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This is a safety, tolerability, pharmacokinetic and efficacy study in subjects with Parkinson's disease
This study is will be conducting to determine if Radotinib is safe and can be tolerated by patients with Parkinson's disease (PD) and to learn if Radotinib can be potential therapeutic agents for the treatment of PD.
Radotinib has been approved by Ministry of Food & Drug Safety of Korea to treat Chronic Myeloid Leukemia (CML) but it has not been approved for PD.
In nonclinical efficacy study, therapeutic effect of Radotinib HCl, c-Abl inhibitor, which exhibits improved pharmacokinetic properties and BBB penetration compared to nilotinib and other c-Abl inhibitors, was tested in a preclinical α-synuclein preformed fibrils (PFF) model of sporadic PD. As a result, the treatment of Radotinib HCl protects the α-synuclein PFFs-induced neuronal toxicity, reduces the PFFs-induced LB/LN-like pathology, and inhibits the PFFs-induced c-Abl activation in neurons. In vivo studies demonstrate that administration of Radotinib HCl prevents dopamine neuron loss and behavioral deficits following α-synuclein PFFs-induced toxicity. Taken together, these findings indicate that Radotinib HCl has beneficial neuroprotective effects in PD and provides strong evidence that selective and brain permeable c-Abl inhibitors can be potential therapeutic agents for the treatment of PD.
These data are very compelling to evaluate the effects of Radotinib in a phase II, randomized, double-blind, placebo-controlled trial in patients with PD.
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| Label | Type | Description | Intervention Names |
|---|---|---|---|
| Placebo: Dose escalation | Placebo Comparator | Forty (40) subject will be recruited and randomized into 4 dosing groups. In each dosing group, ten (10) will be randomized and 8 of 10 will receive the active product (Radotinib) and 2 subjects will receive the matching placebo orally once daily for 6 months at each escalating dose level. |
|
| Radotinib HCl: Dose escalation | Experimental | Forty (40) subject will be recruited and randomized into 4 dosing groups. In each dosing group, ten (10) will be randomized and 8 of 10 will receive the active product (Radotinib) and 2 subjects will receive the matching placebo orally once daily for 6 months at each escalating dose level. The inclusion of subjects in the next dose level will be decided by the sponsor in consultation with a Data Monitoring Committee (DMC). |
|
| Name | Type | Description | Arm Group Labels | Other Names |
|---|---|---|---|---|
| Radotinib HCl 50 mg | Drug | Enrolled subject will continue to administer Radotinib 50mg/day, 100mg/day, 150mg/day, 200mg/day, depending on the dose level once daily for 6 months. |
|
| Measure | Description | Time Frame |
|---|---|---|
| Evaluation of safety parameters: Adverse Events | Incidence and severity of treatment emergent AEs | 12 months after dose administration |
| Measure | Description | Time Frame |
|---|---|---|
| Pharmacokinetics assessments of Radotinib HCl: Cmax | The maximum (peak) observed drug concentration after dose administration | 14 days after dose administration |
| Pharmacokinetics assessments of Radotinib HCl: Tmax |
| Measure | Description | Time Frame |
|---|---|---|
| Brain DaT SPECT to measure dopamine neurons and nerve terminals | DaTscan is a specific type of single-photon emission computed tomography (SPECT) imaging technique that helps visualize dopamine transporter in the brain | 12 months |
| Concentration of α-synuclein in CSF |
Inclusion Criteria:
Exclusion Criteria:
Atypical Parkinsonism or drug-induced Parkinsonism;
Current, or within 60 days of screening, use of any prescription, investigational, or over the counter medication for the symptomatic treatment of PD or to slow the progression of PD.
