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1. Tuberculosis screening improves preventive therapy uptake (TB SCRIPT) trial among people living with HIV in Uganda: a study protocol of an individual randomized controlled trial

Author

Semitala, Fred C, Chaisson, Lelia H, Dowdy, David W, Armstrong, Derek T, Opira, Bishop, Aman, Kyomugisha, Kamya, Moses, Phillips, Patrick PJ, and Yoon, Christina

Subjects
Biomedical and Clinical Sciences, Clinical Sciences, Health Sciences, Clinical Trials and Supportive Activities, Rare Diseases, HIV/AIDS, Comparative Effectiveness Research, Tuberculosis, Infectious Diseases, Health Services, Prevention, Clinical Research, Evaluation of treatments and therapeutic interventions, 4.4 Population screening, 4.2 Evaluation of markers and technologies, Detection, screening and diagnosis, 6.1 Pharmaceuticals, Infection, Good Health and Well Being, Anti-Retroviral Agents, Antitubercular Agents, Clinical Trials, Phase III as Topic, HIV Infections, Humans, Multicenter Studies as Topic, Randomized Controlled Trials as Topic, Uganda, HIV, Screening, C-reactive protein, Tuberculosis preventive therapy, Randomized controlled trial, Cardiorespiratory Medicine and Haematology, Cardiovascular System & Hematology, General & Internal Medicine, Clinical sciences, Epidemiology, Health services and systems
Abstract

BackgroundPeople living with HIV (PLHIV) have an increased risk of developing active tuberculosis (TB). To reduce the burden of TB among PLHIV, the World Health Organization (WHO) recommends systematic TB screening followed by (1) confirmatory TB testing for all who screen positive and (2) TB preventive therapy (TPT) for all TPT-eligible PLHIV who screen negative. Symptom-based screening remains the standard of care in most high TB burden settings, including Uganda. Despite having high sensitivity for active TB among antiretroviral-naïve PLHIV, symptom screening has poor specificity; as such, many high-risk PLHIV without active TB are not referred for TPT. C-reactive protein (CRP) is a promising alternative strategy for TB screening that has comparable sensitivity and higher specificity than symptom screening, and was endorsed by WHO in 2021. However, the impact of CRP-based TB screening on TB burden for PLHIV remains unclear.MethodsTB SCRIPT (TB Screening Improves Preventive Therapy Uptake) is a phase 3, multi-center, single-blinded, individual (1:1) randomized controlled trial evaluating the effectiveness of CRP-based TB screening on clinical outcomes of PLHIV. The trial aims to compare the effectiveness of a TB screening strategy based on CRP levels using a point-of-care (POC) assay on 2-year TB incidence and all-cause mortality (composite primary trial endpoint) and prevalent TB case detection and uptake of TPT (intermediate outcomes), relative to symptom-based TB screening (current practice).DiscussionThis study will be critical to improving selection of eligible PLHIV for TPT and helping guide the scale-up and integration of TB screening and TPT activities. This work will enable the field to improve TB screening by removing barriers to TPT initiation among eligible PLHIV, and provide randomized evidence to inform and strengthen WHO guidelines.Trial registrationClinicalTrials.gov NCT04557176. Registered on September 21, 2020.

Published
2022

2. Direct detection of SARS-CoV-2 RNA using high-contrast pH-sensitive dyes.

Author

Brown, Timothy A, Schaefer, Katherine S, Tsang, Arthur, Yi, Hyun Ah, Grimm, Jonathan B, Lemire, Andrew L, Jradi, Fadi M, Kim, Charles, McGowan, Kevin, Ritola, Kimberly, Armstrong, Derek T, Mostafa, Heba H, Korff, Wyatt, Vale, Ronald D, and Lavis, Luke D

Subjects
Biological Sciences, Pneumonia & Influenza, Vaccine Related, Emerging Infectious Diseases, Clinical Research, Biotechnology, Biodefense, Genetics, Lung, Infectious Diseases, Prevention, Infection, Good Health and Well Being, COVID-19, Coloring Agents, Humans, Hydrogen-Ion Concentration, Molecular Diagnostic Techniques, Nucleic Acid Amplification Techniques, RNA, Viral, SARS-CoV-2, Sensitivity and Specificity, Social Structure, LAMPshade, RT-LAMP, Si-fluorescein, carbofluorescein, Technology, Medical and Health Sciences, Biological sciences
Abstract

The worldwide coronavirus disease 2019 pandemic has had devastating effects on health, healthcare infrastructure, social structure, and economics. One of the limiting factors in containing the spread of this virus has been the lack of widespread availability of fast, inexpensive, and reliable methods for testing of individuals. Frequent screening for infected and often asymptomatic people is a cornerstone of pandemic management plans. Here, we introduce 2 pH-sensitive "LAMPshade" dyes as novel readouts in an isothermal Reverse Transcriptase Loop-mediated isothermal AMPlification amplification assay for severe acute respiratory syndrome coronavirus 2 RNA. The resulting JaneliaLAMP assay is robust, simple, inexpensive, and has low technical requirements, and we describe its use and performance in direct testing of contrived and clinical samples without RNA extraction.

