CT Angiography, Head/Brain - CAM 727

GENERAL INFORMATION

  • It is an expectation that all patients receive care/services from a licensed clinician. All appropriate supporting documentation, including recent pertinent office visit notes, laboratory data, and results of any special testing must be provided. If applicable: All prior relevant imaging results and the reason that alternative imaging cannot be performed must be included in the documentation submitted. 
  • Where a specific clinical indication is not directly addressed in this guideline, medical necessity determination will be made based on widely accepted standard of care criteria. These criteria are supported by evidence-based or peer-reviewed sources such as medical literature, societal guidelines and state/national recommendations. 

Policy 
INDICATIONS FOR BRAIN CTA
Brain CT/CTA are not approvable simultaneously unless they meet the criteria described below in the Indications for Brain CT/Brain CTA combination studies section. If there is a combination request* for an overlapping body part, either requested at the same time or sequentially (within the past 3 months) the results of the prior study should be:

  • Inconclusive or show a need for additional or follow up imaging evaluation OR 
  • The office notes should clearly document an indication why overlapping imaging is needed and how it will change management for the patient.

*Unless approvable in the combination section as noted in the guidelines

Patients with claustrophobia, limited ability to cooperate, an implanted device or in an urgent scenario may be better suited for CTA; whereas those with renal disease or iodine contrast allergy should have MRA.1

For evaluation of suspected intracranial vascular disease2,3

Aneurysm screening

  • Screening for intracranial aneurysm if two or more first-degree family members (parent, brother, sister, or child) of intracranial aneurysm

Note: Repeat study is recommended every 5 years4

  • For one first-degree relative with aneurysm, asymptomatic screening is not indicated - would require a neurological sign or symptom supporting clinical concern for aneurysm5,6,7
  • Screening for aneurysm in polycystic kidney disease (in adults), Loeys-Dietz syndrome, fibromuscular dysplasia, spontaneous coronary arteries dissection (SCAD), or known aortic coarctation (after age 10)8,9,10,11,12,13,14

For Loeys-Dietz, imaging should be repeated at least every two years

Vascular abnormalities 

  • Suspected vascular malformation (arteriovenous malformation (AVM) or dural arteriovenous fistula) in patient with previous or indeterminate imaging study
  • Thunderclap headache with continued concern for underlying vascular abnormality (i.e., aneurysm or reversible cerebral vasoconstriction syndrome) after initial negative brain imaging.15,16,17,18

Note: Negative brain CT < 6 hours after headache onset excludes subarachnoid hemorrhage in neurologically intact patients
15 MRI lacks sensitivity in excluding subarachnoid hemorrhage less than 24 hours after headache onset.16,19

  • Headache associated with exercise, exertion, Valsalva or sexual activity16
  • Isolated third nerve palsy (oculomotor) with pupil involvement to evaluate for aneurysm17
  • Pulsatile tinnitus to identify a suspected arterial vascular etiology18,20

Note: MRI is the study of choice for detecting low flow malformations (see background).21,22,23

Cerebrovascular Disease
Ischemic

  • Recent ischemic stroke or transient ischemic attack (See background section)24,25 Note: For remote strokes with no prior vascular imaging, imaging can be considered based on location/type of stroke and documented potential to change management 
  • Known or suspected vertebrobasilar insufficiency (VBI) in patients with symptoms such as dizziness, vertigo, headaches, diplopia, blindness, vomiting, ataxia, weakness in both sides of the body, or abnormal speech4,26,27

Hemorrhagic

  • Known subarachnoid hemorrhage (SAH)28
  • Known cerebral intraparenchymal hemorrhage with concern for underlying vascular abnormality

Venous and MRV is contraindicated or cannot be performed29 — CTV**

  • Suspected venous thrombosis (dural sinus thrombosis)30,31
  • Distinguishing benign intracranial hypertension (pseudotumor cerebri) from dural sinus thrombosis32,33

Sickle cells disease (ischemic and/or hemorrhagic) and MRA is contraindicated or cannot be performed34

