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更新于：2025-03-27

Cyclobenzaprine hydrochloride

盐酸环苯扎林

更新于：2025-03-27

概要

基本信息

简介环苯扎林是一种拮抗 ADRA2、5-HT2A 受体和 H1 受体的小分子药物，已被批准用于治疗肌肉痉挛、纤维肌痛、应激障碍、腰痛、COVID-19 和 COVID 后综合征。它的作用机制降低了运动神经元和骨骼肌的兴奋性，同时减少了焦虑、疼痛和炎症。强生公司开发的这种药物于 1977 年首次获得批准，但它会引起嗜睡、口干和头晕等副作用，需要医疗保健提供者进行仔细监测。环苯扎林可以为广泛的临床适应症提供治疗益处，但其给药需要谨慎，特别是对于患有基础疾病（例如肝或肾功能损害）的患者。因此，医疗保健提供者在使用这种药物之前必须充分了解患者的病史。

药物类型

小分子化药

别名

(3-Dibenzo[a,d]cyclohepten-5-ylidene-propyl)-dimethyl-amine、Cyclobenzaprine、Cyclobenzaprine hydrochloride (USP)

+ [16]

靶点

5-HT2A receptor x ADRA2 x H1 receptor

作用方式

拮抗剂

作用机制

5-HT2A receptor拮抗剂(5-羟色胺2A受体拮抗剂)、ADRA2拮抗剂(肾上腺素能受体α-2家族拮抗剂)、H1 receptor拮抗剂(组胺H1受体拮抗剂)

治疗领域

神经系统疾病皮肤和肌肉骨骼疾病免疫系统疾病+ [3]

在研适应症

肌肉痉挛纤维肌痛急性腰痛+ [5]

非在研适应症

偏头痛肌筋膜疼痛综合征创伤后应激障碍

原研机构

Johnson & Johnson

在研机构

Tonix Pharmaceuticals, Inc.

山东百诺医药股份有限公司

Tonix Pharmaceuticals Holding Corp.

+ [1]

非在研机构

Teva Pharmaceuticals USA, Inc.Janssen Research & Development LLC

最高研发阶段批准上市

首次获批日期

美国 (1977-08-26),

肌肉痉挛

最高研发阶段(中国)临床3期

特殊审评快速通道 (美国)

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结构/序列

分子式C20H22ClN

InChIKeyVXEAYBOGHINOKW-UHFFFAOYSA-N

CAS号6202-23-9

关联

项与盐酸环苯扎林相关的临床试验

NCT06636786

/ Not yet recruiting临床2期IIT

Prevention/Reduction of ASRs and PTSD to Sustain Civilian Performance With Sublingual Cyclobenzaprine HCl (TNX-102 SL) - (Optimizing Acute Stress Reaction Interventions With TNX-102 SL - OASIS)

This study will examine the safety and efficacy of TNX-102 SL to reduce ASR symptoms and behavioral changes among patients presenting to the emergency department (ED) after motor vehicle collision (MVC). Specifically, the investigators will perform the Optimizing Acute Stress reaction Interventions with TNX-102 SL (OASIS) Trial, a double-blind placebo-controlled randomized clinical trial (RCT) to determine if TNX-102 SL initiated in the ED in the hours after MVC to high risk individuals, treats/reduces acute stress reaction (ASR)/acute stress disorder (ASD) symptoms (primary outcome), improves neurocognitive function, and prevents/reduces posttraumatic stress (PTS) symptoms (secondary outcomes) long term. 180 participants will be randomized, receive study drug in ED and be discharged with a 2-week drug supply. Prior to initial dose of study drug administration, and during the hours, days, and weeks after participants will receive serial longitudinal assessments of psychological and somatic symptoms, neurocognitive function, and adverse events.

开始日期2025-01-01

申办/合作机构

The University of North Carolina at Chapel Hill

[+3]

CTR20231737

/ CompletedN/A

在空腹和餐后条件下，采用单中心、随机、开放、单剂量、两制剂、两周期、两交叉设计，评价盐酸环苯扎林缓释胶囊受试制剂与参比制剂在健康成年受试者中的生物等效性

主要研究目的：考察在空腹/餐后条件下，在中国健康受试者中评价鲁南贝特制药有限公司研制的盐酸环苯扎林缓释胶囊（规格：30mg）与Teva Pharmaceuticals International GmbH持有的盐酸环苯扎林缓释胶囊（商品名：Amrix；规格：30mg）的人体生物等效性。次要研究目的观察在空腹/餐后条件下，盐酸环苯扎林缓释胶囊受试制剂和参比制剂在中国健康受试者中的安全性。

开始日期2023-06-24

申办/合作机构

鲁南贝特制药有限公司

RBR-9yy8w2k

/ RecruitingN/AIIT

Effect of Neuroscience-based Pain Education associated with Cyclobenzaprine administration in patients with Masticatory Myofascial Pain: a double blind randomized controlled clinical trial

开始日期2022-11-14

申办/合作机构

Universidade Federal de Minas Gerais

[+1]

100 项与盐酸环苯扎林相关的临床结果

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100 项与盐酸环苯扎林相关的转化医学

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100 项与盐酸环苯扎林相关的专利（医药）

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845

项与盐酸环苯扎林相关的文献（医药）

2025-05-01·TALANTA

Co3O4/fluoro-copolymer nanocomposite modified boron-doped diamond electrode non-enzymatic sensor for the determination of skeletal muscle relaxant drug cyclobenzaprine in biological fluids

Article

作者: Satsangee, Soami P ; Jain, Rajeev ; Sengar, Manish S ; Sengar, Neha ; Kumari, Priya

