George D. Yancopoulos
Co-Founder, President, Chief Scientific Officer at Regeneron Pharmaceuticals
Thank you, Len, the first quarter of 2023 delivered multiple significant milestones for Regeneron and for our collateral collaborations. From the positive DUPIXENT Phase 3 COPD data to progress in our oncology pipeline as well as exciting new landmarks from our genetic medicines programs.
Starting with DUPIXENT, in March together with our Sanofi collaborators, we announced DUPIXENT was the first new mechanism-of-action treatment to produce statistically significant and clinically meaningful results in a Phase 3 trial for COPD in over a decade. Our BOREAS trial enrolled COPD patients with moderate-to-severe disease and evidence of Type 2 inflammation. DUPIXENT-treated patients demonstrated a clinically meaningful, 30% reduction in exacerbations, a significant improvement in lung function as well as quality-of-life benefits and impressive trifecta and a potential paradigm-changing treatment for this deadly disease. We are looking forward to presenting the details BOREAS result in a late-breaking presentation at the upcoming American Thoracic Society Meeting later this month. We also plan to discuss these exciting results with regulatory authorities and expect to report results mid-next year for the replicate Phase 3 NOTUS study.
I would remind you that we are also trying to address in overlapping COPD population with our IL33 antibody which is in Phase 3 studies, based on positive Phase 2 proof-of-concept data. This approach is further supported by genetic analysis from our Regeneron Genetic Center, which demonstrated association of loss-of-function interleukin 33 with reduced COPD risk. Similar genetic analysis support the role for a DUPIXENT benefit in COPD.
The BOREAS COPD data indicate that DUPIXENTcan help even more patients beyond the five current FDA-approved indications in diseases caused or exacerbated by Type 2 inflammation including atopic dermatitis, asthma, chronic line of sinusitis with nasal polyps eosinophilic esophagitis and prurigo nodularis. We are also expecting an FDA decision for DUPIXENT for chronic spontaneous urticaria on October 22, 2023, and we are continuing to tell DUPIXENT development to patients with other Type 2 inflammatory diseases, most likely to be responsive to this method.
Moving to Oncology, with the progress of our late and early-stage pipeline, we are looking forward to several important milestones this year. Starting with Libtayo, in addition to expanded use in lung cancer, Libtayo was recently added to the NCCN guidelines for new adjuvant treatment of CSCC. Libtayo U.S. label is also recently updated with more mature CSCC and BCC data, supporting its differentiated clinical profile in these tumor settings and satisfying all post-marketing commitments in required full approval in these indications.
Regarding our exciting new combinations with Libtayo, starting with Fianlimab or LAG3 antibody for which we are planning a broad pivotal program spanning several cancer indications. These efforts were triggered by our robust and confirmed data in first line metastatic melanoma patients, which will be presented in further detail at ASCO, suggesting that the Fianlimab-Libtayo combination could produce about double the response rates with longer progression-free survival anti-PD monotherapy standard.
Based on this, we have already initiated pivotal trials in metastatic and adjuvant melanoma and started studying perioperative melanoma in the second half of the year. In addition, based on promising data in similar patient cohorts, we saw a seamless Phase 2/3 pivotal study for treatment of metastatic non-small cell lung cancer, and we will soon start a Phase 2 study in the perioperative setting.
Next bispecific for solid tumors, which are being investigated in combination with Libtayo. Earlier this year at ASCO GU, we presented initial positive first-in human data for our PSMA by CD28 costimulatory bispecific in combination with Libtayo in advanced prostate cancer, a tumor type considered immunologically cold and largely unresponsive to anti-PD-1 therapy alone. Over the next 12 months, we plan to present updated PSMA by CD28 data in more patients, some of which will have been prophylactically treated with our anti-IL 6 receptor antibody, sarilumab to potentially reduce the severity of immune-mediated side-effects, while maintaining or improving anti-tumor activity.
