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  •   Ιδρυματικό Αποθετήριο Πανεπιστημίου Θεσσαλίας
  • Επιστημονικές Δημοσιεύσεις Μελών ΠΘ (ΕΔΠΘ)
  • Δημοσιεύσεις σε περιοδικά, συνέδρια, κεφάλαια βιβλίων κλπ.
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  •   Ιδρυματικό Αποθετήριο Πανεπιστημίου Θεσσαλίας
  • Επιστημονικές Δημοσιεύσεις Μελών ΠΘ (ΕΔΠΘ)
  • Δημοσιεύσεις σε περιοδικά, συνέδρια, κεφάλαια βιβλίων κλπ.
  • Προβολή τεκμηρίου
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Ιδρυματικό Αποθετήριο Πανεπιστημίου Θεσσαλίας
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  • Κοινότητες & Συλλογές
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A systematic review of microbial markers for risk prediction of colorectal neoplasia

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Συγγραφέας
Yu L., Zhao G., Wang L., Zhou X., Sun J., Li X., Zhu Y., He Y., Kofonikolas K., Bogaert D., Dunlop M., Zhu Y., Theodoratou E., Li X.
Ημερομηνία
2022
Γλώσσα
en
DOI
10.1038/s41416-022-01740-7
Λέξη-κλειδί
antibiotic agent
bacterium antibody
tumor marker
biological marker
Actinomyces
antibody blood level
Article
bacterial microbiome
Bifidobacterium
cancer incidence
cancer prognosis
cancer survival
case control study
clinical outcome
cohort analysis
colorectal adenoma
colorectal cancer
colorectal tumor
controlled study
differential diagnosis
Embase
Enterococcus
feces microflora
Fusobacterium
human
Medline
microorganism
nonhuman
observational study
overall survival
Peptostreptococcus
Porphyromonas
prediction
predictive value
Prevotella intermedia
prospective study
Pseudomonas
publication bias
retrospective study
Roseburia
Salmonella
Streptococcus gallolyticus subsp. gallolyticus
systematic review
Treponema denticola
tumor diagnosis
tumor differentiation
validation study
adenoma
dysbiosis
Adenoma
Biomarkers
Colorectal Neoplasms
Dysbiosis
Humans
Prospective Studies
Springer Nature
Εμφάνιση Μεταδεδομένων
Επιτομή
Background: Substantial evidence indicates that dysbiosis of the gut microbial community is associated with colorectal neoplasia. This review aims to systematically summarise the microbial markers associated with colorectal neoplasia and to assess their predictive performance. Methods: A comprehensive literature search of MEDLINE and EMBASE databases was performed to identify eligible studies. Observational studies exploring the associations between microbial biomarkers and colorectal neoplasia were included. We also included prediction studies that constructed models using microbial markers to predict CRC and adenomas. Risk of bias for included observational and prediction studies was assessed. Results: Forty-five studies were included to assess the associations between microbial markers and colorectal neoplasia. Nine faecal microbiotas (i.e., Fusobacterium, Enterococcus, Porphyromonas, Salmonella, Pseudomonas, Peptostreptococcus, Actinomyces, Bifidobacterium and Roseburia), two oral pathogens (i.e., Treponema denticola and Prevotella intermedia) and serum antibody levels response to Streptococcus gallolyticus subspecies gallolyticus were found to be consistently associated with colorectal neoplasia. Thirty studies reported prediction models using microbial markers, and 83.3% of these models had acceptable-to-good discrimination (AUROC > 0.75). The results of predictive performance were promising, but most of the studies were limited to small number of cases (range: 9–485 cases) and lack of independent external validation (76.7%). Conclusions: This review provides insight into the evidence supporting the association between different types of microbial species and their predictive value for colorectal neoplasia. Prediction models developed from case-control studies require further external validation in high-quality prospective studies. Further studies should assess the feasibility and impact of incorporating microbial biomarkers in CRC screening programme. © 2022, The Author(s).
URI
http://hdl.handle.net/11615/80902
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  • Δημοσιεύσεις σε περιοδικά, συνέδρια, κεφάλαια βιβλίων κλπ. [19735]

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