  • Neurological signs or symptoms in sickle cell disease
  • Stroke risk in sickle cell patients (2 – 16 years of age) with a transcranial doppler velocity > 200

Vasculitis with initial laboratory workup (such as ESR, CRP, serology)35

  • Suspected secondary CNS vasculitis based on neurological signs or symptoms in the setting of an underlying systemic disease with abnormal inflammatory markers or autoimmune antibodies
  • Suspected primary CNS vasculitis based on neurological signs and symptoms with completed infectious/inflammatory lab work-up36,37

Other intracranial vascular disease

  • Suspected Moyamoya disease38,39
  • Suspected reversible cerebral vasoconstriction syndrome40
  • Giant cell arteritis with suspected intracranial involvement41

For evaluation of known intracranial vascular disease2, 3

  • Known intracranial aneurysm, treated aneurysm, or known vascular malformation (i.e., AVM or dural arteriovenous fistula)
  • Known vertebrobasilar insufficiency with new or worsening signs or symptoms (VBI)26,27
  • Known vasculitis, reversible cerebral vasoconstriction syndrome or Moyamoya disease36,38,39,40

Pre-operative/procedural evaluation for brain/skull surgery 

  • Pre-operative evaluation for a planned surgery or procedure

Post-operative/procedural evaluation42,43

  • A follow-up study may be needed to help evaluate a patient’s progress after treatment, procedure, intervention, or surgery. Documentation requires a medical reason that clearly indicates why additional imaging is needed for the type and area(s) requested.

Other Indications
Further evaluation of indeterminate findings on prior imaging (unless follow up is otherwise specified within the guideline):

  • For initial evaluation of an inconclusive finding on a prior imaging report that requires further clarification
  • One follow-up exam of a prior indeterminate MR/CT finding to ensure no suspicious interval change has occurred. (No further surveillance unless specified as highly suspicious or change was found on last follow-up exam.)

Indications for brain CTA/neck CTA combination studies

  • Recent ischemic stroke or transient ischemic attack24 (see background) 

Note: For remote strokes with no prior vascular imaging, imaging can be considered based on location/type of stroke and documented potential to change management. 

  • Known or suspected vertebrobasilar insufficiency (VBI) in patients with symptoms such as dizziness, vertigo, headaches, diplopia, blindness, vomiting, ataxia, weakness in both sides of the body, or abnormal speech26,27
  • Suspected carotid or vertebral artery dissection; secondary to trauma or spontaneous due to weakness of vessel wall44,45
  • Follow-up of known carotid or vertebral artery dissection within 3 – 6 months for evaluation of recanalization and/or to guide anticoagulation treatment46,47,48
  • Asymptomatic patients with an abnormal ultrasound of the neck or carotid duplex imaging (e.g., carotid stenosis ≥ 70%, technically limited study, aberrant direction of flow in the carotid or vertebral arteries) and patient is surgery or angioplasty candidate49,50,51
  • Symptomatic patients with an abnormal ultrasound of the neck or carotid duplex imaging (e.g., carotid stenosis ≥ 50%, technically limited study, aberrant direction of flow in the carotid or vertebral arteries) and patient is surgery or angioplasty candidate49,52
  • Pulsatile tinnitus to identify a suspected arterial vascular etiology18,20

Indications for Brain CT/Brain CTA combination studies2,3

  • Recent ischemic stroke or transient ischemic attack (TIA) when MRI is contraindicated or cannot be performed
  • Acute, sudden onset of headache with personal history of a vascular abnormality or first-degree family history of aneurysm
  • Headache associated with exercise, exertion, Valsalva or sexual activity when MRI is contraindicated or cannot be performed16
  • Suspected venous thrombosis (dural sinus thrombosis) and MRI is contraindicated or cannot be performed — CT/CTV**
  • Neurological signs or symptoms in sickle cell patients when MRI is contraindicated or cannot be performed
  • High stroke risk in sickle cell patients (2 – 16 years of age) with a transcranial doppler velocity > 200 when MRI is contraindicated or cannot be performed 

Indications for brain CT/brain CTA/neck CTA combination studies

  • Recent ischemic stroke or transient ischemic attack (TIA)2,3 when MRI is contraindicated or cannot be performed
  • Approved indications as noted above and being performed in high-risk populations (in whom MRI is contraindicated or cannot be performed) and will need anesthesia for the procedure and there is a suspicion of concurrent intracranial pathology

*Note: CTA and MRA are generally comparable noninvasive imaging alternatives each with their own advantages and disadvantages. Brain MRI can be combined with brain CTA/neck CTA.

