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The interaction between vaginal microbiota, cervical length, and vaginal progesterone treatment for preterm birth risk
Authors
A Sundquist
AT Northen
+76 more
B Carbonne
B Chaban
C Nold
CA Blish
CW Africa
DA MacIntyre
DB DiGiulio
DB Hardy
DH Parks
EB Fonseca
F Facchinetti
G Ekman-Ordeberg
G Reid
GG Donders
GG Donders
GT Spear
H Borgdorff
H Borgdorff
H Leitich
H Tan
H Verstraelen
IM Linhares
J Grimes-Dennis
J Martius
J Ravel
J Shen
JA Loudon
JD Iams
JD Iams
JH Wijgert van de
JHHM Wijgert van de
JJ Kozich
JL Gotkin
JM Macklaim
JM O’Brien
JS Joergensen
K Gupta
KL Nunn
L Anderson
L Liu
L Petricevic
LJ Ralph
LJ Resseguie
LM Kindinger
M Chandiramani
MA Os van
MC McCormick
MG Dominguez-Bello
MJ Ferris
MN Anahtar
N Breslow
PB Eckburg
PD Schloss
PJ Turnbaugh
Q Wang
R Rampersaud
R Romero
R Romero
R Romero
R Romero
R Tamrakar
RA Word
RC Edgar
RL Goldenberg
RM Brotman
RM Brotman
S Guaschino
S Hassan
S Srinivasan
SL Hillier
SM Yellon
SY Doerflinger
V Berghella
V Berghella
Y Benjamini
Z Alfirevic
Publication date
15 December 2016
Publisher
'Springer Science and Business Media LLC'
Doi
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on
PubMed
Abstract
© The Author(s) 2017. Background: Preterm birth is the primary cause of infant death worldwide. A short cervix in the second trimester of pregnancy is a risk factor for preterm birth. In specific patient cohorts, vaginal progesterone reduces this risk. Using 16S rRNA gene sequencing, we undertook a prospective study in women at risk of preterm birth (n = 161) to assess (1) the relationship between vaginal microbiota and cervical length in the second trimester and preterm birth risk and (2) the impact of vaginal progesterone on vaginal bacterial communities in women with a short cervix. Results: Lactobacillus iners dominance at 16 weeks of gestation was significantly associated with both a short cervix < 25 mm (n = 15, P < 0.05) and preterm birth < 34+0 weeks (n = 18; P < 0.01; 69% PPV). In contrast, Lactobacillus crispatus dominance was highly predictive of term birth (n = 127, 98% PPV). Cervical shortening and preterm birth were not associated with vaginal dysbiosis. A longitudinal characterization of vaginal microbiota (< 18, 22, 28, and 34 weeks) was then undertaken in women receiving vaginal progesterone (400 mg/OD, n = 25) versus controls (n = 42). Progesterone did not alter vaginal bacterial community structure nor reduce L. iners-associated preterm birth (< 34 weeks). Conclusions: L. iners dominance of the vaginal microbiota at 16 weeks of gestation is a risk factor for preterm birth, whereas L. crispatus dominance is protective against preterm birth. Vaginal progesterone does not appear to impact the pregnancy vaginal microbiota. Patients and clinicians who may be concerned about "infection risk" associated with the use of a vaginal pessary during high-risk pregnancy can be reassured
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