Your search keyword '"Michela Cini"' showing total 52 results

51. G20210A Prothrombin Mutation and Critical Limb Ischaemia in Patients with Peripheral Arterial Disease

Author

Cristina Legnani, Elisabetta Favaretto, M. Sartori, E. Conti, G. Palareti, Michela Cini, C. Pili, M. Sartori, E. Favaretto, C. Legnani, M. Cini, E. Conti, C. Pili, and G. Palareti

Subjects

Male, Lower limb artery disease, medicine.medical_specialty, Ischemia, blood/complications/genetics, Prognosis, Prothrombin, Severity of Illness Index, Gastroenterology, genetics, Retrospective Studies, Severity of Illness Index, genetics, Female, Follow-Up Studies, Genetic Predisposition to Disease, Humans, Ischemia, Diabetes mellitus, Internal medicine, Peripheral arterial disease, medicine, Humans, Genetic Predisposition to Disease, Stage (cooking), Aged, Retrospective Studies, blood/etiology/genetics, Leg, Medicine(all), Peripheral Vascular Diseases, Leg, business.industry, Antithrombin, Arterial thrombosis, R506Q FV Leiden, blood supply, Male, Mutation, Peripheral Vascular Disease, DNA, Odds ratio, Prognosis, medicine.disease, Confidence interval, Surgery, Thrombophilic risk factor, Mutation, Aged, DNA, Platelet aggregation inhibitor, Female, Prothrombin, Cardiology and Cardiovascular Medicine, business, Protein C, Follow-Up Studies, medicine.drug, G20210A prothrombin

Abstract

Objectives To assess the possible association between inherited thrombophilic alterations and the severity of peripheral arterial disease (PAD). Design A case-control study. Methods We evaluated the presence of G20210A prothrombin (FII) and R506Q FV Leiden mutations, antithrombin, protein C and S deficiencies in 176 patients with PAD at Fontaine's stage II and in 106 patients with critical limb ischaemia (Fontaine's stage III/IV) consecutively referred to our unit. As control group, we studied 209 apparently healthy subjects. Results The prevalence of G20210A prothrombin mutation was similar in PAD patients and controls (odds ratio (OR): 1.361; 95% confidence interval (CI): 0.552–3.355; p = 0.503 after adjustment for age, sex, smoking and presence of diabetes), but was significantly higher in patients with Fontaine's stage III/IV vs. those with stage II and controls (10.4% vs. 3.4% vs. 4.3%; p = 0.02, respectively). According to a logistic multivariate model that included all patients with PAD, the presence of the FII G20210A mutation (OR: 4.621; 95% CI: 1.548–13.789; p = 0.006) was associated with critical limb ischaemia after adjustment for age, sex, smoking, presence of diabetes and the use of platelet aggregation inhibitors. The prevalence of the other thrombophilic alterations was not different in patients with Fontaine's stage III/IV, in patients with stage II and in controls. Conclusion These hypothesis-generating data suggest that the FII 20210A allele may be considered as a genetic marker predisposing critical ischaemia in patients with PAD, justifying larger longitudinal studies.

52. Baseline thrombophilic alterations and risk of venous thromboembolism in 266 multiple myeloma patients primarily treated with thalidomide and high-dose dexamethasone

Author

Lelia Valdrè, Michela Ceccolini, Antonio Ledda, Affra Carubelli, Claudia Cellini, Michele Cavo, Annamaria Brioli, MC Pallotti, Giulia Perrone, Cristina Legnani, Lucio Catalano, Elisa Favaretto, Paola Tacchetti, Sadia Falcioni, Francesco Casulli, Alessandro Gozzetti, Francesca Patriarca, Michele Baccarani, Elena Zamagni, Luciano Masini, Catello Califano, Patrizia Tosi, Lucia Pantani, Gualtiero Palareti, Michela Cini, and Silvestro Volpe

Subjects

medicine.medical_specialty, Aspirin, business.industry, medicine.drug_class, Immunology, Warfarin, Low molecular weight heparin, Cell Biology, Hematology, medicine.disease, Biochemistry, Gastroenterology, Surgery, Thalidomide, Internal medicine, Relative risk, medicine, Factor V Leiden, Autologous transplantation, cardiovascular diseases, Activated protein C resistance, business, medicine.drug

Abstract

Venous thromboembolism (VTE) has emerged as a major adverse event of primary induction therapy with thalidomide (thal) and dexamethasone (dex) for newly diagnosed multiple myeloma (MM). Aim of the present study was to investigate the relationship between thrombophilic alterations and the risk of VTE in 266 patients who received four months of therapy with thal (200 mg/d) and pulsed high-dose dex in preparation for double autologous transplantation. The rate of VTE in the whole group of patients was 11.6%. The risk of VTE was 26.3% (86.2% patient-years) among the first 19 patients who entered the study and did not received any prophylaxis against thrombosis. The corresponding value among the remaining 247 patients who received thromboprophylaxis with fixed low-dose (1.25 mg/d) warfarin during the four months of thal-dex therapy was 10.6% (35.5% patient-years) (P=0.04). Episodes of VTE occurred at a median of 53 days from the start of thal therapy and, with the exception of 3 patients, were observed after at least a partial response to thal-dex was documented. No VTE events were recorded during the first two months after the end of the induction phase. After VTE occurrence, the majority of patients went on with thal treatment plus full anticoagulation, without evidence of progression of thrombosis. One hundred and ninety patients were evaluated for the presence of thrombophilic alterations at baseline and at the end of thal-dex therapy. The prevalence of factor V Leiden (3.2%) or g20210A prothrombin (2.1%) polymorphism in patients with MM was similar to that observed in 183 healthy controls (3.3%, P= 0.81; 3.8%, P= 0.50, respectively). The relative risk of VTE for patients carrying one of these thrombophilic alterations was 20% compared with 9.4% for patients who lacked both of them (P= 0.58). Reduced protein C and S activities or acquired activated protein C resistance (aAPCR) were recorded at baseline in 11% and 7.4% of MM patients, respectively. Abnormal values at baseline normalized almost completely at the end of treatment. Carriers of aAPCR and/or of reduced levels of natural anticoagulants at baseline did not have a significantly higher risk of VTE compared with normal patients (15.2% vs 9.3%; P=0.49). In conclusion, no significant relationship was found between baseline thrombophilic alterations, including aAPCR, and the risk of thal-related VTE. Prophylaxis with fixed low-dose warfarin was associated with an apparent decrease in the rate of VTE in comparison with a subgroup of patients who did not receive any thromboprophylaxis. A prospective phase III study comparing low molecular weight heparin with fixed low-dose warfarin with aspirin is currently ongoing in Italy to evaluate the best prophylaxis against the risk of thal-related VTE for patients with newly diagnosed MM.