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Implementing lessons learned from previous bronchial biopsy trials in a new randomized controlled COPD biopsy trial with roflumilast

机译:在新的罗氟司特随机对照COPD活检试验中实施从先前的支气管活检试验中吸取的经验教训

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Background Chronic obstructive pulmonary disease (COPD) is a chronic inflammatory disease mediated by an array of inflammatory cells and mediators, but above all, CD8+ T-lymphocytes, macrophages and neutrophils are important players in disease pathogenesis. Roflumilast, a first-in-class, potent and selective phosphodiesterase 4 (PDE4) inhibitor, reduces the rate of exacerbations in patients with a high risk of future exacerbations and has been shown to reduce inflammatory cells and mediators in induced sputum, a surrogate of airway inflammation. However, these anti-inflammatory effects are yet to be confirmed in another robust study directly assessing inflammatory markers in bronchial sub-mucosa. Methods/Design An international, 16-week, randomized, double-blind, placebo-controlled, parallel-group study investigating the effects of roflumilast 500?μg once-daily versus placebo on inflammatory parameters in bronchial biopsy tissue specimens, sputum and blood serum. One hundred and fifty patients with COPD and chronic bronchitis for at least 12 months will be recruited into the study and randomized in a 1:1 ratio to receive either roflumilast or placebo. The primary endpoint will be the number of CD8+ cells (cell counts per mm2) in bronchial biopsy tissue specimens (sub-mucosa) and the key secondary endpoint will be the number of CD68+ cells (cell counts per mm2), assessed by indirect immunohistochemistry. Discussion It is hypothesized that treatment with roflumilast reduces the characteristic inflammation found in the airways of patients with moderate-to-severe COPD, compared with placebo. The design of the present study has built on the work of previous bronchial biopsy studies available in the literature. It is hoped that it will reveal the cellular mechanisms underlying the anti-inflammatory effects of roflumilast and identify potentially important biomarkers and other surrogate endpoints in patients with COPD. The design and rationale for this trial are described herein. Trial registration Clinical trial identifier: NCT01509677 (clinicaltrials.gov)
机译:背景技术慢性阻塞性肺疾病(COPD)是由一系列炎症细胞和介质介导的慢性炎症性疾病,但最重要的是,CD8 + T淋巴细胞,巨噬细胞和中性粒细胞是疾病发病机理中的重要角色。罗氟司特(Roflumilast)是一流的,有效的选择性磷酸二酯酶4(PDE4)抑制剂,可降低未来病情加重的高危患者的病情加重率,并已证明可减少诱导痰中的炎症细胞和介质,这是一种替代药物。气道发炎。但是,这些抗炎作用尚未在另一项直接评估支气管黏膜下层炎性标志物的可靠研究中得到证实。方法/设计一项国际,为期16周,随机,双盲,安慰剂对照,平行组的研究,研究了每日一次500毫克罗洛司特与安慰剂相比对支气管活检组织标本,痰液和血清中炎症参数的影响。将招募150名COPD和慢性支气管炎患者至少12个月,并按1:1比例随机分配接受罗氟司特或安慰剂治疗的患者。主要终点是支气管活检组织样本(粘膜下层)中CD8 +细胞的数量(每毫米 2 的细胞计数),主要次要终点是CD68 +细胞的数量(每单位细胞计数) mm 2 ),通过间接免疫组织化学评估。讨论假设与安慰剂相比,罗氟司特治疗可减轻中重度COPD患者气道中发现的特征性炎症。本研究的设计基于文献中先前的支气管活检研究的工作。希望它能揭示罗氟司特抗炎作用的细胞机制,并确定COPD患者潜在的重要生物标志物和其他替代终点。本文描述了该试验的设计和原理。试验注册临床试验标识符:NCT01509677(clinicaltrials.gov)

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