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Review

Update on the evaluation of transient vision loss

John H Pula1 Department of Neurology, NorthShore University HealthSystem, Evanston IL, USACorrespondence[email protected]
,
Katherine Kwan2 Department of ophthalmology, NorthShore University HealthSystem, Evanston IL, USA
,
Carlen A Yuen3 University of Illinois College of Medicine at Peoria, Peoria, IL, USA
&
Jorge C Kattah4 Department of Neurology, University of Illinois College of Medicine at Peoria, Peoria, IL, USA
Pages 297-303 | Published online: 11 Feb 2016

Abstract

Transient vision loss may indicate underlying vascular disease, including carotid occlusion and thromboembolism, or it may have a more benign etiology, such as migraine or vasospasm. This review focuses on the differential diagnosis and workup of patients presenting with transient vision loss, focusing on several key areas: the relationship to thromboembolic vascular disease, hypercoagulable testing, retinal migraine, and bilateral vision loss. The objective is to provide the ophthalmologist with information on how to best manage these patients. Thromboembolic etiologies for transient vision loss are sometimes managed with medications, but when carotid surgery is indicated, earlier intervention may prevent future stroke. This need for early treatment places the ophthalmologist in the important role of expediting the management process. Hospital admission is recommended in patients presenting with transient symptoms within 72 hours who meet certain high-risk criteria. When the cause is giant cell arteritis, ocular ischemic syndrome, or a cardioembolic source, early management of the underlying condition is equally important. For nonthromboembolic causes of transient vision loss such as retinal migraine or retinal vasospasm, the ophthalmologist can provide reassurance as well as potentially give medications to decrease the frequency of vision loss episodes.

Introduction

A proper, well-performed history and physical exam after an episode of transient vision loss (TVL) improves the chance of finding its cause. Determining the etiology of TVL will guide management. This is why there is no “cookie-cutter” algorithm which fits all patients with TVL. TVL is a symptom of some underlying pathophysiologic problem, and so management depends on finding the cause that precipitated it.

TVL is not always interchangeable with “amaurosis fugax”. Most ophthalmologists use the term amaurosis fugax when they suspect a thromboembolic vascular etiology as the cause of monocular TVL.Citation1 Amaurosis fugax comes from a combination of the Greek terms “amauroun” (to darken) and the Latin “fugax” (fleeting). Because many patients present to an ophthalmologist with TVL as the harbinger of cerebrovascular disease,Citation2 it is important to be aware of their future potential for stroke, but not pigeonhole all TVL into amaurosis fugax. lists the major causes to consider when a patient presents with TVL.

Table 1 Categories of transient vision loss

Methodology

We conducted a search using the PubMed database up to November 28, 2015. Reference lists were used to obtain additional studies as warranted. Search keywords included “amaurosis fugax”, “transient monocular vision loss”, “transient monocular blindness”, and “transient vision loss”, with special interest given for publications dated later than 2013. We focused the review on several topics of key interest: the relationship of TVL to thromboembolic vascular disease, hypercoagulable testing, retinal migraine, and bilateral vision loss.

Obtaining a history in patients with TVL

Certain information about pattern, timing, provoking factors, and associated symptoms will provide clues to the etiology of TVL. Obtaining this information will improve the yield and efficiency of ordering further diagnostic tests.

The pattern of visual field loss during an episode of TVL provides prognostic information. Patients with altitudinal TVL are more likely to have a carotid or cardiac embolic source compared to patients with diffuse or constricting patterns of vision loss.Citation3 Altitudinal TVL increases the odds of internal carotid artery stenosis by 3.5.Citation4,Citation5 More specifically, altitudinal onset of TVL yields an odds ratio for carotid disease of 4.1; altitudinal disappearance yields an odds ratio of 2.7.Citation4,Citation5 Since ~40% of patients with an altitudinal defect at the start of TVL progress to a diffuse or total vision loss,Citation3 it is important to specifically ask about how the TVL was perceived at its onset. A smaller percentage of patients have a vertical hemifield TVL.Citation3