Published
2021

3. Yield and Efficiency of Novel Intensified Tuberculosis Case-Finding Algorithms for People Living with HIV

Author

Yoon, Christina, Semitala, Fred C, Asege, Lucy, Katende, Jane, Mwebe, Sandra, Andama, Alfred O, Atuhumuza, Elly, Nakaye, Martha, Armstrong, Derek T, Dowdy, David W, McCulloch, Charles E, Kamya, Moses, and Cattamanchi, Adithya

Subjects
Biomedical and Clinical Sciences, Clinical Sciences, Lung, HIV/AIDS, Rare Diseases, Tuberculosis, Sexually Transmitted Infections, Bioengineering, Infectious Diseases, Clinical Research, Emerging Infectious Diseases, 4.2 Evaluation of markers and technologies, Infection, Good Health and Well Being, Adult, Algorithms, C-Reactive Protein, CD4 Lymphocyte Count, Coinfection, Female, HIV Infections, Health Care Costs, Humans, Lipopolysaccharides, Male, Mass Screening, Point-of-Care Systems, Sensitivity and Specificity, Sputum, Tuberculosis, Pulmonary, tuberculosis, intensified case finding, screening, C-reactive protein, urine lipoarabinomannan, Medical and Health Sciences, Respiratory System, Cardiovascular medicine and haematology, Clinical sciences
Abstract

RationaleThe recommended tuberculosis (TB) intensified case finding (ICF) algorithm for people living with HIV (symptom-based screening followed by Xpert MTB/RIF [Xpert] testing) is insufficiently sensitive and results in unnecessary Xpert testing.ObjectivesTo evaluate whether novel ICF algorithms combining C-reactive protein (CRP)-based screening with urine Determine TB-LAM (TB-LAM), sputum Xpert, and/or sputum culture could improve ICF yield and efficiency.MethodsWe compared the yield and efficiency of novel ICF algorithms inclusive of point-of-care CRP-based TB screening and confirmatory testing with urine TB-LAM (if CD4 count ≤100 cells/μl), sputum Xpert, and/or a single sputum culture among consecutive people living with HIV with CD4 counts less than or equal to 350 cells/μl initiating antiretroviral therapy in Uganda.Measurements and main resultsOf 1,245 people living with HIV, 203 (16%) had culture-confirmed TB including 101 (49%) patients with CD4 counts less than or equal to 100 cells/μl. Compared with the current ICF algorithm, point-of-care CRP-based TB screening followed by Xpert testing had similar yield (56% [95% confidence interval, 49-63] vs. 59% [95% confidence interval, 51-65]) but consumed less than half as many Xpert assays per TB case detected (9 vs. 4). Addition of TB-LAM did not significantly increase diagnostic yield relative to the current ICF algorithm but provided same-day diagnosis for 26% of TB patients with advanced HIV. Addition of a single culture to TB-LAM and Xpert substantially improved ICF yield, identifying 78% of all TB cases.ConclusionsPoint-of-care CRP-based screening can improve ICF efficiency among people living with HIV. Addition of TB-LAM and a single culture to Xpert confirmatory testing could enable HIV programs to increase the speed of TB diagnosis and ICF yield.

Published
2019

5. Point-of-care C-reactive protein-based tuberculosis screening for people living with HIV: a diagnostic accuracy study.

Author

Yoon, Christina, Semitala, Fred C, Atuhumuza, Elly, Katende, Jane, Mwebe, Sandra, Asege, Lucy, Armstrong, Derek T, Andama, Alfred O, Dowdy, David W, Davis, J Luke, Huang, Laurence, Kamya, Moses, and Cattamanchi, Adithya

Subjects
Humans, Tuberculosis, HIV Infections, C-Reactive Protein, Anti-HIV Agents, CD4 Lymphocyte Count, Sensitivity and Specificity, Adolescent, Adult, Female, Male, Young Adult, Point-of-Care Testing, Lung, Rare Diseases, Clinical Research, HIV/AIDS, Prevention, Infectious Diseases, 4.2 Evaluation of markers and technologies, Infection, Microbiology, Clinical Sciences, Medical Microbiology, Public Health and Health Services
Abstract

BackgroundSymptom-based screening for tuberculosis is recommended for all people living with HIV. This recommendation results in unnecessary Xpert MTB/RIF testing in many individuals living in tuberculosis-endemic areas and thus poor implementation of intensified case finding and tuberculosis preventive therapy. Novel approaches to tuberculosis screening are needed to help achieve global targets for tuberculosis elimination. We assessed the performance of C-reactive protein (CRP) measured with a point-of-care assay as a screening tool for active pulmonary tuberculosis.MethodsFor this prospective study, we enrolled adults (aged ≥18 years) living with HIV with CD4 cell count less than or equal to 350 cells per μL who were initiating antiretroviral therapy (ART) from two HIV/AIDS clinics in Uganda. CRP concentrations were measured at study entry with a point-of-care assay using whole blood obtained by fingerprick (concentration ≥10 mg/L defined as screen positive for tuberculosis). Sputum samples were collected for Xpert MTB/RIF testing and culture. We calculated the sensitivity and specificity of point-of-care CRP and WHO symptom-based screening in reference to culture results. We repeated the sensitivity analysis with Xpert MTB/RIF as the reference standard.FindingsBetween July 8, 2013, and Dec 15, 2015, 1237 HIV-infected adults were enrolled and underwent point-of-care CRP testing. 60 (5%) patients with incomplete or contaminated cultures were excluded from the analysis. Of the remaining 1177 patients (median CD4 count 165 cells per μL [IQR 75-271]), 163 (14%) had culture-confirmed tuberculosis. Point-of-care CRP testing had 89% sensitivity (145 of 163, 95% CI 83-93) and 72% specificity (731 of 1014, 95% CI 69-75) for culture-confirmed tuberculosis. Compared with WHO symptom-based screening, point-of-care CRP testing had lower sensitivity (difference -7%, 95% CI -12 to -2; p=0·002) but substantially higher specificity (difference 58%, 95% CI 55 to 61; p

