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全反式视黄酰-β-D-葡萄糖醛酸酯和全反式维甲酸对体外培养的小鼠肢芽间充质细胞软骨形成及类视黄醇代谢的影响

Effects of all-trans-retinoyl-beta-D-glucuronide and all-trans-retinoic acid on chondrogenesis and retinoid metabolism in mouse limb bud mesenchymal cells in vitro.

作者信息

Sass J O, Zimmermann B, Rühl R, Nau H

机构信息

Institut für Toxikologie und Embryopharmakologie, Fachbereich Humanmedizin, Freie Universität, Berlin, Germany.

出版信息

Arch Toxicol. 1997;71(3):142-50. doi: 10.1007/s002040050368.

Abstract

Retinoids, derivatives of vitamin A, are essential for many vertebrate functions. Furthermore, several drugs of this class of compounds are valuable in the treatment of certain forms of skin disorders and cancer. However, the therapeutic application of retinoids is limited by their teratogenic potency. The limbs are important sites of retinoid-induced malformations in rodents. Therefore, organoid cultures of limb bud mesenchymal cells have been established for screening of the teratogenic potency of retinoids. We have now applied this system to compare the effects of all-trans-retinoyl-beta-D-glucuronide (all-trans-RAG) with those of all-trans-retinoic acid (all-trans-RA) on chondrogenesis, as assessed by the Alcian blue binding assay and by electron microscopic evaluation including quantitative morphometric analysis. First data of retinoid toxicokinetics in the culture media as well as retinoid concentrations in the cultured mesenchymal limb bud cells were established. While all-trans-RA inhibited chondrogenesis at 10(-7) M by ca. 50%, tenfold higher concentrations of all-trans-RAG were necessary to obtain the same effect. This difference reflects the ratio of RA isomers which were found in the medium after incubation with either all-trans-RAG or all-trans-RA. A pulse experiment (10(-5) M all-trans-RAG or all-trans-RA for the first 2 h of a 6-day incubation period) demonstrated inhibition of chondrogenesis with all-trans-RA, but not with all-trans-RAG. The data indicate that RAG inhibits chondrogenesis upon hydrolysis to RA. Surprisingly, the rather polar RAG isoforms were extensively accumulated in the limb bud mesenchymal cells when compared to the medium. Both all-trans-RAG and all-trans-RA also induced a large increase of retinyl ester concentrations in the chondrocytes compared to vehicle-treated cells. This finding further supports a recent suggestion that RA regulates retinol metabolism via feedback inhibition of retinol oxidation and stimulation of the esterification of retinol.

摘要

类视黄醇是维生素A的衍生物,对许多脊椎动物的功能至关重要。此外,这类化合物中的几种药物在治疗某些形式的皮肤病和癌症方面很有价值。然而,类视黄醇的治疗应用受到其致畸效力的限制。四肢是类视黄醇诱导啮齿动物畸形的重要部位。因此,已经建立了肢芽间充质细胞的类器官培养物用于筛选类视黄醇的致畸效力。我们现在应用这个系统来比较全反式视黄酰-β-D-葡萄糖醛酸(全反式-RAG)和全反式视黄酸(全反式-RA)对软骨生成的影响,并通过阿尔新蓝结合试验以及包括定量形态计量分析在内的电子显微镜评估来进行评估。建立了培养基中类视黄醇毒代动力学的初步数据以及培养的间充质肢芽细胞中的类视黄醇浓度。虽然全反式-RA在10^(-7) M时抑制软骨生成约50%,但需要高十倍的全反式-RAG浓度才能获得相同的效果。这种差异反映了在与全反式-RAG或全反式-RA孵育后在培养基中发现的RA异构体的比例。脉冲实验(在6天孵育期的前2小时用10^(-5) M全反式-RAG或全反式-RA)表明全反式-RA抑制软骨生成,但全反式-RAG没有。数据表明RAG在水解为RA后抑制软骨生成。令人惊讶的是,与培养基相比,极性较强的RAG异构体在肢芽间充质细胞中大量积累。与载体处理的细胞相比,全反式-RAG和全反式-RA还诱导软骨细胞中的视黄酯浓度大幅增加。这一发现进一步支持了最近的一项建议,即RA通过对视黄醇氧化的反馈抑制和对视黄醇酯化的刺激来调节视黄醇代谢。

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