In contrast, characteristics of the TVL are less helpful in predicting the nature of future ocular vascular events. No differences in the character of field defects during a TVL differentiate whether a patient will later develop a central retinal artery occlusion (CRAO), retinal vein occlusion, nonarteritic anterior ischemic optic neuropathy, or giant cell arteritis (GCA). There is also no correlation between time lapse from the TVL to when permanent vision loss would occur and the cause of the permanent vision loss.Citation6 Timing and duration of TVL do provide some information, however: patients with TVL lasting 1–10 minutes are more likely to have carotid stenosis.Citation5 Retinal claudication is one historical feature predicting complete carotid occlusion. Dimming of vision in one eye after exposure to bright light after TVL has an odds ratio of 4.8 for finding 100% ipsilateral carotid occlusion.Citation5 Even if the patient is not able to recall much history, this “lack” of information itself may be helpful: patients unable to remember details of their TVL are more likely to have normal carotid arteries.Citation5

Recent ophthalmologic history and a thorough ocular exam also provide important prognostic clues for TVL. There is a subset of patients who have posturally-induced TVL and increased intraocular pressure after vitrectomy or retinal detachment repair.Citation7 Because none in the cohort developed cardiovascular complications, this may be a subgroup of TVL not requiring extensive cardioembolic evaluation. TVL due to nonembolic causes can occur after exercise, long-distance running, or sexual intercourse.Citation8Citation10 The mechanism is probably vasospasm, although evaluation of one man whose symptoms occurred during orgasm revealed closed angles,Citation10 an ocular cause of TVL.

summarizes historical information important to obtain in a patient with TVL.

Table 2 Patient history of transient vision loss

TVL and thromboembolic vascular disease

General considerations

Public awareness that TVL could be a transient ischemic attack (TIA) is low: between 7% and 44%.Citation11,Citation12 This compares to 80%–90% of people who recognize that speech, face, and arm symptoms are associated with stroke.Citation13 Compared to other TIA symptoms, patients with TVL arrive less quickly to the emergency room.Citation14 Time to referral and time to carotid ultrasound for patients with nonvisual TIA are 10 days and 30 days, respectively, compared to 16 and 46 days for patients with TVL.Citation15 Time to carotid endarterectomy (CEA) is 69 days for cortical-type TIA and 103 days for TVL.Citation16

Regarding the incidence of TVL in TIA, one study examined 2,398 patients with suspected TIA over 5 years. In all, 826 (34.5%) reported transient visual symptoms and 422 (17.6%) had “only” visual symptoms. Of these, 36.3% had TVL, 12.3% transient hemianopia, 10.8% bilateral positive visual phenomena, and 4.5% bilateral total vision loss.Citation17 A study from Japan of 444 patients admitted to a TIA center reported 2.9% presenting as TVL.Citation14 What is the incidence of carotid disease in patients with TVL? Of 337 patients with transient monocular vision loss studied prospectively, 159 had a normal internal carotid artery patency, 33 had 0%–69% stenosis, 100 had 70%–99% stenosis, and 45 had 100%.Citation5

Carotid disease

Both the North American Symptomatic Carotid Endarterectomy Trial (NASCET) and the European Carotid Surgery Trial established that early surgery (within 14 days) reduces risk of stroke in TIA patients with carotid disease.Citation18,Citation19 The highest risk period for stroke after TIA is within the first 7 days.Citation20 Performing a CEA within 2 weeks in 1,000 TIA patients would prevent 185 strokes in 5 years, compared to only eight strokes if performed after 12 weeks.Citation21 Only 19% of ophthalmologists are aware of this 2-week time window.Citation20

However, NASCET also found that there is a relatively decreased stroke risk in TVL versus other types of TIA.Citation22 Since risk is lower, it has been suggested that for TVL, surgical treatment of carotid disease be restricted to patients with only certain features ().Citation23 Carotid surgery in patients with two versus three of these risk factors improves 3-year stroke risk reduction from 4.9 to 14.3. Retinal microaneurysms, cotton wool spots, flame or blot retinal hemorrhages, and arteriovenous nicking on exam after TVL also increase stroke risk in patients with TVL, by a factor of 3.Citation24

Table 3 Treatment of carotid disease after transient vision loss

Twenty percent of all CEAs are performed for TVL.Citation25 Carotid artery plaques have less MMP-8, MMP-9, and interleukin-8 in patients with TVL, suggesting a less atheromatous and more collagen-rich substrate.Citation26 Timely evaluation and early intervention are the most important variables for the ophthalmologist to recognize TVL caused by carotid disease.

