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Neurogene: Developing Life-Changing Genetic Medicines For Rare Neurological Diseases 3EXACT: Expression Attenuation via Construct Tuning Lead program NGN-401 for Rett syndrome demonstrated promising interim clinical data Registrational trial start up activities for NGN-401 underway Rett syndrome represents an attractive commercial opportunity with substantial unmet need NGN-401 uses EXACT , a proprietary transgene regulation technology to overcome a key limitation in gene therapy Internal manufacturing capabilities provide strategic flexibility Cash runway extended to funds operations into early 2028

Product Candidate Indication IND* Enabling Phase I/2 Pivotal Near-Term Expected Milestones NGN-401 Rett Syndrome Registrational Trial Activities Underway Additional Interim Data 2H:25 NGN-101 CLN5 Batten Disease Evaluating Opportunities for Program Neurogene Clinical Stage Pipeline 4 *IND = investigational new drug Transgene Regulation CNS + Ocular Delivery

Wholly Owned and Fully Integrated In-House AAV Manufacturing 5 GMP Manufacturing Toxicology Batch Manufacturing Process Development Quality Assurance Quality Control Analytical Development • Flexibility to manufacture AAV product at low cost • Own product quality and development timelines • Process development expertise supports both HEK293 and Sf9/rBV manufacturing platforms • Flexibility to rapidly adapt CMC execution to program needs 42,000 sq ft facility in Houston, with 6,000 sq ft of cleanrooms Current research and clinical-grade manufacturing capabilities are designed for commercial-grade product to avoid potential future comparability challenges

NGN-401 for Rett Syndrome Leveraging EXACT transgene regulation technology

Rett Syndrome – Devastating Disorder with High Unmet Need 7 Genetics • X-Linked disorder causing mutations in the gene encoding for methyl-CpG binding protein 2 (MeCP2) • Unknown incidence in boys, but typically lethal by ~3 years of age due to no healthy copy of MeCP2 U.S. prevalence estimate based on published incidence rates; Laurvick CL, et al. J Pediatr 2006;148(3):347–35. WW incidence estimate based on published incidence rates; Pini G, et al. Orphanet Journal of Rare Diseases (2016) 11:132. High Unmet Need • There are no approved treatments that address root cause of disease • Significant unmet need remains for new treatment options Compelling Market Opportunity • U.S. prevalence - ~6,000-9,000 patients • WW incidence - 1:10,000 females

Rett Syndrome is a Debilitating, Progressive Neurological Disorder, with No Approved Treatments Addressing Root Cause 8 • Loss of purposeful hand use & involuntary hand movements • Loss of spoken language • Loss of hand function • Gait abnormalities • Ambulation requiring assistance or non-ambulatory • Severe apnea episodes • Hyperventilation • Constipation • Difficulty swallowing • Sleep disturbance • Seizures • Anxiety • Scoliosis • Muscle contractures Inability to Communicate Impaired Fine and Gross Motor Skills Autonomic Dysfunction Additional Disease Manifestations Loss of Function Over Time Early Onset: ~6–18 mos. Developmental Regression: ~1–3 yrs. “Relative Stability:” ~3–10 yrs. Disease Progression: Adolescence to Adulthood Cardinal Clinical Features

NGN-401: Potential to be Best-in-Class Gene Therapy for Rett Syndrome 9ICV = Intracerebroventricular EXACT transgene regulation technology designed to deliver consistent and tightly controlled MeCP2 protein expression on a cell-by-cell basis. ICV route of delivery has been shown in preclinical models to have the broadest targeting of brain and nervous system regions underlying Rett syndrome pathophysiology. An estimated 30,000 ICV procedures are performed by neurosurgeons annually in the U.S. and require minimal downtime/recovery. NGN-401 uses the full-length human MECP2 gene, which translates a fully functioning MeCP2 protein. MeCP2

