MNMD Mind Medicine MindMed Inc

 

 

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): January 10, 2025

 

 

Mind Medicine (MindMed) Inc.

(Exact name of Registrant as Specified in Its Charter)

 

 

British Columbia	001-40360	98-1582438
(State or Other Jurisdiction of Incorporation)	(Commission File Number)	(IRS Employer Identification No.)

 

One World Trade Center Suite 8500
New York, New York	10007
(Address of Principal Executive Offices)	(Zip Code)

 

Registrant’s Telephone Number, Including Area Code: (212) 220-6633

 

 

(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 :

 

¨

Written communications pursuant to Rule 425 under the Securities Act (17 CFR 230.425)

 

¨

Soliciting material pursuant to Rule 14a-12 under the Exchange Act (17 CFR 240.14a-12)

 

¨

Pre-commencement communications pursuant to Rule 14d-2(b) under the Exchange Act (17 CFR 240.14d-2(b))

 

¨

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:

 

Title of each class		Trading Symbol(s)		Name of each exchange on which registered
Common Shares		MNMD		The Nasdaq Stock Market LLC

 

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 x

 

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 5.02 Departure of Directors or Certain Officers; Election of Directors; Appointment of Certain Officers; Compensatory Arrangements of Certain Officers.

 

On January 10, 2025, Mind Medicine (MindMed) Inc. (the "Company") notified Miri Halperin Wernli, the Company's Executive President, that it was terminating her employment without cause, effective February 28, 2025, as the Company centralizes its management team in the United States to enhance collaboration and alignment with its strategic goals.

 

Item 8.01 Other Events.

 

On January 13, 2025, the Company posted an updated corporate presentation on its website. A copy of the presentation is filed herewith as Exhibit 99.1 and is incorporated by reference in this Item 8.01.

 

Item 9.01 Financial Statements and Exhibits.

 

Exhibit No.		Description
99.1		Corporate Presentation, dated January 13, 2025
104		Cover Page Interactive Data File (embedded within the Inline XBRL document)

 

 

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.

 

			Mind Medicine (MindeMed) Inc.
Date:	Janaury 13, 2025	By:	/s/ Robert Barrow
			Name: Robert Barrow Title: Chief Executive Officer

 

 

 Exhibit 99.1 

 

