0
January 1997, Vol 133, No. 1 >
Article | January 1997

Patchy Dermal Hypoplasia as a Characteristic Feature of Proteus Syndrome

Rudolf Happle, MD; Peter M. Steijlen, MD; Ursel Theile, MD; Dietrich Karitzky, MD; Sigrid Tinschert, MD; Helga Albrecht-Nebe, MD; Wolfgang Küster, MD
[+] Author Affiliations

From the Department of Dermatology, Philipp University, Marburg, Germany (Drs Happle and Küster); Department of Dermatology, University Hospital, Nijmegen, the Netherlands (Dr Steijlen); Genetic Counseling Unit of Rheinland-Pfalz, Mainz, Germany (Dr Theile); Department of Pediatrics, Leverkusen Hospital, Leverkusen, Germany (Dr Karitzky); and Departments of Medical Genetics (Dr Tinschert) and Dermatology (Dr Albrecht-Nebe), Charité, Humboldt University, Berlin, Germany.


Arch Dermatol. 1997;133(1):77-80. doi:10.1001/archderm.1997.03890370083012
Text Size: A A A
Published online
Article
References
Comments

Background:  The diagnostic criteria of Proteus syndrome include various lesions of localized overgrowth such as digital gigantism, hemihyperplasia with unilateral macrocephaly, epidermal nevus, and mesodermal hamartomas such as lipoma, lymphangioma, hemangioma, or fibroma. Hyperplasia of the plantar dermal tissue may result in a characteristic cerebriform appearance. However, hypoplastic lesions involving various tissues such as subcutaneous fat or muscles also may be observed in this syndrome. This paradoxical phenomenon has so far been underestimated, and the presence of circumscribed lesions of dermal hypoplasia has been entirely ignored.

Observations:  We report 4 cases of Proteus syndrome associated with large patches of dermal hypoplasia, resulting in a more prominent appearance of venous vasculature.

Conclusions:  Patchy dermal hypoplasia appears to be a characteristic feature within the spectrum of Proteus syndrome. The anomaly should not be confused with partial lipohypoplasia that may likewise be associated with this multisystem birth defect. From a review of the literature, we conclude that patchy dermal hypoplasia may have occurred in several previous cases. In the future, recognition of this cutaneous anomaly may help to establish the diagnosis in otherwise doubtful cases. To explain the coexistence of lesions of dermal hyperplasia and hypoplasia, we propose the genetic concept of "twin spotting." At the gene locus of Proteus syndrome the embryo would carry 1 allele giving rise to dermal overgrowth, whereas the corresponding allele would be responsible for a diminished proliferation of cutaneous fibroblasts. Somatic recombination may result in 2 different populations of cells homozygous for either allele.Arch Dermatol. 1997;133:77-80

REFERENCES

1 +
Wiedemann HR, Burgio GR, Aldenhoff P, Kunze J, Kaufmann HJ, Schirg E.  The Proteus syndrome: partial gigantism of the hands and/or feet, nevi, hemihypertrophy. subcutaneous tumors, macrocephaly or other skull anomalies and possible accerelated growth and visceral affections . Eur J Pediatr. 1983;;140: 5-12.
2 +
Clark RD, Donnai D, Rogers J, Cooper J, Baraitser M.  Proteus syndrome: an expanded phenotype . Am J Med Genet. 1987;;27:99-117.
3 +
Cohen MM Jr.  Understanding Proteus syndrome, unmasking the Elephant Man, and stemming elephant fever . Neurofibromatosis . 1988;;1:260-280.
4 +
Samlaska CP, Levin SW, James WD, Benson PM, Walker JC, Perlik PC.  Proteus syndrome . Arch Dermatol. 1989;;125:1109-1114.
5 +
Happle R.  Mosaicism in human skin: understanding the patterns and mechanisms . Arch Dermatol. 1993;;129:1460-1470.
6 +
Whitehouse HLK. Genetic Recombination: Understanding the Mechanisms . Chichester, England: John Wiley & Sons Ltd; 1982;:214-224.
7 +
Harrison BJ, Carpenter R.  Somatic crossing-over in Antirrhinum majus . Heredity . 1977;:38:169-189.
8 +
Graf U, Würgler FE, Katz AJ, et al.  Somatic mutation and recombination test in Drosophila melanogaster . Environ Mutagen. 1984;:6:153-188.
9 +
Happle R.  Lipomatosis and partial lipohypoplasia in Proteus syndrome: a clinical clue for twin spotting? Am J Med Genet. 1995;;56:332-333.
10 +
Temtamy SA, Rogers JG.  Macrodactyly, hemihypertrophy, and connective tissue nevi: report of a new syndrome and review of the literature . J Pediatr. 1976;;89:924-927.
11 +
Hotamisligil HGS.  Proteus syndrome and hamartoses with overgrowth . Dysmorphol Clin Genet. 1990;;4:87-102.
12 +
Viljoen D, Saxe N, Pearn J, Beighton P.  The cutaneous manifestations of the Klippel-Trenaunay-Weber syndrome . Clin Exp Dermatol. 1987;;12:12-17.
13 +
Goltz RW.  Focal dermal hypoplasia syndrome: an update . Arch Dermatol. 1992;; 128:1108-1111.
14 +
Al-Gazali LI, Donnai D, Berry SA, Say B, Mueller RF.  The oculocerebrocutaneous (Delleman) syndrome . J Med Genet. 1988;:25:773-778.
15 +
Buechner SA, Rufli T.  Atrophodermia of Pasini and Pierini: clinical and histopathological findings and antibodies to Borrelia burgdorferi in thirty-four patients . J Am Acad Dermatol. 1994;;30:441-446.

