Abstract
SUMMARY: Magnetoencephalography, the extracranial detection of tiny magnetic fields emanating from intracranial electrical activity of neurons, and its source modeling relation, magnetic source imaging, represent a powerful functional neuroimaging technique, able to detect and localize both spontaneous and evoked activity of the brain in health and disease. Recent years have seen an increased utilization of this technique for both clinical practice and research, in the United States and worldwide. This report summarizes current thinking, presents recommendations for clinical implementation, and offers an outlook for emerging new clinical indications.
ABBREVIATIONS:
- ACR
- American College of Radiology
- AD
- Alzheimer disease
- ASD
- autism spectrum disorder
- CMS
- Centers for Medicare and Medicaid Services
- CPT
- Current Procedural Terminology
- ECD
- equivalent current dipole
- iEEG
- intracranial electroencephalography
- MEG
- magnetoencephalography
- MSI
- magnetic source imaging
Magnetoencephalography (MEG) is a noninvasive method of detecting neural activity in the brain with millisecond time resolution. The current clinically approved indications for MEG are localization of epileptic foci and localization of eloquent cortices for presurgical planning. The goal of the MEG community at large is to advance current clinical practices and to develop new clinical indications for MEG. Multiple groups have researched the use of MEG in a variety of clinical disorders including concussion, Alzheimer’s disease, autism, and others. Additionally, MEG can be used as an adjunct to other therapies, such as neuromodulation. Multispecialty collaboration is necessary for the successful development of a comprehensive clinical MEG program. The team includes clinicians, MEG scientists, and technologists, often with complementary and/or overlapping skill sets. MEG centers across the United States operate in various clinical departments. Close collaboration with Radiology, Neurology, and Neurosurgery has been instrumental in advancing MEG for clinical use. While there are several publications outlining good clinical practice for acquiring and analyzing clinical MEG data, at the current time, implementation varies across sites. In this report, we describe the current clinical landscape for MEG and emerging applications, as well as provide recommendations for the composition and training of multidisciplinary teams involved in the performance and interpretation of clinical MEG studies, including the roles of the physician, MEG scientist, and MEG technologist in performance of current and future clinically approved MEG studies. We advocate that clinical reporting should be performed after consultation with the entire team, including technologists, MEG scientists, and physicians.
Prior American College of Radiology Involvement in MEG
In 2001, with the joint support of the American College of Radiology (ACR), American Society of Neuroradiology, and American Academy of Neurology, 2 neuroradiologists (Roland Lee, Steven Stufflebeam) and 1 neurologist (Michael Funke) testified at the Centers for Medicare and Medicaid Services (CMS) in support of 3 new Current Procedural Terminology (CPT) codes for MEG:
95965 (MEG recording and analysis of spontaneous brain activity)
95966 (MEG recording and analysis of evoked magnetic fields, single technique)
95967 (MEG recording and analysis of evoked magnetic fields, each additional technique, after invoking 95966 once).
The Relative Value Scale Update Committee reviewed these codes at the April 2001 meeting, and CMS implemented the codes and payment rates in 2002, with subsequent scheduled reviews and revisions of the payment rates.
fMRI versus MEG
fMRI has been in clinical use for over 2 decades, slightly predating the clinical adoption of MEG. Clinical indications for fMRI involve presurgical mapping of eloquent cortex. While fMRI provides complementary information to MEG, the underlying neurophysiologic basis of the signal is quite different. Functional MR imaging relies on changes in blood flow associated with neuronal activity, making it an indirect measure of brain function, whereas MEG provides a more direct measure. Both modalities can provide accurate delineation of eloquent cortex. However, MEG is uniquely suited to identification of epileptogenic activity. Mapping of eloquent cortices can be performed at the same time as the epilepsy study with MEG. Clinical MR imaging scans are obtained separately from fMRI and MEG studies, with distinct CPT codes, and provide anatomic reference for functional maps. For both fMRI and MEG, robust paradigms exist for motor, sensory, and language mapping. For both modalities, areas of activation are mapped onto a structural MR imaging study as part of the presurgical evaluation.
Current Indications for MEG and Magnetic Source Imaging
Presurgical Mapping of Epileptogenic Zones.
