Nieuwenhuizen Natalie E, Nouailles Geraldine, Sutherland Jayne S, Zyla Joanna, Pasternack Arja H, Heyckendorf Jan, Frye Björn C, Höhne Kerstin, Zedler Ulrike, Bandermann Silke, Abu Abed Ulrike, Brinkmann Volker, Gutbier Birgitt, Witzenrath Martin, Suttorp Norbert, Zissel Gernot, Lange Christoph, Ritvos Olli, Kaufmann Stefan H E
Department of Immunology, Max Planck Institute for Infection Biology, Chariteplatz, Berlin, Germany.
Institute for Hygiene and Microbiology, Julius Maximilian University of Würzburg, Würzburg, Germany.
mBio. 2024 Mar 13;15(3):e0340823. doi: 10.1128/mbio.03408-23. Epub 2024 Feb 20.
Activin A strongly influences immune responses; yet, few studies have examined its role in infectious diseases. We measured serum activin A levels in two independent tuberculosis (TB) patient cohorts and in patients with pneumonia and sarcoidosis. Serum activin A levels were increased in TB patients compared to healthy controls, including those with positive tuberculin skin tests, and paralleled severity of disease, assessed by X-ray scores. In pneumonia patients, serum activin A levels were also raised, but in sarcoidosis patients, levels were lower. To determine whether blockade of the activin A signaling axis could play a functional role in TB, we harnessed a soluble activin type IIB receptor fused to human IgG1 Fc, ActRIIB-Fc, as a ligand trap in a murine TB model. The administration of ActRIIB-Fc to -infected mice resulted in decreased bacterial loads and increased numbers of CD4 effector T cells and tissue-resident memory T cells in the lung. Increased frequencies of tissue-resident memory T cells corresponded with downregulated T-bet expression in lung CD4 and CD8 T cells. Altogether, the results suggest a disease-exacerbating role of ActRIIB signaling pathways. Serum activin A may be useful as a biomarker for diagnostic triage of active TB or monitoring of anti-tuberculosis therapy.
Tuberculosis remains the leading cause of death by a bacterial pathogen. The etiologic agent of tuberculosis, , can remain dormant in the infected host for years before causing disease. Significant effort has been made to identify biomarkers that can discriminate between latently infected and actively diseased individuals. We found that serum levels of the cytokine activin A were associated with increased lung pathology and could discriminate between active tuberculosis and tuberculin skin-test-positive healthy controls. Activin A signals through the ActRIIB receptor, which can be blocked by administration of the ligand trap ActRIIB-Fc, a soluble activin type IIB receptor fused to human IgG1 Fc. In a murine model of tuberculosis, we found that ActRIIB-Fc treatment reduced mycobacterial loads. Strikingly, ActRIIB-Fc treatment significantly increased the number of tissue-resident memory T cells. These results suggest a role for ActRIIB signaling pathways in host responses to and activin A as a biomarker of ongoing disease.
激活素A对免疫反应有强烈影响;然而,很少有研究探讨其在传染病中的作用。我们在两个独立的肺结核(TB)患者队列以及肺炎和结节病患者中测量了血清激活素A水平。与健康对照相比,肺结核患者的血清激活素A水平升高,包括结核菌素皮肤试验呈阳性的患者,并且与通过X线评分评估的疾病严重程度平行。肺炎患者的血清激活素A水平也升高,但结节病患者的水平较低。为了确定激活素A信号轴的阻断是否在肺结核中发挥功能作用,我们在小鼠肺结核模型中利用与人类IgG1 Fc融合的可溶性激活素IIB型受体(ActRIIB-Fc)作为配体陷阱。给感染的小鼠施用ActRIIB-Fc导致细菌载量减少,肺中CD4效应T细胞和组织驻留记忆T细胞数量增加。组织驻留记忆T细胞频率的增加与肺CD4和CD8 T细胞中T-bet表达的下调相对应。总之,结果表明ActRIIB信号通路具有疾病加重作用。血清激活素A可能作为活动性肺结核诊断分类或抗结核治疗监测的生物标志物。
结核病仍然是细菌病原体导致死亡的主要原因。结核病的病原体结核分枝杆菌在受感染宿主中可潜伏数年才引发疾病。人们已做出重大努力来识别能够区分潜伏感染个体和活动性疾病个体的生物标志物。我们发现细胞因子激活素A的血清水平与肺部病理变化增加相关,并且可以区分活动性肺结核和结核菌素皮肤试验呈阳性的健康对照。激活素A通过ActRIIB受体发出信号,可通过施用配体陷阱ActRIIB-Fc来阻断,ActRIIB-Fc是一种与人类IgG1 Fc融合的可溶性激活素IIB型受体。在小鼠肺结核模型中,我们发现ActRIIB-Fc治疗可降低分枝杆菌载量。令人惊讶的是,ActRIIB-Fc治疗显著增加了组织驻留记忆T细胞的数量。这些结果表明ActRIIB信号通路在宿主对结核分枝杆菌的反应中发挥作用,并且激活素A作为疾病进展的生物标志物。
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