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长期红霉素治疗对非囊性纤维化支气管扩张患者口咽部微生物组和耐药基因库的影响。

Impact of Long-Term Erythromycin Therapy on the Oropharyngeal Microbiome and Resistance Gene Reservoir in Non-Cystic Fibrosis Bronchiectasis.

机构信息

Infection and Immunity, South Australia Health and Medical Research Institute, Adelaide, South Australia, Australia.

SAHMRI Microbiome Research Laboratory, Flinders University School of Medicine, Adelaide, South Australia, Australia.

出版信息

mSphere. 2018 Apr 18;3(2). doi: 10.1128/mSphere.00103-18. Print 2018 Apr 25.

Abstract

Long-term macrolide therapy reduces rates of pulmonary exacerbation in bronchiectasis. However, little is known about the potential for macrolide therapy to alter the composition and function of the oropharyngeal commensal microbiota or to increase the carriage of transmissible antimicrobial resistance. We assessed the effect of long-term erythromycin on oropharyngeal microbiota composition and the carriage of transmissible macrolide resistance genes in 84 adults with bronchiectasis, enrolled in the Bronchiectasis and Low-dose Erythromycin Study (BLESS) 48-week placebo-controlled trial of twice-daily erythromycin ethylsuccinate (400 mg). Oropharyngeal microbiota composition and macrolide resistance gene carriage were determined by 16S rRNA gene amplicon sequencing and quantitative PCR, respectively. Long-term erythromycin treatment was associated with a significant increase in the relative abundance of oropharyngeal ( = 0.041) and with significant decreases in the relative abundances of ( = 0.024) and ( = 0.027). Validation of the sequencing results by quantitative PCR confirmed a significant decrease in the abundance of spp. ( = 0.046). Erythromycin treatment did not result in a significant increase in the number of subjects who carried (A), (B), (C), (F), (A/E), and macrolide resistance genes. However, the abundance of (B) and (A/E) gene copies within carriers who had received erythromycin increased significantly ( < 0.05). Our findings indicate that changes in oropharyngeal microbiota composition resulting from long-term erythromycin treatment are modest and are limited to a discrete group of taxa. Associated increases in levels of transmissible antibiotic resistance genes within the oropharyngeal microbiota highlight the potential for this microbial system to act as a reservoir for resistance. Recent demonstrations that long-term macrolide therapy can prevent exacerbations in chronic airways diseases have led to a dramatic increase in their use. However, little is known about the wider, potentially adverse impacts of these treatments. Substantial disruption of the upper airway commensal microbiota might reduce its contribution to host defense and local immune regulation, while increases in macrolide resistance carriage would represent a serious public health concern. Using samples from a randomized controlled trial, we show that low-dose erythromycin given over 48 weeks influences the composition of the oropharyngeal commensal microbiota. We report that macrolide therapy is associated with significant changes in the relative abundances of members of the genus and with significant increases in the carriage of transmissible macrolide resistance. Determining the clinical significance of these changes, relative to treatment benefit, now represents a research priority.

摘要

长期大环内酯类治疗可降低支气管扩张症患者肺部恶化的发生率。然而,人们对大环内酯类治疗改变口咽共生菌群的组成和功能,或增加可传播的抗生素耐药性的可能性知之甚少。我们评估了长期红霉素对 84 例支气管扩张症患者口咽微生物群组成和可传播大环内酯类耐药基因携带的影响,这些患者参加了支气管扩张症和低剂量红霉素研究(BLESS),这是一项为期 48 周的、每日两次口服红霉素乙琥酯(400mg)的安慰剂对照试验。通过 16S rRNA 基因扩增子测序和定量 PCR 分别确定口咽微生物群组成和大环内酯类耐药基因携带情况。长期红霉素治疗与口咽微生物群( = 0.041)的相对丰度显著增加相关,与 ( = 0.024)和 ( = 0.027)的相对丰度显著降低相关。通过定量 PCR 对测序结果进行验证,证实了 spp.丰度显著降低( = 0.046)。红霉素治疗并未导致携带(A)、(B)、(C)、(F)、(A/E)和 大环内酯类耐药基因的受试者数量显著增加。然而,接受红霉素治疗的携带者中(B)和(A/E)基因拷贝数的丰度显著增加(<0.05)。我们的研究结果表明,长期红霉素治疗引起的口咽微生物群组成的变化是适度的,并且仅限于一组离散的分类群。与口咽微生物群中可传播抗生素耐药基因水平相关的增加突出表明,该微生物系统可能成为耐药性的储存库。最近的研究表明,长期大环内酯类治疗可以预防慢性气道疾病的恶化,导致其使用量急剧增加。然而,人们对这些治疗方法的更广泛的、潜在的不利影响知之甚少。上呼吸道共生微生物群的大量破坏可能会降低其对宿主防御和局部免疫调节的贡献,而耐大环内酯类药物的携带增加将是一个严重的公共卫生问题。本研究使用随机对照试验的样本,表明低剂量红霉素在 48 周内的使用会影响口咽共生微生物群的组成。我们报告说,大环内酯类治疗与 属成员的相对丰度显著变化相关,并与可传播的大环内酯类耐药性的显著增加相关。确定这些变化与治疗益处相关的临床意义,现在是一个研究重点。

https://cdn.ncbi.nlm.nih.gov/pmc/blobs/06f7/5907653/5415d5e8f2a5/sph0021825230001.jpg

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