Artiva Announces Positive Initial Clinical Data with AlloNK® Across Multiple Autoimmune Diseases and FDA Alignment to Initiate Phase 3 Registrational Trial in Rheumatoid Arthritis in 2026

Rhea-AI Summary

Artiva (Nasdaq: ARTV) reported initial clinical data showing a 71% ACR50 response in refractory rheumatoid arthritis (RA) patients with six months of follow-up in a company-sponsored Phase 2a basket trial and FDA alignment to start a single Phase 3 registrational randomized trial in H2 2026.

As of April 3, 2026, >70 autoimmune patients treated across >40 sites; planned Phase 3 ~150 refractory RA patients, randomized 2:1 AlloNK plus rituximab vs rituximab, primary endpoint ACR50 at six months.

AI-generated analysis. Not financial advice.

Positive

• ACR50 71% in refractory RA patients with six months' follow-up (company-sponsored Phase 2a)
• FDA alignment for a single Phase 3 registrational trial in refractory RA planned for H2 2026
• >70 autoimmune patients treated across >40 clinical sites, mostly outpatient/community settings
• Complete B-cell depletion observed in all 28 RA patients evaluated using a high-sensitivity assay

Negative

• Phase 2a dataset is small: 13 RA patients with six months of follow-up in pooled company-sponsored data
• Planned registrational trial relies on rituximab comparator and crossover at six months, which may affect durability assessment
• Safety database target (>250 patients) is projected and not yet achieved

News Market Reaction – ARTV

-13.02% 7.4x vol

23 alerts

-13.02% News Effect

+22.1% Peak Tracked

-21.9% Trough Tracked

-$46M Valuation Impact

$309.45M Market Cap

7.4x Rel. Volume

On the day this news was published, ARTV declined 13.02%, reflecting a significant negative market reaction. Argus tracked a peak move of +22.1% during that session. Argus tracked a trough of -21.9% from its starting point during tracking. Our momentum scanner triggered 23 alerts that day, indicating elevated trading interest and price volatility. This price movement removed approximately $46M from the company's valuation, bringing the market cap to $309.45M at that time. Trading volume was exceptionally heavy at 7.4x the daily average, suggesting significant selling pressure.

Data tracked by StockTitan Argus on the day of publication.

Key Figures

ACR50 response: 71% RA cohort size: 21 patients Planned Phase 3 size: ≈150 patients +5 more

8 metrics

ACR50 response 71% Refractory RA, 6‑month follow‑up, company Phase 2a basket (5/7 patients)

RA cohort size 21 patients Refractory RA with ≥12 weeks follow‑up across two basket trials

Planned Phase 3 size ≈150 patients Refractory RA Phase 3 randomized trial, AlloNK+rituximab vs rituximab

CDAI reduction 37 points Mean change at 6 months in RA patients with follow‑up

DAS28‑ESR reduction 2.8 points Mean change at 6 months in RA patients with follow‑up

Grade ≥3 infection rate 2% (n=1) Autoimmune patients treated with AlloNK plus rituximab

SjD ClinESSDAI change 8.6‑point improvement Moderate‑to‑severe Sjögren disease at 6 months (n=7)

AlloNK dose 4 billion cells ×2 Proposed Phase 3 regimen on Days 6 and 20 with rituximab

Market Reality Check

Price: $7.27 Vol: Volume 136,764 is below 2...

low vol

$7.27 Last Close

Volume Volume 136,764 is below 20‑day average 360,710 (relative volume 0.38x). low

Technical Price $12.38 is above 200‑day MA at $4.68 and 14.8% below 52‑week high $14.53.

Peers on Argus

Peers show mixed moves: ALXO up 4.28%, while CELU and ACET are down 2.64–3.25%, ...

1 Up 2 Down

Peers show mixed moves: ALXO up 4.28%, while CELU and ACET are down 2.64–3.25%, suggesting this news is more stock‑specific than a uniform sector move.