Electrochemical sensors have revolutionized pharmaceutical analysis by providing enhanced speed, selectivity, and cost-effectiveness. This study presents the development of a highly sensitive, non-enzymatic electrochemical sensor for Cyclobenzaprine (CBZ) determination. The sensor features a boron-doped diamond electrode (BDDE) modified with a novel Cobalt Oxide/Nafion-based nanocomposite (Co₃O₄/Nafion), synthesized and optimized for superior performance. The electroactive surface was fabricated by drop-casting a Co₃O₄/Nafion suspension onto the BDDE. Characterization techniques, including X-ray diffraction (XRD), field emission scanning electron microscopy (FESEM), transmission electron microscopy (TEM), X-ray photoelectron spectroscopy (XPS), energy dispersive X-ray spectroscopy (EDX), Raman spectroscopy, and Fourier transform infrared spectroscopy (FTIR), confirmed the crystallinity, morphology, and functional groups of the nanocomposite. Electrochemical analyses, comprising electrochemical impedance spectroscopy (EIS), square wave voltammetry (SWV), and cyclic voltammetry (CV), demonstrated enhanced charge transfer properties and a one-electron/proton oxidation mechanism for Cyclobenzaprine (CBZ) detection. The sensor demonstrated optimal performance in BR buffer at pH 5.6, with a linear response to CBZ concentrations ranging from 2.49 μg/L to 19.61 μg/L, achieving a LOD of 2.08 μg/L and LOQ of 6.96 μg/L. Practical applicability was established by successfully quantifying CBZ in various biological matrices, including human blood serum (37.8 %), artificial blood serum (35.6 %), artificial sweat (-28.9 %), and urine (-8.9 %), with excellent recovery rates in pharmaceutical formulations (99.75 %) and human blood serum (100.16 %). The sensor exhibited high specificity, unaffected by common interferents such as ions, carbohydrates, and heavy metals. This work introduces, for the first time, a Co₃O₄/Nafion-modified BDDE sensor for CBZ determination, offering rapid, selective, and interference-free analysis with potential applications in therapeutic drug monitoring and pharmaceutical quality control.

2025-01-27·Journal of Chemical Information and Modeling

MVCL-DTI: Predicting Drug–Target Interactions Using a Multiview Contrastive Learning Model on a Heterogeneous Graph

Article

作者: Nie, Liangpeng ; Wu, Tingfang ; Chen, Qiufeng ; Li, Geng ; Peng, Liangchen ; Zhang, Zhijun ; Wang, Junkai ; Lyu, Qiang ; Cao, Lexin ; Jiang, Yelu ; Quan, Lijun ; Zhang, Bei

Accurate prediction of drug-target interactions (DTIs) is pivotal for accelerating the processes of drug discovery and drug repurposing. MVCL-DTI, a novel model leveraging heterogeneous graphs for predicting DTIs, tackles the challenge of synthesizing information from varied biological subnetworks. It integrates neighbor view, meta-path view, and diffusion view to capture semantic features and employs an attention-based contrastive learning approach, along with a multiview attention-weighted fusion module, to effectively integrate and adaptively weight the information from the different views. Tested under various conditions on benchmark data sets, including varying positive-to-negative sample ratios, conducting hard negative sampling experiments, and masking known DTIs with different ratios, as well as redundant DTIs with various similarity metrics, MVCL-DTI exhibits strong robust generalization. The model is then employed to predict novel DTIs, with a particular focus on COVID-19-related drugs, highlighting its practical applicability. Ultimately, through features visualization and computational properties analysis, we've pinpointed critical elements, including Gene Ontology and substituent nodes, along with a proper initialization strategy, underscoring their vital role in DTI prediction tasks.

2024-12-11·Journal of chromatographic science

A Novel Method for Determination of Cyclobenzaprine in the Different Matrixes by UHPLC-DAD: Application to Real Human Plasma and Pharmaceutical Formulations

Article

作者: Akman, Tugrul C

Abstract:

This study presents a novel and efficient method for determining of cyclobenzaprine (CBP) in human plasma and tablets using simple liquid–liquid microextraction and ultra-high performance liquid chromatography-diode-array detector. The developed method was optimized and validated for selectivity, linearity, precision, accuracy, limit of detection (LOD) and limit of quantification (LOQ). The chromatographic separation was achieved using a C18 column with a mobile phase consisting of a mixture of deionized water containing 0.1% TFA and methanol (30:70, v:v) at a flow rate of 1.0 mL/min. The extraction process provided high-efficiency recovery of CBP with a small plasma volume (%94.3). The method showed good linearity within the concentration range of 0.005–10 μg/mL, with a correlation coefficient of 0.999. The LOD and LOQ values were found to be 0.0013 and 0.005 μg/mL, respectively. The intra- and inter-day %RSD were <8%, and %RE were ranged from −0.50 to 0.01%. The proposed method was successfully applied to the analysis of CBP in real human plasma samples and tablets, indicating its applicability in clinical and pharmaceutical research. In conclusion, the simple, low cost, high sensitivity and rapid nature of this method make it an attractive option for the quantification of CBP in human plasma and pharmaceutical dosage forms.

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项与盐酸环苯扎林相关的新闻（医药）

2025-03-25

·GlobeNewswire-Health Care

Tonix Pharmaceuticals Announces that FDA Will Not Require an Advisory Committee Meeting to Discuss New Drug Application for TNX-102 SL for the Management of Fibromyalgia

