This article may incorporate text from a large language model. (December 2024) |
Bosma arhinia microphthalmia ayndrome' (BAMS), Hyposmia-nasal and ocular hypoplasia-hypogonadotropic hypogonadism syndrome, or just Bosma syndrome is a rare genetic disorder characterized by nasal and ocular abnormalities, often accompanied by endocrine dysfunction.
Bosma arhinia microphthalmia syndrome | |
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Other names |
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Specialty | Medical genetics |
Symptoms | |
Causes | Mutations in SMCHD1 gene |
Presentation
editThe typical indicator of BAMS is arrhinia, characterized by the complete absence of an external nose or, in some cases, a severely underdeveloped (hypoplastic) nose.[1][2] This is often accompanied by the absence of olfactory bulb, leading to impaired smell (hyposmia or anosmia) and taste (ageusia).[1] Patients typically exhibit microphthalmia (abnormally small eyeballs) or anophthalmia (absence of eyeballs), resulting in severe vision impairment or blindness.[2][3] Additional eye abnormalities may include colobomas, cataracts, and nasolacrimal duct obstruction.[1] Common craniofacial abnormalities include a high-arched or cleft palate, absence of paranasal sinuses, choanal atresia, and a hypoplastic maxilla. Some patients may also present with external ear abnormalities.[1][2] BAMS is associated with hypogonadotropic hypogonadism, leading to absent or delayed puberty and sexual development. This can manifest as underdeveloped genitals in males and lack of breast development or menstruation in females.[1] Despite the severe craniofacial abnormalities, patients with BAMS typically have normal cognition and intellectual abilities.[1]
Genetics
editBosma arhinia microphthalmia syndrome is primarily caused by mutations in the SMCHD1 gene, which encodes a protein involved in gene silencing during embryonic development and is particularly important to the development of the head and facial features.[4][2][5] These mutations are typically de novo and occur in the N-terminal GHKL-type ATPase domain, suggesting a gain-of-function effect that disrupts normal nasal and ocular development.[6][7] BAMS follows an autosomal dominant inheritance pattern, meaning a single mutated copy of the SMCHD1 gene can cause the disorder.[2] While SMCHD1 is the primary gene implicated, other unknown genetic factors may also contribute to the condition's severity.[2][5]
Pathophysiology
editThe SMCHD1 gene plays a critical role in craniofacial development by regulating chromatin structure and gene expression during embryogenesis.[8] Disruption in these processes due to SMCHD1 mutations can lead to the developmental anomalies observed in BAMS.[8][9]
Diagnosis
editBosma arhinia microphthalmia syndrome is typically diagnosed at birth due to its distinct facial features, such as the absence of the nose and small or absent eyes. The initial diagnosis is primarily based on a thorough physical examination.[5][2] However, genetic testing is needed to confirm the diagnosis by identifying mutations in the SMCHD1 gene. The SMCHD1 gene is analyzed using techniques such as next-generation sequencing to detect pathogenic variants that are characteristic of BAMS.[7] Such analyses are needed to distinguish BAMS from other syndromes that present with similar craniofacial abnormalities, such as CHARGE syndrome or Treacher Collins syndrome.[3][1][10] Due to potential endocrine dysfunctions associated with BAMS, hormonal evaluations may be conducted to assess for hypogonadotropic hypogonadism, which is common in affected individuals.[5][2]
Treatment
editTreatment is primarily symptomatic and focuses on addressing the needs of each individual. Given the complexity and rarity of the syndrome, a multidisciplinary approach is often required, involving specialists such as pediatricians, endocrinologists, ophthalmologists, and craniofacial surgeons. Surgical reconstruction can be considered to improve both function and appearance of the nose. This may involve multiple staged surgeries to create a nasal structure that allows for normal breathing and enhances facial aesthetics. Advances in technology, such as 3D printing, have enhanced the ability to create custom nasal implants, improving cosmetic outcomes.[11][12] For individuals with microphthalmia or anophthalmia, ocular prosthesis can be used to improve cosmetic appearance. In cases where some vision is present, ophthalmologists may provide interventions to maximize visual function.[3][12]
Individuals with BAMS experience hypogonadotropic hypogonadism due to disrupted gonadotropin-releasing hormone (GnRH) neurons. Hormone therapy can help manage this condition by supplementing deficient hormones, thereby supporting normal pubertal development and fertility when appropriate.[4][10] Given the visible nature of craniofacial differences and potential social challenges, psychological support and counseling are often recommended for patients and their families.[5][12] Genetic counseling is also recommended to provide information about the hereditary aspects of BAMS.[12] Regular follow-up care is essential to monitor growth, development, and any emerging complications. This includes managing associated comorbidities such as vitamin D deficiency, which can lead to osteoporosis if untreated.[4][1]
Epidemiology
editBosma arhinia microphthalmia syndrome is an extremely rare genetic disorder, with fewer than 100 reported cases worldwide.[1] Due to its rarity, precise epidemiological data, including incidence and prevalence rates, are not well established. The condition appears to affect both males and females equally, although specific gender-based prevalence data are lacking. BAMS has been documented in various populations globally, but the distribution of cases does not suggest any particular ethnic or geographic predisposition. The rarity of the syndrome means that it often goes unreported in many regions, contributing to the difficulty in gathering comprehensive epidemiological data.[1]
References
edit- ^ a b c d e f g h i j Cong, N. V.; Minh, L. H.; Hoang, L. H.; Do, U.; Dung, N. T. (20 February 2023). "Bosma Arhinia Microphthalmia Syndrome (BAMS): First Report from Vietnam". Cureus. 15 (2): e35222. doi:10.7759/cureus.35222. PMC 10032420. PMID 36968924.
