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Vigil Presents Key Findings from ILLUMINATE & IGNITE Studies in ALSP at the 2024 American Academy of Neurology Annual Meeting

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Vigil Neuroscience, Inc. presents key findings from the ILLUMINATE Natural History Study and the IGNITE Phase 2 study at the 2024 American Academy of Neurology Annual Meeting. The studies demonstrate the potential of iluzanebart (VGL101) as a disease-modifying therapy for Adult-Onset Leukoencephalopathy with Axonal Spheroids and Pigmented Glia (ALSP). Positive interim data show promising results in slowing neurodegeneration and improving clinical outcomes. The findings suggest that MRI and fluid biomarkers could be important measures of ALSP pathophysiology. Vigil aims to advance the development of iluzanebart to offer a transformative treatment for ALSP patients.
Vigil Neuroscience, Inc. presenta i risultati principali dello studio di storia naturale ILLUMINATE e dello studio di fase 2 IGNITE durante il Meeting Annuale 2024 dell'Accademia Americana di Neurologia. Gli studi dimostrano il potenziale di iluzanebart (VGL101) come terapia modificante la malattia per la Leucoencefalopatia con Esordio nell'Adulto con Sferoidi Assonali e Glia Pigmentata (ALSP). I dati intermedi positivi mostrano risultati promettenti nel rallentare la neurodegenerazione e migliorare gli esiti clinici. I risultati suggeriscono che la risonanza magnetica e i biomarcatori fluidi potrebbero essere misure importanti della fisiopatologia dell'ALSP. Vigil mira a progredire nello sviluppo di iluzanebart per offrire un trattamento trasformativo ai pazienti con ALSP.
Vigil Neuroscience, Inc. presenta hallazgos clave del Estudio de Historia Natural ILLUMINATE y del estudio de fase 2 IGNITE en la Reunión Anual de la Academia Americana de Neurología de 2024. Los estudios demuestran el potencial de iluzanebart (VGL101) como terapia modificadora de la enfermedad para la Leucoencefalopatía de Inicio en Adultos con Esferoides Axonales y Glía Pigmentada (ALSP). Datos interinos positivos muestran resultados prometedores en la desaceleración de la neurodegeneración y la mejora de los resultados clínicos. Los hallazgos sugieren que la resonancia magnética y los biomarcadores de fluidos podrían ser medidas importantes de la fisiopatología del ALSP. Vigil tiene como objetivo avanzar en el desarrollo de iluzanebart para ofrecer un tratamiento transformador para los pacientes con ALSP.
Vigil Neuroscience, Inc.는 2024년 미국 신경학 아카데미 연례 회의에서 ILLUMINATE 자연사 연구와 IGNITE 2상 연구의 주요 결과를 발표했습니다. 이 연구들은 성인 발병 백질뇌병증과 색소성 글리아(알스프)에 대한 질병 수정 치료제로서 일루자네바트(VGL101)의 잠재력을 보여줍니다. 긍정적인 중간 데이터는 신경 퇴행을 늦추고 임상 결과를 개선하는 것에서 유망한 결과를 보여줍니다. 연구 결과는 MRI 및 유체 바이오마커가 알스프의 병리생리학의 중요한 측정 방법이 될 수 있음을 제안합니다. Vigil은 알스프 환자들에게 변혁적인 치료를 제공하기 위해 일루자네바트의 개발을 진행하고자 합니다.
Vigil Neuroscience, Inc. présente les principales conclusions de l'étude d'histoire naturelle ILLUMINATE et de l'étude de phase 2 IGNITE lors de la réunion annuelle 2024 de l'Académie américaine de neurologie. Les études démontrent le potentiel d'iluzanebart (VGL101) en tant que thérapie modifiant la maladie pour la leucoencéphalopathie à début adulte avec sphéroïdes axonaux et glie pigmentée (ALSP). Des données intermédiaires positives montrent des résultats prometteurs dans le ralentissement de la neurodégénération et l'amélioration des résultats cliniques. Les résultats suggèrent que l'IRM et les biomarqueurs fluides pourraient être des mesures importantes de la physiopathologie de l'ALSP. Vigil vise à avancer dans le développement d'iluzanebart pour offrir un traitement transformateur aux patients ALSP.
Vigil Neuroscience, Inc. präsentiert wichtige Ergebnisse aus der ILLUMINATE-Natural-History-Studie und der IGNITE-Phase-2-Studie auf der Jahrestagung 2024 der American Academy of Neurology. Die Studien zeigen das Potenzial von Iluzanebart (VGL101) als krankheitsmodifizierende Therapie für die Adult-Onset Leukoencephalopathy mit Axonalen Spheroids und Pigmentierter Glia (ALSP). Positive Zwischendaten zeigen vielversprechende Ergebnisse bei der Verlangsamung der Neurodegeneration und der Verbesserung der klinischen Ergebnisse. Die Befunde deuten darauf hin, dass MRT- und Flüssigbiomarker wichtige Maßnahmen zur Beurteilung der Pathophysiologie der ALSP sein könnten. Vigil beabsichtigt, die Entwicklung von Iluzanebart voranzutreiben, um eine transformative Behandlung für ALSP-Patienten anzubieten.
Positive
  • Positive interim data from the IGNITE Phase 2 study show that iluzanebart is well-tolerated and may slow irreversible neurodegeneration.
  • ILUMINATE Natural History Study findings indicate potential key measures of ALSP pathophysiology through MRI and fluid biomarkers.
  • Iluzanebart (VGL101) shows promise as a disease-modifying therapy for ALSP, with encouraging results in clinical outcomes and biomarker correlations.
  • Vigil Neuroscience aims to provide a transformative treatment option for ALSP patients based on the positive findings from the studies presented at the AAN Annual Meeting.
Negative
  • None.

