Your search keyword '"Richard A. Pearson"' showing total 20 results

1. T-cell activation, senescence, and exhaustion in asymptomatic HIV/Leishmania infantumco-infection

Author

Carolina de Oliveira Mendes-Aguiar, Manoella do Monte Alves, Amanda de Albuquerque Lopes Machado, Glória Regina de Góis Monteiro, Iara Marques Medeiros, Jose Wilton Queiroz, Iraci Duarte Lima, Richard D. Pearson, Mary E. Wilson, Marshall J. Glesby, Eliana Lúcia Tomaz do Nascimento, and Selma Maria Bezerra Jerônimo

Abstract

BackgroundLeishmania infantumis an opportunistic parasitic infection. An immunocompromised state increases the risk of converting asymptomatic infection to symptomatic visceral leishmaniasis (VL), which has a ∼5% fatality rate even with treatment. HIV coinfection increases the risk of death from VL.MethodsA cross-sectional study was performed between 2014 and 2016 to determine the prevalence ofL. infantuminfection in HIV positive subjects residing in the state of Rio Grande do Norte, Brazil (n=1,372) and of these a subgroup of subjects were followed longitudinally. Subsequent incident cases of VL were ascertained from a public health database through 2018. A subgroup (n=69) of the cross-sectional study subjects was chosen to assess immune status (T cell activation, senescence, exhaustion) and outcome. The data were compared between asymptomatic HIV+/L. infantum+(HIV/Leish), symptomatic visceral leishmaniasis (VL), recovered VL, DTH+ (Delayed-Type Hypersensitivity response – Leishmanin skin test), AIDS/VL, HIV+ only (HIV+), and Non-HIV/NonL. infantuminfection (control subjects).ResultsThe cross-sectional study showed 24.2% of HIV+ subjects had positive anti-IgGLeishmaniaantibodies. After 3 years, 2.4% (8 of 333) of these HIV/Leish coinfected subjects developed AIDS/VL, whereas 1.05% (11 of 1,039) of HIV subjects with negative leishmania serology developed AIDS/VL. Poor adherence to antiretroviral therapy (p=0.0008) or prior opportunistic infections (p=0.0007) was associated with development of AIDS/VL. CD4+ (p=0.29) and CD8+ (p=0.38) T cells counts or viral load (p=0.34) were similar between asymptomatic HIV/Leish and HIV subjects. However, activated CD8+CD38+HLA-DR+T cells were higher in asymptomatic HIV/Leish than HIV group. Likewise, senescent (CD57+) or exhausted (PD1+) CD8+T cells were higher in asymptomatic HIV/Leish than in AIDS/VL or HIV groups.ConclusionAlthough asymptomatic HIV/Leish subjects had normal and similar CD4+ and CD8+ T cells counts, their CD8+T cells had increased activation, senescence, and exhaustion, which could contribute to risk of developing VL.Author SummaryThe frequency of asymptomatic HIV/Leishmania infantum(HIV/Leish) infection and the immunological status of subjects with HIV+ residing in the state of Rio Grande do Norte, Brazil, between 2014 and 2016 were studied. A high frequency of asymptomatic HIV/Leishmania infantuminfection (HIV subjects with positive anti-IgG Leishmania antibodies) was found. Asymptomatic HIV/Leish subjects had CD8 T cells with higher markers of activation, senescence and exhaustion than the other groups (HIV-alone, symptomatic VL, Recovered VL, DTH+, AIDS/VL and Controls subjects). Poor adherence to antiretroviral therapy or history of previous opportunistic infection was associated with AIDS/VL. Asymptomatic HIV/Leish had high relative risk of developing AIDS/VL. Thus, subjects with HIV residing in endemic areas for VL should be assessed for theirL. infantuminfection status and advised to closely adhere to ART.

Published

2023

2. Nanopore sequencing for real-time genomic surveillance ofPlasmodium falciparum

Author

Sophia T. Girgis, Edem Adika, Felix E. Nenyewodey, Dodzi K. Senoo Jnr, Joyce M. Ngoi, Kukua Bandoh, Oliver Lorenz, Guus van de Steeg, Sebastian Nsoh, Kim Judge, Richard D. Pearson, Jacob Almagro-Garcia, Samirah Saiid, Solomon Atampah, Enock K. Amoako, Collins M. Morang’a, Victor Asoala, Elrmion S. Adjei, William Burden, William Roberts-Sengier, Eleanor Drury, Sónia Gonçalves, Gordon A. Awandare, Dominic P. Kwiatkowski, Lucas N. Amenga-Etego, and William L. Hamilton

Abstract

Malaria is a global public health priority causing over 600,000 deaths annually, mostly young children living in Sub-Saharan Africa. Molecular surveillance can provide key information for malaria control, such as the prevalence and distribution of antimalarial drug resistance. However, genome sequencing capacity in endemic countries can be limited. Here, we have implemented an end-to-end workflow forP. falciparumgenomic surveillance in Ghana using Oxford Nanopore Technologies, targeting antimalarial resistance markers and the leading vaccine antigencircumsporozoite protein(csp). The workflow was rapid, robust, accurate, affordable and straightforward to implement. We found thatP. falciparumparasites in Ghana had become largely susceptible to chloroquine, with persistent sulfadoxine-pyrimethamine (SP) resistance, and no evidence of artemisinin resistance. Multiple Single Nucleotide Polymorphism (SNP) differences from the vaccinecspsequence were identified, though their significance is uncertain. This study demonstrates the potential utility and feasibility of malaria genomic surveillance in endemic settings using Nanopore sequencing.

Published

2022

3. Generation of a mutator parasite to drive resistome discovery in Plasmodium falciparum

Author

Krittikorn Kümpornsin, Theerarat Kochakarn, Tomas Yeo, Madeline R Luth, Richard D Pearson, Johanna Hoshizaki, Kyra A Schindler, Sachel Mok, Heekuk Park, Anne-Catrin Uhlemann, Sonia Moliner Cubel, Virginia Franco, Maria G Gomez-Lorenzo, Francisco Javier Gamo, Elizabeth A Winzeler, David A Fidock, Thanat Chookajorn, and Marcus CS Lee

Abstract

In vitro evolution of drug resistance is a powerful approach for identifying antimalarial targets, however key obstacles to eliciting resistance are the parasite inoculum size and mutation rate. Here we sought to increase parasite genetic diversity to potentiate resistance selections by editing catalytic residues of Plasmodium falciparum DNA polymerase δ. Mutation accumulation assays revealed a ∼5-8 fold elevation in the mutation rate, with an increase of 13-28 fold in drug-pressured lines. When challenged with KAE609, high-level resistance was obtained more rapidly and at lower inoculum than wild-type parasites. Selections were also successful with an “irresistible” compound, MMV665794 that failed to yield resistance with other strains. Mutations in a previously uncharacterized gene, PF3D7_1359900, which we term quinoxaline resistance protein (QRP1), were validated as causal for resistance to MMV665794 and an analog, MMV007224. The increased genetic repertoire available to this “mutator” parasite can be leveraged to drive P. falciparum resistome discovery.

