Cluster analysis of blood serum inflammation markers of conditionally healthy people

Determination of inflammatory markers in blood of conventionally healthy people is of interest due to opportunity of detecting diseases at early (preclinical) stages, as well as latent forms of pathological processes. The level of inflammation may serve as an additional criterion to forming control groups in clinical and biological studies. The aim of the study is to identify some inflammatory and autoimmune markers in a group of conventionally healthy people and to conduct a cluster analysis of the data obtained. The study involved 100 apparently healthy people (without clinical signs of infections, somatic, neurological or mental diseases) aged 19 to 88 years. The levels of IL-10, TNFα, IL-6 and autoantibodies to S100b and MBP were determined in blood serum using ELISA. Enzymatic activity of leukocyte elastase (LE) and functional activity of the α1-proteinase inhibitor (α1-PI) were determined spectrophotometrically. Protease inhibitory index (PII) was calculated as the ratio of LE to α1-PI. Cluster analysis, as well as the Shapiro–Wilk, Kruskal–Wallis, and ANOVA methods were used as the main approach to statistical data processing. All the subjects were divided into three clusters, according to their immunological parameters. The selected clusters were statistically significantly different from each other, in terms of LE activity, protease-inhibitory index (PII), as well as IL-10 and TNFα levels. The indices of a distinct cluster (43% of total cohort) are most close to average indices assessed for the general sample, which gives ground to consider the values of immune indicators from this cluster as physiological norm, corresponding to the background immunity state in healthy people. Combination of immunological parameters in two other clusters (30 and 27% of the subjects, respectively) may reflect different variants of inflammatory reactions. These clusters are characterized by multidirectional changes in LE activity and protease-inhibitory index, compared to the standard values, thus suggestive for different variants of latent inflammatory reactivity, which are realized in the patients presented in these clusters. The obtained clusters did not differ by age of the subjects (p = 0.3476), which makes it possible to exclude a significant influence of age on the determined immune parameters, and by gender characteristics (p = 0.7233). The selected clusters did not differ statistically in the functional activity of α1-PI and in the level of autoantibodies to S100b and MBP. Thus, the group of conditionally healthy people is heterogeneous in terms of inflammation markers. Inflammatory reactions of varying severity were detected in about half of the cases. Probably, this may indicate the presence of a latent pathological process and requires a detailed clinical examination

Mesalazine use tactics in the ulcerative colitis patients

Aim of the lecture. To specify indications for the administration of the 5-aminosalicylic acid (5-АSA) in the patients with ulcerative colitis (UC) and to discuss the possibility of correlation between the body mass index, the disease activity and reasonability for the prescription of the mesalazine (Pentasa) as a monotherapy.Key points. 5-АSA is the first line drug for the UC patients. The efficacy has been demonstrated in a huge number of studies, the indications for the administration have been determined and are dependent on the disease activity index. 5-АSA are used in moderate rate of the inflammatory activity. This article discusses the question of the possible relation between the body mass loss during the disease, www.m-vesti.ru and the body mass index as the additional factors for the determining of the pathological process activity and the indications for the prescription of the 5-АSA drugs. The article points out the possibility of the mesalazine rectal suppositories use for proctitis in the patients with UC that increases the adhesion of the patients to the treatment.Conclusion. Mesazaline is efficient in the UC patients with both distal as well as extended forms of the disease. The additional factor which determines the disease activity is probably the patients’ nutritional status which is expedient to be taken into account while selecting the therapy

Innate and acquired immunity indices in assessing the clinical severity of patients with childhood schizophrenia

