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UNITED STATES
SECURITIES AND EXCHANGE COMMISSION
WASHINGTON, D.C. 20549
FORM 8-K
CURRENT REPORT
Pursuant to Section 13 or 15(d)
of the Securities Exchange Act of 1934
Date of Report (Date of earliest event reported): December 9, 2024
Vor Biopharma Inc.
(Exact name of registrant as specified in its Charter)
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Delaware |
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001-39979 |
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81-1591163 |
(State or Other Jurisdiction of Incorporation) |
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(Commission File Number) |
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(IRS Employer Identification No.) |
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100 Cambridgepark Drive |
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Suite 101 |
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Cambridge, Massachusetts |
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02140 |
(Address of Principal Executive Offices) |
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Registrant’s telephone number, including area code: (617) 655-6580
(Former Name or Former Address, if Changed Since Last Report)
Check the appropriate box below if the Form 8-K filing is intended to simultaneously satisfy the filing obligation of the registrant under any of the following provisions (see General Instructions A.2. below):
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Written communications pursuant to Rule 425 under the Securities Act (17 CFR 230.425) |
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Soliciting material pursuant to Rule 14a-12 under the Exchange Act (17 CFR 240.14a-12) |
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Pre-commencement communications pursuant to Rule 14d-2(b) under the Exchange Act (17 CFR 240.14d-2(b)) |
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Pre-commencement communications pursuant to Rule 13e-4(c) under the Exchange Act (17 CFR 240.13e-4(c)) |
Securities registered pursuant to Section 12(b) of the Act:
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Title of each class |
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Trading Symbol(s) |
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Name of each exchange on which registered |
Common Stock, $0.0001 par value per share |
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VOR |
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Nasdaq Global Select Market |
Indicate by check mark whether the registrant is an emerging growth company as defined in Rule 405 of the Securities Act of 1933 (§230.405 of this chapter) or Rule 12b-2 of the Securities Exchange Act of 1934 (§240.12b-2 of this chapter).
Emerging growth company ☒
If an emerging growth company, indicate by check mark if the registrant has elected not to use the extended transition period for complying with any new or revised financial accounting standards provided pursuant to Section 13(a) of the Exchange Act. ☐
Item 7.01 Regulation FD Disclosure
On December 9, 2024, Vor Biopharma Inc. (the “Company”) issued a press release announcing updated clinical data, which was presented in a poster at the American Society of Hematology (“ASH”) Annual Meeting & Exposition held on December 8, 2024 and posted to the Company’s website on December 8, 2024 prior to the presentation. In connection with the announcement, the Company will host a call and webcast on December 9, 2024 at 8:00 a.m. ET. Call details are contained in the press release referenced above. Accompanying slides may be accessed through the “Investors” section of the Company’s website at www.vorbio.com. A copy of the press release is attached hereto as Exhibit 99.1 and a copy of these slides is attached hereto as Exhibit 99.2, and each is incorporated herein by reference.
The information furnished under this Item 7.01, including Exhibits 99.1 and 99.2, shall not be deemed “filed” for purposes of Section 18 of the Securities Exchange Act of 1934, as amended, or subject to the liabilities of that section or Sections 11 and 12(a)(2) of the Securities Act of 1933, as amended. The information in this Item 7.01, including Exhibits 99.1 and 99.2, shall not be deemed incorporated by reference into any other filing with the U.S. Securities Exchange Commission made by the Company, whether made before or after the date hereof, regardless of any general incorporation language in such filing.
Item 8.01 Other Events
On December 9, 2024, the Company announced updated clinical data from its ongoing Phase 1/2 VBP101 study of patients with relapsed/refractory AML receiving trem-cel followed by MylotargTM. The data included 25 patients treated with trem-cel, of which 15 had received Mylotarg (six at the 2 mg/m2 dose) as of the data cut-off date of November 1, 2024. The data demonstrated:
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Preliminary evidence of improved relapse-free survival (median RFS not reached with median follow-up duration of 7.4 months) compared to published groups of AML patients at high risk of relapse post hematopoietic stem cell transplant (HCT). |
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Shielding of the blood system, with maintained neutrophil and platelet counts across multiple Mylotarg doses of 0.5, 1, and 2 mg/m2. |
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Broadened therapeutic index for Mylotarg when administered after trem-cel. |
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Reliable engraftment, with 100% of patients achieving primary neutrophil engraftment (median 9.5 days), robust platelet recovery (median 16 days), and full myeloid donor chimerism at Day 28. |
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Trem-cel continues to be manufactured with high CD33 editing efficiency (median 90%, range 71-94%). |
The Company also announced that it received supportive feedback from the Food and Drug Administration (“FDA”) in a Type C meeting. Specifically, there was alignment with the trem-cel + Mylotarg registrational clinical trial design with respect to study population, control arm, primary endpoint, stratification factors, and statistical design. The Company agreed to provide further updates to the FDA alongside submission of the full clinical trial protocol.
Item 9.01 Financial Statements and Exhibits
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 hereunto duly authorized.