Rationale
Computed tomography angiography (CTA) is recognized as a valuable diagnostic tool for the management of patients with cerebrovascular disease. With its three-dimensional 
reconstructions, CTA can simultaneously demonstrate the bony skull base and its related vasculature. CTA use of ionizing radiation and an iodine-based intravascular contrast medium is a disadvantage when compared to magnetic resonance angiography (MRA), but it is quicker and requires less patient cooperation than MRA. CTA is much less invasive than catheter angiography which involves injecting contrast material into an artery. 

CTA for evaluation of aneurysm — CTA is useful in the detection of cerebral aneurysms. The sensitivity of CTA to detect cerebral aneurysms < 5 mm is higher than that with digital subtraction angiography (DSA). Most aneurysms missed with CTA are < 3mm. Aneurysms in the region of the anterior clinoid process may extend into the subarachnoid space where they carry the threat of hemorrhage. CTA can help delineate the borders of the aneurysm in relation to the subarachnoid space and may help detect acute ruptured aneurysms. It may be used in the selection of patients for surgical or endovascular treatment of ruptured intracranial aneurysms. 

CTA for screening of patients with first-degree relative (parent, brother, sister or child) who has a history of aneurysm — Data has suggested that individuals with a parent, brother, sister, or child harboring an intracranial aneurysm are at increased risk of aneurysms. It is likely that multiple genetic and environmental risk factors contribute to the increased risk.

CTA and PCKD
Screening imaging every 5 years, and annual follow-up imaging in patients in with a known intracranial aneurysm is recommended. The current literature recommends initial screening by the age of 30 years and earlier if there is a strong family history of intracranial aneurysm. Screening is generally not recommended is the pediatric population (less than 18 years). No upper age limit for screening patients with ADPKD has been recommended.

CTA for evaluation of arteriovenous malformation (AVM) — A good correlation has been found between catheter angiography and CTA in the detection of arteriovenous malformations. CTA allows calculation of the volume of an AVM nidus and identifies and quantifies embolic material within it. CTA may be used for characterization and stereotactic localization before surgical resection or radiosurgical treatment of arteriovenous malformations. 

CTA and non-aneurysmal vascular malformations — Non-aneurysmal vascular malformations can be divided in low flow vascular malformations and high flow vascular malformations. Low flow vascular malformations include dural venous anomalies (DVA), cavernomas, and capillary telangiectasias. High-flow vascular malformations include AVM and dural arteriovenous fistulas (dAVF). For low flow malformations, MRI is the study of choice. There is limited medical literature to support vascular imagining (CTA or MRA). CTA plays a limited role in the assessment of cavernoma but may be used to demonstrate a DVA. MRA is not usually helpful in the assessment of cavernoma, capillary telangiectasia, and DVA. Vascular imaging is indicated in high flow vascular malformations.2,3,23

MRA vs CTA for CVA — Preferred vascular imaging of the head and neck includes non-contrast head MRA and contrast-enhanced neck MRA. MRA may not be able to be performed in patients with claustrophobia, morbid obesity, or implanted device, but it can be useful in patients with renal failure or contrast allergies. In patients with high radiation exposure, MRA as an alternative should be considered. For acute stroke, CTA is preferred after CT (to rule of hemorrhage) and to look for thrombus/possible intervention that is time-sensitive.53

