Exploratory Tau Biomarker Results From a Multiple Ascending-Dose Study of BIIB080 in Alzheimer Disease

Edwards, Amanda L.; Collins, Jessica A.; Junge, Candice; Kordasiewicz, Holly; Mignon, Laurence; Wu, Shuang; Li, Yumeng; Lin, Lin; DuBois, Jonathan; Hutchison, R. Matthew; Ziogas, Nick; Shulman, Melanie; Martarello, Laurent; Graham, Danielle; Lane, Roger; Budd Haeberlein, Samantha; Beaver, John

doi:10.1001/jamaneurol.2023.3861

Cited by 10 publications

(3 citation statements)

References 24 publications

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“…In a similar manner, antisense oligonucleotide approaches that reduce tau expression would be expected to slow the longitudinal progression of tau pathology, as measured by PET, but remain unlikely to drastically affect established tangles. However, in a phase 1b trial investigating the antisense oligonucleotide termed BIIB080 in subjects with mild AD, a significant reduction of tau PET below baseline was observed in a small imaging cohort ( n = 12) at week 100, likely through reducing the amount of tau protein that can be recruited in the modest ability of turnover in tangles [ 90 , 91 ]. Furthermore, an immunotherapeutic approach targeting an epitope within tau tangles may aim to acutely reduce tau PET signal below that of baseline under the context of target engagement, but it should be noted that extracellular tangles are a small and limited population to target.…”

Section: Bespoke Biomarker Strategies and Interpretations For Differi...mentioning

confidence: 99%

Considerations for biomarker strategies in clinical trials investigating tau-targeting therapeutics for Alzheimer’s disease

Penny,

Lofthouse,

Arastoo

et al. 2024

Transl Neurodegener

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The use of biomarker-led clinical trial designs has been transformative for investigating amyloid-targeting therapies for Alzheimer’s disease (AD). The designs have ensured the correct selection of patients on these trials, supported target engagement and have been used to support claims of disease modification and clinical efficacy. Ultimately, this has recently led to approval of disease-modifying, amyloid-targeting therapies for AD; something that should be noted for clinical trials investigating tau-targeting therapies for AD. There is a clear overlap of the purpose of biomarker use at each stage of clinical development between amyloid-targeting and tau-targeting clinical trials. However, there are differences within the potential context of use and interpretation for some biomarkers in particular measurements of amyloid and utility of soluble, phosphorylated tau biomarkers. Given the complexities of tau in health and disease, it is paramount that therapies target disease-relevant tau and, in parallel, appropriate assays of target engagement are developed. Tau positron emission tomography, fluid biomarkers reflecting tau pathology and downstream measures of neurodegeneration will be important both for participant recruitment and for monitoring disease-modification in tau-targeting clinical trials. Bespoke design of biomarker strategies and interpretations for different modalities and tau-based targets should also be considered.

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Section: Bespoke Biomarker Strategies and Interpretations For Differi...mentioning

confidence: 99%

Considerations for biomarker strategies in clinical trials investigating tau-targeting therapeutics for Alzheimer’s disease

Penny,

Lofthouse,

Arastoo

et al. 2024

Transl Neurodegener

View full text Add to dashboard Cite

show abstract

“…The trial results were recently published [ 209 ], showing a CSF total tau and p-181 tau reduction by 60 percent for six months in the higher-dose cohorts. Also, imaging results were promising, with reduced tau aggregates below baseline levels in all brain regions examined with tau PET [ 210 ]. Phase 2 is ongoing (NCT05399888).…”

Section: Gene Therapymentioning

confidence: 99%

Novel Therapeutic Strategies in Alzheimer’s Disease: Pitfalls and Challenges of Anti-Amyloid Therapies and Beyond

Tondo,

De Marchi,

Bonardi

et al. 2024

JCM

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Alzheimer’s disease (AD) causes a significant challenge to global healthcare systems, with limited effective treatments available. This review examines the landscape of novel therapeutic strategies for AD, focusing on the shortcomings of traditional therapies against amyloid-beta (Aβ) and exploring emerging alternatives. Despite decades of research emphasizing the role of Aβ accumulation in AD pathogenesis, clinical trials targeting Aβ have obtained disappointing results, highlighting the complexity of AD pathophysiology and the need for investigating other therapeutic approaches. In this manuscript, we first discuss the challenges associated with anti-Aβ therapies, including limited efficacy and potential adverse effects, underscoring the necessity of exploring alternative mechanisms and targets. Thereafter, we review promising non-Aβ-based strategies, such as tau-targeted therapies, neuroinflammation modulation, and gene and stem cell therapy. These approaches offer new avenues for AD treatment by addressing additional pathological hallmarks and downstream effects beyond Aβ deposition.

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“…Drugs targeting microtubule-associated protein tau, the primary component of neurofibrillary tangles found in AD, are excellent candidates. Tau reduction using antisense oligonucleotides improved tau biomarkers in a Phase 1 clinical trial (Mummery et al, 2023;Edwards et al, 2023) and a Phase 2 trial is underway (NCT05399888).…”

Section: Introductionmentioning

confidence: 99%

Excitoprotective effects of conditional tau reduction in excitatory neurons and in adulthood

Voskobiynyk,

Li,

Cochran

et al. 2024

Preprint

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Tau reduction is a promising therapeutic strategy for Alzheimer's disease. In numerous models, tau reduction via genetic knockout is beneficial, at least in part due to protection against hyperexcitability and seizures, but the underlying mechanisms are unclear. Here we describe the generation and initial study of a new conditional Tauflox model to address these mechanisms. Given the protective effects of tau reduction against hyperexcitability, we compared the effects of selective tau reduction in excitatory or inhibitory neurons. Tau reduction in excitatory neurons mimicked the protective effects of global tau reduction, while tau reduction in inhibitory neurons had the opposite effect and increased seizure susceptibility. Since most prior studies used knockout mice lacking tau throughout development, we crossed Tauflox mice with inducible Cre mice and found beneficial effects of tau reduction in adulthood. Our findings support the effectiveness of tau reduction in adulthood and indicate that excitatory neurons may be a key site for its excitoprotective effects.

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Exploratory Tau Biomarker Results From a Multiple Ascending-Dose Study of BIIB080 in Alzheimer Disease

Cited by 10 publications

References 24 publications

Considerations for biomarker strategies in clinical trials investigating tau-targeting therapeutics for Alzheimer’s disease

Considerations for biomarker strategies in clinical trials investigating tau-targeting therapeutics for Alzheimer’s disease

Novel Therapeutic Strategies in Alzheimer’s Disease: Pitfalls and Challenges of Anti-Amyloid Therapies and Beyond

Excitoprotective effects of conditional tau reduction in excitatory neurons and in adulthood

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