RESUMEN
Alzheimer's disease (AD) is a progressive neurological illness with few effective treatments. Thus, ameliorating the effects of AD using natural products has attracted global attention with promising efficacy and safety. In this study, ten tropical fruits including Ananas comosus 'Phulae', Ananas comosus 'Pattavia', Carica papaya 'Khaekdum', Carica papaya 'Khaeknuan', Durio zibethinus 'Monthong', Durio zibethinus 'Chanee', Psidium guajava 'Kimju', Psidium guajava 'Keenok', Mangifera indica 'Kaew' and Mangifera indica 'Namdokmai' were screened for their inhibitory activities against the key enzymes, cholinesterases and ß-secretase (BACE-1), involved in AD pathogenesis. The top three fruit extracts with promising in vitro anti-AD activities were further investigated using rat pheochromocytoma PC-12 neuronal cell line and Drosophila AD model. Data showed that M. indica 'Kaew', M. indica 'Namdokmai' and P. guajava 'Kimju' reduced Aß1-42-mediated neurotoxicity by promoting glutathione-dependent enzymes, while M. indica 'Namdokmai' limited Aß1-42 peptide formation via BACE-1 inhibition and amended locomotory behavior of the Drosophila AD model. Results indicated the potential anti-AD properties of tropical fruits, particularly M. indica 'Namdokmai' in the prevention of Aß1-42-mediated neurotoxicity and as a BACE-1 blocker.
RESUMEN
Alzheimer's disease (AD), one type of dementia, is a complex disease affecting people globally with limited drug treatment. Thus, natural products are currently of interest as promising candidates because of their cost-effectiveness and multi-target abilities. Diplazium esculentum (Retz.) Sw., an edible fern, inhibited acetylcholinesterase in vitro, inferring that it might be a promising candidate for AD treatment by supporting cholinergic neurons. However, evidence demonstrating anti-AD properties of this edible plant via inhibiting of neurotoxic peptides production, amyloid beta (Aß), both in vitro and in vivo is lacking. Thus, the anti-AD properties of D. esculentum extract both in vitro and in Drosophila models of Aß-mediated toxicity were elucidated. Findings showed that an ethanolic extract exhibited high phenolics and flavonoids, contributing to antioxidant and inhibitory activities against AD-related enzymes. Notably, the extract acted as a BACE-1 blocker and reduced amyloid beta 42 (Aß42) peptides in Drosophila models, resulting in improved locomotor behaviors. Information gained from this study suggested that D. esculentum showed potential for AD amelioration and prevention. Further investigations in vertebrates or humans are required to determine the effective doses of D. esculentum against AD, particularly via amyloidogenic pathway.
