Structure based molecular inhibition of Caspase-8 for treatment of multi-neurodegenerative diseases using known natural compounds.

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Neurodegenerative disorders are often associated with excessive neuronal apoptosis . It is well known that apoptosis is regulated by some intracellular proteases , such as , Caspases (cysteine-dependent , aspartate-specific proteases ). In fact , Caspase-8 which is an initiator caspase , has been identified as a key mediator of neuronal apoptosis . In addition , Caspase-8 is found to be coupled with the regulation of various neurodegenerative disorders including Alzheimer ׳s disease (AD ), Parkinson ׳s disease (PD ), Huntington ׳s Diseases (HD ) and Dentatorubral Pallidoluysian Atrophy (DRPLA ). Caspase-8 inhibition may provide an effective means of treatment for multiple neurodegenerative disorders . Therefore , the present study describes the molecular interaction of some selected natural compounds with known anti neurodegenerative properties with Caspase-8 . Docking between Caspase-8 and each of these compounds (separately ) was performed using 'Autodock 4 .2 '. Out of all the selected compounds , rosmarinic acid and curcumin proved to be the most potent inhibitors of Caspase-8 with binding energy (ΔG ) of -7 .10 Kcal /mol and -7 .08 Kcal /mol , respectively . However , further in vitro and in vivo studies are needed to validate the anti-neurodegenerative potential of these compounds .