Delving into the Latest Updates on Teriflunomide Sodium with Synapse

Overview

Basic Info

Drug Type

Small molecule drug

Synonyms

CK8

Target

DHODH

Action

inhibitors

Mechanism

DHODH inhibitors(Dihydroorotate dehydrogenase inhibitors)

Therapeutic Areas

Immune System DiseasesSkin and Musculoskeletal Diseases

Active Indication

Systemic Lupus Erythematosus

Inactive Indication-

Originator Organization

Xinkaiyiyao Science & Technology Shanghai Co. Ltd.

Active Organization

Xinkaiyiyao Science & Technology Shanghai Co. Ltd.Xinkai Medicine and Chemical Intermediates (Shanghai) Co., Ltd.

Inactive Organization-

License Organization-

Drug Highest PhasePhase 2

First Approval Date-

RegulationSpecial Review Project (China)

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Structure/Sequence

Molecular FormulaC12H9F3N2NaO2

InChIKeyJPMWNACBXMNYHH-VEZAGKLZSA-N

CAS Registry1260213-11-3

1.探索口服不同剂量泰瑞米特钠片多次给药条件下，用于治疗系统性红斑狼疮患者的安全性及有效性 2.探索稳态血药浓度及体内暴露量 3.探索系统性红斑狼疮的相关药效动力学（PD）生物标记物 4.为III期临床试验确定给药方案和用药剂量提供依据

[Translation]

1. To explore the safety and efficacy of oral taremide sodium tablets at different doses for the treatment of patients with systemic lupus erythematosus under multiple administration conditions 2. To explore the steady-state blood drug concentration and in vivo exposure 3. To explore the relevant pharmacodynamic (PD) biomarkers of systemic lupus erythematosus 4. To provide a basis for determining the dosing regimen and dosage for Phase III clinical trials

Start Date14 May 2019

Sponsor / Collaborator

Suzhou Changzheng Cinkate Pharmaceutical Co., Ltd.

[+2]

CTR20150314

/ CompletedPhase 1

泰瑞米特钠片与来氟米特片的口服相对生物利用度研究

[Translation] Study on the relative oral bioavailability of teremide sodium tablets and leflunomide tablets

1）研究健康受试者单次口服泰瑞米特钠片和来氟米特片后血浆泰瑞米特浓度的经时过程和尿中泰瑞米特及其代谢产物的排泄量，以此确定泰瑞米特的药代动力学特征，为确定泰瑞米特钠片的临床使用剂量提供依据；2）评价泰瑞米特钠片与来氟米特片的口服相对生物利用度；3）评价单次口服泰瑞米特钠片和来氟米特片后的安全性和耐受性。

[Translation]

1) To study the time course of plasma tetamide concentration and urinary excretion of tetamide and its metabolites in healthy subjects after a single oral administration of tetamide sodium tablets and leflunomide tablets, so as to determine the pharmacokinetic characteristics of tetamide and provide a basis for determining the clinical dosage of tetamide sodium tablets; 2) To evaluate the oral relative bioavailability of tetamide sodium tablets and leflunomide tablets; 3) To evaluate the safety and tolerability of tetamide sodium tablets and leflunomide tablets after a single oral administration.

Start Date27 May 2015

Sponsor / Collaborator

Suzhou Changzheng Cinkate Pharmaceutical Co., Ltd.

[+2]

100 Clinical Results associated with Teriflunomide Sodium

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100 Translational Medicine associated with Teriflunomide Sodium

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100 Patents (Medical) associated with Teriflunomide Sodium

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724

Literatures (Medical) associated with Teriflunomide Sodium

01 Jun 2025·JOURNAL OF CLINICAL NEUROSCIENCE

Safety and efficacy of anti-IL-17A use in multiple sclerosis and comorbid rheumatological disease: A multi-center exploratory study

Article

Author: Galetta, Kristin ; Pua, Danielle Kei ; Gandelman, Stephanie ; Bhattacharyya, Shamik ; Opeyemi, Oluwasinmisola ; Chitnis, Tanuja ; Madill, Evan

