TY - JOUR
T1 - Prophylaxis of Thromboembolism in Critical Care (PROTECT) Trial
T2 - A pilot study
AU - Cook, Deborah J.
AU - Rocker, Graeme
AU - Meade, Maureen
AU - Guyatt, Gordon
AU - Geerts, William
AU - Anderson, David
AU - Skrobik, Yoanna
AU - Hebert, Paul
AU - Albert, Martin
AU - Cooper, Jamie
AU - Bates, Shannon
AU - Caco, Christopher
AU - Finfer, Simon
AU - Fowler, Robert
AU - Freitag, Andreas
AU - Granton, John
AU - Jones, Graham
AU - Langevin, Stephan
AU - Mehta, Sangeeta
AU - Pagliarello, Giuseppe
AU - Poirier, Germain
AU - Rabbat, Christian
AU - Schiff, David
AU - Griffith, Lauren
AU - Crowther, Mark
N1 - Funding Information:
This trial was funded by the Canadian Institutes for Health Research (Ottawa, Ontario) and the Father Sean O'Sullivan Research Center (Hamilton, Ontario). Study medication was provided by Pharmacia, which played no role in the design, conduct, analysis, or interpretation of the results.
PY - 2005/12
Y1 - 2005/12
N2 - Purpose: There is no randomized trial comparing low-molecular weight heparin (LMWH) and unfractionated heparin (UFH) for thromboprophylaxis in medical-surgical ICU patients. The primary objective of this randomized pilot study on LMWH vs UFH was to assess the feasibility of conducting a large randomized trial with respect to timely enrollment and blinded study drug administration, practicality of twice-weekly lower limb ultrasounds to screen for deep venous thrombosis, LMWH bioaccumulation and dose adjustment in renal insufficiency, and recruitment rates for a future trial in medical-surgical intensive care unit (ICU) patients. Its additional goals were to evaluate the suitability of the exclusion criteria and to document the range of research activities that precede accrual of patients into a trial to plan multisite management. Materials and Methods: By computerized telephone randomization, we allocated 129 medical-surgical ICU patients to treatment with dalteparin 5000 IU QD SC or that with UFH 5000 IU BID SC. Within each clinical center, only the study pharmacist was not blinded. We performed bilateral lower limb compression ultrasounds within 48 hours of ICU admission, twice weekly, on suspicion of deep venous thrombosis, and 7 days after ICU discharge. Research coordinators and investigators at 7 centers reported the time they engaged in all research activities before the first patient was randomized. Results: Timely complete study drug administration occurred after enrollment. More than 99% of scheduled doses were administered in a blinded fashion. Scheduled ultrasounds were performed without exception. No bioaccumulation of dalteparin was observed when creatinine clearance decreased to lower than 30 mL/min. Average recruitment was 2 patients/center per month before the study exclusion criteria were modified. Study startup activities required, on average, 65.5 hours of combined investigator and research coordinator time at each center. Careful examination of the accrual in the pilot study led to a reexamination of the Prophylaxis of Thromboembolism in Critical Care Trial (PROTECT) study exclusion criteria. Conclusions: This pilot study suggests that a multicenter randomized clinical trial comparing LMWH with UFH in critically ill medical-surgical patients is feasible. Pilot studies can improve the design of larger trials and may enhance successful timely completion.
AB - Purpose: There is no randomized trial comparing low-molecular weight heparin (LMWH) and unfractionated heparin (UFH) for thromboprophylaxis in medical-surgical ICU patients. The primary objective of this randomized pilot study on LMWH vs UFH was to assess the feasibility of conducting a large randomized trial with respect to timely enrollment and blinded study drug administration, practicality of twice-weekly lower limb ultrasounds to screen for deep venous thrombosis, LMWH bioaccumulation and dose adjustment in renal insufficiency, and recruitment rates for a future trial in medical-surgical intensive care unit (ICU) patients. Its additional goals were to evaluate the suitability of the exclusion criteria and to document the range of research activities that precede accrual of patients into a trial to plan multisite management. Materials and Methods: By computerized telephone randomization, we allocated 129 medical-surgical ICU patients to treatment with dalteparin 5000 IU QD SC or that with UFH 5000 IU BID SC. Within each clinical center, only the study pharmacist was not blinded. We performed bilateral lower limb compression ultrasounds within 48 hours of ICU admission, twice weekly, on suspicion of deep venous thrombosis, and 7 days after ICU discharge. Research coordinators and investigators at 7 centers reported the time they engaged in all research activities before the first patient was randomized. Results: Timely complete study drug administration occurred after enrollment. More than 99% of scheduled doses were administered in a blinded fashion. Scheduled ultrasounds were performed without exception. No bioaccumulation of dalteparin was observed when creatinine clearance decreased to lower than 30 mL/min. Average recruitment was 2 patients/center per month before the study exclusion criteria were modified. Study startup activities required, on average, 65.5 hours of combined investigator and research coordinator time at each center. Careful examination of the accrual in the pilot study led to a reexamination of the Prophylaxis of Thromboembolism in Critical Care Trial (PROTECT) study exclusion criteria. Conclusions: This pilot study suggests that a multicenter randomized clinical trial comparing LMWH with UFH in critically ill medical-surgical patients is feasible. Pilot studies can improve the design of larger trials and may enhance successful timely completion.
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U2 - 10.1016/j.jcrc.2005.09.010
DO - 10.1016/j.jcrc.2005.09.010
M3 - Article
C2 - 16310609
AN - SCOPUS:28444475946
SN - 0883-9441
VL - 20
SP - 364
EP - 372
JO - Journal of Critical Care
JF - Journal of Critical Care
IS - 4
ER -