Published
2017

6. Xpert MTB/RIF Ultra for detection of Mycobacterium tuberculosis and rifampicin resistance: a prospective multicentre diagnostic accuracy study

Author

Dorman, Susan E, Schumacher, Samuel G, Alland, David, Nabeta, Pamela, Armstrong, Derek T, King, Bonnie, Hall, Sandra L, Chakravorty, Soumitesh, Cirillo, Daniela M, Tukvadze, Nestani, Bablishvili, Nino, Stevens, Wendy, Scott, Lesley, Rodrigues, Camilla, Kazi, Mubin I, Joloba, Moses, Nakiyingi, Lydia, Nicol, Mark P, Ghebrekristos, Yonas, Anyango, Irene, Murithi, Wilfred, Dietze, Reynaldo, Peres, Renata Lyrio, Skrahina, Alena, Auchynka, Vera, Chopra, Kamal Kishore, Hanif, Mahmud, Liu, Xin, Yuan, Xing, Boehme, Catharina C, Ellner, Jerrold J, Denkinger, Claudia M, Manabe, Yukari C, Hom, David, Aspindzelashvili, Rusudan, David, Anura, Surve, Utkarsha, Kamulegeya, Louis Henry, Nabweyambo, Sheila, Surtie, Shireen, Hapeela, Nchimunya, Cain, Kevin P, Agaya, Janet, McCarthy, Kimberly D, Marques-Rodrigues, Patricia, Schmidt Castellani, Luiz Guilherme, Almeida, Pedro Sousa, Jr, de Aguiar, Paola Poloni Lobo, Solodovnikova, Varvara, Ruan, Xianglin, Liang, Lili, Zhang, Guolong, Zhu, Hong, Xie, Yingda, and Lyrio Peres, Renata

Published
2018
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10. Evaluation of a Rapid Molecular Drug-Susceptibility Test for Tuberculosis

Author

Xie, Yingda L., Chakravorty, Soumitesh, Armstrong, Derek T., Hall, Sandra L., Via, Laura E., Song, Taeksun, Yuan, Xing, Mo, Xiaoying, Zhu, Hong, Xu, Peng, Gao, Qian, Lee, Myungsun, Lee, Jongseok, Smith, Laura E., Chen, Ray Y., Joh, Joon Sung, Cho, YoungSoo, Liu, Xin, Ruan, Xianglin, Liang, Lili, Dharan, Nila, Cho, Sang-Nae, Barry, Clifton E., III, Ellner, Jerrold J., Dorman, Susan E., and Alland, David

Published
2017
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14. The Clinical Course of COVID-19 in the Outpatient Setting: A Prospective Cohort Study

Author

Blair, Paul W, Brown, Diane M, Jang, Minyoung, Antar, Annukka A R, Keruly, Jeanne C, Bachu, Vismaya S, Townsend, Jennifer L, Tornheim, Jeffrey A, Keller, Sara C, Sauer, Lauren, Thomas, David L, Manabe, Yukari C, Cox, Andrea L, Heaney, Chris D, Klein, Sabra L, Mehta, Shruti H, Mostafa, Heba, Pekosz, Andy S, Pisanic, Nora, Smith, L Leigh, Armstrong, Derek T, Azamfirei, Razvan, Barnaba, Brittany, Charles, Curtisha, Church, Taylor, Dai, Weiwei, Fuchs, Joelle, Ganesan, Abhinaya, Hardick, Justin, Holden, Jeffrey, Johnstone, Jaylynn R, Kruczynski, Kate, Kusemiju, Oyinkansola, Lambrou, Anastasia, Li, Lucy, Littlefield, Kirsten, Montana, Manuela Plazas, Park, Han-Sol, Payton, Christine B, Popper, Caroline, Prizzi, Michelle, Reuland, Carolyn J, Sewell, Thelio, Tuchler, Amanda, Ursin, Rebecca L, and Walch, Samantha N

Subjects
Pediatrics, medicine.medical_specialty, Population, Vital signs, Disease, recovery of function, Logistic regression, 01 natural sciences, Major Articles, 03 medical and health sciences, 0302 clinical medicine, Ambulatory care, ambulatory care, Interquartile range, Internal medicine, middle aged, Sore throat, medicine, 030212 general & internal medicine, 0101 mathematics, education, Prospective cohort study, education.field_of_study, business.industry, coronavirus infections/epidemiology, 010102 general mathematics, Emergency department, medicine.disease, Comorbidity, Confidence interval, Infectious Diseases, AcademicSubjects/MED00290, Oncology, Cohort, treatment outcome, Chills, medicine.symptom, business
Abstract

