Search

Your search keyword '"Engelthaler, David M."' showing total 394 results
Start Over Author "Engelthaler, David M." Publication Year Range Last 10 years
394 results on '"Engelthaler, David M."'

1. Bedaquiline resistance in patients with drug-resistant tuberculosis in Cape Town, South Africa: a retrospective longitudinal cohort study

Author

Derendinger, Brigitta, Dippenaar, Anzaan, de Vos, Margaretha, Huo, Stella, Alberts, Rencia, Tadokera, Rebecca, Limberis, Jason, Sirgel, Frik, Dolby, Tania, Spies, Claudia, Reuter, Anja, Folkerts, Megan, Allender, Christopher, Lemmer, Darrin, Van Rie, Annelies, Gagneux, Sebastien, Rigouts, Leen, Riele, Julian te, Dheda, Keertan, Engelthaler, David M, Warren, Robin, Metcalfe, John, Cox, Helen, and Theron, Grant

Subjects
Medical Microbiology, Biomedical and Clinical Sciences, Clinical Sciences, Biological Sciences, Tuberculosis, Genetics, Rare Diseases, Prevention, Antimicrobial Resistance, Infectious Diseases, Orphan Drug, Clinical Research, Human Genome, HIV/AIDS, Biotechnology, Patient Safety, Evaluation of treatments and therapeutic interventions, 2.1 Biological and endogenous factors, 6.1 Pharmaceuticals, Development of treatments and therapeutic interventions, 5.1 Pharmaceuticals, Aetiology, Infection, Good Health and Well Being, Adult, Humans, Adolescent, Antitubercular Agents, South Africa, Mycobacterium tuberculosis, Retrospective Studies, Microbial Sensitivity Tests, Longitudinal Studies, Reinfection, Tuberculosis, Multidrug-Resistant, Microbiology, Immunology, Medical microbiology
Abstract

BackgroundBedaquiline is a life-saving tuberculosis drug undergoing global scale-up. People at risk of weak tuberculosis drug regimens are a priority for novel drug access despite the potential source of Mycobacterium tuberculosis-resistant strains. We aimed to characterise bedaquiline resistance in individuals who had sustained culture positivity during bedaquiline-based treatment.MethodsWe did a retrospective longitudinal cohort study of adults (aged ≥18 years) with culture-positive pulmonary tuberculosis who received at least 4 months of a bedaquiline-containing regimen from 12 drug-resistant tuberculosis treatment facilities in Cape Town, South Africa, between Jan 20, 2016, and Nov 20, 2017. Sputum was programmatically collected at baseline (ie, before bedaquiline initiation) and each month to monitor treatment response per the national algorithm. The last available isolate from the sputum collected at or after 4 months of bedaquiline was designated the follow-up isolate. Phenotypic drug susceptibility testing for bedaquiline was done on baseline and follow-up isolates in MGIT960 media (WHO-recommended critical concentration of 1 μg/mL). Targeted deep sequencing for Rv0678, atpE, and pepQ, as well as whole-genome sequencing were also done.FindingsIn total, 40 (31%) of 129 patients from an estimated pool were eligible for this study. Overall, three (8%) of 38 patients assessable by phenotypic drug susceptibility testing for bedaquiline had primary resistance, 18 (47%) gained resistance (acquired or reinfection), and 17 (45%) were susceptible at both baseline and follow-up. Several Rv0678 and pepQ single-nucleotide polymorphisms and indels were associated with resistance. Although variants occurred in Rv0676c and Rv1979c, these variants were not associated with resistance. Targeted deep sequencing detected low-level variants undetected by whole-genome sequencing; however, none were in genes without variants already detected by whole-genome sequencing. Patients with baseline fluoroquinolone resistance, clofazimine exposure, and four or less effective drugs were more likely to have bedaquiline-resistant gain. Resistance gain was primarily due to acquisition; however, some reinfection by resistant strains occurred.InterpretationBedaquiline-resistance gain, for which we identified risk factors, was common in these programmatically treated patients with sustained culture positivity. Our study highlights risks associated with implementing life-saving new drugs and shows evidence of bedaquiline-resistance transmission. Routine drug susceptibility testing should urgently accompany scale-up of new drugs; however, rapid drug susceptibility testing for bedaquiline remains challenging given the diversity of variants observed.FundingDoris Duke Charitable Foundation, US National Institute of Allergy and Infectious Diseases, South African Medical Research Council, National Research Foundation, Research Foundation Flanders, Stellenbosch University Faculty of Medicine Health Sciences, South African National Research Foundation, Swiss National Science Foundation, and Wellcome Trust.

Published
2023

2. Phylogenomic Placement of American Southwest-Associated Clinical and Veterinary Isolates Expands Evidence for Distinct Cryptococcus gattii VGVI

Author

Monroy-Nieto, Juan, Bowers, Jolene R, Montfort, Parker, Adame, Guillermo, Taverna, Constanza Giselle, Yaglom, Hayley, Sykes, Jane E, Brady, Shane, Mochon, A Brian, Meyer, Wieland, Komatsu, Kenneth, and Engelthaler, David M

Subjects
Biological Sciences, Biomedical and Clinical Sciences, Genetics, Microbiology, Clinical Sciences, Infectious Diseases, Cryptococcus, whole-genome sequencing, VGVI, phylogenomics, molecular type, Medical microbiology
Abstract

Whole-genome sequencing has advanced our understanding of the population structure of the pathogenic species complex Cryptococcus gattii, which has allowed for the phylogenomic specification of previously described major molecular type groupings and novel lineages. Recently, isolates collected in Mexico in the 1960s were determined to be genetically distant from other known molecular types and were classified as VGVI. We sequenced four clinical isolates and one veterinary isolate collected in the southwestern United States and Argentina from 2012 to 2021. Phylogenomic analysis groups these genomes with those of the Mexican VGVI isolates, expanding VGVI into a clade and establishing this molecular type as a clinically important population. These findings also potentially expand the known Cryptococcus ecological range with a previously unrecognized endemic area.

Published
2022

3. Genomic Epidemiology Linking Nonendemic Coccidioidomycosis to Travel

Author

Monroy-Nieto, Juan, Gade, Lalitha, Benedict, Kaitlin, Etienne, Kizee A., Litvintseva, Anastasia P., Bowers, Jolene R., Engelthaler, David M., and Chow, Nancy A.

Subjects
Coccidioidomycosis -- Risk factors, Fungi, Pathogenic -- Identification and classification -- Genetic aspects -- Distribution, Travelers -- Health aspects, Disease transmission -- Risk factors, Company distribution practices, Health
Abstract

Coccidioides immitis and C. posadasii, the etiologic agents of coccidioidomycosis, also known as Valley fever, are environmental filamentous fungi with distinct geographic ranges in the western United States, northern Mexico, [...]

Published
2023
Full Text
View/download PDF

4. Author Correction: Integrating standardized whole genome sequence analysis with a global Mycobacterium tuberculosis antibiotic resistance knowledgebase

Author

Ezewudo, Matthew, Borens, Amanda, Chiner-Oms, Álvaro, Miotto, Paolo, Chindelevitch, Leonid, Starks, Angela M, Hanna, Debra, Liwski, Richard, Zignol, Matteo, Gilpin, Christopher, Niemann, Stefan, Kohl, Thomas Andreas, Warren, Robin M, Crook, Derrick, Gagneux, Sebastien, Hoffner, Sven, Rodrigues, Camilla, Comas, Iñaki, Engelthaler, David M, Alland, David, Rigouts, Leen, Lange, Christoph, Dheda, Keertan, Hasan, Rumina, McNerney, Ruth, Cirillo, Daniela M, Schito, Marco, Rodwell, Timothy C, and Posey, James

Subjects
Microbiology, Biological Sciences, Infection, Good Health and Well Being
Abstract

An amendment to this paper has been published and can be accessed via a link at the top of the paper.

Published
2020

5. Utility of Targeted, Amplicon-Based Deep Sequencing To Detect Resistance to First-Line Tuberculosis Drugs in Botswana.

Author

Wang, Qiao, Modongo, Chawangwa, Allender, Christopher, Engelthaler, David M, Warren, Robin M, Zetola, Nicola M, and Shin, Sanghyuk S

Subjects
Medical Microbiology, Biomedical and Clinical Sciences, Clinical Sciences, Biological Sciences, Tuberculosis, Emerging Infectious Diseases, Rare Diseases, Vaccine Related, Biodefense, Prevention, Intellectual and Developmental Disabilities (IDD), Infectious Diseases, Antimicrobial Resistance, Brain Disorders, HIV/AIDS, Down Syndrome, Development of treatments and therapeutic interventions, 5.1 Pharmaceuticals, Infection, Good Health and Well Being, Adult, Antitubercular Agents, Botswana, Female, High-Throughput Nucleotide Sequencing, Humans, Isoniazid, Male, Microbial Sensitivity Tests, Middle Aged, Mycobacterium tuberculosis, Phenotype, Sensitivity and Specificity, Tuberculosis, Multidrug-Resistant, Young Adult, HIV infections, next-generation sequencing, diagnostics, drug-resistant tuberculosis, heteroresistance, single-molecule overlapping reads, Microbiology, Pharmacology and Pharmaceutical Sciences, Medical microbiology, Pharmacology and pharmaceutical sciences
Abstract

Multidrug-resistant tuberculosis (TB) is an alarming threat, and targeted deep sequencing (DS) may be an effective method for rapid identification of drug-resistant profiles, including detection of heteroresistance. We evaluated the sensitivity and specificity of targeted DS versus phenotypic drug susceptibility testing (pDST) among patients starting first-line anti-TB therapy in Botswana. Overall, we found high concordance between DS and pDST. Lower sensitivity of DS, which targets established high-confidence resistance variants, was observed for detecting isoniazid resistance among HIV-infected patients.

