A study to investigate the prevention of COVID-19 with VYD222 in adults with immune compromise and in participants aged 12 years or older who are at risk of exposure to SARS-CoV-2

Start Date08 Sep 2023

Sponsor / Collaborator

Invivyd, Inc.

NCT05791318

/ CompletedPhase 1

A Phase 1, Randomized, Triple-Blind, Placebo-Controlled, Single Ascending Dose Study to Evaluate the Safety, Tolerability, Pharmacokinetics, and Immunogenicity of the Monoclonal Antibody VYD222 in Healthy Adult Participants

A study to investigate the safety, tolerability, and pharmacokinetics of the monoclonal antibody VYD222 in healthy adult participants.

Start Date28 Mar 2023

Sponsor / Collaborator

Invivyd, Inc.

[+1]

NCT06004128

/ No longer availableNot Applicable

Provide Pre-approval Single-patient Expanded Access (Compassionate Use) of VYD222 for Patients With Symptomatic COVID-19 Refractory to Other Treatments

Provide pre-approval single-patient Expanded Access (Compassionate Use) of VYD222 for patients with symptomatic COVID-19 refractory to other treatments.

Start Date-

Sponsor / Collaborator

Invivyd, Inc.

100 Clinical Results associated with Pemivibart

100 Translational Medicine associated with Pemivibart

100 Patents (Medical) associated with Pemivibart

Literatures (Medical) associated with Pemivibart

16 Jan 2026·CLINICAL INFECTIOUS DISEASES

2024 Clinical Practice Guideline Update by the Infectious Diseases Society of America on the Management of COVID-19: Anti-SARS-CoV-2 Neutralizing Antibody Pemivibart for Pre-exposure Prophylaxis

Review

Author: Dzierba, Amy L ; Gandhi, Rajesh T ; Shafer, Robert W ; Glidden, David V ; Nakamura, Mari M ; Cheng, Vincent Chi-Chung ; Chiotos, Kathleen ; Falck-Ytter, Yngve ; Tien, Phyllis ; Loveless, Jennifer ; MacBrayne, Christine ; Baden, Lindsey R ; Chew, Kara W ; Martin, Greg S ; Bhimraj, Adarsh ; Kim, Arthur Y ; Johnson, Steven ; Morgan, Rebecca L ; Hardy, Erica J ; Shumaker, Amy Hirsch ; Li, Jonathan Z ; Shoham, Shmuel ; Tebas, Pablo ; Nadig, Nandita ; Daar, Eric S ; Bedimo, Roger

Abstract:

This article provides a focused update to the clinical practice guideline on the treatment and management of patients with coronavirus disease 2019, developed by the Infectious Diseases Society of America. The guideline panel presents a recommendation on the use of the anti–severe acute respiratory syndrome coronavirus 2 neutralizing antibody pemivibart as pre-exposure prophylaxis. The recommendation is based on evidence derived from a systematic review and adheres to a standardized methodology for rating the certainty of evidence and strength of recommendation according to the GRADE (Grading of Recommendations, Assessment, Development, and Evaluation) approach. Information on pemivibart is included in the U.S. Food and Drug Administration Emergency Use Authorization for this agent.

25 Nov 2025·JOURNAL OF VIROLOGY

Spike mutations that affect the function and antigenicity of recent KP.3.1.1-like SARS-CoV-2 variants

Article

Author: Larsen, Brendan B. ; Chu, Helen Y. ; Kampman, Lucas ; Elias-Warren, Anna ; Dadonaite, Bernadeta ; Harari, Sheri ; Harteloo, Alex ; Bloom, Jesse D.

ABSTRACT:

