Delving into the Latest Updates on Ibuprofen Lysine with Synapse

Overview

Basic Info

Drug Type

Small molecule drug

Synonyms

Ibuprofen L-lysine (JAN), Ibuprofen lysine (USAN), Solufenum

+ [5]

Target

COXs

Action

inhibitors

Mechanism

COX inhibitors(Cyclooxygenases inhibitors)

Therapeutic Areas

Nervous System DiseasesCardiovascular DiseasesCongenital Disorders+ [3]

Active Indication

Ductus Arteriosus, PatentArthritisBack Pain+ [6]

Inactive Indication-

Originator Organization

Reckitt Benckiser Healthcare (UK) Ltd.

Active Organization

Recordati Rare Diseases, Inc.Senju Pharmaceutical Co., Ltd.Reckitt Benckiser Healthcare (UK) Ltd.

+ [2]

Inactive Organization

Farmacon

Merck Sharp & Dohme Corp.

License Organization-

Drug Highest PhaseApproved

First Approval Date

Australia (12 Aug 2003),

ArthritisBack PainDysmenorrhea+ [5]

RegulationOrphan Drug (United States)

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Structure/Sequence

Molecular FormulaC13H18O2

InChIKeyHEFNNWSXXWATRW-UHFFFAOYSA-N

CAS Registry15687-27-1

View All Structures (2)

Patent ductus arteriosus (PDA), the most common cardiovascular complication of prematurity, is associated with higher mortality and morbidities in extremely low gestational age neonates (ELGANs, < 27+0 weeks). Ibuprofen and acetaminophen, which act by reducing prostaglandin synthesis, are the most commonly used first and second line agents for PDA treatment across Canada. However, initial treatment failure with monotherapy is a major problem, occurring in >60% ELGANs. Treatment failure is associated with worsening rates of mortality and bronchopulmonary dysplasia (BPD), while early treatment success can achieve rates comparable to neonates without PDA. Treatment failure resulting in prolonged disease exposure is thought to be a major contributor. Recently, combination therapy with acetaminophen and ibuprofen has emerged as a new treatment regime. Acetaminophen exerts anti-prostaglandin effect through a different receptor site than ibuprofen, providing a biological rationale for their synergistic action.
The objective of this study is to evaluate the clinical impact, efficacy and safety of combination regime (Ibuprofen + IV Acetaminophen) for the first treatment course for PDA in ELGANs vs. Ibuprofen alone (current standard treatment).

Start Date12 Dec 2022

Sponsor / Collaborator

Mount Sinai Hospital (Canada)

[+5]

IRCT20140527017880N8

/ RecruitingPhase 2/3IIT

Comparative evaluation of the effect of ibuprofen lysine & gelofen - acetaminophen on postoperative endodontic dental pain with irreversible pulpaitis

Start Date21 Apr 2019

Sponsor / Collaborator

Kermanshah University of Medical Sciences

IRCT20130812014333N131

/ RecruitingPhase 2/3IIT

comparison of the effect of ibuprofen lysine with gelofen-acetaminophen on postoperative pain of mandibular third molars surgery

Start Date10 Jan 2019

Sponsor / Collaborator

Kermanshah University of Medical Sciences

100 Clinical Results associated with Ibuprofen Lysine

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100 Translational Medicine associated with Ibuprofen Lysine

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100 Patents (Medical) associated with Ibuprofen Lysine

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25,303

Literatures (Medical) associated with Ibuprofen Lysine

31 Dec 2025·Journal of Enzyme Inhibition and Medicinal Chemistry

Bioactivity profiling of Sanghuangporus lonicerinus : antioxidant, hypoglycaemic, and anticancer potential via in-vitro and in-silico approaches

Article

Author: Abdullaev, Ikram ; Petri, Edward ; Gafforov, Yusufjon ; Ghosh, Soumya ; Lim, Young Won ; Yarasheva, Manzura ; Rašeta, Milena ; Živanović, Nemanja ; Bekić, Sofija ; Chen, Jia Jia ; Abbasi, Arshad Mehmood ; Mišković, Jovana ; Wan-Mohtar, Wan Abd Al Qadr Imad ; Rapior, Sylvie ; Abdullaev, Bekhzod

This study investigates the mycochemical profile and biological activities of hydroethanolic (EtOH), chloroform (CHCl₃), and hot water (H₂O) extracts of Sanghuangporus lonicerinus from Uzbekistan. Antioxidant capacity was assessed using 2,2-diphenyl-1-picrylhydrazyl (DPPH), 2,2'-azino-bis-3-ethylbenzothiazoline-6-sulfonic acid (ABTS), NO, and FRAP assays, and in vitro hypoglycaemic effects were evaluated through α-amylase and α-glucosidase inhibition. Antiproliferative potential was explored by analysing the binding affinities of EtOH and H₂O extracts to estrogen receptor α (ERα), ERβ, androgen receptor (AR), and glucocorticoid receptor (GR), with molecular docking providing structural insights. LC-MS/MS analysis revealed solvent-dependent phenolic profiles, with the EtOH extract containing the highest total phenolic content (143.15 ± 6.70 mg GAE/g d.w.) and the best antioxidant capacity. The EtOH extract showed significant hypoglycaemic effects, with 85.29 ± 5.58% inhibition of α-glucosidase and 41.21 ± 0.79% inhibition of α-amylase. Moderate ERβ binding suggests potential for estrogen-mediated cancer therapy, while strong AKR1C3 inhibition by the EtOH extract supports its therapeutic potential.

