A Multicenter, Open-label, Phase 3 Extension Study to Evaluate the Long-term Efficacy and Safety in Participants Who Are Currently on Treatment in a Belzutifan Study (LITESPARK-043)

Researchers are looking for new ways to treat advanced solid tumors and von Hippel-Lindau (VHL)-related tumors:
* Advanced means the cancer has spread to other parts of the body (metastatic) or cannot be removed with surgery
* Solid tumors are cancers mostly in body organs and tissues, not in the blood or other body liquids
* VHL-related tumors are tumors caused by VHL disease. VHL disease is passed down from parents to children and people with VHL disease have a higher chance of getting certain types of cancer
Researchers want to learn about the long-term effects of a trial medicine called belzutifan. Belzutifan, also called MK-6482, is designed to block a protein that helps tumors grow and survive. This is an extension trial, which means only people who were in certain other belzutifan trials (called parent trials) may be able to join. The goal of this trial is to learn how long people live after they start taking belzutifan.

Start Date23 Mar 2026

Sponsor / Collaborator

Merck Sharp & Dohme LLC

NCT07347600

/ RecruitingNot Applicable

A Prospective Non-interventional Study to Evaluate the Effectiveness and Safety of Inavolisib in Patients With Endocrine-resistant, PIK3CA-mutated, Hormone Receptor-positive, HER2-negative Locally Advanced or Metastatic Breast Cancer (reaINAVO)

The main purpose of this study is to evaluate the effectiveness of inavolisib based regimen in participants with endocrine-resistant, phosphatidylinositol-4,5-bisphosphate 3-kinase catalytic subunit alpha gene (PIK3CA)-mutated, hormone receptor-positive (HR+), human epidermal growth factor receptor 2-negative (HER2-) locally advanced or metastatic breast cancer (LA/mBC), following on or after completing adjuvant endocrine therapy in routine clinical practice in China.

Start Date21 Jan 2026

Sponsor / Collaborator

Roche Holding AG

NCT07191977

/ Not yet recruitingPhase 2IIT

Neoadjuvant Camrelizumab With Palbociclib for the Treatment of Resectable Esophageal Squamous Cell Carcinoma: A Single-Arm Phase 2 Trial

The goal of this Phase 2 clinical trial is to learn if the combination of Camrelizumab and Palbociclib is a safe and effective treatment when given before surgery (neoadjuvant therapy) for patients with esophageal squamous cell carcinoma (ESCC) that can be surgically removed. Camrelizumab is an immunotherapy drug that helps the immune system fight cancer, and Palbociclib is a targeted therapy drug that stops cancer cells from growing.
The main questions it aims to answer are:
Is the combination of Camrelizumab and Palbociclib safe for patients to receive before their surgery? How effective is this treatment combination in shrinking tumors prior to surgery?

Start Date01 Jan 2026

Sponsor / Collaborator

West China Hospital

100 Clinical Results associated with Palbociclib

100 Translational Medicine associated with Palbociclib

100 Patents (Medical) associated with Palbociclib

3,306

Literatures (Medical) associated with Palbociclib

31 Dec 2026·Journal of Pharmaceutical Policy and Practice

Economic evaluation of cyclin-dependent kinases 4 and 6 inhibitors in advanced hormonal receptor-positive and human epidermal growth factor receptor 2 negative breast cancer: a nationwide budget impact analysis

Article

Author: Hamad, Anas ; Shafei, Laila ; Hisham Al-Ziftawi, Nour ; Bojassoum, Salha ; Mohamed Ibrahim, Mohamed Izham ; Elazzazy, Shereen

Background:

Several trials demonstrated improvements in clinical outcomes associated with cyclin-dependent kinase 4 and 6 (CDK4/6) inhibitors in breast cancer patients. The challenge remains regarding their high costs. Ribociclib and Abemaciclib are cost-effective in Qatar. Yet, their affordability was not studied. This budget impact analysis (BIA) is to assess the affordability of adopting CDK4/6 inhibitors in Qatar over five years duration (2024-2028).

Methods:

We ran a BIA to evaluate two scenarios: (1) Increasing abemaciclib's market share from 20% to 60%, replacing both palbociclib and ribociclib. (2) Assuming equal market share for both ribociclib and abemaciclib up to 80%, reducing palbociclib's share. The analysis considered treatment costs, patient population, and disease prevalence. All data were retrieved from the National Center for Cancer Care and Research, and costs were presented in Qatari Riyals (QAR). Sensitivity analyses were run to ensure the robustness of the conclusion. All results were compared to Qatar's budget threshold, which is QAR 453,822.

Results:

Based on a total of 173 patients using CDK4/6 inhibitors, increasing abemaciclib's market share to 60% yielded cumulative savings of QAR 14 million over five years, which is around QAR 14,613 per patient per year. However, equally increasing ribociclib's and abemaciclib's market share to 80% resulted in a modest budget increase, remaining within acceptable thresholds. Sensitivity analyses confirmed the robustness of these findings, showing that cost reductions and higher uptake rates further enhanced savings.

Conclusion:

Abemaciclib is a budget-saving option for HR+/HER2- breast cancer in Qatar, should it replace the market share by up to 60% over five years. In addition, ribociclib and abemaciclib are affordable treatment options if they equally contributes to up to 80% of the market share for the eligible advanced breast cancer patients. The results supported the concept of allocating CDK4/6 inhibitors as they were found to be affordable to the Qatari healthcare system.

