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6-K 1 a231210_morphosysagashpran.htm 6-K Document

UNITED STATES

SECURITIES AND EXCHANGE COMMISSION

Washington, D.C. 20549

FORM 6-K

REPORT OF FOREIGN PRIVATE ISSUER PURSUANT TO RULE 13a-16 OR 15d-16

UNDER THE SECURITIES EXCHANGE ACT OF 1934

For the month of December, 2023

COMMISSION FILE NUMBER 001-38455

MorphoSys AG

Semmelweisstrasse 7

82152 Planegg

Germany

(Address of principal executive offices)

Indicate by check mark whether the registrant files or will file annual reports under cover Form 20-F or Form 40-F: Form 20-F x Form 40-F ¨

Indicate by check mark if the registrant is submitting the Form 6-K in paper as permitted by Regulation S-T Rule 101(b)(1): ¨

Indicate by check mark if the registrant is submitting the Form 6-K in paper as permitted by Regulation S-T Rule 101(b)(7): ¨

On December 10, 2023, MorphoSys AG (the “Company”) issued a press release attached hereto as Exhibit 99.1. On December 11, 2023, MorphoSys AG, held an investor call including a presentation attached hereto as Exhibit 99.2.

Exhibits

99.1 MorphoSys’ Pelabresib Improves All Four Hallmarks of Myelofibrosis in Phase 3 MANIFEST-2 Study

99.2 ASH 2023 Investor Event with MorphoSys Management and Medical Experts

SIGNATURES

Pursuant to the requirements of the Securities Exchange Act of 1934, the registrant has duly caused this report to be signed on its behalf by the undersigned, thereunto duly authorized.

MORPHOSYS AG (Registrant)

Date: December 11, 2023 By: /s/ i.A Inge Altinger-Ralle

Name: Inge Altinger-Ralle

Title: Specialist Corporate Publishing

By: /s/ i.A. Dr. Robert Mayer

Name: Dr. Robert Mayer

Title: Director Investor Relations

EX-99.1 2 exhibit_9917.htm EX-99.1 Document

Media Release

Planegg/Munich, Germany, December 10, 2023

MorphoSys’ Pelabresib Improves All Four Hallmarks of Myelofibrosis in Phase 3 MANIFEST-2 Study

Pelabresib and ruxolitinib combination significantly reduced spleen size, with an SVR35 response rate nearly double that of placebo plus ruxolitinib

Showed a strong positive trend in reducing symptom burden and a twofold increase in patients achieving both SVR35 and TSS50 versus placebo plus ruxolitinib

Improved measures of anemia, including higher hemoglobin response rates, fewer patients requiring transfusions and fewer anemia adverse events versus placebo plus ruxolitinib

Improved bone marrow fibrosis by at least one grade in more patients versus placebo plus ruxolitinib

Demonstrated safety results consistent with prior clinical trials, with fewer grade ≥3 adverse events compared with placebo plus ruxolitinib

MorphoSys will host an investor event to review findings on Monday, December 11

MorphoSys AG (FSE: MOR; NASDAQ: MOR) today announced comprehensive results from the Phase 3 MANIFEST-2 study investigating pelabresib, an investigational BET inhibitor, in combination with the JAK inhibitor ruxolitinib in JAK inhibitor-naïve patients with myelofibrosis. These findings were presented in an oral presentation at the 65th American Society of Hematology (ASH) Annual Meeting and Exposition in San Diego, California.

Myelofibrosis is characterized by four hallmarks: an enlarged spleen, anemia, bone marrow fibrosis and disease-associated symptoms. In MANIFEST-2, all hallmarks were improved with the pelabresib and ruxolitinib combination versus placebo plus ruxolitinib, which is the standard of care in myelofibrosis. Ruxolitinib dosing was similar in both arms of the study and was determined based on its approved myelofibrosis indication.

“The MANIFEST-2 results demonstrated clear benefits across the four hallmarks of myelofibrosis, including a significant reduction in spleen size – a key finding given the known association between spleen volume reduction and patient survival,” said Raajit K. Rampal, M.D., Ph.D., Director, Center for Hematologic Malignancies, and Director, Myeloproliferative Neoplasms Program, Memorial Sloan Kettering Cancer Center. “The comprehensive results presented at ASH also show that the pelabresib combination improves anemia, disease-associated symptoms and bone marrow fibrosis, and that it is well-tolerated. These findings point to pelabresib and ruxolitinib as a potential paradigm-shifting first-line treatment of this debilitating disease.”

MANIFEST-2 Comprehensive Findings

MANIFEST-2 is a global, multicenter, double-blind, Phase 3 study of 430 JAK inhibitor-naïve adults with myelofibrosis, randomized 1:1 to receive the pelabresib and ruxolitinib combination or placebo plus ruxolitinib. MANIFEST-2 is one of the largest studies in this disease to date.

Strong Reductions in Spleen Size and Symptoms

In the MANIFEST-2 study, pelabresib and ruxolitinib demonstrated a near doubling in the proportion of patients achieving a ≥35% reduction in spleen volume (SVR35) at 24 weeks, the primary endpoint, versus placebo plus ruxolitinib (p<0.001).

For the first key secondary endpoint assessing symptom reduction, absolute change in total symptom score (TSS) at 24 weeks, there was a strong numerical improvement for patients receiving pelabresib and ruxolitinib versus placebo plus ruxolitinib. The response rate for the second key secondary endpoint, proportion of patients achieving ≥50% reduction in symptom score (TSS50) at 24 weeks, was also numerically greater for patients receiving pelabresib and ruxolitinib. Significant improvements in both key secondary endpoints were observed with the pelabresib combination for patients classified as intermediate-risk (Dynamic International Prognostic Scoring System [DIPSS] Int-1 and Int-2), who account for over 90% of the MANIFEST-2 population.

The proportion of patients achieving both SVR35 and TSS50 at 24 weeks was doubled with pelabresib and ruxolitinib versus placebo plus ruxolitinib (40.2% vs. 18.5%, respectively).

Details are included in the table below.


Endpoint	Pelabresib + Ruxolitinib (N=214)	Placebo + Ruxolitinib (N=216)	Difference
SVR35	65.9%	35.2%	30.4%* P-value: p<0.001
Absolute Change in TSS	-15.99 (Mean Baseline: 28.26)	-14.05 (Mean Baseline: 27.36)	-1.94** P-value: 0.0545
TSS50	52.3%	46.3%	6.0%* P-value: 0.216

*Difference calculated using Cochran–Mantel–Haenszel (CMH) common risk difference

**Least square mean estimate

Improvement in Anemia

Patients receiving pelabresib in combination with ruxolitinib reported fewer anemia adverse events (43.9%, grade ≥3: 23.1%) compared with placebo plus ruxolitinib (55.6%, grade ≥3: 36.4%). Additionally, by week 24, fewer patients in the pelabresib and ruxolitinib arm required red blood cell transfusions compared with the placebo arm (30.8% vs. 41.2%, respectively).

A greater proportion of patients achieved a hemoglobin response — defined as a ≥1.5 g/dL mean increase in hemoglobin levels over baseline in the absence of transfusions during the previous 12 weeks — with pelabresib and ruxolitinib versus placebo plus ruxolitinib (9.3% vs. 5.6%, respectively). Average hemoglobin levels were greater in patients receiving pelabresib and ruxolitinib than in those receiving placebo plus ruxolitinib, starting at week 9 and continuing to week 24. Anemia benefits were observed across all studied patient risk groups.

