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Analysing the essential proteins set of Plasmodium falciparum PF3D7 for novel drug targets identification against malaria.
Ali, Fawad; Wali, Hira; Jan, Saadia; Zia, Asad; Aslam, Muneeba; Ahmad, Imtiaz; Afridi, Sahib Gul; Shams, Sulaiman; Khan, Asifullah.
Afiliação
  • Ali F; Department of Biochemistry, Abdul Wali Khan University Mardan, Mardan, 23200, Pakistan.
  • Wali H; Department of Biochemistry, Hazara University, Mansehra, 21120, Pakistan.
  • Jan S; Department of Biochemistry, Abdul Wali Khan University Mardan, Mardan, 23200, Pakistan.
  • Zia A; Department of Biochemistry, Abdul Wali Khan University Mardan, Mardan, 23200, Pakistan.
  • Aslam M; Department of Biochemistry, Abdul Wali Khan University Mardan, Mardan, 23200, Pakistan.
  • Ahmad I; Department of Biochemistry, Abdul Wali Khan University Mardan, Mardan, 23200, Pakistan.
  • Afridi SG; Department of Biochemistry, Abdul Wali Khan University Mardan, Mardan, 23200, Pakistan.
  • Shams S; Department of Biochemistry, Abdul Wali Khan University Mardan, Mardan, 23200, Pakistan.
  • Khan A; Department of Biochemistry, Abdul Wali Khan University Mardan, Mardan, 23200, Pakistan.
Malar J ; 20(1): 335, 2021 Aug 03.
Article em En | MEDLINE | ID: mdl-34344361
ABSTRACT

BACKGROUND:

Plasmodium falciparum is an obligate intracellular parasite of humans that causes malaria. Falciparum malaria is a major public health threat to human life responsible for high mortality. Currently, the risk of multi-drug resistance of P. falciparum is rapidly increasing. There is a need to address new anti-malarial therapeutics strategies to combat the drug-resistance threat.

METHODS:

The P. falciparum essential proteins were retrieved from the recently published studies. These proteins were initially scanned against human host and its gut microbiome proteome sets by comparative proteomics analyses. The human host non-homologs essential proteins of P. falciparum were additionally analysed for druggability potential via in silico methods to possibly identify novel therapeutic targets. Finally, the PfAp4AH target was prioritized for pharmacophore modelling based virtual screening and molecular docking analyses to identify potent inhibitors from drug-like compounds databases.

RESULTS:

The analyses identified six P. falciparum essential and human host non-homolog proteins that follow the key druggability features. These druggable targets have not been catalogued so far in the Drugbank repository. These prioritized proteins seem novel and promising drug targets against P. falciparum due to their key protein-protein interactions features in pathogen-specific biological pathways and to hold appropriate drug-like molecule binding pockets. The pharmacophore features based virtual screening of Pharmit resource predicted a lead compound i.e. MolPort-045-917-542 as a promising inhibitor of PfAp4AH among prioritized targets.

CONCLUSION:

The prioritized protein targets may worthy to test in malarial drug discovery programme to overcome the anti-malarial resistance issues. The in-vitro and in-vivo studies might be promising for additional validation of these prioritized lists of drug targets against malaria.
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Texto completo: 1 Base de dados: MEDLINE Assunto principal: Plasmodium falciparum / Proteínas de Protozoários / Malária Falciparum Tipo de estudo: Diagnostic_studies / Prognostic_studies Limite: Humans Idioma: En Ano de publicação: 2021 Tipo de documento: Article
Texto completo
Imprimir
XML
PubMed Links
Buscar no Google

Texto completo: 1 Base de dados: MEDLINE Assunto principal: Plasmodium falciparum / Proteínas de Protozoários / Malária Falciparum Tipo de estudo: Diagnostic_studies / Prognostic_studies Limite: Humans Idioma: En Ano de publicação: 2021 Tipo de documento: Article