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Vor Biopharma Inc. |
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By: |
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/s/ Robert Ang |
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Robert Ang |
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Chief Executive Officer |
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Date: December 9, 2024 |
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Exhibit 99.1
Vor Bio Provides Clinical Update Further Validating Approach of Using Shielded Transplants to Deliver
Targeted Therapies; Receives Supportive Feedback from FDA Regarding Registrational Trial Design
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Preliminary data suggests improved relapse-free survival compared to published groups of acute myeloid
leukemia (AML) patients at high risk of relapse post-transplant |
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Trem-cel + Mylotarg continue to demonstrate engraftment, shielding,
and broadened therapeutic window |
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Company has received supportive feedback from the FDA regarding a registrational clinical trial design
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CAMBRIDGE, Mass., December 9, 2024 (GLOBE NEWSWIRE) Vor Bio (Nasdaq: VOR), a clinical-stage cell and genome engineering
company, today announced updated clinical data from its ongoing Phase 1/2 VBP101 study of patients with relapsed/refractory AML receiving trem-cel followed by MylotargTM. The data, which was presented in a poster at the American Society of Hematology (ASH) Annual Meeting on Sunday, December 8th, demonstrated
durable engraftment, shielding from Mylotarg on-target toxicity, a broadened Mylotarg therapeutic window, and early evidence of improved relapse free survival compared to published high-risk AML comparators.
With additional maturity, we are even more encouraged by this data and the potential of offering AML and MDS patients the opportunity to receive
post-transplant maintenance therapy while still maintaining healthy blood count levels, said Dr. Eyal Attar, Vor Bios Chief Medical Officer.
The data released today included 25 patients treated with trem-cel of which 15 had received Mylotarg (six at the
2 mg/m2 dose) as of the data cut-off date of November 1, 2024. The data demonstrated:
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Preliminary evidence of improved relapse-free survival (median RFS not reached with median follow-up duration of 7.4 months) compared to published groups of AML patients at high risk of relapse post hematopoietic stem cell transplant (HCT)1.
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Shielding of the blood system, with maintained neutrophil and platelet counts across multiple Mylotarg doses of
0.5, 1, and 2 mg/m2. |
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Broadened therapeutic index for Mylotarg when administered after
trem-cel. |
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Reliable engraftment, with 100% of patients achieving primary neutrophil engraftment (median 9.5 days), robust
platelet recovery (median 16 days), and full myeloid donor chimerism at Day 28. |
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Trem-cel continues to be manufactured with high CD33 editing efficiency
(median 90%, range 71-94%). |
Company received supportive feedback from the FDA in a Type C
meeting
The Company had the opportunity to interact with the FDA regarding data from the trem-cel +
Mylotarg study alongside a proposed registrational clinical trial synopsis. The FDA agreed that trem-cel engrafts neutrophils and platelets and has a similar safety profile to unedited CD34+ grafts. In
addition, there was agreement with the trem-cel + Mylotarg registrational clinical trial design with respect to study population, control arm, primary endpoint, stratification factors, and statistical design.
The Company agreed to provide further updates to the FDA alongside submission of the full clinical trial protocol.
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Araki et al. JCO 2016; Jentzsch et al. Blood Cancer Journal 2022. |
Conference Call & Webcast Information
Vor Bio management, joined by Guenther Koehne, MD, PhD, an investigator on the VBP101 study and Deputy Director and Chief of Blood &
Marrow Transplant and Hematologic Oncology at Miami Cancer Institute of Baptist Health South Florida, will host a live webcast
today at
5:00 AM PT / 8:00 AM ET.
Listeners can register for the webcast via this LINK
Analysts wishing to participate in the Q&A session should use this LINK
A replay of the webcast will be available via the investor section of the Companys website
at www.vorbio.com approximately two hours after the calls conclusion.
About Vor Bio
Vor Bio is a clinical-stage cell and
genome engineering company that aims to change the standard of care for patients with blood cancers by engineering hematopoietic stem cells to enable targeted therapies post-transplant. For more information, visit: www.vorbio.com.
Forward-Looking Statements
This press release
contains forward-looking statements within the meaning of the Private Securities Litigation Reform Act of 1995. The words aim, anticipate, can, continue, could, design,
enable, expect, initiate, intend, may, on-track, ongoing, plan, potential, should,
target, update, will, would, and similar expressions are intended to identify forward-looking statements, although not all forward-looking statements contain these identifying words. Forward-looking
statements in this press release include Vor Bios statements regarding the potential of its product candidates to positively impact quality of life and alter the course of disease in the patients it seeks to treat, including potential
improvements in relapse-free survival, the timing of initiation of clinical trials, the potential of trem-cel to enable targeted therapies in the post-transplant setting including Mylotarg and CD33-targeted CAR-Ts while maintaining healthy blood count levels and change the standard of care for patients with blood cancers, the safety profile of trem-cel plus Mylotarg, the
potential design of a registrational trial for trem-cel and plans for regulatory submissions for trem-cel. Vor Bio may not actually achieve the plans, intentions, or
expectations disclosed in these forward-looking statements, and you should not place undue reliance on these forward-looking statements. Actual results or events could differ materially from the plans, intentions and expectations disclosed in these
forward-looking statements as a result of various factors, including: uncertainties inherent in the initiation and completion of preclinical studies and clinical trials and clinical development of Vor Bios product candidates; availability and
timing of results from preclinical studies and clinical trials; whether interim results from a clinical trial will be predictive of the final results of the trial or the results of future trials; uncertainties regarding regulatory approvals to
conduct trials or to market products; the success of Vor Bios in-house manufacturing capabilities and efforts; and availability of funding sufficient for its foreseeable and unforeseeable operating
expenses and capital expenditure requirements and Vor Bios ability to continue as a going concern. These and other risks are described in greater detail under the caption Risk Factors included in Vor Bios most recent annual
or quarterly report and in other reports it has filed or may file with the Securities and Exchange Commission. Any forward-looking statements contained in this press release speak only as of the date hereof, and Vor Bio expressly disclaims any
obligation to update any forward-looking statements, whether because of new information, future events or otherwise, except as may be required by law.