Obtained Written Agreement from FDA on Key Elements of Embolden Registrational Trial Design 11 Design Patient Population Dose Primary Endpoint Open-label, single arm, baseline control (i.e., patient acting as own control) Females ages ≥ 3 years with Rett syndrome, consistent with our natural history study analysis that shows patients rarely learn new skills/reach developmental milestones or relearn skills once lost post-regression (~age ≥ 3)* 1E15 vg Responder-based composite endpoint of: CGI-I of < 3 and Gain of any one developmental milestone/ skill captured through video recordings *U.S. Natural History Study of Rett Syndrome (RNHS), sponsored by NIH, Clinicaltrials.gov identifier: NCT02738281. Accessed from International Rett Syndrome Foundation (IRSF); based on analysis of >400 subjects.

FDA Accepts Conversion of Phase 1/2 to Registrational Trial 12Three pediatric participants previously received 3E15 vg dose in Phase 1/2 portion Open-label, baseline-controlled trial evaluating single dose of NGN-401 (1E15 vg) Embolden Registrational Clinical Trial Ages > 3 years N = 18* Phase 1/2 Portion • Females with Classic Rett syndrome in post regression stage of illness • Clinical diagnosis and genetic confirmation of pathogenic MECP2 mutation • Clinical Global Impression-Severity (CGI-S) score of 4–6 Key Eligibility Criteria Written agreement obtained on open-label arm study design; *N=18 is proposed, subject to feedback from the FDA • 10 participants received NGN-401 (1E15 vg) - 8 females ages 4–10 - 2 females ages > 11 • Initial clinical data reported on 4 participants Nov 2024 • Updated data expected to be reported 2H 2025

28 Developmental Skills/Milestones from the Natural History Study to Be Evaluated in Embolden Trial 13 Fine Motor/Hand Function • Reached for toy • Taken a drink from a cup held without assistance • Used raking grasp to retrieve an object • Used a pincer grasp (either refined or modified) • Finger fed • Transferred an object from one hand to the other • Used a spoon/fork to eat without assistance • Sat with support when placed • Sat without support when placed • Come to sitting • Pulled to standing • Stood while holding on • Stood independently • Cruised around furniture or holding on to someone • Walked independently • Climbed up stairs with help • Climbed up stairs without help • Climbed down stairs with help • Climbed down stairs without help • Ran 10 feet without falling • Responded to familiar names/words • Followed a command with a gesture • Followed a command without a gesture • Pointed for something they want • Waved bye-bye • Babbled • Used words with meaning • Spoken in phrases (2 words or more with meaning) Skills Chosen Based on Meaningfulness to Caregivers and Rarely Learned > 3 Years* *U.S. Natural History Study of Rett Syndrome (RNHS), sponsored by NIH, Clinicaltrials.gov identifier: NCT02738281. Accessed from International Rett Syndrome Foundation (IRSF); based on analysis of >400 subjects. Gross Motor/Ambulation Communication

• Rett syndrome caregivers provided perspective on meaningfulness of gains of developmental milestones/skills in the core domains of Rett syndrome: fine motor, gross motor and communication • All skills queried, across all categories, were considered meaningful by majority of respondents • Caregivers indicated that Rett syndrome burden is immense, with 24-hour care needed to support their daughter’s needs • Skill gains or symptom improvement would provide respite not just to the patients, but to their caregiver(s), siblings, and extended family • Any skill gain or symptom improvement that would provide some level of independence/reduce dependence for their daughter would be highly meaningful 14 Quantitative research conducted in November and December 2024 with 30 Rett syndrome caregivers to daughters aged 3-22 years old; follow-up qualitative research conducted in December 2024 and January 2025 with 27 Rett syndrome caregivers (sub-set of quantitative respondents) to daughters aged 3-22 years old Rett Syndrome Caregiver Research Demonstrated Clinical Meaningfulness of Developmental Milestone/Skill Acquisition

