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两种双氨甲基蒽醌诱导的硫酸化糖胺聚糖在溶酶体中的储存。

Lysosomal storage of sulfated glycosaminoglycans induced by two bis-aminomethyl anthrachinones.

作者信息

Fischer J, Lüllmann-Rauch R, Stubbe E, von Witzendorff B

机构信息

Department of Pharmacology, University of Kiel, Germany.

出版信息

Arch Toxicol. 1996;70(6):373-9. doi: 10.1007/s002040050288.

Abstract

Several immunomomodulatory drugs, all of them symmetrically substituted dicationic amphiphilic compounds, are known to cause lysosomal storage of sulfated glycosaminoglycans (GAGs) in intact animals and cultured fibroblasts. The storage is due to impaired GAG degradation. The standard compound is tilorone (2,7-bis[2-(diethylamino)ethoxy]fluoren-9-one). In the present study two bis-aminomethyl anthrachinones were examined for their ability to induce lysosomal GAG storage in cultured bovine corneal fibroblasts. For reference, a bis-aminoethoxy-anthrachinone compound (RMI-10.024) was included, which is known to be a potent inducer of lysosomal GAG storage. The present morphological, radiochemical, and biochemical results show that the bis-aminomethyl anthrachinone compounds investigated cause lysosomal storage of GAGs, although with significantly lower potencies than the bis-aminoethoxy anthrachinone. Dermatan sulfate contributed approximately 90% to the drug-induced increment of intracellular GAGs. The present results suggest that the length of the side chains, i.e., the distance between the aromatic ring system and the protonizable nitrogen of the side chains, and the position of the side chains relative to the aromatic ring system are important molecular features influencing the potency of inducing lysosomal GAG storage.

摘要

几种免疫调节药物,均为对称取代的双阳离子两亲性化合物,已知会在完整动物和培养的成纤维细胞中导致硫酸化糖胺聚糖(GAGs)的溶酶体储存。这种储存是由于GAG降解受损所致。标准化合物是梯洛龙(2,7-双[2-(二乙氨基)乙氧基]芴-9-酮)。在本研究中,检测了两种双氨甲基蒽醌诱导培养的牛角膜成纤维细胞溶酶体GAG储存的能力。作为对照,纳入了一种双氨基乙氧基蒽醌化合物(RMI-10.024),已知它是溶酶体GAG储存的强效诱导剂。目前的形态学、放射化学和生物化学结果表明,所研究的双氨甲基蒽醌化合物会导致GAGs的溶酶体储存,尽管其效力明显低于双氨基乙氧基蒽醌。硫酸皮肤素约占药物诱导的细胞内GAGs增量的90%。目前的结果表明,侧链的长度,即芳环系统与侧链可质子化氮之间的距离,以及侧链相对于芳环系统的位置,是影响诱导溶酶体GAG储存效力的重要分子特征。

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