Content on this page:
Content on this page:
Monitoring
DVT
and Non-Massive Pulmonary Embolism
Provoked VTE
with persistent risk factors and a second episode of unprovoked VTE have the highest recurrence rates at 1 year and 5 years
after stopping anticoagulation therapy. The rate of recurrent VTE is approximately 10% during the first year and 30% after 5 years,
and approximately 40% in 10 years in patients with unprovoked DVT. Other strong risk factors for recurrence include a pulmonary
embolism, proximal DVT, or a previous VTE. A high (>8%/year) risk for long-term recurrence is seen
in patients with active cancer, antiphospholipid antibody syndrome, and ≥1
prior VTE episodes without a transient factor.
Cumulative VTE risk over
5 years is as
follows:
- Low risk (<14%): Transient risk factors (eg surgery, Estrogen therapy)
- Intermediate risk (14-30%): Non-surgical transient risk factors (eg leg injury, significant medical illness, travel associated)
- High risk (?30%): Unprovoked VTE
Recurrences
tend to develop in a similar site to the initial episode, with more proximal VTE having higher recurrences rates. Risk factors for recurrent
VTE in patients with calf DVT include age >50 years old,
male sex, multiple unilateral thromboses, bilateral DVT, unprovoked DVT, and cancer.
Risk factors for proximal extension of distal DVT
favoring anticoagulation include D-dimer ≥500 ng/mL, non-minor symptoms,
unprovoked event, extensive thrombosis involving multiple veins, persistent or
non-reversible risk factors (eg active cancer, prolonged immobility), prior DVT
or pulmonary embolism, and inpatient status. The risk of proximal extension or
pulmonary embolism in patients with distal DVT
without anticoagulation is >10%.
Factors favoring surveillance of distal DVT include
D-dimer level <500 ng/mL, no or minor symptoms, absence of high-risk
features of proximal extension, minor thrombosis in the muscular veins, high
risk of or contraindications to bleeding and patient preference.
Patients with acute pulmonary embolism are
recommended to follow up 3 to 6 months after an acute episode. These patients have
a high frequency (20 to 50%) of symptomatic extension of thrombus and/or
recurrent VTE and therefore require long-term anticoagulant
treatment.
Extended anticoagulation treatment should be
considered in the following patients with an index pulmonary embolism episode:
Have no identifiable risk factor or with a minor transient risk factor; and
those with a persistent risk factor other than antiphospholipid antibody
syndrome.
Patients receiving extended treatment should be
followed up at least annually and checked for the presence of bleeding and recurrent VTE, changes in hepatic or renal function, adherence to
therapy, treatment preferences, and new drug interactions. Consider further
evaluation for pulmonary embolism survivors who are asymptomatic and at
increased risk for chronic thromboembolic pulmonary hypertension.
If anticoagulation treatment failure occurs, check the
patient's adherence to therapy, check for malabsorption or treatment suspension
for a planned procedure, increase the anticoagulant dose or administration
frequency or switch to an anticoagulant with a different mechanism of action, and
address other causes of hypercoagulability.
LMWH
Treatment options for patients with recurrent VTE unresponsive to vitamin K
antagonist therapy or for those with breakthrough VTE during vitamin K antagonist therapy.
The dose may be increased if there is treatment failure to present the dose.
For patients with pulmonary embolism and cancer, LMWH
is preferred over vitamin K antagonists and should be used for the first 6
months of long-term anticoagulant therapy. After which, these patients should
receive oral anticoagulant therapy indefinitely or until the cancer has
resolved.
Oral Anticoagulant
Treatment with oral anticoagulant is the preferred method of long-term
management of most patients with pulmonary embolism. Adjusted doses of UFH or LMWH
may be indicated for selected patients in whom oral anticoagulants are
contraindicated or impractical.
Venous Thromboembolism - Management_Follow UpDuration of anticoagulation is dependent on the type of event and the coexistence of prolonged risk factors:
- Continue for ≥3 months: First event with provoked risk factors, in cancer patients with symptomatic catheter-related thrombosis, patients with unprovoked proximal DVT with low to moderate bleeding risk, or patients with symptomatic distal DVT (provoked or unprovoked)
- Continue for ≥6 months: First episode, idiopathic VTE
- Continue for ≥12 months: Recurrent, idiopathic VTE or continuing risk factor
- Continue for 6-12 weeks: Symptomatic isolated calf vein thrombosis
- Consider for indefinite anticoagulation: Second episode of unprovoked pulmonary embolism, unprovoked proximal DVT, chronic risk factor (provoked non-surgical and non-reversible risk factors), or patients with pulmonary embolism and cancer without high bleeding risk
For patients with provoked proximal DVT, NOACs are preferred over vitamin K antagonist agents for the
principal treatment phase. For patients with unprovoked proximal DVT, NOACs are recommended over LMWH followed by vitamin K antagonist
agents for the principal treatment phase; NOACs are recommended over vitamin K antagonist agents for extended
anticoagulation.
