MATERIALS & METHODS

A retrospective analysis of patients with OMD referred to Fondation Ophtalmologique Adolphe de Rothschild (Paris, France) from 1989 to 2015 was conducted after approval of the affiliated ethical committee (CE_20150630_7_LSM). Clinical evaluation included a fiberoptic transnasal laryngoscopy with a swallowing test. All patients were evaluated by the same otolaryngologist and neurophysiologist. Patients underwent complete neurological testing, including brain imaging. Patients were rated as having JOOD, JCOD, or mixed OMD, with or without lingual involvement. Data concerning gender, age of onset, family history of dystonia, presence of associated anatomic sites with dystonia (blepharospasm, cervical dystonia, spasmodic dysphonia, or limb dystonia) were collected. The etiology of dystonia (idiopathic, tardive, neurodegenerative, post-anoxic, or post-traumatic) was recorded. Dystonia was defined as idiopathic when etiology was not determined [1]. Clinical symptoms such as impairment of speech, mastication or swallowing, pain, and dental effects were also recorded.

Electromyography was used for accurate identification of the muscles involved with the exception of the platysma and perioral muscles.

Statistical analysis was performed using R-software [9], Fisher’s exact test, and the Kruskal-Wallis test. The criterion for statistical significance was set at p < 0.05.

RESULTS

Two hundred and forty-four patients with OMD were referred to our institution between 1989 and 2015. Four patients who had initial assessment and treatment performed at another center were excluded. A total of 240 patients were included in our study (Table 1).

The mean age of onset was 51.6 years old (range, 3.0–85.5 years; SD = 18.6 years). The majority of patients were referred to us by neurologists (82%). There was a significant female preponderance—165 of 240 (68.8%) patients were women.

A total of 149 out of 240 (62.1%) patients had JOOD, 48 (20.0%) patients had JCOD, and 43 (17.9%) had mixed OMD. There was no significant difference between these groups in gender or age of onset. Lingual dystonia was present in 64 (26.7%) patients and was significantly more associated with JOOD and mixed OMD than with JCOD (32%, 26%, and 10%, respectively).

Eighty-two of 240 (34.2%) patients had a focal dystonia; 131 (54.6%) patients had a segmental dystonia; and 27 (11.3%) patients had a generalized form of OMD. Segmental dystonia categories included blepharospasm as part of Meige syndrome (93/240, 38.8%), cervical dystonia (64/240, 26.7%), spasmodic dysphonia (49/240, 20.4%), and limb dystonia (14/240, 5.8%). There was no correlation between OMD groups and focal versus segmental/generalized presentation.

Dystonic movements impaired speech in 153 (63.8%) patients, mastication in 118 (49.2%) patients, and swallowing in 65 (27.1%) patients. The movements caused pain in 78 (32.5%) patients and dental impairment (wear or early loss of teeth) in 40 (16.7%) patients. Mastication disorders were less present in JCOD than in JOOD and mixed OMD (25%, 56%, and 58%, respectively). Speech impairment was also less frequent in JCOD than in JOOD and mixed OMD (52%, 70%, and 63%, respectively, p < 0.05). There was no significant difference in swallowing impairment between these groups. Pain was common in JCOD, less present in mixed OMD and rare in JOOD (71%, 40%, and 18%, respectively, p < 0.001). Dental impairment was mostly present in JCOD or mixed OMD and almost absent in JOOD (35%, 37%, and 5%, respectively, p < 0.001).

Most patients (171/240, 71.3%) had idiopathic OMD. Thirty-one (12.9%) patients had tardive dystonia, 18 (7.5%) patients suffered from neurodegenerative disease (Parkinson disease n = 9, pantothenate kinase-associated neurodegeneration n = 3, GM1 gangliosidosis n = 1), 16 (6.7%) patients had a post-anoxic form, and 4 (1.6%) patients presented as post-traumatic OMD. Distribution of dystonia varied depending on etiology (p < 0.001). Idiopathic forms were either segmental (63%), focal (29%), or generalized (8%). Tardive dystonia patients were either focal (52%) or segmental (48%) but never generalized. Post-anoxic forms were often generalized (56%). A family history of dystonia was present in 6 patients (2.5%). Five of these patients suffered from an idiopathic focal or segmental dystonia, and one suffered from a generalized dystonia due to a familial mitochondriopathy.

DISCUSSION

Two hundred and forty patients diagnosed with OMD were evaluated over a 25-year period at our institution. To our knowledge, this study is the largest reported in the literature. A comparison of our demographic data with other studies is presented in Table 2.

