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A gut microbial signature for combination immune checkpoint blockade across cancer types

Medicine and Health

A gut microbial signature for combination immune checkpoint blockade across cancer types

A. Gunjur, Y. Shao, et al.

Explore groundbreaking research by Ashray Gunjur and colleagues revealing that metagenomic sequencing of the gut microbiome can enhance predictions of immune checkpoint blockade response in rare cancers. This innovative study demonstrates how strain-resolved microbial data outperforms traditional analyses, hinting at tailored microbiome diagnostics for specific ICB regimens.

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~3 min • Beginner • English
Abstract
Immune checkpoint blockade (ICB) targeting programmed cell death protein 1 (PD-1) and cytotoxic T lymphocyte protein 4 (CTLA-4) can induce remarkable, yet unpredictable, responses across a variety of cancers. Studies suggest that there is a relationship between a cancer patient’s gut microbiota composition and clinical response to ICB; however, defining microbiome-based biomarkers that generalize across cohorts has been challenging. This may relate to previous efforts quantifying microbiota to species (or higher taxonomic rank) abundances, whereas microbial functions are often strain specific. Here, we performed deep shotgun metagenomic sequencing of baseline fecal samples from a unique, richly annotated phase 2 trial cohort of patients with diverse rare cancers treated with combination ICB (n = 106 discovery cohort). We demonstrate that strain-resolved microbial abundances improve machine learning predictions of ICB response and 12-month progression-free survival relative to models built using species-rank quantifications or comprehensive pretreatment clinical factors. Through a meta-analysis of gut metagenomes from a further six comparable studies (n = 364 validation cohort), we found cross-cancer (and cross-country) validity of strain-response signatures, but only when the training and test cohorts used concordant ICB regimens (anti-PD-1 monotherapy or combination anti-PD-1 plus anti-CTLA-4). This suggests that future development of gut microbiome diagnostics or therapeutics should be tailored according to ICB treatment regimen rather than according to cancer type.
Publisher
Nature Medicine
Published On
Mar 01, 2024
Authors
Ashray Gunjur, Yan Shao, Timothy Rozday, Oliver Klein, Andre Mu, Bastiaan W. Haak, Ben Markman, Damien Kee, Matteo S. Carlino, Craig Underhill, Sophia Frentzas, Michael Michael, Bo Gao, Jodie Palmer, Jonathan Cebon, Andreas Behren, David J. Adams, Trevor D. Lawley
Tags
Immune checkpoint blockade
microbiome
metagenomic sequencing
predictive analysis
rare cancers
machine learning
ICB regimens
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