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DOI: 10.1055/s-0044-1787000
Knobloch Syndrome Type 1 with a Novel Pathogenic Variant in the COL18A1 Gene: Case Report and Review of the Literature
Funding None.
Abstract
Knobloch syndrome type 1 (KNO1) is a rare autosomal recessive disorder characterized by various ocular abnormalities, developmental delay, central nervous system, and urogenital tract abnormalities. KNO1 occurs phenotypically in the presence of at least two pathogenic variants of the COL18A1 gene in biallelic state, regardless of the individual's sex. We describe a novel nonsense variant in the COL18A1 gene, associated with KNO1 in a 2-year-old boy, born of a nonconsanguineous couple. This boy was referred for genetic analysis based on clinical evidence of bilateral frontal polymicrogyria of unknown etiology. Whole-exome sequencing and targeted analysis of genes associated with ataxia, polymicrogyria, and hereditary malformations of the brain was employed. One known pathogenic heterozygous splice acceptor variant (NM_001379500.1:c.929–2A > G) and one likely pathogenic novel nonsense heterozygous variant (NM_001379500.1:c.3083C > A) in the COL18A1 gene were identified. The c.929–2A > G substitution affects the splice acceptor sequence and causes impaired messenger ribonucleic acid (mRNA) maturation. The c.3083C > A variant affects the translated sequence and leads to the formation of a stop codon. Both variants are thought to result in a lack of protein product (as a result of nonsense-mediated mRNA decay) or in the production of truncated nonfunctional protein. KNO1 can go undiagnosed, thus, genetic testing can be a powerful tool for disease detection, specifically in cases in which retinal detachment and occipital encephalocele syndrome are present. Timely diagnosis not only ensures that patients are aware of the potential complications resulting from the condition such as lens subluxation, retinal detachment, and glaucoma, but can help plan appropriate disease prevention and therapy measures in affected families.
Keywords
Knobloch syndrome type 1 - COL18A1 gene - retinal detachment - occipital encephalocele syndrome - whole-exome sequencingLocation where the work was performed: Malinov Hospital, 46 Gotse Delchev Blvd, Sofia, Bulgaria.
Publikationsverlauf
Eingereicht: 07. August 2023
Angenommen: 18. April 2024
Artikel online veröffentlicht:
29. Mai 2024
© 2024. Thieme. All rights reserved.
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References
- 1 Knobloch syndrome, type I. Online Mendelian Inheritance in Man;. 2016 . Accessed April 30, 2024 at: http://www.omim.org/entry/267750
- 2 Knobloch WHLJ. Retinal detachment and encephalocele. J Pediatr Ophthalmol 1971; 8: 181-184
- 3 Czeizel AE, Göblyös P, Kustos G, Mester E, Paraicz E. The second report of Knobloch syndrome. Am J Med Genet 1992; 42 (06) 777-779
- 4 Haghighi A, Tiwari A, Piri N. et al. Homozygosity mapping and whole exome sequencing reveal a novel homozygous COL18A1 mutation causing Knobloch syndrome. PLoS One 2014; 9 (11) e112747
- 5 White RJ, Wang Y, Tang P, Montezuma SR. Knobloch syndrome associated with Polymicrogyria and early onset of retinal detachment: two case reports. BMC Ophthalmol 2017; 17 (01) 214
- 6 Antonarakis SE, Holoubek A, Rapti M. et al. Dominant monoallelic variant in the PAK2 gene causes Knobloch syndrome type 2. Hum Mol Genet 2021; 31 (01) 1-9
- 7 Dulac O. Knobloch syndrome. Orphanet; 2008 . Accessed April 30, 2024 at: http://www.orpha.net/consor/cgi-bin/OC_Exp.php?Lng=EN&Expert=1571
- 8 Khan AO, Aldahmesh MA, Mohamed JY, Al-Mesfer S, Alkuraya FS. The distinct ophthalmic phenotype of Knobloch syndrome in children. Br J Ophthalmol 2012; 96 (06) 890-895
- 9 Zhang LS, Li HB, Zeng J, Yang Y, Ding C. Knobloch syndrome caused by homozygous frameshift mutation of the COL18A1 gene in a Chinese pedigree. Int J Ophthalmol 2018; 11 (06) 918-922
- 10 Richards S, Aziz N, Bale S. et al; ACMG Laboratory Quality Assurance Committee. Standards and guidelines for the interpretation of sequence variants: a joint consensus recommendation of the American College of Medical Genetics and Genomics and the Association for Molecular Pathology. Genet Med 2015; 17 (05) 405-424
- 11 Berisio R, Vitagliano L, Mazzarella L, Zagari A. Crystal structure of the collagen triple helix model [(Pro-Pro-Gly)(10)](3). Protein Sci 2002; 11 (02) 262-270
- 12 Popp MW, Maquat LE. Organizing principles of mammalian nonsense-mediated mRNA decay. Annu Rev Genet 2013; 47: 139-165