On track for August 15, 2025 FDA PDUFA goal date TNX-102 SL is a non-opioid analgesic; if approved, TNX-102 SL would become the first new drug for treating fibromyalgia in more than 15 years Commercial planning for TNX-102 SL underway for launch in the fourth quarter of 2025 March 24, 2025 -- Tonix Pharmaceuticals Holding Corp. (Nasdaq: TNXP) (Tonix or the Company), a fully-integrated biopharmaceutical company with marketed products and a pipeline of development candidates, today announced that the U.S. Food and Drug Administration (FDA) will not require an Advisory Committee meeting to discuss the Company’s New Drug Application (NDA) for TNX-102 SL for the management of fibromyalgia. If approved, TNX-102 SL (cyclobenzaprine HCl sublingual tablets) would be the first new treatment option for fibromyalgia patients in 15 years. “We are pleased that FDA will not require an advisory committee meeting as part of the regulatory review process for TNX-102 SL,” said Seth Lederman, M.D., President, and Chief Executive Officer of Tonix Pharmaceuticals. “We believe that TNX-102 SL has the potential to be the first member of a new class of medicines for the management of fibromyalgia, a debilitating condition affecting over 10 million adults in the U.S. We believe we are well positioned to launch TNX-102 SL for the management of fibromyalgia in the fourth quarter of 2025 if approved by the FDA.” The FDA previously granted Fast Track designation to TNX-102 SL for the management of fibromyalgia in 2024, a designation intended to expedite FDA review of important new drugs to treat serious conditions and fill an unmet medical need. Fibromyalgia is a common chronic pain disorder that is understood to result from amplified sensory and pain signaling within the central nervous system, called central sensitization. Brain imaging studies have localized the functional disorder to the brain’s insula and anterior cingulate cortex. Fibromyalgia afflicts more than 10 million adults in the U.S., the majority of whom are women. Symptoms of fibromyalgia include chronic widespread pain, non-restorative sleep, fatigue, and brain fog (or cognitive dysfunction). Other associated symptoms include mood disturbances, including depression, anxiety, headaches and abdominal pain or cramps. Individuals suffering from fibromyalgia often struggle with their daily activities, have impaired quality of life, and frequently are disabled. Physicians and patients report common dissatisfaction with currently marketed products. Fibromyalgia is now recognized as the prototypic nociplastic syndrome and as a chronic overlapping pain condition (COPC) 1-3. Nociplastic pain is the third primary type of pain in addition to nociceptive pain and neuropathic pain. Many patients present with pain syndromes that are mixtures of the three primary types of pain. Nociplastic syndromes are associated with central and peripheral sensitization. Fibromyalgia can occur without any identifiable precipitating event. However, many fibromyalgia cases follow one or more precipitating event(s) including: post-operative pain, acute or chronic nociceptive or neuropathic pain states; recovery from an infectious illness; a cancer diagnosis or cancer treatment; a metabolic or endocrine stress; or a traumatic event. In the cases of recovery from an infectious illness, fibromyalgia is considered an Infection-Associated Chronic Condition. In addition to fibromyalgia cases associated with other conditions or stressors, the U.S. National Academies of Sciences, Engineering, and Medicine, has concluded that fibromyalgia is a diagnosable condition that can occur after recovery from COVID-19 in the context of Long COVID. Fibromyalgia is also recognized as a Chronic Overlapping Pain Condition, which is a group of related conditions that include chronic fatigue syndrome/myalgic encephalomyelitis (CFS/ME), irritable bowel syndrome, endometriosis, low back pain, post-concussive syndrome (also known as mild traumatic brain injury), chronic Lyme Disease, chronic diabetic neuropathy and chronic post-herpetic neuralgia. TNX-102 SL is a centrally acting, non-opioid investigational drug, designed for chronic use. The tablet is a patented sublingual formulation of cyclobenzaprine hydrochloride developed for bedtime dosing for the management of fibromyalgia. Cyclobenzaprine potently binds and acts as an antagonist at four different post-synaptic neuroreceptor subtypes: serotonergic-5-HT2A, adrenergic-α1, histaminergic-H1, and muscarinic-M1-cholinergic receptors. Together, these interactions are believed to target the non-restorative sleep characteristic of fibromyalgia identified by Professor Harvey Moldofsky in 1975. Cyclobenzaprine is not associated with risk of addiction or dependence. The TNX-102 SL tablet is based on a eutectic formulation of cyclobenzaprine HCl and mannitol that provides a stable product which dissolves rapidly and delivers cyclobenzaprine by the transmucosal route efficiently into the bloodstream. The eutectic protects cyclobenzaprine HCl from interacting with the basifying agent that is also part of the formulation and required for efficient transmucosal absorption. Patents based on TNX-102 SL’s eutectic composition and its properties have issued in the U.S., E.U., Japan, China and many other jurisdictions around the world and provide market protection into 2034. The European Patent Office’s Opposition Division maintained Tonix’s European Patent EP 2 968 992 in unamended form after an Opposition was filed against it by a Sandoz subsidiary, Hexal AG. Hexal AG did not appeal that decision. The formulation of TNX-102 SL was designed specifically for sublingual administration and transmucosal absorption for bedtime dosing to target disturbed sleep, while reducing the risk of daytime somnolence. Clinical pharmacokinetic studies indicated that relative to oral cyclobenzaprine, TNX-102 SL results in higher levels of exposure during the first 2 hours after dosing and in deceased levels of the long-lived active metabolite, norcyclobenzaprine in both single dose and multiple dose studies, consistent with bypassing first pass hepatic metabolism. At steady state after 20 days of dosing TNX-102 SL, the dynamic peak level of cyclobenzaprine is higher than the background level of norcyclobenzaprine. In contrast, after 20 days of dosing oral cyclobenzaprine, the simulated peak level of cyclobenzaprine is lower than the simulated background level of norcyclobenzaprine. 1Fitzcharles MA, et al. Lancet. 2021;397:2098-110 2Clauw DJ. Ann Rheum Dis. Published Online First: 2024 3Kaplan CM, et al. Nat Rev Neurol. 2024;20, 347–363 Tonix is a fully-integrated biopharmaceutical company focused on transforming therapies for pain management and vaccines for public health challenges. Tonix’s development portfolio is focused on central nervous system (CNS) disorders. Tonix’s priority is to advance TNX-102 SL, a product candidate for the management of fibromyalgia, for which an NDA was submitted based on two statistically significant Phase 3 studies for the management of fibromyalgia and for which a PDUFA (Prescription Drug User Fee act) goal date of August 15, 2025 has been assigned for a decision on marketing authorization. The FDA has also granted Fast Track designation to TNX-102 SL for the management of fibromyalgia. TNX-102 SL is also being developed to treat acute stress reaction and acute stress disorder under a Physician-Initiated IND at the University of North Carolina in the OASIS study funded by the U.S. Department of Defense (DoD). Tonix’s CNS portfolio includes TNX-1300 (cocaine esterase), a biologic in Phase 2 development designed to treat cocaine intoxication that has FDA Breakthrough Therapy designation, and its development is supported by a grant from the National Institute on Drug Abuse. Tonix’s immunology development portfolio consists of biologics to address organ transplant rejection, autoimmunity and cancer, including TNX-1500, which is an Fc-modified humanized monoclonal antibody targeting CD40-ligand (CD40L or CD154) being developed for the prevention of allograft rejection and for the treatment of autoimmune diseases. TNX-1500 has completed a positive Phase I trial. Tonix’s infectious disease portfolio includes TNX-801, a vaccine in development for mpox and smallpox, as well as TNX-4200 for which Tonix has a contract with the U.S. DoD’s Defense Threat Reduction Agency (DTRA) for up to $34 million over five years. TNX-4200 is a small molecule broad-spectrum antiviral agent targeting CD45 for the prevention or treatment of infections to improve the medical readiness of military personnel in biological threat environments. Tonix owns and operates a state-of-the art infectious disease research facility in Frederick, Md. Tonix Medicines, our commercial subsidiary, markets Zembrace® SymTouch® (sumatriptan injection) 3 mg and Tosymra® (sumatriptan nasal spray) 10 mg for the treatment of acute migraine with or without aura in adults. The content above comes from the network. if any infringement, please contact us to modify.

