Rebalancing β-Amyloid-Induced Decrease of ATP Level by Amorphous Nano/Micro Polyphosphate: Suppression of the Neurotoxic Effect of Amyloid β-Protein Fragment 25-35

6533b831fe1ef96bd12998dd

RESEARCH PRODUCT

Rebalancing β-Amyloid-Induced Decrease of ATP Level by Amorphous Nano/Micro Polyphosphate: Suppression of the Neurotoxic Effect of Amyloid β-Protein Fragment 25-35

Werner E.g. Müller Shunfeng Wang Renate Steffen Rafael Muñoz-espí Heinz C. Schröder Qingling Feng Meik Neufurth Xiaohong Wang Maximilian Ackermann Egherta Mecja

subject

Calcium Phosphates 0301 basic medicine Intracellular Space Peptide lcsh:Chemistry chemistry.chemical_compound Adenosine Triphosphate X-Ray Diffraction Polyphosphates Spectroscopy Fourier Transform Infrared primary rat cortex neurons lcsh:QH301-705.5 Spectroscopy Cerebral Cortex Neurons chemistry.chemical_classification microparticles Chemistry β-amyloid General Medicine pathological conditions signs and symptoms Computer Science Applications neurotoxic effect surgical procedures operative Biochemistry Alzheimer's disease Intracellular Cell Survival β-amyloid; calcium polyphosphate; microparticles; neurotoxic effect; adenosine triphosphate level; PC12 cells; primary rat cortex neurons Article Catalysis Inorganic Chemistry 03 medical and health sciences medicine Extracellular otorhinolaryngologic diseases Animals Physical and Theoretical Chemistry Molecular Biology neoplasms Amyloid beta-Peptides Polyphosphate Organic Chemistry Neurotoxicity PC12 cells medicine.disease In vitro digestive system diseases Rats 030104 developmental biology lcsh:Biology (General)lcsh:QD1-999 Biophysics Nanoparticles Adenosine triphosphate calcium polyphosphate adenosine triphosphate level

description

Morbus Alzheimer neuropathology is characterized by an impaired energy homeostasis of brain tissue. We present an approach towards a potential therapy of Alzheimer disease based on the high-energy polymer inorganic polyphosphate (polyP), which physiologically occurs both in the extracellular and in the intracellular space. Rat pheochromocytoma (PC) 12 cells, as well as rat primary cortical neurons were exposed to the Alzheimer peptide Aβ25-35. They were incubated in vitro with polyphosphate (polyP); ortho-phosphate was used as a control. The polymer remained as Na+ salt; or complexed in a stoichiometric ratio to Ca2+ (Na-polyP[Ca2+]); or was processed as amorphous Ca-polyP microparticles (Ca-polyP-MP). Ortho-phosphate was fabricated as crystalline Ca-phosphate nanoparticles (Ca-phosphate-NP). We show that the pre-incubation of PC12 cells and primary cortical neurons with polyP protects the cells against the neurotoxic effect of the Alzheimer peptide Aβ25-35. The strongest effect was observed with amorphous polyP microparticles (Ca-polyP-MP). The effect of the soluble sodium salt; Na-polyP (Na-polyP[Ca2+]) was lower; while crystalline orthophosphate nanoparticles (Ca-phosphate-NP) were ineffective. Ca-polyP-MP microparticles and Na-polyP[Ca2+] were found to markedly enhance the intracellular ATP level. Pre-incubation of Aβ25-35 during aggregate formation, with the polyP preparation before exposure of the cells, had a small effect on neurotoxicity. We conclude that recovery of the compromised energy status in neuronal cells by administration of nontoxic biodegradable Ca-salts of polyP reverse the β-amyloid-induced decrease of adenosine triphosphate (ATP) level. This study contributes to a new routes for a potential therapeutic intervention in Alzheimer’s disease pathophysiology.

year	journal	country	edition	language
2017-10-01	International Journal of Molecular Sciences

10.3390/ijms18102154 https://www.mdpi.com/1422-0067/18/10/2154