- Findings from ILLUMINATE Natural History Study show that MRI and fluid biomarkers are emerging as key measures of ALSP pathophysiology -

- Positive interim IGNITE Phase 2 data demonstrating iluzanebart (VGL101) as potential disease-modifying therapy for ALSP

WATERTOWN, Mass., April 17, 2024 (GLOBE NEWSWIRE) -- Vigil Neuroscience, Inc. (Nasdaq: VIGL), a clinical-stage biotechnology company committed to harnessing the power of microglia for the treatment of neurodegenerative diseases, today announced the presentation of multiple oral and poster presentations on the Company’s lead clinical candidate iluzanebart at the 2024 American Academy of Neurology (AAN) Annual Meeting.

“We are excited to see our enthusiasm for iluzanebart matched by clinical leaders in the ALSP community. The interim findings from both the IGNITE Phase 2 and ILLUMINATE Natural History studies support the potential of iluzanebart to become the first, disease-modifying therapy for those living with ALSP,” said Petra Kaufmann, M.D., F.A.A.N, Chief Medical Officer of Vigil. “Both trials have led to an incredible step forward – not only in understanding ALSP disease progression, but also in drawing parallels between biomarkers and correlating clinical outcomes. We look forward to advancing the clinical development of iluzanebart in the hopes of providing a potentially transformative treatment option for those who have been impacted by this devastating disease.”

Oral presentation presented by Zbigniew Wszolek, M.D., Mayo Clinic, Jacksonville: Interim Results on iluzanebart (VGL101) From IGNITE: First Interventional Phase 2 Study in Patients with Adult-Onset Leukoencephalopathy with Axonal Spheroids and Pigmented Glia (ALSP)

“Vigil’s interim IGNITE data demonstrated that iluzanebart was well-tolerated, and the data suggest a favorable impact on the protein product of the CSF1R gene whose dysfunction is the causal driver of ALSP,” said Zbigniew Wszolek, M.D., consultant in the Department of Neurology at the Mayo Clinic. “Positive trends on MRI measurements support slowing in irreversible neurodegeneration, and to see these signals in patients as early as six months is very encouraging.”