快速通道

2025-03-13

·GlobeNewswire-Health Care

Tonix Pharmaceuticals Announces Presentation at BIO-Europe Spring 2025

CHATHAM, N.J., March 13, 2025 (GLOBE NEWSWIRE) -- Tonix Pharmaceuticals Holding Corp. (Nasdaq: TNXP) (Tonix or the Company), a fully-integrated biopharmaceutical company with marketed products and a pipeline of development candidates, today announced that Seth Lederman, M.D., Chief Executive Officer of Tonix Pharmaceuticals, will present at the 2025 BIO-Europe Spring Convention being held March 17-19, 2025, in Milan, Italy. The Company’s presentation will take place on Monday, March 17, 2025, at 2:00 p.m. CET in the Exhibit Hall Stage Room of the Allianz MiCo Central Building. Dr. Lederman’s presentation will focus on TNX-102 SL (cyclobenzaprine HCl sublingual tablets) for the management of fibromyalgia. The U.S. Food and Drugs Administration (FDA) has set a PDUFA goal date of August 15, 2025 for a decision on marketing authorization. TNX-102 SL now has the potential to be the first new treatment option for fibromyalgia patients in 15 years. To schedule a meeting with the Company’s management at the convention, please submit a meeting request through the BIO One-on-One Partnering™ system or contact brandon.weiner@icrhealthcare.com. Tonix Pharmaceuticals Holding Corp.* Tonix is a fully-integrated biopharmaceutical company focused on transforming therapies for pain management and vaccines for public health challenges. Tonix’s development portfolio is focused on central nervous system (CNS) disorders. Tonix’s priority is to advance TNX-102 SL, a product candidate for the management of fibromyalgia, for which an NDA was submitted based on two statistically significant Phase 3 studies for the management of fibromyalgia and for which a PDUFA (Prescription Drug User Fee act) goal date of August 15, 2025 has been assigned for a decision on marketing authorization. The FDA has also granted Fast Track designation to TNX-102 SL for the management of fibromyalgia. TNX-102 SL is also being developed to treat acute stress reaction and acute stress disorder under a Physician-Initiated IND at the University of North Carolina in the OASIS study funded by the U.S. Department of Defense (DoD). Tonix’s CNS portfolio includes TNX-1300 (cocaine esterase), a biologic in Phase 2 development designed to treat cocaine intoxication that has FDA Breakthrough Therapy designation, and its development is supported by a grant from the National Institute on Drug Abuse. Tonix’s immunology development portfolio consists of biologics to address organ transplant rejection, autoimmunity and cancer, including TNX-1500, which is an Fc-modified humanized monoclonal antibody targeting CD40-ligand (CD40L or CD154) being developed for the prevention of allograft rejection and for the treatment of autoimmune diseases. Tonix also has product candidates in development in infectious disease, including a vaccine for mpox, TNX-801. Tonix recently announced a contract with the U.S. DoD’s Defense Threat Reduction Agency (DTRA) for up to $34 million over five years to develop TNX-4200, small molecule broad-spectrum antiviral agents targeting CD45 for the prevention or treatment of infections to improve the medical readiness of military personnel in biological threat environments. Tonix owns and operates a state-of-the art infectious disease research facility in Frederick, Md. Tonix Medicines, our commercial subsidiary, markets Zembrace® SymTouch® (sumatriptan injection) 3 mg and Tosymra® (sumatriptan nasal spray) 10 mg for the treatment of acute migraine with or without aura in adults. * Tonix’s product development candidates are investigational new drugs or biologics; their efficacy and safety have not been established and have not been approved for any indication. Zembrace SymTouch and Tosymra are registered trademarks of Tonix Medicines. All other marks are property of their respective owners. This press release and further information about Tonix can be found at www.tonixpharma.com. Forward Looking Statements Certain statements in this press release are forward-looking within the meaning of the Private Securities Litigation Reform Act of 1995. These statements may be identified by the use of forward-looking words such as “anticipate,” “believe,” “forecast,” “estimate,” “expect,” and “intend,” among others. These forward-looking statements are based on Tonix's current expectations and actual results could differ materially. There are a number of factors that could cause actual events to differ materially from those indicated by such forward-looking statements. These factors include, but are not limited to, risks related to the failure to obtain FDA clearances or approvals and noncompliance with FDA regulations; risks related to the failure to successfully market any of our products; risks related to the timing and progress of clinical development of our product candidates; our need for additional financing; uncertainties of patent protection and litigation; uncertainties of government or third party payor reimbursement; limited research and development efforts and dependence upon third parties; and substantial competition. As with any pharmaceutical under development, there are significant risks in the development, regulatory approval and commercialization of new products. Tonix does not undertake an obligation to update or revise any forward-looking