You are seeing this message because your Web browser does not support basic Web standards. Find out more about why this message is appearing and what you can do to make your experience on this site better.

ABOUT ARCHIVES
Advanced Search

Welcome   | My Account | E-mail Alerts | Access Rights | Sign In

Vol. 137 No. 9, September 2001 TABLE OF CONTENTS
  Archives
 •  Online Features
Observation
 This Article
 •Full text
 •PDF
 •Send to a friend
 • Save in My Folder
 •Save to citation manager
 •Permissions
 Citing Articles
 •Citing articles on HighWire
 •Citing articles on ISI (13)
 •Contact me when this article is cited
 Related Content
 •Related articles
 •Similar articles in this journal
 Topic Collections
 •Genetics
 •Genetic Counseling/ Testing/ Therapy
 •Alert me on articles by topic

Phenotypic Heterogeneity in Bullous Congenital Ichthyosiform Erythroderma

Possible Somatic Mosaicism for Keratin Gene Mutation in the Mildly Affected Mother of the Proband

Kazuo Nomura, MD, PhD; Kaoru Umeki, MD, PhD; Ichiro Hatayama, PhD; Tadayuki Kuronuma, MD, PhD

Arch Dermatol. 2001;137:1192-1195.

Background  Bullous congenital ichthyosiform erythroderma (BCIE) shows phenotypic variability. An epidermal nevus may represent somatic mosaicism for keratin gene mutation, which produces generalized BCIE in the next generation. This fact provides evidence that a postzygotic mutation can be passed on to the next generation in BCIE. We hypothesized that the same phenomenon occurred in a family with BCIE whose phenotypes were extremely different.

Observations  We studied a 19-year-old boy with severe ichthyosiform erythroderma and prominent palmoplantar hyperkeratosis with digital contracture. In contrast, the proband's mother exhibited only mild ichthyosiform skin, granular verrucous lesions, and less severe streaky palmoplantar hyperkeratosis. Mutation analysis in the proband showed a keratin K1 mutation (N187S, ie, an A-to-G transition at the second position of codon 187, resulting in an asparagine-to-serine substitution). In the mother, the same keratin gene mutation was recognized, but only faintly in the leukocyte DNA, indicating that the amount of the mutated allele in leukocyte DNA was very low compared with that from the proband.

Conclusions  We speculate that the mildly affected mother showed keratin 1 gene mosaicism, and that the BCIE phenotype had been transmitted in a severe form through a mechanism that passes the keratin gene mutation to the next generation. These results suggest that mild forms of BCIE may actually represent extensive epidermal nevi/keratin gene mosaicism.


From the Department of Dermatology, Aomori Prefectural Central Hospital, Aomori, Japan (Dr Nomura); Division of Dermatology, Hakodate City Hospital, Hakodate, Japan (Dr Umeki); Aomori Prefectural Institute of Environmental Health (Dr Hatayama); and Division of Pediatrics, Iwaki National Sanatorium, Namioka, Japan (Dr Kuronuma).


RELATED ARTICLES

Expanding Our Concepts of Mosaic Disorders of Skin
Amy S. Paller
Arch Dermatol. 2001;137(9):1236-1238.
EXTRACT | FULL TEXT  

Archives of Dermatology Reader's Choice: Continuing Medical Education
Arch Dermatol. 2001;137(9):1262.
FULL TEXT  


THIS ARTICLE HAS BEEN CITED BY OTHER ARTICLES

Genetic Disorders of Skin: A Decade of Progress
Paller
Arch Dermatol 2003;139:74-77.
FULL TEXT  

Expanding Our Concepts of Mosaic Disorders of Skin
Paller
Arch Dermatol 2001;137:1236-1238.
FULL TEXT  




HOME | CURRENT ISSUE | PAST ISSUES | TOPIC COLLECTIONS | CME | SUBMIT | SUBSCRIBE | HELP
CONDITIONS OF USE | PRIVACY POLICY | CONTACT US | SITE MAP
 
© 2001 American Medical Association. All Rights Reserved.