TY - JOUR
T1 - Molecular Genetics and Interferon Signature in the Italian Aicardi Goutières Syndrome Cohort: Report of 12 New Cases and Literature Review
AU - Garau, Jessica
AU - Cavallera, Vanessa
AU - Valente, Marialuisa
AU - Tonduti, Davide
AU - Sproviero, Daisy
AU - Zucca, Susanna
AU - Battaglia, Domenica Immacolata
AU - Battini, Roberta
AU - Bertini, Enrico
AU - Bertini, Enrico Silvio
AU - Cappanera, Silvia
AU - Chiapparini, Luisa
AU - Crasà, Camilla
AU - Crichiutti, Giovanni
AU - Giustina, Elvio Dalla
AU - D’Arrigo, Stefano
AU - De Giorgis, Valentina
AU - De Simone, Micaela
AU - Galli, Jessica
AU - La Piana, Roberta
AU - Messana, Tullio
AU - Moroni, Isabella
AU - Nardocci, Nardo
AU - Panteghini, Celeste
AU - Parazzini, Cecilia
AU - Pichiecchio, Anna
AU - Pini, Antonella
AU - Ricci, Federica
AU - Saletti, Veronica
AU - Salvatici, Elisabetta
AU - Santorelli, Filippo M.
AU - Sartori, Stefano
AU - Tinelli, Francesca
AU - Uggetti, Carla
AU - Veneselli, Edvige
AU - Zorzi, Giovanna
AU - Garavaglia, Barbara
AU - Fazzi, Elisa
AU - Orcesi, Simona
AU - Cereda, Cristina
PY - 2019
Y1 - 2019
N2 - Aicardi-Goutieres syndrome (AGS) is a genetically determined early onset encephalopathy characterized by cerebral calcification, leukodystrophy, and increased expression of interferon-stimulated genes (ISGs). Up to now, seven genes (TREX1, RNASEH2B, RNASEH2C, RNASEH2A, ADAR1, SAMHD1, IFIH1) have been associated with an AGS phenotype. Next Generation Sequencing (NGS) analysis was performed on 51 AGS patients and interferon signature (IS) was investigated in 18 AGS patients and 31 healthy controls. NGS identified mutations in 48 of 51 subjects, with three patients demonstrating a typical AGS phenotype but not carrying mutations in known AGS-related genes. Five mutations, in RNASEH2B, SAMHD1 and IFIH1 gene, were not previously reported. Eleven patients were positive and seven negatives for the upregulation of interferon signaling (IS > 2.216). This work presents, for the first time, the genetic data of an Italian cohort of AGS patients, with a higher percentage of mutations in RNASEH2B and a lower frequency of mutations in TREX1 than those seen in international series. RNASEH2B mutated patients showed a prevalence of negative IS consistent with data reported in the literature. We also identified five novel pathogenic mutations that warrant further functional investigation. Exome/genome sequencing will be performed in future studies in patients without a mutation in AGS-related genes.
AB - Aicardi-Goutieres syndrome (AGS) is a genetically determined early onset encephalopathy characterized by cerebral calcification, leukodystrophy, and increased expression of interferon-stimulated genes (ISGs). Up to now, seven genes (TREX1, RNASEH2B, RNASEH2C, RNASEH2A, ADAR1, SAMHD1, IFIH1) have been associated with an AGS phenotype. Next Generation Sequencing (NGS) analysis was performed on 51 AGS patients and interferon signature (IS) was investigated in 18 AGS patients and 31 healthy controls. NGS identified mutations in 48 of 51 subjects, with three patients demonstrating a typical AGS phenotype but not carrying mutations in known AGS-related genes. Five mutations, in RNASEH2B, SAMHD1 and IFIH1 gene, were not previously reported. Eleven patients were positive and seven negatives for the upregulation of interferon signaling (IS > 2.216). This work presents, for the first time, the genetic data of an Italian cohort of AGS patients, with a higher percentage of mutations in RNASEH2B and a lower frequency of mutations in TREX1 than those seen in international series. RNASEH2B mutated patients showed a prevalence of negative IS consistent with data reported in the literature. We also identified five novel pathogenic mutations that warrant further functional investigation. Exome/genome sequencing will be performed in future studies in patients without a mutation in AGS-related genes.
KW - Aicardi-Goutieres Syndrome
KW - Interferon signature
KW - Next Generation Sequencing
KW - Aicardi-Goutieres Syndrome
KW - Interferon signature
KW - Next Generation Sequencing
UR - http://hdl.handle.net/10807/161719
U2 - 10.3390/jcm8050750
DO - 10.3390/jcm8050750
M3 - Article
SN - 2077-0383
VL - 8
SP - 750-N/A
JO - Journal of Clinical Medicine
JF - Journal of Clinical Medicine
ER -