Retinal artery occlusion

CRAO shares pathophysiologic similarities to stroke, and TVL can be a precursor to both branch retinal artery occlusion (BRAO) and central CRAO.Citation27 The prevalence of TVL prior to CRAO is 12.2%, and BRAO is 15.4%.Citation6 Besides emboli, TVL prior to CRAO could be caused by decreased perfusion pressure due to fall in arterial pressure from comorbid carotid disease or orthostasis, vasospasm, or rise in intraocular pressure.Citation6,Citation28 Because it is difficult to predict which cases of TVL will progress to CRAO,Citation6 management focuses on the diagnostic evaluation and determining the embolic source.

Ocular ischemic syndrome

Carotid disease can produce ocular ischemic syndrome. TVL can occur in ocular ischemic syndrome when bright light saturates the retina. There is often associated dull pain. This light-induced amaurosis may result from failure to regenerate visual pigment due to underlying degenerative changes of the retina from chronic ischemia.Citation29 If TVL is found to be related to ocular ischemic syndrome, management is based on treating the cause of the ischemia, which is often due to severe carotid stenosis.

Cardiac causes

Although most literature on TVL focuses on carotid artery disease, emboli can originate from atrial fibrillation, valvular disease, and other sources from the heart, including mobile masses.Citation30 Management of the TVL when by a cardiac cause is also then dependent on the specific cardiac problem. Recognizing that thromboembolic TVL is not always carotid in origin should prompt evaluation with echocardiogram and electrocardiogram.

Giant cell arteritis

GCA can cause TVL. Fluorescein angiography during an episode of TVL from GCA may show total occlusion of retinal circulation followed by reperfusion.Citation31 The prevalence of TVL in GCA is 32.4%, and the mechanism may be a slight rise in the intraocular pressure (even from rubbing the eyes) in the setting of a thrombosing posterior ciliary artery which compromises optic nerve blood flow.Citation6 One 62-year-old woman was diagnosed with GCA after having painful TVL on awakening. C-reactive protein and sedimentation rates were elevated, and although fundus exam was normal, fluorescein angiography showed delayed and sluggish filling of retinal arterioles, probably due to reversible thrombotic occlusion or retinal vasospasm.Citation32 Management of TVL when caused by GCA is based on proper diagnosis and treatment of the arteritis itself.

Retinal artery stenosis

Approximately 2% of TVL may be due to focal arterial stenosis distal to branching off the internal carotid artery.Citation33 Cerebral angiography may show focal stenosis at the origin of the central retinal artery or ophthalmic artery.Citation34 Viewing the fundus during symptomatic episodes in these cases reveals arteriolar constriction without emboli, and TVL can occur with bending the head down, suggesting hemodynamic change rather than emboli. Treatment with aspirin or calcium channel blockers decreases symptoms, possibly by reducing platelet activation and vasospasm.Citation35

TVL and hypercoagulable states

The role of hypercoagulable states as a cause of TVL is unknown. Hypercoagulability can be caused by acquired or inherited coagulation disorders. A list of common inherited disorders is listed in . Acquired prothrombotic risk factors include immobilization, smoking, and hyperestrogenemia due to pregnancy or exogenous estrogen use.Citation36,Citation37 Although anticoagulation for inherited hypercoagulability may prevent vascular occlusions,Citation36Citation38 a number of recent reviews from the stroke literature have found no correlation between most hypercoagulable states and acute ischemic stroke, and state that there is no indication either for screening or for anticoagulation even if testing is positive.Citation39

Table 4 Hereditable thrombophilias

Indications for thrombophilia testing after TVL should focus on patients with recurrent TVL, or patients with a personal or family history of thrombotic events. Of the inherited thrombophilias, only factor V Leiden was found to have an elevated odds ratio (1.99) for amaurosis fugax and TIA, but only lupus anticoagulant had an increased odds ratio (2.66) for ischemic stroke.Citation40 Because hyperhomocysteinemia is reversible, testing for serum levels may be beneficial. One study including patients with TVL demonstrated 100% normalization of serum homocysteine levels after a median follow-up of 21 months after treatment with folic acid, vitamin B6, and vitamin B12.Citation36 There is no high-level evidence to guide treatment for thrombophilia in the setting of TVL, however, because antiphospholipid antibodies have the highest risk of stroke, and homocysteine can be treated relatively easily with a folate-B6–B12 combination;Citation38,Citation39 these two tests are probably the most appropriate to order in typical TVL. On the other hand, patients with recurrent cryptogenic TVL and other thrombotic history may need a complete hypercoagulable workup, and could require anticoagulation.

