EyePoint Announces Third Consecutive Positive DSMC Recommendation for Phase 3 Wet AMD Trials for DURAVYU™, Building Confidence Ahead of Mid-2026 Topline Data

Rhea-AI Impact

(High)

Rhea-AI Sentiment

(Positive)

Rhea-AI Summary

EyePoint (Nasdaq:EYPT) reported a third consecutive positive recommendation from the independent DSMC for its pivotal Phase 3 DURAVYU wet AMD trials, LUGANO and LUCIA, allowing both to continue without protocol changes.

Enrollment is complete with over 900 patients, topline LUGANO data targeted for mid-2026, and LUCIA to follow. All active treatment-arm patients reached Week 32 for a second dose, with over 35% receiving a third dose at Week 56. Masked safety data remain favorable and consistent with four earlier trials.

AI-generated analysis. Not financial advice.

Positive

Third consecutive positive DSMC recommendation with no protocol modifications for LUGANO and LUCIA
Interim masked Phase 3 data show favorable DURAVYU safety consistent with four prior trials in over 190 patients
All active treatment-arm patients reached Week 32 and received a second DURAVYU dose
Over 35% of treated patients have already received a third DURAVYU dose at Week 56
Phase 3 enrollment completed with over 900 wet AMD patients randomized 1:1 versus aflibercept
LUGANO topline data targeted for mid-2026, with LUCIA readout expected shortly after

Negative

None.

Key Figures

Third DSMC review: 3 consecutive positive DSMC recommendations Phase 3 topline timing: Mid-2026 LUGANO topline; LUCIA shortly after Patients with third dose: Over 35% received third DURAVYU dose +5 more

8 metrics

Third DSMC review 3 consecutive positive DSMC recommendations Pivotal Phase 3 DURAVYU wet AMD program

Phase 3 topline timing Mid-2026 LUGANO topline; LUCIA shortly after Wet AMD Phase 3 trials

Patients with third dose Over 35% received third DURAVYU dose Treatment-arm patients at Week 56

Prior safety database Over 190 patients Four completed DURAVYU clinical trials

Phase 3 enrollment Over 900 patients enrolled LUGANO and LUCIA wet AMD trials

Dosing regimen DURAVYU 2.7mg every six months Randomized 1:1 vs on-label aflibercept

Primary endpoint window BCVA change at weeks 52 and 56 Non-inferiority primary endpoint

DSMC meeting schedule Every six months Safety reviews per trial protocol

Market Reality Check

Price: $13.43 Vol: Volume 837,515 is close t...

normal vol

$13.43 Last Close

Volume Volume 837,515 is close to the 20-day average of 891,835 ahead of this news. normal

Technical Price $13.43 is trading below the 200-day MA $13.89 before this update.

Peers on Argus

Pre-news, EYPT was down 1.4% while scanner activity showed only ABUS moving, dow...

1 Down

Pre-news, EYPT was down 1.4% while scanner activity showed only ABUS moving, down 4.41%, with no same-direction cluster of peers. Sector context peers mostly showed small gains, reinforcing a stock-specific setup.

Previous Clinical trial Reports

5 past events · Latest: Mar 02 (Positive)

Same Type Pattern 5 events

Date	Event	Sentiment	Move	Catalyst
Mar 02	Phase 3 DME dosing	Positive	+4.4%	First patients dosed in global Phase 3 COMO and CAPRI DME trials.
Nov 19	DSMC wet AMD update	Positive	+2.3%	Second DSMC review found no safety issues and trials continued unchanged.
Oct 14	Phase 3 DME initiation	Positive	-10.9%	Initiation of pivotal DME trials with first dosing expected in Q1 2026.
Jul 29	Wet AMD enrollment complete	Positive	-1.8%	Completed enrollment of LUGANO and LUCIA wet AMD Phase 3 trials.
May 27	LUGANO enrollment milestone	Positive	+4.9%	Completed LUGANO enrollment with rapid recruitment and 6‑month dosing focus.

Pattern Detected

Clinical-trial headlines have produced mixed reactions: three positive moves and two selloffs despite constructive updates.

