Apraxia of Lid Opening

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Apraxia of eyelid opening is defined as a non-motor abnormality characterized by the patient's difficulty in eyelid elevation bilaterally. There is an inability of voluntary eye reopening without an orbicularis oculi spasm despite sustained frontalis contraction. This activity describes the evaluation and management of apraxia of eyelid opening and reviews the role of the interprofessional team in improving care for patients with this condition.

Objectives:

  • Identify the etiology and epidemiology of apraxia of lid opening.
  • Review the appropriate evaluation of apraxia of lid opening.
  • Outline the management options available for apraxia of lid opening.
  • Summarize interprofessional team strategies for improving care coordination and communication to advance the care of apraxia of lid opening and improve outcomes.

Introduction

Apraxia of eyelid opening is defined as a non-motor abnormality characterized by the patient's difficulty in eyelid elevation bilaterally. There is an inability of voluntary eye reopening without an orbicularis oculi spasm despite sustained frontalis contraction. It is most commonly associated with blepharospasm (persistent focal dystonia, with eyelid muscle contraction). The definition is a misnomer, given that it is very rarely a pure and true apraxia.[1] Very rarely, it can occur as an isolated idiopathic phenomenon.

Max Heinrich Lewandowsky, a renowned German physician and academician, first described it in 1907 in his essay Über apraxie des Lidschlusses. Later, Schilder reported in 1927 two patients (one with Huntington's chorea) and Riese in 1930 one patient with frontotemporal injury from a bullet. No other reports are found in the literature until 1965 when Goldstein and Cogan reported four patients (Huntington's disease, parkinsonism, parkinsonian syndrome after cyanide attempted suicide, and cerebral diplegia).[2]

Etiology

The most common etiology of apraxia of eyelid opening is idiopathic focal dystonia. Other causes documented in the literature include:

  • Blepharospasm or focal dystonia of the eyelids - idiopathic (also known as benign essential blepharospasm), infectious (keratitis, blepharitis, dacryocystitis, conjunctivitis), toxic exposure (extensive sunlight), autoimmune (keratoconjunctivitis sicca from Sjogren's disease), neurodegenerative (Parkinson's and Huntington's disease)
  • Face or eyebrow ptosis - severe levator palpebrae dysfunction from abnormal development, vascular injury, neuromuscular disease (myasthenia gravis), neuroimmunological (multiple sclerosis), trauma, iatrogenic (eye surgery). Ptosis can easily be corrected by tightening the muscle's tendon that raises the eyelids.
  • Dermatochalasis - refers to excess upper or lower eyelid skin, or both. This is merely baggy eyelids and can be fixed by removing the excess baggage and skin in the eyelids.
  • Psychogenic- photophobia, fatigue

Epidemiology

The most common form of blepharospasm, benign essential blepharospasm, is the etiology where the epidemiology has been studied. The mean annual incidence is about 0.10%, with a peak incidence in the 50-60 year age group (0.19%). It is only slightly more prevalent in females (0.12%) than males (0.07%).[3] It can progress, and within a period of six months to three years, can lead to impairment of functional independence due to visual disability, job loss, and other quality of life measures.

Risk factors include a high level of urbanization and certain occupations. There are several co-morbidities associated, which include dyslipidemia, parasomnias, psychiatric (depression, anxiety, and obsessive-compulsive disorder), dry eye-related diseases (idiopathic or related to Sjögren's syndrome), and to a lesser degree, Parkinson's disease and rosacea.

Pathophysiology

The pathogenesis of apraxia of eyelid opening and blepharospasm is poorly understood, but there a few hypotheses based on animal model studies. Nigro-striatal basal ganglia pathways may project to the premotor control of eyelid coordination. Therefore, it is associated with dysfunction in the corticothalamic, basal ganglia, and focal cranial nerve circuitry.[4] Structures involved include sensorimotor cortical regions, substantia nigra pars reticulata, and brainstem motor nuclei (trigeminal blink reflex arc).

