24 results on '"C. Manotti"'
Search Results
2. Cerebral venous sinus thrombosis in childhood: clinical aspects and neurological and cognitive long-term outcome in three cases
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A. De Fanti, G. Cossu, Giovanni Buccino, G. C. Izzi, Domenico Mancia, C. Manotti, Buccino, G, Cossu, G, DE FANTI, A, Manotti, C, Izzi, Gc, and Mancia, D.
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Male ,Pediatrics ,medicine.medical_specialty ,Neurology ,Fever ,Neurological examination ,Dermatology ,Neuropsychological Tests ,Dyslexia ,Sinus Thrombosis, Intracranial ,Cognition ,Protein C deficiency ,medicine ,Humans ,Neuropsychological assessment ,Cerebral venous sinus thrombosis ,Child ,Neuroradiology ,Paresis ,Neurologic Examination ,Diplopia ,medicine.diagnostic_test ,General Medicine ,medicine.disease ,Magnetic Resonance Imaging ,Psychiatry and Mental health ,Child, Preschool ,Anesthesia ,Neurology (clinical) ,Nervous System Diseases ,medicine.symptom ,Psychology ,Protein C - Abstract
We report clinical findings, risk factors and neurological and cognitive long-term outcome in three Italian children aged 7, 8 and 5, respectively, who experienced cerebral venous sinus thrombosis (CVST). All children presented with headache, associated to nausea, vomiting and papilloedema. None suffered from epileptic seizures. In two of them a paresis of the sixth cranial nerve with diplopia was found. Diagnosis was confirmed by magnetic resonance imaging angiography (angio MRI) in all cases. In all patients plasma levels of protein C, protein S, antithrombin III (AT III), antiphospholipid antibodies (ApA) and homocysteine were detected. Furthermore, factor V Leiden mutation, prothrombin mutation G20210A and MTHFR mutation were searched for. A Protein C reduction was detected in all patients at onset; this finding, however, was not confirmed at follow-up in all of them. At one-year follow-up, neurological examination was normal in all children and neuropsychological assessment, aimed at excluding linguistic and non-linguistic cognitive deficits, revealed normal performances in two of them. In the third child, cognitive assessment confirmed a previously diagnosed developmental dyslexia.
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- 2004
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3. Fibrinogen assays: a collaborative study of six different methods. C.I.S.M.E.L. Comitato Italiano per la Standardizzazione dei Metodi in Ematologia e Laboratorio
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P. M. Mannucci, M Ruggeri, M Maccaferri, G Palareti, C Manotti, Armando Tripodi, F. Rodeghiero, and Veena Chantarangkul
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Radial immunodiffusion ,Prothrombin time ,medicine.medical_specialty ,Chromatography ,medicine.diagnostic_test ,Chemistry ,Biochemistry (medical) ,Clinical Biochemistry ,Fibrinogen ,I²S ,Surgery ,Fibrinogen Measurement ,Coagulation ,Clotting time ,medicine ,Turbidimetry ,medicine.drug - Abstract
This collaborative study, organized by the Hemostasis Subcommittee of C.I.S.M.E.L., evaluated the accuracy, precision, and comparability of the following six widely used fibrinogen assays: total clottable fibrinogen (Blombäck and Blombäck), clotting time (Von Clauss), turbidimetry (Ellis and Stransky), Chromotime System, prothrombin time (PT)-derived, and radial immunodiffusion (RID). The same frozen samples, with normal and high contents of fibrinogen, were examined in four laboratories. The methods were calibrated with an internal standard whose fibrinogen content was determined gravimetrically. Both the Von Clauss and the RID methods were reliable, accurate, and precise, if adequate calibration was used. The PT-derived method was highly reproducible, but had some problems with accuracy. We demonstrate that an adequate calibration procedure is indispensable for reliable fibrinogen measurements whatever method is used. Because neither the calibration procedures proposed by the manufacturers nor the use of lyophilized commercial plasmas is adequate for this purpose, we urge that an international standard for fibrinogen measurement be promptly established.