01 Dec 2026·MOLECULAR BIOLOGY REPORTS

Possible TLR-mediated immunostimulatory effect of Palbociclib in breast cancer

Article

Author: Sağ, Sevda ; Tomatir, Ayse Gaye ; Ergezgin, Huriye ; Bayav, Ibrahim ; Dodurga, Yavuz

BACKGROUND:

Palbociclib, which exerts its effect by inhibiting the cell cycle in cancer cells, is a CDK inhibitor used in the treatment of ER+/HER- breast cancer. In this study, we aimed to investigate the effect of Pablosiklib on TLR, which plays an important role in the immune response, in MCF-7 (ER+/HER2-) and MDA-MB-231 (ER-/PR-/HER2-) cell lines.

METHODS AND RESULTS:

The expression levels of TLR 1-10 genes, cell cycle-related genes (CDK4/6), and genes involved in the apoptotic pathway (Bcl-2, Bax, Cas-3) in MCF-7 and MDA-MB-231 cells treated with palbociclib were evaluated using the real-time PCR (qRT-PCR) method. Additionally, the levels of total retinoblastoma (RB) and phosphorylated retinoblastoma (pRB) proteins were analyzed using the Western blot method. CDK4/6 and pRB expression decreased in MCF-7 and MDA-MB-231 cells treated with palbociclib. Bax and Cas-3 expression increased, while Bcl-2 expression decreased. Changes in TLR expression were also observed.

CONCLUSIONS:

We believe that palbociclib not only stops the cell cycle and induces apoptosis in breast cancer cells, but also activates the immune response via TLRs.

01 Jun 2026·SPECTROCHIMICA ACTA PART A-MOLECULAR AND BIOMOLECULAR SPECTROSCOPY

Novel active site -targeted fluorescent probes for real-time monitoring of CDK4/6 in tumor cells and tissues

Article

Author: Qi, Shixiang ; Qin, Leyan ; Cheng, Mingyu ; Wang, Xu ; Liu, Wenjie ; Chen, Haifeng ; Dong, Gaopan ; Gao, Yuqi ; Wang, Mengqi ; Liu, Tingting ; Zhang, Xinxin

Breast cancer is the leading female malignancy, and CDK4/6, key members the cyclin-dependent kinases (CDK) family, have become validated therapeutic targets. However, small-molecule tools that can track these kinases in living cells and tissues remain scarce. Therefore, guided by the co-crystal structure of the CDK4/6 inhibitor Palbociclib, we carried out two rounds of optimization to develop a mini-library of fluorescent probes (Q1-Q9) and subsequently screened them for selective labeling capability. Docking and biochemical assays confirmed that the new ligands retain the binding mode of Palbociclib. Among them, Q2 exhibited good affinity for CDK4 and CDK6 (IC₅₀ = 151 ± 43 nM and 193 ± 70 nM, respectively) and provided exceptional, higher-resolution images of the kinases in live cells, outperforming antibody staining. The probe may serve as a cost-effective, stable and user-friendly alternative to antibody staining, and a potential visualization tool of drug preliminary screening by showing the changed fluorescent signals when incubated with active compounds. Importantly, Q2 retained bioactivity, inducing cell-cycle arrest and suppressing tumor-cell growth, mirroring the activity of the parent inhibitor Palbociclib. Thus, Q2 is a ready-to-use chemical tool for real-time visualization of CDK4/6 dynamics and holds promise for improving the diagnosis and treatment of breast cancer.

511

News (Medical) associated with Palbociclib

26 Mar 2026

·www.biospace.com

Celcuity Inc. Reports Release of Fourth Quarter and Full Year 2025 Financial Results and Provides Corporate Update