Previous Clinical trial Reports

1 past event · Latest: May 13 (Positive)

Same Type Pattern 1 events

Date	Event	Sentiment	Move	Catalyst
May 13	Oncology trial update	Positive	-11.7%	Longer‑term Phase 1/2 AlloNK plus rituximab data in B‑cell lymphoma.

Pattern Detected

Prior positive AlloNK clinical data in lymphoma coincided with a -11.71% move, indicating past selling pressure on clinical updates.

Recent Company History

Over the past year, Artiva has highlighted AlloNK’s potential through oncology and autoimmune data. A May 13, 2025 update showed a 64% complete response rate and durable benefit in B‑cell non‑Hodgkin lymphoma, but the stock fell 11.71% in the next 24 hours. Today’s RA and broader autoimmune data extend the same AlloNK plus rituximab platform into refractory autoimmune disease, advancing toward a registrational Phase 3 trial in RA.

Historical Comparison

-11.7% avg move · Past clinical‑trial news for AlloNK, such as the May 2025 lymphoma update, saw an average -11.71% mo...

clinical trial

-11.7%

Average Historical Move clinical trial

Past clinical‑trial news for AlloNK, such as the May 2025 lymphoma update, saw an average -11.71% move, giving investors a reference point when assessing today’s autoimmune dataset and FDA‑aligned Phase 3 plan.

AlloNK plus rituximab moved from durable Phase 1/2 lymphoma data toward a Phase 3 registrational strategy in refractory rheumatoid arthritis, extending the same deep B‑cell depletion concept into autoimmune indications.

Regulatory & Risk Context

Active S-3 Shelf

Shelf Active

Active S-3 Shelf Registration 2025-08-06

An effective S‑3 shelf filed on 2025-08-06 remains active through 2028-08-06 with 0 recorded takedowns so far, indicating capacity for future equity issuance if the company chooses to use it.

Market Pulse Summary

The stock dropped -13.0% in the session following this news. A negative reaction despite positive ef...

Analysis

The stock dropped -13.0% in the session following this news. A negative reaction despite positive efficacy data would fit the prior pattern, where a clinical update on AlloNK in lymphoma coincided with a -11.71% move. The RA dataset shows 71% ACR50 in a small six‑month subset and broad B‑cell depletion, but trial timelines extend toward a potential BLA around 2029. Execution, regulatory milestones, and any future use of the shelf could influence sentiment over time.

Key Terms

acr50, icans, cdai, das28-esr

4 terms

acr50 medical

"Initial clinical data demonstrated 71% ACR50 response in refractory rheumatoid..."

ACR50 is a clinical-trial measure that indicates a patient with an inflammatory joint disease has achieved about a 50% improvement in key symptoms and function compared with their baseline. Think of it like a half-strength signal: joint pain, swelling and related daily limitations are reduced by roughly one‑half, and that level of improvement is often used by regulators and drug developers as a clear benchmark of meaningful benefit, so positive ACR50 results can strongly influence a therapy’s commercial and investment prospects.

icans medical

"with no CRS, ICANS, or treatment discontinuations observed in autoimmune patients..."

ICANS (Immune effector Cell-Associated Neurotoxicity Syndrome) is a range of brain-related side effects that can occur after certain immune-cell cancer therapies, such as CAR-T. Symptoms can include confusion, speech problems, seizures or reduced consciousness, and they are caused by an overactive immune response affecting the brain. Investors care because ICANS can influence patient safety, trial outcomes, regulatory approvals, treatment labeling and adoption, all of which affect a therapy’s commercial prospects and development costs.

cdai medical

"improvements across multiple measures of disease activity, including... CDAI, DAS28..."

cDAI is a digital token that serves as a receipt when you deposit DAI stablecoins into a crypto lending pool; its balance increases over time to reflect the interest earned and can be redeemed for the underlying DAI plus yield. Investors pay attention because holding cDAI offers a simple way to earn passive return on idle stablecoins and to track accumulated interest, while exposing them to platform and stablecoin risks much like choosing a non‑bank savings account.

das28-esr medical

"reductions from baseline in both CDAI... and DAS28-ESR (defined as reductions of..."