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- 1991
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4. Computer assisted anticoagulant therapy
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C. Pattacini, M. Lombardi, M. I. Tassoni, C. Manotti, Roberto Quintavalla, and A. Tagliaferri
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medicine.medical_specialty ,Decision support system ,Self-management ,business.industry ,media_common.quotation_subject ,Anticoagulants ,Workload ,Thrombosis ,Hematology ,Primary care ,Clinical decision support system ,Anticoagulant control ,Drug Therapy, Computer-Assisted ,Anticoagulant therapy ,Physiology (medical) ,medicine ,Physical therapy ,Humans ,Quality (business) ,Intensive care medicine ,business ,media_common - Abstract
The constantly workload increase has led to the development of Computerised Decision Support Systems (CDSS) for a better management of patient care. Many clinical situations have been investigated to verify the utility of CDSS: few have demonstrated stable effects. One area where success has been reported is the field of oral anticoagulation management. CDSS system has demonstrated to be able to improve the treatment quality in comparison to manual method. In the future scenario of oral anticoagulant management CDSS will have a pivotal part, the constant increase of patients number and their pressure on thrombosis centres had led to the development of alternative models for delivery OAT: Primary care, General Practitioner, Patient self testing and self management and the use of CDSS has been central to the decentralisation process and may be useful in maintaining the efficacy and quality of anticoagulant control. GP with the aid of CDSS are able to deliver OAT as well as expert physician of Thrombosis Centre in terms of time spent by patient in therapeutic range.
- Published
- 2005
5. Effect of computer-aided management on the quality of treatment in anticoagulated patients: a prospective, randomized, multicenter trial of APROAT (Automated PRogram for Oral Anticoagulant Treatment)
- Author
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C, Manotti, M, Moia, G, Palareti, V, Pengo, L, Ria, and A G, Dettori
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Treatment Outcome ,Anticoagulants ,Disease Management ,Humans ,International Normalized Ratio ,Prospective Studies ,Drug Monitoring ,Algorithms ,Decision Making, Computer-Assisted ,Drug Administration Schedule - Abstract
We carried out a prospective, randomized trial to test whether a computer-based decision support system to initiate and maintain oral anticoagulant (OA) treatment can improve the laboratory quality of therapy.Two separate sets of patients on oral anticoagulants, in five Italian anticoagulant clinics, were studied: 335 patients in the first three months of treatment (stabilization phase), 916 patients (775 patient-years) beyond the third month of treatment (maintenance phase). Patients were randomized to a computerized system, which included algorithms able to suggest OA dosing and to schedule appointments (computer-aided dosing) or to an arm in which OA were prescribed by the same teams of expert physicians without such algorithms (control group). Primary outcomes were: A) the percentage of patients reaching a stable state of anticoagulation during each of the first three months of treatment; B) the percentage of time individuals spent within the aimed therapeutic range (maintenance phase).Patients in the computer-aided dosing group achieved a stable state significantly faster (p0.01) and they spent more time within the therapeutic range during maintenance (p0.001) than controls. The favorable effect of computer-aided dosing was mainly due to a reduction of the time spent below the therapeutic range and was associated with an increase of mean INR value, of anticoagulant drug dosage, and with a reduction of the number of appointments per patient (all changes significant: p0.001).The computer decision-aided support improves the laboratory quality of anticoagulant treatment, both during long-term maintenance and in the early, highly unstable phase of treatment, and it also significantly reduces the number of scheduled laboratory controls.
- Published
- 2001
6. Low oestrogen oral contraceptives as a major risk factor for cerebral venous and sinus thrombosis: evidence from a clinical series
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U. Scoditti, Giovanni Buccino, Domenico Mancia, C. Manotti, A.R. Tagliaferri, M. Pini, Buccino, G, Scoditti, U, Pini, M, Tagliaferri, Ar, Manotti, C, and Mancia, D.