SARS-CoV-2 is under strong evolutionary selection to acquire mutations in its spike protein that reduce neutralization by human polyclonal antibodies. Here, we use pseudovirus-based deep mutational scanning to measure how mutations to the spike from the recent KP.3.1.1 SARS-CoV-2 strain affect cell entry, binding to the ACE2 receptor, RBD up/down motion, and neutralization by human sera and clinically relevant antibodies. The spike mutations that most affect serum antibody neutralization sometimes differ between sera collected before versus after recent vaccination or infection, indicating that these exposures shift the neutralization immunodominance hierarchy. The sites where mutations cause the greatest reduction in neutralization by post-vaccination or infection sera include receptor-binding domain (RBD) sites 475, 478, and 487, all of which have mutated in recent SARS-CoV-2 variants. Multiple mutations outside the RBD affect sera neutralization as strongly as any RBD mutations by modulating the RBD up/down movement. Some sites that affect RBD up/down movement have mutated in recent SARS-CoV-2 variants. Finally, we measure how spike mutations affect neutralization by three clinically relevant SARS-CoV-2 antibodies: VYD222, BD55-1205, and SA55. Overall, these results illuminate the current constraints and pressures shaping SARS-CoV-2 evolution and can help with efforts to forecast possible future antigenic changes that may impact vaccines or clinical antibodies.

IMPORTANCE:

This study measures how mutations to the spike of a SARS-CoV-2 variant that circulated in early 2025 affect its function and recognition by both the polyclonal antibodies produced by the human immune system and monoclonal antibodies used as prophylactics. These measurements are made with a pseudovirus system that enables safe study of viral protein mutations using virions that can only infect cells once. The study identifies mutations that decrease recognition by current human antibody immunity; many of these mutations are increasingly being observed in new viral variants. It also shows the importance of mutations that move the spike’s receptor-binding domain up or down. Overall, these results are useful for forecasting viral evolution and assessing which newly emerging variants have reduced recognition by immunity and antibody prophylactics.

06 Nov 2025·Cureus Journal of Medical Science

Exploring the Effects of Pemivibart Monoclonal Antibody Infusion in Long COVID: A Case Series Offering Initial Clinical Insights

Article

Author: Baratta, John M ; Cobb, Cameron ; Jensen, Kayla A

Long COVID, or post-COVID conditions (PCC), affects a substantial proportion of adults and is characterized by persistent symptoms such as fatigue, postexertional malaise (PEM), cognitive dysfunction, and dysautonomia. At present, no Food and Drug Administration-approved therapies exist. Pemivibart (Pemgarda), a monoclonal antibody (mAb) authorized under Emergency Use Authorization (EUA) for preexposure prophylaxis in immunocompromised individuals, has not been studied for PCC but may theoretically facilitate clearance of viral antigens. We report three individuals with longstanding, debilitating PCC who received pemivibart infusion under EUA. Each experienced rapid symptomatic improvement, most notably in fatigue with PEM, dysautonomia, and cognitive dysfunction. One patient achieved resolution of her most limiting symptoms within a week and sustained functional recovery following repeat infusion. Another demonstrated significant gains across several symptom domains and was able to resume prior physical activities, although benefits waned after two to three weeks. A third with autoimmune comorbidities reported dramatic improvement in energy and cognition, and continued to feel well at six weeks. The rationale for this case series stems from emerging hypotheses that persistent viral antigens may contribute to the pathophysiology of Long COVID and that neutralizing antibodies could facilitate antigen clearance and symptom resolution. In the three cases, pemivibart infusion was temporally associated with rapid and meaningful improvement in fatigue associated with PEM, cognitive dysfunction, and dysautonomia, symptom clusters that often drive functional impairment in PCC. While the magnitude and duration of benefit varied among individuals, the consistent pattern of improvement supports further exploration of mAb therapy as a potential disease-modifying approach. These preliminary findings highlight the need for controlled, biomarker-guided studies to determine efficacy, durability, and patient subgroups most likely to respond. Pemivibart remains authorized only for preexposure prophylaxis in immunocompromised individuals and is not approved for the treatment of PCC.

