A Randomized, Double-blind, Controlled, Phase 2 Study to Assess Efficacy, Long Term Safety and Tolerability of RT001 in Subjects With Progressive Supranuclear Palsy

This is a randomized, placebo-controlled trial of RT001 in patients with PSP.

Start Date23 Jun 2021

Sponsor / Collaborator

Retrotope, Inc.

NCT04762589

/ Unknown statusPhase 2

A Randomized, Double-Blind, Placebo-Controlled, Phase 2 Study to Assess Efficacy, Long Term Safety and Tolerability of RT001 in Subjects With Amyotrophic Lateral Sclerosis

RT001-014 is a Randomized, Double-Blind, Placebo-Controlled, Phase 2 Study to Assess Efficacy, Long Term Safety and Tolerability of RT001 in Subjects with Amyotrophic Lateral Sclerosis

Start Date10 Mar 2021

Sponsor / Collaborator

Retrotope, Inc.

NCT04102501

/ CompletedPhase 3

A Randomized, Double-Blind, Controlled, Phase 2/3 Study to Assess Efficacy, Long Term Safety and Tolerability of RT001 in Subjects With Friedreich's Ataxia

The purpose of this study is to assess the Efficacy, Long Term Safety and Tolerability of RT001 in subjects with Friedreich's Ataxia

Start Date30 Oct 2019

Sponsor / Collaborator

Retrotope, Inc.

100 Clinical Results associated with Deulinoleic acid

100 Translational Medicine associated with Deulinoleic acid

100 Patents (Medical) associated with Deulinoleic acid

Literatures (Medical) associated with Deulinoleic acid

01 Mar 2023·Journal of neurology

Double blind trial of a deuterated form of linoleic acid (RT001) in Friedreich ataxia

Article

Author: Vogel, Adam P ; Heerinckx, Frederic ; Krtolica, Ana ; Litterman, Nadia ; Milner, Peter ; Lynch, David R ; Omidvar, Omid ; Mathews, Katherine D ; Perlman, Susan ; Zesiewicz, Theresa ; Subramony, Sub ; Midei, Mark ; van der Ploeg, Lex

OBJECTIVES:

Friedreich ataxia is (FRDA) an autosomal recessive neurodegenerative disorder associated with intrinsic oxidative damage, suggesting that decreasing lipid peroxidation (LPO) might ameliorate disease progression. The present study tested the ability of RT001, a deuterated form of linoleic acid (D2-LA), to alter disease severity in patients with FRDA in a double-blind placebo-controlled trial.

METHODS:

Sixty-five subjects were recruited across six sites and received either placebo or active drug for an 11-month study. Subjects were evaluated at 0, 4, 9, and 11 months, with the primary outcome measure being maximum oxygen consumption (MVO2) during cardiopulmonary exercise testing (CPET). A key secondary outcome measure was a composite statistical test using results from the timed 1-min walk (T1MW), peak workload, and MVO2.

RESULTS:

Forty-five subjects completed the protocol. RT001 was well tolerated, with no serious adverse events related to drug. Plasma and red blood cell (RBC) membrane levels of D2-LA and its primary metabolite deuterated arachidonic acid (D2-AA) achieved steady-state concentrations by 4 months. No significant changes in MVO2 were observed for RT001 compared to placebo. Similarly, no differences between the groups were found in secondary or exploratory outcome measures. Post hoc evaluations also suggested minimal effects of RT001 at the dosages used in this study.

INTERPRETATIONS:

The results of this study provide no evidence for a significant benefit of RT001 at the dosages tested in this Friedreich ataxia patient population.

01 Nov 2020·Journal of pharmaceutical sciencesQ3 · MEDICINE

Plasma and Red Blood Cell Membrane Accretion and Pharmacokinetics of RT001 (bis-Allylic 11,11-D2-Linoleic Acid Ethyl Ester) during Long Term Dosing in Patients

Q3 · MEDICINE

Article

Author: Brenna, J Thomas ; Fielding, Robert ; James, Genevieve ; van der Ploeg, Lex ; Milner, Peter ; Midei, Mark ; Heerinckx, Frederic ; Shchepinov, Mikhail S ; Atwal, Paldeep ; Schmidt, Karsten

