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Antisense Oligonucleotide
Antisense Oligonucleotide for Progressive Supranuclear Palsy
Phase 1
Waitlist Available
Research Sponsored by Novartis Pharmaceuticals
Eligibility Criteria Checklist
Specific guidelines that determine who can or cannot participate in a clinical trial Must have
If the participant is receiving levodopa/carbidopa, levodopa/benserazide, a dopamine agonist, catechol-o-methyltransferase (COMT) inhibitor, rasagiline, CoQ10 or other Parkinson's medications, acetylcholinesterase inhibitors, antipsychotics, memantine, or other non-tau modifying Alzheimer's medication the dose must have been stable for at least 30 days prior to the screening visit and must remain stable for the duration of the study. No such medication can be initiated during the study.
Vertical supranuclear gaze palsy, or reduced velocity of vertical saccade
Must not have
Evidence of motor neuron disease, or any other neurological disease that could explain symptoms
History of post-lumbar-puncture headache of moderate or severe intensity and/or blood patch
Timeline
Screening 3 weeks
Treatment Varies
Follow Up baseline up to approximately 1 year (3-month treatment plus 9-month follow-up or 9-month treatment plus 3-month follow-up)
Summary
This trial tests a new drug, NIO752, for people with progressive supranuclear palsy (PSP). The drug is injected into the spinal fluid to help it reach the brain. The goal is to find out if NIO752 can better manage PSP symptoms.
Who is the study for?
This trial is for adults aged 40-75 with Progressive Supranuclear Palsy (PSP) diagnosed within the last 5 years, able to walk independently or with minimal assistance. Participants must have a history of postural instability or falls and score below certain thresholds on PSP and cognitive scales. They need a reliable study partner and can't be in nursing care, recently hospitalized, or show significant benefit from levodopa.
What is being tested?
The trial tests multiple doses of NIO752, an antisense oligonucleotide against placebo in people with PSP. It's double-blind meaning neither participants nor researchers know who gets the real treatment versus placebo. The goal is to assess safety, tolerability, and how the body processes the drug.
What are the potential side effects?
Potential side effects are not detailed here but may include reactions related to lumbar puncture procedures such as headache or back pain; other risks could involve typical drug-related adverse events like nausea, fatigue, allergic reactions but specifics will depend on further study results.
Eligibility Criteria
Inclusion Criteria
You may be eligible if you check “Yes” for the criteria belowSelect...
My Parkinson's or Alzheimer's medication dose has been stable for at least 30 days.
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I have difficulty moving my eyes up or down quickly.
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I can safely have lumbar punctures and blood tests.
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I was diagnosed with PSP less than 5 years ago, my condition is likely PSP Richardson syndrome, and my health scores are within a specific range.
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I have had balance problems or falls for at least a year within the first three years of my disease.
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I was diagnosed with PSP less than 5 years ago, have probable PSP Richardson syndrome, a PSPRS score under 40, and a MOCA score over 17.
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I can have spinal taps and blood tests.
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I can walk on my own or with little help.
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I am between 40 and 75 years old.
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I have difficulty moving my eyes up or down quickly.
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I can walk on my own or with little help.
Exclusion Criteria
You may be eligible for the trial if you check “No” for criteria below:Select...
I have a diagnosed neurological condition that could explain my symptoms.
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I've had severe headaches or needed a blood patch after a lumbar puncture.
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I have not been hospitalized for a major procedure under general anesthesia in the last 12 weeks and have no such plans during the study.
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I have seen significant improvement with levodopa treatment.
