Cytokines and their role in immune pathogenesis of allergy

As, Simbirtsev

doi:10.32364/2587-6821-2021-5-1-32-37

Cited by 13 publications

(2 citation statements)

References 36 publications

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“…В настоящее время описано более 240 дифференцировочных антигенов, которые являются мембранными белками клеток иммунной системы [1]. Многие из них имеют растворимые формы, которые циркулируют в кровотоке и являются важнейшими звеньями глобальной иммунологической сети.…”

Section: Introductionunclassified

Concentration of soluble CD 25 in patients with colorectal cancer

Четверяков¹,

Цепелев²

2022

Nauchno-Prakticheskii Zhurnal «Patogenez»

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Актуальность. Растворимая форма CD25 - субъединица альфа рецептора интерлейкина-2 (sIL-2Rα, sСD25) может выступать как диагностический маркёр, определять прогноз течения заболевания и отражать результаты терапии злокачественного новообразования. Цель исследования. Оценка уровня sСD25 в сыворотке крови, ткани опухоли и лимфатических узлов у пациентов с новообразованиями толстого кишечника. Материалы и методы: В исследование были включены 44 пациента с колоректальным раком, 25 больных с доброкачественными опухолями толстого кишечника. Контрольную группу составили 25 пациентов, оперированных в плановом порядке (пластика колостомы), сформированной по поводу травмы толстой кишки. Концентрацию CD25 определяли в сыворотке крови, а также в супернатанте гомогената ткани опухоли (в контроле - ткани кишки) и лимфатических узлов с помощью метода проточной цитофлуометрии на анализаторе CytoFlex LX (Beckman Coulter, США), используя набор для мультиплексного анализа LEGENDplex™ HU (Immune Checkpoint, США). Результаты: Установлено, что высокий уровень sCD25 наблюдается в обеих группах пациентов с новообразованиями толстого кишечника, но в большей степени - у больных с колоректальным раком. У больных с раком толстой кишки в сыворотке крови уровень sCD25 увеличивается в сравнении с группой контроля в 6,9 [5,21; 8,73] раза (p < 0,001). Концентрация sCD25 в сыворотке крови пациентов с колоректальным раком превышала данный показатель у больных с доброкачественными опухолями в 1,59 [1,36; 2,36] раза (p = 0,003). Концентрация sCD25 в опухолевой ткани в группе больных с колоректальным раком была выше в 6,75 [5,73; 8,73] раза в сравнении с группой контроля (p < 0,001) и в 2,06 [1,60; 2,52] раза по отношению к группе больных с доброкачественной опухолью толстого кишечника (p = 0,001). Уровень sCD25 в ткани лимфатических узлов у больных с раком толстой кишки составил 1828,6 [1777,0; 3121,8] пг/мл. Выявлено, что при уровне sCD25 в сыворотке крови выше 85,9 пг/мл имеется высокая вероятность наличия онкологической патологии толстого кишечника. Уровень sCD25 в сыворотке крови обладает относительно сильной теснотой связи с уровнем sCD25 в ткани. Заключение: Результаты исследований показывают увеличение уровня sCD25 в сыворотке крови и ткани опухоли у больных с новообразованием толстого кишечника в сравнении с контрольной группой. Наиболее высокие значения уровня sCD25 отмечается у пациентов с колоректальным раком. Background: Soluble CD25, an interleukin-2 alpha receptor subunit (sIL-2Ra, sSD25), can be considered as a diagnostic marker that predicts the disease course and outcome in patients with malignant tumors. Aim: To assess the concentration of CD25 in blood serum and tumor tissue in patients with colorectal cancer (CRC). Materials and methods: The study enrolled 44 patients with colorectal cancer and 25 patients with benign colon tumors. The control group consisted of 25 patients who had been operated for colon injury. Concentrations of sCD25 were measured in blood serum and in the supernatant of tumor tissue (intestinal tissue in control) and lymph node homogenates by flow cytometry on a CytoFlex LX analyzer (Beckman Coulter, USA) with a LEGENDplex ™ HU multiplex analysis kit (Immune Checkpoint, USA). Significance of differences was determined with the nonparametric Mann-Whitney U test. Results: High concentrations of sCD25 were observed in both patient groups with large intestinal neoplasms, but they were higher in patients with colorectal cancer. In patients with colon cancer, the serum concentration of sCD25 was increased by 6.9 [5.21; 8.73] times compared to the control group (p < 0.001) and by 1.59 [1.36; 2.36] times (p = 0.003) compared to patients with benign tumors. The tumor tissue concentration of sCD25 was 6.75 [5.73; 8.73] times higher in CRC patients than in the control group (p < 0.001) and 2.06 [1.60; 2.52] times higher than in patients with benign colon tumor (p = 0.001). The lymph node tissue concentration of sCD25 was 1828.6 [1777.0; 3121.8] pg/ml in patients with colorectal cancer. It was found that a serum concentration of sCD25 higher than 85.9 pg/ml was associated with a high probability of large intestinal oncology. The serum concentration of sCD25 relatively strongly correlated with its tissue concentration. Conclusion: The study showed than serum and tissue concentrations of sCD25 were increased in patients with colon neoplasms compared to the control group. The highest sCD25 concentrations were observed in patients with colorectal cancer.

