Your search keyword '"Sinclair, Cooper"' showing total 2 results

1. Assembly and annotation of the mitochondrial minicircle genome of a differentiation-competent strain of Trypanosoma brucei

Author

Sinclair Cooper, Achim Schnaufer, Elizabeth S Wadsworth, Torsten Ochsenreiter, Alasdair Ivens, and Nicholas J. Savill

Subjects

Small RNA, Trypanosoma brucei brucei, Respiratory chain, Computational biology, Trypanosoma brucei, Minicircle, Genome, 03 medical and health sciences, 0302 clinical medicine, Gene Order, parasitic diseases, Genetics, Animals, Guide RNA, Molecular Biology, Conserved Sequence, 030304 developmental biology, 0303 health sciences, Base Sequence, biology, DNA, Kinetoplast, Molecular Sequence Annotation, Sequence Analysis, DNA, biology.organism_classification, 3. Good health, RNA editing, Kinetoplast, Genome, Mitochondrial, 570 Life sciences, DNA, Circular, Genome, Protozoan, 030217 neurology & neurosurgery, RNA, Guide, Kinetoplastida

Abstract

Kinetoplastids are protists defined by one of the most complex mitochondrial genomes in nature, the kinetoplast. In the sleeping sickness parasite Trypanosoma brucei, the kinetoplast is a chain mail-like network of two types of interlocked DNA molecules: a few dozen ∼23-kb maxicircles (homologs of the mitochondrial genome of other eukaryotes) and thousands of ∼1-kb minicircles. Maxicircles encode components of respiratory chain complexes and the mitoribosome. Several maxicircle-encoded mRNAs undergo extensive post-transcriptional RNA editing via addition and deletion of uridines. The process is mediated by hundreds of species of minicircle-encoded guide RNAs (gRNAs), but the precise number of minicircle classes and gRNA genes was unknown. Here we present the first essentially complete assembly and annotation of the kinetoplast genome of T. brucei. We have identified 391 minicircles, encoding not only ∼930 predicted ‘canonical’ gRNA genes that cover nearly all known editing events (accessible via the web at http://hank.bio.ed.ac.uk), but also ∼370 ‘non-canonical’ gRNA genes of unknown function. Small RNA transcriptome data confirmed expression of the majority of both categories of gRNAs. Finally, we have used our data set to refine definitions for minicircle structure and to explore dynamics of minicircle copy numbers.

Published

2019

2. Ecological divergence and hybridization of Neotropical Leishmania parasites

Author

Mandy Sanders, David Mateus, Achim Schnaufer, Jorge Arevalo, Sinclair Cooper, Vanessa Adaui, James Cotton, Hideo Imamura, Nicholas J. Savill, Marlene Jara, Matthew Berriman, Frederik Van den Broeck, Jean-Claude Dujardin, Lineth Garcia, Ilse Maes, Michael A. Miles, Alejandro Llanos-Cuentas, Elisa Cupolillo, Clinical sciences, Medical Genetics, and Department of Bio-engineering Sciences

Subjects

Mitochondrial DNA, Species complex, Nuclear gene, population genomics, Genetic Speciation, Leishmaniasis, Cutaneous, interspecific hybridization, Forests, Biology, vector-borne disease, Minicircle, Genome, Leishmania braziliensis, Host-Parasite Interactions, Ecological speciation, Population genomics, Peru, parasitic diseases, ecological speciation, Humans, Molecular clock, Ecosystem, Whole genome sequencing, Multidisciplinary, Population Biology, Biological Sciences, biology.organism_classification, purl.org/pe-repo/ocde/ford#1.06.13 [https], vector-bone disease, Phylogeography, Evolutionary biology, Genome, Mitochondrial, Ecological fitting, Engineering sciences. Technology, speciation genomics, purl.org/pe-repo/ocde/ford#3.03.06 [https]

Abstract

Significance Parasites are interesting models for studying speciation processes because they have a high potential for specialization, thanks to the intimate ecological association with their hosts and vectors. Yet little is known about the circumstances under which new parasite lineages emerge. Here we studied the genome diversity of parasites of the Leishmania braziliensis species complex that inhabit both Amazonian and Andean biotas in Peru. We identify three major parasite lineages that occupy particular ecological niches and show that these emerged during forestation changes over the past 150,000 y. We furthermore discovered that meiotic recombination between Amazonian and Andean lineages resulted in full-genome hybrids presenting mixed mitochondrial genomes, providing insights into the genetic consequences of hybridization in parasitic protozoa., The tropical Andes are an important natural laboratory to understand speciation in many taxa. Here we examined the evolutionary history of parasites of the Leishmania braziliensis species complex based on whole-genome sequencing of 67 isolates from 47 localities in Peru. We first show the origin of Andean Leishmania as a clade of near-clonal lineages that diverged from admixed Amazonian ancestors, accompanied by a significant reduction in genome diversity and large structural variations implicated in host–parasite interactions. Within the Andean species, patterns of population structure were strongly associated with biogeographical origin. Molecular clock and ecological niche modeling suggested that the history of diversification of the Andean lineages is limited to the Late Pleistocene and intimately associated with habitat contractions driven by climate change. These results suggest that changes in forestation over the past 150,000 y have influenced speciation and diversity of these Neotropical parasites. Second, genome-scale analyses provided evidence of meiotic-like recombination between Andean and Amazonian Leishmania species, resulting in full-genome hybrids. The mitochondrial genome of these hybrids consisted of homogeneous uniparental maxicircles, but minicircles originated from both parental species. We further show that mitochondrial minicircles—but not maxicircles—show a similar evolutionary pattern to the nuclear genome, suggesting that compatibility between nuclear-encoded mitochondrial genes and minicircle-encoded guide RNA genes is essential to maintain efficient respiration. By comparing full nuclear and mitochondrial genome ancestries, our data expand our appreciation on the genetic consequences of diversification and hybridization in parasitic protozoa.

Published

2020