At the biochemical level, abnormal dopamine neurotransmission likely underlies the abnormal blinking and eyelid muscle contraction. Secondary causes of eyelid opening problems include neuromuscular junction diseases, neurodegenerative diseases, autoimmune disease, and ocular or central nervous system structural lesions.

History and Physical

Patients describe difficulty opening the eyes voluntarily and feeling persistent periorbital contractions. Most of the time, it occurs after the patient voluntarily closes the eyes. Patients show compensatory behaviors, which may include thrusting the head backward, manually opening the eyes with their fingers, and rubbing the eyebrows.

It is crucial to ascertain the historical progression of symptoms. A thorough past medical and ocular history may reveal risk factors associated with the condition. A focal ocular exam is essential, including visual acuity and field testing, ocular pressure testing, pupillary reflexes, extraocular movements, dilated fundoscopic examination, and slit-lamp examination. The examination can help narrow the etiology of the symptoms.

An external evaluation of the eyelids and facial muscles is essential to assess eyebrow and eyelid ptosis, dermatochalasis, and spasms of the orbicularis oculi, procerus, and corrugator muscles. Assessing mental status, language skills, and other cranial exams may be useful if central causes are suspected.

Evaluation

This condition is a clinical diagnosis; therefore, a thorough medical history and physical, ocular history and focused visual exam are essential. Historical inquiry of progression and risk factors can narrow the differential. There have been clinical criteria established by Defazio and Berardelli for the identification of clinical and physical exam phenomenology, with validation from expert neurologists and neuro-ophthalmologists.[5] These include: orbicularis oculi involuntary spastic eyelid narrowing/closure, bilateral laterality, synchronous spasm frequency, stereotypical spasm pattern, alleviation with a sensory trick, inability to suppress spasms, and high-frequency blink count at rest. A combination of them had a 93% sensitivity and 90% specificity for blepharospasm. A focal physical and ocular exam can help identify and confirm the clinical diagnosis.

If a central nervous system cause is suspected, a head computed tomographic (CT) scan or a brain magnetic resonance imaging (MRI) with and without contrast is performed.

Extensive serum laboratories and cerebrospinal fluid analysis, including systemic immune, autoimmune, and infectious causes, may be useful to exclude secondary causes of blepharospasm.

Treatment / Management

Botulinum toxin A is considered the first-line treatment.[6][7] Baggy eyelids (dermatochalasis) is repaired by removing the excess baggage and skin in the eyelids. Ptosis is corrected by tightening the muscle's tendon that raises the eyelids.

For refractory cases, myectomy with tightening of the levator tendon that elevates the eyelids (also called aponeurotic ptosis repair) and blepharoplasty can be considered. Myectomy of fibers of orbicularis muscle in the central portion of the eyelid can be performed if botulinum toxin does not produce good results. Frontalis suspension is performed as a last resort, by placing a suture between the forehead muscle and the eyelids.

Differential Diagnosis

Apraxia of eyelid opening, as a feature of blepharospasm, carries a complex differential diagnosis that is most consistent with late-onset dystonia phenomenon, affecting patients older than 50 years of age. Several disorders will present like apraxia of eyelid opening and must be excluded to treat them appropriately.