- Subjects
Cerebral veins ,Adult ,Male ,medicine.medical_specialty ,Neurology ,Sinus Thrombosis, Intracranial ,Risk Factors ,medicine ,Sinus thrombosis ,Humans ,Risk factor ,Neuroradiology ,Venous Thrombosis ,medicine.diagnostic_test ,Dose-Response Relationship, Drug ,business.industry ,General Neuroscience ,Factor V ,Magnetic resonance imaging ,Estrogens ,Middle Aged ,Cerebral Veins ,Mutation ,Female ,Neurology (clinical) ,Neurosurgery ,Radiology ,business ,Cerebral angiography ,Contraceptives, Oral - Abstract
Cerebral venous and sinus thrombosis (CVST) is still considered a severe clinical problem that is difficult to diagnose and manage and is linked to a poor prognosis. Nonetheless, conventional cerebral angiography and magnetic resonance imaging (MRI), or more recently, MR angiography allow a more rapid and precise diagnosis, and prognosis has improved with the use of anticoagulant treatment. We report 23 cases of CVST consecutively admitted to the Institute of Neurology of the University of Parma during the period 1990-1997. In all cases diagnosis was confirmed by means of MRI or conventional angiography of brain vessels. Among the patients, 22 were female and 1 was male. In all patients, plasma levels of protein C, protein S, antithrombin III (ATIII) and antiphospholipid antibodies (APA) were evaluated. In 15 of 23 patients, the presence of factor V Leiden mutation was also determined, and found positive in 3 patients (20%). Of the 22 female patients, 15 (68%) were on low-oestrogen (containing less than 50 microg oestrogen) oral contraceptive (OC) treatment. This percentage of OC use by patients with CVST is much higher than that of the rest of the female Italian population. OC use was associated with the presence of factor V Leiden mutation in two cases, with a deficiency of protein C in 1 case and a deficiency of protein S in another.Whether low-oestrogen Ocs may induce cerebral thromboembolic events is an open matter. According to our data, it may be argued that Ocs, even if at low oestrogen content, represent a major risk factor for CVST. The use of Ocs, as is the case for systemic venous thromboembolic events, may further increase the risk of CVST in women carrying the factor V Leiden mutation or other inherited hyperthrombotic conditions.
- Published
- 1999
7. Contents Vol. 33
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K. Lacut, Giancarlo Agnelli, Edward M. Conway, Laurent O. Mosnier, László Muszbek, Augusto Di Castelnuovo, Isabella Fermo, H. Roger Lijnen, Anirban Choudhury, C. Leroyer, L. Salleras, L. Serra-Majem, Carmen Suárez, Anna Falanga, Bonno N. Bouma, Cecilia Becattini, Patricia B. Maguire, Marco Cattaneo, Johann Wojta, Christine Duering, Peter Valent, R. Quintavalla, Kurt Huber, F. Couturaud, Francesco Bertolini, Armando D'Angelo, M. Nijkeuter, A. Tagliaferri, Alexander Woywodt, Rogier M. Bertina, Françoise Dignat-George, Irene Chung, David Bergqvist, Monica Galli, Mojca Stegnar, Gregory Y.H. Lip, Bernhard Lämmle, D. Mottier, J. Montaner, Sabine Eichinger, Éva Katona, Gregory Y. H. Lip, Licia Iacoviello, Giuseppina Mazzola, Nina Vene, Trevor Baglin, Manuel Monreal, Marie-Christine Alessi, Sergio Coccheri, Delphine Bastelica, L. Ribas, R. Valle, Ronald Sträter, J. Monasterio, Pilar Rondón, Andrew D. Blann, Beate Kempf-Bielack, Mojca Bozic, Hugo ten Cate, Federico Leighton, Paolo Prandoni, Irène Juhan-Vague, Gordon .O. Lowe, C. Pattacini, Fernando Uresandi, Ulrike Nowak-Göttl, B. Meneses, Diego Mezzano, Johanna A. Kremer Hovinga, Patrizia Mancuso, M. Lombardi, Zsuzsanna Bereczky, M. Tassoni, C. Kluft, C. Manotti, Cristina Rabascio, D. Quiroga, Giovanni de Gaetano, J. Ngo de la Cruz, Maria Benedetta Donati, Gordon D.O. Lowe, José A.G. Fajardo, José Sampol, Norbert Lubenow, Jan-Dirk Studt, Danijel Kikelj, M.V. Huisman, E. Francisco, P. Bermüdez, Raquel Barba, and Enrico Bernardi
- Subjects
medicine.medical_specialty ,business.industry ,Physiology (medical) ,General surgery ,Medicine ,Hematology ,business ,Surgery - Published
- 2003
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8. Predictive value of preoperative in vitro and in vivo studies for correct individual heparinization in cardiac surgery
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M. Pini, C. Manotti, D. Portioli, O. Ponari, M. Corsi, and R. Poti
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Pulmonary and Respiratory Medicine ,medicine.medical_specialty ,Anticoagulant effect ,business.industry ,Extracorporeal circulation ,Liter ,Heparin ,Predictive value ,In vitro ,Cardiac surgery ,In vivo ,Internal medicine ,Anesthesia ,medicine ,Cardiology ,Surgery ,Cardiology and Cardiovascular Medicine ,business ,medicine.drug - Abstract
