Title | Ocular Motor Manifestations of Multiple Sclerosis |
Creator | Elodie Nerrant, MD; Caroline Tilikete, MD, PhD |
Affiliation | Hospices Civils de Lyon (EN, CT), Neuro-Ophthalmology and Neurology D, Hôpital Neurologique Pierre Wertheimer, Bron, France; Lyon I University (EN, CT), Lyon Est Medical School, Lyon, France; and CRNL (CT), INSERM U1028, CNRS UMR5292, ImpAct Team, Bron, France |
Abstract | Multiple sclerosis (MS) is a demyelinating disease of the central nervous system leading to disability, especially in young patients. Acute or chronic lesions of MS within the brainstem and the cerebellum frequently result in ocular motor disorders. This review encompasses the spectrum of ocular motor disorders in patients with MS emphasizing prevalence, examination findings, diagnostic features, functional consequences, classification of MS course, and management of these disturbances of ocular motility. Ocular motor manifestations of MS can occur acutely in relapse or chronically, the latter as a consequence of previous relapses or as a chronic course of the disease. The most frequent and specific acute ocular motor manifestation is uni- or bilateral internuclear ophthalmoplegia (INO). The most frequent chronic manifestations include INO and cerebellar ocular motor disorders such as gaze-evoked nystagmus, saccadic hypermetria, and lack of vestibulo-ocular reflex inhibition. The most disabling syndrome is pendular nystagmus. The high prevalence of ocular motor manifestations emphasizes the importance of neuro-ophthalmological examination among patients with MS. Because chronic manifestations may cause minimal or no symptoms, a systematic investigation of the most common manifestations should be performed in daily practice. Appropriate treatment may improve visual outcome in some of these ocular motor disorders. |
Subject | Eye Movements; Humans; Multiple Sclerosis; Ocular Motility Disorders; Visual Acuity |
OCR Text | Show State-of-the-Art Review Section Editors: Valerie Biousse, MD Steven Galetta, MD Ocular Motor Manifestations of Multiple Sclerosis Elodie Nerrant, MD, Caroline Tilikete, MD, PhD Background: Multiple sclerosis (MS) is a demyelinating disease of the central nervous system leading to disability, especially in young patients. Acute or chronic lesions of MS within the brainstem and the cerebellum frequently result in ocular motor disorders. Evidence Acquisition: This review encompasses the spectrum of ocular motor disorders in patients with MS emphasizing prevalence, examination findings, diagnostic features, functional consequences, classification of MS course, and management of these disturbances of ocular motility. Results: Ocular motor manifestations of MS can occur acutely in relapse or chronically, the latter as a consequence of previous relapses or as a chronic course of the disease. The most frequent and specific acute ocular motor manifestation is uni- or bilateral internuclear ophthalmoplegia (INO). The most frequent chronic manifestations include INO and cerebellar ocular motor disorders such as gazeevoked nystagmus, saccadic hypermetria, and lack of vestibulo-ocular reflex inhibition. The most disabling syndrome is pendular nystagmus. Conclusions: The high prevalence of ocular motor manifestations emphasizes the importance of neuro-ophthalmological examination among patients with MS. Because chronic manifestations may cause minimal or no symptoms, a systematic investigation of the most common manifestations should be performed in daily practice. Appropriate treatment may improve visual outcome in some of these ocular motor disorders. Journal of Neuro-Ophthalmology 2017;37:332-340 doi: 10.1097/WNO.0000000000000507 © 2017 by North American Neuro-Ophthalmology Society Hospices Civils de Lyon (EN, CT), Neuro-Ophthalmology and Neurology D, Hôpital Neurologique Pierre Wertheimer, Bron, France; Lyon I University (EN, CT), Lyon Est Medical School, Lyon, France; and CRNL (CT), INSERM U1028, CNRS UMR5292, ImpAct Team, Bron, France. The authors report no conflicts of interest. Supplemental digital content is available for this article. Direct URL citations appear in the printed text and are provided in the full text and PDF versions of this article on the journal's Web site (www. jneuro-ophthalmology.com). Address correspondence to Caroline Tilikete, MD, INSERM U1028, CNRS UMR5292, ImpAct Team, 16, Avenue Doyen Lépine, 69676 Bron Cedex, France; E-mail: caroline.tilikete@inserm.fr 332 M ultiple sclerosis (MS) is an immune-mediated disease of the central nervous system, characterized by inflammatory attacks against myelin (relapses) and by progressive axonal degeneration. Many neuroophthalmological manifestations are the consequence of relapses and/or the chronic disease phase of MS (1,2). Optic neuritis, as a classic example of afferent visual system involvement, is the most frequent relapse manifestation, and the most studied in the literature. Patients with MS also develop ocular motor disorders leading to diplopia or oscillopsia. The most common ocular motor abnormalities in patients with MS are internuclear ophthalmoplegia (INO), saccadic hypermetria, gaze-evoked nystagmus (GEN), and impaired vestibulo-ocular reflex (VOR) suppression (3,4). Although some disorders may be manifestations of acute MS relapses, they more frequently occur in the chronic disease phase, in which they persist over time (3,5,6). Although it may be asymptomatic, chronic ocular motor dysfunction can impair visual function and lead to poor visual outcome and reduced quality of life (3). Our objective is not to provide an exhaustive list of ocular motor manifestations of MS, but rather to provide a systematic clinical approach with emphasis on the following questions. What are the techniques to properly examine eye movements in patients with MS? Which ocular motor manifestations suggest an initial demyelinating event in the absence of an existing MS diagnosis? How frequent are ocular motor manifestations in MS? Does the identified ocular motor abnormality result from a relapse or a chronic phase in a patient with previous diagnosis of MS? What should be the therapeutic approach? The contents of this review will be presented as follows: 1) disorders of ocular alignment and diplopia, 2) ocular instability and oscillopsia, and 3) asymptomatic ocular motor disorders. The main ocular motor disorders described are summarized in Table 1. Practical tips on appropriate bedside examination also will be described. Nerrant and Tilikete: J Neuro-Ophthalmol 2017; 37: 332-340 Copyright © North American Neuro-Ophthalmology Society. Unauthorized reproduction of this article is prohibited. Nerrant and Tilikete: J Neuro-Ophthalmol 2017; 37: 332-340 Occurrence and Relative Frequency Treatment (Other Than Steroids for Acute Relapses) Clinical Characteristics Relapse Chronic Disabling Syndrome Limited or slow ipsilateral adduction Abduction nystagmus Bilateral INO + exotropia Loss of convergence Horizontal gaze palsy (nuclear, supranuclear) + INO (one-and-a-half) Abduction palsy or paresis +++ +++ ++ Ipsilateral MLF at pontine or midbrain level + ++ + Midbrain or pons + ? +++ + + ++ Skew deviation Nonparalytic vertical ocular misalignment ++ + ++ Gaze-evoked nystagmus Horizontal nystagmus beating in the direction of eccentric gaze 2 (Not isolated) +++ 2 Upbeat nystagmus Primary position upbeat nystagmus + +/2 +++ Gaze-evoked upbeat nystagmus in upgaze + ++ 2 Bilateral MLF (vertical gazeholding) None Pendular nystagmus Back and forth slow-phase oscillations of eyes, without resetting quick phases 2 ++ +++ Gabapentin; Memantine Saccadic intrusions Square-wave jerks Square-wave pulses Ocular flutter + ++ + to +++ Impairment in the feedback pathways connecting brainstem neural integrators and/or visual afferences Pause neurons in brainstem; cerebellar dysfunction Saccadic hypermetria Overshoots of saccades 2 +++ +/2 None Lack of VOR inhibition Inability to suppress the VOR: catch-up saccades + ++ + Cerebellar oculomotor vermis Vestibulo-cerebellum Clinical Syndromes INO WEBINO One-and-a-half syndrome and nuclear or supranuclear gaze palsy Abducens nerve palsy Localization Ipsilateral MLF + PPRF and/ or VI nucleus at pontine level Fascicular VI nerve at pontine level MLF lesion (+INO) Cerebellar (chronic, alternating) Gaze-holding neuralintegrator dysfunction Cerebellar or brainstem lesions Caudal medulla or midpons Suppress diplopia if necessary, Dalfampridine (?) Suppress diplopia Suppress diplopia if necessary Suppress diplopia if necessary None None Clonazepam; baclofen; 4-aminopyridine Baclofen anticonvulsants None INO, internuclear ophthalmoplegia; MLF, medial longitudinal fasciculus; PPRF, paramedian pontine reticular formation; VOR, vestibulo-ocular reflex; WEBINO, wall-eyed bilateral INO. 2, absent; +/2 exceptional +, infrequent; ++, frequent; +++, highly frequent. State-of-the-Art Review 333 Copyright © North American Neuro-Ophthalmology Society. Unauthorized reproduction of this article is prohibited. TABLE 1. Ocular motor disorders in Multiple Sclerosis State-of-the-Art Review DISORDERS OF OCULAR ALIGNMENT AND DIPLOPIA Paralytic Internuclear Ophthalmoplegia INO is one of the most frequent ocular motor