Investigating Mechanism of Action of DAC HYP in the Treatment of High-Inflammatory Multiple Sclerosis (MS)
Status: | Completed |
---|---|
Conditions: | Neurology, Multiple Sclerosis |
Therapuetic Areas: | Neurology, Other |
Healthy: | No |
Age Range: | 18 - 60 |
Updated: | 10/13/2018 |
Start Date: | May 13, 2010 |
End Date: | August 11, 2017 |
Objective:
The primary goal of this study is to investigate the mechanism of action (MOA) of
CD25-blocking therapies in high inflammatory multiple sclerosis (HI-MS). The secondary goal
of this study is to assess long-term safety and efficacy of CD25-blocking therapies in HI-MS.
Study population:
Two cohorts of patients will be enrolled:
- Long-term daclizumab therapy cohort: Up to 15 daclizumab-treated patients with
relapsing-remitting (RR-MS) or secondary-progressive MS (SP-MS) previously classified as
HI-MS based on MRI/clinical criteria, who have been treated with IV daclizumab for a
minimum of 1 year and responded to this therapy with significant (>70%) decrease in
contrast-enhancing lesions (CEL) or stabilization/improvement of disease activity (>60%
decrease in MS relapses and stable or improved EDSS disability score).
- New treatment cohort: Up to 15 HI-MS patients (RR- or SP-MS) with inadequate therapeutic
response to first-line, FDA-approved immunomodulatory therapies for MS or who cannot,
for any reason, be treated with first-line, FDA-approved immunomodulatory therapies for
MS.
Design:
This is an open label, Phase I trial of 150 mg of daclizumab high yield process (DAC HYP)
administered subcutaneously (SC) every 4 weeks for a total of 3 years.
Outcome measures:
Because the main goal of this study is to investigate the MOA of CD25-blocking therapies in
MS, the primary outcomes are mechanistic immunological studies performed on clinical samples
(peripheral blood mononuclear cells (PBMC), cerebrospinal fluid (CSF) cells and skin
biopsies) derived from DAC HYP-treated patients. The secondary outcome measure is long-term
safety and tolerability of subcutaneous DAC HYP in HI-MS patients.
The primary goal of this study is to investigate the mechanism of action (MOA) of
CD25-blocking therapies in high inflammatory multiple sclerosis (HI-MS). The secondary goal
of this study is to assess long-term safety and efficacy of CD25-blocking therapies in HI-MS.
Study population:
Two cohorts of patients will be enrolled:
- Long-term daclizumab therapy cohort: Up to 15 daclizumab-treated patients with
relapsing-remitting (RR-MS) or secondary-progressive MS (SP-MS) previously classified as
HI-MS based on MRI/clinical criteria, who have been treated with IV daclizumab for a
minimum of 1 year and responded to this therapy with significant (>70%) decrease in
contrast-enhancing lesions (CEL) or stabilization/improvement of disease activity (>60%
decrease in MS relapses and stable or improved EDSS disability score).
- New treatment cohort: Up to 15 HI-MS patients (RR- or SP-MS) with inadequate therapeutic
response to first-line, FDA-approved immunomodulatory therapies for MS or who cannot,
for any reason, be treated with first-line, FDA-approved immunomodulatory therapies for
MS.
Design:
This is an open label, Phase I trial of 150 mg of daclizumab high yield process (DAC HYP)
administered subcutaneously (SC) every 4 weeks for a total of 3 years.
Outcome measures:
Because the main goal of this study is to investigate the MOA of CD25-blocking therapies in
MS, the primary outcomes are mechanistic immunological studies performed on clinical samples
(peripheral blood mononuclear cells (PBMC), cerebrospinal fluid (CSF) cells and skin
biopsies) derived from DAC HYP-treated patients. The secondary outcome measure is long-term
safety and tolerability of subcutaneous DAC HYP in HI-MS patients.
Objective:
The primary goal of this study is to investigate the mechanism of action (MOA) of
CD25-blocking therapies in high inflammatory multiple sclerosis (HI-MS). The secondary goal
of this study is to assess long-term safety and efficacy of CD25-blocking therapies in HI-MS.
Study population:
We will enroll up to 70 patients. We expect to screen up to 40 HI-MS participants to yield 31
patients that will receive study drug. Two cohorts of patients will be enrolled for the
treatment part of the protocol: A. Long-term daclizumab therapy cohort: 16 daclizumab-treated
patients with relapsing-remitting (RR-MS) or secondary-progressive MS (SP-MS) previously
classified as HI-MS based on MRI/clinical criteria, who have been treated with IV daclizumab
for a minimum of 1 year and responded to this therapy with significant (>70%) decrease in
contrast-enhancing lesions (CEL) or stabilization/improvement of disease activity (>60%
decrease in MS relapses and stable or improved EDSS disability score). B. New treatment
cohort: 15 HI-MS patients (RR- or SP-MS) with inadequate therapeutic response to first-line,
FDA-approved immunomodulatory therapies for MS or who choose not to, for any reason, be
treated with first-line, FDAapproved immunomodulatory therapies for MS. Up to 30 subjects
with inflammatory MS will be screened to yield 20 controls for immunization and skin biopsy
studies (Cohort C: MS controls).