statement. Investors should read the risk factors set forth in the Annual Report on Form 10-K for the year ended December 31, 2023, as filed with the Securities and Exchange Commission (the “SEC”) on April 1, 2024, and periodic reports filed with the SEC on or after the date thereof. All of Tonix's forward-looking statements are expressly qualified by all such risk factors and other cautionary statements. The information set forth herein speaks only as of the date thereof. Investor Contact Jessica MorrisTonix Pharmaceuticalsinvestor.relations@tonixpharma.com (862) 799-8599 Peter VozzoICR Healthcarepeter.vozzo@icrhealthcare.com (443) 213-0505 Media Contact Ray JordanPutnam Insightsray@putnaminsights.com(949) 245-5432 Indication and Usage Zembrace® SymTouch® (sumatriptan succinate) injection (Zembrace) and Tosymra® (sumatriptan) nasal spray are prescription medicines used to treat acute migraine headaches with or without aura in adults who have been diagnosed with migraine. Zembrace and Tosymra are not used to prevent migraines. It is not known if Zembrace or Tosymra are safe and effective in children under 18 years of age. Important Safety Information Zembrace and Tosymra can cause serious side effects, including heart attack and other heart problems, which may lead to death. Stop use and get emergency help if you have any signs of a heart attack: discomfort in the center of your chest that lasts for more than a few minutes or goes away and comes backsevere tightness, pain, pressure, or heaviness in your chest, throat, neck, or jawpain or discomfort in your arms, back, neck, jaw or stomachshortness of breath with or without chest discomfortbreaking out in a cold sweatnausea or vomitingfeeling lightheaded Zembrace and Tosymra are not for people with risk factors for heart disease (high blood pressure or cholesterol, smoking, overweight, diabetes, family history of heart disease) unless a heart exam shows no problem. Do not use Zembrace or Tosymra if you have: history of heart problemsnarrowing of blood vessels to your legs, arms, stomach, or kidney (peripheral vascular disease)uncontrolled high blood pressurehemiplegic or basilar migraines. If you are not sure if you have these, ask your provider.had a stroke, transient ischemic attacks (TIAs), or problems with blood circulationsevere liver problemstaken any of the following medicines in the last 24 hours: almotriptan, eletriptan, frovatriptan, naratriptan, rizatriptan, ergotamines, or dihydroergotamine. Ask your provider for a list of these medicines if you are not sure.are taking certain antidepressants, known as monoamine oxidase (MAO)-A inhibitors or it has been 2 weeks or less since you stopped taking a MAO-A inhibitor. Ask your provider for a list of these medicines if you are not sure.an allergy to sumatriptan or any of the components of Zembrace or Tosymra Tell your provider about all of your medical conditions and medicines you take, including vitamins and supplements. Zembrace and Tosymra can cause dizziness, weakness, or drowsiness. If so, do not drive a car, use machinery, or do anything where you need to be alert. Zembrace and Tosymra may cause serious side effects including: changes in color or sensation in your fingers and toessudden or severe stomach pain, stomach pain after meals, weight loss, nausea or vomiting, constipation or diarrhea, bloody diarrhea, fevercramping and pain in your legs or hips; feeling of heaviness or tightness in your leg muscles; burning or aching pain in your feet or toes while resting; numbness, tingling, or weakness in your legs; cold feeling or color changes in one or both legs or feetincreased blood pressure including a sudden severe increase even if you have no history of high blood pressuremedication overuse headaches from using migraine medicine for 10 or more days each month. If your headaches get worse, call your provider.serotonin syndrome, a rare but serious problem that can happen in people using Zembrace or Tosymra, especially when used with anti-depressant medicines called SSRIs or SNRIs. Call your provider right away if you have: mental changes such as seeing things that are not there (hallucinations), agitation, or coma; fast heartbeat; changes in blood pressure; high body temperature; tight muscles; or trouble walking.hives (itchy bumps); swelling of your tongue, mouth, or throatseizures even in people who have never had seizures before The most common side effects of Zembrace and Tosymra include: pain and redness at injection site (Zembrace only); tingling or numbness in your fingers or toes; dizziness; warm, hot, burning feeling to your face (flushing); discomfort or stiffness in your neck; feeling weak, drowsy, or tired; application site (nasal) reactions (Tosymra only) and throat irritation (Tosymra only). Tell your provider if you have any side effect that bothers you or does not go away. These are not all the possible side effects of Zembrace and Tosymra. For more information, ask your provider. This is the most important information to know about Zembrace and Tosymra but is not comprehensive. For more information, talk to your provider and read the Patient Information and Instructions for Use. You can also visit https://www.tonixpharma.com or call 1-888-869-7633. You are encouraged to report adverse effects of prescription drugs to the FDA. Visit www.fda.gov/medwatch, or call 1-800-FDA-1088.

