Neurolixis
A major contributor to this article appears to have a close connection with its subject. (March 2019) |
Industry | Biopharmaceuticals |
---|---|
Founded | 2011 |
Headquarters | |
Key people | Mark A. Varney, Adrian Newman-Tancredi |
Website | https://www.neurolixis.com/en/ |
Neurolixis is a biopharmaceutical company focused on novel drugs for the treatment of human central nervous system diseases.
Neurolixis Inc. was founded in 2011 by Mark A. Varney, PhD, and Adrian Newman-Tancredi, PhD, DSc.. The company's therapeutic focus is on CNS disorders including Parkinson's disease, neurological orphan disorders, depression and cognitive deficits.[1] The company has offices in USA and in France.[2]
In September 2013, Neurolixis in-licensed two clinical-phase drugs, befiradol and F-15599 from Pierre Fabre Laboratories, a French pharmaceutical company.[3] Befiradol (also known as NLX-112) is targeted to the treatment of movement disorders, notably dyskinesia in Parkinson's disease, whereas F-15599 (also known as NLX-101) is intended for the treatment of autism spectrum disorders including Rett syndrome and Fragile X syndrome. In addition, Neurolixis is developing its own novel chemical entities (NCEs), notably NLX-204 (see below).
Neurolixis has been awarded a series of research grants by the Michael J. Fox Foundation and by Parkinson's UK. Neurolixis undertook research examining the effects of novel, highly selective and efficacious serotonergic drugs targeting 5-HT1A receptors in brain regions relevant to therapeutic properties in Parkinson's disease.[4] The Michael J. Fox Foundation subsequently announced that it was supporting proof-of-principle studies on befiradol (also known as NLX-112) in models of Parkinson's disease[5] and showcased Neurolixis in its Partnering Program.[6] In January 2018, the British charity Parkinson's UK announced that it had awarded Neurolixis a grant to advance development of befiradol up to clinical phase in Parkinson's disease patients.[7] In March 2019, Neurolixis announced that the US Food and Drug Administration (FDA) gave a positive response to Neurolixis' Investigational New Drug (IND) application for befiradol to be tested in a Phase 2 clinical study in Parkinson's disease patients with troublesome Levodopa-induced dyskinesia.[8] Studies published in 2020 using non-human primate models of Parkinson's disease, (MPTP-treated marmosets and MPTP-treated macaques), found that befiradol potently reduced Levodopa-induced dyskinesia at oral doses as low as 0.1 to 0.4 mg/kg.[9][10]
On 22 November 2020, The Sunday Times reported that the two charities, Parkinson's UK and Michael J. Fox Foundation, were jointly investing $2 million to support a clinical trial on befiradol in Parkinson's disease patients with troublesome Levodopa-induced dyskinesia, a potentially "life changing" drug.[11] On 23 November 2020, Parkinson's UK and Michael J. Fox Foundation, confirmed their funding in an official announcement.[12] Neurolixis announced on 30 November 2021 the start of patient recruitment in a Phase 2A clinical trial to investigate the safety, tolerability and preliminary efficacy of NLX-112 versus placebo in L-dopa-induced dyskinesia in Parkinson's disease patients.[13] On 20 March 2023, Neurolixis, Parkinson's UK and Michael J. Fox Foundation announced that the clinical trial had met its primary endpoint of safety and tolerability, and also the secondary endpoint of efficacy in reducing Levodopa-induced dyskinesia.[14]
In other studies, befiradol showed pro-motility activity in a transgenic nematode worm model of spinocerebellar ataxia type 3 [15] (also known as SCA3 or Machado-Joseph disease), an orphan disorder. Befiradol also reversed depression-like behavior and catalepsy induced by tetrabenazine, a drug used for the treatment of Huntington's disease.[16]
