Supportive and Preventive Medicine
Rivaroxaban 10 mg orally once daily was compared with enoxaparin 40 mg subcutaneously daily
for 10 days, followed by placebo in acutely ill hospitalized patients. The rates of asymptomatic or
symptomatic VTE, pulmonary embolism, or death were comparable; however, the bleeding rates were
increased in the rivaroxaban group (N Engl J Med 2013;368:513-23). A subsequent study evaluating
rivaroxaban 10 mg/day orally with placebo in patients at high risk of VTE demonstrated a decrease in
rates of symptomatic VTE (0.18 vs 0.42%; HR 0.44, 95% CI, 0.22-0.89); however, low overall VTE and
bleeding event rates limit widespread use. Further studies must identify the populations most likely to
benefit from extended prophylaxis (N Engl J Med. 2018;379:1118-27).
LMWH is preferred to vitamin K antagonists and DOACs for prophylaxis in critically ill patients
HIT is a severe, immune-mediated reaction that potentially leads to life-threatening complications
such as myocardial infarction, skin necrosis, stroke, and VTE (around 50%β75% of patients with HIT
develop symptomatic thrombosis).
(prior 2 weeks) who present with a new thrombosis and low Plt.
Frequency of HIT
Higher in patients receiving unfractionated heparin than in patients receiving LMWH, occurring
in 1%β5% of patients versus less than 1%, respectively
Occurs in less than 1% of ICU patients
Higher risk in cardiac or orthopedic surgical patients receiving unfractionated heparin (15%) than
in medical patients (0.1%β1%)
Alternative causes of thrombocytopenia in critically ill patients include extracorporeal devices, intra-
aortic balloon pumps, sepsis, disseminated intravascular coagulation, bleeding, and medications (eg,
linezolid, carbamazepine, phenytoin, valproic acid). Plts may decrease after surgery on cardiopulmonary
bypass and subsequently recover; however, a secondary decrease in Plt may signal potential HIT.
Clinical diagnosis of HIT
Suspected when a patient has a decrease in absolute Plt to less than 150,000/mm3 or a relative
decrease of at least 50% from baseline, skin lesions at injection sites, or systemic reactions after
intravenous boluses
Typical onset is 5β10 days after heparin exposure, though onset can be delayed and can occur up
to 3 weeks after therapy cessation.
Recent heparin exposure, within the last 90 days, may result in rapid-onset HIT, occurring within
hours after rechallenge.
| d. | Patients with recent unfractionated heparin/LMWH exposure and a new thrombosis should have |
|---|
their Plt checked before anticoagulant therapy is initiated.
Probability of HIT
4T score
Segregates patients into low, intermediate, and high clinical probability on the basis of four
criteria
ii.
Four clinical features incorporated: (1) thrombocytopenia, (2) timing of thrombocytopenia, (3)
presence of thrombosis or other clinical sequelae, and (4) other causes of thrombocytopenia
iii.
A low probability 4T score (3 or less) has a high negative predictive value (0.998), whereas an
intermediate or high probability score (4 or greater) has a low positive predictive value (0.64
and 0.14, respectively) (Blood 2012;120:4160-7).