[ i ] For Patients & Carers — Educational Information Only
This page provides factual clinical background about a class of licensed biologic medicine. It is not an advertisement and does not constitute a recommendation to seek any specific treatment. This page does not promote a prescription-only medicine to the public in accordance with Regulation 279 of the Human Medicines Regulations 2012. All treatment decisions must be made with a qualified clinician following individual assessment.

Reviewed by: Clinical team at the London Allergy & Immunology Centre |
Last reviewed: June 2026 |

Biological Treatment for Nasal Polyps and Atopic Dermatitis

Clinical Information — Prescription Biologic Therapy • London Allergy & Immunology Centre

[ ! ] Important — Prescription-Only Medicine
The biologic therapy described on this page (an IL-4 receptor alpha inhibitor) is a prescription-only medicine (POM) in the United Kingdom. It cannot be obtained without a prescription from a registered medical practitioner. Full prescribing information is available in the
Summary of Product Characteristics (SmPC) on the Electronic Medicines Compendium.

This treatment inhibits IL-4 and IL-13 signalling via IL-4Rα, reducing type 2 inflammation associated with chronic rhinosinusitis with nasal polyps and atopic dermatitis

Our London allergy consultants are specialists in a NICE-recommended biologic therapy that targets the underlying type 2 inflammatory pathway driving two related conditions: severe chronic rhinosinusitis with nasal polyps (CRSwNP) and moderate-to-severe atopic dermatitis (eczema). Where topical treatments, oral corticosteroids, or surgery have not provided adequate long-term disease control, this IL-4/IL-13 pathway inhibitor may represent a clinically appropriate next step — subject to full clinical assessment.

1.4M+

Patients treated
globally

60+

Countries with
regulatory approval

NICE

TA1134 (Feb 2026)

CRSwNP

NICE

TA534 (2018)

Atopic Dermatitis

What Is This Biologic Treatment?

This treatment is a fully human monoclonal antibody that acts on the interleukin-4 receptor alpha (IL-4Rα) subunit, blocking the simultaneous signalling of both IL-4 and IL-13 — the two principal cytokines driving type 2 inflammation in the upper airway and skin. It is licensed in the United Kingdom by the MHRA for the following indications:

Severe CRSwNP in adults aged 18 and over, as add-on therapy to intranasal corticosteroids when disease is inadequately controlled
Moderate-to-severe atopic dermatitis in adults and adolescents aged 12 and over (and for certain regimens, children aged 6 months and older) where topical therapies have failed or are unsuitable

Biologic medicine: Unlike conventional small-molecule drugs, this is a large-molecule biological treatment that must be administered by subcutaneous (under-the-skin) injection. It cannot be taken by mouth.

Mechanism of Action: Targeting Type 2 Inflammation

Both chronic rhinosinusitis with nasal polyps and atopic dermatitis share a common pathophysiological driver — dysregulation of the type 2 (T2) immune pathway. This anti-IL-4/IL-13 biologic works by binding to the IL-4Rα subunit, simultaneously blocking two key inflammatory cytokines:

›› Interleukin-4 (IL-4)

Promotes T-helper 2 cell differentiation, drives IgE production, and sustains the chronic inflammatory cascade in both the sinuses and the skin.

›› Interleukin-13 (IL-13)

Directly stimulates mucus overproduction, nasal polyp growth, skin barrier disruption, and intense itch via epithelial and stromal cell signalling.

By blocking both cytokines simultaneously via the shared IL-4Rα receptor, this biologic delivers a broad and sustained reduction in type 2 inflammation across the upper airway, lower airway, and skin — making it clinically relevant for patients with overlapping type 2 conditions such as asthma, CRSwNP, and eczema.¹

Clinical Evidence and Current Guidelines

Nasal Polyps (CRSwNP)

The landmark Phase 3 SINUS-24 and SINUS-52 trials (Bachert et al., Lancet 2019) demonstrated statistically significant improvements in nasal polyp score, nasal congestion, and loss of the sense of smell compared with placebo, with clinically meaningful benefits observed as early as two weeks after starting treatment.¹ Rates of revision surgery and systemic corticosteroid rescue were also significantly reduced.

In February 2026, NICE published Technology Appraisal TA1134, recommending this IL-4Rα inhibitor as an add-on treatment to intranasal corticosteroids for eligible adults with severe CRSwNP.² Published NICE eligibility criteria include:

Severe CRSwNP inadequately controlled with intranasal corticosteroids
At least one prior sinus surgery
A SNOT-22 symptom score of 50 or above at the start of treatment
Treatment continuation assessed at 24 weeks using validated outcome measures

Atopic Dermatitis (Eczema)

The LIBERTY AD programme, including the pivotal CHRONOS trial (Blauvelt et al., Lancet 2017), established the efficacy of this anti-IL-4/IL-13 biologic in moderate-to-severe atopic dermatitis inadequately controlled by topical therapies. Significant reductions in itch and skin inflammation were demonstrated compared to placebo, with responses generally emerging within four to six weeks.³ Long-term extension data beyond three years continue to support a favourable benefit–risk profile.