Published
2019

6. Whole-genome and targeted sequencing of drug-resistant Mycobacterium tuberculosis on the iSeq100 and MiSeq: A performance, ease-of-use, and cost evaluation

Author

Colman, Rebecca E, Mace, Aurélien, Seifert, Marva, Hetzel, Jonathan, Mshaiel, Haifa, Suresh, Anita, Lemmer, Darrin, Engelthaler, David M, Catanzaro, Donald G, Young, Amanda G, Denkinger, Claudia M, and Rodwell, Timothy C

Subjects
Biomedical and Clinical Sciences, Clinical Sciences, Biotechnology, Vaccine Related, Rare Diseases, Human Genome, Emerging Infectious Diseases, Infectious Diseases, Genetics, Tuberculosis, Infection, Good Health and Well Being, Cost-Benefit Analysis, DNA, Bacterial, Drug Resistance, Multiple, Bacterial, High-Throughput Nucleotide Sequencing, Humans, Mycobacterium tuberculosis, Reproducibility of Results, Sequence Analysis, DNA, Time Factors, Tuberculosis, Multidrug-Resistant, Medical and Health Sciences, General & Internal Medicine, Biomedical and clinical sciences, Health sciences
Abstract

BackgroundAccurate, comprehensive, and timely detection of drug-resistant tuberculosis (TB) is essential to inform patient treatment and enable public health surveillance. This is crucial for effective control of TB globally. Whole-genome sequencing (WGS) and targeted next-generation sequencing (NGS) approaches have potential as rapid in vitro diagnostics (IVDs), but the complexity of workflows, interpretation of results, high costs, and vulnerability of instrumentation have been barriers to broad uptake outside of reference laboratories, especially in low- and middle-income countries. A new, solid-state, tabletop sequencing instrument, Illumina iSeq100, has the potential to decentralize NGS for individual patient care.Methods and findingsIn this study, we evaluated WGS and targeted NGS for TB on both the new iSeq100 and the widely used MiSeq (both manufactured by Illumina) and compared sequencing performance, costs, and usability. We utilized DNA libraries produced from Mycobacterium tuberculosis clinical isolates for the evaluation. We conducted WGS on three strains and observed equivalent uniform genome coverage with both platforms and found the depth of coverage obtained was consistent with the expected data output. Utilizing the standardized, cloud-based ReSeqTB bioinformatics pipeline for variant analysis, we found the two platforms to have 94.0% (CI 93.1%-94.8%) agreement, in comparison to 97.6% (CI 97%-98.1%) agreement for the same libraries on two MiSeq instruments. For the targeted NGS approach, 46 M. tuberculosis-specific amplicon libraries had 99.6% (CI 98.0%-99.9%) agreement between the iSeq100 and MiSeq data sets in drug resistance-associated SNPs. The upfront capital costs are almost 5-fold lower for the iSeq100 ($19,900 USD) platform in comparison to the MiSeq ($99,000 USD); however, because of difference in the batching capabilities, the price per sample for WGS was higher on the iSeq100. For WGS of M. tuberculosis at the minimum depth of coverage of 30x, the cost per sample on the iSeq100 was $69.44 USD versus $28.21 USD on the MiSeq, assuming a 2 × 150 bp run on a v3 kit. In terms of ease of use, the sequencing workflow of iSeq100 has been optimized to only require 27 minutes total of hands-on time pre- and post-run, and the maintenance is simplified by a single-use cartridge-based fluidic system. As these are the first sequencing attempts on the iSeq100 for M. tuberculosis, the sequencing pool loading concentration still needs optimization, which will affect sequencing error and depth of coverage. Additionally, the costs are based on current equipment and reagent costs, which are subject to change.ConclusionsThe iSeq100 instrument is capable of running existing TB WGS and targeted NGS library preparations with comparable accuracy to the MiSeq. The iSeq100 has reduced sequencing workflow hands-on time and is able to deliver sequencing results in

Published
2019

7. Convenience Sampling Yields No Evidence of SARS-CoV-2 Infection in Free-Ranging Mammalian Wildlife in Arizona, USA, 2021–23.

Author

Yaglom, Hayley D., Van Pelt, Lolita, Howard, April L., Jansen, Brian, Smith, Payton, Sorensen, Rebekah, Hecht, Gavriella, Venkat, Heather, Justice-Allen, Anne, Bergman, David L., and Engelthaler, David M.

Abstract

Susceptibility of free-ranging US wildlife to SARS-CoV-2 infection has been documented. Nasal or oral swabs and blood from 337 wild mammals (31 species) in Arizona USA, tested for antibodies and by reverse-transcription PCR, did not reveal evidence of SARS-CoV-2. Broader surveillance efforts are necessary to understand the role of wildlife. [ABSTRACT FROM AUTHOR]

Published
2024
Full Text
View/download PDF

8. The Hidden Epidemic of Isoniazid-Resistant Tuberculosis in South Africa.

Author

Klopper, Marisa, van der Merwe, Charnay J., van der Heijden, Yuri F., Folkerts, Megan, Loubser, Johannes, Streicher, Elizabeth M., Mekler, Kate, Hayes, Cindy, Engelthaler, David M., Metcalfe, John Z., and Warren, Robin M.

Subjects
WHOLE genome sequencing, ISONIAZID, TUBERCULOSIS, GENOTYPES, PHENOTYPES
Abstract

Rationale: Isoniazid-resistant tuberculosis (Hr-TB) is often overlooked in diagnostic algorithms because of reliance on first-line molecular assays testing only for rifampicin resistance. Objectives: To determine the prevalence, outcomes, and molecular mechanisms associated with rifampin-susceptible, isoniazid-resistant TB (Hr-TB) in the Eastern Cape, South Africa. Methods: Between April 2016 and October 2017, sputum samples were collected from patients with rifampin-susceptible TB at baseline and at Weeks 7 and 23 of drug-susceptible TB treatment. We performed isoniazid phenotypic and genotypic drug susceptibility testing, including FluoroTypeMTBDR, Sanger sequencing, targeted next-generation sequencing, and whole-genome sequencing. Results: We analyzed baseline isolates from 766 patients with rifampin-susceptible TB. Of 89 patients (11.7%) who were found to have Hr-TB, 39 (44%) had canonical katG or inhA promoter mutations; 35 (39%) had noncanonical katG mutations (including 5 with underlying large deletions); 4 (5%) had mutations in other candidate genes associated with isoniazid resistance. For 11 (12.4%), no cause of resistance was found. Conclusions: Among patients with rifampin-susceptible TB who were diagnosed using first-line molecular TB assays, there is a high prevalence of Hr-TB. Phenotypic drug susceptibility testing remains the gold standard. To improve the performance of genetic-based phenotyping tests, all isoniazid resistance–associated regions should be included, and such tests should have the ability to identify underlying mutations. [ABSTRACT FROM AUTHOR]

Published
2024
Full Text
View/download PDF

9. Large Clusters of Invasive emm49 Group A Streptococcus Identified Within Arizona Health Care Facilities Through Statewide Genomic Surveillance System, 2019–2021.

Author

Yaglom, Hayley D, Bhattarai, Rachana, Lemmer, Darrin, Rust, Laura, Ridenour, Chase, Chorbi, Kaitlyn, Kim, Elizabeth, Centner, Heather, Sheridan, Krystal, Jasso-Selles, Daniel, Erickson, Daryn E, French, Chris, Bowers, Jolene R, Valentine, Michael, Francis, Drew, Hepp, Crystal M, Brady, Shane, Komatsu, Kenneth K, and Engelthaler, David M

Subjects
LONG-term care facilities, HEALTH facilities, GENOMICS, PUBLIC health, STREPTOCOCCUS
Abstract

A statewide genomic surveillance system for invasive Group A Streptococcus was implemented in Arizona in June 2019, resulting in 1046 isolates being submitted for genomic analysis to characterize emm types and identify transmission clusters. Eleven of the 32 identified distinct emm types comprised >80% of samples, with 29.7% of all isolates being typed as emm 49 (and its genetic derivative emm 151). Phylogenetic analysis initially identified an emm 49 genomic cluster of 4 isolates that rapidly expanded over subsequent months (June 2019 to February 2020). Public health investigations identified epidemiologic links with 3 different long-term care facilities, resulting in specific interventions. Unbiased genomic surveillance allowed for identification and response to clusters that would have otherwise remained undetected. [ABSTRACT FROM AUTHOR]

Published
2024
Full Text
View/download PDF

10. Mixed Mycobacterium tuberculosis-Strain Infections Are Associated With Poor Treatment Outcomes Among Patients With Newly Diagnosed Tuberculosis, Independent of Pretreatment Heteroresistance.

