Effect of IVIG on Cerebral and Retinal Amyloid in Mild Cognitive Impairment Due to Alzheimer Disease
Status: | Enrolling by invitation |
---|---|
Conditions: | Alzheimer Disease, Cognitive Studies, Cognitive Studies |
Therapuetic Areas: | Neurology, Psychiatry / Psychology |
Healthy: | No |
Age Range: | 50 - 84 |
Updated: | 5/9/2018 |
Start Date: | January 4, 2018 |
End Date: | May 2019 |
Proof of Concept of the Effect of Intravenous Immunoglobulin on Cerebral and Retinal Amyloid in Mild Cognitive Impairment Due to Alzheimer Disease
This is a proof of concept study to determine if changes in brain amyloid levels are evident
three months after infusion of 0.4 g/kg of IVIG every 14 days x 5 infusions. Amyloid levels
will be measured by Florbetapir PET and retinal scan.
three months after infusion of 0.4 g/kg of IVIG every 14 days x 5 infusions. Amyloid levels
will be measured by Florbetapir PET and retinal scan.
Study design:
This is a single center, open label, proof of concept, out-patient study. Subjects will
undergo Florbetapir PET and have retinal amyloid levels measured, receive an infusion of IVIG
at 0.4 g/kg every 14 days for a total of five infusions, and repeat PET and retinal amyloid
measures three months after the first infusion.
Subject population:
The study population will consist of male and female subjects diagnosed with mild cognitive
impairment (MCI) due to Alzheimer disease (AD).
Estimated study duration:
The duration of each study subject is approximately 4 months, including one screening visit
over a period of approximately 28 days, 5 days of infusions over a 2-month period of time,
and a follow-up visit at 3 months after the first infusion.
Description of study drug:
Octagam is an FDA approved 10% human normal immunoglobulin solution ready for intravenous
administration.
Study drug dosage:
The dose level of IVIG at 0.4 g/kg will be administered by IV infusion once every 14 days for
two months.
Concomitant therapy:
Concomitant medications will be assessed at all study visits. Concomitant medications are
prescribed or over-the-counter medications and should be consistent with the
inclusion/exclusion criteria. Concomitant medication appropriate to the subject's condition
may be prescribed during the course of the study with the exception of those listed above.
Routine vaccinations (i.e., flu vaccination) with commercially available therapeutics are
permitted but must not be given within four weeks before or after the administration of the
study drug.
Evaluations by visit:
Screening procedures at visit 1 will take place up to 28 days prior to Visit 2 (Day 1)
dosing. Screening labs and assessments will be performed during the screening period. The
first dose of study drug is administered on Day 1. Visits 2 through 6 have a ±1 day window
and occur every 14 days over two months. The investigator will determine if a subject is
suitable to continue following a missed infusion. Visit 7 has a ±7 day window.
All study screening data from Visit 1 including laboratory results must be reviewed for study
eligibility prior to receiving first dose of study drug. Prior to infusion, a review of
concomitant medications and AEs takes place. If the subject continues to be eligible for
enrollment, the subject will be infused with study medication and will remain in the infusion
clinic for at least 1 hour following the infusion for safety assessments on Visit 2 (Day 1),
and 15 minutes for the subsequent visits.
This is a single center, open label, proof of concept, out-patient study. Subjects will
undergo Florbetapir PET and have retinal amyloid levels measured, receive an infusion of IVIG
at 0.4 g/kg every 14 days for a total of five infusions, and repeat PET and retinal amyloid
measures three months after the first infusion.
Subject population:
The study population will consist of male and female subjects diagnosed with mild cognitive
impairment (MCI) due to Alzheimer disease (AD).
Estimated study duration:
The duration of each study subject is approximately 4 months, including one screening visit
over a period of approximately 28 days, 5 days of infusions over a 2-month period of time,
and a follow-up visit at 3 months after the first infusion.
Description of study drug:
Octagam is an FDA approved 10% human normal immunoglobulin solution ready for intravenous
administration.
Study drug dosage:
The dose level of IVIG at 0.4 g/kg will be administered by IV infusion once every 14 days for
two months.
Concomitant therapy:
Concomitant medications will be assessed at all study visits. Concomitant medications are
prescribed or over-the-counter medications and should be consistent with the
inclusion/exclusion criteria. Concomitant medication appropriate to the subject's condition
may be prescribed during the course of the study with the exception of those listed above.
Routine vaccinations (i.e., flu vaccination) with commercially available therapeutics are
permitted but must not be given within four weeks before or after the administration of the
study drug.
Evaluations by visit:
Screening procedures at visit 1 will take place up to 28 days prior to Visit 2 (Day 1)
dosing. Screening labs and assessments will be performed during the screening period. The
first dose of study drug is administered on Day 1. Visits 2 through 6 have a ±1 day window
and occur every 14 days over two months. The investigator will determine if a subject is
suitable to continue following a missed infusion. Visit 7 has a ±7 day window.
All study screening data from Visit 1 including laboratory results must be reviewed for study
eligibility prior to receiving first dose of study drug. Prior to infusion, a review of
concomitant medications and AEs takes place. If the subject continues to be eligible for
enrollment, the subject will be infused with study medication and will remain in the infusion
clinic for at least 1 hour following the infusion for safety assessments on Visit 2 (Day 1),
and 15 minutes for the subsequent visits.