Our results are similar to the data published by others in terms of gender ratio and age of onset [5-8]. The female prevalence has no pathophysiologic explanation.

Focal OMD is rare. OMD is more common as part of a spectrum of cranio-facial segmental or generalized dystonia [5,9,10]. In our study, 34.2% of patients had focal OMD whereas 54.6% had segmental dystonia and 11.3% presented with generalized dystonia. Sinclair et al. [11] reported similar findings with 12 of 59 (34.3%) patients having a focal OMD and 65.7% of patients presenting with a segmental or generalized form. In our study, the segmental form included blepharospasm (Meige syndrome) in 38.8% of patients, cervical dystonia in 26.7%, spasmodic dysphonia in 20.4%, and limb dystonia in 5.8%. Tan and Jankovic [4] also found blepharospasm (50.0%) and cervical dystonia (57.4%) as more frequently associated movement disorders.

In our study, JOOD was the most frequent form of OMD, 62.1% of patients had JOOD, 20.0% had JCOD, and 17.9% had mixed OMD, as opposed to other studies reported in the literature. Sinclair et al. [11] reported 47.4% of patients with JCOD, 35.6% with JOOD, and 16.9% with isolated lateral JD. Tan and Jankovic [4] reported 52.5% of patients with JCOD, 21.6% with JOOD, 1.9% with isolated lateral JD, and 24.0% with mixed OMD. This difference may be explained by a bias in the recruitment of our patients whom were mostly referred to us by neurologists (82%) who typically referred JOOD and mixed OMD patients.

Lingual dystonia was present in 26.7% of our cohort and was significantly more associated with JOOD and mixed OMD than with JCOD. There was no correlation between OMD groups and gender, age at diagnosis, or focal versus segmental/generalized presentation. These results are similar to those of Sinclair et al. [11]

Chewing, swallowing, and speech are frequently impaired in OMD, altering quality of life and social relationships [12]. In our cohort, 63.8% of patients had speech impairment, and 49.2% had mastication disorders. Dystonic movements caused pain in 32.5% of patients and dental troubles in 16.7%. Sinclair et al. [11] described similar results with speech and eating impairment in 54.3% of patients, pain in 34.3% and dental effects in 20.0%. Unlike Sinclair et al. [11], we found a correlation between predominant symptoms and OMD type. Mastication and speech impairments were less present in JCOD than in JOOD or mixed OMD. On the other hand, pain and dental troubles were more common in JCOD and mixed OMD. Dental effects were mostly present in JCOD and mixed OMD and rare in JOOD (35%, 37%, and 5%, respectively). This finding may be due to the hyperactivity of masticatory muscles leading to jaw tension, dental contacts, pain, and other dental effects.

Most patients in our cohort (71.3%) presented as idiopathic OMD. The most frequent secondary form was tardive dystonia (12.9%). Tan and Jankovic [4] observed similar results with 63.0% of patients having idiopathic OMD and 22.8% presenting as tardive type.

Conclusion

OMD is a chronic and disabling focal dystonia. Our study shows a prevalence of female patients, an onset of symptoms between 50 and 60 years of age, and an idiopathic etiology in the majority of patients. JOOD was the most frequent type of OMD, as opposed to other reports.

Notes

Conflicts of Interest

The authors have no financial conflicts of interest.

