Vulvodynia Clinical Trial
Official title:
Dysbiosis in the Vaginal Microbiota May be Associated With the Development of Localized Provoked Vulvodynia (LPV)
Currently, the pathogenesis of Localized Provoked Vulvodynia (LPV) has not been elucidated.
Few observations may point to involvement of the microbiome: the association of LPV with
preceding chronic recurrent candidiasis, and the reports of the beneficial effect of a diet
avoiding oxalate on Vulvodynia.
Studies in the new field of microbiome research focus on the composition of overall
microorganisms in our body and their impacts on our health. Changes in the composition of
the vaginal microbiota (dysbiosis) have been linked with different health and disease
states. We have also shown recently that women can be divided into 2 groups according to the
composition of their vaginal microbiome.
The proposed study will compare the vaginal microbiome of women with severe LPV, not treated
by diet and otherwise healthy, to women without LPV (we will also compare our results to the
NIH HMP data). Vaginal pH and date of menstrual cycle will be checked. We propose that
dysbiosis in the vaginal microbiota may trigger the development of LPV.
Vulvodynia - vulvar pain. The exact etiology has not been elucidated yet, and therapy is
often unsatisfactory. Two main types of Vulvodynia exist, with the far more common type
being Localized provoked vulvodynia (LPV), also known as Vestibulodynia, and in the past -
Vestibulitis. This study will concentrate on this common disorder which affects young women,
whose quality of life deteriorate significantly by the inability to experience vaginal sex.
The vaginal microbiome The new field of microbiome research focuses on the composition of
overall microorganisms in the human body and their impacts on our human health. Amazingly,
the number of microbial cells within our body is 10 times greater than the sum of all our
human somatic and germ cells, and they carry 150 times more genetic information than our
own. Changes in the composition of the vaginal microbiota (dysbiosis) have been linked with
different health and disease states.
The vagina is colonized with around 108-109 bacteria/mL vaginal fluid which is comparable to
the small intestine. Recently, the NIH Human Microbiome Project characterized the bacterial
communities across the human body and found that the vagina harbors low complexity bacterial
communities. These communities had the lowest alpha diversity (within sample diversity)
among the different body sites and low beta diversity (between sample diversity) at the
genus level. This diversity was high at the species level due to distinct Lactobacillus spp.
The communities were sampled at the sub sites that included the posterior fornix, mid vagina
and the vaginal introitus. There was little distinction between the three sites hence we
will focus on posterior fornix. The vaginal communities of healthy women, have also been
repeatedly observed to occupy one of five states, four dominated by Lactobacillus spp. and
one by higher overall microbial diversity. Shifts between the community structures within
individuals (dysbiosis) are associated with disease states so it would be interesting to
study whether women with LPV belong to a different enterotype than healthy women.
The vaginal microbial communities have been shown to change during different stages in a
woman's life and to influence pregnancy. As early as 1930, Cruickshank and Baird described
changes in the vaginal bacterial communities that occurred between the 5th and 7th month of
pregnancy.
In 2010 a study was undertaken among Amerindian women to examine the microbial vaginal
signature at term in relation to delivery mode (n=9). Variability in vaginal taxa was noted
between subjects particularly for Lactobacillus species. Metagenomic analysis of the vaginal
microbiome in a cross-sectional study of 24 healthy pregnant women and 60 non-pregnant
controls at three vaginal sites (introitus, posterior fornix and midvagina) found the
richness and diversity of the vaginal microbiome to be reduced in pregnancy in ways that did
not appear to be driven by BMI, race or ethnicity . As pregnancy progressed and as proximity
to the uterus increased, less diversity and richness were noted. Lactobacillus species were
enriched in pregnancy, which the authors postulated may be biologically significant as
lactic acid bacteria produce bacteriocins that may reduce the risk of ascending infections.
It has also been proposed that the vaginal microbiota has the potential to influence the
conception process by influencing the local production of proinflammatory cytokines which in
turn impact the survival rate and motility of sperm cells.