TVL and retinal migraine

The International Headache Society defines retinal migraine as reversible monocular vision loss in the setting of a typical migraine.Citation41,Citation42 Migraine should occur within 60 minutes of the vision loss.Citation43 Under this definition, retinal migraine is not as common as some would think,Citation44 as most cases in the literature purporting to describe retinal migraine do not fulfill this description. Among 60 articles with 142 patients reported, only 16 fit the International Headache Society criteria.Citation43 Retinal migraine is referred to by numerous other terms, including visual migraine, eye migraine, and anterior visual pathway migraine, but it should not be confused with classic visual auras (cortical-based visual phenomena), ophthalmoplegic migraine (resulting in diplopia), or silent migraine (aura without headache).

What then is the actual cause for those cases of TVL previously thought to be retinal migraine? Although it may be tempting to suggest these episodes represent spreading depression of Leão, homologous to cortical migrainous phenomena, there is no evidence that spreading depression occurs in the human retina.Citation43 The answer appears to be retinal vasospasm.Citation43 Vasospasm can be precipitated by emotional stress, cold, or exercising.Citation45 Examination during an episode of retinal migraine or vasospasm may show an afferent pupil defect and venous boxcarring, denoting decreased arterial perfusion. Vasospasm can occur in the cervical portion of the left internal carotid artery, which diminishes blood flow to the ophthalmic artery.Citation46 Fluorescein angiography may show choroid blush and delayed central retinal artery circulation, with resolution of all abnormalities once the episode resolves.

In a 12-year retrospective study of 77 patients with nonembolic TVL, only 18% had a past or family history of migraine, and only 15% had headaches. Both retinal vasospasm and migraine are more frequent in women of childbearing age.Citation47 That being said, the female preponderance in retinal migraine is only 1.4:1 compared to 3:1 for migraine.Citation48

Regarding management, calcium channel blockers have shown efficacy. Even in patients with low blood pressure, low doses of calcium channel blocker may still be tolerated (eg, nifedipine 10–20 mg/day).Citation49 Triptans, ergots, and beta blockers are best not used in migraine patients with TVL, due to concern for exacerbating vasoconstriction,Citation50 especially since TVL in retinal migraine has been associated with later onset of permanent vision loss from occlusive conditions like CRAO and BRAO.Citation48

Binocular TVL

It is important to determine if TVL is monocular or binocular. Because patients often fail to notice a deficit in binocular, this may be challenging. Often patients will not notice the nasal deficit, and focus only on the side of the temporal loss, assuming for example that a left hemianopia was actually left monocular visual loss. Transient binocular (cortical) vision loss may have similar causes as transient monocular vision loss (eg, thromboembolic, migraine) or have other causes, including epileptic seizures from the occipital cortex.Citation51

Transient cortical blindness can occur during cerebral angiography, with incidence of 0.3%–1%,Citation52 most commonly during vertebral artery angiography. Vision loss may last for 24 hours. The mechanism may be a posterior reversible encephalopathy-like syndrome, but there is some evidence that the cause is a neurotoxic effect from contrast.Citation53 Resolution with time is the rule.

The prevalence of episodic binocular blindness in migraine patients is 1.6%, lasting from seconds to 120 minutes.Citation54 We treated one patient with a 20-year history of minutes-long transient homonymous hemianopia associated with her migraines. One of the episodes of hemianopia was otherwise typical except it persisted after 3 days. Magnetic resonance imaging (MRI) showed restricted diffusion in the associated visual cortex. Embolic workup was negative, and her field defect resolved after 2 weeks.

