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1H NMR- based metabolomics approaches as non-invasive tools for diagnosis of endometriosis A Comparative Study of Blood Levels of Manganese, Some Macroelements and Heavy Metals in Obese and Non-Obese Polycystic Ovary Syndrome Patients A Comparative Study of the Gut Microbiota Associated With Immunoglobulin a Nephropathy and Membranous Nephropathy A comparative study of the gut microbiota in immune-mediated inflammatory diseases-does a common dysbiosis exist? A comprehensive analysis of breast cancer microbiota and host gene expression A comprehensive analysis of breast cancer microbiota and host gene expression A cross-sectional analysis about bacterial vaginosis, high-risk human papillomavirus infection, and cervical intraepithelial neoplasia in Chinese women A cross-sectional pilot study of birth mode and vaginal microbiota in reproductive-age women A metabonomics approach as a means for identification of potentialbiomarkers for early diagnosis of endometriosis A More Diverse Cervical Microbiome Associates with Better Clinical Outcomes in Patients with Endometriosis: A Pilot Study A Multi-Omic Systems-Based Approach Reveals Metabolic Markers of Bacterial Vaginosis and Insight into the Disease A New Approach to Polycystic Ovary Syndrome: The Gut Microbiota A Review of the Anti-inflammatory Properties of Clindamycin in the Treatment of Acne Vulgaris A Systematic Review and Meta-Analysis of Premenstrual Syndrome with Special Emphasis on Herbal Medicine and Nutritional Supplements. Adherence to the Mediterranean Diet, Dietary Patterns and Body Composition in Women with Polycystic Ovary Syndrome (PCOS)

Comprehensive profiles and diagnostic value of menopausal-specific gut microbiota in premenopausal breast cancer Original paper

Researched by:

  • Karen Pendergrass ID
    Karen Pendergrass

    User avatarKaren Pendergrass is a microbiome researcher specializing in microbiome-targeted interventions (MBTIs). She systematically analyzes scientific literature to identify microbial patterns, develop hypotheses, and validate interventions. As the founder of the Microbiome Signatures Database, she bridges microbiome research with clinical practice. In 2012, based on her own investigative research, she became the first documented case of FMT for Celiac Disease—four years before the first published case study.

March 18, 2025

  • Women’s Health
    Women’s Health

    Women’s health, a vital aspect of medical science, encompasses various conditions unique to women’s physiological makeup. Historically, women were often excluded from clinical research, leading to a gap in understanding the intricacies of women’s health needs. However, recent advancements have highlighted the significant role that the microbiome plays in these conditions, offering new insights and potential therapies. MicrobiomeSignatures.com is at the forefront of exploring the microbiome signature of each of these conditions to unravel the etiology of these diseases and develop targeted microbiome therapies.

  • Breast Cancer
    Breast Cancer

    Traditionally linked to genetic predispositions and environmental exposures, emerging evidence highlights the microbiome as a critical and underappreciated factor influencing breast cancer progression, immune response, and treatment outcomes.

Researched by:

  • Karen Pendergrass ID
    Karen Pendergrass

    User avatarKaren Pendergrass is a microbiome researcher specializing in microbiome-targeted interventions (MBTIs). She systematically analyzes scientific literature to identify microbial patterns, develop hypotheses, and validate interventions. As the founder of the Microbiome Signatures Database, she bridges microbiome research with clinical practice. In 2012, based on her own investigative research, she became the first documented case of FMT for Celiac Disease—four years before the first published case study.

Last Updated: 2024

Microbiome Signatures identifies and validates condition-specific microbiome shifts and interventions to accelerate clinical translation. Our multidisciplinary team supports clinicians, researchers, and innovators in turning microbiome science into actionable medicine.

Karen Pendergrass

Karen Pendergrass is a microbiome researcher specializing in microbiome-targeted interventions (MBTIs). She systematically analyzes scientific literature to identify microbial patterns, develop hypotheses, and validate interventions. As the founder of the Microbiome Signatures Database, she bridges microbiome research with clinical practice. In 2012, based on her own investigative research, she became the first documented case of FMT for Celiac Disease—four years before the first published case study.

What was studied?

This study investigated the gut microbiota profiles, diagnostic value, and functional pathways specific to premenopausal breast cancer patients. It aimed to identify unique gut microbial markers distinguishing premenopausal breast cancer patients from postmenopausal patients and age-matched controls. The study also explored functional pathways of gut microbiota linked to breast cancer progression and diagnostic potential.

Who was studied?

The study analyzed 267 participants divided into four groups: premenopausal controls (Pre-C, n=50), premenopausal breast cancer patients (Pre-BC, n=100), postmenopausal controls (Post-C, n=17), and postmenopausal breast cancer patients (Post-BC, n=100). All breast cancer patients were newly diagnosed with stage I–II disease and excluded if they had received treatments or medications affecting gut microbiota before fecal sample collection.

What were the most important findings?

The study highlights significant differences in gut microbial diversity, composition, and functional pathways between premenopausal and postmenopausal breast cancer patients. Premenopausal breast cancer patients showed reduced α-diversity and distinct β-diversity compared to controls, with alterations in specific bacterial taxa linked to inflammation and cancer progression. In contrast, postmenopausal patients exhibited a different microbial profile, including an increase in pathogenic bacteria. Functional pathway analyses revealed steroid-related and oncogenic pathways in premenopausal patients, while postmenopausal patients were associated with chemical carcinogenesis and aldosterone-regulated pathways. The findings emphasize the diagnostic potential of gut microbiota in differentiating breast cancer subtypes and guiding prevention strategies.

AspectPremenopausal Breast CancerPostmenopausal Breast CancerUniversal Markers (Both Types)
α-DiversitySignificantly reduced compared to controlsNo reduction observed compared to postmenopausal controls
β-DiversityDistinct from controlsDistinct from controls
Enriched MicrobesBacteroides fragilis, Anaerostipes (linked to inflammation and progression)Proteobacteria, Klebsiella pneumoniae (pathogenic bacteria)Haemophilus parainfluenzae (increased in both)
Reduced MicrobesBifidobacterium spp. (tumor suppressor)Akkermansia muciniphila (beneficial microbe)Faecalibacterium prausnitzii (decreased in both)
Functional PathwaysSteroid-related pathways; Oncogenic pathways (e.g., Notch/Wnt signaling)Chemical carcinogenesis; Aldosterone-regulated pathways
Diagnostic PotentialStrong microbial markers for distinguishing premenopausal breast cancerStrong microbial markers for distinguishing postmenopausal breast cancer

What are the greatest implications of this study?

The findings underscore the diagnostic potential of microbial markers for early, non-invasive breast cancer detection based on menopausal status. Identifying these microbial and functional pathways expands the understanding of breast cancer pathogenesis, especially in premenopausal women. Moreover, the study highlights the gut microbiota as a modifiable factor, suggesting potential interventions like probiotics or dietary changes to mitigate breast cancer risk.

Breast Cancer

Traditionally linked to genetic predispositions and environmental exposures, emerging evidence highlights the microbiome as a critical and underappreciated factor influencing breast cancer progression, immune response, and treatment outcomes.

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