post-randomization | |
Secondary | Plasma Levels of TNF a | Plasma levels of TNF a at day 7.Cytokines are summarized on log 10 scale. When logged value is negative, the raw value would be less than 1. | at 7 days post-randomization | |
Secondary | Plasma Levels of TNF a | Plasma levels of TNF a from day 0 to day 28 | Day 0 to 28 days post-randomization | |
Secondary | Plasma Levels of IL-6 | Plasma levels of IL-6 at day 28 | at 28 days post-randomization | |
Secondary | Plasma Levels of IL-8 | Plasma levels of IL-8 at day 28 | at 28 days post-randomization | |
Secondary | Plasma Levels of Soluble ICAM-1 | Plasma levels of soluble ICAM-1 at day 28 | at 28 days post-randomization | |
Secondary | Plasma Levels of Soluble ICAM-1 | Plasma levels of soluble ICAM-1 at day 7 | at 7 days post-randomization | |
Secondary | Peak Plasma Levels of Soluble ICAM-1 | Peak Plasma levels of soluble ICAM-1 from day 0 to day 28 | Day 0 to 28 days post-randomization | |
Secondary | Peak Plasma Levels of TNF-a | Peak Plasma levels of TNF-a at day 28 | at 28 days post-randomization | |
Secondary | Peak Plasma Levels of IL-10 | Peak Plasma levels of IL-10 at day 28 | at 28 days post-randomization | |
Secondary | Peak Plasma Levels of IL-8 | Peak Plasma levels of IL-8 at day 28 | at 28 days post-randomization | |
Secondary | Peak Plasma Levels of IL-6 | Peak Plasma levels of IL-6 at day 28 | at 28 days post-randomization | |
Secondary | AUC Plasma Levels of IL-6 | AUC Plasma levels of IL-6 from day 0 to day 28 | Day 0 to 28 days post-randomization | |
Secondary | AUC Plasma Levels of IL-8 | AUC Plasma levels of IL-8 from day 0 to day 28 | Day 0 to 28 days post-randomization | |
Secondary | AUC Plasma Levels of IL-10 | AUC Plasma levels of IL-10 from day 0 to day 28 | at 28 days post-randomization | |
Secondary | AUC Plasma Levels of TNF-a | AUC Plasma levels of TNF-a from day 0 to day 28 | at 28 days post-randomization | |
Secondary | AUC Plasma Levels of Soluble ICAM-1 | AUC Plasma levels of soluble ICAM-1 from day 0 to day 28 | at 28 days post-randomization | |
Secondary | Length of Stay | Hospital days alive and not hospitalized by day 180 | by 180 days post-randomization | |
Secondary | Length of Stay | Hospital days alive and not hospitalized by day 28 | by 28 days post-randomization | |
Secondary | Organ System Failure at 28 Days | Number of participants with organ system failure at 28 days | at 28 days post-randomization | |
Secondary | Duration of Mechanical Ventilation as Assessed by Ventilator Free Days | Number of days of mechanical ventilation duration as assessed by ventilator free days | at 28 days post-randomization | |
Secondary | Duration of Mechanical Ventilation as Assessed by Ventilator Days | Number of days of mechanical ventilation duration as assessed by ventilator days | at 28 days post-randomization | |
Secondary | Bacteremia and/or Fungemia | Number of participants with bacteremia and/or fungemia | at 28 days post-randomization | |
Secondary | Mortality | Mortality at 60 days post randomization | at 60 days post-randomization | |
Secondary | Mortality at 180 Days | Mortality at 180 days post-randomization | at 180 days post-randomization | |
Secondary | SF-36 Functional Assessment Physical Component | Physical Component Summary at 180 days post- randomization. The SF-36 consists of eight scaled scores, which are the weighted sums of the questions in their section. Each scale is directly transformed into a 0-100 scale on the assumption that each question carries equal weight. The lower the score the more disability. The higher the score the less disability | at 180 days post-randomization | |
Secondary | SF-36 Functional Assessment Mental Component | Mental Component Summary at 180 days post-randomization. The SF-36 consists of eight scaled scores, which are the weighted sums of the questions in their section. Each scale is directly transformed into a 0-100 scale on the assumption that each question carries equal weight. The lower the score the more disability. The higher the score the less disability | at 180 days post-randomization | |
