Arteriovenous Malformations

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Practice Essentials

Arteriovenous malformations (AVMs) are congenital lesions composed of a complex tangle of arteries and veins connected by one or more fistulae (see the image below). They most commonly occur in young adults, with morbidity and death occurring in 30–50% and 10–15% of patients, respectively.



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T1 axial MRI showing a small subcortical arteriovenous malformation in the right frontal lobe.

Signs and symptoms

History

Considerations regarding patient history include the following:

Physical examination

Considerations regarding the physical examination of patients with AVM include the following:

See Clinical Presentation for more detail.

Diagnosis

The following imaging studies are used in the diagnosis and assessment of cerebral AVM:

See Workup for more detail.

Management

Invasive treatment is recommended for younger patients with 1 or more high-risk features for an AVM rupture. Older individuals and patients with no high-risk features may be best treated through management of the medical aspects of the illness alone; in such patients, anticonvulsants for seizure control and appropriate analgesia for headaches may be the only treatment recommendations necessary.

Invasive treatment of AVMs may include endovascular embolization, surgical resection, and focal beam radiation, alone or in any combination. The current American Heart Association multidisciplinary management guidelines for the treatment of brain AVMs recommend the following approach:[2]

See Treatment for more detail.

Background

Hemorrhage from cerebral arteriovenous malformations (AVMs) represents 2% of all hemorrhagic strokes. A clear understanding of the diagnostic and treatment algorithms involved with AVM management is imperative, because AVMs are a cause of hemorrhage in young adults.

Pathophysiology

AVMs are congenital lesions composed of a complex tangle of arteries and veins connected by one or more fistulae. The vascular conglomerate is called the nidus. The nidus has no capillary bed, and the feeding arteries drain directly to the draining veins.[3] The arteries have a deficient muscularis layer. The draining veins often are dilated owing to the high velocity of blood flow through the fistulae. How the abnormal vessels appear or exactly when the process begins is unknown. Deranged production of vasoactive proteins is under investigation as the angiogenetic link to pathophysiology.

AVMs produce neurological dysfunction through 3 main mechanisms.[4] First, hemorrhage may occur in the subarachnoid space, the intraventricular space or, most commonly, the brain parenchyma. Second, in the absence of hemorrhage, seizures may occur as a consequence of AVM: approximately 15-40% of patients present with seizure disorder. Finally, but rarely, a progressive neurological deficit may occur in 6-12% of patients over a few months to several years. These slowly progressive neurological deficits are thought to relate to siphoning of blood flow away from adjacent brain tissue (the "steal phenomenon"), a concept that has been recently challenged. Neurological deficits may be explained alternatively by the mass effect of an enlarging AVM or venous hypertension in the draining veins.

Epidemiology

Frequency

United States

The detection rate in the general population based on prospective data from the New York Islands AVM Study is approximately 1.34 per 100,000 person-years.[5] The prevalence of cerebral AVM in the United States is not known. Given the low threshold for MRI neuroimaging, many patients' conditions are now discovered before they experience a brain hemorrhage.[4]

International

Reported detection rates range between 0.89 and 1.24 per 100,000 person-years according to reports from Australia, Sweden, and Scotland. The prevalence of cerebral AVMs in Scotland has been estimated to be 18 per 100,000 person-years.

Mortality/Morbidity

Although 300,000 persons in the United States may harbor AVMs, only 12% of AVMs are estimated to become symptomatic. Death occurs in 10–15% of patients who have hemorrhage, and morbidity of various degrees occurs in approximately 30–50%.

Age

Despite the presumed congenital origin of AVMs, the clinical presentation most commonly occurs in young adults.

AVM hemorrhage or seizure as an incident event may occur in young children or adults older than 40 years; however, childhood migraine is common.

A history of subtle learning disorder is elicited in 66% of adults with AVMs. This suggests early effects that are largely subclinical and do not come to medical attention.

History

AVMs tend to be clinically silent until the presenting event occurs. Therefore, the diagnosis usually is made at the time of the first seizure or hemorrhage.

A history of minor learning disability is present in as many as two thirds of patients; such dysfunction is rarely apparent in adult life.

