746 research outputs found

    Comparative analysis of the concentrations of proinflammatory cytokines and glycosylated ferritin in patients with idiopathic recurrent pericarditis and adult-onset Still's disease

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    Idiopathic recurrent pericarditis (IRP) and adult-onset Still's disease (AOSD) are polygenic autoinflammatory diseases, in the pathogenesis of which pro-inflammatory cytokines from the interleukin-1 superfamily play a central role.Aim. To compare serum concentrations of proinflammatory cytokines and glycosylated ferritin (GF) in patients with IRP and AOSD during an exacerbation.Material and methods. The study included 15 patients with AOSD, 15 — IRP. The diagnosis of AOSD was established using the Yamaguchi criteria (1992). IRP was diagnosed in accordance with the 2015 European Society of Cardiology on the diagnosis and management of pericardial diseases. Blood sampling from all patients was carried out during the recurrence period prior to the anti-inflammatory therapy initiation. The serum levels of interleukin-1β (IL-1β), interleukin-6 (IL-6), interleukin-18 (IL-18), procalcitonin, total ferritin and GF was assessed. The results obtained were compared with levels of biochemical parameters, high-sensitivity C-reactive protein (CRP), as well as with white blood cell (WBC) and neutrophil counts.Results. The median age in the AOSD group was 28 years, and the IRP — 55 years. An increase WBC count >10*109/L was detected in 10 and 9 patients in the AOSD and IRP groups, respectively. The concentration of CRP was increased in all patients and did not differ in the study groups (p=0,836).The highest values of ferritin and GF levels were found in the AOSD group (1416 ng/ml vs 408 ng/ml, p=0,008) and (12% vs 33,9%, p=0,067), respectively. In both groups, increased concentrations of IL-6 and IL-18 were determined. In the AOSD group, the concentration of IL-18 was higher than in the IRP group (2114 pg/ml vs 161,5 pg/ml, p<0,001). IL-6 concentrations in the study groups did not differ (33,9 pg/ml vs 24,9 pg/ml, p=0,4). IL-1β serum concentration in all subjects corresponded to normal values.Correlation analysis in the AOSD group revealed a direct relationship between the IL-18 and ferritin concentrations (rs=0,73, p=0,03).Conclusion. The study established a similar pattern of changes in inflammatory biomarkers in patients with AOSD and IRI. The most informative marker of inflammation was IL-18

    CHARACTERISTICS OF AUTOIMMUNE INFLAMMATION IN THE PATIENTS WITH LUNG TUBERCULOSIS

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    Tuberculosis is a granulomatous disease caused by Mycobacterium tuberculosis, being characterized by the development of caseous granulomas in various organs, mainly in lungs. M. tuberculosis is known to be a trigger for autoimmune inflammation, due to the possible mimicry of bacterial proteins as autoantigens. Recently, a significance of mesenchymal vimentin as an autoantigen in mycobacterial infections has been actively discussed. The aim of the present study was to determine autoantibodies for various vimentin modifications in the patients with tuberculosis.The study was performed in 2014-2017 and included 28 patients with pulmonary tuberculosis (group I), 30 patients with nonspecific lung diseases (group II): 15 with granulomatous polyangiitis, and 15 with different alveolites. Control group consisted of healthy subjects (n = 40). Concentration of antibodies to mutated citrullinated vimentin (anti-MCV) was measured using ELISA (ORGENTEC, Germany). The patients with elevated anti-MCV levels were tested for antibodies to cyclic citrullinated peptide (anti-CCP) using ELISA technique (EUROIMMUN, Germany). Statistical analysis was carried out using GraphPad Prism 6 (GraphPad Software, USA), Statistica 10 (Statsoft, USA) using nonparametric analysis of samples with Mann-Whitney and Chi-square criteria, and Spearman method for correlation analysis. The differences were considered statistically significant at p < 0.05.The anti-MCV concentrations were significantly higher in patients with tuberculosis (group I, 60.7% of cases, 17/28) than in group II, and control group (23.6 and 25.0% of cases, respectively). No statistically significant differences were revealed between the results of anti-MVC and anti-CCP levels in comparison group with the control group (p = 0.18).High levels of anti-MCV antibodies in the patients with pulmonary tuberculosis reflect an opportunity of developing autoimmune process in the disease pathogenesis. Measurement of plasma anti-MCV antibody concentrations may be important for correction of the therapy, especially upon administration of immunosuppressive and hormonal corticosteroid drugs. It has been shown that anti-CCP are not characteristic to the lung diseases

