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Chronic inflammatory demyelinating polyradiculoneuropathy – Treatment

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Living with chronic inflammatory demyelinating polyradiculoneuropathy means navigating a complex journey where treatment choices can significantly shape quality of life, mobility, and independence—yet understanding the options available, from established therapies to emerging research approaches, empowers patients and families to make informed decisions alongside their healthcare teams.

Navigating Treatment Options for a Complex Nerve Condition

When someone receives a diagnosis of chronic inflammatory demyelinating polyradiculoneuropathy, understanding how to manage this condition becomes a central concern. Treatment goals focus on controlling the autoimmune inflammation—the mistaken attack by the immune system on the body’s own nerve tissue—to slow or stop disease progression, restore lost function where possible, and improve day-to-day quality of life. Because the condition affects the protective myelin sheath surrounding peripheral nerves, treatment aims to prevent further damage while helping the body repair what has been harmed.[1]

The approach to managing chronic inflammatory demyelinating polyradiculoneuropathy is highly individualized. What works well for one person may not suit another, depending on disease severity, how symptoms present, which variant of the condition someone has, and how their body responds to treatment. The disease can follow different patterns over time—some people experience steady worsening, while others go through cycles of improvement and relapse. This unpredictability makes ongoing communication with healthcare providers essential, as treatment plans often need adjustment based on changing circumstances.[2]

Medical societies have established guidelines for standard treatments that have proven effective through years of clinical use. At the same time, researchers continue investigating new therapeutic approaches through clinical trials, searching for options that might work better, cause fewer side effects, or help people who don’t respond adequately to existing treatments. Both pathways—proven therapies and experimental ones—offer hope to those affected by this challenging condition.[10]

⚠️ Important
Early diagnosis and prompt treatment significantly improve outcomes in chronic inflammatory demyelinating polyradiculoneuropathy. Delayed treatment can lead to permanent nerve damage that becomes irreversible. If you experience progressive muscle weakness, numbness in your hands or feet, loss of balance, or difficulty walking that worsens over eight weeks or longer, seeking medical evaluation as soon as possible is critical.

Established Treatments That Form the Foundation of Care

Three main therapies have emerged as first-line treatments for chronic inflammatory demyelinating polyradiculoneuropathy, supported by substantial clinical evidence and endorsed by medical guidelines. These treatments work by modulating or suppressing the immune system’s harmful attack on nerve myelin. The choice among them depends on factors including disease severity, patient preferences, access to healthcare facilities, insurance coverage, and individual tolerance of side effects.[9]

Immunoglobulin Therapy

Intravenous immunoglobulin, commonly called IVIg, represents one of the most widely used treatments. This therapy involves infusing antibodies collected from thousands of healthy blood donors directly into the bloodstream. These donor antibodies appear to block the immune system’s attack on myelin, though scientists don’t completely understand all the mechanisms involved. IVIg is typically administered every three to four weeks at a medical facility or sometimes at home with nursing support. Each infusion session usually takes several hours.[1]

A newer option called subcutaneous immunoglobulin (SCIg) allows patients to receive immunoglobulin therapy through smaller needles placed just under the skin rather than through veins. This approach often means more frequent administrations—typically once weekly—but patients can learn to self-administer at home using a pump device. Many people appreciate the flexibility and independence this provides, though it requires training and comfort with self-injection techniques.[15]

Side effects from immunoglobulin therapy can include headache, fever, chills, fatigue, and rarely more serious reactions such as blood clots or kidney problems. Healthcare providers monitor patients closely during and after infusions. Some people tolerate the treatment very well with minimal side effects, while others find the reactions more challenging. The therapy often needs to continue long-term, as symptoms may return when treatment stops.[10]

Corticosteroid Medications

Corticosteroids are powerful anti-inflammatory medications that suppress the immune system broadly. Drugs like prednisone, methylprednisolone, or dexamethasone can be taken by mouth or given intravenously. These medications work by reducing the inflammatory attack on nerve myelin and can be quite effective at improving symptoms. Treatment duration varies—some people need only a few months, while others require long-term therapy, often with gradually decreasing doses.[6]