- ^ a b c d e f g h "Bosma arhinia microphthalmia syndrome" (PDF). MedlinePlus. Retrieved 17 December 2024.
- ^ a b c "Ocular Manifestations of Bosma Arrhinia Microphthalmia Syndrome (BAMS) - EyeWiki". eyewiki.org. Retrieved 2024-12-17.
- ^ a b c Atencia Goñi, José; Orera Clemente, María; Del Valle Diéguez, Mariano José; González Fernández, Laura; González Albarrán, Olga (2024-03-01). "Clinical report of Bosma arhinia microphthalmia syndrome with a new variant on SMCHD1 gene. A case report". Endocrinología, Diabetes y Nutrición (in Spanish). 71 (3): 138–143. doi:10.1016/j.endinu.2023.12.011. ISSN 2530-0164.
- ^ a b c d e A, Syed S. (2024-09-27). "What is Bosma Arhinia Microphthalmia Syndrome?". News-Medical. Retrieved 2024-12-17.
- ^ Gurzau, A. D.; Chen, K.; Xue, S.; Dai, W.; Lucet, I. S.; Ly, T. T.; Reversade, B.; Blewitt, M. E.; Murphy, J. M. (10 May 2018). "FSHD2- and BAMS-associated mutations confer opposing effects on SMCHD1 function". The Journal of Biological Chemistry. 293 (25): 9841–9853. doi:10.1074/jbc.RA118.003104. PMC 6016475. PMID 29748383.
- ^ a b Lemmers, R. J.; Van Der Stoep, N.; Van Der Vliet, P. J.; Moore, S. A.; Granado, D. S.; Johnson, K.; Topf, A.; Straub, V.; Evangelista, T.; Mozaffar, T.; Kimonis, V.; Selvatici, R.; Ferlini, A.; Voermans, N.; Van Engelen, B.; Sacconi, S.; Tawil, R.; Lamers, M.; Van Der Maarel, S. M. (26 June 2019). "SMCHD1 mutation spectrum for facioscapulohumeral muscular dystrophy type 2 (FSHD2) and Bosma arhinia microphthalmia syndrome (BAMS) reveals disease-specific localisation of variants in the ATPase domain". Journal of Medical Genetics. 56 (10): 693–700. doi:10.1136/jmedgenet-2019-106168. PMC 6800092. PMID 31243061.
- ^ a b Schall, Peter Z; Rueben, Meghan L; Latham, Keith E (25 October 2019). "A new role for SMCHD1 in life's master switch and beyond". Trends in Genetics : Tig. 35 (12): 948–955. doi:10.1016/j.tig.2019.10.001. PMC 6884149. PMID 31668908.
- ^ "SMCHD1 gene". Gene Vision. Retrieved 2024-12-17.
- ^ a b Brasseur, Benjamin; Martin, Cindy M.; Cayci, Zuzan; Burmeister, Lynn; Schimmenti, Lisa A. (May 2016). "Bosma arhinia microphthalmia syndrome: Clinical report and review of the literature". American Journal of Medical Genetics. Part A. 170A (5): 1302–1307. doi:10.1002/ajmg.a.37572. ISSN 1552-4833. PMID 26842768.
- ^ Brusati, Roberto; Colletti, Giacomo (May 2012). "The Role of Maxillary Osteotomy in the Treatment of Arhinia". Journal of Oral and Maxillofacial Surgery. 70 (5): e361–e368. doi:10.1016/j.joms.2012.01.009.
- ^ a b c d "Bosma Arhinia Microphthalmia Syndrome - Symptoms, Causes, Treatment | NORD". rarediseases.org. Retrieved 2024-12-17.