Recent Company History

Over the past year, EyePoint has repeatedly advanced DURAVYU through pivotal programs. Prior clinical updates included Phase 3 enrollment completion in wet AMD, multiple positive DSMC recommendations, and the start of global Phase 3 trials in diabetic macular edema. Same‑tag events often highlighted 6‑month redosing and non‑inferiority BCVA endpoints, with average moves around -0.2%. Today’s DSMC confirmation and safety consistency fit this pattern of incremental de‑risking ahead of topline data expected beginning in mid‑2026.

Historical Comparison

-0.2% avg move · Past clinical‑trial headlines moved EYPT by an average of -0.2%. Today’s -1.4% pre‑news level is mod...

clinical trial

-0.2%

Average Historical Move clinical trial

Past clinical‑trial headlines moved EYPT by an average of -0.2%. Today’s -1.4% pre‑news level is modestly more negative but still within the historically mixed range.

Clinical news shows steady DURAVYU progression: rapid enrollment in wet AMD Phase 3, multiple DSMC confirmations, and expansion into DME Phase 3 programs using similar 6‑month dosing and BCVA endpoints.

Market Pulse Summary

This announcement reinforces DURAVYU’s Phase 3 safety profile, with a third consecutive positive DSM...

Analysis

This announcement reinforces DURAVYU’s Phase 3 safety profile, with a third consecutive positive DSMC recommendation and over 900 wet AMD patients enrolled on a 6‑month dosing regimen. Prior clinical updates showed rapid enrollment and expansion into DME, underscoring a broad late‑stage program. Investors may focus on upcoming topline data beginning in mid‑2026, the durability of safety across more than 190 treated patients, and how non‑inferiority in BCVA and treatment burden reduction are ultimately demonstrated.

Key Terms

data safety monitoring committee, phase 3, non-inferiority, best corrected visual acuity (bcva), +4 more

8 terms

data safety monitoring committee medical

"the independent Data Safety Monitoring Committee (DSMC) completed its third scheduled review"

A data safety monitoring committee is an independent panel of medical and statistical experts that regularly reviews patient safety and study results during clinical trials to decide whether the trial can continue, needs changes, or should stop. Think of them as impartial referees who protect participants and ensure results are trustworthy; their assessments matter to investors because safety findings and early stops can speed up, delay, or derail a drug or device’s path to approval and affect a company’s value.

phase 3 medical

"pivotal Phase 3 program evaluating DURAVYU for wet age-related macular degeneration"

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.

non-inferiority medical

"non-inferiority Phase 3 trials assessing the efficacy and safety of DURAVYU"

A non-inferiority trial is a type of clinical test designed to show a new treatment is not meaningfully worse than an existing standard by more than a pre-set, acceptable amount. Think of it like proving a new smartphone model has battery life close enough to the leading model while offering other advantages; for investors, a successful non-inferiority result can clear the way to regulatory approval and market uptake even when the new option isn’t superior in headline effectiveness.

best corrected visual acuity (bcva) medical

"primary endpoint ... change in best corrected visual acuity (BCVA) at weeks 52 and 56"

Best corrected visual acuity (BCVA) measures how clearly a person can see when wearing their optimal glasses or contact lenses, typically tested by reading letters on an eye chart. Investors care because BCVA is a common clinical-trial endpoint and regulatory benchmark for eye treatments and devices—improvements indicate real patient benefit and can drive product approval, market adoption, and revenue potential, much like a performance score that validates a new tool.

optical coherence tomography (oct) medical

"anatomical results as measured by optical coherence tomography (OCT)"

Optical coherence tomography (OCT) is a noninvasive imaging technique that uses light to create detailed, cross‑sectional pictures of internal tissues, most commonly the eye and blood vessels. Investors care because OCT is a diagnostic and procedural guidance tool that drives sales of specialized scanners, software and disposables; think of it as a high‑precision camera that lets doctors see tiny layers and make faster, more accurate treatment decisions.

intravitreal injection medical

"DURAVYU is delivered via a standard intravitreal injection in the physician's office"