Corporate Presentation January 2025

Corporate Presentation | January 2025 This presentation (the “Presentation”) has been prepared by Mind Medicine ( MindMed ) Inc. (“ MindMed ”, the “Company”, “we”, “our” or “us) solely for informational purposes. This Presentation does not constitute an offering of , o r a solicitation of an offer to purchase, securities of MindMed and under no circumstances is it to be construed as a prospectus or advertisement or public offering of securities. Any trade ma rks included herein are the property of the owners thereof and are used for reference purposes only. Such use should not be c ons trued as an endorsement of the products or services of MindMed . Any amounts are in USD unless otherwise noted. MindMed’s securities have not been approved or disapproved by the Securities and Exchange Commission (the "SEC") or by any state, provi nc ial or other securities regulatory authority, nor has the SEC or any state, provincial or other securities regulatory authority passed on the accuracy or adequacy of this Pre sentation. Any representation to the contrary is a criminal offense. Cautionary Note Regarding Forward - Looking Statements This Presentation contains, and our officers and representatives may from time to time make, “forward - looking statements” within the meaning of applicable securities laws and are prospective in nature. Forward - looking statements are not based on historical facts, but rather on current expectations and projections about future events and are therefore subject to risks and uncertainties which could cause actua l r esults to differ materially from the future results expressed or implied by the forward - looking statements. These statements gen erally can be identified by the use of forward - looking words such as “will”, “may", “should”, “could”, “intend”, “estimate”, “plan”, “anticipate”, “expect”, “be lieve”, “potential”, “continue”, “budget”, “scheduled”, “forecasts”, “intends”, “anticipates”, “projects” or the negative the reo f or similar variations. Forward - looking statements in this Presentation include, but are not limited to, statements regarding the anticipated design, timing, progres s a nd results of our investigational programs for MM120, a proprietary, pharmaceutically optimized form of lysergide D - tartrate (including the anticipated topline readouts for the Voyage, Panorama and Emerge studies), MM402, also referred to as R( - ) - MDMA, and any other product candidates; t he success and timing of our development activities; the success and timing of our planned clinical trials; our ability to me et the milestones set forth herein; the likelihood of success of any clinical trials or of obtaining FDA or other regulatory approvals; our cash runway f und ing operations into 2027 based on our current operating plan; the Company's pre - launch strategy; the potential commercial opport unity for MM120, if approved; the potential delivery model for MM120, if approved; and the potential for the markets that the Company is anticipating to acces s. There are numerous risks and uncertainties that could cause actual results, plans and objectives to differ materially from th ose expressed in forward - looking statements, including hist3ory of negative cash flows, limited operating history, incurrence of fu ture losses, availability of additional capital, compliance with laws and regulations, difficulty associated with research and development, risks associated with cli nic al trials or studies, heightened regulatory scrutiny, early stage product development, clinical trial risks, regulatory appro val processes, novelty of the psychedelic inspired medicines industry, as well as those risk factors described in the Company's Annual Report on Form 10 - K for the fiscal year ended December 31, 2023 under headings such as “Special Note Regarding Forward - Looking Statements,” and “Risk Factors” and “Management's Discussion and Analysis of Financial Condition and Results of Operations” and other filings and furnishings made by the Company with the se curities regulatory authorities in all provinces and territories of Canada which are available under the Company's profile on SE DAR+ at www.sedarplus.ca and with the U.S. Securities and Exchange Commission on EDGAR at www.sec.gov. Any forward - looking statement made by MindMed in this Presentation is based only on information currently available to the Company and speaks only as of the date on which it is made. Except as required by law, the Company undertakes no duty or obligation to update any forward - looking statements contained in this Presentation as a result of new information, future events, changes in expectations or o the rwise. Cautionary Note Regarding Regulatory Matters The United States federal government regulates drugs through the Controlled Substances Act. MM120 is a proprietary, pharmaceu tic ally optimized form of lysergide D - tartrate and MM402, or R( - ) - MDMA, is our proprietary form of the R - enantiomer of MDMA (3,4 - methylenedioxymethamphetamine). Lysergide and MDMA are Schedule I substances under the Controlled Substances Act. While the Company is focused on programs using psyche de lic or hallucinogenic compounds and non - hallucinogenic derivatives of these compounds, including in its MM120, MM402 and other product candidates, the Company does not have any direct or indirect involvement with the illegal sel lin g, production or distribution of any substances in the jurisdictions in which it operates. The Company is a neuro - pharmaceutical drug development company and does not deal with psychedelic or hallucinogenic substances except within laboratory and clinical trial settings con ducted within approved regulatory frameworks. The Company's products will not be commercialized prior to applicable regulator y a pproval, which will only be granted if clinical evidence of safety and efficacy for the intended uses is successfully developed. Market and Industry Data This Presentation includes market and industry data that has been obtained from third party sources, including industry publi cat ions. MindMed believes that the industry data is accurate and that the estimates and assumptions are reasonable, but there is no assurance as to the accuracy or completeness of this data. Third party sources generally state that the information contained therein has been obtained fr om sources believed to be reliable, but there is no assurance as to the accuracy or completeness of included information. Althou gh the data is believed to be reliable, MindMed has not independently verified any of the data from third party sources referred to in this Presentation or ascertained the u nd erlying economic assumptions relied upon by such sources. References in this Presentation to research reports or to articles and publications should be not construed as depicting the complete findings of the entire referenced report or article. MindMed does not make any representation as to the accuracy of such information. 2 Disclaimer

Corporate Presentation | January 2025 Heather: the next slide is designed to convey a “bold” mission – I like the abstract image of the tree but open to your suggestions. This slide would follow our title slide. • We could also do something strictly scientific like how this image is used on this slide and incorporate the copy on the next slide 3 Transformational Innovation for Brain Health

