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CD4CD25 T细胞的表面表型变化及对氧化应激反应的增强

Surface Phenotype Changes and Increased Response to Oxidative Stress in CD4CD25 T Cells.

作者信息

Yamamoto Yoshiki, Negoro Takaharu, Tada Rui, Narushima Michiaki, Hoshi Akane, Negishi Yoichi, Nakano Yasuko

机构信息

Department of Paediatrics, Tokyo Metropolitan Ebara Hospital, Tokyo 145-0065, Japan.

Department of Pharmacogenomics, School of Pharmacy, Showa University, Tokyo 142-8555, Japan.

出版信息

Biomedicines. 2021 May 29;9(6):616. doi: 10.3390/biomedicines9060616.

Abstract

Conversion of CD4CD25FOXP3 T regulatory cells (T) from the immature (CD45RA) to mature (CD45RO) phenotype has been shown during development and allergic reactions. The relative frequencies of these T phenotypes and their responses to oxidative stress during development and allergic inflammation were analysed in samples from paediatric and adult subjects. The FOXP3CD45RA population was dominant in early childhood, while the percentage of FOXP3CD45RO cells began increasing in the first year of life. These phenotypic changes were observed in subjects with and without asthma. Further, there was a significant increase in phosphorylated ERK1/2 (pERK1/2) protein in hydrogen peroxide (HO)-treated CD4CD25 cells in adults with asthma compared with those without asthma. Increased pERK1/2 levels corresponded with increased Ca response to T cell receptor stimulation. mRNA expression of peroxiredoxins declined in T from adults with asthma. Finally, CD4CD25 cells from paediatric subjects were more sensitive to oxidative stress than those from adults in vitro. The differential T sensitivity to oxidative stress observed in children and adults was likely dependent on phenotypic CD45 isoform switching. Increased sensitivity of T cells from adults with asthma to HO resulted from a reduction of peroxiredoxin-2, -3, -4 and increased pERK1/2 via impaired Ca response in these cells.

摘要

在发育过程和过敏反应期间,已显示未成熟(CD45RA)的CD4CD25FOXP3调节性T细胞(T细胞)可转变为成熟(CD45RO)表型。在儿科和成人受试者的样本中,分析了这些T细胞表型的相对频率及其在发育和过敏性炎症期间对氧化应激的反应。FOXP3CD45RA群体在幼儿期占主导地位,而FOXP3CD45RO细胞的百分比在生命的第一年开始增加。在有和没有哮喘的受试者中均观察到了这些表型变化。此外,与没有哮喘的成年人相比,哮喘成年人中过氧化氢(HO)处理的CD4CD25细胞中磷酸化ERK1/2(pERK1/2)蛋白显著增加。pERK1/2水平升高与T细胞受体刺激后Ca反应增加相对应。哮喘成年人的T细胞中过氧化物酶的mRNA表达下降。最后,在体外,儿科受试者的CD4CD25细胞比成人的细胞对氧化应激更敏感。儿童和成人中观察到的T细胞对氧化应激的差异敏感性可能取决于表型CD45亚型转换。哮喘成年人的T细胞对HO的敏感性增加是由于这些细胞中过氧化物酶2、3、4减少以及Ca反应受损导致pERK1/2增加所致。

https://cdn.ncbi.nlm.nih.gov/pmc/blobs/a9ad/8229188/9b55f62a832a/biomedicines-09-00616-g001.jpg

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