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Last update 29 Apr 2026

Palbociclib

Last update 29 Apr 2026

Overview

R&D Status

Clinical Result

Translational Medicine

Overview

Basic Info

Drug Type

Small molecule drug

Synonyms

Iburance, Palbociclib (JAN/USAN), Palbociclib Isethionate

+ [16]

Target

CDK4 x CDK6

Action

inhibitors

Mechanism

CDK4 inhibitors(Cyclin-dependent kinase 4 inhibitors), CDK6 inhibitors(Cyclin-dependent kinase 6 inhibitors)

Therapeutic Areas

NeoplasmsSkin and Musculoskeletal DiseasesImmune System Diseases+ [8]

Active Indication

Breast cancer recurrentHormone receptor positive HER2 negative breast cancerER-positive/HER2-negative Breast Cancer+ [102]

Inactive Indication

acute leukemiaAcute myeloid leukaemia with 11q23 abnormalityAdvanced Hepatocellular Carcinoma+ [58]

Originator Organization

Pfizer Inc.

Active Organization

Pfizer Inc.

National Cancer Institute

AstraZeneca PLC

+ [18]

Inactive Organization

Xynomic Pharmaceuticals, Inc.Hoffmann-La Roche, Inc.

SWOG

+ [8]

License Organization

Dr. Reddy's Laboratories Ltd.

Amgen, Inc.

Ascentage Pharma Group International Co., Ltd.

+ [11]

Drug Highest PhaseApproved

First Approval Date

United States (03 Feb 2015),

ER-positive/HER2-negative Breast Cancer

RegulationBreakthrough Therapy (United States), Accelerated Approval (United States), Priority Review (China), Special Review Project (China)

Structure/Sequence

Molecular FormulaC24H29N7O2

InChIKeyAHJRHEGDXFFMBM-UHFFFAOYSA-N

CAS Registry571190-30-2

433

Clinical Trials associated with Palbociclib

NCT07405164

/ RecruitingPhase 3

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

3,313

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.

522

News (Medical) associated with Palbociclib

27 Apr 2026

·www.biospace.com

Relay Therapeutics Announces Clinical Data for Zovegalisib plus Atirmociclib Triplet Combination Supportive of Further Development in Frontline Metastatic Breast Cancer