The results of previous studies suggest pathogenetic role of immune system in the development of schizophrenia. Examination of adolescent and young adult schizophrenic patients showed that the activity/ level of distinct parameters of innate and acquired immunity correlates with acuity and severity of pathological process in the brain. Presumably, evaluation of immune system characteristics in patients with childhood schizophrenia, concerning severity of their clinical symptoms, along with potential therapeutic aspect, may be the basis for early diagnosis of these conditions, and monitoring and prognosis of the further progression of the disease. The objective of our study was to compare clinical and immunological indices in children with schizophrenia to analyze the possibility of using these parameters for determination of the degree of activity of the pathological process. Sixty-two patients (39 boys and 23 girls) from 4 to 17 years of age with childhood schizophrenia were examined. Psychopathological and psychometric methods (PANSS and CGI-S scales) were used to assess mental state of the patients. Immunological parameters were determined in blood serum taken by fingerprick. Activity of leukocyte elastase (LE) and a1-proteinase inhibitor (a1-PI) was determined by spectrophotometric method. To determine the level of autoantibodies to S-100B and MBP, we used enzyme immunoassay. The study revealed activation of innate (by activity of LE and a1-PI) and acquired (by the level of autoantibodies to S-100B and MBP neuroantigens) immunity markers in blood serum of children with schizophrenia. Correlation analysis showed the significant positive correlation between complex evaluation of activation level of the immune system and severity of the patients’ state on the CGI-S scale (r = 0.64, p < 0.0001), as well as severity of negative symptoms according to the PANSS scale (r = 0.34, p = 0.0077). The revealed correlations suggest an opportunity for using immunological parameters (LE and a1-PI activity, and antibodies to neuroantigens), as the additional laboratory criteria for the assessment of clinical state in patients with childhood schizophrenia

Efficacy of mesalazine at ulcerative colitis with nutritional failure

Aim of investigation. To specify relation between trophological status, severity of relapse of ulcerative colitis (UC) and efficacy of 5-aminosalicylic acid (5-ASA) for achievement of clinical remission.Summary. Nutritional status plays important role for body recovery at relapse of chronic diseases, including UC. At patients with nutritional failure remission achievement time becomes longer, bed-stay duration is increased. On the other hand, overweight patients often have more severe course of UC, as it affects important pathogenic processes. This article discusses possible links between trophological status and achievement of clinical remission, as well as between nutritional failure at UC and efficacy of mesalazine monotherapy.Conclusion. More severe course of UC, long bedstay, lower mesalazine efficacy are marked at patients with nutritional failure in comparison with those scores at patients with normal trophological status. At over-weight patients in comparison with patients with normal nutritional status no significant differences in specified parameters is observed

Severe Diverticulitis Associated to <i>Clostridioides difficile</i> Infection in a 91 Year Old Patient (Clinical Case)

Aim. To present a clinical case of a 91-year-old patient with a severe course of diverticulitis combined with the development of Clostridioides difficile-associated disease.Key points. On admission the patient complained of pain in the left iliac region, increased body temperature, constipation and bloating. The medical history showed that constipation increased on the background of prolonged bed rest and discontinuation of psyllium. According to the laboratory and instrumental examinations, the patient had signs of acute diverticulitis, antibacterial therapy was corrected twice, positive dynamics of the condition was noted. However, a few days later, the patient developed a clinic of C. difficile-associated disease, which required the prescription of anticlostridial therapy (vancomycin), until the laboratory confirmation of the accession of this infection was obtained. Combined therapy of exacerbation of diverticular disease and C. difficile-associated disease made it possible to achieve a steady improvement of the condition.Conclusion. The exclusion of possible development of C. difficile-associated disease on the background or prior antibiotic therapy is an important condition for correct and adequate management of a patient with exacerbation of diverticular disease. If the patient develops a clinical picture of C. difficile-associated disease, treatment may be initiated before laboratory confirmation

ТЕХНОЛОГИЧЕСКАЯ ПОДДЕРЖКА ДЛЯ ОБУЧЕНИЯ В УНИВЕРСИТЕТЕ

This paper aims to show the advantages innovative technologies provide in education. The advent of the technological era has indelibly changed the face of education. When appropriately applied in classrooms, technology affects how instruction is delivered, how students access and process information, and how learning is assessed.Эта статья призвана показать преимущества инновационных технологий представленных в образовании. Приход технологической эры изменил лицо образования. При соответствующем применяется в классах, технологии являются инструкцией по доставке информации и тому как студенты получают доступ и обрабатывают информацию и как обучение оценивается

