Interpreting genetic variants in complex genes such as PIEZO1 is challenging because of marked allelic heterogeneity, relative tolerance to missense variation, and overlapping clinical phenotypes. Gain-of-function variants in PIEZO1 cause dehydrated hereditary stomatocytosis (DHS1, or hereditary xerocytosis), a pleiotropic syndrome characterized by anemia of variable severity and iron overload. Herein, we provided and applied an integrative framework combining ACMG guidelines, quantitative in silico predictions, structural domain annotation, and detailed patient phenotyping to classify 2565 PIEZO1 variants. A Bayesian scoring system with weighted evidence and a composite predictive score enabled reclassification of nearly 1,000 variants of uncertain significance and highlighted non-random clustering of pathogenic variants in functionally constrained domains, particularly Anchor, Inner helix, and C-terminal domains. Genotype-phenotype correlation analysis in 176 in-house DHS cases identified three phenotypic clusters, ranging from classic DHS1 with severe hemolysis and iron overload to atypical or subclinical presentations, reflecting domain-specific pathogenic mechanisms. Overall, this reclassification of PIEZO1 variants, integrated with genotype-phenotype correlation analysis, improves diagnostic precision, supports genotype-guided patient management, and underscores the value of integrating structural and clinical data in rare variant interpretation.
Refined classification and phenotype-driven analysis of PIEZO1 variants in hereditary red cell and iron disorders / Rosato, Barbara Eleni; Marra, Roberta; Martone, Stefania; Manno, Mariangela; Dionisi, Manuela; Ribersani, Michela; Pinto, Valeria Maria; Forni, Gian Luca; Balocco, Manuela; Carrara, Paola; Lamagna, Martina; Morisco, Filomena; Guarino, Maria; Cossiga, Valentina; Barbato, Antonio; Arcioni, Francesco; Iolascon, Achille; Russo, Roberta; Andolfo, Immacolata. - In: BLOOD. - ISSN 0006-4971. - (2026). [10.1182/blood.2025031632]
Refined classification and phenotype-driven analysis of PIEZO1 variants in hereditary red cell and iron disorders
Rosato, Barbara Eleni
Primo
;Marra, RobertaSecondo
;Martone, Stefania;Lamagna, Martina;Morisco, Filomena;Guarino, Maria;Cossiga, Valentina;Barbato, Antonio;Iolascon, Achille;Russo, Roberta
;Andolfo, ImmacolataUltimo
2026
Abstract
Interpreting genetic variants in complex genes such as PIEZO1 is challenging because of marked allelic heterogeneity, relative tolerance to missense variation, and overlapping clinical phenotypes. Gain-of-function variants in PIEZO1 cause dehydrated hereditary stomatocytosis (DHS1, or hereditary xerocytosis), a pleiotropic syndrome characterized by anemia of variable severity and iron overload. Herein, we provided and applied an integrative framework combining ACMG guidelines, quantitative in silico predictions, structural domain annotation, and detailed patient phenotyping to classify 2565 PIEZO1 variants. A Bayesian scoring system with weighted evidence and a composite predictive score enabled reclassification of nearly 1,000 variants of uncertain significance and highlighted non-random clustering of pathogenic variants in functionally constrained domains, particularly Anchor, Inner helix, and C-terminal domains. Genotype-phenotype correlation analysis in 176 in-house DHS cases identified three phenotypic clusters, ranging from classic DHS1 with severe hemolysis and iron overload to atypical or subclinical presentations, reflecting domain-specific pathogenic mechanisms. Overall, this reclassification of PIEZO1 variants, integrated with genotype-phenotype correlation analysis, improves diagnostic precision, supports genotype-guided patient management, and underscores the value of integrating structural and clinical data in rare variant interpretation.I documenti in IRIS sono protetti da copyright e tutti i diritti sono riservati, salvo diversa indicazione.