A history of headaches is present in as many as half of patients with cerebral AVM. The headaches subsequently may take the form of classic migraine or more generalized headache.

If seizures have occurred, a careful seizure history should be obtained. Seizures are simple, partial, or secondarily generalized.

The effectiveness of anticonvulsant therapy should be observed carefully and monitored before and during treatment.

Physical

Focal neurologic findings are rare in the absence of seizure or hemorrhage in patients with cerebral AVMs. They are more common in brainstem and deeply located AVMs. They are associated with patient’s age and are more common among women.

Detailed neuropsychological testing may disclose subtle right or left hemisphere dysfunction.

If parenchymal hemorrhage is present, the physical findings are indistinguishable from those due to intracranial hemorrhage of other causes.

Intraventricular hemorrhage generally produces a less severe neurological deficit than hemorrhage into other areas of the brain.

In the rare patients in whom focal neurological deficits are present, the deficit may reflect the location of the AVM.

Causes

No genetic, demographic, or environmental risk factors for cerebral AVM have been identified clearly.

Families with cerebral AVMs are rare, and such pedigrees have been too small to enable linkage studies. From the few family cases reported, the inheritance appears to be autosomal dominant.

In a small minority of cases, cerebral AVMs are associated with other inherited disorders, such as the Osler-Weber-Rendu syndrome (ie, hereditary hemorrhagic telangiectasia), Sturge-Weber disease, neurofibromatosis, and von Hippel-Lindau syndrome.

Imaging Studies

High-quality imaging studies are the key to diagnosis of AVMs.

CT scan

CT scanning easily identifies an intracerebral hemorrhage, raising suspicion of AVM in a younger person or a patient without clear risk factors for hemorrhage.

CT scan can identify only large AVMs.

MRI

MRI is essential for initial diagnosis of AVMs.

AVMs appear as irregular or globoid masses anywhere within the hemispheres or brain stem, as shown in the images below.



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Axial T2 MRI showing an arteriovenous malformation with hemorrhage, in the territory of the left posterior cerebral artery.



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T1 axial MRI showing a small subcortical arteriovenous malformation in the right frontal lobe.



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T2 coronal MRI showing an arteriovenous malformation in the left medial temporal lobe.

AVMs may be cortical, subcortical, or in deep gray or white matter.

Small, round, low-signal spots within or around the mass on T1, T2, or fluid-attenuated inversion recovery (FLAIR) sequences are the "flow voids" of feeding arteries, intranidal aneurysms, or draining veins.

If hemorrhage has occurred, the mass of blood may obscure other diagnostic features, requiring angiogram or follow-up MRI.

Low signal of extracellular hemosiderin may be seen around or within the AVM mass, indicating prior symptomatic or asymptomatic hemorrhage.

Larger aneurysms within the AVM or on feeding arteries may be identified occasionally.

Magnetic resonance angiography (MRA) may identify AVMs greater than 1 cm in size, as in the image below, but is inadequate to delineate the morphology of feeding arteries and draining veins; small aneurysms can be missed easily.



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Magnetic resonance angiography showing a left medial temporal arteriovenous malformation.

A retrospective analysis demonstrated that silent intralesional microhemorrhage on CT/MRI may be a risk factor for intracerbral hemorrhage from a brain AVM rupture.[1]

Cerebral angiography

Angiogram, shown below, is required for hemodynamic assessment, which is essential for planning treatment.



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Angiogram (anteroposterior view) showing an arteriovenous malformation in the deep left middle cerebral artery territory measuring approximately 3 cm ....

The morphology of the AVM determines the treatment algorithm. Important features include feeding arteries, venous drainage pattern, and arterial and venous aneurysms.

Ten to fifty-eight percent of patients with AVM have aneurysms located in vessels remote from the AVM, in arteries feeding the AVM, or within the nidus of the AVM itself.

Intranidal aneurysms may have a higher risk of rupture than those outside the bounds of the AVM.

Other important angiographic features may include kinking or ectasia of draining veins, which can cause venous congestion, thrombosis, or rupture; and stenosis of feeding arteries due to angiopathy caused by high-velocity, turbulent flow into the fistula.