RT001 is the di-deutero isotopologue of linoleic acid ethyl ester (D2-LA). Resistance to oxidative damage at the carbon-deuterium bond depends upon the concentration of D2-LA as a percentage of total LA. We report here on the plasma and red cell (RBC) pharmacokinetics (PK) of D2-LA, and its metabolite 13,13-D2-arachidonic acid (D2-AA), in patients with multiple neurodegenerative diseases (total of 59 participants). In Friedreich's ataxia patients, D2-LA was absorbed and transported similarly to dietary LA, peaking at about 6 h after oral dosing. Plasma D2-LA concentrations approached steady state after 28 days of dosing. After 6 months of daily dosing in subjects with other disorders, D2-LA and D2-AA levels were at or above the 20% of total (D2-LA/total LA, or D2-AA/total AA) therapeutic targets for most subjects. We conclude that chronic dosing of RT001 and associated dietary guidance can be maintained over many months to achieve target plasma and RBC levels, forming a basis for therapeutic dosing across a broad range of conditions. RT001 has been safe and well-tolerated in 59 different participants treated across 10 different neurodegenerative diseases in multiple clinical trials for up to 36 months with no significant drug related adverse events limiting use.

01 Jun 2019·The FEBS journalQ3 · BIOLOGY

Threshold protective effect of deuterated polyunsaturated fatty acids on peroxidation of lipid bilayers

Q3 · BIOLOGY

Article

Author: Vidovic, Dragoslav ; Pratt, Derek A. ; Kotova, Elena A. ; Shmanai, Vadim V. ; Bekish, Andrei V. ; Shchepinov, Mikhail S. ; Sharko, Olga L. ; Antonenko, Yuri N. ; Saal, Harry J. ; Fomich, Maksim A. ; Firsov, Alexander M.

Autoxidation of polyunsaturated fatty acids (PUFAs) damages lipid membranes and generates numerous toxic by‐products implicated in neurodegeneration, aging, and other pathologies. Abstraction of bis‐allylic hydrogen atoms is the rate‐limiting step of PUFA autoxidation, which is inhibited by replacing bis‐allylic hydrogens with deuterium atoms (D‐PUFAs). In cells, the presence of a relatively small fraction of D‐PUFAs among natural PUFAs is sufficient to effectively inhibit lipid peroxidation (LPO). Here, we investigate the effect of various D‐PUFAs on the stability of liposomes under oxidative stress conditions. The permeability of vesicle membranes to fluorescent dyes was measured as a proxy for bilayer integrity, and the formation of conjugated dienes was monitored as a proxy for LPO. Remarkably, both approaches reveal a similar threshold for the protective effect of D‐PUFAs in liposomes. We show that protection rendered by D‐PUFAs depends on the structure of the deuterated fatty acid. Our findings suggest that protection of PUFAs against autoxidation depends on the total level of deuterated bi‐sallylic (CD2) groups present in the lipid bilayer. However, the phospholipid containing 6,6,9,9,12,12,15,15,18,18‐d10‐docosahexaenoic acid exerts a stronger protective effect than should be expected from its deuteration level. These findings further support the application of D‐PUFAs as preventive/therapeutic agents in numerous pathologies that involve LPO.

News (Medical) associated with Deulinoleic acid

15 Dec 2023

·synapse.patsnap.com

Understanding Plasminogen activators Inhibitors and Methods to Keep Abreast of Their Recent Developments