The vaginal microbiome and Vulvodynia Several microorganisms have been discussed for
presumed role in LPV development: LPV is frequently associated with preceding chronic
recurrent candidiasis, LPV may be produced in a mouse model by repeated vulvovaginal fungal
infection, the difficulty in treating women with concomitant LPV and candidiasis
(complicated LPV), the reports of the beneficial effect of treatment with combined
antibiotics, aimed at eradicating H. pylori peptic condition (although H. pylori has not
been detected in LPV tissues).
Indirect evidence of the role of the microbiome with the development of LPV may be deduced
from the beneficial effect (14.3 - 50%), reported by some authors, of a diet avoiding
oxalate and rich in Calcium citrate, on LPV. As women with LPV consume more oxalate -
although not significantly, we suspect that the variability in response rate may be due to
the indirect effect of the diet - through changes in the microbiome, which may be affecting
LPV severity. In addition, the adverse effect of oral contraceptive pills (OCP) in
increasing LPV symptoms; OCP tend to change the composition of the vaginal microbiota,
consequent to their effect of thinning and dehydrating the vaginal mucosa. These finding
prompt us to further inquire the possible association of vaginal microbiome dysbiosis and
the development of LPV.
Objective:
The proposed study will first compare the vaginal microbiome of women with severe LPV, not
treated by diet and otherwise healthy, to women without LPV (we will also compare our
results to the NIH HMP data). At the second stage we will characterize the effect of a
three-month low oxalate diet on the vaginal microbiota of women with LPV and on the outcome
compared to a group of patients with LPV not treated by diet. Vaginal pH and date of
menstrual cycle will be checked. We propose that dysbiosis in the vaginal microbiota may
trigger the development of LPV.
Vulvodynia subtype:
- The research will study women with localized provoked Vulvodynia
- Only secondary type of LPV will be included.
- LPV diagnosis will be based on documenting first two Friedrich's criteria for vulva
vestibulits syndrome: patient's complaint of entry dyspareunia, a positive Q-tip test.
- Only women suffering from levels II or III dyspareunia according to Marinoff : Level II
is where the pain prevents intercourse from taking place on most occasions; and Level
III where pain results in total apareunia.
Methods/Protocol This will be a double blind, prospective study comparing the microbiome of
women with severe LPV to women without LPV, and to compare the effect of consuming the low
oxalate diet with calcium citrate supplements for one month on the microbiome of women with
LPV.
The local Institutional Review Board approval has been requested. Every woman participating
in the study will sign an informed consent prior to enrollment.
Study group
The study group will consist of 35 women:
- Meeting first two Friedrich's criteria for vulva vestibulitis syndrome
- Diagnosed by a gynecological examination with Localized Provoked Vulvodynia
- Diagnosed with a Level II or III degree of the syndrome according to Marinoff Control
group
- The control group will consist of 35 consecutive women who are referred to the
departments of the co-investigators. Presentation of LPV is an exclusion criterion.
Materials and Methods:
Prior to enrollment, the women will be questioned about possible inclusion and exclusion
criteria, and fill in the ISSVD Vulvodynia questionnaire.
Women found suitable for the study will undergo a Q-tip test to confirm the diagnosis of
Vestibulodynia. Women of the LPV group will be instructed to consume a "low oxalate diet"
with calcium citrate supplements, as recommended by Solomons et al for the duration of at
least one month, to assess its impact on the vaginal microbiome.
Clinical pain scores and vulvar sensitivity by Q-tip test will be repeated after one month
and compared to the clinical pain scores at the beginning of the study. Subjective
evaluation will be carried out by comparing personal data from questionnaires filled in at
enrollment and one month later.
Clinical evaluation will be performed by an experienced vulvar expert, using the pain
intensity scale (The 11 points (0-10) pain intensity numerical rating scale-PI-NRS), in
seven foci throughout the vestibule (the Q-tip test) and by comparing patients' responses to
questionnaires evaluating pain during intercourse or other activities (riding a
bicycle/horse), before and after diet.
;
Allocation: Randomized, Endpoint Classification: Efficacy Study, Intervention Model: Parallel Assignment, Masking: Open Label
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