Center for Investigation in Pediatrics, School of Medical Sciences, University of Campinas, Campinas, Brazil.
Clinical Microbiology Department, Rigshospitalet (Copenhagen University Hospital), Copenhagen, Denmark.
Front Cell Infect Microbiol. 2022 Apr 20;12:858398. doi: 10.3389/fcimb.2022.858398. eCollection 2022.
We aimed to characterise the adaptive immune response to complex (MABSC) and its cross-reactivity with complex (MAC) and (Bacille Calmette-Guérin, BCG) in cystic fibrosis (CF) patients and non-CF controls in terms of lymphocyte proliferation and immunophenotyping, cytokine production and anti-MABSC IgG plasma levels.
In this cross-sectional analysis, peripheral blood mononuclear cells (PBMC) from CF patients with MABSC (CF/MABSC, n=12), MAC infection history (CF/MAC, n=5), no NTM history (CF/NTM-, n=15), BCG-vaccinated (C/BCG+, n=9) and non-vaccinated controls (C/BCG-, n=8) were cultured for four days under stimulation with an in-house MABSC lysate and we used flow cytometry to assess lymphocyte proliferation (given by lymphoblast formation) and immunophenotypes. Cytokine production was assessed after overnight whole blood stimulation with the same lysate, and anti-MABSC IgG levels were measured in plasma from non-stimulated blood.
All CF/MABSC patients had increased CD3+ and CD19+ lymphoblast formation upon PBMC stimulation with MABSC lysate. There was a higher rate of CD3+ than CD19+ lymphoblasts, predominance of CD4+ over CD8+ lymphoblasts, IFN-γ, TNF-α and IL-2 production, low production of the Th17-associated IL-17, and discrete or no production of Th2/B cell-associated cytokines soluble CD40 ligand (CD40L), IL-4 and IL-5, indicating a Th1-dominated phenotype and infection restricted to the lungs. A similar pattern was seen in C/BCG+ controls, and CF/MAC patients, pointing to cross-reactivity. MABSC-IgG levels were higher in CF/MABSC patients than in both control groups, but not CF/NTM- patients, most of whom also had CD3+ and/or CD19+ lymphoblast formation upon PBMC stimulation, indicating previous exposure, subclinical or latent infection with MABSC or other NTM.
The anti-MABSC immune response is Th1-skewed and underlines the cross-reactivity in the anti-mycobacterial immune response. The results, together with published clinical observations, indicate that BCG vaccination may cross-react against NTM in CF patients, and this should be investigated. Due to cross-reactivity, it would also be interesting to investigate whether a combination of MABSC-induced cytokine production by blood cells and anti-MABSC IgG measurement can be useful for identifying latent or subclinical infection both with MABSC and other NTM in CF patients.
我们旨在描述囊性纤维化(CF)患者和非 CF 对照者对复杂(MABSC)的适应性免疫反应,并在淋巴细胞增殖和免疫表型、细胞因子产生和抗 MABSC IgG 血浆水平方面比较其与复杂 MAC(MAC)和卡介苗(BCG)的交叉反应性。
在这项横断面分析中,我们培养了 12 例 MABSC 感染的 CF 患者(CF/MABSC)、5 例有 MAC 感染史的 CF 患者(CF/MAC)、15 例无 NTM 病史的 CF 患者(CF/NTM-)、9 例 BCG 接种的 CF 患者(C/BCG+)和 8 例非接种对照者(C/BCG-)的外周血单核细胞(PBMC),在含有内源性 MABSC 裂解物的条件下培养 4 天,并用流式细胞术评估淋巴细胞增殖(由淋巴母细胞形成表示)和免疫表型。用相同的裂解物对过夜全血进行刺激后,评估细胞因子的产生,并用未刺激血液的血浆测量抗 MABSC IgG 水平。
所有 CF/MABSC 患者在 MABSC 裂解物刺激 PBMC 时,CD3+和 CD19+淋巴母细胞的形成均增加。CD3+淋巴母细胞的比例高于 CD19+淋巴母细胞,CD4+淋巴母细胞的比例高于 CD8+淋巴母细胞,IFN-γ、TNF-α和 IL-2 的产生增加,Th17 相关的 IL-17 产生减少,Th2/B 细胞相关细胞因子可溶性 CD40 配体(CD40L)、IL-4 和 IL-5 的产生减少,表明存在 Th1 占优势的表型和肺部感染。C/BCG+对照者和 CF/MAC 患者也出现了类似的模式,表明存在交叉反应性。CF/MABSC 患者的 MABSC-IgG 水平高于两组对照者,但 CF/NTM-患者除外,其中大多数患者在 PBMC 刺激下也形成了 CD3+和/或 CD19+淋巴母细胞,表明存在先前暴露、亚临床或潜伏性 MABSC 或其他 NTM 感染。
抗 MABSC 免疫反应呈 Th1 偏向性,突出了抗分枝杆菌免疫反应中的交叉反应性。这些结果,以及已发表的临床观察结果,表明 BCG 接种可能会使 CF 患者对 NTM 产生交叉反应,这一点值得进一步研究。由于存在交叉反应性,我们也有兴趣研究血液细胞中 MABSC 诱导的细胞因子产生和抗 MABSC IgG 测量相结合,是否可以用于识别 CF 患者潜伏或亚临床感染 MABSC 和其他 NTM。
