Clinical Assessment Scores

As part of the initial evaluation of patients with suspected ICH, the emergency physician should obtain a baseline severity score based on physical examination. The National Institutes of Health Stroke Scale may be used to achieve this purpose and is preferred over the Glasgow Coma Scale. The benefit of scoring systems lies in the ability to communicate effectively about a patient’s dynamic medical condition over time to other medical providers. These providers, whether in the ED or an intensive care unit (ICU), can subsequently repeat the physical examination and identify changes.

Blood Testing

A rapid fingerstick glucose value should be obtained immediately in case the patient’s condition is due to hypoglycemia. Intravenous access should also be obtained immediately upon the patient’s arrival. The following markers should be ordered: complete blood count, basic metabolic panel including electrolytes and creatinine, troponin, prothrombin time, International Normalized Ratio (INR), partial thromboplastin time, and type and screen.

Computed Tomography

The abrupt onset of focal neurologic symptoms should be presumed as an ischemic stroke until proven otherwise, because time-sensitive evidence-based treatments exist for this form of stroke. Rapid neuroimaging with noncontrast computed tomography (CT) scan or MRI should be obtained to distinguish ischemic stroke from ICH. CT scan is the preferred imaging choice owing to its more rapid availability and lower cost. Hemorrhage appears as a high-density lesion. Its size and location can be visualized, as can the presence of intraventricular extension, edema, and/or brain herniation.

Computed Tomography Assessment

In a large retrospective study, ICH hematoma volumes greater than 32 mL supratentorially or 21 mL infratentorially were shown to be significant predictors of 30-day mortality. To communicate hematoma size with neurosurgery and ICU consultants, this measurement can be calculated rapidly and easily using the ABC/2 method ( Fig. 1 ).

The ABC/2 method for rapidly obtaining hematoma volume. CT, computed tomography.

( From Morotti A, Goldstein JN. Diagnosis and management of acute intracerebral hemorrhage. Emerg Med Clin North Am 2016;34(4):883–99.)

Additionally, the ICH score incorporates this volume to predict outcomes and assist with medical decision making. Higher scores are associated with increased risk of mortality and decreased likelihood of good functional outcome. In the initial study of 152 patients with acute ICH, scores of 1, 2, 3, and 4 corresponded with 30-day mortality rates of 13%, 26%, 72%, and 97%, respectively ( Table 1 ). Subsequent studies have supported this positive association with mortality.

Location Corresponds with Etiology

Varying etiologies of spontaneous ICH may exert their effect within characteristic areas of the brain ( Figs. 2–5 ). Accordingly, the location of the hemorrhage may help point to the underlying etiology. For instance, bleeding from hypertensive ICH occurs most commonly in the basal ganglia (40%–50%) and other deeper structures within the parenchyma (thalamus, cerebellum, pons). ICH owing to amyloid (almost exclusively in elderly patients) or arteriovenous malformation (AVM) tends to occur in the lobar regions. Those originating from mass lesions may demonstrate edema surrounding the tumor and be seen in the grey–white junctions. Hemorrhagic conversion of a prior ischemic stroke may show hypodensity and edema in the middle cerebral artery territory with hemorrhage within it. ICH from a cerebral venous sinus thrombosis commonly appear at the sagittal and transverse sinuses.

Hypertensive hemorrhage.

( From Fatterpekar GM, Naidich TP, Som PM. In: Silva IS, Muller NL, editors. The teaching files: chest: expert consult – online and print, 1e (teaching files in radiology). Philadelphia: Elsevier; 2012. p. 210–1.)

Cerebral amyloid lobar hemorrhage.

( From Kase CS, Shoamanesh A, Greenberg SM, et al. Intracerebral Hemorrhage. In: Grotta JC, Albers GW, Broderick JP, et al, editors. Stroke: pathophysiology, diagnosis, and management. vol. 28. Philadelphia: Elsevier; 2016. p. 466–515.e12.)