CTA and recent stroke or transient ischemic attack — A stroke or central nervous system infarction is defined as “brain, spinal cord, or retinal cell death attributable to ischemia, based on neuropathological, neuroimaging, and/or clinical evidence of permanent injury. … Ischemic stroke specifically refers to central nervous system infarction accompanied by overt symptoms, whereas silent infarction causes no known symptoms”.54 If imaging or pathology is not available, a clinical stroke is diagnosed by symptoms persisting for more than 24 hours. Ischemic stroke can be further classified by the type and location of ischemia and the presumed etiology of the brain injury. These include large-artery atherosclerotic occlusion (extracranial or intracranial), cardiac embolism, small-vessel disease and less commonly dissection, hypercoagulable states, sickle cell disease and undetermined causes.55 TIAs in contrast, “are a brief episode of neurological dysfunction caused by focal brain or retinal ischemia, with clinical symptoms typically lasting less than one hour, and without evidence of acute infarction on imaging”.56 On average, the annual risk of future ischemic stroke after a TIA or initial ischemic 
stroke is 3% – 4%, with an incidence as high as 11% over the next 7 days and 24% – 29% over the following 5 years. This has significantly decreased in the last half century due to advances in secondary prevention.57

When revascularization therapy is not indicated or available in patients with an ischemic stroke or TIA, the focus of the work-up is on secondary prevention. This includes noninvasive vascular imaging to identify the underlying etiology, assess immediate complications and risk of future stroke. The majority of stroke evaluations take place in the inpatient setting. Admitting TIA patients is reasonable if they present within 72 hours and have an ABCD (2) score ≥ 3, indicating high risk of early recurrence, or the evaluation cannot be rapidly completed on an outpatient basis.56 Minimally, both stroke and TIA should have an evaluation for high-risk modifiable factors such as carotid stenosis atrial fibrillation as the cause of ischemic symptoms.55 Diagnostic recommendations include neuroimaging evaluation as soon as possible, preferably with magnetic resonance imaging, including DWI; noninvasive imaging of the extracranial vessels should be performed, and noninvasive imaging of intracranial vessels is reasonable.25

Patients with a history of stroke and recent work-up with new signs or symptoms indicating progression or complications of the initial CVA should have repeat brain imaging as an initial study. Patients with remote or silent strokes discovered on imaging should be evaluated for high-risk modifiable risk factors based on the location and type of the presumed etiology of the brain injury.

CTA for evaluation of vertebrobasilar insufficiency (VBI) — Multidetector CT angiography (MDCTA) may be used in the evaluation of vertebral artery pathologies. The correlation between MDCTA and color doppler sonography is moderate. CTA is used for minimally invasive follow-up after intracranial stenting for VBI. It enables visualization of the patency of the stent lumen and provides additional information about all brain arteries and the brain parenchyma. 

CTA and intracerebral hemorrhage — CTA is useful as a screening tool for an underlying vascular abnormality in the evaluation of spontaneous intracerebral hemorrhage (ICH). Etiologies of spontaneous ICH include tumor, vascular malformation, aneurysm, hypertensive arteriopathy, cerebral amyloid angiopathy, venous thrombosis, vasculitis, RCVS, drug-induced vasospasm, venous sinus thrombosis, Moyamoya disease, anticoagulant use and hemorrhagic transformation of an ischemic infarct. History can help point to a specific etiology. Possible risk factors for the presence of underlying vascular abnormalities include age younger than 65, female, lobar or intraventricular location, and the absence of hypertension or impaired coagulation.58

CTV and central venous thrombosis** — a CT venogram is indicated for the evaluation of a central venous thrombosis/dural sinus thrombosis. The most frequent presentations are isolated headache, intracranial hypertension syndrome, seizures, focal neurological deficits, and encephalopathy. Risk factors are hypercoagulable states inducing genetic prothrombotic conditions, antiphospholipid syndrome and other acquired prothrombotic diseases, such as cancer, oral contraceptives, pregnancy, puerperium (6 weeks postpartum), infections, and trauma. Since venous thrombosis can cause SAH, infarctions, and hemorrhage, parenchymal imaging with MRI/CT is also appropriate.29, 59,60,61