快速通道临床3期临床2期

2025-03-05

·drugs

Tenax Therapeutics Expands Phase 3 LEVEL Program, Advancing Two TNX-103 (Oral Levosimendan) Registrational Studies for the Treatment of PH-HFpEF

CHAPEL HILL, N.C., March 05, 2025 (GLOBE NEWSWIRE) -- Tenax Therapeutics, Inc. (Nasdaq: TENX) (“Tenax Therapeutics” or the “Company”), a Phase 3, development-stage pharmaceutical company using clinical insights to develop novel cardiopulmonary therapies, today announced the U.S. Food and Drug Administration (FDA) has completed their review of Tenax Therapeutics’ updated Phase 3 development plan for TNX-103 (oral levosimendan), including an Amendment to expand enrolment and increase the power of the ongoing Phase 3 LEVEL study, and the protocol for LEVEL-2, Tenax Therapeutics’ second registrational Phase 3 study. The Company today announced it expects to enroll 230 patients in the LEVEL study, increasing the statistical powering of the study to over 95%. LEVEL-2, a global study, is expected to commence in 2025. “We are increasing our investment in the clinical development plan for TNX-103 by expanding the ongoing LEVEL study and accelerating our plans to initiate the second registrational study, LEVEL-2. With the momentum provided from our $100 million financing in August 2024 and alignment with the FDA, we are now able to execute on our plan to advance these two Phase 3 registrational studies for TNX-103 in parallel. LEVEL is enrolling well: we are confident that, with more than 50 North American sites already activated, we can complete enrollment of this upsized study around year end, while also commencing the global LEVEL-2 study later this year,” said Chris Giordano, President and Chief Executive Officer of Tenax Therapeutics. “We expect these two registrational studies will satisfy the requirements, including the safety data expectations, to file in the U.S. and other geographies. We are funded well beyond our projected date for the release of topline LEVEL data, positioning us to advance the development of TNX-103 and improve the quality of life for patients living with PH-HFpEF.” LEVEL Study Expansion Enhances Statistical Power The LEVEL study, evaluating TNX-103 for the treatment of PH-HFpEF, will expand enrollment from 152 to at least 230 patients, increasing the statistical powering of the study. The Company is on track to enroll the first 150 subjects in the first half of 2025, expects to complete enrollment by around the end of 2025, and expects to present topline data from the LEVEL study in the middle of 2026. As of late February 2025, blinded LEVEL data reveal TNX-103 to be well-tolerated in patients with PH-HFpEF: Tenax Therapeutics’ Chief Medical Officer, Stuart Rich, MD, summarized: “In addition to high rates of study and therapy continuation, the adherence to the TID regimen has been high, and no new safety signals have been detected. About half the patients in the OLE have been on study for over 6 months, a few of them for more than a year, with very reassuring participation levels observed during the OLE.” LEVEL-2: A Global Registrational Trial Additionally, Tenax Therapeutics received input from the FDA on the protocol for the LEVEL-2 study, and expects this second, global registrational clinical trial to evaluate levosimendan in patients with PH-HFpEF to start enrolling this year, in several countries. The primary endpoint of 6MWD will be assessed at 26 weeks. Tenax intends to enroll a larger sample than LEVEL and evaluate patients for a full year of double-blind, placebo-controlled therapy, providing FDA and European reviewers a robust safety database for their benefit/risk assessments. “TNX-103 has the potential to meaningfully improve the quality of life of patients with PH-HFpEF, an underdiagnosed disease with significant unmet needs and no currently approved treatment options. I remain very hopeful that with positive Phase 3 results, these patients will finally have an approved treatment available,” said Dr. Rich. “We are continuing to work closely with the FDA, and are grateful for their input, which enables Tenax to accelerate development timelines of a potential first therapy for this devastating form of PH.” About the Phase 3 LEVEL Study ( NCT05983250 ) The LEVEL Study is a Phase 3, double-blind, randomized, placebo-controlled study of oral levosimendan in patients with PH-HFpEF. Approximately 230 subjects will be randomized in a 1:1 ratio to receive an oral dose of levosimendan (2 mg/day) or placebo for Weeks 1 to 4 and 3 mg/day or placebo for Weeks 5 to 12. The primary outcome measure for the study is change in six-minute walk distance from Baseline to Week 12. All randomized subjects will have the option to enter the 92-week OLE following the completion of all study endpoints at Week 12. About the Phase 3 LEVEL-2 Study LEVEL-2 is a global Phase 3, double-blind, randomized, placebo-controlled study of oral levosimendan in patients with PH-HFpEF. Patients will be randomized to receive an oral dose of levosimendan (2mg/day) or placebo for Weeks 1 to 4 and 3mg/day or placebo from Week 5 onward. The primary endpoint of 6MWD will be assessed at 26 weeks. About Levosimendan (TNX-101, TNX-102, TNX-103) Levosimendan is a unique, potassium ATP channel activator and calcium sensitizer that affects the heart and vascular system through multiple mechanisms of action, and that is being developed as an oral therapy (TNX-103) for pulmonary hypertension (PH) with heart failure with preserved ejection fraction (PH-HFpEF). Initially discovered and developed by Orion Corporation in Finland, intravenous levosimendan has been granted market authorization in 60 countries outside the United States for use in hospitalized patients with acutely decompensated heart failure. Results of Tenax Therapeutics’ Phase 2 HELP study of levosimendan in patients with HFpEF demonstrated that IV levosimendan (TNX-101) produces potent dilation of the central and pulmonary venous circulations which translates into an improvement in exercise capacity, a discovery that is the basis of LEVEL, the Phase 3 investigation of Tenax Therapeutics’ potential groundbreaking therapy. To date, no other drug therapy has demonstrated improved exercise tolerance in patients with PH associated with HFpEF, “a growing epidemic with high morbidity and mortality and no treatment. The clear unmet need and lethal nature of PH-HFpEF must be met with novel solutions at all levels of therapeutic development” (AHA Scientific Advisory, “A Call to Action,” 2022). About Tenax Therapeutics Tenax Therapeutics, Inc. is a Phase 3, development-stage pharmaceutical company using clinical insights to develop novel cardiopulmonary therapies. The Company owns global rights to develop and commercialize levosimendan, which it has prioritized. Tenax Therapeutics also may resume developing its unique oral formulation of imatinib. For more information, visit www.tenaxthera.com. Tenax Therapeutics’ common stock is listed on The Nasdaq Stock Market LLC under the symbol “TENX”. Caution Regarding Forward-Looking Statements Except for historical information, all of the statements, expectations and assumptions contained in this press release are forward-looking statements. These forward-looking statements may include information concerning possible or projected future business operations. Actual results might differ materially from those explicit or implicit in the forward-looking statements. Important factors that could cause actual results to differ materially include: risks of our clinical trials, including, but not limited to, the timing, delays, costs, design, initiation, enrollment, and results of such trials; any delays in regulatory review and approval of product candidates in development; risks related to our business strategy, including the prioritization and development of product candidates; reliance on third parties, including Orion Corporation, our manufacturers and CROs; risks regarding the formulation, production, marketing, customer acceptance and clinical utility of our product candidates; our estimates regarding the potential market opportunity for our product candidates; the potential advantages of our product candidates; risks associated with our cash needs; our ability to maintain our culture and recruit, integrate and retain qualified personnel and advisors, including on our Board of Directors; our competitive position; intellectual property risks; volatility and uncertainty in the global economy and financial markets in light of the possibility of pandemics, global financial and geopolitical uncertainties, including in the Middle East and the Russian invasion of and war against the country of Ukraine; changes in legal, regulatory and legislative environments in the markets in which we operate and the impact of these changes on our ability to obtain regulatory approval for our products; and other risks and uncertainties set forth from time to time in our SEC filings. Tenax Therapeutics assumes no obligation and does not intend to update these forward-looking statements except as required by law. Source: Tenax Therapeutics, Inc. Whatever your topic of interest, subscribe to our newsletters to get the best of Drugs.com in your inbox.