Interim analysis of the Phase 2 IGNITE proof-of-concept, multicenter, open-label study evaluating safety, tolerability, and clinical effects of iluzanebart demonstrated:

  • A favorable safety and tolerability profile 
  • Predictable pharmacokinetic (PK) profile that is supportive of once-monthly dosing
  • CNS target engagement and downstream pharmacological activity, including increased cerebrospinal fluid (CSF) levels of soluble colony-stimulating factor-1 receptor (sCSF1R), which is emerging as a key biomarker of ALSP disease pathophysiology 
  • Positive trends consistent with slowing of disease progression on key magnetic resonance imaging (MRI) measures in individual patients
  • Encouraging trend emerging on changes in NfL reduction in individual patients

Poster presented by David S. Lynch, M.D., Ph.D., National Hospital for Neurology & Neurosurgery; University College London Institute of Neurology: Findings from the ILLUMINATE Prospective Natural History Study (NHS) in Individuals with Adult-Onset Leukoencephalopathy with Axonal Spheroids and Pigmented Glia (ALSP)

“The findings from ILLUMINATE highlight sensitive markers of ALSP pathophysiology that have the potential to provide valuable insight into clinical endpoints and improve the overall understanding of ALSP disease progression to inform future study designs,” said David Lynch, Ph.D., Honorary Research Fellow, Department of Neuromuscular Diseases, University College London.

Data on clinical measures, biomarkers, and MRI from ILLUMINATE were presented at the conference. Key findings included:

  • Baseline sCSF1R was substantially reduced in prodromal and symptomatic participants vs healthy volunteers, indicating reduced microglial activity
  • At baseline, CSF and serum levels of neurofilament light chain (NfL), a marker of neuroaxonal injury, were elevated multifold in symptomatic participants vs prodromal and healthy volunteers
  • Longitudinally, greater ventricle volume enlargement and gray matter volume reduction were observed in symptomatic vs prodromal participants
  • Symptomatic participants demonstrated greater cognitive impairment at baseline and progression over time, as measured by the Montreal Cognitive Assessment scale (MoCA), vs prodromal participants
  • Changes in ventricle volume over time demonstrated a statistically significant correlation with cognitive decline

Poster presented by Abbie Renoux, Ph.D., Vigil Neuroscience: VGL101: An Immunotherapy that Enhances Microglial Survival for Adult Onset Leukoencephalopathy with Axonal Spheroids and Pigmented Glia (ALSP)

The preclinical study demonstrated iluzanebart as a highly potent human TREM2 (hTREM2) agonist monoclonal antibody, and preclinically validated its pharmacological potential to therapeutically circumvent CSF1R dysfunction in human microglia, the pathophysiological process underlying ALSP. Key supportive findings highlighting the mechanism of action of iluzanebart included:

  • Demonstration that iluzanebart promotes human microglia resilience across multiple CSF1R loss-of-function states, including rescue in an ALSP-associated human genetic model system
  • Mechanistic evidence that iluzanebart potently engages its target TREM2 and thereby indirectly modulates CSF1R biology, including the disease-associated biomarker sCSF1R
  • Unbiased in vivo validation that TREM2-dependent activation of microglia is well-aligned with iluzanebart drug levels in mouse brains supporting its ability to achieve pharmacologically active CNS concentrations

The presentation and posters are accessible on the Publications page of the Company’s website.

About Iluzanebart
Iluzanebart, Vigil’s lead clinical candidate, is a fully human monoclonal antibody targeting human triggering receptor expressed on myeloid cells 2 (TREM2), which is responsible for maintaining microglial cell function. TREM2 deficiency is believed to be a driver of certain neurodegenerative diseases. Iluzanebart is in development for rare microgliopathies, such as ALSP, as well as other neurodegenerative diseases for which TREM2 and/or microglia deficiency is believed to be a key driver of disease pathology.

About ALSP
ALSP is a rare, inherited, autosomal dominant neurological disease with high penetrance. It is caused by a mutation to the CSF1R gene and affects an estimated 10,000 people in the United States, with similar prevalence in Europe and Japan. The disease generally presents in adults in their forties, is diagnosed through genetic testing and established clinical/radiologic criteria and is characterized by cognitive dysfunction, neuropsychiatric symptoms, and motor impairment. These symptoms typically exhibit rapid progression with a life expectancy of approximately six to seven years on average after diagnosis, causing significant patient and caregiver burden. There are currently no approved therapies for the treatment of ALSP, underscoring the high unmet need in this rare indication.