“Anemia can reduce patients’ quality of life by causing severe fatigue and necessitating blood transfusions,” said Professor Claire Harrison, Guy’s and St. Thomas’ NHS Foundation Trust, London, United Kingdom. “In MANIFEST-2, patients receiving the combination therapy showed clear benefits on anemia, including greater hemoglobin levels, fewer red blood cell transfusions and fewer anemia and fatigue adverse events. Given its strong efficacy, safety profile and signs of disease modification, the pelabresib and ruxolitinib combination has the potential to become the new standard of care in the first-line treatment of myelofibrosis.”

Improvement in Bone Marrow Fibrosis

Bone marrow fibrosis, or the replacement of bone marrow with fibrous scar tissue, is a central pathological feature of myelofibrosis. In MANIFEST-2, fibrosis was improved by at least one grade in a greater proportion of patients receiving pelabresib and ruxolitinib (38.5% vs.

24.2% with placebo plus ruxolitinib) and worsened by at least one grade in a smaller proportion of patients receiving pelabresib and ruxolitinib (16.3% vs. 28.3% with placebo plus ruxolitinib) at 24 weeks. Bone marrow fibrosis is graded on a scale from 0 (normal) to 3 (most severe) based on fiber density; studies suggest a correlation between the grade of bone marrow fibrosis and patient prognosis.

Biomarker Analysis Suggests Disease Modification

In a biomarker analysis, average plasma levels of inflammatory cytokines (IL-8, IL-6, TNF-α and NF-κB-regulated cytokines) were reduced in patients receiving pelabresib and ruxolitinib compared with placebo plus ruxolitinib at 24 weeks. Increased cytokine levels are associated with all four disease hallmarks; increased IL-8 levels are also associated with worse survival outcomes. These biomolecular improvements suggest early evidence of a disease-modifying effect.

Well-Tolerated Safety Profile

Overall, grade ≥3 treatment-emergent adverse events (TEAEs) were reported less frequently with pelabresib and ruxolitinib than with placebo plus ruxolitinib (49.1% vs. 57.5%, respectively).

In the pelabresib and ruxolitinib arm, the most common (≥10%) hematologic TEAEs were anemia (43.9%; grade ≥3: 23.1%), thrombocytopenia (32.1%; grade ≥3: 9.0%) and platelet count decrease (20.8%; grade ≥3: 4.2%). In the placebo plus ruxolitinib arm, the most common hematologic TEAEs were anemia (55.6%; grade ≥3: 36.4%), thrombocytopenia (23.4%; grade ≥3: 5.6%) and platelet count decrease (15.9%; grade ≥3: 0.9%).

The most common (≥10%) nonhematologic TEAEs in the pelabresib and ruxolitinib arm were diarrhea (23.1%; grade ≥3: 0.5%), dysgeusia (18.4%; grade ≥3: 0.5%), constipation (18.4%; grade ≥3: 0%), nausea (14.2%; grade ≥3: 0.5%), cough (12.7% grade ≥3: 0), asthenia (11.8% grade ≥3: 0.5%), fatigue (11.8%; grade ≥3: 0.5%), dizziness (11.3%; grade ≥3: 0%), headache (11.3% grade ≥3: 0.5%) and COVID-19 (11.3%; grade ≥3: 0%). The most common nonhematologic TEAEs in the placebo plus ruxolitinib arm were constipation (24.3%; grade ≥3: 0%), diarrhea (18.7%; grade ≥3: 1.4%), fatigue (16.8%; grade ≥3: 0.9%), COVID-19 (15.9%; grade ≥3: 1.9%), nausea (15.0%; grade ≥3: 0%), asthenia (13.6%; grade ≥3: 0%), dyspnea (13.1%; grade ≥3: 0.9%), cough (11.2%; grade ≥3: 0%) and headache (10.7%; grade ≥3: 0%). Discontinuation rates due to adverse events were 10.7% with pelabresib and ruxolitinib and 6.5% with placebo plus ruxolitinib.

The safety profile of the pelabresib and ruxolitinib combination therapy was consistent with previous clinical studies. No new safety signals were observed.

“The four hallmarks of myelofibrosis – enlarged spleen, anemia, bone marrow fibrosis and disease-associated symptoms – have a strong impact on a patient’s life. In MANIFEST-2, the combination of JAK and BET inhibition addressed all four of these hallmarks with the potential to modify the course of the disease,” said Tim Demuth, M.D., Ph.D., MorphoSys Chief Research and Development Officer. “We are confident that the comprehensive data package will provide impactful insights into the promising and well-tolerated combination of pelabresib and ruxolitinib. Our goal now is to bring this first-line therapy to patients with intermediate- and high-risk myelofibrosis as quickly as possible. We look forward to meeting with regulatory agencies regarding these data and are diligently preparing regulatory filings with the intention of submitting applications to the U.S. Food and Drug Administration and the European Medicines Agency in the middle of 2024.”

Investor Event at ASH 2023

MorphoSys will host an in-person investor event to review these detailed findings and address questions with the company’s management team and medical experts, including Professor Claire Harrison, Guy’s and St. Thomas’ NHS Foundation Trust, London, United Kingdom, and Ruben Mesa, M.D., FACP, President and Executive Director, Atrium Health Levine Cancer Center and Atrium Health Wake Forest Baptist Comprehensive Cancer Center.

The event, taking place on Monday, December 11 at the Hilton San Diego Bayfront Hotel, will start with a networking breakfast at 6:30 a.m. PST and continue with a formal presentation at 7:00 a.m. PST (4:00 p.m. CET / 3:00 p.m. GMT / 10:00 a.m. EST). A webcast will also be available for those not attending ASH 2023 in person.

Webcast participants may pre-register and will receive dial-in details to access the call easily and quickly: https://services.choruscall.it/DiamondPassRegistration/register?confirmationNumber=5982651&linkSecurityString=c1a71840b. Please dial in 10 minutes before the beginning of the conference.

The live webcast (audio and presentation) can be directly accessed via https://media.choruscall.eu/mediaframe/webcast.html?webcastid=q3lG25n3 or via the Investors section under "Events & Conferences" on the MorphoSys website, www.morphosys.com; after the call, a slide-synchronized audio replay of the conference call will be available at the same location.

About MorphoSys

At MorphoSys, we are driven by our mission: More life for people with cancer. As a global commercial-stage biopharmaceutical company, we develop and deliver innovative medicines, aspiring to redefine how cancer is treated. MorphoSys is headquartered in Planegg, Germany, and has its U.S. operations anchored in Boston, Massachusetts. To learn more, visit us at www.morphosys.com and follow us on Twitter at X and LinkedIn.

About Pelabresib

Pelabresib (CPI-0610) is an investigational selective small molecule designed to promote anti-tumor activity by inhibiting the function of bromodomain and extra-terminal domain (BET) proteins to decrease the expression of abnormally expressed genes in cancer. Pelabresib is being investigated as a treatment for myelofibrosis and has not yet been approved by any regulatory authorities.

