Ernesto Calderón-Jaimes scite author profile

Giardiasis is a worldwide parasitic disease that affects mainly children and immunosuppressed people. Side effects and the emergence of resistance over current used drugs make imperative looking for new antiparasitics through discovering of new biological targets and designing of novel drugs. Recently, it has determined that gastric proton-pump inhibitors (PPI) have anti-giardiasic activity. The glycolytic enzyme, triosephosphate isomerase (GlTIM), is one of its potential targets. Therefore, we employed the scaffold of PPI to design new compounds aimed to increase their antigiardial capacity by inactivating GlTIM. Here we demonstrated that two novel PPI-derivatives (BHO2 and BHO3), have better anti-giardiasic activity than omeprazole in concentrations around 120–130 µM, without cytotoxic effect on mammal cell cultures. The derivatives inactivated GlTIM through the chemical modification of Cys222 promoting local structural changes in the enzyme. Furthermore, derivatives forms adducts linked to Cys residues through a C-S bond. We demonstrated that PPI can be used as scaffolds to design better antiparasitic molecules; we also are proposing a molecular mechanism of reaction for these novel derivatives.

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Cervicovaginal Infection with Group B Streptococci Among Pregnant Mexican Women

Solórzano-Santos¹,

Echániz-Avilés²,

Conde-Glez³

et al. 1989

Journal of Infectious Diseases

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Prevalence, Incidence, and Determinants of Syphilis in Female Commercial Sex Workers in Mexico City

Uribe-Salas

C²,

Cj³

et al. 1996

Sexually Transmitted Diseases

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