argenx Presents New Efgartigimod Data Showing Long-Term Sustained Patient Benefit in Myositis and Sjogren’s Disease at EULAR 2026

Rhea-AI Summary

argenx (NASDAQ:ARGX) reported new VYVGART (efgartigimod) data in myositis and Sjogren’s disease at EULAR 2026, highlighting sustained benefit and consistent safety.

ALKIVIA+ 52‑week myositis data showed maintained Total Improvement Scores, while RHO+ Sjogren’s results indicated maintained or improved disease activity on long-term, including biweekly dosing, with a reinforced cross-indication safety profile across 834 patients and 1,300+ patient‑years.

AI-generated analysis. Not financial advice.

Positive

• In myositis, 37.5% on continuous efgartigimod maintained major TIS improvement at week 52
• Myositis patients switching from placebo saw 33.3% major and up to 66.7% moderate TIS improvement
• Mean TIS at week 52 remained high: 52.19 (continuous) and 49.62 (placebo-switch) in ALKIVIA+
• Sjogren’s patients switching to biweekly efgartigimod maintained response on clinical measures in RHO+
• At week 72, median ClinESSDAI scores were low (2.5 vs 2.0) in both Sjogren’s groups
• Cross‑indication safety data cover 834 patients and 1,300+ patient‑years with predominantly mild-to-moderate adverse events

Negative

• None.

Key Figures

Major TIS maintained: 37.5% Major TIS after switch: 33.3% Moderate TIS continuous: 75.0% +5 more

8 metrics

Major TIS maintained 37.5% ALKIVIA+ myositis patients continuously on efgartigimod at week 52

Major TIS after switch 33.3% Patients switching from placebo to efgartigimod at week 52

Moderate TIS continuous 75.0% Continuous efgartigimod group with TIS ≥40 at week 52

Moderate TIS switch 66.7% Placebo-to-efgartigimod group with TIS ≥40 at week 52

Mean TIS continuous 52.19 Mean Total Improvement Score at week 52, continuous efgartigimod

Mean TIS switch 49.62 Mean Total Improvement Score at week 52, placebo-to-efgartigimod

ClinESSDAI efgartigimod 2.5 Median ClinESSDAI at week 72 in Sjogren’s efgartigimod arm

Safety population 834 patients; >1,300 patient-years Cross-indication efgartigimod safety database

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Peers on Argus

ARGX fell 4.06% while key biotech peers were mixed: REGN up 1.07%, ALNY down 2.7...

ARGX fell 4.06% while key biotech peers were mixed: REGN up 1.07%, ALNY down 2.73%, VRTX down 1.69%, ONC down 1.24%. With no peers in the momentum scanner and no same-day peer news, today’s move appears stock-specific rather than a broad sector rotation.

Historical Context

5 past events · Latest: May 28 (Neutral)

Pattern 5 events

Date	Event	Sentiment	Move	Catalyst
May 28	R&D webinar announcement	Neutral	+2.2%	Myositis-focused R&D webinar on FcRn biology and ALKIVIA program.
May 27	Investor conferences	Neutral	+1.5%	Participation in two June 2026 healthcare investor conferences.
May 18	Partner pipeline update	Neutral	-2.9%	Partner MindWalk highlighted multiple antibody programs including work with argenx.
May 08	FDA label expansion	Positive	+4.0%	U.S. FDA approval expanding VYVGART labels to all adult gMG serotypes.
May 07	Earnings and update	Positive	-2.5%	Strong Q1 2026 results and pipeline update including multiple upcoming readouts.

Pattern Detected

Recent ARGX news has often led to directional moves, with positive regulatory and R&D updates generally met with gains, while strong earnings sometimes saw profit-taking. Reactions show a mix of three aligned and two divergent outcomes.

Recent Company History

Over the past few months, argenx has combined strong financial execution with expanding clinical and regulatory momentum. Q1 2026 results on May 7 highlighted substantial profitability and growth, followed by a U.S. FDA label expansion for VYVGART in gMG on May 8, which was met with a 3.98% gain. The company also announced investor conferences and a myositis-focused R&D webinar in late May, each coinciding with modest share price moves. Today’s new rheumatology data extend that narrative of broadening efgartigimod’s autoimmune footprint.

Market Pulse Summary

This announcement highlights sustained functional improvements and favorable safety for efgartigimod...

