Sirtuins and chemokines as markers of replicative and induced senescence of human endotheliocytes

Background. One of the factors of the pathogenesis of atherosclerosis and other cardiovascular diseases is induced endothelial senescence. In this regard, the urgent task of molecular biology and medicine is the search for molecules that affect the process of vascular endotheliocytes senescence.The aim. To assess the expression of Sirt-1,3,6 and chemokines IL-4, CXCL11 in the replicative and induced senescence of human endotheliocytes.Materials and methods. The study was conducted on the primary culture of isolated human umbilical vein endothelial cells (HUVECs). HUVECs were cultured under conditions of replicative (natural) and lipopolysaccharide induced senescence.Results. The synthesis of Sirt-1,3,6, IL-4 and CXCL11 was evaluated using western blot analysis. We revealed a decrease in Sirt-1,3,6 synthesis by 1.6–1.8 times (р < 0.05) in the conditions of HUVEC replicative senescence. Induced senescence of endotheliocytes is characterized by a more pronounced decrease (1.7–3.4 times; р < 0.05) in the Sirt-1,3,6 synthesis. CXCL11 synthesis increases by 1.4 times (р < 0.05) in replicative and by 3.4 times (р < 0.05) in induced HUVEC senescence. IL-4 synthesis increases by 4.7 times in conditions of induced HUVEC senescence and doesn’t have changes in replicative senescence of endotheliocytes.Conclusion. These data obtained indicate that sirtuins and chemokines play an important role in the development of endothelial dysfunction observed in natural and induced senescence

Levilimab clinical efficacy for interleukin-6 receptor inhibition in COVID-19 and its potential for treating cytokine release syndrome of other aetiologies

The COVID-19 mortality is associated with an increase in interleukin-6 (IL-6) levels. Levilimab is an anti–IL-6 receptor antibody with proven clinical efficacy in patients with severe COVID-19.The aim of the study was to assess the association of COVID-19 severity and levilimab effectiveness with IL-6 levels and to explore the potential for using levilimab in other conditions accompanied by cytokine release syndrome.Materials and methods: the subgroup analysis was based on the data of COVID patients with known baseline IL-6 levels from the CORONA clinical study. Subgroups were formed according to baseline IL-6 levels: ≤5 pg/mL (normal) and >5 pg/mL (elevated). The subgroup analysis included descriptive statistics of the patients and time courses of their clinical and laboratory findings (at screening, on the day of investigational product administration, and further until day 14). In order to compare the percentages of patients who had required rescue therapy, the authors used Fisher's exact test.Results: the subgroup analysis included 91 patients (47 from the levilimab group and 44 from the placebo group). At baseline, the authors observed elevated levels of IL-6 in 31/47 (66%) subjects in the levilimab group and 29/44 (48.4%) subjects in the placebo group. The subjects with elevated IL-6 demonstrated more pronounced clinical signs of pneumonia and abnormalities in inflammatory markers. Elevated baseline IL-6 levels were associated with the need for rescue therapy (OR=3.714; 95% CI: 1.317–9.747; p=0.0183); this association was stronger in the placebo group (OR=8.889; 95% CI: 2.098–33.31; p=0.0036). Also, the placebo group showed long-term abnormalities in the clinical and laboratory findings.Conclusions: IL-6 is one of the key elements in the pathogenesis of cytokine release syndrome related to COVID-19 and other conditions. Elevated IL-6 levels are associated with the severity of COVID-19. Inhibition of IL-6 receptors by levilimab leads to clinical improvement in patients with severe COVID-19, suggesting the effectiveness of levilimab in pathogenesis-oriented therapy for cytokine release syndrome of other aetiologies

Клиническая эффективность ингибирования рецептора интерлейкина-6 при COVID-19 левилимабом и перспективы его применения при синдроме высвобождения цитокинов другой этиологии