BackgroundOutpatient COVID-19 has been insufficiently characterized.ObjectiveTo determine the progression of disease and subsequent determinants of hospitalization.DesignA prospective outpatient cohort.SettingOutpatients were recruited by phone between April 21 to June 23, 2020 after receiving outpatient or emergency department testing within a large health network in Maryland, USA.ParticipantsOutpatient adults with positive RT-PCR results for SARS-CoV-2.MeasurementsSymptoms, portable pulse oximeter oxygen saturation (SaO2), heart rate, and temperature were collected by participants on days 0, 3, 7, 14, 21, and 28 after enrollment. Baseline demographics, comorbid conditions were evaluated for risk of subsequent hospitalization using negative binomial, logistic, and random effects logistic regression.ResultsAmong 118 SARS-CoV-2 infected outpatients, the median age was 56.0 years (IQR, 50.0 to 63.0) and 50 (42.4%) were male. Among those reporting active symptoms, the most common symptoms during the first week since symptom onset included weakness/fatigue (67.3%), cough (58.0%), headache (43.8%), and sore throat (34.8%). Participants returned to their usual health a median of 20 days (IQR, 13 to 38) from the symptom onset, and only 65.5% of respondents were at their usual health during the fourth week of illness. Over 28 days, 10.9% presented to the emergency department and 7.6% required hospitalization. Individuals at the same duration of illness had a 6.1 times increased adjusted odds of subsequent hospitalization per every percent decrease in home SaO2(95% confidence interval [CI]: 1.41 to 31.23, p=0.02).LimitationsSeverity and duration of illness may differ in a younger population.ConclusionSymptoms often persisted but uncommonly progressed to hospitalization. Home SaO2might be an important adjunctive tool to identify progression of COVID-19.RegistrationClinicaltrials.gov NCT number:NCT04496466Funding SourceThe Sherrilyn and Ken Fisher Center for Environmental Infectious Diseases Discovery Program and the Johns Hopkins University School of Medicine

Published
2021

17. Delayed Rise of Oral Fluid Antibodies, Elevated BMI, and Absence of Early Fever Correlate With Longer Time to SARS-CoV-2 RNA Clearance in a Longitudinally Sampled Cohort of COVID-19 Outpatients

Author

Antar, Annukka A R, primary, Yu, Tong, additional, Pisanic, Nora, additional, Azamfirei, Razvan, additional, Tornheim, Jeffrey A, additional, Brown, Diane M, additional, Kruczynski, Kate, additional, Hardick, Justin P, additional, Sewell, Thelio, additional, Jang, Minyoung, additional, Church, Taylor, additional, Walch, Samantha N, additional, Reuland, Carolyn, additional, Bachu, Vismaya S, additional, Littlefield, Kirsten, additional, Park, Han-Sol, additional, Ursin, Rebecca L, additional, Ganesan, Abhinaya, additional, Kusemiju, Oyinkansola, additional, Barnaba, Brittany, additional, Charles, Curtisha, additional, Prizzi, Michelle, additional, Johnstone, Jaylynn R, additional, Payton, Christine, additional, Dai, Weiwei, additional, Fuchs, Joelle, additional, Massaccesi, Guido, additional, Armstrong, Derek T, additional, Townsend, Jennifer L, additional, Keller, Sara C, additional, Demko, Zoe O, additional, Hu, Chen, additional, Wang, Mei-Cheng, additional, Sauer, Lauren M, additional, Mostafa, Heba H, additional, Keruly, Jeanne C, additional, Mehta, Shruti H, additional, Klein, Sabra L, additional, Cox, Andrea L, additional, Pekosz, Andrew, additional, Heaney, Christopher D, additional, Thomas, David L, additional, Blair, Paul W, additional, and Manabe, Yukari C, additional

Published
2021
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18. Delayed rise of oral fluid antibodies, elevated BMI, and absence of early fever correlate with longer time to SARS-CoV-2 RNA clearance in an longitudinally sampled cohort of COVID-19 outpatients

Author

Antar, Annukka A. R., primary, Yu, Tong, additional, Pisanic, Nora, additional, Azamfirei, Razvan, additional, Tornheim, Jeffrey A., additional, Brown, Diane M., additional, Kruczynski, Kate, additional, Hardick, Justin P., additional, Sewell, Thelio, additional, Jang, Minyoung, additional, Church, Taylor, additional, Walch, Samantha N., additional, Reuland, Carolyn, additional, Bachu, Vismaya S., additional, Littlefield, Kirsten, additional, Park, Han-Sol, additional, Ursin, Rebecca L., additional, Ganesan, Abhinaya, additional, Kusemiju, Oyinkansola, additional, Barnaba, Brittany, additional, Charles, Curtisha, additional, Prizzi, Michelle, additional, Johnstone, Jaylynn R., additional, Payton, Christine, additional, Dai, Weiwei, additional, Fuchs, Joelle, additional, Massaccesi, Guido, additional, Armstrong, Derek T., additional, Townsend, Jennifer L., additional, Keller, Sara C., additional, Demko, Zoe O, additional, Hu, Chen, additional, Wang, Mei-Cheng, additional, Sauer, Lauren M., additional, Mostafa, Heba H., additional, Keruly, Jeanne C., additional, Mehta, Shruti H., additional, Klein, Sabra L., additional, Cox, Andrea L., additional, Pekosz, Andrew, additional, Heaney, Christopher D., additional, Thomas, David L., additional, Blair, Paul W., additional, and Manabe, Yukari C., additional

