Affiliation:
1. Cell and developmental biology special, Department of Zoology, University of Kalyani, Kayani, Nadia- 741235, India
2. Department of Zoology, University of Calcutta, Kolkata- 700019, India
3. Cytogenetics and Molecular Biology Lab., Department of Zoology, University of Kalyani, Kalyani, Nadia- 741235, India
4. Department of Pharmaceutical Chemistry, Global Institute of Pharmaceutical Education and Research (Affiliated to Veer Madho Singh Bhandari Uttarakhand Technical University), Kashipur- 244713, India
Abstract
Abstract:
Synthetic drugs currently prescribed for the treatment of Human African Trypanosomiasis
(HAT) are non-specific, toxic, demand extended therapeutic regimes and are of varying
efficacy. Along with the challenging demographic and socio-economic hurdles, the everincreasing
risk of drug resistance is another major problem to be addressed. Cysteine protease,
Heat shock proteins (HSP-90), Trypanothione reductase (TR), Farnesyl diphosphate synthase,
Glucose-6-phosphate dehydrogenase, UP-4-galactose epimerase, and Cytidine triphosphate synthetase
are potential enzymatic targets for the development of novel inhibitors against HAT
which are the main focus of this review. The potential enzymatic targets of Trypanosoma brucei,
especially small molecules like cysteine proteases and heat shock proteins are identified as major
candidates for the sustenance of the parasite, their proliferation, infection, and spread of the disease.
The development of new compounds to combat the disease by thorough ligand modification
has been explored in the current review. Extracting these compounds and studying their efficacy,
toxicity, and target mechanism extensively, this review has proposed a list of different
compounds, including some synthetic and natural compounds along with multi-target inhibitors
such as acoziborole, fexinidazole, etc. Potential inhibitors against these enzymatic targets of the
T. brucei are important candidates for designing novel therapeutics against HAT. Multi-target
inhibitors have also been identified as crucial molecules because of their potential advantage
against the development of drug resistance.
method:
The potential enzymatic targets of Trypanosoma brucei, especially small molecules like cysteine proteases and heat shock proteins are identified as major candidates for the sustenance of the parasite, their proliferation, infection and spread of the disease. Development of new compounds to combat the disease by thorough ligand modification have been explored in the current review.
result:
Extracting these compounds and studying their efficacy, toxicity, and target mechanism extensively, this review have proposed a list of different compounds, including some synthetic and natural compounds along with multi-target inhibitors such as acoziborole, fexinidazole etc.
Publisher
Bentham Science Publishers Ltd.