The effectiveness of corticosteroids must be weighed against their potential side effects, which become more likely and severe with higher doses and longer treatment duration. Common problems include weight gain, elevated blood sugar (potentially causing or worsening diabetes), high blood pressure, mood changes, difficulty sleeping, weakening of bones (osteoporosis), increased infection risk, and changes in appearance such as facial swelling. Healthcare providers typically prescribe the lowest effective dose and may add medications to protect bone health or control blood sugar.[10]

Plasma Exchange

Plasma exchange, also called plasmapheresis, is a procedure that physically removes harmful antibodies from the blood. During the procedure, blood is drawn from the body, passed through a machine that separates and removes the liquid portion (plasma) containing the problematic antibodies, and then returned to the body with replacement fluids. This process typically requires sessions several times per week for a few weeks, performed at a specialized medical facility.[6]

Plasma exchange can produce rapid improvement in symptoms, making it particularly valuable for people with severe or rapidly worsening disease. However, the procedure requires specialized equipment and trained staff, making it less accessible than other treatments. It also carries risks including infection at the access site, changes in blood pressure, bleeding problems, and allergic reactions to replacement fluids. Like immunoglobulin therapy, the benefits are often temporary, and many people need ongoing maintenance treatment with other therapies.[9]

Additional Immunosuppressive Medications

When first-line treatments don’t work adequately or cause intolerable side effects, doctors may turn to other immune-suppressing drugs. Cyclophosphamide, rituximab, and mycophenolate mofetil are among the medications used in these situations, though they lack the same level of clinical trial evidence as the first-line therapies. These drugs work through different mechanisms to suppress immune system activity more broadly or target specific immune cells involved in the autoimmune attack.[10]

Rituximab deserves particular mention as it targets B cells, a type of white blood cell involved in antibody production. This medication has shown promise in clinical experience and is currently being studied in formal clinical trials specifically for chronic inflammatory demyelinating polyradiculoneuropathy. The drug is given as an infusion, typically in a series of doses, and can provide longer-lasting effects than some other treatments. Side effects can include infusion reactions, increased infection risk, and rarely more serious complications.[10]

In rare cases of extremely resistant disease, haematopoietic autologous stem cell transplant has been attempted. This intensive procedure involves collecting a patient’s own stem cells, using chemotherapy to essentially reset the immune system, then reinfusing the saved stem cells to rebuild it. While potentially offering the chance for prolonged remission, this approach carries significant risks and is reserved for the most severe cases that have failed all other treatments.[10]

Emerging Therapies Being Tested in Clinical Trials

Research into new treatment approaches continues actively, driven by the recognition that current therapies don’t work for everyone and often require lifelong administration. Clinical trials test whether experimental treatments are safe and effective before they can be approved for general use. These studies progress through phases: Phase I focuses primarily on safety, Phase II examines whether the treatment works and at what dose, and Phase III compares the new treatment directly against standard care or placebo in larger groups of patients.[2]

Neonatal Fc Receptor Blockers

One of the most promising recent developments involves drugs that block the neonatal Fc receptor, a protein that helps recycle antibodies in the body. By blocking this receptor, these medications accelerate the breakdown and removal of harmful antibodies, including those attacking nerve myelin. This represents a more targeted approach than broadly suppressing the entire immune system.[10]

Efgartigimod has become the first of these drugs to show positive results in a randomized controlled trial for chronic inflammatory demyelinating polyradiculoneuropathy. The study demonstrated that patients taking efgartigimod experienced significantly fewer relapses compared to those receiving placebo, after both groups stopped their previous immunotherapy. This suggests the drug may help maintain stability while reducing dependence on other treatments. Efgartigimod is given as an intravenous infusion.[10]

Other neonatal Fc receptor blockers currently under investigation include nipocalimab and batoclimab. These drugs work through similar mechanisms but may differ in how they’re administered or how long their effects last. Researchers are conducting studies to understand how well these medications work, what side effects they might cause, and which patients might benefit most. Early results appear promising, though more data is needed before these treatments become widely available.[10]

Complement System Inhibitors

The complement system is part of the immune system that helps antibodies and immune cells destroy targets, including—inappropriately in chronic inflammatory demyelinating polyradiculoneuropathy—the myelin sheath. Blocking components of this system represents another targeted approach to treatment. SAR445088 is a drug that inhibits C1, a protein in the early part of the classical complement pathway. By preventing complement activation, this medication aims to reduce nerve damage while potentially causing fewer side effects than broader immune suppression.[10]