Zovegalisib + atirmociclib + AI selected as triplet regimen for frontline development Compelling efficacy and tolerability data for zovegalisib triplet in median 3L patients 44% ORR in heavily pre-treated, CDK4/6-experienced patients (median third-line); ORR is similar across kinase and non-kinase PIK3CA mutations Phase 3 frontline trial in endocrine sensitive patients expected to initiate in early 2027, subject to regulatory feedback Supply agreement in place with Pfizer to supply atirmociclib for the Phase 3 frontline trial Relay Therapeutics to host a conference call today, April 27, at 8:30am ET CAMBRIDGE, Mass., April 27, 2026 (GLOBE NEWSWIRE) -- Relay Therapeutics, Inc. (Nasdaq: RLAY), a clinical-stage, small molecule precision medicine company developing potentially life-changing therapies for patients living with cancer and genetic disease, today announced plans to move zovegalisib + atirmociclib, Pfizer’s investigational, potential first-in-class CDK4 inhibitor, into Phase 3 development for frontline patients with PI3Kα-mutated, HR+/HER2- metastatic breast cancer. “While PI3Kα inhibition has demonstrated meaningful benefit in breast cancer, its use in the frontline setting has been limited by tolerability challenges with earlier agents,” said Don Bergstrom, M.D., Ph.D., President of R&D at Relay Therapeutics. “We believe that combining the selective profiles of zovegalisib and atirmociclib with endocrine therapy has the potential to enable a well-tolerated, all-oral triplet regimen, and these initial data support advancing this combination into Phase 3 development for patients with frontline metastatic breast cancer.” Zovegalisib + Atirmociclib Data Demonstrate Potential Best-in-Class Triplet Profile Zovegalisib is currently being evaluated in ReDiscover, an ongoing first-in-human study designed to evaluate the safety, tolerability, pharmacokinetics, pharmacodynamics and preliminary antitumor activity of zovegalisib in combination with fulvestrant and CDK inhibitors in patients with PI3Kα-mutated, HR+/HER2- metastatic breast cancer. These data are from the zovegalisib + atirmociclib + fulvestrant dose finding portion of the study. As of the April 13, 2026 data cut-off date, 69 total patients were enrolled, with 62 patients at or below the potential Phase 3 dose and 34 patients with measurable disease evaluable for response. All patients had previously received a CDK4/6 inhibitor and at least one prior endocrine therapy in the advanced setting and could have received a PI3K pathway inhibitor. These heavily pre-treated patients had received a median of 2 prior therapies (21% received 3+ prior therapies) in the metastatic setting with 63% having visceral disease, 29% having received chemotherapy, and 47% being pre-diabetic. The median follow-up was 7.4 months. Expansion cohorts of zovegalisib + atirmociclib + fulvestrant and zovegalisib + atirmociclib + aromatase inhibitor (AI) in the ReDiscover study are ongoing. Safety and Tolerability of Triplet is Critical for Potential Long-Term Treatment in Frontline Endocrine Sensitive Breast Cancer Early safety and tolerability data for zovegalisib in combination with atirmociclib and fulvestrant (N=62) reinforce the potential of this regimen moving forward in frontline endocrine sensitive patients. As of the April 13, 2026 data cut-off date: Only two patients (3%) discontinued zovegalisib and six patients (10%) dose reduced zovegalisib due to treatment-related adverse events (TRAEs) Adverse events were consistent with those previously reported by each molecule Grade 3 hyperglycemia was 0% despite 47% of patients being pre-diabetic Overall grade 3+ TRAE rate in these median third-line patients is 40% Neutropenia accounts for the majority of the grade 3+ events No instance of febrile neutropenia was observed Overall Response Rate in Median Third Line Patients is Approaching ORR Seen in Frontline Breast Cancer with Standard of Care As of the April 13, 2026 data cut-off date, 34 patients had measurable disease to be evaluated for response: Objective response rate (ORR) was 44% (15/34) and was also 44% in both kinase and non-kinase patients ORR in these heavily pre-treated patients has approached that of current standard of care doublets in 1L patients, ranging from 53% to 55% ORR Nearly all patients experienced tumor reduction (85%, 29/34) 48 of 62 patients (77%) remain on study as of the data cut-off date, with a median follow-up of 7.4 months The data are not yet mature enough to estimate median progression-free survival Pharmacokinetics Pharmacokinetic analyses demonstrated that atirmociclib increased the exposure of zovegalisib by about two and half-fold (regardless of atirmociclib dose), while zovegalisib had no impact on atirmociclib exposure. Subject to regulatory feedback, the potential Phase 3 dose of zovegalisib will be 150mg twice daily (BID), which maintains average concentration of zovegalisib just below IC90 throughout the dosing interval. Preliminary Phase 3 Trial Design in Frontline Endocrine Sensitive Patients The planned study, subject to regulatory feedback, is a randomized Phase 3 trial evaluating zovegalisib in combination with atirmociclib and aromatase inhibitor (AI) in frontline endocrine sensitive patients with PIK3CA-mutated, HR+/HER2- advanced or metastatic breast cancer. Population: Frontline endocrine sensitive patients with HR-positive, HER2-negative advanced or metastatic breast cancer harboring a PIK3CA mutation Experimental arm: Zovegalisib + atirmociclib + AI Control arm: CDK4/6 inhibitor (investigator’s choice) + AI Key endpoints: Median progression-free survival (primary) and overall survival (secondary) Pfizer to Supply Atirmociclib and Palbociclib Through Supply Agreement Pfizer has agreed to supply atirmociclib for the experimental arm in combination with zovegalisib and the palbociclib portion of the control arm for use in the planned study. Relay Tx will sponsor, fully operationalize and fund the planned Phase 3 trial. Relay Tx retains full global rights for zovegalisib. Next Steps Conduct regulatory interactions to finalize Phase 3 design and dose with the goal of initiating the study in early 2027 Continued execution of Phase 1/2 dose finding and expansion as part of the ReDiscover study, allowing for larger sample size and longer follow up at potential Phase 3 dose for future disclosures Continued execution of ongoing ReDiscover-2 Phase 3 trial in second line breast cancer Present initial data for zovegalisib in vascular anomalies at ISSVA 2026 (May 20, 2026 in Philadelphia) Conference Call Information Relay Therapeutics will host a conference call and live webcast today, April 27, at 