Author

Shin, Sanghyuk S, Modongo, Chawangwa, Baik, Yeonsoo, Allender, Christopher, Lemmer, Darrin, Colman, Rebecca E, Engelthaler, David M, Warren, Robin M, and Zetola, Nicola M

Subjects
Antimicrobial Resistance, Rare Diseases, Infectious Diseases, Tuberculosis, Orphan Drug, 5.1 Pharmaceuticals, Development of treatments and therapeutic interventions, Infection, Good Health and Well Being, Adult, Antitubercular Agents, Botswana, Female, Genotype, Humans, Male, Middle Aged, Mycobacterium tuberculosis, Tuberculosis, Multidrug-Resistant, Tuberculosis, Pulmonary, Young Adult, Next-generation sequencing, drug-resistant tuberculosis, diagnostics, HIV infections, treatment outcome, Biological Sciences, Medical and Health Sciences, Microbiology
Abstract

BackgroundHeteroresistant Mycobacterium tuberculosis infections (defined as concomitant infection with drug-resistant and drug-susceptible strains) may explain the higher risk of poor tuberculosis treatment outcomes observed among patients with mixed-strain M. tuberculosis infections. We investigated the clinical effect of mixed-strain infections while controlling for pretreatment heteroresistance in a population-based sample of patients with tuberculosis starting first-line tuberculosis therapy in Botswana.MethodsWe performed 24-locus mycobacterial interspersed repetitive unit-variable number tandem-repeat analysis and targeted deep sequencing on baseline primary cultured isolates to detect mixed infections and heteroresistance, respectively. Drug-sensitive, micro-heteroresistant, macro-heteroresistant, and fixed-resistant infections were defined as infections in which the frequency of resistance was

Published
2018

11. Flucytosine resistance in Cryptococcus gattii is indirectly mediated by the FCY2-FCY1-FUR1 pathway

Author

Vu, Kiem, Thompson, George R, Roe, Chandler C, Sykes, Jane E, Dreibe, Elizabeth M, Lockhart, Shawn R, Meyer, Wieland, Engelthaler, David M, and Gelli, Angie

Subjects
Biological Sciences, Biomedical and Clinical Sciences, Genetics, Microbiology, Clinical Sciences, Medical Microbiology, Biotechnology, Human Genome, Infectious Diseases, Aetiology, 2.1 Biological and endogenous factors, Antifungal Agents, Cryptococcosis, Cryptococcus gattii, Cytosine Deaminase, DNA Mutational Analysis, Flucytosine, Fungal Proteins, Humans, Male, Membrane Transport Proteins, Microbial Sensitivity Tests, Pentosyltransferases, Protein Interaction Maps, Sequence Analysis, DNA, flucytosine resistance, cytosine deaminase, FCY1, Clinical sciences, Medical microbiology
Abstract

Cryptococcosis is an opportunistic fungal infection caused by members of the two sibling species complexes: Cryptococcus neoformans and Cryptococcus gattii. Flucytosine (5FC) is one of the most widely used antifungals against Cryptococcus spp., yet very few studies have looked at the molecular mechanisms responsible for 5FC resistance in this pathogen. In this study, we examined 11 C. gattii clinical isolates of the major molecular type VGIII based on differential 5FC susceptibility and asked whether there were genomic changes in the key genes involved in flucytosine metabolism. Susceptibility assays and sequencing analysis revealed an association between a point mutation in the cytosine deaminase gene (FCY1) and 5FC resistance in two of the studied 5FC resistant C. gattii VGIII clinical isolates, B9322 and JS5. This mutation results in the replacement of arginine for histidine at position 29 and occurs within a variable stretch of amino acids. Heterologous expression of FCY1 and spot sensitivity assays, however, demonstrated that this point mutation did not have any effect on FCY1 activities and was not responsible for 5FC resistance. Comparative sequence analysis further showed that no changes in the amino acid sequence and no genomic alterations were observed within 1 kb of the upstream and downstream sequences of either cytosine permeases (FCY2-4) or uracil phosphoribosyltransferase (FUR1) genes in 5FC resistant and 5FC susceptible C. gattii VGIII isolates. The herein obtained results suggest that the observed 5FC resistance in the isolates B9322 and JS5 is due to changes in unknown protein(s) or pathway(s) that regulate flucytosine metabolism.

Published
2018

12. Dating the Cryptococcus gattii Dispersal to the North American Pacific Northwest

Author

Roe, Chandler C, Bowers, Jolene, Oltean, Hanna, DeBess, Emilio, Dufresne, Philippe J, McBurney, Scott, Overy, David P, Wanke, Bodo, Lysen, Colleen, Chiller, Tom, Meyer, Wieland, Thompson, George R, Lockhart, Shawn R, Hepp, Crystal M, and Engelthaler, David M

Subjects
Human Genome, Infectious Diseases, Genetics, Infection, Cryptococcus, genomics, molecular epidemiology, mycology, Immunology, Microbiology
Abstract

The emergence of Cryptococcus gattii, previously regarded as a predominantly tropical pathogen, in the temperate climate of the North American Pacific Northwest (PNW) in 1999 prompted several questions. The most prevalent among these was the timing of the introduction of this pathogen to this novel environment. Here, we infer tip-dated timing estimates for the three clonal C. gattii populations observed in the PNW, VGIIa, VGIIb, and VGIIc, based on whole-genome sequencing of 134 C. gattii isolates and using Bayesian evolutionary analysis by sampling trees (BEAST). We estimated the nucleotide substitution rate for each lineage (1.59 × 10-8, 1.59 × 10-8, and 2.70 × 10-8, respectively) to be an order of magnitude higher than common neutral fungal mutation rates (2.0 × 10-9), indicating a microevolutionary rate (e.g., successive clonal generations in a laboratory) in comparison to a species' slower, macroevolutionary rate (e.g., when using fossil records). The clonal nature of the PNW C. gattii emergence over a narrow number of years would therefore possibly explain our higher mutation rates. Our results suggest that the mean time to most recent common ancestor for all three sublineages occurred within the last 60 to 100 years. While the cause of C. gattii dispersal to the PNW is still unclear, our research estimates that the arrival is neither ancient nor very recent (i.e.,

Published
2018

13. Integrating standardized whole genome sequence analysis with a global Mycobacterium tuberculosis antibiotic resistance knowledgebase

Author

Ezewudo, Matthew, Borens, Amanda, Chiner-Oms, Álvaro, Miotto, Paolo, Chindelevitch, Leonid, Starks, Angela M, Hanna, Debra, Liwski, Richard, Zignol, Matteo, Gilpin, Christopher, Niemann, Stefan, Kohl, Thomas Andreas, Warren, Robin M, Crook, Derrick, Gagneux, Sebastien, Hoffner, Sven, Rodrigues, Camilla, Comas, Iñaki, Engelthaler, David M, Alland, David, Rigouts, Leen, Lange, Christoph, Dheda, Keertan, Hasan, Rumina, McNerney, Ruth, Cirillo, Daniela M, Schito, Marco, Rodwell, Timothy C, and Posey, James

Subjects
Biological Sciences, Bioinformatics and Computational Biology, Biomedical and Clinical Sciences, Genetics, Microbiology, Clinical Sciences, Human Genome, Tuberculosis, Antimicrobial Resistance, Rare Diseases, Biotechnology, Infectious Diseases, Aetiology, 2.1 Biological and endogenous factors, Infection, Good Health and Well Being, Antitubercular Agents, Bacterial Proteins, Drug Resistance, Multiple, Bacterial, Genome, Bacterial, Genotype, Humans, Knowledge Bases, Mutation, Mycobacterium tuberculosis, Polymorphism, Single Nucleotide, Sequence Analysis, DNA, Tuberculosis, Multidrug-Resistant, Whole Genome Sequencing
Abstract

Drug-resistant tuberculosis poses a persistent public health threat. The ReSeqTB platform is a collaborative, curated knowledgebase, designed to standardize and aggregate global Mycobacterium tuberculosis complex (MTBC) variant data from whole genome sequencing (WGS) with phenotypic drug susceptibility testing (DST) and clinical data. We developed a unified analysis variant pipeline (UVP) ( https://github.com/CPTR-ReSeqTB/UVP ) to identify variants and assign lineage from MTBC sequence data. Stringent thresholds and quality control measures were incorporated in this open source tool. The pipeline was validated using a well-characterized dataset of 90 diverse MTBC isolates with conventional DST and DNA Sanger sequencing data. The UVP exhibited 98.9% agreement with the variants identified using Sanger sequencing and was 100% concordant with conventional methods of assigning lineage. We analyzed 4636 publicly available MTBC isolates in the ReSeqTB platform representing all seven major MTBC lineages. The variants detected have an above 94% accuracy of predicting drug based on the accompanying DST results in the platform. The aggregation of variants over time in the platform will establish confidence-graded mutations statistically associated with phenotypic drug resistance. These tools serve as critical reference standards for future molecular diagnostic assay developers, researchers, public health agencies and clinicians working towards the control of drug-resistant tuberculosis.

