Abstract
Abstract
Oculo-auriculo-vertebral spectrum (OAVS) is a rare condition characterized by the involvement of the first branchial arches.
Purpose
To investigate the ear abnormalities of a sample of patients with OAVS.
Materials and methods
The sample consisted of 12 patients with OAVS seen at the Clinical Genetics Unit, UFCSPA/CHSCPA. The study included only patients who underwent mastoid computed tomography and with normal karyotype. We performed a review of its clinical features, giving emphasis to the ear findings.
Results
Nine patients were male, the ages ranged from 1 day to 17 years. Ear abnormalities were observed in all patients and involved the external (n=12), middle (n=10) and inner ear (n=3). Microtia was the most frequent finding (n=12). The most common abnormalities of the middle ear were: opacification (n=2), displacement (n=2) and malformation of the ossicular chain. Agenesis of the internal auditory canal (n=2) was the most frequent alteration of the inner ear.
Conclusions
Ear abnormalities are variable in patients with OAVS and often there is no correlation between findings in the external, middle and inner ear. The evaluation of these structures is important in the management of individuals with OAVS.
Keywords: ear, ear auricle, ear canal, facial asymmetry, goldenhar syndrome
INTRODUCTION
Branchial arch disorders comprise several developmental anomalies including the oculo-auriculo-vertebral spectrum (OAVS), also known as Goldenhar's syndrome, or hemifacial microsomy (OMIM 164210)1. This is a rare, complex, and phenotypically variable condition2,3. Its estimated prevalence is 1 case for every 5,600 to 26,550 births4, 5, 6; the condition affects males more than females (about 3:2)2. The OAVS may range from mild to severe forms; facial involvement is usually asymmetric, occurring mostly on the right2,7.
The origin of the OAVS is unclear, but it is a complex and heterogeneous condition. Two pathophysiologic mechanisms have been proposed for the OAVS: a reduced blood flow, and focal hemorrhage in the development region of the first and second branchial arches around 30 to 45 days of pregnancy, in the blastogenesis period2. These mechanisms explain the outer ear abnormalities in this spectrum, as the first branchial arch gives rise to the anterior ear primordium, and the second branchial arch originates the posterior ear primordium. Also, the outer ear canal derives from the dorsal portion of the first branchial cleft8,9. It is thought that the etiology may be related with a migration anomaly of neural crest cells. Other evidence has suggested that there are genetic determinants in some cases. A few reports have mentioned families with recessive autosomal or dominant autosomal inheritance. The literature contains several descriptions of chromosomal anomalies and gestational exposure that mimic its phenotype (thalidomide, retinoic acid, and diabetes mellitus)2.
Although external ear anomalies have been described in OAVS patients - to the point of being inclusion criteria - middle and especially inner ear alterations have received little attention in the literature9, 10, 11, 12, 13. Thus, the purpose of this study was to investigate the clinical findings in a sample of OAVS patients, focusing on ear alterations.
MATERIAL AND METHODS
The sample comprised 12 patients with the OAVS seen at the Clinical Genetics Unit, UFCSPA/CHSCPA. The inclusion criteria were alterations in at least two of the following bodily regions: oro-cranial-facial, ocular, auricular, and vertebral, according to Strömland et al.'s criteria (2007)12. Only patients with normal GTG banded karyotypes (to exclude patients with chromosomal alterations that mimic the OAVS), according to the Yunis modified technique (1981)14, and in which computed tomography of the mastoid including middle and inner ear assessments had been done were included. All patients belonged to the sample described by Rosa et al. (2010)15; these authors evaluated the frequency and type of cardiac anomalies in OAVS patients.
The registries of patients were reviewed to gather clinical data and the results of diagnostic tests (focusing on ear anomalies). Fisher's exact test (bicaudate) was applied to compare the frequencies were found. The software was the PEPI program. Values of p<0.05 were considered statistically significant. The institutional review board approved this study (Opinion no. 581/08 of 25/01/2008).