Current studies of SAR445088 are enrolling different groups of patients: those who respond well to current treatment, those whose disease is resistant to standard therapies, and those who have never received treatment. This comprehensive approach helps researchers understand whether the drug works in various stages and types of the disease. The medication is being evaluated for both its ability to prevent relapses and to improve symptoms in people with active disease.[10]

Bruton Tyrosine Kinase Inhibitors

Bruton Tyrosine Kinase inhibitors represent another class of drugs being explored for autoimmune conditions. These medications work by blocking an enzyme important for B cell function—the immune cells responsible for producing antibodies. By interfering with B cell activity, these drugs may reduce the production of harmful antibodies attacking nerve myelin. While primarily used in cancer treatment and certain other immune disorders, their potential in chronic inflammatory demyelinating polyradiculoneuropathy is being investigated.[10]

Research into Bruton Tyrosine Kinase inhibitors for this condition is still in earlier stages compared to neonatal Fc receptor blockers. Scientists are working to understand the correct doses, administration schedules, and whether the anti-B cell effects translate into meaningful clinical improvement. As with all experimental treatments, balancing potential benefits against possible side effects remains a key consideration.[10]

⚠️ Important
Participating in clinical trials for chronic inflammatory demyelinating polyradiculoneuropathy offers potential access to cutting-edge treatments before they’re widely available, while contributing to medical knowledge that helps future patients. However, experimental treatments may not work and could cause unexpected side effects. Trials often have specific eligibility requirements and may require frequent medical visits. Discussing the risks and benefits with your healthcare team and thoroughly reviewing the informed consent documents helps ensure clinical trial participation aligns with your personal circumstances and treatment goals.

Beyond Medication: Comprehensive Management Strategies

While immune-modulating treatments address the underlying disease process, comprehensive care for chronic inflammatory demyelinating polyradiculoneuropathy includes supportive therapies that help maintain function and quality of life. Physical therapy plays a crucial role in maintaining muscle strength, improving balance, and preventing complications from immobility. Therapists design exercise programs tailored to individual abilities, ensuring activities strengthen muscles without causing excessive fatigue or injury. Regular exercise has been shown to improve nerve and muscle function when done at appropriate intensity levels.[13]

Occupational therapy helps people adapt daily activities to work around physical limitations. Therapists can recommend assistive devices, suggest modifications to home or work environments, and teach energy-conservation techniques. Simple adaptations—special utensils for eating, grab bars in bathrooms, or tools to help with dressing—can preserve independence and reduce frustration. For people experiencing hand weakness or numbness, occupational therapy exercises can improve grip strength and fine motor control.[3]

Pain management deserves attention, as some people with chronic inflammatory demyelinating polyradiculoneuropathy experience neuropathic pain—a burning, shooting, or electric sensation caused by nerve damage. While pain is less common in this condition than in some other neuropathies, when present it can significantly impact quality of life. Medications specifically for nerve pain, physical modalities like heat or cooling, and complementary approaches may provide relief. Working with a pain specialist can help identify the most effective combination of strategies.[1]

Mental health support is equally important. Living with a chronic, unpredictable condition that affects physical abilities can lead to anxiety, depression, frustration, and fear about the future. These emotional responses are normal and understandable. Connecting with mental health professionals, joining support groups with others facing similar challenges, and maintaining open communication with family and friends helps people cope with the psychological burden of the disease. Some organizations offer online forums and local meetings specifically for people with chronic inflammatory demyelinating polyradiculoneuropathy and their caregivers.[13]