Published
2021
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19. Direct detection of SARS-CoV-2 RNA using high-contrast pH-sensitive dyes

Author

Brown, Timothy A., primary, Schaefer, Katherine S., additional, Tsang, Arthur, additional, Yi, Hyun Ah, additional, Grimm, Jonathan B., additional, Lemire, Andrew L., additional, Jradi, Fadi M., additional, Kim, Charles, additional, McGowan, Kevin, additional, Ritola, Kimberly, additional, Armstrong, Derek T., additional, Mostafa, Heba H., additional, Korff, Wyatt, additional, Vale, Ronald D., additional, and Lavis, Luke D., additional

Published
2021
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20. Repeated Coronavirus Disease 2019 Molecular Testing: Correlation of Severe Acute Respiratory Syndrome Coronavirus 2 Culture With Molecular Assays and Cycle Thresholds

Author

Gniazdowski, Victoria, primary, Paul Morris, C, additional, Wohl, Shirlee, additional, Mehoke, Thomas, additional, Ramakrishnan, Srividya, additional, Thielen, Peter, additional, Powell, Harrison, additional, Smith, Brendan, additional, Armstrong, Derek T, additional, Herrera, Monica, additional, Reifsnyder, Carolyn, additional, Sevdali, Maria, additional, Carroll, Karen C, additional, Pekosz, Andrew, additional, and Mostafa, Heba H, additional

Published
2020
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21. Repeated Coronavirus Disease 2019 Molecular Testing: Correlation of Severe Acute Respiratory Syndrome Coronavirus 2 Culture With Molecular Assays and Cycle Thresholds.

Author

Gniazdowski, Victoria, Morris, C Paul, Wohl, Shirlee, Mehoke, Thomas, Ramakrishnan, Srividya, Thielen, Peter, Powell, Harrison, Smith, Brendan, Armstrong, Derek T, Herrera, Monica, Reifsnyder, Carolyn, Sevdali, Maria, Carroll, Karen C, Pekosz, Andrew, and Mostafa, Heba H

Subjects
RNA analysis, CELL culture, MOLECULAR diagnosis, COVID-19, SEQUENCE analysis, MEDICAL screening, RETROSPECTIVE studies, GENOTYPES, DESCRIPTIVE statistics, COVID-19 testing, SARS virus, POLYMERASE chain reaction, DIAGNOSTIC errors, LONGITUDINAL method
Abstract

Background Repeated coronavirus disease 2019 (COVID-19) molecular testing can lead to positive test results after negative results and to multiple positive results over time. The association between positive test results and infectious virus is important to quantify. Methods A 2-month cohort of retrospective data and consecutively collected specimens from patients with COVID-19 or patients under investigation were used to understand the correlation between prolonged viral RNA positive test results, cycle threshold (Ct) values and growth of severe acute respiratory syndrome coronavirus 2 (SARS-CoV-2) in cell culture. Whole-genome sequencing was used to confirm virus genotype in patients with prolonged viral RNA detection. Droplet digital polymerase chain reaction was used to assess the rate of false-negative COVID-19 diagnostic test results. Results In 2 months, 29 686 specimens were tested and 2194 patients underwent repeated testing. Virus recovery in cell culture was noted in specimens with a mean Ct value of 18.8 (3.4) for SARS-CoV-2 target genes. Prolonged viral RNA shedding was associated with positive virus growth in culture in specimens collected up to 21 days after the first positive result but mostly in individuals symptomatic at the time of sample collection. Whole-genome sequencing provided evidence the same virus was carried over time. Positive test results following negative results had Ct values >29.5 and were not associated with virus culture. Droplet digital polymerase chain reaction results were positive in 5.6% of negative specimens collected from patients with confirmed or clinically suspected COVID-19. Conclusions Low Ct values in SARS-CoV-2 diagnostic tests were associated with virus growth in cell culture. Symptomatic patients with prolonged viral RNA shedding can also be infectious. [ABSTRACT FROM AUTHOR]

Published
2021
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22. Clustering of SARS-CoV-2 Infections in Households of Patients Diagnosed in the Outpatient Setting in Baltimore, Maryland.

Author

Demko, Zoe O, Antar, Annukka A R, Blair, Paul W, Lambrou, Anastasia S, Yu, Tong, Brown, Diane, Walch, Samantha N, Armstrong, Derek T, Mostafa, Heba H, Keruly, Jeanne C, Thomas, David L, Manabe, Yukari C, Mehta, Shruti H, and Team, Ambulatory COVID Study

Subjects
SARS-CoV-2, HOUSEHOLDS
Abstract

In an outpatient cohort in Maryland, clustering of severe acute respiratory syndrome coronavirus 2 (SARS-CoV-2) positivity within households was high, with 76% of 74 households reporting at least 1 other symptomatic person and 66% reporting another person who tested SARS-CoV-2 positive. SARS-CoV-2 positivity among household members was associated with larger household size and bedroom sharing. [ABSTRACT FROM AUTHOR]

Published
2021
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23. Genomic analysis of globally diverse Mycobacterium tuberculosis strains provides insights into the emergence and spread of multidrug resistance

