HPV-related anal cancer is associated with changes in the anorectal microbiome during cancer development

Jacob H. Elnaggar; Victoria O. Huynh; Daniel Lin; R. Tyler Hillman; Chike O. Abana; Molly B. El Alam; Katarina C. Tomasic; Tatiana V. Karpinets; Ramez Kouzy; Jae L. Phan; Jennifer Wargo; Emma B. Holliday; Prajnan Das; Melissa P. Mezzari; Nadim J. Ajami; Erica J. Lynn; Bruce D. Minsky; Van K. Morris; Andrea Milbourne; Craig A. Messick; Ann H. Klopp; P. Andrew Futreal; Cullen M. Taniguchi; Kathleen M. Schmeler; Lauren E. Colbert

doi:10.3389/fimmu.2023.1051431

HPV-related anal cancer is associated with changes in the anorectal microbiome during cancer development

Jacob H. Elnaggar, Victoria O. Huynh, Daniel Lin, R. Tyler Hillman, Chike O. Abana, Molly B. El Alam, Katarina C. Tomasic, Tatiana V. Karpinets, Ramez Kouzy, Jae L. Phan, Jennifer Wargo, Emma B. Holliday, Prajnan Das, Melissa P. Mezzari, Nadim J. Ajami, Erica J. Lynn, Bruce D. Minsky, Van K. Morris, Andrea Milbourne, Craig A. MessickAnn H. Klopp, P. Andrew Futreal, Cullen M. Taniguchi, Kathleen M. Schmeler, Lauren E. Colbert

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

4 Scopus citations

Abstract

Background: Squamous cell carcinoma of the anus (SCCA) is a rare gastrointestinal cancer. Factors associated with progression of HPV infection to anal dysplasia and cancer are unclear and screening guidelines and approaches for anal dysplasia are less clear than for cervical dysplasia. One potential contributing factor is the anorectal microbiome. In this study, we aimed to identify differences in anal microbiome composition in the settings of HPV infection, anal dysplasia, and anal cancer in this rare disease. Methods: Patients were enrolled in two prospective studies. Patients with anal dysplasia were part of a cross-sectional cohort that enrolled women with high-grade lower genital tract dysplasia. Anorectal tumor swabs were prospectively collected from patients with biopsy-confirmed locally advanced SCCA prior to receiving standard-of-care chemoradiotherapy (CRT). Patients with high-grade lower genital tract dysplasia without anal dysplasia were considered high-risk (HR Normal). 16S V4 rRNA Microbiome sequencing was performed for anal swabs. Alpha and Beta Diversity and composition were compared for HR Normal, anal dysplasia, and anal cancer. Results: 60 patients with high-grade lower genital tract dysplasia were initially enrolled. Seven patients had concurrent anal dysplasia and 44 patients were considered HR Normal. Anorectal swabs from 21 patients with localized SCCA were included, sequenced, and analyzed in the study. Analysis of weighted and unweighted UniFrac distances demonstrated significant differences in microbial community composition between anal cancer and HR normal (p=0.018). LEfSe identified that all three groups exhibited differential enrichment of specific taxa. Peptoniphilus (p=0.028), Fusobacteria (p=0.0295), Porphyromonas (p=0.034), and Prevotella (p=0.029) were enriched in anal cancer specimens when compared to HR normal. Conclusion: Although alpha diversity was similar between HR Normal, dysplasia and cancer patients, composition differed significantly between the three groups. Increased anorectal Peptoniphilus, Fusobacteria, Porphyromonas, and Prevotella abundance were associated with anal cancer. These organisms have been reported in various gastrointestinal cancers with roles in facilitating the proinflammatory microenvironment and neoplasia progression. Future work should investigate a potential role of microbiome analysis in screening for anal dysplasia and investigation into potential mechanisms of how these microbial imbalances influence the immune system and anal carcinogenesis.