CTA and dissection — Craniocervical dissections can be spontaneous or traumatic. Patients with blunt head or neck trauma who meet Denver Screening criteria should be assessed forcerebrovascular injury (although about 20% will not meet criteria). The criteria include: focal or lateralizing neurological deficits (not explained by head CT), infarct on head CT, face, basilar skull, or cervical spine fractures, cervical hematomas that are not expanding, Glasgow coma score less than 8 without CT findings, massive epistaxis, cervical bruit or thrill.44,62,63,64 Spontaneous dissection presents with headache, neck pain with neurological signs or symptoms. There is often minor trauma or precipitating factor (i.e., exercise, neck manipulation). Dissection is thought to occur due to weakness of the vessel wall, and there may be an underlying connective tissue disorder. Dissection of the extracranial vessels can extend intracranially and/or lead to thrombus which can migrate into the intracranial circulation causing ischemia. Therefore, vascular imaging of the head and neck is warranted.45,65

Rationale
Computed tomography angiography (CTA) is recognized as a valuable diagnostic tool for the management of patients with cerebrovascular disease. With its three-dimensional 
reconstructions, CTA can simultaneously demonstrate the bony skull base and its related vasculature. CTA use of ionizing radiation and an iodine-based intravascular contrast medium is a disadvantage when compared to magnetic resonance angiography (MRA), but it is quicker and requires less patient cooperation than MRA. CTA is much less invasive than catheter angiography which involves injecting contrast material into an artery. 

CTA for evaluation of aneurysm — CTA is useful in the detection of cerebral aneurysms. The sensitivity of CTA to detect cerebral aneurysms < 5 mm is higher than that with digital subtraction angiography (DSA). Most aneurysms missed with CTA are < 3mm. Aneurysms in the region of the anterior clinoid process may extend into the subarachnoid space where they carry the threat of hemorrhage. CTA can help delineate the borders of the aneurysm in relation to the subarachnoid space and may help detect acute ruptured aneurysms. It may be used in the selection of patients for surgical or endovascular treatment of ruptured intracranial aneurysms. 

CTA for screening of patients with first-degree relative (parent, brother, sister or child) who has a history of aneurysm — Data has suggested that individuals with a parent, brother, sister,or child harboring an intracranial aneurysm are at increased risk of aneurysms. It is likely that multiple genetic and environmental risk factors contribute to the increased risk.

CTA and PCKD
Screening imaging every 5 years, and annual follow-up imaging in patients in with a known intracranial aneurysm is recommended. The current literature recommends initial screening by the age of 30 years and earlier if there is a strong family history of intracranial aneurysm. Screening is generally not recommended is the pediatric population (less than 18 years). No upper age limit for screening patients with ADPKD has been recommended.

CTA for evaluation of arteriovenous malformation (AVM) — A good correlation has been found between catheter angiography and CTA in the detection of arteriovenous malformations. CTA allows calculation of the volume of an AVM nidus and identifies and quantifies embolic material within it. CTA may be used for characterization and stereotactic localization before surgical resection or radiosurgical treatment of arteriovenous malformations. 

CTA and non-aneurysmal vascular malformations — Non-aneurysmal vascular malformations can be divided in low flow vascular malformations and high flow vascular malformations. Low flow vascular malformations include dural venous anomalies (DVA), cavernomas, and capillary telangiectasias. High flow vascular malformations include AVM and dural arteriovenous fistulas (dAVF). For low flow malformations, MRI is the study of choice. There is limited medical literature to support vascular imagining (CTA or MRA). CTA plays a limited role in the assessment of cavernoma but may be used to demonstrate a DVA. MRA is not usually helpful in the assessment of cavernoma, capillary telangiectasia, and DVA. Vascular imaging is indicated in high flow vascular malformations.2,3,23

MRA vs CTA for CVA — Preferred vascular imaging of the head and neck includes non-contrast head MRA and contrast-enhanced neck MRA. MRA may not be able to be performed in patients with claustrophobia, morbid obesity, or implanted device, but it can be useful in patients with renal failure or contrast allergies. In patients with high radiation exposure, MRA as an alternative should be considered. For acute stroke, CTA is preferred after CT (to rule of hemorrhage) and to look for thrombus/possible intervention that is time-sensitive.53