The development of pelabresib was funded in part by The Leukemia and Lymphoma Society®.

About MANIFEST-2

MANIFEST-2 (NCT04603495) is a global, double-blind, Phase 3 clinical trial that randomized 430 JAK inhibitor-naïve adult patients with myelofibrosis 1:1 to receive pelabresib in combination with ruxolitinib or placebo plus ruxolitinib. The primary endpoint of the study is a 35% or greater reduction in spleen volume (SVR35) from baseline at 24 weeks. The key secondary endpoints of the study are the absolute change in total symptom score (TSS) from baseline at 24 weeks and the proportion of patients achieving a 50% or greater improvement in total symptom score (TSS50) from baseline at 24 weeks. TSS is measured using the myelofibrosis self-assessment form (MFSAF) v4.0, which asks patients to report the severity of seven common symptoms, rating each of them on a scale from 0 (absent) to 10 (worst imaginable).

The new key secondary endpoint, absolute change in TSS, was added to directly measure change in the average TSS from baseline to week 24 of treatment and is listed as the first key secondary endpoint in the MANIFEST-2 hierarchical testing scheme. The decision to update the MANIFEST-2 clinical trial protocol was made following a Type C meeting with the U.S. Food and Drug Administration (FDA) in September 2023. The final clinical protocol amendment is subject to approvals by health authorities outside of the U.S.

Additional secondary endpoints include progression-free survival, overall survival, duration of the splenic and total symptom score response, hemoglobin response rate and improvement in bone marrow fibrosis, among others.

Constellation Pharmaceuticals, Inc., a MorphoSys company, is the MANIFEST-2 trial sponsor.

About Myelofibrosis

Myelofibrosis is a blood cancer – belonging to a group of diseases called myeloproliferative neoplasms – caused by genetic abnormalities in bone marrow stem cells and characterized by four hallmarks: enlarged spleen, anemia, impaired bone marrow microenvironment causing fibrosis, and debilitating disease-associated symptoms, including severe fatigue, night sweats, itching, increased bleeding and significant pain caused by their enlarged spleen. For many living with myelofibrosis, the combination of symptoms often severely impacts their quality of life. At diagnosis, several factors, such as age, genetics and bloodwork, help determine a patient’s long-term prognosis. About 90% of newly diagnosed patients have intermediate- to high-risk disease, which has a worse prognosis and a higher likelihood of disease-associated symptoms. While JAK inhibitors, the current standard of care, address some aspects of the disease, no agent provides broad disease control. There is an urgent need for novel, well-tolerated therapeutic options capable of changing the natural course of myelofibrosis to provide patients with deep and durable responses across its four hallmarks.

Forward-Looking Statements

This communication contains certain forward-looking statements concerning the MorphoSys group of companies. The forward-looking statements contained herein represent the judgment of MorphoSys as of the date of this release and involve known and unknown risks and uncertainties, which might cause the actual results, financial condition and liquidity, performance or achievements of MorphoSys, or industry results, to be materially different from any historic or future results, financial conditions and liquidity, performance or achievements expressed or

implied by such forward-looking statements. In addition, even if MorphoSys' results, performance, financial condition and liquidity, and the development of the industry in which it operates are consistent with such forward-looking statements, they may not be predictive of results or developments in future periods. Among the factors that may result in differences are that MorphoSys' expectations may be incorrect, the inherent uncertainties associated with competitive developments, clinical trial and product development activities and regulatory approval requirements, MorphoSys' reliance on collaborations with third parties, estimating the commercial potential of its development programs and other risks indicated in the risk factors included in MorphoSys' Annual Report on Form 20-F and other filings with the U.S. Securities and Exchange Commission. Given these uncertainties, the reader is advised not to place any undue reliance on such forward-looking statements. These forward-looking statements speak only as of the date of publication of this document. MorphoSys expressly disclaims any obligation to update any such forward-looking statements in this document to reflect any change in its expectations with regard thereto or any change in events, conditions or circumstances on which any such statement is based or that may affect the likelihood that actual results will differ from those set forth in the forward-looking statements, unless specifically required by law or regulation.

For more information, please contact:


Media Contacts: Thomas Biegi Vice President Tel: +49 (0)151 / 74612318 thomas.biegi@morphosys.com			Investor Contact: Dr. Julia Neugebauer Head of Investor Relations Tel: +49 (0)89 / 899 27 179 julia.neugebauer@morphosys.com
Eamonn Nolan Director Tel: +1 617-548-9271 eamonn.nolan@morphosys.com

EX-99.2 3 exhibit_992.htm EX-99.2 exhibit_992

ASH 2023 Investor Event with Medical Experts December 11, 2023 Gail, Living with Myelofibrosis since 2018 Pelabresib in First-Line Myelofibrosis – Phase 3 MANIFEST-2 Results

This communication contains certain forward-looking statements concerning the MorphoSys group of companies, including the expectations regarding Monjuvi's ability to treat patients with relapsed or refractory diffuse large B-cell lymphoma ("DLBCL"), the further clinical development of tafasitamab, including ongoing confirmatory trials, additional interactions with regulatory authorities and expectations regarding future regulatory filings and possible additional approvals for tafasitamab as well as the commercial performance of Monjuvi. The words "anticipate", "believe", "estimate", "expect", "intend", "may", "plan", "predict", "project", "would", "could", "potential", "possible", "hope" and similar expressions are intended to identify forward-looking statements, although not all forward-looking statements contain these identifying words. The forward-looking statements contained herein represent the judgment of MorphoSys as of the date of this release and involve known and unknown risks and uncertainties, which might cause the actual results, financial condition and liquidity, performance or achievements of MorphoSys, or industry results, to be materially different from any historic or future results, financial conditions and liquidity, performance or achievements expressed or implied by such forward-looking statements. In addition, even if MorphoSys' results, performance, financial condition and liquidity, and the development of the industry in which it operates are consistent with such forward-looking statements, they may not be predictive of results or developments in future periods. Among the factors that may result in differences are MorphoSys' expectations regarding risks and uncertainties related to the impact of the COVID-19 pandemic to MorphoSys' business, operations, strategy, goals and anticipated milestones, including its ongoing and planned research activities, ability to conduct ongoing and planned clinical trials, clinical supply of current or future drug candidates, commercial supply of current or future approved products, and launching, marketing and selling current or future approved products, the global collaboration and license agreement for tafasitamab, the further clinical development of tafasitamab, including ongoing confirmatory trials, and MorphoSys' ability to obtain and maintain requisite regulatory approvals and to enroll patients in its planned clinical trials, additional interactions with regulatory authorities and expectations regarding future regulatory filings and possible additional approvals for tafasitamab as well as the commercial performance of Monjuvi, MorphoSys' reliance on collaborations with third parties, estimating the commercial potential of its development programs and other risks indicated in the risk factors included in MorphoSys' Annual Report on Form 20-F and other filings with the U.S. Securities and Exchange Commission. Given these uncertainties, the reader is advised not to place any undue reliance on such forward-looking statements. These forward-looking statements speak only as of the date of publication of this document. MorphoSys expressly disclaims any obligation to update any such forward-looking statements in this document to reflect any change in its expectations with regard thereto or any change in events, conditions or circumstances on which any such statement is based or that may affect the likelihood that actual results will differ from those set forth in the forward-looking statements, unless specifically required by law or regulation. The compounds discussed in this slide presentation are investigational products being developed by MorphoSys and its partners and are not currently approved by the U.S. Food and Drug Administration (FDA), European Medicines Agency (EMA) or any other regulatory authority (except for tafasitamab/Monjuvi® and tafasitamab/Minjuvi® in relapsed or refractory DLBCL). The safety and efficacy of these investigational products have not been established and there is no guarantee any investigational product will be approved by regulatory authorities. Monjuvi® and Minjuvi® are registered trademarks of MorphoSys AG. Forward-Looking Statements 2© MorphoSys – ASH 2023 MANIFEST-2 Investor Event – December 2023