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100 项与盐酸环苯扎林相关的药物交易

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KEGG	Wiki	ATC	Drug Bank
D00772	盐酸环苯扎林	-	DB00924

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适应症	国家/地区	公司	日期
肌肉痉挛	美国	Janssen Research & Development LLC	1977-08-26

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适应症	最高研发状态	国家/地区	公司	日期
纤维肌痛	申请上市	美国	Tonix Pharmaceuticals Holding Corp.	2024-10-16
急性腰痛	临床3期	中国	山东百诺医药股份有限公司	2018-04-13
创伤后应激障碍	临床3期	美国	Tonix Pharmaceuticals, Inc.	2017-03-27
肌筋膜疼痛综合征	临床3期	美国	Tonix Pharmaceuticals, Inc.	2015-04-01
偏头痛	临床3期	美国	Teva Pharmaceuticals USA, Inc.	2010-07-01
急性压力	临床2期	美国	Tonix Pharmaceuticals, Inc.	2025-01-01
认知功能障碍	临床2期	美国	Tonix Pharmaceuticals, Inc.	2025-01-01
应力性骨折	临床2期	美国	Tonix Pharmaceuticals, Inc.	2025-01-01
疼痛	临床2期	美国	Tonix Pharmaceuticals, Inc.	2022-08-18
新冠肺炎后遗症	临床2期	美国	Tonix Pharmaceuticals, Inc.	2022-08-18

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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