RESULTS
There were 9 male and 3 female subjects. The ages at the first visit ranged from 1 day to 17 years (10 were aged 1 year or less). Most of these patients were referred from the pediatrics unit (n= 7); two others were referred from the plastic surgery unit, one from the cardiology unit, one from the otorhinolaryngology unit, and one from the pediatric surgery unit. Eight subjects had two of the inclusion criteria, three subjects had three, and one had four. All subjects had ear anomalies, affecting the external ear (n= 12), the middle ear (n= 8), and the inner ear (n= 3). Microtia was the most frequent finding - it was observed in all cases (ranging from grades I to IV). It was mostly unilateral, to the left, and grade III. Four patients had bilateral microtia (33%). The most common middle ear anomaly was opacification (n= 2), and displaced (n= 2) and malformed ossicular chains (n= 2). Agenesis of the inner ear canal (n= 2) was the most frequent inner ear anomaly. The most common finding in the temporal bone was a non-aerated mastoid (n= 5). Additional alterations in other organs or systems consisted of low height (n=4), craniofacial anomalies (n= 11), ophthalmologic anomalies (n= 2), esophageal/ pulmonary anomalies (n= 6), cardiac anomalies (n= 7), abdominal anomalies (n= 4), skeletal anomalies (n= 6), and cerebral anomalies (n= 5) (Figs. 1 and 2; Table 1).
Table 1.
Oculo-auriculo-vertebral spectrum (OAVS) | |||||||||||||
---|---|---|---|---|---|---|---|---|---|---|---|---|---|
Clinical findings | 1 | 2 | 3 | 4 | 5 | 6 | 7 | 8 | 9 | 10 | 11 | 12 | Total |
Sex | F | F | F | M | M | M | M | M | M | M | M | M | M-9 / F-3 |
Ethnic group | C | M | C | C | C | M | C | C | C | C | C | C | C-2 / M-2 |
Age at first visit | 1y | 6m | 2m | 2d | 1d | 17y | 2d | 1m | 6d | 2m | 5y | 1m | 1d - 17y |
Strömland et al.'s criteria (2007)11 | 3 | 2 | 3 | 2 | 4 | 2 | 2 | 2 | 2 | 2 | 3 | 2 | 2-8 / 3-3 / 4-1 |
Low height | + | + | + | + | 4 | ||||||||
Craniofacial anomalies | + | + | + | + | + | + | + | + | + | + | + | 11 | |
Facial hypoplasia (asymmetry) | L | L | L | L | L | L | L | R | L-7 / R-1 | ||||
Facial palsy | L | L | L | R | L-3 / R-1 | ||||||||
Others | + | + | + | + | + | + | + | + | + | 9 | |||
Eye anomalies | + | + | 2 | ||||||||||
Ear anomalies | + | + | + | + | + | + | + | + | + | + | + | + | 12 |
- External ear | + | + | + | + | + | + | + | + | + | + | + | + | 12 |
Preauricular appendages | R | R | L | R | R | B | L | L | L-3 / R-4 / B-1 | ||||
Microtia | + | + | + | + | + | + | + | + | + | + | + | + | 12 |
Grade I | L | B | L | B | L-2 / B-2 | ||||||||
Grade II | L | L-1 | |||||||||||
Grade III | L | R | L | L | L | L | R | L-5 / R-2 | |||||
Grade IV | B | B-1 | |||||||||||
Agenesis of the outer ear canal | L | L | L | L | L | L | B | L | L-7 / R-1 / B-1 | ||||
Stenotic outer ear canal | L | R | L-1 / R-1 | ||||||||||
- Middle ear | + | + | + | + | + | + | + | + | 8 | ||||
Opacified middle ear | R | R | R-2 | ||||||||||
Agenesis of the middle ear | B | B-1 | |||||||||||
Hypoplasic tympanic cleft | R | R-1 | |||||||||||
Agenesis of the tympanic cleft | L | L-1 | |||||||||||
Hypoplasic ossicular chain | L | L-1 | |||||||||||
Displaced ossicular chain | L | B | L-1 / B-1 | ||||||||||
Malformed ossicular chain | L | R | L-1 / R-1 | ||||||||||
Widened tympanic cavity | L | L | L-2 | ||||||||||
Decreased tympanic cavity | L | L-1 | |||||||||||
- Inner ear | + | + | + | 3 | |||||||||
Hypoplasic inner ear | L | L-1 | |||||||||||
Agenesis of the inner ear canal | B | L | L-1 / B-1 | ||||||||||
Altered cochlear morphology | L | L-1 | |||||||||||
Altered semicircular canals | L | L-1 | |||||||||||
Temporal bone anomalies | + | + | + | + | + | 5 | |||||||
Non-aerated mastoid | L | B | B | B | B | L-1 / B-4 | |||||||
Lengthened mastoid antrum | B | B-1 | |||||||||||
Esophageal/lung anomalies | + | + | + | + | + | + | 6 | ||||||
Congenital cardiopathies | + | + | + | + | + | + | + | 7 | |||||
Abdominal anomalies | + | + | + | + | 4 | ||||||||
Skeletal anomalies | + | + | + | + | + | + | 6 | ||||||
CNS anomalies | + | + | + | + | + | 5 |
M: male; F: female; C: Caucasian; M: mixed color; d: day(s); m: month(s); y: year(s); NA: not applicable; NE: not examined; L: left; R: right; B: bilateral.