An intravitreal injection is a medical procedure that delivers medicine directly into the gel-like center of the eye to reach the retina at the back of the eye, much like putting a targeted dose into a small reservoir. It matters to investors because this delivery method affects how often patients need treatment, the complexity and cost of care, reimbursement decisions, and the commercial prospects and safety profile of eye drugs being developed or sold.

aflibercept medical

"randomized, double-masked, aflibercept controlled, non-inferiority Phase 3 trials"

Aflibercept is a lab-made protein drug that blocks the signals that tell the body to grow new blood vessels; it is used as an injected treatment for certain eye diseases that cause vision loss and in some cancer therapies to slow tumor blood supply. Investors care because its sales, patent protection, regulatory approvals, and competition directly affect a drugmaker’s revenue stream and future growth prospects, much like a key product line in any business.

topline data technical

"LUGANO topline data on track for mid-2026, with LUCIA readout to follow"

Topline data are the initial, high-level results from a clinical study that show whether the main goals of the trial were met, much like the headline of a news story that summarizes the most important point. Investors care because these early outcomes quickly indicate a drug’s commercial potential and regulatory path — positive topline results can boost a company’s value, while disappointing ones can sharply reduce expected future revenue.

AI-generated analysis. Not financial advice.

05/14/2026 - 07:00 AM

– LUGANO topline data on track for mid-2026, with LUCIA readout to follow shortly after –

– Continued favorable safety profile observed in masked Phase 3 DURAVYU data, consistent with four previously completed clinical trials –

– All active patients in the treatment arm have reached their second DURAVYU dosing visit, with over 35% receiving a third dose –

WATERTOWN, Mass., May 14, 2026 (GLOBE NEWSWIRE) -- EyePoint, Inc. (Nasdaq: EYPT), a company committed to developing and commercializing innovative therapeutics to improve the lives of patients with serious retinal diseases, today announced that the independent Data Safety Monitoring Committee (DSMC) completed its third scheduled review of the Company’s pivotal Phase 3 program evaluating DURAVYU for wet age-related macular degeneration (wet AMD) and recommended that both the LUGANO and LUCIA trials continue as planned with no protocol modifications. As of May 2, 2026, all active patients in the treatment arm have reached the Week 32 visit, during which patients received their second DURAVYU dose. Over 35% of those patients have also received their third planned dose at Week 56.

Interim masked safety data from the Phase 3 trials show a continued favorable safety profile for DURAVYU, consistent with the safety observed in over 190 patients across four completed clinical trials. The DSMC is an independent panel of experts in ophthalmology and biostatistics who are responsible for reviewing safety data to ensure the welfare of trial participants and to provide recommendations regarding trial conduct. DSMC meetings are scheduled to occur every six months per the trial protocol, and this is the last anticipated DSMC meeting ahead of topline data.

“Safety is paramount in retinal disease therapies, and receiving three consecutive positive DSMC recommendations to continue our Phase 3 wet AMD trials without modification reflects the consistency of DURAVYU’s safety profile and the rigor of our Phase 3 wet AMD program design,” said Ramiro Ribeiro, M.D., Ph.D., Chief Medical Officer at EyePoint. “This continued independent validation, together with the favorable safety profile observed across four completed clinical trials, reinforces our confidence as we approach Phase 3 topline data beginning in mid-2026. If successful, we believe that DURAVYU is well-positioned to be a first and best-in-class therapy with the potential to establish a new treatment paradigm for patients who have long needed better options.”

LUGANO and LUCIA are identical, randomized, double-masked, aflibercept controlled, non-inferiority Phase 3 trials assessing the efficacy and safety of DURAVYU in patients with active wet AMD including both treatment naïve and treatment experienced patients. Enrollment is complete in both trials with over 900 patients enrolled. At Day 1, patients are randomized 1:1 to receive either DURAVYU 2.7mg every six months or on-label aflibercept as control. All active patients in the treatment arm have reached the Week 32 visit, during which patients received their second DURAVYU dose. The LUGANO and LUCIA trials are the only sustained release wet AMD pivotal Phase 3 trials evaluating 6-month redosing in both trials over two years. DURAVYU is delivered via a standard intravitreal injection in the physician's office, similar to current practice with FDA approved anti-VEGF treatments. The primary endpoint of the Phase 3 pivotal trials is non-inferiority in the average change in best corrected visual acuity (BCVA) at weeks 52 and 56 compared to baseline. Secondary endpoints include safety, reduction in treatment burden, percentage of eyes free of supplemental aflibercept injections, and anatomical results as measured by optical coherence tomography (OCT). More information about the trial is available at www.clinicaltrials.gov (LUGANO identifier: NCT06668064; LUCIA identifier: NCT06683742).

