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免疫检查点抑制剂治疗脓毒症:临床前和临床开发的新视角。

Immune checkpoint inhibitors for the treatment of sepsis:insights from preclinical and clinical development.

机构信息

AP-HP, Bichat Hospital, Medical and Infectious Diseases Intensive Care Unit (MI2), Paris, France.

Laboratory of Flow Cytometry, Centre of Postgraduate Medical Education, Warsaw, Poland.

出版信息

Expert Opin Investig Drugs. 2022 Sep;31(9):885-894. doi: 10.1080/13543784.2022.2102477. Epub 2022 Aug 18.

Abstract

INTRODUCTION

It is now well established that sepsis induces a state of acquired immunosuppression, with an increased risk of secondary infections that contributes to patients' worsening. Thus, tackling sepsis-induced immunosuppression represents a promising perspective.

AREAS COVERED

Of mechanisms responsible for sepsis-induced immunosuppression, the increased expression of co-inhibitory receptors such as PD-1, CTLA4, TIM-3, LAG-3, or BTLA and their ligands recently received considerable interest since their inhibition, thanks to the so-called checkpoint inhibitors (CPI), provided astonishing results in cancer by rebooting immune functions. This review reports on the first landmarks of these molecules in sepsis.

EXPERT OPINION

Preclinical results are positive and the first human early phase clinical trials showed a beneficial effect on immunological functions and/or markers and suggested that tolerance of CPIs side effects, mainly auto-immune disorders, is acceptable in sepsis. Elsewhere, in some specific severe ICU infections such as fungal infections, preliminary convincing case reports have been published. Overall, the first results regarding CPIs in sepsis appear encouraging. However, further efforts are warranted, especially in defining the right patients to be treated (i.e. in an individualized approach) and establishing the optimal time to start an immune restoration. Larger trials are now mandatory to confirm CPIs' potential in sepsis.

摘要

简介

现在已经明确,脓毒症会导致获得性免疫抑制,增加继发感染的风险,进而使患者病情恶化。因此,解决脓毒症引起的免疫抑制是一个很有前途的研究方向。

涵盖领域

在导致脓毒症免疫抑制的机制中,共抑制受体(如 PD-1、CTLA4、TIM-3、LAG-3 或 BTLA)及其配体的表达增加受到了相当大的关注,因为这些受体的抑制作用(多亏了所谓的检查点抑制剂(CPI))在癌症中通过重新激活免疫功能而产生了惊人的效果。这篇综述报告了这些分子在脓毒症中的最初研究进展。

专家意见

临床前的结果是积极的,首批人类早期临床试验表明,CPI 对免疫功能和/或标志物有有益的影响,并表明在脓毒症中,CPI 的副作用(主要是自身免疫紊乱)的耐受性是可以接受的。此外,在一些特定的严重 ICU 感染(如真菌感染)中,已经发表了一些初步的有说服力的病例报告。总的来说,CPI 治疗脓毒症的初步结果令人鼓舞。然而,仍需要进一步的努力,特别是在确定合适的治疗患者(即采用个体化方法)和确定开始免疫恢复的最佳时机方面。现在必须进行更大规模的试验来证实 CPI 在脓毒症中的潜力。

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