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Transcriptome and microbiome-immune changes across preinvasive and invasive anal cancer lesions
Ezequiel Lacunza, Valeria Fink, María E. Salas, Ana M. Gun, Jorge A. Basiletti, María A. Picconi, Mariano Golubicki, Juan Robbio, Mirta Kujaruk, Soledad Iseas, Sion Williams, María I. Figueroa, Omar Coso, Pedro Cahn, Juan C. Ramos, Martín C. Abba
Ezequiel Lacunza, Valeria Fink, María E. Salas, Ana M. Gun, Jorge A. Basiletti, María A. Picconi, Mariano Golubicki, Juan Robbio, Mirta Kujaruk, Soledad Iseas, Sion Williams, María I. Figueroa, Omar Coso, Pedro Cahn, Juan C. Ramos, Martín C. Abba
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Research Article Cell biology Oncology

Transcriptome and microbiome-immune changes across preinvasive and invasive anal cancer lesions

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Abstract

Anal squamous cell carcinoma (ASCC) is a rare gastrointestinal malignancy linked to high-risk human papillomavirus (HPV) infection, which develops from precursor lesions like low-grade squamous intraepithelial lesions and high-grade squamous intraepithelial lesions (HGSILs). ASCC incidence varies across populations and poses increased risk for people living with HIV. Our investigation focused on transcriptomic and metatranscriptomic changes from squamous intraepithelial lesions to ASCC. Metatranscriptomic analysis highlighted specific bacterial species (e.g., Fusobacterium nucleatum, Bacteroides fragilis) more prevalent in ASCC than precancerous lesions. These species correlated with gene-encoding enzymes (Acca, glyQ, eno, pgk, por) and oncoproteins (FadA, dnaK), presenting potential diagnostic or treatment markers. Unsupervised transcriptomic analysis identified distinct sample clusters reflecting histological diagnosis, immune infiltrate, HIV/HPV status, and pathway activities, recapitulating anal cancer progression’s natural history. Our study unveiled molecular mechanisms in anal cancer progression, aiding in stratifying HGSIL cases based on low or high risk of progression to malignancy.

Authors

Ezequiel Lacunza, Valeria Fink, María E. Salas, Ana M. Gun, Jorge A. Basiletti, María A. Picconi, Mariano Golubicki, Juan Robbio, Mirta Kujaruk, Soledad Iseas, Sion Williams, María I. Figueroa, Omar Coso, Pedro Cahn, Juan C. Ramos, Martín C. Abba

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Figure 8

Comparative analysis of gene signature expression patterns and enriched pathways in HNSCC, cervical lesions, and anal lesions.

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Comparative analysis of gene signature expression patterns and enriched ...
(A) Heatmap visualization of HNSCC gene signature across our sample cohort, grouped by immune score within each diagnosis category. Additionally, the epidermal differentiation score is displayed. (B) Heatmap visualization of the ASCC gene signature expression profile in HNSCC samples organized by subtype classification according to Zhang et al., 2016 (48). (C) Heatmap visualization of CSCC gene signature across our sample cohort grouped by immune score within each diagnosis category. (D) Heatmap visualization of the ASCC gene signature across cervical lesions, arranged in ascending order based on the immune gene profile within each diagnosis category.

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