Potential Protein Synthesis Inhibitors 11a (Tsinghua University)(Potential Protein Synthesis Inhibitors 11a (Tsinghua University))

概要

基本信息

药物类型

小分子化药

别名

1,4-benzodiazepine-2,5-dione、BZD、Compound 11a(Tsinghua University)

+ [2]

靶点-

作用方式

抑制剂

作用机制

蛋白合成抑制剂

治疗领域

肿瘤呼吸系统疾病

在研适应症

非小细胞肺癌肿瘤

非在研适应症-

原研机构

清华大学中国医学科学院北京协和生物工程联合公司

在研机构

中国医学科学院

清华大学

非在研机构

北京协和生物工程联合公司

权益机构-

最高研发阶段临床前

首次获批日期-

最高研发阶段(中国)临床前

特殊审评-

结构/序列

分子式C29H29N3O8

InChIKeyDVDVSFBXVYTQJL-DEOSSOPVSA-N

CAS号1961253-54-2

关联

2

项与 Potential Protein Synthesis Inhibitors 11a (Tsinghua University) 相关的临床试验

JPRN-UMIN000026332

/ CompletedN/AIIT

The placebo controlled randomized double blind multicenter study to investigate effectiveness and safety of combination use of melatonin receptor agonist for dose reduction or interruptions of BZD and non-BZD hypnotics on chronic insomnia. - The study of combination use of melatonin receptor agonist for dose reduction or interruptions of BZD and non-BZD hypnotics on chronic insomnia

开始日期2018-01-04

申办/合作机构-

JPRN-UMIN000004008

/ CompletedN/AIIT

Effects of discontinuation of long-term benzodiazepine use on cognitive function in schizophrenia - Effects of discontinuation of benzodiazepine on cognitive function in schizophrenia (BZD discontinuation study)

开始日期2010-09-01

申办/合作机构-

100 项与 Potential Protein Synthesis Inhibitors 11a (Tsinghua University) 相关的临床结果

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100 项与 Potential Protein Synthesis Inhibitors 11a (Tsinghua University) 相关的转化医学

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100 项与 Potential Protein Synthesis Inhibitors 11a (Tsinghua University) 相关的专利（医药）

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927

项与 Potential Protein Synthesis Inhibitors 11a (Tsinghua University) 相关的文献（医药）

2026-04-01·DRUG AND ALCOHOL DEPENDENCE

Long-term use of Benzodiazepines and Z-drugs: A register-based cohort study in Taiwan

Article

作者: Chou, Meng-Chiao ; Pan, Chun-Hung ; Kuo, Chian-Jue ; Su, Sheng-Siang ; Chen, Chiao-Chicy ; Lin, Yueh-Pin ; Tsai, Shang-Ying

BACKGROUND:

Benzodiazepines (BZDs) and Z-drugs are commonly prescribed for anxiety and insomnia, but their long-term use remains a public health concern. Evidence from Asia remains limited. This study investigated trajectories and predictors of long-term use in Taiwan by using a population-based cohort.

METHODS:

We conducted a register-based cohort study by using a nationally representative sample from Taiwan's National Health Insurance Research Database (NHIRD), covering a 20-year period from January 1, 2000, to December 31, 2019 after a 1-year washout. Incident users were identified and followed to evaluate long-term use patterns on the basis of two discontinuation thresholds: 90 days and 365 days. Cox regression models were used to estimate adjusted hazard ratios (aHRs) for long-term use by demographic, physical, and psychiatric factors.

RESULTS:

Among 896,163 incident users, 3.8% progressed to long-term use under the 90-day definition, increasing to 14.7% under the 365-day definition. Under the 90-day definition, clonazepam and hypnotic BZDs showed the highest persistence (10.3% and 8.4%). More than 70% of initiations occurred in nonpsychiatric specialties. Long-term use was associated with male sex, older age, and higher Charlson Comorbidity Index; strong predictors included cancer, pneumonia, moderate-to-severe renal disease, alcohol- or drug-induced mental disorders, and personality disorders.

CONCLUSION:

In Taiwan, most BZD and Z-drug use is short-term, and their usage patterns are affected by both clinical and system-level factors. These findings highlight the need for risk-based monitoring, cross-specialty prescribing oversight, and further research into treatment substitution strategies.