Analysis

This announcement highlights sustained functional improvements and favorable safety for efgartigimod across myositis and Sjogren’s disease, supported by long-term data up to 52 and 72 weeks and a safety set of 834 patients with over 1,300 patient‑years. In context of argenx’s recent regulatory wins and strong financial performance, these rheumatology data underscore continued pipeline diversification. Investors may monitor upcoming Phase 3 readouts and further autoimmune indications to gauge how broadly the FcRn franchise can extend.

Key Terms

fcrn, total improvement score (tis), phase 2, phase 3, +3 more

7 terms

fcrn medical

"support the rationale for targeting FcRn in autoimmune rheumatic diseases"

The neonatal Fc receptor (FCRN or FcRn) is a protein that controls how long antibodies and the blood protein albumin stay in circulation by protecting them from being broken down. For investors, therapies that block or harness FcRn can change a drug’s dosing, effectiveness and market appeal—either by lengthening beneficial antibodies for longer-lasting treatments or by reducing harmful antibodies in autoimmune disease—so progress in FcRn-targeted programs can materially affect a biotech’s commercial value.

total improvement score (tis) medical

"A key metric in ALKIVIA+ is Total Improvement Score (TIS). TIS is a composite"

Total Improvement Score (TIS) is a single numeric summary that combines several individual clinical measures into one percentage or point value to show how much patients improved in a trial. For investors, TIS turns complex medical results into an easy-to-compare “overall grade” that can influence regulators, prescribing labels and market confidence—so a higher TIS often supports a stronger commercial and regulatory outlook.

phase 2 medical

"completed the 24-week, double-blind, placebo-controlled Phase 2 ALKIVIA trial"

Phase 2 is the mid-stage clinical trial where a new drug or treatment is tested in a larger group of patients to see if it works and to keep checking safety after initial human testing. Think of it as a field test that proves whether a product actually delivers its promised benefit. Investors watch Phase 2 closely because its results strongly influence a medicine’s chances of reaching the market, the size of its potential sales, and the company’s valuation.

phase 3 medical

"Topline results from the Phase 3 ALKIVIA study are expected in the third quarter"

Phase 3 is the late-stage clinical testing step for a new drug or medical treatment, where the product is given to large groups of patients to confirm effectiveness, monitor side effects, and compare it to standard care. Successful Phase 3 results are often the final scientific hurdle before regulators decide on approval and market launch—like passing a final exam before graduation—and can sharply change a company's valuation and future revenue prospects.

open-label extension medical

"ALKIVIA+ is an ongoing open-label extension study that enrolled patients"

An open-label extension is a continuation of a clinical trial where all participants and researchers know which treatment is being given, often after an initial blinded phase. It allows further study of a drug's long-term safety and effectiveness. For investors, it can indicate ongoing interest and confidence in a product's potential, influencing perceptions of its future value.

cress medical

"assessed using the Composite of Relevant Endpoints for Sjogren’s Syndrome (CRESS)"

Cress is a group of small, fast-growing leafy plants eaten raw or lightly cooked for a peppery, mustard-like flavor, similar to salad greens with a spicy kick. Investors pay attention to cress in company announcements because it can influence product recipes, ingredient costs, supply-chain risks, safety or regulatory scrutiny, and consumer demand—like how one key ingredient can alter a food product’s appeal and profit margins.

igg-mediated autoimmune diseases medical

"clinical trials in Immunoglobulin G-Mediated Autoimmune Diseases With Emerging Data"

IgG-mediated autoimmune diseases are conditions in which the body's IgG antibodies, a common class of immune proteins, mistakenly attack the body's own cells or tissues—like well-trained soldiers turning on their own side. For investors, these diseases matter because they define a clear biological target for therapies, influence the size and urgency of drug and diagnostic markets, and affect regulatory and reimbursement prospects tied to treatment effectiveness and safety.

AI-generated analysis. Not financial advice.

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• ALKIVIA+ data in myositis indicate efgartigimod provides sustained, clinically meaningful improvements and consistent safety
• RHO+ data in Sjogren’s disease indicate maintenance of response following switch to biweekly dosing
• Cross-indication analysis of efgartigimod data across rheumatology studies underscores consistent safety profile in large patient population
  
  

June 3, 2026, 7:00 AM CEST

Amsterdam, the Netherlands – argenx SE (Euronext & Nasdaq: ARGX), a global immunology company committed to improving the lives of people suffering from severe autoimmune diseases, today announced the presentation of new data evaluating VYVGART® (IV: efgartigimod alfa-fcab and SC or Hytrulo: efgartigimod alfa and hyaluronidase-qvfc) across autoimmune rheumatic diseases, including myositis and Sjogren’s disease, to be presented at the European Alliance of Associations for Rheumatology (EULAR) 2026 Congress from June 3-6, 2026, in London, UK.