4 Corporate Presentation | January 2025 2024 1H2025 2H2025 1H2026 2H2026 MM120 - 310 for MDD Phase 3 Initiation MM120 - 310 for MDD Phase 3 Readout MM120 - 301 for GAD Phase 3 Readout MM120 - 301 for GAD Phase 3 initiation MM120 - 300 for GAD Phase 3 Readout Expected cash runway through key clinical readouts and into 2027 1 x $250 million in equity investment x MM120 Phase 2b results presented at APA Annual Meeting x MM120 granted breakthrough designation by U.S. FDA x Successful end - of - phase 2 meeting with U.S. FDA supporting pivotal trial plans x MM120 ODT patent issued covering pharmaceutical formulation, methods of manufacturing and treatment; patent life through 2041 x MM120 ODT awarded Innovation Passport by the U.K. MHRA x Initiation of Phase 3 program for MM120 ODT in GAD (first patient dosed in Phase 3 Voyage study) 1. The Company’s cash and cash equivalents of $295.3 million as of September 30, 2024, expected to fund operations into 2027 bas ed on our current operating plan and anticipated R&D milestones. The Company expects its cash runway to extend at least 12 month s beyond the first Phase 3 topline data readout for MM120 ODT in GAD. GAD: Generalized Anxiety Disorder; MDD: Major Depressive Disorder; APA: American Psychiatric Association; ODT: Orally Disinte gra ting Tablet; U.K. MHRA: United Kingdom Medicines and Healthcare Products Regulatory Agency Maintaining Momentum with Multiple Upcoming Milestones

Corporate Presentation | January 2025 Advancing Our Pipeline with Broad Therapeutic Potential 1. Full trial details and clinicaltrials.gov links available at mindmed.co/clinical - digital - trials/ 2. Studies in exploration and/or planning stage. LSD: lysergide; R( - ) - MDMA: rectus - 3,4 - methylenedioxymethamphetamine 5 Registration Pivotal / Phase 3 Phase 2 Phase 1 Preclinical Indication Product Candidate Generalized Anxiety Disorder (GAD) 1 MM120 ODT (Lysergide D - tartrate) Major Depressive Disorder (MDD) 1,2 Additional Indication(s) 2 Autism Spectrum Disorder (ASD) 1 MM402 (R( - ) - MDMA)

Corporate Presentation | January 2025 Current Standard of Care is Failing Patients with GAD and MDD 1. Bystritsky A. Treatment - resistant anxiety disorders. Mol Psychiatry. (2006) 11:805 – 14; 2. Birkett MA, Shinday NM, Kessler EJ, Meyer JS, Ritchie S, Rowlett JK. Acute anxiogenic - like effects of selective serotonin reuptake inhibitors are attenuated by the benzodiazepine diazepam in BALB/c mice. Pharmacol Biochem Behav. 2011 Jun;98(4):544 - 51; 3. Zhdanava M, Pilon D, Ghelerter I, et al. The Prevale nce and National Burden of Treatment - Resistant Depression and Major Depressive Disorder in the United States. J Clin Psychiatry. 2021;82(2):20m13699. Published 2021 Mar 16; 4. APA. Practice Guideline for the Treatment of Patients With Major Depressive Di sor der. Published 2010; 5. Center for Drug Evaluation and Research (CDER). Major Depressive Disorder: Developing Drugs for Treat men t Guidance for Industry. Food and Drug Administration. Published 2018; 6. Grenard JL, et al. Depression and medication adherenc e i n the treatment of chronic diseases in the United States: a meta - analysis. J Gen Intern Med. 2011 Oct;26(10):1175 - 82; 7. DiMatte o MR, et al.. Depression is a risk factor for noncompliance with medical treatment: Meta - analysis of the effects of anxiety and depression on patient adherence. Arch Intern Med. 2000;160:2101 – 7; 8. Braund, T.A., Tillman, G., Palmer, D.M. et al. Antidepressant side effec ts and their impact on treatment outcome in people with major depressive disorder: an iSPOT - D report. Transl Psychiatry 11, 417 (2021); 9. Pr oprietary MindMed Primary Market Research SRI: serotonin reuptake inhibitor 6 - Payer “The lack of efficacy of current treatment, the poor tolerability of current treatment. It either doesn't work, it doesn't work fast enough, or patients can't tolerate it. So…there is a clear need for something that works better, more tolerable than the current standard of care.” 9 “It’s frustrating, the trial and error, we flip a coin and try medication. It might work and you don't know how long it will take and what the side effects will be. It’s not a good experience.” 9 - Patient “There is lack of new drugs with a different mechanism of action and more efficacious in symptom control … you end up prescribing similar treatments from the same family.” 9 - Psychiatrist Treatment Landscape Currently Dominated by SRIs • GAD: 50% failure rate 1 , limited/delayed anxiolytic effect 2 • MDD: 31% failed by 1 st and 2 nd line treatments 3 • Extended time to response (average of 6 - 8 weeks) 4,5 • Poor tolerability leads to suboptimal adherence 6,7 • Common side effects 8 • loss of appetite, weight loss, drowsiness, dizziness, fatigue, headaches, nausea & vomiting, sexual dysfunction

