Syndromic epidermal differentiation disorders: a new classification toward pathogenesis-based therapy

Amy S Paller; Joyce Teng; Juliette Mazereeuw-Hautier; Ángela Hernández-Martín; Céline Granier Tournier; Alain Hovnanian; Mandy Aldwin-Easton; Gianluca Tadini; Schwartz Janice; Eli Sprecher; Kiril Malovitski; Akemi Ishida-Yamamoto; Keith Choate; Masashi Akiyama; Edel A O'Toole; Judith Fischer; Christine Bodemer; Antoni Gostynski; Matthias Schmuth

doi:10.1093/bjd/ljaf123

Syndromic epidermal differentiation disorders: a new classification toward pathogenesis-based therapy

Amy S Paller
, Joyce Teng
, Juliette Mazereeuw-Hautier
, Ángela Hernández-Martín
, Céline Granier Tournier
, Alain Hovnanian
, Mandy Aldwin-Easton
, Gianluca Tadini
, Schwartz Janice
, Eli Sprecher
, Kiril Malovitski
, Akemi Ishida-Yamamoto
, Keith Choate
, Masashi Akiyama
, Edel A O'Toole
, Judith Fischer
, Christine Bodemer
, Antoni Gostynski
, Matthias Schmuth^*

^*Corresponding author for this work

Research output: Contribution to journal › Article › Academic › peer-review

Abstract

Since the 2010 classification of ichthyoses, our understanding of hereditary epidermal differentiation disorders (EDDs) has markedly increased, allowing for consideration of new therapeutic targets based on disease pathogenesis. A new gene- and protein product function-based classification focuses on shared mechanisms of disease pathogenesis, with the possibility that grouped disorders may respond similarly to new therapeutics. These EDDs have been subdivided into syndromic (sEDD), nonsyndromic with features limited to skin and appendages, and predominantly palmoplantar skin involvement (nonsyndromic and syndromic). sEDDs have clinically important extracutaneous features related to the gene alteration. Often, recognition based on skin manifestations facilitates early gene-based diagnosis, discussion of prognosis, genetic counselling and the initiation of therapy. All sEDDs are rare; the most common are STS-sEDD (formerly known as X-linked ichthyosis) and SPINK5-sEDD (formerly known as Netherton syndrome). Given the rarity, frequent association with early demise and variable clinical features of sEDDs, the natural history of the diseases with advancing age and genotype-phenotype relationships are poorly defined. Of the 51 sEDDs, associated neurological (n = 36; 71%) and/or ophthalmological (n = 25; 49%) findings are most common, and 39% (n = 20) have associated hair abnormalities. The widespread use of topical lovastatin for cholesterol synthesis-related sEDDs represents the prototype of pathogenesis-based therapy. This concept of upstream inhibition to prevent metabolite accumulation and supplementation with the pathway end product potentially applies to other sEDDs, such as those affecting ceramide synthesis and transport. Topical or systemically administered inhibition of activated pathways is another potential approach, exemplified by the emerging treatment of SPINK5-sEDD with kallikrein inhibitors. Many sEDDs may be amenable to gene editing or the introduction of functional cDNA. However, even systemic treatments targeting cutaneous diseases may not address extracutaneous manifestations that arise during embryological development.

Original language	English
Pages (from-to)	592-618
Number of pages	27
Journal	British Journal of Dermatology
Volume	193
Issue number	4
Early online date	4 Apr 2025
DOIs	https://doi.org/10.1093/bjd/ljaf123
Publication status	Published - 18 Sept 2025

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Paller, A. S., Teng, J., Mazereeuw-Hautier, J., Hernández-Martín, Á., Tournier, C. G., Hovnanian, A., Aldwin-Easton, M., Tadini, G., Janice, S., Sprecher, E., Malovitski, K., Ishida-Yamamoto, A., Choate, K., Akiyama, M., O'Toole, E. A., Fischer, J., Bodemer, C., Gostynski, A., & Schmuth, M. (2025). Syndromic epidermal differentiation disorders: a new classification toward pathogenesis-based therapy. British Journal of Dermatology, 193(4), 592-618. https://doi.org/10.1093/bjd/ljaf123

