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KERATIN-13 POINT MUTATION UNDERLIES THE HEREDITARY MUCOSAL EPITHELIA DISORDER WHITE SPONGE NEVUS

被引:88
作者
RICHARD, G
DELAURENZI, V
DIDONA, B
BALE, SJ
COMPTON, JG
机构
[1] NIAMSD,SKIN BIOL LAB,BETHESDA,MD 20892
[2] UNIV ROMA TOR VERGATA,DEPT EXPTL MED,BIOCHEM LAB,IRCCS,IST DERMOPATICO IMMACOLATA,I-00167 ROME,ITALY
[3] IRCCS,IST DERMOPATICO IMMACOLATA,I-00167 ROME,ITALY
来源
NATURE GENETICS | 1995年 / 11卷 / 04期
关键词
D O I
10.1038/ng1295-453
中图分类号
Q3 [遗传学];
学科分类号
071007 ; 090102 ;
摘要
Although pathogenic keratin mutations have been well characterized in inherited epidermal disorders, analogous defects in keratins expressed in non-epidermal epithelia have yet to be described. White sponge nevus (WSN) is a rare autosomal dominant disorder of non-cornifying squamous epithelial differentiation that presents clinically as bilateral white, soft, thick plaques of the oral mucosa. Less frequently the mucous membranes of the nose, esophagus, genitalia and rectum are involved1,2. Histopathological features, including epithelial thickening, parakeratosis, extensive vacuolization of the suprabasal keratinocytes2 and compact aggregates of keratin intermediate filaments (KIF) in the upper spinous layers3,4, resemble those found in epidermal disorders due to keratin defects. We analysed a multigenerational family with WSN and found cosegregation of the disease with the keratin gene cluster on chromosome 17. We identified a missense mutation in one allele of keratin 13 that leads to proline substitution for a conserved leucine. The mutation occurred within the conserved 1A region of the helical rod domain, which is critical for KIF stability and is the site of most pathogenic keratin mutations. This mutation enlarges the spectrum of keratins with disease-causing defects to include mucosally expressed keratin 13, and extends the known keratin diseases to disorders of non-cornifying stratified squamous epithelia. © 1995 Nature Publishing Group.
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页码:453 / 455
页数:3
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