Corporate Presentation | January 2025 MM120 Has the Potential to Redefine Treatment for Patients 7 DESIRED FUTURE STATE Rapid & Durable Improvement CURRENT STATE Chronic Symptom Suppression • Cycles of medication failure • Delayed onset • Poor tolerability • Low remission rate • Loss of efficacy • Symptom masking • Fast onset • Single administration • Favorable tolerability • High remission rates • Durable response • Restores neural pathways

Corporate Presentation | January 2025 …And Represents a Welcome Breakthrough for Providers 1. Psychiatrists and Psychiatry Nurse Practitioners 2. Propietary MindMed Primary Market Research – Key Customer Perceptions Among Spravato® Providers and GAD Prescribers (February 20 24). Total Non - Spravato® Providers (n=125), Spravato® Providers (n=50). 3. Spravato Providers: recommended, referred or prescribed Spravato® treatment and monitored or administered Spravato® treatment, p ersonally or someone in her/his clinic or office. 8 % of Surveyed Providers 1 Agree All psychiatric providers 2 Interventional psychiatric providers 3 Availability of psychedelics for GAD and MDD will change my approach to treatment I expect psychedelic treatments to radically transform the treatment of GAD and MDD 62% 78% 74% 86%

MM120 ODT LSD D - tartrate Program Overview

Corporate Presentation | January 2025 Clinical Rationale and Mechanism of Action 10

Corporate Presentation | January 2025 The Impact of Generalized Anxiety Disorder 1. National Health Statistics Report. 2024; 213:1 - 12; 2. American Psychiatric Association. Diagnostic and Statistical Manual of Mental Disorders. 5th ed. Washington, DC: American Psychiatric Association; 2013:222; 3. https://www.nimh.nih.gov/health/statistics/any - anxiety - disorder; 4. Revicki DA, et al. J Affect Disord. 2012;140(2):103 - 112. 5. Duong P, et al. Association Between Generalized Anxiety Disorder Scale (GAD - 7) and 5 - Level EQ - 5D Index Scores Among US Adults Diagnosed with GAD. Presented at ECNP 2024. Milan, Italy; 6. Duong P, et al. Work Productivity and Activity Impairment Associ ate d with Generalized Anxiety Disorder among Adults in the United States. Presented at ISPOR. 2024. Atlanta, GA; 7. Kavelaars R. Th e burden of anxiety among a nationally representative U.S. adult population, Journal of Affective Disorders. 2023; 336: 81 - 91; 8. Kessler RC, Sampson NA, Berglund P, et al: Anxious and non - anxious major depressive disorder in the World Health Organization Wo rld Mental Health Surveys. Epidemiol Psychiatr Sci 2015; 24:210 – 226; 9. Carter R. M., et al. One - year prevalence of subthreshold and threshold DSM - IV generalized anxiety disorder in a nationally representative sample. Depress Anxiety. 13, 78 – 88 (2001); 10. Kas per S. Anxiety disorders: under - diagnosed and insufficiently treated. Int J PsychiatryClin Pract. 2006;10(supp1):3 - 9 11 A chronic, debilitating disorder lasting for 6 months or more. Patients find it difficult to control the worry , often resulting in impairment in social, occupational, or other areas of functioning 2 Anxiety disorders are the most common mental health disorders in the U.S. 3 Poor health - related quality of life 4 which worsens with increased GAD severity 5 Work productivity loss and daily activity impairment 6 Substantial economic burden due to higher direct and indirect costs 4,7 High comorbidity burden ; >50% of patients with GAD also have MDD 8,9 Despite high prevalence, GAD is underdiagnosed , often leading to undertreatment 10 In 2022, approximately 18% of U.S. adults reported living with anxiety symptoms 1