NICE Technology Appraisal TA534 (2018) recommends this biologic for adults whose eczema has not responded adequately to at least one systemic therapy (such as ciclosporin, methotrexate, azathioprine, or mycophenolate mofetil), or where these are contraindicated or not tolerated.⁴ Response is assessed at 16 weeks using EASI and DLQI scores.

The 2025–2026 updated EuroGuiDerm guidelines (Wollenberg et al., JEADV 2025) and the UK STRIVE AD consensus (Luger et al., JEADV 2026) both provide a strong recommendation for this class of IL-4Rα inhibitor as the benchmark biologic for moderate-to-severe atopic dermatitis, reflecting an extensive safety record across age groups from 6 months upwards.^5,6

Limitations of the evidence: Clinical trial participants may not represent all real-world populations. Individual responses vary. Not all patients achieve an adequate response, and treatment should be discontinued if there is no clinically meaningful improvement at the scheduled review point. These outcomes should be discussed in full with your clinician.

Who May Be Suitable for This Treatment?

Following comprehensive clinical assessment, this biologic may be a consideration for patients with one or more of the following:

✓	Severe nasal polyps not adequately controlled by intranasal corticosteroids or systemic steroids, or recurring after prior sinus surgery
✓	Moderate-to-severe eczema that has failed to respond to conventional systemic treatments, or where those treatments are contraindicated or not tolerated
✓	Co-existing type 2 conditions such as asthma, allergic rhinitis, food allergy, or eosinophilic oesophagitis — the shared IL-4/IL-13 pathway means improvements may be seen across multiple conditions simultaneously
✓	Frequent courses of oral steroids and a wish to reduce long-term corticosteroid exposure and its associated systemic risks
✓	Significant quality of life impairment including sleep disturbance, loss of sense of smell, facial pressure and pain, or chronic skin discomfort

Safety Information

The following is a summary only. Always read the full Patient Information Leaflet and discuss your complete medical history, current medicines, and any concerns with your prescribing clinician before starting treatment. The complete safety profile, including rare and very rare adverse reactions and all contraindications, is available in the SmPC and Patient Information Leaflet.

Commonly reported adverse reactions

Injection site reactions — redness, mild swelling, or discomfort; generally transient
Conjunctivitis (eye irritation or inflammation) — more frequently reported in patients with atopic dermatitis; typically manageable
Blepharitis (eyelid inflammation) — reported in some patients with atopic dermatitis
Keratitis (corneal inflammation) — less common; report any eye pain or visual changes to your clinician promptly
Oral herpes (cold sores) — reported at higher rates than placebo in some clinical trials
Transient eosinophilia (temporary rise in white blood cell count) — generally clinically insignificant but monitored
Headache — reported in clinical trials

Important safety considerations

This biologic acts on a specific inflammatory pathway and does not broadly suppress the immune system. However, it should only be initiated and monitored by a suitably qualified specialist.
Live vaccines must not be administered during treatment. Discuss your vaccination history with your clinician before starting.
Inform your clinician of all medicines — including over-the-counter products and supplements — before starting this treatment.
Use in pregnancy and breastfeeding: data are limited. Discuss the benefits and risks with your clinician if you are pregnant, planning a pregnancy, or breastfeeding.
Report any new or worsening symptoms — particularly eye symptoms, skin infections, or allergic reactions — to your clinical team promptly.

This is not a complete list of side effects. You can also report suspected side effects directly to the MHRA via the Yellow Card scheme.

Accessing This Treatment Through Our Clinic

This is a prescription-only biologic therapy that can only be initiated by a suitably qualified specialist following thorough individual clinical assessment. London Allergy & Immunology Centre is a private specialist clinic offering assessment and, where clinically appropriate following individual evaluation, initiation of biologic therapies. All treatment decisions are made by our consultants following your consultation.

Please note: This is a private clinic. Private assessment and treatment involve costs for consultation, investigations, and the medicine itself, which your clinician will discuss transparently with you in advance.

