MedPath

To Assess Efficacy and Safety of Batoclimab in Adult Participants With Active CIDP

Phase 2
Active, not recruiting
Conditions
Chronic Inflammatory Demyelinating Polyneuropathy
Interventions
Drug: Batoclimab 680 milligrams (mg) subcutaneous (SC) weekly
Drug: Batoclimab 340 mg SC weekly
Drug: Placebo
Registration Number
NCT05581199
Lead Sponsor
Immunovant Sciences GmbH
Brief Summary

This is a multi-center, randomized, quadruple-blind, placebo-controlled study to evaluate the efficacy and safety of batoclimab in adult participants with active CIDP. The study includes an up to 4-week Screening Period, an up to 12-week Washout Period, a 12-week Randomized Treatment Period (Period 1), an up to 24-week Randomized Withdrawal Period (Period 2), an up to 52-week Long-term Extension (LTE) Period (optional), and Safety Follow-up 4 weeks after the last dose of study treatment. The total study duration will be up to approximately 109 weeks. Eligible participants will be assigned to one of four cohorts based upon their baseline CIDP treatment (Cohorts A and D - immunoglobulin \[Ig\] or plasma exchange \[PLEX\]; Cohort B - corticosteroids; Cohort C - naive or untreated in previous 3-24 months) and whether they meet diagnosis according to the European Academy of Neurology/Peripheral Nerve Society (EAN/PNS) criteria (Cohorts A, B, and C) or clinical criteria only (Cohort D) at the time of screening.

Detailed Description

Not available

Recruitment & Eligibility

Status
ACTIVE_NOT_RECRUITING
Sex
All
Target Recruitment
277
Inclusion Criteria

Not provided

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Exclusion Criteria

All Cohorts:

  1. Have current or prior history of immunoglobulin M (IgM) paraproteinemia with or without anti-myelin-associated-glycoprotein antibodies.

  2. Have Distal CIDP, Sensory CIDP or are suspected of having a diagnosis of auto-immune nodopathy in accordance with the EAN/PNS Guideline on Diagnosis and Treatment of CIDP.

  3. Have polyneuropathy of causes other than CIDP including but not limited to:

    1. Multifocal motor neuropathy
    2. Hereditary demyelinating neuropathy
    3. Polyneuropathy, organomegaly, endocrinopathy, monoclonal protein and skin change syndromes (i.e., POEMS)
    4. Lumbosacral radiculoplexus neuropathy
    5. Systemic illnesses including vitamin deficiency syndromes and paraneoplastic neuropathies
    6. Drug- or toxin-induced

  4. Have diabetes mellitus (DM) and meets any of the following criteria:

    1. Does not meet inclusion criteria 2(a) and 3(a).
    2. In the opinion of the Investigator, there is evidence of poorly controlled DM preceding the diagnosis of CIDP.
    3. In the opinion of the Investigator, there is evidence of poorly controlled DM at screening.

  5. Have a history of myelopathy or evidence of central demyelination.

  6. Are receiving chronic oral corticosteroids monotherapy at a dose > 40 mg/day prednisolone/prednisone or its equivalent at the Screening Visit.

  7. Are receiving chronic oral corticosteroid at a dose > 10 mg/day prednisolone/prednisone or equivalent in combination with immunoglobulin therapy or PLEX at the Screening Visit.

Additional exclusion criteria are defined in the protocol.