News (Medical) associated with Pemivibart

15 Apr 2026

·adimab.com

Adimab Collaborator GSK Receives Additional Marketing Approval for Depemokimab

Lebanon, New Hampshire – April 15, 2026 – Adimab, LLC, the global leader in the discovery and engineering of fully human monoclonal and multispecific antibodies, congratulates GSK plc for recently receiving approvals by the European Commission (EC) and China’s National Medical Products Administration (NMPA) for depemokimab. This adds to recent marketing approvals in the United States, Japan, and the United Kingdom. Depemokimab is the first ultra-long-acting biologic product approved for use in its indicated conditions and was developed internally by GSK with an extended half-life and engineered high binding affinity to enable twice-yearly dosing, as demonstrated in GSK’s pivotal trials. To support in the engineering of the molecule, GSK internalized Adimab’s proprietary yeast-based technology, enabling in-house antibody discovery, optimization, production, and characterization on any target of GSK’s choosing. GSK’s research team used the Adimab Platform for depemokimab, a product tailored to meet GSK’s target product profile, including low picomolar affinity. GSK continues to use the Adimab platform to support other internal programs. “Depemokimab is the first approved product to emerge from our Platform Transfer collaborations, further validating this portion of our business model. Fittingly, GSK was our first Platform Transfer collaborator, and we congratulate them on this tremendous success,” said Philip T. Chase, Chief Executive Officer of Adimab. “Depemokimab is just one example of GSK’s adoption of the Adimab technology to pursue innovative therapeutic products,” added Eric Krauland, President and Chief Scientific Officer of Adimab. “GSK’s use of the platform, exemplified through ongoing investment in the Adimab team’s expertise and the use of Adimab's technological advances such as new library diversities, has translated into other GSK clinical programs that aim to make a real difference for patients.” Adimab’s other Platform Transfer collaborators include Biogen, Lilly, Merck, Novo Nordisk, and Takeda. Each Platform Transfer collaborator has been enabled, through training at Adimab and their own site, to operate Adimab’s proprietary platform independently. Further, each Platform Transfer collaborator has their own unique diversity, ensuring non-overlapping outputs. The Adimab technology can be used on any biologic target, in any format, and in any therapeutic area, allowing flexibility from discovery through engineering and generation of multispecifics. Support is always available, including access to Adimab scientists, biannual technology summits, and regular updates to strains, libraries, and in silico tools. Other commercial products containing molecules from Adimab include: Innovent’s TYVYT® (sintilimab injection), a PD1 program approved in China for the treatment of multiple cancers. Innovent’s SINTBILO® (tafolecimab injection), a PCSK9 program approved in China for the treatment of adult patients with primary hypercholesterolemia and mixed dyslipidemia. IASO Bio’s FUCASO® (equecabtagene autoleucel), a BCMA CAR-T program approved in China for the treatment of patients with multiple myeloma. Invivyd’s PEMGARDA™ (pemivibart), a SARS-CoV-2 monoclonal antibody authorized for prophylactic emergency use in the United States to prevent COVID-19 infection. Sun Pharma’s UNLOXCYT™ (cosibelimab), a PD-L1 program approved in the United States for the treatment of metastatic or locally advanced cutaneous squamous cell carcinoma. There are numerous additional Adimab-associated programs that are currently in Phase II or Phase III (pivotal) trials. The total number of Adimab-associated clinical programs initiated by our collaborators has now reached 90. About Adimab Adimab is the leading provider of therapeutic antibody discovery and engineering technologies. Our suite of technologies includes naïve discovery from synthetic libraries in yeast or B cells (mice, llamas, and humans), antibody engineering and optimization, bi- and multispecific antibody engineering, and a portfolio of proprietary CD3 and CD28 antibodies with complementary heterodimerization mutations that are licensed non-exclusively for bi- and multispecific applications. Adimab focuses solely on its partners and not on developing an internal product pipeline. Since 2009, Adimab has partnered with over 140 pharmaceutical and biotechnology companies, generating more than 650 therapeutic programs, 90 clinical programs, and 6 approved products. The Adimab technology has been transferred and implemented at GSK, Biogen, Novo Nordisk, Merck, Lilly, and Takeda. Funded discovery partners include leading pharmaceutical companies, such as Alnylam, Bristol Myers Squibb, Innovent, Novartis, Regeneron, Vertex and others. Adimab has also partnered with many early-stage venture-backed companies, including Dragonfly, NextPoint Therapeutics, Santa Ana Bio, Tizona, Kelonia, and others, as well as mid-size public biopharmaceutical companies such as Alector, Cullinan Therapeutics, Scholar Rock, and others. Adimab’s integrated antibody discovery and engineering platform provides unprecedented speed from antigen to purified, full-length human IgGs. Adimab offers fundamental advantages by delivering diverse panels of therapeutically relevant antibodies that meet the most demanding standards for affinity, epitope coverage, species cross-reactivity, and developability. Adimab enables its partners to rapidly expand their biologics pipelines through a broad spectrum of technology access arrangements. For more information, visit http://www.adimab.com.