Hemorrhagic brain metastasis. ( A ) The initial axial CT image at the level of the basal ganglia showed a hemorrhagic lesion with a slightly undulated or finger-in-glove appearance in the right lentiform nucleus ( thin arrows ) along with perifocal edema ( bold arrow ). ( B ) A subsequent axial CT image disclosed a growing hemorrhagic lesion with a remarkable finger-in-glove sign ( thin arrows ) and more pronounced perifocal edema ( bold arrow ).

( From Juan YH, Hsuan HF, Cheung YC. Pointing to the diagnosis: hemorrhagic brain metastasis. Am J Med 2016;129(12):1268–9.)

Cerebral venous infarction owing to superior sagittal sinus thrombosis. A 32-year-old representative female presented with acute onset severe headache, vomiting and left hemiparesis. ( A ) CT scan revealed intracranial hemorrhage and infarct; ( B ) DSA revealed features of cerebral venous sinus thrombosis involving superior sagittal sinus, left transverse sinus; ( C ) microcatheter was advanced into the SSS; ( D ) MRV showed complete recanalization of superior sagittal sinus after 6-day local urokinase administration. She was asymptomatic at the time of discharge.

( From Guo XB, Fu Z, Song LJ, et al. Local thrombolysis for patients of severe cerebral venous sinus thrombosis during puerperium. Eur J Radiol 2013;82(1):165–8.)

Computed Tomography Angiography of the Brain

Follow-up brain imaging is less useful when hypertensive hemorrhage is suspected, such as in patients with a history of poorly controlled hypertension and a CT image showing a deep bleeding pattern. However, beyond the noncontrast CT scan, additional imaging modalities may provide important information about the underlying cause of an ICH. CT head angiography is performed routinely for patients in whom spontaneous ICH is suspected owing to secondary etiology, such as aneurysm, AVM, tumor, or cerebral venous thrombosis. Certain indicators for such bleeds include lobar ICH, young age, and absence of cardiovascular disease risk factors. Suggestive radiologic evidence for vascular abnormalities causing ICH includes subarachnoid hemorrhage, enlarged vessels or calcifications along hemorrhage margins, hyperattenuation within a dural venous sinus, unusual hematoma shape and/or location, edema out of proportion with the presumed onset time, and the presence of a mass.

Furthermore, CT angiographic studies may identify contrast extravasation that is predictive of hematoma growth and 30-day mortality. Extravasation is reflected by tiny enhancing foci within the acute hematoma called spot signs ( Fig. 6 ). Spot signs are associated with intraoperative bleeding, postoperative bleeding, and larger residual ICH volumes during surgical evacuation. Their number, diameter, and attenuation are used to calculate the Spot Sign Score, which has been shown to independently predict poor functional outcomes and in-hospital mortality. This diagnostic marker does not have a clear role in determining management.

A sign with spot-like appearance on CT angiography (CTA) in a patient with intracerebral haemorrhage. The spot sign ( green arrow ) measures 2·2 mm in maximal axial diameter, and has a density of 173 Hounsfield units.

( From Demchuk AM et al. Prediction of haematoma growth and outcome in patients with intracerebral haemorrhage using the CT-angiography spot sign (PREDICT): a prospective observational study. Lancet Neurology 2012;11(4):307–14.)

MRI

MRI takes longer to perform and is more expensive than CT imaging. Although much less frequently used, MRI may nevertheless be performed to evaluate for secondary causes of ICH, including hemorrhagic conversion of prior ischemic stroke. With high diagnostic accuracy, it may also detect AVMs, tumors, and cerebral venous thrombosis. MRI without contrast may be most useful in patients who are unable to receive intravenous (IV) contrast agents owing to allergy or renal disease.

