Renal Insufficiency Clinical Trial
Official title:
Dalteparin's Influence on Renally Compromised: Anti-Ten-A Study (DIRECT)
The investigators' primary research objective is:
- To determine the safety of dalteparin prophylaxis, 5,000 IU once-daily, in Intensive
Care Unit (ICU) patients based on:
- the proportion of patients with trough anti-Xa > 0.40 IU/mL during dalteparin
prophylaxis after 3 + 1 days, 10 + 1 days, and 17 + 1 days of dalteparin
prophylaxis;
- the risk of major bleeding during the treatment period.
The investigators' secondary research objectives are:
- To determine the pharmacokinetic properties of dalteparin prophylaxis in ICU patients
with severe renal insufficiency;
- To identify clinical and laboratory factors that predict an excessive anticoagulant
effect (anti-Xa > 0.10 IU/mL);
- To estimate the relationship between trough anti-Xa levels and bleeding.
The DIRECT Pilot Study:
Before embarking on a large trial of low molecular weight heparin (LMWH) versus standard
unfractionated heparin (UFH), the DIRECT Study is needed to observe whether bioaccumulation
of LMWH occurs in ICU patients with moderate to severe renal insufficiency, and to address
potential problems with protocol implementation.
Critically ill patients who are admitted to an intensive care unit (ICU) are at high risk
for deep vein thrombosis (DVT), with an estimated 20-40% of patients developing DVT without
prophylaxis. Preventing DVT is important because DVT is usually clinically silent in such
patients, and its first manifestation may be life-threatening pulmonary embolism.
About 30% of ICU patients have renal insufficiency, based on a calculated creatinine
clearance (CrCl), and such patients have 4-fold higher risk of DVT than those with normal
renal function.
The current anticoagulant regimen that is used to prevent DVT in such patients, consisting
of unfractionated heparin (UFH), 5000 IU twice-daily, may be inadequate.
A recent prospective cohort study by our research group that investigated the risk of DVT in
261 ICU patients found that 10% of patients developed proximal vein DVT after admission to
the ICU despite receiving UFH, 5000 IU twice-daily.
In other patient groups at high risk for DVT, low-molecular-weight heparins (LMWHs) have
replaced UFH for DVT prophylaxis because of superior efficacy.
Despite superior efficacy and safety in many patients, there is concern about using LMWHs in
patients with renal insufficiency because LMWHs are cleared by the kidney. LMWH use in such
patients might result in an excessive anticoagulant effect, with the potential to increase
bleeding.
Much of the concern about the safety of LMWH in patients with renal insufficiency pertains
to therapeutic-dose LMWH used to treat DVT. Prophylactic-(or low) dose LMWH that is used to
prevent DVT in ICU patients is about 25-33% of a therapeutic-dose.
Three sources of evidence suggest that prophylactic-dose LMWH may be safe in patients with
renal insufficiency. First, current evidence does not support the fact that
prophylactic-dose LMWH accumulates and should be avoided in such patients. Second,
prophylactic-dose LMWH appears to be safe in hemodialysis patients. Third, preliminary work
by our research group suggests that dalteparin, 5000 IU once-daily, does not accumulate in
ICU patients with renal insufficiency. Thus, 0 of 10 ICU patients with a CrCl <50
mL/min/1.73m2 who received dalteparin had a detectable trough anticoagulant effect (anti-Xa
>0.10 IU/mL). Further, when the relationship between CrCl and peak anti-Xa levels was
assessed, there was no correlation (r<0.2). Finally, in 2 patients with severe renal
insufficiency (CrCl<30 mL/min/1.73m2) who received dalteparin, 5000 IU once-daily, all 9
trough anti-Xa values were <0.10 IU/mL.
No study has investigated the safety of low-dose LMWH in ICU patients with impaired renal
function; until such a study is completed, randomized trials assessing the efficacy of
low-dose LMWH for DVT prophylaxis among ICU patients will not be feasible.
As a first step in addressing this problem, we propose an open-label pilot study to assess
the safety of dalteparin prophylaxis, 5000 IU once-daily, in ICU patients with severe renal
insufficiency.
The safety of the proposed dalteparin prophylaxis regimen will be assessed by determining
the risk of an excessive anticoagulant effect and the risk of major bleeding. Dalteparin
prophylaxis will be considered safe if 2 criteria are satisfied by the end of the treatment
period:
- proportion of patients with trough anti-Xa level >0.40 IU/mL is ~10% or less (exclude
17% with 95% confidence);
- risk of major bleeding is ~4% or less (exclude 10% with 95% confidence).
If we show that dalteparin prophylaxis is safe in ICU patients with severe renal
insufficiency, this will improve patient care in 2 ways:
- dalteparin may reduce the risk of DVT (although this should be tested in future
trials); and
- dalteparin would reduce heparin induced thrombocytopenia (HIT), an infrequent but
serious complication of UFH.
;
Observational Model: Defined Population, Primary Purpose: Screening, Time Perspective: Longitudinal
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