Timeline
Screening ~ 3 weeks3 visits
Treatment ~ Varies
Follow Up ~ baseline up to approximately 1 year (3-month treatment plus 9-month follow-up or 9-month treatment plus 3-month follow-up)
Screening ~ 3 weeks
Treatment ~ Varies
Follow Up ~baseline up to approximately 1 year (3-month treatment plus 9-month follow-up or 9-month treatment plus 3-month follow-up)
Treatment Details
Study Objectives
Study objectives can provide a clearer picture of what you can expect from a treatment.Primary study objectives
Change in severity scores for Columbia-Suicide Severity Rating Scale (C-SSRS)
Levels of infection indicators in Cerebrospinal fluid (CSF)
Number of adverse events and serious adverse events
Secondary study objectives
AUCinf in blood plasma
Plasma
Cmax, Ctrough in blood plasma
+3 moreTrial Design
6Treatment groups
Experimental Treatment
Placebo Group
Group I: Cohort E NIO752Experimental Treatment1 Intervention
4 injections of NIO752 at dose E
Group II: Cohort D NIO752Experimental Treatment1 Intervention
4 injections of NIO752 at dose D
Group III: Cohort C NIO752Experimental Treatment1 Intervention
4 injections of NIO752 at dose C
Group IV: Cohort B NIO752Experimental Treatment1 Intervention
4 injections of NIO752 at dose B
Group V: Cohort A NIO752Experimental Treatment1 Intervention
4 injections of NIO752 at dose A
Group VI: PlaceboPlacebo Group1 Intervention
4 injections of placebo
Research Highlights
Information in this section is not a recommendation. We encourage patients to speak with their healthcare team when evaluating any treatment decision.Mechanism Of Action
Side Effect Profile
Prior Approvals
Other Research
The most common treatments for Progressive Supranuclear Palsy (PSP) include medications like levodopa, amantadine, and investigational drugs such as NIO752. Levodopa works by replenishing dopamine levels in the brain, which can help improve motor symptoms.
Amantadine acts as an NMDA receptor antagonist, which may help reduce motor symptoms and dyskinesias. NIO752, an investigational drug, is being studied for its potential to modify disease progression or alleviate symptoms by targeting specific pathways involved in PSP.
These treatments are crucial for PSP patients as they aim to manage symptoms, improve quality of life, and potentially slow disease progression.
Memantine exerts neuroprotective effects by modulating α-synuclein transmission in a parkinsonian model.Structural and functional evidence for citicoline binding and modulation of 20S proteasome activity: Novel insights into its pro-proteostatic effect.Alpha7 nicotinic receptors as therapeutic targets for Parkinson's disease.
Memantine exerts neuroprotective effects by modulating α-synuclein transmission in a parkinsonian model.Structural and functional evidence for citicoline binding and modulation of 20S proteasome activity: Novel insights into its pro-proteostatic effect.Alpha7 nicotinic receptors as therapeutic targets for Parkinson's disease.
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Who is running the clinical trial?
Novartis PharmaceuticalsLead Sponsor
2,905 Previous Clinical Trials
4,208,056 Total Patients Enrolled
Media Library
Eligibility Criteria:
This trial includes the following eligibility criteria:- I have a diagnosed neurological condition that could explain my symptoms.My Parkinson's or Alzheimer's medication dose has been stable for at least 30 days.You have recently shown signs of wanting to harm yourself or others, have had a major episode of feeling very sad, confused, or violent.You live in a nursing home or a place for people with memory problems.I have difficulty moving my eyes up or down quickly.I can safely have lumbar punctures and blood tests.I've had severe headaches or needed a blood patch after a lumbar puncture.I have not been hospitalized for a major procedure under general anesthesia in the last 12 weeks and have no such plans during the study.You cannot have an MRI or have medical reasons that make MRI unsafe for you.You have a significant abnormality in your lab test results.I was diagnosed with PSP less than 5 years ago, my condition is likely PSP Richardson syndrome, and my health scores are within a specific range.I have had balance problems or falls for at least a year within the first three years of my disease.I have not taken any drugs for PSP or experimental therapy recently.I was diagnosed with PSP less than 5 years ago, have probable PSP Richardson syndrome, a PSPRS score under 40, and a MOCA score over 17.My medication doses have been stable for the last 30 days and will remain so.I have someone over 18 who can come with me to my study visits and knows about my health condition.I can have spinal taps and blood tests.I have seen significant improvement with levodopa treatment.I am at high risk for meningitis but am on preventive treatment.You have other important brain abnormalities found in your medical history or during the screening process.I can walk on my own or with little help.I am between 40 and 75 years old.I have difficulty moving my eyes up or down quickly.I can walk on my own or with little help.
Research Study Groups:
This trial has the following groups:- Group 1: Placebo
- Group 2: Cohort A NIO752
- Group 3: Cohort C NIO752
- Group 4: Cohort D NIO752
- Group 5: Cohort E NIO752
- Group 6: Cohort B NIO752
Awards:
This trial has 0 awards, including:Timeline:
This trial has the following timeline:- Screening: It may take up to 3 Weeks to process to see if you qualify in this trial.
- Treatment: The duration you will receive the treatment varies.
- Follow Ups: You may be asked to continue sharing information regarding the trial for 6 Months after you stop receiving the treatment.
PSP Patient Testimony for trial: Trial Name: NCT04539041 — Phase 1
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