  • Idiopathic
    • Benign essential blepharospasm with or without sensory features including eye-burning pain, keratoconjunctivitis sicca, sensory trick, and photophobia[8][9]
    • Meige's syndrome: a triad of blepharospasm, oromandibular dystonia, and cervical dystonia
    • Brueghel's syndrome: blepharospasm, oromandibular dystonia, +/- torticollis,  +/- dystonic writer's cramp, appendicular dystonic posturing of the arms, dystonic respiration, and spasmodic torticollis[10][11]
  • Iatrogenic
    • Drug-induced: associated with tardive dyskinesias with use of mood stabilizers (antidepressants, antipsychotics, antiepileptics), antimicrobials, and antiarrhythmics[12]
    • Levodopa and apomorphine in progressive supranuclear palsy[13]
    • Deep brain stimulation on the subthalamic nucleus and the globus pallidus internus for Parkinson's disease patients[14][15]  
  • Genetic
    • Primary blepharospasm and dystonias: they can be accompanied by cervical dystonia. Torsin family 1 member A polymorphism with mutation on dystonia 1 protein,[16][17][18] guanine nucleotide-binding protein,[19] anoctamin 3,[20] tubulin beta4A,[21] and zinc finger protein 1[16][22]
  • Structural
    • Vascular or traumatic injury of the midbrain, basal ganglia, thalamus, cerebellum, and motor cortex[23]
    • Hemifacial spasm: spasmodic unilateral facial contractions including eyelid blepharospasm due to facial nerve irritation
  • Neuroinflammatory
    • Bell's palsy: unilateral facial hemiparesis, constitutional symptoms (fever, chills), headaches, neck rigidity, retro auricular or jaw pain, hypersalivation, hyper acoustic phonophobia, dysgeusia, keratoconjunctivitis sicca
    • Myasthenia gravis: oculomotor fatigue[24][25]
  • Neurodegenerative
    • Parkinson's disease[26][27] 
    • Focal, segmental or generalized dystonia: uncontrolled hyperkinetic movements, including blepharospasm

Prognosis

The prognosis is dependent on the chronicity, etiology, and responsiveness to the first-line treatment. Apraxia of lid opening may be challenging to treat in many cases. In general, responsiveness to treatment is a good prognostic factor, in terms of morbidity. Chronicity and refraction to treatment can lead to more disruption in functional independence and disability.

Complications

Treatments with botulinum toxin can produce uncommon and transient adverse side effects such as ptosis, blurry vision, and diplopia that spontaneously resolves in a few weeks.[26][27][28]

Consultations

  • Neurologists
  • Movement disorder specialists
  • Social workers
  • Case managers
  • Occupational therapists

Deterrence and Patient Education

There are no avoidable factors to prevent the occurrence of apraxia of eyelid opening. The functional independence of the patient can be affected by unresponsiveness to treatment. Disability can occur from impairment in visual integrity, causing job loss and the performance of activities of daily living.

Treatment with botulinum toxin frequently produces good results, but complications from its use can occur. Patients should seek medical attention as apraxia of eyelid opening can be a symptom of numerous disorders that require additional treatments, including Parkinson's and Huntington's disease, myasthenia gravis, Sjogren's disease, multiple sclerosis, and psychiatric disorders.

Pearls and Other Issues

  • Apraxia of eyelid opening is defined as a non-motor abnormality characterized by the patient's difficulty in eyelid elevation bilaterally.
  • Commonly occurs after the patient voluntarily close the eyes.
  • The definition is a misnomer, given that it is very rarely pure and true apraxia.
  • It is associated with dysfunction in the corticothalamic, basal ganglia, and focal cranial nerve circuitry.
  • Structures involved include sensorimotor cortical regions, substantia nigra pars reticulata, and brainstem motor nuclei.
  • The most common etiology of apraxia of eyelid opening is idiopathic focal dystonia.
  • Other causes include blepharospasm or focal dystonia of the eyelids, infectious, toxic exposure, autoimmune, neurodegenerative, face or eyebrow ptosis, neuromuscular, trauma, iatrogenic, dermatochalasis, ptosis, psychogenic, and fatigue.
  • Patients show compensatory behaviors, which may include thrusting the head backward, manually opening the eyes with their fingers, and rubbing the eyebrows.
  • Botulinum toxin A is considered the first-line treatment.
  • Several disorders will present like apraxia of eyelid opening and must be excluded to treat them appropriately.
  • The prognosis is dependent on the chronicity, etiology, and responsiveness to the first-line treatment.
  • Chronicity and refraction to treatment can lead to more disruption in functional independence and disability.