Heparin administration for operations with extracorporeal circulation (ECC) usually is performed following prefixed, standardized protocols. These regimens secure an adequate level of anticoagulation, hut they often involve prolonged periods of overheparinization associated with an undue risk of hemorrhage. The predictive value of preoperative studies on the anticoagulant effect of heparin was investigated in 10 patients. The study was performed both in vitro and in vivo using the Xa inhibitor assay as an index of the anticoagulation induced by heparin. Adding variable amounts of heparin in vitro to patient’s plasma resulted in straight (at least up to 7 U. per milliliter) and parallel, but not coincident, dose/response curves, so confirming a different individual sensitivity to heparin. Disappearance curves of the anticoagulant effect in plasma following intravenous administration of a single standard dose of heparin in the same patients showed an even greater patient-to-patient variability, with “half-life” times ranging from 30 to 150 minutes. No relationship was found between the two parameters (in vitro sensitivity to heparin and clearance rate from plasma in vivo). Moreover, neither of them could be correlated with the response to heparin, subsequently observed during ECC in the same patients. Preoperative investigations with the methods presently available are not adequate to choose individual heparin administration regimens for cardiac operations.
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- 1979
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9. Contents, Vol. 19, 1989
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Peter Baumann, Utako Okamoto, L. Stigendahl, Junichiro Yamamoto, Thomas Jürgensen, Roberto Quintavalla, M. Jeran, Zoltán Boda, S. Bjoern, M. Paolicelli, Duncan P. Thomas, Ulla Hedner, R. Ádány, Kálmán Rák, Peter H. Domer, Y. Okada, C. Manotti, György Pfliegler, A. Tóth, László Muszbek, Y. Nagamatsu, H.C. Hemker, Z. Papp, S. Béguin, A.G. Dettori, Y. Tsuda, Hau C. Kwaan, M. Pini, Jolan Harsfalvi, Trevor W. Barrowcliffe, István Tornai, Ma Xi, S.S. Bernvil, Claus-Ch. Heuck, and L. Tengborn
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Physiology (medical) ,Hematology - Published
- 1989
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10. Predictive value of preoperative in vitro and in vivo studies for correct individual heparinization in cardiac surgery
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O, Ponari, M, Corsi, C, Manotti, M, Pini, D, Portioli, and R, Poti
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Adult ,Male ,Analysis of Variance ,Extracorporeal Circulation ,Dose-Response Relationship, Drug ,Heparin ,Heart Valve Diseases ,Middle Aged ,Injections ,Postoperative Complications ,Thromboembolism ,Injections, Intravenous ,Humans ,Regression Analysis ,Female ,Heart Atria ,Protamines ,Cardiac Surgical Procedures ,Aged ,Half-Life - Abstract
Heparin administration for operations with extracorporeal circulation (ECC) usually is performed following prefixed, standardized protocols. These regimens secure an adequate level of anticoagulation, but they often involve prolonged periods of overheparinization associated with an undue risk of hemorrhage. The predictive value of preoperative studies in the anticoagulant effect of heparin was investigated in 10 patients. The study was performed both in vitro and in vivo using the Xa inhibitor assay as an index of the anticoagulation induced by heparin. Adding variable amounts of heparin in vitro to patient's plasma resulted in straight (at least up to 7 U. per milliliter) and parallel, but not coincident, dose/response curves, so confirming a different individual sensitivity to heparin. Disappearance curves of the anticoagulant effect in plasma following intravenous administration of a single standard dose of heparin in the same patients showed an even greater patient-to-patient variability, with "half-life" times ranging from 30 to 150 minutes. No relationship was found between the parameters (in vitro sensitivity to heparin and clearance rate from plasma in vivo). Moreover, neither of them could be correlated with the response to heparin, subsequently observed during ECC in the same patients. Preoperative investigations with the methods presently available are not adequate to choose individual heparin administration regimens for cardiac operations.