Drug ApprovalPhase 3Phase 2

09 Apr 2026

·www.biopharmadive.com

Invivyd reveals plans to test an antibody drug against measles

Dive Brief:Invivyd said Thursday it has discovered and is preparing for human testing an antibody drug for measles, infections of which have spiked as of late in the U.S. due in part to rising vaccine hesitancy. The Connecticut-based biotechnology company also provided an update for its lead program, an antibody for COVID-19 prevention, alongside its plans for the new drugs development. Invivyd sees the antibody, known as VMS063, as a possible treatment for the disease or a preventive option for those who cant, or wont, get vaccinated.VMS063 uses a similar strategy as approved antibody drugs for respiratory syncytial virus, which work by latching onto a surface fusion protein and blocking entry into cells. Invivyd said VMS063 could be the first precision therapy for measles and address the immunity gap emerging due to lower vaccination rates.Dive Insight:Measles is one of the worlds most contagious infectious diseases, a potentially deadly infection that can cause pneumonia, brain swelling and weaken immune memory. Vaccines had nearlyeradicatedmeasles in the U.S. for decades. But a persistent rise in vaccine skepticism and rhetoric downplaying the diseases severity has led to a series of outbreaks thats left its elimination status in the U.S. in doubt.In its statement, Invivydhighlighted the newfound need that exists. Outbreaks occurred in more than 30 states in 2025, as well as the first measles deaths on U.S. soil in a decade. Dipping vaccination rates have put communities below the thresholds required for herd immunity, leaving what the company said are more than 9 million school-age children as well as millions more adults with weak immune systems vulnerable.Michael Mina, Invivyd's chief medical officer, noted in the company's statement that there aren't any approved treatments for symptomatic disease. And while the measles vaccine is the “cornerstone of measles prevention,“ doctors haven't had an option for those who are susceptible, such as infants too young to get vaccinated.As a treatment,VMS063 might be useful for eradicating symptoms more quickly or avoid the diseases worst complications. It could provide passive immunity to babies prior to vaccination, or be used in pre- or post-exposure settings to prevent or respond to outbreaks, the company said.Invivyd has advanced the therapy towards the studies that precede human testing and begun regulatory outreach that might support rapid development. The company hopes to be ready for those studies by late 2026.The program represents another chance at a rebound for Invivyd. Once known as Adagio Therapeutics, the company raised hundreds of millions of dollars in the early days of the COVID-19 pandemic, aiming to support development of antibodies that could treat or prevent coronavirus infections. The companys initial efforts fell short, however, causing its shares to plunge and its former CEO to resign.Afterwards, though, the company rebranded to Invivydand kept pushing ahead against COVID-19. It won an emergency use authorization in the U.S. for one antibody, Pemgarda, and has brought to late-stage testing a more advanced therapy, VYD2311,that it hopes to prove is more able to deal with evasive viral variants.Invivyd is approaching a Phase 3 readout for VYD2311 and, on Monday, said it boosted the size of its pivotal study. Results are now expected in the third quarter of 2026. '

VaccinePhase 3Emergency Use Authorization

09 Apr 2026

·www.biospace.com

Invivyd Announces REVOLUTION Program Progress and Advancement of Novel, Potential First- and Best-in-Class Measles Monoclonal Antibody Candidate VMS063 for Treatment and Prevention of Measles