Contact:
Investors & Media
Sarah Spencer
+1 857-242-6076
sspencer@vorbio.com
Exhibit 99.2 Ambition: Curing Blood Cancers through cell and genome
engineering 1 December 2024
Disclaimer This presentation (the “Presentation”) contains
forward-looking statements within the meaning of the Private Securities Litigation Reform Act of 1995 about Vor Biopharma Inc. (“Vor,” “Vor Bio” or the “Company”). The words “aim,”
“anticipate,” “believe,” “can,” “could,” “design,” “enable” “estimate,” “expect,” “intend,” “may,” “ongoing,”
“plan,” “potential,” “project,” “should,” “target,” “towards,” “will,” and similar expressions are intended to identify forward-looking statements, although not all
forward-looking statements contain these identifying words. Forward-looking statements in this Presentation include those regarding the potential of trem-cel, alone or as part of a treatment system, to replace standard of care, the ALLO potential of
VCAR33 and ADCs in combination with trem-cel as a treatment system, the potential of trem-cel to enable targeted therapies in the post-transplant setting including Mylotarg and CD33-targeted CAR-Ts, the approach and potential opportunities for
VADC45, potential opportunities for next-generation approaches including multi-targeted CAR-Ts and multiplex-edited grafts, the potential of Vor Bio’s platform to enable potentially curative therapies and change the standard of care in blood
cancers, the intended benefits of Vor Bio’s product candidates and approach, including the potential of trem-cel + Mylotarg to improve relapse-free survival, Vor Bio’s plans, strategies, expectations and anticipated milestones for its
preclinical and clinical programs, including the availability and timing of results from preclinical studies and clinical trials, the potential design of future clinical trials, the timing of regulatory filings, and the timing of dosing patients,
the potential design, endpoints and timing of a Phase 3 registrational trial for trem-cel, and Vor Bio’s expectations regarding expedited regulatory review of its product candidates as a result of Fast Track designation or otherwise, the
expected safety profile of Vor Bio’s product candidates, cash runway and expected capital requirements, and Vor Bio’s expectations regarding commercial opportunity, addressable patient population and reimbursement rates for its product
candidates, if approved. Vor Bio may not actually achieve the plans, intentions, or expectations disclosed in these forward-looking statements, and you should not place undue reliance on these forward-looking statements. Actual results or events
could differ materially from the plans, intentions and expectations disclosed in these forward-looking statements as a result of various factors, including: uncertainties inherent in the initiation, completion of, and availability and timing of
results from, preclinical studies and clinical trials and clinical development of Vor Bio’s product candidates; whether preclinical data or interim results from a clinical trial will be predictive of the final results of the trial or the
results of future trials; the uncertainty of regulatory approvals to conduct trials or to market products; the success of Vor Bio’s in-house manufacturing capabilities and efforts; and availability of funding sufficient for its foreseeable and
unforeseeable operating expenses and capital expenditure requirements. The interim data for trem-cel presented in this Presentation is based on eight patients and future results for these patients or additional patients may not produce the same or
consistent results. These and other risks are described in greater detail under the caption “Risk Factors” included in Vor Bio’s most recent annual or quarterly report and in other reports it has filed or may file with the
Securities and Exchange Commission. Any forward-looking statements contained in this Presentation speak only as of the date of this Presentation, and Vor Bio expressly disclaims any obligation to update any forward-looking statements, whether
because of new information, future events or otherwise, except as may be required by law. Certain information contained in this Presentation relates to or is based on studies, publications, surveys and other data obtained from third party sources
and Vor Bio’s own internal estimates and research. While we believe these third-party sources to be reliable as of the date of this Presentation, we have not independently verified, and make no representation as to the adequacy, fairness,