Design:
This is an open label, Phase I trial of 150 mg of daclizumab high yield process (DAC HYP)
administered subcutaneously (SC) every 4 weeks for a total of 3 years.
Outcome measures:
Because the main goal of this study is to investigate the MOA of CD25-blocking therapies in
MS, the primary outcomes are mechanistic immunological studies performed on clinical samples
(peripheral blood mononuclear cells (PBMC), cerebrospinal fluid (CSF) cells and skin
biopsies) derived from DAC HYP-treated patients. The secondary outcome measure is long-term
safety and tolerability of subcutaneous DAC HYP in HI-MS patients.
The primary goal of this study is to investigate the mechanism of action (MOA) of
CD25-blocking therapies in high inflammatory multiple sclerosis (HI-MS). The secondary goal
of this study is to assess long-term safety and efficacy of CD25-blocking therapies in HI-MS.
Study population:
We will enroll up to 70 patients. We expect to screen up to 40 HI-MS participants to yield 31
patients that will receive study drug. Two cohorts of patients will be enrolled for the
treatment part of the protocol: A. Long-term daclizumab therapy cohort: 16 daclizumab-treated
patients with relapsing-remitting (RR-MS) or secondary-progressive MS (SP-MS) previously
classified as HI-MS based on MRI/clinical criteria, who have been treated with IV daclizumab
for a minimum of 1 year and responded to this therapy with significant (>70%) decrease in
contrast-enhancing lesions (CEL) or stabilization/improvement of disease activity (>60%
decrease in MS relapses and stable or improved EDSS disability score). B. New treatment
cohort: 15 HI-MS patients (RR- or SP-MS) with inadequate therapeutic response to first-line,
FDA-approved immunomodulatory therapies for MS or who choose not to, for any reason, be
treated with first-line, FDAapproved immunomodulatory therapies for MS. Up to 30 subjects
with inflammatory MS will be screened to yield 20 controls for immunization and skin biopsy
studies (Cohort C: MS controls).
Design:
This is an open label, Phase I trial of 150 mg of daclizumab high yield process (DAC HYP)
administered subcutaneously (SC) every 4 weeks for a total of 3 years.
Outcome measures:
Because the main goal of this study is to investigate the MOA of CD25-blocking therapies in
MS, the primary outcomes are mechanistic immunological studies performed on clinical samples
(peripheral blood mononuclear cells (PBMC), cerebrospinal fluid (CSF) cells and skin
biopsies) derived from DAC HYP-treated patients. The secondary outcome measure is long-term
safety and tolerability of subcutaneous DAC HYP in HI-MS patients.
- The study population will consist of 2 cohorts of patients with an accrual ceiling of
40 subjects:
A. Long-term daclizumab therapy cohort: Up to 16 patients with HI-MS (both RR-MS and SP-MS)
who have been successfully treated with IV daclizumab for a minimum of 1 year.
B. New treatment cohort: Up to 15 patients with HI-MS (both RR-MS and SP-MS) who have not
been successfully treated with or have not tolerated standard FDA-approved immunomodulatory
therapies, or who, for whatever reason, choose not to be treated with standard FDA approved
immunomodulatory therapies.
INCLUSION CRITERIA:
- MS as defined by the modified McDonald criteria (Polman, Reingold et al. 2005)
- HI-MS (RR-MS or SP-MS) before initiation of daclizumab therapy, defined as:
- greater than or equal to 3 CEL on a single pre-daclizumab MRI or
- greater than or equal to 1 MS exacerbation per year before initiation of
daclizumab therapy or
- progression of sustained disability by greater than or equal to 1.0 point on the
expanded disability status scale (EDSS) in the year preceding daclizumab therapy
- Age 18-60, inclusive
- EDSS 0 to 6.0, inclusive
- Able to provide informed consent
- Willing to participate in all aspects of trial design and follow-up
- Females of childbearing potential are willing to commit to the use of a reliable
method of birth control (i.e., hormonal contraception including birth control
pills, injected hormones or vaginal ring; intrauterine device; barrier methods
with spermicide, specifically diaphragms or condoms they have undergone surgical
sterilization, such as hysterectomy or tubal ligation) for the duration of the
study and continued 4 months after conclusion of the study.
ADDITIONAL INCLUSION CRITERION FOR THE LONG-TERM DACLIZUMAB THERAPY COHORT ONLY:
-IV daclizumab therapy for at least 1 year with a treatment response consisting of:
- greater than or equal to 70% reduction of CEL after starting daclizumab; or
- stabilization or improvement of sustained neurological disability on daclizumab.
EXCLUSION CRITERIA (FOR BOTH COHORTS):
- PP-MS or low-inflammatory SP-MS
- Alternative diagnoses that can explain neurological disability and MRI findings (e.g.,
ischemia/gliosis, CNS lyme disease, SLE, sarcoidosis, etc.)
