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#451
09.11.2011, 16:24
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[Ссылки доступны только зарегистрированным пользователям ]
[Ссылки доступны только зарегистрированным пользователям ] [Ссылки доступны только зарегистрированным пользователям ] 
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#452
09.11.2011, 19:27
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Интересные выводы делают исследователи из Stanford Univercity
[Ссылки доступны только зарегистрированным пользователям ] Цитата:
[Ссылки доступны только зарегистрированным пользователям ]
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#453
14.11.2011, 13:03
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QT-Interval Duration and Mortality Rate
Results From the Third National Health and Nutrition Examination Survey Yiyi Zhang, MHS; Wendy S. Post, MD, MS; Darshan Dalal, MD, PhD; Elena Blasco-Colmenares, MD, PhD; Gordon F. Tomaselli, MD; Eliseo Guallar, MD, DrPH Arch Intern Med. 2011;171(19):1727-1733. doi:10.1001/archinternmed.2011.433 Background Extreme prolongation or reduction of the QT interval predisposes patients to malignant ventricular arrhythmias and sudden cardiac death, but the association of variations in the QT interval within a reference range with mortality end points in the general population is unclear. Methods We included 7828 men and women from the Third National Health and Nutrition Examination Survey. Baseline QT interval was measured via standard 12-lead electrocardiographic readings. Mortality end points were assessed through December 31, 2006 (2291 deaths). Results After an average follow-up of 13.7 years, the association between QT interval and mortality end points was U-shaped. The multivariate-adjusted hazard ratios comparing participants at or above the 95th percentile of age-, sex-, race-, and R-R interval–corrected QT interval (439 milliseconds) with participants in the middle quintile (401 to <410 milliseconds) were 2.03 (95% confidence interval, 1.46-2.81) for total mortality, 2.55 (1.59-4.09) for mortality due to cardiovascular disease (CVD), 1.63 (0.96-2.75) for mortality due to coronary heart disease, and 1.65 (1.16-2.35) for non-CVD mortality. The corresponding hazard ratios comparing participants with a corrected QT interval below the fifth percentile (<377 milliseconds) with those in the middle quintile were 1.39 (95% confidence interval, 1.02-1.88) for total mortality, 1.35 (0.77-2.36) for CVD mortality, 1.02 (0.44-2.38) for coronary heart disease mortality, and 1.42 (0.97-2.08) for non-CVD mortality. Increased mortality also was observed with less extreme deviations of QT-interval duration. Similar, albeit weaker, associations also were observed with Bazett-corrected QT intervals. Conclusion Shortened and prolonged QT-interval durations, even within a reference range, are associated with increased mortality risk in the general population. [Ссылки доступны только зарегистрированным пользователям ]
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#454
15.11.2011, 17:55
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PALLAS
"Dronedarone increased rates of heart failure, stroke, and death from cardiovascular causes in patients with permanent atrial fibrillation who were at risk for major vascular events".
[Ссылки доступны только зарегистрированным пользователям ]
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#455
16.11.2011, 11:21
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The VeriQ system for assessing graft flow during coronary artery bypass graft
surgery Issued: November 2011 NICE medical technology guidance [Ссылки доступны только зарегистрированным пользователям ]
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#456
12.12.2011, 22:23
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Bleeding risk assessment and management in atrial fibrillation patients
Executive Summary# of a Position Document from the European Heart Rhythm Association [EHRA], endorsed by the European Society of Cardiology [ESC] Working Group on Thrombosis [Ссылки доступны только зарегистрированным пользователям ]
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#458
21.01.2012, 13:49
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Соду нафиг?
Sodium chloride vs. sodium bicarbonate for the prevention of contrast medium-induced nephropathy: a randomized controlled trial Theresia Klima et al. Aims The most effective regimen for the prevention of contrast-induced nephropathy (CIN) remains uncertain. Our purpose was to compare two regimens of sodium bicarbonate with 24 h sodium chloride 0.9% infusion in the prevention of CIN. Methods and results We performed a prospective, randomized trial between March 2005 and December 2009, including 258 consecutive patients with renal insufficiency undergoing intravascular contrast procedures. Patients were randomized to receive intravenous volume supplementation with either (A) sodium chloride 0.9% 1 mL/kg/h for at least 12h prior and after the procedure or (B) sodium bicarbonate (166 mEq/L) 3 mL/kg for 1h before and 1 mL/kg/h for 6h after the procedure or (C) sodium bicarbonate (166 mEq/L) 3 mL/kg over 20min before the procedure plus sodium bicarbonate orally (500 mg per 10 kg). The primary endpoint was the change in estimated glomerular filtration rate (eGFR) within 48h after contrast. Secondary endpoints included the development of CIN. The maximum change in eGFR was significantly greater in Group B compared with Group A {mean difference −3.9 [95% confidence interval (CI), −6.8 to −1] mL/min/1.73 m2, P = 0.009} and similar between Groups C and B [mean difference 1.3 (95% CI, −1.7–4.3) mL/min/1.73 m2, P = 0.39]. The incidence of CIN was significantly lower in Group A (1%) vs. Group B (9%, P = 0.02) and similar between Groups B and C (10%, P = 0.9). Conclusion Volume supplementation with 24 h sodium chloride 0.9% is superior to sodium bicarbonate for the prevention of CIN. A short-term regimen with sodium bicarbonate is non-inferior to a 7 h regimen. Там же: Contrast-induced kidney injury: mechanisms, risk factors, and prevention Если нужен полный текст, готов поделиться
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#459
24.01.2012, 16:17