The U.S. Food and Drug Administration (“FDA”) accepted Celcuity’s New Drug Application (“NDA”) and granted Priority Review with a Prescription Drug User Fee Act (“PDUFA”) goal date of July 17, 2026, for gedatolisib in HR+/HER2-/PIK3CA wild-type (“WT”) advanced breast cancer (“ABC”) Results from PIK3CA WT cohort of Phase 3 VIKTORIA-1 study of gedatolisib regimens in HR+/HER2- ABC published in Journal of Clinical Oncology Topline results from the PIK3CA mutant cohort of the Phase 3 VIKTORIA-1 study are expected to be released in the second quarter of 2026 Management to host webcast and conference call today, March 25, 2026, at 4:30 p.m. EDT MINNEAPOLIS, March 25, 2026 (GLOBE NEWSWIRE) -- Celcuity Inc. (Nasdaq: CELC), a clinical-stage biotechnology company pursuing development of targeted therapies for oncology, today announced financial results for the fourth quarter and full year ended December 31, 2025, and other recent business developments. “We expect this year to be a transformative one for Celcuity. We plan to release topline results from the PIK3CA mutant cohort of our Phase 3 VIKTORIA-1 study in the second quarter of 2026, which, if positive, could potentially advance the standard-of-care second line therapy for a significant number of patients with HR+/HER2- advanced breast cancer,” said Brian Sullivan, CEO and co-founder of Celcuity. “Additionally, our efforts remain on track to launch gedatolisib commercially in anticipation of its potential FDA approval in the third quarter of 2026.” Fourth Quarter 2025 Business Highlights and Other Recent Developments In December 2025, updated efficacy and safety results from the Phase 3 VIKTORIA-1 PIK3CA WT cohort were presented at the 2025 San Antonio Breast Cancer Symposium including patient sub-group analyses, safety analyses and patient reported outcomes for well-being measures. For patients enrolled in the U.S., Canada, Western Europe, and Asia Pacific, median progression free survival (“PFS”) was 16.6 months with the gedatolisib triplet (gedatolisib + fulvestrant + palbociclib) versus 1.9 months for fulvestrant (HR=0.14; 95% CI: 0.08-0.28; p<0.0001). The gedatolisib triplet delayed time to definitive deterioration versus fulvestrant according to patient reported outcomes for well-being measures that included mobility, self-care, usual activities, pain/discomfort, and anxiety/depression (the EQ-5D-5L score). The median time to definitive deterioration was 23.7 months (HR=0.39; 95% CI: 0.25-0.67; p = 0.0003) for patients treated with the gedatolisib triplet versus 4.0 months for fulvestrant. Additionally, for the first 8 cycles of treatment, the patients’ assessment of their well-being remained stable relative to their assessment prior to starting treatment with gedatolisib. As reported earlier, the gedatolisib triplet was generally well tolerated in the trial with mostly low-grade treatment-related adverse events (“TRAEs”). The most common Grade 3+ TRAEs for the gedatolisib triplet and fulvestrant included neutropenia (62.3% and 0.8% of patients, respectively); stomatitis (19.2% and 0%); rash (4.6% and 0%); and hyperglycemia (2.3% and 0%). No patients experienced Grade 4 hyperglycemia. TRAEs led to the discontinuation of study treatment in 2.3% of patients in the gedatolisib triplet group and 0% in the fulvestrant group. In January 2026, the FDA accepted for filing Celcuity’s NDA for gedatolisib in HR+/HER2- PIK3CA WT ABC. The FDA granted Priority Review and assigned a PDUFA goal date of July 17, 2026. In March 2026, efficacy and safety results from the PIK3CA WT cohort of the Phase 3 VIKTORIA-1 clinical trial of gedatolisib were published in the Journal of Clinical Oncology . The cohort consisted of patients with HR+/HER2-/ PIK3CA WT ABC whose disease progressed while on or after treatment with a CDK4/6 inhibitor and an aromatase inhibitor. As reported previously, the results from the VIKTORIA-1 Phase 3 PIK3CA WT cohort, established several new milestones in the history of drug development for HR+/HER2- ABC: The hazard ratio for the gedatolisib triplet is more favorable than has ever been reported by any Phase 3 trial for patients with HR+/HER2- ABC. The 7.3 months incremental improvements in median PFS for the gedatolisib triplet over fulvestrant is higher than has ever been reported by any Phase 3 trial for patients with HR+/HER2- ABC receiving at least their second line of endocrine therapy-based regimen. Gedatolisib is the first inhibitor targeting the PI3K/AKT/mTOR (“PAM”) pathway to demonstrate positive Phase 3 results in patients with HR+/HER2-/ PIK3CA WT ABC whose disease progressed on or after treatment with a CDK4/6 inhibitor. Median duration of response (“DOR”) of 17.5 months and incremental objective response rate (“ORR”) improvement of 31% relative to control for the gedatolisib triplet is the highest reported for an endocrine therapy-based regimen in second line HR+/HER2- ABC. Fourth Quarter and Full Year 2025 Financial Results Unless otherwise stated, all comparisons are for the fourth quarter and full year ended December 31, 2025, compared to the fourth quarter and full year ended December 31, 2024. Total operating expenses were $49.2 million for the fourth quarter of 2025, compared to $36.4 million for the fourth quarter of 2024. Operating expenses for the full year 2025 were $172.2 million, compared to $113.3 million for the full year 2024. Research and development (“R&D”) expenses were $37.6 million for the fourth quarter of 2025, compared to $33.5 million for the prior-year period. Of the $4.1 million increase in R&D expenses, $8.6 million was related to increased employee and consulting expenses, of which $5.3 million related to commercial headcount additions and other launch-related activities. These amounts were partially offset by a $4.5 million decrease primarily related to costs supporting ongoing activities for the VIKTORIA-1 Phase 3 trial. R&D expenses for the full year 2025 were $145.0 million, compared to $104.2 million for the prior year. Of the $40.8 million increase in R&D expenses, $26.7 million was related to increased employee and consulting expenses, of which $13.1 million