Though most literature regarding thromboembolism is focused on monocular vision loss, transient homonymous hemianopia is also an important warning sign of stroke. TIAs are actually more common prior to vertebrobasilar stroke than anterior circulation stroke (odds ratio 2.92).Citation55 Furthermore, the most common TIA in vertebrobasilar stenosis is binocular vision disturbance.Citation55 Management in these cases is similar to that of suspected anterior circulation ischemia.

Acute management of TVL

When TVL is suspected to be caused by thromboembolism, what is the workup? Regarding timing and location of workup, different communities have their own limitations in resources. That being said, there are some data to help guide recommendations. If presentation is within 72 hours, the American Heart Association recommends admission to a hospital setting when age, blood pressure, clinical features, and duration of symptoms (ABCD) score is 3, or for ABCD score of 2 with either uncertainty that outpatient treatments will be done or other evidence of an embolic source.Citation56 For presentation between 3 and 7 days, hospitalization is still recommended if the patient already had a known untreated source of ischemia (carotid stenosis, atrial fibrillation).Citation57 Regarding workup, the most important tests are those which could change management based on finding an active embolic source. This includes large vessel vascular imaging (computed tomography angiogram/magnetic resonance angiogram head/neck, or carotid Doppler for monocular vision loss) and cardiac evaluation (electrocardiogram, echocardiogram). Some sources recommend brain imaging as part of the TVL workup.Citation56,Citation58 One study looked at 213 consecutive patients with BRAO, CRAO, or amaurosis fugax. In all, 23% of patients were found to have infarctions on MRI, most of them asymptomatic.Citation59 However, it is unclear if brain imaging adds information which would change management assuming an otherwise complete vascular workup is performed. There are no clear-cut guidelines regarding when or if to order many of the other ancillary tests discussed earlier (orbital ultrasound, hypercoagulable serum markers, electroencephalogram, etc), but this is why the history and physical examination are so important as they guide the clinician to other appropriate tests.

Conclusion

Managing TVL begins with a focused history and examination. Once a preliminary diagnosis is made, evaluation and treatment depend on the findings. Amaurosis fugax requires workup with carotid and cardiac imaging. Hypercoagulable testing and angiography may be helpful in certain cases. Carotid surgery or antithrombotic medications (antiplatelet/anticoagulation) can prevent future stroke. Retinal vasospasm could be treated with aspirin or calcium channel blockers. Retinal migraine responds to standard migraine treatments. Ocular causes such angle closure are treated accordingly. First and foremost, however, the patient must get evaluated. Therefore, we must continue to educate the public and our medical colleagues about the importance of getting an ophthalmologic evaluation in patients with TVL.

Acknowledgments

The authors wish to thank the OSF Peoria Medical Center Library for their assistance in acquiring references.

Disclosure

The authors report no conflicts of interest in this work.