accuracy or completeness of, any information obtained from third party sources. In addition, there can be no guarantee as to the accuracy or reliability of any assumptions or limitations that may be included in such third-party information. While we
believe our own internal research is reliable, such research has not been verified by any independent source. All brand names or trademarks appearing in this Presentation, including Mylotarg, are the property of their respective owners. 2
Vor Bio Clinical Strategy Thesis: Trem-cel as a Therapeutic Platform
Enabling multiple targeted therapy modalities ADCs CAR-Ts Early Clinical Strategy Current Clinical Findings • Demonstrate clinical proof-of-principle Encouraging data with commercial promise with Mylotarg as approved agent Trem-cel •
100% engraftment -Engraftment of gene engineered graft + • Robust shielding of the blood system -Shielding the blood system • Broadened therapeutic index for Mylotarg Mylotarg • Most rapid path to Treatment System • Early
evidence of patient benefit (RFS) • Testing as monotherapy in post- • Encouraging biomarker data at lowest ALLO VCAR33 transplant relapse dose 3
Even After Transplant, High-Risk AML Has Poor Outcomes Transplant After
Transplant Watchful Waiting Outcomes for High-Risk Patients 100 50 Maintenance therapy unfeasible due to drug toxicity 0 0 6 12 18 24 Araki et al. JCO 2016 Months post-transplant A mainstay treatment Frequent leukemia relapses and death, poor
outcomes 4 Probability of relapse-free survival (%)
What If Shielding Could Lead to Improved Outcomes? …enabling use A
shielded … can shield …potentially leading of otherwise toxic graft… a blood system… to improved outcomes maintenance therapies… ADC CAR-T Required Shielded Graft Attributes Engraftment Therapeutic Index Reliably
reconstitute the blood system Optimize efficacy and safety of maintenance therapies Shielding Patient Benefit Protect against otherwise toxic therapies Prolong relapse-free survival 5
What is Trem-Cel? Stem cell CRISPR/Cas9 selection gene engineering
• Removes T cells to reduce • High-efficiency editing of Trem-cel: Starting Material graft-vs-host disease CD33 protein Stem Cell Graft Apheresis Product from Healthy Matched Donor Shielded from • Allows for large CD34+ dose
• Results in blood system that CD33-Targeted to accelerate engraftment is shielded from Therapy CD33-targeted therapy ~7 day manufacturing process 6
VBP101: Trem-cel Phase 1/2a Clinical Trial Engraftment Shielding Patient
Journey Transplant Decision Trem-cel Infusion Engraftment Maintenance Mylotarg Transplant-eligible Starting ~day 60 up to 8 cycles Consolidation/Salvage Conditioning AML and MDS patients 2 Dose escalation 0.5-2 mg/m at high risk of relapse No delay
in typical patient transplant process Therapeutic Patient Benefit Index Stem Cell Mobilization, Screening Collection Trem-cel Manufacturing Related Unrelated ~7-day process Unedited back-up graft 7 Donor Journey
üTherapeutic üPatient üEngraftment üShielding Index
Benefit Trem-cel Achieved Timely Engraftment Neutrophil Engraftment (n=25) Platelet Engraftment (n=25) Neutrophil Engraftment Platelet Recovery Trem-cel Trem-cel 1.0 1.0 median: median: Day 9.5 0.8 Day 16 0.8 0.6 0.6 0.4 0.4 Median engraftment for
0.2 0.2 Median recovery for unmodified CD34+ graft D11 unmodified CD34+ graft D17 0.0 0.0 0 7 14 21 28 0 7 14 21 28 Days Post Trem-cel Days Post Trem-cel High CD33 editing efficiency 100% neutrophil 100% achieved full (median 90%, range 71-94%)
engraftment myeloid chimerism at D28 Data cut-off: 1-NOV-2024 8 Neutrophil Engfraftment Platelet Recovery
üTherapeutic üPatient üEngraftment üShielding Index
Benefit Trem-cel Demonstrated Shielding Across Mylotarg Doses Neutrophil and Platelet Peripheral Blood Counts with Mylotarg Doses 2 0.5 mg/m 2 Platelets 1 mg/m 2 2 mg/m Each point indicates a Mylotarg dose 2 0.5 mg/m 2 Neutrophils 1 mg/m 2 2 mg/m
Mylotarg commonly results in severe myelosuppression and is the most clinically 1,2 significant adverse event Days from start of Mylotarg dosing 1. Sievers et al. Blood 1999 2. Mylotarg prescribing information 9 Data cut-off: 1-NOV-2024 Cell
counts/µL
üTherapeutic üPatient üEngraftment üShielding Index
Benefit Trem-cel Enabled Broadened Therapeutic Index for Mylotarg C and AUC Across Mylotarg Doses max Mylotarg Pharmacokinetic Profile Mylotarg PK analysis Mylotarg Pharmacokinetic Profile (2017, FDA ODAC) n=3 n=5 n=5 Safety threshold: probability
of veno-occlusive disease > 5% Hours post-Mylotarg infusion 2 Mylotarg first dose (mg/m ) Data cut-off: 1-NOV-2024 Approved doses 10 Anti-CD33 mAb concentration (ng/mL)
Baseline Risk Factor Demographics for AML Patients: VBP101 vs.