Feedback on Meaningfulness of Developmental Milestones/Skills Showed Real-Life Examples of Potential Impact 15 Even a small improvement would definitely be meaningful because even if she could stand with support or bear her own weight, even for 30 seconds or less, that would allow us to be able to pivot her into her wheelchair versus having to lift her. Fine Motor Gains: • Increase communication abilities • Provide level of independence in eating • Social improvements/ participating in mealtimes Gross Motor Gains: • Foster greater physical autonomy • Reduce caregiver physical strain • Enhance safety by lowering fall risks • Enhance feeding safety by holding body upright • Provide dignity and independence Communication Gains: • Decrease suffering if daughter could indicate injuries/pain • Better ensure daughter’s needs and wants are appropriately met without guessing • Eliminate safety concerns around interactions with others/strangers You immediately go to the usual, ‘Is your tummy hurting? Is this? Is that?’ …It’s hard to tell if she’s just uncomfortable or something is happening to her…The frustration on her part is, as you can imagine, it’s just trying to tell someone and nobody’s understanding what she is trying to tell. I have to feed her every spoonful, every bite that she eats. But if we could scatter some food in front of her and she could feed herself, that would be a huge help. It is probably one of the bigger things for her to do to be independent. Quantitative research conducted in November and December 2024 with 30 Rett syndrome caregivers to daughters aged 3-22 years old; follow-up qualitative research conducted in December 2024 and January 2025 with 27 Rett syndrome caregivers (sub-set of quantitative respondents) to daughters aged 3-22 years old Caregiver Feedback

Phase 1/2 Data Support Registrational Trial Design 16 As of data cut-off date of 17 October 2024 *As of 2 June 2025; HLH monitoring and treatment protocol added to Phase 1/2 protocol in January 2025 HLH = Hemophagocytic lymphohistiocytosis NGN-401 Durable improvements observed across multiple scales, incl. two-point improvement in CGI-I in all participants, with concordance of benefit across scales Consistent gains observed across core clinical domains of hand function, gross motor and communication, despite heterogeneous presentation Objective improvements in autonomic domains of sleep and constipation Clinically meaningful gain of skills and developmental milestones beyond those observed in natural history data Rapid response post-treatment, with deepening of response over time 1E15 vg NGN-401 dose believed to be generally well-tolerated • No evidence of HLH*

Baseline Characteristics of Dosed Participants Range from Moderate to Severe Disease 17 As of data cut-off date of 17 October 2024 As of 11 November 2024, Neurogene discontinued use of 3E15 vg dose and updated Phase 1/2 protocol to use 1E15 vg dose for all future participants 1E15 vg Participant 1 (Pt:1) Participant 2 (Pt:2) Participant 3 (Pt:3) Participant 4 (Pt:4) Participant 5 (Pt:5) Age at Dosing in Years 7 4 6 7 6 MECP2 Mutation Severity Mild Severe Severe Severe Severe Baseline Disease Severity as Indicated by CGI-S Score 4 (moderately ill) 5 (markedly ill) 5 (markedly ill) 5 (markedly ill) 5 (markedly ill) Time Post Treatment with NGN-401 in Months ~15 ~12 ~9 <6 ~1 Despite Similar CGI-S Scores, Individual Baseline Presentations Vary Widely Across Core Clinical Domains

Participants* Achieved CGI-I Rating of “Much Improved” CGI-I Score ≤ 3 = Clinically Meaningful Improvement Pt:1 3 – Minimally Improved 2 – Much Improved 2 – Much Improved 2 – Much Improved 2 – Much Improved Pt:2 2 – Much Improved 2 – Much Improved 2 – Much Improved 2 – Much Improved Pt:3 3 – Minimally Improved 3 – Minimally Improved 2 – Much Improved Pt:4 2 – Much Improved 3 mos. 6 mos. 9 mos. 12 mos. 15 mos. 18 Post Treatment with NGN-401 *Efficacy data from the first four participants; as of data cut-off date of 17 October 2024 Clinically Meaningful Improvement Observed Early After Treatment, with Deepening Response and Durability Over Time