8:30 a.m. ET. Registration and dial-in for the conference call may be accessed through Relay Therapeutics’ website under Events in the News & Events section through the following link: . An archived replay of the webcast will be available following the event. About Zovegalisib Zovegalisib is the lead program in Relay Therapeutics’ efforts to discover and develop mutant selective inhibitors of PI3Kα, the most frequently mutated kinase in all cancers and all vascular anomalies. Zovegalisib has the potential, if approved, to address a significant portion of the approximately 140,000 patients with HR+/HER2- breast cancer with a PI3Kα mutation and the estimated 170,000 patients with vascular anomalies driven by a PI3Kα mutation per year in the United States, one of the largest patient populations for a precision medicine. Traditionally, the development of PI3Kα inhibitors has focused on the active, or orthosteric, site. The therapeutic index of orthosteric inhibitors is limited by the lack of clinically meaningful selectivity for mutant versus wild-type (WT) PI3Kα and off-isoform activity. Toxicity related to inhibition of WT PI3Kα and other PI3K isoforms results in sub-optimal inhibition of mutant PI3Kα with reductions in dose intensity and frequent discontinuation. The Dynamo® platform enabled the discovery of zovegalisib, the first known allosteric, pan-mutant, and isoform-selective PI3Kα inhibitor, designed to overcome these limitations. Relay Therapeutics solved the full-length cryo-EM structure of PI3Kα, performed computational long time-scale molecular dynamic simulations to elucidate conformational differences between WT and mutant PI3Kα, and leveraged these insights to support the design of zovegalisib. Zovegalisib is currently being evaluated in multiple metastatic breast cancer studies and a first-in-human study designed to treat patients with PIK3CA (PI3Kα) mutation driven vascular anomalies. For more information on zovegalisib, please visit here . About Relay Therapeutics Relay Therapeutics (Nasdaq: RLAY) is a clinical-stage, small molecule precision medicine company developing potentially life-changing therapies for patients living with cancer and genetic disease. Relay Therapeutics’ Dynamo® platform integrates an array of leading-edge computational and experimental approaches designed to drug protein targets that have previously been intractable or inadequately addressed. The company’s lead clinical asset, zovegalisib, is the first pan-mutant selective PI3Kα inhibitor to enter clinical development and is currently in a Phase 3 clinical trial (ReDiscover-2) in HR+/HER2- metastatic breast cancer. Zovegalisib is also being investigated in a group of genetic disease indications called PI3Kα-driven vascular anomalies. Relay Therapeutics’ pipeline also includes programs for NRAS-driven solid tumors and Fabry disease. For more information, please visit or follow us on LinkedIn . 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, as amended, including, without limitation, implied and express statements regarding Relay Therapeutics’ strategy, business plans and focus; the progress and timing of the clinical development of the programs across Relay Therapeutics’ portfolio, including the timing of initiation of a frontline Phase 3 clinical trial for zovegalisib in combination with atirmociclib and AI; the timing of clinical data readouts for zovegalisib; the expected therapeutic benefits and potential efficacy and tolerability of zovegalisib, both as a monotherapy and in combination with other agents, including the combination of zovegalisib and atirmociclib, and its other programs; the clinical data for zovegalisib; the interactions with regulatory authorities and any related approvals; the potential commercialization and market opportunity for zovegalisib; and the expected strategic benefits under Relay Therapeutics' clinical trial supply agreement with Pfizer. The words “may,” “might,” “will,” “could,” “would,” “should,” “plan,” “anticipate,” “intend,” “believe,” “expect,” “estimate,” “seek,” “predict,” “future,” “project,” “potential,” “continue,” “target” and similar words or expressions, or the negative thereof, are intended to identify forward-looking statements, although not all forward-looking statements contain these identifying words. Any forward-looking statements in this press release are based on management's current expectations and beliefs and are subject to a number of risks, uncertainties and important factors that may cause actual events or results to differ materially from those expressed or implied by any forward-looking statements contained in this press release, including, without limitation, risks associated with: the impact of global economic uncertainty, geopolitical instability and conflicts, or public health epidemics or outbreaks of an infectious disease on countries or regions in which Relay Therapeutics has operations or does business, as well as on the timing and anticipated results of its clinical trials, strategy, future operations and profitability; significant political, trade or regulatory developments, such as tariffs, beyond Relay Therapeutics’ control; the delay or pause of any current or planned clinical trials or the development of Relay Therapeutics’ drug candidates; the risk that the preliminary or interim results of its preclinical or clinical trials may not be predictive of future or final results in connection with future clinical trials of its product candidates and that interim and early clinical data may change as more patient data become available and are subject to audit and verification procedures; Relay Therapeutics’ ability to successfully demonstrate the safety and efficacy of its drug candidates; the timing and outcome of its planned interactions with regulatory authorities; and obtaining, maintaining and protecting its intellectual property. These and other risks and uncertainties are described in greater detail in the section entitled “Risk Factors” in Relay Therapeutics’ most recent Annual Report on Form 10-K and Quarterly Report on Form 10-Q, as well as any subsequent filings with the Securities and Exchange Commission. In addition, any forward-looking statements represent Relay Therapeutics' views only as of today and should not be relied upon as representing its views as of any subsequent date. Relay Therapeutics explicitly disclaims any obligation to update any forward-looking statements. No representations or warranties (expressed or implied) are made about the accuracy of any such forward-looking statements. Contact: Pete Rahmer prahmer@relaytx.com Media: Dan Budwick 1AB 973-271-6085 dan@1abmedia.com