Prior use of dopaminergic therapy (e.g., levodopa, dopamine agonist, amantadine, rasagiline) for 30 or more days any time in the past;
Cognitive impairment (MMSE ≤ 24);
Active psychiatric disorder (mood disorders, hallucinations or delirium with strong functional impact and not controlled by medication or which happened during the last 3 months before inclusion);
Severe or uncontrolled chronic disease;
Significant medical history of congenital or acquired bleeding disorders;
Treatment by Deep Brain Stimulation or continuous infusion of apomorphin/dopa gel;
Any below impaired cardiac function:
Participation in other investigational drug trials within 30 days prior to Screening;
Any concomitant medication or medication excluded that could put subject at risk, or interfere with study evaluations;
Subjects currently receiving treatment with a strong CYP3A4 inhibitors (e.g. erythromycin, ketoconazole, itraconazole, voriconazole, clarithromycin, telithromycin, ritonavir, mibefradil) or strong CYP3A4 inducers (e.g. dexamethasone, phenytoin, carbamazepine, rifampin, rifabutin, rifapentine, phenobarbitol, St. John's Wort) or therapeutic Cumarin derivatives (e.g. warfarin, acenocoumarol, phenprocoumon) and that can neither stop the administration of these drugs before the start of the IP administration nor switch to other drugs
Subjects who are currently receiving treatment with a medication that has the potential to extend QT intervals and can neither stop the administration of the drugs before the start of the IP administration nor switch to other drugs (list of medications that have the potential to prolong QT interval is provided in the Appendix II) If subjects need to start such drug treatments during the study, this will be discussed with the sponsor, IL-YANG PHARM. Co., Ltd.
Subjects who are currently receiving treatment with P-gp inducers (e.g. (Ritonavir, Saquinavir, Nelfinavir, Indinavir, Amprenavir, Tipranavir…), Apalutamide, Estrone, Estriol, Trazodone, Vincristine, Tamoxifen, Doxorubicin, Carbamazepine, Oxcarbazepine, Fosphenytoin, Lorlatinib, Phenobarbital, Phenytoin, Propofol, beclomethasone, Dexamethasone, Prednisone, Hydrocortisone, Diclofenac, Rifampicin, Reserpine, Nifedipine, Digoxine, Amiodarone, Spironolactone, Levothyroxine, Tacrolimus, Sirolimus, St. John's Wort (herbal ingredient)) and that can neither stop the administration of these drugs before the start of the IP administration nor switch to other drugs;
Gastrointestinal disorder or gastrointestinal disease that may result in a significant change in the absorption of the investigational product;
Medical history of acute or chronic pancreatitis within the past one year;
Acute or chronic liver, pancreas, or severe kidney disease that are not associated with the disease;
Subjects known seropositive to human immunodeficiency virus (HIV), current acute or chronic hepatitis B (hepatitis B surface-antigen positive), hepatitis C, or cirrhosis. Inactive hepatitis B surface antigen (HBsAg) carriers, treated and stable hepatitis B (HBV DNA < 500 IU/mL or site specific local lab normal range lower limit assessed by investigator), and cured hepatitis C subjects can be enrolled;
Men subjects who are unwilling to use and appropriate method of contraception during the study;
Subjects who have hypersensitivity to active ingredient or any of the excipients of this investigational product;
Any medical condition that might interfere with the protocol except those defined in Section 5.3 of the study protocol;
Subject unable to attend scheduled visits or to comply to the protocol;
Subject under legal guardianship or judicial protection;
Subject in the exclusion period of another protocol;
No possibility of contact in case of emergency.
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| Name | Role | Phone | Extension | |
|---|---|---|---|---|
| IL-YANG CR | Contact | +82.70.7165.7316 | nykim@ilyanga.co.kr |
| Name | Affiliation | Role |
|---|---|---|
| Philippe DAMIER, Pr. | CHU Nantes - Hôpital Nord Guillaume et René Laennec | Principal Investigator |
| Facility | Status | City | State | ZIP | Country | Contacts |
|---|---|---|---|---|---|---|
| CHRU de Lille - Hôpital Roger Salengro | Not yet recruiting | Lille | France |
| PubMed Identifier | Type | Citation | Retractions |
|---|---|---|---|
| 40680102 | Derived | Joshi D, Kulkarni M, Parekh P, Shah S, Greig NH, Acharya S. Targeting protein kinases in Parkinson's disease: the emerging role of phytoconstituents. Nutr Neurosci. 2025 Dec;28(12):1532-1563. doi: 10.1080/1028415X.2025.2531356. Epub 2025 Jul 18. |
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| ID | Term |
|---|---|
| D010300 | Parkinson Disease |
| ID | Term |
|---|---|
| D020734 | Parkinsonian Disorders |
| D001480 | Basal Ganglia Diseases |
| D001927 | Brain Diseases |
| D002493 | Central Nervous System Diseases |
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| ID | Term |
|---|---|