Comparators VBP101 AML Araki Jentzsch VBP101 AML ITT Disease Characteristic Treated with Mylotarg MRD+ Cohort (2016) Adverse Risk Cohort (2022) (n=24) (n=76) (n=271) (n=15) Cytogenetics Risk ELN 2022 Favorable 8% 13% 3% N/A Intermediate 33% 27% 58%
N/A Adverse 58% 60% 39%** 100%* Other AML Risk Factors TP53 mutation 33% 40% NR NR a Secondary AML 42% 33% 42% 49% Disease Burden Status Remission (MRDneg) 75% 73% N/A 20% MRD+ (>0.1-<5% blasts by flow) 13% 20% 100%* 13% Active disease
(≥5% blasts) 13% 7% N/A 32%*** AML Disease Status CR1 63% 60% 67% 61% CR2 25% 33% 33% 7% Relapsed or refractory 13% 7% 0 32%*** Adverse Risk Features (Adverse ELN/molecular/cytogenetic, Secondary AML, MRD or active disease, CR2 or
Relapsed/Refractory), n (%) 1 11 (46%) 6 (40%) 2 or more 13 (54%) 9 (60%) *Selected comparison cohort (n) from published studies. **Adverse cytogenetics. ***Includes partial remission, relapsed, refractory. Jentzsch values for disease burden status
do not total 100% due to data not reported. a Defined as AML with myelodysplasia-related change and therapy-related AML, NR=not reported, N/A=not applicable Data cut-off: 01-NOV-2024 11
üTherapeutic üPatient üEngraftment üShielding Index
Benefit Trem-cel+Mylotarg RFS Appears Favorable vs Published High-Risk AML Comparators Relapse-Free Survival of VBP101 (intention-to-treat) vs Araki and Jentzsch (historical controls) Median RFS P value vs Hazard HR (mo) VBP101* Ratio* (HR) 95% CI*
ITT Not reached Jentzsch 6.2 0.02 0.36 0.21-0.64 Araki 3.8 0.0004 0.23 0.14-0.40 VBP101 (n=25) Median duration of follow-up: 7.4 mo • Four relapses observed: (all CD33 positive at relapse) – 2/4 relapsed prior to Mylotarg treatment
– 3/4 transplanted with active disease; 1/4 with MRD Jentzsch (Adverse Risk EFS) (n=271) – 4/4 adverse risk cytogenetics • One patient died off-study due to complications of viral infection Araki (MRD+ PFS) (n=76) Months
post-transplant VBP101 data cut-off: 1-NOV-2024. Adapted from Fig 2B MRD+ PFS line from Araki et al. JCO 2016; Adapted from Fig 1C, ELN 2022 Adverse risk EFS line from Jentzsch et al. Blood Cancer Journal 2022. * = individual comparison to VBP101
using log-rank Mantel-Cox test. Data not from head-to-head trial. 12 Relapse-free survival (%)
Low Rate of Relapse (2/15) Among Patients Receiving Mylotarg 0 30 60 90
120 150 180 210 240 270 300 330 360 390 420 450 480 510 540 570 600 630 660 Patient withdrawal from study Engraftment Mylotarg dose Relapse CD34 boost Backup graft Off study Ongoing Long-term follow-up study Back-up graft after coronavirus Stem cell
boost for ITP Off study due to DLI use for viral infections Mylotarg not yet started due to active infection Patient Demography (n=25) Relapse prior to Mylotarg Age (years) 59 (22 – 68) Relapse prior to Mylotarg Sex Not yet eligible for
Mylotarg Female 14 (56%) Not yet eligible for Mylotarg Male 11 (44%) Not yet eligible for Mylotarg Weight (kg) 72.6 (47.9 – 120.7) Not yet eligible for Mylotarg Primary Disease Diagnosis AML 24 (96%) MDS 1 (4%) ITP: idiopathic thrombocytopenic
purpura or similar immune-mediated thrombocytopenia 13 Data cut-off: 1-NOV-2024 Not yet 2 2 2 started Untreated 2 mg/m 1 mg/m 0.5 mg/m
Any Grade Treatment Adverse Events After Receiving Mylotarg (n=15)
Adverse Event Grade 1 Grade 2 Grade 3 Grade 4 Hematologic Anemia - 1/15 (7%) 3/15 (20%) - Autoimmune hemolytic anemia - - 1/15 (7%) - Leukopenia - - 1/15 (7%) - Lymphocyte count decreased 1/15 (7%) - - - Lymphopenia - - 1/15 (7%) - Neutropenia -
2/15 (13%) 3/15 (20%) - Platelet count decreased - - 2/15 (13%) - a Thrombocytopenia - 1/15 (7%) 1/15 (7%) 1/15 (7%) Hepatobiliary b ALT increased 2/15 (13%) 1/15 (7%) - - b AST increased 1/15 (7%) - 1/15 (7%) - Biliary colic 1/15 (7%) - - - Alk
Phos increased 3/15 (20%) - - - Blood bilirubin increased 1/15 (7%) - - - LDH increased 2/15 (13%) - - - Cholecystitis - 2/15 (13%) - - c Veno-occlusive disease 1/15 (7%) - - - a Following adverse event, patient continued to receive multiple cycles
of Mylotarg b ALT/AST elevation attributed to fluconazole toxicity and resolved after discontinuation c 2 Mild grade late-onset veno-occlusive disease occurred 97 days after 0.5 mg/m Mylotarg dose. Predisposing factors included azole toxicity,
concurrent norovirus infection and gram-negative bacteremia. ALT = Alanine aminotransferase; AST = Alanine aminotransferase; Alk Phos = blood alkaline phosphatase; LDH = blood lactate dehydrogenase Data cut-off: 1-NOV-2024 14
Clinical Update Summary • Robust neutrophil engraftment, platelet