Corporate Presentation | January 2025 The Impact of Major Depressive Disorder 1. SAMHSA. 2023 NSDUH detailed tables. Published July 2024; 2. APA. Diagnostic and statistical manual of mental disorders: DSM - 5 - TR. Fifth edition, text revision. ed. Washington, DC: American Psychiatric Association Publishing; 2022 3. Kessler RC, et al. T welve - month and lifetime prevalence and lifetime morbid risk of anxiety and mood disorders in the United States. Int J Methods Psyc hia tr Res. 2012 Sep;21(3):169 - 84. 4. McLaughlin KA. The public health impact of major depression: a call for interdisciplinary prevention efforts. Prev Sci 2011;12:361 – 71 5.Otte C,, et al. Major depressive disorder. Nat Rev Dis Prim. 2016 Dec 22;2(1):160 65; 6. Hofmann SG, Curtiss J, Carpenter JK, Kind S. Effect of treatments for depression on quality of life: a meta - analysis. Cog n Behav Ther. 2017;46(4):265 – 86; 7. Bromet E, Andrade LH, Hwang I, Sampson NA, Alonso J, de Girolamo G, et al. Cross - national epidemiolo gy of DSM - IV major depressive episode. BMC Med. 2011;9:90 8. Greenberg P, et al. Impact of living with an adult with depressive symptoms among households in the United States. Journal of Affective Disorders. 2024;349:107 - 115; 9. Rush AJ, et al. Acute and l onger - term outcomes in depressed outpatients requiring one or several treatment steps: A STAR*D Report. Am J Psychiatry. 2006;163(11):1905 - 17. 12 Characterized by the presentation of five or more depressive symptoms , occurring for at least 2 weeks 2 Second most common mental health disorder in the U.S. 3 Symptoms may include feelings of worthlessness, fatigue, impaired social functioning and recurrent thoughts of death 2 Associated with significant morbidity and mortality , 4 serious functional impairment, and reduced quality of life 5,6,7 Substantial economic burden due to higher direct and indirect costs 8 For patients who experience an MDE, fewer than half will receive adequate or any pharmacotherapy . Among those treated, approximately 1/3 will achieve remission from 1 st line therapy 9 21.9 million U.S. adults experienced a major depressive episode (MDE) in 2023 1

Corporate Presentation | January 2025 1. Studies will employ an adaptive design with interim blinded sample size re - estimation based on nuisance parameters (e.g. patient retention rate, variability of primary outcome measure) which allows for an increase of sample size up to 50% to maintain statistical power. 2. Clinical study designs subject to ongoing regulatory discussion and review, including of Phase 3 clinical trial protocols. 3. Expected first patient dosing DB: double blind; ODT: orally disintegrating tablet; OL: open - label; RCT: randomized controlled trial; HAM - A: Hamilton Anxiety S cale; MADRS: Montgomery - Åsberg Depression Rating Scale 13 MM120 - 300 MM120 - 301 Aligned clinical trial designs across indications maximize operational efficiencies Generalized Anxiety Disorder (GAD) Major Depressive Disorder (MDD) MM120 - 310 N=200 1,2 (1 :1 randomization) MM120 ODT vs. Placebo • Part A: 12 - week DB, RCT • Part B: 40 - week Extension with OL Treatment N=250 1,2 ( 2 :1:2 randomization) MM120 ODT vs. Placebo (including 50 µg control) • Part A: 12 - week DB, RCT • Part B: 40 - week Extension with OL Treatment N=140 2 (1:1 randomization) MM120 ODT vs. Placebo • Part A: 12 - week DB, RCT • Part B: 40 - week Extension with OL Treatment Initiated 4Q2024 Initiation: 1H2025 3 Initiation: 1H2025 3 Name TBA MM120 - 311 Design TBA Primary Endpoint : HAM - A at Week 12 Primary Endpoint : MADRS at Week 6 Robust Phase 3 MM120 Development Program Aiming for Broad Label

