Noncontrast computed tomography

Noncontrast computed tomography (NCCT) is a fast technique with excellent sensitivity for identifying acute ICH, and given its wide availability is considered the gold standard for the diagnosis of ICH in the emergency department (ED). Beyond the diagnosis of ICH, NCCT can provide useful elements such as ICH location, intraventricular extension, hydrocephalus, presence and degree of edema, and midline shift or brainstem compression secondary to the mass effect from the hematoma. Furthermore, ICH volume is a strong predictor of ICH outcome and can be rapidly estimated in the ED with the ABC/2 technique ( Fig. 1 ).

ABC/2 method for ICH volume estimation. CT, computed tomography.

Computed tomography angiography

Computed tomography angiography (CTA) is a useful diagnostic tool in the acute setting of ICH. It is the most widely available noninvasive technique for the detection of vascular abnormalities as secondary causes of ICH. The presence of lobar ICH, significant IVH, young age, and absence of traditional cerebrovascular risk factors should trigger the suspicion of ICH secondary to vascular malformation or other intracranial disorder. Prompt detection of these lesions is crucial and has a significant impact on patient management. Although CTA is an excellent noninvasive screening tool, digital subtraction angiography remains the gold standard investigation for diagnosis, and frequently endovascular treatment, of cerebral vascular malformations.

Presence of contrast extravasation within the hematoma on CTA images, also termed spot sign, is an independent predictor of hematoma expansion and poor outcome in patients with supratentorial ICH ( Fig. 2 ). Furthermore, CTA spot sign is associated with active bleeding during surgical evacuation, and may help indicate which patients may benefit from surgery. The main drawback of CTA is cost and the additional radiation exposure. Although some clinicians are concerned about the risk of contrast-induced nephropathy, there is debate in the literature about whether this entity exists, and there is no evidence that CTA increases the risk of nephropathy in patients with ICH.

Spot sign and hematoma expansion. ( A ) Left deep ICH on NCCT, with baseline volume of 45 mL; ( B ) CTA showing presence of spot sign ( arrow ); ( C ) follow-up NCCT at 19 hours showed significant hematoma growth to a volume of 192 mL with severe midline shift and massive intraventricular extension.

MRI

MRI sensitivity for the diagnosis of ICH is equivalent to that of NCCT. MRI can be a useful technique to detect underlying secondary causes of ICH, such as neoplastic lesions or hemorrhagic transformation of ischemic stroke. In addition, in patients with poor kidney function, contrast allergies, or other contraindications to CTA, brain vessel imaging can be achieved without contrast through magnetic resonance angiography. Given the cost, duration of the examination, and poor tolerability for some patients, MRI is rarely used in the ED work-up of ICH.

Platelet function

The utility and safety of platelet transfusion in patients with ICH taking antiplatelet medications remains unclarified and there is not enough evidence to support routine application of a reversal strategy to improve platelet function. Platelet transfusion is indicated in patients with severe thrombocytopenia, with suggested thresholds between 50,000 and 100,000 platelets per microliter.

Warfarin-associated coagulopathy

OAT is associated with higher baseline ICH volume, increased risk of hematoma expansion, and poor outcome. Coagulopathy correction is designed to prevent continued bleeding. Warfarin discontinuation and IV administration of vitamin K are the first therapeutic steps. Vitamin K should be infused slowly (over 10 minutes), at a dose of 10 mg with close monitoring of vital signs given the rare but not negligible risk of anaphylaxis (1 in 10,000). Given its slow onset of action (6–24 hours), emergent factor repletion is typically also provided. Fresh frozen plasma (FFP) and prothrombin complex concentrates (PCCs) are commonly used. According to the AHA/ASA guidelines, PCCs may be preferred to FFP because of more rapid action. Two randomized controlled trials of PCC versus FFP showed that PCCs restore coagulation factors and reverse the International Normalized Ratio (INR) more rapidly than FFP, with no clear difference in thromboembolic risk. Although these trials failed to show improved clinical outcome in patients with ICH, some observational studies have suggested improved outcome from more rapid INR reversal. The optimal INR target is still debated and proposed target values range from 1.3 to 1.5. Although it is not clear whether INR values less than 1.7 represent clinically relevant coagulation abnormalities, 1 observational study found that achievement of an INR value less than 1.3 within 4 hours from admission was associated with reduced risk of hematoma expansion. The European Stroke Organization guidelines do not provide a specific recommendation about the warfarin reversal strategy, whereas the Neurocritical Care Society recommends warfarin reversal with either PCCs or FFP with a target INR less than 1.5. Characteristics of FFP and PCCs and 1 reasonable reversal strategy for warfarin-associated ICH are shown in Table 1 and Box 2 .

