AI Article Synopsis

  • Preterm delivery (PTD) significantly contributes to neonatal mortality and morbidity, with its underlying causes often unclear, especially in Northeast India, where PTD rates are high.
  • A study involving 109 PTD cases and 100 term delivery cases examined the relationship between deregulation in the progesterone receptor (PR) pathway and immune responses related to PTD.
  • Findings indicated that downregulation of PR and its downstream effectors like PIBF correlates with increased susceptibility to PTD, lower gestational periods, and poor pregnancy outcomes, linked to an inflammatory immune response characterized by higher TNF-α and lower IL-10 levels.

Article Abstract

Preterm delivery (PTD) is one of the potent contributor of neonatal mortality and morbidity, and the underlying cause in some situation is elusive. This study attempts to delineate the association of deregulation in progesterone receptor (PR) pathway and deleterious immune responses in predisposing patients to PTD in Northeast India, a region with high rate of PTD cases. A total of 109 cases of PTD and 100 term delivery cases were enrolled with all clinical details. The PTD cases were stratified based on gestation age at delivery. The differential expression of PR and key downstream effectors and cytokines were evaluated for correlation with PTD susceptibility, gestational period, and pregnancy outcome. The results indicated a sharp downregulation in PR expression is associated with PTD susceptibility, lower gestational period and negative pregnancy outcome. The PR downstream effector PIBF was also found to be downregulated in PTD, and is associated with gestational period and negative pregnancy outcome. The downregulation of PR and PIBF expression was found to correlate with a predominant Th1 state with higher CD56+NK cell counts and pro-inflammatory burst lead by hyper TNF-α, NF-kB and IFNγ expression, and complicated by lower IL10 expression, contributing to PTD as well as negative pregnancy outcome in the PTD cases. TNF-α expression in placenta inversely correlated with placental PR expression. To conclude, deregulation in PR pathway is a hallmark of preterm delivery and negative pregnancy outcome. Differential expression of several markers such as PR, PIBF and TNF-α has prognostic significance, and hence is of clinical significance.

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Source
http://dx.doi.org/10.1016/j.jri.2016.10.001DOI Listing

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