Confirmed, pooled, blinded COVID-19 events in the ongoing Phase 3 DECLARATION study of VYD2311 accumulated to date (~ 50% of study progress) can already provide sufficient statistical power to support the high end of anticipated VYD2311 efficacy Invivyd conducted a pre-specified sample size re-estimation analysis when 1,500 of 1,818 enrolled patients reached Day 45 of 90 total days (April 6 th ), designed to add robustness given future event rate variability; that upsizing was triggered and increases confidence in overall study statistical power DECLARATION upsizing provides ~500 additional subjects and will likely shift study result timing modestly, by approximately two months, from original “mid-year” guidance to Q3 2026 Invivyd and the U.S. FDA have aligned on an initial Pediatric Study Plan for the BLA-directed pivotal pediatric immunobridging and safety “DRUMMER” clinical trial for VYD2311 Invivyd today announced the discovery and advancement of VMS063, a novel, highly potent, broadly in vitro neutralizing, high resistance barrier, half-life-extended, potentially first- and best-in-class monoclonal antibody candidate for the treatment and prevention of measles Invivyd has begun IND-enablement and regulatory outreach to support rapid VMS063 development; goal is expedited development with target IND readiness in late 2026 Management to host conference call this morning, April 9 th , at 8:30AM ET NEW HAVEN, Conn., April 09, 2026 (GLOBE NEWSWIRE) -- Invivyd, Inc. (Nasdaq: IVVD) today announced progress in its REVOLUTION clinical program for VYD2311, a novel monoclonal antibody investigational candidate for the prevention of symptomatic COVID-19. Invivyd also announced today the discovery and advancement of a novel, potentially first- and best-in-class measles monoclonal antibody candidate for treatment and prevention of measles discovered using Invivyd’s proprietary technology. DECLARATION Study Update and New “DRUMMER” Study The DECLARATION Phase 3 pivotal study is Invivyd’s Biologics License Application (BLA)-directed clinical trial assessing the safety and efficacy of single and multi-dose VYD2311 for the pre-exposure prophylaxis of COVID-19 compared to placebo over 90 days. The study includes a prospectively designed, conservative, algorithmic sample size re-estimation pooled, blinded analysis aimed at ensuring adequate COVID-19 clinical events and associated statistical power given the variability of COVID-19 attack rates in community. As of the sample-size re-estimation analysis, conducted when the first 1,500 (of 1,818 total) subjects reached Day 45 (April 6 th ), clinical events already accrued to date can support statistical powering for the high end of anticipated VYD2311 efficacy levels with approximately half of the base DECLARATION study still to go. The sample size re-estimation algorithm was designed conservatively with the aim of accomplishing strong statistical power to accommodate a range of potential VYD2311 efficacy results and COVID events in the trial, and upsizing was triggered. DECLARATION study upsizing includes approximately 500 additional subjects, in addition to 1,818 total randomized subjects in the initial population. Depending on recruitment rates, top-line results are now expected to shift from “mid-year” 2026 (defined as either 2 nd or 3 rd quarter), to in the third quarter of 2026. Invivyd will provide more detailed timing guidance as recruitment proceeds. The upsizing, combined with event accumulation to date, provides strong additional confidence and projected statistical support for a wider range of observed VYD2311 efficacy levels. Invivyd has also aligned with the U.S. Food and Drug Administration (FDA) on an initial Pediatric Study Plan for an efficient safety and immunobridging study to support potential BLA for VYD2311 in children aged 0-11 years. The “DRUMMER” study will be actioned only if the pivotal DECLARATION study is successful. Invivyd will provide more detailed guidance on DRUMMER study design and timing when appropriate. “We are thrilled with our progress in the DECLARATION study. Pooled, blinded COVID-19 event accumulation is already robust, and our conservative upsizing algorithm means that we can move to higher confidence in statistical power with very modest additional time. This re-sizing was designed prospectively with our rapid recruitment speed in mind and our desire for the most robust potential dataset. We have an extraordinary, high-value opportunity to change infectious disease medicine near-term,” noted Marc Elia, Chairman of the Invivyd Board of Directors. “We are pleased to add more confidence to our efforts to cement long-term change in COVID-19 prevention by making the multi-billion dollar category of repeat mRNA COVID vaccine boosts a second-line option, if indeed these vaccines remain on the market at all going forward. We continue to make great progress in the REVOLUTION program with the U.S. FDA, including aligning on a rapid pathway to pediatrics. This pathway, combined with our measles and previous RSV discoveries, should indicate that we are building on our work in COVID to create a fully integrated multi-virus platform company capable of rapidly generating high value medicines that have immediate utility in American infectious disease.” Novel Measles Antibody VMS063 Invivyd today also announced the discovery and advancement of a novel, highly potent, half-life-extended, high resistance barrier measles monoclonal antibody candidate, VMS063. VMS063 targets the measles Fusion (F) protein and is designed to lock the trimeric measles Fusion protein into a pre-fusion configuration, thereby preventing cell entry, similar to approved pediatric respiratory syncytial virus (RSV) monoclonal antibodies. VMS063 could be the first precision therapy for measles, as well as a potentially important passive prophylaxis option to supplement or enhance measles vaccination for certain populations at increased risk of symptomatic disease. VMS063 demonstrates highly potent in vitro neutralization of measles virus in gold-standard assays including in