Plasminogen activators are enzymes that play a crucial role in the human body's fibrinolytic system. They are responsible for converting plasminogen, an inactive precursor, into plasmin, an active enzyme that breaks down blood clots. Plasminogen activators are essential in maintaining the balance between clot formation and dissolution, preventing excessive clotting and ensuring proper blood flow. They are used therapeutically in the treatment of conditions such as acute ischemic stroke, deep vein thrombosis, and pulmonary embolism, where rapid clot dissolution is necessary. Plasminogen activators, such as tissue plasminogen activator (tPA), are administered intravenously to restore blood flow and prevent tissue damage caused by blood clots. The Plasminogen Activator Inhibitor (PAI) was first discovered in the plasma of pregnant women by Brakman and Astrup in 1963, and subsequently identified by other researchers. Currently, four types of PAIs have been identified in humans: PAI-1, PAI-2, PAI-3, and PAI-4. Among these, PAI-1 accounts for 99% of the activity and plays a major role. PAI-1 is widely distributed in the body’s endothelial cells, smooth muscle cells, liver cells, fat cells, macrophages, neutrophils, glomerular mesangial cells, platelets, and some malignant tumor cells. Plasma PAI-1 is mainly produced by endothelial cells and liver cells. PAI-1 is extremely unstable both in vivo and in vitro, with a half-life of about 20 minutes. This is mainly due to the oxidation of the active center of glutamic acid and the degradation of PAI-1 by cell phagocytosis after forming a complex with tissue-type plasminogen activator (t-PA) or urokinase-type plasminogen activator (u-PA). Plasma PAI-1 mainly exists in two forms: one is active, known as activated PAI-1; the other is inactive, known as latent PAI-1. These two forms of PAI-1 have the same molecular weight and immunoreactivity, but different conformations. The active PAI-1 can be stabilized and maintain its activity by binding to vitronectin. The analysis of the target Plasminogen activators reveals a competitive landscape with companies such as Hunan Er-Kang Pharmaceutical Co., Ltd., Akorn Operating Co. LLC, Hainan Sihuan Pharmaceutical Co. Ltd., and Beijing Science Sun Pharmaceutical Co., Ltd. leading the way with approved drugs. These drugs have been approved for indications such as Conjunctivitis, Hemorrhage, Hordeolum, and more. The development of small molecule drugs and enzymes is progressing rapidly, indicating potential breakthroughs in the treatment of various medical conditions. China is at the forefront of the development of Plasminogen activators, followed by the United States. Other countries/locations are also actively involved in the development of drugs for this target. Overall, the target Plasminogen activators show promise in the pharmaceutical industry, with potential for further growth and development in the future. How do they work?Plasminogen activators inhibitors are substances that inhibit the activity of plasminogen activators. Plasminogen activators are enzymes that convert plasminogen, an inactive precursor, into plasmin, an active enzyme involved in the breakdown of blood clots. Plasminogen activators inhibitors, as the name suggests, prevent or inhibit the activation of plasminogen, thereby reducing the breakdown of blood clots. From a biomedical perspective, plasminogen activators inhibitors play a crucial role in regulating the clotting and fibrinolysis processes in the body. They help maintain the balance between clot formation and clot dissolution. By inhibiting plasminogen activators, these inhibitors can prevent excessive clot breakdown, which may be beneficial in certain medical conditions where clot formation is necessary, such as during surgery or in the treatment of bleeding disorders. In the context of biomedicine, plasminogen activators inhibitors have therapeutic implications. They can be used as medications to prevent the breakdown of blood clots in conditions such as deep vein thrombosis, pulmonary embolism, or stroke. By inhibiting plasminogen activators, these inhibitors can help stabilize blood clots and prevent their dissolution, promoting clot stability and reducing the risk of complications. It is important to note that the use of plasminogen activators inhibitors should be carefully monitored and administered under medical supervision, as their effects on the clotting system need to be balanced to avoid excessive clot formation or inhibition. List of Plasminogen activators InhibitorsThe currently marketed Plasminogen activators inhibitors include: PlasminAminocaproic AcidTaurine/Aminocaproic Acid/Aspartic Acid/Chlorphenamine MaleateTaurine/Aminocaproic Acid/Potassium L-aspartate/Chlorphenamine MaleateLTI-01O2L-001APT-912BM-06021CVS-3083M-5For more information, please click on the image below. What are Plasminogen activators inhibitors used for?Plasminogen activators inhibitors are used therapeutically in the treatment of conditions such as acute ischemic stroke, deep vein thrombosis, and pulmonary embolism, where rapid clot dissolution is necessary. For more information,please click on the image below to log in and search. How to obtain the latest development progress of Plasminogen activators inhibitors?In the Synapse database, you can keep abreast of the latest research and development advances of Plasminogen activators inhibitors anywhere and anytime, daily or weekly, through the "Set Alert" function. Click on the image below to embark on a brand new journey of drug discovery!