Published
2018

14. A standardised method for interpreting the association between mutations and phenotypic drug resistance in Mycobacterium tuberculosis

Author

Miotto, Paolo, Tessema, Belay, Tagliani, Elisa, Chindelevitch, Leonid, Starks, Angela M, Emerson, Claudia, Hanna, Debra, Kim, Peter S, Liwski, Richard, Zignol, Matteo, Gilpin, Christopher, Niemann, Stefan, Denkinger, Claudia M, Fleming, Joy, Warren, Robin M, Crook, Derrick, Posey, James, Gagneux, Sebastien, Hoffner, Sven, Rodrigues, Camilla, Comas, Iñaki, Engelthaler, David M, Murray, Megan, Alland, David, Rigouts, Leen, Lange, Christoph, Dheda, Keertan, Hasan, Rumina, Ranganathan, Uma Devi K, McNerney, Ruth, Ezewudo, Matthew, Cirillo, Daniela M, Schito, Marco, Köser, Claudio U, and Rodwell, Timothy C

Subjects
Biomedical and Clinical Sciences, Clinical Sciences, Infectious Diseases, Tuberculosis, HIV/AIDS, Antimicrobial Resistance, Genetics, Rare Diseases, Development of treatments and therapeutic interventions, 5.1 Pharmaceuticals, Infection, Good Health and Well Being, Antitubercular Agents, Bacterial Proteins, DNA, Bacterial, Data Interpretation, Statistical, Drug Resistance, Multiple, Bacterial, Genotype, Humans, Microbial Sensitivity Tests, Mutation, Mycobacterium tuberculosis, Phenotype, Sequence Analysis, DNA, Systematic Reviews as Topic, Tuberculosis, Multidrug-Resistant, Medical and Health Sciences, Respiratory System, Cardiovascular medicine and haematology
Abstract

A clear understanding of the genetic basis of antibiotic resistance in Mycobacterium tuberculosis is required to accelerate the development of rapid drug susceptibility testing methods based on genetic sequence.Raw genotype-phenotype correlation data were extracted as part of a comprehensive systematic review to develop a standardised analytical approach for interpreting resistance associated mutations for rifampicin, isoniazid, ofloxacin/levofloxacin, moxifloxacin, amikacin, kanamycin, capreomycin, streptomycin, ethionamide/prothionamide and pyrazinamide. Mutation frequencies in resistant and susceptible isolates were calculated, together with novel statistical measures to classify mutations as high, moderate, minimal or indeterminate confidence for predicting resistance.We identified 286 confidence-graded mutations associated with resistance. Compared to phenotypic methods, sensitivity (95% CI) for rifampicin was 90.3% (89.6-90.9%), while for isoniazid it was 78.2% (77.4-79.0%) and their specificities were 96.3% (95.7-96.8%) and 94.4% (93.1-95.5%), respectively. For second-line drugs, sensitivity varied from 67.4% (64.1-70.6%) for capreomycin to 88.2% (85.1-90.9%) for moxifloxacin, with specificity ranging from 90.0% (87.1-92.5%) for moxifloxacin to 99.5% (99.0-99.8%) for amikacin.This study provides a standardised and comprehensive approach for the interpretation of mutations as predictors of M. tuberculosis drug-resistant phenotypes. These data have implications for the clinical interpretation of molecular diagnostics and next-generation sequencing as well as efficient individualised therapy for patients with drug-resistant tuberculosis.

Published
2017

18. Mycobacterium tuberculosis Subculture Results in Loss of Potentially Clinically Relevant Heteroresistance.

Author

Metcalfe, John Z, Streicher, Elizabeth, Theron, Grant, Colman, Rebecca E, Penaloza, Renee, Allender, Christopher, Lemmer, Darrin, Warren, Robin M, and Engelthaler, David M

Subjects
Humans, Mycobacterium tuberculosis, Tuberculosis, Multidrug-Resistant, Isoniazid, Fluoroquinolones, Rifampin, DNA Gyrase, DNA-Directed RNA Polymerases, Bacterial Proteins, Antitubercular Agents, Drug Resistance, Multiple, Bacterial, High-Throughput Nucleotide Sequencing, drug-resistant tuberculosis, gyrA, heteroresistance, rpoB, rrs, Biodefense, Infectious Diseases, Prevention, Rare Diseases, Antimicrobial Resistance, Vaccine Related, Tuberculosis, Aetiology, 2.1 Biological and endogenous factors, Infection, Good Health and Well Being, Microbiology, Medical Microbiology, Pharmacology and Pharmaceutical Sciences
Abstract

Multidrug-resistant tuberculosis (TB) presents a major public health dilemma. Heteroresistance, the coexistence of drug-resistant and drug-susceptible strains or of multiple drug-resistant strains with discrete haplotypes, may affect accurate diagnosis and the institution of effective treatment. Subculture, or passage of cells onto fresh growth medium, is utilized to preserve Mycobacterium tuberculosis cell lines and is universally employed in TB diagnostics. The impact of such passages, typically performed in the absence of drug, on drug-resistant subpopulations is hypothesized to vary according to the competitive costs of genotypic resistance-associated variants. We applied ultradeep next-generation sequencing to 61 phenotypically rifampin-monoresistant (n = 17) and preextensively (n = 41) and extensively (n = 3) drug-resistant isolates with presumptive heteroresistance at two time points in serial subculture. We found significant dynamic loss of minor-variant resistant subpopulations across all analyzed resistance-determining regions, including eight isolates (13%) whose antibiogram data would have transitioned from resistant to susceptible for at least one drug through subculture. Surprisingly, some resistance-associated variants appeared to be selected for in subculture.

Published
2017

19. Cryptic Microheteroresistance Explains Mycobacterium tuberculosis Phenotypic Resistance

Author

Metcalfe, John Z, Streicher, Elizabeth, Theron, Grant, Colman, Rebecca E, Allender, Christopher, Lemmer, Darrin, Warren, Rob, and Engelthaler, David M

Subjects
Prevention, HIV/AIDS, Tuberculosis, Genetics, Rare Diseases, Antimicrobial Resistance, Biodefense, Vaccine Related, Infectious Diseases, Aetiology, 2.1 Biological and endogenous factors, Infection, Good Health and Well Being, Drug Resistance, Bacterial, Microbial Sensitivity Tests, Mycobacterium tuberculosis, Sequence Analysis, next-generation sequencing, Sanger sequencing, drug-resistant tuberculosis, diagnostics, Medical and Health Sciences, Respiratory System
Abstract

RationaleMinority drug-resistant Mycobacterium tuberculosis subpopulations can be associated with phenotypic resistance but are poorly detected by Sanger sequencing or commercial molecular diagnostic assays.ObjectivesTo determine the role of targeted next-generation sequencing in resolving these minor variant subpopulations.MethodsWe used single molecule overlapping reads (SMOR), a targeted next-generation sequencing approach that dramatically reduces sequencing error, to analyze primary cultured isolates phenotypically resistant to rifampin, fluoroquinolones, or aminoglycosides, but for which Sanger sequencing found no resistance-associated variants (RAVs) within respective resistance-determining regions (study group). Isolates also underwent single-colony selection on antibiotic-containing agar, blinded to sequencing results. As a positive control, isolates with multiple colocalizing chromatogram peaks were also analyzed (control group).Measurements and main resultsAmong 61 primary culture isolates (25 study group and 36 control group), SMOR described 66 (49%) and 45 (33%) of 135 total heteroresistant RAVs at frequencies less than 5% and less than 1% of the total mycobacterial population, respectively. In the study group, SMOR detected minor resistant variant subpopulations in 80% (n = 20/25) of isolates with no Sanger-identified RAVs (median subpopulation size, 1.0%; interquartile range, 0.2-3.9%). Single-colony selection on drug-containing media corroborated SMOR results for 90% (n = 18/20) of RAV-containing specimens, and the absence of RAVs in 60% (n = 3/5) of isolates. Overall, Sanger sequencing was concordant with SMOR for 77% (n = 53/69) of macroheteroresistant (5-95% total population), but only 5% of microheteroresistant (

Published
2017

20. MLST-Based Population Genetic Analysis in a Global Context Reveals Clonality amongst Cryptococcus neoformans var. grubii VNI Isolates from HIV Patients in Southeastern Brazil

Author

Ferreira-Paim, Kennio, Andrade-Silva, Leonardo, Fonseca, Fernanda M, Ferreira, Thatiana B, Mora, Delio J, Andrade-Silva, Juliana, Khan, Aziza, Dao, Aiken, Reis, Eduardo C, Almeida, Margarete TG, Maltos, Andre, R., Virmondes, Trilles, Luciana, Rickerts, Volker, Chindamporn, Ariya, Sykes, Jane E, Cogliati, Massimo, Nielsen, Kirsten, Boekhout, Teun, Fisher, Matthew, Kwon-Chung, June, Engelthaler, David M, Lazéra, Marcia, Meyer, Wieland, and Silva-Vergara, Mario L

Subjects
Biological Sciences, Biomedical and Clinical Sciences, Microbiology, Clinical Sciences, Medical Microbiology, HIV/AIDS, Genetics, Infectious Diseases, Aetiology, 2.2 Factors relating to the physical environment, Infection, Good Health and Well Being, AIDS-Related Opportunistic Infections, Adult, Brazil, Cryptococcosis, Cryptococcus neoformans, Female, Genotype, HIV Infections, Humans, Male, Middle Aged, Multilocus Sequence Typing, Mycological Typing Techniques, Phylogeny, Young Adult, Medical and Health Sciences, Tropical Medicine, Biological sciences, Biomedical and clinical sciences, Health sciences
Abstract

Cryptococcosis is an important fungal infection in immunocompromised individuals, especially those infected with HIV. In Brazil, despite the free availability of antiretroviral therapy (ART) in the public health system, the mortality rate due to Cryptococcus neoformans meningitis is still high. To obtain a more detailed picture of the population genetic structure of this species in southeast Brazil, we studied 108 clinical isolates from 101 patients and 35 environmental isolates. Among the patients, 59% had a fatal outcome mainly in HIV-positive male patients. All the isolates were found to be C. neoformans var. grubii major molecular type VNI and mating type locus alpha. Twelve were identified as diploid by flow cytometry, being homozygous (AαAα) for the mating type and by PCR screening of the STE20, GPA1, and PAK1 genes. Using the ISHAM consensus multilocus sequence typing (MLST) scheme, 13 sequence types (ST) were identified, with one being newly described. ST93 was identified from 81 (75%) of the clinical isolates, while ST77 and ST93 were identified from 19 (54%) and 10 (29%) environmental isolates, respectively. The southeastern Brazilian isolates had an overwhelming clonal population structure. When compared with populations from different continents based on data extracted from the ISHAM-MLST database (mlst.mycologylab.org) they showed less genetic variability. Two main clusters within C. neoformans var. grubii VNI were identified that diverged from VNB around 0.58 to 4.8 million years ago.