JEAN-PAUL KRESS, M.D. Chief Executive Officer, MorphoSys Welcome & Opening Remarks 01 © MorphoSys – ASH 2023 MANIFEST-2 Investor Event – December 2023

MANIFEST-2 Most Impressive Benefits Seen in Myelofibrosis File for Approval in the U.S. and Ex-U.S. Multi-Billion Dollar Market Opportunity Excellent Operational Execution (Data readout six months ahead of schedule) Pelabresib and Ruxolitinib Combination Therapy: Potential to Shift Treatment Paradigm in Myelofibrosis 4© MorphoSys – ASH 2023 MANIFEST-2 Investor Event – December 2023 STRONG RUNWAY, WITH CASH AVAILABLE INTO 2025 OUR VISION: Pelabresib Combination Therapy Becomes New Standard of Care in Myelofibrosis

© MorphoSys – Q2 2023 Results 5 Welcome & Opening Remarks Jean-Paul Kress, M.D., Chief Executive Officer, MorphoSys01 Myelofibrosis Burden of Disease and Medical Need Claire Harrison, DM, FRCP, FRCPath, Professor and Clinical Director Department of Hematology Guy’s and St. Thomas’ NHS Foundation Trust, London, United Kingdom02 Phase 3 MANIFEST-2 Trial Results Claire Harrison, DM, FRCP, FRCPath, Professor and Clinical Director Department of Hematology Guy’s and St. Thomas’ NHS Foundation Trust, London, United Kingdom Ruben Mesa, M.D., FACP, President and Executive Director, Atrium Health Levine Cancer Center and Atrium Health Wake Forest Baptist Comprehensive Cancer Center 03 Pelabresib Clinical Development Next Steps Tim Demuth, M.D., Ph.D., Chief Research and Development Officer, MorphoSys 04 Q&A Moderated Q&A05 Agenda

PROFESSOR CLAIRE HARRISON Guy’s and St. Thomas’ NHS Foundation Trust, London, United Kingdom Myelofibrosis Disease Burden and Medical Need 02 © MorphoSys – ASH 2023 MANIFEST-2 Investor Event – December 2023

7 Enlarged Spleen Anemia Bone Marrow Fibrosis 4 2 1 3 Disease-Associated Symptoms MEDIAN OVERALL SURVIVAL (DIPSS)* + ~4 – 14.2 years for intermediate-risk** + ~1.5 years for high-risk DIAGNOSIS (DIPSS)* + ~77-86% of patients have intermediate-risk** + ~9-11% of patients have high-risk disease Myelofibrosis is a Debilitating, Progressive and Often Deadly Blood Cancer, Characterized by Four Hallmarks *Measured by Dynamic International Prognostic Scoring System (DIPSS) | **Int-1 and Int-2 Harrison C, et al. Expert Rev Hematol 2013; Al-Ali HK, et al. Haematologica 2016; Primary myelofibrosis. Orphanet. Accessed August 2023; Primary Myelofibrosis. MPN Research Foundation. Accessed August 2023; Mehta J, et al. Leuk Lymphoma 2014; Panda A, et al. Decision Resources Group 2022; Passamonti, F et al. Hematological Oncology 2021; Szuber N, et al. Mayo Clinic 2019; Passamonti, F et al. Blood 2010. No currently approved myelofibrosis treatment addresses all four hallmarks of disease THE FOUR HALLMARKS © MorphoSys – ASH 2023 MANIFEST-2 Investor Event – December 2023

JAK-STAT Pathway and BET Proteins Are Central to Myelofibrosis Pathology © MorphoSys – ASH 2023 MANIFEST-2 Investor Event – December 2023 8 JAK JAK ruxolitinib JAKi pelabresib TGFβ NF-kB BCL-2 cMyc Cell survival Aberrant erythroid and megakaryocytic differentiation Increased inflammatory factors Bone marrow fibrosis Cytokine receptor Extracellular Intracellular nucleus BETi The combination of BET and JAK inhibition: • Showed broad suppression of the proinflammatory molecules involved in bone marrow fibrosis in vivo • Normalized the balance of precursor red blood cells and precursor platelet-forming cells in the bone marrow in vivo Tefferi A, et al. Am J Hematol 2021; Shorstova T, et al. Br J Cancer 2021; Mughal TI, et al. Int J Gen Med 2014; Kleppe M, et al. Cancer Cell 2018; Albrecht BK, et al. J Med Chem 2016; Mascarenhas J, et al. J Clin Oncol 2023; Harrison CN, et al. Future Oncol 2022.

JAK-inhibitor-naïve myelofibrosis patients Primary: SVR35 at 24 Weeks Key Secondary: TSS50 at 24 weeks (MFSAF v4.0) Phase 2 MANIFEST Arm 3: Strong Improvements in Spleen Volume and Symptoms Across All Patient Risk Groups Form Basis for Phase 3 Study © MorphoSys – ASH 2023 MANIFEST-2 Investor Event – December 2023 9 TSS50 (24 Weeks) SVR35 (24 Weeks) PATIENT POPULATION BY DIPSS RISK CATEGORY 56%68%All Patients (N = 84) 42%70% Intermediate-1 (DIPSS) (N = 20) 57%71% Intermediate-2 (DIPSS) (N = 51) 85%54% High-Risk (DIPSS) (N = 13) STUDY POPULATION ENDPOINTS Mascarenhas J, et al. J Clin Oncol. 2023;41(32): 4993-5004. Durable responses were seen in SVR35 and TSS50 at 48 and 60 weeks

PROFESSOR CLAIRE HARRISON Guy’s and St. Thomas’ NHS Foundation Trust, London, United Kingdom Phase 3 MANIFEST-2 Trial Results 03 © MorphoSys – ASH 2023 MANIFEST-2 Investor Event – December 2023 RUBEN MESA, M.D., FACP President and Executive Director, Atrium Health Levine Cancer Center and Atrium Health Wake Forest Baptist Comprehensive Cancer Center