DISCUSSION
External ear malformations in OAVS patients ranged from slightly dysmorphic to absent ears (or anotia - the most severe form of microtia)16. The term microtia literally means “small ear” although in the literature it applies to small or malformed ears. These ears are often implanted lower down17,18. A few authors have suggested that microtia is the minimum form of the OAVS8; microtia alone or with other minor ear malformations is commonly viewed as one of the minimal criteria for diagnosing this syndrome3,7,19. Thus, as observed in our study (all subjects presented microtia), its frequency is high in OAVS patients (82 to 100%)7,16,17,19. In the literature, microtia has been described as being mostly unilateral and to the right9, which differed from our findings, where a left incidence predominated. Microtia is usually associated with the involved side of the face16,17, as shown on Table 1. Occasionally both ears may be involved (18% to 50% of cases)7,16, as seen in 33% of our study subjects. Common minor ear anomalies in these patients include preauricular appendages and pits. The former consist of skin and cartilage appendages located in any area between the tragus and the angle of the mouth. The latter consist of small depressions generally located on the anterior margin of the ascending portion of the ear helix18. Both may be unilateral or bilateral, and have been described in 53% to 90% of OAVS patients16,19; in our sample, 8 patients (67%) had these anomalies. Other external ear alterations were stenosis (usually in mild cases) and atresia (usually in more severe cases) of the outer ear canal (Table 1 and Frame 1).
Because the ossicles of the ear develop from the dorsolateral terminations of the cartilage in the first (Meckel's cartilage) and second (Reichert's cartilage) branchial arches, anomalies of these structures are often found in the OAVS. Anomalies in the stapedial and tympanic tensor muscle suggest that these structures originate from the first and second branchial arches9. In our sample, 8 patients (67%) had middle ear anomalies, which is a similar to previously reported rates (75%)12. The main middle ear anomalies we encountered were opacification, and displaced or malformed ossicles.
Although external middle ear anomalies are well known, inner ear alterations are rarely observed; these anomalies vary widely and range from mild to severe11, 12, 13.
- Temporal bone anomalies
Poorly pneumatized mastoid antrum
Enlarged cartilaginous portion of the Eustachian tube lumen and absence of the cartilaginous lateral lamina of the Eustachian tube
Lengthened mastoid antrum
- Outer ear malformations
Preauricular appendages and pits
Ear anomalies
Atresia/stenosis of the outer ear canal
Undeveloped tympanic membrane
Microtia/anotia
- Middle ear malformations
Incomplete development of the tympanic cavity
Immature and malformed ear ossicles
Absent oval and round window
Absence of the tympanic tensor muscle
Abnormal path of the facial nerve and absence of the chorda tympani nerve
- Inner ear malformations
Distorted and hypoplasic cochlea
Absence of the cochlear aqueduct
Immature vestibular system and absence/fusion of semicircular canals
Displaced endolymphatic duct
Widened vestibular aqueduct
Absent/abnormally coursing facial nerve canal
Small, wide, and/or duplicated inner ear canal
Agenesis of the inner ear canal
Duplicated inner ear canal
The frequency of these anomalies in our sample (25%) was similar to previously reported rates (27% to 36%)11,12. Inner ear malformations may be agenesis of the inner ear canal, and altered cochlear and semicircular canal morphology - as seen in our study sample. Walking late in children may be associated with malformed vestibular organs, which may be seen in computed tomography12. Inner ear anomalies - in contrast with external and middle ear - go beyond the concept of first and second branchial arch development; in this case a neural crest cell migration disorder is an added pathogenic factor in the OAVS9. Stoll et al. (1998)20 have suggested that there are several pathogenic mechanisms causing the OAVS. Goret-Nicaise et al. (1997)21 have proposed that a defect in blastogenesis may explain its origin.