recovery and full donor myeloid chimerism • Consistent shielding from Mylotarg-related cytopenias during repeated 2 0.5, 1, and 2 mg/m doses • Immune reconstitution, multilineage chimerism, and safety profile similar to unedited
CD34-selected grafts • Broadened Mylotarg therapeutic index following trem-cel • Preliminary data suggesting improved RFS compared to published groups of AML patients at high risk of relapse post-HCT 15
Trem-cel Platform with Potential >$1B Commercial Opportunity
Transformative Treatment Opportunity to Replace Standard of Care Transplant o Shielded transplants to prevent on-target toxicity 8000 o Targeted treatments to improve relapse free survival 7000 AML MDS 6000 Concentrated Market Opportunity 5000 o
~80% of transplants in 65 US centers 4000 o ~5,000 AML & MDS transplants per year 3000 Trem-cel 3% Y-o-Y projected growth in 2000 + AML & MDS transplants Reimbursement Pathway Mylotarg 1000 o 100% cost-based reimbursement for eHSCs* 0 ®
'24 '25 '26 '27 '28 '29 '30 '31 '32 '33 o Commercial example: Omisirge at $338,000 *2020 - IPPS (Inpatient Prospective Payment System), MS DRG-014 – Section 108, stem cell acquisition & processing for allo-SCTs 16
Physician Feedback on Trem-cel + Mylotarg Value Proposition Trem-Cel +
Mylotarg SoC Transplant Perceptions of Trem-Cel • Streamlined manufacturing with consistent engraftment • Provides protection of donor cells from on-target toxicity • Positive impact on patient outcomes and reduced GvHD 22% •
Enable maintenance therapy to reduce relapse is compelling 78% Perceptions of Mylotarg • As monotherapy, concern for hepatoxicity and neutropenia Share of Eligible Transplants • With trem-cel, relative safety concerns are alleviated I
think using that [Trem-Cel + Mylotarg] would aid in the optimization of • Benefit of protection with improved RFS vs. traditional HSCT transplant outcomes and reduce relapse, which is one of the major causes for post transplant
mortality.” Hematologist-Oncologist Trinity qual/quant demand research with 12 transplant specialists (Sept ’24); shares based on low sample size and directional only 17
Potential Registrational Trial Design for Trem-cel/Mylotarg Patient
Journey AML Myeloablative Mylotarg Key Eligibility Trem-cel Potential registrational (n~80) conditioning 30d (8 cycles) Criteria endpoint: or later Relapse-free survival • 18-70 years of age (RFS) • 8/8 HLA-matched related or unrelated
donor Proposed key secondaries: • Suitable for myeloablative • GVHD-free RFS conditioning • Overall survival • CD33+ AML • cGVHD free survival • High-risk features: • Time to neutrophil – MRD+ Standard
of care AML Myeloablative engraftment – Adverse genetics (T-cell replete) (n~80) conditioning transplant – 2°AML or AML-MRC 18
Summary of FDA Response to Type C Meeting Request • Agreement
that trem-cel engrafts neutrophils and platelets and has a similar safety profile to unedited CD34+ grafts • Agreement with the trem-cel-Mylotarg registrational clinical trial design with respect to study population, control arm, primary
endpoint, stratification factors, and statistical design • Agreement to provide further updates to FDA from the VBP101 trial alongside submission of the full registrational clinical trial protocol 19
ALLO VCAR33 : CD33-Directed Healthy Donor-Derived CAR-T T cells exactly
matched to patient’s immune system ~7-day Healthy, stem-like cells more likely manufacturing to expand and less prone to exhaustion Cells harvested from Rapid process to Terminally frozen for Clinically validated construct: prior transplant
donor preserve stemness convenience NIH study using autologous cells showed 7 efficacy at 1 x 10 CAR+ cells/kg 1 (2/5 assessable pts) 1. Shah et al. ASH 2023 20
ALLO VBP301: VCAR33 Phase 1/2 Clinical Trial Patient Journey ALLO
Enroll VCAR33 Infusion Day 28 Follow-up + MRD or relapsed AML Arm A: Blasts ≥ 5% nd 2 transplant following standard or Lymphodepletion if required + Arm B: MRD trem-cel transplant 3x3 dose escalation 6 starting at 1 x 10 + CAR cells/kg Key
Endpoints Consent ALLO Collect VCAR33 01 Safety Manufacturing ~7-day process 02 Expansion, persistence 03 Disease control/response 21 Prior Transplant Donor
ALLO VCAR33 : Encouraging Signs of In Vivo Expansion Peripheral Blood
40,000 6 Kymriah: Mean CAR copies in responders; 0.2-5 x 10 CAR T cells/ kg 6 Bryanzi: Median CAR copies in responders; 100 x 10 CAR T cells (flat dose) • Dose escalation schedule: 30,000 6 15,000 - 1 x 10 CAR+ cells/kg Patient 1 Pt 1
(301-108-1001) 6 - 3 x 10 CAR+ cells/kg 7 Patient 2 Pt 2 (301-104-1001) - 1 x 10 CAR+ cells/kg 10,000 Pt 3 (301-117-1003) Patient 3 • NCI CD33CART trial (autologous) saw in vivo expansion and 2 responses out of 5 7 assessable patients at 1 x
