Cervicovaginal-Microbiome Analysis by 16S Sequencing and Real-Time PCR in Patients from Novosibirsk (Russia) with Cervical Lesions and Several Years after Cancer Treatment

Cervicovaginal-Microbiome Analysis by 16S Sequencing and Real-Time PCR in Patients from Novosibirsk (Russia) with Cervical Lesions and Several Years after Cancer Treatment

Disturbed cervicovaginal-microbiome (CVM) structure promotes human papillomavirus (HPV) persistence and reflects risks of cervical lesions and cancer onset and recurrence. Therefore, microbiomic biomarkers may be useful for cervical disease screening and patient management. Here, by 16S rRNA gene se...

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Published in:Diagnostics (Basel) Vol. 13; no. 1; p. 140
Main Authors: Ivanov, Mikhail K, Brenner, Evgeny V, Hodkevich, Anastasia A, Dzyubenko, Victoria V, Krasilnikov, Sergey E, Mansurova, Alphiya S, Vakhturova, Irina E, Agletdinov, Eduard F, Shumeikina, Anastasia O, Chernyshova, Alyona L, Titov, Sergei E
Format: Journal Article
Language:English
Published: Switzerland MDPI AG 01-01-2023
MDPI
Subjects:
16S rRNA gene sequencing
Age
Cancer
Cancer therapies
cancer treatment
Care and treatment
Cellular biology
Cervical cancer
cervicovaginal microbiome
Clinics
Health aspects
high-grade squamous intraepithelial lesion
Human papillomavirus
Medical screening
Microbiota (Symbiotic organisms)
Patient outcomes
Polymerase chain reaction
post-treatment effect
Regions
Thermal cycling
Vagina
Womens health
Russia
United States > US
Lactobacillus iners
cancer treatment
cervicovaginal microbiome
Cutibacterium acnes
post-treatment effect
human papillomavirus
16S rRNA gene sequencing
high-grade squamous intraepithelial lesion
real-time PCR
cervical cancer
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Summary:Disturbed cervicovaginal-microbiome (CVM) structure promotes human papillomavirus (HPV) persistence and reflects risks of cervical lesions and cancer onset and recurrence. Therefore, microbiomic biomarkers may be useful for cervical disease screening and patient management. Here, by 16S rRNA gene sequencing and commercial PCR-based diagnostic kits, we profiled CVM in cytological preparations from 140 HPV-tested women (from Novosibirsk, Russia) with normal cytological findings, cervical lesions, or cancer and from 101 women who had recently received different cancer therapies. An increase in lesion severity was accompanied by higher HPV prevalence and elevated CVM biodiversity. Post-treatment CVM was found to be enriched with well-known microbial biomarkers of dysbiosis, just as in cervical disease. Nonetheless, concentrations of some skin-borne and environmental species (which gradually increased with increasing lesion severity)-especially spp., spp., and -was low in post-treatment patients and depended on treatment types. Frequency of dominance was high in all groups and depended on treatment types in post-treatment patients. Microbiome analysis via PCR-based kits revealed statistically significant differences among all groups of patients. Thus, microbiome profiling may help to find diagnostic and prognostic markers for management of cervical lesions; quantitative PCR-based kits may be suitable for these purposes.
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ISSN:2075-4418
2075-4418
DOI:10.3390/diagnostics13010140