Characterization of Fusobacterium varium Fv113-g1 isolated from a patient with ulcerative colitis based on complete genome sequence and transcriptome analysis

Sekizuka, Tsuyoshi; Ogasawara, Yumiko; Ohkusa, Toshifumi; Kuroda, Makoto

doi:10.1371/journal.pone.0189319

Cited by 21 publications

(23 citation statements)

References 35 publications

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“…nucleatum , F . varium [9] has also recently gained notoriety as a gastrointestinal pathogen [10, 11]. Indeed, links between the enrichment of Fusobacterium spp.…”

Section: Introductionmentioning

confidence: 99%

Metagenomic analyses of the gut microbiota associated with colorectal adenoma

et al. 2019

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Recent studies have suggested an association between certain members of the Fusobacterium genus, especially F . nucleatum , and the progression of advanced colorectal carcinoma (CRC). We assessed such an association of the gut microbiota in Japanese patients with colorectal adenoma (CRA) or intramucosal CRC using colonoscopy aspirates. We analyzed samples from 81 Japanese patients, including 47 CRA and 24 intramucosal CRC patients, and 10 healthy subjects. Metagenomic analysis of the V3-V4 region of the 16S ribosomal RNA gene was performed. The linear discriminant analysis (LDA) effect size (LEfSe) method was used to examine microbial dysbiosis, revealing significant differences in bacterial abundances between the healthy controls and CRA or intramucosal CRC patients. In particular, F . varium was statistically more abundant in patients with CRA and intramucosal CRC than in healthy subjects. Here, we present the metagenomic profile of CRA and intramucosal CRC and demonstrate that F . varium is at least partially involved in the pathogenesis of CRA and intramucosal CRC.

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“…nucleatum , F . varium [9] has also recently gained notoriety as a gastrointestinal pathogen [10, 11]. Indeed, links between the enrichment of Fusobacterium spp.…”

Section: Introductionmentioning

confidence: 99%

Metagenomic analyses of the gut microbiota associated with colorectal adenoma

et al. 2019

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“…Gut microbiota surveys in Japanese cohorts have indicated that F. varium is associated with UC, 21 22 and a genome sequencing study of F. varium strain Fv113-g1 isolated from a UC patient reported expression of FadA homologues in monocultures simulating in vivo conditions within the human gut. 68 Our data on FadA homologues show that sequences from the Fusobacterium _A clade ( F. varium , F. ulcerans and other uncharacterised sister taxa) are not identical to sequences from the Fusobacterium clade (in which the CRC-associated F. nucleatum is located) ( figure 4 ), thereby suggesting distinct functions or targets among these homologues. While the presence/absence of these gene homologues do not directly translate to invasiveness, 69 we postulate that Fusobacterium _A taxa and their copies of the FadA homologue can be risk factors for diseases other than CRC.…”

Section: Discussionmentioning

confidence: 85%

“…As for F. varium and F. ulcerans , less is known about their distribution and association with cancers or disease. Gut microbiota surveys in Japanese cohorts have indicated that F. varium is associated with UC,21 22 and a genome sequencing study of F. varium strain Fv113-g1 isolated from a UC patient reported expression of FadA homologues in monocultures simulating in vivo conditions within the human gut 68. Our data on FadA homologues show that sequences from the Fusobacterium _A clade ( F. varium , F. ulcerans and other uncharacterised sister taxa) are not identical to sequences from the Fusobacterium clade (in which the CRC-associated F. nucleatum is located) (figure 4), thereby suggesting distinct functions or targets among these homologues.…”

Section: Discussionmentioning

confidence: 99%

Southern Chinese populations harbour non-nucleatum Fusobacteria possessing homologues of the colorectal cancer-associated FadA virulence factor