Also during this timeframe, we plan to present data in advanced ovarian cancer for both our MUC16xCD3 bispecific and our MUC16xCD28 costimulatory bispecific as well as data in several tumor types from our EGFRxCD28 costimulatory bispecific, all-in combination with Libtayo.
Our hematology oncology pipeline continues to advance. In an oral presentation at the upcoming ASCO Annual Meeting, we will present updated data for linvoseltamab, our BCMAxCD3 bispecific tested in late-line multiple myeloma. We believe these data will show that linvoseltamab has the best-in class potential with differentiated efficacy, safety and a favorable dosing schedule in the competitive environment of relapsed-refractory multiple myeloma treatment candidates. We remain on track for a regulatory submission in the United States in the second half of this year for linvoseltamab. For Odronextamab, our CD20xCD3 bispecific, we are on track to complete U.S. and EU regulatory submissions for both relapsed or refractory follicular lymphoma and diffuse large B-cell lymphoma in the second half of this year. Odronextamab in late-line relapsed refractory follicular lymphoma has a potential best-in class efficacy profile and our optimized step of dosing regimen has improved Odronextamab safety profile without impacting efficacy.
Also, we have initiated a first in-human study of our CD22xCD28 costimulatory bispecific in combination with Odronextamab in relapsed-refractory DLBCL, which we hope could further improve upon the anticancer benefit for these patients.
Now the Genetics Medicines, starting with our collaboration with Alnylam an siRNA therapeutics. Just last week, Alnylam announced an important update for ALN-APP program in early onset, Alzheimer's disease. For the first time an RNAi Therapeutic demonstrates sustained silencing of a pathological team in the central nervous system in a clinical trial. In our earnings call this morning, our Alnylam collaborator provided additional details on these results. Our siRNA approach aims to prevent production of amyloid precursor protein as opposed to clearing existing amyloid plaques after they have already formed, providing a new way to potentially address Alzheimer's disease, which we'll still have a devastating impact on patients and their families even with the emergence of amyloid clearing antibodies.
Patients treated with single doses of ALN-APP experienced dose dependent rapid and sustained reduction of up to 90% in APP production as assessed by biomarkers in cerebrospinal spinal fluid. The safety and tolerability profile with single dosing is encouraging so far. While, the multi-dose Part B portion of the studies on partial clinical hold in the United States due to findings observed in prior non-clinical chronic toxicology studies Part B has already received regulatory approval to proceed in Canada with the majority of the Part A clinical trial patients had been enrolled. Detailed results from the study will be presented at upcoming medical meeting. We are looking forward to advancing additional development candidates for the many other neurodegenerative diseases that currently have few or no therapeutic options, such as other targets for Alzheimer's, as well as for ALS or Lou Gehrig's disease, Parkinson's and Huntington's.
In addition to these exciting developments in the central nervous system diseases, we are continuing our progress with liver-targeted medicines, including a broad and multi-pronged approach to develop treatments for NASH or Non-Alcoholic Steatohepatitis. We're enrolling a Phase 2 study of ALN-HSD in NASH patients with genetic risk factors continuing claims development of ALN-PNP and we are planning to progress additional more recently genetically validated NASH targets as well.
Finally. I would like to highlight our recently announced collaboration with Sonoma Biotherapeutics' discover, develop and commercialize regulatory T-cell therapies for autoimmune and inflammatory diseases. This collaboration will bring together our industry-leading technologies for the discovery and characterization of fully human antibodies and T-cell receptors, as well as our additional biologics candidates with Sonoma's pioneering approach to developing and manufacturing gene-modified T-reg cell therapies. In conclusion, Regeneron's R&D engine truly continues its productivity in both late and early-stage pipeline.
Before turning the call over to Marion, I would also like to thank Roy Vagelos for serving as a role model for all of us at Regeneron as well as for so many others across the industry. I hope that we can continue to live up to the high stage that Roy has set over his distinguished career.
With that, I will turn the call over to Marion.