- History of malignancy, with the following exceptions: excised or treated basal cell
carcinoma or fewer than 3 squamous cell carcinomas, grade 1 endometrial carcinomas
treated with total hysterectomy and without evidence for recurrence for greater than
or equal to 3 years
- Clinically significant medical disorders that, in the judgment of the investigators,
could cause CNS tissue damage or limit its repair, expose the patient to undue risk of
harm or prevent the patient from completing the study (e.g., immunodeficiency
disorders, other autoimmune or immune-mediated disorders or chronic infections).
Specific exclusions (based on baseline laboratory evaluation) are:
- positive HIV or HTLV-1 serology;
- positive hepatitis B or C serology;
- pregnant or breastfeeding female;
- known history of severe allergic or anaphylactic reactions;
- known hypersensitivity to study drug or its excipients;
- varicella or herpes zoster virus infection or any severe viral infection within
the 6 weeks prior to screening; or
- exposure to varicella zoster virus within 21 days before screening.
- Abnormal screening/baseline blood tests exceeding any of the limits defined below:
- serum alanine aminotransferase/serum glutamate pyruvate transaminase (ALT/SGPT),
aspartate aminotransferase/serum glutamic oxaloacetic transaminase (AST/SGOT), or
gamma-glutamyl-transferase greater than or equal to 2 times the upper limit of
normal (ULN);
- total white blood cell count <3,000/mm(3);
- hemoglobin greater than or equal to 9.0 g/dL;
- platelets greater than or equal to 100 x 10(9)/L;
- lymphocytes greater than or equal to 1.0 x 10(9)/L;
- neutrophils greater than or equal to 1.5 x 10(9)/L;
- serum creatinine greater than or equal to the ULN.
- Any of the following treatment history:
- any type of live virus vaccine in the 4 weeks prior to initiation of therapy,
including but not limited to: measles/mumps/rubella vaccine, varicella zoster
virus vaccine, oral polio vaccine, and nasal influenza vaccine;
- infection (viral, fungal, bacterial) requiring hospitalization or intravenous
(IV) antibiotics within the 8 weeks prior to initiation of therapy;
- another investigational drug or approved therapy for investigational use (except
daclizumab) within the 6 months prior to initiation of therapy.
- Prior treatment with the any of the following:
- total lymphoid irradiation;
- cladribine;
- T cell or T cell receptor vaccination; or
- any therapeutic monoclonal antibody, except natalizumab and daclizumab.
- Prior treatment with any of the following medications or procedures within 1 year
prior to initiation of therapy:
- mitoxantrone;
- cyclophosphamide;
- fingolimod; or
- natalizumab.
- Prior treatment with any of the following medications or procedures within 6 months
prior to initiation of therapy:
- cyclosporine;
- azathioprine;
- methotrexate;
- mycophenolate mofetil;
- intravenous immunoglobulin (IVIg); or
- plasmapheresis or cytapheresis.
- Treatment with any of the following medications within the 30 days prior to initiation
of therapy:
- IV corticosteroid treatment;
- oral corticosteroid treatment;
- glatiramer acetate; or
- interferon-beta
- For immunizations studies, known history of hypersensitivity or severe allergic
reaction to vaccine components (subjects with such history can participate in the
trial, but will not be immunized)
- For patients in the extension phase: Patients may be excluded if they did not
demonstrate an adequate clinical response in the first phase of the trial while
receiving DAC HYP.
Inclusion criteria for MS controls for immunization and skin biopsy studies:
- MS as defined by the modified McDonald criteria
- RR-MS or SP-MS
- Age 18-60, inclusive
- EDSS 0 to 7.0, inclusive
- Able to provide informed consent
- Willing to participate in all aspects of trial design and follow-up
Exclusion criteria for MS controls for immunization and skin biopsy studies:
- Treatment with immunomodulatory therapies that may have a negative impact on
development of antigen-specific responses after immunization, including steroids
within the last 60 days before the immunization study
- Clinically significant medical disorders that, in the judgment of the investigators,
could invalidate the person as appropriate control (e.g., immunodeficiency disorders,
other autoimmune or immunemediated disorders or chronic infections). Specific
exclusions (based on baseline laboratory evaluation) are:
- positive HIV or HTLV-1 serology;
- positive hepatitis B or C serology;
- pregnant or breastfeeding female;
- known history of severe allergic or anaphylactic reactions to vaccine components;
- Abnormal screening/baseline blood tests exceeding any of the limits defined below:
- serum alanine aminotransferase/serum glutamate pyruvate transaminase (ALT/SGPT),
aspartate aminotransferase/serum glutamic oxaloacetic transaminase (AST/SGOT), or
gamma-glutamyl-transferase (Bullet)2 times the upper limit of normal (ULN);
- total white blood cell count <3,000/mm3;
- hemoglobin less than or equal to 9.0 g/dL
We found this trial at
1
site
9000 Rockville Pike
Bethesda, Maryland 20892
Bethesda, Maryland 20892
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