The COVID-19 mortality is associated with an increase in interleukin-6 (IL-6) levels. Levilimab is an anti–IL-6 receptor antibody with proven clinical efficacy in patients with severe COVID-19.The aim of the study was to assess the association of COVID-19 severity and levilimab effectiveness with IL-6 levels and to explore the potential for using levilimab in other conditions accompanied by cytokine release syndrome.Materials and methods: the subgroup analysis was based on the data of COVID patients with known baseline IL-6 levels from the CORONA clinical study. Subgroups were formed according to baseline IL-6 levels: ≤5 pg/mL (normal) and >5 pg/mL (elevated). The subgroup analysis included descriptive statistics of the patients and time courses of their clinical and laboratory findings (at screening, on the day of investigational product administration, and further until day 14). In order to compare the percentages of patients who had required rescue therapy, the authors used Fisher's exact test.Results: the subgroup analysis included 91 patients (47 from the levilimab group and 44 from the placebo group). At baseline, the authors observed elevated levels of IL-6 in 31/47 (66%) subjects in the levilimab group and 29/44 (48.4%) subjects in the placebo group. The subjects with elevated IL-6 demonstrated more pronounced clinical signs of pneumonia and abnormalities in inflammatory markers. Elevated baseline IL-6 levels were associated with the need for rescue therapy (OR=3.714; 95% CI: 1.317–9.747; p=0.0183); this association was stronger in the placebo group (OR=8.889; 95% CI: 2.098–33.31; p=0.0036). Also, the placebo group showed long-term abnormalities in the clinical and laboratory findings.Conclusions: IL-6 is one of the key elements in the pathogenesis of cytokine release syndrome related to COVID-19 and other conditions. Elevated IL-6 levels are associated with the severity of COVID-19. Inhibition of IL-6 receptors by levilimab leads to clinical improvement in patients with severe COVID-19, suggesting the effectiveness of levilimab in pathogenesis-oriented therapy for cytokine release syndrome of other aetiologies.Смертность при COVID-19 ассоциирована с повышением уровня интерлейкина-6 (ИЛ-6). Левилимаб – моноклональное антитело к рецептору ИЛ-6 с доказанной клинической эффективностью у пациентов с тяжелым течением COVID-19.Цель работы: уточнить ассоциацию тяжести клинических проявлений COVID-19 и эффективности левилимаба с уровнем ИЛ-6 и определить возможность применения левилимаба при других состояниях, сопровождающихся синдромом высвобождения цитокинов.Материалы и методы: для подгруппового анализа использованы данные пациентов с COVID-19, участников клинического исследования CORONA, у которых был определен исходный уровень ИЛ-6. Подгруппы были сформированы на основании исходных значений уровня ИЛ-6: ≤5 пг/мл (нормальный уровень) и >5 пг/мл (повышенный уровень). Подгрупповой анализ включал описательную статистику и динамику клинико-лабораторных параметров пациентов изучаемых подгрупп на этапе скрининга, в день введения исследуемого препарата и далее до 14 суток. Сравнение долей пациентов, которым потребовалось назначения терапии спасения, было выполнено точным тестом Фишера.Результаты: в анализ включили 91 пациента (47 из группы пациентов, получивших левилимаб, и 44 из группы пациентов, получивших плацебо). Исходно повышенный уровень ИЛ-6 наблюдался у 31 (66%) из 47 в группе пациентов, получивших левилимаб, и 29 (48,4%) из 44 в группе пациентов, получивших плацебо. У пациентов с высоким уровнем ИЛ-6 наблюдались более выраженные клинические проявления пневмонии и отклонения показателей маркеров воспаления. Высокий уровень ИЛ-6 был ассоциирован с необходимостью назначения терапии спасения (ОШ=3,714; 95% ДИ 1,317–9,747; p=0,0183), в большей степени в группе пациентов, получивших плацебо (ОШ=8,889; 95% ДИ 2,098–33,31; p=0,0036), в которой также наблюдались длительно сохраняющиеся отклонения клинико-лабораторных параметров.Выводы: ИЛ-6 является одним из важнейших элементов патогенеза синдрома высвобождения цитокинов при COVID-19 и других состояниях. Повышенный уровень ИЛ-6 ассоциирован с более тяжелым течением COVID-19. Ингибирование рецепторов ИЛ-6 левилимабом приводит к клиническому улучшению у пациентов с тяжелым течением COVID-19, что позволяет предположить эффективность левилимаба в качестве патогенетической терапии синдрома высвобождения цитокинов различной этиологии

Эффективность и безопасность левилимаба в сочетании с метотрексатом при лечении пациентов с активным ревматоидным артритом, устойчивым к монотерапии метотрексатом (двойное слепое рандомизированное плацебо-контролируемое исследование III фазы, SOLAR)

