CASE REPORT article
Front. Med.
Sec. Dermatology
This article is part of the Research TopicInnovations in Dermatopathology: Emerging Diagnostic Strategies and Molecular BiomarkersView all 6 articles
CYLD Cutaneous Syndrome with Malignant Transformation to Spiradenocarcinoma: Cooperative Effects of CYLD Truncation and an MSH2 Clamp-Domain Variant in an Ecuadorian Patient
Provisionally accepted
Carlos Reyes-Silva1
Gabriela Jaramillo-Koupermann1
Maritza Quishpe1Rosa Pacheco1
Skehirly Burgos-Tapia2
Ana Karina Zambrano3
Alejandro Cabrera-Andrade2*- 1Hospital de Especialidades Eugenio Espejo, Quito, Ecuador
- 2Universidad de Las Americas, Quito, Ecuador
- 3Universidad UTE, Quito, Ecuador
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Background: CYLD cutaneous syndrome (CCS) is a rare autosomal dominant disorder caused by germline CYLD variants and characterized by multiple skin adnexal tumors. Malignant transformation is uncommon, and cooperative genetic events remain poorly defined, particularly in underrepresented populations. Case Presentation: We report a 61-year-old Ecuadorian woman with multiple scalp cylindromas and spiradenomas, including one spiradenocarcinoma. Family history was notable for malignancies in first- and second-degree relatives. Whole-exome sequencing identified a heterozygous nonsense CYLD variant (c.1207C>T; p.Gln403Ter), classified as likely pathogenic, and a homozygous missense MSH2 variant (c.1609A>G; p.Lys537Glu) of uncertain significance. Histopathology confirmed malignant transformation, while immunohistochemistry showed preserved MSH2 expression with a microsatellite-stable phenotype. Nevertheless, a functional impact of the MSH2 variant cannot be excluded. Consistent with these observations, in silico modeling demonstrated that CYLD truncation eliminates the catalytic USP domain and regulatory motifs, abolishing deubiquitinase activity, whereas the MSH2 substitution affects a conserved residue in the clamp domain, likely destabilizing the MSH2–MSH6 complex despite intact nuclear localization. Conclusion: This is the first genetically confirmed case of CCS in Ecuador and among the few reported in South America. Beyond expanding the geographic spectrum, our findings highlight the value of integrating genomic and protein analyses to uncover cooperative mechanisms of malignant progression. Such integrative genomic approaches refine diagnosis, enhance genotype–phenotype interpretation, and deepen understanding of malignant transformation in CCS, particularly in underrepresented populations.
Keywords: CYLD cutaneous syndrome1, CYLD3, dermatologic neoplasm6, Ecuador8, mismatchrepair5, MSH24, rare genetic disorders7, spiradenocarcinoma2
Received: 12 Sep 2025; Accepted: 20 Jan 2026.
Copyright: © 2026 Reyes-Silva, Jaramillo-Koupermann, Quishpe, Pacheco, Burgos-Tapia, Zambrano and Cabrera-Andrade. This is an open-access article distributed under the terms of the Creative Commons Attribution License (CC BY). The use, distribution or reproduction in other forums is permitted, provided the original author(s) or licensor are credited and that the original publication in this journal is cited, in accordance with accepted academic practice. No use, distribution or reproduction is permitted which does not comply with these terms.
* Correspondence: Alejandro Cabrera-Andrade
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