10 CAR+ cells/kg* 5,000 * 0 01 3 7 14 21 28 42 56 70 84 98 Days Post CAR-T Infusion Days Post VCAR33 Infusion *Data from ASH 2023 Abstract: https://ash.confex.com/ash/2023/webprogram/Paper179667.html 22 *Assessment conducted after Pt 1 received stem
cell boost on Day 37 D1, D3: BLQ D7, D10: BLQ D1, D3, D7: BLQ (DNA yield was low) CD33 CAR transgene copies/µg CD33 CAR transgene copies/µg
VADC45, a Novel CD45-Targeted Antibody Drug Conjugate CD45 is highly
expressed throughout the Novel pan-CD45 heme compartment (minus mature RBCs) humanized antibody cross-reactive to NHP Clinically validated linker-payload (Immunogen, alkylating agent) DGN549 payload with cleavable linker Robust preclinical data
package Fc silencing to avoid effector function IND-enabling studies progressing to completion 23
VADC45: Potential Commercial Opportunities Treating Relapse - Heme
Malignancies Non-Chemo Conditioning - Gene Therapies • CD45 is highly expressed in AML and DLBCL • Gene therapies such as for sickle cell urgently need non-chemo conditioning agents • Target may be oncogenic, driving tissue
infiltration, high expression and poor prognosis • Could avoid oncogenicity and sterility concerns • Opportunity: R/R AML and MDS • Opportunity: SCD, TDT alternative conditioning Immune Reset - Autoimmune Diseases Epitope
Engineering - Shielded Grafts • Immune disorders that may require more holistic • Precise epitope for VADC45 has been identified reset of the entire immune system • Experiments are ongoing for epitope modification •
Holistically remove immune cell compartments which retains protein functionality • Opportunity: Refractory MS, SLE, SSc • Opportunity: Heme malignancies 24 DLBCL= Diffuse large B-cell lymphoma, TDT= Transfusion-dependent
β-thalassemia, SLE= Systemic lupus erythematosus, SSc = Systemic sclerosis
Single Dose of VADC45 Enabled Gene-edited HSC Engraftment Engraftment
and Persistence of Gene-edited Stem Cells NHPs received autologous transplantation of BCL11A- edited HSCs with conditioning via chemo (busulfan) Granulocyte Gene Editing compared to single Editing Frequency in Granulocytes dose of VADC45 100 80 60
Very high myeloid chimerism 40 achieved within days of Busulfan (QDx4) N=3 transplant 20 0.3 mg/kg VADC45 N=2 0 0 8 16 24 32 40 48 Weeks After Transplantation Persistently high edited Weeks After Transplantation populations through one year from
transplant 25 Tisdale et al. (NIH), preclinical data Overall editing efficiency (%) Overall +58 editing (%)
Single Dose of VADC45 Efficiently Depleted Immune Cells Immune Cell
Depletion from Peripheral Blood (NHP) T Cell Depletion B Cell Depletion 7 6 1x10 2.5x10 6 6 8x10 2.0x10 6 6 6x10 1.5x10 6 6 4x10 1.0x10 6 5 2x10 5.0x10 0 0.0 Pre Dose Day 13 Pre Dose Day 13 0.3 mg/kg 0.3 mg/kg Monocyte Depletion Granulocyte
Depletion 5 6 6x10 5x10 6 4x10 5 4x10 6 3x10 6 2x10 5 2x10 6 1x10 0 0 Pre Dose Day 13 Pre Dose Day 13 0.3 mg/kg 0.3 mg/kg 26 Preclinical data No. Monocytes/mL No. T cells/mL No. Granulocyte/mL No. B cells/mL
Next-Generation Approaches Expansion into Targets Beyond CD33
additional indications Avoidance of potential Multi-targeted CAR-Ts tumor escape Broader options Multiplex-edited grafts for treatment 27
In Vitro PoC for Multi-Specific CAR-T: Cell Killing and Shielding pos
pos neg neg CD33 CD33 CD33 CD33 • 2 independent T cell donors pos neg pos neg CLL-1 CLL-1 CLL-1 CLL-1 • 48h co-culture of CAR-T cells AML (HL-60) with HL60 (AML) target cells Target Cells • E:T ratio 1:1 100 Multi-Specific CAR-T
cell 80 (CD33+CLL-1) 60 • Highly effective AML target cell killing 40 • “OR gated” CAR which eliminates target cells expressing both OR one target only 20 • Highly specific CAR leaving double knock-out target cells
intact 0 • Can be paired with Multiplex (CD33+CLL-1)- wildtype CLL-1 KO CD33 KO double KO edited HSPCs which provide shielding 28 Vor internal data. UTD: untransduced T cell control, KO: knock-out Target Cell Killing (%, increase over
UTD)
Multiplex HSC Editing: Minimize Translocations Mock Minimized
Translocation + + CD33 CLL-1 0.4 Double Pos 82.6% 0.3 0.2 0.1 Base Edited - - 0 CD33 CLL-1 Simultaneous Sequential Sequential Base Editing Double KO Cas9 Cas9 Cas + Inhibitor 79.5% Genome Engineering Strategies Adapted from Precision Genome
Engineering Keystone Symposia – 2022 Poster 3002 29 Precision Genome Engineering Keystone Symposia – 2022 Poster 3001 Translocation (%)
Vor Bio Unique Approach to Potentially Cure Blood Cancers Trem-cel, a
