Frontiers in Pediatrics (Mar 2023)

Case report: De novo SAMD9L truncation causes neonatal-onset autoinflammatory syndrome which was successfully treated with hematopoietic stem cell transplantation

  • María Soledad Caldirola,
  • María Soledad Caldirola,
  • Analía Gisela Seminario,
  • Analía Gisela Seminario,
  • Paula Carolina Luna,
  • Renata Curciarello,
  • Guillermo Horacio Docena,
  • Nicolás Fernandez Escobar,
  • Guillermo Drelichman,
  • Marco Gattorno,
  • Adriana A. de Jesus,
  • Raphaela Goldbach-Mansky,
  • María Isabel Gaillard,
  • María Isabel Gaillard,
  • Liliana Bezrodnik

DOI
https://doi.org/10.3389/fped.2023.1108207
Journal volume & issue
Vol. 11

Abstract

Read online

During recent years, the identification of monogenic mutations that cause sterile inflammation has expanded the spectrum of autoinflammatory diseases, clinical disorders characterized by uncontrolled systemic and organ-specific inflammation that, in some cases, can mirror infectious conditions. Early studies support the concept of innate immune dysregulation with a predominance of myeloid effector cell dysregulation, particularly neutrophils and macrophages, in causing tissue inflammation. However, recent discoveries have shown a complex overlap of features of autoinflammation and/or immunodeficiency contributing to severe disease phenotypes. Here, we describe the first Argentine patient with a newly described frameshift mutation in SAMD9L c.2666delT/p.F889Sfs*2 presenting with a complex phenotypic overlap of CANDLE-like features and severe infection-induced cytopenia and immunodeficiency. The patient underwent a fully matched unrelated HSCT and has since been in inflammatory remission 5 years post-HSCT.

Keywords