@article{6d9bf8f2e50d494f8e9310592baba8cd,

title = "Syndromic epidermal differentiation disorders: a new classification toward pathogenesis-based therapy",

abstract = "Since the 2010 classification of ichthyoses, our understanding of hereditary epidermal differentiation disorders (EDDs) has markedly increased, allowing for consideration of new therapeutic targets based on disease pathogenesis. A new gene- and protein product function-based classification focuses on shared mechanisms of disease pathogenesis, with the possibility that grouped disorders may respond similarly to new therapeutics. These EDDs have been subdivided into syndromic (sEDD), nonsyndromic with features limited to skin and appendages, and predominantly palmoplantar skin involvement (nonsyndromic and syndromic). sEDDs have clinically important extracutaneous features related to the gene alteration. Often, recognition based on skin manifestations facilitates early gene-based diagnosis, discussion of prognosis, genetic counselling and the initiation of therapy. All sEDDs are rare; the most common are STS-sEDD (formerly known as X-linked ichthyosis) and SPINK5-sEDD (formerly known as Netherton syndrome). Given the rarity, frequent association with early demise and variable clinical features of sEDDs, the natural history of the diseases with advancing age and genotype-phenotype relationships are poorly defined. Of the 51 sEDDs, associated neurological (n = 36; 71\%) and/or ophthalmological (n = 25; 49\%) findings are most common, and 39\% (n = 20) have associated hair abnormalities. The widespread use of topical lovastatin for cholesterol synthesis-related sEDDs represents the prototype of pathogenesis-based therapy. This concept of upstream inhibition to prevent metabolite accumulation and supplementation with the pathway end product potentially applies to other sEDDs, such as those affecting ceramide synthesis and transport. Topical or systemically administered inhibition of activated pathways is another potential approach, exemplified by the emerging treatment of SPINK5-sEDD with kallikrein inhibitors. Many sEDDs may be amenable to gene editing or the introduction of functional cDNA. However, even systemic treatments targeting cutaneous diseases may not address extracutaneous manifestations that arise during embryological development.",

author = "Paller, \{Amy S\} and Joyce Teng and Juliette Mazereeuw-Hautier and {\'A}ngela Hern{\'a}ndez-Mart{\'i}n and Tournier, \{C{\'e}line Granier\} and Alain Hovnanian and Mandy Aldwin-Easton and Gianluca Tadini and Schwartz Janice and Eli Sprecher and Kiril Malovitski and Akemi Ishida-Yamamoto and Keith Choate and Masashi Akiyama and O'Toole, \{Edel A\} and Judith Fischer and Christine Bodemer and Antoni Gostynski and Matthias Schmuth",

year = "2025",

month = sep,

day = "18",

doi = "10.1093/bjd/ljaf123",

language = "English",

volume = "193",

pages = "592--618",

journal = "British Journal of Dermatology",

issn = "0007-0963",

publisher = "Oxford University Press",

number = "4",

}

Paller, AS, Teng, J, Mazereeuw-Hautier, J, Hernández-Martín, Á, Tournier, CG, Hovnanian, A, Aldwin-Easton, M, Tadini, G, Janice, S, Sprecher, E, Malovitski, K, Ishida-Yamamoto, A, Choate, K, Akiyama, M, O'Toole, EA, Fischer, J, Bodemer, C, Gostynski, A & Schmuth, M 2025, 'Syndromic epidermal differentiation disorders: a new classification toward pathogenesis-based therapy', British Journal of Dermatology, vol. 193, no. 4, pp. 592-618. https://doi.org/10.1093/bjd/ljaf123

