Study Purpose:Washington University in St. Louis is seeking participants with ALS for a study to determine the half-life of the protein SOD1 in the cerebral spinal fluid. Mutations in the SOD1 gene are known to cause some forms of familial ALS. Researchers are developing a treatment to reduce the level of SOD1 in familial ALS, but need to know more about how long SOD1 stays in the body ("half-life") to help determine if the new treatment is effective.
Amyotrophic Lateral Sclerosis, Familial , Amyotrophic Lateral Sclerosis, Sporadic
Type of Intervention:
Study Chair(s)/Principal Investigator(s):
Coordinating Center Contact Information
Washington University in St. Louis
St. Louis, Missouri, 63110 United States
Full Study Summary:
The Investigator's previous data suggest that SOD1 in the cerebral spinal fluid (CSF) will be an excellent pharmacodynamics marker for an SOD1-focused therapeutic approach. However, one of the central missing components in understanding SOD1 as a marker is SOD1 CSF half-life data. The half-life of this protein will aid in clinical trial planning since half-life influences the amount of SOD1 protein reduction by ASO and thus dictates the optimal timing of drug administration and CSF collection for pharmacodynamics measures.
- Enroll a total of 86 ALS participants
- Determine the kinetics for total SOD1 protein, as well as the wild type and mutant protein separately
- Determine this in patients with known SOD1 mutation as well as sporadic ALS patients Eligibility
- Adults over age 18
- fALS with confirmed genetic testing showing a mutation in the SOD1 gene; asymptomatic SOD1 gene carriers and sporadic ALS patients.
Measures: The key outcome of this study is to determine the half-life of the SOD1 protein in symptomatic and asymptomatic ALS patients which will provide critical information to inform future therapeutic studies in ALS. For ALS patients, The Investigators will also perform Slow Vital Capacity testing and the ALSFRS-R at the screening visit and at each lumbar puncture visit.
Measures: Participants will have up to 7 in-person visits over 4 months. The study involves labeling or marking SOD1 with a special type of leucine. Leucine is an essential amino acid that is found in the foods we eat. This method involves an overnight stay for a 16 hour intravenous infusion of labeled leucine along with a collection blood and urine followed by 5 lumbar punctures scheduled over the period of 4 months.
At each subsequent visit, subjects will undergo a blood draw, urine collection, lumbar puncture, a questionnaire (ALS Functional Rating Scale) which measures motor function, and a breathing test to determine Slow Vital Capacity (SVC) measurements.
Analysis: In addition to determining the half-life of the SOD1 protein in ALS patients, the Investigators will also analyze the kinetics of wild type SOD1 protein separately from mutant SOD1 protein to determine differences in half life. The Investigators will also compare CSF Tau half-life between ALS patients and controls as a disease specificity control. The Investigators hope to correlate this data with clinical measures which may reveal other important hypotheses regarding SOD1 kinetic rates and disease manifestations.
Washington University School of Medicine
1 overnight stay for leucine infusion. 4-5 lumbar punctures performed over a period of 3-4 months at Washington University. Each lumbar puncture visit takes approximately three hours.
Estimated Study Start Date:
12 / 01 / 2012
Estimated Study Completion Date:
12 / 01 / 2024
Posting Last Modified Date:
04 / 24 / 2023
Date Study Added to neals.org:
02 / 28 / 2018
Can participants use Riluzole?
YesInclusion Criteria (with exceptions for each group):
- Males or females of any race aged 18 or older
- Positive for SOD1 mutation (SOD1 ALS only)
- Diagnosed with Definite, Probable or Possible ALS in accordance with El Escorial criteria (ALS and SOD1 Positive ALS only)
- Able to hold position and breathe comfortably for the duration of the LP procedure as determined by the LP physician or Nurse Practitioner
- Subjects must be able to provide informed consent
Exclusion Criteria for all groups:
- Invasive ventilator dependence, such as tracheostomy
- Medically unable to undergo lumbar puncture (LP) as determined by the investigator (i.e.,bleeding disorder, allergy to local anesthetics, a skin infection at or near the LP site, or evidence of high intracranial pressure).
- Any active dermatologic disease.
- Any connective tissue disease including systemic lupus erythematous, Sjögren's syndrome, scleroderma or mixed connective tissue disease.
- Any known or suspected abnormal CSF pressure or intracranial/intraspinal tumors.
- Use of anticoagulant medication (eg. warfarin, dalteparin, enoxaparin, rivaroxaban, fondaparinux, dabigatran) that cannot be safely withheld until coagulation parameters have normalized prior to lumbar puncture and for up to a week following the lumbar puncture.
- Blood dyscrasia, abnormal bleeding diathesis, or the use of dialysis for renal failure.
- Clinical judgment of the Site Investigator that the subject would be unable to undergo multiple lumbar punctures.
- Safety lab values greater than 2X the upper limit of normal
- Allergy to Lidocaine
- Any contraindication for lumbar puncture
Washington University in St. Louis
Saint Louis, Missouri