Anti-IL-17A antibodies are used in rheumatological conditions. While not approved for multiple sclerosis (MS), anti-IL-17As reduce new gadolinium-enhancing lesions. Optimal treatment for those with MS and comorbid rheumatological conditions remains unclear. We report safety and efficacy outcomes for anti-IL-17A treatment with and without concurrent MS disease modifying therapy (DMT). Patients with MS and anti-IL-17A use were identified using electronic medical records. Primary outcomes were severe infections and markers of immunosuppression. Secondary outcomes were MS relapses and new MRI lesions. Six patients (median age: 50.1) without recent MS disease activity had anti-IL-17A monotherapy exposures (17.4 total patient-years); seven (median age: 48.2) had concurrent MS DMT use (8.8 patient-years), including anti-CD20 treatment in three patients. One patient on anti-IL-17A monotherapy had a serious infection. No patients had new or worsening lymphopenia. Four of six patients on anti-IL-17A monotherapy had new MS disease activity. No relapses or new MRI lesions occurred during concurrent MS DMT use. No significant safety concerns were identified with anti-IL-17A and MS DMT combination therapy, although exposure duration was limited. More MS disease activity was seen with anti-IL-17A monotherapy. Dual therapy with an MS DMT may be reasonable for MS patients who require anti-IL-17A treatment.

01 May 2025·EUROPEAN JOURNAL OF PHARMACEUTICS AND BIOPHARMACEUTICS

Intradermal delivery of teriflunomide loaded emulsomes using hollow microneedles for effective minimally invasive psoriasis management

Article

Author: Abbas, Haidy ; Zewail, Mariam ; Abd-El-Azim, Heba ; Sayed, Nesrine El

Conventional topical psoriasis treatments suffer from limited delivery to affected areas along with skin irritation due to high local drug concentration. Herein an attempt to improve the delivery of leflunomide's active metabolite (teriflunomide (TER)) by improving its solubility through nanoencapsulation in emulsomes (EMLs) besides ensuring effective intradermal delivery using hollow microneedles. Evaluation of colloidal characteristics of EMLs, encapsulation efficiency and drug release were performed. Additionally, the antipsoriatic activity in an imiquimod-induced psoriatic mouse model was evaluated by the measurement of inflammatory mediators' levels and histopathological assessment of anatomized skin. The particle size of the chosen EMLs formulation was 147.9 nm and the zeta potential value was -21.7. Entrapment efficiency was 97.23 % and EMLs provided sustained drug release for 48 h. No statistically significant differences in the in vivo levels of NF-KB, IL 8, MMP1, GSH, SOD and catalase between the animals treated by TER-EMLs and the negative control cohort were observed. Also, histopathological inspection of dissected skin samples reflected the superiority of TER-EMLs over TER suspension. Collectively, combining nanoencapsulation and hollow microneedles application improved TER properties and ensured effective TER delivery to the affected psoriatic areas.

01 Apr 2025·CHROMATOGRAPHIA

A Comprehensive Stability-indicating Method for Teriflunomide: Impurity Profiling and Degradation Analysis in Tablet Formulations

Author: Sarracoglu, Nagehan ; Ozgen, Bahar Koksel ; Pinarbasli, Onur ; Gayretli, Hande ; Halici, Egesen ; Doganay, Asuman Aybey

This study presents a stability-indicating method for teriflunomide, a drug administered to adults for the treatment of multiple sclerosis (MS) in its various forms, including clin. isolated syndrome, relapsing-remitting, and active secondary progressive disease.The method, which has been validated comprehensively for both impurities and the assay, plays a key role in determining teriflunomide in tablet formulations.It successfully separates two specified degradation impurities in line with the European Pharmacopeia (EP) standardsTo assess the stability of teriflunomide, the method subjects it to stress conditions such as acid/base hydrolysis, oxidation, photodegradation, and thermal degradationUsing a C18 column at 30, with a mobile phase of pH 3.4 solutions and acetonitrile at 0.8 mL/min, and UV detection at 248 nm, the method ensures the resolution of degradation products from the primary teriflunomide peak.The teriflunomide peak remained pure under all stress conditions, confirming the specificity and stability-indicating nature of the method.The validation followed FDA and ICH guidelines, with results for linearity, accuracy, precision, specificity, robustness, limit of detection, limit of quantification, and system suitability all meeting established acceptance criteria.

100 Deals associated with Teriflunomide Sodium

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R&D Status

10 top R&D records.

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Indication	Highest Phase	Country/Location	Organization	Date
Systemic Lupus Erythematosus	Phase 2	China	Xinkaiyiyao Science & Technology Shanghai Co. Ltd.	14 May 2019
Systemic Lupus Erythematosus	Phase 2	China	Xinkai Medicine and Chemical Intermediates (Shanghai) Co., Ltd.	14 May 2019