Bioelectric Artifacts

Eye-movement artifacts are generated by the corneoretinal potential, which is in the order of 100 mV and has been likened to a dipole with the positive pole at the cornea and the negative pole at the retina. Eye movement leads to a positive potential recorded by the electrodes closest to the cornea. Thus, with upward movement of the eyes (such as occurs during a blink), a positive potential is recorded at the frontopolar (supraorbital) electrodes relative to more posteriorly placed electrodes, and thus a downward deflection occurs at these electrodes. Such eye movement is easily distinguished from frontal slow EEG activity by recording from an infraorbital electrode referenced to the mastoid process; the former leads to activity that is out of phase between the supra- and infraorbital electrodes, whereas frontal EEG activity is in phase. Similarly, horizontal eye movements lead to a positivity at the frontotemporal electrode on the side to which the eyes are moved and a corresponding negativity on the opposite side ( Fig. 3-4 ). Nystagmus or eyelid flutter, for example, produces a rhythmic discharge in the frontal electrodes (see Fig. 3-4 ). Oblique eye movements and asymmetric eye movements may be confusing, but are usually easily distinguished by experienced electroencephalographers.

Eye movements. A , Eye closure. B , Lateral eye movement. C , Eyelid flutter. LIO, left infraorbital; LOC, left outer canthus.

Cardiac artifacts are related to the ECG or ballistocardiogram and are especially conspicuous when monitoring for electrocerebral inactivity in brain-death suspects or in referential recordings involving the ears (see Fig. 3-2 ). The ECG can be monitored by electrodes placed on the chest and recorded on a separate channel, thereby facilitating recognition of such artifacts in the scalp recording, which may otherwise be misinterpreted as sharp waves or spike discharges. Conspicuous ECG artifact may obscure underlying low-voltage electrocerebral activity, a point of concern when comatose patients are being examined for possible brain death. Pulse artifact may occur at any site but typically is localized to a single electrode and appears as a recurrent slow wave that sometimes has a saw-toothed appearance and is time-locked to the ECG. It occurs when an electrode is placed over or close to an artery, and movement of the electrode will eliminate it. Pacemaker artifacts consist of spike discharges that precede the ECG.

Muscle artifact is composed of brief-duration spike discharges that are too rapid to be cerebral in origin. Chewing artifacts are electromyographic (EMG) artifacts produced by the temporalis muscles (see Fig. 3-2 ). Sucking artifact (in infants) is characterized by bitemporal sharp activity that may be difficult to identify without careful observation of the baby. Lateral rectus spikes are recorded from the anterior temporal electrodes and relate to horizontal eye movements; they are out of phase on the two sides of the head. Attempting to relax or quieten the patient should reduce muscle artifact. In most instances, high-frequency filters should not be used for this purpose, except as a last resort, because they simply alter the appearance of the artifact (sometimes so that it looks more like EEG fast activity) and also influence the background EEG.

Movement produces artifact in addition to muscle activity. Any movements may produce such artifacts, and these will vary in appearance depending on the nature and site of the movement. Movements arising at a consistent site may be monitored by a pair of electrodes and recorded on a separate channel. Hiccups produce a brief generalized movement artifact that may have a pseudo-periodic quality; this is not confined to the EEG but is seen also in, for example, the ECG channel. Glossokinetic artifact relates to the difference in potential between the tip of the tongue and its base; tongue movements generate slow waves that are recorded over one or both temporal regions ( Fig. 3-5 ). When suspected, tongue movements may be monitored by a submental electrode.

EEG showing rhythmic slow waves in the temporal regions relating to glossokinetic artifact. It can be seen that the cerebral activity is in phase with activity recorded infraorbitally (indicating that it is not eye movement artifact) and out of phase with activity recorded submentally.

Sweat artifact is common and is characterized by high-amplitude potentials of very low frequency. Low-frequency filters can attenuate these slow waves.

Instrumental Artifacts

Background 60-Hz noise in a restricted number of channels is often related to mismatched electrical impedance of electrode pairs or to the poor application of electrodes so that slight movement alters transiently the impedance of an individual electrode. A 60-Hz interference signal normally is common to the pair of electrodes connected to an amplifier; the differential amplifier essentially discards this common signal. If the electrical impedance of one of the electrodes is altered, however, the current flowing across that electrode–skin interface will be altered, thereby leading to voltage differences between one electrode and the other of the pair. The differential amplifier will magnify these differences so that the 60-Hz artifact then becomes obtrusive. In addition, other artifacts related to movement arise at that electrode and are limited to the channel with which the faulty electrode is connected, causing “mirror-image” phase reversals when these channels are part of a linked bipolar montage. Widespread 60-Hz artifact is of concern because it may indicate a safety problem warranting attention as discussed in Chapter 2 , where the various artifacts that arise in digital equipment also are considered.