“Our presentations at EULAR further support the rationale for targeting FcRn in autoimmune rheumatic diseases and underscore its potential to address significant unmet patient need,” said Luc Truyen, M.D., Ph.D., Chief Medical Officer at argenx. “We are encouraged by the consistency of the long-term data as well as data underscoring efgartigimod's favorable safety profile across multiple autoimmune rheumatic diseases. We are looking forward to additional results evaluating efgartigimod in myositis later this year as well as in Sjogren’s disease next year.”

Myositis and Sjogren’s disease are both chronic, progressive autoimmune diseases that are generally more common in women than men. Myositis can cause serious and irreversible damage to muscles and organs, leading to a loss of independence and a significant burden for patients. Sjogren’s disease can cause dry eyes and mouth, chronic fatigue, and joint pain. It can also affect multiple organ systems and lead to nervous system complications.

Efgartigimod provides sustained functional improvement in patients with myositis

ALKIVIA+ is an ongoing open-label extension study that enrolled patients who completed the 24-week, double-blind, placebo-controlled Phase 2 ALKIVIA trial, including those who continued efgartigimod treatment and those who transitioned from placebo to efgartigimod. Results presented at EULAR are an interim analysis through Week 52.

A key metric in ALKIVIA+ is Total Improvement Score (TIS). TIS is a composite index based on six core set measures, including muscle strength, physician and patient global assessments of disease activity, physical function, enzyme levels, and extramuscular activity. Higher TIS values reflect greater overall clinical improvement. Moderate and major improvement are defined as TIS ≥40 and ≥60, respectively.

Results showed:

• At 52 weeks, 37.5% of patients who had continuously received efgartigimod maintained their major TIS improvement from week 24. 33.3% of patients switching from placebo to efgartigimod achieved a similar major TIS improvement. Rates of moderate TIS improvement were also similar between the groups, at 75.0% and 66.7%, respectively.
• Sustained mean TIS benefit: Patients receiving continuous efgartigimod maintained clinically meaningful improvement through 52 weeks, with a mean TIS of 52.19. Patients who switched from placebo to efgartigimod achieved comparable improvement, with a mean TIS of 49.62 at week 52.
• The safety profile was consistent over the course of the study, with no increase in adverse events with longer exposure.
• These results further support the mechanistic relevance of FcRn blockade in myositis, providing further evidence that pathogenic autoantibodies are the underlying driver of disease.

“Patients with autoimmune myositis face the serious challenge that their immune system attacks their own body, causing irreversible muscle loss, weakness, pain and reduced quality of life, while the limited available treatments can carry significant side effects and be difficult to tolerate long term,” said Hector Chinoy, M.D., Ph.D., presenting study author and Professor of Rheumatology and Neuromuscular Disease at The University of Manchester. “Emerging results from the ALKIVIA+ study suggest that efgartigimod has the potential to deliver meaningful and sustained clinical benefit for patients with myositis, with a favorable tolerability profile.”

Topline results from the Phase 3 ALKIVIA study are expected in the third quarter of 2026.

Efgartigimod achieved maintenance of response in Sjogren’s disease

RHO+, a 48-week open-label extension study, evaluated patients with Sjogren's disease who continued to receive efgartigimod, and those who transitioned from placebo to efgartigimod after completing the 24-week double-blind treatment period of the Phase 2 RHO study.

Response to efgartigimod was assessed using the Composite of Relevant Endpoints for Sjogren’s Syndrome (CRESS), a composite endpoint designed to capture overall treatment benefit across multiple clinical domains, including disease activity as measured by ClinESSDAI. Patients in the efgartigimod arm were switched to biweekly dosing based on ClinESSDAI response.

Results showed:

• Patients in the efgartigimod arm switching to biweekly dosing experienced maintenance of response on clinical measures.
• Patients in the placebo arm switching to efgartigimod experienced improvements in ClinESSDAI and increased CRESS response.
• At week 72, median ClinESSDAI scores were low in both groups: 2.5 in the efgartigimod arm and 2.0 in patients who transitioned from placebo to efgartigimod. Low disease activity is indicated by a ClinESSDAI score of <5.
• Efgartigimod was well tolerated, with no new safety signals identified following long-term use in participants with Sjogren’s disease.

