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Effect of indole-3-carbinol on transcriptional profiling of wound-healing genes in macrophages of systemic lupus erythematosus patients: an RNA sequencing assay

机译:吲哚-3-甲醇对系统性红斑狼疮患者巨噬细胞造成伤口愈合基因转录分析的影响:RNA测序测定

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Background Relapses and flares with delayed wound healing are among the main symptoms of systemic lupus erythematosus (SLE), a rheumatic autoimmune disease. The orientation of immune responses in SLE disease depends on the function of the population of macrophages. This study investigated the effect of indole-3-carbinol (I3C) on transcriptional profiling of macrophage-derived monocytes (MDMs) in four stages of the wound-healing process. Methods In the first phase of study, MDMs were generated from peripheral blood mononuclear cells of three new SLE cases (unmedicated) and two healthy controls. The cases and controls were then divided into I3C treated and untreated groups after 24 hours of exposure to I3C. Single-end RNA sequencing was performed using an Illumina NextSeq 500 platform. After comprehensive analysis among differentially expressed genes,CDKN1A,FN1andMMP15were validated by quantitative real-time polymerase chain reaction as upregulated ranked genes involved in wound-healing stages. Results The RNA sequencing analysis of treated cases and treated controls versus untreated cases and untreated controls (group 3 vs. group 4) revealed upregulation of various genes, for example:C1S,C1R,IGKV1-5,IGKV4-1,SERPING1,IGLC1andIGLC2in coagulation;ADAM19,CEACAM1andCEACAM8in M2 reprogramming;IRS1,FN1,THBS1andLIMS2in extracellular matrix organization; andSTAT1,THBS1andATP2A3in the proliferation stage of wound healing. Conclusions The results showed that treatment with I3C could modulate the gene expression involved in wound healing in SLE cases and healthy controls.
机译:背景技术与延迟伤口愈合的复发和耀斑是全身性狼疮红斑狼疮(SLE)的主要症状,是一种风湿的自身免疫疾病。 SLE疾病中免疫应答的取向取决于巨噬细胞群的功能。本研究研究了吲哚-3-甲烯醇(I3C)对伤口愈合过程的四个阶段的巨噬细胞衍生的单核细胞(MDMS)转录分析的影响。方法在第一阶段的研究中,从三个新的SLE病例(未学)和两种健康对照的外周血单核细胞产生MDMS。然后在暴露于I3C的24小时后将病例和对照分为I3C处理和未处理的基团。使用Illumina NextSeq 500平台进行单端RNA测序。通过定量实时聚合酶链反应进行差异表达基因,CDKN1A,FN1Admp115were验证,作为伤口愈合阶段的上调排名基因验证。结果治疗病例及治疗对照对未处理病例和未处理对照(第3组第4组)的RNA测序分析显示出各种基因的上调,例如:C1S,C1R,IGKV1-5,IGKV4-1,六r,IgLC1AdtiGLC2IN凝固; adam19,ceacam1andceacam8in m2重新编程; IRS1,FN1,THBS1ANDLIMS2IN细胞外矩阵组织; Andstat1,thbs1andatp2a3在伤口愈合的增殖阶段。结论结果表明,用I3C治疗可以调节SLE病例和健康对照中伤口愈合所涉及的基因表达。

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