- Published
- 1979
11. [Antithrombin III deficiency in an Italian family. case report]
- Author
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C, Manotti, R, Quintavalla, T, Poli, and D, Portioli
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Adult ,Male ,Antithrombin III Deficiency ,Humans ,Female ,Thrombosis ,Middle Aged ,Thrombophlebitis ,Child ,Aged - Published
- 1982
12. [Increased blood level of factor VIII. A critical review (author's transl)]
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O, Ponari and C, Manotti
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Factor VIII ,Vasopressins ,Liver Diseases ,Physical Exertion ,Nicotinic Acids ,Blood Coagulation Disorders ,Delivery, Obstetric ,Pregnancy Complications ,Catecholamines ,Immune System Diseases ,Pregnancy ,Surgical Procedures, Operative ,Humans ,Insulin ,Female ,Kidney Diseases ,Blood Coagulation ,Contraceptives, Oral - Published
- 1981
13. [Study of platelet function in patients with migraine]
- Author
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C, Manotti, G C, Manzoni, G, Moretti, R, Potì, and A, Tagliaferri
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Adenosine Diphosphate ,Adult ,Male ,Platelet Aggregation ,Migraine Disorders ,Prostaglandins ,Humans ,Female ,Middle Aged ,beta-Thromboglobulin - Published
- 1983
14. ‘In Vivo’ and ‘In Vitro’ Effects of Some Vasoactive Drugs on Platelet Function and on Coagulation/Fibrinolysis System
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A. Megha, A.G. Dettori, C. Manotti, O. Ponari, and M. Pini
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business.industry ,In vivo ,Vasoactive ,Medicine ,Platelet ,Coagulation fibrinolysis ,Pharmacology ,business ,Function (biology) ,In vitro - Abstract
Three substances widely used as vasoactive drugs are known to have an inhibiting effect on platelet aggregation ‘in vitro’. We investigated the changes induced on thrombelastogram, routine clotting tests, euglobulin lysis time (ELT), platelet count, aggregation, and adhesiveness by i, v. administration of these drugs to man. The same indices were also studied ‘in vitro’ by adding comparable concentrations of the substances to human blood or plasma.Aminophilline did not produce any significant variation in ADP-or collagen-induced aggregation either ‘in vitro’ (50 to 200 μg/ml) or ‘in vivo’ (240 mg). A trend to disaggregation was seen only in a few cases. Shorter ELT were found 30 and 120 minutes after injection.A papaverine derivative (Metaverinum, 150 mg) showed a similar ‘in vivo’ pattern: minor changes in platelet function tests and a moderate activation of fibrinolysis were seen. The drug acted ‘in vitro’ as a powerful inhibitor of aggregation (from 30 µg/ml)while fibrinolysis was only activated at the highest concentration (120 µg/ml).Bencyclan, capable of inhibiting platelet function ‘in vitro’ at very low concentrations (0.25µM) did not show similar effects ‘in vivo’ (50 mg) apart from a reduced platelet adhesiveness to glass.
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- 1977
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15. Subject Index, Vol. 19, 1989
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M. Paolicelli, Y. Okada, C. Manotti, A. Tóth, Y. Nagamatsu, Zoltán Boda, Ma Xi, R. Ádány, Hau C. Kwaan, Ulla Hedner, Peter Baumann, György Pfliegler, István Tornai, S.S. Bernvil, A.G. Dettori, Z. Papp, Trevor W. Barrowcliffe, Y. Tsuda, L. Stigendahl, M. Pini, Junichiro Yamamoto, László Muszbek, L. Tengborn, H.C. Hemker, Claus-Ch. Heuck, Kálmán Rák, S. Bjoern, S. Béguin, Utako Okamoto, M. Jeran, Thomas Jürgensen, Roberto Quintavalla, Jolan Harsfalvi, Duncan P. Thomas, and Peter H. Domer
- Subjects
medicine.medical_specialty ,Index (economics) ,business.industry ,Physiology (medical) ,medicine ,Physical therapy ,Subject (documents) ,Hematology ,business ,Surgery - Published
- 1989
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16. Book Review / Announcement
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Kálmán Rák, S. Béguin, Duncan P. Thomas, A. Tóth, Peter H. Domer, Y. Nagamatsu, Utako Okamoto, László Muszbek, H.C. Hemker, L. Stigendahl, Peter Baumann, Junichiro Yamamoto, S. Bjoern, Claus-Ch. Heuck, Y. Tsuda, Ma Xi, Roberto Quintavalla, Trevor W. Barrowcliffe, L. Tengborn, Ulla Hedner, M. Pini, István Tornai, S.S. Bernvil, Y. Okada, Thomas Jürgensen, Zoltán Boda, Hau C. Kwaan, Z. Papp, Jolan Harsfalvi, György Pfliegler, R. Ádány, A.G. Dettori, M. Paolicelli, M. Jeran, and C. Manotti
- Subjects
medicine.medical_specialty ,business.industry ,Physiology (medical) ,General surgery ,Medicine ,Hematology ,business ,Surgery - Published
- 1989
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17. Position Paper on laboratory testing for patients on direct oral anticoagulants. A Consensus Document from the SISET, FCSA, SIBioC and SIPMeL.
