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Microarray data of transcriptome shifts in blood cell subsets during S1P receptor modulator therapy

机译:S1P受体调节剂治疗期间血细胞亚群转录组转移的微阵列数据

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摘要

Treatment with fingolimod, a sphingosine-1-phosphate (S1P) receptor modulator, prevents the egress of immune cell subpopulations from lymphoid tissues into the blood. We obtained peripheral blood samples from patients with relapsing multiple sclerosis before the initiation of fingolimod therapy, after one day and after 3 months. To investigate the differential expression induced by the drug, five different cell populations were isolated. We then employed 150 Human Transcriptome Arrays (HTA 2.0) interrogating >245,000 protein-coding and >40,000 non-coding transcript isoforms. After 3 months of treatment, CD4+ and CD8+ T-cells showed huge transcriptome shifts, whereas the profiles of B-cells (CD19+) were slightly altered and those of monocytes (CD14+) and natural killer cells (CD56+) remained unaffected. With >6 million probes for exons and splice junctions, our large HTA 2.0 dataset provides a deep view into alternative splicing patterns in immune cell subsets. Our data may also be useful for comparing the effects on gene expression signatures of novel S1P receptor modulators, which are currently tested in clinical trials for other autoimmune and neurodegenerative diseases.
机译:用芬戈莫德(一种鞘氨醇1磷酸酯(S1P)受体调节剂)进行治疗,可防止免疫细胞亚群从淋巴组织渗入血液。我们从芬戈莫德治疗开始前,一天后和3个月后从患有复发性多发性硬化症的患者中获取外周血样本。为了研究药物诱导的差异表达,分离了五个不同的细胞群。然后,我们采用了150个人类转录组阵列(HTA 2.0)来询问> 245,000个蛋白质编码和> 40,000个非编码转录本亚型。经过3个月的治疗,CD4 +和CD8 + T细胞显示出巨大的转录组移动,而B细胞(CD19 +)的分布略有改变,单核细胞(CD14 +)和自然杀伤细胞(CD56 +)的分布不受影响。我们的大型HTA 2.0数据集拥有600万个外显子和剪接点探针,可深入了解免疫细胞亚群中的其他剪接模式。我们的数据还可用于比较新型S1P受体调节剂对基因表达特征的影响,这些调节剂目前正在其他自体免疫和神经退行性疾病的临床试验中进行测试。

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