Phase 3Clinical ResultPhase 2

23 Apr 2026

·www.prnewswire.com

AACR 2026 | Abbisko Therapeutics Showcases Six Research Advances Highlighting pan-KRAS, 4th Generation EGFR, and Synthetic Lethality Approaches

SAN DIEGO, April 22, 2026 /PRNewswire/ -- Abbisko Therapeutics (HKEX: 02256) announced that the company presented six latest preclinical and translational research findings in poster sessions at the American Association for Cancer Research (AACR) Annual Meeting, held from April 17 to 22, 2026, in San Diego, USA. The presentations span multiple key innovation areas, including the pan-KRAS inhibitor ABSK211, the 4 th generation EGFR inhibitor ABK-EGFR-1, the CDK4 selective inhibitor ABK-CDK4, the MTA-cooperative PRMT5 inhibitor ABSK131, as well as a ctDNA-based study investigating resistance mechanisms to the FGFR2/3 inhibitor ABSK061. pan-KRAS Inhibitor ABSK211 ABSK211 is a potent, highly selective, and orally bioavailable small-molecule pan-KRAS inhibitor developed by Abbisko Therapeutics. It demonstrates broad inhibitory activity against multiple KRAS mutations, addressing significant unmet medical needs in KRAS-driven cancers. At AACR 2026, Abbisko presented preclinical data for both monotherapy and combination strategies of ABSK211. Monotherapy: Broad and Potent Inhibition Across KRAS Mutations KRAS mutations are highly prevalent across multiple cancers, including pancreatic (~90%), colorectal (~35%), and lung cancer (~25%). While several pan-KRAS inhibitors have entered clinical development, there remains a critical need for enhanced potency. In preclinical studies, ABSK211 demonstrated: Robust in vitro activity: ABSK211 significantly reduced cell viability across multiple KRAS alterations (including G12, G13, Q61, and WT amplification) at sub-nanomolar to nanomolar concentrations. Meanwhile ABSK211 displayed marginal inhibition in KRAS wild-type cell line with normal copy. Strong in vivo efficacy: Oral administration induced deep tumor regression in multiple KRAS G12V xenograft models, with robust target engagement. Broad mutation coverage: Consistent and significant antitumor activity was observed in models harboring KRAS G12D/C/S and G13D mutations. These findings support the clinical advancement of ABSK211, which is currently undergoing IND-enabling studies. Poster Information Title: Preclinical characterization of ABSK211: A highly potent, orally bioavailable and selective pan-KRAS inhibitor with broad and robust activity in KRAS-driven tumors Time: April 22, 2026, 9:00 AM – 12:00 PM (PT) Location: Poster Section 13, Board #10 Abstract #: 7090 Combination Therapy: Multi-Mechanistic Synergy Enhances Antitumor Activity Combination therapy is widely considered a key strategy to improve treatment outcomes in KRAS-mutant cancers. ABSK211 demonstrated synergistic antitumor activity with multiple therapeutic agents: In vitro synergy: Significant anti-proliferative synergy with PRMT5 inhibitors across KRAS mutations; strong synergy observed with EGFR monoclonal antibodies and chemotherapy in KRAS G12D/G12V models. Enhanced in vivo efficacy: Combination regimens with PRMT5 inhibitors, cetuximab, immunotherapies, and chemotherapy showed superior tumor growth inhibition and improved durability compared to monotherapy. These results demonstrate that ABSK211 can significantly enhance antitumor efficacy through multi-mechanistic synergy, supporting its further development in combination strategies. Poster Information Title: ABSK211, a highly potent and orally available pan-KRAS inhibitor, demonstrates robust antitumor efficacy in combination with multiple agents Time: April 22, 2026, 9:00 AM – 12:00 PM (PT) Location: Poster Section 13, Board #3 Abstract #: 7083 4 th Generation EGFR Inhibitor ABK-EGFR-1 ABK-EGFR-1 is a novel 4th generation EGFR inhibitor developed by Abbisko Therapeutics, specifically designed to target the EGFR C797S resistance mutation. It combines high selectivity with central nervous system (CNS) penetration to address key clinical challenges following resistance to 3rd generation EGFR TKIs. Targeting C797S-Mediated Resistance The EGFR C797S mutation is a clinically validated mechanism of resistance to third-generation EGFR TKIs, with an estimated 51,000–146,000 cases annually worldwide. Currently, no approved therapies specifically target this mutation, representing a significant unmet clinical need. Preclinical studies showed that ABK-EGFR-1: Exhibits high selectivity over wild-type EGFR and other kinases. Demonstrates significant in vivo antitumor activity in multiple EGFR C797S-driven xenograft models, effectively inhibiting tumor growth. Possesses excellent blood-brain barrier penetration and favorable drug-like properties. These findings support further development of ABK-EGFR-1 as a next-generation targeted therapy for EGFR-resistant cancers, particularly for patients with brain metastases. Poster Information Title: Discovery and characterization of ABK-EGFR-1, a 4th generation EGFR C797S Inhibitor with excellent selectivity and brain penetration Time: April 21, 2026, 2:00 PM – 5:00 PM (PT) Location: Poster Section 53, Board #7 Abstract #: LB350 CDK4 Selective Inhibitor ABK-CDK4 ABK-CDK4 is a highly selective, brain-penetrant small-molecule CDK4 inhibitor developed by Abbisko Therapeutics. It is designed to selectively target CDK4, reduce CDK6-related toxicity, and expand treatment potential for patients with brain metastases. Differentiation Through Selectivity and CNS Penetration 1st generation CDK4/6 inhibitors (e.g., palbociclib, ribociclib, and abemaciclib) have demonstrated clinical benefit in breast cancer, but CDK6 inhibition is associated with dose-limiting hematologic toxicities. In addition, 20–40% of breast cancer patients develop brain metastases, while current therapies have limited CNS exposure. Preclinical studies showed that ABK-CDK4: High selectivity: Over 50-fold selectivity for CDK4 versus CDK6, potentially reducing CDK6-related toxicity. CNS penetration: Favorable CNS exposure (Kpuu > 0.5) and drug-like properties. Antitumor activity: Effective inhibition of Rb phosphorylation and tumor growth in HR+/HER2− breast cancer models These results suggest that ABK-CDK4 may overcome key limitations of current CDK4/6 inhibitors and provide a differentiated therapeutic option. Poster Information Title: Discovery of ABK-CDK4, a selective and brain-penetrant CDK4 inhibitor Time: April 20, 2026, 9:00 AM - 12:00 PM (PT) Location: Poster Section 20, Board #13 Abstract #: 1905 MTA-cooperative PRMT5 inhibitor ABSK131 ABSK131 is a potent and selective small-molecule MTA-cooperative PRMT5 inhibitor developed by Abbisko Therapeutics, targeting MTAP-deleted tumors, and is currently in clinical development. Broad Synergy Across Multiple Therapeutic Modalities MTAP homozygous deletion occurs in approximately 10–15% of solid tumors and frequently co-exists with oncogenic drivers such as KRAS and EGFR. In addition, MTAP abnormities are associated with poor prognosis following standard-of-care therapies across multiple cancer types. Therefore, there remains a significant unmet need for novel and effective combination therapies centered on MTA-cooperative PRMT5 inhibitor for MTAP-deleted tumors, with the potential to enable precision patient stratification and deliver synergistic therapeutic benefits. Preclinical studies demonstrated that ABSK131 exhibits strong synergistic activity with multiple therapies: KRAS inhibitors: Enhanced tumor growth inhibition in KRAS-mutant, MTAP-deleted models when combined with AMG 510 or ABSK141. EGFR inhibitors: Improved anti-proliferative and in vivo antitumor activity in EGFR-mutant, MTAP-deleted NSCLC models when combined with osimertinib. MAT2A inhibitors: Consistent synergistic effects across multiple tumor models when combined with IDE397. Chemotherapy: Synergistic activity observed both in vitro and in vivo when combined with carboplatin in NSCLC models. These findings support ABSK131 as a potential backbone therapy for combination strategies in MTAP-deleted tumors. Poster Information Title: Synergistic antitumor activity of the MTA-cooperative PRMT5 inhibitor ABSK131 in combination with multiple therapeutic agents in diverse cancer models Time: April 21, 2026, 9:00 AM - 12:00 PM (PT) Location: Poster Section 14, Board #23 Abstract #: 4504 FGFR2/3 Inhibitor ABSK061 ABSK061 is a highly potent and selective small-molecule FGFR2/3 inhibitor developed by Abbisko Therapeutics. It has demonstrated encouraging efficacy and safety in Phase I studies and is currently being evaluated in a Phase II trial for gastric cancer. ctDNA Analysis Reveals Resistance Mechanisms Acquired resistance remains a major challenge limiting the long-term benefit of targeted therapies. Using ctDNA-based next-generation sequencing (NGS), Abbisko conducted longitudinal genomic analyses comparing baseline and progression samples to elucidate resistance mechanisms to ABSK061: On-target resistance: Polyclonal acquired FGFR2 mutations in the FGFR2 kinase domain were commonly observed in gastric cancer and cholangiocarcinoma. Off-target resistance: FGFR2-Atered NSCLC was prone to develop acquired alterations in genes involved in RTK/RAS pathways. These findings provide important molecular insights into resistance mechanisms and inform the design of future combination and sequential treatment strategies. Poster Information Title: Circulating tumor DNA (ctDNA)-based profiling of acquired resistance to the fibroblast growth factor receptor (FGFR)2/3 inhibitor lavengratinib(ABSK061) in patient(pt)s with advanced solid tumors Time: April 21, 2026, 9:00 AM - 12:00 PM (PT) Location: Poster Section 45, Board #14 Abstract #: 5319 At AACR 2026, Abbisko Therapeutics showcased the latest preclinical and translational research advances across multiple pipeline programs, demonstrating its strong capabilities in drug discovery and development. As these programs continue to advance into clinical stages, the company is further strengthening its globally competitive R&D platform. Looking ahead, Abbisko Therapeutics will continue to focus on addressing unmet medical needs and accelerating the translation of innovative discoveries into clinical applications, with the goal of delivering more first-in-class and best-in-class therapies to patients worldwide. SOURCE Abbisko Therapeutics 21% more press release views with Request a Demo