disturbances in patients with MS (7). INO is characterized by ipsilateral adduction palsy and horizontal jerk nystagmus of the contralateral eye during abduction. Ipsilateral adduction should be preserved during convergence, but this dissociation may be lacking. INO is due to a lesion within the medial longitudinal fasciculus (MLF) (8), carrying adduction signal during horizontal versions from the contralateral abducens nucleus to the ipsilateral oculomotor nucleus (Fig. 1). In patients with MS, INO is frequently bilateral (9). Slowing of adducting saccades may, at times, be the only manifestation of INO. In this setting, adduction range may appear full and abducting nystagmus may be absent (10) (Practical tip E1). Recording of eye movements will increase detection of slowed adduction in INO (11). The MLF also carries vertical, torsional, and velocity eye movement information. Thus, unilateral INO can be associated with skew deviation (with the eye contralateral to the MLF lesion being lower), whereas bilateral INO is associated with gaze-evoked upbeat nystagmus in upgaze (1,11). INO in MS can occur either as an acute symptom of an MS attack, or as a chronic condition (Table 1). In the latter case, this results from either incomplete recovery of previous attack or from the chronic phase of the disease. Typically, patients with chronic INO are asymptomatic or have nonspecific visual complaints. In MS, unilateral INO is observed in 30% of patients, and bilateral INO in 12% (12,13), rising to 56% (31% if bilateral) in patients with persistent visual complaints (3). Although there are no data regarding the frequency of acute INO in patients with MS, MS is the cause in 32%-34% of cases of INO, 27%-28% if unilateral, and 17%-41% if bilateral (9,14). After at least 9 months, up to 60% of INO cases in patients with MS may recover (9). MLF lesions generally are very small and may, or may not, be seen on MRI. T2 sequences are best to detect MLF involvement and are superior to fluidattenuated inversion recovery images (8). WEBINO, the acronym for wall-eyed bilateral INO, encompasses bilateral adduction deficits and bilateral abduction nystagmus (Fig. 2). The basis for exotropia, the cardinal sign of WEBINO syndrome is unknown, as it appears not be caused by loss of vergence or involvement of the medial rectus subnuclei of the third nerve nuclear complex (15,16). WEBINO may occur as a relapse or in the chronic phase of MS. Other Brainstem Disorders The one-and-a-half syndrome consists of an INO and an ipsilateral horizontal gaze palsy. The only remaining horizontal eye movement is abduction contralateral to the lesion. Adduction with convergence is preserved. The oneand-a-half syndrome is secondary to a lesion of the MLF and either the ipsilateral abducens nucleus (nuclear oneand-a-half) or the paramedian pontine reticular formation (PPRF) (supranuclear one-and-a-half syndrome). In nuclear syndrome, all eye movements are impaired; whereas in supranuclear dysfunction, limited voluntary rapid eye movements (saccades) can be overcome by oculocephalic stimulations (Practical tip E2). If there is ipsilateral peripheral facial nerve involvement, the clinical presentation is designated as the eight-and-a-half syndrome. Approximately 30% of cases of one-and-a-half syndrome are due to MS, mainly from acute relapses (17,18) (Table 1). In many cases, patients partially recover from a one-and-a-half syndrome, and are left with a residual INO. Uni- or bilateral horizontal nuclear or supranuclear gaze palsies (without INO) have been reported in patients with MS (19,20). Rarely, dorsal midbrain syndrome has also been documented (21). Ocular Motor Cranial Nerve Palsy Ocular motor cranial nerve palsies in patients with MS are due to demyelination of the fascicular portion of the cranial nerves within the brainstem. Typically, these result from clinical relapses. Most often the sixth nerve is involved, but occurs during a relapse in only 0.4%-1% FIG. 1. Right internuclear ophthalmoplegia. Right gaze (A) is intact, whereas exotropia in left gaze (B) is due to adduction weakness of the right eye. The horizontal lines denote that the left eye is lower than the right, consistent with a skew deviation. C. Axial FLAIR image on MRI reveals a lesion (arrow) of the right medial longitudinal fasciculus. FLAIR, fluidattenuated inversion recovery. 