Alpha Rhythm

Alpha rhythm may have a frequency of between 8 and 13 Hz, but in most adults it is between 9 and 11 Hz. This rhythm is found most typically over the posterior portions of the head during wakefulness, but it may also be present in the central or temporal regions. Alpha rhythm is seen best when the patient is resting with the eyes closed. Immediately after eye closure, its frequency may be increased transiently (the “squeak” phenomenon). The alpha rhythm is not strictly monorhythmic but varies over a range of about 1 Hz, even under stable conditions. It is usually sinusoidal in configuration, may wax and wane spontaneously in amplitude, and sometimes has a spiky appearance; a spindle configuration denotes a beating phenomenon that results from the presence of two (or more) dominant frequencies.

The alpha rhythm is attenuated or abolished by visual attention ( Fig. 3-6 ) and affected transiently by other sensory stimuli and by other mental alerting activities (e.g., mental arithmetic) or by anxiety. The term paradoxical alpha rhythm refers to the appearance of alpha rhythm on eye-opening in drowsy subjects; this represents an alerting response. Alpha activity is well formed and prominent in many normal subjects but is relatively inconspicuous or absent in about 10 percent of instances. Its precise frequency is usually of little diagnostic significance unless information is available about its frequency on earlier occasions. In children, the dominant, posterior responsive rhythm reaches about 8 Hz by the age of 3 years and reaches 10 Hz by approximately 10 years of age. Slowing occurs with advancing age; as a consequence of certain medication (e.g., anticonvulsant drugs); and in patients with clouding of consciousness, metabolic disorders, or virtually any type of cerebral pathology. The alpha activity may increase in frequency in children as they mature and in older subjects who are thyrotoxic. A slight asymmetry is often present between the two hemispheres with regard to the amplitude of alpha activity and the degree to which it extends anteriorly. In particular, alpha rhythm may normally be up to 50 percent greater in amplitude over the right hemisphere, possibly because this is the nondominant hemisphere or because of variation in skull thickness. A more marked asymmetry of its amplitude may have lateralizing significance but is difficult to interpret unless other EEG abnormalities are present, because either depression or enhancement may occur on the side of a hemispheric lesion. Similarly, a persistent difference in alpha frequency of more than 1 to 2 Hz between the two hemispheres is generally regarded as abnormal. The side with the slower rhythm is more likely to be the abnormal one, but it is usually difficult to be certain unless other abnormalities are also found.

Normal 9- to 10-Hz alpha rhythm recorded in the electroencephalogram of a 64-year-old man. The posterior distribution and responsiveness to eye-opening of the rhythm can be seen.

Unilaterally attenuated or absent responsiveness of the alpha rhythm sometimes occurs with lesions of the parietal or temporal lobe (Bancaud phenomenon). Asymmetric attenuation of the alpha rhythm during mental alerting procedures with the eyes closed may also be helpful for lateralizing any impairment of cerebral function.

Some normal adults have an alpha rhythm that is more conspicuous centrally or temporally than posteriorly, or has a widespread distribution. Care must be taken not to misinterpret such findings as evidence of abnormality. The so-called slow alpha variant resembles normal alpha rhythm in distribution and reactivity but has a frequency of about 4 to 5 Hz, which approximates one-half that of any alpha rhythm in the same record. This variant is of no pathologic significance.

Other Rhythms of Alpha Frequency

Not all activity having a frequency of 8 to 13 Hz is necessarily an alpha rhythm. Alpha-frequency activity that is widespread in distribution and unresponsive to external stimulation is found in some comatose patients ( p. 79 ). Temporal alpha activity is sometimes found in elderly subjects and may be asynchronous, episodic, and persistent during drowsiness. Runs of activity in the alpha range of frequencies are occasionally found frontally in children immediately after arousal from sleep (frontal arousal rhythm) and are not of pathologic significance.