    RANGING OF ANTIPHOSPOLIPID ANTIBODIES IN THE PATIENTS WITH THROMBOPHILIA AND RECURRENT MISCARRIAGE

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    Laboratory diagnosis of antiphospholipid syndrome (APS) is based on detection of antiphospholipid antibodies (aPLs). E.g., aPLs are directed against conformational epitopes of the so-called “co-factor” proteins: β2-gycoprotein 1 (β2-GP1), annexin V (An V) and prothrombin (Pt) that are formed during interaction with phospholipids – cardiolipin (CL), phosphatic acid (Pha), phosphatidylcholine (Pch), phosphatidylethanolamine (Pe), phosphatidylglycerol (Pg), phosphatidylinositol (Pi), phosphatidylserine (Ps). A routine methodology of detection based on ELISA testing is challenged by new tests when the antigen is absorbed on another kind of support like microbeads or membranes that can influence density of conformational epitopes for aPL’s binding. The aim of our study was to compare the results of aPLs detection by ELISA and multi-line immunodot assay (MLD). We collected blood serum samples from 45 patients with noncardioembolic ischemic strokes, 19 patients with recurrent deep vein thrombosis of lower limbs, 44 females with recurrent miscarriages, and 50 clinically healthy donors. To compare the results of aPL detection by ELISA and MLD kits, the test systems from different manufacturers were evaluated. We used an ELISA kits for detection of antibodies to CL IgG, aCL IgM, β2-GP1 produced by Euroimmun AG (Mr1) and Orgentec Diagnostica GmbH (Mr2) and MLD – for detection of antibodies to CL, β2-GP1, Pch, Pe, Pg, Pi, Ps, AnV and Pt (Medipan GmbH, Mr3). When a cut-off titer was used as the main index, 30.5% of patients were aPLs-positive with ELISA method by Mr1 and 38%, wiht Mr2. By MLD aPls were detected in 30% of patients. In the same cohort, medium and high aPLs titers (> 40 U/mL) were determined in 12% of patients using ELISA kits. Positive and highly positive aPLs titers were determined in 16% when using a new method by Mr3. Medium and high titer were detected only for antibodies to β2-GP1, CL, An V, Pha and Phs. The use of ELISA approach for detection of aPLs in patients with thrombosis and obstetric pathology is associated with relatively high number of low-positive ELISA results. Due to higher sensitivity for medium and high aPLs titers, MLD testing may be used as a confirming method for APS diagnosis

    The Splicing Efficiency of Activating HRAS Mutations Can Determine Costello Syndrome Phenotype and Frequency in Cancer

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    Costello syndrome (CS) may be caused by activating mutations in codon 12/13 of the HRAS proto-oncogene. HRAS p.Gly12Val mutations have the highest transforming activity, are very frequent in cancers, but very rare in CS, where they are reported to cause a severe, early lethal, phenotype. We identified an unusual, new germline p.Gly12Val mutation, c.35_36GC>TG, in a 12-year-old boy with attenuated CS. Analysis of his HRAS cDNA showed high levels of exon 2 skipping. Using wild type and mutant HRAS minigenes, we confirmed that c.35_36GC>TG results in exon 2 skipping by simultaneously disrupting the function of a critical Exonic Splicing Enhancer (ESE) and creation of an Exonic Splicing Silencer (ESS). We show that this vulnerability of HRAS exon 2 is caused by a weak 3' splice site, which makes exon 2 inclusion dependent on binding of splicing stimulatory proteins, like SRSF2, to the critical ESE. Because the majority of cancer- and CS- causing mutations are located here, they affect splicing differently. Therefore, our results also demonstrate that the phenotype in CS and somatic cancers is not only determined by the different transforming potentials of mutant HRAS proteins, but also by the efficiency of exon 2 inclusion resulting from the different HRAS mutations. Finally, we show that a splice switching oligonucleotide (SSO) that blocks access to the critical ESE causes exon 2 skipping and halts proliferation of cancer cells. This unravels a potential for development of new anti-cancer therapies based on SSO-mediated HRAS exon 2 skipping

    Характеристика клинических, лабораторных и иммунологических проявлений у пациентов с болезнью Шёгрена, ассоциированной с антицентромерными антителами

