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ALZ-801 has now progressed to the phase 3 APOLLOE4 study, designed to evaluate efficacy, safety, and biomarker and imaging effects.
In addition to the growing body of infusion-based treatments for Alzheimer disease, a new, oral option has shown encouraging results in clinical trials.
Valiltramiprosate (ALZ-801; Alzheon) is an investigational disease-modifying therapy currently in phase 3 development. When administered at the phase 3 clinical dose, ALZ-801 was able to fully block the formation of neurotoxic soluble beta amyloid (Ab) oligomers and has shown potential for patients with 2 copies of the apolipoprotein e4 allele (APOE4). This patient population is the focus of the 78-week APOLLOE4 phase 3 trial.1
“What’s striking is that all of these proteins that ultimately become toxic have a very important function in brain health, for normal brain function,” Martin Tolar, MD, PhD, founder, president, and CEO or Alzheon, said in an interview. “The monomeric amyloid, which is about 1% of our brains, is a system that protects the brain against injury, infection, stress, you name it. The problem…is if you lose the ability in your 40s and 50s to [effectively clear] these proteins from the brain.”
Importantly, 15% of patients with Alzheimer disease are APOE4/4 homozygous and two-thirds of patients are APOE4 carriers. This patient population can experience clinical onset as much as 10 years earlier than non-carriers, highlighting the significant unmet medical need for this subset of patients.2
In an open-label, multicenter, single-arm phase 2 biomarker trial, researchers found that there was a statistically significant and clinically relevant reduction in plasma biomarkers of neurodegeneration, preservation of brain volume, and encouraging cognitive effects in patients with early Alzheimer disease who are carriers of APOE4, following 24 months of treatment.1
At baseline, trial participants were 52% female with a mean age of 69 years, a mean Mini-Mental Status Examination (MMSE) score of 26 (range 22-30 years), and 70% with cognitive impairment. A total of 70 participants completed the week 104 visit and 68 provided evaluable plasma for biomarker assays, allowing inclusion in the study’s primary analysis.2 Participants received the ALZ-801 265 mg tablet once daily for 2 weeks and twice daily thereafter over the 104-week treatment period.1
Notably, investigators saw early, sustained, and statistically significant reductions in plasma P-tau181 reaching 31% at 24 months. They also observed 28% preservation of hippocampal volume compared with external controls of matched subjects, supporting the drug’s neuroprotective effects. Additionally, participants performed better on cognitive tests at 6 months and showed sustained stabilization of cognition above baseline for 24 months.1
In a news release, Tolar said, “[These data] reinforces our conviction that ALZ-801 has the potential to disrupt the Alzheimer treatment paradigm by halting the progression of this relentless and debilitating disease.”1
The study also showed a favorable safety profile with no events of vasogenic edema,1 which is particularly notable given the significant adverse effects seen with other investigational and available treatments for Alzheimer disease.
ALZ-801 has now progressed to the phase 3 APOLLOE4 study, designed to evaluate the efficacy, safety, and biomarker and imaging effects of ALZ-801 265 mg twice daily in patients with early Alzheimer disease and 2 copies of APOE4. Topline findings are expected in 2024.3
This 78-week study enrolled patients between the ages of 50 and 80 years with MMSE scores of 22 or greater and Clinical Dementia Rating-Global Scores of 0.5 or 1. In total, 325 participants were enrolled with a mean age of 60 years, 51% female, a mean MMSE of 25.6, and 65% cognitive impairment.3
Although the brain cannot regenerate, Tolar said ALZ-801 is showing exciting potential to prevent the accumulation of damage in patients with Alzheimer disease.
“Our goal has always been to have a treatment that can be used preventively for a very long time and in patients way before they have the onset of the clinically terminal stage of the disease,” Tolar said. “In clinical studies, with all of the anti-amyloid treatments that have shown efficacy, you have better efficacy the earlier you start treating. Now, we need to prove to regulatory agencies efficacy at the beginning of this terminal stage.”