Author

Manson, Abigail L. (author), Cohen, Keira A (author), Abeel, T.E.P.M.F. (author), Desjardins, Christopher A. (author), Armstrong, Derek T. (author), Barry III, Clifton E. (author), Brand, Jeannette (author), Chapman, Sinéad B. (author), Cho, Sang-Nae (author), Gabrielian, Andrei (author), Salazar, A.N. (author), Manson, Abigail L. (author), Cohen, Keira A (author), Abeel, T.E.P.M.F. (author), Desjardins, Christopher A. (author), Armstrong, Derek T. (author), Barry III, Clifton E. (author), Brand, Jeannette (author), Chapman, Sinéad B. (author), Cho, Sang-Nae (author), Gabrielian, Andrei (author), and Salazar, A.N. (author)

Abstract

Multidrug-resistant tuberculosis (MDR-TB), caused by drug-resistant strains of Mycobacterium tuberculosis, is an increasingly serious problem worldwide. Here we examined a data set of whole-genome sequences from 5,310 M. tuberculosis isolates from five continents. Despite the great diversity of these isolates with respect to geographical point of isolation, genetic background and drug resistance, the patterns for the emergence of drug resistance were conserved globally. We have identified harbinger mutations that often precede multidrug resistance. In particular, the katG mutation encoding p.Ser315Thr, which confers resistance to isoniazid, overwhelmingly arose before mutations that conferred rifampicin resistance across all of the lineages, geographical regions and time periods. Therefore, molecular diagnostics that include markers for rifampicin resistance alone will be insufficient to identify pre-MDR strains. Incorporating knowledge of polymorphisms that occur before the emergence of multidrug resistance, particularly katG p.Ser315Thr, into molecular diagnostics should enable targeted treatment of patients with pre-MDR-TB to prevent further development of MDR-TB., Accepted author manuscript, Pattern Recognition and Bioinformatics

Published
2017
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24. A Phase 2 Randomized Trial of a Rifapentine plus Moxifloxacin-Based Regimen for Treatment of Pulmonary Tuberculosis

Author

Conde, Marcus B., primary, Mello, Fernanda C. Q., additional, Duarte, Rafael Silva, additional, Cavalcante, Solange C., additional, Rolla, Valeria, additional, Dalcolmo, Margareth, additional, Loredo, Carla, additional, Durovni, Betina, additional, Armstrong, Derek T., additional, Efron, Anne, additional, Barnes, Grace L., additional, Marzinke, Mark A., additional, Savic, Radojka M., additional, Dooley, Kelly E., additional, Cohn, Silvia, additional, Moulton, Lawrence H., additional, Chaisson, Richard E., additional, and Dorman, Susan E., additional

Published
2016
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25. Analytical and Clinical Evaluation of the Epistem Genedrive Assay for Detection of Mycobacterium tuberculosis

Author

Shenai, Shubhada, primary, Armstrong, Derek T., additional, Valli, Eloise, additional, Dolinger, David L., additional, Nakiyingi, Lydia, additional, Dietze, Reynaldo, additional, Dalcolmo, Margareth Pretti, additional, Nicol, Mark P., additional, Zemanay, Widaad, additional, Manabe, Yuka, additional, Hadad, David Jamil, additional, Marques-Rodrigues, Patricia, additional, Palaci, Moises, additional, Peres, Renata L., additional, Gaeddert, Mary, additional, Armakovitch, Sandra, additional, Nonyane, Bareng A. S., additional, Denkinger, Claudia M., additional, Banada, Padmapriya, additional, Joloba, Moses L., additional, Ellner, Jerrold, additional, Boehme, Catharina, additional, Alland, David, additional, and Dorman, Susan E., additional

Published
2016
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27. Improving the Sensitivity of the Xpert MTB/RIF Assay on Sputum Pellets by Decreasing the Amount of Added Sample Reagent: a Laboratory and Clinical Evaluation

Author

Dharan, Nila J., primary, Amisano, Danielle, additional, Mboowa, Gerald, additional, Ssengooba, Willy, additional, Blakemore, Robert, additional, Kubiak, Rachel W., additional, Armstrong, Derek T., additional, Jones, Martin, additional, Manabe, Yukari C., additional, Joloba, Moses L., additional, Ellner, Jerrold J., additional, Dorman, Susan E., additional, and Alland, David, additional

Published
2015
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29. Multidrug-Resistant Nontuberculous Mycobacteria Isolated from Cystic Fibrosis Patients

Author

Cândido, Pedro Henrique Campanini, primary, Nunes, Luciana de Souza, additional, Marques, Elizabeth Andrade, additional, Folescu, Tânia Wrobel, additional, Coelho, Fábrice Santana, additional, de Moura, Vinicius Calado Nogueira, additional, da Silva, Marlei Gomes, additional, Gomes, Karen Machado, additional, Lourenço, Maria Cristina da Silva, additional, Aguiar, Fábio Silva, additional, Chitolina, Fernanda, additional, Armstrong, Derek T., additional, Leão, Sylvia Cardoso, additional, Neves, Felipe Piedade Gonçalves, additional, Mello, Fernanda Carvalho de Queiroz, additional, and Duarte, Rafael Silva, additional

Published
2014
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30. Diagnostic Accuracy of a Rapid Urine Lipoarabinomannan Test for Tuberculosis in HIV-Infected Adults