A reduced dose of NOACs
may be an option for extended anticoagulation. Reduced
doses of Apixaban or Rivaroxaban may be options for patients with unprovoked
proximal DVT requiring extended
anticoagulation for >6 months but without high risk for recurrence.
Dabigatran is effective for extended anticoagulation
therapy for VTE in patients with a high risk of recurrence.
For patients with
leg DVT or pulmonary embolism, NOACs are preferred
over vitamin K antagonist agents for the first 3 months of long-term
anticoagulant therapy. Vitamin K antagonist agents are preferred over LMWH for
patients with VTE. For VTE patients with cancer, LMWH is preferred over vitamin K
antagonist agents and NOACs are alternative agents.
For patients who need to continue on extended
anticoagulant therapy, therapeutic or low-dose NOACs (eg Apixaban or Rivaroxaban) can be given after the first 6
months and are preferred over Warfarin if without contraindications.
Warfarin
An INR range of 2.0-3.0 is recommended for
patients with VTE who will continue vitamin K antagonist
therapy as extended anticoagulation after having completed the primary
treatment.
Aspirin
Aspirin may be considered for the prevention of
recurrent VTE in patients with unprovoked
proximal DVT or pulmonary
embolism who refused continued anticoagulant therapy. Aspirin or Sulodexide may
be considered for an extended VTE prophylaxis in patients who refuse or cannot tolerate oral
anticoagulation.
For patients who sustained a VTE while taking Aspirin for primary cardiovascular disease prevention or for
stable coronary artery disease, it is advised to suspend Aspirin while taking
anticoagulant therapy.
International
Medical Prevention Registry on Venous Thromboembolism (IMPROVE) Bleeding Risk
IMPROVE is used to assess a confined patient’s risk for bleeding prior
to initiation of therapy. A score of ≥7 signifies increased bleeding risk.
| Score | Medical History |
| 4.5 | Active gastric or duodenal ulcer |
| 4 | Bleeding event <3 months before consultation; thrombocytopenia (platelet count <50 x 103/L) |
| 3.5 | ≥85 years of age |
| 2.5 | Liver failure (INR >1.5); severe renal failure (GFR <30 mL/min/1.73 m2); ICU/CCU admission |
| 2 | Central venous catheter; rheumatic/autoimmune disease; current malignancy |
| 1 | 40-84 years of age; male; moderate renal failure (GFR 30-59 mL/min/1.73 m2) |
Risk Factors for Major Bleeding During Anticoagulation
Patients without risk factors have an absolute
risk of major bleeding of 0.8% per year, 1 risk factor is 1.6% per year, and ≥2
risk factors are ≥6.5% per year.
The risk factors for major bleeding during
anticoagulation are as follows:
- Age >75 years
- History of previous bleeding
- Previous non-cardioembolic stroke
- Chronic hepatic and renal disease
- Concomitant antiplatelet or nonsteroidal anti-inflammatory (NSAID) therapy
- Poor anticoagulant control
- Suboptimal monitoring of therapy
- Comorbid illness (eg cancer, hypertension, thrombocytopenia, anemia, diabetes mellitus)
- Frequent falls, alcohol abuse
- Recent surgery
Monitoring during Anticoagulation Therapy
INR should be checked at least weekly during the first
several weeks of Warfarin therapy. If stable, monitor every 2 weeks then every
4 weeks. The target INR is 2.5 for most patients and 3.0 for patients with recurrent
VTE. Regularly monitor
therapeutic levels to ensure effective anticoagulation in patients weighing
<50 kg or >120 kg. Monitor patient for recurrence, bleeding, adverse
effects of medication and signs and symptoms of conditions that could alter the
half-life of the anticoagulant used (eg kidney failure, weight loss or gain).
Monitoring without Anticoagulation Therapy
Monitoring without anticoagulation
therapy is recommended for patients with isolated distal leg DVT and no severe symptoms or risk factors for proximal extension, and those with high bleeding risk.
Serial ultrasound imaging of both legs for 2 weeks is suggested.
Surveillance is recommended in
patients with subsegmental pulmonary embolism and without proximal DVT and low risk of recurrence for VTE.