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首页> 外文期刊>Journal of Molecular Endocrinology >Identification of protein kinases that control ovarian hormone release by selective siRNAs
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Identification of protein kinases that control ovarian hormone release by selective siRNAs

机译:通过选择性siRNA识别控制卵巢激素释放的蛋白激酶

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摘要

The goal of this study was to identify protein kinases (PKs) that control the secretory activity of human ovarian cells. Cultured ovarian granulosa cells were transfected with 264 siRNA constructs that selectively block the expression of 88 known PKs. The efficiency of transfection and of silencing marker molecules (glyceraldehyde 3-phosphate dehydrogenase, GAPDH and CDC2/p34 PK) was validated by fluorescence microscopy, real-time reverse transcription-PCR, and immunocytochemistry. Release of steroid hormones (progesterone, P4) and IGF1 was determined by RIA. siRNA suppressed the expression of marker molecules by up to 84%. P4 release was suppressed after inhibiting 34 individual PKs and was stimulated after inhibiting 12 PKs. Blocking nine individual PKs inhibited IGF1 release, while the inactivation of 17 others stimulated IGF1 release. Together, these results demonstrate that the release of both steroid and peptide hormones by human ovarian cells is controlled by a large number of PKs, and that siRNA constructs may be useful tools for further defining the role of PKs in controlling ovarian secretory function.
机译:这项研究的目的是确定控制人类卵巢细胞分泌活性的蛋白激酶(PKS)。用264 siRNA构建体转染培养的卵巢颗粒细胞,该构建体选择性阻断88种已知PK的表达。转染和沉默标记分子(3-磷酸甘油醛脱氢酶,GAPDH和CDC2 / p34 PK)的效率已通过荧光显微镜,实时逆转录PCR和免疫细胞化学验证。 RIA测定了类固醇激素(孕酮,P4)和IGF1的释放。 siRNA抑制标记分子的表达高达84%。抑制34个个体PK后抑制P4释放,抑制12个PK后刺激P4释放。阻断9种个体PK抑制了IGF1的释放,而其他17种的失活刺激了IGF1的释放。总之,这些结果表明人卵巢细胞释放甾体和肽激素均受大量PK的控制,而siRNA构建体可能是进一步定义PK在控制卵巢分泌功能中的作用的有用工具。

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