| C000606751 | 4-methyl-N-(3-(4-methylimidazol-1-yl)-5-trifluoromethylphenyl)-3-(4-pyrazin-2-ylpyrimidin-2-ylamino)benzamide |
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|
| Placebo | Drug | Placebo |
|
The time to reach maximum (peak) drug concentration after dose administration
| 14 days after dose administration |
| Pharmacokinetics assessments of Radotinib HCl: Ctrough | Trough plasma concentration (measured concentration at the end of a dosing interval at steady state) | 14 days after dose administration |
| Pharmacokinetics assessments of Radotinib HCl: AUCt | Area under the plasma concentration-time curve from time zero to time t | 14 days after dose administration |
| Pharmacokinetics assessments of Radotinib HCl: AUCinf | Area under plasma concentration-time curve from time 0 to infinity | 14 days after dose administration |
| Pharmacokinetics assessments of Radotinib HCl: AUC0-12h | Area under the plasma concentration-time curve over the last 24-h dosing interval | 14 days after dose administration |
| Pharmacokinetics assessments of Radotinib HCl: t1/2 | Elimination half-life of Radotinib after dose administration | 14 days after dose administration |
| Pharmacokinetics assessments of Radotinib HCl: Vd/F | Apparent volume of distribution after non-intravenous administration | 14 days after dose administration |
| Pharmacokinetics assessments of Radotinib HCl: CL/F | Apparent total clearance of the drug from plasma after oral administration | 14 days after dose administration |
| Change from Baseline in the sum of MDS-UPDRS Parts I, II and III | The Movement Disorders Society Unified Parkinson's Disease Rating Scale (MDS-UPDRS) is a clinimetric assessment of subjective and objective symptoms and signs of Parkinson's disease created by the Movement Disorder Society. The MDS-UPDRS has four parts: Part I (non-motor experiences of daily living), Part II (motor experiences of daily living, Part III (motor examination) and Part IV (motor complications). Only Parts I, II and III will be completed in this study. MDS-UPDRS retains the four-scale structure with a reorganization of the various subscales. The subscale has a 0-4 rating, where 0 = normal, 1 = slight, 2 = mild, 3 = moderate, and 4 = severe. Higher MDS-UPDRS scores reflect worse tremor/motor function. Larger differences will infer greater effect size for the intervention. Score drops over time imply improvement in tremor/motor function. | 6 months |
| Time from baseline to initiation of dopamine-replacement medication. | Time from baseline to initiation of dopamine replacement therapy following randomization | 6 months |
| Change in health related quality of life as measured by a quality of life questionnaire (PDQ-39) | The Parkinson's Disease Questionnaire (PDQ-39) is a 39-item quality of life questionnaire for patients with Parkinson's Disease (PD) that evaluates the 8 dimensions of mobility, activities of daily living, emotional well-being, stigma, social support, cognition, and communication. The PDQ-39 Single Index (SI) score is the weighted addition of scores on all 8 dimension and ranges from 0 (no disease impact) to 100 (severe disease impact). | 12 months |
| Subject's clinical global impression of change. | The CGI Scale of Global Clinical Impressions (see Appendix VI) allows an overall assessment of the subject's condition. The CGI addresses the majority of mental disorders. In its first item, rated from 1 to 7 (the rating 1 corresponding to the normal state), it allows a good overall measurement of the subject's condition. The 2nd item proposes to the Investigator to evaluate the overall improvement of the subject compared to his/her condition at the admission to the research. As before, this item has 7 quantified degrees (from 1 = "very strongly improved" to 7 = "very strongly aggravated"). | 12 months |
Quantification of α-synuclein concentration in CSF |
| 6 months |
| Concentration of Tau and phospho-Tau (p-181) in CSF | Quantification of Tau and phospho-Tau (p-181) concentration in CSF | 6 months |
| Concentration of β-amyloid peptide 1-42 in CSF | Quantification of β-amyloid peptide 1-42 concentration in CSF | 6 months |
| Concentration of NF-L in the serum | Quantification of NF-L concentration in CSF | 6 months |
| Concentration of Radotinib HCl in the CSF and plasma | Quantification of Radotinib HCl concentration in CSF | 6 months |
| CHU Limoges | Recruiting | Limoges | France |
|
| CHU de Lyon HCL | Recruiting | Lyon | France |
|
| Hôpital Nantes-Hotel Dieu | Recruiting | Nantes | France |
|
| Hôpital Pitié-Salpêtrière | Recruiting | Paris | France |
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| Chu La Miletrie | Recruiting | Poitiers | France |
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| CHU de Rouen | Recruiting | Rouen | France |
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| D009422 | Nervous System Diseases |
| D009069 | Movement Disorders |
| D000080874 | Synucleinopathies |
| D019636 | Neurodegenerative Diseases |