AI Article Synopsis

  • - The crystal structure of cathepsin B (CTSB) was revealed in the early 90s, leading to insights into its diverse catalytic roles in physiological processes and how these roles can switch under different conditions.
  • - Over-expression of CTSB is linked to multiple diseases, including Alzheimer's and cancer, prompting increased research interest and the development of CTSB inhibitors for potential treatments.
  • - This review focuses on the inhibition potential of natural and synthetic heterocyclic compounds against CTSB, providing valuable information for researchers in molecular modeling and drug development.

Article Abstract

The identification of x-ray crystal structure of cathepsin B (CTSB) in the early 90's enabled researchers to embark on a journey to understand and demystify its multiple catalytic mechanisms (endopeptidase/carboxypeptidase/peptidyl-dipeptidase) in diverse physiological processes and their switching into one another under different conditions. The engagement of CTSB in different pathological conditions due to its over-expression further highlighted the enhanced research interest around the domain. The occurrence of over-expressed CTSB in various diseases like Alzheimer's, cancer, arthritis, cardiovascular, etc., and the use of CTSB inhibitors for the treatment of these diseases have established its involvement in different pathological conditions. Such an understanding tempted researchers to design, synthesize, and screen diverse classes of compounds against CTSB. This in turn, helped in understanding their interactions with the active sites of the enzyme. Heterocyclic compounds comprise a very rich and broad class of medicinally important compounds that also hold great potential for CTSB inhibition. This review covers the CTSB inhibition potential of various natural and synthetic heterocyclic scaffolds. Researchers working in the fields of molecular modeling, drug design and development, and enzyme inhibitors can benefit significantly from this review.

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http://dx.doi.org/10.1016/j.ijbiomac.2022.10.017DOI Listing

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