Mu rhythm has a frequency that usually is in the alpha range, is seen intermittently over the central region of one or both hemispheres, is unaffected by eye-opening, and is blocked unilaterally or bilaterally by movement or the thought of movement ( Fig. 3-7 ). It is also blocked by sensory stimulation. Bilateral mu rhythm is often asynchronous and may exhibit amplitude asymmetries between the two hemispheres. The negative portions of the waves are sharpened, and the positive portions are generally rounded. Mu rhythm is often associated with a centrally located beta rhythm that is also attenuated by contralateral movement. In most instances, mu rhythm has no diagnostic significance. It is found in about 20 percent of young adults. When recorded over a skull defect, it may be mistaken for a potential epileptogenic abnormality.

Bilateral mu rhythm recorded in the electroencephalogram of a 26-year-old woman with no neurologic disorder. The effect on the rhythm of clenching the right fist can be seen.

Polymorphic Delta Activity

Polymorphic delta activity is continuous, irregular, slow activity that varies considerably in duration and amplitude with time; it persists during sleep, and shows little variation with change in the physiologic state of the patient ( Fig. 3-8 ). It has been related to deafferentation of the involved area of the cortex and to metabolic factors. Such activity may be found postictally and in patients with metabolic disorders. It is commonly seen, with a localized distribution, over destructive cerebral lesions involving subcortical white matter ( Fig. 3-9 ), but it generally is not found with lesions restricted to the cerebral cortex itself. It may be found either unilaterally or bilaterally in patients with thalamic tumors or lesions of the midbrain reticular formation, but its distribution in such circumstances is somewhat variable. Thus, although diffuse irregular slow activity is found over one hemisphere in some cases, in others it has a more restricted distribution.

Electroencephalogram of a 19-year-old patient with encephalitis, showing a background of diffuse, irregular theta and delta activity.

Electroencephalogram of a 52-year-old man who had a right parietal glioma. Note the polymorphic slow-wave focus in the right central region and the diffusely slowed background.

The EEG finding of focal polymorphic delta activity correlates with the presence of focal abnormalities on neuroimaging, but nonfocal abnormalities (e.g., diffuse atrophy or cerebral edema) are sometimes found. The maximal delta focus may not always overlie the structural abnormality, even though it is in the same hemisphere. The amplitude, frequency, and distribution of focal slow waves do not relate to lesion size or to mass effect. In some patients with focal polymorphic slow-wave activity, no abnormalities whatsoever are present on CT scans; such patients usually have seizure disorders, cerebral trauma, or cerebral ischemia.

Diffuse polymorphic delta activity occurs in patients with white matter encephalopathies and following acute or extensive lesions of the upper brainstem.

Intermittent Rhythmic Delta Activity

Intermittent rhythmic delta activity is paroxysmal, has a relatively constant frequency, and is usually synchronous over the two hemispheres. It is often more prominent occipitally in children or frontally in adults ( Fig. 3-10 ), may be enhanced by hyperventilation or drowsiness, and usually is attenuated by attention. Its origin is unclear, but it probably relates to dysfunction of subcortical centers influencing the activity of cortical neurons. Its significance is considered on page 51 .

Frontal intermittent rhythmic delta activity recorded in the electroencephalogram of a 14-year-old boy with obstructive hydrocephalus.

Spike-Wave Activity

Generalized, bilaterally symmetric and bisynchronous 2.5- to 3-Hz spike-wave activity is the expected finding in patients with primary or idiopathic generalized epilepsy; it is enhanced by hyperventilation or hypoglycemia. More is known about the fundamental mechanisms underlying the absence seizures that occur in primary generalized epilepsy than about other types of generalized seizure. Gloor and Fariello related the generalized spike-wave activity associated with absence seizures to abnormal oscillatory discharges between cortical and thalamic neurons. This oscillation involves the regular alternation of brief periods of neuronal excitation (associated with a markedly increased firing probability) during the spike phase with longer periods of neuronal silence during the slow-wave phase. Large populations of cortical and thalamic neurons are affected in near-synchrony, and the brainstem reticular formation also participates.

Generalized 2.5- to 3-Hz spike-wave activity may also be found in secondary generalized epilepsy (i.e., in patients with generalized seizures secondary to known pathology), but it is then superimposed on a diffusely abnormal background and is often accompanied by other EEG abnormalities. In the secondary generalized epilepsies, however, slow ( p. 62 ) or atypical ( p. 63 ) spike-wave activity is found more commonly. Generalized, bisynchronous spike-wave activity rarely may arise from a unilateral cortical focus, particularly on the medial surface of the hemisphere; this phenomenon is referred to as secondary bilateral synchrony . In such circumstances, the paroxysmal activity usually has a faster or slower frequency than that in primary generalized epilepsy, and the form and relationship of the spike to the wave component of the complex are less regular. Further, a consistent asymmetry of amplitude and waveform may exist between the hemispheres, the activity being either more or less conspicuous on the affected side. Recognition of the cortical origin of such activity is facilitated when isolated focal discharges arise from one side, particularly if they consistently precede the bursts of bilaterally synchronous activity; otherwise, recognition can be difficult unless the paroxysmal discharges have a focal or lateralized onset.