Improvements in Clinician and Caregiver Assessments with Aggregate 23 Skills Acquired Across 4 Participants 19*Each participant achieved a 2-point improvement, or “much improved” from baseline CGI-I CGI-S Total Score RSBQ Improved? How many points?* Improved? How many points? Improved? How many points? (% Change) Pt:1 15 mos. post-NGN- 401 2 pts. 10 pts. (-28%) Pt:2 12 mos. post-NGN- 401 2 pts. 1 pt. 32 pts. (-52%) Pt:3 9 mos. post-NGN- 401 2 pts. 5 pts. (-29%) Pt:4 3 mos. post-NGN- 401 2 pts. 8 pts. (-28%) Gain of Skills, Developmental Milestones and Symptom Improvement in RTT Clinical Domains Hand Function Gross Motor Communi- cation Autonomic Attentive- ness Consistent Improvement Across Key Rett Syndrome Scales, Bolstered by Functional Improvements in Core Clinical Domains Efficacy data from the first four participants; as of data cut-off date of 17 October 2024

Pt:1 Multi-Domain Improvements Deepened Over Time, and Not Expected Based on Rett Syndrome Natural History 20 *Skill learned is “Wave hello;” however, RNHS tracked “Waves Bye Bye” As of data cut-off date of 17 October 2024 Images are representative of skills and are not photos of participants in the NGN-401 clinical trial Select Pt:1 Developmental Skills Post-NGN-401 Months Post-NGN-401 3 6 9 12 15 Uses a pincer grasp Holds bottle or cup unpropped Uses spoon/fork to self-feed Transfers objects between hands Heel-to-toe walking Climbs up stairs without help Climbs down stairs without help Follows a command without gesture Waves hello* Taps for wants Fine Motor Gross Motor Communication Baseline: 7 Yrs Old Mild Disease Walking, ataxic gait, no ability to climb stairs Raking, no ability to hold objects Severe impairment, unable to follow commands Post Treatment with NGN-401

Pt:2 Multi-Domain Improvements from Severe Impairments at Baseline Deepened Over Time, and Not Expected 21 As of data cut-off date of 17 October 2024 Images are representative of skills and are not photos of participants in the NGN-401 clinical trial Select Pt:2 Developmental Skills Post-NGN-401 Months Post-NGN-401 3 6 9 12 Reaches for an object Uses raking grasp to retrieve an object Self-feeds Stands independently from seated position Bends down, touches floor, and recovers Steps off curb with help Follows a command without a gesture Uses words with meaning Fine Motor Gross Motor Communication Baseline: 4 Yrs Old Impaired, ataxic, help to stand Severe impairment, unable to use hands Severe impairment, unable to follow commands, non-verbal Based on Rett Syndrome Natural History Post Treatment with NGN-401

Fine Motor Gross Motor Pt:3 Multi-Domain Improvements Not Expected Based on Rett Syndrome Natural History 22 As of data cut-off date of 17 October 2024 Images are representative of skills and are not photos of participants in the NGN-401 clinical trial Select Pt:3 Developmental Skills Months Post-NGN-401 3 6 9 Uses a pincer grasp Able to self-feed Sits independently Baseline: 6 Yrs Old Cannot sit, stand or walk Raking grasp Post Treatment with NGN-401 Severe Dysphagia

Pt:4 Early Improvements in Hand Function Not Expected Based on Rett Syndrome Natural History 23 Fine Motor Baseline: 7 Yrs Old Raking grasp, unable to hold objects Select Pt:4 Developmental Skills Months Post-NGN-401 3 Uses a pincer grasp Can use utensils to self-feed (without assistance) Post Treatment with NGN-401 As of data cut-off date of 17 October 2024 Images are representative of skills and are not photos of participants in the NGN-401 clinical trial