2026-02-01·ENCEPHALE-REVUE DE PSYCHIATRIE CLINIQUE BIOLOGIQUE ET THERAPEUTIQUE

Coprescription of antipsychotics and benzodiazepines at hospital discharge

Article

作者: Thiec, Julie ; Queuille, Emmanuelle ; Tournier, Marie ; Richaud, Alexandre ; Salvo, Francesco ; Debruyne, Anne-Laure ; Demourgues, Maxime ; Guillemin, Sacha

INTRODUCTION:

Antipsychotics and benzodiazepines (BZD) are known to increase the risk of sedation, dizziness, cognitive impairment and even confusion when used in combination because of their psycholeptic properties. Antipsychotics and BZD coprescription should therefore be minor at discharge from a psychiatric hospital, especially for conventional sedative antipsychotics (CS-AP), such as cyamemazine, levomepromazine, or loxapine which are often used as adjunctive treatments like BZD.

OBJECTIVES:

The primary objective was to investigate the prevalence of prescription of CS-AP, long-term antipsychotics (LT-AP), and BZD among patients discharged from hospitalization in psychiatry. The secondary objective was to assess factors associated with CS-AP and BZD coprescription.

MATERIAL AND METHODS:

A retrospective study was conducted by collecting all discharge prescriptions from patients discharged from a psychiatric hospital in 2022 and 2023. To assess prevalence, antipsychotic and BZD use was registered when at least one medication from these classes was prescribed at discharge. Multivariate logistic regression analysis was used to assess factors associated with CS-AP and BZD coprescription. Sensitivity analyses were performed to corroborate our results.

RESULTS:

In total, 5,733 psychiatric stays were associated with prescribed medications at discharge, corresponding to 4,131 different patients. Mean age was 39.8 (±18.7) years. Women represented 56.3% of the studied population. The prevalence of psychotropic drugs on discharge prescriptions was 38.7% for CS-AP, 69.1% for LT-AP, and 48.3% for BZD. The most prescribed drugs, respectively for CS-AP, LT-AP, and BZD, were cyamemazine (24.3% of prescriptions), aripiprazole (16.2%), and diazepam (24.7%). Prevalence of CS-AP+BZD and CS-AP+LT-AP+BZD coprescriptions was respectively 14.8% and 10.1%. After adjustment for age, sex, mode of admission, length of stay class, and prescription of at least one LT-AP at discharge, the CS-AP+BZD coprescription at discharge was associated with two factors: length of hospital stay≤14 days and an initial admission to a psychiatric emergency department (aOR: 1.35, 95% CI [1.14; 1.59], and aOR: 1.23, 95% CI [1.05; 1.45], respectively). Sensitivity analyses showed a similar trend, although results were not always statistically significant.

DISCUSSION:

Our results highlight the importance of an effective hospital-to-community care transition to optimize psycholeptic treatments and minimize the risk of adverse drug reactions in outpatient settings. Cyamemazine was the most prescribed CS-AP at discharge, probably due to its anxiolytic properties. This trend raises concerns regarding its appropriateness when combined with other anxiolytic treatments, such as BZD. The association between CS-AP+BZD coprescription and length of stay<14 days shows that the short hospitalization may hinder proper adaptation of pharmacological treatments. The association between CS-AP+BZD coprescription and initial admission to a psychiatric emergency department may reflect insufficient re-evaluation of the coprescribed drugs probably introduced during acute crisis management. However, our study has several limitations, including reliance on our classification of CS-AP and BZD, and lack of data on key confounders such as diagnoses, seriousness of the acute episode, prior treatments, and post-discharge care.

CONCLUSION:

Prevalence of CS-AP with BZD is high at discharge from a psychiatric hospital, especially in patients with short hospital stays (≤14 days).