About Wet AMD

Wet age-related macular degeneration (wet AMD) is a leading cause of vision loss and irreversible blindness in people over the age of fifty. Wet AMD is an advanced form of AMD that develops when abnormal blood vessels grow under the macular retina, leaking blood and/or fluid, and leading to potentially severe vision loss. Wet AMD is a lifelong disease that requires continuous treatment so that patients may maintain visual function. Although multiple treatments are now available, challenges still exist as the current standard-of-care is dosed on average every two months in the United States under a treat-and-extend protocol, and these large molecule anti-VEGF treatments only target one pathology of the disease. This lifetime of frequent treatment represents a tremendous burden for patients, physicians, and the health care system, potentially leading to patient noncompliance and further vision loss.

About DURAVYU^™

DURAVYU^™ (vorolanib intravitreal insert), is an investigational sustained-delivery treatment for patients suffering from serious retinal diseases. DURAVYU combines vorolanib, a selective and patent-protected tyrosine kinase inhibitor (TKI), in next-generation bioerodible Durasert E^™, a proprietary and best-in-class IVT delivery technology designed to provide sustained release of drug for at least six months without free-floating drug particles.

DURAVYU brings a potential new multi-mechanism of action and treatment paradigm for retinal diseases beyond existing anti-VEGF large molecule ligand blocking therapies, as vorolanib acts intracellularly to suppress angiogenesis through the inhibition of all VEGF receptors and PDGFR, while also suppressing inflammation through the inhibition of interleukin 6 (IL-6)/JAK1 signaling. In addition to the safety and efficacy demonstrated in the DAVIO, DAVIO 2 and VERONA clinical trials, vorolanib has also demonstrated neuroprotection in an in-vivo model of retinal detachment.

DURAVYU has established safety and efficacy data from both Phase 1 and 2 trials in wet AMD and DME that demonstrate stability in vision and anatomical control with a single dose of DURAVYU. No drug-related safety concerns were observed in over 190 patients across four completed clinical trials, including three Phase 2 trials.

Informed by the robust Phase 2, DAVIO trial, which achieved statistically positive and clinically meaningful results vs. on-label aflibercept, the fully enrolled wet AMD Phase 3 pivotal program (LUGANO and LUCIA) is the only investigational program evaluating every six-month dosing of DURAVYU, which enables the potential to support a compelling competitive label and advantage for DURAVYU. With over 900 patients randomized across both trials, the Phase 3 pivotal program follows a well-established regulatory approval pathway with a patient-centric noninferiority design comparing DURAVYU to on-label standard of care to inform real-word treatment practices. Data from the Phase 3 program are anticipated to be reported beginning in mid-2026.

DURAVYU is also being evaluated for the treatment of DME, with both Phase 3 trials (COMO and CAPRI) underway and actively recruiting patients. The Phase 2 VERONA trial in DME met primary and secondary endpoints and demonstrated a rapid and sustained improvement in vision and anatomy and a continued favorable safety and tolerability profile with superior dosing intervals to standard of care. Data from the Phase 3 program is anticipated to be reported in the second half of 2027.

About EyePoint

EyePoint, Inc. (Nasdaq: EYPT) is a clinical-stage biopharmaceutical company committed to developing and commercializing innovative therapeutics to improve the lives of patients with serious retinal diseases. The Company’s lead product candidate, DURAVYU^™, is an innovative investigational sustained delivery treatment for serious retinal diseases combining vorolanib, a selective and patent-protected tyrosine kinase inhibitor, in next-generation bioerodible Durasert E^™ technology. Supported by robust safety and efficacy data across multiple clinical trials and indications, DURAVYU is currently being evaluated in Phase 3 pivotal trials for wet age-related macular degeneration (wet AMD) and diabetic macular edema (DME). Topline data is expected for wet AMD beginning in mid-2026.