The mechanisms generating secondary bilateral synchrony of spike-wave discharges are not fully established but may involve either the propagation of discharges from one hemisphere to the other along the forebrain commissures or the activation by a cortical focus of diencephalic or other midline structures, which then elicit a synchronous discharge from both hemispheres. Studies have shown diminished but persistent bisynchronous epileptiform discharges after corpus callosotomy in patients with seizure disorders, suggesting that both mechanisms may be important.

It should be noted that bilaterally synchronous spike-wave activity may also be seen in rare instances in patients with structural subtentorial or midline lesions, as well as in unselected nonepileptic patients and in the clinically unaffected siblings of patients with primary generalized epilepsy.

Generalized paroxysmal EEG disturbances, consisting of either slow activity, spike-wave activity, or sharp transients, occur in patients with a diffuse encephalopathic process involving predominantly the cortical and subcortical gray matter, but not when the white matter alone is involved. If both gray and white matter are affected, generalized paroxysmal activity occurs on a background of continuous polymorphic slow activity. Bilaterally synchronous spike-wave activity is seen in diffuse gray matter encephalopathies and is usually more slow and irregular than that in patients with primary epilepsy.

Intermittent Rhythmic Delta Activity

Intermittent rhythmic delta activity (see Fig. 3-10 ) with a frontal predominance (often designated FIRDA) in adults and an occipital emphasis in children was referred to on page 48 . It may result from a destructive lesion or from pressure and concomitant distortion affecting midline subcortical structures, in particular the diencephalon and rostral midbrain; it also occurs with deep frontal lesions. However, such activity is nonspecific and of no particular diagnostic significance. There is no means of clearly distinguishing the EEG pattern in deep midline lesions from that in diffuse cortical or subcortical encephalopathies or in metabolic encephalopathies. In most patients with FIRDA a diffuse encephalopathic process is present rather than a lesion limited to deep midline structures. FIRDA is occasionally present in otherwise healthy subjects during hyperventilation.

Burst-Suppression Pattern

The so-called burst-suppression pattern is characterized by bursts of high-voltage, mixed-frequency activity separated by intervals of marked quiescence or apparent inactivity that may last for no more than a few seconds or as long as several minutes. It occurs with a generalized distribution during the deeper stages of anesthesia; in patients who are comatose following overdosage with central nervous system (CNS) depressant drugs; and in any severe diffuse encephalopathy, such as that following anoxia ( Fig. 3-12 ). The bursts may be asymmetric or bisynchronous. The prognostic significance of a burst-suppression pattern depends on the circumstances in which it is found. When it follows cerebral anoxia, it is associated with a poor outcome. Spontaneous eye-opening, nystagmoid movements, pupillary changes, facial movements, myoclonus, and limb movements have occasionally been associated with the EEG bursts, and these sometimes mimic volitional activity. In other instances, movements occur exclusively between EEG bursts. Experimental studies in animals indicate that approximately 95 percent of cortical neurons become hyperpolarized and then electrically silent during periods of EEG suppression; this results from increased inhibition at cortical synapses, which also leads to functional disconnection of the cortex from its thalamic input.

Burst-suppression pattern recorded in the electroencephalogram of a 70-year-old man after a cardiac arrest from which he was resuscitated.

Periodic Complexes

Repetitive paroxysmal slow- or sharp-wave discharges, or both, may occur with a regular periodicity in a number of conditions. Such periodic complexes are seen most conspicuously and with a generalized distribution in subacute sclerosing panencephalitis and Creutzfeldt–Jakob disease, and are sometimes found in patients with liver failure. Periodic complexes that exhibit, to a greater or lesser extent, a regular rhythmicity in their occurrence may also be found in patients with certain lipidoses, progressive myoclonus epilepsy, drug toxicity, anoxic encephalopathy, head injury, subdural hematoma, occasionally after tonic-clonic seizures, and in rare instances in other circumstances. Their diagnostic value therefore depends on the clinical circumstances in which they are found.

