Tumour microbiomes and Fusobacterium genomics in Vietnamese colorectal cancer patients

Hoang N.H. Tran; Trang Nguyen Hoang Thu; Phu Huu Nguyen; Chi Nguyen Vo; Khanh Van Doan; Chau Nguyen Ngoc Minh; Ngoc Tuan Nguyen; Van Ngoc Duc Ta; Khuong An Vu; Thanh Danh Hua; To Nguyen Thi Nguyen; Tan Trinh Van; Trung Pham Duc; Ba Lap Duong; Phuc Minh Nguyen; Vinh Chuc Hoang; Duy Thanh Pham; Guy E. Thwaites; Lindsay J. Hall; Daniel J. Slade; Stephen Baker; Vinh Hung Tran; Hao Chung The

doi:10.1038/s41522-022-00351-7

Tumour microbiomes and Fusobacterium genomics in Vietnamese colorectal cancer patients

Hoang N.H. Tran, Trang Nguyen Hoang Thu, Phu Huu Nguyen, Chi Nguyen Vo, Khanh Van Doan, Chau Nguyen Ngoc Minh, Ngoc Tuan Nguyen, Van Ngoc Duc Ta, Khuong An Vu, Thanh Danh Hua, To Nguyen Thi Nguyen, Tan Trinh Van, Trung Pham Duc, Ba Lap Duong, Phuc Minh Nguyen, Vinh Chuc Hoang, Duy Thanh Pham, Guy E. Thwaites, Lindsay J. Hall, Daniel J. SladeStephen Baker, Vinh Hung Tran, Hao Chung The^*

^*Corresponding author for this work

Microbiology and Infection

Research output: Contribution to journal › Article › peer-review

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Abstract

Perturbations in the gut microbiome have been associated with colorectal cancer (CRC), with the colonic overabundance of Fusobacterium nucleatum shown as the most consistent marker. Despite its significance in the promotion of CRC, genomic studies of Fusobacterium is limited. We enrolled 43 Vietnamese CRC patients and 25 participants with non-cancerous colorectal polyps to study the colonic microbiomes and genomic diversity of Fusobacterium in this population, using a combination of 16S rRNA gene profiling, anaerobic microbiology, and whole genome analysis. Oral bacteria, including F. nucleatum and Leptotrichia, were significantly more abundant in the tumour microbiomes. We obtained 53 Fusobacterium genomes, representing 26 strains, from the saliva, tumour and non-tumour tissues of six CRC patients. Isolates from the gut belonged to diverse F. nucleatum subspecies (nucleatum, animalis, vincentii, polymorphum) and a potential new subspecies of Fusobacterium periodonticum. The Fusobacterium population within each individual was distinct and in some cases diverse, with minimal intra-clonal variation. Phylogenetic analyses showed that within four individuals, tumour-associated Fusobacterium were clonal to those isolated from non-tumour tissues. Genes encoding major virulence factors (Fap2 and RadD) showed evidence of horizontal gene transfer. Our work provides a framework to understand the genomic diversity of Fusobacterium within the CRC patients, which can be exploited for the development of CRC diagnostic and therapeutic options targeting this oncobacterium.

Original language	English
Article number	87
Number of pages	13
Journal	npj Biofilms and Microbiomes
Volume	8
Issue number	1
DOIs	https://doi.org/10.1038/s41522-022-00351-7
Publication status	Published - 29 Oct 2022

Bibliographical note

Funding Information:
HCT is a Wellcome International Training Fellow (218726/Z/19/Z). LJH is supported by Wellcome Trust Investigator Awards 100974/C/13/Z and 220876/Z/20/Z; the Biotechnology and Biological Sciences Research Council (BBSRC), Institute Strategic Programme Gut Microbes and Health BB/R012490/1, and its constituent projects BBS/E/F/000PR10353 and BBS/E/F/000PR10356. SB is a Wellcome Senior Research Fellow (215515/Z/19/Z). The authors wish to thank all participants and their caretakers for their participation in the study, and the pathology laboratory of Binh Dan Hospital for the tumour/biopsy pathology results.

Publisher Copyright:
© 2022, The Author(s).

