Moratti Mattia, Schifino Gioacchino, Baccelli Francesco, Ferrari Simona, Magrini Elisabetta, Bassi Mirna, Guerrieri Aldo, Zompatori Maurizio, Lanari Marcello, Conti Francesca
Specialty School of Paediatrics, University of Bologna, Bologna, Italy.
Department of Biomedicine and Prevention, Molecular Medicine and Applied Biotechnology, University of Rome Tor Vergata, Rome, Italy.
Front Immunol. 2025 May 15;16:1589052. doi: 10.3389/fimmu.2025.1589052. eCollection 2025.
Common variable immune deficiency (CVID) is the most prevalent inborn error of immunity (IEI), marked by diverse clinical-immunological phenotypes and significant immune-dysregulation, including granulomatous lymphocytic interstitial lung disease (GLILD). GLILD is a severe manifestation of CVID, contributing to reduced life expectancy and a challenging diagnosis due to its insidious and non-specific clinical course. Current management strategies for GLILD rely on expert opinion due to a lack of randomized controlled trials (RCTs).
This study aims to provide a comprehensive immunophenotypical characterization of CVID patients with and without GLILD, investigate predictive biomarkers for GLILD development, and explore therapeutic strategies, particularly during concomitant SARS-CoV-2 and chronic cytomegalovirus (CMV) infections.
Primary data were collected from a cohort of 25 patients with CVID who underwent high-resolution computed tomography (HRCT), immunophenotyping, and serum immunoglobulin analysis at diagnosis and after immunoglobulin replacement therapy. Existing literature on CVID and GLILD biomarkers, immunological profiles, and therapeutic interventions informed comparative analyses.
Patients with GLILD exhibited distinct immunophenotypical features, including reduced regulatory T-cells, CD8+ naïve, central memory T-cells, and B-cell subsets (memory and switched memory), alongside increased CD21low B-cells and naïve B-cells, indicative of chronic inflammation-driven immune activation. IgA and IgG4 concentrations were significantly lower in patients with GLILD at diagnosis. Immunosuppressive therapy, predominantly mycophenolate mofetil (MMF), demonstrated favorable clinical and functional outcomes, though radiological progression persisted in some cases. CMV infection in patients with GLILD on immunosuppressants resulted in favorable outcomes, underscoring the importance of personalized treatment strategies.
This study highlights novel immunological markers and clinical-radiological patterns as potential predictors for GLILD, advocating for their integration into diagnostic and monitoring frameworks to reduce reliance on invasive histopathology. Future research should focus on validating biomarkers and conducting RCTs to establish evidence-based guidelines for GLILD management.
普通可变免疫缺陷(CVID)是最常见的先天性免疫缺陷(IEI),其特征为多样的临床免疫表型和显著的免疫失调,包括肉芽肿性淋巴细胞间质性肺病(GLILD)。GLILD是CVID的一种严重表现,因其隐匿且非特异性的临床病程,导致预期寿命缩短且诊断具有挑战性。由于缺乏随机对照试验(RCT),目前GLILD的管理策略依赖专家意见。
本研究旨在全面描述有和没有GLILD的CVID患者的免疫表型特征,研究GLILD发生的预测生物标志物,并探索治疗策略,特别是在合并严重急性呼吸综合征冠状病毒2(SARS-CoV-2)和慢性巨细胞病毒(CMV)感染期间。
从一组25例CVID患者中收集原始数据,这些患者在诊断时和接受免疫球蛋白替代治疗后接受了高分辨率计算机断层扫描(HRCT)、免疫表型分析和血清免疫球蛋白分析。关于CVID和GLILD生物标志物、免疫谱和治疗干预的现有文献为比较分析提供了依据。
患有GLILD的患者表现出独特的免疫表型特征,包括调节性T细胞、CD8 + 初始、中枢记忆T细胞和B细胞亚群(记忆和转换记忆)减少,同时CD21低表达B细胞和初始B细胞增加,这表明慢性炎症驱动免疫激活。诊断时,GLILD患者的IgA和IgG4浓度显著降低。免疫抑制治疗,主要是霉酚酸酯(MMF),显示出良好的临床和功能结果,尽管在某些情况下放射学进展仍持续存在。接受免疫抑制剂治疗的GLILD患者发生CMV感染后结果良好,这突出了个性化治疗策略的重要性。
本研究强调了新的免疫标志物和临床放射学模式作为GLILD潜在预测指标的作用,主张将其纳入诊断和监测框架,以减少对侵入性组织病理学的依赖。未来的研究应侧重于验证生物标志物并进行RCT,以建立基于证据的GLILD管理指南。
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