Enhancing Healthcare Team Outcomes

The outcomes of apraxia of eyelid opening depend on the cause. However, to improve outcomes, prompt consultation with an interprofessional group of specialists is recommended. The neurologist, in conjunction with occupational therapists, plays an integral part in the treatment. Botulinum toxin injections are usually performed by the ophthalmologist, oculoplastic surgeon, or plastic surgeon. Sometimes it can be injected by the neurologist or movement disorder specialist. Shared decision making and communication are recommended elements for a good outcome. Social worker and case management evaluation may be required for unresponsive cases as apraxia of eyelid opening can cause disability to the patient with impairment of activities of daily living and job performance.

Details

Author

Franklyn Rocha Cabrero

Editor:

Orlando De Jesus

Updated:

8/8/2023 1:42:36 AM

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References

[1]

Boghen D. Apraxia of lid opening: a review. Neurology. 1997 Jun:48(6):1491-4     [PubMed PMID: 9191752]

[2]

GOLDSTEIN JE, COGAN DG. APRAXIA OF LID OPENING. Archives of ophthalmology (Chicago, Ill. : 1960). 1965 Feb:73():155-9     [PubMed PMID: 14237780]

[3]

Sun Y, Tsai PJ, Chu CL, Huang WC, Bee YS. Epidemiology of benign essential blepharospasm: A nationwide population-based retrospective study in Taiwan. PloS one. 2018:13(12):e0209558. doi: 10.1371/journal.pone.0209558. Epub 2018 Dec 26     [PubMed PMID: 30586395]

Level 2 (mid-level) evidence

[4]

Weiss D, Wächter T, Breit S, Jacob SN, Pomper JK, Asmus F, Valls-Solé J, Plewnia C, Gasser T, Gharabaghi A, Krüger R. Involuntary eyelid closure after STN-DBS: evidence for different pathophysiological entities. Journal of neurology, neurosurgery, and psychiatry. 2010 Sep:81(9):1002-7. doi: 10.1136/jnnp.2009.196691. Epub 2010 Jun 20     [PubMed PMID: 20562465]

[5]

Defazio G, Hallett M, Jinnah HA, Berardelli A. Development and validation of a clinical guideline for diagnosing blepharospasm. Neurology. 2013 Jul 16:81(3):236-40. doi: 10.1212/WNL.0b013e31829bfdf6. Epub 2013 Jun 14     [PubMed PMID: 23771487]

Level 1 (high-level) evidence

[6]

Simpson DM, Hallett M, Ashman EJ, Comella CL, Green MW, Gronseth GS, Armstrong MJ, Gloss D, Potrebic S, Jankovic J, Karp BP, Naumann M, So YT, Yablon SA. Practice guideline update summary: Botulinum neurotoxin for the treatment of blepharospasm, cervical dystonia, adult spasticity, and headache: Report of the Guideline Development Subcommittee of the American Academy of Neurology. Neurology. 2016 May 10:86(19):1818-26. doi: 10.1212/WNL.0000000000002560. Epub 2016 Apr 18     [PubMed PMID: 27164716]

Level 1 (high-level) evidence

[7]

Wilkes J. AAN Updates Guidelines on the Uses of Botulinum Neurotoxin. American family physician. 2017 Feb 1:95(3):198-199     [PubMed PMID: 28145664]

[8]

Patel N, Jankovic J, Hallett M. Sensory aspects of movement disorders. The Lancet. Neurology. 2014 Jan:13(1):100-12. doi: 10.1016/S1474-4422(13)70213-8. Epub     [PubMed PMID: 24331796]

[9]

Ramos VF, Karp BI, Hallett M. Tricks in dystonia: ordering the complexity. Journal of neurology, neurosurgery, and psychiatry. 2014 Sep:85(9):987-93. doi: 10.1136/jnnp-2013-306971. Epub 2014 Jan 31     [PubMed PMID: 24487380]