CTA and recent stroke or transient ischemic attack — A stroke or central nervous system infarction is defined as “brain, spinal cord, or retinal cell death attributable to ischemia, based on neuropathological, neuroimaging, and/or clinical evidence of permanent injury. … Ischemic stroke specifically refers to central nervous system infarction accompanied by overt symptoms, whereas silent infarction causes no known symptoms”.54 If imaging or pathology is not available, a clinical stroke is diagnosed by symptoms persisting for more than 24 hours. Ischemic stroke can be further classified by the type and location of ischemia and the presumed etiology of the brain injury. These include large-artery atherosclerotic occlusion (extracranial or intracranial), cardiac embolism, small-vessel disease and less commonly dissection, hypercoagulable states, sickle cell disease and undetermined causes.55 TIAs in contrast, “are a brief episode of neurological dysfunction caused by focal brain or retinal ischemia, with clinical symptoms typically lasting less than one hour, and without evidence of acute infarction on imaging”.56 On average, the annual risk of future ischemic stroke after a TIA or initial ischemic 
stroke is 3% – 4%, with an incidence as high as 11% over the next 7 days and 24% – 29% over the following 5 years. This has significantly decreased in the last half century due to advances in secondary prevention.57

When revascularization therapy is not indicated or available in patients with an ischemic stroke or TIA, the focus of the work-up is on secondary prevention. This includes noninvasive vascular imaging to identify the underlying etiology, assess immediate complications and risk of future stroke. The majority of stroke evaluations take place in the inpatient setting. Admitting TIA patients is reasonable if they present within 72 hours and have an ABCD (2) score ≥ 3, indicating high risk of early recurrence, or the evaluation cannot be rapidly completed on an outpatient basis.56 Minimally, both stroke and TIA should have an evaluation for high-risk modifiable factors such as carotid stenosis atrial fibrillation as the cause of ischemic symptoms.55 Diagnostic recommendations include neuroimaging evaluation as soon as possible, preferably with magnetic resonance imaging, including DWI; noninvasive imaging of the extracranial vessels should be performed, and noninvasive imaging of intracranial vessels is reasonable.25

Patients with a history of stroke and recent work-up with new signs or symptoms indicating progression or complications of the initial CVA should have repeat brain imaging as an initial study. Patients with remote or silent strokes discovered on imaging should be evaluated for high-risk modifiable risk factors based on the location and type of the presumed etiology of the brain injury.

CTA for evaluation of vertebrobasilar insufficiency (VBI) — Multidetector CT angiography (MDCTA) may be used in the evaluation of vertebral artery pathologies. The correlation between MDCTA and color doppler sonography is moderate. CTA is used for minimally invasive follow-up after intracranial stenting for VBI. It enables visualization of the patency of the stent lumen and provides additional information about all brain arteries and the brain parenchyma. 

CTA and intracerebral hemorrhage — CTA is useful as a screening tool for an underlying vascular abnormality in the evaluation of spontaneous intracerebral hemorrhage (ICH). Etiologies of spontaneous ICH include tumor, vascular malformation, aneurysm, hypertensive arteriopathy, cerebral amyloid angiopathy, venous thrombosis, vasculitis, RCVS, drug-induced vasospasm, venous sinus thrombosis, Moyamoya disease, anticoagulant use and hemorrhagic transformation of an ischemic infarct. History can help point to a specific etiology. Possible risk factors for the presence of underlying vascular abnormalities include age younger than 65, female, lobar or intraventricular location, and the absence of hypertension or impaired coagulation.58

CTV and central venous thrombosis** — a CT venogram is indicated for the evaluation of a central venous thrombosis/dural sinus thrombosis. The most frequent presentations are isolated headache, intracranial hypertension syndrome, seizures, focal neurological deficits, and encephalopathy. Risk factors are hypercoagulable states inducing genetic prothrombotic conditions, antiphospholipid syndrome and other acquired prothrombotic diseases, such as cancer, oral contraceptives, pregnancy, puerperium (6 weeks postpartum), infections, and trauma. Since venous thrombosis can cause SAH, infarctions, and hemorrhage, parenchymal imaging with MRI/CT is also appropriate.29, 59,60,61