Original language	English (US)
Article number	1051431
Journal	Frontiers in immunology
Volume	14
DOIs	https://doi.org/10.3389/fimmu.2023.1051431
State	Published - 2023

Keywords

anal cancer
anal dysplasia
anorectal microbiome
cancer biology
HPV-related cancer

ASJC Scopus subject areas

Immunology and Allergy
Immunology

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10.3389/fimmu.2023.1051431

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Elnaggar, J. H., Huynh, V. O., Lin, D., Hillman, R. T., Abana, C. O., El Alam, M. B., Tomasic, K. C., Karpinets, T. V., Kouzy, R., Phan, J. L., Wargo, J., Holliday, E. B., Das, P., Mezzari, M. P., Ajami, N. J., Lynn, E. J., Minsky, B. D., Morris, V. K., Milbourne, A., ... Colbert, L. E. (2023). HPV-related anal cancer is associated with changes in the anorectal microbiome during cancer development. Frontiers in immunology, 14, Article 1051431. https://doi.org/10.3389/fimmu.2023.1051431

Elnaggar, JH, Huynh, VO, Lin, D, Hillman, RT, Abana, CO, El Alam, MB, Tomasic, KC, Karpinets, TV, Kouzy, R, Phan, JL, Wargo, J , Holliday, EB , Das, P, Mezzari, MP, Ajami, NJ, Lynn, EJ, Minsky, BD, Morris, VK , Milbourne, A , Messick, CA , Klopp, AH , Futreal, PA, Taniguchi, CM, Schmeler, KM & Colbert, LE 2023, 'HPV-related anal cancer is associated with changes in the anorectal microbiome during cancer development', Frontiers in immunology, vol. 14, 1051431. https://doi.org/10.3389/fimmu.2023.1051431

@article{a0c880ab394c4c34b8f682bf6480b210,

title = "HPV-related anal cancer is associated with changes in the anorectal microbiome during cancer development",

abstract = "Background: Squamous cell carcinoma of the anus (SCCA) is a rare gastrointestinal cancer. Factors associated with progression of HPV infection to anal dysplasia and cancer are unclear and screening guidelines and approaches for anal dysplasia are less clear than for cervical dysplasia. One potential contributing factor is the anorectal microbiome. In this study, we aimed to identify differences in anal microbiome composition in the settings of HPV infection, anal dysplasia, and anal cancer in this rare disease. Methods: Patients were enrolled in two prospective studies. Patients with anal dysplasia were part of a cross-sectional cohort that enrolled women with high-grade lower genital tract dysplasia. Anorectal tumor swabs were prospectively collected from patients with biopsy-confirmed locally advanced SCCA prior to receiving standard-of-care chemoradiotherapy (CRT). Patients with high-grade lower genital tract dysplasia without anal dysplasia were considered high-risk (HR Normal). 16S V4 rRNA Microbiome sequencing was performed for anal swabs. Alpha and Beta Diversity and composition were compared for HR Normal, anal dysplasia, and anal cancer. Results: 60 patients with high-grade lower genital tract dysplasia were initially enrolled. Seven patients had concurrent anal dysplasia and 44 patients were considered HR Normal. Anorectal swabs from 21 patients with localized SCCA were included, sequenced, and analyzed in the study. Analysis of weighted and unweighted UniFrac distances demonstrated significant differences in microbial community composition between anal cancer and HR normal (p=0.018). LEfSe identified that all three groups exhibited differential enrichment of specific taxa. Peptoniphilus (p=0.028), Fusobacteria (p=0.0295), Porphyromonas (p=0.034), and Prevotella (p=0.029) were enriched in anal cancer specimens when compared to HR normal. Conclusion: Although alpha diversity was similar between HR Normal, dysplasia and cancer patients, composition differed significantly between the three groups. Increased anorectal Peptoniphilus, Fusobacteria, Porphyromonas, and Prevotella abundance were associated with anal cancer. These organisms have been reported in various gastrointestinal cancers with roles in facilitating the proinflammatory microenvironment and neoplasia progression. Future work should investigate a potential role of microbiome analysis in screening for anal dysplasia and investigation into potential mechanisms of how these microbial imbalances influence the immune system and anal carcinogenesis.",

keywords = "anal cancer, anal dysplasia, anorectal microbiome, cancer biology, HPV-related cancer",