16 Sep 2022

·www.globenewswire.com

BioJiva Reports Results of Pilot Phase 2 Clinical Trial of RT001 in Patients with Amyotrophic Lateral Sclerosis (ALS)

LOS ALTOS, Calif., Sept. 15, 2022 (GLOBE NEWSWIRE) -- BioJiva, a clinical-stage biopharmaceutical company focused on the development of novel, first-in-class therapies for degenerative diseases, today reported data from its completed multicenter, randomized, double-blind, placebo-controlled pilot Phase 2 clinical trial evaluating RT001, the company’s lead development candidate, in patients with amyotrophic lateral sclerosis (ALS or Lou Gehrig’s disease). The trial’s prespecified primary endpoint was change from baseline in the revised ALS Functional Rating Scale (ALSFRS-R) following 24 weeks of treatment. At 24 weeks, data demonstrated that patients treated with RT001 experienced less worsening (a 3.3-point reduction from baseline) in ALSFRS-R score as compared to greater worsening (4.6-point reduction from baseline) for the placebo group. Similarly, patients treated with RT001 experienced less worsening (a 13.3-point increase from baseline) in their score on the 40-item ALS assessment questionnaire (ALSAQ40) as compared to the placebo group (a 17.2-point increase from baseline). While suggesting a signal of directional improvement with RT001 treatment, these findings did not achieve statistical significance due to the small size of the study. This six-month randomized Phase 2 pilot study (NCT04762589), which was followed by a six-month open-label extension during which all patients received RT001, was conducted at four ALS Centers of Excellence in Europe. Investigators enrolled 43 patients with ALS who had symptom duration of less than three years. Enrolled patients had baseline ALSFRS-R scores ranging from 25 to 44, with a mean of 38.2 (+/-5.0.). Thirty-nine of the 43 enrolled subjects completed the initial 24-week randomized phase, with 32 of those also completing the open-label extension for a full year of treatment. At Week 24, patients receiving RT001 demonstrated a worsening from baseline in ALSFRS-R score of 3.3 points (from 38.2 to 34.9), as compared to a 4.6-point worsening from baseline for the placebo group (from 38.2 to 33.6). For patients who were enrolled with more severe disease (ALSFRS-R Data from the study’s 24-week open-label extension portion demonstrated that a signal of clinical benefit with RT001 treatment was also evident at 12 months. As no concurrent placebo was administered after 24 weeks, 12-month comparisons were made using data from the PRO ACT Database1, a validated and predictive historical control database of ALS progression. At 12 months, RT001-treated patients demonstrated a decrease in ALSFRS-R score of 7.2 +/- 6.7 points, whereas the PRO ACT Database shows an expected worsening on the ALSFRS score at 12 months of 10.1 points. For the study’s most severe patients that completed 12 months (ALSFRS-R “The promising signal of clinical benefit shown in this study with RT001 in a small group of ALS patients, combined with the continued demonstration of the well tolerated nature of the treatment, provides support for considering a larger clinical trial,” said Leonard H. van den Berg, M.D., Ph.D., professor of neurology at UMC Utrecht in the Netherlands, director of the Netherlands ALS Center, Chairman of TRICALS, an ALS clinical trial-focused European research initiative spanning 42 top research centers in 15 countries, and the principal investigator of the study. “Additionally, the study data suggest that patients with more severe ALS may have a higher likelihood of benefitting from RT001 treatment, which provides important context for considering the design and enrollment criteria for the next clinical trial.” “We conducted this trial with the dual goals of better understanding the manner in which RT001 may potentially impact the progression of ALS and detecting a signal of therapeutic benefit for patients receiving the treatment. While a small study that was not powered to demonstrate significance, we did see trends for RT001-treated patients compared to the placebo group that suggest the potential for RT001 to offer patients meaningful clinical benefit. The learnings from this study position us to continue development of RT001 for ALS, advancing next to a larger, statistically powered study focused on the more severe patient population that appears more likely to benefit from the treatment,” said Mark G. Midei, M.D., BioJiva’s vice president for medical affairs. About RT001 RT001 is a clinical stage isotopically stabilized, synthetic linoleic acid (LA) designed to combat the oxidative stress and cellular degeneration that arises from lipid peroxidation (LPO). While all healthy human tissues undergo this physiological process of cell degeneration and repair, it is well-established that a wide range of serious degenerative diseases are precipitated when the LPO process becomes out of balance. Polyunsaturated fatty acids (PUFAs), which make up cell and mitochondrial membranes throughout the body and are vital to healthy cellular function, are the target of the LPO process due to their inherent instability. Free radicals in the body exploit the instability of PUFAs to trigger chain reactions that drive LPO and the resulting breakdown of these vital PUFAs. Stabilized PUFAs, such as RT001, that become an integral part of all membranes are capable of down-regulating LPO to protect these membranes. About ALS Amyotrophic lateral sclerosis (ALS) is a rare, progressive neurodegenerative disease that primarily involves the nerve cells, or neurons, which are responsible for controlling voluntary muscle movements such as walking, talking and chewing. ALS and its related disorders are caused by the gradual degeneration of motor neurons, which are responsible for controlling communication between the brain and muscles responsible for voluntary movements. As these motor neurons deteriorate, communication between the brain and these muscles is impaired, leading to difficulty for patients in performing voluntary movements. As the disease progresses, voluntary muscle control becomes more difficult for patients, leading to an inability to breathe on their own and ultimately death. There is currently no cure for ALS and no effective treatment to halt, or reverse, the progression of the disease. About BioJiva BioJiva is a clinical-stage biopharmaceutical company focused on the development of first-in-class therapies for degenerative diseases ranging from orphan neurodegenerative indications to large market degenerative conditions. The company’s therapeutic pipeline consists of disease-modifying, isotopically stabilized synthetic versions of polyunsaturated fatty acids (PUFAs) that are designed to combat the oxidative stress and cellular degeneration by downregulation the lipid peroxidation (LPO) process. The company’s lead development candidate, RT001, is an isotopically stabilized, synthetic linoleic acid (LA) that is in clinical development for a range of orphan neurodegenerative diseases, including infantile neuroaxonal dystrophy (INAD), amyotrophic lateral sclerosis (ALS or Lou Gehrig’s disease) and progressive supranuclear palsy (PSP). In addition, the company is advancing its second development candidate, RT011, an isotopically stabilized, synthetic docosahexaenoic acid (DHA), toward the clinic for the treatment of dry age-related macular degeneration (AMD). BioJiva was founded in 2022 and is advancing the development assets formerly owned by Retrotope, which it purchased through a Delaware bankruptcy proceeding under Chapter 7. BioJiva is not a progression of Retrotope and BioJiva is not the former Retrotope. Several employees, advisors, and other service providers of Retrotope have joined BioJiva as part of the new company’s efforts to develop the previously Retrotope-owned assets.