AACRPhase 1Phase 2Clinical Result

23 Apr 2026

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[Ad hoc announcement pursuant to Art. 53 LR] Roche reports strong sales growth of +6% at constant exchange rates in the first quarter of 2026; -5% in CHF due to the significant appreciation of the Swiss franc

Group sales were +6% at constant exchange rates (CER) 1 , -5% when reported in CHF and +9% in USD 2 , in the first three months, driven by high demand for our innovative medicines and diagnostics. Pharmaceuticals Division sales were +7% at CER, -4% when reported in CHF and +10% in USD, due to continued high growth in sales of medicines for the treatment of severe diseases; Xolair (chronic hives, food allergies), Phesgo (breast cancer), Hemlibra (haemophilia A), Vabysmo (severe eye diseases) and Ocrevus (multiple sclerosis) were the top growth drivers. Diagnostics Division sales were +3% at CER, -7% when reported in CHF and +7% in USD, as demand for core lab and pathology solutions more than offset the impact of healthcare pricing reforms in China. Highlights: Positive data for: fenebrutinib for multiple sclerosis (phase III), Gazyva/Gazyvaro for an autoimmune condition affecting kidney function (phase III); and petrelintide for obesity (phase II) CE mark for new Elecsys NfL blood test to detect neuroinflammation in multiple sclerosis, representing a breakthrough in disease management Launch of the cobas MPX-E assay , a new 4-in-1 test to screen blood donors for HIV and hepatitis viruses Launch of the AI factory to accelerate the development of new therapeutics and diagnostics solutions Entry into a definitive agreement to acquire SAGA Diagnostics : SAGA’s proprietary cancer therapy response monitoring platform will strengthen Roche’s industry leading portfolio of oncology diagnostics and medicines Inauguration of the new research home for the Institute of Human Biology to enable scientists to pioneer human model systems for research Outlook for 2026 confirmed Roche CEO Thomas Schinecker : “We delivered a strong start to the year, achieving 6% Group sales growth at constant exchange rates. Our pipeline continued to advance in areas where patients face significant unmet need, including multiple sclerosis, obesity and a severe autoimmune disease that can lead to kidney failure. We also received EU approval for a new test to detect neuroinflammation in multiple sclerosis, marking a meaningful step forward in disease management. Our diversified portfolio across both divisions, together with continued pipeline progress, positions us well for sustained future growth in a dynamic geopolitical environment. We confirm our full-year outlook.” Outlook for 2026 Roche (SIX: RO, ROP; OTCQX: RHHBY) expects an increase in Group sales in the mid single digit range (CER) for 2026. Core earnings per share are targeted to develop in the high single digit range (CER). Roche expects to further increase its dividend in Swiss francs. Sales CHF millions As % of sales % change January–March 2026 2025 2026 2025 At CER In CHF In USD Group 14,722 15,440 100.0 100.0 +6 -5 +9 Pharmaceuticals Division 11,469 11,949 77.9 77.4 +7 -4 +10 United States 5,693 6,224 38.7 40.3 +5 -9 Europe 2,234 2,320 15.2 15.0 -1 -4 Japan 649 671 4.4 4.3 +14 -3 International 2,893 2,734 19.6 17.8 +16 +6 Diagnostics Division 3,253 3,491 22.1 22.6 +3 -7 +7 International: Asia-Pacific, CEETRIS (Central Eastern Europe, Türkiye, Russia and Indian subcontinent), Latin America, Middle East, Africa, Canada, others Group sales In the first three months of 2026, Roche sales were +6% at CER, -5% when reported in CHF, to CHF 14.7 billion due to strong demand for pharmaceutical products and diagnostic solutions. The appreciation of the Swiss franc against most currencies, notably the US dollar, had a significant impact on the results reported in Swiss francs compared to constant exchange rates. Sales in the Pharmaceuticals Division were +7% at CER, -4% when reported in CHF, to CHF 11.5 billion, with medicines for severe diseases continuing their strong growth. The top five growth drivers – Xolair, Phesgo, Hemlibra, Vabysmo and Ocrevus – achieved total sales of CHF 5.3 billion, an increase of 14% at CER, or 2% in CHF, compared to the first three months of 2025. Sales of products with expired patents (Avastin, Herceptin, MabThera/Rituxan, Lucentis and Actemra/RoActemra) decreased by a combined CHF 0.1 billion at CER, or CHF 0.2 billion in CHF. In the United States , sales were +5% at CER, -9% when reported in CHF, due to continued growth of Xolair and continuing uptake of Hemlibra, Polivy (blood cancer), Ocrevus and Vabysmo. This growth more than compensated for the lower sales of Perjeta (breast cancer) and Kadcyla (breast cancer). Sales in Europe were -1% at CER, or -4% when reported in CHF, due to lower sales of Polivy, the impact of biosimilar competition on Actemra/RoActemra and Perjeta (breast cancer) due to conversion to Phesgo. This decrease was partially offset by the demand for Ocrevus and Evrysdi (spinal muscular atrophy). In Japan , sales were +14% at CER, -3% when reported in CHF, mainly due to product supply to third parties, as well as a strong uptake of Hemlibra, Vabysmo and Polivy. Sales growth was partially offset by the decline in sales of Tamiflu and the impact of biosimilar erosion on Avastin. Sales in the International region were +16% at CER, or +6% when reported in CHF, led by Phesgo, Vabysmo, Polivy, Alecensa (lung cancer) and Ocrevus and partially offset by lower sales of influenza medicines Xofluza and Tamiflu. In China, sales were +14% at CER, or +5% when reported in CHF, as the uptake of Phesgo, Polivy and Vabysmo gained momentum following their inclusion in the government drug reimbursement list. The continued roll-out of Alecensa was the other growth driver. The increase was partially offset by lower sales of Xofluza and Perjeta. The Diagnostics Division’s sales were +3% at CER, -7% when reported in CHF, to CHF 3.3 billion as growth in demand for core lab and pathology solutions more than offset the impact of healthcare pricing reforms in China. Sales in the Europe, Middle East and Africa (EMEA) region were +3% at CER, -2% when reported in CHF, driven by higher sales of clinical chemistry and immunodiagnostic products. In North America , sales were +6% at CER, -7% when reported in CHF, with growth across core, pathology and molecular lab areas. Sales in Asia-Pacific were -5% at CER, or -15% when reported in CHF, due to the healthcare pricing reforms in China. In Latin America , sales growth was +10% at CER, or 0% when reported in CHF. Pharmaceuticals: key developments Compound Milestone Regulatory Gazyva/Gazyvaro Lupus FDA accepts application for Gazyva/Gazyvaro for the treatment of the most common form of lupus The filing was accepted based on phase III ALLEGORY data for Gazyva/Gazyvaro showing a significant reduction in disease activity compared with placebo in people with systemic lupus erythematosus (SLE). If approved, Gazyva/Gazyvaro would be the first anti-CD20 therapy to directly target B cells in SLE, potentially becoming the new standard of care for this condition. SLE is a potentially life-threatening autoimmune disease affecting more than three million people worldwide – achieving better disease control can reduce flares and may prevent irreversible organ damage. More information: Media Release , 21 April 2026 Giredestrant Breast cancer FDA accepts New Drug Application for giredestrant in ESR1-mutated, ER-positive advanced breast cancer Filing was accepted based on phase III data showing giredestrant plus everolimus reduced the risk of disease progression or death by 44% and 62% in ITT and ESR1-mutated populations, respectively, versus standard-of-care endocrine therapy plus everolimus. Strength of evERA data demonstrates the potential for giredestrant combination to help address resistance to standard-of-care therapies, and that it could be the first and only oral SERD combination approved in the post-CDK4/6 inhibitor setting. The FDA has set a Prescription Drug User Fee Act date of 18 December 2026. More information: Media Release , 20 February 2026 Phase III, pivotal and other key read-outs Enspryng MOGAD Enspryng reduces risk of relapses by 68%, demonstrating potential to become first treatment for MOGAD The phase III METEOROID study met its primary endpoint in patients with myelin oligodendrocyte glycoprotein antibody-associated disease (MOGAD). MOGAD is a rare autoimmune disease of the central nervous system characterised by unpredictable attacks of the optic nerves, spinal cord or brain that are often severe and debilitating. The data will be submitted to the regulatory authorities. More information: Media Release , 21 April 2026 Giredestrant Breast cancer Roche provides update on phase III persevERA study in ER-positive advanced breast cancer The persevERA breast cancer study did not meet the primary objective of a statistically significant improvement in progression-free survival, but a numerical improvement was observed. Giredestrant plus palbociclib was well tolerated and adverse events were consistent with the known safety profiles of each individual treatment. The FDA recently accepted the New Drug Application based on evERA data; phase III lidERA data has been submitted to the FDA. More information: Media Release , 9 March 2026 Petrelintide Obesity Roche announces positive phase II results for petrelintide, an amylin analogue developed for people living with overweight and obesity Petrelintide achieved up to 10.7% mean body weight reduction at week 42 versus 1.7% with placebo (p-value <0.001) while demonstrating placebo-like tolerability. At the maximally effective dose, there were no cases of vomiting and no treatment discontinuations due to gastrointestinal adverse events. The data support further development of petrelintide in chronic weight management as monotherapy and its tolerability pro confirms its value as a combination partner. More information: Media Release , 5 March 2026 Fenebrutinib Multiple sclerosis Fenebrutinib confirms its potential as first and only BTK inhibitor for relapsing and primary progressive multiple sclerosis (MS) in third positive phase III study (FENhance 1) FENhance 1 met its primary endpoint, showing that investigational fenebrutinib significantly reduced relapses by 51% compared to teriflunomide in relapsing multiple sclerosis (RMS), which is consistent with FENhance 2 results showing 59% reduction. FENhance 1 is the final study read-out of the fenebrutinib pivotal clinical development programme in MS, following positive results for FENhance 2 in RMS and for FENtrepid in primary progressive multiple sclerosis (PPMS). Fenebrutinib has the potential to become the first and only high-efficacy oral, brain-penetrant treatment for both RMS and PPMS, showing a profound benefit on relapsing and progressive disease biology. More information: Media Release , 2 March 2026 Gazyva/Gazyvaro Membranous nephropathy Roche announces positive phase III results for Gazyva/Gazyvaro in primary membranous nephropathy, marking a significant milestone in treatment of this autoimmune disease MAJESTY, the first global phase III study in primary membranous nephropathy, met its primary endpoint of complete remission at two years. Up to 30% of people with membranous nephropathy progress to kidney failure over 10 years despite current treatment approaches; achieving complete remission can help delay or prevent this. Gazyva/Gazyvaro could become the first approved treatment for primary membranous nephropathy, having already achieved positive results in lupus nephritis, systemic lupus erythematosus and idiopathic nephrotic syndrome. More information: Media Release , 16 February 2026 Fenebrutinib Multiple sclerosis Fenebrutinib is the first investigational medicine in over a decade that reduces disability progression in primary progressive multiple sclerosis (PPMS) Late-breaking phase III FENtrepid results presented at the Americas Committee for Treatment and Research in Multiple Sclerosis (ACTRIMS) Forum 2026 show investigational fenebrutinib met its primary endpoint of non-inferiority compared to the current standard of care, Ocrevus, in reducing disability progression in PPMS. Fenebrutinib numerically reduced the risk of disability progression by 12% compared to Ocrevus as early as 24 weeks; additional analysis showed potential benefit in upper limb function. Fenebrutinib has the potential to become a first-in-class therapy in multiple sclerosis, as an oral, brain-penetrant BTK inhibitor for PPMS and relapsing multiple sclerosis (RMS) More information: Media Release , 7 February 2026 Other Institute of Human Biology Roche inaugurates new research home for the Institute of Human Biology (IHB), pioneering human model systems to accelerate drug discovery and development The new building is part of a CHF 1.4 billion site investment, reinforcing Roche’s commitment to Switzerland and the Basel life sciences cluster. The IHB enables scientists to pioneer human model systems, accelerating the development of new medicines to improve the lives of patients. Federal Councillor Elisabeth Baume-Schneider, Head of the Federal Department of Home Affairs (FDHA), attended the official opening ceremony. More information: Media Release , 23 March 2026 AI factory Roche launches NVIDIA AI factory to accelerate the development of new therapeutics and diagnostics solutions With the addition of 2,176 NVIDIA Blackwell GPUs, Roche now operates the pharmaceutical industry’s largest announced hybrid-cloud AI factory, totalling more than 3,500 GPUs. The new computational infrastructure supports Roche’s vision of building an AI-accelerated healthcare organisation. NVIDIA AI factories help accelerate discoveries, enable more efficient clinical trials and unlock data insights at scale, ultimately advancing innovation and improved healthcare outcomes. More information: Media Release , 16 March 2026 Annual General Meeting Roche Annual General Meeting 2026 Shareholders approved all proposals of the Board of Directors. Severin Schwan was re-elected as Chairman of the Board of Directors; all other Board members standing for election were confirmed. Shareholders approved an increase of the dividend to CHF 9.80 per share; this is the 39th consecutive dividend increase. Shareholders approved the exchange of non-voting equity securities ( Genussscheine ) for participation certificates. More information: Media Release , 10 March 2026 Gazyva/Gazyvaro Lupus New England Journal of Medicine publishes phase III ALLEGORY data showing Gazyva/Gazyvaro significantly reduces disease activity in the most common form of lupus Over three quarters of people on Gazyva/Gazyvaro plus standard therapy achieved at least a four-point improvement in SRI-4, a measure that assesses disease severity and symptoms. Gazyva/Gazyvaro has the potential to become a new standard of care for people living with systemic lupus erythematosus (SLE). If approved, Gazyva/Gazyvaro would be the first type II anti-CD20 therapy for SLE to directly target B cells, a key driver of inflammation and disease activity. More information: Media Release , 6 March 2026 Change in Enlarged Corporate Executive Committee Change to the Roche Enlarged Corporate Executive Committee Roche announced the appointment of Mark Dawson, MD, PhD, as the new Head of Roche Pharma Research and Early Development (pRED), effective 1 May 2026. Based in Basel, he will also become a member of the Enlarged Corporate Executive Committee. Mark Dawson joins Roche from the Peter MacCallum Cancer Centre, where he serves as Associate Director of Research. A leading expert in cancer biology, his work on chromatin regulation and epigenetics has been instrumental in defining the molecular mechanisms that drive cancer initiation and progression. More information: Media Release , 17 February 2026 Pharmaceuticals sales Sales CHF millions As % of sales % change January–March 2026 2025 2026 2025 At CER In CHF Pharmaceuticals Division 11,469 11,949 100.0 100.0 +7 -4 United States 5,693 6,224 49.6 52.1 +5 -9 Europe 2,234 2,320 19.5 19.4 -1 -4 Japan 649 671 5.7 5.6 +14 -3 International 2,893 2,734 25.2 22.9 +16 +6 International: Asia-Pacific, CEETRIS (Central Eastern Europe, Türkiye, Russia and Indian subcontinent), Latin America, Middle East, Africa, Canada, others Top 20 best-selling pharmaceuticals (% change at CER 1 ) Total United States Europe Japan International CHF m % CHF m % CHF m % CHF m % CHF m % Ocrevus Multiple sclerosis 1,692 +6 1,117 +3 363 +9 - - 212 +24 Hemlibra Haemophilia A 1,190 +13 613 +15 252 +5 81 +18 244 +14 Vabysmo Eye diseases (nAMD, DME, RVO) 1,024 +13 652 +4 190 0 37 +39 145 +126 Tecentriq Cancer immunotherapy 811 +4 378 +6 202 -6 69 0 162 +14 Xolair 3 Chronic hives, food allergies 708 +26 708 +26 - - - - - - Phesgo Breast cancer 686 +27 159 +2 206 +7 42 +23 279 +78 Perjeta 3 Breast cancer 672 -11 263 -12 119 -15 12 -19 278 -9 Actemra/RoActemra 3 RA, COVID-19 534 -4 248 -3 124 -16 66 +9 96 +5 Evrysdi Spinal muscular atrophy 464 +19 160 +15 159 +13 18 +4 127 +40 Kadcyla 3 Breast cancer 439 -4 156 -11 123 -6 19 +6 141 +5 Polivy Blood cancer 407 +26 171 +26 63 -32 46 +24 127 +120 Alecensa Lung cancer 401 +12 105 -7 63 -5 43 +4 190 +39 MabThera/Rituxan 3 Blood cancer, RA 292 +10 183 +16 31 -8 3 -6 75 +6 Activase/TNKase 3 Cardiac diseases 255 -2 244 -2 - - - - 11 -4 Gazyva/Gazyvaro 3 Blood cancer, lupus nephritis 247 +10 115 +1 57 -2 9 +28 66 +45 Herceptin 3 Breast and gastric cancer 234 -12 44 -16 69 -7 1 -24 120 -14 Avastin 3 Various cancer types 224 -9 59 -15 14 +3 21 -29 130 -1 CellCept 3 Immunosuppressant 99 +10 4 -5 28 -14 9 -16 58 +37 Enspryng Acute inflammation of brain, spinal cord and optic nerves 96 +31 22 +20 11 +20 35 +13 28 +93 Columvi Blood cancer 95 +77 43 +35 21 +84 - - 31 +204 DME: diabetic macular edema / nAMD: neovascular or ‘wet’ age-related macular degeneration / RVO: retinal vein occlusion / RA: rheumatoid arthritis Diagnostics: key developments Product Milestone Elecsys NfL blood test Multiple sclerosis Roche receives CE mark for new Elecsys NfL blood test to detect neuroinflammation in multiple sclerosis (MS) The Elecsys NfL blood test detects neuroaxonal damage associated with neuroinflammation in adults diagnosed with relapsing remitting multiple sclerosis. This minimally invasive blood test enables greater patient access to monitoring of neuroinflammatory status versus current standard of care methods. By providing deeper insight into underlying neuroinflammatory activity, the Elecsys NfL blood test has the potential to enable effective MS monitoring and earlier clinical intervention. More information: Media Release , 13 April 2026 cobas MPX-E assay HIV and hepatitis viruses Roche launches the cobas MPX-E assay, a new 4-in-1 donor screening test to further safeguard the global blood supply The cobas MPX-E test provides four critical results (for HIV, HCV, HBV and HEV) in a single test, increasing laboratory efficiency and decreasing healthcare costs. The new test delivers faster turnaround times and allows labs to implement hepatitis E (HEV) screening without requiring additional instrumentation. This assay is designed for use on the fully automated cobas x800 systems, enabling high-throughput screening with up to 8 hours of walk-away time. More information: Media Release , 30 March 2026 Diagnostics sales Sales CHF millions As % of sales % change January–March 2026 2025 2026 2025 At CER In CHF Diagnostics Division 3,253 3,491 100.0 100.0 +3 -7 Customer areas Core Lab 1,798 1,904 55.3 54.5 +4 -6 Molecular Lab 571 634 17.5 18.2 0 -10 Near Patient Care 465 536 14.3 15.4 -5 -13 Pathology Lab 419 417 12.9 11.9 +12 0 Regions Europe, Middle East, Africa 1,206 1,236 37.1 35.4 +3 -2 North America 1,073 1,154 33.0 33.1 +6 -7 Asia-Pacific 725 853 22.3 24.4 -5 -15 Latin America 249 248 7.6 7.1 +10 0 More information on Roche’s performance in the first three months of 2026: Q1 2026 presentation Appendix with tables About Roche Roche (SIX: RO, ROP; OTCQX: RHHBY) is a healthcare company uniquely placed to prevent, stop and cure diseases by uniting leading science and technology across diagnostics, medicines and digital solutions. Roche was founded in Basel, Switzerland in 1896 and today is a leading provider of transformative medicines and diagnostics for millions of people in over 150 countries around the world. It is dedicated to tackling healthcare challenges that place the greatest strain on patients, families, communities and healthcare systems. Across its Diagnostics and Pharmaceutical divisions, Roche focuses on areas including oncology, neurology, cardiovascular and metabolic diseases, ophthalmology, infectious diseases and immunology with the aim of providing real and positive change for patients, the people they love and the professionals who care for them. Genentech in the United States is a fully owned subsidiary in the Roche Group. Roche is the majority shareholder in Chugai Pharmaceutical, a major innovator in the Japanese therapeutic antibody market. For more information, please visit . All trademarks used or mentioned in this release are protected by law. References [1] CER (Constant Exchange Rates). The percentage changes at constant exchange rates are calculated using simulations by reconsolidating both the 2026 and 2025 results at constant exchange rates (the average rates for the year ended 31 December 2025). For the definition of CER, see page 178 of the Roche Finance Report 2025. [2] USD (US dollars). The percentage changes for selected sales figures at US dollars are calculated by translating both the 2026 and 2025 sales figures at the respective average US dollar exchange rate for the period in question. This supplementary information is provided to assist readers when assessing comparability with other companies. [3] Products launched before 2015. Cautionary statement regarding forward-looking statements This document contains certain forward-looking statements. These forward-looking statements may be identified by words such as ‘believes’, ‘expects’, ‘anticipates’, ‘projects’, ‘intends’, ‘should’, ‘seeks’, ‘estimates’, ‘future’ or similar expressions or by discussion of, among other things, strategy, goals, plans or intentions. Various factors may cause actual results to differ materially in the future from those reflected in forward-looking statements contained in this document, such as: (1) pricing and product initiatives of competitors; (2) legislative and regulatory developments and economic conditions; (3) delay or inability in obtaining regulatory approvals or bringing products to market; (4) fluctuations in currency exchange rates and general financial market conditions; (5) uncertainties in the discovery, development or marketing of new products or new uses of existing products, including without limitation negative results of clinical trials or research projects, unexpected side effects of pipeline or marketed products; (6) increased government pricing pressures; (7) interruptions in production; (8) loss of or inability to obtain adequate protection for intellectual property rights; (9) litigation; (10) loss of key executives or other employees; and (11) adverse publicity and news coverage. The statement regarding earnings per share growth is not a profit forecast and should not be interpreted to mean that Roche’s earnings or earnings per share for this or any subsequent period will necessarily match or exceed the historical published earnings or earnings per share of Roche. Roche Global Media Relations Phone: +41 61 688 8888 / e-mail: media.relations@roche.com Hans Trees, PhD Phone: +41 79 407 72 58 Lorena Corfas Phone: +41 79 568 24 95 Simon Goldsborough Phone: +44 797 32 72 915 Karsten Kleine Phone: +41 79 461 86 83 Kirti Pandey Phone: +41 79 398 38 53 Yvette Petillon Phone: +41 79 961 92 50 Dr Rebekka Schnell Phone: +41 79 205 27 03 Irène Stephan Phone: +41 79 377 83 75 Roche Investor Relations Dr Bruno Eschli Phone: +41 61 68-75284 e-mail: bruno.eschli@roche.com Dr Sabine Borngräber Phone: +41 61 68-88027 e-mail: sabine.borngraeber@roche.com Dr Birgit Masjost Phone: +41 61 68-84814 e-mail: birgit.masjost@roche.com Investor Relations North America Loren Kalm Phone: +1 650 225 3217 e-mail: kalm.loren@gene.com Attachments Q1 appendix tables Media Investor Release Q1 2026 English