Rampal R, et al. ASH 2023. Oral 628 Pelabresib (CPI-0610) is an investigational new drug and has not been approved by any regulatory authority Global, Randomized, Double-Blind, Active-Control, Phase 3 Study 11 Study population Treatment arm 1:1 randomization stratified by:  DIPSS risk category: Int-1 vs Int-2 vs high  Platelet count: >200 × 109/L vs 100–200 × 109/L  Spleen volume: ≥1800 cm3 vs <1800 cm3 Double-blind randomization (1:1) JAKi-naïve patients with MF (N=430) (primary or post-ET/PV)  DIPSS Int-1 or higher  Splenomegaly (≥450 cm3) by CT/MRI  TSS ≥10 (≥3 for two symptoms, MFSAF v4.0) 21-day cycles Pelabresib 125 mg* PO QD Day 1–14 Ruxolitinib Per label with a 5-mg BID lower starting dose† Day 1–21 Placebo PO QD Day 1–14 Primary endpoint  SVR35 at Week 24 Key secondary endpoints  TSS absolute change from baseline at Week 24  TSS50 at Week 24 Safety  AEs of all grades and serious AEs AE, adverse event; BID, twice daily; CT, computed tomography; DIPSS, Dynamic International Prognostic Scoring System; ET, essential thrombocythemia; Int, intermediate; JAKi, Janus kinase inhibitor; MF, myelofibrosis; MFSAF, Myelofibrosis Symptom Assessment Form; MRI, magnetic resonance imagining; PO, orally; PV, polycythemia vera; QD, once daily; SVR35, ≥35% reduction in spleen volume; TSS, total symptom score; TSS50, ≥50% reduction in total symptom score. *The starting dose for pelabresib was 125 mg QD and protocol-defined dose modifications based on AEs and treatment response allowed a dose range between 50 mg and 175 mg QD; †Ruxolitinib was started at 10 mg BID (baseline platelet count 100–200 × 109/L) or 15 mg BID (baseline platelet count >200 × 109/L) with a mandatory dose increase by 5 mg BID after one cycle and a maximum dose of 25 mg BID per label. Harrison CN, et al. Future Oncol. 2022;18(27):2987-29977. Ruxolitinib Per label with a 5-mg BID lower starting dose† Day 1–21 + +

Rampal R, et al. ASH 2023. Oral 628 Pelabresib (CPI-0610) is an investigational new drug and has not been approved by any regulatory authority Patient disposition Data cut off: August 31, 2023. N/A, not applicable. *Other: non-compliance, withdrawal of consent. The study opened for enrollment in November 2020; the first patient received their initial treatment on April 22, 2021, and the last patient received their first treatment on March 2, 2023. Percentages reported are based on the number of patients randomized (intent-to-treat set). 214 (100%) 216 (100%)Randomized Treated Discontinued double-blind treatment Pelabresib + ruxolitinib Placebo + ruxolitinib Ongoing on double-blind treatment 212 (99.1%) 214 (99.1%) 58 (27.1%) 54 (25.0%) 154 (72.0%) 160 (74.1%) Placebo + ruxolitinib Pelabresib + ruxolitinib N/A108 mg Mean daily dose for pelabresib (14 days per 21-day cycle) 31.3 mg29.3 mgMean daily dose for ruxolitinib (daily) 45.4Median follow-up on study (weeks) 23 (10.7%)Adverse event 9 (4.2%)Physician decision (including lack of benefit) 5 (2.3%)Disease progression 8 (3.7%)Eligible for transplant 13 (6.0%)Other* 14 (6.5%) 20 (9.3%) 5 (2.3%) 9 (4.2%) 6 (2.8%) 12

Rampal R, et al. ASH 2023. Oral 628 Pelabresib (CPI-0610) is an investigational new drug and has not been approved by any regulatory authority Baseline disease characteristics 13 Placebo + ruxolitinib (N=216) Pelabresib + ruxolitinib (N=214)Characteristic 66 (26, 88)66 (19, 84)Median (min, max)Age — years 94 (43.5) / 122 (56.5)85 (39.7) / 129 (60.3)Female / maleSex — n (%) 163 (75.5) / 42 (19.4) / 0160 (74.8) / 35 (16.4) / 2 (0.9)White / Asian / Black Race — n (%) 01 (0.5)American Indian or Alaska Native 11 (5.1) / 015 (7.0) / 1 (0.5)Not reported / Unknown 110 (50.9) 107 (50) Primary myelofibrosis Myelofibrosis subtype — n (%) 53 (24.5) 45 (21) Post-polycythemia vera myelofibrosis 53 (24.5) 62 (29) Post-essential thrombocytopenia myelofibrosis 127 (58.8) 128 (59.8) Intermediate-1 Dynamic International Prognostic Scoring System — n (%) 74 (34.3) 75 (35) Intermediate-2 15 (6.9) 11 (5.1) High-risk 122 (64.6) 125 (67.2) JAK2 V617F Mutations — n (%)* 50 (26.5) 45 (24.2) CALR 13 (6.9) 11 (5.9) MPL 5 (2.6) 8 (4.3) Triple negative 88 (46.6 )72 (38.7) High-molecular risk mutations 27 (12.5 )28 (13.1 )Missing 11.0 (6.7–17.9)10.9 (5.8–18.0)Median (range) Hemoglobin — g/dL 76 (35.2) 70 (32.7) ≤10 — n (%) 287 (66, 1084)285 (99, 1303)Median (min, max) Platelets — × 109/L 157 (72.7) 154 (72) >200 × 109/L — n (%) 0.8 (1.25)‡0.8 (1.18)†Mean (SD)Peripheral blasts 25 (12) 35 (16) Requiring RBC transfusion at baselineRBC transfusions — patient n (%) 109 (50.5) 107 (50) 0 ECOG performance status — n (%) 95 (44.0) 97 (45.3) 1 10 (4.6) 10 (4.7) ≥2 2 (0.9)0Missing 1382.97 (277.87–5540.45)1308.89 (200.24–7117.03)Median spleen volume (range) — ccSpleen volume (central read)§ 24.7 (9.0–68.4)26.6 (7.3–66.4)Median total symptom score (range)Total symptom score¶ Data cut off: August 31, 2023. CALR, calreticulin; ECOG, Eastern Cooperative Oncology Group; JAK, Janus kinase; max, maximum; min, minimum; MPL, MPL proto-oncogene, thrombopoietin receptor; RBC red blood cell; SD, standard deviation. *Results do not originate from a validated programming environment. †n=208. ‡n=207. §Randomization of patients was based on local read. ¶Patients with baseline TSS values of <10 have at least 2 individual symptoms score ≥ 3 at baseline.

Rampal R, et al. ASH 2023. Oral 628 Pelabresib (CPI-0610) is an investigational new drug and has not been approved by any regulatory authority 14 Significantly greater response in patients treated with pelabresib + ruxolitinib vs placebo + ruxolitinib p-value Placebo + ruxolitinib (N=216) Pelabresib + ruxolitinib (N=214) 35.2% 65.9%SVR35 at Week 24 <0.00130.4 (21.6, 39.3)Difference† (95% CI) ITT population Data cut off: August 31, 2023. CI, confidence interval; ITT, intent-to-treat; SVR35, ≥35% reduction in spleen volume. Spleen volume assessed by central read. *Waterfall plots represent patients who have baseline and Week 24 data. †Calculated by stratified Cochran–Mantel–Haenszel test; ‡Patients without Week 24 assessment are considered non-responders. MANIFEST-2 study achieved its primary endpoint: SVR35 at Week 24 -30.6 (n=183)-50.6 (n=171) Mean % change in spleen volume at Week 24‡ -33.7, -27.5-53.2, -4895% CI 50 0 -50 -100 SVR35 35% reduction % c h an g e in s p le e n v o lu m e f ro m b a se lin e Pelabresib + ruxolitinib (n=171*) Placebo + ruxolitinib (n=183*)