REFERENCES

• 1. Albanese A, Bhatia K, Bressman SB, Delong MR, Fahn S, Fung VS, et al. Phenomenology and classification of dystonia: a consensus update. Mov Disord 2013;28:863–873.ArticlePubMedPMC
• 2. Merz RI, Deakin J, Hawthorne MR. Oromandibular dystonia questionnaire (OMDQ-25): a valid and reliable instrument for measuring health-related quality of life. Clin Otolaryngol 2010;35:390–396.ArticlePubMed
• 3. Balasubramaniam R, Rasmussen J, Carlson LW, Van Sickels JE, Okeson JP. Oromandibular dystonia revisited: a review and a unique case. J Oral Maxillofac Surg 2008;66:379–386.ArticlePubMed
• 4. Tan EK, Jankovic J. Botulinum toxin A in patients with oromandibular dystonia: long-term follow-up. Neurology 1999;53:2102–2107.ArticlePubMed
• 5. Lee KH. Oromandibular dystonia. Oral Surg Oral Med Oral Pathol Oral Radiol Endod 2007;104:491–496.ArticlePubMed
• 6. Marsden CD. Blepharospasm-oromandibular dystonia syndrome (Brueghel’s syndrome). A variant of adult-onset torsion dystonia? J Neurol Neurosurg Psychiatry 1976;39:1204–1209.ArticlePubMedPMC
• 7. Epidemiological Study of Dystonia in Europe (ESDE) Collaborative Group. A prevalence study of primary dystonia in eight European countries. J Neurol 2000;247:787–792.ArticlePubMedPDF
• 8. Blanchet PJ, Rompré PH, Lavigne GJ, Lamarche C. Oral dyskinesia: a clinical overview. Int J Prosthodont 2005;18:10–19.ArticlePubMed
• 9. Singer C, Papapetropoulos S. A comparison of jaw-closing and jaw-opening idiopathic oromandibular dystonia. Parkinsonism Relat Disord 2006;12:115–118.ArticlePubMed
• 10. Scott BL. Evaluation and treatment of dystonia. South Med J 2000;93:746–751.ArticlePubMed
• 11. Sinclair CF, Gurey LE, Blitzer A. Oromandibular dystonia: long-term management with botulinum toxin. Laryngoscope 2013;123:3078–3083.ArticlePubMed
• 12. Papapetropoulos S, Singer C. Eating dysfunction associated with oromandibular dystonia: clinical characteristics and treatment considerations. Head Face Med 2006;2:47.ArticlePubMedPMCPDF