All Participants* Experienced Improvements in Autonomic Function, as Measured by Objective Assessments 24Detailed data provided in Appendix Pt:1 and Pt:2 Pt:1, Pt:2 and Pt:4 Pt:3 Had sleep deficits at Baseline, and experienced improvements in sleep parameters, as measured by a wearable device • LD:1 sleep efficiency increased from 83% to 90% at 6 months • LD:2 sleep efficiency increased from 90% to >95% at 6 months, considered ideal Had constipation at Baseline, and experienced improvements over time as measured by the caregiver- reported modified Bristol Stool Form Scale Had dysphagia, or difficulty swallowing, at Baseline, requiring a pureed diet and had to be spoon-fed by caregiver due to aspiration; at 9 months after dosing, she gained the ability to swallow liquids from a cup and chew and swallow food items *Efficacy data from the first four participants; as of data cut-off date of 17 October 2024

• In 2025, dosed 3 participants in the 4–10 years cohort and 2 participants in the > 11 years cohort - No evidence of HLH • HLH risk mitigation included in Phase 1/2 and registrational trial design - Dose level at/above 1E14 vg/kg not allowed - In the first week post dosing: employ daily monitoring of HLH, focused on “the three Fs” – ferritin, fever, and falling blood counts (cytopenia) - Exclude subjects with any illness within 30 days of dosing and COVID within 6 weeks of screening - Prior to dosing, require sites to have anakinra available and encourage availability of a local HLH expert - Included HLH treatment algorithm: 1st line – high-dose corticosteroids, 2nd line – anakinra 25As of 2 June 2025 Phase 1/2 Trial Update

• No participants have presented with the “three Fs” – Fever, elevated Ferritin, and Falling blood counts (cytopenia) • Transient ferritin elevations observed in 4 of 5 subjects recently dosed, peaking at Study Day 5-6 with recovery to Baseline by Day 10–12 with no intervention • No clinical symptoms of HLH/ hyperinflammatory syndrome have been observed 26As of 2 June 2025 1Galletta et al. JClin Pharm Ther. 2022:47(9):1478-1481.; 2Byrne et al Mol Ther. 2022;30(12):3503-3504. No Evidence of HLH/Hyperinflammatory Syndrome at the 1E15 vg Dose Level Ferritin Levels of Most Recently Dosed Participants – 1E15vg Galletta et al. publication reported case of HLH following high-dose systemic AAV treatment (1.1E14 vg/kg); the patient presented with the "three Fs" - fever, falling blood counts (cytopenia) and ferritin of 2,959 ng/ml 36 hours post-dose. The patient was treated with high-dose steroids and recovered1.

Key Upcoming Anticipated Milestones and Pipeline Developments 28 Provide regulatory update in 1H:25 regarding registrational trial Initiate registrational trial activities Announce additional Phase 1/2 clinical data in 2H:25 Cash Runway Expected to Fund Operations Into Early 2028 Rett Syndrome (NGN-401) CLN5 Batten Disease (NGN-101) Evaluate opportunities for the program

Pt:1 Autonomic Function: Objective Improvements Observed in Sleep Parameters and Constipation 30 Total sleep time increased from 6.6 to 7 hrs./night Number of position changes decreased from 37 to 18 per night Sleep efficiency* increased from 83% to ~90% (95% is ideal) Improvements in All Sleep Parameters, as Assessed by Wearable Device Constipation Improved Over Time, as Measured by Stool Consistency and Frequency** % o f R ep or te d S to ol Ty pe s E ac h M on th 0% 20% 40% 60% 80% 100% Month 0 Month 1 Month 2 Month 3 Month 4 Month 5 Month 6 None Type 1 - Separate hard lumps, like nuts Type 2 - Sausage-like, but lumpy Type 3 - Like a sausage or snake, smooth and soft Type 4 - Fluffy pieces with ragged edges, a mushy stool Type 5 - Watery, no solid pieces Baseline BL 3M 6M 9M 12M 4 6 8 10 12 To ta l S le ep T im e (h r) BL 3M 6M 9M 12M 0 20 40 60 80 100 120 # Sl ee p Po si tio n C ha ng es BL 3M 6M 9M 12M 70 80 90 100 Sl ee p Ef fic ie nc y (% ) *Sleep efficiency defined as time spent asleep vs. total time spent in bed **As measured by Caregiver on modified Bristol Stool Form Scale As of data cut-off date of 17 October 2024