CTA and dissection — Craniocervical dissections can be spontaneous or traumatic. Patients with blunt head or neck trauma who meet Denver Screening criteria should be assessed for cerebrovascular injury (although about 20% will not meet criteria). The criteria include: focal or lateralizing neurological deficits (not explained by head CT), infarct on head CT, face, basilar skull, or cervical spine fractures, cervical hematomas that are not expanding, Glasgow coma score less than 8 without CT findings, massive epistaxis, cervical bruit or thrill.44,62,63,64 Spontaneous dissection presents with headache, neck pain with neurological signs or symptoms. There is often minor trauma or precipitating factor (i.e., exercise, neck manipulation). Dissection is thought to occur due to weakness of the vessel wall, and there may be an underlying connective tissue disorder. Dissection of the extracranial vessels can extend intracranially and/or lead to thrombus which can migrate into the intracranial circulation causing ischemia. Therefore, vascular imaging of the head and neck is warranted.45,65

References  

  1. Chen X, Liu Y, Tong H, et al. Meta-analysis of computed tomography angiography versus magnetic resonance angiography for intracranial aneurysm. Medicine (Baltimore). May 2018;97(20):e10771. doi:10.1097/md.0000000000010771 
  2. Robertson RL, Palasis S, Rivkin MJ, et al. ACR Appropriateness Criteria® Cerebrovascular Disease-Child. J Am Coll Radiol. May 2020;17(5s):S36-s54. doi:10.1016/j.jacr.2020.01.036
  3. Salmela MB, Mortazavi S, Jagadeesan BD, et al. ACR Appropriateness Criteria(®) Cerebrovascular Disease. J Am Coll Radiol. May 2017;14(5s):S34-s61.  doi:10.1016/j.jacr.2017.01.051
  4. Chalouhi N, Chitale R, Jabbour P, et al. The case for family screening for intracranial aneurysms. Neurosurg Focus. Dec 2011;31(6):E8. doi:10.3171/2011.9.Focus11210
  5. Rinkel GJ, Ruigrok YM. Preventive screening for intracranial aneurysms. Int J Stroke. Jan 2022;17(1):30-36. doi:10.1177/17474930211024584
  6. Risks and benefits of screening for intracranial aneurysms in first-degree relatives of patients with sporadic subarachnoid hemorrhage. N Engl J Med. Oct 28  1999;341(18):1344-50. doi:10.1056/nejm199910283411803
  7. Brown RD, Jr., Huston J, Hornung R, et al. Screening for brain aneurysm in the Familial Intracranial Aneurysm study: frequency and predictors of lesion detection. J Neurosurg. Jun 2008;108(6):1132-8. doi:10.3171/jns/2008/108/6/1132
  8. Hayes SN, Kim ESH, Saw J, et al. Spontaneous Coronary Artery Dissection: Current State of the Science: A Scientific Statement From the American Heart Association. Circulation. May 8 2018;137(19):e523-e557. doi:10.1161/cir.0000000000000564
  9. Hitchcock E, Gibson WT. A Review of the Genetics of Intracranial Berry Aneurysms and Implications for Genetic Counseling. J Genet Couns. Feb 2017;26(1):21-31. doi:10.1007/s10897-016-0029-8
  10. Jung WS, Kim JH, Ahn SJ, et al. Prevalence of Intracranial Aneurysms in Patients with Aortic Dissection. AJNR Am J Neuroradiol. Nov 2017;38(11):2089-2093. doi:10.3174/ajnr.A5359
  11. Egbe AC, Padang R, Brown RD, et al. Prevalence and predictors of intracranial aneurysms in patients with bicuspid aortic valve. Heart. Oct 2017;103(19):1508-1514. doi:10.1136/heartjnl-2016-311076
  12. Rouchaud A, Brandt MD, Rydberg AM, et al. Prevalence of Intracranial Aneurysms in Patients with Aortic Aneurysms. AJNR Am J Neuroradiol. Sep 2016;37(9):1664-8.doi:10.3174/ajnr.A4827
  13. Malhotra A, Wu X, Matouk CC, Forman HP, Gandhi D, Sanelli P. MR Angiography Screening and Surveillance for Intracranial Aneurysms in Autosomal Dominant Polycystic Kidney Disease: A Cost-effectiveness Analysis. Radiology. May 2019;291(2):400-408. doi:10.1148/radiol.2019181399
  14. Flahault A, Joly D. Screening for Intracranial Aneurysms in Patients with Autosomal Dominant Polycystic Kidney Disease. Clin J Am Soc Nephrol. Aug 7 2019;14(8):1242-1244. doi:10.2215/cjn.02100219
  15. Chen CY, Fuh JL. Evaluating thunderclap headache. Curr Opin Neurol. Jun 1 2021;34(3):356-362. doi:10.1097/wco.0000000000000917
  16. Headache Classification Committee of the International Headache Society (IHS) The International Classification of Headache Disorders, 3rd edition. Cephalalgia. Jan 2018;38(1):1-211. doi:10.1177/0333102417738202
  17. Pula JH, Kwan K, Yuen CA, Kattah JC. Update on the evaluation of transient vision loss. Clin Ophthalmol. 2016;10:297-303. doi:10.2147/opth.S94971
  18. Hofmann E, Behr R, Neumann-Haefelin T, Schwager K. Pulsatile tinnitus: imaging and differential diagnosis. Dtsch Arztebl Int. Jun 2013;110(26):451-8. doi:10.3238/arztebl.2013.0451
  19. Marcolini E, Hine J. Approach to the Diagnosis and Management of Subarachnoid Hemorrhage. West J Emerg Med. Mar 2019;20(2):203-211.  doi:10.5811/westjem.2019.1.37352
  20. Pegge SAH, Steens SCA, Kunst HPM, Meijer FJA. Pulsatile Tinnitus: Differential Diagnosis and Radiological Work-Up. Curr Radiol Rep. 2017;5(1):5. doi:10.1007/s40134-017-0199-7
  21. Morrison L, Akers A. Cerebral Cavernous Malformation, Familial. University of Washington, . Updated August 4, 2016. Accessed January 29, 2023. https://www.ncbi.nlm.nih.gov/books/NBK1293/
  22. Zyck S, Gould GC. Cavernous Venous Malformation. StatPearls Publishing. Updated May 9, 2022. Accessed January 23, 2023.  https://www.ncbi.nlm.nih.gov/books/NBK526009/
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Coding Section