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Tripodi A, Ageno W, Ciaccio M, Legnani C, Lippi G, Manotti C, Marcucci R, Moia M, Morelli B, Poli D, Steffan A, and Testa S
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- Administration, Oral, Anticoagulants administration & dosage, Anticoagulants adverse effects, Humans, Italy, Societies, Scientific, Anticoagulants pharmacokinetics, Drug Monitoring methods, Drug Monitoring standards
- Abstract
Although direct oral anticoagulants (DOAC) do not require dose-adjustment on the basis of laboratory test results, the measurement of their anticoagulant effect is useful in special situations. This position paper issued by the Italian Scientific Societies that are mainly involved in the management of patients on DOAC is aimed at providing guidance to care-givers on which tests should be used and the situations in which testing is useful. The guidance is based on the data from the literature so far available and/or on consensus among experts.
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- 2018
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18. Increased dabigatran plasma concentration during Ibrutinib treatment: a case of cerebral hemorrhage and successful dabigatran reversal by idarucizumab.
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Quintavalla R, Lombardi M, Prandoni P, Manotti C, Tadonio I, Re F, Ferrini PM, Tassoni MI, Rossetti P, and Quaini F
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- 2018
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19. Center-Related Determinants of VKA Anticoagulation Quality: A Prospective, Multicenter Evaluation.
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Tosetto A, Manotti C, and Marongiu F
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- Aged, Aged, 80 and over, Female, Humans, Male, Prospective Studies, Anticoagulants administration & dosage, Anticoagulants pharmacokinetics, Drug Monitoring, International Normalized Ratio, Quality of Health Care
- Abstract
Background: Center-specific TTR (c-TTR) is a measure reporting the mean patient TTR within an anticoagulation clinic describing the quality of anticoagulant monitoring offered by that clinic. c-TTR has a considerable between-center variation, but its determinants are poorly understood., Objectives: We aimed at evaluating which clinical, procedural or laboratory factors could be associated with c-TTR variability in a multicenter, observational cross-sectional study over a five-year period., Patients/methods: Data from 832,204 individual patients followed for VKA therapy in 292 Centers affiliated with the Italian Federation of Anticoagulation Clinics (FCSA) were analyzed. c-TTR was computed based on the TTR of patients followed at each Center, and a mixed linear regression model was used for a predefined set of explanatory variables., Results: The Center next-visit interval ratio (the mean number of days after a visit with an INR outside the therapeutic range, divided by the days after a visit with an INR within the therapeutic range), the Center mean patient INR and the Center laboratory performance at EQA proficiency testing were the only variables that were independently associated with c-TTR (β-coefficients -17.32, 9.67, and -0.11, respectively; r2 = 0.635)., Conclusions: These findings suggest that c-TTR associates with proactive strategies aimed at keeping patients very close to their target INR with a prompt re-evaluation of those patients with under- or over-therapeutic INR.
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- 2015
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20. Phase III studies on novel oral anticoagulants for stroke prevention in atrial fibrillation: a look beyond the excellent results.