Most Common Treatment Methods

  • Immunoglobulin Therapy
    • Intravenous immunoglobulin (IVIg) infused through veins every three to four weeks, providing donor antibodies that block immune attack on nerves
    • Subcutaneous immunoglobulin (SCIg) administered under the skin weekly, often self-administered at home with training
    • Side effects may include headache, fever, fatigue, and rarely blood clots or kidney problems
    • Often requires long-term or indefinite treatment to maintain symptom control
  • Corticosteroid Medications
    • Prednisone, methylprednisolone, or dexamethasone taken orally or given intravenously
    • Broadly suppress immune system inflammation attacking nerve myelin
    • Common side effects include weight gain, elevated blood sugar, high blood pressure, mood changes, bone weakening, and increased infection risk
    • Typically prescribed at lowest effective dose with gradual tapering when possible
  • Plasma Exchange (Plasmapheresis)
    • Procedure that physically removes harmful antibodies from blood through specialized machine
    • Typically performed several times weekly for a few weeks at medical facility
    • Can produce rapid improvement in severe or rapidly worsening disease
    • Risks include infection, blood pressure changes, bleeding problems, and allergic reactions
  • Additional Immunosuppressive Drugs
    • Cyclophosphamide, rituximab, and mycophenolate mofetil used when first-line treatments fail
    • Work through different mechanisms to suppress immune system or target specific immune cells
    • Rituximab targets B cells involved in antibody production and is currently in clinical trials
    • Generally have less clinical trial evidence but may help treatment-resistant cases
  • Experimental Therapies in Clinical Trials
    • Neonatal Fc receptor blockers (efgartigimod, nipocalimab, batoclimab) that accelerate breakdown of harmful antibodies
    • Complement system inhibitors (SAR445088) that block immune system proteins damaging nerves
    • Bruton Tyrosine Kinase inhibitors affecting B cell function and antibody production
    • Available only through participation in research studies with specific eligibility criteria
  • Supportive Care and Rehabilitation
    • Physical therapy to maintain strength, improve balance, and prevent complications from immobility
    • Occupational therapy providing assistive devices and home modifications to preserve independence
    • Pain management strategies for neuropathic pain when present
    • Mental health support including counseling and support groups

Living With the Condition: Practical Considerations

Managing chronic inflammatory demyelinating polyradiculoneuropathy extends beyond medical treatments to encompass daily life adjustments. The condition’s unpredictability—with symptoms that may fluctuate or gradually worsen—requires flexibility and planning. Many people find that accepting limitations while focusing on what remains possible helps maintain a positive outlook. Setting boundaries around activities, knowing when to rest, and communicating openly with friends and family about changing abilities helps manage social relationships.[12]

Common symptoms like muscle weakness in hands and feet, difficulty walking, balance problems, and fatigue affect everyday tasks. Simple activities such as buttoning clothes, opening jars, carrying groceries, or climbing stairs may become challenging. Some people experience “foot drop”—an inability to lift the front part of the foot—which increases fall risk and makes walking difficult. Adaptive equipment like ankle-foot orthoses, canes, walkers, or wheelchairs can help maintain mobility and safety. Using these aids isn’t giving up; it’s making smart choices to preserve energy and prevent injury.[3]

Diet and lifestyle choices support overall health, though no specific diet has been proven to treat chronic inflammatory demyelinating polyradiculoneuropathy. A balanced, nutritious diet rich in fruits, vegetables, lean proteins, and whole grains provides vitamins and minerals important for nerve health. Some evidence suggests anti-inflammatory foods—including those rich in omega-3 fatty acids like fish and nuts, and foods high in antioxidants—may help reduce inflammation generally. Maintaining a healthy weight prevents extra strain on weakened muscles. Staying well-hydrated and limiting alcohol consumption also support overall wellness.[17]

Employment and financial concerns often arise, as physical limitations may affect job performance or ability to work. Some people need to reduce hours, change job duties, or stop working altogether. Understanding disability rights, exploring workplace accommodations, and investigating financial assistance programs helps address these practical challenges. Social security disability benefits, patient assistance programs for medications, and insurance resources may provide financial support. Healthcare navigators and social workers can help identify available resources.[3]

The disease affects not just patients but also family members and caregivers. Spouses, partners, children, and parents often take on new responsibilities—helping with physical tasks, providing transportation to medical appointments, managing medications, and offering emotional support. Caregiver burden is real, and those supporting someone with chronic inflammatory demyelinating polyradiculoneuropathy need their own support systems. Respite care, caregiver support groups, and attention to their own physical and mental health helps caregivers continue providing care without burning out.[16]