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Study & Design

Study Type
INTERVENTIONAL
Study Design
SEQUENTIAL
Arm && Interventions
GroupInterventionDescription
LTE Period: With Relapse in Period 2: Dose 1 and Dose 2Batoclimab 680 milligrams (mg) subcutaneous (SC) weeklyParticipants will receive Dose 1 for the initial 4 weeks only and Dose 2 for the remaining 48 weeks.
Withdrawal Period 2: Cohort A, Dose 2Batoclimab 340 mg SC weekly-
Treatment Period 1: Cohort B, Dose 2Batoclimab 340 mg SC weekly-
Treatment Period 1: Cohort B, Dose 1Batoclimab 680 milligrams (mg) subcutaneous (SC) weekly-
Treatment Period 1: Cohort C, Dose 1Batoclimab 680 milligrams (mg) subcutaneous (SC) weekly-
Treatment Period 1: Cohort D, Dose 1Batoclimab 680 milligrams (mg) subcutaneous (SC) weekly-
Treatment Period 1: Cohort A, Dose 2Batoclimab 340 mg SC weekly-
Treatment Period 1: Cohort A, Dose 1Batoclimab 680 milligrams (mg) subcutaneous (SC) weekly-
Treatment Period 1: Cohort C, Dose 2Batoclimab 340 mg SC weekly-
Withdrawal Period 2: Cohort B, PlaceboPlacebo-
Withdrawal Period 2: Cohort D, PlaceboPlacebo-
Withdrawal Period 2: Cohort A, PlaceboPlacebo-
LTE Period: Without Relapse in Period 2: Dose 2Batoclimab 340 mg SC weeklyParticipants will receive Dose 2 for all 52 weeks.
Treatment Period 1: Cohort D, Dose 2Batoclimab 340 mg SC weekly-
Withdrawal Period 2: Cohort D, Dose 2Batoclimab 340 mg SC weekly-
LTE Period: With Relapse in Period 2: Dose 1 and Dose 2Batoclimab 340 mg SC weeklyParticipants will receive Dose 1 for the initial 4 weeks only and Dose 2 for the remaining 48 weeks.
Withdrawal Period 2: Cohort C, PlaceboPlacebo-
Withdrawal Period 2: Cohort B, Dose 2Batoclimab 340 mg SC weekly-
Withdrawal Period 2: Cohort C, Dose 2Batoclimab 340 mg SC weekly-
Primary Outcome Measures
NameTimeMethod
Period 2, Cohort A: Proportion of participants who remain relapse-free at Week 36Week 36

Relapse is defined as a worsening (increase) of \>=1 point on adjusted inflammatory neuropathy cause and treatment (AdjINCAT) score at any time point during Period 2 relative to Period 2 Baseline which is sustained at a Follow-Up visit 1 week later. The INCAT disability scale is a widely used and validated efficacy assessment of neurologic dysfunction in CIDP. Upper and lower limb dysfunction are each separately assessed on a scale of 0-5 and results are summed together for a total composite score of 0-10. Higher scores represent greater disability. The Adj INCAT disability score is identical to INCAT disability score with exception that changes in upper limb function from 0 (normal) to 1 (minor symptoms) and vice versa are excluded since minor symptoms in the fingers, which are implied by an upper limb score of 1, are not considered clinically significant in all participants. The Adj INCAT disability score will be used for participant selection and measurement of clinical response.

Secondary Outcome Measures
NameTimeMethod
Period 2, Cohort A: Change from Period 2 Baseline in Adj INCAT scoreBaseline (Week 12) and up to Week 36
Period 2, Cohort A: Time to first relapse relative to Period 2 BaselineBaseline (Week 12) to Week 36
Period 2, Cohorts A and B combined: Change from Period 2 Baseline in Mean Grip StrengthBaseline (Week 12) and up to Week 36
Period 2, Cohort A: Change from Period 2 Baseline in Inflammatory Rasch-built Overall Disability Scale (I-RODS)Baseline (Week 12) and up to Week 36

The I-RODS for immune-mediated peripheral neuropathies is a patient-based linearly weighted scale that captures activity and social participation limitations in patients with CIDP. The assessment consists of a 24-question instrument that addresses upper and lower limb tasks that range in difficulty from reading a book and eating to standing and running. Answers are scored on a scale of 0-2 (complete disability to no disability) and the raw scores are then transformed into a final score ranging from 0-100.

Period 2, Cohorts A and B combined: Change from Period 2 Baseline in Adj INCAT scoreBaseline (Week 12) and up to Week 36
Period 2, Cohorts A, B, and C: Proportion of participants who remain relapse-free at Week 36Week 36
Period 2, Cohort A: Change from Period 2 Baseline in Medical Research Council (MRC) Sum ScoreBaseline (Week 12) and up to Week 36

The MRC sum score is a standardized methodology for objectively assessing and reporting muscle function. Six muscle groups are assessed bilaterally, and each scored on a scale of 0 (no visible contraction) to 5 (normal) yielding a sum ranging from 0 (paralysis) to 60 (normal strength). Higher scores indicate normal muscle strength.

Period 2, Cohort A: Change from Period 2 Baseline in Mean grip strengthBaseline (Week 12) and up to Week 36

Mean Grip strength provides an objective, quantitative and immediate assessment of strength impairment. The Jamar dynamometer and the Martin vigorimeter are both commonly used to assess mean grip strength.