The Phase 3 UNITY trial is currently ongoing to assess efficacy and safety of efgartigimod in patients with moderate to severe Sjogren’s disease. Topline results are expected in the second half of 2027.

Efgartigimod safety profile reinforced across autoantibody-driven autoimmune diseases

A cross-indication safety analysis of efgartigimod spanning multiple global clinical studies, including autoimmune rheumatic diseases, indicated that efgartigimod is consistently well-tolerated across diseases and administration methods.

• Data showed a consistent safety profile across 834 treated patients and more than 1,300 patient-years of follow-up. Efgartigimod was well tolerated in participants with autoimmune rheumatic diseases (myositis, Sjogren's disease, and lupus nephritis), consistent with findings from prior studies in other IgG-mediated autoimmune diseases and also consistent with what has been observed in approved indications globally.
• Adverse events were predominantly mild-to-moderate, and no increased event rates were seen in studies with a longer treatment duration.

Deepening understanding of the underlying biology

Additional argenx activities include: the presentation of the Phase 2 eSScape study design, evaluating the potential of efgartigimod in Systemic Sclerosis (SSc); an FcRn symposium exploring the role of autoantibodies in autoimmune rheumatic diseases and highlighting the potential of targeting FcRn; and the launch of a new myositis disease education campaign.

argenx additional information on the data at EULAR 2026 can be found here. Details for argenx presentations are as follows:

Title	Lead Author	Presentation
Myositis
The Long-Term Safety and Efficacy of Efgartigimod PH20 SC in Adult Participants With Active Idiopathic Inflammatory Myopathy: Results From the Phase 2 Randomized ALKIVIA and Open-Label Extension ALKIVIA+ Trials	Rohit Aggarwal	Poster #POS0261 Friday, June 5 13:36 BST
Sjogren’s Disease
Long-Term Efficacy and Safety of Efgartigimod in Sjogren’s Disease: Findings from the RHO+ Open-Label Extension Study	Isabelle Peene	Oral Presentation #130 Wednesday, June 3 17:30-17:40 BST
Systemic Sclerosis
Efgartigimod PH20 Subcutaneous in Adults With Systemic Sclerosis: Design of a Phase 2, Randomized, Double-Blinded, Placebo-Controlled, Parallel-Group Study (eSScape)	Dinesh Khanna	Poster #POS0326 Friday, June 5 16:30 BST
Multiple Disease Areas
Safety Profile of Efgartigimod Across Multiple Global Clinical Trials in Immunoglobulin G-Mediated Autoimmune Diseases With Emerging Data in Idiopathic Inflammatory Myopathy, Sjogren’s Disease, and Lupus Nephritis	Hector Chinoy	Poster #POS1200 Saturday, June 6 10:15 BST

About Efgartigimod and Efgartigimod SC

Efgartigimod (efgartigimod alfa fcab) is a human IgG1 antibody fragment that binds to the neonatal Fc receptor (FcRn), resulting in the reduction of circulating IgG autoantibodies. It is the first approved FcRn blocker for the treatment of generalized myasthenia gravis (gMG) and chronic inflammatory demyelinating polyneuropathy (CIDP) globally, and for primary immune thrombocytopenia (ITP) in Japan. Efgartigimod SC is a subcutaneous combination of efgartigimod alfa and recombinant human hyaluronidase PH20 (rHuPH20), Halozyme’s ENHANZE® drug delivery technology to facilitate subcutaneous injection delivery of biologics.

About Myositis

Myositis is an autoimmune rheumatic disease that can be progressive and may lead to significant muscle and organ involvement, resulting in functional impairment and substantial burden for patients. It is characterized by skeletal muscle weakness with possible extramuscular manifestations involving the skin, joints, lungs, gastrointestinal tract, and heart. Major subtypes include immune-mediated necrotizing myopathy (IMNM), dermatomyositis (DM), polymyositis (PM), antisynthetase (ASyS), and inclusion body myositis, with muscle involvement being a common manifestation across most subtypes.