Author

Nakiyingi, Lydia, primary, Moodley, Vineshree Mischka, additional, Manabe, Yukari C., additional, Nicol, Mark P., additional, Holshouser, Molly, additional, Armstrong, Derek T., additional, Zemanay, Widaad, additional, Sikhondze, Welile, additional, Mbabazi, Olive, additional, Nonyane, Bareng A.S., additional, Shah, Maunank, additional, Joloba, Moses L., additional, Alland, David, additional, Ellner, Jerrold J., additional, and Dorman, Susan E., additional

Published
2014
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31. Sensititre MYCOTB MIC Plate for Testing Mycobacterium tuberculosis Susceptibility to First- and Second-Line Drugs

Author

Lee, Jongseok, primary, Armstrong, Derek T., additional, Ssengooba, Willy, additional, Park, Jeong-ae, additional, Yu, Yeuni, additional, Mumbowa, Francis, additional, Namaganda, Carolyn, additional, Mboowa, Gerald, additional, Nakayita, Germine, additional, Armakovitch, Sandra, additional, Chien, Gina, additional, Cho, Sang-Nae, additional, Via, Laura E., additional, Barry, Clifton E., additional, Ellner, Jerrold J., additional, Alland, David, additional, Dorman, Susan E., additional, and Joloba, Moses L., additional

Published
2014
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32. Genomic analysis of globally diverse Mycobacterium tuberculosis strains provides insights into the emergence and spread of multidrug resistance

Author

Manson, Abigail L, Cohen, Keira A, Abeel, Thomas, Desjardins, Christopher A, Armstrong, Derek T, Barry, Clifton E, Brand, Jeannette, Chapman, Sinéad B, Cho, Sang-Nae, Gabrielian, Andrei, Gomez, James, Jodals, Andreea M, Joloba, Moses, Jureen, Pontus, Lee, Jong Seok, Malinga, Lesibana, Maiga, Mamoudou, Nordenberg, Dale, Noroc, Ecaterina, Romancenco, Elena, Salazar, Alex, Ssengooba, Willy, Velayati, A A, Winglee, Kathryn, Zalutskaya, Aksana, Via, Laura E, Cassell, Gail H, Dorman, Susan E, Ellner, Jerrold, Farnia, Parissa, Galagan, James E, Rosenthal, Alex, Crudu, Valeriu, Homorodean, Daniela, Hsueh, Po-Ren, Narayanan, Sujatha, Pym, Alexander S, Skrahina, Alena, Swaminathan, Soumya, Van der Walt, Martie, Alland, David, Bishai, William R, Cohen, Ted, Hoffner, Sven, Birren, Bruce W, and Earl, Ashlee M

Abstract

Multidrug-resistant tuberculosis (MDR-TB), caused by drug-resistant strains of Mycobacterium tuberculosis, is an increasingly serious problem worldwide. Here we examined a data set of whole-genome sequences from 5,310 M. tuberculosis isolates from five continents. Despite the great diversity of these isolates with respect to geographical point of isolation, genetic background and drug resistance, the patterns for the emergence of drug resistance were conserved globally. We have identified harbinger mutations that often precede multidrug resistance. In particular, the katG mutation encoding p.Ser315Thr, which confers resistance to isoniazid, overwhelmingly arose before mutations that conferred rifampicin resistance across all of the lineages, geographical regions and time periods. Therefore, molecular diagnostics that include markers for rifampicin resistance alone will be insufficient to identify pre-MDR strains. Incorporating knowledge of polymorphisms that occur before the emergence of multidrug resistance, particularly katG p.Ser315Thr, into molecular diagnostics should enable targeted treatment of patients with pre-MDR-TB to prevent further development of MDR-TB.

Published
2017
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35. Sensititre MYCOTB MIC Plate for Testing Mycobacterium tuberculosisSusceptibility to First- and Second-Line Drugs

Author

Lee, Jongseok, Armstrong, Derek T., Ssengooba, Willy, Park, Jeong-ae, Yu, Yeuni, Mumbowa, Francis, Namaganda, Carolyn, Mboowa, Gerald, Nakayita, Germine, Armakovitch, Sandra, Chien, Gina, Cho, Sang-Nae, Via, Laura E., Barry, Clifton E., Ellner, Jerrold J., Alland, David, Dorman, Susan E., and Joloba, Moses L.

Abstract

ABSTRACTFor Mycobacterium tuberculosis, phenotypic methods for drug susceptibility testing of second-line drugs are poorly standardized and technically challenging. The Sensititre MYCOTB MIC plate (MYCOTB) is a microtiter plate containing lyophilized antibiotics and configured for determination of MICs to first- and second-line antituberculosis drugs. To evaluate the performance of MYCOTB for M. tuberculosisdrug susceptibility testing using the Middlebrook 7H10 agar proportion method (APM) as the comparator, we conducted a two-site study using archived M. tuberculosisisolates from Uganda and the Republic of Korea. Thawed isolates were subcultured, and dilutions were inoculated into MYCOTB wells and onto 7H10 agar. MYCOTB results were read at days 7, 10, 14, and 21; APM results were read at 21 days. A total of 222 isolates provided results on both platforms. By APM, 106/222 (47.7%) of isolates were resistant to at least isoniazid and rifampin. Agreement between MYCOTB and APM with respect to susceptibility or resistance was ≥92% for 7 of 12 drugs when a strict definition was used and ≥96% for 10 of 12 drugs when agreement was defined by allowing a ± one-well range of dilutions around the APM critical concentration. For ethambutol, agreement was 80% to 81%. For moxifloxacin, agreement was 83% to 85%; incorporating existing DNA sequencing information for discrepant analysis raised agreement to 91% to 96%. For MYCOTB, the median time to plate interpretation was 10 days and interreader agreement was ≥95% for all drugs. MYCOTB provided reliable results for M. tuberculosissusceptibility testing of first- and second-line drugs except ethambutol, and results were available sooner than those determined by APM.