DAS28-ESR is a numeric score doctors use to measure how active rheumatoid arthritis is by checking 28 specific joints, a blood inflammation test (ESR), and how the patient feels. Think of it like a speedometer for disease activity: lower scores mean better control. Investors watch it because changes in this score in clinical trials and approvals show whether a treatment works and how big its market or regulatory value might be.

AI-generated analysis. Not financial advice.

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Initial clinical data demonstrated 71% ACR50 response in refractory rheumatoid arthritis (RA) patients with at least six months of follow-up in the company-sponsored Phase 2a basket trial, with no patients relapsing or requiring new immunomodulatory agents

AlloNK treatment regimen demonstrated tolerability results supportive of outpatient administration in community rheumatology settings, with no CRS, ICANS, or treatment discontinuations observed in autoimmune patients treated with AlloNK

More than 70 autoimmune patients treated with AlloNK across more than 40 active clinical sites, mostly in community settings, providing a strong foundation for planned registrational trial initiation in H2 2026

U.S. Food and Drug Administration (FDA) alignment on a single registrational randomized controlled trial evaluating AlloNK plus rituximab versus rituximab alone in approximately 150 refractory RA patients, with ACR50 at six months as the primary endpoint

Multiple oral and poster presentations at EULAR 2026, including a late-breaking oral presentation on AlloNK clinical efficacy in refractory RA, Sjögren disease (SjD) and systemic sclerosis (SSc)

SAN DIEGO, May 08, 2026 (GLOBE NEWSWIRE) -- Artiva Biotherapeutics, Inc. (Nasdaq: ARTV) (Artiva), a clinical-stage biotechnology company whose mission is to develop effective, safe and accessible cell therapies for patients with debilitating autoimmune diseases, today announced positive initial clinical data from ongoing clinical trials evaluating AlloNK^® (also known as AB-101) in combination with rituximab. As of the April 3, 2026 data cutoff, the initial clinical dataset includes 21 refractory RA patients with at least 12 weeks of follow-up, including 13 patients with six months of follow-up, from Artiva’s company-sponsored Phase 2a basket trial and an investigator-initiated basket trial evaluating AlloNK in B-cell driven autoimmune diseases. The broader autoimmune dataset also includes 11 SjD patients and five SSc patients, including seven SjD patients and four SSc patients with at least six months of follow-up.

Artiva also announced alignment with the FDA on a single registrational randomized controlled trial design for AlloNK in refractory RA expected to enroll approximately 150 RA patients who have had an inadequate response to two or more biologic or targeted synthetic disease modifying anti-rheumatic drugs (b/tsDMARDs) of distinct classes. Patients are expected to be randomized 2:1 to receive AlloNK plus rituximab or rituximab alone, with ACR50 response at six months as the primary efficacy endpoint.

“A new chapter begins for Artiva as we advance the first deep B-cell depleting therapy into a registrational trial in RA and share clinical data demonstrating AlloNK’s potential to drive auto-CAR-T-like activity across indications through an off-the-shelf, more scalable and cost-effective therapeutic approach that could address refractory patients in the community setting,” said Fred Aslan, M.D., president and chief executive officer of Artiva Biotherapeutics. “I am very proud of the Artiva team. In less than four years since the seminal deep B-cell depletion work was published by Schett et al., we rapidly initiated and supported trials in autoimmune diseases, activated more than 40 sites globally, treated more than 70 autoimmune patients and built a robust clinical trial network, mostly in the community setting, to support our efforts to conduct an efficient randomized controlled trial in RA, one of the largest refractory autoimmune patient populations.”

“After reviewing AlloNK’s initial clinical data in refractory RA, I am encouraged by the magnitude and consistency of improvements across multiple measures of disease activity, including swollen and tender joint counts, CDAI, DAS28 and ACR responses,” said Stanley Cohen, M.D., adjunct professor of internal medicine at University of Texas Southwestern Medical School and program director of rheumatology at THR Presbyterian Dallas. “Patients who have had an inadequate response to multiple distinct b/tsDMARDs remain difficult to treat, and there is a significant need for new therapeutic approaches that can deliver meaningful clinical benefit. I am pleased to be advising Artiva on their planned Phase 3 registrational trial of AlloNK in refractory RA.”