first-in-class investigational* shielded stem cell transplant • Reliable engraftment, robust shielding of the blood system • Platform therapy addressing >$1B potential market opportunity Trem-cel + Mylotarg combination •
Broadened Mylotarg therapeutic index • Early evidence of patient benefit prolonging relapse-free survival • Supportive feedback from FDA on registrational trial design ALLO VCAR33 , differentiated transplant donor CAR-T therapy •
Encouraging signs of in vivo expansion with strong trial enrollment VADC45 • Four distinct potential commercial opportunities 30 *Potential to be first-in-class if approved
www.vorbio.com
Pipeline to Change the Standard of Care in Blood Cancers Description
Preclinical Clinical Anticipated Milestones Discovery/ IND- Phase Program / Trial Modality Indication Phase 1/2 Validation Enabling 2/3 Trem-cel + Mylotarg / Shielded CD33-deleted transplant + AML, MDS VBP101 CD33-directed ADC ALLO VCAR33 (healthy
AML transplant donor CAR-T) / post- CD33-directed transplant donor CAR-T VBP301 transplant Trem-cel + VCAR33 Shielded CD33-deleted transplant + IND filing following initial AML ALLO Treatment System CD33-directed transplant donor CAR-T trem-cel and
VCAR33 data AML, conditioning, VADC45 ADC CD45-directed ADC Finalizing IND preparedness immune reset Multi-specific CAR-T AML CD33-CLL1 Treatment System Multiplex-edited shielded transplant AML 32
Experienced Leadership Team Robert Ang, MBBS, MBA Han Choi, M.D., LL.M
Eyal Attar, MD Chief Financial Officer President and CEO Chief Medical Officer John King, MBA Tirtha Chakraborty, PhD Tania Philipp Chief Commercial Officer & Head Chief Scientific Officer Chief People Officer of Business Development David
Phillips, MBA Samir Vattompadam, MS Senior Vice President, Head of Quality Senior Vice President, Portfolio Strategy and Program Management Deep Cell & Gene Therapy Expertise 33
CD33 is Amongst Highest Quality Targets in AML Ubiquity of Antigen
Expression (Flow Cytometry) Density of Antigen Expression (QuantiBRITE) CD33 CLL-1 CD123 EMR2 EMR2 CD33 CLL-1 CD123 100 100000 80 10000 60 40 1000 20 0 100 Vor internal data 34 D = Diagnosis R = Relapse D R D R D R D R D R D R D R D R + Antigen
positivity on AML blasts (%) % Antigen on AML Blasts # of Antigens per Cell (ABC) # Antigens per cell
CD33 Negative Cells Enriched with Mylotarg Doses Data cut-off:
1-NOV-2024 35
Immune Reconstitution, Full and Sustained Myeloid Chimerism, and
CD33-negative Myeloid Cells Are Observed B-lymphoid Cell Count T-lymphoid Cell Count 1000 1000 CD3 800 750 CD4 600 CD8 500 400 250 200 0 0 D100 D180 M12 D100 D180 M12 16 7 1 n: 16 7 1 n: Time Post Transplant with Trem-cel Time Post Transplant with
Trem-cel Natural Killer Cell Count 1000 750 500 250 % CD33-Negative Analysis Drug Product* D28* D60* NGS Gene Editing 90 (78-94) n=18 94 (85-98) n=19 94 (86-97) n=16 0 Flow Cytometry N/E 93 (74-98) n=22 94 (78-99) n=19 D100 D180 M12 *Mean % (range),
Editing and flow data from peripheral blood monocytes and myeloid cells respectively n: 16 7 1 N/E: not evaluated Time Post Transplant with Trem-cel Data cut-off: 1-NOV-2024. Reference unedited CD34-selected reconstitution: Goldberg et al Leuk and
Lymph 58 (217); Llaurador et al. Transplantation and Cellular Therapy 27 (2021) 36 Absolute Number (cells/µL) Absolute Number (cells/µL) Absolute Number (cells/µL)
Risk of Veno-Occlusive Disease Related to Mylotarg C max Probability of
Veno-occlusive Disease in Patients with Prior Transplant VBP101 mean C max 2 0.5 mg/m 2 1.0 mg/m 2 2.0 mg/m C after first dose of Mylotarg (μg/mL) max Geometric mean (R/R AML) 95% CI Mylotarg ODAC 2017 37 Probability of VOD (%)
Selected Precedent Randomized Trials in AML AML Studies Transplant
Studies MORPHO SIERRA ALFA-0701 Precision-T Omidubicel 131 Gilteritinib vs I-apamistamab + Daunorubicin + Orca-T transplant vs Omidubicel vs double cord Drug and placebo Flu-TBI + alloHCT vs cytarabine ± Mylotarg SoC alloHCT graft Comparisons
conventional care (D1, 4, 7) Post-HCT maintenance, R/R AML Newly-diagnosed de Transplant-eligible AML, Transplant-eligible Treatment FLT3-ITD AML novo AML ALL, MDS high-risk malignancies Setting o RFS Rate of dCR EFS (induction failure, Survival
free of moderate- Time to neutrophil 1 Endpoint (CR/CRp ≥ 180 days) relapse, or death) to-severe chronic GVHD engraftment (cGFS) o OS (key), EFS, Time to OS, EFS Rate of CR/CRp, OS, Time to moderate-to- Platelet engraftment by 42 2 Endpoints
NRM, Relapse, GVHD, RFS, Safety severe GVHD, GRFS, OS days, grade 2-3 bacterial MRD or invasive inf, NRM, OS 178 per arm 76 per arm 140 per arm 85 per arm 62 per arm Sample Size 38
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