A MUTATION IN THE MUCOSAL KERATIN K4 IS ASSOCIATED WITH ORAL WHITE SPONGE NEVUS

被引：101

作者：

RUGG, EL

MCLEAN, WHI

ALLISON, WE

LUNNY, DP

MACLEOD, RI

FELIX, DH

LANE, EB

MUNRO, CS

机构：

[1] EDINBURGH DENT HOSP,DEPT ORAL MED,EDINBURGH EH3 9YW,MIDLOTHIAN,SCOTLAND

[2] GLASGOW DENT HOSP,DEPT ORAL MED,GLASGOW G2 3JZ,LANARK,SCOTLAND

[3] SO GEN HOSP,DEPT DERMATOL,GLASGOW G51 4TF,LANARK,SCOTLAND

来源：

NATURE GENETICS | 1995年 / 11卷 / 04期

基金：

英国惠康基金;

关键词：

D O I：

10.1038/ng1295-450

中图分类号：

Q3 [遗传学];

学科分类号：

071007 ; 090102 ;

摘要：

White sponge nevus (WSN) is a benign autosomal dominant disorder which affects non-cornifying stratified squamous epithelia (MIM 193900) (ref. 1). Phenotypically it presents as white ‘spongy’ plaques (oral leukokeratoses), most commonly in the mouth but also reported in the esophagus and anogenital mucosa2. Histologically, the plaques show evidence of hyperproliferation, acanthosis and tonofilament aggregation3–5. These types of pathogenic changes are characteristic of many of the epidermal keratin disorders6. Keratins are expressed in pairs by epithelial cells in a tissue and cell specific manner. The major differentiation specific keratins of the buccal mucosa, nasal, esophageal and anogenital epithelia are K4 and K13 (ref. 7). The tissue distribution and nature of the lesions in patients affected by WSN suggested that mutations in K4 and/or K13 might be responsible for this disorder. We have now confirmed this hypothesis and report here a three base-pair (bp) deletion in the helix initiation peptide of K4 in affected members from two families with this condition. © 1995 Nature Publishing Group.

引用

页码：450 / 452

页数：3

共 21 条

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