Rampal R, et al. ASH 2023. Oral 628 Pelabresib (CPI-0610) is an investigational new drug and has not been approved by any regulatory authority TSS50 Limits Detection of Symptom Benefit, Absolute Change More Comprehensive View of Symptom Improvement 15 -70 -60 -50 -40 -30 -20 -10 0 P e rc e n tC h a n g e in T S S a t w e e k 2 4 • Continuous TSS change will detect the difference between the arms in ALL 3 situations • TSS50 will only be able to detect a difference between the arms in Situation 2 N o n -R es p o n d er R esp o n d er 3 POSSIBLE SITUATIONS OF PERCENT CHANGE IN TSS IN TREATMENT VS. CONTROL ARM Situation 1 Situation 2 Situation 3 CONCLUSIONS: Treatment arm Control arm

Rampal R, et al. ASH 2023. Oral 628 Pelabresib (CPI-0610) is an investigational new drug and has not been approved by any regulatory authority Absolute TSS at Week 24 16 Data cut off: August 31, 2023. ANCOVA, analysis of covariance; CI, confidence interval; ITT, intent-to-treat; TSS, total symptom score. *Waterfall plots represent patients who have baseline and Week 24 data. †Change from baseline determined by ANCOVA model using Multiple Imputation. ‡Least square mean difference from ANCOVA model using baseline DIPSS, baseline platelet count and baseline spleen volume as factors, and baseline TSS as covariate.  Absolute change in TSS is a continuous endpoint that estimates magnitude of symptom burden reduction with enhanced precision Strong numerical improvements for patients treated with pelabresib + ruxolitinib vs placebo + ruxolitinib p-value Placebo + ruxolitinib (N=216) Pelabresib + ruxolitinib (N=214) -14.05-15.99 TSS change† from baseline at Week 24 0.0545 -1.94 (-3.92, 0.04) Mean difference‡ (95% CI) ITT population 20 0 -20 -40 -60M ea n a b so lu te c h an g e in T S S f ro m b a se lin e Pelabresib + ruxolitinib (n=175*) Placebo + ruxolitinib (n=182*)

Rampal R, et al. ASH 2023. Oral 628 Pelabresib (CPI-0610) is an investigational new drug and has not been approved by any regulatory authority TSS50 Response at Week 24 17 Data cut off: August 31, 2023. CI, confidence interval; ITT, intent-to-treat; TSS, total symptom score; TSS50, ≥50% reduction in total symptom score. Patients are evaluable for TSS50 at Week 24 if they have had Week 24 TSS assessment by the data cutoff date or discontinued without Week 24 assessment at any time. *Waterfall plots represent patients who have baseline and Week 24 data. †Difference in treatment groups analyzed by stratified Cochran–Mantel–Haenszel test (weighted 95% CI adjusted across strata). Pelabresib + ruxolitinib (n=184*) Placebo + ruxolitinib (n=193*) p-value Placebo + ruxolitinib (N=216) Pelabresib + ruxolitinib (N=214) 46.3%52.3%TSS50 at Week 24 0.2166.0 (-3.5, 15.5)Difference† (95% CI) ITT population Numerically greater in patients treated with pelabresib + ruxolitinib vs placebo + ruxolitinib % c h an g e in T S S f ro m b as el in e 200 150 100 50 0 -50 -100 TSS50 50% reduction

Rampal R, et al. ASH 2023. Oral 628 Pelabresib (CPI-0610) is an investigational new drug and has not been approved by any regulatory authority TSS Domains at Week 24 18 Data cut off: August 31, 2023. CI, confidence interval; ITT, intent-to-treat; TSS, total symptom score; TSS50, ≥50% reduction in total symptom score. Patients are evaluable for TSS50 at Week 24 if they have had Week 24 TSS assessment by the data cutoff date or discontinued without Week 24 assessment at any time. †Difference in treatment groups analyzed by stratified Cochran–Mantel–Haenszel test (weighted 95% CI adjusted across strata). Pelabresib + ruxolitinib Placebo + ruxolitinib p-value Placebo + ruxolitinib (N=216) Pelabresib + ruxolitinib (N=214) 46.3%52.3%TSS50 at Week 24 0.2166.0 (-3.5, 15.5)Difference† (95% CI) ITT population Numerically greater in patients treated with pelabresib + ruxolitinib vs placebo + ruxolitinib with benefit balanced across all TSS domains -47.46 -39.51 -53.27 -43.19 -56.48 -52.27 -38.55 -31.05 -35.20 -45.18 -36.31 -41.37 -50.45 -34.9 M e an ( S D ) % c h an g e fr o m b a se li n e a t W ee k 24 0 25 50 100 Bone pain Fullness after eating Pain under left rib Abdominal discomfort Itching Night sweats Fatigue 75 192184178165168162191182176171162163191n= 178 175

Rampal R, et al. ASH 2023. Oral 628 Pelabresib (CPI-0610) is an investigational new drug and has not been approved by any regulatory authority Dual SVR35 / TSS50 Responders at Week 24 19 Two-fold increase in patients achieving both SVR35 and TSS50 with pelabresib + ruxolitinib vs placebo + ruxolitinib Placebo + ruxolitinib (N=216) TSS50 response: 112 patients (52.3%) Pelabresib + ruxolitinib (N=214) Both SVR35 and TSS50: n=86 40.2% Both SVR35 and TSS50: n=40 18.5% SVR35 response: 76 patients (35.2%) TSS50 response: 100 patients (46.3%) Only TSS50: n=26 12.1% Only SVR35: n=55 25.7% Only TSS50: n=60 27.8% Only SVR35: n=36 16.7% SVR35 response: 141 patients (65.9%) Data cut off: August 31, 2023. N, number of patients; SVR35, ≥35% reduction in spleen volume; TSS50, ≥50% reduction in total symptom score. Diagrams are not drawn to scale.

Rampal R, et al. ASH 2023. Oral 628 Pelabresib (CPI-0610) is an investigational new drug and has not been approved by any regulatory authority Prespecified Subgroup Analyses at Week 24 20 Data cut off: August 31, 2023. CI, confidence interval; DIPSS, Dynamic International Prognostic Scoring System; MF, myelofibrosis; PET-MF, post-essential thrombocythemia myelofibrosis; PMF, primary myelofibrosis; PPV-MF, post-polycythemia vera myelofibrosis; Resp, number of responders; SVR35, ≥35% reduction in spleen volume; TSS, total symptom score. *Number of patients with Week 24 observations. SVR35 response consistently higher in pelabresib + ruxolitinib vs placebo + ruxolitinib across all predefined subgroups Pelabresib + ruxolitinib (N=214) Placebo + ruxolitinib (N=216) (95% CI)Rate (%)Resp (64.9, 80.4)72.793 (29.4, 46.2)37.848 (43.4, 65.9)54.741 (23.0, 44.6)33.825 (30.8, 89.1)63.67 (4.3, 48.1)20.03 (56.4, 74.4)65.470 (24.0, 41.5)32.736 (65.6, 89.9)77.835 (28.2, 54.8)41.522 (45.8, 70.3)58.136 (21.2, 46.7)34.018 (59.6, 83.8)71.738 (20.3, 44.1)32.219 (56.6, 71.4)64.0103 (28.8, 43.8)36.357 1009080706050403020100 SVR35 (%) (95% CI) Change from baseline N* (17.88, 13.0)15.44113 (15.76, 11.11)13.44112 (21.77, 13.29)17.5355 (14.83, 8.99)11.9158 (24.21, 0.80)12.507 (25.47, 8.46)16.9612 (18.85, 12.73)15.7988 (15.40, 10.58)12.9992 (22.77, 14.99)18.8839 (19.88, 11.47)15.6848 (18.12, 9.84)13.9848 (13.69, 7.82)10.7542 (19.04, 12.25)15.6543 (19.04, 13.22)16.1348 (18.63, 13.55)16.09132 (14.28, 9.98)12.13134 302520151050 TSS improvement (absolute change) DIPSS: Intermediate-1 risk DIPSS: Intermediate-2 risk DIPSS: High risk MF subtype: PMF MF subtype: PPV-MF MF subtype: PET-MF Baseline spleen volume: ≥1800 cm3 Baseline spleen volume: <1800 cm3