The Importance of Ongoing Monitoring and Follow-Up

Chronic inflammatory demyelinating polyradiculoneuropathy requires regular medical monitoring even when symptoms are stable. The disease can relapse unexpectedly, and early detection of worsening allows for prompt treatment adjustment. Neurologists typically schedule regular appointments to assess muscle strength, sensation, reflexes, and functional abilities. Tracking symptoms through diaries or apps helps both patients and doctors notice subtle changes that might otherwise be missed.[2]

Diagnostic tests may be repeated periodically to objectively measure disease activity. Nerve conduction studies and electromyography (EMG) measure how well electrical signals travel through nerves and can detect changes in nerve function. While these tests can be uncomfortable—involving small electrical shocks and needle insertions—they provide valuable information about treatment effectiveness and disease progression. Blood tests may monitor for side effects of medications, particularly immunosuppressive drugs that can affect blood counts, liver function, or kidney function.[2]

Treatment response varies considerably between individuals. Some people achieve complete remission with minimal ongoing treatment, while others require continuous therapy to maintain stability. Still others experience treatment-resistant disease that doesn’t respond adequately to available options. This variability makes it difficult to predict outcomes for any individual patient. Regular communication with healthcare providers, honest reporting of symptoms and side effects, and patience with the trial-and-error process of finding the right treatment approach are essential components of long-term disease management.[10]

Ongoing Clinical Trials on Chronic inflammatory demyelinating polyradiculoneuropathy

  • A Study of IMVT-1402 in Adults with Chronic Inflammatory Demyelinating Polyneuropathy to Prevent Disease Relapse

    Recruiting

    1
    Investigated diseases:
    Investigated drugs:
    Austria Belgium Bulgaria Denmark Estonia Finland +13

  • Study of DNTH103 Treatment for Adults with Chronic Inflammatory Demyelinating Polyneuropathy: Comparing Effectiveness with Placebo

    Recruiting

    1 1
    Investigated diseases:
    Investigated drugs:
    Belgium Bulgaria Croatia Denmark France Germany +6

  • Study on the Safety and Effects of NVG-2089 for Patients with Chronic Inflammatory Demyelinating Polyneuropathy (CIDP)

    Not recruiting

    1 1
    Investigated diseases:
    Investigated drugs:
    Belgium Bulgaria France Italy Poland Spain

  • Study on the Long-term Safety of Batoclimab for Adults with Chronic Inflammatory Demyelinating Polyneuropathy (CIDP)

    Not recruiting

    1 1
    Investigated diseases:
    Investigated drugs:
    Belgium Bulgaria Denmark Germany Greece Italy +4

  • Study on Batoclimab for Adults with Chronic Inflammatory Demyelinating Polyneuropathy (CIDP)

    Not recruiting

    1
    Investigated diseases:
    Investigated drugs:
    Belgium Bulgaria Denmark Finland Germany Greece +8

  • Study on the Effects of Riliprubart for Adults with Chronic Inflammatory Demyelinating Polyneuropathy (CIDP)

    Not recruiting

    1 1 1
    Investigated diseases:
    Investigated drugs:
    France Germany Italy The Netherlands Poland Spain

  • Study Comparing Subcutaneous and Intravenous Human Normal Immunoglobulin for New Patients with Chronic Inflammatory Demyelinating Polyneuropathy (CIDP)

    Not recruiting

    1 1 1 1
    Investigated diseases:
    Investigated drugs:
    Denmark

References

https://my.clevelandclinic.org/health/diseases/cidp-chronic-inflammatory-demyelinating-polyneuropathy

https://www.ncbi.nlm.nih.gov/books/NBK563249/

https://www.knowingpn.com/cidp/about-cidp

https://www.gbs-cidp.org/cidp/

https://www.vaccineinjuryteam.com/blog/2023/november/first-symptoms-of-chronic-inflammatory-demyelina/

https://medlineplus.gov/ency/article/000777.htm

https://en.wikipedia.org/wiki/Chronic_inflammatory_demyelinating_polyneuropathy

https://my.clevelandclinic.org/health/diseases/cidp-chronic-inflammatory-demyelinating-polyneuropathy