related to commercial headcount additions and other launch-related activities. The remaining $14.1 million increase was primarily related to activities supporting our ongoing clinical trials, a development milestone payment under the license agreement with Pfizer, and other commercial launch-related activities. General and administrative (“G&A”) expenses were $11.6 million for the fourth quarter of 2025, compared to $3.0 million for the prior year period. Of the $8.6 million increase, $6.9 million was related to increased employee-related and consulting expenses, of which $5.4 million related to non-cash stock-based compensation. The remaining $1.7 million increase was primarily related to professional fees, expanding infrastructure costs, and other administrative expenses. G&A expenses for the full year 2025 were $27.2 million, compared to $9.1 million for the prior year. Of the $18.1 million increase in G&A expenses, $14.9 million was related to increased employee-related and consulting expenses, of which $10.4 million related to non-cash stock-based compensation. The remaining $3.2 million increase was primarily related to professional fees, expanding infrastructure costs, and other administrative expenses. Net loss for the fourth quarter of 2025 was $51.0 million, or $0.97 per share, compared to a net loss of $36.7 million, or $0.85 per share, for the fourth quarter of 2024. Net loss for the full year 2025 was $177.0 million, or $3.79 per share, compared to a net loss of $111.8 million, or $2.83 per share, in 2024. Non-GAAP adjusted net loss for the fourth quarter of 2025 was $38.4 million, or $0.73 per share, compared to non-GAAP adjusted net loss of $32.3 million, or $0.75 per share, for the fourth quarter of 2024. Non-GAAP adjusted net loss for the full year 2025 was $150.8 million, or $3.22 per share, compared to non-GAAP adjusted net loss of $101.9 million, or $2.58 per share, for 2024. Non-GAAP adjusted net loss excludes stock-based compensation expense, non-cash interest expense, and non-cash interest income. Because these items have no impact on Celcuity’s cash position, management believes non-GAAP adjusted net loss better enables Celcuity to focus on cash used in operations. For a reconciliation of financial measures calculated in accordance with generally accepted accounting principles in the United States (“GAAP”) to non-GAAP financial measures, please see the financial tables at the end of this press release. Net cash used in operating activities for the fourth quarter of 2025 was $36.4 million, compared to $27.8 million for the fourth quarter of 2024. Net cash used in operating activities for the full year 2025 was $153.3 million, compared to $83.5 million for the full year 2024. Cash, cash equivalents and short-term investments were $441.5 million at the end of fiscal year 2025 and are expected to finance our operations through 2027. Webcast and Conference Call Information To participate in the teleconference, domestic callers should dial 1-800-717-1738 and international callers should dial 1-646-307-1865. A live webcast presentation can also be accessed using the weblink below. A replay of the webcast will be available on the Celcuity website following the live event. . About Celcuity Celcuity is a clinical-stage biotechnology company pursuing the development of targeted therapies for the treatment of multiple solid tumor indications. The company's lead therapeutic candidate is gedatolisib, a potent, pan-PI3K and mTORC1/2 inhibitor that comprehensively blockades the PI3K/AKT/mTOR (“PAM”) pathway. Its mechanism of action and pharmacokinetic properties are differentiated from other currently approved and investigational therapies that target PI3Kα, AKT, or mTORC1 alone or together. A Phase 3 clinical trial, VIKTORIA-1, evaluating gedatolisib in combination with fulvestrant, with or without palbociclib, in patients with HR+/HER2- advanced breast cancer (“ABC”), has completed enrollment, and the company has reported detailed results for the PIK3CA wild-type cohort. A Phase 3 clinical trial, VIKTORIA-2, evaluating gedatolisib plus a CDK4/6 inhibitor and fulvestrant as first-line treatment for patients with endocrine treatment resistant HR+/HER2- ABC, is ongoing. A Phase 1/2 clinical trial, CELC-G-201, evaluating gedatolisib in combination with darolutamide in patients with metastatic castration resistant prostate cancer, is ongoing. More detailed information about Celcuity’s active clinical trials can be found at ClinicalTrials.gov . Celcuity is headquartered in Minneapolis. Further information about Celcuity can be found at . Follow us on LinkedIn and X . Forward Looking Statements This press release contains statements that constitute "forward-looking statements" within the meaning of the Private Securities Litigation Reform Act of 1995 including statements relating to the potential therapeutic benefits of gedatolisib; the size, design and timing of our clinical trials; our interpretation of clinical trial data; the status and timing of the FDA’s review of our New Drug Application for gedatolisib, including the PDUFA goal date assigned by the FDA; the market opportunity for gedatolisib; our expectations regarding the timing of and our ability to obtain FDA approval to commercialize gedatolisib; our strategy, marketing and commercialization plans, including the benefits of strategic decisions regarding studies and trials; other expectations with respect to gedatolisib; our anticipated use of cash; and the strength of our balance sheet. Words such as, but not limited to, “look forward to,” “believe,” “expect,” “anticipate,” “estimate,” “intend,” "confidence," "encouraged," “potential,” “plan,” “targets,” “likely,” “may,” “will,” “would,” “should” and “could,” and similar expressions or words identify forward-looking statements. The forward-looking statements included in this press release are based on management's current expectations and beliefs which are subject to a number of risks, uncertainties and factors, including that our clinical results are based on an ongoing analysis of key efficacy and safety data, and such data may change