pseudovirus assays (high picogram / milliliter IC50s) and authentic measles virus assays (low single digit nanogram / milliliter IC50s) across relevant measles lineages such as currently circulating B3, D8, and ancestral Edmonston lineages, as well as against multiple polymorph variants derived from current clinical sequencing. The epitope targeted by VMS063 on the measles F protein is conserved across all described measles variants in global circulation across the past ~50 years. VMS063 is half-life extended to support the best possible prophylactic and therapeutic pro a single dose, and exhibits excellent biophysical characteristics associated with high developability, stability, and manufacturing yields. Invivyd has moved VMS063 towards IND-enabling studies and manufacturing for near-term clinical development. The United States is facing a critical measles virus inflection point in 2026, with measles incidence reaching levels not seen in decades. In 2025, outbreaks spanned more than thirty states and the first measles deaths in a decade were reported on U.S. soil. As of March 2026, U.S. disease burden in 2026 is on track to exceed 2025. As pediatric and community vaccination rates dip below the thresholds required for herd immunity, a significant “immunity gap” has emerged. More than nine million school-age children are estimated to be unprotected against measles in the U.S. today along with many millions more adults who are immune compromised. More, as one of the most infectious viruses known to exist, and as a virus uniquely capable of destroying human immunologic memory, measles has the potential to impose a substantial burden on the healthcare system as infection spreads. “There is no authorized or approved treatment for symptomatic measles, which, while often self-limiting, carries meaningful probability of serious complications including encephalitis and other inflammatory acute manifestations of disease, up to and including death.” said Michael Mina, M.D., Ph.D., Chief Medical Officer of Invivyd. “The measles vaccine is among the greatest achievements in the history of public health and remains the cornerstone of measles prevention. But vaccines have limits, and for too long, clinicians have lacked an adequate option for a range of patients left vulnerable, including infants too young for vaccination, pregnant women, and immunocompromised persons. These populations represent millions of Americans facing a rapidly resurging virus with nothing between them and infection. This is the gap we are proudly working to fill.” The potential therapeutic and prophylactic applications of VMS063 include the following unmet needs and major medical use cases: 1) Treatment of symptomatic measles, with the aim of shortening duration of symptoms and reducing severe complications such as encephalitis or opportunistic infections subsequent to measles’ post-acute “immune amnesia.” 2) Pre- and post-exposure passive prophylaxis to prevent or respond to outbreaks, and to provide a more physiologic, targeted alternative to the measles vaccine, with the aim of re-establishing functional eradication without requiring additional vaccination or vaccination of vaccine-hesitant populations. 3) Early childhood passive prophylaxis (akin to RSV) to cover the pre-vaccine pediatric risk window and bridge infants to safe, optimal vaccination. Such strategy can include the aim of improving measles vaccination by safely delaying vaccination to enable greater early childhood immunologic and neurocognitive development prior to vaccination. Invivyd plans to provide further discovery updates on additional pathogens that may offer similar opportunities for advancing standard of care via monoclonal antibody later in 2026. Conference Call & Webcast Listeners can register for the webcast via this link . Analysts wishing to participate in the question-and-answer session should use this link . A replay of the webcast will be available via the company’s investor website approximately two hours after the call’s conclusion. Those who plan on participating are advised to join 15 minutes prior to the start time. About VYD2311 VYD2311 is a novel monoclonal antibody (mAb) candidate being developed for COVID-19 to continue to address the urgent need for new prophylactic and therapeutic options. The pharmacokinetic pro antiviral potency of VYD2311 may offer the ability to deliver clinically meaningful titer levels through more patient-friendly means such as an intramuscular route of administration. VYD2311 was engineered using Invivyd’s proprietary integrated technology platform and is the product of serial molecular evolution designed to generate an antibody optimized for neutralizing contemporary virus lineages. VYD2311 leverages the same antibody backbone as pemivibart, Invivyd’s investigational mAb granted emergency use authorization in the U.S. for the pre-exposure prophylaxis (PrEP) of symptomatic COVID-19 in certain immunocompromised patients, and adintrevimab, Invivyd’s investigational mAb that has a robust safety data package and demonstrated clinically meaningful results in global Phase 2/3 clinical trials for the prevention and treatment of COVID-19. About DECLARATION DECLARATION (NCT07298434) is a Phase 3, randomized, triple-blind, placebo-controlled trial to evaluate VYD2311 efficacy and safety in prevention of symptomatic COVID in a broad population of participants including adults and adolescents both with and without risk factors for progression to severe COVID-19, at three months. Participants will receive either a single dose or a monthly dose of VYD2311, each administered via intramuscular (IM) injection, compared to placebo. Total enrollment of the trial is expected to be 1770 participants. About VMS063 VMS063 is a monoclonal antibody candidate engineered via Invivyd’s proprietary antibody discovery platform to target a highly conserved protein of a measles virus. The antibody has shown sub-nanomolar potencies across all variants tested in vitro to date. About Invivyd Invivyd, Inc. (Nasdaq: IVVD) is a biopharmaceutical company