334 Nerrant and Tilikete: J Neuro-Ophthalmol 2017; 37: 332-340 Copyright © North American Neuro-Ophthalmology Society. Unauthorized reproduction of this article is prohibited. State-of-the-Art Review FIG. 2. Wall-eyed bilateral internuclear ophthalmolplegia (WEBINO). In primary gaze, the patient is exotropic, with bilateral adduction weakness in both directions of horizontal gaze. of patients with MS (Table 1) (Fig. 3) (22-24). Whether MS represents a frequent etiology of sixth nerve palsy is controversial; it is reported to range from 1% (24) to 12% (25,26) of causes of the sixth nerve palsy. Third nerve palsy as the presenting sign of MS occurs in 2.8% of cases (27). Partial involvement is typical with or without pupil involvement (17,28). The fourth nerve is rarely affected in MS (29). Nonparalytic In cases of nonparalytic strabismus, range of eye movements appears full. Demonstration of small amounts of ocular misalignment requires careful assessment of eye position using the cover-uncover and alternate cover tests (Practical tip E3). Skew deviation is a nonparalytic vertical ocular misalignment observed in all directions of gaze (30). It is typically caused by lesions of central graviceptive vestibular pathways, including the cerebellum. Description of skew deviation is conventionally given by the side of the lower eye. With a lesion below the decussation of the vestibular pathways at the pontine level, the lower eye is on the opposite side of the lesion. In MS, acute skew deviation is frequently observed in association with contralateral INO (Table 1) (31). In the chronic phase, skew deviation reflects cerebellar involvement and may be seen as an alternating skew deviation (32). The cerebellum also has a role in the control of the alignment of the eyes, and esophoria or esotropia (nonparalytic strabismus) occurs in chronic cerebellar disorders (33). These chronic cerebellar ocular misalignments are not specific for MS, but may suggest a chronic disease phase in patients with known MS. Therapeutic Management of Ocular Motor Palsies or Misalignments During attacks, corticosteroids remain essential to improve clinical outcomes, although patients may need to temporarily use ocular occlusion. Of interest, dalfampridine, a potassium channel blocker prescribed for gait impairment in MS, has led to improved adduction in INO in patients with MS (34). In some very rare cases, prism glasses, botulinum toxin, or eye muscle surgery may be warranted (9,35-37). OCULAR INSTABILITY AND OSCILLOPSIA Ocular instability in MS may be due to nystagmus, saccadic intrusions, or saccadic hypermetria (Practical tip E4). Those occurring most frequently in MS are GEN and saccadic hypermetria, but the most disabling disorder is pendular nystagmus (3,39). With the exception of upbeat nystagmus, which occurs in acute attacks, the other types of ocular instability reflect a chronic disease phase. Nystagmus Jerk Nystagmus Different forms of jerk nystagmus have been reported in patients with MS; by far the most frequent being GEN, followed by primary position upbeat nystagmus. GEN has been described in 16% of patients with MS (12) and up to 44% of patients with MS complaining of visual dysfunction (3). With GEN, the fast phase is in the direction of eccentric gaze, horizontal in lateral gaze, and/or vertical in upgaze. GEN is the result of a gaze-holding neural integrator dysfunction (velocityto-position integrator). In horizontal gaze, this neural FIG. 3. Right sixth nerve paresis. There is mild limitation of abduction of the right eye (A) compared with the left (B). C. Axial T2 MRI shows a lesion involving the fascicular portion of the right sixth nerve (arrow). Nerrant and Tilikete: J Neuro-Ophthalmol 2017; 37: 332-340 335 Copyright © North American Neuro-Ophthalmology Society. Unauthorized reproduction of this article is prohibited. State-of-the-Art Review network involves the prepositus hypoglossi and the medial vestibular nuclei. Superior vestibular nuclei/ MLF/midbrain interstitial nucleus of Cajal integrate ocular motor parameters in vertical gaze (16). Cerebellar flocculus and paraflocculus are connected to the brainstem network, and a feedback mechanism controls their function. Therefore, GEN may be caused by brainstem and/or cerebellar lesions. Patients with GEN are rarely symptomatic from this eye movement disorder, and it usually represents chronic disease (Table 1). Gaze-evoked upbeat nystagmus in upgaze in patients with MS may occur in association with bilateral INO, either as a result of acute relapse or as a chronic manifestation. Primary position upbeat nystagmus is the result of a discrete lesion located in caudal medullary or pontine tegmentum level (30-43). This nystagmus can change with head position, that is, dampen or reverse in the prone or supine position. Downbeat nystagmus (DBN) rarely has been reported in MS (44,45). It is due to bilateral flocculus impairment resulting in vestibular nuclei disinhibition (40). In MS, DBN reflects a chronic disease phase. Other kinds of jerk nystagmus have been described in MS, including periodic alternating nystagmus (46) and nystagmus associated to central vestibular disorders (47). Pendular Nystagmus Acquired pendular nystagmus (APN) is rare and defined by a regular back and forth slow-phase oscillation of the eyes. APN in patients with MS is characterized by small amplitude, high frequency, and great regularity (38). APN may be horizontal, vertical, or torsional, most often bilateral, and can be conjugate or dysconjugate. The persistence of APN in primary gaze results in disabling oscillopsia. At times, it is only triggered by convergence (48). It has always been described as permanent, mainly in chronic disease phase (Table 1). Mechanisms postulated for causing pendular nystagmus in MS include abnormal delays in the ocular motor feedback loops due to demyelination. This abnormal feedback loop could involve the velocity-to-position neural integrators, which normally stabilize gaze (49) and/or an abnormal visual feedback due to optic nerve pathology (50,51). Indeed, this nystagmus often is associated with chronic optic neuropathy and/or to diffuse pontine tegmental lesions. APN has been described in 11% of 284 patients with MS referred to an ophthalmologic department (52) and up to 20% in a cohort of 73 patients with MS complaining of persistent visual impairment (3). One publication has reported dampening of APN in a patient with MS with vibration of the skull using a hand held muscle massager (53). See-saw nystagmus is characterized by supraduction and incyclotorsion of one eye, and infraduction and 336 excycolotorsion of the other eye. A parasellar, chiasmal, or midbrain lesion often is identified, but occasionally see-saw nystagmus has been reported in patients with MS (54,55). Saccadic Intrusions and Hypermetria Saccadic Intrusions The most common saccadic intrusions in MS are squarewave jerks and macrosaccadic square-wave jerks, both occurring in association with cerebellar syndrome (56) (Fig. 4). Ocular flutter (horizontal) and opsoclonus (multidirectional) are commonly part of a paraneoplastic syndrome or following viral infections, but occasionally are caused by MS (44). These saccadic oscillations can occur either in relapse (17,57,58) or in chronic forms for ocular flutter. FIG. 4. Saccadic intrusions. Two main types of saccadic intrusions can be distinguished by the presence or absence of an intersaccadic interval defined by a latent period that usually lasts 180-200 milliseconds between sequential saccades. Saccadic intrusions with a normal intersaccadic interval include square wave jerks (A), square wave pulses (or macrosaccadic square wave jerks) (B), macrosaccadic oscillations (C), and saccadic pulses (D). The latency and amplitude of to-and-fro saccades can differentiate square waves (200 ms, ,4°) from square wave pulses (80 ms, .5°). Macrosaccadic oscillation is composed of a run of saccades following change of fixation in a crescendodecrescendo pattern, with a 200-millisecond interval. Saccadic pulses are brief saccadic intrusions that take the eye away from the fixation point, and are immediately followed by a slow drift to the previous position. Saccadic intrusions without intersaccadic interval correspond to ocular flutter and opsoclonus (E). Ocular flutter consists of back-to-back horizontal saccades, whereas opsoclonus (or saccadomania) is composed of multidirectional saccades of varying amplitudes. Adapted with permission from (56). Nerrant and Tilikete: J Neuro-Ophthalmol 2017; 37: 332-340 Copyright © North American Neuro-Ophthalmology Society. Unauthorized reproduction of this article is prohibited. State-of-the-Art Review Saccadic Dysmetria Saccadic dysmetria is one of the most common chronic ocular movement abnormalities in MS, primarily as saccadic hypermetria and directional dysmetria (Practical tip E5) (7). Lesions of the dorsal oculomotor vermis and the fastigial oculomotor region are responsible for abnormal accuracy and trajectory of saccades (60,61), and observed only in chronic cerebellar syndrome (Table 1). Saccadic dysmetria is present in approximately 30%-40% of patients with MS (3,12). Therapeutic Management of Nystagmus and Other Ocular Instability Because nystagmus and other disorders of ocular stability are very disabling in patients with MS, a variety of treatments have been used (Table 1). Gabapentin (1,200- 2,400 mg/d) and