Secondary | SF-36 Functional Assessment Mental Component on Day 1 | SF-36 Mental Component Summary at 1 day post-randomization. The SF-36 consists of eight scaled scores, which are the weighted sums of the questions in their section. Each scale is directly transformed into a 0-100 scale on the assumption that each question carries equal weight. The lower the score the more disability. The higher the score the less disability | at 1 day post-randomization | |
Secondary | Patients With Serious Adverse Events | Number of patients with Serious Adverse Events by day 35 | by 35 days post-randomization | |
Secondary | Time to Neutropenia | Time to neutropenia by 35 days post-randomization | by 35 days post-randomization | |
Secondary | Use of Granulocyte-colony Stimulating Factor | Number of participants requiring Granulocyte-colony stimulating factor | by 35 days post-randomization | |
Secondary | Renal Insufficiency | Number of patients experiencing a glomerular filtration rate < 60mL/min at day 35 | by 35 days post-randomization | |
Secondary | Red Blood Cell Transfusions Required Per Patients | Red blood cell transfusions required per patients by day 35 | by 35 days post-randomization | |
Secondary | Platelet Transfusions | Platelet transfusions per patient | by 35 days post-randomization | |
Secondary | Clinical Outcomes | Composite of survival status and >7 days ventilation status, and IL-6 levels. In the composite analysis, the endpoint is composed by death, ventilation status and change of cytokine. | at 14 days post-randomization | |
Secondary | Bacteremia and Fungemia Outcomes | Bacteremia and fungemia outcomes among subjects who survive at least 7 days | at 7 days post-randomization | |
Secondary | Bacteremia and Fungemia Outcomes in Mechanically Ventilated Subjets | Bacteremia and fungemia events among subjects who are mechanically ventilated for at least 7 through 14 days after randomization | at 7 through 14 days post-randomization | |
Secondary | Overall Mortality | Overall mortality amongst subjects who survive at least 7 days after randomization | at 7 days post-randomization | |
Secondary | Number of Mechanical Ventilated Days | Number of mechanical ventilated days amongst subjects who survive at least 7 days after randomization | at 7 days post-randomization | |
Secondary | Number of Ventilator-free Days | Number of ventilator-free days amongst subjects who survive at least 7 days after randomization | at 7 days post-randomization | |
Secondary | Number of Days in the ICU | Number of days in the ICU amongst subjects who survive at least 7 days after randomization | at 7 days post-randomization | |
Secondary | Number of ICU-free Days | Number of ICU-free days amongst subjects who survive at least 7 days after randomization | at 7 days post-randomization | |
Secondary | Number of Days in the Hospital | Number of days in the hospital amongst subjects who survive at least 7 days after randomization | at 7 days post-randomization | |
Secondary | Number of Hospital-free Days | Number of hospital-free days amongst subjects who survive at least 7 days after randomization | at 7 days post-randomization | |
Secondary | Mortality Among Subjects Mechanically Ventilated From Day 7 to 14 | Mortality among subjects by day 28 who are mechanically ventilated for at least 7 through 14 days after randomization | 28 days | |
Secondary | Number of Mechanically Ventilated Days Among Subjects by Day 28 | Number of mechanically ventilated days among subjects by day 28 who are mechanically ventilated for at least 7 through 14 days after randomization | 28 days | |
Secondary | Number of Ventilator-free Days Among Subjects by Day 28 | Number of ventilator-free days among subjects by day 28 who are mechanically ventilated for at least 7 through 14 days after randomization | 28 days | |
Secondary | Number of Days in ICU Amongst Subjects by Day 28 | Number of days in ICU amongst subjects by day 28 who are mechanically ventilated for at least 7 through 14 days after randomization | 28 days | |
Secondary | Number of ICU-free Days Amongst Subjects by Day 28 | Number of ICU-free days amongst subjects by day 28 who are mechanically ventilated for at least 7 through 14 days after randomization | 28 days | |
Secondary | Number of Hospital-free Days Among Subjects by Day 28 | Number of hospital-free days among subjects by day 28 who are mechanically ventilated for at least 7 through 14 days after randomization | 28 days |
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