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表达肿瘤坏死因子受体2型的循环调节性T细胞在感染性休克患者中导致脓毒症诱导的免疫抑制。

Circulating Regulatory T Cells Expressing Tumor Necrosis Factor Receptor Type 2 Contribute to Sepsis-Induced Immunosuppression in Patients During Septic Shock.

作者信息

Gaborit Benjamin Jean, Chaumette Tanguy, Chauveau Marie, Asquier-Khati Antoine, Roquilly Antoine, Boutoille David, Josien Régis, Salomon Benoit L, Asehnoune Karim

机构信息

EA3826 Thérapeutiques Anti-Infectieuses, Nantes Université, Nantes, France.

Department of Infectious Diseases, Centre Hospitalier Universitaire Nantes, Nantes, France.

出版信息

J Infect Dis. 2021 Dec 15;224(12):2160-2169. doi: 10.1093/infdis/jiab276.

DOI:10.1093/infdis/jiab276
PMID:34019653
Abstract

BACKGROUND

Septic shock remains a major cause of death that can be complicated by long-term impairment in immune function. Among regulatory T (Treg) cells, the tumor necrosis factor receptor 2 positive (TNFR2pos) Treg-cell subset endorses significant immunosuppressive functions in human tumors and a sepsis mouse model but has not been investigated during septic shock in humans.

METHODS

We prospectively enrolled patients with septic shock hospitalized in intensive care units (ICU). We performed immunophenotyping and functional tests of CD4+ T cells, Treg cells, and TNFR2pos Treg cells on blood samples collected 1, 4, and 7 days after admission to ICU.

RESULTS

We investigated 10 patients with septic shock compared to 10 healthy controls. Although the proportions of circulating Treg cells and TNFR2pos Treg-cell subsets were not increased, their CTLA4 expression and suppressive functions in vitro were increased at 4 days of septic shock. Peripheral blood mononuclear cells from healthy donors cultured with serum from septic shock patients had increased CTLA4 expression in TNFR2pos Treg cells compared to TNFR2neg Treg cells.

CONCLUSIONS

In patients with septic shock, CTLA4 expression and suppressive function were increased in circulating TNFR2pos Treg cells. We identify TNFR2pos Treg cells as a potential attractive target for therapeutic intervention.

摘要

背景

脓毒性休克仍然是主要的死亡原因,可能会因免疫功能的长期损害而复杂化。在调节性T(Treg)细胞中,肿瘤坏死因子受体2阳性(TNFR2pos)Treg细胞亚群在人类肿瘤和脓毒症小鼠模型中具有显著的免疫抑制功能,但在人类脓毒性休克期间尚未进行研究。

方法

我们前瞻性地纳入了入住重症监护病房(ICU)的脓毒性休克患者。我们对入住ICU后第1、4和7天采集的血样进行了CD4 + T细胞、Treg细胞和TNFR2pos Treg细胞的免疫表型分析和功能测试。

结果

我们研究了10例脓毒性休克患者,并与10名健康对照进行比较。尽管循环Treg细胞和TNFR2pos Treg细胞亚群的比例没有增加,但在脓毒性休克第4天时,它们的CTLA4表达和体外抑制功能增加。与TNFR2neg Treg细胞相比,用脓毒性休克患者血清培养的健康供体外周血单核细胞中,TNFR2pos Treg细胞的CTLA4表达增加。

结论

在脓毒性休克患者中,循环TNFR2pos Treg细胞中的CTLA4表达和抑制功能增加。我们将TNFR2pos Treg细胞确定为治疗干预的潜在有吸引力的靶点。

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Circulating Regulatory T Cells Expressing Tumor Necrosis Factor Receptor Type 2 Contribute to Sepsis-Induced Immunosuppression in Patients During Septic Shock.表达肿瘤坏死因子受体2型的循环调节性T细胞在感染性休克患者中导致脓毒症诱导的免疫抑制。
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