Activated CD27+PD-1+ CD8 T Cells and CD4 T Regulatory Cells Dominate the Tumor Microenvironment in Refractory Celiac Disease Type II

Gastro hep advances Pub Date : 2025-01-01 DOI:10.1016/j.gastha.2024.08.023

Tessa Dieckman , Mette Schreurs , Ciska Lindelauf , Ahmed Mahfouz , Caroline R. Meijer , Louise Pigeaud , Vincent van Unen , Gerd Bouma , Frits Koning

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Abstract

Background and Aims

Refractory celiac disease type II (RCDII) is characterized by a clonally expanded aberrant cell population in the small intestine. The role of other tissue-resident immune subsets in RCDII is unknown. Here, we characterized CD8 and CD4 T cells in RCDII duodenum at the single-cell level and in situ.

Methods

We applied mass cytometry on CD45⁺ duodenal cells derived from intestinal biopsies (n = 23) and blood samples (n = 20) from RCDII patients and controls. Additionally, we analyzed intestinal biopsies from celiac disease (n = 11) and RCDI (n = 2) patients. We performed single-cell RNA-sequencing on CD45⁺ duodenal cells derived from a RCDII patient, immunofluorescence staining for in situ analysis and flow cytometry for phenotyping of RCDII aberrant and CD8 T cells.

Results

Compared to healthy controls, we observed that CD27⁺PD-1⁺ memory CD8αβ cells and CD4 T regulatories (Tregs) were more abundant in RCDII duodenum (CD8 ∗∗0.0029; CD4 ∗∗∗0.0001). The CD27⁺PD-1⁺ memory CD8αβ cells expressed the tissue-resident marker CD69, immunoregulatory markers (TIGIT, HAVCR2, TNFRSF9), NKG2A, were enriched for activated pathways and displayed cytotoxic gene signatures (NKG7, PRF1, GZMA). The absence of CD103 accords with their localization in the lamina propria as determined by in situ analysis. The CD25⁺FoxP3⁺CD27⁺CD127^dim/- CD4 Tregs expressed IL1R2 and IL32 and costimulatory molecules (TNFSRS4, ICOS and TNFRSF18) and resided in the lamina propria as well. Flow cytometry confirmed the presence of the inhibitory receptor NKG2A on expanded duodenal CD8 T cells and HLA-E, the ligand for NKG2A, on expanded aberrant cells.

Conclusion

RCDII is characterized by the simultaneous presence of an activated CD27⁺PD-1⁺ memory CD8αβ T cell subset and CD4 Tregs, suggesting that checkpoint blockade with anti-NKG2A/PD-1 and/or anticytotoxic T lymphocyte antigen 4 may be an attractive treatment option.

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活化的CD27+PD-1+ CD8 T细胞和CD4 T调节细胞主导难治性乳糜泻II型肿瘤微环境

背景和目的：难治性乳糜泻II型（RCDII）的特点是小肠中细胞群的克隆扩增。其他组织驻留免疫亚群在RCDII中的作用尚不清楚。在这里，我们在单细胞水平和原位鉴定了RCDII十二指肠中的CD8和CD4 T细胞。方法：我们对来自RCDII患者和对照组的肠道活检（n = 23）和血液样本（n = 20）的CD45+十二指肠细胞进行了大规模细胞计数。此外，我们还分析了乳糜泻（n = 11）和RCDI （n = 2）患者的肠道活检。我们对来自RCDII患者的CD45+十二指肠细胞进行单细胞rna测序，免疫荧光染色进行原位分析，流式细胞术进行RCDII异常细胞和CD8 T细胞的表型分析。结果：与健康对照组相比，我们观察到CD27+PD-1+记忆性CD8αβ细胞和CD4 T调节细胞（Tregs）在RCDII十二指肠中更丰富(CD8∗0.0029；CD4∗∗∗0.0001)。CD27+PD-1+记忆性CD8αβ细胞表达组织驻留标记CD69、免疫调节标记（TIGIT、HAVCR2、TNFRSF9）、NKG2A，激活通路富集，显示细胞毒性基因特征（NKG7、PRF1、GZMA）。CD103的缺失符合原位分析确定的它们在固有层的定位。CD25+FoxP3+CD27+CD127dim/- CD4 treg表达IL1R2、IL32和共刺激分子（TNFSRS4、ICOS和TNFRSF18），也驻留在固有层中。流式细胞术证实抑制受体NKG2A存在于扩大的十二指肠CD8 T细胞上，而NKG2A的配体HLA-E存在于扩大的异常细胞上。结论：RCDII的特点是同时存在活化的CD27+PD-1+记忆CD8αβ T细胞亚群和CD4 Tregs，提示用抗nkg2a /PD-1和/或抗细胞毒性T淋巴细胞抗原4阻断检查点可能是一种有吸引力的治疗选择。

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