As mentioned above, the most frequently reported ear anomalies in the OAVS are external and middle ear abnormalities. Thus, secondary conductive hearing loss predominates in these patients2,22; the degree of hearing loss correlates directly with the level of involvement of structures9,13. However, at times a sensorineural component has been observed, which is evidenced by inner ear malformations9,13. Bilateral profound hearing loss is rare in these patients. As described in the literature, these hearing losses may cause impaired language acquisition, because speech and language develop as hearing matures23.
Surgery is difficult because of the complexity of this condition and the number of factors that may affect the outcome of surgical therapy. On the other hand, hearing loss is generally unilateral in the OAVS; the majority of patients develop speech, and their level of hearing enables them to be socially active. However, patients with bilateral mixed profound hearing loss or pure sensorineural hearing loss required more advanced forms of treatment, such as cochlear implants or bone anchored hearing aids13.
CONCLUSION
Ear anomalies are frequent and varied in OAVS patients; often there is no correlation among external, middle, and inner ear findings. Therefore, it is important to assess these structures using radiologic methods (such as computed tomography of the mastoid) when managing patients with OAVS.
Footnotes
Paper submitted to the BJORL-SGP (Publishing Management System – Brazilian Journal of Otorhinolaryngology) on August 17, 2009; and accepted on January 4, 2011. cod. 7273
REFERENCES
- 1.Online Mendelian Inheritance in Man, OMIM (TM) [homepage on the Internet]. Baltimore e Bethesda: BeMcKusick-Nathans Institute for Genetic Medicine, Johns Hopkins University and National Center for Biotechnology Information, National Library of Medicine [cited 2010 Aug 10]. Available from: http://www.ncbi.nlm.nih.gov/omim/.
- 2.Cohen Jr MM, Rollinck BR, Kaye CI. Oculoauriculoveretbral spectrum: an updated critique. Cleft Palate J. 1989;26(4):276–286. [PubMed] [Google Scholar]
- 3.Tasse C, Böhringer S, Fischer S, Lüdecke HJ, Albrecht B, Horn D, et al. Oculo-auriculo-vertebral spectrum (OAVS): clinical evaluation and severity scoring of 53 patients and proposal for a new classification. Eur J Med Genet. 2005;48(4):397–411. doi: 10.1016/j.ejmg.2005.04.015. [DOI] [PubMed] [Google Scholar]
- 4.Grabb WC. The first and second branchial arch syndrome. Plast Reconstr Surg. 1965;36(5):485–508. doi: 10.1097/00006534-196511000-00001. [DOI] [PubMed] [Google Scholar]
- 5.Stoll C, Roth MP, Dott B, Bigel T. Discordance for skeletal and cardiac defect in monozygotic twins. Acta Genet Med Gemellol. 1984;33(3):501–504. doi: 10.1017/s0001566000005961. [DOI] [PubMed] [Google Scholar]
- 6.Melnick M. The etiology of external ear malformations and its relation to abnormalities of the middle ear, inner ear and other organ systems. Birth Defects Orig Artic Ser. 1980;16(4):303–331. [PubMed] [Google Scholar]
- 7.Rollnick BR, Kaye CI, Nagatoshi K, Hauck W, Martin AO. Oculoauriculovertebral dysplasia and variants: phenotypic characteristic of 294 patients. Am J Med Genet. 1987;26(2):361–375. doi: 10.1002/ajmg.1320260215. [DOI] [PubMed] [Google Scholar]
- 8.Pearson A. In: Otolaryngology. English M, editor. Harper and Row; New York: 1978. Developmental anatomy of the ear. pp. 1–68. [Google Scholar]
