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在体内昼夜节律调节过程中,不同的肝细胞表达胆固醇7α-羟化酶基因。

Different hepatocytes express the cholesterol 7 alpha-hydroxylase gene during its circadian modulation in vivo.

作者信息

Berkowitz C M, Shen C S, Bilir B M, Guibert E, Gumucio J J

机构信息

Department of Medicine, Veterans Affairs Medical Center, MI 48105, USA.

出版信息

Hepatology. 1995 Jun;21(6):1658-67. doi: 10.1016/0270-9139(95)90472-7.

DOI:10.1016/0270-9139(95)90472-7
PMID:7768512
Abstract

Cholesterol 7 alpha-hydroxylase, the rate-limiting enzyme in bile salt synthesis from cholesterol is a P450 enzyme (CYP7A). Its expression and activity are regulated by bile salts, cholesterol, hormones and a circadian modulator. Here we define the hepatocytes contributing to the expression of the rat CYP7A gene during its in vivo circadian variation. The diurnal expression of the CYP7A messenger RNA (mRNA) was studied by in situ hybridization and correlated with the diurnal rate of CYP7A gene transcription and mRNA expression. At 10 AM, the time of lowest mRNA expression and gene transcription rate, only four to five hepatocytes, located close to the hepatic venules ("perivenular"), contained the CYP7A mRNA. At 10 PM, the time of highest mRNA expression and fastest in vitro transcription rate, approximately one half of the hepatocytes (still in a "perivenular" location) contained the cholesterol 7 alpha-hydroxylase mRNA. In addition, the measured half-life of the CYP7A mRNA was shorter at 10 AM than at 10 PM suggesting that posttranscriptional mechanisms also contributed to the observed circadian differences. Therefore, the basal transcription rate of the CYP7A gene is maintained by four to five "perivenular" hepatocytes. During the circadian variation, the rate of gene transcription increases in these "perivenular" hepatocytes, but in addition, there is recruitment of other more proximal hepatocytes to transcribe the gene. It is proposed here that the response of specific hepatocytes to the various modulators of CYP7A gene expression is dependent on the relative position of these hepatocytes within the liver cell plate.

摘要

胆固醇7α-羟化酶是胆固醇合成胆盐过程中的限速酶,是一种细胞色素P450酶(CYP7A)。其表达和活性受胆盐、胆固醇、激素和昼夜调节因子的调控。在此,我们确定了在大鼠CYP7A基因体内昼夜变化过程中,哪些肝细胞参与了该基因的表达。通过原位杂交研究了CYP7A信使核糖核酸(mRNA)的昼夜表达,并将其与CYP7A基因转录和mRNA表达的昼夜速率相关联。上午10点,即mRNA表达和基因转录速率最低的时间,只有四到五个靠近肝静脉(“中央静脉周围”)的肝细胞含有CYP7A mRNA。晚上10点,即mRNA表达最高且体外转录速率最快的时间,大约一半的肝细胞(仍处于“中央静脉周围”位置)含有胆固醇7α-羟化酶mRNA。此外,上午10点时测得的CYP7A mRNA半衰期比晚上10点时短,这表明转录后机制也导致了观察到的昼夜差异。因此,CYP7A基因的基础转录速率由四到五个“中央静脉周围”的肝细胞维持。在昼夜变化过程中,这些“中央静脉周围”的肝细胞中基因转录速率增加,但此外,还有其他更靠近中央静脉的肝细胞被募集来转录该基因。本文提出,特定肝细胞对CYP7A基因表达各种调节因子的反应取决于这些肝细胞在肝板内的相对位置。

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Different hepatocytes express the cholesterol 7 alpha-hydroxylase gene during its circadian modulation in vivo.在体内昼夜节律调节过程中,不同的肝细胞表达胆固醇7α-羟化酶基因。
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Insulin suppresses bile acid synthesis in cultured rat hepatocytes by down-regulation of cholesterol 7 alpha-hydroxylase and sterol 27-hydroxylase gene transcription.胰岛素通过下调胆固醇7α-羟化酶和甾醇27-羟化酶基因转录,抑制培养的大鼠肝细胞中的胆汁酸合成。
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Suppression of sterol 27-hydroxylase mRNA and transcriptional activity by bile acids in cultured rat hepatocytes.胆汁酸对培养大鼠肝细胞中胆固醇27-羟化酶mRNA及转录活性的抑制作用。
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CPF: an orphan nuclear receptor that regulates liver-specific expression of the human cholesterol 7alpha-hydroxylase gene.CPF:一种孤儿核受体,可调节人类胆固醇7α-羟化酶基因的肝脏特异性表达。
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Transcriptional regulation of cholesterol 7 alpha-hydroxylase mRNA by conjugated bile acids in primary cultures of rat hepatocytes.结合胆汁酸对大鼠肝细胞原代培养物中胆固醇7α-羟化酶mRNA的转录调控
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