Period 2, Cohort A: Change from Period 2 Baseline in Overall Neuropathy Limitations Scale (ONLS)Baseline (Week 12) and up to Week 36

The ONLS is a scale that focuses on upper and lower limb functions and was designed to assess the limitations of participants with immune-mediated peripheral neuropathies. This scale is completed by adding the total of the arm grade from zero point (less limitation) to 5 points (most limitation) and leg grade from zero point (less limitation) to 7 points (more limitation) yielding a total score of 0 (no disability) to 12 (maximum disability). Lower values in the ONLS indicate a better clinical condition.

Period 2, Cohorts A and B combined: Change from Period 2 Baseline in I-RODSBaseline (Week 12) and up to Week 36
Period 2, Cohorts A and B combined: Change from Period 2 Baseline in MRC sum scoreBaseline (Week 12) and up to Week 36
Period 2, Cohorts A and B combined: Change from Period 2 Baseline in ONLSBaseline (Week 12) and up to Week 36

Trial Locations

Locations (116)

Site Number - 8403

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TimiÅŸoara, Timis, Romania

SIte Number - 8400

🇷🇴

Constanta, Romania

Site Number - 8501

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Belgrade, Serbia

Site Number - 8502

🇷🇸

Belgrade, Serbia

Site Number - 8500

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Niš, Serbia

Site Number - 8503

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Novi Sad, Serbia

Site Number - 8600

🇸🇰

Liptovský Mikuláš, Slovakia

Site Number - 8601

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Martin, Slovakia

Site Number - 8603

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Prešov, Slovakia

Site Number - 8602

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Trnava, Slovakia

Site Number - 3701

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Hospitalet de Llobregat, Barcelona, Spain

Site Number - 3704

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Sant Cugat Del Vallès, Barcelona, Spain

Site Number - 3700

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San Sebastián, Gipuzkoa, Spain

Site Number - 3703

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Barcelona, Spain

Site Number - 4891

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Göteborg, Vastra Gotalands Lan, Sweden

Site Number - 7405

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Cambridge, Cambridgeshire, United Kingdom

Site Number - 7402

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Southampton, Hampshire, United Kingdom

Site Number - 7404

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Glasgow, Lanarkshire, United Kingdom

Site Number - 7403

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Preston, Lancashire, United Kingdom

Site Number - 7401

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Sheffield, South Yorkshire, United Kingdom

Site Number - 7400

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Manchester, United Kingdom

Site Number - 1634

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Los Angeles, California, United States

Site Number - 1603

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Scottsdale, Arizona, United States

Site Number - 1618

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Carlsbad, California, United States

Site Number - 1619

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Orange, California, United States

Site Number - 1608

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San Francisco, California, United States

Site Number - 1625

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Aurora, Colorado, United States

Site Number - 1636

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Fort Collins, Colorado, United States

Site Number - 1621

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New Haven, Connecticut, United States

Site Number - 1630

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Washington, District of Columbia, United States

Site Number - 1600

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Boca Raton, Florida, United States

Site Number - 1609

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Jacksonville, Florida, United States

Site Number - 1631

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Orlando, Florida, United States

Site Number - 1629

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Orlando, Florida, United States

Site Number - 1617

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Ormond Beach, Florida, United States

Site Number - 1620

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Port Charlotte, Florida, United States

Site Number - 1633

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Rockledge, Florida, United States

Site Number - 1604

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Saint Petersburg, Florida, United States

Site Number - 1607

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O'Fallon, Illinois, United States

Site Number - 1602

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Kansas City, Kansas, United States

Site Number - 1611

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Nicholasville, Kentucky, United States

Site Number - 1622

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Brooklyn, New York, United States

Site Number - 1605

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New York, New York, United States

Site Number - 1635

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Chapel Hill, North Carolina, United States

Site Number - 1610

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Charlotte, North Carolina, United States

Site Number - 1614

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Portland, Oregon, United States

Site Number - 1623

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Philadelphia, Pennsylvania, United States

Site Number - 1624

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Philadelphia, Pennsylvania, United States

Site Number -1601

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Austin, Texas, United States

Site Number - 1606

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Houston, Texas, United States

Site Number - 1628

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San Antonio, Texas, United States

Site Number - 1627

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Richmond, Virginia, United States

Site Number - 1632

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Seattle, Washington, United States

Site Number - 1613

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Milwaukee, Wisconsin, United States