0% 20% 40% 60% 80% 100% Month 0 Month 1 Month 2 Month 3 Month 4 Month 5 Month 6 None Type 1 - Separate hard lumps, like nuts Type 2 - Sausage-like, but lumpy Type 3 - Like a sausage or snake, smooth and soft Type 4 - Fluffy pieces with ragged edges, a mushy stool Type 5 - Watery, no solid pieces Pt:2 Autonomic Function: Objective Improvements Observed in Sleep Parameters and Constipation 31 Transition to More Restful Sleep, as Assessed by Wearable Device Constipation Improved Over Time, as Measured by Stool Consistency and Frequency** Total sleep time decreased; however, more restful sleep occurring Number of position changes decreased from 37 to 8 per night Sleep efficiency* increased to >95%, which is ideal % o f R ep or te d S to ol Ty pe s E ac h M on th BL 3M 6M 9M 4 6 8 10 12 To ta l S le ep T im e (h r) BL 3M 6M 9M 0 20 40 60 80 100 120 # Sl ee p Po si tio n C ha ng es BL 3M 6M 9M 70 80 90 100 Sl ee p Ef fic ie nc y (% ) Baseline *Sleep efficiency defined as time spent asleep vs. total time spent in bed **As measured by Caregiver on modified Bristol Stool Form Scale As of data cut-off date of 17 October 2024

Beginning 3 months post-NGN-401, Pt:3 could swallow liquids, such as clear soup and water from a sippy cup, and chew and swallow soft items, such as meatballs and cooked carrots, without choking At 9 months post-NGN-401, she is now able to grasp food such as apple slices and self-feed At Baseline, Pt:3 had dysphagia requiring a pureed diet and had to be spoon- fed by caregiver due to aspiration Pt:3 Autonomic Function: Experienced Clinically Meaningful Improvement in Swallowing and Gained Ability to Self-feed 32 Pt:3 did not have Baseline deficits in autonomic categories of sleep or constipation • Sleep duration and quality maintained post-treatment • No change in Modified Bristol Stool Form Scale scores post-treatment As of data cut-off date of 17 October 2024

Pt:4 did not have Baseline deficits in autonomic category of sleep Sleep quality maintained post-treatment Pt:4 Autonomic Function: Objective Improvement Observed in Constipation 33 Constipation Improved in Month 4, as Measured by Stool Consistency and Frequency* *As measured by Caregiver on modified Bristol Stool Form Scale 0% 20% 40% 60% 80% 100% Baseline Month 1 Month 2 Month 3 Month 4 None Type 1 Type 2 Type 3 Type 4 Type 5 % o f R ep or te d S to ol Ty pe s E ac h M on th As of data cut-off date of 17 October 2024

NGN-401 Demonstrated Efficacy and Safety in Mecp2 Mouse Models 34 Survival in Male Knockout 0 5 10 15 20 25 30 35 40 45 50 0 25 50 75 100 Su rv iv al (% ) 9 23 37wks Age (weeks) 0 5 10 15 20 25 0 25 50 75 100 Age (weeks) Su rv iv al (% ) Survival in Female Het NGN-401 1E11 vg NGN-401 3E11 vg MECP2EXACT1 NGN-401 (regulated) MECP2 Unregulated Unregulated 1E11 vg Unregulated 3E11 vg WT + Vehicle Male or female + Vehicle Het=heterozygous for Mecp2, mirroring genetic makeup of human females with Rett syndrome ICV Delivery of NGN-401 Delivered Targeted MeCP2 Levels Complementary Recognition Sites

Delivers Consistent Levels of MECP2 Expression on Cell- by-Cell Basis 35 Conventional NGN-MECP2 Achieves Narrow Expression of MECP2* 0 50 100 150 200 0 200 400 600 800 1000 Intensity (AU) Nu m be r o f c el ls Unregulated Regulated EXACT GTx Conventional GTx *mouse cortex immunohistochemistry