The goal of this clinical trial is to evaluate safety and tolerability of multiple oral doses of EC5026 in male and female patients with neuropathic pain due to spinal cord injury. The main question it aims to answer is whether EC5026 is safe and well tolerated in SCI patients with neuropathic pain. In addition, this trial will also study the effects of EC5026 on pain.
Researchers will compare EC5026 to placebo.
Participants will be asked to:
Take EC5026 or placebo in a masked fashion, once daily, for 14 consecutive days.
Undergo physical exams, vital signs assessments, ECGs, and blood draws
Complete assessments of pain, sleep, functional status, and perception of change

Start Date01 Jul 2024

Sponsor / Collaborator

Eicosis Human Health, Inc.

NCT06089837 / RecruitingPhase 1

A Phase 1b Multiple Ascending Dose (MAD) Study of EC5026 in Healthy Volunteers

EC5026 has been shown to be effective in preclinical pain models of pain, including inflammatory and neuropathic pain subtypes. Two Phase 1a studies - a Phase 1a single ascending dose (SAD) study and a Phase 1a fed-fasted study - have been conducted, evaluating the safety, tolerability, PK, and food effects of single oral doses of EC5026 ranging 0.5 to 24 mg. The present study will evaluate the safety, tolerability, and PK of 2 sequential ascending dose regimens of EC5026, administered once daily for 7 consecutive days, in healthy volunteers.

Start Date28 Nov 2023

Sponsor / Collaborator

Eicosis Human Health, Inc.

NCT04908995 / CompletedPhase 1

A Single-Center, Double-Blind, Placebo-Controlled, Phase 1a, Fed-Fasted, Crossover Study To Investigate The Safety, Tolerability, Pharmacokinetics, And Food Effects Of A Single Oral Dose Of EC5026 In Healthy Male And Female Subjects

The purpose of the study is to provide safety, tolerability, pharmacokinetics and food effects data of a single 8 mg oral dose of EC5026 in healthy subjects.

Start Date30 Apr 2021

Sponsor / Collaborator

Eicosis Human Health, Inc.

100 Clinical Results associated with EC-5026

100 Translational Medicine associated with EC-5026

100 Patents (Medical) associated with EC-5026

Literatures (Medical) associated with EC-5026

01 Jan 2024·Journal of pharmaceutical and biomedical analysis

Development and validation of LC-MS/MS method for estimating the pharmacokinetics, protein binding, and metabolic stability of soluble epoxide hydrolase inhibitor EC5026

Article

Author: Dey, Shankha ; Biradar, Rushikesh ; Dengale, Swapnil J ; Mane, Sayalee Sanjay

EC5026 is a soluble epoxide hydrolase (SEH) inhibitor which is being developed clinically (Phase-1) as a first-in-class analgesic for the treatment of pain. In the present study, we report the development and validation of the LC-MS/MS method for the estimation of EC5026 from rat plasma. The developed method is simple, specific, and sensitive for the quantification of EC5026 from rat plasma. The method was applied to investigate in-vivo pharmacokinetics after single oral administration (P.O.) of EC5026 (5.0 mg/kg) in Wistar rats. Further, the in-vitro metabolic stability and rat plasma protein binding of EC5026 were evaluated using the developed method. The in-vitro results demonstrated a moderate clearance with a value of 10.8 mL/min/kg and half-life (t1/2) of 57.75 min. The results show moderate clearance by the liver manifesting in satisfactory oral bioavailability. The rat plasma protein binding was estimated to be 96.24% ± 0.97% and 96.38% ± 0.56% at 1 µM and 10 µM concentrations, respectively. The developed analytical method is expected to facilitate future pre-clinical, clinical investigations of EC5026.

01 Sep 2023·Journal of pharmaceutical analysis

Quantification of soluble epoxide hydrolase inhibitors in experimental and clinical samples using the nanobody-based ELISA.