Токсичность и эффективность комбинации гемцитабина и nab-паклитаксела (паклитаксел + альбумин) в Российской популяции больных раком поджелудочной железы: результаты многоцентрового ретроспективного исследования

Introduction. The results of randomized MPACT study have demonstrated that the addition of nab-paclitaxel to gemcitabine leads to a statistically significant increase in life expectancy. The main objective of this retrospective study was to obtain up-to-date efficacy and toxicity data for this drug combination in Russian real-world clinical setting.Materials and methods. The study enrolled patients with morphologically confirmed locally advanced or metastatic pancreatic cancer who had ECOG Performance Status scores of 0-2 and received treatment with gemcitabine and nab-paclitaxel. Immediate and long-term outcomes, as well as treatment toxicity and dose modifications, were assessed.Results. The study included 142 patients who received treatment from 2009 to 2019 at 17 centers in 11 regions of Russia. Full dose gemcitabine and nab-paclitaxel were administered at baseline in 74 % of the cases. The median number of chemotherapy cycles was 4 (range, from 1 to 16). Nab-paclitaxel dose was reduced in 32 % of the cases, and that of gemcitabine in 23 % of them. Regression analysis revealed no prognostic factors associated with increased toxicity of gemcitabine and nab-paclitaxel administration. However, previous use of two or more chemotherapy lines had an impact on decisions made by physicians, making them reduce the baseline dose of gemcitabine and/or nab-paclitaxel (OR=6.1, 95% CI 1.5-24.2, р=0.010). An objective response was assessed in 134 subjects with positive response observed in 34 cases (25.4 %). The median time to progression was found to be 6.1 months, and the median life expectancy was 14.2 months.Conclusions. The combination of gemcitabine and nab-paclitaxel exhibits comparatively high efficacy. The acceptable toxicity profile allows its use in selected patients even with ECOG 2 and in the presence of serious comorbidities.Введение. Результаты рандомизированного исследования MPACT продемонстрировали, что добавление к гемцитабину nab-паклитаксела приводит к статистически значимому увеличению продолжительности жизни. Задачей данного ретроспективного исследования является получение актуальных данных об эффективности и токсичности данной комбинации в реальной клинической практике в России.Материалы и методы. В исследование включались пациенты с морфологически доказанным местнораспространенным или метастатическим раком поджелудочной железы, имеющие общее состояние по шкале ECOG 0-2, которым проводилась терапия гемцитабином и nab-паклитакселом. Оценивались непосредственные и отдаленные результаты лечения, а также токсичность лечения и модификации доз препаратов.Результаты. В исследование включено 142 пациента, получивших лечение в период с 2009 по 2019 гг. в 17 центрах из 11 регионов России. Гемцитабин и nab-паклитаксел назначались исходно в полных дозах в 74% случаев. Медиана числа проведенных курсов химиотерапии составила 4 (1-16 курсов). В процессе химиотерапии доза nab-паклитаксела редуцировалась в 32 % случаев, гемцитабина — в 23 % случаев. Регрессионный анализ не выявил прогностических факторов, ассоциированных с повышенной токсичностью гемцитабина и nab-паклитаксела. Однако назначение ранее двух или более линий химиотерапии влияло на решение врачей в пользу исходной редукции дозы гемцитабина и/ или nab-паклитаксела (ОШ=6,1, 95 % ДИ 1,5-24,2, р=0,010). Оценка объективного эффекта произведена у 134 пациентов. Объективный ответ зарегистрирован в 34 (25,4%) случаях. Медиана времени без прогрессирования составила 6,1 месяца, медиана продолжительности жизни составила 14,2 месяца.Выводы. Комбинация гемцитабина и nab-паклитаксела обладает сравнительно высокой эффективностью. Приемлемый профиль токсичности позволяет применять ее у отобранных пациентов даже при статусе ECOG 2 и наличии серьезной сопутствующей патологии

Сравнение эффективности и токсичности афлиберцепта и бевацизумаба в комбинации с режимом FOLFIRI во 2‑й линии лечения пациентов с метастатическим раком толстой кишки: ретроспективный анализ многоцентрового исследования