memantine (20-40 mg/d) are effective in the treatment of APN leading to an improved visual outcome (59-61). However, memantine should be used cautiously as it has been associated with a risk of worsening MS (62). Clonazepam (1.5-3.0 mg/d) and the potassium channel antagonists 3,4-diaminopyridine (40-60 mg/d) and 4-aminopyridine (10-15 mg/d) have demonstrated significant improvement of DBN (63-65). Periodic alternating nystagmus may be treated with baclofen (15-30 mg/d) (66). Saccadic intrusions may improve with baclofen or anticonvulsants (67). ASYMPTOMATIC OCULAR MOTOR DISORDERS Examination of eye movements, with attention to dynamic properties of saccades, smooth pursuit, and visual inhibition of VOR, may provide valuable information in detecting chronic brainstem and cerebellar disorders. Important examples include adduction saccade slowing in INO and saccadic hypermetria. An examination of patients with MS should include evaluation of smooth pursuit (See Supplemental Digital Content, Video 1, http://links.lww.com/ WNO/A221). Jerk or saccadic pursuit in a nonspecific finding as it may be found in any individual who is tired, visually handicapped, or uncooperative and in patients taking sedative drugs (44). The smooth pursuit network is large and its impairment is not topographically specific, limiting the usefulness of its testing. Examination of VOR inhibition by fixation can be more valuable to detect dysfunction of the smooth pursuit/fixation system (See Supplemental Digital Content, Video 2, http://links. lww.com/WNO/A222). Smooth pursuit has been found to be chronically impaired in 30% of patients with MS (4), and lack of VOR inhibition is reported in 70%-75% of patients with MS (3,68). Although impaired smooth pursuit may be due to cerebellar, brainstem, and hemispheric lesions, lack of Nerrant and Tilikete: J Neuro-Ophthalmol 2017; 37: 332-340 VOR inhibition seems to be more specific of chronic cerebellar involvement, related to diffuse lesions of vestibulocerebellum (Table 1) (69). CONCLUSION Patients with MS may develop a broad range of efferent visual disorders due to brainstem and cerebellar dysfunction. Visual symptoms of efferent system disorders may occur at onset of disease, during relapse, or with the chronic course of MS. Moreover, patients may not notice any visual difficulty, or may report nonspecific visual complains and a systematic clinical examination is essential to recognize these ocular motor disorders. Improving ocular motor diagnosis ensures the best clinical evaluation of patients with MS to classify them, score the handicap, and propose effective treatments to limit visual disability. PRACTICAL TIPS Practical Tip E1: How to Examine for an Internuclear Ophthalmoplegia? INO in MS is more frequently characterized by slowing of the adducting eye rather than adduction palsy of the ipsilateral eye. Amplitude of adduction is then maintained during slow eye movements such as smooth pursuit. Therefore, saccades should be examined by asking the patient to fixate alternatively 2 peripheral targets: a slower adduction saccade relative to a normal abduction one is easy to identify. INO in MS can be chronic, asymptomatic, and resulting either from incomplete recovery of attack or as manifestation of chronic phase. A specific search for INO as described above should be part of systematic ocular motor examination in suspected or known patients with MS. Practical Tip E2: How to Differentiate Nuclear From Supranuclear Horizontal or Vertical Gaze Palsy? When a patient presents with a horizontal or vertical gaze palsy, the examiner must identify if the gaze palsy is due to nuclear or supranuclear (structures that trigger saccades) dysfunction. In horizontal gaze palsy, abducens nucleus syndrome should be distinguished from PPRF syndrome. In vertical gaze palsy, oculomotor nucleus syndrome should be distinguished from dorsal midbrain syndrome, which reflects the involvement of structures that trigger vertical saccades. The oculocephalic reflex plays a key role. To evaluate the oculocephalic response, the examiner has to swiftly rotate the patient's head horizontally then vertically while the patient is fixating a stationary target such as the examiner's nose. The input that triggers the stabilizing eye movements comes either from the VOR, the visual system, and/or the neck proprioceptive afferences. Limited voluntary rapid eye movements 337 Copyright © North American Neuro-Ophthalmology Society. Unauthorized reproduction of this article is prohibited. State-of-the-Art Review (saccades) can be overcome by oculocephalic