细胞因子产生检测揭示了患有反复感染和非感染性炎症的成年人存在有区别的免疫缺陷。
Cytokine production assays reveal discriminatory immune defects in adults with recurrent infections and noninfectious inflammation.
作者信息
Ten Oever Jaap, van de Veerdonk Frank L, Joosten Leo A B, Simon Anna, van Crevel Reinout, Kullberg Bart-Jan, Gyssens Inge C, van der Meer Jos W M, van Deuren Marcel, Netea Mihai G
机构信息
Department of Internal Medicine, Radboud University Medical Center, Nijmegen, The Netherlands
Department of Internal Medicine, Radboud University Medical Center, Nijmegen, The Netherlands.
出版信息
Clin Vaccine Immunol. 2014 Aug;21(8):1061-9. doi: 10.1128/CVI.00152-14. Epub 2014 May 28.
Cytokine production assays have been primarily used in research settings studying novel immunodeficiencies. We sought to determine the diagnostic value of cytokine production assays in patients with recurrent and/or severe infectious diseases (IDs) without known immunodeficiencies and unclassified noninfectious inflammatory disorders (NIIDs). We retrospectively examined cytokine production in whole-blood and peripheral blood mononuclear cell samples from 157 adult patients. A cytokine production rate of <5% of that of healthy controls was considered defective. While monocyte-derived cytokine (tumor necrosis factor alpha [TNF-α], interleukin-1β [IL-1β], and IL-6) production was rarely affected, 30% of all included patients had deficient production of interferon gamma (IFN-γ), IL-17A, or IL-22. Twenty-five percent of the NIID patients displayed defective IFN-γ production, whereas IL-17A production was generally unaffected. In the group of ID patients, defective IFN-γ production was found in 19% and 14% of the patients with viral and bacterial infections, respectively, and in 38%, 24%, and 50% of patients with mycobacterial, mucocutaneous, and invasive fungal infections, respectively. Defective IL-17A and IL-22 production was mainly confined to ID patients with mucocutaneous fungal infections. In conclusion, cytokine production assays frequently detect defective Th1 responses in patients with mycobacterial or fungal infections, in contrast to patients with respiratory tract infections or isolated bacterial infections. Defective IL-17A and IL-22 production was primarily found in patients with fungal infections, while monocyte-derived cytokine production was unaffected. Thus, lymphocyte-derived cytokine production assays are helpful in the diagnostic workup of patients with recurrent infections and suspected immunodeficiencies and have the potential to reveal immune defects that might guide adjunctive immunomodulatory therapy.
细胞因子产生检测主要用于研究新型免疫缺陷的研究环境中。我们试图确定细胞因子产生检测在患有复发性和/或严重感染性疾病(ID)但无已知免疫缺陷以及未分类的非感染性炎症性疾病(NIID)患者中的诊断价值。我们回顾性检查了157例成年患者全血和外周血单核细胞样本中的细胞因子产生情况。细胞因子产生率低于健康对照的5%被认为有缺陷。虽然单核细胞衍生的细胞因子(肿瘤坏死因子α [TNF-α]、白细胞介素-1β [IL-1β]和IL-6)产生很少受到影响,但所有纳入患者中有30%的人干扰素γ(IFN-γ)、IL-17A或IL-22产生不足。25%的NIID患者表现出IFN-γ产生缺陷,而IL-17A产生通常未受影响。在ID患者组中,分别有19%和14%的病毒感染和细菌感染患者存在IFN-γ产生缺陷,而分别有38%、24%和50%的分枝杆菌、皮肤黏膜和侵袭性真菌感染患者存在该缺陷。IL-17A和IL-22产生缺陷主要局限于皮肤黏膜真菌感染的ID患者。总之,与呼吸道感染或单纯细菌感染患者相比,细胞因子产生检测经常在分枝杆菌或真菌感染患者中检测到有缺陷的Th1反应。IL-17A和IL-22产生缺陷主要见于真菌感染患者,而单核细胞衍生的细胞因子产生未受影响。因此,淋巴细胞衍生的细胞因子产生检测有助于对复发性感染和疑似免疫缺陷患者进行诊断检查,并有可能揭示可能指导辅助免疫调节治疗的免疫缺陷。
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