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Genetic variation in bactericidal/permeability-increasing protein influences the risk of developing rapid airflow decline after hematopoietic cell transplantation

机译:杀菌/通透性增加蛋白的遗传变异影响造血细胞移植后气流迅速下降的风险

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摘要

Innate immunity is involved in the biology of graft versus host disease and common airway diseases. We screened 15 genes in this pathway using a linkage disequilibrium-based approach to identify potential candidate genes that may be involved in the development of airflow obstruction after hematopoietic cell transplantation. Sixty-nine single-nucleotide polymorphisms were selected for assessment in a discovery cohort (n = 363). Significant associations were validated in a validation cohort (n = 209). Expression of the candidate gene was demonstrated by detecting gene transcript and protein in malignant and normal small airway epithelial cells. In the discovery cohort, 133 patients developed significant airflow decline. Four patient and donor bactericidal/permeability-increasing (BPI) haplotypes were associated with a 2-fold to 3-fold increased risk of developing significant airflow decline (P values, .004-.038). This association was confirmed in the validation cohort, which had 66 patients with significant airflow decline, with 9 significant haplotypes (P values, .013-.043). BPI gene transcript and protein were detected in airway epithelial cells. These results suggest mutations in the BPI gene significantly influence the risk of developing rapid airflow decline after hematopoietic cell transplantation and may represent a novel therapeutic target for this form of airway disease.
机译:先天免疫涉及移植物抗宿主疾病和常见气道疾病的生物学。我们使用基于连锁不平衡的方法筛选了该途径中的15个基因,以鉴定可能参与造血细胞移植后气流阻塞发展的潜在候选基因。在一个发现队列中选择了69个单核苷酸多态性进行评估(n = 363)。在验证队列中验证了重要的关联(n = 209)。通过检测恶性和正常小气道上皮细胞中的基因转录物和蛋白质来证明候选基因的表达。在发现队列中,有133名患者出现了明显的气流下降。四种患者和供体杀菌/通透性增加(BPI)单倍型与显着气流减少的风险增加了2到3倍相关(P值,0.004-0.038)。该关联在验证队列中得到确认,该队列有66例气流明显下降的患者,有9个显着的单倍型(P值,.013-.043)。在气道上皮细胞中检测到BPI基因的转录本和蛋白质。这些结果表明,BPI基因的突变显着影响造血细胞移植后发展迅速气流下降的风险,并且可能代表这种气道疾病的新型治疗靶点。

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