Code Number Description
CPT 70496 Diagnostic Radiology (Diagnostic Imaging) Procedures of the Head and Neck

Procedure and diagnosis codes on Medical Policy documents are included only as a general reference tool for each policy. They may not be all-inclusive. 

This medical policy was developed through consideration of peer-reviewed medical literature generally recognized by the relevant medical community, U.S. FDA approval status, nationally accepted standards of medical practice and accepted standards of medical practice in this community, Blue Cross Blue Shield Association technology assessment program (TEC) and other nonaffiliated technology evaluation centers, reference to federal regulations, other plan medical policies, and accredited national guidelines.

"Current Procedural Terminology © American Medical Association. All Rights Reserved" 

History From 2019 Forward     

11/09/2023 Annual review. Adding language related to indeterminate prior imaging, follow up of known carotid or vertebral artery dissection. Notes added related CTA vs MRA and remote strokes. Also adding clarifying language to policy verbiage that does not change the policy intent. Updating entire policy for consistency.
11/10/2022 Annual review, adding statement regarding documentation needed to support combination studies or overlapping body parts. Also reformatting policy for clarity and specificity.)

11/29/2021 

Annual review, added criteria regarding giant cell arteritis, Loeys-Dietz, vertebrobasilar insufficiency and vasculitis.

11/04/2020 

Annual review, multiple additions and revisions to the policy criteria. Also updating description and references. 

11/19/2019

New Policy

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