Article

Author: He, Qiyi ; Yang, Huiyi ; Yang, Jun ; Hwang, Sung Hee ; McCoy, Mark ; Qi, Meng ; Hammock, Bruce D ; Morisseau, Christophe ; Zhao, Suqing

To ensure proper dosage of a drug, analytical quantification of it in biofluid is necessary. Liquid chromatography mass spectrometry (LC-MS) is the conventional method of choice as it permits accurate identification and quantification. However, it requires expensive instrumentation and is not appropriate for bedside use. Using soluble epoxide hydrolase (sEH) inhibitors (EC5026 and TPPU) as examples, we report development of a nanobody-based enzyme-linked immunosorbent assay (ELISA) for such small molecules and its use to accurately quantify the drug chemicals in human samples. Under optimized conditions, two nanobody-based ELISAs were successfully established for EC5026 and TPPU with low limits of detection of 0.085 ng/mL and 0.31 ng/mL, respectively, and two order of magnitude linear ranges with high precision and accuracy. The assay was designed to detect parent and two biologically active metabolites in the investigation of a new drug candidate EC5026. In addition, the ELISAs displayed excellent correlation with LC-MS analysis and evaluation of inhibitory potency. The results indicate that nanobody-based ELISA methods can efficiently analyze drug like compounds. These methods could be easily implemented by the bedside, in the field in remote areas or in veterinary practice. This work illustrates that nanobody based assays offer alternative and supplementary analytical tools to mass spectrometry for monitoring small molecule medicines during clinical development and therapy. Attributes of nanobody based pharmaceutical assays are discussed.

01 Mar 2022·Acta pharmaceutica Sinica. BQ1 · CHEMISTRY

Structure-guided discovery of potent and oral soluble epoxide hydrolase inhibitors for the treatment of neuropathic pain

Q1 · CHEMISTRY

ArticleOA

Author: Chen, Guoliang ; Chen, Lu ; Liu, Zhongbo ; Fu, Yang ; Cao, Ruolin ; Hammock, Bruce D ; Du, Fangyu ; Sun, Jianwen ; Shi, Yajie ; Zheng, Zhonghui

Soluble epoxide hydrolase (sEH) is related to arachidonic acid cascade and is over-expressed in a variety of diseases, making sEH an attractive target for the treatment of pain as well as inflammatory-related diseases. A new series of memantyl urea derivatives as potent sEH inhibitors was obtained using our previous reported compound 4 as lead compound. A preferential modification of piperidinyl to 3-carbamoyl piperidinyl was identified for this series via structure-based rational drug design. Compound A20 exhibited moderate percentage plasma protein binding (88.6%) and better metabolic stability in vitro. After oral administration, the bioavailability of A20 was 28.6%. Acute toxicity test showed that A20 was well tolerated and there was no adverse event encountered at dose of 6.0 g/kg. Inhibitor A20 also displayed robust analgesic effect in vivo and dose-dependently attenuated neuropathic pain in rat model induced by spared nerve injury, which was better than gabapentin and sEH inhibitor (±)-EC-5026. In one word, the oral administration of A20 significantly alleviated pain and improved the health status of the rats, demonstrating that A20 was a promising candidate to be further evaluated for the treatment of neuropathic pain.