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    Objective: to study clinical and laboratory features in patients with anticentromere antibody (ACA)-positive SjЪgren's disease (SD), as well as the sensitivity of different methods for determination of ACA, and to elaborate an algorithm for differential diagnosis in ACA-positive patients.Patients and methods. The V.A. Nasonova Research Institute of Rheumatology followed up 136 patients who were highly positive for ACA. The investigators used the 2001 Russian criteria for the diagnosis for SD; the 2013 ACR/European League Against Rheumatism (EULAR) criteria for that of scleroderma systematica (SDS); the guidelines of the American Association for the Study of Liver Diseases, the Russian Gastroenterological Association, and the Russian Society for the Study of the Liver for that of primary biliary cholangitis (PBC)/biliary duct epitheliitis in the presence of SD. Lymphomas were diagnosed by biopsies of affected organs according to the WHO classification. SD was diagnosed in 119 patients; SDS in 49 cases (37 with SDS concurrent with SD and 12 with isolated SDS), PBC/biliary duct epitheliitis in 23 (all cases with PBC/biliary duct epitheliitis concurrent with SD and/or SDS); 5 patients were excluded from the investigation. Further analysis included 131 ACA-positive patients. The patients were divided into three groups: SD (n=82 or 62.6%); SD+SDS (n=37 or 28.24%); SDS (n=12 or 9.16%).Results and discussion. Autoantibodies to centromere peptide (CENP) A and CENP-B in the same titers were detected in all ACA-positive patients, regardless of diagnosis. Comparative analysis of three patient groups revealed no statistically significant differences in the frequency of laboratory deviations. The signs characteristic of classical SD (rheumatoid factor (RF)), anti-Ro and anti-La antibodies, leukopenia, higher ESR values, hypergammaglobulinemia, and elevated IgG/IgA levels) were found in a small proportion of patients. The frequency and severity of glandular manifestations did not differ in SD and SD + SDS. PBC/biliary duct epitheliitis was present in 17.5% of ACA-positive patients (in most antimitochondrial antibody-positive cases); no statistically significant differences in its frequency were found between the groups. Other extraglandular manifestations in SD and SD + SDS were identified in a smaller number of patients. All sclerodermic spectrum manifestations were more common in SD and SD + SDS than in BS. Pulmonary arterial hypertension was not diagnosed in any patient from the SD group. MALT lymphomas were detected in 19 ACA-positive patients. Those were present only in BS patients and absent in the SDS group. MALT lymphomas developed in the first 10 years after the onset of SD. The transformation of MALT lymphoma into diffuse large B-cell lymphoma was observed in 2 patients. The main signs of lymphomas in SD patients were persistent parotid salivary gland enlargement, decreased levels of complement C4 and peripheral blood CD19+ cells, as well as cryoglobulinemic vasculitis, serum monoclonal secretion, lymphoid infiltration in the minor salivary glands (a focus score of >4), and severe damage to the salivary and lacrimal glands.Conclusion. ACA-associated SD is an independent disease subtype characterized by an increased risk for SDS, PBC, and MALT lymphomas and by a low frequency of the systemic manifestations and laboratory signs characteristic of classical SD. Regardless of the detected type of antibodies and the presence or absence of extraglandular manifestations, damage to the salivary and lacrimal glands progresses in SD, which often leads to lymphomas; therefore, the therapy that may prevent this complication should be initiated as soon as possible after SD diagnosis. The lymphoproliferation signs identified in this investigation should be taken into account in all ACA-positive patients with SD for the early diagnosis of lymphoid tumors before therapy is prescribed. An algorithm for differential diagnosis in seropositivity for ACA is presented. Determination of autoantibodies to CENP-A and CENP-B does not allow the differential diagnosis in ACA-positive patients.