References

  • PetzoldAIslamNHuH-HPlantGTEmbolic and nonembolic transient monocular visual field loss: a clinicopathologic reviewSurv Ophthalmol2013581426223217587
  • LawlorMPerryRHuntBJPlantGTStrokes and vision: the management of ischemic arterial disease affecting the retina and occipital lobeSurv Ophthalmol201560429630925937273
  • BrunoACorbettJJBillerJAdamsHPJrQuallsCTransient monocular visual loss patterns and associated vascular abnormalitiesStroke199021134392300989
  • DondersRCDutch TMB Study GroupClinical features of transient monocular blindness and the likelihood of atherosclerotic lesions of the internal carotid arteryJ Neurol Neurosurg Psychiatry200171224724911459904
  • BagheriNMehtaSAcute vision lossPrim Care201542334736126319342
  • HayrehSSZimmermanMBAmaurosis fugax in ocular vascular occlusive disorders: prevalence and pathogenesesRetina201434111512223632956
  • SubramanianPSHow urgent is the treatment of transient vision loss?Br J Ophthalmol201498671972024344224
  • PetzoldAIslamNPlantGTPatterns of non-embolic transient monocular visual field lossJ Neurol201326071889190023564298
  • KofoedPKMileaDLarsenMTransient monocular blindness precipitated by sexual intercourseBr J Ophthalmol2009939119918658172
  • LeeMDOdelJGRudichDSRitchRVision loss with sexual activity. J GlaucomaEpub201492625265010
  • PancioliAMBroderickJKothariRPublic perception of stroke warning signs and knowledge of potential risk factorsJAMA199827916128812929565010
  • Sug YoonSHellerRFLeviCWiggersJFitzgeraldPEKnowledge of stroke risk factors, warning symptoms, and treatment among an Australian urban populationStroke20013281926193011486127
  • RobinsonTGReidAHauntonVJWilsonANaylorARThe face arm speech test: does it encourage rapid recognition of important stroke warning symptoms?Emerg Med J201330646747122764171
  • TanakaKUeharaTKimuraKJapan TIA Research Group 2009–2011Features of patients with transient monocular blindness: a multicenter retrospective study in JapanJ Stroke Cerebrovasc Dis2014233e151e15524144597
  • FairheadJFMehtaZRothwellPMPopulation based study of delays in carotid imaging and surgery and the risk of recurrent strokeNeurology200565337137516087900
  • JettyPHusereauDKubelikDWait times among patients with symptomatic carotid artery stenosis requiring carotid endarterectomy for stroke preventionJ Vasc Surg201256366166722608182
  • LavalléePCCabrejoLLabreucheJSpectrum of transient visual symptoms in a transient ischemic attack cohortStroke201344123312331724178913
  • RothwellPMEliasziwMGutnikovSAWarlowCPBarnettHJCarotid Endarterectomy Trialists CollaborationEndarterectomy for symptomatic carotid stenosis in relation to clinical subgroups and timing of surgeryLancet200436394191592415043958
  • KulkamiSRGohelMSBulbuliaRAWhymanMRPoskittKRThe importance of early carotid endarterectomy in symptomatic patientsAnn R Coll Surg Engl200991321021319220938
  • NaylorARRobinsonTGEvesonDBurnsJAn audit of management practices in patients with suspected temporary monocular blindnessBr J Ophthalmol201498673073324187055
  • NaylorARTime is brain!Surgeon200751233017313125
  • FergusonGGEliasziwMBarrHWThe North American Symptomatic Carotid Endarterectomy TrialStroke19993091751175810471419
  • BenaventeOEliasziwMStreiflerJYPrognosis after transient monocular blindness associated with carotid-artery stenosisN Engl J Med2001345151084109011596587
  • WongTYKleinRCouperDJRetinal microvascular abnormalities and incident stroke: the Atherosclerosis Risk in Communities StudyLancet200135892881134114011597667
  • UK Carotid Endarterectomy Audit: Round 4 Public Report (01.10.10–30.09.12) Available from: http://www.vascularsociety.orgAccessed April 2, 2013
  • CheungNKleinRWangJJTraditional and novel cardiovascular risk factors for retinal vein occlusion: the multiethnic study of atherosclerosisInvest Ophthalmol Vis Sci200849104297430218539932
  • GeorgalasIKoutsandreaCImages in clinical medicine. Amaurosis Fugax Caused by a Branch Retinal Artery EmbolusN Engl J Med201537322e2626605943
  • ShahRPMenzoianJOSleep-induced amaurosis fugaxJ Vasc Surg20115451492149421723066
  • ShinYWKimJMJungKHLight-induced amaurosis fugax due to severe distal internal carotid artery stenosis: in view of managing ocular ischemic syndromeJ Neurol201326061655165723568216
  • MehrzadRBajajRA rare but important differential diagnosis in transient monocular blindnessBMJ Case Rep20142014
  • AlwitryARegarding ‘transient visual loss due to reversible ‘pending’ central retinal artery occlusion in occult giant cell arteritis’Eye (Lond)2015298111110.1038/eye.2015.5525857610
