NS-2359(NS-2359) - 药物靶点：DAT x SERT_在研适应症：可卡因相关疾病_专利_临床

概要

基本信息

药物类型

小分子化药

别名

GSK 372475、GSK-372475、NS 2359

靶点

DAT x SERT

作用机制

多巴胺重摄取抑制剂、5-羟色胺重摄取抑制剂

治疗领域

其他疾病

在研适应症

可卡因相关疾病

非在研适应症

酗酒注意缺陷障碍伴多动抑郁症+ [2]

原研机构

NTG Nordic Transport Group A/S

在研机构

NTG Nordic Transport Group A/S

非在研机构

GSK Plc

Saniona AB

最高研发阶段临床2期

首次获批日期-

最高研发阶段(中国)-

特殊审评-

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结构

分子式C15H19Cl2NO

InChIKeyFPTPUYCHSWIWIB-FUTJPDQTSA-N

CAS号195875-87-7

关联

15

项与 NS-2359 相关的临床试验

NCT02798627 / Completed临床2期IIT

A Phase II, Double-Blind, Placebo-Controlled, Trial Of NS2359 For The Treatment of Cocaine Dependence

NS2359 attenuates the euphoria associated with cocaine use. In a manner parallel to cocaine, NS2359 blocks the reuptake of dopamine (DA), norepinephrine (NE), and serotonin (5HT) with nanomolar affinities at the 3 transporters. In primates NS2359 significantly attenuated cocaine self-administration. In several phase II clinical trials for major depressive disorder and adult attention deficit disorder, NS2359 did not cause euphoria. NS2359 exhibited no abuse potential in a human laboratory study comparing NS2359 with amphetamine. In a phase I human laboratory interaction study, NS2359 showed no toxicity after 20 or 40 mg of cocaine, but it attenuated the both the rewarding and cardiovascular effects of intravenous cocaine. On the basis of these promising studies, investigators propose a Phase II double-blind clinical trial of NS2359 in cocaine addiction (CA). The proposed trial will involve 100 CA subjects participating in an eight week trial, including a 1-week baseline and 8 weeks of NS2359 or placebo treatment. Four weeks after completing the medication phase, there will be one follow-up visit. Subjects will be randomly assigned to treatment with placebo or 2 mg NS2359 daily, with a possible decrease to 1 mg daily for adverse events. This dose range is selected on the basis of phase I and II evidence of tolerability and NS2359 plasma levels which were associated with blockade of cocaine reward. This project has the potential to identify the first effective pharmacotherapy for CA.

开始日期2016-05-01

申办/合作机构

University of Pennsylvania

[+2]

NCT00728208 / Completed临床1期

A Placebo-controlled, Single-blind, Randomised, Parallel Group, 28-day Repeat Dose Study to Investigate the Tolerability, Safety and Steady State Pharmacokinetics of GSK372475 in Healthy Young and Elderly, Male and Female Subjects

This study will consist of 4 parallel cohorts of healthy volunteers (elderly male, elderly female, young male and young female). Subjects will receive either GSK372475 1.5mg or placebo for 28 days.

开始日期2008-07-28

申办/合作机构

GSK Plc

NCT00488098 / Completed临床1期

An Open Label, Randomized, Parallel Groups, Bioequivalence Study to Compare a Single Oral Dose of GSK372475B or GSK372475C in Male and Female Healthy Volunteers.

The study is to show the new salt formulation of GSK372475 is equivalent to the old salt formulation of GSK372475.

