Žilní tromboembolická nemoc (TEN), zahrnující žilní trombózu stejně jako plicní embolii, je časté a potencionálně fatální onemocnění. S uvedením nízkomolekulárních heparinů (LMWH) do praxe bylo prokázáno, že ambulantní léčba žilní trombózy je efektivní a bezpečná pro velkou část nemocných s TEN. Vzrůstající data o ambulantní léčbě LMWH v posledních letech ukazují, že až 50 % pacientů s klinicky stabilní plicní embolií může být léčeno doma. I přes tato fakta dosud neměla domácí léčba plicní embolie pevnou pozici v běžné praxi. Pokud bychom měli sumarizovat podmínky pro domácí léčbu, potom by bylo možné uvažovat o ambulantní léčbě u nemocných s nízkým rizikem dle pomocných kritérií, bez hemodynamické nestability (především bez šokového stavu), bez selhávání pravé komory, bez předchozího chronického srdečního či plicního onemocnění, bez závažných komorbidit (onemocnění gastrointestinálního traktu, onemocnění ledvin, krevní choroby, pokročilá nádorová onemocnění), s nízkým rizikem časné rekurence tromboembolické nemoci, bez jiných indikací pro hospitalizaci (bolest vyžadující parenterální analgetika, infekce apod), s nízkým rizikem krvácení a s garantovanou spoluprací nemocného a dobře organizovanou domácí péčí., Venous thromboembolic disease which includes both venous thrombosis and pulmonary embolism, is a frequent and potentially fatal disease. Based on the introduction of low-molecular-weight heparins (LMWH) into practice it has been proved that outpatient treatment of venous thrombosis is effective and safe for a large number of patients with VTE. The growing volume of data on LMWH outpatient treatment in recent years shows that up to 50 % of patients with clinically stable pulmonary embolism can be treated at home. In spite of these facts home treatment of pulmonary embolism has not been established as part of common practice as yet. If we were to summarize the conditions for home treatment, we would consider outpatient care for patients at low risk based on auxiliary criteria, free from hemodynamic instability (primarily without a shock state), free from right ventricular failure, prior chronic heart or lung disease, serious comorbidities (gastrointestinal tract disease, kidney disease, blood diseases, advanced cancers), at low risk of early thromboembolism recurrence, free from other indications for hospitalization (pain requiring parenteral analgesics, infections etc.), at low risk of bleeding and with guaranteed patient‘s cooperation and well-organized home care., and Radovan Malý, Jaroslav Malý
INTRODUCTION: The issue of resistance to antiplatelet therapy has raised many questions in the area of neurovascular diseases. The first objective of this work was to determine the prevalence of aspirin resistance in neurovascular patients with clinical non-responsiveness to aspirin treatment and a high-risk of atherothrombotic complications using two interpretable and independent methods (aggregation and PFA 100). The second objective was to find the correlation between both assays and to evaluate the results in groups at risk for various cerebrovascular diseases. MATERIAL AND METHODS: Laboratory tests of aspirin resistance were performed in 79 patients with clinical non-responsiveness to aspirin treatment suffering from neurovascular diseases. Patients were divided into the two groups: expected low risk for aspirin resistance due to the first manifestation of a neurovascular disease (n = 34) and expected high risk due to the second clinical manifestation of a neurovascular disease (n = 45). RESULTS: The prevalence of aspirin resistance in both groups combined as determined by the PFA-100 and CPG techniques were 50.6% and 17.7%, respectively. No correlation was found between the two techniques. CONCLUSIONS: No significant prevalence of aspirin resistance was demonstrated by either method despite the heterogeneous pathophysiological mechanisms. However, we are presently unable to provide an accurate opinion on the value of laboratory test result or routine monitoring in clinical neurology. and M. Vališ, D. Krajíčková, J. Malý, R. Malý, I. Fátorová, O. Vyšata, R. Herzig