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Literature DB >> 31311649

HIV protease inhibitors block parasite signal peptide peptidases and prevent growth of Babesia microti parasites in erythrocytes.

Christopher Schwake¹, Michael R Baldwin², William Bachovchin³, Shreeya Hegde⁴, James Schiemer², Carolyn Okure⁴, Andrew E Levin⁵, Edouard Vannier⁶, Toshihiko Hanada⁷, Athar H Chishti⁸.

Abstract

Malaria and babesiosis are bloodborne protozoan infections for which the emergence of drug-resistant strains poses a threat. Our previous phage display cDNA screens established the essentiality of Plasmodium falciparum signal peptide peptidase (SPP) in asexual development at the blood stage of malaria infection. Given the structural similarities between SPP inhibitors and HIV protease inhibitors, we screened ten HIV protease inhibitors and selected Lopinavir and Atazanavir for their ability to inhibit PfSPP activity. Using a transcription-based assay, we observed that Lopinavir inhibits both parasite-and host-derived SPP activities whereas Atazanavir inhibited only parasite derived SPP activity. Consistent with their inhibitory effect on Plasmodium growth, both Lopinavir and Atazanavir strongly inhibited intraerythrocytic Babesia microti growth ex vivo. Moreover, Lopinavir prevented the steep rise in Babesia microti parasitemia typically observed in rag1-deficient mice. Our data provide first evidence that inhibition of parasite-derived SPPs by HIV protease inhibitors offers a promising therapeutic avenue for the treatment of severe babesiosis and infections caused by other Apicomplexa parasites.

Entities: CellLine Chemical Disease Gene Species

Keywords: Atazanavir; Babesia microti; Erythrocyte; HIV protease inhibitor; Lopinavir; Signal peptide peptidase (SPP)

Mesh：

Substances：

Year: 2019 PMID： 31311649 PMCID： PMC6707064 DOI： 10.1016/j.bbrc.2019.07.031

Source DB: PubMed Journal: Biochem Biophys Res Commun ISSN： 0006-291X Impact factor: 3.575

36 in total

Review 1. Nonclinical vehicle use in studies by multiple routes in multiple species.

Authors: Shayne C Gad; Crystal D Cassidy; Nicolas Aubert; Bart Spainhour; Heide Robbe
Journal: Int J Toxicol Date: 2006 Nov-Dec Impact factor: 2.032

2. Potencies of human immunodeficiency virus protease inhibitors in vitro against Plasmodium falciparum and in vivo against murine malaria.

Authors: Katherine T Andrews; David P Fairlie; Praveen K Madala; John Ray; David M Wyatt; Petrina M Hilton; Lewis A Melville; Lynette Beattie; Donald L Gardiner; Robert C Reid; Martin J Stoermer; Tina Skinner-Adams; Colin Berry; James S McCarthy
Journal: Antimicrob Agents Chemother Date: 2006-02 Impact factor: 5.191

3. Intramembrane proteolytic cleavage by human signal peptide peptidase like 3 and malaria signal peptide peptidase.

Authors: Andrew C Nyborg; Thomas B Ladd; Karen Jansen; Thomas Kukar; Todd E Golde
Journal: FASEB J Date: 2006-08 Impact factor: 5.191

4. Babesia microti primarily invades mature erythrocytes in mice.

Authors: Ingo Borggraefe; Jie Yuan; Sam R Telford; Sanjay Menon; Rouette Hunter; Sohela Shah; Andrew Spielman; Jeffrey A Gelfand; Henry H Wortis; Edouard Vannier
Journal: Infect Immun Date: 2006-06 Impact factor: 3.441

5. Antimalarial activity of human immunodeficiency virus type 1 protease inhibitors.

Authors: Sunil Parikh; Jiri Gut; Eva Istvan; Daniel E Goldberg; Diane V Havlir; Philip J Rosenthal
Journal: Antimicrob Agents Chemother Date: 2005-07 Impact factor: 5.191

6. Consensus analysis of signal peptide peptidase and homologous human aspartic proteases reveals opposite topology of catalytic domains compared with presenilins.

Authors: Elena Friedmann; Marius K Lemberg; Andreas Weihofen; Kumlesh K Dev; Uwe Dengler; Giorgio Rovelli; Bruno Martoglio
Journal: J Biol Chem Date: 2004-09-21 Impact factor: 5.157

7. Dematin and adducin provide a novel link between the spectrin cytoskeleton and human erythrocyte membrane by directly interacting with glucose transporter-1.

Authors: Anwar A Khan; Toshihiko Hanada; Morvarid Mohseni; Jong-Jin Jeong; Lixiao Zeng; Massimiliano Gaetani; Donghai Li; Brent C Reed; David W Speicher; Athar H Chishti
Journal: J Biol Chem Date: 2008-03-17 Impact factor: 5.157

HIV protease inhibitors block parasite signal peptide peptidases and prevent growth of Babesia microti parasites in erythrocytes.

Review 1. Nonclinical vehicle use in studies by multiple routes in multiple species.

2. Potencies of human immunodeficiency virus protease inhibitors in vitro against Plasmodium falciparum and in vivo against murine malaria.

3. Intramembrane proteolytic cleavage by human signal peptide peptidase like 3 and malaria signal peptide peptidase.

4. Babesia microti primarily invades mature erythrocytes in mice.

5. Antimalarial activity of human immunodeficiency virus type 1 protease inhibitors.

6. Consensus analysis of signal peptide peptidase and homologous human aspartic proteases reveals opposite topology of catalytic domains compared with presenilins.

7. Dematin and adducin provide a novel link between the spectrin cytoskeleton and human erythrocyte membrane by directly interacting with glucose transporter-1.

8. A Presenilin-like protease associated with Plasmodium falciparum micronemes is involved in erythrocyte invasion.

9. Identification of signal peptide peptidase, a presenilin-type aspartic protease.

10. HIV protease inhibitors inhibit the development of preerythrocytic-stage plasmodium parasites.

Review 1. Malaria parasite plasmepsins: More than just plain old degradative pepsins.

Review 2. Signal peptide peptidase: a potential therapeutic target for parasitic and viral infections.