Цель исследования – изучение клинических и лабораторных особенностей у пациентов с болезнью Шёгрена (БШ), позитивных по антицентромерным антителам (АЦА), а также чувствительности разных методов определения АЦА, разработка алгоритма дифференциальной диагностики у АЦА-позитивных пациентов.Пациенты и методы. В ФГБНУ «Научно-исследовательский институт ревматологии им. В.А. Насоновой» под наблюдением находилось 136 высокопозитивных по АЦА пациентов. Для диагностики БШ использовались отечественные критерии 2001 г., системной склеродермии (ССД) – критерии ACR/EULAR 2013 г., первичного билиарного холангита (ПБХ)/эпителиита билиарных протоков в рамках БШ – рекомендации Американской ассоциации по изучению заболеваний печени, Российской гастроэнтерологической ассоциации и Российского общества по изучению печени. Диагностика лимфом осуществлялась на основании исследований биоптатов пораженных органов согласно классификации ВОЗ. БШ диагностирована у 119 пациентов, ССД – у 49 (у 37 в сочетании с БШ и у 12 – изолированная ССД), ПБХ/эпителиит билиарных протоков – у 23 (во всех случаях в сочетании с БШ и/или ССД), 5 пациентов были исключены из исследования. В дальнейший анализ вошел 131 АЦА-позитивный пациент. Больные были разделены на три группы: БШ (n=82, или 62,6%); БШ + ССД (n=37, или 28,24%); ССД (n=12, или 9,16%).Результаты и обсуждение. Аутоантитела к центромерному пептиду (CENP) A и CENP-B в одинаковых титрах выявлены у всех АЦА-позитивных пациентов независимо от диагноза. При сравнительном анализе трех групп пациентов статистически значимых различий в частоте лабораторных отклонений не выявлено. Характерные для классической БШ признаки – ревматоидный фактор (РФ), антитела к Ro и La, лейкопения, повышение СОЭ, гипергаммаглобулинемия, увеличение уровня IgG/IgA – обнаружены у незначительной части пациентов. Частота и выраженность железистых проявлений при БШ и БШ + ССД не различались. ПБХ/эпителиит билиарных протоков имелся у 17,5% АЦА-позитивных пациентов (в большинстве случаев позитивных по антимитохондриальным антителам), статистически значимых различий в его частоте между группами не обнаружено. Другие внежелезистые проявления при БШ и БШ + ССД выявлены у меньшего числа пациентов. Все проявления склеродермического спектра при ССД и БШ + ССД встречались чаще, чем при БШ. Легочная артериальная гипертензия не диагностирована ни у одного пациента из группы БШ. MALT-лимфомы обнаружены у 19 АЦА-позитивных пациентов. Они встречались только у пациентов с БШ, в группе ССД лимфом не было. MALT-лимфомы развивались в первые 10 лет после начала БШ. Трансформация MALT-лимфомы в диффузную В-клеточную крупноклеточную лимфому наблюдалась у 2 пациентов. Основными признаками лимфом у пациентов с БШ были: стойкое увеличение околоушных слюнных желез, снижение уровня С4-компонента комплемента, а также CD19+ клеток в периферической крови, криоглобулинемический васкулит, моноклональная секреция в сыворотке крови, лимфоидная инфильтрация малых слюнных желез >4 фокуса, а также тяжелое поражение слюнных и слезных желез.Заключение. БШ, ассоциированная с АЦА, является самостоятельным субтипом заболевания, отличающимся повышенным риском возникновения ССД, ПБХ и MALT-лимфом, низкой частотой характерных для классической БШ системных проявлений и лабораторных признаков. При БШ, независимо от выявляемого типа антител и наличия или отсутствия внежелезистых проявлений, прогрессирует поражение слюнных и слезных желез, что нередко приводит к развитию лимфом, поэтому терапия, способная предотвратить возникновение данного осложнения, должна быть инициирована сразу после установления диагноза БШ. Выявленные в настоящем исследовании признаки лимфопролиферации должны учитываться у всех АЦА-позитивных пациентов с БШ для ранней диагностики лимфоидных опухолей до назначения терапии. Приведен алгоритм дифференциальной диагностики при серопозитивности по АЦА. Определение аутоантител к CENP-A и CENP-B не позволяет осуществлять дифференциальную диагностику у АЦА-позитивных пациентов

