Vaginal Microbiome Clinical Trial
Official title:
The Human Microbiome in pPROM, Preterm Birth and the Neonatal Infant: a Prospective Longitudinal Pilot-study
The aims of this prospective longitudinal case-control pilot-study are (1) to characterize
the changes of the vaginal, uterine and placental microbiome in pregnant women experiencing
pPROM with immediate hospitalization and consecutive caesarean section at preterm, in
comparison to uneventful term births with elective cesarean section, as well as (2) to
evaluate the influence of the maternal on the neonatal microbiome and the early neonatal
outcome in pPROM preterm cases, in comparison to uneventful term births.
The first aim will be achieved by collecting vaginal and rectal swabs for microbiome analysis
in women experiencing pPROM, followed by uterine and placental swabs that are collected
during the caesarean section. Control samples will be collected at the same time points from
women undergoing elective caesarean section at term. The second aim will be achieved by
microbiome analysis of rectal, oral/buccal, and skin swabs taken from newborns that are
either born preterm after pPROM, or at term, both by caesarean section.
A total of 100 study participants will be included, assigned to one of the following groups:
Study group:
• This group will consist of 50 pregnant women, who experienced pPROM between 22+5 and 28+0
gestational weeks, either presenting at the primary study site, or being referred from other
hospitals, and delivered at preterm by cesarean section.
Control group:
• This group will consist of 50 pregnant women, who are scheduled for elective cesarean
section at the outpatient department of the primary study site, between a 32+0 and 37+0
gestational weeks, and delivered at term by cesarean section.
Recruitment:
Recruitment of all patients will take place at the Medical University of Vienna, Department
of Obstetrics and Gynecology. Women in the study group will be referred from outside
hospitals or will present for any reason at our department. Verification of pPROM will be
performed by speculum examination and detection of amniotic fluid pooling. In case of unclear
findings, an enzymatic test (e.g., Amnisure®, QUIAGEN Sciences, LLC; Germantown, MD 20874,
USA) will be conducted. Following pPROM verification, women who meet the inclusion criteria
will be offered to participate in the study. Those who experience a spontaneous vaginal
delivery instead of a cesarean section due to any reason, will be considered as drop-out.
Women in the control group will be recruited during their routine presentation for elective
cesarean section (for any reason that does not meet the exclusion criteria of the study) that
will be scheduled at term. Those who experience preterm birth although being scheduled for
elective cesarean at term, will be considered as drop-out. During their consultation at the
outpatient department, these women will be offered to participate in the study.
Sampling:
All swabs will be collected from sub-investigators of this study using a standardized
procedure. For anonymization, only the collection time point, location and ward will be
marked on the swab tubes. After informed consent, vaginal swabs will be collected during
speculum examination from the lateral vaginal wall and posterior fornix vaginae using a
sterile cotton swab combined with an epithelial brush. A rectal swab will be collected by
insertion of a sterile swab into the anal sphincter. Intraoperative swabs of the placenta and
uterine cavity will be collected during caesarean section under sterile conditions. Neonatal
swabs (buccal mucosa and skin) will be collected directly after delivery and in the neonatal
period. Stool samples will be taken from the meconium, defined as first stool of the infant
and the stool of the newborn in the neonatal period. All specimens will immediately be stored
at -80°C after collection. The epithelial brush will be put into RNAlater® RNA stabilization
solution and stored at -80°C.
Microbiome analysis:
Microbiome analysis will be performed at the Joint Microbiome Facility (JMF) of the Medical
University of Vienna and the University of Vienna. Testing will be performed by sub-
investigators at the JMF. The microbial community composition in collected stool swab samples
will be determined by 16S rRNA gene amplicon sequencing. Briefly, DNA will be extracted with
the QIAamp Microbiome Kit or QIAamp DNA Mini Kit (for swab and stool samples, respectively),
followed by 16S rRNA gene amplification and barcoding as previously described. Multiplexed
amplicon samples sequenced on the Illumina MiSeq platform at the JMF. Negative controls
performed during DNA extraction and 16S rRNA gene amplification are routinely included in the
sample processing workflow. The obtained sequence data will be quality-filtered and
demultiplexed, followed by amplicon sequencing variant (ASV) inference with DADA2,16 enabling
analysis at the highest possible taxonomic resolution. Resulting ASV sequences will be
taxonomically classified using SINA with the newest release of the the SILVA SSU rRNA
database. If necessary, contaminants will be removed in silico using the decontam software
package.
Perinatal data:
In addition to swab sampling and analysis, the following perinatal parameters will be
collected, using the PIA Fetal Database, version 5.6.16.917 (GE Viewpoint, Munich, Germany):
Maternal age [number], parity [number], tertiary education [yes/no], ethnicity [category],
relationship status [category], body mass index [number], nicotine abuse [yes/no], history of
pPROM [yes/no], history of PTB [yes/no], preexisting diseases [category], vaginal infection
screening [yes/no], cervical insufficiency [yes/no], preeclampsia [yes/no], bleeding
[yes/no], antenatal steroid prophylaxis [yes/no], ongoing antibiotic treatment [yes/no],
tocolysis [yes/no], magnesium prophylaxis [yes/no], gestational week at delivery [number],
birthweight [number], Apgar score at 1/5/10 minutes [number], umbilical cord arterial pH
[number], transfer to neonatal intensive care unit [yes/no].
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