About ALKIVIA and ALKIVIA+ Study Design

The ALKIVIA study is a randomized, double-blind, placebo-controlled, multicenter, operationally seamless Phase 2/3 study of efgartigimod SC for the treatment of autoimmune myositis across IMNM, DM and PM. The ALKIVIA study enrolled 240 patients in total and is being conducted in two phases, with an analysis of the Phase 2 portion of the clinical trial after the first 90 patients completed the study, followed by a Phase 3 portion if a signal is observed in the Phase 2 portion. The primary endpoint is the mean total improvement score (TIS) at the end of the treatment period (24 weeks in Phase 2 and 52 weeks in Phase 3) of all treated patients (IMNM, DM and PM) compared to placebo. Key secondary endpoints include response rates at the end of treatment, time to response, and duration of response in TIS, as well as change from baseline in individual TIS components. Other secondary endpoints include quality of life and other functional scores. ALKIVIA+ is a 28-week open-label extension study that evaluated myositis patients who received continuous efgartigimod treatment and those who transitioned from placebo to efgartigimod after completing the 24-week double-blind, placebo-controlled Phase 2 ALKIVIA study. The primary endpoint of ALKIVIA+ is long-term safety and tolerability.

About Sjogren’s Disease

Sjogren’s disease is a chronic and progressive, systemic, autoimmune rheumatic disease associated with elevated autoantibodies and characterized by immune-mediated dysfunction of exocrine glands and extraglandular organ manifestations. Sjogren's disease can be severely debilitating and have a negative impact on patient quality of life, with common symptoms reported as dry eyes and mouth, fatigue, and joint pain. Sjogren's disease predominantly impacts women with a 9:1 female:male incidence ratio. Given the heterogeneous nature of the disease, the treatment journey can be challenging with long delays and high rates of misdiagnosis. There are no FDA-approved treatments targeting the disease itself, leaving current treatments to focus primarily on individual symptom management.

About RHO and RHO+ Study Design

The Phase 2 RHO study was a randomized, double-blinded, placebo-controlled multicenter proof-of-concept study to evaluate the safety and efficacy of efgartigimod in adults with Sjogren’s disease. In order to enter the study, patients needed to test positive for anti-Ro autoantibodies and maintain residual salivary flow. Thirty-four patients were randomized 2:1 to receive either efgartigimod or placebo for up to 24 weeks. Multiple endpoints and biomarkers were evaluated in the signal-finding study, including the primary endpoint of CRESS (Composite of Relevant Endpoints for Sjogren’s Syndrome). Within CRESS there are five components, spanning: systemic disease activity as measured by the ESSDAI (EULAR Sjogren’s Syndrome Activity Index), patient reported outcomes as measured by the ESSPRI (EULAR Sjogren’s Syndrome Patient Reported Index), tear and salivary gland function, and serology. To be a CRESS responder, patients needed to demonstrate a clinically meaningful benefit in at least 3 of the 5 composite items. Additional datapoints were gathered including the ClinESSDAI, STAR (Sjogren’s Tool for Assessing Response), biomarker data, and the change in lymphocytic infiltrate levels through parotid biopsies.

RHO+ was a 48-week open-label extension study that evaluated the safety of efgartigimod in adult patients with Sjogren's disease who continued to receive efgartigimod IV, and those who transitioned from placebo to efgartigimod IV after completing the 24-week double-blind treatment period of the Phase 2 RHO study. The primary endpoint of RHO+ was incidence and severity of AEs and AESIs, incidence of SAEs, changes in laboratory test results, vital signs, and ECG results.

About UNITY Study Design

UNITY is an ongoing Phase 3 randomized, double-blinded, placebo-controlled multicenter study with open-label extension to evaluate the efficacy, safety, and tolerability of subcutaneously administered efgartigimod PH20, in adult participants with moderate-to-severe primary Sjogren’s disease.

About argenx

argenx is a global immunology company committed to improving the lives of people suffering from severe autoimmune diseases. Partnering with leading academic researchers through its Immunology Innovation Program (IIP), argenx aims to translate immunology breakthroughs into a world-class portfolio of novel antibody-based medicines. argenx developed and is commercializing the first approved neonatal Fc receptor (FcRn) blocker and is evaluating its broad potential in multiple serious autoimmune diseases while advancing several earlier stage experimental medicines within its therapeutic franchises. For more information, visit  www.argenx.com  and follow us on LinkedIn, Instagram, Facebook, and YouTube.