    Hadron Energy Reconstruction for the ATLAS Calorimetry in the Framework of the Non-parametrical Method

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    This paper discusses hadron energy reconstruction for the ATLAS barrel prototype combined calorimeter (consisting of a lead-liquid argon electromagnetic part and an iron-scintillator hadronic part) in the framework of the non-parametrical method. The non-parametrical method utilizes only the known e/he/h ratios and the electron calibration constants and does not require the determination of any parameters by a minimization technique. Thus, this technique lends itself to an easy use in a first level trigger. The reconstructed mean values of the hadron energies are within ±1\pm 1% of the true values and the fractional energy resolution is [(58±3)/E+(2.5±0.3)[(58\pm3)% /\sqrt{E}+(2.5\pm0.3)%]\oplus (1.7\pm0.2)/E. The value of the e/he/h ratio obtained for the electromagnetic compartment of the combined calorimeter is 1.74±0.041.74\pm0.04 and agrees with the prediction that e/h>1.7e/h > 1.7 for this electromagnetic calorimeter. Results of a study of the longitudinal hadronic shower development are also presented. The data have been taken in the H8 beam line of the CERN SPS using pions of energies from 10 to 300 GeV.Comment: 33 pages, 13 figures, Will be published in NIM

    Treatment of the chronic hepatitis C complicated by mixed cryoglobulinemia with direct-acting antiviral agents

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    The aim of the study was to evaluate clinical, immunologic and anti-viral efficacy of antiviral therapy (АVT) with drugs of the direct antiviral action (DAA) of the chronic hepatitis C (CHC) complicated with secondary mixed cryoglobulinemia in small cohort of patients. Patients and methods: The cohort consisted of 12 patients with CHC (without signs of a coinfection of HIV, a hepatitis B virus) complicated with mixed cryoglobulinemia (criocrit more than 5% and presence of cryoglobulinemia-related symptoms). Standard DAA based therapy was indicated in all patients: 2 cases daclatasvir and asunaprevir, 3 cases daclatasvir and sofosbuvir and 7 cases Dasabuvir;Ombitasvir+Paritaprevir+Ritonavir. Results: Anti-viral response at 12 and 24 weeks was found in 91,6% (11/12) treated patients. In one case (on the daclatasvir and asunaprevir) resistance to both drugs developed. Clinical response was confirmed in 83% – 10/12 (25% – the complete response, 58% – the partial response). Despite of anti-viral response kidney damage persisted in 2 patients without apparent improvement. There was one lethal outcome at 25th week since the beginning of treatment because of bilateral pneumonia and thromboembolism in patient with kidney involvement treated with steroids and cytostatics. In 25% of patients total elimination of cryoglobulins was confirmed by the end of AVT and in 75% dramatic decrease of criocrit was found. Conclusion: We confirmed good virologic, clinical and immunologic response and safety of AVT with DDA in patients with HCV induced crioglobulinemia, especially when using schemes with a high genetic barrier (daclatasvir and sofosbuvir, Dasabuvir;Ombitasvir+Paritaprevir+Ritonavir).Цель: изучить вирусологическую клиническую и иммунологическую эффективность противовирусной терапии (ПВТ) хронического гепатита С (ХГС), осложнённого развитием вторичной cмешанной криоглобулинемии с использованием препаратов прямого противовирусного действия (ППД) в условиях реальной клинической практики. Материалы и методы: в исследование включено 12 больных ХГС (без ко-инфекции ВИЧ, вирусом гепатита В), осложнённым развитием смешанной криоглобулинемии с криокритом более 5% и наличием клинических проявлений криоглобулинемии. Проводилась терапия препаратами ППД: 2 пациента получали даклатасвир и асунапревир, 3 пациента – даклатасвир и софосбувир и 7 пациентов – Дасабувир; Омбитасвир+Паритапревир+Ритонавир. Результаты: среди всех включённых в исследование пациентов устойчивый вирусологический ответ на 12-й и 24-й неделях наблюдения отмечен у 91,6% (11/12). У 1 пациентки (на схеме даклатасвир и асунапревир) развилась резистентность к обоим препаратам. Клиническая эффективность составила 83% – 10/12 (25% – полный ответ, 58% – частичный ответ). Два пациента с тяжёлой нефрологической патологией, достигнув УВО, клинического ответа со стороны почек не достигли. В случаях частичного ответа чаще всего персистировали (с положительной тенденцией) нефрологические симптомы. Летальных исходов в ходе терапии и в периоде 24-недельного наблюдения не было. Один пациент умер на 25-й неделе наблюдения от двусторонней пневмонии на фоне тромбоэмболии мелких ветвей лёгочной артерии, осложнившей патогенентическую терапию преднизолоном и цитостатиками, назначенную в связи с отсутствием клинического ответа на ПВТ со стороны почек. Иммунологическая эффективность: у 25% пациентов произошла элиминация криоглобулинов уже к моменту завершения ПВТ, у 75% – снижение уровня криокрита. Заключение: полученные данные демонстрируют вирусологическую, клиническую и иммунологическую эффективность и безопасность ПВТ ППД, особенно при использованием схем с высоким генетическим барьером (даклатасвир и софосбувир, Дасабувир; Омбитасвир+Паритапревир+Ритонавир)

    Влияние дексаметазона и лидокаина на цитокиновый профиль и кровоточивость при эндоскопических риносинусохирургических вмешательствах

