Extracranial Vascular Anomalies Driven by RAS/MAPK Variants: Spectrum and Genotype–Phenotype Correlations

Author:

Schmidt Vanessa F.12ORCID,Kapp Friedrich G.3ORCID,Goldann Constantin4ORCID,Huthmann Linda4,Cucuruz Beatrix4,Brill Richard4ORCID,Vielsmeier Veronika5,Seebauer Caroline T.5,Michel Armin‐Johannes6ORCID,Seidensticker Max12ORCID,Uller Wibke7ORCID,Weiß Jakob B. W.8,Sint Alena12,Häberle Beate29,Haehl Julia29ORCID,Wagner Alexandra29ORCID,Cordes Johanna3,Holm Annegret3ORCID,Schanze Denny10ORCID,Ricke Jens12,Kimm Melanie A.12ORCID,Wohlgemuth Walter A.4,Zenker Martin10,Wildgruber Moritz12ORCID,

Affiliation:

1. Department of Radiology LMU University Hospital, LMU Munich München Germany

2. Interdisziplinäres Zentrum für Gefäßanomalien (IZGA) LMU University Hospital, LMU Munich München Germany

3. Division of Pediatric Hematology and Oncology, Department of Pediatric and Adolescent Medicine University Medical Center Freiburg, University of Freiburg Germany

4. Clinic and Policlinic of Radiology Martin‐Luther University Halle‐Wittenberg Halle (Saale) Germany

5. Department of Otorhinolaryngology Regensburg University Medical Center Regensburg Germany

6. Department of Pediatric and Adolescent Surgery Paracelsus Medical University Hospital Salzburg Austria

7. Department of Diagnostic and Interventional Radiology University of Freiburg Medical Centre, Medical Faculty of the University of Freiburg Freiburg Germany

8. Department of Plastic and Hand Surgery University of Freiburg Medical Centre, Medical Faculty of the University of Freiburg Freiburg Germany

9. Department of Pediatric Surgery, Dr. von Hauner Children’s Hospital LMU University Hospital, LMU Munich München Germany

10. Institute of Human Genetics, University Hospital Magdeburg Magdeburg Germany

Abstract

Background We aimed to correlate alterations in the rat sarcoma virus (RAS)/mitogen‐activated protein kinase pathway in vascular anomalies to the clinical phenotype for improved patient and treatment stratification. Methods and Results This retrospective multicenter cohort study included 29 patients with extracranial vascular anomalies containing mosaic pathogenic variants (PVs) in genes of the RAS/mitogen‐activated protein kinase pathway. Tissue samples were collected during invasive treatment or clinically indicated biopsies. PVs were detected by the targeted sequencing of panels of genes known to be associated with vascular anomalies, performed using DNA from affected tissue. Subgroup analyses were performed according to the affected genes with regard to phenotypic characteristics in a descriptive manner. Twenty‐five vascular malformations, 3 vascular tumors, and 1 patient with both a vascular malformation and vascular tumor presented the following distribution of PVs in genes: Kirsten rat sarcoma viral oncogene (n=10), neuroblastoma ras viral oncogene homolog (n=1), Harvey rat sarcoma viral oncogene homolog (n=5), V‐Raf murine sarcoma viral oncogene homolog B (n=8), and mitogen‐activated protein kinase kinase 1 (n=5). Patients with RAS PVs had advanced disease stages according to the Schobinger classification (stage 3–4: RAS , 9/13 versus non‐ RAS , 3/11) and more frequent progression after treatment ( RAS , 10/13 versus non‐ RAS , 2/11). Lesions with Kirsten rat sarcoma viral oncogene PVs infiltrated more tissue layers compared with the other PVs including other RAS PVs (multiple tissue layers: Kirsten rat sarcoma viral oncogene, 8/10 versus other PVs, 6/19). Conclusions This comparison of patients with various PVs in genes of the RAS/MAPK pathway provides potential associations with certain morphological and clinical phenotypes. RAS variants were associated with more aggressive phenotypes, generating preliminary data and hypothesis for future larger studies.

Publisher

Ovid Technologies (Wolters Kluwer Health)

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