stimulations, suggesting a supranuclear (or nonorganic) origin. Practical Tip E3: How to Diagnose an Ocular Misalignment? Cover tests are helpful to demonstrate a small ocular misalignment. These tests are based on the principle that if the visual axis is not aligned with the target, a rapid eye movement (saccade) will be performed to foveate the presented target. The detection and the amplitude of this corrective saccade indicate the misalignment of the visual axis to the clinician. The patient also can verbally describe the change in the position of the target, from one covering condition to the other. Using a translucent occluder may be useful for the examiner to observe the movement of the covered eye. The cover-uncover test reveals heterotropia or ocular deviation with binocular fixation. If the cover-uncover test does not demonstrate ocular misalignment (eyes are in orthotropic position), the examiner should proceed to the cross-cover test to demonstrate heterophoria. With both testing techniques, esotropia(phoria) is denoted by an outward movement, exotropia(phoria) by an inward movement, hypertropia(phoria) by a downward movement, and an hypotropia(phoria) by an upward movement of the ipsilateral eye. Practical Tip E4: How to Examine for Ocular Instability? The patient initially should be examined with eyes in the primary position of gaze, while looking at a small object located in front of him/her, with binocular then monocular viewing. Next, ocular stability have to be looked for when the patient fixates 20° to the right, to the left, up and down, and in convergence. Looking at the pupil helps to identify horizontal or vertical instability, and at conjunctival vessels for instability in the torsional plane. Focus on eyelids may detect small amplitude vertical ocular instability. To identify tiny ocular instability, optic disk stability should be checked through the ophthalmoscope or using magnification such as Frenzel goggles. Nystagmus present in primary position of gaze is always pathological. GEN is specifically triggered in eccentric gaze and consists of centrifugal slow phases followed by centripetal fast phases. GEN has to be differentiated from end-point nystagmus seen in extreme lateral gaze (30-40°) in normal individuals as a consequence of ocular fatigue with prolonged lateral gaze. Saccadic intrusions such as square wave jerks can be seen in normal individuals, particularly in the elderly. Practical Tip E5: How to Look for Saccadic Dysmetria? Saccades should be examined by asking the patient to fixate a central target (i.e., the examiner's nose) then a peripheral target (i.e., the examiner's finger or the tip 338 of a pen) and back again to the central target. Saccades in each direction should be checked. This bedside examination allows the analysis of velocity, initiation (latency), accuracy, and conjugacy of saccadic eye movements. Saccades can be inaccurate, either hypometric or hypermetric, leading to forward or backward correction, respectively. This corrective saccade is then detected clinically. A directional dysmetria may also be found, such as a vertical movement in horizontal saccade. Saccadic hypometria is a frequent observation in normal subjects. In MS, saccadic dysmetria can be either saccadic hypermetria or directional dysmetria. STATEMENT OF AUTHORSHIP Category 1: a. Conception and design: E. Nerrant and C. Tilikete; b. Acquisition of data: E. Nerrant and C. Tilikete; c. Analysis and interpretation of data: E. Nerrant and C. Tilikete. Category 2: a. Drafting the manuscript: E. Nerrant and C. Tilikete; b. Revising it for intellectual content: C. Tilikete. Category 3: a. Final approval of the completed manuscript: E. Nerrant and C. Tilikete. REFERENCES 1. Frohman EM, Frohman TC, Zee DS, McColl R, Galetta S. The neuro-ophthalmology of multiple sclerosis. Lancet Neurol. 2005;4:111-121. 2. 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Date | 2017-09 |
Language | eng |
Format | application/pdf |
Type | Text |
Publication Type | Journal Article |
Source | Journal of Neuro-Ophthalmology, September 2017, Volume 37, Issue 3 |
Collection | Neuro-Ophthalmology Virtual Education Library - Journal of Neuro-Ophthalmology Archives: https://novel.utah.edu/jno/ |
Publisher | Lippincott, Williams & Wilkins |
Holding Institution | Spencer S. Eccles Health Sciences Library, University of Utah, 10 N 1900 E SLC, UT 84112-5890 |
Rights Management | © North American Neuro-Ophthalmology Society |
ARK | ark:/87278/s65q949d |
Setname | ehsl_novel_jno |
ID | 1374459 |
Reference URL | https://collections.lib.utah.edu/ark:/87278/s65q949d |