Published

2022

4. Genetic analysis of a malaria outbreak in Laos driven by a selective sweep for Plasmodium falciparum kelch13 R539T mutants

Author

Varanya Wasakul, Areeya Disratthakit, Mayfong Mayxay, Keobouphaphone Chindavongsa, Viengphone Sengsavath, Nguyen Thuy-Nhien, Richard D Pearson, Sonexay Phalivong, Saiamphone Xayvanghang, Sonia Gonçalves, Nicholas P Day, Paul N Newton, Elizabeth A Ashley, Dominic P Kwiatkowski, Arjen M Dondorp, and Olivo Miotto

Abstract

Malaria outbreaks are an important public health concern in endemic regions approaching elimination. Genetic surveillance of malaria parasites can elucidate the population dynamics of an outbreak, and help identify its causes. We investigated the epidemiology of a Plasmodium falciparum outbreak in Attapeu Province, Laos, during the 2020-2021 season. An analysis of 249 samples, collected by routine genetic surveillance during the outbreak, revealed a massive loss of genetic diversity in the parasite population, primarily caused by the rapid expansion of a multidrug resistant strain, named LAA1. This strain carried the kelch13 R539T mutation and expanded clonally, replacing the previously dominant kelch13 C580Y mutants (KEL1/PLA1) resistant to dihydroartemisinin-piperaquine. Identity by descent (IBD) patterns showed that LAA1 was a recombinant that inherited 60% of its genome from a strain first sampled in Cambodia over a decade ago. A less common outbreak strain (LAA2) carried the kelch13 C580Y allele, but was distinct from KEL1/PLA1, its genome essentially identical to that of a Cambodian parasite from 2009. A third, low-frequency strain (LAA7) was a recombinant of KEL1/PLA1 with a R539T mutant, the latter providing the kelch13 variant. These results strongly suggest that the outbreak was driven by a selective sweep, possibly associated with drug-resistant phenotypes of the outbreak strains. The observation that new variants of established multidrug resistant populations can overwhelm previously dominant strains so rapidly has implications for elimination of malaria. Genetic surveillance provides the tools for characterizing outbreaks, and for monitoring the evolution and spread of the populations involved.

Published

2022

5. An amino acid transporter AAT1 plays a pivotal role in chloroquine resistance evolution in malaria parasites

Author

Alfred Amambua-Ngwa, Katrina A. Button-Simons, Xue Li, Sudhir Kumar, Katelyn Vendrely Brenneman, Marco Ferrari, Lisa A. Checkley, Meseret T. Haile, Douglas A. Shoue, Marina McDew-White, Sarah M. Tindall, Ann Reyes, Elizabeth Delgado, Haley Dalhoff, James K. Larbalestier, Roberto Amato, Richard D. Pearson, Alexander B. Taylor, François H. Nosten, Umberto D’Alessandro, Dominic Kwiatkowski, Ian H. Cheeseman, Stefan H. I. Kappe, Simon V. Avery, David J. Conway, Ashley M. Vaughan, Michael T. Ferdig, and Timothy J. C. Anderson

Abstract

Malaria parasites break down host hemoglobin into peptides and amino acids in the digestive vacuole for export to the parasite cytoplasm for growth: interrupting this process is central to the mode of action of several antimalarial drugs. Mutations in the chloroquine (CQ) resistance transporter,pfcrt, located in the digestive vacuole membrane, confer CQ resistance inPlasmodium falciparum, but typically affect parasite fitness. However, the role of other parasite loci in the evolution of CQ resistance is unclear. Here we use a combination of population genomics, genetic crosses and gene editing to demonstrate that a second vacuolar transporter plays a key role in both resistance and compensatory evolution. Longitudinal genomic analyses of the Gambian parasites revealed temporal signatures of selection on an amino acid transporter (pfaat1)S258Lvariant which increased from 0-87% in frequency between 1984 and 2014 in parallel withpfcrt1K76T. Parasite genetic crosses then identified a chromosome 6 quantitative trait locus containingpfaat1that is selected by CQ treatment. Gene editing demonstrated thatpfaat1S258Lpotentiates CQ-resistance but at a cost of reduced fitness, whilepfaat1F313S, a common Southeast Asian polymorphism, reduces CQ-resistance while restoring fitness. Our analyses reveal hidden complexity in CQ-resistance evolution, suggesting thatpfaat1may underlie regional differences in the dynamics of resistance evolution, and modulate parasite resistance or fitness by manipulating the balance between both amino acid and drug transport.

Published

2022

6. Cystathionine-β-synthase is essential for AKT-induced senescence and suppresses the development of gastric cancers with PI3K/AKT activation

Author

Jian Kang, Huang X, Jana M, Fu C, Anna S Trigos, Creek D, Xiaofang Wang, Shaun Blake, Elaine Sanij, Hong-Jian Zhu, Richard B. Pearson, De Souza Dp, Keefe T. Chan, and Anderson D

Subjects

Senescence, Programmed cell death, biology, Chemistry, Cancer cell, biology.protein, Transsulfuration pathway, Cell cycle, Cystathionine beta synthase, Protein kinase B, PI3K/AKT/mTOR pathway, Cell biology

Abstract

Hyperactivation of oncogenic pathways downstream of RAS and PI3K/AKT in normal cells induces a senescence-like phenotype that acts as a tumor-suppressive mechanism that must be overcome during transformation. We previously demonstrated that AKT-induced senescence (AIS) is associated with profound transcriptional and metabolic changes. Here, we demonstrate that human fibroblasts undergoing AIS display increased Cystathionine-β-synthase (CBS) expression and consequent activation of the transsulfuration pathway controlling hydrogen sulfide (H2S) and glutathione (GSH) metabolism. Activated transsulfuration pathway during AIS maintenance enhances the antioxidant capacity, protecting senescent cells from ROS-induced cell death via GSH and H2S. Importantly, CBS depletion allows cells that have undergone AIS to escape senescence and re-enter the cell cycle, indicating the importance of CBS activity in maintaining AIS. Mechanistically, we show this restoration of proliferation is mediated through suppressing mitochondrial respiration and reactive oxygen species (ROS) production and increasing GSH metabolism. These findings implicate a potential tumor-suppressive role for CBS in cells with inappropriately activated PI3K/AKT signaling. Consistent with this concept, in human gastric cancer cells with activated PI3K/AKT signaling, we demonstrate that CBS expression is suppressed due to promoter hypermethylation. CBS loss cooperates with activated PI3K/AKT signaling in promoting anchorage-independent growth of gastric epithelial cells, while CBS restoration suppresses the growth of gastric tumors in vivo. Taken together, we find that CBS is a novel regulator of AIS and a potential tumor suppressor in PI3K/AKT-driven gastric cancers, providing a new exploitable metabolic vulnerability in these cancers.