Figures

Tables

Interactive Graphics

Video

Country-Specific Mortality and Growth Failure in Infancy and Yound Children and Association With Material Stature

Use interactive graphics and maps to view and sort country-specific infant and early dhildhood mortality and growth failure data and their association with maternal

1 +
Wiedemann HR, Burgio GR, Aldenhoff P, Kunze J, Kaufmann HJ, Schirg E.  The Proteus syndrome: partial gigantism of the hands and/or feet, nevi, hemihypertrophy. subcutaneous tumors, macrocephaly or other skull anomalies and possible accerelated growth and visceral affections . Eur J Pediatr. 1983;;140: 5-12.
2 +
Clark RD, Donnai D, Rogers J, Cooper J, Baraitser M.  Proteus syndrome: an expanded phenotype . Am J Med Genet. 1987;;27:99-117.
3 +
Cohen MM Jr.  Understanding Proteus syndrome, unmasking the Elephant Man, and stemming elephant fever . Neurofibromatosis . 1988;;1:260-280.
4 +
Samlaska CP, Levin SW, James WD, Benson PM, Walker JC, Perlik PC.  Proteus syndrome . Arch Dermatol. 1989;;125:1109-1114.
5 +
Happle R.  Mosaicism in human skin: understanding the patterns and mechanisms . Arch Dermatol. 1993;;129:1460-1470.
6 +
Whitehouse HLK. Genetic Recombination: Understanding the Mechanisms . Chichester, England: John Wiley & Sons Ltd; 1982;:214-224.
7 +
Harrison BJ, Carpenter R.  Somatic crossing-over in Antirrhinum majus . Heredity . 1977;:38:169-189.
8 +
Graf U, Würgler FE, Katz AJ, et al.  Somatic mutation and recombination test in Drosophila melanogaster . Environ Mutagen. 1984;:6:153-188.
9 +
Happle R.  Lipomatosis and partial lipohypoplasia in Proteus syndrome: a clinical clue for twin spotting? Am J Med Genet. 1995;;56:332-333.
10 +
Temtamy SA, Rogers JG.  Macrodactyly, hemihypertrophy, and connective tissue nevi: report of a new syndrome and review of the literature . J Pediatr. 1976;;89:924-927.
11 +
Hotamisligil HGS.  Proteus syndrome and hamartoses with overgrowth . Dysmorphol Clin Genet. 1990;;4:87-102.
12 +
Viljoen D, Saxe N, Pearn J, Beighton P.  The cutaneous manifestations of the Klippel-Trenaunay-Weber syndrome . Clin Exp Dermatol. 1987;;12:12-17.
13 +
Goltz RW.  Focal dermal hypoplasia syndrome: an update . Arch Dermatol. 1992;; 128:1108-1111.
14 +
Al-Gazali LI, Donnai D, Berry SA, Say B, Mueller RF.  The oculocerebrocutaneous (Delleman) syndrome . J Med Genet. 1988;:25:773-778.
15 +
Buechner SA, Rufli T.  Atrophodermia of Pasini and Pierini: clinical and histopathological findings and antibodies to Borrelia burgdorferi in thirty-four patients . J Am Acad Dermatol. 1994;;30:441-446.

Correspondence

Submit a Letter
CME Course for:


You need to register in order to view this quiz.


To understand the clinical management of acute heart failure syndromes.
Accreditation Information The American Medical Association is accredited by the Accreditation Council for Continuing Medical Education to provide continuing medical education for physicians.
The AMA designates this journal-based CME activity for a maximum of 1 AMA PRA Category 1 CreditTM per course. Physicians should claim only the credit commensurate with the extent of their participation in the activity.
Physicians who complete the CME course and score at least 80% correct on the quiz are eligible for AMA PRA Category 1 CreditTM.
Note: You must get at least of the answers correct to pass this quiz.
Note: You must get at least of the answers correct to pass this quiz.
You have not filled in all the answers to complete this quiz
The following questions were not answered:
Sorry, you have unsuccessfully completed this CME quiz with a score of
The following questions were not answered correctly:
For CME Course: A Proposed Model for Initial Assessment and Management of Acute Heart Failure Syndromes
Indicate what changes(s) you will implement in your practice, if any, based on this CME course.
To view and print your certificate and access a summary of your CME courses go to My CME.
NOTE:
Citing articles are presented as examples only. In non-demo SCM6 implementation, integration with CrossRef’s “Cited By” API will populate this tab (http://www.crossref.org/citedby.html).
Compression-Only CPR: Pushing the Science Forward
Cone
AAM 2010;304:1493-1495.
All you need to read in the other general journals
BMJ 2010;341:c5893-c1494.
Submit a Comment

Some tools below are only available to our subscribers or users with an online account.

Related Content

Customize your page view by dragging & repositioning the boxes below.

© 2012 American Medical Association. All Rights Reserved.
Powered bySilverchair Information Systems