[10]

Marsden CD. Blepharospasm-oromandibular dystonia syndrome (Brueghel's syndrome). A variant of adult-onset torsion dystonia? Journal of neurology, neurosurgery, and psychiatry. 1976 Dec:39(12):1204-9     [PubMed PMID: 1011031]

[11]

Marsden CD. The problem of adult-onset idiopathic torsion dystonia and other isolated dyskinesias in adult life (including blepharospasm, oromandibular dystonia, dystonic writer's cramp, and torticollis, or axial dystonia). Advances in neurology. 1976:14():259-76     [PubMed PMID: 941774]

Level 3 (low-level) evidence

[12]

Zádori D, Veres G, Szalárdy L, Klivényi P, Vécsei L. Drug-induced movement disorders. Expert opinion on drug safety. 2015 Jun:14(6):877-90. doi: 10.1517/14740338.2015.1032244. Epub     [PubMed PMID: 25981904]

Level 3 (low-level) evidence

[13]

Defazio G, De Mari M, De Salvia R, Lamberti P, Giorelli M, Livrea P. "Apraxia of eyelid opening" induced by levodopa therapy and apomorphine in atypical parkinsonism (possible progressive supranuclear palsy): a case report. Clinical neuropharmacology. 1999 Sep-Oct:22(5):292-4     [PubMed PMID: 10516881]

[14]

Umemura A, Toyoda T, Yamamoto K, Oka Y, Ishii F, Yamada K. Apraxia of eyelid opening after subthalamic deep brain stimulation may be caused by reduction of levodopa. Parkinsonism & related disorders. 2008 Dec:14(8):655-7. doi: 10.1016/j.parkreldis.2007.12.008. Epub 2008 Mar 3     [PubMed PMID: 18316231]

[15]

Vagefi MR, Lin CC, McCann JD, Anderson RL. Exacerbation of blepharospasm associated with craniocervical dystonia after placement of bilateral globus pallidus internus deep brain stimulator. Movement disorders : official journal of the Movement Disorder Society. 2008 Feb 15:23(3):454-6     [PubMed PMID: 18074391]

[16]

Defazio G, Matarin M, Peckham EL, Martino D, Valente EM, Singleton A, Crawley A, Aniello MS, Brancati F, Abbruzzese G, Girlanda P, Livrea P, Hallett M, Berardelli A. The TOR1A polymorphism rs1182 and the risk of spread in primary blepharospasm. Movement disorders : official journal of the Movement Disorder Society. 2009 Mar 15:24(4):613-6. doi: 10.1002/mds.22471. Epub     [PubMed PMID: 19202559]

[17]

Siokas V, Dardiotis E, Tsironi EE, Tsivgoulis G, Rikos D, Sokratous M, Koutsias S, Paterakis K, Deretzi G, Hadjigeorgiou GM. The Role of TOR1A Polymorphisms in Dystonia: A Systematic Review and Meta-Analysis. PloS one. 2017:12(1):e0169934. doi: 10.1371/journal.pone.0169934. Epub 2017 Jan 12     [PubMed PMID: 28081261]

Level 1 (high-level) evidence

[18]

Chen Y, Chen K, Burgunder JM, Song W, Huang R, Zhao B, Cao B, Chen X, Jiang Y, Shang HF. Association of rs1182 polymorphism of the DYT1 gene with primary dystonia in Chinese population. Journal of the neurological sciences. 2012 Dec 15:323(1-2):228-31. doi: 10.1016/j.jns.2012.09.025. Epub 2012 Oct 9     [PubMed PMID: 23058565]

[19]

Fuchs T, Saunders-Pullman R, Masuho I, Luciano MS, Raymond D, Factor S, Lang AE, Liang TW, Trosch RM, White S, Ainehsazan E, Hervé D, Sharma N, Ehrlich ME, Martemyanov KA, Bressman SB, Ozelius LJ. Mutations in GNAL cause primary torsion dystonia. Nature genetics. 2013 Jan:45(1):88-92. doi: 10.1038/ng.2496. Epub 2012 Dec 9     [PubMed PMID: 23222958]