Figure & Data

References

Citations

Citations to this article as recorded by  

• Surface electromyography for evaluating patients with oromandibular dystonia
  Jae-Hyung Kim, Byung-Gook Kim, Yeong-Gwan Im
  CRANIO®.2024; 42(3): 316.     CrossRef
• Tongue dystonia as CIS and presenting symptom of multiple sclerosis
  Farid Shamlou, Narges Ebrahimi, Ahmad Chitsaz
  Neuroimmunology Reports.2024; 5: 100191.     CrossRef
• Oromandibular dystonia: from onset to spread a multicenter italian study
  Assunta Trinchillo, Marcello Esposito, Carmen Terranova, Vincenzo Rizzo, Giovanni Fabbrini, Gina Ferrazzano, Daniele Belvisi, Roberto Erro, Paolo Barone, Francesco Bono, Francesca Di Biasio, Anna Rita Bentivoglio, Christian Lettieri, Maria Concetta Altavi
  Neurological Sciences.2024;[Epub]     CrossRef
• Oromandibular Dystonia: Clinical and Demographic Data from Eight-Two Patients
  Mehmet Balal, Meltem Demirkiran
  Tremor and Other Hyperkinetic Movements.2023;[Epub]     CrossRef
• Oromandibular Dystonia is a Prominent Feature in Patients with Aromatic L-Amino Acid Decarboxylase (AADC) Deficiency
  Helio van der Linden Jr., Christiane Cobas, Andre Felipe Pinto Duarte, Marcelo Rodrigues Masruha
  Journal of Inborn Errors of Metabolism and Screening.2023;[Epub]     CrossRef
• Clinical Presentation and Management of Peripheral-induced Oromandibular Dystonia in Nigeria: A Case Report and Literature Update
  Nonso Emmanuel Onyia, Mercy Okoh, Obinna Francis Igwilo, Izegboya Vivian Ukpebor, Eze Stephen Nwauzor
  Nigerian Journal of Medicine.2023; 32(4): 433.     CrossRef
• Oromandibular dystonia – A systematic review
  Udit Saraf, Mitesh Chandarana, KP Divya, Syam Krishnan
  Annals of Indian Academy of Neurology.2022; 25(1): 26.     CrossRef
• Botulinum Toxin Therapy for Oromandibular Dystonia and Other Movement Disorders in the Stomatognathic System
  Kazuya Yoshida
  Toxins.2022; 14(4): 282.     CrossRef
• Botulinum toxin injections in jaw-opening dystonia. The lateral pterygoid – maxillary artery problem
  Sena Ünal, F. Tugra Karaarslan-Turk, Muhittin Cenk Akbostanci, Elif Peker, Rezzak Yilmaz
  Journal of Clinical Neuroscience.2022; 101: 217.     CrossRef
• Oromandibular dystonia seen during pramipexole treatment: A rare case
  Fatma KARA, Mehmet Fatih GÖL, Ayhan VARLIBAŞ
  Journal of Surgery and Medicine.2022; 6(6): 1.     CrossRef
• Dystonia, chorea, hemiballismus and other dyskinesias
  Matteo Bologna, Josep Valls-Solè, Nitish Kamble, Pramod Kumar Pal, Antonella Conte, Andrea Guerra, Daniele Belvisi, Alfredo Berardelli
  Clinical Neurophysiology.2022; 140: 110.     CrossRef
• Movement disorders of the mouth: a review of the common phenomenologies
  C. M. Ghadery, L. V. Kalia, B. S. Connolly
  Journal of Neurology.2022; 269(11): 5812.     CrossRef
• Botulinum Toxin in Movement Disorders: An Update
  Charenya Anandan, Joseph Jankovic
  Toxins.2021; 13(1): 42.     CrossRef
• Temporomandibular disorder–related characteristics and treatment outcomes in Oromandibular Dystonia patients in two different clinical settings: A cross‐sectional study
  Asha Sude, Joseph Matsumoto, Shanti Kaimal, Ashley Petersen, Donald R. Nixdorf
  Journal of Oral Rehabilitation.2021; 48(5): 542.     CrossRef
• Jaw Pain and Oromandibular Dysfunction After a Complex Hospital Course
  Sarah Smith, Ny-Ying Lam
  American Journal of Physical Medicine & Rehabilitation.2021; 100(5): e62.     CrossRef
• Oromandibular Dystonia: A Clinical Examination of 2,020 Cases
  Laura M. Scorr, Stewart A. Factor, Sahyli Perez Parra, Rachel Kaye, Randal C. Paniello, Scott A. Norris, Joel S. Perlmutter, Tobias Bäumer, Tatiana Usnich, Brian D. Berman, Marie Mailly, Emmanuel Roze, Marie Vidailhet, Joseph Jankovic, Mark S. LeDoux, Ric
  Frontiers in Neurology.2021;[Epub]     CrossRef
• Evaluation of Treatment Outcomes in Oromandibular Dystonia Using Surface Electromyography: A Case Series
  Yeong-Gwan Im, Jae-Hyung Kim, Byung-Gook Kim
  Journal of Oral Medicine and Pain.2021; 46(4): 143.     CrossRef
• Application of botulinum toxin in pregnancy and its impact on female reproductive health
  Wu Li, Min Tang
  Expert Opinion on Drug Safety.2020; 19(1): 83.     CrossRef
• Prevalence and clinical characteristics of patients with oromandibular dystonia seen in the orofacial pain clinic: a retrospective study
  Asha Sude, Donald R. Nixdorf
  Oral Surgery, Oral Medicine, Oral Pathology and Oral Radiology.2020; 130(2): 169.     CrossRef
• Clinical spectrum of focal dystonias: Experience from a tertiary care center
  Rupesh Prasad, Deepika Joshi, VijayN Mishra, RameshwarN Chaurasia, Abhishek Pathak
  Annals of Movement Disorders.2020; 3(2): 99.     CrossRef
• Bite injury related to oromandibular dystonia extending to the maxillary sinus: A case report
  Yoshiro Koma, Takehiro Fujimoto, Shinji Uejima, Kotaro Sato, Keisuke Sugimoto, Satoshi Yamaguchi, Jun Ishikawa, Kazuya Nambu, Hideharu Hibi
  Journal of Oral and Maxillofacial Surgery, Medicine, and Pathology.2020; 32(6): 503.     CrossRef
• Botulinum neurotoxin a therapy efficacy and safety for oromandibular dystonia: a meta-analysis
  Pariessa D. Dadgardoust, Raymond L. Rosales, Ria Monica Asuncion, Dirk Dressler
  Journal of Neural Transmission.2019; 126(2): 141.     CrossRef
• Botulinum Neurotoxin Therapy for Lingual Dystonia Using an Individualized Injection Method Based on Clinical Features
  Kazuya Yoshida
  Toxins.2019; 11(1): 51.     CrossRef
• Oromandibular dystonia, mental distress and oro‐facial dysfunction—A follow‐up 8‐10 years after start of treatment with botulinum toxin
  Merete Bakke, Sara Baram, Torben Dalager, Heidi Bryde Biernat, Eigild Møller
  Journal of Oral Rehabilitation.2019; 46(5): 441.     CrossRef
• Pseudodystonia: A new perspective on an old phenomenon
  Rok Berlot, Kailash P. Bhatia, Maja Kojović
  Parkinsonism & Related Disorders.2019; 62: 44.     CrossRef
• Severe Jaw‐Opening Dystonia as an Unusual Manifestation of Levodopa‐Related Wearing‐Off in Parkinson's Disease, and Successful Treatment With Botulinum Toxin Injection
  Pankaj Ashok Agarwal
  Movement Disorders Clinical Practice.2019; 6(6): 500.     CrossRef

Comments on this article