Bilateral Sixth Nerve Palsy

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Identifier 944-5
Title Bilateral Sixth Nerve Palsy
Creator Shirley H. Wray, MD, PhD, FRCP
Contributors Ray Balhorn, Video Compressionist; Steve Smith, Videographer
Affiliation (SHW) Professor of Neurology, Harvard Medical School; Director, Unit for Neurovisual Disorders, Massachusetts General Hospital, Boston, Massachusetts
Subject Voluntary Ptosis; Bilateral Sixth Nerve Palsy; Esotropia; Paresis of Conjugate Upgaze; Acute Inflammatory Demyelinating Neuropathy; Guillian Barre Syndrome - Miller Fisher Syndrome
History The patient is a 22 year old man. Five days prior to admission (PTA) he developed a sore throat, non-productive cough and a temperature of 99.8 during the day and chills and diaphoresis at night. Four days PTA he had double vision in primary gaze, difficulty with his balance and gait, and a tingling sensation in the fingers bilaterally and to a less extent in the toes. Twelve days PTA he felt that he had a "flu-like" illness with mild headache, fever, and some blood-tinged diarrhea. He was seen at an outside hospital where blood, urine and stool cultures were done. The stool culture was positive for Campylobacter jejuni. (This result was not available until after his admission to the Massachusetts General Hospital (MGH)). Because his symptoms progressed he was unable to work and he came to the MGH ER and was admitted. Past History: Negative for any major illness Family History: Non-contributory On day 14 Neuro-ophthalmic Examination: Visual acuity 20/20 OU Pupils equal and briskly reacting to light and near Ocular Motility: Voluntary ptosis Bilateral esotropia in primary gaze Bilateral paresis of abduction left eye greater than right. Impaired vertical upgaze Full downgaze Normal convergence No nystagmus Neurological Examination: No facial weakness Motor strength 5/5 Deep tendon reflexes present, 2+ symmetric Plantar responses flexor Gait ataxia and inability to tandem walk No limb ataxia Sensory examination normal Investigations: The most important investigations in suspected cases of the Guillian Barré syndrome (GBS) or the variant, the Miller Fisher syndrome (MFS) are: 1. Electrodiagnostic studies and 2. Examination of the cerebrospinal fluid (CSF) The most frequent early electrodiagnostic findings in GBS and MFS are: 1. A reduction in the amplitude of muscle action potentials 2. Slow nerve conduction velocity 3. Conduction block in motor nerves singly or in combination 4. Prolonged distal latencies (reflecting distal conduction block) 5. Prolonged or absent F-responses (indicating involvement of proximal parts of nerves and roots) and reflecting focal demyelination. 6. Delayed or absent H-reflex (which really just confirms the loss of ankle jerks). A limited electrodiagnostic examination may be normal early in the illness as in this case. A more thorough study, which includes measurement of late responses, almost invariably shows disordered conduction in an affected limb within days of the first symptom. Electrodiagnostic studies: Limited to nerve conduction velocity normal in this patient. Lumbar Puncture on day 15. CSF protein normal 17 mg/dl Glucose 63 mg/dl. No white blood cells Usually, the CSF protein is normal in the first few days of the illness. Then the protein level begins to rise reaching a peak in 4 to 6 weeks and persisting elevated for several weeks. In Dr. Ropper's experience patients with MFS have a higher incidence of normal or only slightly elevated CSF protein during the course of their illness. Brain MRI with gadolinium: No abnormality Stool Culture (from outside hospital) Campylobacter jejuni Antibody studies: To check for Anti-GQ1b antibody, I sent the serum of this patient and the serum from a second case of MFS, a young man presenting with bilateral sixth nerve palsy, (ID944-5) to Professor Newsom-Davis in Oxford to study. Both these patients were found to have the Anti-GQ1b IgG antibody. Diagnosis: Miller Fisher Syndrome Serum protein electrophoresis revealed IgG kappa M components in the slow gamma region and there were oligoclonal bands present also. Treatment: On the 2nd hospital day, the patient was already beginning to improve. He received intravenous hydration and no other medication. He was discharged home the next day. He recovered fully over the following three weeks. (View ID925-2 and 944-1 alongside this case)
Pathology In 1993, Chiba et al reported the presence of serum IgG antibody against ganglioside GQ1b in patients in the acute phase of the Miller Fisher syndrome and pointed out that this immunologic feature was common to both MFS and GBS. To check for Anti-GQ1b antibody, I sent the serum of this patient and the serum from a second case of MFS, a young man presenting with bilateral sixth nerve palsy, (ID944-5) to Professor Newsom-Davis in Oxford to study. Both these patients were found to have the Anti-GQ1b IgG antibody. Both GBS and MFS are cell mediated immunological diseases directed at peripheral nerve resulting in acute inflammatory demyelinating neuropathy. Autoantibodies: A number of autoantibodies directed at components of nerve ganglioside are detected inconsistently in patients with GBS. Anti-GQ1b IgG is the most important and is the autoantibody found in almost all patients with ophthalmoplegia. Antibodies against the ganglioside GQ1b have also been detected in patients with Bickerstaff's brainstem encephalitis. Bickerstaff's encephalitis is characterized by ophthalmoplegia and ataxia but is also accompanied by pyramidal and sensory tract findings and cerebrospinal fluid pleocytosis. GM1 autoantibody may be found in approximately one-third of patients with GBS early in their course, corresponding in most instances to a predominantly motor presentation and to axonal damage. The highest titres of anti-GM1 antibody are usually associated with cases that follow Campylobacter infections. Autoantibodies directed against GD1a or GT1b have been associated in some cases with the pharyngeal-brachial-cervical variant. Pathology: Pathological studies in cases of GBS have failed to demonstrate any changes within the neuroaxis, and there is thus no morbid anatomic basis for attributing the clinical picture to a disturbance within the brainstem. Virtually all cases have shown perivascular (mainly perivenous) lymphocytic infiltrates scattered throughout the cranial nerves, ventral and dorsal nerve roots and dorsal root ganglia and along the entire length of the peripheral nerves. Swelling of nerve roots at the site of their dural exit has been emphasized by some authors and theorized to cause root damage. In patient's whose electrophysiologic tests display severe axonal damage early in the illness, the pathologic findings corroborate the predominately axonal nature of the disease with secondary myelin damage and little inflammatory response.