Initial Assessment

Even before the patient is taken for CT imaging, the initial evaluation for any patient with suspected ICH begins with assessment of airway, breathing, and circulation (ABCs). Given the varying etiologies of ICH, it is also important for the emergency physician to obtain a focused yet detailed history from the patient, family members, and/or emergency medical services personnel ( Table 2 ). Although there is some overlap, the different etiologies call for certain focused management strategies, with the major difference being blood pressure control parameters.

Intervention Overview

Overall, treatment is generally supportive and aimed at preventing further injury to the brain by preventing the following complications: (1) hematoma expansion, (2) development of edema, (3) obstructive hydrocephalus, and (4) brain herniation. Some interventions must be taken immediately, whereas others may come secondarily ( Table 3 ).

Rapid initiation of interventions may improve functional outcomes, because clinical deterioration may occur early. For instance, early hematoma expansion occurs in 18% to 38% of patients who receive repeat CT scan within 3 hours of onset. This has been shown to carry an association with poor clinical outcomes including an increased mortality rate of up to 30% to 55% at 30 days. These sobering statistics highlight the importance of mitigating ICH growth in the ED.

Antithrombotic Agents

Patients taking the vitamin K antagonist warfarin carry a 5- to 10-fold increased risk of suffering an ICH, and approximately 15% of cases are associated with its use. Once the ICH occurs, prolonged bleeding causes 27% to 54% of patients to develop early hematoma expansion that is associated with doubling of the mortality risk. These life-threatening risks are further exacerbated when coagulopathy is not corrected rapidly.

Current guidelines recommend administration of IV vitamin K (5–10 mg) by slow push over 10 minutes. Although long lasting, it takes 6 to 24 hours for vitamin K to achieve its reversal effects.

Fresh frozen plasma (FFP) contains factors I (fibrinogen), II, V, VII, IX, X, XI, XIII, and antithrombin. Relatively large volumes of FFP (10–15 mL/kg) are administered, which puts patients at risk for volume overload and pulmonary edema. Moreover, the INR of FFP itself is about 1.6, limiting the extent to which the coagulopathy can be reversed. Along with its required blood type matching, thawing time, and longer duration of administration, FFP takes several hours to achieve its INR reversal effects.

Prothrombin complex concentrate (PCC) contains vitamin K–dependent coagulation factors II, VII, IX, and X. Compared with FFP, the vials contain a higher concentration of clotting factors within a smaller volume and take only minutes to fully administer. PCC can normalize the INR completely within 10 minutes, although it brings a higher risk of disseminated intravascular coagulation. The INR needs to be checked within 30 minutes and redosed as needed.

Research shows that PCC should be the first-line reversal agent for most patients with therapeutic warfarin levels ( Table 4 ). Three randomized controlled trials comparing the two reversal agents found that PCC lowered the INR more rapidly than FFP and with no clear difference in thromboembolic risk. In terms of outcomes research supporting PCC, one prospective observational study showed a lower risk of death or severe disability at 3 months, whereas a retrospective study showed an increased 1-year survival. Another study comparing the two treatments for Warfarin reversal showed that in patients whose INR was corrected within 2 hours, there was no difference in hematoma growth incidence or extent. Even if it may not necessarily be the agent but rather the timing of coagulopathy reversal that imparts a greater effect, FFP takes longer than PCC to administer for the reasons mentioned.

Table 4

PCC dosing recommendations

Pre-treatment INR	2–4	4–6	>6
4-Factor PCC dose (units of factor IX/kg)	25	35	50
Maximum dose (units of Factor IX)	2500	3500	5000

Only gold members can continue reading. Log In or Register to continue

Share this:

• Click to share on Twitter (Opens in new window)
• Click to share on Facebook (Opens in new window)

Related

Related posts:

Extracranial Cervical Artery Dissections Deep Venous Thrombosis Acute Limb Ischemia Mesenteric Ischemia Extracranial Cervical Artery Dissections Acute Limb Ischemia

Stay updated, free articles. Join our Telegram channel

Join