Universitat Internacional de Catalunya. Departament de Ciències Bàsiques
Brain lipid metabolism has a key role in many physiological processes, and its malfunction is associated with a plethora of diseases, such as obesity and glioblastoma multiforme (GBM). Carnitine palmitoyl transferase 1A (CPT1A), an important protein in the fatty acid oxidation (FAO) pathway, has a prominent role in this association. In the brain, activation of CPT1A in hypothalamic neurons increases food intake and body weight in mice, while its inhibition causes the opposite effect, indicating its antiobesity potential. In GBM cells, overexpression of CPT1A and other lipid metabolism proteins has been described as a crucial pathway for GBM cell survival. Then, pharmacological inhibition of CPT1A and therefore fatty acid oxidation, could constitute a promising treatment for these diseases. However, targeting CPT1A in brain cells is difficult to reach with the current formulations in vivo. The racemic drug Compound 75 (C75) is a well-known CPT1A inhibitor when conjugated with Coenzyme A, but with important constraints such as polarity and low cell-permeability that limit the cellular uptake.
Obesity; Glioblastoma Multiforme; Brain Lipid Metabolism; C75; PIC micelle; Nanocarrier; Metabolic disease; CPT1A; Hypothalamus; Arcuate nucleus
616.8 - Neurologia. Neuropatologia. Sistema nerviós
Ciències de la salut