CollaborateFirst in ClassPhase 2Clinical Result

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Indication	Highest Phase	Country/Location	Organization	Date
Friedreich Ataxia	Phase 3	United States	Retrotope, Inc.	30 Oct 2019
Neuroaxonal Dystrophies	Phase 3	United States	Retrotope, Inc.	05 Nov 2018
Supranuclear Palsy, Progressive	Phase 2	Germany	Retrotope, Inc.	23 Jun 2021
Amyotrophic Lateral Sclerosis	Phase 2	Estonia	Biojiva LLC	22 Feb 2021
Amyotrophic Lateral Sclerosis	Phase 2	Latvia	Biojiva LLC	22 Feb 2021
Amyotrophic Lateral Sclerosis	Phase 2	Netherlands	Biojiva LLC	22 Feb 2021
Amyotrophic Lateral Sclerosis	Phase 2	Sweden	Biojiva LLC	22 Feb 2021
Nasolabial fold wrinkles	Phase 2	United States	Revance Therapeutics, Inc.	01 Nov 2008

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Study	Phase	Population	Analyzed Enrollment	Group	Results	Evaluation	Publication Date


NCT04102501 (CTgov)	Phase 3	Friedreich Ataxia	65	RT001 (RT001)	ikylglzmuq(jzccgpkaae) = mczazafbty hsvzyhtnxz (sxbojkhdcp, 0.04) View more	-	27 May 2022
				Placebo (Placebo)	ikylglzmuq(jzccgpkaae) = ctkrscndwh hsvzyhtnxz (sxbojkhdcp, 0.04) View more
NCT02445794 (CTgov)	Phase 1/2	Friedreich Ataxia	19	High dose cohort+Low dose cohort (RT001, Oral, 1.8 g/Day)	pxtkovscbi(hvwdmgmjuz) = mamokibjzk qszcgsfggp (hjtrfvaayw, 86)	-	27 Nov 2020
				High dose cohort+Low dose cohort (RT001, Oral, 9 g/Day)	pxtkovscbi(hvwdmgmjuz) = jzallicxko qszcgsfggp (hjtrfvaayw, 251)

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