Corporate Presentation | January 2025 1. Study MMED008 internal study documents and calculations. Comparisons to standard of care/other drug classes based on histo ric al comparison not head - to - head comparison trial; 2. HAM - A scores based on ANCOVA LS Mean. in Study MMED008. Effect size based on post hoc calculation using LS Mean change between group and pooled standard deviation of wee k 12 HAM - A scores between groups; 3. Based on 100 µg dose group; 4. RB Hidalgo, J Psychopharmacol. 2007 Nov;21(8):864 - 72; 5. p - values not calculated for remission rates between groups. CGI - S: Clinical Global Impressions – Severity; HAM - A: Hamilton Anxiety Scale. Maximum effect size d =0.81 more than double the standard of care 1,2,3 ^Z/Ɛ ϰ ĞŶnjŽĚŝĂnj Ğ ƉŝŶĞ s 4 0 0.2 0.4 0.6 0.8 0.38 0.36 ƵƐƉŝƌŽŶĞ ϰ 0.17 0.81 MM120 100 µg 2 Comparative Effect Sizes in GAD Rapid and durable response after single administration 3 14 Rapid Response & Remission Durable Scalability, Access & Value Limited Adverse Event (AE) Burden 1.8 - point reduction in CGI - S within 24 hours (p<0.0001) 21.9 - point improvement on the HAM - A at Week 12 (p=0.003) 48% of participants in remission at Week 12 5 Favorable tolerability with most AEs on dosing day Drug effect without psychotherapy Cohen’s d MM120 Phase 2b Efficacy and Durability Support GAD Phase 3 Trial Plans 1,3

Corporate Presentation | January 2025 -25 -20 -15 -10 -5 0 LS Mean Change (SEM) in HAM - A score Primary Outcome: HAM - A Change from Baseline MM120 Phase 2b Showed Statistically & Clinically Significant Improvements on Anxiety and Depression Symptoms 1,2 1. Source: Study MMED008 internal study documents and calculations. Full analysis set population. 2. Based on 100 µg dose group. 3. Based on observed MADRS score at each timepoint. μ g: microgram; HAM - A: Hamilton Anxiety Rating Scale; MADRS: Montgomery - Åsberg Depression Rating Scale NOTE: Significance achieved despite study not being powered for these pairwise comparisons. 15 *p<0.05; **p≤0.01; ***p≤0.001 *** *** *** ** MADRS Change from Baseline -20 -15 -10 -5 0 LS Mean Change (SEM) in MADRS score ** ** * ** Change from Baseline 2 • Week 12: - 21.9 points Improvement over Placebo 2 • Week 12: - 7.7 pts, p=0.003 Change from Baseline 2,3 • Week 12: - 18.7 points Improvement over Placebo 2,3 • Week 12: - 6.4 points, p<0.01

Corporate Presentation | January 2025 MM120 Phase 2b Produced Profound Changes in GAD Severity 1. Source: Study MMED008 internal study documents and calculations. Full analysis set population. 2. Response is a 50% or greater improvement on HAM - A score; Remission is a HAM - A score of ≤ 7; p - values not calculated. μ g: microgram; HAM - A: Hamilton Anxiety Rating Scale 16 21 48 Placebo 100 µg % Remitters 31 65 0 10 20 30 40 50 60 70 Placebo 100 µg Percent of Participants Meeting Criteria at Week 12 % Responders HAM - A Response and Remission at Week 12 Median HAM - A Through Week 12 HAM - A Severity & Clinical Symptoms Very Severe Symptoms are incapacitating Severe (≥ 24) Symptoms are severe and persistent or result in severe distress or marked impairment in functioning Moderate (15 - 23) Symptoms are more frequent, with moderate distress or limited interference with usual activities Mild (8 - 14) Symptoms are infrequent, with no impairment and no more than mild distress Remission (≤ 7) Symptoms are absent, insignificant, or clearly due to causes other than anxiety 0 10 20 30 100 µg Placebo

Corporate Presentation | January 2025 MM120 Phase 2b was Well - tolerated with Mostly Expected Transient, Mild - to - Moderate Adverse Events on Dosing Day 1. Source: Study MMED008 internal study documents and calculations. Safety population. 2. One serious adverse event (SAE) was observed in the 50 µg dose group: panic attack on study day 98 that was deemed not relate d t o treatment. 3. Suicidality assessment based on reported adverse events. 17 • Virtually all (99%) adverse events (AEs) were mild - to - moderate in severity • Minimal (2.5%) treatment emergent AEs (TEAEs) led to study withdrawal • No drug - related serious AEs (SAEs) 2 Favorable tolerability profile No SAEs related to study drug No suicidal behavior or suicidality signal 3 • Only SAE was in 50 µg dose group and deemed unrelated • AE profile consistent with historical studies and drug class • No suicidal or self - injurious behavior • No indication of increased suicidality or suicide - related risk • ≤ 2 participants per arm reported suicidal ideation during the study