Disease/Diagnosis Miller Fisher Syndrome; Acute inflammatory demyelinating neuropathy
Clinical This young man with the Miller Fisher Variant of the GBS presented with bilateral 6th nerve paralysis. He had: Voluntary ptosis of the left eye to correct diplopia Bilateral esotropia in primary gaze Abduction weakness of the left eye Abduction weakness of the right eye Impaired vertical upgaze Downgaze normal Convergence normal No facial weakness In 1956 Miller Fisher published a paper in the New England Journal of Medicine describing an unusual acute idiopathic polyneuritis characterized by: 1. Total external ophthalmoplegia 2. Severe ataxia and 3. Loss of the deep tendon reflexes. The nature of the illness was not recognized until he saw the third case, when, in association with a mild peripheral neuropathy, the cerebrospinal fluid showed an albuminocytologic dissociation with a total protein of 348 mg/100 ml. and no cells. The syndrome Miller Fisher described proved to be a variant of the GBS acute idiopathic polyneuritis in which limb involvement was minimal or absent. In two of Miller Fisher's cases, (case 1 and 2) external ophthalmoplegia was complete and the eyes fixed in primary gaze. Case 3 had bilateral sixth nerve paralysis and slight rotary nystagmus on attempted lateral gaze. Bilateral ptosis was added to the picture two days later. GBS is now viewed as a group of distinct disorders which include the following variants, tabulated by Ropper and Brown (Table 46-3 (18)). Regional Fisher syndrome of ophthalmoplegia, ataxia and areflexia Cervico-brachial-pharyngeal, often with ptosis Oculopharyngeal weakness Predominant paraparesis Bilateral facial or abducens weakness with distal paresthesias Ophthalmoplegia with GQ1b autoantibodies Functional Generalized ataxia without dysarthria or nystagmus Pure sensory Pure motor Pandysautonomia Axonal The degree of ophthalmoparesis is variable but certain patterns suggest involvement of either the peripheral or central nervous system. The ophthalmoplegia may resemble: Horizontal or vertical gaze palsy Internuclear ophthalmoplegia, and Ptosis is often absent even in the presence of significant ophthalmoparesis. Bell's phenomenon is often preserved even when vertical eye movements are absent. Signs pointing to cerebellar dysfunction are: Rebound nystagmus Impairment of smooth pursuit Suppression of the vestibular ocular reflex Dr. Fisher was himself impressed by the presence of ataxia unaccompanied by sensory loss, and "reluctantly interpreted" the clinical signs as "manifestations of an unusual and unique disturbance of peripheral neurons".
Presenting Symptom Diplopia
Ocular Movements Voluntary Ptosis; Bilateral Sixth Nerve Palsy; Esotropia; Paresis of Conjugate Upgaze
Neuroimaging No imaging studies are available in this patient. The MRI findings in another patient with the MFS have been reported. The patient was a 25 year old woman with complete external ophthalmoplegia, ptosis, limb ataxia and areflexia. Brain MRI: T1-weighted images with Gd-DTPA on day 15 of her illness, demonstrated enhancement of the posterior nerve roots of the cauda equina. MRI on day 32 revealed swelling and enhancement bilaterally of cranial nerves 3, 6 and 6. The patient received high-dose intravenous immunoglobulin therapy and had marked improvement in her ophthalmoplegia. Repeat MRI with gadolinium, after recovery, showed no enhancement of the cauda equina nor of the cranial nerves. In this patient IgG anti-GQ1b and GD1b antibodies were detected.
Treatment Specific treatment of the presumed immune disorder that underlies GBS and the MFS include plasma exchange and intravenous immunoglobulin IVIG (0.4 g/kg per day for five consecutive days). IVIG stops Anti-GQ1b antibodies from binding to GQ1b ganglioside receptors and thereby prevents the electrophysiological effects. Approximately 3 to 5% of patients do not survive an attack of GBS.
Etiology Campylobacter jejuni may be the responsible trigger in GBS and MFS since Anti-GQ1b antibodies bind to surface epitopes on this organism, and its lipopolysaccharide fraction may molecularly mimic the ganglioside.
Supplementary Materials Miller Fisher Syndrome: https://collections.lib.utah.edu/details?id=2174209
Date 1993
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Language eng
Format video/mp4
Type Image/MovingImage
Source 3/4" Umatic master videotape
Relation is Part of 925-2, 944-1
Collection Neuro-Ophthalmology Virtual Education Library - Shirley H. Wray Neuro-Ophthalmology Collection: https://novel.utah.edu/Wray/
Publisher North American Neuro-Ophthalmology Society
Holding Institution Spencer S. Eccles Health Sciences Library, University of Utah
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ARK ark:/87278/s6z065qz
Setname ehsl_novel_shw
ID 188515
Reference URL https://collections.lib.utah.edu/ark:/87278/s6z065qz