Inclusion Criteria:
1. Age 50 to <85 years.
2. Evidence of amyloid pathology on Florbetapir PET at screening.
3. Diagnosis of MCI due to AD based on NIA-AA criteria. (APPENDIX A)
4. MRI brain (with past 24 months) which shows evidence of mild hippocampal atrophy
and/or bilateral parietal atrophy.
5. CDR score of 0.5
6. Mini-Mental State Examination (MMSE) score of 24-30, inclusive.
7. Rosen Modified Hachinski Ischemic score ≤4.
8. Receiving stable doses of medication(s) for the treatment of non-excluded medical
condition(s) for at least 30 days prior to screening. Cholinesterase inhibitors and
memantine are allowed if doses have stable been least 30 days prior to screening.
9. Agree to refrain from participating in any treatment or clinical trial targeting
amyloid for the duration of the study.
10. Agree to refrain from taking any herbal supplement considered to enhance cognition
unless approved by the investigator for the duration of the study.
11. Ability to attend all clinical visits and have an informant capable of accompanying
the subject on specific clinic visits.
12. The subject's collaborative informant (support person) must be someone who has known
the subject for at least 4 years and has had approximately 2 or more separate
communications with the study participant per month (at least one of these
communications in person).
13. Fluency in English and evidence of adequate premorbid intellectual functioning.
14. Adequate manual dexterity, visual, and auditory abilities to perform all aspects of
the cognitive and functional assessments.
15. Venous access suitable for repeated infusions and phlebotomy.
16. In the opinion of the investigator, the subject and informant will be compliant and
have a high probability of completing the study, including all scheduled evaluations
and required tests.
Exclusion Criteria:
1. Has significant neurological disease other than MCI that in the opinion of the
investigator may affect cognition.
2. History of clinically evident stroke or history of clinically significant carotid or
vertebrobasilar stenosis or plaque.
3. History of seizures, excluding febrile seizures in childhood.
4. History of screening visit brain MRI scan indicative of any other significant
abnormality, including but not limited to multiple microhemorrhages (2 or more),
history or evidence of a single prior hemorrhage > 1 cm3, multiple lacunar infarcts (2
or more) or evidence of a single prior infarct > 1 cm3, evidence of a cerebral
contusion, encephalomalacia, aneurysms, vascular malformations, subdural hematoma, or
space occupying lesions of significance as determined by the PI (e.g., arachnoid cysts
or brain tumors such as meningioma).
5. Brain MRI shows moderate or severe cortical or hippocampal atrophy.
6. Sensitivity to Florbetapir.
7. Other present/planned ionized radiation that, in combination with planned exposure to
PET ligands for this study, would result in cumulative exposure that would exceed
recommended limits.
8. Ophthalmologic condition that would interfere with retinal amyloid imaging.
9. Current presence of a clinically significant major psychiatric disorder (e.g., Major
Depressive Disorder) according to the criteria of the Diagnostic and Statistical
Manual of Mental Disorders, Fourth Edition (DSM-IV-TR) or symptom (e.g.,
hallucinations) that in the opinion of the investigator could affect the subject's
ability to complete the study.
10. Current clinically significant systemic illness that is likely to result in
deterioration of the subject's condition or affect the subject's safety during the
study including but not limited to renal failure or myocardial infarction.
11. History of cancer within the last 5 years, with the exception of nonmetastatic basal
cell carcinoma, and squamous cell carcinoma of the skin.
12. Uncontrolled hypertension (diastolic BP> 100 mmHg or systolic BP> 160 mmHg, sitting).
13. History or evidence of any clinically significant autoimmune disease or disorder of
the immune system (e.g., Crohn's Disease, Rheumatoid Arthritis)
14. Clinically significant infection within the last 30 days (e.g., chronic persistent or
acute infection (eg, upper respiratory infection [URI], urinary tract infection
[UTI]).
15. Female subjects of childbearing potential.
16. Other clinically significant abnormality on physical, neurological, laboratory, vital
signs or ECG examination (e.g., atrial fibrillation) that could compromise the study
or be detrimental to the subject.
17. Weight greater than 120 kg (264 lbs).
18. Excessive smoking defined as more than 20 cigarettes per day.
19. History of alcohol or drug dependence or abuse as defined by DSM-IV criteria within
the last 2 years.
20. Severe liver or kidney disease verified by the PI review of ALT, AST and creatinine.
21. Known coagulopathy, thrombosis, or low platelet count.
22. Hemoglobin less than 11 g/dL.
23. Known deficiency to IgA.
24. Positive serology for Hepatitis B or C, or HIV.
25. History of anti-amyloid treatment, immunotherapy, or other experimental treatment for
MCI or Alzheimer disease.
26. Concurrent use of anticholinergic drugs including diphenhydramine.
27. Current use of anticoagulant medications (except the use of aspirin 325 mg/day or
less, plavix, aggrenox, and persantine but not for stroke).
28. Concurrent use of opioid pain relievers and related synthetic derivatives.
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