Abstract

BackgroundLeishmaniasis is a disease caused by protozoan forms called Leishmania which infect animals and humans. The drugs have been in use since half a century due to which there have been mutations in the microbe-facilitating drug resistance. So this provides a reason for searching for effective drugs for the disease. In the current work, an effort has been to find such drugs that act on disease-relevant receptors by similarity indexing method, molecular docking, and dynamics studies. The study focused on the rapid expansion of potential anti-leishmanial compounds that could function as novel natural compound structures for future drugResultsSimilarity indexing of existing drugs with natural compounds using Tanimoto clustering resulted in 4 compounds with similarity index of greater than 0.7 (70% similarity). The molecular docking of the resulted compounds was carried out with therapeutic targets CYP51 and GP63 proteins. N-methyltyrosyl-N-methyltyrosyl-leucyl-alanine from Streptomyces griseus showed higher binding affinity in comparison to inhibitor and other selected natural compounds. Simulation studies revealed that the binding configuration of the compound with targets was highly stable all through 10 ns of simulation time with intact hydrogen bonding.ConclusionsThe molecular docking and molecular dynamics studies for the selected natural bioactive compound N-methyltyrosyl-N-methyltyrosyl-leucyl-alanine from Streptomyces griseus showed better binding affinity with the selected therapeutics targets and can be further considered for in vitro and in vivo studies which may lead to a possible new drug for the treatment of Leishmaniasis.

Highlights

  • Leishmaniasis is a disease caused by protozoan forms called Leishmania which infect animals and humans

  • Similarity indexing The results from similarity indexing were obtained in terms of similarity coefficient and based on the similarity coefficient values, and 4 compounds from natural compound databases were selected having similarity more than 70%, i.e., similarity coefficient more than 0.7 (Table 1)

  • The source of natural compounds was identified to be from bacteria, fungi, and plant family based on the literature, and the 2D structures of the compounds are given in figures (Fig. 4a-d)

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Summary

Introduction

Leishmaniasis is a disease caused by protozoan forms called Leishmania which infect animals and humans. The drugs have been in use since half a century due to which there have been mutations in the microbefacilitating drug resistance This provides a reason for searching for effective drugs for the disease. It is transmitted to humans by the bite of certain species of sand fly (subfamily Phlebotominae). It is transmitted through zoonosis and human infection is Yaraguppi et al Future Journal of Pharmaceutical Sciences. The disease is endemic in the eastern States of Bihar, Jharkhand, Uttar Pradesh, and West Bengal. It is marginalized communities living in rural poverty who bear the greatest disease burden [3]

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