Corporate Presentation | January 2025 MM120 - 301 MM120 - 300 MM120 for GAD | Two Complementary Pivotal Phase 3 Study Designs 1 1. Studies will employ an adaptive design with interim blinded sample size re - estimation based on nuisance parameters (e.g. pati ent retention rate, variability of primary outcome measure) to maintain statistical power. Clinical study designs subject to ongoing regulatory discussion and review, including of Phase 3 cli nical trial protocols. 18 MM120 ODT 1 00 µg N=100 Placebo N=100 Part A 12 Week Randomized, Double - Blind Part B 40 Week Extension with Opportunity for Open - Label Treatment MM120 ODT 1 00 µg N=100 Placebo N=100 MM120 ODT 50 µg N=50 PHASE 3 STUDY 1 Single Dose Potential treatment if HAM - A ≥16 Primary Endpoint HAM - A at Week 12 Up to four open - label doses of MM120 ODT 1 00 µg Single Dose Follow - up Observation GAD - 7 (ePRO): biweekly HAM - A (central rater): monthly or when GAD - 7 ≥10 Potential Treatment Eligible for open - label treatment if HAM - A ≥16

Corporate Presentation | January 2025 Primary Endpoint MADRS at Week 6 MM120 - 311 MM120 - 310 MM120 for MDD | Phase 3 Study Design 1 1. Clinical study designs subject to ongoing regulatory discussion and review, including of Phase 3 clinical trial protocols. 19 MM120 ODT 1 00 µg N=70 Placebo N=70 Part A 12 Week Randomized, Double - Blind Part B 40 Week Extension with Opportunity for Open - Label Treatment PHASE 3 STUDY 1 Single Dose Potential treatment if MADRS ≥20 Up to four open - label doses of MM120 ODT 1 00 µg [Design TBA] Follow - up Observation PHQ - 9 (ePRO): biweekly MADRS (central rater): monthly or when PHQ - 9 ≥10 Potential Treatment Eligible for open - label treatment if MADRS ≥20

Corporate Presentation | January 2025 Today. Regulatory Elements Supporting MM120 ODT NDA Filing Requirements Study designs that demonstrate standalone drug effect FDA breakthrough therapy designation Phase 2b demonstrated substantial improvement over current therapies Phase 3 program in alignment with FDA guidance Phase 3 study design mirrors positive Phase 2b study 20

MM120 ODT LSD D - tartrate Commercial Framework

Corporate Presentation | January 2025 Integrate MM120 ODT Delivery into Current Infrastructure Maximize Access and Reimbursement Educate Stakeholders about MM120 and Burden of GAD & MDD Bold Strategy to Deliver on the Commercial Opportunity for MM120 ODT 22 MM120 Value Proposition

Corporate Presentation | January 2025 Unique Opportunity to Deliver on the Quadruple Aim 23 Better Outcomes New mechanism of action may restore neural pathways for potential sustained remission Improved Patient Experience Potential for single administration with rapid onset of clinical activity , well - tolerated treatment , reduced burden of clinical visits , and improved productivity and activity Lower Costs Decreased healthcare utilization through timely screening and early treatment could avoid disorder progression and cost of treating co - morbidities Improved Clinician Experience High satisfaction expected for providers with access to a potential treatment that delivers meaningful improvement for patients and with the possibility for attractive practice economics $ Lower Costs Better Outcomes Improved Clinician Experience Improved Patient Experience

Corporate Presentation | January 2025 Potential Launch Can Leverage and Expand on Rapidly Growing Interventional Psychiatry Infrastructure 1. As of 2Q2024; centers certified under the Spravato REMS 2. J&J Investor Day presentation, July 2024, Johnson & Johnson Spravato® website, July 2024. Compiled by company. IQVIA Rx data analysis; June 2023 3. Clinic and prescriber numbers are approximate and compiled by company. 24 Emerging Network of Interventional Psychiatry Clinics 1,2,3 4,500 certified delivery clinics/offices • 60+% growth in 18 months • Geographic concentration in key metro hubs 2,800 Spravato ® prescribers • High prescription concentration • 200 prescribers generate 50% of prescriptions • 620 prescribers generate 80% of prescriptions Proven reimbursement, documentation and logistics pathways

