沙美特罗的副作用:一个有关神经方面的前瞻性研究
2010/01/07
体外试验发现:沙美特罗可增加单核细胞释放BDNF,而加入氟替卡松可抑制这种情况。血清中及血小板中BDNF的浓度的增加与沙美特罗单一治疗后气道高反应恶化有关。相反,β2受体多形性和气道高反应性的改变无关系。
该研究发现哮喘患者BDNF浓度的升高可预测单一应用沙美特罗治疗气道高反应性上的副作用。
(Thorax 2009;64:763-769 )
Thorax 2009;64:763-769
Correspondence to:
Correspondence to Dr M Lommatzsch, Abteilung für Pneumologie, Klinik und Poliklinik für Innere Medizin, Universität Rostock, Ernst-Heydemann-Str 6, D-18057 Rostock, Germany; marek.lommatzsch@med.uni-rostock.de
ABSTRACT
Background: Regular use of inhaled β2-agonists has been associated with a paradoxical loss of asthma control and a deterioration of airway hyper-responsiveness, but the underlying mechanism is unknown. The neurotrophin brain-derived neurotrophic factor (BDNF) has recently been identified as a mediator of airway hyper-responsiveness in asthma.
Methods: Eighteen patients with mild allergic asthma who did not use any regular antiasthmatic therapy inhaled the long-acting β2-agonist salmeterol for 2 weeks followed by 2 weeks of combination therapy with salmeterol and the corticosteroid fluticasone. Airway responsiveness to histamine and BDNF concentrations in blood were assessed prior to entry, after 14 days of salmeterol therapy and after 14 days of combination therapy. In a separate experiment, salmeterol effects on BDNF release by human peripheral blood mononuclear cells were assessed.
Results: Monotherapy with salmeterol significantly increased BDNF concentrations in serum and platelets. This increase was abolished by the addition of fluticasone to the treatment. The findings were confirmed in vitro: salmeterol increased the release of BDNF by mononuclear cells, and this was inhibited by co-incubation with fluticasone. Increased BDNF concentrations in serum and platelets correlated with the deterioration of airway hyper-responsiveness following salmeterol monotherapy. In contrast, there was no association between β2-receptor polymorphisms and changes in airway responsiveness.
Conclusion: Increased BDNF concentrations may underly the adverse effects of salmeterol monotherapy on airway responsiveness in asthma.
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