鼻腔炎症细胞因子特征与同种异体造血细胞移植后早期肺部移植物抗宿主疾病有关：概念证明。

ImmunoHorizons Pub Date : 2023-06-01 DOI:10.4049/immunohorizons.2300031

Edwin J Ostrin, Nicholas L Rider, Amin M Alousi, Ehsan Irajizad, Liang Li, Qian Peng, Sang T Kim, Lara Bashoura, Muhammad H Arain, Laila Z Noor, Nikul Patel, Rohtesh Mehta, Uday R Popat, Chitra Hosing, Robert R Jenq, Gabriela Rondon, Samir M Hanash, Sophie Paczesny, Elizabeth J Shpall, Richard E Champlin, Burton F Dickey, Ajay Sheshadri

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引用次数: 0

摘要

人们对造血细胞移植（HCT）后阻塞性支气管炎综合征（BOS）的呼吸道炎症知之甚少。早期 BOS（0p 期）的临床标准往往捕捉到没有 BOS 的 HCT 受者。测量呼吸道炎症可能有助于识别 BOS，尤其是早期 BOS。我们对新发 BOS（n = 14）、BOS 0p 期（n = 10）和无肺功能损害且伴有（n = 3）或不伴有（n = 8）慢性移植物抗宿主病的 HCT 受者进行了一项前瞻性观察研究，并在入组时使用鼻吸附法测量鼻腔炎症，然后在 1 年内每 3 个月测量一次。我们将 BOS 0p 期分为未恢复到基线值的功能损害（preBOS，n = 6）或一过性功能损害（n = 4）。我们使用多重磁珠免疫测定法检测了从鼻吸附基质中洗脱的鼻粘膜内壁液中的炎症趋化因子和细胞因子。我们使用 Kruskal-Wallis 方法分析了组间差异，并对多重比较进行了调整。我们发现前鼻炎患者的鼻腔炎症加重，因此直接将前鼻炎患者与一过性损伤患者进行比较，因为这与诊断最相关。与一过性损伤相比，BOS 前患者的中性粒细胞活化（CXCL2、IL-8）、T 细胞活化（CD40 配体、IL-2、IL-12p70、IL-15）、2 型炎症（eotaxin、IL-4、IL-13）、17 型炎症（IL-17A）、树突状细胞成熟（FLT3 配体、IL-7）和反调节分子（PD-L1、IL-1 受体拮抗剂、IL-10）均与一过性损伤不同。随着时间的推移，这些差异逐渐减弱。总之，一过性的多方面鼻腔炎症反应与前鼻炎患者有关。我们的研究结果需要在更大的纵向队列中进行验证。

本文章由计算机程序翻译，如有差异，请以英文原文为准。

A Nasal Inflammatory Cytokine Signature Is Associated with Early Graft-versus-Host Disease of the Lung after Allogeneic Hematopoietic Cell Transplantation: Proof of Concept.

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A Nasal Inflammatory Cytokine Signature Is Associated with Early Graft-versus-Host Disease of the Lung after Allogeneic Hematopoietic Cell Transplantation: Proof of Concept.

Respiratory inflammation in bronchiolitis obliterans syndrome (BOS) after hematopoietic cell transplantation (HCT) is poorly understood. Clinical criteria for early-stage BOS (stage 0p) often capture HCT recipients without BOS. Measuring respiratory tract inflammation may help identify BOS, particularly early BOS. We conducted a prospective observational study in HCT recipients with new-onset BOS (n = 14), BOS stage 0p (n = 10), and recipients without lung impairment with (n = 3) or without (n = 8) chronic graft-versus-host disease and measured nasal inflammation using nasosorption at enrollment and then every 3 mo for 1 y. We divided BOS stage 0p into impairment that did not return to baseline values (preBOS, n = 6), or transient impairment (n = 4). We tested eluted nasal mucosal lining fluid from nasosorption matrices for inflammatory chemokines and cytokines using multiplex magnetic bead immunoassays. We analyzed between-group differences using the Kruskal-Wallis method, adjusting for multiple comparisons. We found increased nasal inflammation in preBOS and therefore directly compared patients with preBOS to those with transient impairment, as this would be of greatest diagnostic relevance. After adjusting for multiple corrections, we found significant increases in growth factors (FGF2, TGF-α, GM-CSF, VEGF), macrophage activation (CCL4, TNF-α, IL-6), neutrophil activation (CXCL2, IL-8), T cell activation (CD40 ligand, IL-2, IL-12p70, IL-15), type 2 inflammation (eotaxin, IL-4, IL-13), type 17 inflammation (IL-17A), dendritic maturation (FLT3 ligand, IL-7), and counterregulatory molecules (PD-L1, IL-1 receptor antagonist, IL-10) in preBOS patients compared to transient impairment. These differences waned over time. In conclusion, a transient multifaceted nasal inflammatory response is associated with preBOS. Our findings require validation in larger longitudinal cohorts.

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ImmunoHorizons

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