Site Number - 7753

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Rosario, Santa Fe, Argentina

Site Number - 7751

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Rosario, Santa Fe, Argentina

Site Number - 7752

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Tucumán, Tucuman, Argentina

Site Number - 7750

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Ciudad Autónoma de Buenos Aires, Argentina

Site Number - 4681

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Gent, Oost-Vlaanderen, Belgium

Site Number - 4680

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Leuven, Vlaams Brabant, Belgium

Site Number - 9103

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Brasília, Distrito Federal, Brazil

Site Number - 9101

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Curitiba, Paraná, Brazil

Site Number - 9100

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Ribeirão Preto, São Paulo, Brazil

Site Number - 9102

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Rio De Janeiro, Brazil

Site Number - 9105

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São Paulo, Brazil

Site Number - 9111

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Sofia, Sofia-Grad, Bulgaria

Site Number - 9110

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Sofia, Sofia-Grad, Bulgaria

Site Number - 9112

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Pleven, Bulgaria

Site Number - 2600

🇨🇦

Edmonton, Alberta, Canada

Site Number - 2603

🇨🇦

Vancouver, British Columbia, Canada

Site Number - 4740

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Copenhagen, Denmark

Site Number - 3241

🇫🇮

Turku, Varsinais-Suomi, Finland

Site Number - 6704

🇩🇪

München, Bayern, Germany

Site Number - 6705

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Bochum, Nordrhein-Westfalen, Germany

Site Number - 6700

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Dresden, Sachsen, Germany

Site Number - 6702

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Leipzig, Sachsen, Germany

Site Number - 6706

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Berlin, Germany

Site Number - 6341

🇬🇷

Patras, Achaïa, Greece

Site Number - 6344

🇬🇷

Athens, Attiki, Greece

Site Number - 6345

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Athens, Attiki, Greece

Site Number - 6343

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Alexandroupolis, Evros, Greece

Site Number - 6346

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Ioánnina, Ioannina, Greece

Site Number - 6342

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Heraklion, Irakleio, Greece

Site Number - 6347

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Larisa, Greece

Site Number - 6302

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Gussago, Brescia, Italy

Site Number - 6305

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Bologna, Emilia-Romagna, Italy

Site Number - 6304

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Udine, Friuli-Venezia Giulia, Italy

Site Number - 6309

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Roma, Lazio, Italy

Site Number - 6306

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Roma, Lazio, Italy

Site Number - 6301

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Bergamo, Lombardia, Italy

Site Number - 6307

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Milano, Lombardia, Italy

Site Number - 6303

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Pisa, Toscana, Italy

Site Number - 6308

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Siena, Toscana, Italy

Site Number - 6300

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Pavia, Italy

Site Number - 9901

🇰🇷

Seoul, Korea, Republic of

Site Number - 9900

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Seoul, Korea, Republic of

Site Number - 6491

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Oslo, Norway

Site Number - 3204

🇵🇱

Wroclaw, Dolnoslaskie, Poland

Site Number - 3211

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Bydgoszcz, Kujawsko-pomorskie, Poland

Site Number - 3210

🇵🇱

Lublin, Lubelskie, Poland

Site Number - 3206

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Lublin, Lubelskie, Poland

Site Number - 3202

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Mazurki, Lubelskie, Poland

Site Number - 3209

🇵🇱

Krakow, Malopolskie, Poland

Site Number - 3200

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Krakow, Malopolskie, Poland

Site Number - 3208

🇵🇱

Kraków, Malopolskie, Poland

Site Number - 3205

🇵🇱

Gdańsk, Pomorskie, Poland

Site Number - 3201

🇵🇱

Katowice, Slaskie, Poland

Site Number - 3207

🇵🇱

Poznan, Wielkopolskie, Poland

Site Number - 3203

🇵🇱

Bydgoszcz, Województwo Kujawsko-pomorskie, Poland

Site Number - 3742

🇵🇹

Senhora Da Hora, Porto, Portugal

Site Number - 3745

🇵🇹

Vila Nova De Gaia, Porto, Portugal

Site Number - 3743

🇵🇹

Almada, Setubal, Portugal

Site Number - 3741

🇵🇹

Lisboa, Portugal

Site Number - 3744

🇵🇹

Porto, Portugal

Site Number - 8406

🇷🇴

Bucharest, Bucuresti, Romania

Site Number - 8401

🇷🇴

Targu Mures, Mures, Romania

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