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Pengo V, Crippa L, Falanga A, Finazzi G, Marongiu F, Moia M, Palareti G, Poli D, Testa S, Tiraferri E, Tosetto A, Tripodi A, Siragusa S, and Manotti C
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- Administration, Oral, Aged, Aged, 80 and over, Anticoagulants adverse effects, Anticoagulants pharmacokinetics, Atrial Fibrillation blood, Atrial Fibrillation complications, Benzimidazoles administration & dosage, Clinical Trials, Phase III as Topic, Dabigatran, Evidence-Based Medicine, Female, Hemorrhage chemically induced, Humans, Male, Middle Aged, Morpholines administration & dosage, Patient Safety, Pyrazoles administration & dosage, Pyridones administration & dosage, Randomized Controlled Trials as Topic, Rivaroxaban, Stroke blood, Stroke etiology, Thiophenes administration & dosage, Treatment Outcome, Warfarin administration & dosage, beta-Alanine administration & dosage, beta-Alanine analogs & derivatives, Anticoagulants administration & dosage, Atrial Fibrillation drug therapy, Preventive Health Services, Stroke prevention & control
- Abstract
In this overview we address the three phase III studies that compared new oral anticoagulants (dabigatran, rivaroxaban and apixaban) with warfarin in the setting of stroke prevention in atrial fibrillation. Strengths and weaknesses of the studies were examined in detail through indirect comparison. We analyze and comment the inclusion and exclusion criteria, the characteristics of randomized patients, the primary efficacy and safety end points and side effects. All new oral anticoagulants resulted in being non-inferior to vitamin K antagonists in reducing stroke or systemic embolism in patients with atrial fibrillation. Dabigatran 150 mg and apixaban were superior to vitamin K antagonists. Importantly, new oral anticoagulants significantly reduced hemorrhagic stroke in all three studies. Major differences among new oral anticoagulants include the way they are eliminated and side effects. Both dabigatran and apixaban were tested in low- to moderate-risk patients (mean CHADS2 [Congestive heart failure, Hypertension, Age, Diabetes, Stroke] score = 2.1-2.2) whereas rivaroxaban was tested in high-risk patients (mean CHADS2 score = 3.48) and at variance with dabigatran and apixaban was administered once daily. Apixaban significantly reduced mortality from any cause. The choice of a new oral anticoagulant should take into account these and other differences between the new drugs., (© 2012 International Society on Thrombosis and Haemostasis.)
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- 2012
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21. Intron factor VIII gene inversion in a population of Italian hemophilia A patients.
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Riccardi F, Tagliaferri A, Manotti C, Pattacini C, and Neri TM
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- Gene Frequency, Hemophilia A epidemiology, Humans, Italy epidemiology, Male, Chromosome Inversion, DNA Mutational Analysis, Factor VIII genetics, Hemophilia A genetics, Introns genetics, Polymerase Chain Reaction methods
- Published
- 2002
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22. Effect of computer-aided management on the quality of treatment in anticoagulated patients: a prospective, randomized, multicenter trial of APROAT (Automated PRogram for Oral Anticoagulant Treatment).
- Author
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Manotti C, Moia M, Palareti G, Pengo V, Ria L, and Dettori AG
- Subjects
- Disease Management, Drug Administration Schedule, Drug Monitoring, Humans, International Normalized Ratio, Prospective Studies, Treatment Outcome, Algorithms, Anticoagulants administration & dosage, Decision Making, Computer-Assisted
- Abstract
Background and Objectives: We carried out a prospective, randomized trial to test whether a computer-based decision support system to initiate and maintain oral anticoagulant (OA) treatment can improve the laboratory quality of therapy., Design and Methods: Two separate sets of patients on oral anticoagulants, in five Italian anticoagulant clinics, were studied: 335 patients in the first three months of treatment (stabilization phase), 916 patients (775 patient-years) beyond the third month of treatment (maintenance phase). Patients were randomized to a computerized system, which included algorithms able to suggest OA dosing and to schedule appointments (computer-aided dosing) or to an arm in which OA were prescribed by the same teams of expert physicians without such algorithms (control group). Primary outcomes were: A) the percentage of patients reaching a stable state of anticoagulation during each of the first three months of treatment; B) the percentage of time individuals spent within the aimed therapeutic range (maintenance phase)., Results: Patients in the computer-aided dosing group achieved a stable state significantly faster (p<0.01) and they spent more time within the therapeutic range during maintenance (p<0.001) than controls. The favorable effect of computer-aided dosing was mainly due to a reduction of the time spent below the therapeutic range and was associated with an increase of mean INR value, of anticoagulant drug dosage, and with a reduction of the number of appointments per patient (all changes significant: p<0.001)., Interpretation and Conclusions: The computer decision-aided support improves the laboratory quality of anticoagulant treatment, both during long-term maintenance and in the early, highly unstable phase of treatment, and it also significantly reduces the number of scheduled laboratory controls.