Published

2021

7. The protective effect of sickle cell haemoglobin against severe malaria depends on parasite genotype

Author

Jim Stalker, Ellen M. Leffler, Kalifa Bojang, Kevin Marsh, Fatoumatta Sisay-Joof, Norbert Peshu, Dominic P. Kwiatkowski, Sónia Gonçalves, Carolyne M. Ndila, Eleanor Drury, Umberto D'Alessandro, Cristina V. Ariani, Roberto Amato, Giorgio Sirugo, Richard D. Pearson, Anna E. Jeffreys, Thuy Nguyen, Thomas N. Williams, Alexander Macharia, Gavin Band, Kate Rowlands, Christina Hubbart, Muminatou Jallow, Kirk A. Rockett, and David J. Conway

Subjects

Genetics, Linkage disequilibrium, education.field_of_study, biology, Population, Plasmodium falciparum, biology.organism_classification, medicine.disease, Structural variation, parasitic diseases, Genetic variation, Genotype, medicine, Parasite hosting, education, Malaria

Abstract

Host genetic factors can confer resistance against malaria, raising the question of whether this has led to evolutionary adaptation of parasite populations. In this study we investigated the correlation between host and parasite genetic variation in 4,171 Gambian and Kenya children ascertained with severe malaria due to Plasmodium falciparum. We identified a strong association between sickle haemoglobin (HbS) in the host and variation in three regions of the parasite genome, including nonsynonymous variants in the acyl-CoA synthetase family member PfACS8 on chromosome 2, in a second region of chromosome 2, and in a region containing structural variation on chromosome 11. The HbS-associated parasite alleles are in strong linkage disequilibrium and have frequencies which covary with the frequency of HbS across populations, in particular being much more common in Africa than other parts of the world. The estimated protective effect of HbS against severe malaria, as determined by comparison of cases with population controls, varies greatly according to the parasite genotype at these three loci. These findings open up a new avenue of enquiry into the biological and epidemiological significance of the HbS-associated polymorphisms in the parasite genome, and the evolutionary forces that have led to their high frequency and strong linkage disequilibrium in African P. falciparum populations.

Published

2021

8. Nuclear stabilisation of p53 requires a functional nucleolar surveillance pathway

Author

Justine K. Lee, Ulrike Kutay, Sheren Al-Obaidi, Mei S. Wong, Priscilla Soo, Lorena Núñez-Villacís, Christian Montellese, Ross D. Hannan, Rita Ferreira, Kate M Parsons, Amee J George, Gaetan Burgio, Kaylene J. Simpson, Christoph Engel, Nicholas J. Watkins, Katherine M. Hannan, Tobias D. Williams, Johan Flygare, Cathryn M. Gould, Kira D. Wysoke, Maurits Evers, Zhi-Ping Feng, Thomas J. Gonda, Lorey K. Smith, Nadine Hein, Richard B. Pearson, Jeannine Diesch, Perlita Poh, Piyush B. Madhamshettiwar, Megan Pavy, and Jin-Shu He

Subjects

biology, Ribosomal protein, DNA damage, Ribonucleoprotein particle, biology.protein, Mdm2, Ribosome biogenesis, Gene, Biogenesis, Ubiquitin ligase, Cell biology

Abstract

The nucleolar surveillance pathway (NSP) monitors nucleolar fidelity and responds to nucleolar stresses (i.e., inactivation of ribosome biogenesis) by mediating the inhibitory binding of ribosomal proteins (RPs) to mouse double minute 2 homolog (MDM2), a nuclear-localised E3 ubiquitin ligase, which results in p53 accumulation. Inappropriate activation of the NSP has been implicated in the pathogenesis of collection of human diseases termed “ribosomopathies”, while drugs that selectively activate the NSP are now in trials for cancer. Despite the clinical significance, the precise molecular mechanism(s) regulating the NSP remain poorly understood. Using genome-wide loss of function screens, we demonstrate the ribosome biogenesis (RiBi) axis as the most potent class of genes whose disruption stabilises p53. Furthermore, we identified a novel suite of genes critical for the NSP, including a novel mammalian protein implicated in 5S ribonucleoprotein particle (5S-RNP) biogenesis, HEATR3. By selectively disabling the NSP, we unexpectedly demonstrate that a functional NSP is required for the ability of all nuclear acting stresses tested, including DNA damage, to robustly induce p53 accumulation. Together, our data demonstrates that the NSP has evolved as the dominant central integrator of stresses that regulate nuclear p53 abundance, thus ensuring RiBi is hardwired to cellular proliferative capacity.

Published

2021

9. Artemisinin-resistant malaria parasites show enhanced transmission to mosquitoes under drug pressure

Author

Lawniczak Mkn., Kesinee Chotivanich, Arjen M. Dondorp, Oliver J Watson, S Pukrittayakamee, Ursula Straschil, Michael J. Delves, Kathrin Witmer, D Chiwcharoen, Farah A. Dahalan, Virginia M. Howick, Sabrina Yahiya, B Sornboon, Richard D. Pearson, Nicholas J. White, Jake Baum, Lucy C Okell, and Andrea Ruecker

Subjects

0303 health sciences, biology, Combination therapy, 030306 microbiology, medicine.medical_treatment, Dihydroartemisinin, Plasmodium falciparum, biology.organism_classification, medicine.disease, Virology, 3. Good health, Multiple drug resistance, 03 medical and health sciences, parasitic diseases, medicine, Parasite hosting, Artemisinin, Anopheles stephensi, Malaria, 030304 developmental biology, medicine.drug

