Boulet L P, Turcotte H, Laviolette M, Naud F, Bernier M C, Martel S, Chakir J
Institut de Cardiologie et de Pneumologie de L'Université Laval, H opital Laval, Sainte-Foy, Québec, Canada.
Am J Respir Crit Care Med. 2000 Oct;162(4 Pt 1):1308-13. doi: 10.1164/ajrccm.162.4.9910051.
This study aimed at documenting airway inflammation and subepithelial collagen deposition in patients using only inhaled beta(2)-agonists with either recently diagnosed asthma (RDA: </= 2 yr, n = 16) or long-standing asthma (LSA: >/= 13 yr, n = 16) and at the influence of an intense inhaled corticosteroid (ICS) treatment on these parameters, in relation to changes in airway responsiveness. Patients had a methacholine inhalation test and a bronchoscopy with bronchial biopsies before and after an 8-wk treatment with inhaled fluticasone propionate (FP), 1,000 microgram/day. Baseline FEV(1) (mean +/- SEM) was normal and similar in both groups (RDA: 98.1 +/- 2.7, LSA: 94.5 +/- 4.6%). Geometric mean methacholine PC(20) was lower in LSA than in RDA (0.44 versus 3.37 mg/ml) at baseline and improved similarly by 1.85 and 1.86 double concentrations with FP treatment. PC(20) normalized (>/= 16 mg/ml) in five patients with RDA and two patients with LSA. Baseline mean bronchial cell counts (per mm(2) connective tissue surface) for CD3(+), CD4(+), CD8(+), CD25(+), EG1(+), CD45ro(+), and AA1(+) cells were similar in both groups. With FP, EG1(+) (p < 0.001), EG2(+) (p = 0.018), and AA1(+) counts (p = 0.009) decreased significantly in both groups while CD45ro(+) (p = 0.02) counts decreased only in LSA. Baseline type 1 and type 3 collagen deposition underneath the basement membrane was similar in RDA and LSA and did not change significantly after FP. This study shows that recent compared to long-standing mild asthma is associated with a similar degree of airway inflammation and subepithelial fibrosis, and a similar improvement in airway hyperresponsiveness after 8 wk on high-dose ICS. It also indicates that once asthma becomes symptomatic, airway responsiveness cannot normalize in most subjects over such a time period, even with a high dose of ICS.
本研究旨在记录仅使用吸入性β₂受体激动剂的新近诊断哮喘患者(RDA:≤2年,n = 16)和长期哮喘患者(LSA:≥13年,n = 16)的气道炎症和上皮下胶原沉积情况,以及强化吸入性糖皮质激素(ICS)治疗对这些参数的影响,并探讨其与气道反应性变化的关系。患者在接受每日1000微克丙酸氟替卡松(FP)吸入治疗8周前后,进行了乙酰甲胆碱吸入试验和支气管镜检查及支气管活检。两组患者的基线第一秒用力呼气容积(FEV₁)(均值±标准误)均正常且相似(RDA:98.1±2.7,LSA:94.5±4.6%)。基线时,LSA患者的乙酰甲胆碱PC₂₀几何均值低于RDA患者(0.44对3.37毫克/毫升),经FP治疗后,二者的改善程度相似,均提高了1.85和1.86倍浓度。5例RDA患者和2例LSA患者的PC₂₀恢复正常(≥16毫克/毫升)。两组患者的基线支气管细胞计数(每平方毫米结缔组织表面),CD3⁺、CD4⁺、CD8⁺、CD25⁺、EG1⁺、CD45ro⁺和AA1⁺细胞均相似。使用FP治疗后,两组患者的EG1⁺(p < 0.001)、EG2⁺(p = 0.018)和AA1⁺细胞计数(p = 0.009)均显著下降,而CD45ro⁺细胞计数(p = 0.02)仅在LSA患者中下降。RDA和LSA患者基底膜下的I型和III型胶原沉积在基线时相似,FP治疗后无显著变化。本研究表明,与长期轻度哮喘相比,新近诊断的轻度哮喘患者的气道炎症和上皮下纤维化程度相似,高剂量ICS治疗8周后气道高反应性的改善程度也相似。研究还表明,一旦哮喘出现症状,即使使用高剂量ICS,大多数患者在这段时间内气道反应性也无法恢复正常。
