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    Home»Longevity»NRG doses first volunteers in mitochondrial ALS trial
    Longevity

    NRG doses first volunteers in mitochondrial ALS trial

    adminBy adminJanuary 11, 2026No Comments4 Mins Read
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    NRG doses first volunteers in mitochondrial ALS trial
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    NRG Therapeutics takes a first-in-human step toward disease-modifying treatments for ALS and Parkinson’s, targeting aging at cellular level.

    There are clinical trial announcements that feel routine, and then there are those that quietly redraw the map of where medicine is heading. UK-based clinical-stage neuroscience company NRG Therapeutics has completed its first-in-human dosing of NRG5051, which belongs firmly in the latter category.

    The company has begun its Phase 1 clinical trial of NRG5051, an experimental drug designed to slow or potentially halt the progression of ALS/MND and Parkinson’s by targeting a shared biological weak point: mitochondrial failure [1]. It is a modest step on paper – healthy volunteers, safety data, dose escalation – but an ambitious one in implication.

    For decades, neurodegenerative drug development has largely chased symptoms. NRG is betting that the real leverage lies deeper, at the level of cellular energy and resilience – a territory increasingly central to longevity science.

    Neurons are among the most energy-hungry cells in the human body. When their mitochondria falter, neurons do not recover; they degenerate. In both ALS and Parkinson’s, this collapse of energy production accelerates inflammation and cell death long before clinical symptoms peak.

    NRG5051 is designed to intervene precisely at that point. Rather than targeting disease-specific proteins alone, the drug aims to stabilize mitochondrial function by inhibiting a process that becomes toxic when dysregulated [1]. In simple terms, it is an attempt to keep neurons alive longer by protecting the systems that power them.

    The latest announcement from NRG closely aligns with how aging researchers increasingly view neurodegeneration: not as isolated diseases, but as downstream expressions of failing cellular infrastructure.

    The Phase 1 study, now underway at the Centre for Human Drug Research in Leiden, is testing NRG5051 in healthy volunteers using a randomized, double-blind design. Researchers will evaluate the drug’s safety, tolerability and behavior in the human body across increasing doses.

    This stage does not promise efficacy headlines. What it offers instead is proof that a mitochondria-targeting approach can safely move from theory to humans. Results are expected by the end of 2026 and will guide future trials in ALS/MND and Parkinson’s patients.

    Neil Miller is the co-founder and CEO of NRG Therapeutics

    For NRG, this marks its transition from a preclinical science story to a clinical-stage company. Neil Miller, the co-founder and CEO of NRG Therapeutics, highlighted the company’s evolution, noting that the commencement of its first clinical trial represented a significant achievement and signaled its transition into a clinical-stage organization [2].

    The unmet need is stark. ALS remains rapidly fatal, with few disease-modifying options, especially for sporadic cases, which represent the majority of patients. Parkinson’s, meanwhile, is projected to double in prevalence by 2050, driven largely by global population aging.

    Despite decades of research, available Parkinson’s treatments still focus on symptom management, not disease progression. That failure has prompted growing interest in upstream mechanisms – mitochondria, inflammation and cellular stress responses – that cut across diagnostic labels.

    NRG’s approach reflects this shift: target the engine, not the dashboard.

    What makes NRG5051 especially relevant to the longevity sector is that mitochondrial dysfunction is not unique to ALS or Parkinson’s. It is a defining feature of aging itself.

    As cells lose their ability to generate energy efficiently, tissues become more vulnerable to stress, inflammation rises and recovery slows. Neurodegenerative diseases may be the most visible outcome, but they are not the only one.

    If mitochondrial-targeted therapies can preserve function in neurons, the same logic may eventually apply to other age-related systems. From an investment and strategy perspective, this places NRG’s work squarely within the broader effort to extend healthspan by maintaining cellular performance over time.

    NRG plans to advance NRG5051 into Phase 2 proof-of-concept studies in ALS/MND and to generate clinical data in Parkinson’s patients. The company’s backing, from venture funds, pharma-linked investors and disease foundations, signals confidence in both its science and its positioning.

    The first dose has now been given. The long work begins. In longevity science, progress typically occurs quietly; however, when a treatment focuses on safeguarding the biological systems most vulnerable to aging and failure, its impact can extend well beyond the scope of any individual illness.

    Photograph of Neil Miller courtesy of NRG Therapeutics

    [1] https://www.nrgtherapeutics.com/pipeline 
    [2] https://www.nrgtherapeutics.com/news/22/51/NRG-Therapeutics-Announces-First-Participants-Dosed-in-its-First-in-Human-Phase-1-Clinical-Trial-of-NRG5051-Which-is-Being-Developed-as-a-Disease-modifying-Treatment-for-ALSMND-and-Parkinsons.html 

    ALS doses Mitochondrial NRG trial volunteers
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