Clinical ResultPhase 3Executive ChangeDrug ApprovalPhase 2

100 Deals associated with Palbociclib

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D10372	Palbociclib	L01XE33	DB09073

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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

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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

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Study	Phase	Population	Analyzed Enrollment	Group	Results	Evaluation	Publication Date


NCT02693535 (TAPUR, AACR2026)	Phase 2	Lung Cancer CCND1 amplification	29	Palbociclib (CCND1 amplification + Lung Cancer)	kokhbiwzbh(iaycowqspv) = bltypzuigz yicbznxnnj (ytmhjccmsj, 10 - 100) View more	Negative	21 Apr 2026
AACR2026	Phase 2/3	Hormone receptor positive HER2 negative breast cancer HR Positive \| HER2 Negative	16	Imlunestrant alone	suxbuubxbh(fcwajooufs) = hehhodttol buudyhfabj (wmghxdwpaa ) View more	Positive	21 Apr 2026
				Camizestrant 75mg	suxbuubxbh(vzeqqpmzmh) = sexvdilrtc yzhqpwmdwi (mwqhafdfhd ) View more
NCT06495164 (Pubmed \| Breast)	Not Applicable	Metastatic breast cancer First line HR Positive \| HER2 Negative	974	Palbociclib + Aromatase Inhibitor	fzkmzzeyeg(kqkynpvfzw) = mezmkdlvsa pwchttjuoj (lmtylprazo ) View more	Positive	01 Apr 2026
				Aromatase Inhibitor	fzkmzzeyeg(kqkynpvfzw) = rqoenxupts pwchttjuoj (lmtylprazo ) View more
ESGO2026	Phase 1/2	Ovarian Serous Adenocarcinoma	70	Ribociclib + letrozole	trdbsilhjw(goybqfcnly) = zvabjccbaf zlpwwsmcuo (ciyyeufhub ) View more	Positive	28 Feb 2026
				Ribociclib + letrozole	trdbsilhjw(goybqfcnly) = wvalgnjpyh zlpwwsmcuo (ciyyeufhub )
NCT05468697 (LITESPARK-024, ASCO_GU2026)	Phase 1/2	Locally Advanced Clear Cell Renal Cell Carcinoma	59	Belzutifan 120 mg QD + Palbociclib 75 mg QD	vcwnmzmqgy(wknewfzxws) = hrcnehlmzo wvjliyjzez (uzocpnpkxn ) View more	Positive	26 Feb 2026
				Belzutifan 120 mg QD + Palbociclib 100 mg QD	vcwnmzmqgy(wknewfzxws) = mouljoydvy wvjliyjzez (uzocpnpkxn ) 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	yrsptsvzaa = vvewjibofp dcjhxmicgo (ngtesatfpe, wjgztwlfgw - exxblagfde) 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)	lsvifowbyx(cslvjxhbgw) = slqkvntzib zlecmiahtx (tidtpomuqu, yuwancalec - lnqxznscap) View more	-	12 Feb 2026
				fulvestrant+Letrozole+pertuzumab+Exemestane+anastrozole (Arm B)	lsvifowbyx(cslvjxhbgw) = qeaowhugca zlecmiahtx (tidtpomuqu, homvlhmxjz - crvszythox) 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	mewujofimb(abxvvslfhm) = lqnthyvdby cpchknzumc (abtthdawqj ) View more	Positive	29 Jan 2026
				maintenance HER2-targeted and endocrine therapies	mewujofimb(abxvvslfhm) = abpnttnagq cpchknzumc (abtthdawqj ) View more
NCT02513394 (PALLAS, SABCS2025)	Phase 3	Hormone receptor positive HER2 negative breast cancer Adjuvant HR+ \| HER2-	5,736	Palbociclib + Endocrine Therapy	pjqamisete(vhfninckop) = hjtefscegi igqfdjvvll (igzgghqwda ) View more	Negative	11 Dec 2025
NCT03870919 (palatine, SABCS2025)	Phase 2	ER-positive/HER2-negative Breast Cancer ER positive \| HER2 negative	191	Palbociclib + letrozole combination therapy	gmaznnuqxu(lyjbhqzepk) = areheugljc dfixqbzxrh (zbronzrboj ) View more	Negative	10 Dec 2025

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