Published
2013
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36. Specimen Dilution Improves Sensitivity of the Amplified Mycobacterium tuberculosisDirect Test for Smear Microscopy-Positive Respiratory Specimens

Author

Guerra, Renata L., Baker, James F., Alborz, Roya, Armstrong, Derek T., Kiehlbauch, Julia A., Conde, Marcus B., Dorman, Susan E., and Hooper, Nancy M.

Abstract

ABSTRACTSpecimen dilution has been proposed as a strategy to minimize amplified Mycobacterium tuberculosisdirect (MTD) test inhibition (N. Pollock, J. Westerling, and A. Sloutsky, Am. J. Clin. Pathol. 126:142-147, 2006; A. Sloutsky, L. L. Han, and B. G. Werner, J. Clin. Microbiol. 42:1547-1551, 2004). We evaluated the impact of respiratory specimen dilution on MTD test accuracy in a public health laboratory. The difference in MTD test sensitivity between the dilution and conventional methods was 15.9% (P= 0.001) for smear microscopy-positive specimens and -3.6% (P= 0.38) for smear microscopy-negative specimens.

Published
2008
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37. Cost-Effectiveness of Different Strategies for Amplified Mycobacterium tuberculosisDirect Testing for Cases of Pulmonary Tuberculosis

Author

Guerra, Renata L., Hooper, Nancy M., Baker, James F., Alborz, Roya, Armstrong, Derek T., Kiehlbauch, Julia A., Conde, Marcus B., and Dorman, Susan E.

Abstract

ABSTRACTWe conducted a decision analysis to assess and compare four algorithms for amplified Mycobacterium tuberculosisdirect (MTD) testing of respiratory specimens in terms of cost-effectiveness. The most cost-effective strategy was one in which smear-positive specimens but not smear-negative specimens were diluted prior to MTD testing.

Published
2008
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38. Delayed rise of oral fluid antibodies, elevated BMI, and absence of early fever correlate with longer time to SARS-CoV-2 RNA clearance in an longitudinally sampled cohort of COVID-19 outpatients.

Author

Antar AAR, Yu T, Pisanic N, Azamfirei R, Tornheim JA, Brown DM, Kruczynski K, Hardick JP, Sewell T, Jang M, Church T, Walch SN, Reuland C, Bachu VS, Littlefield K, Park HS, Ursin RL, Ganesan A, Kusemiju O, Barnaba B, Charles C, Prizzi M, Johnstone JR, Payton C, Dai W, Fuchs J, Massaccesi G, Armstrong DT, Townsend JL, Keller SC, Demko ZO, Hu C, Wang MC, Sauer LM, Mostafa HH, Keruly JC, Mehta SH, Klein SL, Cox AL, Pekosz A, Heaney CD, Thomas DL, Blair PW, and Manabe YC

Abstract

Background: Sustained molecular detection of SARS-CoV-2 RNA in the upper respiratory tract (URT) in mild to moderate COVID-19 is common. We sought to identify host and immune determinants of prolonged SARS-CoV-2 RNA detection., Methods: Ninety-five outpatients self-collected mid-turbinate nasal, oropharyngeal (OP), and gingival crevicular fluid (oral fluid) samples at home and in a research clinic a median of 6 times over 1-3 months. Samples were tested for viral RNA, virus culture, and SARS-CoV-2 and other human coronavirus antibodies, and associations were estimated using Cox proportional hazards models., Results: Viral RNA clearance, as measured by SARS-CoV-2 RT-PCR, in 507 URT samples occurred a median (IQR) 33.5 (17-63.5) days post-symptom onset. Sixteen nasal-OP samples collected 2-11 days post-symptom onset were virus culture positive out of 183 RT-PCR positive samples tested. All participants but one with positive virus culture were negative for concomitant oral fluid anti-SARS-CoV-2 antibodies. The mean time to first antibody detection in oral fluid was 8-13 days post-symptom onset. A longer time to first detection of oral fluid anti-SARS-CoV-2 S antibodies (aHR 0.96, 95% CI 0.92-0.99, p=0.020) and BMI ≥ 25kg/m 2 (aHR 0.37, 95% CI 0.18-0.78, p=0.009) were independently associated with a longer time to SARS-CoV-2 viral RNA clearance. Fever as one of first three COVID-19 symptoms correlated with shorter time to viral RNA clearance (aHR 2.06, 95% CI 1.02-4.18, p=0.044)., Conclusions: We demonstrate that delayed rise of oral fluid SARS-CoV-2-specific antibodies, elevated BMI, and absence of early fever are independently associated with delayed URT viral RNA clearance.

Published
2021
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