Periodontitis Clinical Trial
Official title:
Inflammatory Cytokines in Gingival Crevicular Fluid and Placental Tissues in Chronic Periodontitis Patients With Preterm Delivery
Investigators have shown the presence of elevated proinflammatory cytokines in amniotic
fluid in patients in preterm labor.However, there is limited and mostly negative evidence
that the elevation of these mediators in gingival crevicular fluid (GCF), and amniotic fluid
are associated with pregnancy complications in periodontitis patients. Thus this case
control study will be conducted to
1. To determine the level of proinflammatory cytokines in gingival crevicular fluid in
women with spontaneous preterm delivery with chronic periodontitis.
2. To investigate the expression of macrophage inflammatory protein-1α in placental
tissues.
3. To assess the possible correlation between chronic periodontitis and preterm delivery.
Periodontal disease is a commonGram-negative chronic anaerobic infection of the
periodontium, with an estimatedworld prevalence of 10% to 15% (Genco RJ, et al. 1992,
Petersen PE & Ogawa H. 2005). It Involves both direct tissue damage resulting from plaque
bacterial products, and indirect damage via host inflammatory and immune responsesmediated by
interactions between numerous cell populations and inflammatory mediators (Yucel-Lindberg
T&Båge T.2013).
Periodontal infections have been associated with different systemic diseases; cardiovascular
disease, cerebrovascular disease, diabetes mellitus, respiratory infections and others
including osteoporosis, cancer, rheumatoid arthritis, erectile dysfunction, Alzheimer's
disease, gastrointestinal disease, prostatitis and renal diseases(Gulati M, et al. 2013).
Moreover, many investigators have reported an association between periodontal disease and
adverse pregnancy outcomes, including preterm birth, low birth weight, foetal growth
restriction, preeclampsia and perinatal mortality (Ide M&Papapanou PN.2013).
Preterm birth, defined as a live birth before 37 weeks of gestation, is the leading cause of
infant mortality in both developed and developing countries (Saigal S & Doyle LW. 2008),
whether following spontaneous preterm labour, premature rupture of membranes, or caesarean
section due to foetal distress or maternal medical conditions (Goldenberg RL, et al.
2008).The World Health Organization has recently estimated that annually 12.9 million or
9.6% of all children are born preterm worldwide, despite extensive research and public
health efforts(Beck S, et al. 2010).
Major causes for preterm birth are intra-amniotic infections which subsequently cause
inflammation, as well as sterile inflammation (Madan I, et al 2010). Moreover, smoking,
alcohol consumption, black race, low socio-economic status, low or high maternal body mass
index, stress, previous preterm birth, advanced maternal age and short cervix are other
associated risk factors (DjelantikA, et al. 2012).
Offenbacher et al in 1996 first hypothesized that gram-negative anaerobic pathogens from
periodontium and associated endotoxins and maternal inflammatory mediators could have a
possible adverse effect on the developing fetus (Offenbacher S, et al. 1996), whether
through translocation of periodontal pathogens to the feto-placental unit or the action of
the periodontal reservoir of inflammatory mediators, which elaborated at the remote site of
infection and trigger prostaglandins synthesis, resulting in cervical dilation, entry of
more microbes into the uterus, and continuation of the "viscous cycle" resulting in
premature birth (Gibbas RS, 2001).
Investigators have shown the presence of elevated proinflammatory cytokines in amniotic
fluid, such as interleukin-1α (IL-1α), interleukin-1β (IL-1β), interleukin-6 (IL-6),
interleukin-8 (IL-8), and tumor necrosis factor alpha (TNF-α) in patients in preterm
labor(Hillier SL, et al. 1993, Hitti J, et al. 2001, Figueroa R, et al. 2005).However, there
is limited and mostly negative evidence that the elevation of these mediators in gingival
crevicular fluid (GCF), and amniotic fluid are associated with pregnancy complications in
periodontitis patients(Madianos PN, et al. 2013).
Macrophage inflammatory proteins 1 alpha (MIP-1α/CCL3) is a member of the cysteine-cysteine
chemokine family which is secreted by macrophages, neutrophils, basophils, dendritic cells,
lymphocytes and epithelial cells and mediates granulocyte migration and adhesion. It
stimulates monocytes and/or osteoclast progenitor cells to become active osteoclasts(Menten
P, et al. 2002), as well as regulating hematopoiesis and stimulating production of other
inflammatory mediators such as IL-1, TNF alpha(Maurer M & von Stebut E. 2004).
The Level of MIP-1 in GCF found to discriminate between diseased and healthy periodontal
sites(Tymkiw KD, et al. 2011). Moreover, its presence whether in cord blood or amniotic
fluid was elevated in cases of preterm labor (Matoba N, et al 2009, Weissenbacher T, et al.
2013).
Deliveries prior to 35 weeks of gestation was typically associated with subclinical
chorioamnionitis, which is considered the most common manifestation and is defined
histologically by inflammation of the chorion, amnion, and placenta, and found to be
associated with chronic infections of low virulence organisms (Hagberg H, et al. 2002).
However, variability in the assessment criteria for the diagnosis of histological
chorioamnionitis exists within the literature (Holzman C, et al. 2007).
Since 1996, a number of studies have investigated the potential relationship between
periodontitis and preterm and low birth weight. However, results have been controversial,
suggesting the need for more research to confirm or discard this association(Sanz M, et al
2013). Thus this case control study will be conducted to investigate the association between
chronic periodontitis and preterm labor through possible correlation between Macrophage
Inflammatory Protein-1 alpha (MIP-1α), Tumor necrosis factor alpha (TNF-α) and pentrixin 3
in placental tissues and its level in GCF.
;
Observational Model: Case Control, Time Perspective: Retrospective
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