Objective: to compare the efficacy and toxicity of aflibercept and bevacizumab in combination with fOLfIRI in secondline therapy for patients with metastatic colon cancer.Materials and methods. we performed a retrospective analysis of data on patients with metastatic colon cancer treated in 9 clinics in the Russian federation. The inclusion criteria were as follows: metastatic or locally advanced colon cancer; treatment with bevacizumab or aflibercept plus fOLfIRI in the second-line therapy. The primary outcome measure was progression-free survival (PfS). Secondary outcome measures included objective response rate and incidence of adverse events.Results. A total of 271 patients with metastatic colon cancer who received second-line therapy with bevacizumab (n = 81) or aflibercept (n = 190) between 2014 and 2018 were selected for this study. Study groups were matched for main prognostic signs. The objective response rate was 18.1 % in the bevacizumab group and 20.5 % in the aflibercept group (p = 0.7). The median PfS was 5 months (95 % confidence interval 3.8–6.1) in the aflibercept group and 7 months (95 % confidence interval 0.81–2.1) in the bevacizumab group (hazard ratio 1.4; 95 % confidence interval 0.99–2.1; p = 0.04). multivariate regression analysis demonstrated that the type of the targeted drug independently had no effect on PfS (hazard ratio 1.3; 95 % confidence interval 0.9–1.9; p = 0.2). we observed no statistically significant differences in the incidence of complications of any grades between the groups (58 % vs 72 %, p = 0.1). Patients receiving aflibercept were more likely to develop grade III–Iv arterial hypertension (2 % vs 9.5 %) and diarrhea (0 % vs 5.4 %), whereas thrombotic complications were more common in the bevacizumab group (10 % vs 1.8 %).Conclusion. we observed no significant differences in objective response rate and PfS between patients with metastatic colon cancer receiving bevacizumab or aflibercept in combination with fOLfIRI as second-line therapy. The toxicity profiles were different. Our findings can be used for choosing an optimal targeted drug for second-line treatment.Цель исследования – сравнение эффективности и токсичности афлиберцепта и бевацизумаба в комбинации с режимом fOLfIRI во 2-й линии лечения пациентов с метастатическим раком толстой кишки.Материалы и методы. Проведен ретроспективный анализ базы данных пациентов с метастатическим раком толстой кишки в рамках наблюдательного исследования работы 9 клиник РФ. Критерии включения в исследование: больные метастатическим или местно-распространенным раком толстой кишки; проведение терапии с включением бевацизумаба или афлиберцепта в комбинации с режимом fOLfIRI во 2-й линии лечения. Основной критерий эффективности – выживаемость без прогрессирования (ВбП). дополнительные критерии: частота объективных эффектов, частота развития нежелательных явлений.Результаты. Отобран 271 пациент с метастатическим раком толстой кишки, которым в 2014–2018 гг. проводилась 2-я линия терапия с включением бевацизумаба (n = 81) и афлиберцепта (n = 190). группы статически значимо не различались по основным прогностическим признакам. частота объективных эффектов составила 18,1 % в группе бевацизумаба и 20,5 % в группе афлиберцепта (р = 0,7). медиана ВбП составила 5 мес (95 % доверительный интервал 3,8–6,1) в группе афлиберцепта и 7 мес (95 % доверительный интервал 0,81–2,1) в группе бевацизумаба (отношение рисков 1,4; 95 % доверительный интервал 0,99–2,1; р = 0,04). многофакторный регрессионный анализ не подтвердил независимого влияния характера таргетного препарата на ВбП (отношение рисков 1,3; 95 % дИ 0,9–1,9; р = 0,2). Не отмечено статистически значимых различий в частоте развития осложнений всех степеней (58 % против 72 %, р = 0,1); среди негематологических осложнений артериальная гипертензия III–Iv степени (2 % против 9,5 %) и диарея (0 % против 5,4 %) чаще наблюдались в группе афлиберцепта, тромботические осложнения чаще наблюдались в группе бевацизумаба (10 % против 1,8 %).Выводы. Не отмечено статистически значимых различий между бевацизумабом и афлиберцептом в сочетании с режимом fOLfIRI во 2-й линии терапии пациентов с метастатическим раком толстой кишки ни в отношении достижения объективного эффекта, ни в отношении ВбП. Профили токсических реакций были различными. Полученные данные можно учитывать при выборе таргетного препарата во 2-й линии терапии