Published
2017

21. Sequencing by binding rivals SMOR error-corrected sequencing by synthesis technology for accurate detection and quantification of minor (< 0.1%) subpopulation variants.

Author

Allender, Christopher J., Wike, Candice L., Porter, W. Tanner, Ellis, Dean, Lemmer, Darrin, Pond, Stephanie J. K., and Engelthaler, David M.

Subjects
WHOLE genome sequencing, ERROR rates, SINGLE molecules, NUCLEOTIDE sequencing, BASIC needs
Abstract

Background: Detecting very minor (< 1%) subpopulations using next-generation sequencing is a critical need for multiple applications, including the detection of drug resistant pathogens and somatic variant detection in oncology. A recently available sequencing approach termed 'sequencing by binding (SBB)' claims to have higher base calling accuracy data "out of the box." This paper evaluates the utility of using SBB for the detection of ultra-rare drug resistant subpopulations in Mycobacterium tuberculosis (Mtb) using a targeted amplicon assay and compares the performance of SBB to single molecule overlapping reads (SMOR) error corrected sequencing by synthesis (SBS) data. Results: SBS displayed an elevated error rate when compared to SMOR error-corrected SBS and SBB techniques. SMOR error-corrected SBS and SBB technologies performed similarly within the linear range studies and error rate studies. Conclusions: With lower sequencing error rates within SBB sequencing, this technique looks promising for both targeted and unbiased whole genome sequencing, leading to the identification of minor (< 1%) subpopulations without the need for error correction methods. [ABSTRACT FROM AUTHOR]

Published
2024
Full Text
View/download PDF

22. A framework for integrating wastewater-based epidemiology and public health.

Author

Brosky, Hanna, Prasek, Sarah M., Innes, Gabriel K., Pepper, Ian L., Miranda, Jasmine, Brierley, Paul E., Slinski, Stephanie L., Polashenski, Lois, Betancourt, Walter Q., Gronbach, Katie, Gomez, Diana, Neupane, Reshma, Johnson, Jasmine, Weiss, Joli, Yaglom, Hayley D., Engelthaler, David M., Hepp, Crystal M., Crank, Katherine, Gerrity, Daniel, and Stewart, Jill R.

Published
2024
Full Text
View/download PDF

23. DETECTION OF SARS-COV-2 IN A SQUIRREL MONKEY (SAIMIRI SCIUREUS): A ONE HEALTH INVESTIGATION AND RESPONSE.

Author

Yaglom, Hayley D., Roth, Alexis, Alvarez, Carolina, Corbus, Elaine, Ghai, Ria R., Ferguson, Sylvia, Ritter, Jana M., Hecht, Gavriella, Rekant, Steven, Engelthaler, David M., Venkat, Heather, and Tygielski, Sue

Abstract

Through collaborative efforts, One Health partners have responded to outbreaks of COVID-19 among animals, including those in human care at zoos. Zoos have been faced with numerous challenges, including the susceptibility of many mammalian species, and therefore the need to heighten biosecurity measures rapidly. Robust One Health collaborations already exist in Arizona to address endemic and emerging zoonoses, but these have rarely included zoos. The pandemic shed light on this, and Arizona subsequently expanded its SARS-CoV-2 surveillance efforts to include zoo animals. Testing and epidemiologic support was provided to expedite the detection of and response to zoonotic SARS-CoV-2 infection in zoo animals, as well as to understand possible transmission events. Resulting from this program, SARS-CoV-2 was detected from a rectal swab collected from an 8-yr-old squirrel monkey (Saimiri sciureus) from a zoo in Southern Arizona. The animal had rapidly become ill with nonrespiratory symptoms and died in July 2022. Genomic sequencing from the swab revealed mutations consistent with the Omicron (BA.2) lineage. An epidemiologic investigation identified an animal caretaker in close proximity to the affected squirrel monkey who tested positive for COVID-19 the same day the squirrel monkey died. Critical One Health partners provided support to the zoo through engagement of local, state, and federal agencies. Necropsy and pathologic evaluation showed significant necrotizing colitis; the overall clinical and histopathological findings did not implicate SARS-CoV-2 infection alone as a causal or contributing factor in the squirrel monkey's illness and death. This report documents the first identification of SARS-CoV-2 in a squirrel monkey and highlights a successful and timely One Health investigation conducted through multisectoral collaboration. [ABSTRACT FROM AUTHOR]

Published
2024
Full Text
View/download PDF

24. Investigation of SARS-CoV-2 Infection among Companion Animals in Households with Confirmed Human COVID-19 Cases.

Author

Venkat, Heather, Yaglom, Hayley D., Hecht, Gavriella, Goedderz, Andrew, Ely, Jennifer L., Sprenkle, Michael, Martins, Taylor, Jasso-Selles, Daniel, Lemmer, Darrin, Gesimondo, Jordan, Ruberto, Irene, Komatsu, Kenneth, and Engelthaler, David M.

Subjects
PETS, COVID-19 pandemic, WHOLE genome sequencing, SARS-CoV-2, VIRAL transmission, HOUSEHOLDS
Abstract

We aimed to characterize SARS-CoV-2 infection in companion animals living in households with COVID-19-positive people and understand the dynamics surrounding how these animals become infected. Public health investigators contacted households with at least one confirmed, symptomatic person with COVID-19 for study recruitment. Blood, nasal, and rectal swab specimens were collected from pet dogs and cats and a questionnaire was completed. Specimens were tested for SARS-CoV-2 by RT-PCR, and for neutralizing antibodies; genomic sequencing was performed on viral-positive samples. A total of 36.4% of 110 pets enrolled had evidence of infection with SARS-CoV-2. Pets were more likely to test positive if the pet was immunocompromised, and if more than one person in the home was positive for COVID-19. Among 12 multi-pet households where at least one pet was positive, 10 had at least one other pet test positive. Whole-genome sequencing revealed the genomes of viral lineages circulating in the community during the time of sample collection. Our findings suggest a high likelihood of viral transmission in households with multiple pets and when pets had very close interactions with symptomatic humans. Further surveillance studies are needed to characterize how new variants impact animals and to understand opportunities for infection and spillover in susceptible species. [ABSTRACT FROM AUTHOR]

Published
2024
Full Text
View/download PDF

26. Lyssa excreta: Defining parameters for fecal samples as a rabies virus surveillance method

Author

Walker, Faith M., primary, Upton, Jordyn R., additional, Erickson, Daryn, additional, Barrand, Zachary A., additional, Brock, Breezy, additional, Valentine, Michael, additional, Federman, Emma L., additional, Froehlich, Emma M., additional, Van Pelt, Lolita, additional, Hastings, Lias, additional, Sanchez, Daniel E., additional, Bergman, David L., additional, Engelthaler, David M., additional, and Hepp, Crystal M., additional

Published
2024
Full Text
View/download PDF

27. Coyotes as Reservoirs for Onchocerca lupi, United States, 2015-2018

Author

Roe, Chandler C., Yaglom, Hayley, Howard, April, Urbanz, Jennifer, Verocai, Guilherme G., Andrews, Lela, Harrison, Veronica, Barnes, Riley, Lyons, Ted, Bowers, Jolene R., and Engelthaler, David M.

Subjects
Roundworm infections -- Risk factors -- Distribution, Zoonoses -- Risk factors -- Distribution, Coyotes -- Health aspects, Host-parasite relationships, Company distribution practices, Health
Abstract

Onchocerca lupi is a species of zoonotic, filarial nematode that causes onchocerciasis in dogs, cats, and humans. It was first described in 1967 in Georgia, then part of the USSR, [...]