开始日期2007-07-01

申办/合作机构

GSK Plc

100 项与 NS-2359 相关的临床结果

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100 项与 NS-2359 相关的转化医学

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100 项与 NS-2359 相关的专利（医药）

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3

项与 NS-2359 相关的文献（医药）

2021-06-02·ACS chemical neuroscience3区 · 医学

Understanding the Polypharmacological Profiles of Triple Reuptake Inhibitors by Molecular Simulation

3区 · 医学

Article

作者: Yao, Xiaojun ; Tu, Gao ; Xue, Weiwei ; Fu, Tingting ; Yang, Jingyi ; Zhang, Zhao ; Zhu, Feng ; Yang, Fengyuan

The triple reuptake inhibitors (TRIs) class is a class of effective inhibitors of human monoamine transporters (hMATs), which includes dopamine, norepinephrine, and serotonin transporters (hDATs, hNETs, and hSERTs). Due to the high degree of structural homology of the binding sites of those transporters, it is a great challenge to design potent TRIs with fine-tuned binding profiles. The molecular determinants responsible for the binding selectivity of TRIs to hDATs, hNETs, and hSERTs remain elusive. In this study, the solved X-ray crystallographic structure of hSERT in complex with escitalopram was used as a basis for modeling nine complexes of three representative TRIs (SEP225289, NS2359, and EB1020) bound to their corresponding targets. Molecular dynamics (MD) and effective post-trajectory analysis were performed to estimate the drug binding free energies and characterize the selective profiles of each TRI to hMATs. The common binding mode of studied TRIs to hMATs was revealed by hierarchical clustering analysis of the per-residue energy. Furthermore, the combined protein-ligand interaction fingerprint and residue energy contribution analysis indicated that several conserved and nonconserved "Warm Spots" such as S149, V328, and M427 in hDAT, F317, F323, and V325 in hNET and F335, F341, and V343 in hSERT were responsible for the TRI-binding selectivity. These findings provided important information for rational design of a single drug with better polypharmacological profiles through modulating multiple targets.

2012-05-01·Journal of psychopharmacology (Oxford, England)3区 · 医学

Efficacy, safety, and tolerability of a triple reuptake inhibitor GSK372475 in the treatment of patients with major depressive disorder: two randomized, placebo- and active-controlled clinical trials

3区 · 医学

Article

作者: Ratti, Emiliangelo ; Lavergne, Agnes ; Moate, Rachel ; Graff, Ole ; Alexander, Robert ; Learned, Susan ; Archer, Graeme ; Roychowdhury, Suraja ; Zamuner, Stefano ; Modell, Jack G ; Krishnan, K Ranga ; Evoniuk, Gary

GSK372475 is a triple reuptake inhibitor with approximately equipotent inhibition of serotonin, norepinephrine, and dopamine transporters. Two randomized, placebo- and active-controlled, double-blind studies examined the efficacy and safety of GSK372475 in outpatients (aged 18–64 years) with a diagnosis of major depressive episode associated with major depressive disorder (MDD). Patients were randomized 1:1:1 to placebo, GSK372475 (1–2 mg/d), or active control (Study 1: venlafaxine XR 150–225 mg/d; Study 2: paroxetine 20–30 mg/d). GSK372475 did not significantly differ from placebo on any of the key efficacy endpoints (six-item Bech scale, IDS-Clinician Rated, MADRS) in either study. Both active controls demonstrated significant antidepressant activity compared with placebo on both primary and secondary endpoints. The most common adverse effects (AEs) with GSK372475 were dry mouth, headache, insomnia, and nausea. AEs were more frequent for GSK372475 versus placebo for sleep, anxiety-related, gastrointestinal, and tachycardia events. Increases in mean change from baseline in heart rate and sitting blood pressure were greater for GSK372475 than observed for either placebo or active control groups. Completion rates were lower for GSK372475 (49%, 58%) compared with placebo (67%, 74%), venlafaxine XR (63%), or paroxetine (77%). GSK372475 was neither efficacious nor well tolerated in patients with MDD in two 10-week studies.

2008-01-01·Behavioral and brain functions : BBF2区 · 心理学

A randomized controlled trial of a novel mixed monoamine reuptake inhibitor in adults with ADHD

2区 · 心理学

ArticleOA

作者: Keith Wesnes ; Birgit Mikkelsen ; Lenard Adler ; Timothy Edwin Wilens ; Ole Graff ; Thorsten Klint ; Scott West

BACKGROUND:

NS2359 is a potent reuptake blocker of noradrenalin, dopamine, and serotonin. The aim of the study was to investigate the efficacy, safety and cognitive function of NS2359 in adults with a DSM IV diagnosis of ADHD.