F-15599 (also known as NLX-101) was awarded Orphan Drug Status by the United States Food and Drug Administration (FDA) in October 2013[17] and Orphan Medicinal Product designation by the European Medicines Agency in March 2014.[18] In collaboration with researchers at the University of Bristol, Neurolixis has been awarded a grant by the International Rett Syndrome Foundation to study F-15599 in animal models of Rett syndrome.[19] In June 2015, Neurolixis was awarded a grant by the Rett Syndrome Research Trust to advance F-15599 to clinical development.[20] Subsequent studies on F-15599 investigated its functional selectivity (also referred to as 'biased agonism') at cortical serotonin 5-HT1A receptors using brain imaging techniques in rat: functional magnetic resonance imaging[21] and positron emission tomography.[22] The functional selectivity of F-15599 was considered to underlie its rapid-acting antidepressant-like activity in the 'chronic mild stress' (CMS) model of depression. F-15599 reversed CMS-induced anhedonia (measured as a deficit in sucrose solution consumption) after a single day of treatment.[23] More recently, Neurolixis has broadened its characterization of F-15599 to other autism spectrum disorders, notably Fragile X syndrome. Researchers at the University of California, Riverside showed that F-15599 protected transgenic Fragile X syndrome mice from audiogenic seizures and death.[24]
Preclinical drug discovery
[edit]In addition to developing befiradol and F-15599, Neurolixis is also developing its own novel chemical entities (NCEs) in collaboration with a team at Jagiellonian University in Krakow, Poland. Scientists from Neurolixis and Jagiellonian University filed a patent application on the NCEs in 2016,[25] and it issued in the USA under patent number US10562853B2.[26] The NCEs are selective serotonin 5-HT1A receptor agonists that show functional selectivity for either extracellular signal-regulated kinases activation[27] or for beta arrestin activation.[28] It has been suggested that such compounds may have utility for treatment of distinct CNS disorders.[29] In particular, NLX-204 shows preferential activation of extracellular signal-regulated kinases[30] and exhibits rapid-acting antidepressant-like activity in rodent models.[31]
External links
[edit]References
[edit]- ^ "neurolixis.com". neurolixis.com. Archived from the original on 2014-05-17. Retrieved 2014-05-17.
- ^ "Pôles Sud n°50 - le magazine de l'agglomération de Castres-Mazamet". Archived from the original on 2015-06-26. Retrieved 2015-06-25.
- ^ "NEUROLIXIS ANNOUNCES IN-LICENSING OF TWO CLINICAL COMPOUNDS FROM PIERRE FABRE MEDICAMENT" (PDF). neurolixis.com. September 23, 2013. Retrieved 2019-06-05.
- ^ "Parkinson's Disease Grants funded by the Michael J. Fox Foundation | The Michael J. Fox Foundation". Michaeljfox.org. 2012-10-26. Retrieved 2014-05-17.
- ^ "Predicting the Efficacious Dose of the Selective 5-HT1A Agonist NLX-112". The Michael J. Fox Foundation for Parkinson's Research - Parkinson's Disease.
- ^ "Partnering Program of the Michael J. Fox Foundation for Parkinson?s Research | Parkinson's Disease Information". Archived from the original on 2015-06-26. Retrieved 2015-06-25.
- ^ "Investing in a new treatment for dyskinesia - Parkinson's UK". www.parkinsons.org.uk. 24 January 2018.
- ^ Inc, Neurolixis. "FDA Approves Neurolixis IND Application for a Clinical Trial with NLX-112 in Parkinson's Disease". PRLog.
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has generic name (help) - ^ Depoortere, R.; Johnston, T.H.; Fox, S.H.; Brotchie, J.M.; Newman-Tancredi, A. (September 2020). "The selective 5-HT1A receptor agonist, NLX-112, exerts anti-dyskinetic effects in MPTP-treated macaques". Parkinsonism & Related Disorders. 78: 151–157. doi:10.1016/j.parkreldis.2020.08.009. PMID 32846366. S2CID 221343904.
- ^ Fisher, Ria; Hikima, Atsuko; Morris, Rebecca; Jackson, Michael J.; Rose, Sarah; Varney, Mark A.; Depoortere, Ronan; Newman-Tancredi, Adrian (May 2020). "The selective 5-HT1A receptor agonist, NLX-112, exerts anti-dyskinetic and anti-parkinsonian-like effects in MPTP-treated marmosets". Neuropharmacology. 167: 107997. doi:10.1016/j.neuropharm.2020.107997. PMC 7103782. PMID 32057799.
- ^ "'Life-changing' drug to calm Parkinson's twitches set for human trials".
- ^ "Global charities join forces to drive forward new drug for Parkinson's" (Press release).