MEG is clinically approved for preoperative planning in patients with intractable, or drug-resistant, epilepsy. The millisecond time resolution of MEG is ideally suited to capture bursts of abnormal neuroelectrical activity, as seen in epilepsy, and the spatial precision of magnetic source imaging (MSI) allows the accurate localization of the epileptogenic zone(s) (ie, seizure-generating tissue).1 The onset of each interictal epileptiform discharge is projected to source space (ie, brain space) as an equivalent current dipole (ECD) to visualize the location of potential seizure onset zone(s). In this way, MEG and MSI can provide unique information for presurgical planning in intractable epilepsy. MEG is optimally beneficial during presurgical planning for cases in which common noninvasive modalities result in an inconclusive hypothesis regarding epileptogenic zone location, MR imaging–negative (ie, nonlesional) cases, cases in which MR imaging identifies multiple lesions (eg, tuberous sclerosis), and patients with large lesions, anatomical malformations, and/or prior resection.1⇓-3
Empirical investigations have found that MEG and MSI contribute added clinical value during presurgical planning in patients with intractable epilepsy, as surgical resection of the epileptogenic zone(s) can eliminate or reduce seizures.4⇓-6 Presurgical planning often involves the acquisition of multiple neuroimaging modalities (eg, MR imaging, FDG-PET, ictal-SPECT, single-photon emission CT). These data are used to plan intracranial electroencephalography (iEEG), in which a grid of subdural electrodes and/or depth electrodes is implanted directly into the brain to confirm epileptogenic zone localization. Recent studies have revealed good concordance between MEG and iEEG in localizing epileptogenic activity, bolstering MEG’s potential as an alternative, noninvasive tool for preoperative planning.7
Inclusion of MEG in the presurgical neuroimaging battery bestows better clinical outcomes and correlates with postoperative seizure freedom.8,9 Specifically, resection patients in whom the MEG dipole cluster was completely sampled by iEEG had a strikingly higher chance of seizure freedom relative to patients with incomplete/no iEEG sampling. A similar finding was observed for patients in whom the MEG dipole cluster was completely resected relative to those with partial/no resection of the MEG cluster.9 Finally, patients with a single tight dipole cluster, those with a cluster that had stable orientation perpendicular to the closest major sulcus, and those with agreement between MEG and iEEG localization were more likely to be seizure-free postresection.
Presurgical Mapping of Eloquent Cortices.
MEG is used to noninvasively map the eloquent cortex in patients before they undergo epilepsy or brain tumor surgery. The goals are to minimize deleterious postoperative functional outcomes and/or identify whether functional reorganization has occurred. Specifically, localization of somatosensory, motor, auditory, and/or visual cortices, as well as localization and lateralization of language cortices may be performed to predict postsurgical outcomes and optimize the preservation of these functions postoperatively.10
Eloquent cortex mapping requires the application of specific tasks during MEG recording that are designed to elicit the functions of interest. These tasks generate magnetic evoked fields, and MSI is employed to localize stereotyped deflections in, or components of, the evoked magnetic field. The ability to capture different neurophysiological responses within 1 recording is a distinct advantage of MEG relative to fMRI, and MEG may be superior for functional mapping in patients who have cerebrovascular malformations or tumors near the functional cortex. However, MEG and fMRI often serve complementary roles in eloquent cortex mapping, and their amalgamation can enhance the reliability of functional localization.11,12
With respect to each function, somatosensory responses reliably map to the posterior bank of the central sulcus contralateral to the side of stimulation in a manner that follows expected somatotopic organization. In a similar fashion, motor responses localize to the primary motor cortex contralateral to the side of movement. Both contralateral and ipsilateral auditory responses may be localized and map to Heschl’s gyri. Visual responses localize to the primary visual cortex contralateral to the stimulated visual hemifield near the calcarine fissure.13,14 Importantly, prior research has found that such MEG-based localizations have high concordance with intraoperative cortical mapping. Finally, a distributed network of bilateral cortical regions often underlies language processing. Receptive language responses often localize to the posterior superior temporal gyrus (ie, Wernicke’s area), supramarginal gyrus, and angular gyrus, while expressive language responses often map to the pars triangularis and pars opercularis in the inferior frontal cortex (ie, Broca’s area). A laterality index is computed to determine hemispheric dominance of language function. Multiple studies have demonstrated high concordance between MEG-based language mapping and invasive procedures (eg, intracarotid amobarbital procedure or Wada), favoring MEG as a noninvasive option for language mapping and lateralization.10,15⇓⇓-18
A key transformative step is the integration of source-modeled MEG data with MR imaging to yield MSI, either by the overlay of single equivalent dipole sources or by statistical mapping of either spontaneous or event-related changes.19,20 This renders MEG data directly interpretable by the neuroradiologist in a fashion very analogous to fMRI, but combining both mapping of functional, eloquent cortex, as well as the sources of interictal spontaneous discharges (dysfunctional MR imaging).