- 9.Scholtz AW, Fish III JH, Kammen-Jolly K, Ichiki H, Hussl B, Kreczy A, et al. Goldenhar's syndrome: congenital hearing deficit of conductive or sensorineural origin? Temporal bone histopathologic study. Otol Neurotol. 2001;22(4):501–505. doi: 10.1097/00129492-200107000-00016. [DOI] [PubMed] [Google Scholar]
- 10.Phelps PD, Lloyd GA, Poswillo DE. The ear deformities in craniofacial microsomia and oculo-auriculo-vertebral dysplasia. J Laryngol Otol. 1983;97(11):995–1005. doi: 10.1017/s0022215100095888. [DOI] [PubMed] [Google Scholar]
- 11.Bisdas S, Lenarz M, Lenarz T, Becker H. Inner ear abnormalities in patients with Goldenhar syndrome. Otol Neurotol. 2005;26(3):398–404. doi: 10.1097/01.mao.0000169796.83695.56. [DOI] [PubMed] [Google Scholar]
- 12.Strömland K, Miller M, Sjögreen L, Johansson M, Joelsson B-ME, Billstedt E, et al. Oculo-auriculo-vertebral spectrum: associated anomalies, functional deficits and possible development risk factors. Am J Med Genet. 2007;143A(12):1317–1325. doi: 10.1002/ajmg.a.31769. [DOI] [PubMed] [Google Scholar]
- 13.Skarżyński H, Porowski M, Podskarbi-Fayette R. Treatment of ontological features of the oculoauriculovertebral dysplasia (Goldenhar syndrome). Int J Pediatr Otorhinolaryngol. 2009;73(7):915–921. doi: 10.1016/j.ijporl.2009.01.015. [DOI] [PubMed] [Google Scholar]
- 14.Yunis JJ. New chromosome techniques in the study of human neoplasia. Hum Pathol. 1981;12(6):540–549. doi: 10.1016/s0046-8177(81)80068-8. [DOI] [PubMed] [Google Scholar]
- 15.Rosa RFM, Dall'Agnol L, Zen PRG, Pereira VLB, Graziadio C, Paskulin GA. Espectro óculo-aurículo-vertebral e malformações cardíacas. Rev Assoc Med Bras. 2010;56(1):62–66. doi: 10.1590/s0104-42302010000100018. [DOI] [PubMed] [Google Scholar]
- 16.Engyz O, Balel S, Unsal M, Ozer S, Oguz KK, Aktas D. 31 cases with oculoauriculovertebral dysplasia (Goldenhar syndrome): clinical, neuroradiologic, audiologic and cytogenetic findings. Genet Couns. 2007;18(3):277–288. [PubMed] [Google Scholar]
- 17.Touliatou V, Fryssira H, Mavrou A, Kanavakis E, Kitsiou-Tzeli S. Clinical manifestations in 17 Greek patients with Goldenhar syndrome. Genet Couns. 2006;17(3):359–370. [PubMed] [Google Scholar]
- 18.Carey JC. In: Human malformations and related anomalies, 2e. Stevenson RE, Hall JG, editors. University Press; Oxford: 2006. Ear. pp. 935–1022. [Google Scholar]
- 19.Digilio MC, Calzolari F, Capolino R, Toscano A, Sarkozy A, de Zorzi A, et al. Congenital heart defects in patients with oculoauriculo-vertebral spectrum (Goldenhar syndrome). Am J Med Genet. 2008;146A(14):1815–1819. doi: 10.1002/ajmg.a.32407. [DOI] [PubMed] [Google Scholar]
- 20.Stoll C, Viville B, Treisser A, Gasser B. A family with dominant oculoaurivertebral spectrum. Am J Med Genet. 1998;78(4):345–349. doi: 10.1002/(sici)1096-8628(19980724)78:4<345::aid-ajmg8>3.0.co;2-k. [DOI] [PubMed] [Google Scholar]
- 21.Goret-Nicaise M, Baertz G, Saussoy P, Dhem A. Oculo-auriculovertebral spectrum: cranial and vertebral malformations due to focal disturbed chondrogenesis. J Craniofac Genet Dev Biol. 1997;17(1):35–42. [PubMed] [Google Scholar]
- 22.Brosco KC, Zorzetto NL, da Richieri Costa A. Perfil audiológico de indivíduos portadores da síndrome de Goldenhar. Rev Bras Otorrinolaringol. 2004;70:645–649. [Google Scholar]
- 23.Lima FT, de Araújo CB, Sousa EC, Chiari BM. Alterações fonoaudiológicas em um caso de síndrome de Goldenhar. Rev Soc Bras Fonoaudiol. 2007;12:141–145. [Google Scholar]