Rampal R, et al. ASH 2023. Oral 628 Pelabresib (CPI-0610) is an investigational new drug and has not been approved by any regulatory authority Prespecified Hematologic Subgroup Analyses at Week 24 21 Data cut off: August 31, 2023. CI, confidence interval; Resp, number of responders; SVR35, ≥35% reduction in spleen volume; TSS, total symptom score. *Number of patients with Week 24 observations. SVR35 response consistently higher in pelabresib + ruxolitinib combination vs placebo + ruxolitinib across hematologic subgroups (95% CI)Rate (%)Resp (62.7, 77.6)70.1101 (26.4, 42.1)34.348 (45.5, 68.7)57.140 (26.0, 47.7)36.828 (63.6, 78.0)70.8109 (32.5, 47.8)40.163 (40.7, 66.0)53.332 (11.5, 32.6)22.013 Baseline hemoglobin: >10 g/dL Baseline hemoglobin: ≤10 g/dL Baseline platelet count: >200 × 109/L Baseline platelet count: 100–200 × 109/L 1009080706050403020100 SVR35 (%) (95% CI) Change from baseline N* (18.37, 13.70)16.04121 (15.85, 11.30)13.57121 (20.21, 11.51)15.8654 (15.21, 9.60)12.4061 (17.67, 13.13)15.40132 (15.53, 11.31)13.42138 (22.68, 12.86)17.7743 (15.67, 9.22)12.4444 2520151050 TSS improvement (absolute change) Pelabresib + ruxolitinib (N=214) Placebo + ruxolitinib (N=216)

High-Risk Patient SVR35 and TSS50 Response: Phase 2 MANIFEST Arm 3 vs. Phase 3 MANIFEST-2 22 TSS50 (24 WEEKS) SVR35 (24 WEEKS) PATIENT POPULATION (PELABRESIB + RUXOLITINIB) Phase 3 MANIFEST-2 52%66%All Patients (N = 214) 21%64%High-Risk DIPSS (N = 11) Phase 2 MANIFEST Arm 3 56%68%All Patients (N = 84) 85%54%High-Risk DIPSS (N = 13) Symptom response seen in the high-risk patient group (5% of pelabresib/ruxolitinib MANIFEST-2 arm) is a numerical anomaly Mascarenhas J, et al. J Clin Oncol. 2023;41(32): 4993-5004; Rampal R, et al. ASH 2023. Oral 628 Pelabresib (CPI-0610) is an investigational new drug and has not been approved by any regulatory authority

Rampal R, et al. ASH 2023. Oral 628 Pelabresib (CPI-0610) is an investigational new drug and has not been approved by any regulatory authority Hemoglobin Response 23 Preliminary Analyses from Data cut off: August 31, 2023. CI, confidence interval; RBC, red blood cell. *Hemoglobin response is defined as a ≥1.5 g/dL mean increase in hemoglobin from baseline in the absence of transfusions during the previous 12 weeks. Baseline hemoglobin defined as the last assessment prior to or on Cycle 1 Day 1, regardless of blood transfusions. A similar effect was observed across DIPSS categories. Placebo + ruxolitinib (N=216) Pelabresib + ruxolitinib (N=214) 5.6% (2.50, 8.61) 9.3% (5.45, 13.25) Hemoglobin response* ≥1.5 g/dL mean increase (95% CI) 25 (11.6)35 (16.4) Patients requiring RBC transfusion during screening, n (%) 89 (41.2)66 (30.8) Patients requiring RBC transfusion during first 24 weeks of study treatment, n (%) ITT population A numerically greater proportion of patients achieved hemoglobin response with pelabresib + ruxolitinib vs placebo + ruxolitinib 110 100 90 184185186189193199209204212 Pelabresib + ruxolitinib 196199204205207209211206214 Placebo + ruxolitinib Pelabresib + ruxolitinib (N=214) Placebo + ruxolitinib (N=216) 105 115 95M e a n o f h e m o g lo b in ( g /L ) Number of patients

Rampal R, et al. ASH 2023. Oral 628 Pelabresib (CPI-0610) is an investigational new drug and has not been approved by any regulatory authority Reduction in Bone Marrow Fibrosis and Inflammatory Cytokines Improvement of reticulin fibrosis grade in central read by Week 24 Preliminary Analyses from Data cut off: August 31, 2023. IL-6, interleukin 6; IL-8, interleukin 8; NF𝜅B, Nuclear factor kappa-light-chain-enhancer of activated B cells; TNF, tumor necrosis factor. *n=203 evaluable patients (baseline & C9D1). †NF𝜅B - set includes: B2M, CRP, CD40-L, HEPCIDIN, IL-6, IL-12p40, MIP-1 BETA, MPIF-1, RANTES, TNFR2, TNF alpha, VCAM-1. Reduction of inflammatory cytokines by Week 24 Pelabresib + ruxolitinib (N=214) Placebo + ruxolitinib (N=216) 24 Odds ratio Placebo + ruxolitinib Pelabresib + ruxolitinib 0.47 (0.23-0.92) 28.316.3Worsened ≥1 grade (%) 2.09 (1.14-3.93) 24.238.5Improved ≥1 grade (%) 38.5% improved 16.3% worsened 45.2% unchanged Pelabresib + ruxolitinib (n=104*) 24.2% improved 28.3% worsened 47.5% unchanged Placebo + ruxolitinib (n=99*) 6040200204060 Mean change from baseline (%) Mean reduction (95% CI) n 33.1 (35.9, 30.2) 161 19.1 (22.1, 15.9) 179 35.5 (44.7, 24.8) 141 10.9 (23.7, -2.7) 153 8.8 (17.2, -0.5) 139 -35.3 (-20.9, -51.3) 153 42.4 (46, 38.6) 141 23.6 (28.1, 18.9) 151 NFkB – set† IL-6 IL-8 TNF alpha Reduction in inflammatory cytokines Increase in inflammatory cytokines