following a more comprehensive review of the data related to the clinical trial; unforeseen delays in our clinical trials or the FDA’s review of our NDA for gedatolisib; our ability to obtain and maintain regulatory approvals to commercialize gedatolisib, and the market acceptance of gedatolisib; the development of therapies and tools competitive with gedatolisib; and our ability to access capital upon favorable terms. In addition, all forward-looking statements are subject to other risks detailed in our Annual Report on Form 10-K for the year ended December 31, 2025, as such risks may be updated in our subsequent filings with the Securities and Exchange Commission. You are cautioned not to place undue reliance on these forward-looking statements, which speak only as of the date hereof. All forward-looking statements are qualified in their entirety by these cautionary statements, and we undertake no obligation to revise or update this press release to reflect events or circumstances after the date hereof. Contacts: Celcuity Inc. Brian Sullivan, bsullivan@celcuity.com Vicky Hahne, vhahne@celcuity.com (763) 392-0123 Jodi Sievers, jsievers@celcuity.com (415) 494-9924 Celcuity Inc. Balance Sheets (in thousands) December 31, 2025 December 31, 2024 Assets Current assets: Cash and cash equivalents $ 165,703 $ 22,515 Investments 275,794 212,589 Other current assets 24,162 9,467 Total current assets 465,659 244,571 Property and equipment, net 499 336 Operating lease right-of-use assets 51 216 Other non-current assets 349 — Total assets $ 466,558 $ 245,123 Liabilities and stockholders' equity Current liabilities: Accounts payable $ 6,407 $ 9,366 Accrued expenses 37,691 22,185 Operating lease liabilities, current 54 172 Total current liabilities 44,152 31,723 Operating lease liabilities, non-current — 54 Convertible debt 195,324 — Note payable, non-current 126,527 97,727 Total liabilities 366,003 129,504 Total stockholders' equity 100,555 115,619 Total liabilities and stockholders' equity $ 466,558 $ 245,123 Celcuity Inc. Statements of Operations (in thousands, except share and per share amounts) Three Months Ended December 31, Year Ended December 31, 2025 2024 2025 2024 (unaudited) Operating expenses: Research and development $ 37,631 $ 33,471 $ 144,995 $ 104,203 General and administrative 11,570 2,959 27,197 9,064 Total operating expenses 49,201 36,430 172,192 113,267 Loss from operations (49,201 ) (36,430 ) (172,192 ) (113,267 ) Other (expense) income: Interest expense (6,166 ) (3,275 ) (17,148 ) (10,280 ) Interest income 4,394 3,052 12,298 11,768 Other (expense) income, net (1,772 ) (223 ) (4,850 ) 1,488 Net loss before income taxes (50,973 ) (36,653 ) (177,042 ) (111,779 ) Income taxes — — — — Net loss $ (50,973 ) $ (36,653 ) $ (177,042 ) $ (111,779 ) Net loss per share, basic and diluted $ (0.97 ) $ (0.85 ) $ (3.79 ) $ (2.83 ) Weighted average common shares outstanding, basic and diluted 52,539,744 42,873,934 46,757,691 39,449,393 Cautionary Statement Regarding Non-GAAP Financial Measures This press release contains references to non-GAAP adjusted net loss and non-GAAP adjusted net loss per share. Management believes these non-GAAP financial measures are useful supplemental measures for planning, monitoring, and evaluating operational performance as they exclude stock-based compensation expense, non-cash interest expense, and non-cash interest income from net loss and net loss per share. Management excludes these items because they do not impact Celcuity’s cash position, which management believes better enables Celcuity to focus on cash used in operations. However, non-GAAP adjusted net loss and non-GAAP adjusted net loss per share are not recognized measures under GAAP and do not have a standardized meaning prescribed by GAAP. As a result, management’s method of calculating non-GAAP adjusted net loss and non-GAAP adjusted net loss per share may differ materially from the method used by other companies. Therefore, non-GAAP adjusted net loss and non-GAAP adjusted net loss per share may not be comparable to similarly titled measures presented by other companies. Investors are cautioned that non-GAAP adjusted net loss and non-GAAP adjusted net loss per share should not be construed as alternatives to net loss, net loss per share or other statements of operations data (which are determined in accordance with GAAP) as an indicator of Celcuity’s performance or as a measure of liquidity and cash flows. Celcuity Inc. Reconciliation of GAAP Net Loss to Non-GAAP Adjusted Net Loss and GAAP Net Loss Per Share to Non-GAAP Adjusted Net Loss Per Share (in thousands, except share and per share amounts) Three Months Ended December 31, Year Ended December 31, 2025 2024 2025 2024 GAAP net loss $ (50,973 ) $ (36,653 ) $ (177,042 ) $ (111,779 ) Adjustments to net loss: Stock-based compensation Research and development (1) 3,124 1,404 8,409 4,405 General and administrative (2) 6,332 911 12,974 2,583 Non-cash interest expense (3) 1,602 803 4,241 2,695 Non-cash interest income (4) 1,470 1,263 630 150 Non-GAAP adjusted net loss $ (38,445 ) $ (32,272 ) $ (150,788 ) $ (101,946 ) GAAP net loss per share - basic and diluted $ (0.97 ) $ (0.85 ) $ (3.79 ) $ (2.83 ) Adjustments to net loss: Stock-based compensation Research and development 0.06 0.03 0.18 0.11 General and administrative 0.12 0.02 0.29 0.07 Non-cash interest expense 0.03 0.02 0.09 0.07 Non-cash interest income 0.03 0.03 0.01 — Non-GAAP adjusted net loss per share - basic and diluted $ (0.73 ) $ (0.75 ) $ (3.22 ) $ (2.58 ) Weighted average common shares outstanding, basic and diluted 52,539,744 42,873,934 46,757,691 39,449,393 (1) To reflect a non-cash charge to operating expenses for research and development stock-based compensation. (2) To reflect a non-cash charge to operating expenses for general and administrative stock-based compensation. (3) To reflect a non-cash charge to other expense for amortization of debt issuance costs and discount and payment-in-kind interest related to the issuance of a note payable. (4) To reflect a non-cash adjustment to other income for accretion on investments and change in accrued interest income.