METHODS:

The study was a multi-centre, double-blind, randomized placebo-controlled, parallel group design in outpatient adults (18-55 years) testing 0.5 mg NS2359 vs. placebo for 8 weeks. Multiple assessments including computerized neuropsychological evaluation were performed.

RESULTS:

There was no significant difference between NS2359 (n = 63) versus placebo (n = 63) on the primary outcome measure reduction in investigator rated ADHD-RS total score (7.8 versus 6.4; p < 0.45). However, in subjects with the inattentive subtype, there were significantly more responders in the NS2359 group compared to placebo (41% versus 7%; p < 0.01). For all secondary variables (ADHD-RS patient rated; The Conners Adult ADHD Scale; The Brown Adult Scale, and CGI-improvement scale) there were no significant differences between the two groups; however, in the inattentive subgroup, the response to treatment was significantly larger than to placebo. NS2359 improved composite factor scores of attention, episodic- and working memory. No serious adverse events were reported with insomnia, headaches and loss of appetite most commonly reported as side effects.

CONCLUSION:

No overall effect of NS2359 was found on overall symptoms of ADHD. There was also a modest signal of improvement in the inattentive adults with ADHD and cognition warranting further exploration using differing doses.

100 项与 NS-2359 相关的药物交易

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外链

KEGG	Wiki	ATC	Drug Bank
-	NS-2359	-	DB05805

研发状态

10 条进展最快的记录,

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适应症	最高研发状态	国家/地区	公司	日期
可卡因相关疾病	临床2期	美国	Saniona AB	2016-05-01
抑郁症	临床2期	澳大利亚	GSK Plc	2007-04-01
抑郁症	临床2期	比利时	GSK Plc	2007-04-01
抑郁症	临床2期	爱沙尼亚	GSK Plc	2007-04-01
抑郁症	临床2期	芬兰	GSK Plc	2007-04-01
抑郁症	临床2期	斯洛伐克	GSK Plc	2007-04-01
抑郁症	临床2期	南非	GSK Plc	2007-04-01
重度抑郁症	临床2期	保加利亚	GSK Plc	2006-12-19
重度抑郁症	临床2期	加拿大	GSK Plc	2006-12-19
重度抑郁症	临床2期	智利	GSK Plc	2006-12-19

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临床结果

适应症

分期

评价

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研究	分期	人群特征	评价人数	分组	结果	评价	发布日期


NCT02798627 (CTgov)	临床2期	可卡因相关疾病	55	NS2359 (NS2359)	壓壓願築鑰衊範構積繭(選鑰網廠鹽鏇遞壓鑰淵) = 膚鏇遞鹽獵憲窪築襯構遞窪憲選壓觸鬱夢簾鹽 (蓋淵壓簾積糧衊淵廠膚, 築襯網積築鏇獵淵鏇簾 ~ 醖製遞壓製窪壓糧襯餘) 更多	-	2021-05-24
NCT02798627 (CTgov)	临床2期	可卡因相关疾病	55	placebo (Placebo)	壓壓願築鑰衊範構積繭(選鑰網廠鹽鏇遞壓鑰淵) = 鏇構積壓觸鏇繭艱鬱簾遞窪憲選壓觸鬱夢簾鹽 (蓋淵壓簾積糧衊淵廠膚, 遞獵糧淵觸鹹選憲鏇齋 ~ 壓艱壓網觸鹹蓋遞餘鏇) 更多	-	2021-05-24
NCT00420641 (CTgov)	临床2期	中度重度抑郁症 \| 重度抑郁症	492	Placebo	夢積餘糧憲鹽齋築顧範(膚製簾鬱蓋築襯積淵醖) = 範齋憲遞夢構齋壓構構窪壓鑰構壓網願鬱艱鹽 (觸觸淵壓積襯廠醖醖夢, 觸製築鏇鏇鏇憲觸鏇蓋 ~ 蓋鹽構蓋鹽膚顧獵鑰膚) 更多	-	2018-02-05