Abstract
AbstractSchistosomiasis is a neglected parasitosis caused by Schistosoma spp. Praziquantel is used for the chemoprophylaxis and treatment of this disease. Although this monotherapy is effective, the risk of resistance and its low efficiency against immature worms compromises its effectiveness. Therefore, it is necessary to develop new schistosomicide drugs. However, the development of new drugs is a long and expensive process. The repositioning of approved drugs has been proposed as a quick, cheap, and effective alternative to solve this problem. This study employs chemogenomic analysis with use of bioinformatics tools to search, identify, and analyze data on approved drugs with the potential to inhibit Schistosoma mansoni energy metabolism enzymes. The TDR Targets Database, Gene DB, Protein, DrugBank, Therapeutic Targets Database (TTD), Promiscuous, and PubMed databases were used. Fifty-nine target proteins were identified, of which 18 had one or more approved drugs. The results identified 20 potential drugs for schistosomiasis treatment, all approved for use in humans.
Publisher
Cold Spring Harbor Laboratory
Reference37 articles.
1. Schistosomiasis and soiltransmitted helminthiases: number of people treated in 2016;World Health Organization;Wkly Epidemiol Rec,2017
2. World Health Organization. Preventive chemotherapy for helminth diseases: progress report, 2014. Wkly Epidemiol Rec. 2016; 89–104.
3. Praziquantel Treatment in Trematode and Cestode Infections: An Update
4. Praziquantel: mechanisms of action, resistance and new derivatives for schistosomiasis
5. Antischistosomal activity of a calcium channel antagonist on schistosomula and adult Schistosoma mansoni worms