Phase 3NDAFinancial StatementClinical ResultPriority Review

25 Mar 2026

·allsci.com

Pfizer’s CDK4 atirmociclib cuts progression risk by 40% in second-line metastatic breast cancer trial

Pfizer (NYSE: PFE) reported Phase II results for atirmociclib in HR-positive, HER2-negative metastatic breast cancer, with the FOURLIGHT-1 trial meeting its primary endpoint by demonstrating a 40% reduction in the risk of disease progression or death compared to standard-of-care options. The data mark the first randomized Phase II readout for a selective CDK4 inhibitor in patients whose disease has progressed on prior CDK4/6 inhibitor therapy, a population with limited treatment options and no established targeted retreatment strategy. Trial specifics FOURLIGHT-1 is an open-label, randomized, multicenter Phase II study that enrolled 264 patients across 14 countries with HR-positive, HER2-negative advanced or metastatic breast cancer who had progressed after CDK4/6 inhibitor-based treatment. Patients were randomized to atirmociclib plus fulvestrant versus physician’s choice of fulvestrant alone or everolimus plus exemestane. The primary endpoint was investigator-assessed progression-free survival. Atirmociclib plus fulvestrant reduced the risk of progression or death by 40% versus control, with a hazard ratio of 0.60 (95% CI: 0.440–0.825; p=0.0007). The benefit was consistent across prespecified subgroups, including patients with visceral disease, those with prior CDK4/6 inhibitor treatment lasting less than or more than 12 months, and regardless of which CDK4/6 inhibitor was previously received. More than 90% of enrolled patients initiated atirmociclib within three months of their last CDK4/6 inhibitor treatment, indicating a population with recent disease progression rather than a prolonged treatment-free interval. Overall survival data were not mature, with approximately 20% of participants having had an event at the time of analysis. The safety profile was consistent with prior studies of atirmociclib. Discontinuation due to treatment-emergent adverse events occurred in 6.4% of patients on the atirmociclib arm, and no new safety signals were identified, according to the company. Detailed safety data were not disclosed and are expected at a future medical meeting. Development context Atirmociclib is an oral, selective inhibitor of cyclin-dependent kinase 4 (CDK4), a protein that drives the transition from G1 to S phase of the cell cycle. Unlike currently approved CDK4/6 inhibitors such as palbociclib, ribociclib, and abemaciclib, which inhibit both CDK4 and CDK6, atirmociclib targets CDK4 alone. The rationale for selective CDK4 inhibition centers on the hypothesis that sparing CDK6 may reduce hematologic toxicity, particularly neutropenia, which is the dose-limiting side effect of dual CDK4/6 inhibitors. Whether CDK4 selectivity translates into a clinically distinct efficacy or tolerability profile remains to be established in larger trials. The post-CDK4/6 inhibitor treatment landscape in HR-positive, HER2-negative metastatic breast cancer lacks a consensus targeted retreatment approach. Current options after progression on a CDK4/6 inhibitor include fulvestrant monotherapy, everolimus combined with exemestane, and more recently, agents such as elacestrant, an oral selective estrogen receptor degrader approved by the US FDA in 2023 for patients with ESR1-mutated tumors. The PI3K inhibitor alpelisib combined with fulvestrant is approved for PIK3CA-mutated disease. Capivasertib, an AKT inhibitor, received US FDA approval in 2023 in combination with fulvestrant for patients with PIK3CA/AKT1/PTEN-altered tumors. None of these therapies directly address the question of whether continued cell cycle inhibition through a next-generation mechanism can extend disease control after CDK4/6 inhibitor failure. Pfizer stated that a Phase III registrational study for atirmociclib in the first-line metastatic setting is ongoing, and results from a Phase II neoadjuvant study in early breast cancer will be presented at a future medical meeting. The company did not disclose a timeline for regulatory filing based on the FOURLIGHT-1 data or whether the Phase II results alone would support an accelerated approval pathway. The broader competitive context for next-generation CDK4 inhibitors includes programs from other companies, though atirmociclib is the first to report randomized Phase II data in the post-CDK4/6 inhibitor setting. Pfizer’s decision to advance atirmociclib into first-line and early-stage disease reflects a strategy to position the molecule as a potential replacement for, rather than a successor to, existing CDK4/6 inhibitors across treatment lines. Leave a Reply Cancel reply Your email address will not be published. Required fields are marked * Comment * Name * Email * Website

Phase 2Clinical ResultDrug ApprovalPhase 3Accelerated Approval

20 Mar 2026

·allsci.com

Novartis to acquire Synnovation’s PI3Kα inhibitor program for up to USD 3b.

