TY - JOUR AU - Luciana Teofili, AU - Fiorina Giona, AU - Lorenza Torti, AU - Tonia Cenci, AU - Bianca Maria Ricerca, AU - Carlo Rumi, AU - Vittorio Nunes, AU - Robin FoĆ , AU - Giuseppe Leone, AU - Maurizio Martini, AU - Luigi Maria Larocca, PY - 2010/01/11 Y2 - 2024/03/28 TI - Hereditary thrombocytosis caused by MPLSer505Asn is associated with a high thrombotic risk, splenomegaly and progression to bone marrow fibrosis JF - Haematologica JA - haematol VL - 95 IS - 1 SE - Articles DO - 10.3324/haematol.2009.007542 UR - https://haematologica.org/article/view/5478 SP - 65-70 AB - Background The MPLSer505Asn mutation has been reported to be a cause of hereditary thrombocythemia. Recently, we detected this mutation in a large proportion of children with familial thrombocythemia, suggesting that in Italy the incidence of MPLSer505Asn mutation could be underestimated.Design and Methods We extended the search for this mutation to all patients with essential thrombocythemia who had a positive family history for thrombocytosis or essential thrombocythemia. We identified eight Italian families positive for the MPLSer505Asn mutation. Clinical and hematologic data were available for members of seven families, including 21 patients with a proven mutation and 20 relatives with thrombocytosis.Results Fifteen major thrombotic episodes, nine of which were fatal, were recorded among 41 patients. The thrombotic manifestation was stroke in four cases, myocardial infarction in seven cases, fetal loss in two cases, deep vein thrombosis of the leg in one case and Budd Chiari syndrome in one case. Almost all patients over 20 years old had splenomegaly and bone marrow fibrosis, while these were rarely observed in patients under 20 years old, suggesting that these manifestations are associated with aging. Finally, the life expectancy of family members with thrombocytosis was significantly shorter than that of members without thrombocytosis (P=0.003).Conclusions Patients with familial thrombocytosis caused by a MPLSer505Asn mutation have a high risk of thrombosis and, with aging, develop splenomegaly and bone marrow fibrosis, significantly affecting their life expectancy. ER -