About Vigil Neuroscience  
Vigil Neuroscience is a clinical-stage biotechnology company focused on developing treatments for both rare and common neurodegenerative diseases by restoring the vigilance of microglia, the sentinel immune cells of the brain. Vigil is utilizing the tools of modern neuroscience drug development across multiple therapeutic modalities in its efforts to develop precision-based therapies to improve the lives of patients and their families. Iluzanebart, Vigil’s lead clinical candidate, is a fully human monoclonal antibody agonist targeting human triggering receptor expressed on myeloid cells 2 (TREM2) in people with adult-onset leukoencephalopathy with axonal spheroids and pigmented glia (ALSP), a rare and fatal neurodegenerative disease. Vigil is also developing VG-3927, a novel small molecule TREM2 agonist, to treat common neurodegenerative diseases associated with microglial dysfunction, with an initial focus on Alzheimer’s disease (AD) in genetically defined subpopulations.  
  
Forward-Looking Statements 
This press release includes certain disclosures that contain “forward-looking statements” of Vigil Neuroscience (“Vigil” or the “Company”) that are made pursuant to the safe harbor provisions of the federal securities laws, including, without limitation, express or implied statements regarding: the potential therapeutic benefit of iluzanebart, beliefs about observations made analyzing preclinical study and clinical trial data to date; and our ability to advance the clinical development of iluzanebart. Forward-looking statements are based on Vigil’s current expectations and are subject to inherent uncertainties, risks and assumptions that are difficult to predict. Factors that could cause actual results to differ include, but are not limited to, risks and uncertainties related to uncertainties inherent in the development of product candidates, including the conduct of research activities and the conduct of clinical trials; whether results from preclinical studies and clinical trials will be predictive of the results of later preclinical studies and clinical trials; the timing and content of additional regulatory information from the FDA;; as well as the risks and uncertainties identified in the Company’s filings with the Securities and Exchange Commission (SEC), including Vigil’s Quarterly Report on Form 10-K for the year ended December 31, 2023 and in any subsequent filings Vigil makes with the SEC. Forward-looking statements contained in this announcement are made as of this date, and Vigil undertakes no duty to update such information except as required under applicable law. Readers should not rely upon the information on this page as current or accurate after its publication date.

Internet Posting of Information 
Vigil Neuroscience routinely posts information that may be important to investors in the 'Investors' section of its website at https://www.vigilneuro.com. The company encourages investors and potential investors to consult our website regularly for important information about Vigil Neuroscience. 

Investor Contact:  
Leah Gibson   
Vice President, Investor Relations & Corporate Communications   
Vigil Neuroscience, Inc.  
lgibson@vigilneuro.com  
  
Media Contact:  
Megan McGrath   
MacDougall Advisors  
mmcgrath@macdougall.bio

 


FAQ

What key findings were presented by Vigil Neuroscience, Inc. at the 2024 American Academy of Neurology Annual Meeting?

Vigil Neuroscience presented findings from the ILLUMINATE Natural History Study and the IGNITE Phase 2 study, showcasing the potential of iluzanebart as a disease-modifying therapy for ALSP.

What is the significance of the positive interim data from the IGNITE Phase 2 study?

The positive interim data suggest that iluzanebart is well-tolerated and may have a favorable impact on slowing neurodegeneration in ALSP patients.

What do the findings from the ILUMINATE Natural History Study indicate?

The findings suggest that MRI and fluid biomarkers could serve as important measures of ALSP pathophysiology, providing valuable insights into disease progression.

What is the goal of Vigil Neuroscience regarding the development of iluzanebart?

Vigil aims to advance the clinical development of iluzanebart to potentially offer a transformative treatment option for individuals affected by ALSP.

Who presented the oral presentation on iluzanebart from the IGNITE Phase 2 study?

Zbigniew Wszolek, M.D., from Mayo Clinic, Jacksonville, presented the interim results on iluzanebart at the AAN Annual Meeting.

What were some key findings from the ILLUMINATE Natural History Study presented by David S. Lynch, M.D., Ph.D.?

Key findings included reduced microglial activity in ALSP participants, elevated levels of neurofilament light chain in symptomatic individuals, and cognitive decline correlations.

What did the preclinical study on iluzanebart by Abbie Renoux, Ph.D., demonstrate?

The study highlighted iluzanebart as a potent human TREM2 agonist monoclonal antibody with the potential to address CSF1R dysfunction in ALSP.

Where can the presentation and posters from Vigil Neuroscience be accessed?

The presentation and posters are available on the Publications page of the Company's website for further review.

Vigil Neuroscience, Inc.

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