Novartis is moving to acquire Pikavation Therapeutics, a wholly-owned subsidiary of Synnovation Therapeutics, to gain control of SNV4818 and related PI3Kα inhibitor programs. The deal covers a pan-mutant selective PI3K alpha small molecule inhibitor currently in Phase I/II trials for HR+/HER2- metastatic breast cancer and other solid tumors. Synnovation is a clinical-stage company headquartered in Wilmington, Delaware, focused on small-molecule targeted therapies in oncology and immunology. Under the agreement, Novartis will pay Synnovation USD 2 billion in upfront cash and up to USD 1 billion in development, regulatory, and commercial milestone payments, for total potential consideration of up to USD 3 billion. Deal closure is expected in H1 2026, subject to antitrust review. Novartis will assume sole responsibility for all future development and commercialization of the acquired programs. SNV4818 is a small molecule designed to selectively inhibit multiple oncogenic mutations of PI3Kα while sparing the wild-type enzyme. PIK3CA mutations encoding PI3Kα are among the most common oncogenic alterations in HR+/HER2- breast cancer and occur across other solid tumor types. First-generation PI3Kα inhibitors, including Novartis’s own alpelisib (trade name: Piqray), inhibit both mutant and wild-type forms of the enzyme. This lack of mutant selectivity drives on-target toxicities including hyperglycemia, rash, and diarrhea. Pan-mutant selective inhibitors aim to widen the therapeutic window by concentrating activity on the disease-driving mutant protein. A Phase I/II trial evaluating SNV4818 as monotherapy and in combination with fulvestrant or palbociclib in patients with advanced PIK3CA-mutant solid tumors is ongoing, with enrollment of 320 participants across sites in Canada and Australia (see NCT06736704). No clinical data from this trial have been publicly reported. For Novartis, this deal represents an effort to defend and extend its position in the PI3Kα pathway. Alpelisib generated the company’s initial franchise in PIK3CA-mutant breast cancer but faces displacement by agents with improved tolerability profiles. Acquiring SNV4818 allows Novartis to develop a next-generation successor using its existing breast cancer commercial infrastructure. Synnovation retains its remaining pipeline, including SNV1521, a PARP1-selective inhibitor in Phase I, along with additional oncology and immunology programs. The PI3Kα inhibitor landscape has become competitive. Several companies are developing next-generation mutant-selective agents targeting the same biology. Tersolisib (STX-478) — Eli Lilly (acquired from Scorpion Therapeutics) — Phase III pivotal trial; allosteric, pan-mutant selective, CNS-penetrant Zovegalisib (RLY-2608) — Relay Therapeutics — Phase III; allosteric, pan-mutant and isoform-selective OKI-219 — OnKure Therapeutics — Phase I; mutation-specific (H1047R only) LY4045004 — Eli Lilly (internal) — preclinical/early clinical; pan-mutant selective Inavolisib (Itovebi) — Roche/Genentech — approved 2024; PI3Kα-selective but not mutant-selective Lilly’s tersolisib is the most advanced next-generation program and has already entered a front-line pivotal study. Relay’s zovegalisib showed consistent efficacy and tolerability in updated data presented at ASCO 2025. Lilly’s earlier mutation-specific candidate LOXO-783 was discontinued after showing limited monotherapy activity in Phase 1, which has shifted competitive consensus toward pan-mutant approaches. SNV4818 enters this field behind at least two competitors with more advanced clinical data, though Novartis’s existing commercial presence in PI3Kα-mutant breast cancer and its global development capabilities could accelerate the program’s path through later-stage trials. Your email address will not be published. Required fields are marked * Comment * Name * Email * Website

Phase 1Phase 3AcquisitionDrug ApprovalPhase 2

100 Deals associated with Palbociclib

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KEGG	Wiki	ATC	Drug Bank
D10372	Palbociclib	L01XE33	DB09073

R&D Status

Approved

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Indication	Country/Location	Organization	Date
Breast cancer recurrent	Japan	Pfizer Japan, Inc.	27 Sep 2017
Hormone receptor positive HER2 negative breast cancer	United States	Pfizer Inc.	19 Feb 2016
ER-positive/HER2-negative Breast Cancer	United States	Pfizer Inc.	03 Feb 2015

Developing

10 top R&D records.

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Indication	Highest Phase	Country/Location	Organization	Date
Human Papillomavirus-Related Squamous Cell Carcinoma	Phase 3	United States	Pfizer Inc.	06 Apr 2022
Squamous Cell Carcinoma of Head and Neck	Phase 3	United States	Pfizer Inc.	06 Apr 2022
Squamous cell carcinoma of head and neck metastatic	Phase 3	United States	Pfizer Inc.	06 Apr 2022
HR Positive/HER2 Negative/Node positive breast cancer	Phase 3	Austria	Pfizer Inc.	27 Aug 2019
HR Positive/HER2 Negative/Node positive breast cancer	Phase 3	France	Pfizer Inc.	27 Aug 2019
HR Positive/HER2 Negative/Node positive breast cancer	Phase 3	Hungary	Pfizer Inc.	27 Aug 2019
HR Positive/HER2 Negative/Node positive breast cancer	Phase 3	Italy	Pfizer Inc.	27 Aug 2019
HR Positive/HER2 Negative/Node positive breast cancer	Phase 3	Spain	Pfizer Inc.	27 Aug 2019
HR Positive/HER2 Negative/Node positive breast cancer	Phase 3	Switzerland	Pfizer Inc.	27 Aug 2019
HER2-negative breast cancer	Phase 3	Japan	Pfizer Inc.	16 Jul 2019