CLINICAL MEG RECOMMENDATIONS
Roles, Training, and Certification/Accreditation
Qualifications of Physicians Interpreting Clinical MEG Studies.
Physicians interpreting and reporting clinical MEG studies should have appropriate medical licensure and proper training for the clinical application. For radiologists, this may include specialized clinical knowledge of neurophysiology, neuroanatomy, brain mapping, neuropsychology, and image acquisition and interpretation such as required through the American Board of Radiology Subspecialty Certification in Neuroradiology. In addition, MEG-specific training is recommended to include supervised learning or clinical practice of at least 50 MEG studies for the specific indication being reported. Alternatively, a minimum of 2 years of experience interpreting clinical fMRI or MEG brain mapping studies is recommended.
Qualifications of MEG Scientists Involved in Clinical MEG Studies.
MEG scientists involved in clinical MEG studies should be well-versed in signal processing, source analysis, neurophysiology, cognitive neuroscience, image processing, physics, and other scientific aspects of MEG and its application to patient care. In addition, MEG-specific training is recommended to include supervised learning or clinical practice of at least 50 MEG studies for the specific indication being reported, which can also be fulfilled through a minimum of 2 years of experience in the source modeling of MEG studies by a postdoctoral fellowship with a clinical MEG component, or through rotations at clinical MEG facilities.
Qualifications of MEG Technologists.
The MEG technologist should have a background in either EEG or imaging (eg, MR imaging) or related disciplines. Supervised learning or clinical practice of at least 50 MEG studies, including a review of the principles of MEG technology, technical aspects of the MEG systems, patient preparation, data acquisition, operational routines, tuning procedures, testing procedures, troubleshooting, artifact identification, prevention, and elimination, data storage, and basic source localization procedures. Alternatively, a minimum of 6 months of supervised clinical experience in an active MEG center is recommended.
Procedure/Workflow of Clinical MEG Examination, Analysis, and Reporting
MEG-guided localization of epileptogenic zones involves several key steps. Before recording, surface EEG electrodes and head position indicator coils are affixed to manufacturer-specified locations on the patient’s head. These coils generate a specific frequency during MEG recording to allow for head localization. The patient’s head shape and location of head position indicator coils is digitized for subsequent co-registration of MEG and structural MR imaging data. Simultaneous MEG and scalp EEG data are recorded. Typically, 40–120 minutes of spontaneous (ie, resting-state) data are collected. Due to the limited duration of recordings and the movement-related artifact introduced by seizures, ictal discharges are rarely captured. Rather, MEG recordings primarily capture interictal epileptiform discharges.8 To increase the yield of interictal epileptiform discharges during the scan, patients are asked to come sleep-deprived and sleep in the scanner.21 These data are preprocessed to remove noise and co-register the MEG data with a structural MR imaging (typically a 3D T1). Preprocessing algorithms and steps vary depending on the manufacturer. A professional with specialized training (eg, epileptologist, neurophysiologist, etc) reads the time-series EEG and MEG data and identifies epileptic discharges. The identified discharges are localized to source space via the ECD model, referred to as modeling in this article.22 Modeling can be completed by anyone with specialized training in the neuroscience, physics, and mathematical concepts behind the dipole model (eg, scientist, physician, technologist). Dipoles that meet statistical cutoff criteria (eg, goodness of fit, volume of confidence) are displayed on a structural MR imaging scan, which can be exported to PACS.
Dipoles may form clusters within a specific region. The clustering of 5 or more dipoles within a region is considered a reliable indicator of an epileptogenic zone.23 Both the tightness and orientation of the dipoles within a cluster have clinical relevance.1,9 The location of these dipoles and characteristics of any clusters formed are reported by a physician. A suggested template for reporting is located in the Appendix.