Published
2020
Full Text
View/download PDF

28. Local Population Structure and Patterns of Western Hemisphere Dispersal for Coccidioides spp., the Fungal Cause of Valley Fever

Author

Engelthaler, David M, Roe, Chandler C, Hepp, Crystal M, Teixeira, Marcus, Driebe, Elizabeth M, Schupp, James M, Gade, Lalitha, Waddell, Victor, Komatsu, Kenneth, Arathoon, Eduardo, Logemann, Heidi, Thompson, George R, Chiller, Tom, Barker, Bridget, Keim, Paul, and Litvintseva, Anastasia P

Subjects
Biodefense, Prevention, Emerging Infectious Diseases, Genetics, Orphan Drug, Rare Diseases, Infectious Diseases, Vaccine Related, Valley Fever, Aetiology, 2.2 Factors relating to the physical environment, Infection, Good Health and Well Being, Central America, Coccidioides, Coccidioidomycosis, Phylogeny, South America, Southwestern United States, Microbiology
Abstract

UnlabelledCoccidioidomycosis (or valley fever) is a fungal disease with high morbidity and mortality that affects tens of thousands of people each year. This infection is caused by two sibling species, Coccidioides immitis and C. posadasii, which are endemic to specific arid locales throughout the Western Hemisphere, particularly the desert southwest of the United States. Recent epidemiological and population genetic data suggest that the geographic range of coccidioidomycosis is expanding, as new endemic clusters have been identified in the state of Washington, well outside the established endemic range. The genetic mechanisms and epidemiological consequences of this expansion are unknown and require better understanding of the population structure and evolutionary history of these pathogens. Here we performed multiple phylogenetic inference and population genomics analyses of 68 new and 18 previously published genomes. The results provide evidence of substantial population structure in C. posadasii and demonstrate the presence of distinct geographic clades in central and southern Arizona as well as dispersed populations in Texas, Mexico, South America, and Central America. Although a smaller number of C. immitis strains were included in the analyses, some evidence of phylogeographic structure was also detected in this species, which has been historically limited to California and Baja, Mexico. Bayesian analyses indicated that C. posadasii is the more ancient of the two species and that Arizona contains the most diverse subpopulations. We propose a southern Arizona-northern Mexico origin for C. posadasii and describe a pathway for dispersal and distribution out of this region.ImportanceCoccidioidomycosis, or valley fever, is caused by the pathogenic fungi Coccidioides posadasii and C. immitis The fungal species and disease are primarily found in the American desert southwest, with spotted distribution throughout the Western Hemisphere. Initial molecular studies suggested a likely anthropogenic movement of C. posadasii from North America to South America. Here we comparatively analyze eighty-six genomes of the two Coccidioides species and establish local and species-wide population structures to not only clarify the earlier dispersal hypothesis but also provide evidence of likely ancestral populations and patterns of dispersal for the known subpopulations of C. posadasii.

Published
2016

29. MLST and Whole-Genome-Based Population Analysis of Cryptococcus gattii VGIII Links Clinical, Veterinary and Environmental Strains, and Reveals Divergent Serotype Specific Sub-populations and Distant Ancestors

Author

Firacative, Carolina, Roe, Chandler C, Malik, Richard, Ferreira-Paim, Kennio, Escandón, Patricia, Sykes, Jane E, Castañón-Olivares, Laura Rocío, Contreras-Peres, Cudberto, Samayoa, Blanca, Sorrell, Tania C, Castañeda, Elizabeth, Lockhart, Shawn R, Engelthaler, David M, and Meyer, Wieland

Subjects
Biological Sciences, Biomedical and Clinical Sciences, Genetics, Microbiology, Clinical Sciences, Biotechnology, Infectious Diseases, 2.1 Biological and endogenous factors, Aetiology, 2.2 Factors relating to the physical environment, Infection, Good Health and Well Being, Americas, Animals, Australia, Cryptococcosis, Cryptococcus gattii, Genetic Variation, Genome, Fungal, Genotype, Guatemala, Humans, Metagenomics, Mexico, Multilocus Sequence Typing, Phylogeny, Serogroup, Venezuela, Virulence, Medical and Health Sciences, Tropical Medicine, Biological sciences, Biomedical and clinical sciences, Health sciences
Abstract

The emerging pathogen Cryptococcus gattii causes life-threatening disease in immunocompetent and immunocompromised hosts. Of the four major molecular types (VGI-VGIV), the molecular type VGIII has recently emerged as cause of disease in otherwise healthy individuals, prompting a need to investigate its population genetic structure to understand if there are potential genotype-dependent characteristics in its epidemiology, environmental niche(s), host range and clinical features of disease. Multilocus sequence typing (MLST) of 122 clinical, environmental and veterinary C. gattii VGIII isolates from Australia, Colombia, Guatemala, Mexico, New Zealand, Paraguay, USA and Venezuela, and whole genome sequencing (WGS) of 60 isolates representing all established MLST types identified four divergent sub-populations. The majority of the isolates belong to two main clades, corresponding either to serotype B or C, indicating an ongoing species evolution. Both major clades included clinical, environmental and veterinary isolates. The C. gattii VGIII population was genetically highly diverse, with minor differences between countries, isolation source, serotype and mating type. Little to no recombination was found between the two major groups, serotype B and C, at the whole and mitochondrial genome level. C. gattii VGIII is widespread in the Americas, with sporadic cases occurring elsewhere, WGS revealed Mexico and USA as a likely origin of the serotype B VGIII population and Colombia as a possible origin of the serotype C VGIII population. Serotype B isolates are more virulent than serotype C isolates in a murine model of infection, causing predominantly pulmonary cryptococcosis. No specific link between genotype and virulence was observed. Antifungal susceptibility testing against six antifungal drugs revealed that serotype B isolates are more susceptible to azoles than serotype C isolates, highlighting the importance of strain typing to guide effective treatment to improve the disease outcome.

Published
2016

30. Rhizopus microsporus Infections Associated with Surgical Procedures, Argentina, 2006-2014

Author

Bowers, Jolene R., Monroy-Nieto, Juan, Gade, Lalitha, Travis, Jason, Refojo, Nicolas, Abrantes, Ruben, Santander, Jorge, French, Chris, Dignani, Maria Cecilia, Hevia, Alejandra Ines, Roe, Chandler C., Lemmer, Darrin, Lockhart, Shawn R., Chiller, Tom, Litvintseva, Anastasia P., Clara, Liliana, and Engelthaler, David M.

Subjects
Surgery -- Health aspects, Mycoses -- Health aspects, Fungi -- Health aspects, DNA sequencing -- Health aspects, Single nucleotide polymorphisms -- Health aspects, Medical research -- Health aspects, Infection -- Health aspects, Genomes -- Health aspects, Epidemiology -- Health aspects, Genomics -- Health aspects, Hospital patients, Genetic polymorphisms, Health
Abstract

Mucormycosis is a debilitating fungal infection; the mortality rate among persons with predisposing factors such as skin trauma (e.g., surgery), diabetes mellitus, or organ transplant is high. The fungus can [...]

Published
2020
Full Text
View/download PDF

31. Suspected Locally Acquired Coccidioidomycosis in Human, Spokane, Washington, USA

Author

Oltean, Hanna N., Springer, Mark, Bowers, Jolene R., Barnes, Riley, Reid, George, Valentine, Michael, Engelthaler, David M., Toda, Mitsuru, and McCotter, Orion Z.

Subjects
Sentinel surveillance, Coccidioidomycosis -- Diagnosis -- Care and treatment, Lung diseases, Diseases, Health
Abstract

Coccidioides immitis is a rare but emerging fungal pathogen in Washington, USA; Only the south-central region of Washington has been established as an area to which Coccidioides spp. are endemic; [...]

Published
2020
Full Text
View/download PDF

32. Valley Fever: Finding New Places for an Old Disease: Coccidioides immitis Found in Washington State Soil Associated With Recent Human Infection

Author

Litvintseva, Anastasia P, Marsden-Haug, Nicola, Hurst, Steven, Hill, Heather, Gade, Lalitha, Driebe, Elizabeth M, Ralston, Cindy, Roe, Chandler, Barker, Bridget M, Goldoft, Marcia, Keim, Paul, Wohrle, Ron, Thompson, George R, Engelthaler, David M, Brandt, Mary E, and Chiller, Tom

Subjects
Medical Microbiology, Biomedical and Clinical Sciences, Clinical Sciences, Vaccine Related, Prevention, Valley Fever, Human Genome, Rare Diseases, Infectious Diseases, Biodefense, Emerging Infectious Diseases, Genetics, 2.2 Factors relating to the physical environment, Aetiology, Infection, Cluster Analysis, Coccidioides, Coccidioidomycosis, DNA, Fungal, Endemic Diseases, Genome, Fungal, Humans, Microbiological Techniques, Molecular Sequence Data, Real-Time Polymerase Chain Reaction, Sequence Analysis, DNA, Sequence Homology, Soil Microbiology, Washington, valley fever, soil detection, WGS typing, Biological Sciences, Medical and Health Sciences, Microbiology, Clinical sciences
Abstract

We used real-time polymerase chain reaction and culture to demonstrate persistent colonization of soils by Coccidioides immitis, an agent of valley fever, in Washington State linked to recent human infections and located outside the endemic range. Whole-genome sequencing confirmed genetic identity between isolates from soil and one of the case-patients.