Special expertise is required to perform superselective catheterization into AVM feeding arteries, which allows both pressure measurements and superselective anesthetic injections to map neurological function in and around the AVM (see Superselective angiography in Procedures).

Other Tests

Based on flow-velocity and resistance pattern, transcranial Doppler (TCD) has been demonstrated to be a noninvasive and cost-effective means to detect and follow brain AVMs. Recently, TCD has been found to be a reliable, safe, and noninvasive method to monitor the outcome of gamma knife surgery for brain AVMs.[8]

Procedures

Superselective angiography

Superselective angiography is performed with standard cerebral angiography, with access via a femoral artery puncture.

A special, flexible, directable catheter is threaded up into one of the main cerebral arteries (carotid or vertebral), then into sequentially smaller branch arteries, until the catheter tip is near or within the AVM nidus.

Pressure measurements can be obtained via a coaxial catheter. Higher feeding pressures increase the risk of subsequent hemorrhage.

Sodium amytal, an anesthetic agent, can be injected to produce temporary anesthesia of the area perfused by the artery. In this so-called "superselective Wada testing," language, memory, visual-spatial, sensory, and motor function can be tested during 5 minutes of anesthetic effect to determine whether "eloquent" function originates in that region, which would therefore be at risk for neurological deficits should that brain area be injured during embolization or surgery. Arteries directly feeding the AVM or "en passage" vessels that feed the AVM but continue past the AVM to feed normal brain tissue can be studied.

Medical Care

Treatment planning for AVMs depends on risk of subsequent hemorrhage, which is determined by the demographic, historical, and angiographic features of the individual patient as discussed above. Prior hemorrhage, smaller AVM size, deep venous drainage, and relatively high arterial feeding pressures make subsequent hemorrhage more likely.

No randomized clinical trial comparing invasive treatment (staged embolization followed by either neurosurgical resection or radiosurgery) versus medical management alone of patients with a known brain AVM is available. There is little disagreement that patients with an AVM-related hemorrhage need treatment to avoid subsequent hemorrhages given the high recurrent hemorrhage rates. However, until recently, most patients with a diagnosis of an unruptured brain AVM were also considered candidates for invasive treatment to prevent a devastating hemorrhage. This concept has been challenged because of the low annual hemorrhage rates in patients who did not present with a brain hemorrhage.

To answer this question, the NIH-sponsored, multicenter Unruptured Brain Arteriovenous Malformations Trial (ARUBA) is conducted in the United States, Canada, Europe, and Australia.[9, 10] A total of 800 patients will be randomly assigned in 90 centers to invasive therapy (endovascular, surgical, and/or radiation therapy) versus medical management alone. Patients will be followed for a minimum of 5 years and a maximum of 7.5 years (mean, 6.25 y) from randomization. Final study results will not be available until 2012.

Until the ARUBA study results are available, treatment is recommended for the younger patient with one or more of the high-risk features for an AVM rupture, whereas an older individual or a patient with no high-risk features may be best treated by managing the medical aspects of the illness alone. In such patients, anticonvulsants for seizure control and appropriate analgesia for headaches may be the only treatment recommendations necessary.

Surgical Care

Invasive treatment of AVMs may include endovascular embolization, surgical resection, and focal beam radiation, alone or in any combination. The surgical treatment risk has traditionally been estimated by the Spetzler-Martin grading scale, which includes grades I-V. This grading system assigns 1 point to AVMs smaller than 3 cm in largest diameter, 2 points to AVMs between 3 and 6 cm in largest diameter, and 3 points for AVMs larger than 6 cm. A further point is added if the AVM is located in functionally critical brain (eg, language, motor, sensory, or visual cortex), and another point if the AVM has a deep venous drainage.

