Inflammatory Bowel Disease-Associated Changes in the Gut: Focus on Kazan Patients

被引:45
作者
Lo Sasso, Giuseppe [1 ]
Khachatryan, Lusine [1 ]
Kondylis, Athanasios [1 ]
Battey, James N. D. [1 ]
Sierro, Nicolas [1 ]
Danilova, Natalia A. [2 ]
Grigoryeva, Tatiana, V [2 ]
Markelova, Maria, I [2 ]
Khusnutdinova, Dilyara R. [2 ]
Laikov, Alexander, V [2 ]
Salafutdinov, Ilnur I. [2 ]
Romanova, Yulia D. [2 ]
Siniagina, Mariia N. [2 ]
Vasiliev, Ilya Yu [2 ]
Boulygina, Eugenia A. [2 ]
Solovyeva, Valeriya V. [2 ]
Garanina, Ekaterina E. [2 ]
Kitaeva, Kristina, V [2 ]
Ivanov, Konstantin Y. [2 ]
Chulpanova, Darja S. [2 ]
Kletenkov, Konstantin S. [2 ]
Valeeva, Alina R. [3 ]
Odintsova, Alfiya Kh [4 ]
Ardatskaya, Maria D. [5 ]
Abdulkhakov, Rustam A. [3 ]
Ivanov, Nikolai, V [1 ]
Peitsch, Manuel C. [1 ]
Hoeng, Julia [1 ]
Abdulkhakov, Sayar R. [2 ]
机构
[1] Philip Morris Prod SA, Philip Morris Int Res & Dev, Quai Jeanrenaud 5, CH-2000 Neuchatel, Switzerland
[2] Kazan Fed Univ, Inst Fundamental Med & Biol, Kazan, Tatarstan, Russia
[3] Kazan State Med Univ, Dept Clin Immunol & Allergol, Kazan, Tatarstan, Russia
[4] Republican Clin Hosp Tatarstan Republ, Dept Gastroenterol, Kazan, Tatarstan, Russia
[5] Cent State Med Acad Adm, Dept President Russian Federat, Moscow, Russia
关键词
inflammatory bowel disease; microbial dysbiosis; short-chain fatty acids; CROHNS-DISEASE; GEN; NOV; MICROBIOTA; DYSBIOSIS; BIFIDOBACTERIUM; RELEVANCE; SELECTION; BACTERIA; COLITIS; MARKERS;
D O I
10.1093/ibd/izaa188
中图分类号
R57 [消化系及腹部疾病];
学科分类号
摘要
Background: Several studies have highlighted the role of host-microbiome interactions in the pathogenesis of inflammatory bowel disease (IBD), resulting in an increasing amount of data mainly focusing on Western patients. Because of the increasing prevalence of IBD in newly industrialized countries such as those in Asia, the Middle East, and South America, there is mounting interest in elucidating the gut microbiota of these populations. We present a comprehensive analysis of several IBD-related biomarkers and gut microbiota profiles and functions of a unique population of patients with IBD and healthy patients from Kazan (Republic of Tatarstan, Russia). Methods: Blood and fecal IBD biomarkers, serum cytokines, and fecal short-chain fatty acid (SCFA) content were profiled. Finally, fecal microbiota composition was analyzed by 16S and whole-genome shotgun sequencing. Results: Fecal microbiota whole-genome sequencing confirmed the presence of classic IBD dysbiotic features at the phylum level, with increased abundance of Proteobacteria, Actinobacteria, and Fusobacteria and decreased abundance of Firmicutes, Bacteroidetes, and Verrucomicrobia. At the genus level, the abundance of both fermentative (SCFA-producing and hydrogen (H-2)-releasing) and hydrogenotrophic (H-2-consuming) microbes was affected in patients with IBD. This imbalance was confirmed by the decreased abundance of SCFA species in the feces of patients with IBD and the change in anaerobic index, which mirrors the redox status of the intestine. Conclusions: Our analyses highlighted how IBD-related dysbiotic microbiota-which are generally mainly linked to SCFA imbalance-may affect other important metabolic pathways, such as H-2 metabolism, that are critical for host physiology and disease development.
引用
收藏
页码:418 / 433
页数:16
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