Structural modeling identifies Plasmodium vivax 4-diphosphocytidyl-2C-methyl-d-erythritol kinase (IspE) as a plausible new antimalarial drug target

Kavita Kadian; Sonam Vijay; Yash Gupta; Ritu Rawal; Jagbir Singh; Anup Anvikar; Veena Pande; Arun Sharma

doi:10.1016/j.parint.2018.03.001

Structural modeling identifies Plasmodium vivax 4-diphosphocytidyl-2C-methyl-d-erythritol kinase (IspE) as a plausible new antimalarial drug target

Parasitol Int. 2018 Aug;67(4):375-385. doi: 10.1016/j.parint.2018.03.001. Epub 2018 Mar 14.

Authors

Kavita Kadian¹, Sonam Vijay¹, Yash Gupta¹, Ritu Rawal¹, Jagbir Singh¹, Anup Anvikar², Veena Pande³, Arun Sharma⁴

Affiliations

¹ Protein Biochemistry and Structural Biology Laboratory, National Institute of Malaria Research (ICMR), Sector-8, Dwarka, New Delhi, India.
² Epidemiology and Clinical Research, National Institute of Malaria Research (ICMR), Sector-8, Dwarka, New Delhi, India.
³ Department of Biotechnology, Kumaun University, Nainital, Uttarakhand, India.
⁴ Protein Biochemistry and Structural Biology Laboratory, National Institute of Malaria Research (ICMR), Sector-8, Dwarka, New Delhi, India. Electronic address: arushar@gmail.com.

PMID: 29550587
DOI: 10.1016/j.parint.2018.03.001

Abstract

Malaria parasites utilize Methylerythritol phosphate (MEP) pathway for synthesis of isoprenoid precursors which are essential for maturation and survival of parasites during erythrocytic and gametocytic stages. The absence of MEP pathway in the human host establishes MEP pathway enzymes as a repertoire of essential drug targets. The fourth enzyme, 4-diphosphocytidyl-2C-methyl-d-erythritol kinase (IspE) has been proved essential in pathogenic bacteria, however; it has not yet been studied in any Plasmodium species. This study was undertaken to investigate genetic polymorphism and concomitant structural implications of the Plasmodium vivax IspE (PvIspE) by employing sequencing, modeling and bioinformatics approach. We report that PvIspE gene displayed six non-synonymous mutations which were restricted to non-conserved regions within the gene from seven topographically distinct malaria-endemic regions of India. Phylogenetic studies reflected that PvIspE occupies unique status within Plasmodia genus and reflects that Plasmodium vivax IspE gene has a distant and non-conserved relation with human ortholog Mevalonate Kinase (MAVK). Structural modeling analysis revealed that all PvIspE Indian isolates have critically conserved canonical galacto-homoserine-mevalonate-phosphomevalonate kinase (GHMP) domain within the active site lying in a deep cleft sandwiched between ATP and CDPME-binding domains. The active core region was highly conserved among all clinical isolates, may be due to >60% β-pleated rigid architecture. The mapped structural analysis revealed the critically conserved active site of PvIspE, both sequence, and spacially among all Indian isolates; showing no significant changes in the active site. Our study strengthens the candidature of Plasmodium vivax IspE enzyme as a future target for novel antimalarials.

Keywords: 4-Diphosphocytidyl-2C-methyl-d-erythritol kinase (IspE) gene; Antimalarial; Drug target; Genetic diversity; Methylerythritol phosphate (MEP) pathway; Molecular modeling; Phylogenetic analysis; Plasmodium vivax.

MeSH terms

Antimalarials / pharmacology*
Catalytic Domain
Computational Biology
Drug Delivery Systems / methods*
Erythritol / analogs & derivatives*
Erythritol / chemistry
Erythritol / metabolism
Genetic Variation
Humans
India
Kinetics
Malaria, Vivax / parasitology
Models, Structural*
Phosphotransferases (Alcohol Group Acceptor) / drug effects
Phosphotransferases / drug effects
Phosphotransferases / genetics
Phylogeny
Plasmodium vivax / chemistry
Plasmodium vivax / drug effects*
Plasmodium vivax / enzymology*
Plasmodium vivax / genetics
Polymorphism, Genetic
Protozoan Proteins / genetics

Substances

4-diphosphocytidyl-2-C-methylerythritol
Antimalarials
Protozoan Proteins
Phosphotransferases
Phosphotransferases (Alcohol Group Acceptor)
erythritol kinase
Erythritol