Twelve Variants Polygenic Score for Low-Density Lipoprotein Cholesterol Distribution in a Large Cohort of Patients With Clinically Diagnosed Familial Hypercholesterolemia With or Without Causative Mutations.

Elena Olmastroni,Fabio Fimiani,Anna Rita Roscini,Sergio D’Addato,Francesco Cipollone,Maria Cinquegrani,Vincenzo D’Ambrosio,Andrea Bartuli,Sebastiano Calandra,Anna Laura Cremonini,Patrizia Suppressa,Emanuele Alberto Negri,Chiara Trenti,Pierandrea Vinci,Sabina Zambon,Claudio Borghi,Cristina Pederiva,Andrea Benso,Francesco Baratta,Lorenzo Iughetti,Liliana Grigore,Gianni Biolo,Livia Pisciotta,Elena Sani,Roberto Scicali,Marta Gazzotti,Stefano Bertolini,Giancarla Meregalli,Gabriella Iannuzzo,Alessia Di Costanzo,Manuela Casula,Fabio Nascimbeni,Ornella Guardamagna,Chiara Di Pentima,Giovanni Battista Vigna,Rossella Marcucci,Patrizia Tarugi,Paola Sabrina Buonuomo,Giuliana Mombelli,Fabio Pellegatta,Claudio Ferri,Maria Elena Capra,Ilenia Minicocci,Lorenzo Maroni,Antonio Pujia,Simona Moffa,Maria Del Ben,Graziana Lupattelli,Elena Repetti,Arcangelo Iannuzzi,Francesco Purrello,Giulia Massini,Marco Bucci,Alon Schaffer,Nadia Citroni,Enzo Manzato,Chiara Pavanello,Iris Cardolini,Giuseppe Mandraffino,Davide Baldera,Katia Bonomo,Maurizio Averna,Rossella Spina,Guglielmo Beccuti,Giacomo Biasucci,Riccardo Sarzani,Emanuela Colombo,Sandro Muntoni,Lucia Prati,Omar Ghirardello,Tiziana Montalcini,Valerio Pecchioli,Massimo Federici,Maria Grazia Zenti,Betti Giusti,Paolo Calabrò,Patrizia Bruzzi,Giuliana Fortunato,Andrea Giaccari,Francesca Carubbi,Ada Cutolo,Giuseppe Banderali,Marco Gentile,Carlo Sabbà,Sandra Bertocco,Giuseppe De Corrado,Elena Tragni,Marcello Arca,Alessandro Lupi,Angela Pirillo,Adriana Branchi,Luca Bonanni,Giuseppe Covetti,Antonio Bossi ,A E Pípolo ,Alberico L Catapano ,D Grassi ,A.m Fiorenza ,José Pablo Werba ,Michèle Tedeschi ,Angelo B Cefalù ,V Zampoleri

doi:10.1161/jaha.121.023668

Abstract

BackgroundA significant proportion of individuals clinically diagnosed with familial hypercholesterolemia (FH), but without any disease‐causing mutation, are likely to have polygenic hypercholesterolemia. We evaluated the distribution of a polygenic risk score, consisting of 12 low‐density lipoprotein cholesterol (LDL‐C)‐raising variants (polygenic LDL‐C risk score), in subjects with a clinical diagnosis of FH.Methods and ResultsWithin the Lipid Transport Disorders Italian Genetic Network (LIPIGEN) study, 875 patients who were FH‐mutation positive (women, 54.75%; mean age, 42.47±15.00 years) and 644 patients who were FH‐mutation negative (women, 54.21%; mean age, 49.73±13.54 years) were evaluated. Patients who were FH‐mutation negative had lower mean levels of pretreatment LDL‐C than patients who were FH‐mutation positive (217.14±55.49 versus 270.52±68.59 mg/dL, P<0.0001). The mean value (±SD) of the polygenic LDL‐C risk score was 1.00 (±0.18) in patients who were FH‐mutation negative and 0.94 (±0.20) in patients who were FH‐mutation positive (P<0.0001). In the receiver operating characteristic analysis, the area under the curve for recognizing subjects characterized by polygenic hypercholesterolemia was 0.59 (95% CI, 0.56–0.62), with sensitivity and specificity being 78% and 36%, respectively, at 0.905 as a cutoff value. Higher mean polygenic LDL‐C risk score levels were observed among patients who were FH‐mutation negative having pretreatment LDL‐C levels in the range of 150 to 350 mg/dL (150–249 mg/dL: 1.01 versus 0.91, P<0.0001; 250–349 mg/dL: 1.02 versus 0.95, P=0.0001). A positive correlation between polygenic LDL‐C risk score and pretreatment LDL‐C levels was observed among patients with FH independently of the presence of causative mutations.ConclusionsThis analysis confirms the role of polymorphisms in modulating LDL‐C levels, even in patients with genetically confirmed FH. More data are needed to support the use of the polygenic score in routine clinical practice.

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