Periodic Lateralized Epileptiform Discharges

Repetitive epileptiform discharges sometimes occur periodically as a lateralized phenomenon (designated periodic lateralized epileptiform discharges , or PLEDs), although they are often reflected to some extent over the homologous region of the opposite hemisphere as well. Their amplitude has ranged between 50 and 300 μV, and their periodicity between 0.3 and 4 seconds in different series. Structural cortical or subcortical lesions often—but not always—underlie the occurrence of these discharges. They typically are seen in patients with hemispheric lesions caused, most commonly, by cerebral infarction ( Fig. 3-13 ), hemorrhage, or tumors. In patients with acute hemispheric stroke, PLEDs are more likely when there are associated metabolic derangements, especially hyperglycemia and fever. Patients with herpes simplex encephalitis may have PLEDs, especially in the first 2 weeks of the illness, but their absence in no way excludes the diagnosis. Other infections occasionally associated with PLEDs include neurosyphilis, cysticercosis, bacterial meningitis, mononucleosis encephalitis, and early Creutzfeldt–Jakob disease. PLEDs may also be found in patients with chronic seizure disorders or long-standing static lesions (e.g., old infarcts), sometimes as a persistent phenomenon but more often for a brief period, especially when seizures or toxic metabolic disturbances have occurred recently. They or more generalized periodic epileptiform discharges are found occasionally with metabolic disorders that more typically produce diffuse EEG disturbances (e.g., anoxia, hepatic encephalopathy, and abnormal blood levels of glucose or calcium), and PLEDs also have been reported with head injury, lupus cerebritis, subdural hematoma, cerebral abscess or other cystic lesions, and sickle cell disease. In many cases, no specific cause can be found.

Periodic lateralized epileptiform discharges over the left hemisphere in the electroencephalogram of a 78-year-old woman with a recent stroke.

In one series, acute stroke, tumor, and CNS infection were the most common causes of PLEDs, accounting for 26, 12, and 12 percent of cases, respectively. Acute hemorrhage and traumatic brain injury combined were responsible for another 12 percent. Other, previously unreported, causes included posterior reversible encephalopathy syndrome, familial hemiplegic migraine, and cerebral amyloidosis. In 9 cases, chronic PLEDs were related to underlying cortical dysplasia or severe remote cerebral injury, all with an accompanying partial seizure disorder. Alcohol withdrawal was sometimes a precipitant, and in a few cases was seemingly the sole cause. Seizure activity occurred in 85 percent of patients. The overall mortality rate was 27 percent.

During the acute stage of illness, patients with PLEDs are usually obtunded and commonly have seizures (especially focal seizures) and a focal neurologic deficit. The PLEDs themselves are usually an interictal pattern, being replaced or obscured by other activity as a seizure develops. They may also occur ictally, however, particularly in patients with partial seizures, status epilepticus, or epilepsia partialis continua. The intense hypermetabolism and increased blood flow revealed by positron emission tomography (PET) and single-photon emission computed tomography (SPECT) scans provide some support for the belief that this EEG pattern is sometimes ictal in nature. Moreover, patients have been described with recurrent or prolonged confusional episodes during which PLEDs were present in the EEG; with clinical improvement, the EEG normalized.

PLEDs typically occur every 1 to 2 seconds; vary in morphology in different patients; and usually (but not always) disappear over the course of a few days or weeks, to be replaced by a focal or lateralized polymorphic slow-wave disturbance or by isolated spike discharges. The underlying disease determines the prognosis of patients with PLEDs. The absence of clinical seizures when PLEDs are detected is also associated with a poor prognosis for survival.

The pathophysiologic basis of PLEDs is not understood. Some have considered PLEDs to be equivalent to the terminal phase of status epilepticus; others have reported their association with rhythmic discharges that have a stereotyped distribution, frequency, configuration, and amplitude for individual patients, and that may be obscured by the development of frank electrographic seizure discharges.

PLEDs may occur independently over both hemispheres; they are then designated BiPLEDs. The complexes over the two hemispheres differ in their morphology and repetition rate. BiPLEDs are caused most commonly by anoxic encephalopathy, multiple vascular lesions, and CNS infection with either herpes simplex or other agents, but they may also be found in patients with chronic seizure disorders or with recent onset of seizures. BiPLEDs are usually found in comatose patients and are associated with a much higher mortality than are PLEDs.