2026-02-01·Pharmacology Research & Perspectives

The Risk Factors and Mortality Among Patients With Different Combination Patterns of Opioids and Benzodiazepines: A Retrospective Study

Article

作者: Su, Fang‐Yu ; Wu, Shiao‐Chi ; Tsai, Ming‐Che ; Ng, Yee‐Yung

ABSTRACT:

The concurrent use of opioids and benzodiazepines (BZDs) has raised safety concerns due to increased risks of respiratory depression and death. To evaluate mortality risks linked to different patterns of co‐prescription, we conducted a retrospective cohort study using data from a private hospital system between 2008 and 2018. A total of 418 549 opioid users were classified into four groups based on BZD use: opioids only, past use, continuous use, and new initiation. Cox proportional hazards regression model was used to estimate adjusted hazard ratios (aHRs) for 1‐year all‐cause mortality following 1‐year of concomitant use, adjusting for past medical history and Charlson Comorbidity Index (CCI). Compared to the opioids‐only group, mortality risks were significantly higher in the continuous (aHR = 1.78), new (aHR = 1.56), and past BZD use groups (aHR = 1.29). Higher mortality was also associated with older age, cancer, and greater comorbidity burden. These findings emphasize the need for cautious prescribing of opioids and BZDs, especially in older adults and those with complex medical conditions.

5

项与 Potential Protein Synthesis Inhibitors 11a (Tsinghua University) 相关的新闻（医药）

2024-03-18

·PRNewswire

Gabather files two new patent applications to secure novel findings on the effects of GT-002 for the treatment of psychiatric disorders

STOCKHOLM, March 18, 2024 /PRNewswire/ -- G abather AB (Nasdaq First North Growth Market: GABA) today reports that two new US provisional patent applications based on novel findings from the EEG/fMRI target engagement study with GT-002, a selective positive allosteric GABAA-receptor modulator. The inventions relate to the medical use of GT-002 in psychiatric disorders. The claims based on inventions from the results from our EEG/fMRI target engagement study are both novel and unexpected and will strengthen Gabather's intellectual property right (IPR) position in the field of GABAA receptor modulators, and the medical use of GT-002. Our IPR strategy is to build layers of patents around our drug products, generating a strong and attractive IPR position for the products that generates an extended patent protection of the drug product. Gabather has an active portfolio of patents and patent applications covering key products and methods that create significant value to the company, giving Gabather the freedom to operate, product differentiation, as well as a strong negotiation position in potential agreement negotiations. "When approved by USPTO these patent's will further strengthen our drug products and market position, giving Gabather a strong competitive advantage in providing the next generation neuropsychiatric drugs to the patients. We will move forward into clinical trials in patients and identify the right partner for the continued development of GT-002" says Michael-Robin Witt, CEO of Gabather AB. About GT-002 GT-002 is a small molecule GABAA receptor Positive Allosteric Modulator (PAM) eliciting both tonic and phasic inhibitory currents. GT-002 improves learning and memory in preclinical models. It restores ketamine induced cognitive deficits in the discrimination learning task model, and inhibits the behavioural effects induced by phencyclidine in the in-vivo model of schizophrenia. GT-002 has been shown to be anxiolytic and to promote social interaction in rats. GT-002 targets a novel binding site on GABAA receptors, different from benzodiazepines (BZD), and has not shown any of the side effects known for BZD. Long-term treatment (28 days) with GT-002 has not shown any withdrawal symptoms upon cessation of treatment both in mice and dogs, indicating no drug abuse liability associated with this drug candidate. GT-002 has completed 3 phase I clinical trials in healthy volunteers. Both single ascending dose (SAD) and multiple ascending dose (MAD) studies have been completed. The results from these studies show that GT-002 is safe and well tolerated and that it has excellent pharmacokinetics, allowing for once-a-day oral dosing. An EEG/fMRI target engagement study in healthy volunteers aimed to determine the effects of GT-002 on brain activity across different brain regions and neuronal networks has recently been completed. Contact Information Michael-Robin Witt, CEO Phone: 073-687 28 39 E-mail: [email protected] About Gabather Gabather is a clinical-stage pharmaceutical company aiming to transform the treatment of neuropsychiatric disorders. The Company was founded as a response to the significant unmet need and lack of innovative therapeutics in the mental health treatment landscape. Gabather is dedicated to developing innovative therapeutics for the treatment of a broad range of neuropsychiatric disorders. The goal is to accelerate the development of new groundbreaking medicines to achieve clinically meaningful therapies for the patients. For more information, please visit: Certified Adviser Corpura Fondkommission AB Phone: +4672-252 34 51 Email: [email protected] Forward-looking statement This press release contains forward-looking statements that constitute subjective estimates and forecasts about the future. Assessments about the future are only valid on the date they are made and are, by their nature, similar to research and development work in the biotech field, associated with risk and uncertainty. In light of this, actual outcomes may differ substantially from what is described in this press release. Gabather is listed on First North Growth Market and Corpura Fondkommission AB is Certified Advisor. This information was brought to you by Cision The following files are available for download:

2024-03-18

·PRNewswire

Gabather files two new patent applications to secure novel findings on the effects of GT-002 for the treatment of psychiatric disorders

STOCKHOLM, March 18, 2024 /PRNewswire/ -- G abather AB (Nasdaq First North Growth Market: GABA) today reports that two new US provisional patent applications based on novel findings from the EEG/fMRI target engagement study with GT-002, a selective positive allosteric GABAA-receptor modulator. The inventions relate to the medical use of GT-002 in psychiatric disorders. The claims based on inventions from the results from our EEG/fMRI target engagement study are both novel and unexpected and will strengthen Gabather's intellectual property right (IPR) position in the field of GABAA receptor modulators, and the medical use of GT-002. Our IPR strategy is to build layers of patents around our drug products, generating a strong and attractive IPR position for the products that generates an extended patent protection of the drug product. Gabather has an active portfolio of patents and patent applications covering key products and methods that create significant value to the company, giving Gabather the freedom to operate, product differentiation, as well as a strong negotiation position in potential agreement negotiations. "When approved by USPTO these patent's will further strengthen our drug products and market position, giving Gabather a strong competitive advantage in providing the next generation neuropsychiatric drugs to the patients. We will move forward into clinical trials in patients and identify the right partner for the continued development of GT-002" says Michael-Robin Witt, CEO of Gabather AB. About GT-002 GT-002 is a small molecule GABAA receptor Positive Allosteric Modulator (PAM) eliciting both tonic and phasic inhibitory currents. GT-002 improves learning and memory in preclinical models. It restores ketamine induced cognitive deficits in the discrimination learning task model, and inhibits the behavioural effects induced by phencyclidine in the in-vivo model of schizophrenia. GT-002 has been shown to be anxiolytic and to promote social interaction in rats. GT-002 targets a novel binding site on GABAA receptors, different from benzodiazepines (BZD), and has not shown any of the side effects known for BZD. Long-term treatment (28 days) with GT-002 has not shown any withdrawal symptoms upon cessation of treatment both in mice and dogs, indicating no drug abuse liability associated with this drug candidate. GT-002 has completed 3 phase I clinical trials in healthy volunteers. Both single ascending dose (SAD) and multiple ascending dose (MAD) studies have been completed. The results from these studies show that GT-002 is safe and well tolerated and that it has excellent pharmacokinetics, allowing for once-a-day oral dosing. An EEG/fMRI target engagement study in healthy volunteers aimed to determine the effects of GT-002 on brain activity across different brain regions and neuronal networks has recently been completed. Contact Information Michael-Robin Witt, CEO Phone: 073-687 28 39 E-mail: [email protected] About Gabather Gabather is a clinical-stage pharmaceutical company aiming to transform the treatment of neuropsychiatric disorders. The Company was founded as a response to the significant unmet need and lack of innovative therapeutics in the mental health treatment landscape. Gabather is dedicated to developing innovative therapeutics for the treatment of a broad range of neuropsychiatric disorders. The goal is to accelerate the development of new groundbreaking medicines to achieve clinically meaningful therapies for the patients. For more information, please visit: Certified Adviser Corpura Fondkommission AB Phone: +4672-252 34 51 Email: [email protected] Forward-looking statement This press release contains forward-looking statements that constitute subjective estimates and forecasts about the future. Assessments about the future are only valid on the date they are made and are, by their nature, similar to research and development work in the biotech field, associated with risk and uncertainty. In light of this, actual outcomes may differ substantially from what is described in this press release. Gabather is listed on First North Growth Market and Corpura Fondkommission AB is Certified Advisor. This information was brought to you by Cision The following files are available for download: SOURCE Gabather AB

2024-03-07

·PRNewswire

Gabather reports initial positive results from the EEG/fMRI target engagement study

