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Significant association between FGFR1 mutation frequency and age in central giant cell granuloma

Stefania Niada, Andrea Varazzani, Chiara Giannasi, Nicola Fusco, Elisabetta Armiraglio, Andrea Di Bernardo, Alessandro Cherchi, Alessandro Bai, Domenico Corradi, Alessandro Tafuni, Antonina Parafioriti, Stefano Ferrero, Andrea Edoardo Bianchi, Aldo Bruno Gianni, Tito Poli, Farida Latif, Teresa Brini

Pathology(2023)

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Abstract
Central giant cell granulomas (CGCG) are rare intra-osseous osteolytic lesions of uncertain aetiology. Despite the benign nature of this neoplasia, the lesions can rapidly grow and become large, painful, invasive, and destructive. The identification of molecular drivers could help in the selection of targeted therapies for specific cases. TRPV4, KRAS and FGFR1 mutations have been associated with these lesions but no correlation between the mutations and patient features was observed so far. In this study, we analysed 17 CGCG cases of an Italian cohort and identified an interesting and significant (p=0.0021) correlation between FGFR1 mutations and age. In detail, FGFR1 mutations were observed frequently and exclusively in CGCG from young (<18 years old) pa-tients (4/5 lesions, 80%). Furthermore, the combination between ours and previously published data confirmed a significant difference in the frequency of FGFR1 mutations in CGCG from patients younger than 18 years at the time of diagnosis (9/23 lesions, 39%) when compared to older patients (1/31 lesions, 0.03%; p=0.0011), thus corrobo-rating our observation in a cohort of 54 patients. FGFR1 variants in young CGCG patients could favour fast lesion growth, implying that they seek medical attention earlier. Our observation might help prioritise candidates for FGFR1 testing, thus opening treatment options with FGFR inhibitors.
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Key words
Central giant cell granuloma,FGFR1,mutation frequency,age
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