Rampal R, et al. ASH 2023. Oral 628 Pelabresib (CPI-0610) is an investigational new drug and has not been approved by any regulatory authority Summary of Safety 25 The safety profile of the pelabresib + ruxolitinib combination was consistent with prior trials Any grade Grade ≥3 Associated with pelabresib or placebo discontinuation Associated with pelabresib or placebo dose reduction Associated with pelabresib or placebo interruption Associated with death TEAE, % 2.4 23.1 32.1 47.6 32.5 9.9 12.3 29.7 49.1 96.7 050100 2.8 16.4 22.9 41.6 29 6.5 7.9 29.4 57.5 97.2 50 100 Associated with ruxolitinib dose reduction Associated with ruxolitinib interruption Preliminary Analyses from Data cut off: August 31, 2023. TEAE, treatment-emergent adverse event; SAE, serious adverse event. *Safety population: received at least one dose of study drug. TEAEs are regardless of relationship to study drug. A TEAE for the double-blinded treatment period is defined as an adverse event that has a start date on or after the first dose of the pelabresib/placebo and before 30 days after the last dose of pelabresib/placebo or before the start of alternative (off-study) treatment for MF, whichever occurs first. MF, myelofibrosis. SAEs Associated with ruxolitinib discontinuation Pelabresib + ruxolitinib (N=212) Placebo + ruxolitinib (N=214) Safety population*

Rampal R, et al. ASH 2023. Oral 628 Pelabresib (CPI-0610) is an investigational new drug and has not been approved by any regulatory authority Treatment-Emergent Adverse Events 26 13.1 15.9 10.7 8.9 16.8 13.6 11.2 15 24.3 3.7 18.7 15.9 23.4 55.6 9 11.3 11.3 11.3 11.8 11.8 12.7 14.2 18.4 18.4 23.1 20.8 32.1 43.9 0.5 0 0.5 0 0.5 0.5 0 0.5 0 0.5 0.5 4.2 9 23.1 0.9 1.9 0 0 0.9 0 0 0 0 0 1.4 0.9 5.6 36.4 % TEAEs of all grades that occurred in ≥10% of patients Safety population* Anemia Thrombocytopenia Diarrhea Platelet count decreased† Dysgeusia Constipation Nausea Cough Asthenia Fatigue Dizziness Headache COVID-19 Hematologic events Non-hematologic events Dyspnea Preliminary Analyses from Data cut off: August 31, 2023. TEAE, treatment-emergent adverse event. *Safety population: received at least one dose of study drug. † Platelet count decreased was classified under the system organ class of investigation. TEAEs are regardless of relationship to study drug. A TEAE for the double-blinded treatment period is defined as an adverse event that has a start date on or after the first dose of the pelabresib/placebo and before 30 days after the last dose of pelabresib/placebo or before the start of alternative (off-study) treatment for MF, whichever occurs first. MF, myelofibrosis; COVID-19, coronavirus disease 2019. Pelabresib + ruxolitinib (N=212) Placebo + ruxolitinib (N=214) % Grade ≥3 % Grade ≥3 Adverse events of anemia were reported less frequently with pelabresib + ruxolitinib combination than with placebo + ruxolitinib; no new safety signals were observed 100 50 0 10050

Rampal R, et al. ASH 2023. Oral 628 Pelabresib (CPI-0610) is an investigational new drug and has not been approved by any regulatory authority Conclusions 27  Pelabresib in combination with ruxolitinib compared with placebo in combination with ruxolitinib in JAK inhibitor treatment-naïve patients at Week 24: – Significantly reduced splenomegaly (SVR35: 66% vs 35%; p<0.001) – Demonstrated strong trends in reducing the mean absolute TSS (p=0.0545) and improving TSS50 response – Doubled the percentage of patients with dual SVR35 / TSS50 response  Fewer anemia adverse events, higher rates of hemoglobin responses and fewer patients with transfusion requirement  The safety profile appeared generally comparable to the established safety profile of ruxolitinib with fewer grade ≥ 3 events  Pelabresib in combination with ruxolitinib showed reduction of pro-inflammatory cytokines, and improvement in bone marrow fibrosis and anemia response, addressing the four hallmarks of myelofibrosis JAK, Janus kinase; SVR35, ≥35% reduction in spleen volume; TSS50, ≥50% reduction in total symptom score. These results support a potential paradigm shift in the treatment of patients with myelofibrosis

TIM DEMUTH, M.D., Ph.D. Chief Research & Development Officer, MorphoSys Pelabresib First-line Myelofibrosis Clinical Development Next Steps 04 © MorphoSys – ASH 2023 MANIFEST-2 Investor Event – December 2023

Majority of U.S. Physicians View Combination Therapy as the “Way of the Future” in Myelofibrosis 29 MF Drivers and Barriers Qualitative Market Research, Aug 2023 | N=23 MF treating US Hem Oncs & Med Oncs; Product attributes rated based on Target Product Profile for pelabresib OPEN TO UTILIZE (87%) HESITANT TO UTILIZE (13%) MAJORITY IMPRESSED BY THE IMPROVED EFFICACY OF COMBINATION THERAPY PELABRESIB RANKED AMONG THE HIGHEST IN TOP ATTRIBUTES DRIVING TREATMENT DECISIONS IMPRESSIVE EFFICACY (Spleen Volume Reduction, Symptom Improvement) Mentioned by ~85% of HCPs HEMATOLOGIC FUNCTION (Transfusion Dependency, Hemoglobin Count, Quality of Life) Mentioned by ~70% of HCPs LOW RATES OF HEMATOLOGIC ADVERSE EVENTS (Anemia, Thrombocythemia, Neutropenia) Mentioned by ~70% of HCPs © MorphoSys – ASH 2023 MANIFEST-2 Investor Event – December 2023

Execution and Next Steps of Pivotal MANIFEST-2 Results © MorphoSys – ASH 2023 MANIFEST-2 Investor Event – December 2023 30 • Collect longer-term data, including quality of life and duration of treatment • Leverage experienced U.S. Medical Science Liaison team with established physician relationships Prepare and File Regulatory Submissions Advance Scientific Publications and Medical Education • Intend to file for approval in U.S. and Europe in mid-2024 • Submit comprehensive MANIFEST-2 data package

MANIFEST-2 demonstrated clear benefits across the four hallmarks, including a significant reduction in spleen size – a key finding given the known association between spleen volume reduction and patient survival. “ “ RAAJIT K. RAMPAL, M.D., PH.D. Director, Center for Hematologic Malignancies, and Director, Myeloproliferative Neoplasms Program, Memorial Sloan Kettering Cancer Center Committed to Bringing Pelabresib to Myelofibrosis Patients in Dire Need Of New Treatment Options © MorphoSys – ASH 2023 MANIFEST-2 Investor Event – December 2023 31 The combination of pelabresib and ruxolitinib, for the first time demonstrates, with strong clinical data, a potential paradigm shift to combination therapy. “ “ JOHN MASCARENHAS, M.D. Director of the Adult Leukemia Program at The Tisch Cancer Institute at Mount Sinai, New York

PROFESSOR CLAIRE HARRISON Q&A 05 RUBEN MESA, M.D., FACP TIM DEMUTH, M.D., Ph.D. JEAN-PAUL KRESS, M.D. LUCINDA CRABTREE, Ph.D. © MorphoSys – ASH 2023 MANIFEST-2 Investor Event – December 2023