Your search keyword '"Nicholas Hathaway"' showing total 4 results

1. Targeted and whole-genome sequencing reveal a north-south divide in P. falciparum drug resistance markers and genetic structure in Mozambique

Author

Clemente da Silva, Simone Boene, Debayan Datta, Eduard Rovira-Vallbona, Andrés Aranda-Díaz, Pau Cisteró, Nicholas Hathaway, Sofonias Tessema, Arlindo Chidimatembue, Glória Matambisso, Abel Nhama, Eusebio Macete, Arnau Pujol, Lidia Nhamussua, Beatriz Galatas, Caterina Guinovart, Sónia Enosse, Eva De Carvalho, Eric Rogier, Mateusz M. Plucinski, James Colborn, Rose Zulliger, Abuchahama Saifodine, Pedro L. Alonso, Baltazar Candrinho, Bryan Greenhouse, Pedro Aide, Francisco Saute, and Alfredo Mayor

Subjects

Biology (General), QH301-705.5

Abstract

Abstract Mozambique is one of the four African countries which account for over half of all malaria deaths worldwide, yet little is known about the parasite genetic structure in that country. We performed P. falciparum amplicon and whole genome sequencing on 2251 malaria-infected blood samples collected in 2015 and 2018 in seven provinces of Mozambique to genotype antimalarial resistance markers and interrogate parasite population structure using genome-wide microhaplotyes. Here we show that the only resistance-associated markers observed at frequencies above 5% were pfmdr1-184F (59%), pfdhfr-51I/59 R/108 N (99%) and pfdhps-437G/540E (89%). The frequency of pfdhfr/pfdhps quintuple mutants associated with sulfadoxine-pyrimethamine resistance increased from 80% in 2015 to 89% in 2018 (p

Published

2023

2. Hypnozoite depletion in successive Plasmodium vivax relapses.

Author

Rintis Noviyanti, Kelly Carey-Ewend, Leily Trianty, Christian Parobek, Agatha Mia Puspitasari, Sujata Balasubramanian, Zackary Park, Nicholas Hathaway, Retno A S Utami, Saraswati Soebianto, Jeny Jeny, Frilasita Yudhaputri, Aditya Perkasa, Farah N Coutrier, Yusrifar K Tirta, Lenny Ekawati, Bagus Tjahyono, Inge Sutanto, Erni J Nelwan, Herawati Sudoyo, J Kevin Baird, and Jessica T Lin

Subjects

Arctic medicine. Tropical medicine, RC955-962, Public aspects of medicine, RA1-1270

Abstract

Genotyping Plasmodium vivax relapses can provide insights into hypnozoite biology. We performed targeted amplicon sequencing of 127 relapses occurring in Indonesian soldiers returning to malaria-free Java after yearlong deployment in malarious Eastern Indonesia. Hepatic carriage of multiple hypnozoite clones was evident in three-quarters of soldiers with two successive relapses, yet the majority of relapse episodes only displayed one clonal population. The number of clones detected in relapse episodes decreased over time and through successive relapses, especially in individuals who received hypnozoiticidal therapy. Interrogating the multiplicity of infection in this P. vivax relapse cohort reveals evidence of independent activation and slow depletion of hypnozoites over many months by multiple possible mechanisms, including parasite senescence and host immunity.

Published

2022

3. A novel CRISPR-based malaria diagnostic capable of Plasmodium detection, species differentiation, and drug-resistance genotyping

Author

Clark H. Cunningham, Christopher M. Hennelly, Jessica T. Lin, Ratawan Ubalee, Ross M. Boyce, Edgar M. Mulogo, Nicholas Hathaway, Kyaw L. Thwai, Fernandine Phanzu, Albert Kalonji, Kashamuka Mwandagalirwa, Antoinette Tshefu, Jonathan J. Juliano, and Jonathan B. Parr

Subjects

SHERLOCK, Malaria, CRISPR, Cas13a, Diagnostic, Medicine, Medicine (General), R5-920

Abstract

Background: CRISPR-based diagnostics are a new class of highly sensitive and specific assays with multiple applications in infectious disease diagnosis. SHERLOCK, or Specific High-Sensitivity Enzymatic Reporter UnLOCKing, is one such CRISPR-based diagnostic that combines recombinase polymerase pre-amplification, CRISPR-RNA base-pairing, and LwCas13a activity for nucleic acid detection. Methods: We developed SHERLOCK assays capable of detecting all Plasmodium species known to cause human malaria and species-specific detection of P. vivax and P. falciparum, the species responsible for the majority of malaria cases worldwide. We further tested these assays using a diverse panel of clinical samples from the Democratic Republic of the Congo, Uganda, and Thailand and pools of Anopheles mosquitoes from Thailand. In addition, we developed a prototype SHERLOCK assay capable of detecting the dihydropteroate synthetase (dhps) single nucleotide variant A581G associated with P. falciparum sulfadoxine resistance. Findings: The suite of Plasmodium assays achieved analytical sensitivities ranging from 2•5-18•8 parasites per reaction when tested against laboratory strain genomic DNA. When compared to real-time PCR, the P. falciparum assay achieved 94% sensitivity and 94% specificity during testing of 123 clinical samples. Compared to amplicon-based deep sequencing, the dhps SHERLOCK assay achieved 73% sensitivity and 100% specificity when applied to a panel of 43 clinical samples, with false-negative calls only at lower parasite densities. Interpretation: These novel SHERLOCK assays demonstrate the versatility of CRISPR-based diagnostics and their potential as a new generation of molecular tools for malaria diagnosis and surveillance. Funding: National Institutes of Health (T32GM007092, R21AI148579, K24AI134990, R01AI121558, UL1TR002489, P30CA016086)

Published

2021

4. Sex-based differences in clearance of chronic Plasmodium falciparum infection

Author

Jessica Briggs, Noam Teyssier, Joaniter I Nankabirwa, John Rek, Prasanna Jagannathan, Emmanuel Arinaitwe, Teun Bousema, Chris Drakeley, Margaret Murray, Emily Crawford, Nicholas Hathaway, Sarah G Staedke, David Smith, Phillip J Rosenthal, Moses Kamya, Grant Dorsey, Isabel Rodriguez-Barraquer, and Bryan Greenhouse

Subjects

molecular epidemiology, asymptomatic malaria infection, amplicon deep sequencing, duration of infection, sex-based differences, Medicine, Science, Biology (General), QH301-705.5

Abstract

Multiple studies have reported a male bias in incidence and/or prevalence of malaria infection in males compared to females. To test the hypothesis that sex-based differences in host-parasite interactions affect the epidemiology of malaria, we intensively followed Plasmodium falciparum infections in a cohort in a malaria endemic area of eastern Uganda and estimated both force of infection (FOI) and rate of clearance using amplicon deep-sequencing. We found no evidence of differences in behavioral risk factors, incidence of malaria, or FOI by sex. In contrast, females cleared asymptomatic infections at a faster rate than males (hazard ratio [HR]=1.82, 95% CI 1.20 to 2.75 by clone and HR = 2.07, 95% CI 1.24 to 3.47 by infection event) in multivariate models adjusted for age, timing of infection onset, and parasite density. These findings implicate biological sex-based differences as an important factor in the host response to this globally important pathogen.

Published

2020