De Santis W, Esposito A, Conti V, Fantauzzi A, Guerra A, Mezzaroma I, Aiuti F
Dottorato di Ricerca in Scienze Infettivologiche e delle Terapie Immunologiche, Università degli Studi di Roma, La Sapienza, Roma, Italy.
Infez Med. 2006 Mar;14(1):13-23.
Common variable immunodeficiency (CVID) is a chronic condition characterised by a predominant defect of humoral immunity. In most cases the diagnosis of CVID is made during adulthood; the main clinical features of CVID are chronic and relapsing infections (mainly of respiratory and gastroenteric tracts). CVID patients may also develop neoplastic and autoimmune diseases. In our centre (the Regional Centre for Primary Immunodeficiencies of the Lazio Regional Authority) we administered a 23-item questionnaire to 60 patients with CVID undergoing substitutive therapy with intravenous immunoglobulins (IVIG) about their demographic characteristics, time of clinical onset, time of diagnosis of CVID, clinical features, IVIG doses and administration intervals, and self-assessment of health status. In addition, the clinical history of all patients was reviewed, and the levels of serum IgG, IgA and IgM were evaluated and compared with the pre-therapy serum concentration. Moreover, an analysis of the treatment costs was performed. At onset, 67.2% of patients presented recurrent respiratory infections, and 50% had infections of the lower respiratory tract; 39.6% of the patients had gastroenteric infections. Most patients (57%) had recurrent infections of at least 2 of the respiratory, gastroenteric and/or urogenital tracts. In 37.9% of the group the diagnosis of CVID was made in less than 2 years after the beginning of symptoms, but in many cases (22.4%) the diagnosis took more than 10 years. 93% of patients are treated with a dose of IVIG between 6 and 15 g per administration, with intervals between 2 and 3 weeks. The review of patients'clinical history showed that 43% of patients have had respiratory infections during the follow-up in our Centre, 43% have splenomegaly (3% were also subjected to splenectomy) and 18.3% have autoimmune diseases. The mean concentration of IgG before the beginning of IVIG therapy was 235 mg/dl, while during the follow-up it was 664 mg/dl. Given the long time often required for diagnosis, general physicians and specialists should be better informed in order to make diagnosis swifter. The substitutive therapy with IVIG is effective in preventing recurrent infections and complications. A thorough follow-up is important for diagnosing neoplastic and autoimmune complications; in addition, immunologic analysis of peripheral blood and bone marrow are useful in identifying subgroups of patients with more severe clinical features. Finally, in selected patients, treatment costs may be controlled by modifying the dosage of IVIG or the intervals between administrations.
普通可变免疫缺陷(CVID)是一种以体液免疫主要缺陷为特征的慢性疾病。在大多数情况下,CVID的诊断是在成年期做出的;CVID的主要临床特征是慢性复发性感染(主要是呼吸道和胃肠道感染)。CVID患者还可能发生肿瘤和自身免疫性疾病。在我们中心(拉齐奥地区当局原发性免疫缺陷区域中心),我们对60例接受静脉注射免疫球蛋白(IVIG)替代治疗的CVID患者进行了一项包含23个项目的问卷调查,内容涉及他们的人口统计学特征、临床发病时间、CVID诊断时间、临床特征、IVIG剂量和给药间隔,以及健康状况自我评估。此外,回顾了所有患者的临床病史,并评估了血清IgG、IgA和IgM水平,并与治疗前血清浓度进行比较。此外,还进行了治疗费用分析。发病时,67.2%的患者出现反复呼吸道感染,50%有下呼吸道感染;39.6%的患者有胃肠道感染。大多数患者(57%)至少在呼吸道、胃肠道和/或泌尿生殖道中的2个部位出现反复感染。在该组中,37.9%的患者在症状出现后不到2年就被诊断为CVID,但在许多情况下(22.4%)诊断花费超过10年。93%的患者每次接受6至15克剂量的IVIG治疗,给药间隔为2至3周。对患者临床病史的回顾显示,43%的患者在我们中心随访期间曾患呼吸道感染,43%有脾肿大(3%还接受了脾切除术),18.3%有自身免疫性疾病。IVIG治疗开始前IgG的平均浓度为235毫克/分升,而在随访期间为664毫克/分升。鉴于诊断通常需要很长时间,应让普通医生和专科医生了解更多信息,以便更快地做出诊断。IVIG替代治疗在预防反复感染和并发症方面是有效的。全面的随访对于诊断肿瘤和自身免疫性并发症很重要;此外,外周血和骨髓的免疫学分析有助于识别临床特征更严重的患者亚组。最后,在选定的患者中,可以通过调整IVIG剂量或给药间隔来控制治疗费用。