Published
2015

33. Pan-Enterovirus Characterization Reveals Cryptic Circulation of Clinically Relevant Subtypes in Arizona Wastewater

Author

Erickson, Daryn E, primary, Simmons, Kyle M, additional, Barrand, Zachary A, additional, Ridenour, Chase L, additional, Hawkinson, Paige B, additional, Lemke, Lacey, additional, Sellner, Shayne P, additional, Brock, Breezy N, additional, Rivas, Alexis N, additional, Sheridan, Krystal, additional, Lemmer, Darrin, additional, Yaglom, Hayley D, additional, Porter, W Tanner, additional, Belanger, Monique, additional, Torrey, Rachel M, additional, Stills, Aidan James R, additional, McCormack, Kiley, additional, Black, Matt, additional, Holmes, Wydale, additional, Rostain, Drew, additional, Mikus, Jeremy, additional, Sotelo, Kimberly, additional, Haq, Emmen, additional, Neupane, Reshma, additional, Weiss, Joli, additional, Johnson, Jasmine, additional, Collins, Clancey, additional, Avalle, Sarah, additional, White, Chelsi, additional, Howard, Brandon J, additional, Maltinsky, Sarah A, additional, Whealy, Ryann N, additional, Barber, Jarrett, additional, Gordon, Nathaniel B, additional, Sahl, Jason W, additional, Pearson, Talima, additional, Fofanov, Viacheslav Y, additional, Furstenau, Tara, additional, Driebe, Elizabeth M, additional, Caporaso, J Gregory, additional, Terriquez, Joel, additional, Engelthaler, David M, additional, and Hepp, Crystal M, additional

Published
2023
Full Text
View/download PDF

34. Comparison of carbapenem-susceptible and carbapenem-resistant Enterobacterales at nine sites in the USA, 2013–2016: a resource for antimicrobial resistance investigators

Author

Lutgring, Joseph D., primary, Kent, Alyssa G., additional, Bowers, Jolene R., additional, Jasso-Selles, Daniel E., additional, Albrecht, Valerie, additional, Stevens, Valerie A., additional, Pfeiffer, Ashlyn, additional, Barnes, Riley, additional, Engelthaler, David M., additional, Johnson, J. Kristie, additional, Gargis, Amy S., additional, Rasheed, J. Kamile, additional, Limbago, Brandi M., additional, Elkins, Christopher A., additional, Karlsson, Maria, additional, and Halpin, Alison L., additional

Published
2023
Full Text
View/download PDF

35. Contributors

Author

Allard, M.W., primary, Allen, Jonathan, additional, Amara, Philip S., additional, Barnaby, Neel G., additional, Barr, John R., additional, Belk, Aeriel, additional, Bergman, Nicholas H., additional, Bidwell, Christopher A., additional, Birdsell, Dawn, additional, Blake, Thomas A., additional, Brown, E.W., additional, Bucheli, Sibyl, additional, Budowle, Bruce, additional, Bull, Robert L., additional, Burans, James, additional, Carter, David O., additional, Choi, Angela, additional, Deatherage Kaiser, Brooke L., additional, Decker, R. Scott, additional, Deel, Heather, additional, Engelthaler, David M., additional, Espitia-Navarro, Hector F., additional, Fletcher, Jacqueline, additional, Foster, Jeffrey T., additional, García-Sastre, Adolfo, additional, Goodrich, Jennifer S., additional, Hart, Bradley, additional, Hodge, David R., additional, Jackson, Paul J., additional, Jaing, Crystal, additional, Johnson, Rudolph C., additional, Jordan, I. King, additional, Kalb, Suzanne R., additional, Kaufmann, Arnold F., additional, Keim, Paul, additional, Kerns, Terry L., additional, Khan, Ali S., additional, Kieser, Rachel E., additional, Knight, Rob, additional, Korajkic, Asja, additional, Lee, Steven B., additional, Litvintseva, Anastasia P., additional, Luster, Douglas G., additional, Lynne, Aaron, additional, Mayer, Leonard W., additional, Melcher, Ulrich, additional, Merkley, Eric D., additional, Metcalf, Jessica L., additional, Mills, DeEtta K., additional, Morse, Stephen A., additional, Mullins, Ted D., additional, Murch, Randall, additional, Nutter, Forrest W., additional, Ochoa Corona, Francisco M., additional, Ogden, Sam, additional, Okinaka, Richard T., additional, Pearson, Talima, additional, Quigley, Bernard R., additional, Rishishwar, Lavanya, additional, Sahl, Jason W., additional, Saltzburg, Stephen A., additional, Scherm, Harald, additional, Schmale, David G., additional, Schmedes, Sarah E., additional, Schutzer, Steven E., additional, Shanks, Orin C., additional, Simione, Frank P., additional, Slezak, Tom, additional, Smith, Jenifer A.L., additional, Thomas, Carla S., additional, Velsko, Stephan P., additional, Vines, Richard R., additional, Vogler, Amy, additional, Wagner, David M., additional, Wahl, Karen L., additional, Williamson, Charles H., additional, Wilson, Mark, additional, Woerner, August, additional, and Wunschel, David S., additional

Published
2020
Full Text
View/download PDF

37. Utility of Whole-Genome Sequencing to Ascertain Locally Acquired Cases of Coccidioidomycosis, Washington, USA

Author

Oltean, Hanna N., Etienne, Kizee A., Roe, Chandler C., Gade, Lalitha, McCotter, Orion Z., Engelthaler, David M., and Litvintseva, Anastasia P.

Subjects
United States. Centers for Disease Control and Prevention -- International economic relations, Coccidioidomycosis -- Health aspects, DNA sequencing -- Health aspects, Mycoses, Company acquisition/merger, Health
Abstract

Coccidioidomycosis, also known as Valley fever, is a disease of growing public health concern and is caused by 2 closely related fungal species, Coccidioides immitis and C. posadasii. Coccidioides spp. [...]

Published
2019
Full Text
View/download PDF

38. Zoonotic Source Attribution of Salmonella enterica Serotype Typhimurium Using Genomic Surveillance Data, United States

Author

Zhang, Shaokang, Li, Shaoting, Gu, Weidong, den Bakker, Henk, Boxrud, Dave, Taylor, Angie, Roe, Chandler, Driebe, Elizabeth, Engelthaler, David M., Allard, Marc, Brown, Eric, McDermott, Patrick, Zhao, Shaohua, Bruce, Beau B., Trees, Eija, Fields, Patricia I., and Deng, Xiangyu

Subjects
Salmonellosis -- Genetic aspects -- Causes of, Zoonoses -- Genetic aspects -- Causes of, Genotypes -- Identification and classification, Sentinel surveillance -- Technology application, Intelligence gathering, Salmonella typhimurium, DNA sequencing, Beef cattle, Epidemiology, Pathogenic microorganisms, Genomics, Machine learning, Salmonella, Food contamination, Phylogeny, Swine, Livestock, Genomes, Medical research, Technology application, Health
Abstract

Each year, 9.4 million episodes of foodborne illness occur in the United States (1). According to the Centers for Disease Control and Prevention, -95% of these infections are sporadic, nonoutbreak [...]

Published
2019
Full Text
View/download PDF

39. Phylogeography and transmission of M. tuberculosis in Moldova: A prospective genomic analysis

Author

Yang, Chongguang, Sobkowiak, Benjamin, Naidu, Vijay, Codreanu, Alexandru, Ciobanu, Nelly, Gunasekera, Kenneth S., Chitwood, Melanie H., Alexandru, Sofia, Bivol, Stela, Russi, Marcus, Havumaki, Joshua, Cudahy, Patrick, Fosburgh, Heather, Allender, Christopher J., Centner, Heather, Engelthaler, David M., Menzies, Nicolas A., Warren, Joshua L., Crudu, Valeriu, Colijn, Caroline, and Cohen, Ted

Subjects
Medical research, Medicine, Experimental, Medical geography -- Research, Disease transmission -- Forecasts and trends, Mycobacterium tuberculosis -- Distribution -- Genetic aspects, Market trend/market analysis, Company distribution practices, Biological sciences
Abstract

Background The incidence of multidrug-resistant tuberculosis (MDR-TB) remains critically high in countries of the former Soviet Union, where >20% of new cases and >50% of previously treated cases have resistance to rifampin and isoniazid. Transmission of resistant strains, as opposed to resistance selected through inadequate treatment of drug-susceptible tuberculosis (TB), is the main driver of incident MDR-TB in these countries. Methods and findings We conducted a prospective, genomic analysis of all culture-positive TB cases diagnosed in 2018 and 2019 in the Republic of Moldova. We used phylogenetic methods to identify putative transmission clusters; spatial and demographic data were analyzed to further describe local transmission of Mycobacterium tuberculosis. Of 2,236 participants, 779 (36%) had MDR-TB, of whom 386 (50%) had never been treated previously for TB. Moreover, 92% of multidrug-resistant M. tuberculosis strains belonged to putative transmission clusters. Phylogenetic reconstruction identified 3 large clades that were comprised nearly uniformly of MDR-TB: 2 of these clades were of Beijing lineage, and 1 of Ural lineage, and each had additional distinct clade-specific second-line drug resistance mutations and geographic distributions. Spatial and temporal proximity between pairs of cases within a cluster was associated with greater genomic similarity. Our study lasted for only 2 years, a relatively short duration compared with the natural history of TB, and, thus, the ability to infer the full extent of transmission is limited. Conclusions The MDR-TB epidemic in Moldova is associated with the local transmission of multiple M. tuberculosis strains, including distinct clades of highly drug-resistant M. tuberculosis with varying geographic distributions and drug resistance profiles. This study demonstrates the role of comprehensive genomic surveillance for understanding the transmission of M. tuberculosis and highlights the urgency of interventions to interrupt transmission of highly drug-resistant M. tuberculosis., Author(s): Chongguang Yang 1,2, Benjamin Sobkowiak 3, Vijay Naidu 3, Alexandru Codreanu 4, Nelly Ciobanu 4, Kenneth S. Gunasekera 2, Melanie H. Chitwood 2, Sofia Alexandru 4, Stela Bivol 5, [...]

Published
2022
Full Text
View/download PDF

41. Understanding the exposure risk of aerosolized Coccidioides in a Valley fever endemic metropolis.

Author

Porter, W. Tanner, Gade, Lalitha, Montfort, Parker, Mihaljevic, Joseph R., Bowers, Jolene R., Willman, Andrew, Klimowski, Brian A., LaFleur, Bonnie J., Sunenshine, Rebecca H., Collins, Jennifer, Adame, Guillermo, Brady, Shane, Komatsu, Kenneth K., Williams, Samantha, Toda, Mitsuru, Chiller, Tom, Litvintseva, Anastasia P., and Engelthaler, David M.

