Diffuse panbronchiolitis: role of macrolides in therapy.

Naoto Keicho, Shoji Kudoh
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引用次数: 80

Abstract

Diffuse panbronchiolitis (DPB) is characterized by chronic sinobronchial infection and diffuse bilateral micronodular pulmonary lesions consisting of inflammatory cells. Studies on disease etiology point to a genetic predisposition unique to Asians. Early therapy for DPB was largely symptomatic. The advent of macrolide antibiotics, including erythromycin, roxithromycin and clarithromycin, has strikingly changed disease prognosis. Low-dose, long-term macrolide therapy for DPB originated from detailed observations of response to therapy in a single patient. The bactericidal activity of macrolides, particularly erythromycin, is not a significant factor for their clinical efficacy in DPB. Firstly, irrespective of bacterial clearance, clinical improvement is observed in patients treated with erythromycin. Secondly, even in cases with bacterial superinfection with Pseudomonas aeruginosa resistant to macrolides, treatment has proved effective. Thirdly, the recommended dosage of macrolides produces peak levels in tissue that are below the minimum inhibitory concentrations for major pathogenic bacteria that colonize the airway. In the last two decades, the possible mechanism underlying the effectiveness of macrolide therapy has been extensively studied. The proposed mechanism of action includes inhibition of excessive mucus and water secretion from the airway epithelium, inhibition of neutrophil accumulation in the large airway, inhibition of lymphocyte and macrophage accumulation around the small airway, and modulation of bacterial virulence. The great success of macrolide therapy in diffuse panbronchiolitis may extend its application to the treatment of other chronic inflammatory disorders. If the anti-inflammatory activity of macrolides is independent of their bactericidal effect, new anti-inflammatory macrolides without antimicrobial activity should be developed to minimize emergence of macrolide-resistant micro-organisms.

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弥漫性泛细支气管炎:大环内酯类药物在治疗中的作用。
弥漫性泛细支气管炎(DPB)的特征是慢性支气管感染和由炎症细胞组成的弥漫性双侧小结节性肺病变。病因学研究指出了亚洲人特有的遗传易感性。DPB的早期治疗主要是对症治疗。大环内酯类抗生素的出现,包括红霉素、罗红霉素和克拉霉素,显著地改变了疾病的预后。低剂量、长期大环内酯治疗DPB源于对单个患者治疗反应的详细观察。大环内酯类药物,尤其是红霉素的杀菌活性并不是影响其治疗DPB临床疗效的重要因素。首先,不考虑细菌清除率,红霉素治疗的患者临床改善。其次,即使是对大环内酯类耐药的铜绿假单胞菌的细菌重复感染病例,治疗也证明是有效的。第三,推荐剂量的大环内酯类药物在组织中产生的峰值水平低于定植在气道上的主要致病菌的最低抑制浓度。在过去的二十年中,大环内酯类药物治疗有效性的可能机制已被广泛研究。提出的作用机制包括抑制气道上皮分泌过多的粘液和水分,抑制大气道中性粒细胞积聚,抑制小气道周围淋巴细胞和巨噬细胞积聚,以及调节细菌毒力。大环内酯治疗弥漫性泛细支气管炎的巨大成功可能将其应用于其他慢性炎性疾病的治疗。如果大环内酯类药物的抗炎活性独立于其杀菌作用,则应开发新的无抗菌活性的抗炎大环内酯类药物,以尽量减少大环内酯类药物耐药微生物的出现。
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