What a Clinical Assessment Involves

1	Comprehensive Initial Assessment A detailed consultation with one of our allergy consultants, including full review of your medical history, symptom severity scoring (SNOT-22 for nasal symptoms; EASI and DLQI for eczema), and impact on quality of life.
2	Investigations and MDT Review Depending on your presentation, this may include allergy testing (skin prick testing, specific IgE blood tests), spirometry, ENT assessment, or dermatology review. We operate a multidisciplinary approach with allergy, ENT, and dermatology consultants.
3	Discussion of All Appropriate Options Your clinician will discuss all treatment options relevant to your diagnosis — this biologic therapy is one of several possible approaches. Alternatives, risks, and benefits will all be explained before any treatment decision is made.
4	Treatment Initiation and Ongoing Monitoring If biologic therapy is dispensed by specialised pharmacy and initiated. A structured monitoring schedule using validated outcome measures. Direct access to our clinical team is available between appointments should any concerns arise.

Frequently Asked Questions

How quickly does this treatment work?

Clinical trials report meaningful improvements in nasal symptoms within as early as two weeks for CRSwNP,¹ and significant reductions in itch and skin inflammation within four to six weeks for atopic dermatitis.³ Full benefit typically continues to develop over three to six months. Not all patients respond, and your clinician will assess your response at defined review points.

Is this biologic safe for long-term use?

Long-term clinical trial data extending beyond three years, alongside ongoing post-marketing pharmacovigilance, support a favourable safety profile. Because this treatment acts on a specific pathway rather than broadly suppressing immunity, it does not carry the increased risk of serious opportunistic infections associated with conventional immunosuppressants.^5,6 Ongoing monitoring is required and will be structured into your treatment plan.

I have both nasal polyps and eczema — can one treatment address both?

Because both conditions share the same underlying type 2 inflammatory pathway driven by IL-4 and IL-13, this IL-4Rα inhibitor holds regulatory approvals for both indications. Clinical trials have also reported improvements in co-existing asthma in some patients. Whether it is appropriate for your specific combination of conditions requires individual clinical assessment.

Do I need to continue using intranasal steroids alongside this biologic?

For CRSwNP, NICE TA1134 recommends this treatment as add-on therapy to intranasal corticosteroids. For atopic dermatitis, it is typically used alongside topical therapies, though many patients are able to substantially reduce their topical steroid use once their condition is controlled. Your clinician will advise on the full regimen appropriate for you.

What if this treatment does not work for me?

Response is assessed at defined time points using validated tools: 16 weeks for atopic dermatitis (EASI/DLQI) and 24 weeks for CRSwNP (SNOT-22/nasal polyp score). If there is no adequate response, treatment should be discontinued and alternative options discussed. Your clinician will advise on next steps.

Are there other biologic options for these conditions?

Yes. Other biologic therapies targeting different parts of the type 2 inflammatory pathway are licensed or in development for CRSwNP and atopic dermatitis. Your clinician will review all options relevant to your individual circumstances and explain which may be most appropriate for you.

Further Information and Resources

References

Bachert C et al. Efficacy and safety of dupilumab in patients with severe chronic rhinosinusitis with nasal polyps (SINUS-24 and SINUS-52). Lancet. 2019;394(10209):1638–1650. doi:10.1016/S0140-6736(19)31881-1
National Institute for Health and Care Excellence. Technology Appraisal TA1134: biologic therapy for treating severe chronic rhinosinusitis with nasal polyps. NICE; February 2026. nice.org.uk/guidance/ta1134
Blauvelt A et al. Long-term management of moderate-to-severe atopic dermatitis with dupilumab and concomitant topical corticosteroids (LIBERTY AD CHRONOS). Lancet. 2017;389(10086):2287–2303. doi:10.1016/S0140-6736(17)31191-1
National Institute for Health and Care Excellence. Technology Appraisal TA534: biologic therapy for treating moderate to severe atopic dermatitis. NICE; 2018. nice.org.uk/guidance/ta534
Wollenberg A et al. EuroGuiDerm guideline on atopic eczema — updated recommendations including IL-4Rα inhibitor therapy across age groups. J Eur Acad Dermatol Venereol. 2025. doi:10.1111/jdv.20639
Luger T et al. STRIVE AD: UK consensus statements for optimised management of atopic dermatitis. J Eur Acad Dermatol Venereol. 2026. doi:10.1111/jdv.20640

Disclaimer and Regulatory Statement
This page provides factual, educational information about a class of licensed prescription-only biologic medicine. It does not constitute an advertisement for a prescription-only medicine directed at the public as defined under Regulation 279 of the Human Medicines Regulations 2012, nor does it constitute medical advice. All treatment decisions must be made by a qualified clinician following individual assessment. Information is accurate to the best of our knowledge as of June 2026 and will be reviewed annually or sooner if significant changes occur. Our clinicians are registered with the General Medical Council (GMC).