TY - JOUR

T1 - Syndromic epidermal differentiation disorders

T2 - a new classification toward pathogenesis-based therapy

AU - Paller, Amy S

AU - Teng, Joyce

AU - Mazereeuw-Hautier, Juliette

AU - Hernández-Martín, Ángela

AU - Tournier, Céline Granier

AU - Hovnanian, Alain

AU - Aldwin-Easton, Mandy

AU - Tadini, Gianluca

AU - Janice, Schwartz

AU - Sprecher, Eli

AU - Malovitski, Kiril

AU - Ishida-Yamamoto, Akemi

AU - Choate, Keith

AU - Akiyama, Masashi

AU - O'Toole, Edel A

AU - Fischer, Judith

AU - Bodemer, Christine

AU - Gostynski, Antoni

AU - Schmuth, Matthias

PY - 2025/9/18

Y1 - 2025/9/18

N2 - Since the 2010 classification of ichthyoses, our understanding of hereditary epidermal differentiation disorders (EDDs) has markedly increased, allowing for consideration of new therapeutic targets based on disease pathogenesis. A new gene- and protein product function-based classification focuses on shared mechanisms of disease pathogenesis, with the possibility that grouped disorders may respond similarly to new therapeutics. These EDDs have been subdivided into syndromic (sEDD), nonsyndromic with features limited to skin and appendages, and predominantly palmoplantar skin involvement (nonsyndromic and syndromic). sEDDs have clinically important extracutaneous features related to the gene alteration. Often, recognition based on skin manifestations facilitates early gene-based diagnosis, discussion of prognosis, genetic counselling and the initiation of therapy. All sEDDs are rare; the most common are STS-sEDD (formerly known as X-linked ichthyosis) and SPINK5-sEDD (formerly known as Netherton syndrome). Given the rarity, frequent association with early demise and variable clinical features of sEDDs, the natural history of the diseases with advancing age and genotype-phenotype relationships are poorly defined. Of the 51 sEDDs, associated neurological (n = 36; 71%) and/or ophthalmological (n = 25; 49%) findings are most common, and 39% (n = 20) have associated hair abnormalities. The widespread use of topical lovastatin for cholesterol synthesis-related sEDDs represents the prototype of pathogenesis-based therapy. This concept of upstream inhibition to prevent metabolite accumulation and supplementation with the pathway end product potentially applies to other sEDDs, such as those affecting ceramide synthesis and transport. Topical or systemically administered inhibition of activated pathways is another potential approach, exemplified by the emerging treatment of SPINK5-sEDD with kallikrein inhibitors. Many sEDDs may be amenable to gene editing or the introduction of functional cDNA. However, even systemic treatments targeting cutaneous diseases may not address extracutaneous manifestations that arise during embryological development.

AB - Since the 2010 classification of ichthyoses, our understanding of hereditary epidermal differentiation disorders (EDDs) has markedly increased, allowing for consideration of new therapeutic targets based on disease pathogenesis. A new gene- and protein product function-based classification focuses on shared mechanisms of disease pathogenesis, with the possibility that grouped disorders may respond similarly to new therapeutics. These EDDs have been subdivided into syndromic (sEDD), nonsyndromic with features limited to skin and appendages, and predominantly palmoplantar skin involvement (nonsyndromic and syndromic). sEDDs have clinically important extracutaneous features related to the gene alteration. Often, recognition based on skin manifestations facilitates early gene-based diagnosis, discussion of prognosis, genetic counselling and the initiation of therapy. All sEDDs are rare; the most common are STS-sEDD (formerly known as X-linked ichthyosis) and SPINK5-sEDD (formerly known as Netherton syndrome). Given the rarity, frequent association with early demise and variable clinical features of sEDDs, the natural history of the diseases with advancing age and genotype-phenotype relationships are poorly defined. Of the 51 sEDDs, associated neurological (n = 36; 71%) and/or ophthalmological (n = 25; 49%) findings are most common, and 39% (n = 20) have associated hair abnormalities. The widespread use of topical lovastatin for cholesterol synthesis-related sEDDs represents the prototype of pathogenesis-based therapy. This concept of upstream inhibition to prevent metabolite accumulation and supplementation with the pathway end product potentially applies to other sEDDs, such as those affecting ceramide synthesis and transport. Topical or systemically administered inhibition of activated pathways is another potential approach, exemplified by the emerging treatment of SPINK5-sEDD with kallikrein inhibitors. Many sEDDs may be amenable to gene editing or the introduction of functional cDNA. However, even systemic treatments targeting cutaneous diseases may not address extracutaneous manifestations that arise during embryological development.

U2 - 10.1093/bjd/ljaf123

DO - 10.1093/bjd/ljaf123

M3 - Article

SN - 0007-0963

VL - 193

SP - 592

EP - 618

JO - British Journal of Dermatology

JF - British Journal of Dermatology

IS - 4

ER -

Syndromic epidermal differentiation disorders: a new classification toward pathogenesis-based therapy

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