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Любопытная ссылка - [Ссылки доступны только зарегистрированным пользователям ]
Скорее не для врачей, а для студентов и пациентов - собраны понятные и наглядные видеоролики, часть рекомендации по кардиологии, атласы по ЭКГ, ЭхоКС. _______________________ P.S.: Имеется даже свой форум, который пытается набрать обороты (рекорд посещаемости 3, тем 5, ответов 7) 
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#462
02.02.2012, 04:39
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Цитата:
Among the subgroup of major bleeding patients with warfarin-associated ICH, those not correcting to INR of ≤1.5 with the use of FFP have an increased rate of mortality at 30 days (adjusted OR=2.55; 95% CI 1.04-6.28)... Failure to Correct International Normalized Ratio and Mortality Among Patients with Warfarin-Related Major Bleeding: an Analysis of Electronic Health Records. Menzin J, Hoesche J, Friedman M, Nichols C, Bergman GE, Crowther M, Garcia D, Jones C. J Thromb Haemost. 2012 Jan 18 Другие публикации предлагают корректировать препаратом протромбинового комплекса как более эффективной/беzопасной опцией, но в Штатах это не всегда доступно... Complete and rapid reversal of warfarin-induced bleeding can be achieved more successfully with PCC than with FFP. In addition, PCC is associated with a more rapid normalisation of the INR and a better clinical outcome due to the balanced ratio of four vitamin-K-dependent clotting factors plus the coagulation inhibitors protein C and Protein S. PCC products containing four factors are the preferred option for the emergency reversal of OAC, according to some clinical treatment guidelines. Other advantages of PCC over FFP include smaller infusion volumes, no blood group testing and virus-inactivated blood product. Warfarin-induced bleeding complications - clinical presentation and therapeutic options. Wiedermann CJ, Stockner I. Thromb Res. 2008;122 Suppl 2:S13-8. +++ Role of prothrombin complex concentrates in reversing warfarin anticoagulation: a review of the literature. Leissinger CA, Blatt PM, Hoots WK, Ewenstein B. Am J Hematol. 2008 Feb;83(2):137-43.
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#463
02.02.2012, 21:19
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Вадим Валерьевич, спасибо за ссылку, но нам-то в РФ что делать? Лить плазму 15 мл на 1 кг живого веса? Нам и это не слишком доступно. PCC это вообще недостижимая мечта (диализ доступнее). Кстати, что Вы думаете о Новосевен?
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#464
03.02.2012, 21:33
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Михаил Юрьевич, думаю, что неплохая опция, но очень дорогая даже по американским меркам и впечатляюще тромбогенна:
Stroke. 2010 Jul;41(7):1459-63. Safety of recombinant activated factor VII in patients with warfarin-associated hemorrhages of the central nervous system. [Ссылки доступны только зарегистрированным пользователям ] всякие сравнения коррекций в полном тексте еще здесь: Int J Emerg Med. 2011 Jul 8;4(1):40. Treatments for reversing warfarin anticoagulation in patients with acute intracranial hemorrhage: a structured literature review. [Ссылки доступны только зарегистрированным пользователям ]
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#465
08.02.2012, 15:07
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При наличии ингибиторов Xа фактора существование ингибиторов тромбина бессмысленно. У них нет никаких преимуществ, даже ценовых, а потенциальные риски длительного полного ингибирования тромбина никем не изучены. У тромбина полно других функций в организме, помимо участия в образовании фибрина, и подавление даже базального уровня антифизиологично.
Похоже, что над Прадаксой начинают сгущаться тучи. Количество кровотечений на дабигатране в реальной клинической практике намного превышает число кровотечений на варфарине. Dabigatran (PRADAXA). This drug, which was launched in October 2010 to reduce the risk of stroke in patients with atrial fibrillation, generated hundreds of adverse event reports during the first quarter of 2011. Overall, 932 serious adverse events were linked to this drug, including 120 deaths, 25 cases of permanent disability, and 543 cases requiring hospitalization. Of the 932 events, 505 cases involved hemorrhage, more than any other monitored drug including warfarin, which ranked second with 176 cases of hemorrhage. The total included 120 cases that described the event with terms indicating hemorrhagic stroke, which is particularly problematic given that the drug’s primary indication is to prevent ischemic strokes. [Ссылки доступны только зарегистрированным пользователям ] Похожие проблемы и в Японии. In August 2011, the Japanese MHLW issued a safety advisory to warn of the potential for serious adverse events with dabigatran (Pradaxa®) which was approved in Japan in January 2011. This was following the death of five patients who were taking the drug. Between January and 11 August 2011, the patient exposure in Japan was about 64,000 people. At the time of publication of the advisory, there were 81 cases of serious side effects associated with dabigatran reported in Japan, including cases of gastrointestinal bleeding . The five patients who had bleeding events contributory to their death were elderly, aged between 76 and 100 years old. They were prescribed with age-adjusted doses of dabigatran. The events leading to death include haemorrhage of the digestive tract, pulmonary alveolar haemorrhage, respiratory failure and haemorrhagic shock. The time to onset for these events ranged from eight days to 104 days. Two of these patients had taken aspirin concomitantly. Based on limited data available and a post-hoc estimation of creatinine clearance (CLcr), four of the patients were suspected to have severe renal impairment while on dabigatran therapy. Physicians in Japan were advised to carefully monitor for signs of anaemia and bleeding and the need for immediate response should these side effects develop. They were also recommended to perform renalfunction tests before and during treatment, and to reduce the dose of dabigatran or stop treatment upon signs of renal impairment or bleeding. [Ссылки доступны только зарегистрированным пользователям ]
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Линейный вид
