Allosteric Inhibition and Pharmacochaperoning of the Serotonin Transporter by the Antidepressant Drugs Trazodone and Nefazodone.

IF 4.3 3区 材料科学 Q1 ENGINEERING, ELECTRICAL & ELECTRONIC
Ali El-Kasaby, Danila Boytsov, Ameya Kasture, Günther Krumpl, Thomas Hummel, Michael Freissmuth, Walter Sandtner
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引用次数: 0

Abstract

The antidepressants trazodone and nefazodone were approved some 4 and 3 decades ago, respectively. Their action is thought to be mediated, at least in part, by inhibition of the serotonin transporter [SERT/solute carrier (SLC)-6A4]. Surprisingly, their mode of action on SERT has not been characterized. Here, we show that, similar to the chemically related drug vilazodone, trazodone and nefazodone are allosteric ligands: trazodone and nefazodone inhibit uptake by and transport-associated currents through SERT in a mixed-competitive and noncompetitive manner, respectively. Contrary to noribogaine and its congeners, all three compounds preferentially interact with the Na+-bound outward-facing state of SERT. Nevertheless, they act as pharmacochaperones and rescue the folding-deficient variant SERT-P601A/G602A. The vast majority of disease-associated point mutations of SLC6 family members impair folding of the encoded transporter proteins. Our findings indicate that their folding defect can be remedied by targeting allosteric sites on SLC6 transporters. SIGNIFICANCE STATEMENT: The serotonin transporter is a member of the solute carrier-6 family and is the target of numerous antidepressants. Trazodone and nefazodone have long been used as antidepressants. Here, this study shows that their inhibition of the serotonin transporter digressed from the competitive mode seen with other antidepressants. Trazodone and nefazodone rescued a folding-deficient variant of the serotonin transporter. This finding demonstrates that folding defects of mutated solute carrier-6 family members can also be corrected by allosteric ligands.

抗抑郁药物曲唑酮和奈法唑酮对羟色胺转运体的异位抑制和药效诱导
抗抑郁药曲唑酮和奈法唑酮分别在大约四十年和三十年前获得批准。它们的作用被认为至少部分是通过抑制血清素转运体(SERT/SLC6A4)来实现的。令人惊讶的是,它们对 SERT 的作用模式还没有定性。在这里,我们发现曲唑酮和奈法唑酮与化学相关药物维拉唑酮类似,都是异位配体,它们分别以混合竞争性和非竞争性方式抑制 SERT 的吸收和通过 SERT 的转运相关电流。与 noribogaine 及其同系物相反,这三种化合物都优先与 SERT 的 Na+ 结合外向状态发生作用。尽管如此,这三种化合物仍能发挥药合作用,挽救折叠缺陷变体 SERT-P601A/G602A。绝大多数与疾病相关的 SLC6(溶质运载体-6)家族成员的点突变都会影响编码的转运蛋白的折叠。我们的研究结果表明,可以通过靶向 SLC6 转运体上的异构位点来弥补其折叠缺陷。意义声明 血清素转运体是溶质载体 6 家族的成员,也是许多抗抑郁药物的靶点。曲唑酮和奈法唑酮长期以来一直被用作抗抑郁药。在这里,我们发现它们对血清素转运体的抑制作用偏离了其他抗抑郁药的竞争模式。曲唑酮和奈法唑酮能挽救折叠缺陷的血清素转运体变体。这一发现表明,异位配体也可纠正突变溶质运载体-6 家族成员的折叠缺陷。
本文章由计算机程序翻译,如有差异,请以英文原文为准。
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来源期刊
CiteScore
7.20
自引率
4.30%
发文量
567
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