From Tg O/GABA-AT, GABA, and T-263 Mutant to Conception of Toxoplasma

从 Tg O/GABA-AT、GABA 和 T-263 突变体到弓形虫的受孕

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作者:Joseph Lykins, Matthew J Moschitto, Ying Zhou, Ekaterina V Filippova, Hoang V Le, Tadakimi Tomita, Barbara A Fox, David J Bzik, Chunlei Su, Seesandra V Rajagopala, Kristin Flores, Furio Spano, Stuart Woods, Craig W Roberts, Cong Hua, Kamal El Bissati, Kelsey M Wheeler, Sarah Dovgin, Stephen P Muench

Abstract

Toxoplasma gondii causes morbidity, mortality, and disseminates widely via cat sexual stages. Here, we find T. gondii ornithine aminotransferase (OAT) is conserved across phyla. We solve TgO/GABA-AT structures with bound inactivators at 1.55 Å and identify an inactivator selective for TgO/GABA-AT over human OAT and GABA-AT. However, abrogating TgO/GABA-AT genetically does not diminish replication, virulence, cyst-formation, or eliminate cat's oocyst shedding. Increased sporozoite/merozoite TgO/GABA-AT expression led to our study of a mutagenized clone with oocyst formation blocked, arresting after forming male and female gametes, with "Rosetta stone"-like mutations in genes expressed in merozoites. Mutations are similar to those in organisms from plants to mammals, causing defects in conception and zygote formation, affecting merozoite capacitation, pH/ionicity/sodium-GABA concentrations, drawing attention to cyclic AMP/PKA, and genes enhancing energy or substrate formation in TgO/GABA-AT-related-pathways. These candidates potentially influence merozoite's capacity to make gametes that fuse to become zygotes, thereby contaminating environments and causing disease.

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