“Since the inception of Artiva’s clinical trials in autoimmune diseases, I have treated more than 20 patients with AlloNK in my community practice and have observed meaningful improvements in many refractory patients across indications,” said Guillermo J. Valenzuela, M.D., F.A.C.R., medical director of Integral Rheumatology & Immunology Specialists (IRIS). “Importantly, these clinical responses have been observed alongside a favorable tolerability profile that supports administration and management in the community setting. I am enthusiastic to see AlloNK advance into a Phase 3 trial for refractory RA.”

As of April 30, 2026, more than 70 autoimmune patients had initiated treatment with AlloNK across ongoing clinical trials, with more than 40 clinical sites activated globally. All patients have been treated in the outpatient setting, with the majority treated in community rheumatology clinics, providing a strong foundation to support Artiva’s planned Phase 3 registrational trial in refractory RA.

Key Data Highlights

Initial clinical activity observed in refractory RA patients

• As of the April 3, 2026 data cutoff, pooled data included 21 refractory RA patients with at least 12 weeks of follow-up, including 13 patients with six months of follow-up, from Artiva’s company-sponsored Phase 2a basket trial and an investigator-initiated basket trial.
  
• Patients had longstanding and highly active disease, with mean disease duration of 14.8 years. All patients had high disease activity at baseline and 81% had failed two or more prior b/tsDMARD classes.
  
• Five of seven patients (71%) with six months of follow-up in the company-sponsored Phase 2a basket trial achieved an ACR50 response. In the investigator-initiated basket trial, five of six patients (83%) with six months of follow-up demonstrated greater than 50% improvement on at least four of five measured components; HAQ-DI and Pain scores were not collected in the IIT, and therefore ACR50 could not be adequately assessed. Patients with only 12 weeks of follow-up demonstrated early improvements across disease activity measures consistent with those observed in patients with six or more months of follow-up. As of the data cutoff, no patients started a new b/tsDMARD following treatment with AlloNK plus rituximab.
  
• Nineteen of 21 patients demonstrated clinically meaningful reductions from baseline in both CDAI (defined as reductions of at least 12 points) and DAS28-ESR (defined as reductions of at least 1.2 points). Clinically meaningful reductions in CDAI and DAS28-ESR were observed by three months and deepened at six months, with mean reductions from baseline at six months of 37 points in CDAI and 2.8 points in DAS28-ESR.
  
  

Tolerability profile of AlloNK plus rituximab continues to support outpatient administration in community rheumatology settings

• All patients have been treated in the outpatient setting, with the majority treated in community rheumatology clinics.
  
• No cytokine release syndrome (CRS) or immune effector cell-associated neurotoxicity syndrome (ICANS) was reported.
  
• No treatment discontinuations due to adverse events and no serious adverse events related to AlloNK were reported.
  
• The most common treatment-emergent adverse events were consistent with those associated with rituximab or cyclophosphamide/fludarabine conditioning. The Grade 3 or higher infection rate was 2% (n=1), which is comparable to serious infection rates reported for approved RA therapies, including rituximab and other biologic or targeted therapies.
  
• During the initial 28-day post-treatment period, no patients were hospitalized for infection. Two of 55 autoimmune patients treated with AlloNK plus rituximab were hospitalized for treatment-emergent adverse events during this period: one admission for dehydration in a SjD patient with diarrhea and one admission for diabetic ketoacidosis in a RA patient with insulin-dependent Type 2 diabetes. Neither hospitalization was deemed related to AlloNK.
  
  

Deep B-cell depletion and B-cell reconstitution profile support proposed mechanism of action

• Uniform and consistent B-cell depletion in peripheral blood was observed by Day 13 in all 51 patients treated with cyclophosphamide/fludarabine, AlloNK and rituximab who had available samples as of the April 3, 2026 data cutoff.
  
• Complete B-cell depletion was observed using a high-sensitivity assay in all 28 RA patients evaluated as of the data cutoff.
  