  • SaneMSelvaduraiAReidyJHiggsDGonzalez-FernandezFLincoffNTransient visual loss due to reversible ‘pending’ central retinal artery occlusion in occult giant cell arteritisEye (Lond)201428111387139025081291
  • AdamsHPPutmanSFCorbettJJSiresBPThompsonHSAmaurosis fugax: the results of arteriography in 59 patientsStroke19831457427446658958
  • ParkMSKimJTLeeKRRecurrent transient monocular blindness with ophthalmic artery stenosisEur Neurol2008593–420220418230884
  • ChoiSYMoonHJHuhYERecurrent transient monocular blindness from stenotic central retinal arteryJ Clin Neurosci201320111603160523830588
  • GlueckCJHutchinsRKJuranteeJKhanZWangPThrombophilia and retinal vascular occlusionClin Ophthalmol201261377138422969282
  • SchockmanSGlueckCJHutchinsRKPatelJShahPWangPDiagnostic ramifications of ocular vascular occlusion as a first thrombotic event associated with factor V Leiden and prothrombin gene heterozygosityClin Ophthalmol2015959160025897198
  • GlueckCJGoldenbergNBellHGolnikKWangPAmaurosis fugax: associations with heritable thrombophiliaClin Appl Thromb Hemost200511323524116015408
  • KalariaCKittnerSThe therapeutic value of laboratory testing for hypercoagulable states in secondary stroke preventionNeurol Clin201533250151325907919
  • PahusSHHansenATHvasAMThrombophilia testing in young patients with ischemic strokeThromb Res2015S004938481530182110.1016/j.thromres.2015.11.006.26585761
  • Headache Classification Committee of the International Headache SocietyClassification and diagnostic criteria for headache disorders, cranial neuralgias, and facial painCephalalgia19888Suppl 7196
  • Headache Classification Subcommittee of the International Headache SocietyThe International Classification of Headache Disorders, 2nd editionCephalalgia200424Suppl 11160
  • EvansRWGrosbergBMRetinal migraine: migraine associated with monocular visual symptomsHeadache200848114214518184296
  • HillDLDaroffRBDucrosANewmanNJBiousseVMost cases labeled as “retinal migraine” are not migraineJ Neuroophthalmol20072713817414865
  • FlammerJPacheMResinkTVasospasm, its role in the pathogenesis of diseases with particular reference to the eyeProg Retin Eye Res200120331934911286896
  • ShimDHChaJKKangMJChoiJHNahHWVasospastic amaurosis fugax diagnosed by cerebral angiographyJ Stroke Cerebrovasc Dis20152411e323e32526283520
  • JohanssonEPArnerlövCWesterPRisk of recurrent stroke before carotid endarterectomy: the ANSYSCAP studyInt J Stroke20138422022722494778
  • GrosbergBMSolomonSFriedmanDILiptonRBRetinal migraine reappraisedCephalalgia200626111275128617059434
  • PitkänenHSaarelaVVasospastic transient monocular visual loss: effect of treatment with different doses of nifedipineJ Neuroophthalmol201434438638824905274
  • KowacsPAUtiumiMAPiovesanEJThe visual system in migraine: from the bench side to the officeHeadache201555Suppl 1849825659971
  • SinghiPSainiAGSankhyanNAmaurosis fugax caused by neurocysticercosisPediatr Infect Dis J201433442724632665
  • HorwitzNHWenerLTemporary cortical blindness following angiographyJ Neurosurg19744055835864817802
  • LoLWChanHFMaKFChengLFChanTKTransient cortical blindness following vertebral angiography: a case reportNeurointervention2015101394225763297
  • RozenTDMigraine with binocular blindness: a clinic-based studyHeadache201151101529153621812773
  • PaulNLSimoniMRothwellPMOxford Vascular StudyTransient isolated brainstem symptoms preceding posterior circulation stroke: a population-based studyLancet Neurol201312165123206553
  • EastonJDSaverJLAlbersGWDefinition and evaluation of transient ischemic attack: a scientific statement for healthcare professionals from the American Heart Association/American Stroke Association Stroke Council; Council on Cardiovascular Surgery and Anesthesia; Council on Cardiovascular Radiology and Intervention; Council on Cardiovascular Nursing; and the Interdisciplinary Council on Peripheral Vascular DiseaseStroke20094062276229319423857
  • JohnstonSCNguyen-HuynhMNSchwarzMENational Stroke Association guidelines for the management of transient ischemic attacksAnn Neurol200660330131316912978
  • HeleniusJArsavaEMGoldsteinJNConcurrent acute brain infarcts in patients with monocular visual lossAnn Neurol201272228629322926859
  • LaudaFNeugebauerHReiberLJüttlerEAcute Silent Brain Infarction in Monocular Visual Loss of Ischemic OriginCerebrovasc Dis2015403–415115626278894
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