https://pmc.ncbi.nlm.nih.gov/articles/PMC5468847/

https://pmc.ncbi.nlm.nih.gov/articles/PMC10906673/

https://www.gbs-cidp.org/cidp/

https://www.shiningthroughcidp.com/everyday-life-with-cidp/adapting-your-social-life

https://www.cidphub.com.au/living-cidp

https://my.clevelandclinic.org/health/diseases/cidp-chronic-inflammatory-demyelinating-polyneuropathy

https://www.hizentra.com/cidp/understanding-cidp/

https://www.gbs-cidp.org/cidp/loved-one-or-friend-with-cidp/

https://ameripharmaspecialty.com/cidp/what-is-a-healthy-diet-for-cidp/

https://www.healthline.com/program/living-with-chronic-inflammatory-demyelinating-polyradiculoneuropathy

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FAQ

What is the difference between CIDP and Guillain-Barré syndrome?

Both conditions involve autoimmune attack on peripheral nerve myelin, but Guillain-Barré syndrome develops rapidly—reaching its worst point within two to three weeks—and most people then begin recovering. Chronic inflammatory demyelinating polyradiculoneuropathy progresses more slowly, with symptoms worsening over at least eight weeks, and often requires long-term treatment. Healthcare providers consider CIDP the chronic form of Guillain-Barré syndrome.

Can CIDP go into remission without treatment?

While remission is possible, it’s relatively uncommon without treatment, and untreated disease risks permanent nerve damage. Early treatment significantly improves the chances of recovery and helps prevent irreversible disability. Some people do achieve remission with treatment and may be able to stop therapy, though many require ongoing treatment to maintain stability and prevent relapse.

How long do I need to continue treatment for CIDP?

Treatment duration varies greatly between individuals. Some people need therapy for only months to a few years, while others require lifelong treatment. The disease can relapse when treatment stops, so doctors typically monitor closely when attempting to reduce or discontinue therapy. Regular follow-up allows early detection of relapse and prompt treatment restart if needed.

Are there any vaccines I should avoid if I have CIDP?

Most people with chronic inflammatory demyelinating polyradiculoneuropathy can safely receive standard vaccines, and vaccination against serious infections like influenza and pneumonia is generally recommended. However, you should discuss your vaccination schedule with your neurologist, especially if you’re taking immunosuppressive medications. While rare cases of CIDP following vaccination have been reported, the risk of serious infection typically outweighs vaccination concerns.

Will I eventually need a wheelchair?

Not everyone with chronic inflammatory demyelinating polyradiculoneuropathy requires a wheelchair. Many people maintain the ability to walk with or without assistive devices like canes or walkers, especially with early diagnosis and effective treatment. Some use wheelchairs temporarily during severe relapses, while others find them helpful for conserving energy during longer outings even when they can walk short distances. Using mobility aids when needed helps maintain independence and prevent falls rather than representing treatment failure.

🎯 Key Takeaways

  • Three evidence-based first-line treatments—immunoglobulin therapy, corticosteroids, and plasma exchange—form the foundation of care for chronic inflammatory demyelinating polyradiculoneuropathy, though choosing among them depends on individual circumstances and preferences.
  • The unpredictable nature of CIDP, with its pattern of possible relapses and remissions, makes long-term monitoring essential even when symptoms are stable.
  • Exciting new treatments targeting neonatal Fc receptors and complement system proteins are showing promise in clinical trials, potentially offering more targeted approaches with fewer side effects than current broad immune suppression.
  • Physical and occupational therapy aren’t just add-ons—they’re crucial components of comprehensive care that help maintain function, prevent complications, and preserve independence in daily activities.
  • Early treatment makes a profound difference in outcomes, with prompt intervention helping prevent permanent nerve damage that becomes irreversible once it occurs.
  • Living successfully with CIDP extends beyond medical treatments to include practical adaptations, mental health support, caregiver assistance, and connecting with others who understand the unique challenges of this rare condition.
  • Treatment response varies dramatically between individuals—what works well for one person may not suit another, requiring patience and willingness to try different approaches to find the most effective strategy.
  • While no cure currently exists, many people with chronic inflammatory demyelinating polyradiculoneuropathy achieve good symptom control and maintain quality of life through appropriate treatment and comprehensive disease management.

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