Protocol summary
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Study aim
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Pegylated interferon beta-1a (CinnaGen) is non-inferior to CinnoVex® (CinnaGen) for treatment of relapsing-remitting Multiple Sclerosis.
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Design
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Phase III, randomized, parallel-group, and non-inferiority.
The patient randomization process will be centrally conducted by simple randomization method (complete algorithm) in PASS software for a total of 168 patients (with a 1: 1 allocation ratio). After the randomization procedure, a code will be allocated to each patient that will be used as patient identifier throughout the study.
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Settings and conduct
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The trial will be performed by principle and co-investigators in Tehran (Sina, Imam Hossein, and Amiralam hospitals), Isfahan (Kashani hospital), Mashhad (Ghaem hospital), Sari (Buali hospital), Tabriz (Imam Reza hospital) and Rasht (Ghaem hospital), Hamedan (Sina).
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Participants/Inclusion and exclusion criteria
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Inclusion Criteria: Age 18-50 years, RRMS diagnosis, EDSS 0–5, At least one relapse within the past 12 months, Signed Informed Consent.
Exclusion Criteria: Other types of MS, Surgery or treatment with other agents to treat MS symptoms or underlying disease as specified in the protocol, Abnormal screening lab tests, History of any medical condition that would preclude participation in the trial, MS relapse within 30 days prior to randomization and/or not stabilized from a previous relapse prior to randomization, Pregnancy and lactation, Unwillingness or inability to comply with the requirements of the protocol, The decision of the Investigator and Others specified in the protocol.
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Intervention groups
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Group I: Pegylated interferon beta-1a (CinnaGen), Physioject™ autoinjector, 125mcg, subcutaneous, every 2 weeks for 96 weeks.
Group II: CinnoVex® (CinnaGen), prefilled syringe, 30mcg, intramuscular, once a week for 96 weeks.
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Main outcome variables
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The annualized relapse rate in a 96 weeks study period
General information
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Reason for update
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AMENDMENT
*Change in Randomization
*Changes in study schedule from month to week
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Acronym
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IRCT registration information
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IRCT registration number:
IRCT201612306135N8
Registration date:
2017-01-14, 1395/10/25
Registration timing:
prospective
Last update:
2020-11-25, 1399/09/05
Update count:
3
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Registration date
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2017-01-14, 1395/10/25
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Registrant information
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Recruitment status
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Recruitment complete
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Funding source
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CinnaGen Pharmaceutical Company
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Expected recruitment start date
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2018-03-15, 1396/12/24
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Expected recruitment end date
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2019-09-22, 1398/06/31
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Actual recruitment start date
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empty
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Actual recruitment end date
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empty
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Trial completion date
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empty
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Scientific title
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Efficacy and safety of peginterferon beta-1a (CinnaGen) versus CinnoVex® (CinnaGen) in reducing the annualized relapse rate (ARR) in participants with relapsing-remitting multiple sclerosis: A phase III, randomized, parallel, non-inferiority study.
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Public title
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Efficacy and safety of peginterferon beta-1a (CinnaGen) in relapsing-remitting multiple sclerosis patients.
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Purpose
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Treatment
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Inclusion/Exclusion criteria
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Inclusion criteria:
Age 18-50 years
Relapsing-remitting multiple sclerosis (RRMS) (McDonald criteria 2010)
Expanded Disability Status Scale (EDSS) is 0–5
At least one relapse having occurred within the past 12 months
Subjects have refused alternative treatments and other available therapies
Ability to understand the purpose and risks of the study and provide signed and dated an informed consent
Negative pregnancy test for childbearing women
Exclusion criteria:
Primary progressive, secondary progressive, or progressive- relapsing MS
Female subjects considering becoming pregnant while in the study or currently breastfeeding
Subjects for whom MRI was contraindicated, i.e., who had pacemakers or were allergic to gadolinium,...
