Literature DB >> 31513773

A Family of Dual-Activity Glycosyltransferase-Phosphorylases Mediates Mannogen Turnover and Virulence in Leishmania Parasites.

M Fleur Sernee1, Julie E Ralton1, Tracy L Nero2, Lukasz F Sobala3, Joachim Kloehn1, Marcel A Vieira-Lara1, Simon A Cobbold1, Lauren Stanton1, Douglas E V Pires1, Eric Hanssen4, Alexandra Males3, Tom Ward3, Laurence M Bastidas3, Phillip L van der Peet5, Michael W Parker2, David B Ascher1, Spencer J Williams5, Gideon J Davies3, Malcolm J McConville6.   

Abstract

Parasitic protists belonging to the genus Leishmania synthesize the non-canonical carbohydrate reserve, mannogen, which is composed of β-1,2-mannan oligosaccharides. Here, we identify a class of dual-activity mannosyltransferase/phosphorylases (MTPs) that catalyze both the sugar nucleotide-dependent biosynthesis and phosphorolytic turnover of mannogen. Structural and phylogenic analysis shows that while the MTPs are structurally related to bacterial mannan phosphorylases, they constitute a distinct family of glycosyltransferases (GT108) that have likely been acquired by horizontal gene transfer from gram-positive bacteria. The seven MTPs catalyze the constitutive synthesis and turnover of mannogen. This metabolic rheostat protects obligate intracellular parasite stages from nutrient excess, and is essential for thermotolerance and parasite infectivity in the mammalian host. Our results suggest that the acquisition and expansion of the MTP family in Leishmania increased the metabolic flexibility of these protists and contributed to their capacity to colonize new host niches.
Copyright © 2019 The Authors. Published by Elsevier Inc. All rights reserved.

Entities:  

Keywords:  GT108; X-ray crystallography; carbohydrate reserve; central carbon metabolism; glycan phosphorylase; glycosyltransferase; horizontal gene transfer; mannan; parasite pathogenesis

Mesh:

Substances:

Year:  2019        PMID: 31513773     DOI: 10.1016/j.chom.2019.08.009

Source DB:  PubMed          Journal:  Cell Host Microbe        ISSN: 1931-3128            Impact factor:   21.023


  11 in total

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3.  Mannogen-ing Central Carbon Metabolism by Leishmania.

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Journal:  Trends Parasitol       Date:  2019-10-26

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8.  Leishmania Encodes a Bacterium-like 2,4-Dienoyl-Coenzyme A Reductase That Is Required for Fatty Acid β-Oxidation and Intracellular Parasite Survival.

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9.  Transcriptional Shift and Metabolic Adaptations during Leishmania Quiescence Using Stationary Phase and Drug Pressure as Models.

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Review 10.  Discovery and Biotechnological Exploitation of Glycoside-Phosphorylases.

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