• B-cell reconstitution in all patients treated with AlloNK plus rituximab demonstrated a predominance of naïve/transitional B cells, consistent with the hypothesized B-cell “reset” mechanism.
  
  

Initial clinical responses in Sjögren disease and systemic sclerosis support broader potential across B-cell-driven autoimmune diseases

• As of the April 3, 2026 data cutoff, initial clinical data included 11 patients with moderate-to-severe SjD and five patients with moderate-to-severe SSc. Clinical responses observed in these patient populations were consistent with the RA data and support the potential of AlloNK across B-cell driven autoimmune diseases.
  
• In SjD, patients demonstrated mean improvements at six months (n=7) of 8.6 points in ClinESSDAI, 6.6 points in ESSDAI and 3.0 points in ESSPRI, with a mean increase of 0.76 mL/min in stimulated salivary flow. All patients were off steroids as of the April 3, 2026 data cutoff.
  
• In SSc, patients demonstrated a mean improvement in mRSS of 9.5 points at six months (n=4), with 100% achieving rCRISS25 and 50% achieving rCRISS50 responses among patients with six months of follow-up. No patients were on steroids as of the April 3, 2026 data cutoff.
  
  

FDA Alignment and Registrational Strategy in Refractory RA
Following a recent FDA interaction, Artiva plans to initiate a Phase 3 randomized controlled trial evaluating AlloNK in approximately 150 RA patients who have had an inadequate response to two or more b/tsDMARDs of distinct classes. Artiva has alignment with the FDA on its plans to conduct a single registrational trial. Patients are expected to be randomized 2:1 to receive AlloNK plus rituximab or rituximab alone, with ACR50 response at six months as the primary efficacy endpoint. Rituximab was selected as the active comparator because it is a component of the proposed AlloNK treatment regimen, is approved for the treatment of RA and has demonstrated ACR50 responses at six months in line with other approved RA therapies. Patients randomized to the rituximab-alone control arm who do not respond are expected to have the opportunity to cross over to the AlloNK plus rituximab arm at six months.

The proposed AlloNK dosing regimen is expected to include two doses of 4 billion AlloNK cells administered on Days 6 and 20 together with rituximab, following conditioning with low-dose cyclophosphamide and fludarabine on Days 1, 2 and 3.

Assuming a favorable risk-benefit profile, Artiva believes its ongoing and planned autoimmune clinical trials, including the planned Phase 3 registrational trial in refractory RA, will generate a safety database of more than 250 patients treated with AlloNK plus rituximab, consisting primarily of RA patients and including patients with other autoimmune diseases, to support a potential biologics license application (BLA) submission for RA. Based on FDA feedback, Artiva believes pooled safety data across multiple autoimmune indications may supplement RA-specific safety data.

Subject to final protocol and regulatory considerations, the trial is expected to be conducted globally across more than 80 sites, including approximately 40 sites already active in Artiva’s ongoing autoimmune clinical program. Artiva expects to initiate the registrational trial in the second half of 2026 and report primary efficacy data in the second half of 2028, with a potential BLA submission in 2029.

Significant opportunity and unmet need in refractory RA
RA remains a large and underserved autoimmune disease, particularly among patients who have had an inadequate response to two or more b/tsDMARD classes, also known as difficult-to-treat RA under EULAR guidelines. Artiva estimates that between 150,000 to 200,000 patients in the U.S. have failed two or more b/tsDMARDs, representing approximately 25% of the U.S. b/tsDMARD-treated RA population. Real-world registry analyses and published data suggest that patients in this setting only have an 11% to 19% likelihood of achieving an ACR50 response with currently available therapies.

Artiva’s objective is to develop AlloNK as a deep B-cell depleting therapy in combination with rituximab with the potential to deliver ACR50 responses in at least 50% of refractory RA patients at six months, provide durable clinical benefit and offer an outpatient treatment profile that can be administered and managed in community rheumatology settings. Artiva expects patients in the rituximab-alone control arm to achieve ACR50 responses of approximately 20% to 25% at six months.