STOCKHOLM, March 7, 2024 /PRNewswire/ -- Gabather AB (Nasdaq First North Growth Market: GABA) today reports initial positive results from the EEG/fMRI target engagement study, a double-blinded placebo-controlled, cross-over phase Ib study of Gabather's GABAA-receptor positive allosteric modulator, GT-002, in healthy volunteers. The study met the primary objective to confirm a favourable safety and tolerability profile of GT-002. The secondary objective to demonstrate target engagement in human brain was also met. The study clearly demonstrated that GT-002 is safe and well tolerated at dose levels expected to be effective for treatment of patients with neuropsychiatric disorders. Clinically relevant effects of GT-002 were observed on modulation of EEG frequency band power with a significant increase in alpha band power, compared to Lorazepam at the 2-hour after treatment. This effect spanned various brain regions, including frontal and occipital areas. No significant effect of Lorazepam on EEG alpha band power compared to placebo was observed. The results suggest a distinct effect of GT-002 to modulate alpha band power across specific cortical regions. EEG alpha band power is recognized as a marker of cognitive activity such as attention and associated with relaxation and less anxiety, an increase in alpha band may be beneficial for a number of different neuropsychiatric conditions. Of particular clinical interest are the reports that negative symptoms in schizophrenia patients are associated with reduced EEG alpha band power. "We have now proven clinically relevant target engagement in the human brain following oral administration of GT-002 showing that EEG and neuroimaging techniques can indeed open 'a window into the brain' and drive the drug development process of our candidate drugs. The next data to be presented will be a refined analysis of the EEG data during task performance and the fMRI neuroimaging data. With these results at hand, we will move forward into clinical trials in patients and identify the right partner for the continued development of GT-002," says Michael-Robin Witt, CEO of Gabather AB. GT-002 Background GT-002 is a small molecule GABAA receptor Positive Allosteric Modulator (PAM) eliciting both tonic and phasic inhibitory currents. GT-002 improves learning and memory in preclinical models. It restores ketamine induced cognitive deficits in the discrimination learning task model, and inhibits the behavioural effects induced by phencyclidine in the in-vivo model of schizophrenia. GT-002 has been shown to be anxiolytic and to promote social interaction in rats. GT-002 targets a novel binding site on GABAA receptors, different from benzodiazepines (BZD), and has not shown any of the side effects known for BZD. Long-term treatment (28 days) with GT-002 has not shown any withdrawal symptoms upon cessation of treatment both in mice and dogs, indicating no drug abuse liability associated with this drug candidate. GT-002 has successfully completed three phase I clinical trials in healthy volunteers. Both single ascending dose (SAD) and multiple ascending dose (MAD) studies have been completed. The results from these studies show that GT-002 is safe and well tolerated and that it has excellent pharmacokinetic properties, allowing for once-a-day oral dosing. Contact Information Michael-Robin Witt, CEO Phone: 073-687 28 39 E-mail: [email protected] About Gabather Gabather is a clinical-stage pharmaceutical company aiming to transform the treatment of neuropsychiatric disorders. The Company was founded as a response to the significant unmet need and lack of innovative therapeutics in the mental health treatment landscape. Gabather is dedicated to developing innovative therapeutics for the treatment of a broad range of neuropsychiatric disorders. The goal is to accelerate the development of new groundbreaking medicines to achieve clinically meaningful therapies for the patients. For more information, please visit: Certified Adviser Corpura Fondkommission AB Phone: +4672-252 34 51 Email: [email protected] Forward-looking statement This press release contains forward-looking statements that constitute subjective estimates and forecasts about the future. Assessments about the future are only valid on the date they are made and are, by their nature, similar to research and development work in the biotech field, associated with risk and uncertainty. In light of this, actual outcomes may differ substantially from what is described in this press release. Gabather is listed on First North Growth Market and Corpura Fondkommission AB is Certified Advisor. The following files are available for download:

临床1期临床结果

100 项与 Potential Protein Synthesis Inhibitors 11a (Tsinghua University) 相关的药物交易

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研发状态

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适应症	最高研发状态	国家/地区	公司	日期
非小细胞肺癌	临床前	中国	清华大学	2022-10-19
肿瘤	药物发现	中国	北京协和生物工程联合公司	-
肿瘤	药物发现	中国	中国医学科学院	-