- ^ Clinical trial number NCT05148884 for "Study to Assess the Safety, Tolerability and Preliminary Efficacy of NLX-112 Versus Placebo in L-dopa-induced Dyskinesia" at ClinicalTrials.gov
- ^ "Neurolixis Announces Positive Ph2A Proof-of-Concept on NLX-112 in Levodopa-Induced Dyskinesia in Parkinson's Disease". 20 March 2023 – via Newsmatics Inc.
- ^ Pereira-Sousa, Joana; Ferreira-Lomba, Bruna; Bellver-Sanchis, Aina; Vilasboas-Campos, Daniela; Fernandes, Jorge H.; Costa, Marta D.; Varney, Mark A.; Newman-Tancredi, Adrian; Maciel, Patrícia; Teixeira-Castro, Andreia (May 2021). "Identification of the 5-HT1A serotonin receptor as a novel therapeutic target in a C. elegans model of Machado-Joseph disease". Neurobiology of Disease. 152: 105278. doi:10.1016/j.nbd.2021.105278. ISSN 1095-953X. PMID 33516872.
- ^ Jastrzębska-Więsek, Magdalena; Wesołowska, Anna; Kołaczkowski, Marcin; Varney, Mark A.; Newman-Tancredi, Adrian; Depoortere, RonanY (2022-08-01). "The selective 5-HT 1A receptor agonist, NLX-112, overcomes tetrabenazine-induced catalepsy and depression-like behavior in the rat". Behavioural Pharmacology. 33 (5): 333–341. doi:10.1097/FBP.0000000000000681. ISSN 1473-5849. PMID 35695543.
- ^ "Search Orphan Drug Designations and Approvals". Accessdata.fda.gov. 2013-10-25. Retrieved 2014-05-17.
- ^ "Community register of orphan medicinal products". Ec.europa.eu. Retrieved 2014-05-17.
- ^ Bristol, University of. "April: Rett syndrome research - News - University of Bristol". www.bristol.ac.uk.
- ^ "RSRT Awards $530,000 to Neurolixis for Clinical Development of NLX-101". 24 June 2015.
- ^ Vidal, Benjamin; Fieux, Sylvain; Redouté, Jérôme; Villien, Marjorie; Bonnefoi, Frédéric; Le Bars, Didier; Newman-Tancredi, Adrian; Costes, Nicolas; Zimmer, Luc (October 2018). "In vivo biased agonism at 5-HT1A receptors: characterisation by simultaneous PET/MR imaging". Neuropsychopharmacology. 43 (11): 2310–2319. doi:10.1038/s41386-018-0145-2. PMC 6135772. PMID 30030540.
- ^ Levigoureux, Elise; Vidal, Benjamin; Fieux, Sylvain; Bouillot, Caroline; Emery, Stéphane; Newman-Tancredi, Adrian; Zimmer, Luc (17 July 2019). "Serotonin 5-HT 1A Receptor Biased Agonists Induce Different Cerebral Metabolic Responses: A [ 18 F]-Fluorodesoxyglucose Positron Emission Tomography Study in Conscious and Anesthetized Rats". ACS Chemical Neuroscience. 10 (7): 3108–3119. doi:10.1021/acschemneuro.8b00584. PMID 30576601. S2CID 58663413.
- ^ Depoortère, Ronan; Papp, Mariusz; Gruca, Piotr; Lason-Tyburkiewicz, Magdalena; Niemczyk, Monika; Varney, Mark A; Newman-Tancredi, Adrian (November 2019). "Cortical 5-hydroxytryptamine 1A receptor biased agonist, NLX-101, displays rapid-acting antidepressant-like properties in the rat chronic mild stress model". Journal of Psychopharmacology. 33 (11): 1456–1466. doi:10.1177/0269881119860666. PMID 31290370. S2CID 195871156.
- ^ Tao, X.; Newman-Tancredi, A.; Varney, M. A.; Razak, K. A. (2023-01-15). "Acute and Repeated Administration of NLX-101, a Selective Serotonin-1A Receptor Biased Agonist, Reduces Audiogenic Seizures in Developing Fmr1 Knockout Mice". Neuroscience. 509: 113–124. doi:10.1016/j.neuroscience.2022.11.014. ISSN 1873-7544. PMID 36410632.
