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TVP ed Embolia Polmonare: Definizione
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TVP Sintomi & Segni NON SPECIFICI o ASSENTI Dolore Tensione Edema
DD: crampi o strappi muscolari, rottura cisti poplitea, contusioni, artriti anca-ginocchio, gotta, tendiniti.
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EP Sintomi & Segni NON SPECIFICI, dipendono da: Entità dell’ostruzione
Rapidità dell’ostruzione Vaso-broncocostrizione associata Stato cardiopolmonare preesistente
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EP:Ostruzione completa e rapida
Sincope Shock Ipotensione prolungata Diagnosi urgente Diagnosi differenziale: Infarto miocardico, Tamponamento cardiaco, Emorragia massiva, Setticemia, Pneumotorace, Aneurisma dissecante
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Ostruzione parziale Sintomi* Segni* Dispnea Dolore toracico Tosse
Dolore AAII Tachipnea (>20 min) Rantoli (crepitii) Tachicardia IV tono * Più frequenti Diagnosi differenziale (dispnea): Polmonite, Ostruzione vie aeree, Pneumotorace, Edema polmonare, Atelettasia
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ECG Diagnosi Differenziale: IMA Negativo Suggestivo per EP
(emodinamicamente significativa): Sottoslivellamento ST Inversione onda T Nuovo Blocco di branca dx S1Q3T3 non preesistente
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Rx torace Spesso Negativo Esclude: Pneumotorace Aneurisma aorta Altro Alterazioni Non-specifiche
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Emogasanalisi Ridotta PO2: aspecifica Puntura Arteriosa: Attenzione! Normale nel 10-15% di EP
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Presentazione Esami semplici (Sintomi e segni) Sospetto clinico Situazione clinica Anamnesi
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Situazione clinica Anamnesi Periodo Postoperatorio
Trauma arti inferiori Allettamento Gravidanza/puerperio Neoplasia Pregresso VTE Trombofilia Famigliarità Estroprogestinici
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Sospetto clinico EP DEBOLE FORTE Solo agitazione + tachicardia
+ dipnea non spiegabile + storia di tromboembolismo venoso + trombofilia famigliare + estroprogestinici + recente trauma arti inferiori + allettamento FORTE
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Trattamento Sospetto clinico Diagnosi
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Sospetto clinico UFH Bolo (5.000 IU or 80 IU/kg IV)
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3 alta 1-2 moderata <1 bassa
SCORE di Wells 1 -2 Neoplasia in fase attiva (trattamento in corso o nei 6 mesi precedenti o palliativo) Paralisi , paresi o recente immobilizzazione degli arti inferiori Chirurgia maggiore nelle 4 settimane precedenti o paziente allettato e da poco rimesso in piedi Gonfiore localizzato lungo la distribuzione del sistema venoso profondo Gonfiore di tutta la gamba Gonfiore del polpaccio > 3 cm rispetto all’arto asintomatico (misurati 10cm sotto la tuberosità tibiale) Edema con fovea maggiore nell’arto interessato Vene collaterali superficiali (non varicose) Diagnosi alternativa altrettanto o più probabile della TVP 3 alta 1-2 moderata <1 bassa
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Diagnosi D-dimero CUS Ecocolordoppler TAC spirale Clinica +
Angiografia polmonare Scintigrafia v/p Clinica
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Scintigrafia perfusoria
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Risonanza magnetica
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Risonanza magnetica
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Angiopneumografia
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Flebografia
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TRATTAMENTO
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Anticoagulant drugs in the treatment of pulmonary
embolism: a controlled clinical trial Patients with PE (clinical signs, EKG, chest x-rays) Treated group: heparin U IV every 6h for 36 h plus nicoumalone, orally for 14 days Trial terminated after randomization of 35 patients Among 19 control pts, 5 fatal (autopsy-verified) and 5 nonfatal recurrent PE Among 16 treated pts, 1 death from pneumonia and a bleeding duodenal ulcer Barritt, Lancet 1960
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A.T.H.O.S Randomized trial comparing heparin plus acenocoumarol (n=60)
with acenocoumarol alone (=60) in proximal vein thrombosis Brandjes, N Engl J Med 1992
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LMWH vs standard heparin in proximal DVT
-85 patients in each group, follow-up 6 mo. -No difference in bleeding complications Prandoni, Lancet 1992
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Koopman et al. N Engl J Med 1996