In contrast to presurgical mapping of epileptogenic zones, which relies on resting-state recordings, eloquent cortex mapping relies on task-based recordings. The patient should be awake and alert. During a task, identical or similar stimuli are repetitively delivered to the patient, and a corresponding trigger (eg, number) is time-stamped into the data. Offline, the data are epoched into meaningful windows of time surrounding each stimulus, baseline-normalized, and averaged together to enhance the signal-to-noise ratio. This distinguishes the magnetic evoked field generated by the stimuli, and components of the field are modeled to localize the functional cortex. The time and location of each component modeled are reported by a physician.
Somatosensory cortex mapping most often employs brief electrical stimulations to the median nerve. However, stimulation of the posterior tibial nerve and/or mechanical stimulation of the hand, foot, or other body regions may also be performed. To map the motor cortex, the patient is asked to perform a simple movement such as pressing a button, tapping a finger, or moving a foot at either a self-paced or visually- or auditorily-cued time interval. For auditory cortex mapping, often 1000-Hz tones are briefly presented through inserted ear tubes at 60 dB above the patient’s hearing threshold, either monaurally or binaurally.10,13 To map the visual cortex, stimuli, often checkerboards, are presented on a projector screen to the full visual field, each hemifield, or each quadrant. Language cortex mapping may utilize auditory and/or visual stimuli and can be grouped into 2 categories: receptive or expressive. Receptive language tasks include passively listening to words or silently reading words presented on the projector screen. Expressive language tasks include covert verb generation and picture naming.10,14,24
Many of the patients undergoing MEG have epilepsy that is poorly controlled by medications. It is important that safeguards be put in place for responding to medical emergencies. This includes the availability of emergency personnel and supplies depending on the setting.
Billing and Reimbursement
As noted in the Background, since 2002, the CMS has authorized and implemented 3 CPT codes and their payment rates for MEG: 95965, 95966, 95967. Using these 3 codes, clinical MEG is a well-established reimbursable procedure and is accepted as the standard of care in evaluation of patients with epilepsy and in the presurgical mapping of eloquent cortices.
Quality Improvement and Quality Control
A critical component of establishing and maintaining a high-quality clinical MEG program is to invest in the training and education of all team members. Most manufacturers offer training programs for new sites. The American Board of Registration of Electroencephalographic and Evoked Potential Technologists offers a MEG technologist certification program. Both the American Clinical MEG Society and the American Society for Functional Neuroradiology offer clinical guidelines, continuing education at annual meetings, and clinical MEG fellowship training programs for neurologists and neuroradiologists, respectively. Other relevant conferences include the biannual meeting of the International Society for the Advancement of Clinical MEG and the biannual International Conference on Biomagnetism. A number of excellent publications are available, including the MEG-EEG Primer textbook, Clinical Magnetoencephalography and Magnetic Source Imaging textbook, the November 2020 issue of the Journal of Clinical Neurophysiology, and clinical MEG guideline articles published by the International Federation of Clinical Neurophysiology and American Clinical MEG Society.13,24,25
A clear protocol for assessing the technical quality of the data is vital. Noise measurements and empty room recordings are often collected daily or before recording each patient to monitor changes in the environment and identify issues with equipment. During data acquisition, the position of the patient’s head within the MEG helmet is monitored for proper placement, observations of artifact and noise are documented, and averages of events during evoked testing may be computed online to visually inspect for the presence of the expected magnetic evoked fields. Routine (eg, monthly) quality-assurance testing of the digitization equipment, MEG system, and software is often conducted by utilizing a phantom for recordings. Collaborative interdepartmental conferences should also be held regularly to compare MEG results with clinical outcomes (eg, stereoelectroencephalography data).