14- and 6-Hz Positive Spikes

During drowsiness and light sleep, especially in adolescents, runs of either 14- or 6-Hz positive spikes, or both, may occur, superimposed on slower waves; generally they last for less than about 1 second. They are found especially in the posterior temporal or parietal regions on one or both sides and are best seen as surface-positive waveforms on referential recordings. They are of no pathologic relevance, although bursts of such activity have been described in comatose patients with Reye syndrome and in adults with hepatic or renal disease.

Small Sharp Spikes or Benign Epileptiform Transients of Sleep

Small sharp spikes or benign epileptiform transients of sleep are found during drowsiness or light sleep in as many as one-quarter of normal adults. Generally, they consist of monophasic or biphasic spikes; they are sometimes followed by a slow wave but are unaccompanied by sharp waves or rhythmic focal slowing of the background. They usually occur independently over the two hemispheres with sporadic shifting localization, but are best seen in the anteromesial temporal regions. Their appearance varies in different patients. They are distinguished from transients of pathologic significance by their bilateral occurrence, failure to occur in trains, and disappearance as the depth of sleep increases, and by the absence of abnormal background activity. Although commonly less than 50 μV, they are sometimes larger, so that size is not a reliable distinguishing feature. Such discharges are best regarded as normal and are of no diagnostic help in the evaluation of patients with suspected epilepsy.

6-Hz Spike-Wave Activity

Brief bursts of 6-Hz spike-wave activity, usually lasting for less than 1 second, may occasionally be seen in normal adolescents or young adults, especially during drowsiness, and are sometimes referred to as phantom spike-waves. They disappear during deeper levels of sleep, unlike pathologically significant spike-wave discharges. In some instances, the discharges are bilaterally symmetric and synchronous, but in others they are asymmetric. The spike is usually small compared with the slow wave and may be hard to recognize; when the spike is large, the discharges are more likely to be of pathologic significance. Discharges that are frontally predominant are also more likely to be associated with epilepsy than are discharges that are accentuated occipitally.

Wicket Spikes

A wicket spike pattern usually is found in adults, most commonly in drowsiness or light sleep but also during wakefulness. It may consist of intermittent trains of sharp activity resembling a mu rhythm, or of sporadic single spikes that are surface-negative and essentially monophasic. Its frequency is usually between 6 and 12 Hz. Wicket spikes are generally best seen over the temporal regions, either bilaterally or independently over the two sides, and sometimes have a shifting lateralized emphasis. The spikes are not associated with a subsequent slow wave or with any background abnormality. Wicket spikes have no diagnostic significance and, in particular, do not correlate with any particular symptom complex, including epilepsy. When these spikes occur singly, however, they may be mistaken for interictal temporal spike discharges.

Rhythmic Temporal Theta Bursts of Drowsiness (Psychomotor Variant)

During drowsiness or light sleep, especially in young adults, bursts of rhythmic sharpened theta waves with a notched appearance sometimes occur, predominantly in the midtemporal regions either unilaterally or bilaterally ( Fig. 3-14 ). If bilateral, they may occur synchronously or independently, with a shifting emphasis from one side to the other. Individual bursts commonly last for at least 10 seconds. Unlike electrographic seizure discharges, the bursts of activity do not show an evolution in frequency, amplitude, or configuration. They are of no pathologic significance.

Rhythmic sharpened theta activity seen bilaterally during drowsiness in the electroencephalogram of a 16-year-old boy. Bursts of such activity are a normal variant (sometimes called psychomotor variant) without pathologic significance.

Rhythmic Theta Discharges

In patients older than about 40 years, bursts of rhythmic sharpened theta activity at about 5 to 7 Hz may occur, often with an abrupt onset and termination. In contrast to seizures, they typically show no evolution of their frequency, distribution, or configuration, and they are not followed by focal or diffuse slow activity. These subclinical rhythmic electrographic discharges in adults (known by the acronym SREDA) usually are distributed bilaterally and diffusely, but occasionally are focal or lateralized. When diffuse, the discharges are often most conspicuous over the parietal and posterior temporal regions. They can occur at rest, during hyperventilation, or with drowsiness. The bursts may last up to 1 or 2 minutes, or even longer, and may be mistaken for a subclinical seizure. Digital analysis has revealed that the bursts are maximal in the parietal or parietocentrotemporal region and that they consist of a complex mixture of rapidly shifting frequencies that show little spatial or temporal correlation. Such discharges are probably of no diagnostic relevance and do not correlate with epilepsy or any specific clinical complaints.

Unusual variants of SREDA include predominantly delta frequencies, notched waveforms, or discharges having a frontal or more focal distribution; bursts that are more prolonged in duration; and discharges that occur during sleep.