Frontiers in Immunology (Sep 2022)

A catalog of the genetic causes of hereditary angioedema in the Canary Islands (Spain)

  • Alejandro Mendoza-Alvarez,
  • Eva Tosco-Herrera,
  • Adrian Muñoz-Barrera,
  • Luis A. Rubio-Rodríguez,
  • Aitana Alonso-Gonzalez,
  • Aitana Alonso-Gonzalez,
  • Almudena Corrales,
  • Almudena Corrales,
  • Antonio Iñigo-Campos,
  • Lourdes Almeida-Quintana,
  • Elena Martin-Fernandez,
  • Dara Martinez-Beltran,
  • Eva Perez-Rodriguez,
  • Ariel Callero,
  • Jose C. Garcia-Robaina,
  • Rafaela González-Montelongo,
  • Itahisa Marcelino-Rodriguez,
  • Itahisa Marcelino-Rodriguez,
  • Jose M. Lorenzo-Salazar,
  • Carlos Flores,
  • Carlos Flores,
  • Carlos Flores,
  • Carlos Flores

DOI
https://doi.org/10.3389/fimmu.2022.997148
Journal volume & issue
Vol. 13

Abstract

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Hereditary angioedema (HAE) is a rare disease where known causes involve C1 inhibitor dysfunction or dysregulation of the kinin cascade. The updated HAE management guidelines recommend performing genetic tests to reach a precise diagnosis. Unfortunately, genetic tests are still uncommon in the diagnosis routine. Here, we characterized for the first time the genetic causes of HAE in affected families from the Canary Islands (Spain). Whole-exome sequencing data was obtained from 41 affected patients and unaffected relatives from 29 unrelated families identified in the archipelago. The Hereditary Angioedema Database Annotation (HADA) tool was used for pathogenicity classification and causal variant prioritization among the genes known to cause HAE. Manual reclassification of prioritized variants was used in those families lacking known causal variants. We detected a total of eight different variants causing HAE in this patient series, affecting essentially SERPING1 and F12 genes, one of them being a novel SERPING1 variant (c.686-12A>G) with a predicted splicing effect which was reclassified as likely pathogenic in one family. Altogether, the diagnostic yield by assessing previously reported causal genes and considering variant reclassifications according to the American College of Medical Genetics guidelines reached 66.7% (95% Confidence Interval [CI]: 30.1-91.0) in families with more than one affected member and 10.0% (95% CI: 1.8-33.1) among cases without family information for the disease. Despite the genetic causes of many patients remain to be identified, our results reinforce the need of genetic tests as first-tier diagnostic tool in this disease, as recommended by the international WAO/EAACI guidelines for the management of HAE.

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