Оценка токсичности и эффективности терапии комбинацией FOLFIRI и афлиберцепта при метастатическом раке толстой кишки в РФ: первые результаты многоцентрового ретроспективного исследования

oai:oai.tumors.elpub.ru:article/629Purpose. To assess the incidence and severity of adverse events; to explore clinical factors associated with grade 3–4 non-hematologic toxicity; to assess the immediate efficacy and progression-free survival during treatment with the FOLFIRI regimen in combination with aflibercept in Russia.Materials and Methods. A retrospective multicenter study has been conducted with data collected from 20 clinics in 15 regions of Russia. There was no statistical hypothesis. Progression-free survival was the main efficacy criterion. The statistical analysis was performed using IBM SPPS Statistics v. 20 software.Results. FOLFIRI and Aflibercept combination was administered to 264 patients. The mean number of treatment cycles was 6 (1 to 29). The toxicity of aflibercept was addressed by dose reduction and dosing delay in 10.1 % and 11.4 % of patients, respectively, and dose reductions and dosing delays in any of FOLIFRI components were reported in 20.1 % of participants. The objective response rate was 20.3 %. The median progression-free survival in patients receiving second-line treatment was 6 months (95 % CI: 5.3–6.6 months). Seventy-two percent of patients experienced any grade of adverse events most of which were limited to grade 1–2 (62.1 %). Non-hematologic toxicity was reported in 64 % of patients (grade 3–4 in 17.9 %). Hematologic events were detected in only 17.9 % of patients. Multifactorial analysis has shown that drug therapy for concomitant diseases (OR 1.98, 95 % CI: 1.04–3.78, p = 0.037) and the number of chemotherapy lines prior to aflibercept (ОR 1.5, 95 % CI: 1.06–2.11, p = 0.02) were independent predictors of grade 3–4 non-hematologic toxicity.Conclusions. Objective response rate, progression-free survival, and frequency of toxicity-related aflibercept discontinuations in the Russian study with patients receiving aflibercept in combination with FOLFIRI regimen as a second-line treatment has shown the results that were comparable with VELOUR study. Comorbidities requiring drug treatment and the number of prior chemotherapy lines appear to be risk factors for grade 3–4 nonhematological toxicity events. Цель исследования. Оценить частоту развития и тяжесть нежелательных явлений; изучить клинические факторы, ассоциированные с развитием негематологической токсичности 3-4 степени; оценить непосредственную эффективность выживаемость без прогрессирования при применении комбинации FOLFIRI с афлиберцептом в РФ.Материалы и методы. Проведено ретроспективное многоцентровое исследование. Собраны данные 20 клиник 15 регионов РФ. Статистическая гипотеза отсутствовала. В качестве основного критерия эффективности рассматривалась выживаемость без прогрессирования. Статистический анализ проводился с помощью программ статистического пакета SPSS (IBM SPPS Statistics v. 20).Результаты. Режим FOLFIRI афлиберцепт был назначен у 264 пациентов. Среднее число составило 6 (от 1 до 29). В связи с токсичностью доза афлиберцепта в процессе терапии была редуцирована у 10,1% пациентов, задержали очередное введение афлиберцепта — у 11,4%; отсрочка и редукция доз химиопрепаратов в режиме FOLFIRI описана у 20,1 %. Частота объективных эффектов составила 20,3%. Во второй линии терапии медиана выживаемости без прогрессирования составила 6 месяцев (95% ДИ 5,3-6,6 месяцев). Нежелательные явления любой степени зарегистрированы у 72 % пациентов и чаще были ограничены 1-2 степенью (62,1%). Негематологические осложнения развились у 64% (3-4 степень — у 17,9%). Гематологические осложнения представлены только у 17,9 % пациентов. По результатам многофакторного анализа лекарственная терапия по поводу сопутствующей патологии (ОШ 1,98, 95%ДИ 1,04-3,78, р=0,037) и число линий терапии (ОШ 1,5, 95%ДИ 1,06-2,11, р=0,02), предшествующих афлиберцепту, явились независимыми предсказывающими факторами развития нежелательных явлений негематологического профиля 3-4 степени.Выводы. Частота объективных эффектов, выживаемость без прогрессирования и частота отмены афлиберцепта в связи с токсическими реакциями при применении комбинации FOLFIRI + афлиберцепт во второй линии среди пациентов в РФ аналогична результатам исследования VELOUR. Сопутствующая патология, требующая медикаментозной коррекции, и число линий терапии предшествующих афлиберцепту, по-видимому, являются факторами риска развития негематологических явлений 3-4 степени