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The Columbus investigators. N Engl J Med 1997
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Gould et al. Ann Intern Med 1999
Major bleeding complications occurred in 1.9% of the participants treated with unfractionated heparin. The results of seven studies favored low-molecular-weight heparins for this outcome; one study (3) demonstrated a statistically significant advantage (Figure 1 ). For all studies combined, we obtained different results depending on the statistical model and the measure of treatment effect. When the fixed-effects model was used, the odds ratio for major bleeding favored low-molecular-weight heparins (0.57 [95% CI, 0.33 to 0.99]; P = 0.047), but the absolute risk reduction was small and not statistically significant (0.61% [CI, 0.04% to 1.26%]; P = 0.07; NNT, 164). When the random-effects model was used, we did not detect a statistically significant difference between treatment groups in the frequency of major bleeding complications (odds ratio, 0.71 [CI, 0.40 to 1.27]; P > 0.2). Gould et al. Ann Intern Med 1999
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LMWH therapy in VTE Nadroparin calcium (Fraxiparine) 85 IU/kg q12h or 170 IU/kg/d Enoxaparin sodium (Clexane) 100 U/kg q12h (1mg/kg q12h or 1.5 mg/kg/d) Dalteparin sodium (Fragmin) 200 IU/kg/d Tinzaparin sodium 175 IU/kg/d
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LMWH - Criteria for early discharge or outpatient therapy
Patient in stable condition Patient willingness to collaborate Low bleeding risk and normal renal function Oral anticoagulant surveillance facilities Early medical contact facilities
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Baseline lab in suspected VTE
APTT, PT-INR, CBC Sceening for thrombophylia in selected patients (idiopathic VTE, transient risk factors but age < 50 years, recurrent VTE, positive family history) Antithrombin III, Protein C, Protein S, APC resistance, Factor V Leiden, Prothrombin G210A, homocysteinemia, lupus anticoagulant, antiphospholipid antibodies (anti-beta-2-glycoprotein I)
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Heparin - VTE UFH Bolus (5.000 IU or 80 IU/kg IV,suspected VTE)
UFH: maintenance infusion IU IV/SC or 18 IU/kg/h; appropriate dosage of LMWH UFH: Lab after 6h to keep aPTT times the control Check platelet count between days 3 to 5 Start warfarin at day 1 at 5 mg/day Continue both drugs at least 5 days Stop heparin when INR>2 fot 2 consecutive days Continue warfarin to keep INR between 2.0 and 3.0
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A study demonstrated that recurrent VTE is infrequent if continuous
IV heparin is administered in doses Adjusted to prolong the APTT > 1.5. Basu D et al., N Engl J Med 1972 Blood heparin level of at least 0.2 IU/ml Heparin infused IV in a dose of at least 1250 U/h
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Heparin dose-adjustment nomogram
APTT Bolus Hold Rate change (U/h) Repeat APTT < 50 50-59 60-85 86-95 96-120 > 120 5000 30 60 +120 -80 -160 6 h Next morn Next morn Cruickshank et al, Arch Intern Med 1991; 151:333
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Weight-based nomogram
Initial dose APTT, < 35 s (<1.2 x control) APTT, 35 to 45 s (1.2 to 1.5 x control) APTT, 46 to 70 s (1,5 to 2.3 x control) APTT, 71 to 90 s (2,3 to 3.0 x control) APTT, > 90 s (> 3 x control) 80 U/Kg bolus, then 18 U/Kg/h 80 U/Kg bolus, increase by 4 U/Kg/h 40 U/Kg bolus, increase by 2 U/Kg/h NO CHANGE Decrease infusion by 2 U/Kg/h Hold infusion 1 h, then decrease by 3U/Kg/h Raschke et al., Ann Intern Med 1993; 119:874
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Thrombolytic therapy Usually not indicated in DVT
Reserved to hemodinamically unstable patients with proven PE in the absence of bleeding risk
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Duration of oral anticoagulant treatment
First event associated with transient or reversible risk factors (patients may have underlying eterozygous factor V Leiden or prothrombin G20210A) 3-6 mo > 6 mo First event of idiopathic VTE. First event associated with permanent high risk factors (unresolved cancer, high risk thrombophilia) Recurrent VTE, idiopathic or associated with thrombophilia 12 mo or lifelong
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Indications to inferior vena cava filters
Contraindication/complication of anticoagulation in high risk patients Recurrent VTE despite adequate anticoagulation Pulmonary embolectomy or endarterectomy
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Chronic thromboembolic pulmonary hypertension
Not rare (2-5%?) Perfusion defects at pulmonary scan Proximal obstruction: pulmonary thromboendarterectomy Nonproximal obstruction: angioplasty
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