The Company is committed to partnering with the retina community to improve patient lives while creating long-term value, with four approved drugs over three decades and tens of thousands of eyes treated with EyePoint innovation.

EyePoint is headquartered in Watertown, Massachusetts, with a commercial manufacturing facility in Northbridge, Massachusetts.

Vorolanib is licensed to EyePoint exclusively by Equinox Sciences, a Betta Pharmaceuticals affiliate, for the localized treatment of all ophthalmic diseases outside of China, Macao, Hong Kong and Taiwan.

DURAVYU^™ has been conditionally accepted by the FDA as the proprietary name for EYP-1901. DURAVYU is an investigational product; it has not been approved by the FDA. FDA approval and the timeline for potential approval is uncertain.

Forward Looking Statements

EYEPOINT SAFE HARBOR STATEMENTS UNDER THE PRIVATE SECURITIES LITIGATION ACT OF 1995: To the extent any statements made in this press release deal with information that is not historical, these are forward-looking statements under the Private Securities Litigation Reform Act of 1995. Such statements include, but are not limited to, statements regarding our expectations regarding our clinical development and regulatory plans; our belief that DURAVYU^™ is well-positioned to be the first-to-market among all investigational sustained release treatments for the two largest retinal disease markets, wet AMD and DME; our belief that DURAVYU is the only TKI in development for DME; our belief that DURAVYU is uniquely positioned to potentially address both VEGF-mediated vascular leakage and IL-6 mediated inflammatory drivers of DME as a sustained delivery therapy; our belief that DURAVYU’s potential real-world application in multiple retinal disease indications and established trial designs position DURAVYU for clinical and commercial success; our expectations regarding the timing of the availability and release of wet AMD and DME clinical data; our financial position and expected cash runway; our belief that DURAVYU has the potential to maintain a majority of patients with active disease with no supplemental anti-VEGF therapy for six months or longer; our beliefs regarding the potential market opportunity for DURAVYU in wet AMD and DME; our ability to continue to scale operations at our commercial manufacturing facility in Northbridge, Massachusetts; our expectations that our manufacturing facility will continue to meet FDA and EMA standards and support commercialization efforts of DURAVYU upon regulatory approval; and our expectations regarding the timing and clinical development of our other product candidates; and other statements regarding the Company’s future plans, objectives, strategies and beliefs, as identified by words such as “will,” “potential,” “could,” “can,” “believe,” “intends,” “continue,” “plans,” “expects,” “anticipates,” “estimates,” “may,” or other words of similar meaning or the use of future dates.

Forward-looking statements by their nature address matters that are, to different degrees, uncertain. Uncertainties and risks may cause EyePoint’s actual results to be materially different than those expressed in or implied by EyePoint’s forward-looking statements. For EyePoint, these risks and uncertainties include the timing, progress and results of the Company’s clinical development activities; uncertainties and delays relating to communications with the U.S. Food and Drug Administration and the ability to obtain regulatory approval from FDA for the commercialization of DURAVYU; unanticipated costs and expenses; the Company’s cash and cash equivalents may not be sufficient to support its operating plan for as long as anticipated; the risk that results of clinical trials may not be predictive of future results, and interim and preliminary data are subject to further analysis and may change as more data becomes available; unexpected safety or efficacy data observed during clinical trials; uncertainties related to the regulatory authorization or approval process, and available development and regulatory pathways for approval of the Company’s product candidates; changes in the regulatory environment; disruptions at the FDA; changes in U.S. and international trade policies; changes in expected or existing competition; the success of current and future license agreements; our dependence on contract research organizations, and other outside vendors and service providers; product liability; the impact of general business and economic conditions; protection of our intellectual property and avoiding intellectual property infringement; retention of key personnel; delays, interruptions or failures in the manufacture and supply of our product candidates, including due to unanticipated regulatory compliance issues or warning letters relating to the Company’s manufacturing facilities; the availability of and the need for additional financing; our ability to obtain additional funding to support our clinical development programs; our ability to enter into a settlement agreement and corporate integrity agreement with the government regarding the DOJ investigation and uncertainties related to the impact such agreements would have on our business, financial condition and operations; uncertainties regarding the FDA warning letter pertaining to the Company’s Watertown, MA manufacturing facility; and other factors described in our filings with the Securities and Exchange Commission. We cannot guarantee that the results and other expectations expressed, anticipated or implied in any forward-looking statement will be realized. A variety of factors, including these risks, could cause our actual results and other expectations to differ materially from the anticipated results or other expectations expressed, anticipated or implied in our forward-looking statements. Should known or unknown risks materialize, or should underlying assumptions prove inaccurate, actual results could differ materially from past results and those anticipated, estimated or projected in the forward-looking statements. You should bear this in mind as you consider any forward-looking statements. A more complete discussion of the risks and uncertainties that may cause our actual results to differ materially from those expressed or implied in the forward-looking statements in this press release are described under the heading "Risk Factors" in our most recent Annual Report on Form 10-K, in our other filings with the Securities and Exchange Commission (SEC) and in our future reports to be filed with the SEC, which are available at www.sec.gov. Our forward-looking statements speak only as of the dates on which they are made. EyePoint undertakes no obligation to update or revise any forward-looking statement, whether as a result of new information, future events, or otherwise.