- Published
- 2001
23. An acquired hemorrhagic disorder of fibrin crosslinking due to IgG antibodies to FXIII, successfully treated with FXIII replacement and cyclophosphamide.
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Tosetto A, Rodeghiero F, Gatto E, Manotti C, and Poli T
- Subjects
- Aged, Aged, 80 and over, Drug Therapy, Combination, Factor XIII immunology, Factor XIII physiology, Factor XIII Deficiency complications, Factor XIII Deficiency immunology, Female, Fibrin physiology, Humans, Immunoglobulin G immunology, Cyclophosphamide therapeutic use, Factor XIII therapeutic use, Factor XIII Deficiency drug therapy, Fibrin antagonists & inhibitors, Hematoma drug therapy, Hematoma etiology
- Abstract
We report a new case of severe bleeding diathesis due to an acquired inhibitor of fibrin crosslinking. The patient, an 80-year-old woman, was admitted to the hospital for a massive subcutaneous hematoma, with severe anemia requiring red cell transfusion; a subsequent retroperitoneal hematoma developed 2 weeks later. Coagulation studies were normal except for a thromboelastographic pattern suggestive of FXIII deficiency. Clot solubility test was abnormal even after 1:1 mix with normal plasma. Immunochemical studies confirmed the presence of a monoclonal IgG lambda inhibitor directed against FXIII activity (type II FXIII inhibitor). The patient IgG fraction selectively inhibited FXIII transamidating activity but did not inhibit the thrombin-mediated activation of FXIII. The patient was treated with high doses of FXIII concentrate to overcome the inhibitor and immunosuppressive therapy with cyclophosphamide and discharged in good conditions. High doses of commercially available FXIII appear to be a safe and effective method of controlling acute episodes of bleeding in patients with acquired FXIII deficiency.
- Published
- 1995
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24. Predictive value of preoperative in vitro and in vivo studies for correct individual heparinization in cardiac surgery.
- Author
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Ponari O, Corsi M, Manotti C, Pini M, Portioli D, and Poti R
- Subjects
- Adult, Aged, Analysis of Variance, Dose-Response Relationship, Drug, Female, Half-Life, Heart Atria, Heart Valve Diseases prevention & control, Heparin blood, Heparin therapeutic use, Humans, Injections, Injections, Intravenous, Male, Middle Aged, Postoperative Complications prevention & control, Protamines therapeutic use, Regression Analysis, Cardiac Surgical Procedures, Extracorporeal Circulation methods, Heparin administration & dosage, Thromboembolism prevention & control
- Abstract
Heparin administration for operations with extracorporeal circulation (ECC) usually is performed following prefixed, standardized protocols. These regimens secure an adequate level of anticoagulation, but they often involve prolonged periods of overheparinization associated with an undue risk of hemorrhage. The predictive value of preoperative studies in the anticoagulant effect of heparin was investigated in 10 patients. The study was performed both in vitro and in vivo using the Xa inhibitor assay as an index of the anticoagulation induced by heparin. Adding variable amounts of heparin in vitro to patient's plasma resulted in straight (at least up to 7 U. per milliliter) and parallel, but not coincident, dose/response curves, so confirming a different individual sensitivity to heparin. Disappearance curves of the anticoagulant effect in plasma following intravenous administration of a single standard dose of heparin in the same patients showed an even greater patient-to-patient variability, with "half-life" times ranging from 30 to 150 minutes. No relationship was found between the parameters (in vitro sensitivity to heparin and clearance rate from plasma in vivo). Moreover, neither of them could be correlated with the response to heparin, subsequently observed during ECC in the same patients. Preoperative investigations with the methods presently available are not adequate to choose individual heparin administration regimens for cardiac operations.
- Published
- 1979
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