Yeoh

Chen

Wong

et al. 2020

Gut

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ObjectiveFusobacteria are not common nor relatively abundant in non-colorectal cancer (CRC) populations, however, we identified multiple Fusobacterium taxa nearly absent in western and rural populations to be comparatively more prevalent and relatively abundant in southern Chinese populations. We investigated whether these represented known or novel lineages in the Fusobacterium genus, and assessed their genomes for features implicated in development of cancer.MethodsPrevalence and relative abundances of fusobacterial species were calculated from 3157 CRC and non-CRC gut metagenomes representing 16 populations from various biogeographies. Microbial genomes were assembled and compared with existing reference genomes to assess novel fusobacterial diversity. Phylogenetic distribution of virulence genes implicated in CRC was investigated.ResultsIrrespective of CRC disease status, southern Chinese populations harboured increased prevalence (maximum 39% vs 7%) and relative abundances (average 0.4% vs 0.04% of gut community) of multiple recognised and novel fusobacterial taxa phylogenetically distinct from Fusobacterium nucleatum. Genomes assembled from southern Chinese gut metagenomes increased existing fusobacterial diversity by 14.3%. Homologues of the FadA adhesin linked to CRC were consistently detected in several monophyletic lineages sister to and inclusive of F. varium and F. ulcerans, but not F. mortiferum. We also detected increased prevalence and relative abundances of F. varium in CRC compared with non-CRC cohorts, which together with distribution of FadA homologues supports a possible association with gut disease.ConclusionThe proportion of fusobacteria in guts of southern Chinese populations are higher compared with several western and rural populations in line with the notion of environment/biogeography driving human gut microbiome composition. Several non-nucleatum taxa possess FadA homologues and were enriched in CRC cohorts; whether this imposes a risk in developing CRC and other gut diseases deserves further investigation.

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“…(one OTU) and Veillonella dispar (one OTU). Specific species of Fusobacterium, such as F. nucleatum and F. varium, were reported to be associated with the promotion of intestinal inflammation 18,19 . The population of V. dispar was shown to be significantly larger in patients with severe disease compared to those with mild disease in a large-scale study of gut bacterial communities affected by IBD 20 .…”

Section: Discussionmentioning

confidence: 99%

Mucosal microbiota and gene expression are associated with long-term remission after discontinuation of adalimumab in ulcerative colitis

Sakurai

Nishiyama

Sakai

et al. 2020

Sci Rep

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Given that sustained remission is the ultimate treatment goal in the management of patients with ulcerative colitis (UC), the decision to stop anti-tumor necrosis factor (anti-TNF) treatment in UC patients is difficult. The aim of this study was to evaluate mucosal microbiota and gene expression profiles associated with long-term remission after discontinuation of anti-TNF therapy. In nine UC patients who received anti-TNF therapy for 6 months, microbiota isolated from uninflamed mucosae and gene expression in inflamed and uninflamed mucosae were investigated at week 0 and at week 24. At treatment initiation, Fusobacterium sp. and Veillonella dispar were over-represented in the relapse group compared with the non-relapse group. After treatment, Dorea sp. and Lachnospira sp. were over-represented in the non-relapse group. In the relapse group only, a significant shift in gut bacterial community composition was found between week 0 and week 24. Gene expression of ALIX (PDCD6IP) and SLC9A3 was significantly higher in the non-relapse group than in the relapse group. Lastly, we used machine learning methods to identify relevant gene signatures associated with sustained remission. Statistical analyses of microbiota and expression profiles revealed differences between UC patients who did or did not keep remission after the discontinuation of TNF inhibitors. Trial registration: UMIN000020785: Evaluation of adalimumab therapy in mesalazine-resistant or -intolerant ulcerative colitis; an observational study (EARLY study).

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Characterization of Fusobacterium varium Fv113-g1 isolated from a patient with ulcerative colitis based on complete genome sequence and transcriptome analysis

Cited by 21 publications

References 35 publications

Metagenomic analyses of the gut microbiota associated with colorectal adenoma

Metagenomic analyses of the gut microbiota associated with colorectal adenoma

Southern Chinese populations harbour non-nucleatum Fusobacteria possessing homologues of the colorectal cancer-associated FadA virulence factor

Mucosal microbiota and gene expression are associated with long-term remission after discontinuation of adalimumab in ulcerative colitis

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