Corporate Presentation | January 2025 Building on Existing Infrastructure, Practice Patterns & Reimbursement Pathways 1. HCP that is licensed to prescribe medications to patients. 2. HCP that is licensed to practice, which may include physicians, clinical psychologists, nurse practitioners, nurses, licensed cl inical social workers, licensed family and marriage therapists and others. 3. Existing coding systems could potentially be applied or be changed for MM120. Reimbursement and coding for MM120 have yet to be established. 25 Office - based or Telehealth Prescriber 1 Evaluation & Prescribing MindMed MM120 ODT Site of delivery Session Delivery Activity Medical Benefit E&M Code (992XX) or G Code Pharmacy Benefit J or S Code + dispensing fee Medical Benefit E&M Code per hour of clinical monitoring and services Stakeholder Reimbursement/Coding 3 HCP 2 to monitor session

Appendix

Corporate Presentation | January 2025 27 MM120 - 301 250 participants (2:1:2) 2 Randomize Screen Dose Follow - Up MM120 ODT 1 00 µg (n=100) 2 MM120 ODT 50 µg (n=50) 2 Placebo (n=100) 2 MM120 - 300 200 participants (1:1) 2 MM120 ODT 1 00 µg (n=100) 2 Placebo (n=100) 2 Week - 30 to - 1 1 2 4 8 12 16 20 24 28 32 36 40 44 48 52 MM120 for GAD | Phase 3 Study Design Leverages Phase 2b Results 1 1. Source: Study MM120 - 300 and Study MM120 - 301 internal study documents. 2. Study will employ an adaptive design with interim blinded sample size re - estimation based on nuisance parameters (e.g. patient r etention rate, variability of primary outcome measure) allowing for up to 50% more subjects in each arm to maintain statistical power. Clinical study designs subject to on goi ng regulatory discussion and review, including of Phase 3 clinical trial protocols. μ g: microgram; CGI - S: Clinical Global Impressions - Severity; GAD: generalized anxiety disorder; HAM - A: Hamilton Anxiety Rating S cale; ODT: orally disintegrating tablet MM120 - 300 & 301 | Parts A & B KEY SECONDARY ENDPOINTS • HAM - A at Week 1 • CGI - S at Day 2 • Time to retreatment / inefficacy SELECT ENTRY CRITERIA • Men and Women • Ages 18 - 74 • Diagnosis of GAD • HAM - A ≥20 Part A 12 Week Randomized, Double - Blind Part B 40 Week Extension with Opportunity for Open - Label Treatment Primary Endpoint: HAM - A at Week 12 PART B ENDPOINTS • Safety of repeated treatment • Time to retreatment / inefficacy • Average treatments per year • Response to retreatment

Corporate Presentation | January 2025 Strategies to Address Key Drug Class Methodological Considerations AE: adverse event; ECG: electrocardiogram; MOA: mechanism of action; TQT: thorough QT 28 Expectancy Bias & Functional Unblinding Cardiovascular Safety Adverse Event Collection • Independent central raters blinded to treatment and visit number for primary outcome measure • Dose - response in Phase 2b across ‘functionally active’ doses • Complementary studies with multiple ‘functionally masking’ arms • Pre - and post - dose expectancy assessment (participants) • Post - dose (participant) and rating (raters) blinding assessment • Drug effect isolated from psychotherapeutic intervention • Collection of ECGs in Phase 3 Clinical Trials • Dedicated TQT study in parallel with Phase 3 • Collection of all AEs, including “positive” and MOA - related • Frequent assessment to define time course for resolution of drug effects

v3.24.4

Cover	Jan. 10, 2025
Cover [Abstract]
Document Type	8-K
Amendment Flag	false
Document Period End Date	Jan. 10, 2025
Entity File Number	001-40360
Entity Registrant Name	Mind Medicine (MindMed) Inc.
Entity Central Index Key	0001813814
Entity Tax Identification Number	98-1582438
Entity Incorporation, State or Country Code	A1
Entity Address, Address Line One	One World Trade Center
Entity Address, Address Line Two	Suite 8500
Entity Address, City or Town	New York
Entity Address, State or Province	NY
Entity Address, Postal Zip Code	10007
City Area Code	212
Local Phone Number	220-6633
Written Communications	false
Soliciting Material	false
Pre-commencement Tender Offer	false
Pre-commencement Issuer Tender Offer	false
Title of 12(b) Security	Common Shares
Trading Symbol	MNMD
Security Exchange Name	NASDAQ
Entity Emerging Growth Company	true
Elected Not To Use the Extended Transition Period	false

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