Kumiko Temma-Asano scite author profile

Kumiko Temma-Asano

3Publications

41Citation Statements Received

17Citation Statements Given

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Affiliations

Osaka University, Takara (Japan), Shimizu (Japan)

Publications

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Prospective study of non‐closure or closure of the peritoneum at cesarean delivery in 124 women: Impact of prior peritoneal closure at primary cesarean on the interval time between first cesarean section and the next pregnancy and significant adhesion at second cesarean

Komoto

Shimoya

Shimizu

et al. 2006

J of Obstet and Gynaecol

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Non-closure of the peritoneum at cesarean delivery appears to have no adverse effect on postoperative recovery, it also decreases the number of analgesic doses and shortens the operating time and may be more desirable in achieving a next pregnancy. The present study demonstrated that surgical peritoneal closure resulted in more advanced adhesion formation. The practice of non-closure of the peritoneum should be performed at cesarean.

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Prospective Study of Non-Closure or Closure of the Peritoneum at Cesarean Delivery in 124 Women: Impact of Prior Peritoneal Closure at Primary Cesarean on the Interval Time Between First Cesarean Section and the Next Pregnancy and Significant Adhesion at Second Cesarean

Komoto

Shimoya

Shimizu

et al. 2007

Obstetrical & Gynecological Survey

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Oxidative stress-induced S100B protein from placenta and amnion affects soluble Endoglin release from endothelial cells

Tskitishvili

Sharentuya

Temma-Asano

et al. 2009

Molecular Human Reproduction

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Oxidative stress with elevated intracellular Ca(2+) concentration as well as endothelial dysfunction is a component of pre-eclampsia. Our aim was to investigate the oxidative stress-dependent expression of Endoglin and Ca(2+)-binding S100B protein from villous and amniotic tissue cultures, and to assess sEng expression from S100B protein-stimulated endothelial cells. We initially examined Endoglin and Hydroxy-nonenal-(HNE)-modified proteins in the placentas and amnion obtained from women with pre-eclampsia (n = 8), and healthy controls (n = 8) by immunohistochemistry. To examine oxidative stress and the S100B protein effect on sEng expression from endothelial cells, normal villous and amniotic tissue cultures were stimulated by 4-HNE, sodium fluoride and xanthine/xanthine oxidase, whereas human umbilical vein endothelial cell cultures were treated with S100B protein in a dose- and time-dependent manner at 37 degrees C in an environment of 95% air and 5% of CO(2). Culture supernatants were assessed using ELISA. Cell viability was determined using MTS assay. The concentrations of sEng and S100B protein were significantly increased in the villous and amniotic tissue culture supernatants under oxidative stress. S100B protein-stimulated endothelial cells released sEng into conditioned media with a significantly higher expression levels at a concentration of 200 pM-20 nM S100B by 2 h, whereas treated with 200 nM of S100B endothelial cells significantly expressed sEng by 12 h and stimulated the cell proliferation by the same period of time. Our findings show that oxidative stress affects sEng and S100B protein expression from villous and amniotic tissues, and picomolar and low nanomolar concentrations of S100B protein significantly up-regulate sEng release from endothelial cells leading to endothelial dysfunction.

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