News (Medical) associated with EC-5026

30 Jan 2024

·www.prnewswire.com

EicOsis Initiates Phase 1b Clinical Trial of EC5026

EC5026 is the first soluble epoxide hydrolase inhibitor (sEHI) developed to treat pain DAVIS, Calif., Jan. 30, 2024 /PRNewswire/ -- EicOsis Human Health, a pharmaceutical company engaged in the development of a novel category of non-narcotic oral analgesics centered around the inhibition of the soluble epoxide hydrolase (sEH) enzyme, today announced the next step in its ongoing human clinical trials: the initiation of Phase 1b multiple-ascending dose clinical trial to test the safety of its drug candidate, EC5026. Continue Reading The double-blind, placebo-controlled Phase 1b study is designed to investigate the safety and pharmacokinetics of daily doses of EC5026 or placebo over seven days. Initial results show no apparent changes in vital signs, behavior effects, or clinically significant adverse effects in any subjects. EicOsis Initiates Multiple Dose Clinical Trial of Soluble Epoxide Hydrolase (sEH) Inhibitor Post this EC5026, a small molecule drug that is a potent and highly selective inhibitor of the sEH enzyme, plays a crucial role in regulating the metabolism of signaling lipids and responding to inflammation and other stress responses caused by trauma or disease. By inhibiting sEH, EC5026 alleviates pain by preventing the breakdown of natural analgesic and anti-inflammatory fatty acids, which represents a potential non-opioid approach to treat moderate to severe pain. Preclinical studies demonstrate no sedation or other adverse behavioral effects and no signs of addiction. UC Davis distinguished professor and founder of EicOsis, Bruce Hammock, who holds a joint appointment with the Department of Entomology and the UC Davis Comprehensive Cancer Center, discovered the enzyme inhibitor. "Many regulatory molecules are controlled as much by degradation as biosynthesis," Hammock explained. "The epoxy fatty acids rapidly degraded by the sEH regulate inflammation and control pain, fibrosis, depression, and neuroinflammation, to name a few processes." Dr. William K Schmidt, Vice President of Clinical Development at EicOsis, expressed optimism about the Phase 1b study and emphasized the promising safety and tolerability profile of EC5026. "The initial results from cohort 1 appear to replicate the very favorable safety profile we observed in our Phase 1a clinical studies where there were no adverse behavioral, cardiovascular, or neurological effects over five ascending single-dose levels and the maximum dose level that was 5 to 10-fold higher than the anticipated analgesic dose in humans." EicOsis is developing an sEH inhibitor EC5026 to treat pain and inflammation in multiple conditions and plans to initiate its first pain patient study in April 2024 to evaluate safety and analgesic effects in patients with a spinal cord injury who have failed to achieve satisfactory pain relief with existing non-opioid chronic pain medications. The FDA granted Fast Track status to EC5026 due to the unmet medical need for safe and effective non-opioid analgesics. "Initiation of the Phase 1b program represents a significant milestone for EicOsis Human Health and demonstrates the success and dedication of our team to make this happen. Demonstrating safety in Phase 1b studies will allow us to evaluate efficacy in patients and bring forward safe and effective treatments for serious disease," said Cindy McReynolds, Chief Executive Officer of EicOsis. The National Institutes of Health (NIH) supported the progression of EC5026 into clinical trials through the Small Business Innovation Research (SBIR), Blueprint Neurotherapeutics Network and the Helping to End Addiction Long-termSM Initiative (NIH HEAL InitiativeSM). 'Both our commitment and focus at EicOsis Human Health are guided by a genuine concern for the well-being of patients and recognizing the importance of identifying effective pain management alternatives," commented EicOsis clinical scientist Irene Cortes-Puch. "Therefore, the initiation of this Phase 1b clinical trial is an exciting step in advancing our mission to provide safer and effective treatments." EicOsis (pronounced eye-co-sis), derives its name from eicosanoids, "the major backbone of chemical mediators in the arachidonate cascade," said McReynolds. "It symbolizes the epoxide group in chemistry, which is key to the anti-inflammatory chemical mediators and where the biochemical target called soluble epoxide hydrolase works." Approximately 50 million Americans (20 percent of the population) suffer from chronic pain, according to the Centers for Disease Control and Prevention. The annual economic toll is $560 billion, encompassing direct medical expenses, lost productivity, and disability claims. Phase 1b multiple-ascending dose clinical study details can be found in the following link: . SOURCE EicOsis

Phase 1Fast Track

100 Deals associated with EC-5026

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Indication	Highest Phase	Country/Location	Organization	Date
Neuralgia	Phase 1	US	Eicosis Human Health, Inc.	17 Oct 2019
Diabetic Neuropathies	Phase 1	-	University Of California - Davis Branch (513968)	-

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NCT04228302 (CTgov)	Phase 1	-	40	Placebo oral capsule	fzihvofqzw(rrjokigzqh) = qqjmdstmsp wcvpsfzprj (zzgtetjqrd, zyfkibpsqd - wzlmcfldmw) View more	-	30 Jun 2021

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