EMERGING INDICATIONS
Concussion
Many articles in the peer-reviewed literature show that MEG can objectively diagnose concussions (mild traumatic brain injury) with significantly more sensitivity (about 85% sensitivity) than the relatively insensitive standard neuroimaging techniques such as CT or MR imaging.26⇓⇓⇓⇓⇓⇓-33 EEG has long demonstrated that low-frequency activity in the delta-band (1–4 Hz) is abnormal in awake, alert adults. Studies in animal models confirm that deafferentation of neurons due to traumatic injury to axons or blockage of cholinergic transmission will generate these slow/delta-waves.31,34 Resting-state MEG more sensitively detects delta waves than EEG, with about 85% sensitivity in diagnosing concussions compared with normal controls, even in single subjects when using an automated voxelwise algorithm, which also localizes the areas of abnormal slow-waves.26
Another MEG finding in patients with concussion is excessive synchronous resting-state high-frequency gamma-band activity (30–80 Hz) in certain frontal and other brain regions, which may be due to selective vulnerability of inhibitory GABAergic interneurons due to head trauma.29
Resting-state functional connectivity studies with MEG reveal various patterns of aberrant functional connectivity in patients with mild traumatic brain injury, likely reflecting differing mechanisms of injury, including disruption of networks, and injury to inhibitory GABAergic interneurons.32,33
Post-Traumatic Stress Disorder
Post-traumatic stress disorder affects about 7% of American adults during their lifetime and is especially prevalent in combat veterans. Compared with normal controls, MEG in patients with post-traumatic stress disorder shows differences in resting-state neurocircuitry, including hyperactivity in the amygdala, hippocampus, posterolateral orbitofrontal cortex, dorsomedial prefrontal cortex, and insular cortex in high-frequency (beta and gamma) bands; hypoactivity from the ventromedial prefrontal cortex, frontal pole, dorsolateral prefrontal cortex in high-frequency bands; and hypoactivity in the precuneus, dorsolateral prefrontal cortex, temporal and frontal poles, and sensorimotor cortex in alpha and low-frequency bands.35
Autism Spectrum Disorder
The physical properties of MEG offer sensitivity not only to spatial localization of detected signals but also characterization in terms of the time course and spectral content of such brain activity. As such, it may allow description of not just functional centers but also “when” the brain activity is occurring and, indeed, “what” is the nature of such activity. This opens up considerable promise for application to psychiatric disorders, commonly with no MR imaging–visible structural anomaly. One promising target disorder is autism spectrum disorder (ASD), a highly prevalent (∼2%) neurodevelopmental disorder. Although there is indeed an ultimate possibility (and current exploration) of identifying early electrophysiologic predictors of ASD in infants and young children, an alternative promising role for MEG lies in the stratification, or subtyping, of the remarkably heterogeneous ASD population. Such stratification may have value in terms of potential enrichment of clinical trials for behavioral/pharmaceutical therapies as well as potentially providing early “brain-level” indices of drug “target-engagement” as a predictor of ultimate efficacy. Considerable promise is shown in the latency of simple sensory evoked responses (eg, the auditory cortex 50-ms [M50] and 100-ms [M100] components, which tend to be delayed in children with ASD, perhaps triggering a cascade of delayed neural communication, with ultimate behavioral sequelae).36⇓-38
Dementia
Dementia is a neurodegenerative condition that usually affects people aged older than 65 years that causes major cognitive dysfunction, loss of independence, and reduced quality of life. The ever-increasing proportion of aged people in modern societies is leading to a substantial increase in the number of people affected by dementia and Alzheimer’s disease (AD) in particular, which is the most common cause for dementia. Several resting-state MEG studies have shown frequency-specific alterations in local and long-range neural synchrony in various dementias, even at the earliest prodromal stages of AD manifestation.39 Increased synchrony delta-theta bands and decreased alpha or beta bands are consistently reported not only in patients with the AD neuropathological spectrum including those who are asymptomatic but carry higher risk of AD, as well as in clinically symptomatic individuals with positive AD biomarkers,40⇓⇓⇓⇓⇓-46 but also in patients with variants of primary progressive aphasia, a form of dementia that impacts language function.47 Disruption of information flow quantified by MEG source imaging may also underlie clinical symptoms in AD.48 Studies have also reported task-induced MEG activity changes in AD with mismatch paradigms that highlight the translational potential for neurophysiological “signatures” of dementia, to understand disease mechanisms in humans and facilitate experimental medicine studies.49
CONCLUSIONS
MEG and MSI provide a powerful tool for characterizing brain activity in health and disease. Clinical applications as of this date are in the localization of spontaneous epileptiform activity as part of surgical work-up of patients with seizure disorders as well as presurgical mapping of eloquent cortex for patients undergoing resective surgery of tumors, AVMs, etc. However, there are many emerging applications being researched currently.
A neuroradiologist can be a key member of the team conducting and interpreting MEG studies. Promising future areas of MEG/MSI application will also likely capitalize on the neuroradiologist’s ability to work in a multidisciplinary team, integrating anatomic, physiologic, functional, and clinical information.
Footnotes
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References
- Received September 30, 2022.
- Accepted after revision October 4, 2022.
- © 2022 by American Journal of Neuroradiology