The current American Heart Association multidisciplinary management guidelines for the treatment of brain AVMs recommend the following approach:[2]

  1. Surgical extirpation is strongly suggested as the primary treatment for Spetzler-Martin grade I and II if surgically accessible with low risk.
  2. Radiation therapy alone is recommended for Spetzler-Martin grade I or II if the AVM is less than 3 cm in size and surgery has an increased surgical risk based on location and vascular anatomy.
  3. Brain AVM of Spetzler-Martin grades III can often be treated by a multimodal approach with embolization followed by surgical extirpation. If the lesion has a high surgical risk based on location and vascular anatomy, radiation therapy may be performed after embolization.
  4. AVMs of Spetzler-Martin grade IV and V are often not amenable to surgical treatment alone because of the high procedural risk. These AVMs can be approached by a combined multimodal approach of a combination of embolization, radiosurgery, and/or surgery.
  5. In general, embolization should only be performed if the goal is complete AVM eradication with other treatment modalities. The only exception is palliative embolization in patients with an AVM of Spetzler-Martin grade IV or V with venous outflow obstruction or true steal phenomenon in order to reduce arterial inflow to control edema or to reduce the amount of shunt, respectively.

A recent supplementary grading system used patient age, hemorrhagic presentation, nidal diffuseness, and deep perforating artery supply when selecting patients with brain AVMs for surgery. When used along with the Spetzler-Martin grading system, this grading system has been shown to have higher predictive accuracy, improving preoperative risk prediction and patient selection for surgery.[11]

Surgical resection

Surgical resection is the mainstay of definitive treatment and is most effective with more easily accessible lesions of smaller size.[12]

AVMs may be approached with craniotomy over the cerebral convexity, via the skull base, or via the ventricular system.

Arterial feeders are isolated and ligated. Then the nidus is resected. The draining veins are ligated last so that the pressure is not increased while the nidus is being resected. Arterial aneurysms may be clipped surgically as well. Intranidal aneurysms are resected with the AVM. Distal aneurysms are usually flow related and resolve when the AVM is resected.

Postsurgical angiography is done routinely to ensure that no residual AVM exists; however, cases of reappearance of AVMs, years after a negative postresection angiogram, have been reported.

Endovascular embolization

Superselective endovascular treatment includes delivery of thrombosing agents such as quick-acting acrylate glue (N -butyl cyanoacrylate [NBCA]), thrombus-inducing coils, Onyx liquid embolic fluid, or small balloons into the AVM nidus.

The goal of embolization is to block the high-velocity shunting of blood from the high-pressure arterial system into the venous system. Serial embolization sessions may whittle the AVM down to a fraction of its original size; the reduced AVM size and the presence of embolic material within the AVM make surgery and radiosurgery safer and more accurate. However, embolization can increase the pressure inside the nidus of the AVM due to the changes in blood flow and increases the rupture risk in the short term. Thus, if surgery is anticipated, it is usually scheduled 1-2 days after embolization. Embolization may be used to produce relief of neurologic symptoms caused by a large lesion, even if the goal of treatment is not complete obliteration. In most cases, embolization alone is not sufficient to completely obliterate the AVM. However, isolated case series have reported 11-40% of AVM obliteration with only endovascular embolization.

Embolization may be performed in a single-stage versus multistage approach. Although most literature support the use of the multistage approach, a retrospective study supports the safety and effectiveness of the aggressive single-stage embolization.[13] The single-stage approach has the inherent benefit of reducing the overall under treatment time reducing the intertreatment bleeding risk and brain AVM collateral reconstitution.

Radiosurgery

Radiosurgery is an option that is generally used to treat AVMs that are approximately 3 cm in diameter or less. Proton beam, linear accelerator, or gamma knife methods are used to deliver a high dose of radiation to the AVM, while minimizing the effects to surrounding brain tissue; a single dose generally is given. However, staged radiosurgery procedures are being used more frequently to treat symptomatic large AVMs in conjunction with embolization. During embolization, keep in mind if the patient is going to undergo radiosurgery, since patchy embolization of an AVM can make radiosurgery even more difficult. Radiotherapy is thought to work by inducing thrombosis. This approach is appealing because of its apparent noninvasiveness.