Abstract

Resistance to artemisinin combination therapy (ACT) in the Plasmodium falciparum parasite is threatening to reverse recent gains in reducing global deaths from malaria. Whilst resistance manifests as delayed asexual parasite clearance in patients following ACT treatment, the phenotype can only spread geographically via the sexual cycle and subsequent transmission through the mosquito. Artemisinin and its derivatives (such as dihydroartemisinin, DHA) as well as killing the asexual parasite form are known to sterilize male, sexual-stage gametes from activation. Whether resistant parasites overcome this artemisinin-dependent sterilizing effect has not, however, been fully tested. Here, we analysed five P. falciparum clinical isolates from the Greater Mekong Subregion, each of which demonstrated delayed clinical clearance and carried known resistance-associated polymorphisms in the Kelch13 gene (PfK13var). As well as demonstrating reduced sensitivity to artemisinin-derivates in in vitro asexual growth assays, certain PfK13var isolates also demonstrated a marked reduction in sensitivity to these drugs in an in vitro male gamete activation assay compared to a sensitive control. Importantly, the same reduction in sensitivity to DHA was observed when the most resistant isolate was assayed by standard membrane feeding assays using Anopheles stephensi mosquitoes. These results indicate that ACT use can favour resistant over sensitive parasite transmission. A selective advantage for resistant parasite transmission could also favour acquisition of further polymorphisms, such as mosquito host-specificity or antimalarial partner–drug resistance in mixed infections. Favoured transmission of resistance under ACT coverage could have profound implications for the spread of multidrug resistant malaria beyond Southeast Asia.ONE SENTENCE SUMMARYArtemisinin-resistant clinical isolates can also demonstrate resistance to the transmission-blocking effects of artemisinin-based drugs, favouring resistance transmission to the mosquito.

Published

2020

10. Reprogrammed mRNA translation drives resistance to therapeutic targeting of ribosome biogenesis

Author

Eric P Kusnadi, Katherine M. Hannan, Gretchen Poortinga, Grant A. McArthur, David L Goode, Ross D. Hannan, Jennifer R. Devlin, Ola Larsson, George Thomas, Elaine Sanij, Malcolm J. McConville, Richard B. Pearson, David P De Souza, Anna S Trigos, Jian Kang, Carleen Cullinane, and Keefe T. Chan

Subjects

Transcription (biology), Cancer research, Ribosome biogenesis, Myeloid leukemia, Translation (biology), mTORC1, Biology, Protein kinase B, Ribosome, PI3K/AKT/mTOR pathway

Abstract

Elevated ribosome biogenesis in oncogene-driven cancers is commonly targeted by DNA-damaging cytotoxic drugs. Our first-in-human trial of CX-5461, a novel, less genotoxic agent that specifically inhibits ribosome biogenesis via suppression of RNA Polymerase I (Pol I) transcription, revealed single agent efficacy in refractory blood cancers. Despite this clinical response, patients were not cured. In parallel, we demonstrated a marked improvement in thein vivoefficacy of CX-5461 in combination with PI3K/AKT/mTORC1 pathway inhibitors. Here we show that this improved efficacy is associated with specific suppression of translation of mRNAs encoding regulators of cellular metabolism. Importantly, acquired resistance to this co-treatment is driven by translational re-wiring that results in dysregulated cellular metabolism and induction of a cAMP-dependent pathway critical for the survival of blood cancers including lymphoma and acute myeloid leukemia. Our studies identify the molecular mechanisms underpinning the response of blood cancers to selective ribosome biogenesis inhibitors and identify metabolic vulnerabilities that will facilitate the rational design of more effective regimens for Pol I-directed therapies.

Published

2019

11. Targeting RNA Polymerase I transcription synergises with TOP1 inhibition in potentiating the DNA damage response in high-grade serous ovarian cancer

Author

Ross D. Hannan, Elaine Sanij, Jian Kang, Carleen Cullinane, Piyush B. Madhamshettiwar, Kaylene J. Simpson, Richard B. Pearson, Karen E. Sheppard, Sarah Ellis, Shunfei Yan, Keefe T. Chan, and Katherine M. Hannan

Subjects

biology, DNA repair, DNA damage, Poly ADP ribose polymerase, Topoisomerase, Cancer research, biology.protein, medicine, Topotecan, Ataxia telangiectasia and Rad3 related, Replication protein A, Polymerase, medicine.drug

Abstract

Limited effective therapeutic options are available for patients with recurrent high-grade serous carcinoma (HGSC), the most common histological subtype accounting for the majority of ovarian cancer deaths. We have shown efficacy in poly-ADP ribose polymerase (PARP) inhibitor-resistant HGSC for the RNA Polymerase I (Pol I) transcription inhibitor CX-5461 through its ability to activate a nucleolar-associated DNA damage response (DDR). Here, we screen the protein-coding genome to identify potential targets whose inhibition enhances the efficacy of CX-5461. We identify a network of cooperating inhibitory interactions, including components of homologous recombination (HR) DNA repair and DNA topoisomerase 1 (TOP1). We highlight that CX-5461 combined with topotecan, a TOP1 inhibitor used as salvage therapy in HGSC, induces robust cell cycle arrest and cell death in a panel of HR-proficient HGSC cell lines. The combination potentiates a nucleolar-associated DDR via recruitment of phosphorylated replication protein A (RPA) and ataxia telangiectasia and Rad3 related protein (ATR). CX-5461 plus low-dose topotecan cooperate to potently inhibit xenograft tumour growth, indicating the potential for this strategy to improve salvage therapeutic regimens to treat HGSC.

Published

2019

12. A molecular barcode and online tool to identify and map imported infection with Plasmodium vivax

Author

Nguyen Hoang Chau, François Nosten, Alberto Tobón-Castaño, Alistair Miles, Ric N. Price, Alyssa E. Barry, Nicholas J. White, Matthew J. Grigg, Ishag Adam, Lidia Madeline Montenegro, Yaobao Liu, Bridget E. Barber, Marcelo U. Ferreira, A G Rahim, Leily Trianty, Hidayat Trimarsanto, Rintis Noviyanti, Tatiana M. Lopera-Mesa, Kamala Thriemer, Dominic P. Kwiatkowski, Sisay Getachew, Kanlaya Sriprawat, Ashenafi Assefa, Sónia Gonçalves, Ivo Mueller, Wasif A. Khan, Abraham Aseffa, E Sutanto, Jutta Marfurt, Victoria Simpson, Roberto Amato, Sarah Auburn, Mohammad Shafiul Alam, Yaghoob Hamedi, Zuleima Pava, Olivo Miotto, Richard D. Pearson, S Wangchuck, Timothy William, Tran Tinh Hien, Benedikt Ley, Qi Gao, Nicholas M. Anstey, Diego F. Echeverry, Eleanor Drury, and Beyene Petros

Subjects

0303 health sciences, education.field_of_study, biology, 030231 tropical medicine, Plasmodium vivax, Population, Decision tree, Single-nucleotide polymorphism, Computational biology, biology.organism_classification, Missing data, Barcode, Matthews correlation coefficient, 3. Good health, law.invention, 03 medical and health sciences, 0302 clinical medicine, law, education, Genotyping, 030304 developmental biology

