Galloway-Peña Jessica R, Smith Daniel P, Sahasrabhojane Pranoti, Ajami Nadim J, Wadsworth W Duncan, Daver Naval G, Chemaly Roy F, Marsh Lisa, Ghantoji Shashank S, Pemmaraju Naveen, Garcia-Manero Guillermo, Rezvani Katayoun, Alousi Amin M, Wargo Jennifer A, Shpall Elizabeth J, Futreal Phillip A, Guindani Michele, Petrosino Joseph F, Kontoyiannis Dimitrios P, Shelburne Samuel A
Department of Infectious Disease, Infection Control, and Employee Health, The University of Texas MD Anderson Cancer Center, Houston, Texas.
The Alkek Center for Metagenomics and Microbiome Research, Department of Molecular Virology and Microbiology, Baylor College of Medicine, Houston, Texas.
Cancer. 2016 Jul 15;122(14):2186-96. doi: 10.1002/cncr.30039. Epub 2016 May 3.
Despite increasing data on the impact of the microbiome on cancer, the dynamics and role of the microbiome in infection during therapy for acute myelogenous leukemia (AML) are unknown. Therefore, the authors sought to determine correlations between microbiome composition and infectious outcomes in patients with AML who were receiving induction chemotherapy (IC).
Buccal and fecal specimens (478 samples) were collected twice weekly from 34 patients with AML who were undergoing IC. Oral and stool microbiomes were characterized by 16S ribosomal RNA V4 sequencing using an Illumina MiSeq system. Microbial diversity and genera composition were associated with clinical outcomes.
Baseline stool α-diversity was significantly lower in patients who developed infections during IC compared with those who did not (P = .047). Significant decreases in both oral and stool microbial α-diversity were observed over the course of IC, with a linear correlation between α-diversity change at the 2 sites (P = .02). Loss of both oral and stool α-diversity was associated significantly with the receipt of a carbapenem P < 0.001. Domination events by the majority of genera were transient (median duration, 1 sample), whereas the number of domination events by pathogenic genera increased significantly over the course of IC (P = .002). Moreover, patients who lost microbial diversity over the course of IC were significantly more likely to contract a microbiologically documented infection within the 90 days after IC neutrophil recovery (P = .04).
The current data present the largest longitudinal analyses to date of oral and stool microbiomes in patients with AML and suggest that microbiome measurements could assist with the mitigation of infectious complications of AML therapy. Cancer 2016;122:2186-96. © 2016 American Cancer Society.
尽管关于微生物组对癌症影响的数据不断增加,但微生物组在急性髓系白血病(AML)治疗期间感染中的动态变化和作用尚不清楚。因此,作者试图确定接受诱导化疗(IC)的AML患者微生物组组成与感染结局之间的相关性。
每周两次从34例接受IC的AML患者中采集颊部和粪便标本(共478份样本)。使用Illumina MiSeq系统通过16S核糖体RNA V4测序对口腔和粪便微生物组进行表征。微生物多样性和属组成与临床结局相关。
与未发生感染的患者相比,在IC期间发生感染的患者基线粪便α多样性显著更低(P = 0.047)。在IC过程中,观察到口腔和粪便微生物α多样性均显著下降,两个部位的α多样性变化之间存在线性相关性(P = 0.02)。口腔和粪便α多样性的丧失均与碳青霉烯类药物的使用显著相关(P < 0.001)。大多数属的优势事件是短暂的(中位持续时间为1个样本),而致病属的优势事件数量在IC过程中显著增加(P = 0.002)。此外,在IC过程中微生物多样性丧失的患者在IC中性粒细胞恢复后90天内发生微生物学记录感染的可能性显著更高(P = 0.04)。
目前的数据是迄今为止对AML患者口腔和粪便微生物组进行的最大规模纵向分析,表明微生物组检测有助于减轻AML治疗的感染并发症。《癌症》2016年;122:2186 - 2196。© 2016美国癌症协会
