Breast Cancer Survivors and Healthy Women: Could Gut Microbiota Make a Difference?-"BiotaCancerSurvivors": A Case-Control Study

Breast Cancer Survivors and Healthy Women: Could Gut Microbiota Make a Difference?-"BiotaCancerSurvivors": A Case-Control Study

In this first analysis, samples from 23 BC survivors (group 1) and 291 healthy female controls (group 2) were characterised through the V3 and V4 regions that encode the "16S rRNA" gene of each bacteria. The samples were sequenced by next-generation sequencing (NGS), and the taxonomy was i...

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Bibliographic Details
Published in:Cancers Vol. 15; no. 3; p. 594
Main Authors: Caleça, Telma, Ribeiro, Pedro, Vitorino, Marina, Menezes, Maria, Sampaio-Alves, Mafalda, Mendes, Ana Duarte, Vicente, Rodrigo, Negreiros, Ida, Faria, Ana, Costa, Diogo Alpuim
Format: Journal Article
Language:English
Published: Switzerland MDPI AG 18-01-2023
MDPI
Subjects:
Bar codes
Body mass index
Breast cancer
Cancer survivors
Cancer therapies
Dysbacteriosis
Family medical history
Genera
Health aspects
Intestinal microflora
Metabolism
Metabolites
Microbiota
Microbiota (Symbiotic organisms)
Next-generation sequencing
Patient outcomes
Patients
Population
Quality of life
rRNA 16S
Survival
Taxonomy
Womens health
Portugal
United States > US
microbiota
survivorship
case-control study
survivors
breast cancer
cancer
microbiome
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Summary:In this first analysis, samples from 23 BC survivors (group 1) and 291 healthy female controls (group 2) were characterised through the V3 and V4 regions that encode the "16S rRNA" gene of each bacteria. The samples were sequenced by next-generation sequencing (NGS), and the taxonomy was identified by resorting to Kraken2 and improved with Bracken, using a curated database called 'GutHealth_DB'. The α and β-diversity analyses were used to determine the richness and evenness of the gut microbiota. A non-parametric Mann-Whitney test was applied to assess differential abundance between both groups. The Firmicutes/Bacteroidetes (F/B) ratio was calculated using a Kruskal-Wallis chi-squared test. The α-diversity was significantly higher in group 1 ( = 0.28 × 10 for the Chao index and = 1.64 × 10 for the ACE index). The Shannon index, a marker of richness and evenness, was not statistically different between the two groups ( = 0.72). The microbiota composition was different between the two groups: a null hypothesis was rejected for PERMANOVA ( = 9.99 × 10 ) and Anosim ( = 0.04) and was not rejected for β-dispersion ( = 0.158), using Unifrac weighted distance. The relative abundance of 14 phyla, 29 classes, 25 orders, 64 families, 116 genera, and 74 species differed significantly between both groups. The F/B ratio was significantly lower in group 1 than in group 2, < 0.001. Our study allowed us to observe significant taxonomic disparities in the two groups by testing the differences between BC survivors and healthy controls. Additional studies are needed to clarify the involved mechanisms and explore the relationship between microbiota and BC survivorship.
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content type line 23
ISSN:2072-6694
2072-6694
DOI:10.3390/cancers15030594