Abstract

Imported cases present a considerable challenge to the elimination of malaria. Traditionally, patient travel history has been used to identify imported cases, but the long-latency liver stages confound this approach in Plasmodium vivax. Molecular tools to identify and map imported cases offer a more robust approach, that can be combined with drug resistance and other surveillance markers in high-throughput, population-based genotyping frameworks. Using a machine learning approach incorporating hierarchical FST (HFST) and decision tree (DT) analysis applied to 831 P. vivax genomes from 20 countries, we identified a 28-Single Nucleotide Polymorphism (SNP) barcode with high capacity to predict the country of origin. The Matthews correlation coefficient (MCC), which provides a measure of the quality of the classifications, ranging from −1 (total disagreement) to 1 (perfect prediction), exceeded 0.9 in 15 countries in cross-validation evaluations. When combined with an existing 37-SNP P. vivax barcode, the 65-SNP panel exhibits MCC scores exceeding 0.9 in 17 countries with up to 30% missing data. As a secondary objective, several genes were identified with moderate MCC scores (median MCC range from 0.54-0.68), amenable as markers for rapid testing using low-throughput genotyping approaches. A likelihood-based classifier framework was established, that supports analysis of missing data and polyclonal infections. To facilitate investigator-lead analyses, the likelihood framework is provided as a web-based, open-access platform (vivaxGEN-geo) to support the analysis and interpretation of data produced either at the 28-SNP core or full 65-SNP barcode. These tools can be used by malaria control programs to identify the main reservoirs of infection so that resources can be focused to where they are needed most.

Published

2019

13. Emergence of artemisinin-resistant Plasmodium falciparum with kelch13 C580Y mutations on the island of New Guinea

Author

Jun Ohashi, Makoto Hirai, Alyssa E. Barry, Toshiyuki Mori, Francis Hombhanje, Rintis Noviyanti, Toshihiro Mita, Ric N. Price, Masato Yamauchi, Pascal Ringwald, Sarah Auburn, Richard D. Pearson, Mehra Somya, Makoto Sekihara, Roberto Amato, Shin-Ichiro Tachibana, Livingstone Tavul, Moses Laman, Sónia Gonçalves, Dominic P. Kwiatkowski, Olivo Miotto, Mie Ikeda, Jutta Marfurt, Manuel W Hetzel, and Ivo Mueller

Subjects

Heredity, Single Nucleotide Polymorphisms, Genes, Protozoan, Drug Resistance, Drug resistance, medicine.disease_cause, Identity by descent, Geographical locations, Medical Conditions, 0302 clinical medicine, Anti-Infective Agents, Medicine and Health Sciences, Malaria, Falciparum, Biology (General), Artemisinin, Genetics, 0303 health sciences, Mutation, Drugs, Genomics, Artemisinins, 3. Good health, Genetic Mapping, Research Article, medicine.drug, Asia, Lineage (genetic), QH301-705.5, Oceania, Plasmodium falciparum, 030231 tropical medicine, Immunology, Biology, Microbiology, Deep sequencing, Papua New Guinea, Antimalarials, 03 medical and health sciences, Antibiotic resistance, Virology, parasitic diseases, Parasitic Diseases, medicine, Humans, Gene, Molecular Biology, 030304 developmental biology, Pharmacology, Haplotype, Biology and Life Sciences, RC581-607, medicine.disease, biology.organism_classification, Cross-Sectional Studies, Haplotypes, Parasitology, Indonesia, People and places, Immunologic diseases. Allergy, Malaria

Abstract

The rapid and aggressive spread of artemisinin-resistant Plasmodium falciparum carrying the C580Y mutation in the kelch13 gene is a growing threat to malaria elimination in Southeast Asia, but there is no evidence of their spread to other regions. We conducted cross-sectional surveys in 2016 and 2017 at two clinics in Wewak, Papua New Guinea (PNG) where we identified three infections caused by C580Y mutants among 239 genotyped clinical samples. One of these mutants exhibited the highest survival rate (6.8%) among all parasites surveyed in ring-stage survival assays (RSA) for artemisinin. Analyses of kelch13 flanking regions, and comparisons of deep sequencing data from 389 clinical samples from PNG, Indonesian Papua and Western Cambodia, suggested an independent origin of the Wewak C580Y mutation, showing that the mutants possess several distinctive genetic features. Identity by descent (IBD) showed that multiple portions of the mutants’ genomes share a common origin with parasites found in Indonesian Papua, comprising several mutations within genes previously associated with drug resistance, such as mdr1, ferredoxin, atg18 and pnp. These findings suggest that a P. falciparum lineage circulating on the island of New Guinea has gradually acquired a complex ensemble of variants, including kelch13 C580Y, which have affected the parasites’ drug sensitivity. This worrying development reinforces the need for increased surveillance of the evolving parasite populations on the island, to contain the spread of resistance., Author summary Artemisinin is the most widely used drug against Plasmodium falciparum malaria. In southeast Asia, parasites have evolved genetic changes making them resistant to artemisinin. The elimination of resistant strains is a global priority, since their global spread could result in massive loss of lives. In Papua New Guinea, we found three patients infected with parasites carrying the most widespread resistant variant in southeast Asia, and they were confirmed to be artemisinin resistant. We established that the mutations were not imported from southeast Asia, and found other drug resistance variants in their genetic background, including some shared with parasites in Indonesia. This indicates that artemisinin resistance has emerged in New Guinea separately from southeast Asia, not by a chance event, but by a gradual process of evolution which may still be ongoing undetected on the island. These resistant strains could undermine malaria local control efforts, and constitute a global threat.

Published

2019

14. Evolution and expansion of multidrug resistant malaria in Southeast Asia: a genomic epidemiology study

Author

Arjen M. Dondorp, Yok Sovann, Tran Tinh Hien, Christopher G Jacob, Kirk A. Rockett, Mehul Dhorda, Huy Rekol, Rick M. Fairhurst, Nicholas P. J. Day, Nguyen Hoang Chau, Thomas J. Peto, Eleanor Drury, Cheah Huch, Nguyen Thuy-Nhien, Rob W. van der Pluijm, Nicholas J. White, Dominic P. Kwiatkowski, Sónia Gonçalves, Rithea Leang, William L Hamilton, Roberto Amato, Borimas Hanboonkunupakarn, Rupam Tripura, Bouasy Hongvanthong, Olivo Miotto, Podjanee Jittamala, Mayfong Mayxay, Ranitha Vongpromek, Xin Hui S Chan, Thuy Nguyen, Chanaki Amaratunga, Sasithon Pukrittayakamee, Keobouphaphone Chindavongsa, Richard D. Pearson, Seila Suon, Richard J. Maude, Lek Dysoley, Huynh Hong Quang, and Mallika Imwong