Multiple abstracts accepted for presentation at EULAR 2026

• Late Breaking Oral Abstract Presentation - LB0003: AB-101, an Outpatient-Administered Allogeneic NK Cell Therapy Combined with Rituximab, Generates Robust Clinical Efficacy Responses Comparable with Autologous CAR T in 31 Patients with Rheumatologic Diseases
  
• Oral Abstract Presentation - OP0129: AB-101, an Allogeneic NK Cell Therapy, Combined with Rituximab was Highly Effective in Severe Sjögren Disease: Experience in First Patient Treated
  
• Poster View Presentation - POS1177: Robust and Durable Clinical Responses Observed Following Treatment with AB-101, an Allogeneic NK Cell Therapy, Combined with Rituximab in Patients with Severe Rheumatoid Arthritis and Inadequate Response to Multiple Prior Targeted Therapies
  
• Poster Tour - POS0355: AB-101, an Allogeneic NK Cell Therapy, in Combination with Anti-CD20 Monoclonal Antibodies, Consistently Achieves Deep B-cell Depletion Comparable with CAR T Cell Therapies in Patients with Rheumatologic Diseases
  
  

About AlloNK^®
AlloNK^® (also known as AB-101) is an allogeneic, off-the-shelf, non-genetically modified, cryopreserved natural killer (NK) cell therapy candidate designed to enhance the antibody-dependent cellular cytotoxicity effect of monoclonal antibodies to drive B-cell depletion. In rheumatoid arthritis (RA) and other autoimmune diseases, AlloNK is being evaluated in combination with anti-CD20 monoclonal antibodies following a standard conditioning regimen of low-dose cyclophosphamide and fludarabine. AlloNK is currently being evaluated across multiple ongoing clinical trials in B-cell driven autoimmune diseases, including refractory RA, Sjögren disease, systemic sclerosis and idiopathic inflammatory myopathies (myositis).

About Artiva Biotherapeutics
Artiva is a clinical-stage biotechnology company whose mission is to develop effective, safe and accessible cell therapies for patients with debilitating autoimmune diseases. Artiva’s lead program, AlloNK^® (also known as AB-101), is an allogeneic, off-the-shelf, non-genetically modified, cryopreserved NK cell therapy candidate designed to enhance the antibody-dependent cellular cytotoxicity effect of monoclonal antibodies to drive B-cell depletion. AlloNK is currently being evaluated in three ongoing clinical trials for the treatment of B-cell driven autoimmune diseases, including a company-sponsored basket trial across autoimmune diseases that includes rheumatoid arthritis and Sjögren disease and an investigator-initiated basket trial in B-cell driven autoimmune diseases. Artiva plans to initiate a Phase 3 registrational trial evaluating AlloNK in refractory RA in 2026. Artiva was founded in 2019 as a spin out of GC Cell, formerly GC Lab Cell Corporation, a leading healthcare company in the Republic of Korea, pursuant to a strategic partnership granting Artiva exclusive worldwide rights (excluding Asia, Australia and New Zealand) to GC Cell’s NK cell manufacturing technology and programs.

Artiva is headquartered in San Diego, California. For more information, please visit www.artivabio.com.

