George Yancopoulos
Board Co-Chair, Co-Founder, President and Chief Scientific Officer at Regeneron Pharmaceuticals
Thank you, Len. I would like to start with our recent update on aflibercept 8-milligram data in DME that Len referred to. At the Annual American Society of Retina Specialists Meeting, we presented the two-year results from our PHOTON study. These data demonstrated that the vast majority of aflibercept 8-milligram patients randomized to the 12-week and 16-week dosing intervals continued to sustain vision and anatomic improvements through 96 weeks. 89% of all aflibercept 8-milligram patients were able to maintain at least every 12-week dosing intervals for the entire two-year period, while 84% of patients assigned to every 16-week dosing at baseline were able to maintain that interval or extend beyond it. On that point, many patients met the criteria for extension to longer intervals, with 44% meeting the criteria for greater than 20-week dosing intervals, including 27% who were eligible for 24-week dosing intervals.
The safety profile of aflibercept 8-milligram remained consistent with EYLEA. Sustaining vision and anatomic improvements while maintaining such extended dosing intervals over two years is unprecedented in the field. Our results further strengthen the clinical profile of aflibercept 8-milligram and position this investigational medicine to become the future standard of care for retinal diseases. Later in the third quarter, we and Bayer are planning to share initial results from the second year analysis of the PULSAR study in patients with wet AMD.
Moving to our immunology and inflammation pipeline on Dupixent. We look forward to the FDA decision for our sBLA in chronic spontaneous urticaria by October 22, 2023. In terms of Dupixent in patients with COPD, we and Sanofi are pleased to announce that Dupixent was granted breakthrough designation for uncontrolled COPD with an eosinophilic phenotype based on the positive results of the Phase 3 BOREAS study. Based on ongoing discussions with the FDA, we expect that in addition to the BOREAS study results, we will need to provide data from the replicate Phase 3 NOTUS study to support a BLA and such data requirements remain under discussion with the FDA. We continue to expect final results for the NOTUS study by mid-2024.
Moving to itepekimab, our anti-IL-33 antibody, which is being evaluated for COPD in former smokers. In May, Sanofi announced that the Phase 3 AERIFY-1 and AERIFY-2 studies had passed an interim futility analysis. These studies remain on track for readout and regulatory submissions in 2025. Both the itepekimab and Dupixent could transform the treatment paradigm for COPD by levering their distinct mechanism of action in reducing different types of inflammation that contribute to COPD.
Moving to oncology and combinations with Libtayo. In June, in an oral presentation at the ASCO conference, we presented data for the combination of fianlimab, our LAG-3 antibody, plus Libtayo, which showed consistent response rates ranging from 56% to 63% across three independent cohorts of advanced melanoma patients, including a new cohort of patients who had received prior anti-PD-1 therapy in the adjuvant melanoma setting. These response rates represent about double the rate historically seen with anti-PD-1 monotherapy in similar settings and clinically meaningful responses were observed in post-hoc analysis of various populations of interest, including patients with poor prognosis factors and varying tumor PD-L1 expression levels.
The safety profile of fianlimab and Libtayo combination in these cohorts appears to be generally consistent with the safety profile of Libtayo monotherapy and other anti-PD-1 or PD-L1 agents, except for the higher rates of adrenal insufficiency, which were Grade 2 or lower in the majority of cases, with all cases successfully managed with steroid replacement. Our fianlimab plus Libtayo Phase 3 studies in metastatic and adjuvant melanoma are enrolling patients as are the Phase 2 portions of the Phase 2/3 studies in advanced non-small cell lung cancer.
Next on to bispecifics for solid tumors, which are being investigated in combination with Libtayo and other modalities. Later this year, we are planning to share initial clinical data for the combination of ubamatamab, our MUC16xCD3 bispecific plus Libtayo in advanced ovarian cancer. Last year we showed encouraging ubamatamab monotherapy data in advanced ovarian cancer and we believe that combining it with Libtayo may lead to enhanced anti-tumor activity.
Moving to costimulatory bispecifics. We are currently exploring multiple different CD28 costimulatory bispecific antibodies in early clinical trials in a variety of tumor settings, in combination with Libtayo, or with corresponding CD3 bispecifics.
In our Phase 1 study of REGN5678, our PSMAxCD28 costimulatory bispecific in advanced prostate cancer in combination with Libtayo which has demonstrated promising anti-tumor activity. The safety profile of this combination continues to pose a challenge, highlighted by a recently observed second Grade 5 adverse event or death. Although serious immune-mediated adverse events continue to be highly correlated to patients who experience profound responses, we have decided to discontinue enrollment of new patients with the full dose Libtayo combination. And explore PSMAxCD28 combination with lower doses of Libtayo. We also will continue to explore PSMAxCD28 as a monotherapy where we are seeing antitumor activity in some patients and we will explore PSMAxCD20 in combination with other immunotherapy modalities.
We believe our prostate cancer data support the exciting potential of costimulatory bispecifics, but with the challenge of focusing the response solely to the tumor. Our preclinical studies and mechanistic insights suggest a degree of immune-related adverse events seen when combining costims with PD-1 blockade may depend on the particular costim target and tumor types.
Moreover, combining costims with CD3 bispecifics may not result in these types of severe immune-mediated adverse events. Along these lines, our other costimulatory bispecifics programs continue, including our MUC16xCD28 costim with Libtayo and our MUC16xCD28 costim with ubamatamab, both in ovarian cancer. As well as our EGFRxCD28 costim with Libtayo in colorectal and other cancers.
In these early dose escalation studies, we have observed limited immune-mediated toxicities to date. We're also excited about combining our costimulatory bispecifics with our CD3 bispecifics in our hem/onc programs, which continue to progress. We have initiated dosing of our CD22xCD28 costimulatory bispecifics with odronextamab, our CD20xCD3 bispecific in relapsed/refractory diffuse large B-cell lymphoma, which we hope can improve on the impressive efficacy demonstrated by odronextamab alone in that setting. In terms of odronextamab monotherapy, U.S. and EU regulatory submissions for both relapsed or refractory follicular lymphoma and diffuse large B-cell lymphoma remain on track.
Regarding linvoseltamab, or BCMAxCD3 bispecific, we recently presented updated data at the ASCO annual meeting, demonstrating early, deep and durable responses in patients with heavily pretreated multiple myeloma with 71% objective response rate and 59% of patients achieving a very good partial response or better at the recommended 200-milligram dose with a median follow-up of only six months with the data potentially improving as they mature.
We believe these data support linvoseltamab's best-in-class potential with differentiated efficacy, safety, hospital requirements and favorable dosing schedule. In the fourth quarter of this year, we are planning to present additional data with longer follow-up and to submit regulatory applications for linvoseltamab. We also plan to start combination studies with a myeloma-specific costim next year.
Next, to genetic medicines. In the second quarter, we and Alnylam jointly announced the first human data suggesting that an siRNA can be used to silence pathological genes in the brain, which may open up an entirely new approach for fighting back against neurodegenerative and other central nervous system diseases. We plan to initiate additional clinical programs for CNS diseases next year.
As announced by our collaboration with Intellia, we plan to initiate the first in vivo CRISPR-based Phase 3 clinical program by year-end, subject to regulatory feedback in patients with transthyretin amyloidosis cardiomyopathy. And in terms of our targeted gene delivery pipeline, we hope to initiate our first clinical program in 2024 for hemophilia B.
In conclusion, Regeneron's R&D engine continues to grow and deliver differentiated late and early-stage opportunities, and we are looking forward to several important clinical milestones in the second half of this year.
With that, I will turn the call over to Marion.