ASJC Scopus subject areas

Biotechnology
Microbiology
Applied Microbiology and Biotechnology

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This output contributes to the following UN Sustainable Development Goals (SDGs)

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Tran, H. N. H., Thu, T. N. H., Nguyen, P. H., Vo, C. N., Doan, K. V., Nguyen Ngoc Minh, C., Nguyen, N. T., Ta, V. N. D., Vu, K. A., Hua, T. D., Nguyen, T. N. T., Van, T. T., Pham Duc, T., Duong, B. L., Nguyen, P. M., Hoang, V. C., Pham, D. T., Thwaites, G. E., Hall, L. J., ... Chung The, H. (2022). Tumour microbiomes and Fusobacterium genomics in Vietnamese colorectal cancer patients. npj Biofilms and Microbiomes, 8(1), Article 87. https://doi.org/10.1038/s41522-022-00351-7

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title = "Tumour microbiomes and Fusobacterium genomics in Vietnamese colorectal cancer patients",

abstract = "Perturbations in the gut microbiome have been associated with colorectal cancer (CRC), with the colonic overabundance of Fusobacterium nucleatum shown as the most consistent marker. Despite its significance in the promotion of CRC, genomic studies of Fusobacterium is limited. We enrolled 43 Vietnamese CRC patients and 25 participants with non-cancerous colorectal polyps to study the colonic microbiomes and genomic diversity of Fusobacterium in this population, using a combination of 16S rRNA gene profiling, anaerobic microbiology, and whole genome analysis. Oral bacteria, including F. nucleatum and Leptotrichia, were significantly more abundant in the tumour microbiomes. We obtained 53 Fusobacterium genomes, representing 26 strains, from the saliva, tumour and non-tumour tissues of six CRC patients. Isolates from the gut belonged to diverse F. nucleatum subspecies (nucleatum, animalis, vincentii, polymorphum) and a potential new subspecies of Fusobacterium periodonticum. The Fusobacterium population within each individual was distinct and in some cases diverse, with minimal intra-clonal variation. Phylogenetic analyses showed that within four individuals, tumour-associated Fusobacterium were clonal to those isolated from non-tumour tissues. Genes encoding major virulence factors (Fap2 and RadD) showed evidence of horizontal gene transfer. Our work provides a framework to understand the genomic diversity of Fusobacterium within the CRC patients, which can be exploited for the development of CRC diagnostic and therapeutic options targeting this oncobacterium.",

author = "Tran, {Hoang N.H.} and Thu, {Trang Nguyen Hoang} and Nguyen, {Phu Huu} and Vo, {Chi Nguyen} and Doan, {Khanh Van} and {Nguyen Ngoc Minh}, Chau and Nguyen, {Ngoc Tuan} and Ta, {Van Ngoc Duc} and Vu, {Khuong An} and Hua, {Thanh Danh} and Nguyen, {To Nguyen Thi} and Van, {Tan Trinh} and {Pham Duc}, Trung and Duong, {Ba Lap} and Nguyen, {Phuc Minh} and Hoang, {Vinh Chuc} and Pham, {Duy Thanh} and Thwaites, {Guy E.} and Hall, {Lindsay J.} and Slade, {Daniel J.} and Stephen Baker and Tran, {Vinh Hung} and {Chung The}, Hao",

note = "Funding Information: HCT is a Wellcome International Training Fellow (218726/Z/19/Z). LJH is supported by Wellcome Trust Investigator Awards 100974/C/13/Z and 220876/Z/20/Z; the Biotechnology and Biological Sciences Research Council (BBSRC), Institute Strategic Programme Gut Microbes and Health BB/R012490/1, and its constituent projects BBS/E/F/000PR10353 and BBS/E/F/000PR10356. SB is a Wellcome Senior Research Fellow (215515/Z/19/Z). The authors wish to thank all participants and their caretakers for their participation in the study, and the pathology laboratory of Binh Dan Hospital for the tumour/biopsy pathology results. Publisher Copyright: {\textcopyright} 2022, The Author(s).",

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doi = "10.1038/s41522-022-00351-7",

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Tran, HNH, Thu, TNH, Nguyen, PH, Vo, CN, Doan, KV, Nguyen Ngoc Minh, C, Nguyen, NT, Ta, VND, Vu, KA, Hua, TD, Nguyen, TNT, Van, TT, Pham Duc, T, Duong, BL, Nguyen, PM, Hoang, VC, Pham, DT, Thwaites, GE, Hall, LJ, Slade, DJ, Baker, S, Tran, VH & Chung The, H 2022, 'Tumour microbiomes and Fusobacterium genomics in Vietnamese colorectal cancer patients', npj Biofilms and Microbiomes, vol. 8, no. 1, 87. https://doi.org/10.1038/s41522-022-00351-7

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T1 - Tumour microbiomes and Fusobacterium genomics in Vietnamese colorectal cancer patients

AU - Tran, Hoang N.H.