Levilimab is anti-interleukin-6 receptor (IL6R) monoclonal antibody. The article presents data obtained during 24 weeks of the SOLAR phase III study.Objective: to confirm efficacy and safety of levilimab in combination with methotrexate (MTX) in patients with methotrexate resistant active rheumatoid arthritis (RA).Patients and methods. 154 adult patients, aged ≥18 years with the diagnosis of RA (ACR/EULAR 2010) and confirmed disease activity at screening despite treatment with MTX for at least 12 weeks (in a stable dose 15-25 mg/week). Patients were randomized 2:1 in levilimab (162 mg once a week, subcutaneously) + MTX (n=102) or placebo + MTX (n=52) group.The hypothesis of superiority of levilimab over placebo was tested for two co-primary efficacy endpoints: proportion of subjects who achieved ACR20 at week 12 and proportion of subjects who achieved low disease activity (LDA) of RA (DAS28-CRP <3.2) at week 24. Safety was assessed through monitoring of adverse events (AEs).Results and discussion. Seventy (68.6%) subjects who received levilimab and 20 (38.5%) who received placebo achieved ACR20 response at week 12. Fifty three (52%) subjects who received levilimab and 3 (5,8%) subjects who received placebo achieved LDA at week 24. The most common adverse events (reported in ≥5% of subjects) in levilimab and placebo arms, respectively were (by decreasing frequency): blood c holesterol increase (24% vs 12%), alanine aminotransferase elevation (11% vs 8%), lymphocyte count decrease (9% vs 8%), blood total bilirubin increase (11% vs 0%), blood triglycerides increase (10% vs 2%), aspartate aminotransferase elevation (7% vs 4%), positive interferon-gamma release assay (IGRA) with M.tuberculosis antigen blood test (5% vs 6%), absolute neutrophil count decrease (8% vs 0%). No deaths were occurred.Conclusion. The study confirmed superior efficacy of levilimab + MTX over placebo + MTX in subjects with MTX resistant active RA. Levilimab showed favorable safety profile and low immunogenicity. No new important safety risks were detected.Левилимаб – моноклональное антитело к рецептору интерлейкина 6. В статье приведены данные, полученные в ходе 24 нед исследования III фазы SOLAR.Цель исследования – подтвердить эффективность и безопасность левилимаба в комбинации с метотрексатом (МТ) у пациентов с активным ревматоидным артритом (РА), устойчивым к монотерапии МТ.Пациенты и методы. Рандомизировано 154 пациента в возрасте 18 лет и старше с установленным диагнозом РА (критерии ACR/EULAR, 2010) и подтвержденной активностью заболевания, несмотря на терапию МТ (в стабильной дозе 15–25 мг/нед) в течение ≥12 нед. Рандомизация проводилась в соотношении 2:1 в группу левилимаба (162 мг, 1 раз в неделю, подкожно) в комбинации с МТ (n=102) или плацебо в комбинации с МТ (n=52).Превосходство левилимаба над плацебо было оценено по двум ко-первичным конечным точкам: доля пациентов, достигших 20% улучшения в течении РА в соответствии с ACR20 на 12-й неделе исследования; доля пациентов с низкой активностью РА (DAS28-СРБ <3,2) на 24-й неделе. Безопасность лечения левилимабом в сочетании с МТ оценивалась на основании мониторинга нежелательных явлений (НЯ).Результаты и обсуждение. На 12-й неделе терапии ACR20 достигли 70 (68,6%) и 20 (38,5%) пациентов группы левилимаба и группы плацебо соответственно. Низкая активность РА на 24-й неделе исследования выявлена у 53 (52%) пациентов, получавших левилимаб в сочетании с МТ, и у 3 (5,8%) пациентов группы плацебо. Среди наиболее частых (развившихся у ≥5% пациентов) НЯ в группах левилимаба и плацебо соответственно были зарегистрированы (в порядке убывания частоты) следующие отклонения в показателях крови: повышение уровня холестерина (24 и 12%), повышение активности аланинаминотрансферазы (11 и 8%), снижение числа лимфоцитов (9 и 8%), повышение уровня общего билирубина (11 и 0%), повышение уровня триглицеридов (10 и 2%), повышение активности аспартатаминотрансферазы (7 и 4%), положительный тест высвобождения интерферона гамма с антигеном M. tuberculosis (5 и 6%) и снижение абсолютного числа нейтрофилов (8 и 0%). Летальных исходов не было.Заключение. Результаты исследования подтвердили, что у пациентов с РА, устойчивых к монотерапии МТ, левилимаб в комбинации с МТ превосходит по эффективности плацебо с МТ. Левилимаб продемонстрировал благоприятный профиль безопасности и низкую иммуногенность. Не выявлено новых важных рисков, связанных с безопасностью

Analysis of CRP-CytR interactions at the Escherichia coli udp promoter.