author = "Elnaggar, {Jacob H.} and Huynh, {Victoria O.} and Daniel Lin and Hillman, {R. Tyler} and Abana, {Chike O.} and {El Alam}, {Molly B.} and Tomasic, {Katarina C.} and Karpinets, {Tatiana V.} and Ramez Kouzy and Phan, {Jae L.} and Jennifer Wargo and Holliday, {Emma B.} and Prajnan Das and Mezzari, {Melissa P.} and Ajami, {Nadim J.} and Lynn, {Erica J.} and Minsky, {Bruce D.} and Morris, {Van K.} and Andrea Milbourne and Messick, {Craig A.} and Klopp, {Ann H.} and Futreal, {P. Andrew} and Taniguchi, {Cullen M.} and Schmeler, {Kathleen M.} and Colbert, {Lauren E.}",

note = "Publisher Copyright: Copyright {\textcopyright} 2023 Elnaggar, Huynh, Lin, Hillman, Abana, El Alam, Tomasic, Karpinets, Kouzy, Phan, Wargo, Holliday, Das, Mezzari, Ajami, Lynn, Minsky, Morris, Milbourne, Messick, Klopp, Futreal, Taniguchi, Schmeler and Colbert.",

year = "2023",

doi = "10.3389/fimmu.2023.1051431",

language = "English (US)",

volume = "14",

journal = "Frontiers in immunology",

issn = "1664-3224",

publisher = "Frontiers Media S. A.",

}

TY - JOUR

T1 - HPV-related anal cancer is associated with changes in the anorectal microbiome during cancer development

AU - Elnaggar, Jacob H.

AU - Huynh, Victoria O.

AU - Lin, Daniel

AU - Hillman, R. Tyler

AU - Abana, Chike O.

AU - El Alam, Molly B.

AU - Tomasic, Katarina C.

AU - Karpinets, Tatiana V.

AU - Kouzy, Ramez

AU - Phan, Jae L.

AU - Wargo, Jennifer

AU - Holliday, Emma B.

AU - Das, Prajnan

AU - Mezzari, Melissa P.

AU - Ajami, Nadim J.

AU - Lynn, Erica J.

AU - Minsky, Bruce D.

AU - Morris, Van K.

AU - Milbourne, Andrea

AU - Messick, Craig A.

AU - Klopp, Ann H.

AU - Futreal, P. Andrew

AU - Taniguchi, Cullen M.

AU - Schmeler, Kathleen M.

AU - Colbert, Lauren E.

N1 - Publisher Copyright: Copyright © 2023 Elnaggar, Huynh, Lin, Hillman, Abana, El Alam, Tomasic, Karpinets, Kouzy, Phan, Wargo, Holliday, Das, Mezzari, Ajami, Lynn, Minsky, Morris, Milbourne, Messick, Klopp, Futreal, Taniguchi, Schmeler and Colbert.