AU - Thu, Trang Nguyen Hoang

AU - Nguyen, Phu Huu

AU - Vo, Chi Nguyen

AU - Doan, Khanh Van

AU - Nguyen Ngoc Minh, Chau

AU - Nguyen, Ngoc Tuan

AU - Ta, Van Ngoc Duc

AU - Vu, Khuong An

AU - Hua, Thanh Danh

AU - Nguyen, To Nguyen Thi

AU - Van, Tan Trinh

AU - Pham Duc, Trung

AU - Duong, Ba Lap

AU - Nguyen, Phuc Minh

AU - Hoang, Vinh Chuc

AU - Pham, Duy Thanh

AU - Thwaites, Guy E.

AU - Hall, Lindsay J.

AU - Slade, Daniel J.

AU - Baker, Stephen

AU - Tran, Vinh Hung

AU - Chung The, Hao

N1 - Funding Information: HCT is a Wellcome International Training Fellow (218726/Z/19/Z). LJH is supported by Wellcome Trust Investigator Awards 100974/C/13/Z and 220876/Z/20/Z; the Biotechnology and Biological Sciences Research Council (BBSRC), Institute Strategic Programme Gut Microbes and Health BB/R012490/1, and its constituent projects BBS/E/F/000PR10353 and BBS/E/F/000PR10356. SB is a Wellcome Senior Research Fellow (215515/Z/19/Z). The authors wish to thank all participants and their caretakers for their participation in the study, and the pathology laboratory of Binh Dan Hospital for the tumour/biopsy pathology results. Publisher Copyright: © 2022, The Author(s).

PY - 2022/10/29

Y1 - 2022/10/29

N2 - Perturbations in the gut microbiome have been associated with colorectal cancer (CRC), with the colonic overabundance of Fusobacterium nucleatum shown as the most consistent marker. Despite its significance in the promotion of CRC, genomic studies of Fusobacterium is limited. We enrolled 43 Vietnamese CRC patients and 25 participants with non-cancerous colorectal polyps to study the colonic microbiomes and genomic diversity of Fusobacterium in this population, using a combination of 16S rRNA gene profiling, anaerobic microbiology, and whole genome analysis. Oral bacteria, including F. nucleatum and Leptotrichia, were significantly more abundant in the tumour microbiomes. We obtained 53 Fusobacterium genomes, representing 26 strains, from the saliva, tumour and non-tumour tissues of six CRC patients. Isolates from the gut belonged to diverse F. nucleatum subspecies (nucleatum, animalis, vincentii, polymorphum) and a potential new subspecies of Fusobacterium periodonticum. The Fusobacterium population within each individual was distinct and in some cases diverse, with minimal intra-clonal variation. Phylogenetic analyses showed that within four individuals, tumour-associated Fusobacterium were clonal to those isolated from non-tumour tissues. Genes encoding major virulence factors (Fap2 and RadD) showed evidence of horizontal gene transfer. Our work provides a framework to understand the genomic diversity of Fusobacterium within the CRC patients, which can be exploited for the development of CRC diagnostic and therapeutic options targeting this oncobacterium.

AB - Perturbations in the gut microbiome have been associated with colorectal cancer (CRC), with the colonic overabundance of Fusobacterium nucleatum shown as the most consistent marker. Despite its significance in the promotion of CRC, genomic studies of Fusobacterium is limited. We enrolled 43 Vietnamese CRC patients and 25 participants with non-cancerous colorectal polyps to study the colonic microbiomes and genomic diversity of Fusobacterium in this population, using a combination of 16S rRNA gene profiling, anaerobic microbiology, and whole genome analysis. Oral bacteria, including F. nucleatum and Leptotrichia, were significantly more abundant in the tumour microbiomes. We obtained 53 Fusobacterium genomes, representing 26 strains, from the saliva, tumour and non-tumour tissues of six CRC patients. Isolates from the gut belonged to diverse F. nucleatum subspecies (nucleatum, animalis, vincentii, polymorphum) and a potential new subspecies of Fusobacterium periodonticum. The Fusobacterium population within each individual was distinct and in some cases diverse, with minimal intra-clonal variation. Phylogenetic analyses showed that within four individuals, tumour-associated Fusobacterium were clonal to those isolated from non-tumour tissues. Genes encoding major virulence factors (Fap2 and RadD) showed evidence of horizontal gene transfer. Our work provides a framework to understand the genomic diversity of Fusobacterium within the CRC patients, which can be exploited for the development of CRC diagnostic and therapeutic options targeting this oncobacterium.

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Tumour microbiomes and Fusobacterium genomics in Vietnamese colorectal cancer patients

Abstract

Bibliographical note

ASJC Scopus subject areas

UN SDGs

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