Clinical Result

Indication

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Evaluation

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Study	Phase	Population	Analyzed Enrollment	Group	Results	Evaluation	Publication Date


AACR2026	Phase 2/3	Hormone receptor positive HER2 negative breast cancer HR Positive \| HER2 Negative	16	Imlunestrant alone	wjdgdrepab(mitkvftgrt) = widwpxnsyr ctrgvxpmuu (eoaxexbxok ) View more	Positive	21 Apr 2026
				Camizestrant 75mg	wjdgdrepab(bhyuhgkpzr) = aphcitglat skjxzritkx (asvbmauliy ) View more
ESGO2026	Phase 1/2	Ovarian Serous Adenocarcinoma	70	Ribociclib + letrozole	szuaqirxhg(llimyzetjo) = fohegbhprc xnfoalorff (rvydubrmfl ) View more	Positive	28 Feb 2026
				Ribociclib + letrozole	szuaqirxhg(llimyzetjo) = vaxhhurzio xnfoalorff (rvydubrmfl )
NCT05468697 (LITESPARK-024, ASCO_GU2026)	Phase 1/2	Locally Advanced Clear Cell Renal Cell Carcinoma	59	Belzutifan 120 mg QD + Palbociclib 75 mg QD	uzykvgziom(snkbgnajkd) = vnivsqqkyo jvbeyumvvi (bkjvtfhczn ) View more	Positive	26 Feb 2026
				Belzutifan 120 mg QD + Palbociclib 100 mg QD	uzykvgziom(snkbgnajkd) = sodwerupya jvbeyumvvi (bkjvtfhczn ) View more
NCT02778685 (OT2-01-06, CTgov)	Phase 2	Metastatic breast cancer \| Metastatic human epidermal growth factor 2 positive carcinoma of breast \| Estrogen receptor positive breast cancer	47	Laboratory Biomarker Analysis+fulvestrant+Letrozole+palbociclib+Pembrolizumab	ebnweoahje = ucyyuzrbqv bglruvulup (uohaflxoul, reyrwugkff - xxtccwkshm) View more	-	24 Feb 2026
NCT02947685 (PATINA \| AFT-38, CTgov)	Phase 3	Metastatic human epidermal growth factor 2 positive carcinoma of breast \| Estrogen receptor positive breast cancer	518	fulvestrant+Letrozole+palbociclib+pertuzumab+Exemestane+trastuzumab+anastrozole (Arm A)	rqmzhjmxmn(aavofiymfj) = cdirxzvhho lkfzewjlmv (enrzhrvwaq, pfrcpvujsw - rtwgvzyysh) View more	-	12 Feb 2026
				fulvestrant+Letrozole+pertuzumab+Exemestane+anastrozole (Arm B)	rqmzhjmxmn(aavofiymfj) = gwtgkpuupc lkfzewjlmv (enrzhrvwaq, makmfqnvyu - vptxarzmmt) View more
NCT02947685 (PATINA, Pubmed \| N Engl J Med)	Phase 3	Hormone receptor positive HER2 positive breast cancer Maintenance hormone-receptor-positive \| HER2-positive	518	Palbociclib + maintenance HER2-targeted and endocrine therapies	ewzbhoyxst(qalezvoenb) = joohvobukw ryuvvbzahh (yugcdzzsyq ) View more	Positive	29 Jan 2026
				maintenance HER2-targeted and endocrine therapies	ewzbhoyxst(qalezvoenb) = qdefmkhvke ryuvvbzahh (yugcdzzsyq ) View more
NCT02513394 (PALLAS, SABCS2025)	Phase 3	Hormone receptor positive HER2 negative breast cancer Adjuvant HR+ \| HER2-	5,736	Palbociclib + Endocrine Therapy	fgpjeablky(depjkjuehm) = moincalhrb wuakpaqlej (yigoqqdbzt ) View more	Negative	11 Dec 2025
SABCS2025	Not Applicable	Hormone receptor positive HER2 negative breast cancer First line HR+/HER2-	2,267	Palbociclib + Endocrine Therapy	engcmmkvqc(lnuenyptuz) = wyksfshnmx pbbbblfcxg (watlyhwrok, 47.4 - 52.3) View more	Positive	10 Dec 2025
				Palbociclib + Endocrine Therapy (Age <65)	engcmmkvqc(lnuenyptuz) = oxnvzehewh pbbbblfcxg (watlyhwrok, 49.3 - 56.5) View more
SABCS2025	Not Applicable	Hormone receptor positive HER2 negative breast cancer First line HR+/HER2–	8,076	Palbociclib plus an aromatase inhibitor (AI)	icpjozcqnb(hrhjyrpggq) = kwgpmbbwow nqgxpkmjgz (wdxaxkznko, 48.7 - 53.1) View more	Positive	10 Dec 2025
				an aromatase inhibitor (AI)	icpjozcqnb(hrhjyrpggq) = lcfdxomjzy nqgxpkmjgz (wdxaxkznko, 39.8 - 44.7) View more
SABCS2025	Not Applicable	Hormone receptor positive HER2 negative breast cancer First line HR+ \| HER2-	323	Palbociclib + Endocrine Therapy	tfhshwqdxg(fjspzxikxv) = qhgsjrbslu socxyyxyts (gsbascviyx ) View more	Positive	10 Dec 2025

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