Subjects
COCCIDIOIDOMYCOSIS, RISK exposure, AIR sampling, METROPOLIS, METROPOLITAN areas
Abstract

Coccidioides is the fungal causative agent of Valley fever, a primarily pulmonary disease caused by inhalation of fungal arthroconidia, or spores. Although Coccidioides has been an established pathogen for 120 years and is responsible for hundreds of thousands of infections per year, little is known about when and where infectious Coccidioides arthroconidia are present within the ambient air in endemic regions. Long-term air sampling programs provide a means to investigate these characteristics across space and time. Here we present data from > 18 months of collections from 11 air sampling sites across the Phoenix, Arizona, metropolitan area. Overall, prevalence was highly variable across space and time with no obvious spatial or temporal correlations. Several high prevalence periods were identified at select sites, with no obvious spatial or temporal associations. Comparing these data with weather and environmental factor data, wind gusts and temperature were positively associated with Coccidioides detection, while soil moisture was negatively associated with Coccidioides detection. These results provide critical insights into the frequency and distribution of airborne arthroconidia and the associated risk of inhalation and potential disease that is present across space and time in a highly endemic locale. [ABSTRACT FROM AUTHOR]

Published
2024
Full Text
View/download PDF

42. Novel Presentation of Coccidioidomycosis with Myriad Free-Floating Proteinaceous Spheres in the Pericardial Sac of a Southern Sea Otter (Enhydra lutris nereis).

Author

Harris, Heather S., Harris, Michael D., Thompson III, George R., Engelthaler, David M., Montfort, Parker L., Leviner, Alexis L., and Miller, Melissa A.

Abstract

A southern sea otter (Enhydra lutris nereis) stranded dead in central California, USA, with a distended pericardial sac containing thousands of free-floating proteinaceous masses. Serology, fungal culture, PCR, and sequencing confirmed the etiology of this novel lesion as Coccidioides immitis. Range expansion of this zoonotic pathogen is predicted with climate change. [ABSTRACT FROM AUTHOR]

Published
2024
Full Text
View/download PDF

43. Lyssa excreta: Defining parameters for fecal samples as a rabies virus surveillance method

Author

Walker, Faith M., primary, Upton, Jordyn R., additional, Erickson, Daryn, additional, Barrand, Zackary, additional, Brock, Breezy, additional, Valentine, Michael, additional, Federman, Emma L., additional, Froehlich, Emma M., additional, Van Pelt, Lolita, additional, Hastings, Lias, additional, Bergman, David L., additional, Engelthaler, David M., additional, and Hepp, Crystal M., additional

Published
2023
Full Text
View/download PDF

45. Comparing genomic variant identification protocols for Candida auris

Author

Li, Xiao, primary, Muñoz, José F., additional, Gade, Lalitha, additional, Argimon, Silvia, additional, Bougnoux, Marie-Elisabeth, additional, Bowers, Jolene R., additional, Chow, Nancy A., additional, Cuesta, Isabel, additional, Farrer, Rhys A., additional, Maufrais, Corinne, additional, Monroy-Nieto, Juan, additional, Pradhan, Dibyabhaba, additional, Uehling, Jessie, additional, Vu, Duong, additional, Yeats, Corin A., additional, Aanensen, David M., additional, d’Enfert, Christophe, additional, Engelthaler, David M., additional, Eyre, David W., additional, Fisher, Matthew C., additional, Hagen, Ferry, additional, Meyer, Wieland, additional, Singh, Gagandeep, additional, Alastruey-Izquierdo, Ana, additional, Litvintseva, Anastasia P., additional, and Cuomo, Christina A., additional

Published
2023
Full Text
View/download PDF

46. Multi-faceted metagenomic analysis of spacecraft associated surfaces reveal planetary protection relevant microbial composition

Author

Highlander, Sarah K., primary, Wood, Jason M., additional, Gillece, John D., additional, Folkerts, Megan, additional, Fofanov, Viacheslav, additional, Furstenau, Tara, additional, Singh, Nitin K., additional, Guan, Lisa, additional, Seuylemezian, Arman, additional, Benardini, James N., additional, Engelthaler, David M., additional, Venkateswaran, Kasthuri, additional, and Keim, Paul S., additional

Published
2023
Full Text
View/download PDF

48. Comparing genomic variant identification protocols for Candida auris

Author

Li, Xiao, Muñoz, José F, Gade, Lalitha, Argimon, Silvia, Bougnoux, Marie-Elisabeth, Bowers, Jolene R, Chow, Nancy A, Cuesta, Isabel, Farrer, Rhys A, Maufrais, Corinne, Monroy-Nieto, Juan, Pradhan, Dibyabhaba, Uehling, Jessie, Vu, Duong, Yeats, Corin A, Aanensen, David M, d'Enfert, Christophe, Engelthaler, David M, Eyre, David W, Fisher, Matthew C, Hagen, Ferry, Meyer, Wieland, Singh, Gagandeep, Alastruey-Izquierdo, Ana, Litvintseva, Anastasia P, Cuomo, Christina A, Li, Xiao, Muñoz, José F, Gade, Lalitha, Argimon, Silvia, Bougnoux, Marie-Elisabeth, Bowers, Jolene R, Chow, Nancy A, Cuesta, Isabel, Farrer, Rhys A, Maufrais, Corinne, Monroy-Nieto, Juan, Pradhan, Dibyabhaba, Uehling, Jessie, Vu, Duong, Yeats, Corin A, Aanensen, David M, d'Enfert, Christophe, Engelthaler, David M, Eyre, David W, Fisher, Matthew C, Hagen, Ferry, Meyer, Wieland, Singh, Gagandeep, Alastruey-Izquierdo, Ana, Litvintseva, Anastasia P, and Cuomo, Christina A

Abstract

Genomic analyses are widely applied to epidemiological, population genetic and experimental studies of pathogenic fungi. A wide range of methods are employed to carry out these analyses, typically without including controls that gauge the accuracy of variant prediction. The importance of tracking outbreaks at a global scale has raised the urgency of establishing high-accuracy pipelines that generate consistent results between research groups. To evaluate currently employed methods for whole-genome variant detection and elaborate best practices for fungal pathogens, we compared how 14 independent variant calling pipelines performed across 35 Candida auris isolates from 4 distinct clades and evaluated the performance of variant calling, single-nucleotide polymorphism (SNP) counts and phylogenetic inference results. Although these pipelines used different variant callers and filtering criteria, we found high overall agreement of SNPs from each pipeline. This concordance correlated with site quality, as SNPs discovered by a few pipelines tended to show lower mapping quality scores and depth of coverage than those recovered by all pipelines. We observed that the major differences between pipelines were due to variation in read trimming strategies, SNP calling methods and parameters, and downstream filtration criteria. We calculated specificity and sensitivity for each pipeline by aligning three isolates with chromosomal level assemblies and found that the GATK-based pipelines were well balanced between these metrics. Selection of trimming methods had a greater impact on SAMtools-based pipelines than those using GATK. Phylogenetic trees inferred by each pipeline showed high consistency at the clade level, but there was more variability between isolates from a single outbreak, with pipelines that used more stringent cutoffs having lower resolution. This project generated two truth datasets useful for routine benchmarking of C. auris variant calling, a consensus VCF of g

Published
2023

49. Phylogenetic Analysis of Francisella tularensis Group A.II Isolates from 5 Patients with Tularemia, Arizona, USA, 2015-2017

Author

Birdsell, Dawn N., Yaglom, Hayley, Rodriguez, Edwin, Engelthaler, David M., Maurer, Matthew, Gaither, Marlene, Vinocur, Jacob, Weiss, Joli, Terriquez, Joel, Komatsu, Kenneth, Ormsby, Mary Ellen, Gebhardt, Marette, Solomon, Catherine, Nienstadt, Linus, Williamson, Charles H.D., Sahl, Jason W., Keim, Paul S., and Wagner, David M.

Subjects
Resveratrol -- Analysis, Phylogeny -- Analysis, Tularemia -- Analysis, Health
Abstract

Francisella tularensis, a Tier 1 select agent (7), has 3 subspecies: tularensis (type A), holarctica (type B), and mediasiatica (Appendix 1 Figure, https://wwwnc. cdc.gov/EID/article/25/5/18-0363-App1.pdf). In humans, disease is caused by [...]

Published
2019
Full Text
View/download PDF

50. Unique Genomic Epidemiology of COVID-19 in the White Mountain Apache Tribe, April to August 2020, Arizona

Author

Bowers, Jolene R., primary, Yaglom, Hayley D., additional, Hepp, Crystal M., additional, Pfeiffer, Ashlyn, additional, Jasso-Selles, Daniel, additional, Bratsch, Nicole, additional, Nashio, J. T., additional, Folkerts, Megan, additional, Wilbur, Sara M., additional, French, Chris, additional, Lemmer, Darrin, additional, Fitzpatrick, Kathryn, additional, Huynh, Trung, additional, Komatsu, Kenneth, additional, McAuley, James B., additional, Close, Ryan, additional, and Engelthaler, David M., additional

Published
2023
Full Text
View/download PDF

Catalog

Books, media, physical & digital resources
See catalog results