[20]

Charlesworth G, Plagnol V, Holmström KM, Bras J, Sheerin UM, Preza E, Rubio-Agusti I, Ryten M, Schneider SA, Stamelou M, Trabzuni D, Abramov AY, Bhatia KP, Wood NW. Mutations in ANO3 cause dominant craniocervical dystonia: ion channel implicated in pathogenesis. American journal of human genetics. 2012 Dec 7:91(6):1041-50. doi: 10.1016/j.ajhg.2012.10.024. Epub 2012 Nov 29     [PubMed PMID: 23200863]

[21]

Hersheson J, Mencacci NE, Davis M, MacDonald N, Trabzuni D, Ryten M, Pittman A, Paudel R, Kara E, Fawcett K, Plagnol V, Bhatia KP, Medlar AJ, Stanescu HC, Hardy J, Kleta R, Wood NW, Houlden H. Mutations in the autoregulatory domain of β-tubulin 4a cause hereditary dystonia. Annals of neurology. 2013 Apr:73(4):546-53. doi: 10.1002/ana.23832. Epub 2013 Feb 19     [PubMed PMID: 23424103]

[22]

Xiao J,Uitti RJ,Zhao Y,Vemula SR,Perlmutter JS,Wszolek ZK,Maraganore DM,Auburger G,Leube B,Lehnhoff K,LeDoux MS, Mutations in CIZ1 cause adult onset primary cervical dystonia. Annals of neurology. 2012 Apr;     [PubMed PMID: 22447717]

[23]

Khooshnoodi MA, Factor SA, Jinnah HA. Secondary blepharospasm associated with structural lesions of the brain. Journal of the neurological sciences. 2013 Aug 15:331(1-2):98-101. doi: 10.1016/j.jns.2013.05.022. Epub 2013 Jun 6     [PubMed PMID: 23747003]

[24]

Hara K, Matsuda A, Kitsukawa Y, Tanaka K, Nishizawa M, Tagawa A. Botulinum toxin treatment for blepharospasm associated with myasthenia gravis. Movement disorders : official journal of the Movement Disorder Society. 2007 Jul 15:22(9):1363-4     [PubMed PMID: 17486596]

[25]

Kurlan R, Jankovic J, Rubin A, Patten B, Griggs R, Shoulson I. Coexistent Meige's syndrome and myasthenia gravis. A relationship between blinking and extraocular muscle fatigue? Archives of neurology. 1987 Oct:44(10):1057-60     [PubMed PMID: 3632379]

[26]

Ramirez-Castaneda J,Jankovic J, Long-term efficacy, safety, and side effect profile of botulinum toxin in dystonia: a 20-year follow-up. Toxicon : official journal of the International Society on Toxinology. 2014 Nov;     [PubMed PMID: 25130293]

[27]

Jochim A, Meindl T, Huber C, Mantel T, Zwirner S, Castrop F, Haslinger B. Treatment of blepharospasm and Meige's syndrome with abo- and onabotulinumtoxinA: long-term safety and efficacy in daily clinical practice. Journal of neurology. 2020 Jan:267(1):267-275. doi: 10.1007/s00415-019-09581-w. Epub 2019 Oct 19     [PubMed PMID: 31630241]

[28]

Diep D, Ko J, Lan J, Koprowicz KT, Ko G. Benefits, Safety, and Adjunct Modality Prevalences of Long-Term Botulinum Toxin Injections for Cervical Dystonia and Myofascial Neck Pain: A Retrospective Cohort Study. Journal of pain research. 2020:13():1297-1304. doi: 10.2147/JPR.S254032. Epub 2020 Jun 3     [PubMed PMID: 32581571]

Level 2 (mid-level) evidence