HDAC2 was involved in placental P-glycoprotein regulation both in vitro and vivo

HDAC2 参与体内和体外胎盘 P 糖蛋白的调节

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作者:Hongyu Duan, Kaiyu Zhou, Yi Zhang, Peng Yue, Tao Wang, Yifei Li, Dajian Qiu, Jinlin Wu, Yimin Hua, Chuan Wang

Conclusion

HDAC2 inhibition could result in induction of placental P-gp expression and functionality both in vitro and in vivo.

Methods

BeWo and JAR cells were transfected with HDAC1/2/3 specific siRNA. After 48 h of transfection, cells were harvested for real-time quantitative PCR (qRT-PCR), Western blot, immunofluorescence and fluorescent dye efflux assay to evaluate P-gp expression, localization, and efflux activity, respectively. Hdac2 siRNA was intraperitoneally injected to pregnant mice every 48 h from E7.5 to E15.5 and digoxin was administered by gavages 1 h prior to euthanasia at E16.5. Placental Hdac1/2/3 and P-gp expression were determined by qRT-PCR and Western blot. Maternal plasma and fetal-unit digoxin concentrations were detected by enzyme-multiplied immunoassay.

Results

In vitro, HDAC2 inhibition could significantly elevate P-gp expression and reduce intracellular accumulation of P-gp substrates (DiOC2 (3) and Rh 123) both in BeWo and JAR, while knockdown of HDAC1/3 had no influence on P-gp expression and its efflux activity. Additionally, in vivo, Hdac2 silencing in pregnant mice also elevated placental P-gp expression and decreased digoxin transplacental transfer rate.

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