Subjects

0303 health sciences, medicine.medical_specialty, education.field_of_study, Population, Context (language use), Plasmodium falciparum, Biology, medicine.disease, biology.organism_classification, 3. Good health, Multiple drug resistance, 03 medical and health sciences, 0302 clinical medicine, Genetic marker, Piperaquine, Epidemiology, parasitic diseases, medicine, 030212 general & internal medicine, education, Malaria, 030304 developmental biology, Demography

Abstract

SummaryBackgroundA multidrug resistant co-lineage of Plasmodium falciparum malaria, named KEL1/PLA1, spread across Cambodia c.2008-2013, causing high treatment failure rates to the frontline combination therapy dihydroartemisinin-piperaquine. Here, we report on the evolution and spread of KEL1/PLA1 in subsequent years.MethodsWe analysed whole genome sequencing data from 1,673 P. falciparum clinical samples collected in 2008-2018 from northeast Thailand, Laos, Cambodia and Vietnam. By investigating genome-wide relatedness between parasites, we inferred patterns of shared ancestry in the KEL1/PLA1 population.FindingsKEL1/PLA1 spread rapidly from 2015 into all of the surveyed countries and now exceeds 80% of the P. falciparum population in several regions. These parasites maintained a high level of genetic relatedness reflecting their common origin. However, several genetic subgroups have recently emerged within this co-lineage with diverse geographical distributions. Some of these emerging KEL1/PLA1 subgroups carry recent mutations in the chloroquine resistance transporter (crt) gene, which arise on a specific genetic background comprising multiple genomic regions.InterpretationAfter emerging and circulating for several years within Cambodia, the P. falciparum KEL1/PLA1 co-lineage diversified into multiple subgroups and acquired new genetic features including novel crt mutations. These subgroups have rapidly spread into neighbouring countries, suggesting enhanced fitness. These findings highlight the urgent need for elimination of this increasingly drug-resistant parasite co-lineage, and the importance of genetic surveillance in accelerating elimination efforts.FundingWellcome Trust, Bill & Melinda Gates Foundation, UK Medical Research Council, UK Department for International Development.Research in contextEvidence before this studyThis study updates our previous work describing the emergence and spread of a multidrug resistant P. falciparum co-lineage (KEL1/PLA1) within Cambodia up to 2013. Since then, a regional genetic surveillance project, GenRe-Mekong, has reported that markers of dihydroartemisinin-piperaquine (DHA-PPQ) resistance have increased in frequency in neighbouring countries. A PubMed search (terms: “artemisinin”, “piperaquine”, “resistance”, “southeast asia”) for articles listed since our previous study (from 30/10/2017 to 05/01/2019) yielded 28 results, including reports of a recent sharp decline in DHA-PPQ clinical efficacy in Vietnam; the spread of genetic markers of DHA-PPQ resistance into neighbouring countries by Imwong and colleagues; and multiple reports associating mutations in the crt gene with piperaquine resistance, including newly emerging crt variants in Southeast Asia.Added value of this studyWe analysed P. falciparum whole genomes collected up to early 2018 from Eastern Southeast Asia (Cambodia and surrounding regions), describing the fine-scale epidemiology of multiple KEL1/PLA1 genetic subgroups that have spread out from Cambodia since 2015 and taken over indigenous parasite populations in northeastern Thailand, southern and central Vietnam and parts of southern Laos. Several newly emerging crt mutations accompanied the spread and expansion of KEL1/PLA1 subgroups, suggesting an active proliferation of biologically fit, multidrug resistant parasites.Implications of all the available evidenceThe problem of P. falciparum multidrug resistance has dramatically worsened in Eastern Southeast Asia since previous reports. KEL1/PLA1 has diversified and spread widely across Eastern Southeast Asia since 2015, becoming the predominant parasite group in several regions. This may have been fuelled by continued parasite exposure to DHA-PPQ, resulting in sustained selection after KEL1/PLA1 became established. Continued drug pressure enabled the acquisition of further mutations, resulting in higher levels of resistance. These data demonstrate the value of pathogen genetic surveillance and the urgent need to eliminate these dangerous parasites.

Published

2019

15. Adaptive post-transcriptional reprogramming of metabolism limits response to targeted therapy in BRAFV600 melanoma

Author

Grant A. McArthur, Margarete Kleinschmidt, David L Goode, Jian Kang, Anna S Trigos, Vihandha O. Wickramasinghe, Peter Lau, Rodney J. Hicks, Karen E. Sheppard, Teresa Ward, Lorey K. Smith, Tony Tiganis, Richard B. Pearson, Carleen Cullinane, Kaylene J. Simpson, Emily J. Lelliott, Aparna D. Rao, Tiffany Parmenter, Claire Martin, Ola Larsson, Eric P Kusnadi, and Julie Lorent

Subjects

0303 health sciences, Combination therapy, business.industry, Kinase, medicine.medical_treatment, Melanoma, Cancer, medicine.disease, 3. Good health, Targeted therapy, Gene expression profiling, 03 medical and health sciences, 0302 clinical medicine, 030220 oncology & carcinogenesis, Gene expression, Cancer research, Medicine, MRNA transport, business, neoplasms, 030304 developmental biology

Abstract

Despite the success of therapies targeting oncogenes in cancer, clinical outcomes are limited by a residual disease that results in relapse. This residual disease is characterized by drug-induced adaptation, that in melanoma includes altered metabolism. Here, we examined how targeted therapy reprograms metabolism in BRAF-mutant melanoma cells using a genome-wide RNAi screen and global gene expression profiling. This systematic approach revealed post-transcriptional regulation of metabolism following BRAF inhibition, involving selective mRNA transport and translation. As proof of concept we demonstrate the RNA binding kinase UHMK1 interacts with mRNAs that encode metabolic proteins and selectively controls their transport and translation during adaptation to BRAF targeted therapy. Inactivation of UHMK1 improves metabolic response to BRAF targeted therapy and delays resistance to BRAF and MEK combination therapy in vivo. Our data support a model wherein post-transcriptional gene expression pathways regulate metabolic adaptation underpinning targeted therapy response and suggest inactivation of these pathways may delay disease relapse.