01 Jul 2025·Separation and Purification Technology

Degradation of multicomponent pharmaceutical mixtures by electrochemical oxidation: Insights about the process evolution at varying applied currents and concentrations of organics and supporting electrolyte

Author: Perez-Herranz, V. ; Giner-Sanz, J. J. ; Balseviciute, A. ; Garcia-Gabaldon, M. ; Patino-Cantero, I. ; Carrillo-Abad, J. ; Marti-Calatayud, M. C.

Electrochem. oxidation is a treatment process that can achieve high degrees of removal of organic emerging pollutants from wastewater.The present study evaluates the removal and mineralization degrees achieved when treating by electrochem. oxidation multicomponent mixtures containing three model pharmaceuticals: atenolol, ibuprofen and norfloxacin.The progress of the removal process at different applied currents was followed through the evolution of the degree of mineralization and the concentration of ionic byproducts.The three compounds can be effectively removed, although atenolol was found to be the most recalcitrant one.An increase in the degree of mineralization with current was noted for currents above 200 mA, reaching a maximum value of 98.8% for an operation current of 800 mA.In general, total organic carbon declines linearly during the first stages of the process, while an exponential trend appears at the latter stages when complete mineralization is approached.Peak concentrations of some byproducts, such as formate, ammonia and nitrite ions, were detected at intermediate operating times.Such compounds are further oxidized, thus being depleted from the solution towards the end of the process.On the contrary, a final plateau concentration is reached for fluoride and nitrate ions.Such events occur faster at higher operation currents, thus denoting an accelerated process of mineralization.However, higher currents also induce a decrease in the mineralization current efficiency and an increase in the specific energy consumption.Notably, for a given current, the process evolves at a similar pace regardless of the concentration of organics and supporting electrolyte.In terms of net mineralization, this implies a more efficient utilization of the generated hydroxyl radicals in the removal of organics for higher solution concentrationsExperiments conducted at constant current and organics concentration, but varying the concentration of sodium sulfate, confirmed that hydroxyl radicals are the main species responsible for the removal of pharmaceuticals, whereas the oxidation of the supporting electrolyte only plays a secondary role.

01 Jul 2025·Separation and Purification Technology

Performance and mechanism of emerging-contaminant degradation by UV photoelectrochemical oxidation/boiling process for improving tap water quality

Author: Chen, Rui ; Wang, Xuan ; Yang, Qing ; Yang, Haocheng ; Huang, Xingxing ; Lu, Jinsuo ; Feng, Muyu ; Ao, Yujie

The continued detection of emerging contaminants (ECs) in water has raised the demand for high-quality drinking water.However, few water-treatment plants are willing to upgrade their existing facilities specifically to remove trace levels of ECs.Inspired by the cultural practices of boiling water in China and brewing coffee or tea with hot water in Western countries, this study explores the feasibility of UV photoelectrochem. oxidation and boiling (E-UV/BO) as an enhanced tap-water treatment method.The removal efficiency of E-UV/BO is tested using ibuprofen (IBU), atrazine (ATZ), trichloroacetic acid (TCA) and bisphenol A (BPA) as representative non-volatile ECs in tap water.Boiling alone removed less than 10% of the four non-volatile ECs, but E-UV at 100°C improved the removal efficiencies of IBU, TCA and BPA by 10%-25% and the degradation rate of ATZ by 15%-32% compared to those achieved in the case of E-UV at room temperature, while reducing the energy consumption by approx. 50%.In addition, boiling increased the kinetic energy of water mols. and the collision frequency between the mols., enhancing the mass transfer efficiency and promoting the reaction between the pollutants and reactive species.The oxidation products of IBU and ATZ were analyzed with gas chromatog.-mass spectrometry to identify possible degradation pathways.Toxicity assessments indicated lower toxicity of the IBU and ATZ oxidation intermediates than that of the parent compoundsThese findings demonstrate that the E-UV/BO technique can effectively remove various ECs from tap water, offering a new approach and tech. support for safe-drinking-water production

100 Deals associated with Ibuprofen Lysine

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External Link

KEGG	Wiki	ATC	Drug Bank
D06606	Ibuprofen Lysine	M02AA13 R02AX02 M01AE01 G02CC01 C01EB16	DBSALT001397

R&D Status

Approved

10 top approved records.

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Indication	Country/Location	Organization	Date
Ductus Arteriosus, Patent	United States	Recordati Rare Diseases, Inc.	13 Apr 2006
Arthritis	Australia	Reckitt Benckiser (Australia) Pty Ltd.	12 Aug 2003
Back Pain	Australia	Reckitt Benckiser (Australia) Pty Ltd.	12 Aug 2003
Dysmenorrhea	Australia	Reckitt Benckiser (Australia) Pty Ltd.	12 Aug 2003
Headache	Australia	Reckitt Benckiser (Australia) Pty Ltd.	12 Aug 2003
Migraine Disorders	Australia	Reckitt Benckiser (Australia) Pty Ltd.	12 Aug 2003
Musculoskeletal Pain	Australia	Reckitt Benckiser (Australia) Pty Ltd.	12 Aug 2003
Tension-Type Headache	Australia	Reckitt Benckiser (Australia) Pty Ltd.	12 Aug 2003
Toothache	Australia	Reckitt Benckiser (Australia) Pty Ltd.	12 Aug 2003