Multiprotein complexes regulate the transcription of certain bacterial genes in a sensitive, physiologically responsive manner. In particular, the transcription of genes needed for utilization of nucleosides in Escherichia coli is regulated by a repressor protein, CytR, in concert with the cyclic AMP (cAMP) activated form of cAMP receptor protein (CRP). We studied this regulation by selecting and characterizing spontaneous constitutive mutations in the promoter of the udp (uridine phosphorylase) gene, one of the genes most strongly regulated by CytR. We found deletions, duplications, and point mutations that affect key regulatory sites in the udp promoter, insertion sequence element insertions that activated cryptic internal promoters or provided new promoters, and large duplications that may have increased expression by udp gene amplification. Unusual duplications and deletions that resulted in constitutive udp expression that depended on the presence of CytR were also found. Our results support the model in which repression normally involves the binding of CytR to cAMP-CRP to form a complex which binds to specific sites in the udp promoter, without direct interaction between CytR protein and a specific operator DNA sequence, and in which induction by specific inducer cytidine involves dissociation of CytR from cAMP-CRP and the RNA polymerase interaction with cAMP-CRP bound to a site upstream of then transcription start point. The stimulation of udp expression by CytR in certain mutants may reflect its stabilization of cAMP-CRP binding to target DNA and illustrates that only modest evolutionary changes could allow particular multiprotein complexes to serve as either repressors or transcriptional activators

Biological Characteristics of Polyurethane-Based Bone-Replacement Materials

A study is presented on four polymers of the polyurethane family, obtained using a two-stage process. The first composition is the basic polymer; the others differ from it by the presence of a variety of fillers, introduced to provide radiopacity. The fillers used were 15% bismuth oxide (Composition 2), 15% tantalum pentoxide (Composition 3), or 15% zirconium oxide (Composition 4). Using a test culture of human fibroblasts enabled the level of cytotoxicity of the compositions to be determined by MTT (3-[4,5-dimethylthiazol-2-yl]-2,5 diphenyl tetrazolium bromide) assay, along with variations in the characteristics of the cells resulting from their culture directly on the specimens. The condition of cells on the surfaces of the specimens was assessed using fluorescence microscopy. It was shown that introducing 15% bismuth, tantalum, or zinc compounds as fillers produced a range of effects on the biological characteristics of the compositions. With the different fillers, the levels of toxicity differed and the cells’ proliferative activity or adhesion was affected. However, in general, all the studied compositions may be considered cytocompatible in respect of their biological characteristics and are promising for further development as bases for bone-substituting materials. The results obtained also open up prospects for further investigations of polyurethane compounds

Effects of the chymase inhibitor fulacimstat on adverse cardiac remodeling after acute myocardial infarction—Results of the Chymase Inhibitor in Adverse Remodeling after Myocardial Infarction (CHIARA MIA) 2 trial

Background: Adverse cardiac remodeling is a major risk factor for the development of post myocardial infarction (MI) heart failure (HF). This study investigates the effects of the chymase inhibitor fulacimstat on adverse cardiac remodeling after acute ST-segment-elevation myocardial infarction (STEMI). Methods: In this double-blind, randomized, placebo-controlled trial patients with first STEMI were eligible. To preferentially enrich patients at high risk of adverse remodeling, main inclusion criteria were a left-ventricular ejection fraction (LVEF) ≤45% and an infarct size >10% on day 5 to 9 post MI as measured by cardiac MRI. Patients were then randomized to 6 months treatment with either 25 mg fulacimstat (n = 54) or placebo (n = 53) twice daily on top of standard of care starting day 6 to 12 post MI. The changes in LVEF, LV end-diastolic volume index (LVEDVI), and LV end-systolic volume index (LVESVI) from baseline to 6 months were analyzed by a central blinded cardiac MRI core laboratory. Results: Fulacimstat was safe and well tolerated and achieved mean total trough concentrations that were approximately tenfold higher than those predicted to be required for minimal therapeutic activity. Comparable changes in LVEF (fulacimstat: 3.5% ± 5.4%, placebo: 4.0% ± 5.0%, P = .69), LVEDVI (fulacimstat: 7.3 ± 13.3 mL/m2, placebo: 5.1 ± 18.9 mL/m2, P = .54), and LVESVI (fulacimstat: 2.3 ± 11.2 mL/m2, placebo: 0.6 ± 14.8 mL/m2, P = .56) were observed in both treatment arms. Conclusion: Fulacimstat was safe and well tolerated in patients with left-ventricular dysfunction (LVD) after first STEMI but had no effect on cardiac remodeling