Investors:

Tanner Kaufman / Jenni Lu
FTI Consulting
tanner.kaufman@fticonsulting.com / jenni.lu@fticonsulting.com

Media:

Helen O’Gorman
FTI Consulting
helen.ogorman@fticonsulting.com

FAQ

What did EyePoint (NASDAQ:EYPT) announce about its DURAVYU Phase 3 wet AMD trials on May 14, 2026?

EyePoint announced a third positive DSMC recommendation to continue its Phase 3 DURAVYU wet AMD trials without changes. According to EyePoint, the LUGANO and LUCIA studies remain on track, supported by favorable interim masked safety data and completed enrollment of over 900 patients.

What is the DSMC’s latest recommendation for EyePoint’s DURAVYU LUGANO and LUCIA Phase 3 trials (EYPT)?

The DSMC recommended that both LUGANO and LUCIA continue as planned with no protocol modifications. According to EyePoint, this was the third scheduled DSMC review, based on interim masked safety data, and is expected to be the final meeting before topline Phase 3 results.

When is EyePoint expecting topline Phase 3 data for DURAVYU in wet AMD (EYPT)?

EyePoint expects topline data from the LUGANO Phase 3 DURAVYU wet AMD trial in mid-2026, with LUCIA results to follow shortly afterward. According to EyePoint, DSMC reviews occur every six months, and this latest meeting is the last anticipated before these topline readouts.

How many patients are enrolled in EyePoint’s LUGANO and LUCIA DURAVYU Phase 3 trials for wet AMD?

Enrollment is complete in both LUGANO and LUCIA, with over 900 patients enrolled. According to EyePoint, patients were randomized 1:1 to DURAVYU 2.7 mg every six months or on-label aflibercept, and all active treatment-arm patients have reached the Week 32 second-dose visit.

What dosing schedule is being tested for DURAVYU in EyePoint’s Phase 3 wet AMD trials (EYPT)?

The trials evaluate DURAVYU 2.7 mg dosed every six months over two years, compared with on-label aflibercept. According to EyePoint, all active treatment-arm patients have received a second dose at Week 32 and over 35% have received a third dose at Week 56.

What safety profile has DURAVYU shown so far in EyePoint’s Phase 3 wet AMD program?

Interim masked Phase 3 data indicate a continued favorable safety profile for DURAVYU. According to EyePoint, this safety experience is consistent with results seen in more than 190 patients across four completed clinical trials, supporting ongoing evaluation in LUGANO and LUCIA.

What are the primary and secondary endpoints in EyePoint’s DURAVYU LUGANO and LUCIA Phase 3 trials?

The primary endpoint is non-inferiority in average change in best corrected visual acuity at Weeks 52 and 56 versus baseline. According to EyePoint, secondary endpoints include safety, treatment-burden reduction, percentage of eyes free of supplemental aflibercept, and OCT-based anatomical outcomes.