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Article Dans Une Revue PLoS Biology Année : 2017

Extreme genome diversity in the hyper-prevalent parasitic eukaryote Blastocystis

Bruce Curtis
  • Fonction : Auteur
Courtney Stairs
Vladimír Klimeš
  • Fonction : Auteur
Marek Eliáš
  • Fonction : Auteur
Dayana Salas-Leiva
  • Fonction : Auteur
Emily Herman
  • Fonction : Auteur
Laura Eme
Maria Arias
  • Fonction : Auteur
Mary Klute
  • Fonction : Auteur
Hiroshi Suga
  • Fonction : Auteur
Shehre-Banoo Malik
  • Fonction : Auteur
Arthur Pightling
  • Fonction : Auteur
Martin Kolisko
Richard Rachubinski
  • Fonction : Auteur
Alexander Schlacht
  • Fonction : Auteur
Darren Soanes
  • Fonction : Auteur
Anastasios Tsaousis
John Archibald
  • Fonction : Auteur
C Graham Clark
Mark van Der Giezen
  • Fonction : Auteur
Andrew Roger

Résumé

Blastocystis is the most prevalent eukaryotic microbe colonizing the human gut, infecting approximately 1 billion individuals worldwide. Although Blastocystis has been linked to intestinal disorders, its pathogenicity remains controversial because most carriers are asymptomatic. Here, the genome sequence of Blastocystis subtype (ST) 1 is presented and compared to previously published sequences for ST4 and ST7. Despite a conserved core of genes, there is unexpected diversity between these STs in terms of their genome sizes, guanine-cytosine (GC) content, intron numbers, and gene content. ST1 has 6,544 protein-coding genes, which is several hundred more than reported for ST4 and ST7. The percentage of proteins unique to each ST ranges from 6.2% to 20.5%, greatly exceeding the differences observed within parasite genera. Orthologous proteins also display extreme divergence in amino acid sequence identity between STs (i.e., 59%-61% median identity), on par with observations of the most distantly related species pairs of parasite genera. The STs also display substantial variation in gene family distributions and sizes, especially for protein kinase and protease gene families, which could reflect differences in virulence. It remains to be seen to what extent these inter-ST differences persist at the intra-ST level. A full 26% of genes in ST1 have stop codons that are created on the mRNA level by a novel polyadenylation mechanism found only in Blastocystis. Reconstructions of pathways and organellar systems revealed that ST1 has a relatively complete membrane-trafficking system and a near-complete meiotic toolkit, possibly indicating a sexual cycle. Unlike some intestinal protistan parasites, Blastocystis ST1 has near-complete de novo pyrimidine, purine, and thiamine biosynthesis pathways and is unique amongst studied stramenopiles in being able to metabolize α-glucans rather than β-glucans. It lacks all genes encoding heme-containing cytochrome P450 proteins. Predictions of the mitochondrion-related organelle (MRO) proteome reveal an expanded repertoire of functions, including lipid, cofactor, and vitamin biosynthesis, as well as proteins that may be involved in regulating mitochondrial morphology and MRO/endoplasmic reticulum (ER) interactions. In sharp contrast, genes for peroxisome-associated functions are absent, suggesting Blastocystis STs lack this organelle. Overall, this study provides an important window into the biology of Blastocystis, showcasing significant differences between STs that can guide future experimental investigations into differences in their virulence and clarifying the roles of these organisms in gut health and disease.
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hal-01802863 , version 1 (25-09-2018)

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Eleni Gentekaki, Bruce Curtis, Courtney Stairs, Vladimír Klimeš, Marek Eliáš, et al.. Extreme genome diversity in the hyper-prevalent parasitic eukaryote Blastocystis. PLoS Biology, 2017, 15 (9), pp.e2003769. ⟨10.1371/journal.pbio.2003769⟩. ⟨hal-01802863⟩
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