- ^ "Compounds for treating disorders sensitive to serotoninergic regulation controlled by the 5-ht1a receptors". 23 June 2017.
- ^ "Compounds for treating disorders sensitive to serotoninergic regulation controlled by the 5-HT1A receptors".
- ^ Sniecikowska, Joanna; Gluch-Lutwin, Monika; Bucki, Adam; Więckowska, Anna; Siwek, Agata; Jastrzebska-Wiesek, Magdalena; Partyka, Anna; Wilczyńska, Daria; Pytka, Karolina; Pociecha, Krzysztof; Cios, Agnieszka; Wyska, Elżbieta; Wesołowska, Anna; Pawłowski, Maciej; Varney, Mark A.; Newman-Tancredi, Adrian; Kolaczkowski, Marcin (14 March 2019). "Novel Aryloxyethyl Derivatives of 1-(1-Benzoylpiperidin-4-yl)methanamine as the Extracellular Regulated Kinases 1/2 (ERK1/2) Phosphorylation-Preferring Serotonin 5-HT 1A Receptor-Biased Agonists with Robust Antidepressant-like Activity". Journal of Medicinal Chemistry. 62 (5): 2750–2771. doi:10.1021/acs.jmedchem.9b00062. PMID 30721053.
- ^ Sniecikowska, Joanna; Gluch-Lutwin, Monika; Bucki, Adam; Więckowska, Anna; Siwek, Agata; Jastrzebska-Wiesek, Magdalena; Partyka, Anna; Wilczyńska, Daria; Pytka, Karolina; Latacz, Gniewomir; Przejczowska-Pomierny, Katarzyna; Wyska, Elżbieta; Wesołowska, Anna; Pawłowski, Maciej; Newman-Tancredi, Adrian; Kolaczkowski, Marcin (8 October 2020). "Discovery of Novel pERK1/2- or β-Arrestin-Preferring 5-HT 1A Receptor-Biased Agonists: Diversified Therapeutic-like versus Side Effect Profile". Journal of Medicinal Chemistry. 63 (19): 10946–10971. doi:10.1021/acs.jmedchem.0c00814. PMC 7586344. PMID 32883072.
- ^ Sniecikowska, Joanna; Newman-Tancredi, Adrian; Kolaczkowski, Marcin (10 December 2019). "From Receptor Selectivity to Functional Selectivity: The Rise of Biased Agonism in 5-HT1A Receptor Drug Discovery". Current Topics in Medicinal Chemistry. 19 (26): 2393–2420. doi:10.2174/1568026619666190911122040. PMID 31544717. S2CID 202731822.
- ^ Sniecikowska, Joanna; Gluch-Lutwin, Monika; Bucki, Adam; Więckowska, Anna; Siwek, Agata; Jastrzebska-Wiesek, Magdalena; Partyka, Anna; Wilczyńska, Daria; Pytka, Karolina; Pociecha, Krzysztof; Cios, Agnieszka; Wyska, Elżbieta; Wesołowska, Anna; Pawłowski, Maciej; Varney, Mark A. (2019-03-14). "Novel Aryloxyethyl Derivatives of 1-(1-Benzoylpiperidin-4-yl)methanamine as the Extracellular Regulated Kinases 1/2 (ERK1/2) Phosphorylation-Preferring Serotonin 5-HT1A Receptor-Biased Agonists with Robust Antidepressant-like Activity". Journal of Medicinal Chemistry. 62 (5): 2750–2771. doi:10.1021/acs.jmedchem.9b00062. ISSN 1520-4804. PMID 30721053.
- ^ Głuch-Lutwin, Monika; Sałaciak, Kinga; Pytka, Karolina; Gawalska, Alicja; Jamrozik, Marek; Śniecikowska, Joanna; Kołaczkowski, Marcin; Depoortère, Ronan Y.; Newman-Tancredi, Adrian (2023-02-13). "The 5-HT1A receptor biased agonist, NLX-204, shows rapid-acting antidepressant-like properties and neurochemical changes in two mouse models of depression". Behavioural Brain Research. 438: 114207. doi:10.1016/j.bbr.2022.114207. ISSN 1872-7549. PMID 36368443.