Forward-Looking Statements
This press release contains forward-looking statements within the meaning of the Private Securities Litigation Reform Act of 1995. Statements in this press release that are not statements of historical fact are forward-looking statements. Such forward-looking statements include, without limitation, statements regarding: expectations of Artiva regarding the potential benefits, accessibility, effectiveness and safety of AlloNK, including based on interim pooled data across clinical trials; Artiva’s registrational strategy, including trial design, plans to conduct a single registrational Phase 3 trial for AlloNK and generate sufficient trial and pooled safety data to support a BLA submission, and Artiva’s expectations on timing and FDA alignment with such strategy; Artiva’s expectations on the timing to initiate and report data for the Phase 3 trial; Artiva’s expectations with respect to ACR50 responses in the Phase 3 trial for both AlloNK and the control arm; estimates regarding the size of patient populations and response rates to existing therapies; and the potential market opportunity for AlloNK. These forward-looking statements are based on the beliefs of the management of Artiva as well as assumptions made by and information currently available Artiva. Such statements reflect the current views of Artiva with respect to future events and are subject to known and unknown risks and uncertainties, including, without limitation, risks inherent in developing product candidates; Artiva’s ability to obtain adequate financing to fund its planned clinical trials and other expenses; risks that future clinical trial results may not be consistent with interim, initial, preliminary, or topline results or results from prior preclinical studies or clinical trials; the risk that Artiva’s registrational strategy is based in part on its views following its recent meeting with the FDA and later feedback from the FDA may be inconsistent with such meeting or its views from such meeting, including the risk that the official FDA minutes which Artiva expects to receive in the coming weeks may include interpretations, requests for additional data, or conclusions that differ from Artiva’s understanding of prior discussions; the risk that differences exist between trial designs, patient characteristics and other factors for the Artiva-sponsored Phase 2a basket trial and an investigator-initiated basket trial, and caution should be exercised in drawing any conclusions from such data across separate trials as such pooling and comparative data is inherently limited and such data may not be directly comparable; and risks related to the legal and regulatory framework for the industry. In light of these risks and uncertainties, the events or circumstances referred to in the forward-looking statements may not occur. These and other factors that may cause Artiva’s actual results to differ from current expectations are described in further detail under the section titled “Risk Factors” contained in Artiva’s filings with the Securities and Exchange Commission (the “SEC”), including Artiva’s Annual Report on Form 10-K for the year ended December 31, 2025, and its subsequent Quarterly Reports on Form 10-Q, each as filed or to be filed with the SEC. You are cautioned not to place undue reliance on these forward-looking statements, which speak only as of the date this press release is given. Except as required by law, Artiva undertakes no obligation to publicly update any forward-looking statements, whether as a result of new information, future events or otherwise.

Contacts

Investors
Noopur Batsha Liffick, MPH
NBL LifeSci Advisory LLC
ir@artivabio.com

Media
Jessica Yingling, Ph.D.
Little Dog Communications Inc.
jessica@litldog.com

FAQ

What initial ACR50 results did Artiva (ARTV) report for AlloNK in refractory RA on May 8, 2026?

Artiva reported a 71% ACR50 response in refractory RA patients with six months' follow-up. According to the company, this figure reflects five of seven patients in the company-sponsored Phase 2a cohort with six months of data as of April 3, 2026.

When will the Artiva (ARTV) Phase 3 registrational trial for AlloNK in refractory RA begin and what is the design?

Artiva expects to initiate the Phase 3 trial in H2 2026 with ~150 refractory RA patients randomized 2:1. According to the company, the trial will compare AlloNK plus rituximab versus rituximab alone with ACR50 at six months as the primary endpoint.

How many patients and sites have received AlloNK across Artiva's autoimmune trials as of April 30, 2026?

More than 70 autoimmune patients have been treated across over 40 active clinical sites. According to the company, most treatments occurred outpatient in community rheumatology settings, supporting feasibility for a larger registrational trial.

What safety and tolerability observations did Artiva report for AlloNK plus rituximab in autoimmune patients?

Artiva reported no CRS or ICANS, no treatment discontinuations due to adverse events, and no AlloNK-related serious adverse events. According to the company, Grade ≥3 infection rate was 2% (n=1) and no post-treatment infection hospitalizations occurred in the initial 28 days.

What biomarker effects did Artiva observe with AlloNK treatment in RA patients?

Artiva observed uniform peripheral B-cell depletion by Day 13 and complete B-cell depletion in 28 RA patients using a high-sensitivity assay. According to the company, reconstituted B cells were predominantly naïve/transitional, consistent with a proposed B-cell “reset.”

What timeline did Artiva give for Phase 3 readout and a potential BLA for AlloNK in RA?

Artiva expects primary Phase 3 efficacy data in H2 2028 and a potential BLA submission in 2029. According to the company, these projections assume a favorable risk-benefit profile and completion of the planned registrational trial and pooled safety database.