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   <ref-type name="Journal Article">17</ref-type>
   <contributors>
    <authors>
     <author>Bikbova, M.M.</author>
     <author>Usubova, E.L.</author>
     <author>Oganisyana, K.Kh.</author>
     <author>Lobov, S.L.</author>
     <author>Khasanovad, R.R.</author>
     <author>Dzhemilevab, L.U.</author>
     <author>Khusnutdinova, E.K.</author>
    </authors>
   </contributors>
   <titles>
    <title></title>
   </titles>
   <dates>
    <year>2017</year>
    <pub-dates>
     <date>2018-03-07</date>
    </pub-dates>
   </dates>
   <doi>10.1134/S1022795417040020</doi>
   <abstract>Keratoconus (KC) is the most common form of keratoectasia characterized by changes in corneal&#13;
topography and its thinning, stretching, and protrusion. The hereditary or genetic theory of keratoconus&#13;
development is widely recognized. To date, a large number of candidate genes have been investigated in&#13;
patients with KC. One of the most important of them are the gene encoding a homeodomain-containing protein&#13;
that belongs to the subfamily of paired-like homeodomain proteins (VSX1), superoxidedismutase 1&#13;
(SOD1) gene, and the gene of lysyloxidase (LOX). The linkage analysis reveals over 17 chromosomal regions&#13;
mutations in which can lead to the development of KC. In families with a hereditary form of keratoconus by&#13;
GWAS analysis, the association of central corneal thickness (CCT) with a number of genetic loci is revealed.&#13;
Thus, diverse results of genetic studies and a large number of identified chromosomal regions associated with&#13;
keratoconus, firstly, show marked genetic heterogeneity of the disease and, secondly, are associated with&#13;
challenges in DNA diagnosis of this disease. However, there are prerequisites that keratoconus belongs to&#13;
both hereditary and genetically caused diseases and identified genetic variants are specific both to individual&#13;
populations and to certain ethnic groups in general.</abstract>
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     <url>https://repo.bashgmu.ru/publication/230</url>
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