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两性霉素B刺激新生小鼠颅骨净钙外流的机制。

Mechanism of amphotericin B stimulation of net calcium efflux from neonatal mouse calvariae.

作者信息

Blair N F, Krieger N S, Bushinsky D A

机构信息

Nephrology Section, Pritzker School of Medicine, University of Chicago, IL 60637.

出版信息

J Bone Miner Res. 1990 Jul;5(7):725-32. doi: 10.1002/jbmr.5650050709.

Abstract

Amphotericin B is a polyene antifungal agent that binds to membrane sterols, creating aqueous pores that permit ion fluxes sufficient to cause cell lysis. It has also been shown to alter ion transport in mammalian cells, including proton secretion from renal tubular cells. The latter effect can lead to distal renal tubular acidosis in patients treated for systemic fungal infections. Based on the understanding that osteoclast-mediated bone resorption is dependent on proton secretion, we examined the effect of amphotericin B on calcium efflux from neonatal mouse calvariae in organ culture. Amphotericin B (5 micrograms/ml) stimulated net calcium efflux from calvariae within 24 h to a level almost as great as that produced by a maximally effective concentration of parathyroid hormone. The stimulated calcium efflux was completely inhibited by both 10 ng/ml salmon calcitonin, a physiologic inhibitor of osteoclast activity, and 4 x 10(-4) M acetazolamide, a specific inhibitor of carbonic anhydrase, the enzyme necessary for substantial proton generation by osteoclasts. These results indicate a direct effect of amphotericin B on bone in vitro to stimulate osteoclast-mediated calcium efflux.

摘要

两性霉素B是一种多烯类抗真菌药物,它与膜固醇结合,形成水通道,允许离子通量足以导致细胞裂解。它还被证明会改变哺乳动物细胞中的离子转运,包括肾小管细胞的质子分泌。后一种效应可导致接受系统性真菌感染治疗的患者发生远端肾小管酸中毒。基于破骨细胞介导的骨吸收依赖于质子分泌这一认识,我们研究了两性霉素B对器官培养的新生小鼠颅骨钙流出的影响。两性霉素B(5微克/毫升)在24小时内刺激颅骨的净钙流出,达到几乎与最大有效浓度的甲状旁腺激素所产生的水平一样高的水平。10纳克/毫升的鲑鱼降钙素(一种破骨细胞活性的生理抑制剂)和4×10⁻⁴M的乙酰唑胺(一种碳酸酐酶的特异性抑制剂,碳酸酐酶是破骨细胞大量产生质子所必需的酶)都能完全抑制这种刺激的钙流出。这些结果表明两性霉素B在体外对骨有直接作用,可刺激破骨细胞介导的钙流出。

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