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Section: Introductionunclassified

Concentration of soluble CD 25 in patients with colorectal cancer

Четверяков¹,

Цепелев²

2022

Nauchno-Prakticheskii Zhurnal «Patogenez»

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“…A mechanism that underlies developing allergic diseases is known to be associated with the disrupted immune regulation, imbalanced activation of allergen-specific Тh2clones, IgE synthesis by В-lymphocytes, infiltration and activation of eosinophils, basophils and mast cells in an inflammatory nidus migrating through capillary vessel walls and intersticium. All this makes high demands of extracellular matrix degradation determined by matrix metalloproteinases [12,13]. MMP9 is assumed to play a key role in tissue remodeling and recovery by degrading IV and V type collagen and elastin thereby facilitating cell migration.…”

mentioning

confidence: 99%

Risk of allergy and its immune phenotypes in children with MMP9 Q279R gene polymorphism

Starkova¹,

Dolgikh²,

Legostaeva³

et al. 2022

Health Risk Analysis

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Scientific research with its focus on allergic diseases relies on up-to-date molecular-genetic methods for identifying individual genetic variability; it seems an important stage in the implementation of programs with their aim to early detect and mitigate risks of such diseases. In this study, our aim was to identify features of immune regulation associated with Q279R MMP9 gene polymorphism (rs17576) and benzene contamination in biological media in children with allergic diseases. The test group included 33 children with allergic diseases; the reference group consisted of 40 relatively healthy children. CD-markers were identified with flow cytometry. Genotyping was performed with a real-time polymerase chain reaction. The research revealed elevated levels of total IgE, IL-4 and TNFalfa under elevated benzene contamination in biological media that were by 1.2–4.2 times higher in the examined children with allergic diseases than in the reference group (р = 0.006–0.03). Q279R MMP9 gene polymorphismin in children from the test group had authentically more frequent oc-currence of the GG and AG genotypes, by 1.7 times higher than in the reference group. This allows considering the allele G of the MMP9 gene as a sensitivity marker in children with allergic diseases (OR = 2.34; 95 % CI = 1.17–4.65). We established a growth by 2.8 times in total IgE level and greater IL-4 and TNFalfa expression, by 1.4 and 1.3 times accordingly, in carriers of the allele G against those carrying the homozygote AA genotype among the examined children with allergic diseases (р = 0.020–0.042). Logistic regression analysis established the adequacy of the dominant model (p = 0.01) and revealed a possible association between carriage of the AG and GG genotypes of Q279R MMP9 gene polymorphism and developing allergy (OR = 3.61; 95 % CI = 1.34–9.71). A risk of developing allergy combined with benzene contamination in biological media and gene polymorphism of matrix metalloproteinase MMP9 (rs17576) is by 2.1 times higher for the allele G carriers against the AA genotype carriers (RR = 2.08; 95 % CI = 1.13–3.83). This allows considering the allele G of the MMP9 Q279R gene as a sensitivity marker in children with allergic diseases.

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