OBJECTIVE: Several matrix metalloproteinases (MMP) have been implicated in preterm parturition. We hypothesized that administration of a MMP inhibitor would reduce the rate of inflammation-mediated preterm delivery and prolong gestation in a mouse model. STUDY DESIGN: We utilized an animal model of endotoxin-induced preterm delivery using timed pregnant C57Bl6 mice. Test animals received lipopolysaccharide (LPS) followed by the MMP inhibitor at 1 dose 12 hours after the LPS. Control mice received the same dose of LPS, followed by a control solution 12 hours after the LPS. The primary outcome was preterm delivery rate. RESULTS: Mice in the study group had a significantly lower rate of preterm delivery (44%) compared to 100% in the controls (P = .009). Furthermore, the latency between the administration of injection and delivery was also longer in the study group (means 28.3 hours, standard deviation 9.4 hours) than among controls (mean 15.7 hours, standard deviation 1.8 hours) (P < .001). CONCLUSION: Administration of an MMP inhibitor results in a decreased rate of inflammation-mediated preterm delivery in this animal model.
OBJECTIVE: Several matrix metalloproteinases (MMP) have been implicated in preterm parturition. We hypothesized that administration of a MMP inhibitor would reduce the rate of inflammation-mediated preterm delivery and prolong gestation in a mouse model. STUDY DESIGN: We utilized an animal model of endotoxin-induced preterm delivery using timed pregnant C57Bl6 mice. Test animals received lipopolysaccharide (LPS) followed by the MMP inhibitor at 1 dose 12 hours after the LPS. Control mice received the same dose of LPS, followed by a control solution 12 hours after the LPS. The primary outcome was preterm delivery rate. RESULTS:Mice in the study group had a significantly lower rate of preterm delivery (44%) compared to 100% in the controls (P = .009). Furthermore, the latency between the administration of injection and delivery was also longer in the study group (means 28.3 hours, standard deviation 9.4 hours) than among controls (mean 15.7 hours, standard deviation 1.8 hours) (P < .001). CONCLUSION: Administration of an MMP inhibitor results in a decreased rate of inflammation-mediated preterm delivery in this animal model.
Authors: Seung Mi Lee; Roberto Romero; Jeong Woo Park; Sun Min Kim; Chan-Wook Park; Steven J Korzeniewski; Tinnakorn Chaiworapongsa; Bo Hyun Yoon Journal: J Matern Fetal Neonatal Med Date: 2012-04-25
Authors: Sruthi Sundaram; Charles R Ashby; Ryan Pekson; Vaishali Sampat; Ravikumar Sitapara; Lin Mantell; Chih-Hung Chen; Haoting Yen; Khushboo Abhichandani; Swapna Munnangi; Nikhil Khadtare; Ralph A Stephani; Sandra E Reznik Journal: Am J Pathol Date: 2013-06-12 Impact factor: 4.307
Authors: Laura A McCallum; Stephanie L Pierce; Sarah K England; Iain A Greenwood; Rachel M Tribe Journal: J Cell Mol Med Date: 2011-03 Impact factor: 5.310