PY - 2023

Y1 - 2023

N2 - Background: Squamous cell carcinoma of the anus (SCCA) is a rare gastrointestinal cancer. Factors associated with progression of HPV infection to anal dysplasia and cancer are unclear and screening guidelines and approaches for anal dysplasia are less clear than for cervical dysplasia. One potential contributing factor is the anorectal microbiome. In this study, we aimed to identify differences in anal microbiome composition in the settings of HPV infection, anal dysplasia, and anal cancer in this rare disease. Methods: Patients were enrolled in two prospective studies. Patients with anal dysplasia were part of a cross-sectional cohort that enrolled women with high-grade lower genital tract dysplasia. Anorectal tumor swabs were prospectively collected from patients with biopsy-confirmed locally advanced SCCA prior to receiving standard-of-care chemoradiotherapy (CRT). Patients with high-grade lower genital tract dysplasia without anal dysplasia were considered high-risk (HR Normal). 16S V4 rRNA Microbiome sequencing was performed for anal swabs. Alpha and Beta Diversity and composition were compared for HR Normal, anal dysplasia, and anal cancer. Results: 60 patients with high-grade lower genital tract dysplasia were initially enrolled. Seven patients had concurrent anal dysplasia and 44 patients were considered HR Normal. Anorectal swabs from 21 patients with localized SCCA were included, sequenced, and analyzed in the study. Analysis of weighted and unweighted UniFrac distances demonstrated significant differences in microbial community composition between anal cancer and HR normal (p=0.018). LEfSe identified that all three groups exhibited differential enrichment of specific taxa. Peptoniphilus (p=0.028), Fusobacteria (p=0.0295), Porphyromonas (p=0.034), and Prevotella (p=0.029) were enriched in anal cancer specimens when compared to HR normal. Conclusion: Although alpha diversity was similar between HR Normal, dysplasia and cancer patients, composition differed significantly between the three groups. Increased anorectal Peptoniphilus, Fusobacteria, Porphyromonas, and Prevotella abundance were associated with anal cancer. These organisms have been reported in various gastrointestinal cancers with roles in facilitating the proinflammatory microenvironment and neoplasia progression. Future work should investigate a potential role of microbiome analysis in screening for anal dysplasia and investigation into potential mechanisms of how these microbial imbalances influence the immune system and anal carcinogenesis.

AB - Background: Squamous cell carcinoma of the anus (SCCA) is a rare gastrointestinal cancer. Factors associated with progression of HPV infection to anal dysplasia and cancer are unclear and screening guidelines and approaches for anal dysplasia are less clear than for cervical dysplasia. One potential contributing factor is the anorectal microbiome. In this study, we aimed to identify differences in anal microbiome composition in the settings of HPV infection, anal dysplasia, and anal cancer in this rare disease. Methods: Patients were enrolled in two prospective studies. Patients with anal dysplasia were part of a cross-sectional cohort that enrolled women with high-grade lower genital tract dysplasia. Anorectal tumor swabs were prospectively collected from patients with biopsy-confirmed locally advanced SCCA prior to receiving standard-of-care chemoradiotherapy (CRT). Patients with high-grade lower genital tract dysplasia without anal dysplasia were considered high-risk (HR Normal). 16S V4 rRNA Microbiome sequencing was performed for anal swabs. Alpha and Beta Diversity and composition were compared for HR Normal, anal dysplasia, and anal cancer. Results: 60 patients with high-grade lower genital tract dysplasia were initially enrolled. Seven patients had concurrent anal dysplasia and 44 patients were considered HR Normal. Anorectal swabs from 21 patients with localized SCCA were included, sequenced, and analyzed in the study. Analysis of weighted and unweighted UniFrac distances demonstrated significant differences in microbial community composition between anal cancer and HR normal (p=0.018). LEfSe identified that all three groups exhibited differential enrichment of specific taxa. Peptoniphilus (p=0.028), Fusobacteria (p=0.0295), Porphyromonas (p=0.034), and Prevotella (p=0.029) were enriched in anal cancer specimens when compared to HR normal. Conclusion: Although alpha diversity was similar between HR Normal, dysplasia and cancer patients, composition differed significantly between the three groups. Increased anorectal Peptoniphilus, Fusobacteria, Porphyromonas, and Prevotella abundance were associated with anal cancer. These organisms have been reported in various gastrointestinal cancers with roles in facilitating the proinflammatory microenvironment and neoplasia progression. Future work should investigate a potential role of microbiome analysis in screening for anal dysplasia and investigation into potential mechanisms of how these microbial imbalances influence the immune system and anal carcinogenesis.

KW - anal cancer

KW - anal dysplasia

KW - anorectal microbiome

KW - cancer biology

KW - HPV-related cancer

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U2 - 10.3389/fimmu.2023.1051431

DO - 10.3389/fimmu.2023.1051431

M3 - Article

C2 - 37063829

AN - SCOPUS:85152631962

SN - 1664-3224

VL - 14

JO - Frontiers in immunology

JF - Frontiers in immunology

M1 - 1051431

ER -

HPV-related anal cancer is associated with changes in the anorectal microbiome during cancer development

Abstract

Keywords

ASJC Scopus subject areas

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