常见可变免疫缺陷和 X 连锁无丙种球蛋白血症的肺部疾病比较。
Comparison of pulmonary diseases in common variable immunodeficiency and X-linked agammaglobulinaemia.
机构信息
Department of Pediatrics, Pediatrics Center of Excellence, Children's Medical Center, Tehran University of Medical Sciences, Tehran, Iran.
出版信息
Respirology. 2010 Feb;15(2):289-95. doi: 10.1111/j.1440-1843.2009.01679.x. Epub 2009 Dec 27.
UNLABELLED
Patients with CVID are at greater risk of developing lung complications than patients with XLA because of delayed diagnosis and possible immune dysregulation. Early diagnosis and appropriate treatment reduces the incidence of pulmonary infections in both groups of patients. However, CVID patients are prone to progressive lung disease despite optimal immunoglobulin therapy.
BACKGROUND AND OBJECTIVE
Pulmonary disease is the most common complication in patients with common variable immunodeficiency (CVID) or X-linked agammaglobulinaemia (XLA). Pulmonary disease may progress despite immunoglobulin replacement therapy. In this study pulmonary complications were compared in patients with CVID or XLA.
METHODS
Pulmonary complications were evaluated in 115 patients (76 with CVID and 39 with XLA) by reviewing hospital records of chest infections, pulmonary function tests and high-resolution CT scans.
RESULTS
Thirty-two patients with XLA (82%) presented with 59 episodes of pneumonia before diagnosis, whereas 15 patients (38.4%) experienced pneumonia after immunoglobulin replacement therapy (1.67 vs 0.45 episodes per patient per year). Among the CVID patients, 196 episodes of pneumonia were documented in 59 patients (77.6%) before diagnosis, while 36 patients (47.3%) experienced pneumonia after therapy (1.11 vs 0.58 episodes of pneumonia per patient per year). Forty-seven (41%) patients (38 with CVID and 9 with XLA) developed chronic lung disease. The CVID patients developed more complications, including bronchiectasis and lymphoid interstitial pneumonitis, than the XLA patients.
CONCLUSIONS
Patients with CVID had a greater likelihood of developing lung disease, possibly due to delayed diagnosis and immune dysregulation, as compared with XLA patients. Early diagnosis of patients with primary antibody deficiencies and adequate i.v. immunoglobulin replacement therapy substantially reduces the number of pulmonary infections. However, CVID patients are prone to progression of lung disease despite optimal immunoglobulin therapy because of the nature of the disease. This important issue should be addressed in further studies.
未加标签
与 X 连锁无丙种球蛋白血症(XLA)患者相比,由于诊断延迟和可能的免疫失调,普通可变免疫缺陷(CVID)患者发生肺部并发症的风险更高。早期诊断和适当的治疗可降低两组患者肺部感染的发生率。然而,尽管进行了最佳的免疫球蛋白治疗,CVID 患者仍容易发生进行性肺部疾病。
背景和目的
肺部疾病是普通可变免疫缺陷(CVID)或 X 连锁无丙种球蛋白血症(XLA)患者最常见的并发症。尽管进行了免疫球蛋白替代治疗,肺部疾病仍可能进展。在这项研究中,比较了 CVID 和 XLA 患者的肺部并发症。
方法
通过回顾胸部感染、肺功能检查和高分辨率 CT 扫描的病历,评估了 115 例患者(76 例 CVID 和 39 例 XLA)的肺部并发症。
结果
39 例 XLA 患者(82%)在诊断前出现 59 次肺炎发作,而 15 例患者(38.4%)在免疫球蛋白替代治疗后出现肺炎(1.67 与 0.45 例/患者/年)。在 CVID 患者中,59 例患者(77.6%)在诊断前记录了 196 次肺炎发作,而 36 例患者(47.3%)在治疗后出现肺炎(1.11 与 0.58 例/患者/年)。47 例(41%)患者(38 例 CVID 和 9 例 XLA)出现慢性肺部疾病。与 XLA 患者相比,CVID 患者发生更多并发症,包括支气管扩张和淋巴样间质肺炎。
结论
与 XLA 患者相比,CVID 患者发生肺部疾病的可能性更大,这可能是由于诊断延迟和免疫失调所致。对原发性抗体缺陷患者进行早期诊断并进行充分的静脉注射免疫球蛋白替代治疗可显著减少肺部感染的发生次数。然而,尽管进行了最佳的免疫球蛋白治疗,CVID 患者仍容易发生肺部疾病进展,这是由于疾病的性质所致。这一重要问题应在进一步的研究中加以解决。
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