Факторы, ассоциированные с эффективностью комбинации FOLFIRI и афлиберцепта при метастатическом раке толстой кишки

Objective: to identify factors associated with efficacy of an aflibercept-chemotherapy combination in patients with metastatic colon cancer.Materials and methods. This retrospective multicenter study was conducted in 20 clinics from 15 regions of the Russian Federation. The main efficacy outcome was progression-free survival (PFS). We performed univariate and multivariate analysis to assess the impact of various factors of PFS.Results. Two hundred and fifty-seven patients received aflibercept-containing chemotherapy; of them, 175 participants (68.1 %) received it as a second-line therapy. The objective response rate and median PFS were 18.7% and 5 months (95% confidence interval (CI) 4.2—5.8) respec -tively. The following factors were found to have a positive effect of PFS at multivariate analysis: grade I—II adverse events to aflibercept therapy (hazard ratio (HR) 0.58; 95 % CI 0.38—0.89; p = 0.01), therapy for concomitant diseases (HR 0.47; 95 % CI 0.29—0.76; p = 0.002), and ECOG performance status of 0 (HR 0.53; 95 % CI 0.34—0.81; p = 0.004). Patient with all 3 factors present had median PFS of 9 months, whereas patients without them demonstrated PFS of only 3 months (HR 1.9; 95 % CI 1.5—2.6; p &lt;0.001).Conclusions. Satisfactory performance status, adequate therapy for concomitant diseases, and adverse events to aflibercept therapy were associated with better PFS in patients receiving aflibercept-containing chemotherapy.Цель исследования — выявить факторы, ассоциированные с эффективностью комбинации химиотерапии и афлиберцепта у больных метастатическим раком толстой кишки.Материалы и методы. Проведено ретроспективное многоцентровое исследование. Собраны данные 20 клиник из 15 регионов Российской Федерации. В качестве основного критерия эффективности рассматривали выживаемость без прогрессирования (ВБП). Был проведен одно- и многофакторный анализ влияния различных признаков на ВБП.Результаты. Двести пятьдесят семь пациентов получали терапию с включением афлиберцепта, в том числе во 2-й линии — 175 (68,1 %) больных. Объективный эффект и медиана ВБП составили 18,7 % и 5 мес (95 % доверительный интервал (ДИ) 4,2—5,8) соответственно. По результатам многофакторного анализа благоприятными факторами прогноза в отношении ВБП выступали развитие побочных явлений I—II степени тяжести при терапии афлиберцептом (отношение рисков (ОР) 0,58; 95 % ДИ 0,38—0,89; p = 0,01), назначение терапии по поводу сопутствующих заболеваний (ОР 0,47; 95 % ДИ 0,29—0,76; p = 0,002) и функциональный статус пациента ECOG 0 (ОР 0,53; 95 % ДИ 0,34—0,81; p = 0,004). При наличии всех 3 факторов медиана ВБП составила 9 мес, при их отсутствии — 3 мес (ОР 1,9; 95 % ДИ 1,5—2,6; p &lt;0,001).Выводы. Удовлетворительный функциональный статус пациента, медикаментозный контроль сопутствующей патологии и развитие нежелательных явлений в процессе терапии афлиберцептом ассоциированы с улучшением ВБП в популяции пациентов, которым проводится терапия с включением афлиберцепта