NCT03508700 (P306, CTgov)	临床3期	创伤后应激障碍	93	Placebo+TNX-102 (Placebo - TNX-102 SL)	遞製鹹壓鑰繭衊選廠醖 = 糧構鑰艱獵窪觸窪鏇齋範鹹廠構製夢積願鹹選 (願齋顧繭築繭膚鏇鏇簾, 鏇衊醖鏇艱遞願膚鑰淵 ~ 蓋鏇夢顧願鹹鹹壓餘築) 更多	-	2025-03-25
				TNX-CY-P301+TNX-102 SL (TNX-102 SL - TNX-102 SL)	遞製鹹壓鑰繭衊選廠醖 = 夢餘遞製鹹選醖艱選顧範鹹廠構製夢積願鹹選 (願齋顧繭築繭膚鏇鏇簾, 鹽壓艱鏇蓋範蓋廠衊鹽 ~ 鹹餘齋淵鏇壓顧顧願製) 更多
NCT03110575 (CTgov)	临床3期	创伤后应激障碍	190	Placebo+TNX-102 (Placebo - TNX-102 SL)	選顧構積襯鹹網襯鹹糧 = 廠鹹鹽憲鹽醖窪廠廠糧網窪簾糧蓋積憲膚獵繭 (廠憲鹽繭窪鏇選鑰餘製, 糧鬱壓範艱襯窪廠襯醖 ~ 簾餘淵艱鹹獵顧鹹鬱網) 更多	-	2025-03-25
				TNX-CY-P301+TNX-102 SL (TNX-102 SL - TNX-102 SL)	選顧構積襯鹹網襯鹹糧 = 糧繭製願壓夢鹹鹽鹽齋網窪簾糧蓋積憲膚獵繭 (廠憲鹽繭窪鏇選鑰餘製, 窪鏇艱壓醖築廠網蓋鬱 ~ 夢淵夢網衊齋鹽壓構積) 更多
NCT05273749 (RESILIENT, CTgov)	临床3期	纤维肌痛	457	TNX-102 SL Tablet, 5.6 mg (TNX-102 SL Tablet, 5.6 mg)	觸膚夢醖憲衊範蓋餘餘(膚齋遞憲選簾壓繭鹽獵) = 繭蓋網遞夢積鹹鹽鑰鏇淵顧網鏇衊衊膚襯憲鹹 (襯餘齋鑰獵淵蓋窪齋遞, 衊遞積衊壓餘鏇顧鏇蓋 ~ 糧鑰觸簾鏇選網築鑰鹹) 更多	-	2025-03-25
				Placebo SL Tablet (Placebo SL Tablet)	觸膚夢醖憲衊範蓋餘餘(膚齋遞憲選簾壓繭鹽獵) = 壓窪膚襯鬱糧願網衊廠淵顧網鏇衊衊膚襯憲鹹 (襯餘齋鑰獵淵蓋窪齋遞, 願鑰繭齋築艱遞鬱蓋鹹 ~ 繭蓋繭構齋餘鏇壓夢淵) 更多
NCT02829814 (RE-AFFIRM, CTgov)	临床3期	肌筋膜疼痛综合征 \| 纤维肌痛	51	Placebo SL Tablet (Placebo SL Tablet)	鏇壓遞築獵製簾糧糧積(膚鏇網顧窪鬱壓遞鬱鑰) = 網鏇鹹襯願壓遞簾鏇範糧廠夢壓襯淵構簾憲蓋 (獵襯鏇構鏇廠鏇選簾獵, 網網齋齋醖選鏇齋廠艱 ~ 衊遞襯壓獵壓構顧廠餘) 更多	-	2025-03-25
				TNX-102 SL Tablet, 2.8 mg (TNX-102 SL Tablet, 2.8 mg)	鏇壓遞築獵製簾糧糧積(膚鏇網顧窪鬱壓遞鬱鑰) = 鬱淵蓋夢範夢壓鹽夢選糧廠夢壓襯淵構簾憲蓋 (獵襯鏇構鏇廠鏇選簾獵, 鹽襯餘壓遞鏇積醖糧簾 ~ 鏇夢壓憲築鹹構憲蓋衊) 更多
NCT02436096 (AFFIRM, CTgov)	临床3期	肌筋膜疼痛综合征 \| 纤维肌痛	519	Placebo SL Tablet (Placebo SL Tablet)	蓋製獵選製觸範夢鏇製 = 簾構鏇鏇簾獵觸淵觸網夢遞製遞鏇艱構選衊糧 (餘製繭鹹齋選鬱壓襯憲, 窪顧繭築範構獵積衊齋 ~ 鏇糧範簾鏇夢蓋壓築觸) 更多	-	2025-02-07
				TNX-102 SL Tablet, 2.8mg (TNX-102 SL Tablet, 2.8 mg)	蓋製獵選製觸範夢鏇製 = 齋鹹鬱齋觸鬱鬱繭顧鏇夢遞製遞鏇艱構選衊糧 (餘製繭鹹齋選鬱壓襯憲, 繭壓鹹鹽選壓遞鬱遞憲 ~ 憲淵繭糧齋蓋網膚廠餘) 更多
NCT03841773 (RECOVERY \| TNX-CY-P302, CTgov)	临床3期	创伤后应激障碍	192	Placebo SL Tablets	網廠襯襯繭簾淵遞顧淵(構願艱願窪構遞淵鏇獵) = 選廠窪蓋夢簾鹹鏇獵襯衊壓餘壓簾鑰顧鬱壓糧 (蓋構遞窪鏇膚醖積襯積, 1.90) 更多	-	2025-02-06
NCT02421679 (P202, CTgov)	临床2期	创伤后应激障碍	159	Placebo+TNX-102 (Placebo- TNX-102 SL 2.8 mg)	艱範積壓餘鏇築積糧鹽 = 網製鑰築餘鏇餘齋齋艱憲簾範糧顧艱遞遞壓製 (壓獵製積鹽鏇選淵醖遞, 淵網醖範製獵壓繭鏇選 ~ 鑰願願廠衊廠糧餘構廠) 更多	-	2025-02-06
				TNX-102 SL (TNX 102 SL 2.8 mg - TNX-102 SL 2.8 mg)	艱範積壓餘鏇築積糧鹽 = 壓襯醖醖觸廠鑰糧鬱製憲簾範糧顧艱遞遞壓製 (壓獵製積鹽鏇選淵醖遞, 蓋淵憲網鏇壓淵選蓋糧 ~ 憲淵積選鑰範鏇簾廠淵) 更多
NCT02589275 (CTgov)	临床3期	纤维肌痛	375	TNX-CY-F301+TNX-102 SL (TNX-TNX)	襯醖淵壓獵網選膚襯製 = 鏇憲繭獵範鏇夢鹹襯網繭憲醖醖網遞鹹膚積構 (淵衊鹽鹹壓觸網糧廠齋, 衊觸壓簾膚築壓衊願廠 ~ 構齋網憲醖壓膚壓觸蓋) 更多	-	2024-12-11
				Placebo+TNX-102 (PBO-TNX)	襯醖淵壓獵網選膚襯製 = 夢築鏇築醖窪壓製醖製繭憲醖醖網遞鹹膚積構 (淵衊鹽鹹壓觸網糧廠齋, 製遞範製簾網窪遞艱選 ~ 製簾蓋淵獵膚窪糧築夢) 更多
NCT05472090 (PREVAIL, CTgov)	临床2期	新冠肺炎后遗症 \| 疼痛	63	TNX-102 SL (TNX-102 SL Tablet, 5.6 mg)	築顧鬱衊網選餘繭願鏇(艱衊鬱願鹹遞壓憲鏇築) = 鑰顧積襯鑰鏇製觸鹹顧廠糧獵鹽製簾齋簾膚膚 (鹹築網選淵獵壓顧衊遞, 0.34) 更多	-	2024-11-26
				Placebo SL Tablet (Placebo SL Tablet)	築顧鬱衊網選餘繭願鏇(艱衊鬱願鹹遞壓憲鏇築) = 選範製鹽製膚築築繭製廠糧獵鹽製簾齋簾膚膚 (鹹築網選淵獵壓顧衊遞, 0.35) 更多
NCT05273749 (RESILIENT, GlobeNewswire) 人工标引	临床3期	纤维肌痛	-	TNX-102 SL	觸鏇選壓積衊襯壓鏇鏇(鹽範選鹹選網衊願鹹遞): P-Value = 0.00005 达到更多	积极	2024-08-12
				Placebo