During the period after radiosurgery, the vessels are thrombosing and those AVMs that have ruptured are at a higher risk of rehemorrhage during that time. A single-center observational study from Spain has shown that radiosurgical therapy gradually decreases the long-term bleeding rates of both hemorrhagic and nonhemorrhagic AVM.[14]

MRI often shows high signal in surrounding brain white matter following treatment; actual mass effect from edema can be seen when larger territories are covered. Radiosurgery may take 1-3 years to achieve thrombosis of an AVM, thus the patient remains at risk for hemorrhage from AVM during the treatment period.

Combined radiosurgery and embolization

Controversies are noted in regard to the sequence of combined treatment commonly advocated to treat large AVMs. Kano et al reported their experience with stereotactic radiosurgery in patients harboring AVMs who had undergone prior embolization. Using a case-control matched approach, the authors determined that previously embolized AVMs have a lower rate of obliteration after SRS. This finding mirrors reports by other groups.[15] A long-term follow-up review is needed to determine the precise effects of partial or complete embolization on rebleeding, on seizures, and on progressive neurological deficits.[16] A systematic study of outcomes is needed so as to determine the best combination of approaches for such patients.

Consultations

Treatment of AVMs is best achieved with a multispecialty team comprising a neurologist, neuropsychologist, neurosurgeon, interventional neuroradiologist, and neuroanesthesiologist.

Activity

No particular activity restrictions are placed on patients with AVMs, besides the usual postsurgical care.

AVM patients with seizures should follow the same protocols as patients with epilepsy without AVM.

Further Outpatient Care

Seizure and/or headache medications usually are managed by the neurologist or referring physician.

Follow-up neuropsychological assessments may be helpful if subtle cognitive impairments are noted.

Patients who have suffered hemorrhage may need inpatient or outpatient rehabilitation like other patients with stroke.

Further Inpatient Care

The algorithm for surgical treatment is highly individual and is based on the angiographic characteristics of the AVM.

The most common treatment scenario is one or more endovascular embolization sessions during separate hospitalizations, followed by surgical resection or radiosurgery.

When hemorrhages occur as the presenting event, a longer hospitalization may be required, with supportive care during recovery from the brain hemorrhage.

Complications

The most dreaded complication of an AVM's natural history is intracerebral hemorrhage (see Prognosis). Treatment decisions are based on the natural history-risk of first or subsequent hemorrhage versus the risk-benefit ratio of treatment.

Surgical complications

Surgical complications may include persistent neurological deficits associated with hemorrhage and stroke.

Surgical outcome risk correlates with score on the Spetzler-Martin scale; higher scores, seen with large-sized AVMs, deep venous drainage, and location of the AVM in eloquent brain regions, increase the surgical risk.

A recent meta-analysis reports a morbidity of 8.6% and mortality of 3.3% after mostly surgical treatment in a series of 2452 patients.[17] The surgical risk for morbidity and mortality for Spetzler-Martin grade of less or equal to 3 has been reported to be 2-6.3% and 0-2%, respectively. The surgical risk for morbidity and mortality for Spetzler-Martin grade IV and V has been reported to be 9-39% and 0-9%, respectively.

Complications of endovascular embolization

Complications of endovascular embolization include persistent neurological deficits related to inadvertent embolization of arteries supplying normal brain tissue or obliteration of the venous outflow leading to intracerebral hemorrhages. The procedure carries an associated risk for morbidity and mortality in the range of 9-22% and 0-9%, respectively.

No long-term outcome studies are yet available; however, as endovascular techniques continue to improve, complication rates are likely to diminish.

Complications of radiosurgery

Complications depend on the size and location of the AVM. AVMs located in eloquent areas and in central locations are more prone to radiation-induced complications.

White matter edema and radiation-induced necrosis may occur during the 1- to 3-year treatment period. Persistent neurological deficits after radiation have been reported in 8% of treated patients.Patients with hemorrhagic presentation have a higher mean annual risk for hemorrhage until radiation-induced obliteration of the AVM is achieved compared to patients with a nonhemorrhagic presentation (6.3% vs 3.9%). The risk for hemorrhage seems to be lower after radiation therapy in patients with hemorrhagic presentation compared to the period before gamma knife radiotherapy was initiated.