Heparin-associated coagulopathy

If ICH occurs during IV heparin or low-molecular-weight heparin treatment, protamine sulfate administration can be used for coagulopathy reversal, at the dose of 1 mg per 100 units of heparin. The maximum dose should be 50 mg and the infusion must be slow (maximum infusion speed: 5 mg/min) with vital signs monitoring given the significant risk of hypotension.

Direct oral anticoagulants

Alternatives to warfarin are now available, and the most commonly used are the factor Xa inhibitors apixaban, rivaroxaban, and edoxaban, and the direct thrombin inhibitor dabigatran. These agents were traditionally termed novel oral anticoagulants but the International Society of Thrombosis and Hemostasis has recommended the term direct oral anticoagulants (DOACs); this article uses this new terminology. Unlike warfarin, there is no specific commercially available laboratory test to assess level of DOAC function; however, some traditional and novel blood tests may assist clinical providers in estimation of anticoagulant effect. These tests are listed in Table 2 . Compared with warfarin, DOACs have shorter half-lives and their blood concentrations typically follow a peak-trough format. Therefore, timing of last intake and renal function should always take into consideration whether the patient is still, at the time of presentation, coagulopathic. Current evidence for DOACs reversal is limited and comes from in-vitro and animal models or studies on healthy volunteers. For dabigatran reversal, a specific antagonist is now available that addresses coagulopathy but has not yet been shown to reduce expansion. For reversal of other agents, it may be that no currently available product is effective for this purpose, although more specific reversal agents are under investigation ( ClinicalTrials.gov identifiers NCT02329327 and NCT02220725 ). Patients taking DOACs are not deficient in vitamin K–dependent factors, so vitamin K administration is not likely to be of value. Some authorities use activated PCCs for this purpose, to provide excess coagulation factor activity. Activated charcoal can be considered if administered within 2 to 3 hours from the last drug intake.

Table 2

Effect of DOACs on blood tests

	Dabigatran	Rivaroxaban	Apixaban	Edoxaban
aPTT	• Abnormal only at moderate/high levels of drug. • Provides only qualitative indication	• Low sensitivity • Possible paradoxic response	• Low sensitivity • Possible paradoxic response	• Low sensitivity
PT/INR	• High interindividual variability • Mild effect (INR 0.9–1.2)	• Provides qualitative indication only with specific reagents	• Unaffected	• Linear dose-dependent association but low sensitivity at lower therapeutic drug levels
dTT	• Already prolonged at low drug concentration • Normal dTT can rule out anticoagulant activity • Needs calibration	—	—	—
ECT	• Sensitive indicator • Not widely available • Time consuming	—	—	—
Anti-Xa activity	—	• Sensitive indicator • Normal value rules out anticoagulant activity • Not widely available • Needs calibration	• Sensitive indicator • Normal value rules out anticoagulant activity • Not widely available • Needs calibration	• Sensitive indicator • Normal value rules out anticoagulant activity • Not widely available • Needs calibration
Specific test system	Hemoclot: dabigatran-calibrated dTT	Rivaroxaban-calibrated anti-Xa activity	Apixaban-calibrated anti-Xa activity	Edoxaban-calibrated anti-Xa activity

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