For further information, please contact:

Media:

Kate Dion
kdion@argenx.com

Colin McBean
cmcbean@argenx.com

Investors:

Alexandra Roy
aroy@argenx.com

Forward-looking Statements

The contents of this announcement include statements that are, or may be deemed to be, “forward-looking statements.” These forward-looking statements generally can be identified by the use of forward-looking words, such as “aim”, “anticipate”, “aspire”, “believe”, “can”, “continue”, “could”, “estimate”, “expect”, “entail”, “forecast”, “future”, “goals”, “hope”, “intend”, “is designed to”, “likely”, “may”, “might”, “objective”, “plan”, “possible”, “potential”, “pursue”, “project”, “predict”, “seek”, “should”, “strategy”, “target”, “will” and other words and terms of similar meaning and expression, including in connection with any discussion of future operating or financial performance. By their nature, forward-looking statements involve risks and uncertainties and readers are cautioned that any such forward-looking statements are not guarantees of future performance. argenx’s actual results may differ materially from those predicted by the forward-looking statements as a result of various important factors, including but not limited to, the results of argenx’s clinical trials; uncertainties associated with the development of novel drug therapies; preclinical and clinical trial and product development risks and setbacks; interpretation of argenx’s clinical trial data by regulatory authorities and argenx’s ability to obtain regulatory approval; the risk that early stage clinical trials may not be predictive of results in later stage or large scale clinical trials; the occurrence of adverse safety events or participant dropouts; the acceptance of its products and product candidates by its patients as safe, effective, and cost-effective; the impact of governmental laws and regulations, including tariffs, export controls, sanctions and other regulations on its business; the impact of healthcare regulations, including rules on reimbursement for argenx’s products; competition in drug discovery, development and commercialization efforts; its reliance on third-party suppliers, service providers and manufacturers; and instability and conflicts in the regions in which the company has suppliers or markets for its products. A further list and description of these and other risks, uncertainties, and factors that could cause actual results to differ materially from those referred to in the forward-looking statements can be found in argenx’s U.S. Securities and Exchange Commission (SEC) filings and reports, including in argenx’s most recent annual report on Form 20-F filed with the SEC as well as subsequent filings and reports filed by argenx with the SEC. Given these risks and uncertainties, the reader is advised not to place undue reliance on such forward-looking statements. These forward-looking statements speak only as of the date of publication of this press release. argenx undertakes no obligation to publicly update or revise the information in this press release, including any forward-looking statements, except as may be required by law.

FAQ

What myositis results did argenx (ARGX) present from the ALKIVIA+ efgartigimod study at EULAR 2026?

argenx reported that many myositis patients on efgartigimod maintained or achieved meaningful Total Improvement Scores through 52 weeks. According to argenx, 37.5% on continuous therapy maintained major improvement and 75.0% showed at least moderate improvement, with similar rates in placebo-switch patients.

How did efgartigimod perform in Sjogren’s disease in the RHO+ extension study presented by argenx (ARGX)?

Efgartigimod showed maintenance or improvement of Sjogren’s disease activity over 72 weeks in RHO+. According to argenx, biweekly dosing maintained response, placebo-switch patients improved, and median ClinESSDAI scores were low (2.5 and 2.0), indicating low disease activity.

What do the new argenx (ARGX) data say about efgartigimod’s long-term safety across autoimmune diseases?

argenx reported a consistent efgartigimod safety profile across multiple autoimmune indications and routes of administration. According to argenx, data from 834 treated patients and over 1,300 patient-years showed predominantly mild-to-moderate adverse events, without increased event rates over longer treatment durations.

When are the next clinical milestones for efgartigimod in myositis and Sjogren’s disease for argenx (ARGX)?

Key readouts are scheduled over the next two years. According to argenx, topline Phase 3 ALKIVIA myositis results are expected in the third quarter of 2026, and topline Phase 3 UNITY Sjogren’s disease results are anticipated in the second half of 2027.

How clinically meaningful were the Total Improvement Score results in the ALKIVIA+ myositis study for argenx (ARGX)?

ALKIVIA+ showed sustained, clinically meaningful TIS improvements after 52 weeks of efgartigimod treatment. According to argenx, continuous-treatment patients had a mean TIS of 52.19, while placebo-switch patients reached 49.62, with moderate and major improvement thresholds at TIS ≥40 and ≥60.

What other autoimmune rheumatic disease programs using efgartigimod did argenx (ARGX) highlight at EULAR 2026?

argenx highlighted broader development of efgartigimod in rheumatology beyond myositis and Sjogren’s. According to argenx, activities included presenting the Phase 2 eSScape study design in systemic sclerosis and a symposium on FcRn and autoantibodies in autoimmune rheumatic diseases.