Seizure frequency may increase in the first days to weeks after radiosurgery.

The potential for late effects from radiation, such as accelerated atherosclerosis in surrounding blood vessels, does exist.

Prognosis

With an overall risk of intracerebral hemorrhage of 2-4% per year, angiographic assessment is recommended to further define prognosis for patients with AVM.

Those with superficial, moderate-sized AVMs have a good long-term prognosis and may not have any additional benefit with interventional treatment.

Lifetime risk of hemorrhage may be substantial for young patients with AVM.

Prognosis after AVM hemorrhage is generally better than that after intracerebral hemorrhage from other causes. Better prognosis may be due to the relatively younger age of patients and a greater potential for reorganization of brain function. More accurate prognosis awaits the results of currently active, long-term, population-based outcome studies.

Patient Education

For excellent patient education resources, visit eMedicineHealth's Brain and Nervous System Center. Also, see eMedicineHealth's patient education article Stroke.

Author

Souvik Sen, MD, MPH, MS, FAHA, Professor and Chair, Department of Neurology, University of South Carolina School of Medicine

Disclosure: Nothing to disclose.

Coauthor(s)

James Selph, MD, Assistant Professor of Neurology, University of South Carolina School of Medicine; Director of Neurophysiology Lab and Services, Palmetto Richland Hospital

Disclosure: Nothing to disclose.

Specialty Editors

Francisco Talavera, PharmD, PhD, Adjunct Assistant Professor, University of Nebraska Medical Center College of Pharmacy; Editor-in-Chief, Medscape Drug Reference

Disclosure: Received salary from Medscape for employment. for: Medscape.

Howard S Kirshner, MD, Professor of Neurology, Psychiatry and Hearing and Speech Sciences, Vice Chairman, Department of Neurology, Vanderbilt University School of Medicine; Director, Vanderbilt Stroke Center; Program Director, Stroke Service, Vanderbilt Stallworth Rehabilitation Hospital; Consulting Staff, Department of Neurology, Nashville Veterans Affairs Medical Center

Disclosure: Nothing to disclose.

Chief Editor

Helmi L Lutsep, MD, Professor and Vice Chair, Department of Neurology, Oregon Health and Science University School of Medicine; Associate Director, OHSU Stroke Center

Disclosure: Medscape Neurology Editorial Advisory Board for: Stroke Adjudication Committee, CREST2; Physician Advisory Board for Coherex Medical; National Leader and Steering Committee Clinical Trial, Bristol Myers Squibb; Consultant, Abbott Vascular, Inc. .

Additional Contributors

Edward L Hogan, MD, Professor, Department of Neurology, Medical College of Georgia; Emeritus Professor and Chair, Department of Neurology, Medical University of South Carolina

Disclosure: Nothing to disclose.

Sharon W Webb, MD, Assistant Professor of Clinical Neurosurgery, University of South Carolina School of Medicine

Disclosure: Nothing to disclose.

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T1 axial MRI showing a small subcortical arteriovenous malformation in the right frontal lobe.

Axial T2 MRI showing an arteriovenous malformation with hemorrhage, in the territory of the left posterior cerebral artery.

T1 axial MRI showing a small subcortical arteriovenous malformation in the right frontal lobe.

T2 coronal MRI showing an arteriovenous malformation in the left medial temporal lobe.

Magnetic resonance angiography showing a left medial temporal arteriovenous malformation.

Angiogram (anteroposterior view) showing an arteriovenous malformation in the deep left middle cerebral artery territory measuring approximately 3 cm in diameter, with a deep draining vein (arrow).

Axial T2 MRI showing an arteriovenous malformation with hemorrhage, in the territory of the left posterior cerebral artery.

T1 axial MRI showing a small subcortical arteriovenous malformation in the right frontal lobe.

T2 coronal MRI showing an arteriovenous malformation in the left medial temporal lobe.

Magnetic resonance angiography showing a left medial temporal arteriovenous malformation.

Angiogram (anteroposterior view) showing an arteriovenous malformation in the deep left middle cerebral artery territory measuring approximately 3 cm in diameter, with a deep draining vein (arrow).