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Type XVIII Collagen and Knobloch Syndrome

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Knobloch Syndrome is a type of inherited autosomal recessive disorder in which a mutation occurs in the endostatin COL18A1 protein encoding gene, which codes for production of type XVIII collagen.[1] It is speculated that the mutation of type XVIII collagen that occurs in Knobloch syndrome can be located in several variants of endostatin, a gene that interacts with type XVIII collagen to not only develop the ocular system, but to also maintain its visual functionality.[2] Evidence has been found for Knobloch syndrome development in genomes containing no mutations in the COL18A1 gene, and thus different variants of endostatin genes can also be responsible for the disease.[2] One such variant of endostatin genes is the D1437N gene, which occurs after two mutations in the COL18A1 gene: the first is a one-base pair mutation insertion, and the other is an amino acid substitution of a conserved amino acid of endostatin. This amino acid substitution is deleterious because it blocks the endostatin variant from interacting with laminin.[3] This discovery was significant in that it provided a new genetic locus for Knobloch syndrome, which helped to explain the development of the disease from genomes free of mutation in the COL18A1 gene.

The mutations in type XVIII collagen result in a multitude of abnormalities in vision and eye structure, some of which include high myopia, vitreoretinal degeneration, retinal detachment, macular abnormalities, and occipital encephalocele. Additionally, fragile iris, overgrowth of blood vessels in the retina, and an excess of electron-dense deposits, which leads to a disease called dense deposit disease, may also occur in Knobloch syndrome.[4] Type XVIII collagen functions to provide strength, structural integrity, and cohesiveness to the basement membrane region in endothelial and epithelial cells of many different types of tissues. When type XVIII collagen is mutated at the COL18A1 gene, exon 2 in the sequence is skipped, which results in production of an early termination codon in exon 4 of this gene's transcript. This type of mutation particularly affects only one isoform of type XVIII collagen - the short isoform type, while the medium and long isoforms are unaffected.[2]

  1. ^ Manon‐Jensen, T.; Kjeld, N. G.; Karsdal, M. A. (2016). "Collagen-mediated hemostasis". Journal of Thrombosis and Haemostasis. 14 (3): 438–448. doi:10.1111/jth.13249. ISSN 1538-7836.
  2. ^ a b c Alexander G. Marneros, Bjorn R. Olsen. "Physiological role of collagen XVIII and endostatin". The FASEB Journal – via Research Gate.
  3. ^ Menzel, Olivier; Bekkeheien, Reidunn C. J.; Reymond, Alexandre; Fukai, Naomi; Boye, Eileen; Kosztolanyi, Gyorgy; Aftimos, Salim; Deutsch, Samuel; Scott, Hamish S.; Olsen, Bjorn R.; Antonarakis, Stylianos E. (2004). "Knobloch syndrome: Novel mutations in COL18A1, evidence for genetic heterogeneity, and a functionally impaired polymorphism in endostatin". Human Mutation. 23 (1): 77–84. doi:10.1002/humu.10284. ISSN 1098-1004.
  4. ^ Manon‐Jensen, T.; Kjeld, N. G.; Karsdal, M. A. (2016). "Collagen-mediated hemostasis". Journal of Thrombosis and Haemostasis. 14 (3): 438–448. doi:10.1111/jth.13249. ISSN 1538-7836.