Published

2019

16. Inhibition of RNA Polymerase I Transcription Activates Targeted DNA Damage Response and Enhances the Efficacy of PARP Inhibitors in High-Grade Serous Ovarian Cancer

Author

Purba Nag, Els M.J.J. Berns, Anna S Trigos, Sarah Ellis, Ross D. Hannan, Matthew Wakefield, Jian Kang, Karen E. Sheppard, Richard B. Pearson, Gretchen Poortinga, Clare L. Scott, Jinbae Son, Jiachen Xuan, Grant A. McArthur, John Soong, Carleen Cullinane, Jessica E. Ahern, Elaine Sanij, Linda Mileshkin, Daniel Frank, Shunfei Yan, Keefe T. Chan, Olga Kondrashova, Elizabeth Lieschke, Katherine M. Hannan, and Kum Kum Khanna

Subjects

0303 health sciences, business.industry, DNA damage, Poly ADP ribose polymerase, medicine.disease, 3. Good health, 03 medical and health sciences, chemistry.chemical_compound, 0302 clinical medicine, chemistry, Transcription (biology), 030220 oncology & carcinogenesis, Gene expression, Cancer research, medicine, RNA polymerase I, Ovarian cancer, business, Homologous recombination, DNA, 030304 developmental biology

Abstract

High-grade serous ovarian cancer (HGSOC) accounts for the majority of ovarian cancer and has a dismal prognosis. PARP inhibitors (PARPi) have revolutionized disease management of patients with homologous recombination (HR) DNA repair-deficient HGSOC. However, acquired resistance to PARPi by complex mechanisms including HR restoration and stabilisation of replication forks is a major challenge in the clinic. Here, we demonstrate CX-5461, an inhibitor of RNA polymerase I transcription of ribosomal RNA genes (rDNA), induces replication stress at rDNA leading to activation of DNA damage response and DNA damage involving MRE11-dependent degradation of replication forks. CX-5461 cooperates with PARPi in exacerbating DNA damage and enhances synthetic lethal interactions of PARPi with HR deficiency in HGSOC-patient-derived xenograft (PDX)in vivo. We demonstrate CX-5461 has a different sensitivity spectrum to PARPi and destabilises replication forks irrespective of HR pathway status, overcoming two well-known mechanisms of resistance to PARPi. Importantly, CX-5461 exhibits single agent efficacy in PARPi-resistant HGSOC-PDX. Further, we identify CX-5461-sensitivity gene expression signatures in primary and relapsed HGSOC. Therefore, CX-5461 is a promising therapy alone and in combination therapy with PARPi in HR-deficient HGSOC. CX-5461 is also an exciting treatment option for patients with relapsed HGSOC tumors that have poor clinical outcome.

Published

2019

17. Origins of the current outbreak of multidrug resistant malaria in Southeast Asia: a retrospective genetic study

Author

Roberto Amato, Seila Suon, Olivo Miotto, Dominic P. Kwiatkowski, Rick M. Fairhurst, Chanaki Amaratunga, Richard D. Pearson, Jacob Almagro-Garcia, Sokunthea Sreng, Eleanor Drury, Jim Stalker, and Pharath Lim

Subjects

0303 health sciences, education.field_of_study, medicine.medical_specialty, 030306 microbiology, Population, Outbreak, Plasmodium falciparum, Biology, medicine.disease, biology.organism_classification, 3. Good health, Multiple drug resistance, 03 medical and health sciences, Piperaquine, parasitic diseases, Epidemiology, medicine, Global health, education, Malaria, 030304 developmental biology, Demography

Abstract

BackgroundAntimalarial failure is rapidly spreading across parts of Southeast Asia where dihydroartemisinin-piperaquine (DHA-PPQ) is used as first line treatment. The first published reports came from western Cambodia in 2013. Here we analyse genetic changes in the Plasmodium falciparum population of western Cambodia in the six years prior to that.MethodsWe analysed genome sequence data on 1492 P. falciparum samples from Southeast Asia, including 464 collected in western Cambodia between 2007 and 2013. Different epidemiological origins of resistance were identified by haplotypic analysis of the kelch13 artemisinin resistance locus and the plasmepsin 2-3 piperaquine resistance locus.FindingsWe identified over 30 independent origins of artemisinin resistance, of which the KEL1 lineage accounted for 91% of DHA-PPQ-resistant parasites. In 2008, KEL1 combined with PLA1, the major lineage associated with piperaquine resistance. By 2012, the KEL1/PLA1 co-lineage had reached over 60% frequency in western Cambodia and had spread to northern Cambodia.InterpretationThe KEL1/PLA1 co-lineage emerged in the same year that DHA-PPQ became the first line antimalarial drug in western Cambodia and spread aggressively thereafter, displacing other artemisinin-resistant parasite lineages. These findings have significant implications for management of the global health risk associated with the current outbreak.FundingWellcome Trust, Bill & Melinda Gates Foundation, Medical Research Council, UK Department for International Development, and Intramural Research Program of the US National Institute of Allergy and Infectious Diseases, National Institutes of Health.

Published

2017

18. A novel role for the Pol I transcription factor UBTF in maintaining genome stability through the regulation of highly transcribed Pol II genes

Author

Izhak Haviv, Elaine Sanij, Jason Ellul, Amardeep S. Dhillon, Gretchen Poortinga, Tom Moss, Lawrence I. Rothblum, Analia Lesmana, Jeannine Diesch, Nourdine Hamdane, Ross D. Hannan, Richard B. Pearson, Gregory J. Goodall, Nadine Hein, Grace E. Lidgerwood, Lee H. Wong, Donald P. Cameron, Sanjie, Elaine, Diesch, Jeannine, Lesmana, Analia, Poortinga, Gretchen, Hein, Nadine, Lidgerwood, Grace, Cameron, Donald P, Ellul, Jason, Goodall, Gregory J, Wong, Lee H, Dhillon, Amardeep S, Hamdane, Nourdine, Rothblum, Lawrence I, Pearson, Richard B, Haviv, Izhak, Moss, Tom, and Hannan, Ross D

Subjects

Chromatin Immunoprecipitation, Transcription, Genetic, RNA polymerase II, Genomic Instability, Histones, Mice, 03 medical and health sciences, 0302 clinical medicine, UBF, RNA Polymerase I, Genetics, Transcriptional regulation, Animals, Humans, Nucleosome, Transcription factor, Genetics (clinical), Cell Line, Transformed, 030304 developmental biology, Regulation of gene expression, 0303 health sciences, Binding Sites, cellular homeostasis and growth, biology, Research, Computational Biology, High-Throughput Nucleotide Sequencing, Promoter, Chromatin, Nucleosomes, Histone, Gene Expression Regulation, RNA polymerase, Gene Knockdown Techniques, Multigene Family, 030220 oncology & carcinogenesis, NIH 3T3 Cells, biology.protein, RNA Polymerase II, Transcription Initiation Site, Pol1 Transcription Initiation Complex Proteins, Chromatin immunoprecipitation, DNA Damage, Protein Binding

