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大鼠γ-谷氨酰转移酶基因的三个替代启动子在发育中的肺中具有活性,并且在出生后受氧气的差异调节。

Three alternative promoters of the rat gamma-glutamyl transferase gene are active in developing lung and are differentially regulated by oxygen after birth.

作者信息

Joyce-Brady M, Oakes S M, Wuthrich D, Laperche Y

机构信息

Pulmonary Center, Department of Medicine, Boston University School of Medicine, MA, 02118, USA.

出版信息

J Clin Invest. 1996 Apr 1;97(7):1774-9. doi: 10.1172/JCI118605.

Abstract

The rat gamma-glutamyl transferase mRNA transcripts I, II, and III are derived from three alternative promoters, P(I), P(II), and P(III). In the adult only mRNA III is expressed in the lung. We show that mRNA III gene expression is developmentally regulated in the fetal lung; it is first expressed in gestation. In contrast to the adult lung, the fetal lung expresses mRNA I, II, and III. The switch from the fetal to the adult pattern of gammaGT mRNA expression begins within the first 24 h of birth and is complete by 10 d of age. gammaGT mRNA II disappears within 24 h, mRNA I disappears by 10 d leaving mRNA III as the sole transcript. Alveolar epithelial type 2 cells (AT2) isolated from the adult lung express only mRNA III. When cultured in 21% O2 mRNA III is maintained, but when cultured in 3% O2 the fetal pattern of mRNA I, II and III expression is induced. When AT2 cells in hypoxia are exposed to carbon monoxide, mRNA II is suppressed suggesting that a heme-binding protein (responsive to oxygen) may suppress mRNA II expression and may be responsible for the decrease in lung mRNA II seen after birth. A reporter gene under the control of DNA sequences from the gammaGT P(III) promoter is activated in transient transfection studies in response to hyperoxia, while a deletion construct retaining an antioxidant responsive element is not. Oxygen appears to regulate each of the alternative promoters of the gammaGT gene, such that P(II) is rapidly repressed by a heme-dependent mechanism, P(I), is more gradually repressed by a nonheme mechanism and P(III) is activated by a putative oxygen response element. We hypothesize that similar oxygen-dependent mechanisms regulate other genes in the developing lung at birth.

摘要

大鼠γ-谷氨酰转移酶mRNA转录本I、II和III源自三个可变启动子,即P(I)、P(II)和P(III)。在成年大鼠中,只有mRNA III在肺中表达。我们发现,mRNA III基因表达在胎儿肺中受到发育调控;它在妊娠期首次表达。与成年肺不同,胎儿肺表达mRNA I、II和III。γGT mRNA表达从胎儿模式向成年模式的转变在出生后的头24小时内开始,并在出生后10天时完成。γGT mRNA II在24小时内消失,mRNA I在10天时消失,仅留下mRNA III作为唯一的转录本。从成年肺中分离出的肺泡II型上皮细胞(AT2)仅表达mRNA III。当在21%氧气中培养时,mRNA III得以维持,但当在3%氧气中培养时,会诱导出胎儿模式的mRNA I、II和III表达。当缺氧的AT2细胞暴露于一氧化碳时,mRNA II受到抑制,这表明一种血红素结合蛋白(对氧气有反应)可能会抑制mRNA II的表达,并且可能是出生后肺中mRNA II减少的原因。在瞬时转染研究中,受γGT P(III)启动子DNA序列控制的报告基因在高氧条件下被激活,而保留抗氧化反应元件的缺失构建体则未被激活。氧气似乎调节γGT基因的每个可变启动子,使得P(II)通过血红素依赖性机制迅速被抑制,P(I)通过非血红素机制更缓慢地被抑制,而P(III)通过假定的氧反应元件被激活。我们推测,类似的氧依赖性机制在出生时调节发育中的肺中的其他基因。

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