Phycocyanobilin as a Functional Food-Derived Nutraceutical Candidate for Modulating the RAGE/NOX4 Axis in Neurodegenerative Disorders
Mei Chou Lai, Yu-Cheng Tzeng, Wayne Young Liu, I-Min Liu

TL;DR
This paper explores how phycocyanobilin, a compound from algae, may protect neurons from damage linked to diabetes and neurodegenerative diseases.
Contribution
The study identifies phycocyanobilin as a potential nutraceutical that modulates the RAGE/NOX4 pathway in neuronal stress.
Findings
Phycocyanobilin pretreatment improved neuronal viability and reduced oxidative stress in AGE-exposed neurons.
Phycocyanobilin suppressed RAGE and NOX4 expression and ER stress signaling.
The protective effects of phycocyanobilin were comparable to a known RAGE antagonist.
Abstract
Background/Objectives: Neurodegeneration associated with diabetes and metabolic dysfunction involves interconnected processes, including advanced glycation end product (AGE)-related signaling, RAGE/NOX4-dependent oxidative stress, dysregulated endoplasmic reticulum (ER) stress, and mitochondrial apoptosis. Phycocyanobilin (PCB), a tetrapyrrolic chromophore of C-phycocyanin, has been proposed to exert pleiotropic cytoprotective effects; however, its actions within glycation-associated neuronal stress pathways remain incompletely defined. Methods: Differentiated SH-SY5Y neurons were exposed to AGEs (300 μg/mL) for a 24 h period to examine whether PCB modulates neuronal injury along the RAGE–NOX4–oxidative-stress–ER-stress–mitochondrial axis. The selective RAGE antagonist TTP488 (100 μmol/L) was included as a pharmacological reference. Neuronal viability, neurite integrity, intracellular…
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Taxonomy
TopicsAdvanced Glycation End Products research · Ginkgo biloba and Cashew Applications · Flavonoids in Medical Research