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    The objective: to evaluate the feasibility of using dexamethasone and lidocaine to potentiate the effect of anesthesia in patients with chronic polypous rhinosinusitis during functional endoscopic sinus surgery (FESS) interventions.Subjects and Methods. Clinical data, blood serum samples were collected prospectively from 52 patients who underwent FESS intervention. The patients were divided into 3 groups: Control Group ‒ C (n = 26), anti-inflammatory drugs were not administered; Dexamethasone Group ‒ D (n = 13), dexamethasone was administered (0.10‒0.15 mg/kg); and Lidocaine Group ‒ L (n = 13), a 1% solution of lidocaine was administered intravenously. The following parameters were studied: IL-6, IL-10, IL-18, alpha1-antitrypsin, and ferritin.Results. An increase of IL-6, IL-6/IL-10 was observed in Group C. An increase of IL-10 and a decrease of IL-6, IL-6/IL-10 were noted in Group D. In Group L, IL-6, IL-6/IL-10 did not change significantly. The intensity of bleeding was lower in Groups L (p < 0.001) and D (p < 0.05) versus Group C. Relative changes in the concentration of biomarkers within the normal range were detected in all groups.Conclusions. Changes in the cytokine profile are insignificant in patients with chronic polyposis rhinosinusitis during FESS performed under combined anesthesia.No convincing data on the need for intraoperative use of dexamethasone or intravenous lidocaine have been received.Цель: оценить целесообразность использования дексаметазона и лидокаина для потенцирования эффекта анестезии у больных хроническим полипозным риносинуситом при эндоскопических риносинусохирургических (ЭРСХ) вмешательствах.Материалы и методы. Клинические данные, образцы сыворотки крови были собраны проспективно у 52 больных, перенесших ЭРСХ-вмешательства. Сформировано три группы: контрольная (К, n = 26), в которой больным не вводили дексаметазон и лидокаин; группа Д (n =13), в которой использовали дексаметазон (0,10‒0,15 мг/кг), и группа Л (n = 13), где во время анестезии внутривенно вводили 1%-ный раствор лидокаина. Исследуемые показатели: ИЛ-6, ИЛ-10, ИЛ-18, альфа1-антитрипсин и ферритин.Результаты. Прирост ИЛ-6, ИЛ-6/ИЛ-10 наблюдался в группе К. В группе Д концентрация ИЛ-6 и соотношение ИЛ-6/ИЛ-10 снижались, а уровень ИЛ-10 нарастал. В группе Л ИЛ-6, ИЛ-6/ИЛ-10 значимо не изменились. Проявления кровоточивости в группах Л (p < 0,001) и Д (p < 0,05) были ниже, чем в группе К. Изменения концентрации других изученных биомаркеров не выходили за пределы нормы.Выводы. Изменения цитокинового профиля у больных с хроническим полипозным риносинуситом при ЭРСХ-вмешательствах, выполняемых в условиях сочетанной анестезии, являются незначительными. Убедительных данных о необходимости интраоперационного применения дексаметазона или внутривенного лидокаина не получено

    Эрадикация вируса гепатита с у пациентки с криоглобулинемическим васкулитом и наличием мутаций D168E, L31V

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    The case of chronic hepatitis C 1b genotype with grade 3 fibrosis according to Metavir, complicated by the development  of mixed  type  III  cryoglobulinemia,  cryoglobulinemic vasculitis with damage to the skin vessels of the skin (hemorrhagic vasculitis), and the liver (alternatively proliferative vasculitis) is demonstrated. The introduction of daclatasvir + asunaprevir was virologically unsuccessful: mutations D168E and L31V were detected against  the background of a  virological breakthrough. A repeated course of antiviral therapy with the combination of Grazoprevir + Elbasvir in combination with sofosbuvir led to a stable virologic response, partial immunological and clinical remission.В статье демонстрируется случай хронического гепатита С 1b генотипа с фиброзом 3 степени по Metavir, осложнённый развитием  смешанной криоглобулинемии III типа, криоглобулинемическим васкулитом с поражением сосудов кожи  (геморрагический васкулит), печени (альтеративно-пролиферативный  васкулит).  Назначение  режима  даклатасвир  +  асунапревир  оказалось вирусологически  неудачным:  на  фоне  вирусологического прорыва были  выявлены мутации D168E и L31V. Повторный  курс противовирусной терапии  комбинацией Гразопревир+Элбасвир  в  сочетании  с  софосбувиром привел  к  достижению  устойчивого  вирусологического ответа,  частичным  иммунологической  и  клинической ремиссиям
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