devoted to delivering protection from serious viral infectious diseases, beginning with SARS-CoV-2. Invivyd deploys a proprietary integrated technology platform unique in the industry designed to assess, monitor, develop, and adapt to create best in class antibodies. In March 2024, Invivyd received emergency use authorization (EUA) from the U.S. FDA for a monoclonal antibody (mAb) in its pipeline of innovative antibody candidates. Visit to learn more. Trademarks are the property of their respective owners. Cautionary Note Regarding Forward-Looking Statements This press release contains forward-looking statements within the meaning of the Private Securities Litigation Reform Act of 1995. Words such as “anticipates,” “believes,” “could,” “expects,” “estimates,” “intends,” “plans,” “potential,” “predicts,” “projects,” “future,” and “target” or similar expressions (as well as other words or expressions referencing future events, conditions or circumstances) are intended to identify forward-looking statements. Forward-looking statements include statements concerning, among other things, plans related to the company’s research and development activities, and the timing and potential results thereof; expectations regarding the company’s clinical trial designs, enrollment, event accumulation and progress, regulatory pathway, product profile, indication, patient populations, and administration paradigm for VYD2311, including the company’s REVOLUTION clinical program and the timing of results related thereto; the potential of VYD2311 as a novel mAb candidate for the prevention of COVID-19; the estimated market for COVID-19 vaccination; the company’s devotion to delivering protection from serious viral infectious diseases; the potential of VMS063 as a potential first- and best-in-class mAb candidate for treatment and prevention of measles; expectations regarding the measles landscape, including the potential burden of measles on the healthcare system, and beliefs about the potential therapeutic and prophylactic applications of VMS063; the potential of Invivyd to create a fully integrated multi-virus platform company capable of rapidly generating high value medicines that have immediate utility in American infectious disease; the company’s expectations about potential pipeline expansion and future announcements related thereto; and other statements that are not historical fact. The company may not actually achieve the plans, intentions, or expectations disclosed in the company’s forward-looking statements and you should not place undue reliance on the company’s forward-looking statements. These forward-looking statements involve risks and uncertainties that could cause the company’s actual results to differ materially from the results described in or implied by the forward-looking statements, including, without limitation: the timing, progress, and results of the company’s discovery, preclinical, and clinical development activities, including with respect to VYD2311 and VMS063; whether or not any preclinical candidate identified by the company is determined to be suitable for clinical development; clinical trial site activation, enrollment, and event accumulation rates; the risk that results of nonclinical studies or clinical trials may not be predictive of future results, and interim data are subject to further analysis; the predictability of clinical success of the company’s product candidates based on neutralizing activity in nonclinical studies and the assessment of other in vitro properties; potential variability in neutralizing activity of product candidates tested in different assays, such as pseudovirus assays and authentic assays; unexpected safety or efficacy data observed during preclinical studies or clinical trials; variability of results in models and methods used to predict neutralizing activity; changes in the regulatory environment; the outcome of the company’s engagement with regulators; uncertainties related to the regulatory authorization or approval process, and available development and regulatory pathways; the company’s ability to generate the data needed to support a potential BLA submission for VYD2311; how long the EUA granted by the FDA for pemivibart will remain in effect and whether such EUA is revised or revoked by the FDA; the ability to maintain a continued acceptable safety, tolerability, and efficacy pro any product candidate following regulatory authorization or approval; whether the epitopes that pemivibart and VYD2311 target remain structurally intact and the company’s product candidates are able to demonstrate and sustain neutralizing activity against major SARS-CoV-2 variants, particularly in the face of viral evolution; the risk that a lack of awareness of mAb therapies and regulatory scrutiny of mAb therapies to prevent or treat COVID-19 or other infectious diseases may adversely impact the development or commercial success of the company’s product candidates; changes in expected or existing competition; the company’s reliance on third parties; complexities of manufacturing mAb therapies; macroeconomic and political uncertainties; and whether the company has adequate funding to meet future operating expenses and capital expenditure requirements. Other factors that may cause the company’s 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 the company’s Annual Report on Form 10-K for the year ended December 31, 2025, as filed with the Securities and Exchange Commission (SEC), and in the company’s other filings with the SEC, and in its future reports to be filed with the SEC and available at Forward-looking statements contained in this press release are made as of this date, and Invivyd undertakes no duty to update such information whether as a result of new information, future events or otherwise, except as required under applicable law. This press release contains hyperlinks to information that is not deemed to be incorporated by reference in this press release. Contacts: Media Relations (781) 208-0160 media@invivyd.com Investor Relations (781) 208-1747 investors@invivyd.com