Unwillingness or inability to comply with the requirements of the protocol
Pre-specified laboratory abnormalities
History of any clinically significant that would preclude participation in a clinical trial
History of malignant disease (with the exception of squamous cell carcinomas of the skin that are cured)
History of seizure disorder or unexplained blackouts OR history of a seizure within 3 months prior to Baseline
History of suicidal ideation or an episode of severe depression within 3 months prior to Baseline
Alanine transaminase/serum glutamate pyruvate transaminase (ALT/SGPT) greater than 2 times the upper limit of normal
Aspartate transaminase/serum glutamic oxaloacetic transaminase (AST/SGOT) greater than 2 times the upper limit of normal
Bilirubin greater than 1.5 times the upper limit of normal
Total white blood cell count (WBC) <4000 /mm3
Absolute Neutrophil Count (ANC) of < 1500 /mm3
Platelet count <120,000 c/mm3
Hemoglobin <10 g/dL in female subjects; <11 g/dL in male subjects
Serum creatinine upper limit of normal lab value
An MS relapse that has occurred within the 30 days prior to randomization or the subject has not stabilized from a previous relapse prior
Elective surgery performed from 2 weeks prior or scheduled through the end of the study
Any prior treatment with Total Lymphoid Irradiation, Cladribine, T-cell Vaccine, Natalizumab, Rituximab, BIIB017, Fingolimod, Dimethyl fumarate, and Teriflunomide
Prior treatment within 1 with Cyclophosphamide– Mitoxantrone
Prior treatment within 6 months with Cyclosporine, Plasma exchange, Intravenous immunoglobulin (IVIG), Azathioprine, Methotrexate
Any prior treatment within 6 months with interferon
Prior treatment within 30 days prior with Systemic Corticosteroids
Prior treatment with Glatiramer Acetate within 4 weeks prior to randomization
Treatment with another investigational drug within the 6 months prior to randomization
Other reasons, that in the opinion of the investigator, made the subject unsuitable for enrolment
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Age
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From 18 years old to 50 years old
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Gender
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Both
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Phase
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3
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Groups that have been masked
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No information
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Sample size
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Target sample size:
168
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Randomization (investigator's opinion)
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Randomized
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Randomization description
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The patient randomization process will be centrally conducted by simple randomization method (complete algorithm) in PASS software for a total of 168 patients (with a 1: 1 allocation ratio). After the randomization procedure, a code will be allocated to each patient that will be used as patient identifier throughout the study. The code will consist of four numbers (corresponding to the randomization number), 4 initials (corresponding to the first two letters of first name, first two letters of surname), and 3 numbers (center code), e.g. ABCD001PE3-0001. Randomization numbers will be determined sequentially.
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Blinding (investigator's opinion)
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Not blinded
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Blinding description
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Placebo
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Not used
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Assignment
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Parallel
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Other design features
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Ethics committees
1
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Ethics committee
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Approval date
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2016-11-05, 1395/08/15
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Ethics committee reference number
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IR.TUMS.REC.1395.2868
2
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Ethics committee
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Approval date
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2016-10-17, 1395/07/26
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Ethics committee reference number
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IR.TBZMED.REC.1395.759
Health conditions studied
1
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Description of health condition studied
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Multiple sclerosis
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ICD-10 code
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G35
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ICD-10 code description
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Multiple sclerosis
Primary outcomes
1
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Description
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Annual relapse rate
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Timepoint
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Ralapse rate counts during 96 weeks/ every 4 weeks visits
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Method of measurement
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A relapse is defined as an episode of neurological symptoms that happens at least 30 days after any previous episode began, lasts at least 24 h and is not attributable to another cause and occurs in the absence of an infection or fever.
Secondary outcomes
1
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Description
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Number of new or newly enlarging hyperintense lesions on T2-weighted images (relative to baseline MRI)
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Timepoint
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Baseline, 24th, 48th, 96th week
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Method of measurement
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MRI evaluation
2
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Description
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Proportion of patients with 12 weeks of sustained disability progression
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Timepoint
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During 96 weeks of study follow up
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Method of measurement
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Clinical evaluation
3
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Description
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Gadolinium-enhancing lesions, New active lesions (T2), Volume of new or newly enlarging T2 hyperintense, gadolinium-enhancing, and T1 hypointense lesions, brain atrophy
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Timepoint
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24th, 48th, 96th week
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Method of measurement
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MRI evaluation
4
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Description
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Any - Adverse events (AEs), Adverse drug reactions (ADR) including: o Flu-like symptoms, injection site reaction (redness, pain, itching, necrosis), o Rising AST, ALT or ALP 2.5 times more than normal value,or Hyperbilirubinemia: 1.5 Times more than Upper normal limit, Leukopenia (WBC <3000), Thrombocytopenia (Platelet count < 100,000),..
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Timepoint
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During 96 weeks of study follow up
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Method of measurement
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Clinical and laboratory evaluation
Intervention groups
1
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Description
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Intervention group 1: Pegylated interferon beta-1a (CinnaGen) autoinjector (Physioject™) for patients with dose of 125micrograms, subcutaneous (S/C) injection every 2weeks for 96 weeks
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Category
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Treatment - Drugs
2
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Description
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Intervention group 2: CinnoVex® (CinnaGen) 30 mcg, prefilled syringe, injected intramuscularly once a week for 96 weeks
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Category
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Treatment - Drugs
1
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Sponsor
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Grant name
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Grant code / Reference number
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Is the source of funding the same sponsor organization/entity?
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Yes
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Title of funding source
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CinnaGen Pharmaceutical Company
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Proportion provided by this source
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100
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Public or private sector
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Private
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Domestic or foreign origin
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Domestic
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Category of foreign source of funding
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empty
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Country of origin
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Type of organization providing the funding
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Persons
Sharing plan
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Deidentified Individual Participant Data Set (IPD)
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Undecided - It is not yet known if there will be a plan to make this available
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Study Protocol
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Undecided - It is not yet known if there will be a plan to make this available
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Statistical Analysis Plan
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Undecided - It is not yet known if there will be a plan to make this available
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Informed Consent Form
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Undecided - It is not yet known if there will be a plan to make this available
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Clinical Study Report
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Undecided - It is not yet known if there will be a plan to make this available
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Analytic Code
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Undecided - It is not yet known if there will be a plan to make this available
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Data Dictionary
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Undecided - It is not yet known if there will be a plan to make this available