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Humoral Immunity to Lung Antigens Early Post-Transplant Confers Risk for Chronic Lung Allograft Dysfunction.

The Journal of heart and lung transplantation the official publication of the International Society for Heart Transplantation(2025)

Latner Thoracic Research Laboratories | Toronto Lung Transplant Program | Biostatistical Research Unit | Toronto General Hospital Research Institute

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Abstract
BACKGROUND:Autoantibodies and de novo donor HLA-specific antibodies (dnDSA) may contribute to chronic lung allograft dysfunction (CLAD). However, the breadth of reactivities against self-antigens and their association with CLAD has been underexamined. In a single-center study, we screened lung transplant (LTx) recipients for novel autoantibodies at transplant and 6 months post-LTx, assessed dnDSA exposure, and CLAD-free survival. METHODS:Serum samples were collected from 89 crossmatch-negative bilateral LTx recipients at the time of LTx and 6 months post-LTx, before a CLAD diagnosis, for autoantibody screening using a custom antigen microarray. RESULTS:Patients who developed CLAD by 5 years post-LTx demonstrated a decrease in average IgG reactivity, but no decrease in IgM reactivity when measured at 6 months post-LTx. IgG anti-tropoelastin, SP-D, and thyroglobulin autoantibodies were significantly elevated 6 months post-LTx in patients who developed CLAD by 5 years, compared to those who remained CLAD-free at 5 years. In contrast, patients who remained CLAD-free at 5 years had elevated levels of IgG anti-CENP-B at both timepoints and PM/SCL100 at 6 months post-LTx, suggesting these may confer protection. Exposure to autoantibodies against lung-enriched targets and dnDSA conferred increased CLAD risk. CONCLUSIONS:We identified novel autoantibodies associated with CLAD-free survival, bolstering the independent relationship between autoantibodies and CLAD. We also identified autoantibody signatures that are associated with a marked increase in CLAD risk. Exposure to lung-enriched targets and dnDSA may have a reciprocal amplifying effect that lies on a tissue-specific mechanistic pathway leading to CLAD.
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要点】:本研究发现特定的新型自身抗体与移植后五年内慢性肺移植物功能障碍(CLAD)的发生风险有关,揭示了自身抗体在CLAD发展中的独立作用及其保护性或风险性特征。

方法】:研究者使用定制抗原微阵列技术对89名交叉配型阴性双肺移植受体在移植时及移植后六个月的血清样本进行了自身抗体筛查。

实验】:通过分析移植后六个月及五年内CLAD诊断前血清样本,发现CLAD患者IgG对某些自身抗原的平均反应性下降,而IgM反应性无变化。实验使用的数据集为89名LTx受者移植时及移植后六个月的血清样本。结果显示,五年内发展为CLAD的患者移植后六个月对某些自身抗原的IgG抗体水平显著升高,而五年内保持CLAD-free的患者则表现出对其他自身抗原的IgG抗体水平升高,表明这些抗体可能具有保护作用。