Abstract

Mechanisms to coordinate programs of highly transcribed genes required for cellular homeostasis and growth are unclear. Upstream binding transcription factor (UBTF, also called UBF) is thought to function exclusively in RNA polymerase I (Pol I)-specific transcription of the ribosomal genes. Here, we report that the two isoforms of UBTF (UBTF1/2) are also enriched at highly expressed Pol II-transcribed genes throughout the mouse genome. Further analysis of UBTF1/2 DNA binding in immortalized human epithelial cells and their isogenically matched transformed counterparts reveals an additional repertoire of UBTF1/2-bound genes involved in the regulation of cell cycle checkpoints and DNA damage response. As proof of a functional role for UBTF1/2 in regulating Pol II transcription, we demonstrate that UBTF1/2 is required for recruiting Pol II to the highly transcribed histone gene clusters and for their optimal expression. Intriguingly, lack of UBTF1/2 does not affect chromatin marks or nucleosome density at histone genes. Instead, it results in increased accessibility of the histone promoters and transcribed regions to micrococcal nuclease, implicating UBTF1/2 in mediating DNA accessibility. Unexpectedly, UBTF2, which does not function in Pol I transcription, is sufficient to regulate histone gene expression in the absence of UBTF1. Moreover, depletion of UBTF1/2 and subsequent reduction in histone gene expression is associated with DNA damage and genomic instability independent of Pol I transcription. Thus, we have uncovered a novel role for UBTF1 and UBTF2 in maintaining genome stability through coordinating the expression of highly transcribed Pol I (UBTF1 activity) and Pol II genes (UBTF2 activity). Refereed/Peer-reviewed

Published

2014

19. Natural diversity of the malaria vectorAnopheles gambiae

Author

Bradley J. White, Craig S. Wilding, Dan Mead, Rachel Giacomantonio, Abdoulaye Diabaté, Kate Rowlands, Dominic P. Kwiatkowski, Charles M. Mbogo, Jim Stalker, Kenneth D. Vernick, Victoria Cornelius, Andrew D. Kern, Krzysztof Kluczynski, Ben Jeffrey, Joao Dinis, Alessandra della Torre, David Weetman, Matthew W. Hahn, Beniamino Caputo, Alison T. Isaacs, Lee Hart, Christina Hubbart, Kyanne R. Rohatgi, Martin J. Donnelly, Nohal Elissa, Ian Wright, Chris S Clarkson, Richard D. Pearson, Daniel E. Neafsey, Krzysztof Kozak, Christina M. Bergey, Diego Ayala, Mara K. N. Lawniczak, Anna E. Jeffreys, Paul Vauterin, Charles Godfray, Seth Redmond, Bronwyn MacInnis, Christa Henrichs, Michelle M. Riehle, João Pinto, Nicholas J. Harding, Cinzia Malangone, Kirk A. Rockett, Samantha M. O’Loughlin, Dushyanth Jyothi, Tiago Antao, Arlete D. Troco, Austin Burt, Henry Mawejje, Carlo Costantini, Janet Midega, Boubacar Coulibaly, Eleanor Drury, Michael C Fontaine, Igor V. Sharakhov, Giordano Bottà, Daniel R. Schrider, Philip Bejon, Alistair Miles, and Nora J. Besansky

Subjects

0301 basic medicine, Genetic diversity, biology, Anopheles gambiae, biology.organism_classification, medicine.disease, Genome, 03 medical and health sciences, Mosquito control, 030104 developmental biology, Evolutionary biology, parasitic diseases, Threatened species, medicine, Genetic variability, Selection (genetic algorithm), Malaria

Abstract

The sustainability of malaria control in Africa is threatened by rising levels of insecticide resistance, and new tools to prevent malaria transmission are urgently needed. To gain a better understanding of the mosquito populations that transmit malaria, we sequenced the genomes of 765 wild specimens ofAnopheles gambiaeandAnopheles coluzziisampled from 15 locations across Africa. The data reveal high levels of genetic diversity, with over 50 million single nucleotide polymorphisms across the 230 Mbp genome. We observe complex patterns of population structure and marked variations in local population size, some of which may be due at least in part to malaria control interventions. Insecticide resistance genes show strong signatures of recent selection associated with multiple independent mutations spreading over large geographical distances and between species. The genetic variability of natural populations substantially reduces the target space for novel gene-drive strategies for mosquito control. This large dataset provides a foundation for tracking the emergence and spread of insecticide resistance and developing new vector control tools.

Published

2016

20. Genome variation and meiotic recombination in Plasmodium falciparum: insights from deep sequencing of genetic crosses

Author

Zamin Iqbal, Michel Theron, Paul Vauterin, Kelda Gould, Susana Campino, Julian C. Rayner, Eleanor Drury, Daniel Mead, Upeka Samarakoon, Bronwyn MacInnis, Karen Hayton, Xin-zhuan Su, Michael T. Ferdig, Lisa C. Ranford-Cartwright, Thomas E. Wellems, Alistair Miles, Jonathan M. Mwangi, Gil McVean, Richard D. Pearson, Dominic P. Kwiatkowski, Valentin Ruano Rubio, and John O'Brien

Subjects

Genetics, 0303 health sciences, Genomics, Single-nucleotide polymorphism, Biology, Genome, Deep sequencing, 3. Good health, 03 medical and health sciences, symbols.namesake, 0302 clinical medicine, Genotype, Mendelian inheritance, symbols, Copy-number variation, Indel, 030217 neurology & neurosurgery, 030304 developmental biology

Abstract

The malaria parasite Plasmodium falciparum has a great capacity for evolutionary adaptation to evade host immunity and develop drug resistance. Current understanding of parasite evolution is impeded by the fact that a large fraction of the genome is either highly repetitive or highly variable, and thus difficult to analyse using short read technologies. Here we describe a resource of deep sequencing data on parents and progeny from genetic crosses, which has enabled us to perform the first genome-wide, integrated analysis of SNP, INDEL and complex polymorphisms, using Mendelian error rates as an indicator of genotypic accuracy. These data reveal that INDELs are exceptionally abundant, being more common than SNPs and thus the dominant mode of polymorphism within the core genome. We use the high density of SNP and INDEL markers to analyse patterns of meiotic recombination, confirming a high rate of crossover events, and providing the first estimates for the rate of non-crossover events and the length of conversion tracts. We observe several instances of recombination that modify copy number variants associated with drug resistance, demonstrating a mechanism whereby fitness costs associated with resistance mutations could be compensated and greater phenotypic plasticity could be acquired. We describe a novel web application that allows these data to be explored in detail.

Published

2015