- 13 Suzuki O, Kague E, Bagatini K. et al. Novel pathogenic mutations and skin biopsy analysis in Knobloch syndrome. Mol Vis 2009; 15: 801-809
- 14 Bhattacharjee A, Bansal M. Collagen structure: the Madras triple helix and the current scenario. IUBMB Life 2005; 57 (03) 161-172
- 15 Elamaa H, Snellman A, Rehn M, Autio-Harmainen H, Pihlajaniemi T. Characterization of the human type XVIII collagen gene and proteolytic processing and tissue location of the variant containing a frizzled motif. Matrix Biol 2003; 22 (05) 427-442
- 16 Määttä M, Heljasvaara R, Pihlajaniemi T, Uusitalo M. Collagen XVIII/endostatin shows a ubiquitous distribution in human ocular tissues and endostatin-containing fragments accumulate in ocular fluid samples. Graefes Arch Clin Exp Ophthalmol 2007; 245 (01) 74-81
- 17 Chong SC, Yuen YP, Cao Y. et al. Case report: novel biallelic variants in the COL18A1 gene in a Chinese Family with Knobloch syndrome. Front Neurol 2022; 13: 853918
- 18 Seppinen L, Pihlajaniemi T. The multiple functions of collagen XVIII in development and disease. Matrix Biol 2011; 30 (02) 83-92
- 19 Shi H, Huang Y, Zhou H. et al. Nucleolin is a receptor that mediates antiangiogenic and antitumor activity of endostatin. Blood 2007; 110 (08) 2899-2906
- 20 Paisán-Ruiz C, Scopes G, Lee P, Houlden H. Homozygosity mapping through whole genome analysis identifies a COL18A1 mutation in an Indian family presenting with an autosomal recessive neurological disorder. Am J Med Genet B Neuropsychiatr Genet 2009; 150B (07) 993-997
- 21 Suzuki OT, Sertié AL, Der Kaloustian VM. et al. Molecular analysis of collagen XVIII reveals novel mutations, presence of a third isoform, and possible genetic heterogeneity in Knobloch syndrome. Am J Hum Genet 2002; 71 (06) 1320-1329
- 22 Mahajan VB, Olney AH, Garrett P. et al. Collagen XVIII mutation in Knobloch syndrome with acute lymphoblastic leukemia. Am J Med Genet A 2010; 152A (11) 2875-2879
- 23 Joyce S, Tee L, Abid A, Khaliq S, Mehdi SQ, Maher ER. Locus heterogeneity and Knobloch syndrome. Am J Med Genet A 2010; 152A (11) 2880-2881
- 24 Elahi E. Genetic basis of primary angle closure glaucoma: the role of collagens and extracellular matrix. J Ophthalmic Vis Res 2020; 15 (01) 1-3
- 25 Suri F, Yazdani S, Chapi M. et al. COL18A1 is a candidate eye iridocorneal angle-closure gene in humans. Hum Mol Genet 2018; 27 (21) 3772-3786
- 26 Seaver LH, Joffe L, Spark RP, Smith BL, Hoyme HE. Congenital scalp defects and vitreoretinal degeneration: redefining the Knobloch syndrome. Am J Med Genet 1993; 46 (02) 203-208
- 27 Passos-Bueno MR, Marie SK, Monteiro M. et al. Knobloch syndrome in a large Brazilian consanguineous family: confirmation of autosomal recessive inheritance. Am J Med Genet 1994; 52 (02) 170-173
- 28 Sniderman LC, Koenekoop RK, O'Gorman AM. et al. Knobloch syndrome involving midline scalp defect of the frontal region. Am J Med Genet 2000; 90 (02) 146-149
- 29 Menzel O, Bekkeheien RC, Reymond A. et al. Knobloch syndrome: novel mutations in COL18A1, evidence for genetic heterogeneity, and a functionally impaired polymorphism in endostatin. Hum Mutat 2004; 23 (01) 77-84
- 30 Khaliq S, Abid A, White DR. et al. Mapping of a novel type III variant of Knobloch syndrome (KNO3) to chromosome 17q11.2. Am J Med Genet A 2007; 143A (23) 2768-2774
- 31 Caglayan AO, Baranoski JF, Aktar F. et al. Brain malformations associated with Knobloch syndrome–review of literature, expanding clinical spectrum, and identification of novel mutations. Pediatr Neurol 2014; 51 (06) 806-813.e8
- 32 Charsar BA, Goldberg EM. Polymicrogyria and intractable epilepsy in siblings with Knobloch syndrome and homozygous mutation of COL18A1. Pediatr Neurol 2017; 76: 91-92
- 33 Corbett MA, Turner SJ, Gardner A. et al. Familial epilepsy with anterior polymicrogyria as a presentation of COL18A1 mutations. Eur J Med Genet 2017; 60 (08) 437-443
- 34 Hull S, Arno G, Ku CA. et al. Molecular and clinical findings in patients with Knobloch syndrome. JAMA Ophthalmol 2016; 134 (07) 753-762
- 35 Keren B, Suzuki OT, Gérard-Blanluet M. et al. CNS malformations in Knobloch syndrome with splice mutation in COL18A1 gene. Am J Med Genet A 2007; 143A (13) 1514-1518
- 36 Kliemann SE, Waetge RT, Suzuki OT, Passos-Bueno MR, Rosemberg S. Evidence of neuronal migration disorders in Knobloch syndrome: clinical and molecular analysis of two novel families. Am J Med Genet A 2003; 119A (01) 15-19