Phase 3VaccineClinical ResultEmergency Use AuthorizationImmunotherapy

100 Deals associated with Pemivibart

R&D Status

10 top approved records.

to view more data

Indication	Country/Location	Organization	Date
COVID-19	United States	Invivyd, Inc.	22 Mar 2024

Clinical Result

Indication

Phase

Evaluation

View All Results

Study	Phase	Population	Analyzed Enrollment	Group	Results	Evaluation	Publication Date


NCT06039449 (CANOPY, Pubmed \| Infect Dis Ther)	Phase 3	COVID-19	1,500	Pemivibart	ntwvcsvlla(cictgpxgxd) = qfgfixixpm pnhuqjosdm (xlyijyephu )	Positive	16 Feb 2026
				ChulaVac	ntwvcsvlla(cictgpxgxd) = yyefujaoul pnhuqjosdm (xlyijyephu )
NCT06039449 (CANOPY, Pubmed) Manual	Phase 3	COVID-19	-	Pemivibart (cohort A)	qxojimgicr(ubnnfsbfjk) = bvbgxqhhpl gmedleihdc (nvdvgtewgh ) View more	Positive	24 May 2025
				Pemivibart (cohort B)	qxojimgicr(ubnnfsbfjk) = xuvciwheqb gmedleihdc (nvdvgtewgh ) View more
NCT06039449 (CANOPY, GlobeNewswire) Manual	Phase 3	COVID-19	-	Pemivibart (0-9 months; Following Cessation of Dosing)	ztopsdoimv(tuxtvrhfqc) = yoizqnksjb zbasdgdguj (wzdzsoetvm )	Positive	29 Oct 2024
				Placebo (0-9 months; Following Cessation of Dosing)	ztopsdoimv(tuxtvrhfqc) = sjgfnffagl zbasdgdguj (wzdzsoetvm )
NCT06039449 (CANOPY, GlobeNewswire) Manual	Phase 3	COVID-19	-	Pemivibart	oradksxors(rbhvlzrsbv) = zsllofnnej nfkmfeexyv (ohqcfbpjye )	Positive	27 Aug 2024
				Placebo	oradksxors(rbhvlzrsbv) = fcpwettomm nfkmfeexyv (ohqcfbpjye )
NCT06039449 (CANOPY, Biospace) Manual	Phase 3	COVID-19	790	VYD222 (moderate-to-severe immune compromise)	dmwffgerwv(qhxwiakuae) = anpqkkmldh tmwbxjxsri (gkqsmafkud )	Positive	22 Mar 2024
				VYD222 (without moderate-to-severe immune compromise)	dmwffgerwv(qhxwiakuae) = qrxwajsxgo tmwbxjxsri (gkqsmafkud )
NCT06039449 (CANOPY, Corporate Publications) Manual	Phase 3	COVID-19	790	VYD222	bconnlwelh(amdbiipddf) = no report hlevictrqt (jdqysfcznp ) View more	Positive	18 Dec 2023

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