TY - JOUR
T1 - Tau-Centric Targets and Drugs in Clinical Development for the Treatment of Alzheimer's Disease
AU - Panza, Francesco
AU - Solfrizzi, Vincenzo
AU - Seripa, Davide
AU - Imbimbo, Bruno P.
AU - Lozupone, Madia
AU - Santamato, Andrea
AU - Zecca, Chiara
AU - Barulli, Maria Rosaria
AU - Bellomo, Antonello
AU - Pilotto, Alberto
AU - Daniele, Antonio
AU - Greco, Antonio
AU - Logroscino, Giancarlo
PY - 2016
Y1 - 2016
N2 - The failure of several Phase II/III clinical trials in Alzheimer's disease (AD) with drugs targeting β-amyloid accumulation in the brain fuelled an increasing interest in alternative treatments against tau pathology, including approaches targeting tau phosphatases/kinases, active and passive immunization, and anti-tau aggregation. The most advanced tau aggregation inhibitor (TAI) is methylthioninium (MT), a drug existing in equilibrium between a reduced (leuco-methylthioninium) and oxidized form (MT+). MT chloride (methylene blue) was investigated in a 24-week Phase II clinical trial in 321 patients with mild to moderate AD that failed to show significant positive effects in mild AD patients, although long-term observations (50 weeks) and biomarker studies suggested possible benefit. The dose of 138 mg/day showed potential benefits on cognitive performance of moderately affected AD patients and cerebral blood flow in mildly affected patients. Further clinical evidence will come from the large ongoing Phase III trials for the treatment of AD and the behavioral variant of frontotemporal dementia on a new form of this TAI, more bioavailable and less toxic at higher doses, called TRx0237. More recently, inhibitors of tau acetylation are being actively pursued based on impressive results in animal studies obtained by salsalate, a clinically used derivative of salicylic acid.
AB - The failure of several Phase II/III clinical trials in Alzheimer's disease (AD) with drugs targeting β-amyloid accumulation in the brain fuelled an increasing interest in alternative treatments against tau pathology, including approaches targeting tau phosphatases/kinases, active and passive immunization, and anti-tau aggregation. The most advanced tau aggregation inhibitor (TAI) is methylthioninium (MT), a drug existing in equilibrium between a reduced (leuco-methylthioninium) and oxidized form (MT+). MT chloride (methylene blue) was investigated in a 24-week Phase II clinical trial in 321 patients with mild to moderate AD that failed to show significant positive effects in mild AD patients, although long-term observations (50 weeks) and biomarker studies suggested possible benefit. The dose of 138 mg/day showed potential benefits on cognitive performance of moderately affected AD patients and cerebral blood flow in mildly affected patients. Further clinical evidence will come from the large ongoing Phase III trials for the treatment of AD and the behavioral variant of frontotemporal dementia on a new form of this TAI, more bioavailable and less toxic at higher doses, called TRx0237. More recently, inhibitors of tau acetylation are being actively pursued based on impressive results in animal studies obtained by salsalate, a clinically used derivative of salicylic acid.
KW - Alzheimer Disease
KW - Biochemistry, Genetics and Molecular Biology (all)
KW - Brain
KW - Evidence-Based Medicine
KW - Humans
KW - Immunology and Microbiology (all)
KW - Methylene Blue
KW - Molecular Targeted Therapy
KW - Neuroprotective Agents
KW - Treatment Outcome
KW - tau Proteins
KW - Alzheimer Disease
KW - Biochemistry, Genetics and Molecular Biology (all)
KW - Brain
KW - Evidence-Based Medicine
KW - Humans
KW - Immunology and Microbiology (all)
KW - Methylene Blue
KW - Molecular Targeted Therapy
KW - Neuroprotective Agents
KW - Treatment Outcome
KW - tau Proteins
UR - http://hdl.handle.net/10807/95328
UR - http://www.hindawi.com/journals/biomed/
U2 - 10.1155/2016/3245935
DO - 10.1155/2016/3245935
M3 - Article
SN - 2314-6133
VL - 2016
SP - N/A-N/A
JO - BioMed Research International
JF - BioMed Research International
ER -