Exhausted Lag-3+ CD4+ T cells are increased in pediatric Inflammatory Bowel Disease.

IF 3.4 3区 医学 Q3 IMMUNOLOGY Clinical and experimental immunology Pub Date : 2024-07-24 DOI:10.1093/cei/uxae066
Alexander Schnell, Carmen Aicher, Philipp A Schnegelsberg, Benedikt Schwarz, Hannah Schmidt, Ida Allabauer, Aline Rückel, Adrian P Regensburger, Joachim Woelfle, André Hoerning
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Abstract

T cells are one of the main drivers of inflammatory bowel diseases (IBD). Infliximab (IFX) is used in the treatment of IBD as an anti-inflammatory drug to induce remission by neutralizing TNFα. We determined the individual chemokine/homing receptor and cytokine profile in pediatric IBD patients before and during IFX therapy to identify predictive biomarkers for therapy success. Peripheral blood CD4+ cells from pediatric patients with IBD were immunomagnetically isolated and either directly analyzed by FACS for cell distribution and chemokine/homing receptor expression or evaluated for cytokine production after in-vitro-stimulation. 21 responders (RS) and 21 non-responders (NRS) were recruited. Before IFX therapy, flow cytometry revealed decreased percentages of naïve conventional T cells in pediatric IBD patients. The proportions of CD62-L+ T cells were decreased in both CD and UC therapy responders. The cytokine profile of T cells was highly altered in IBD patients compared to healthy controls (HC). During IFX therapy, the frequencies of conventional memory and regulatory memory T cells expanded in both cohorts. IFX response was marked by a decrease of α4β7+ and IFNγ+ memory T cells in both CD and UC. In contrast, frequencies of Lag-3+ T cells proved to be significantly increased in NRS. These observations were irrespective of the underlying disease. T cells of pediatric IBD patients display an activated and rather Th1/Th17 shifted phenotype The increased expression of the checkpoint molecule Lag-3 on T cells of NRS resembles a more exhausted phenotype than in RS and HC which appeared to be a relevant predictive marker for therapy failure.

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小儿炎症性肠病中衰竭的 Lag-3+ CD4+ T 细胞增多。
T 细胞是炎症性肠病(IBD)的主要诱因之一。英夫利昔单抗(IFX)作为一种抗炎药物被用于治疗 IBD,通过中和 TNFα 诱导病情缓解。我们测定了小儿 IBD 患者在 IFX 治疗前和治疗期间的趋化因子/归巢受体和细胞因子谱,以确定治疗成功的预测性生物标志物。对小儿 IBD 患者的外周血 CD4+ 细胞进行免疫磁分离,并通过 FACS 直接分析细胞分布和趋化因子/归巢受体的表达,或在体外刺激后评估细胞因子的产生。共招募了 21 名应答者(RS)和 21 名非应答者(NRS)。在接受 IFX 治疗前,流式细胞术显示小儿 IBD 患者的幼稚常规 T 细胞比例下降。CD和UC治疗应答者的CD62-L+ T细胞比例均有所下降。与健康对照组(HC)相比,IBD 患者 T 细胞的细胞因子谱发生了很大变化。在 IFX 治疗期间,两组患者的常规记忆和调节性记忆 T 细胞的频率都有所增加。IFX反应的显著特点是,CD和UC患者的α4β7+和IFNγ+记忆T细胞均减少。相反,Lag-3+ T 细胞的频率在 NRS 中明显增加。这些观察结果与基础疾病无关。小儿 IBD 患者的 T 细胞表现出活化和 Th1/Th17 转移的表型 NRS T 细胞中检查点分子 Lag-3 表达的增加与 RS 和 HC 相比更像一种衰竭的表型,这似乎是治疗失败的相关预测指标。
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来源期刊
CiteScore
8.40
自引率
2.20%
发文量
101
审稿时长
3-8 weeks
期刊介绍: Clinical & Experimental Immunology (established in 1966) is an authoritative international journal publishing high-quality research studies in translational and clinical immunology that have the potential to transform our understanding of the immunopathology of human disease and/or change clinical practice. The journal is focused on translational and clinical immunology and is among the foremost journals in this field, attracting high-quality papers from across the world. Translation is viewed as a process of applying ideas, insights and discoveries generated through scientific studies to the treatment, prevention or diagnosis of human disease. Clinical immunology has evolved as a field to encompass the application of state-of-the-art technologies such as next-generation sequencing, metagenomics and high-dimensional phenotyping to understand mechanisms that govern the outcomes of clinical trials.
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