Publications by authors named "Shirlee Wohl"

Highly Pathogenic Avian Influenza strain H5N1 has caused a multi-state outbreak among US dairy cattle, spreading across 15 states and infecting hundreds of herds since its onset. We rapidly developed and optimized PCR-based detection assays and sequencing protocols to support H5N1 molecular surveillance. Using 214 retail milk from 20 states for methods development, we found that H5N1 concentrations by digital PCR strongly correlated with qPCR cycle threshold (Ct) values, with dPCR exhibiting greater sensitivity.

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Article Synopsis
  • The accuracy of pathogen sequence data analysis relies heavily on the number and type of sequences included in the sample, impacting the conclusions drawn from phylogenetic studies.
  • There is a lack of clear guidance on designing effective studies for phylogenetic inference, specifically regarding how to determine which individuals are more likely to spread pathogens.
  • The study introduces a new estimator for measuring differential pathogen transmission among individuals, provides sample size calculations, and offers an R package called phylosamp for practical implementation and validation of the method.
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Despite ongoing containment and vaccination efforts, cholera remains prevalent in many countries in sub-Saharan Africa. Part of the difficulty in containing cholera comes from our lack of understanding of how it circulates throughout the region. To better characterize regional transmission, we generated and analyzed 118 genomes collected between 2007-2019 from five different countries in Southern and Eastern Africa.

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The maturation of genomic surveillance in the past decade has enabled tracking of the emergence and spread of epidemics at an unprecedented level. During the COVID-19 pandemic, for example, genomic data revealed that local epidemics varied considerably in the frequency of severe acute respiratory syndrome coronavirus 2 (SARS-CoV-2) lineage importation and persistence, likely due to a combination of COVID-19 restrictions and changing connectivity. Here, we show that local COVID-19 epidemics are driven by regional transmission, including across international boundaries, but can become increasingly connected to distant locations following the relaxation of public health interventions.

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Long non-coding RNAs (lncRNAs) are involved in numerous biological processes and are pivotal mediators of the immune response, yet little is known about their properties at the single-cell level. Here, we generate a multi-tissue bulk RNAseq dataset from Ebola virus (EBOV) infected and not-infected rhesus macaques and identified 3979 novel lncRNAs. To profile lncRNA expression dynamics in immune circulating single-cells during EBOV infection, we design a metric, Upsilon, to estimate cell-type specificity.

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Tracking the emergence and spread of pathogen variants is an important component of monitoring infectious disease outbreaks. To that end, accurately estimating the number and prevalence of pathogen variants in a population requires carefully designed surveillance programs. However, current approaches to calculating the number of pathogen samples needed for effective surveillance often do not account for the various processes that can bias which infections are detected and which samples are ultimately characterized as a specific variant.

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RNA viruses have short generation times and high mutation rates, allowing them to undergo rapid molecular evolution during epidemics. However, the extent of RNA virus phenotypic evolution within epidemics and the resulting effects on fitness and virulence remain mostly unknown. Here, we screened the 2015-2016 Zika epidemic in the Americas for lineage-specific fitness differences.

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Regional connectivity and land travel have been identified as important drivers of SARS-CoV-2 transmission. However, the generalizability of this finding is understudied outside of well-sampled, highly connected regions. In this study, we investigated the relative contributions of regional and intercontinental connectivity to the source-sink dynamics of SARS-CoV-2 for Jordan and the Middle East.

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During the last decades, antimicrobial resistance (AMR) has become a global public health concern. Nowadays multi-drug resistance is commonly observed in strains of , the etiological agent of cholera. In order to limit the spread of pathogenic drug-resistant bacteria and to maintain treatment options the analysis of clinical samples and their AMR profiles are essential.

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Article Synopsis
  • Effective detection of SARS-CoV-2 variants through wastewater analysis can complement existing clinical testing methods, especially in resource-limited areas where traditional testing may be biased.* -
  • The study implemented improved virus concentration techniques and software to enhance the sequencing of multiple virus strains from wastewater, resulting in high-resolution data over 295 days at a university and its surrounding county.* -
  • Wastewater surveillance identified emerging variants up to 14 days earlier than clinical methods and revealed instances of virus spread that clinical testing missed, highlighting its potential for public health monitoring.*
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As SARS-CoV-2 continues to spread and evolve, detecting emerging variants early is critical for public health interventions. Inferring lineage prevalence by clinical testing is infeasible at scale, especially in areas with limited resources, participation, or testing/sequencing capacity, which can also introduce biases. SARS-CoV-2 RNA concentration in wastewater successfully tracks regional infection dynamics and provides less biased abundance estimates than clinical testing.

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Sample size calculations are an essential component of the design and evaluation of scientific studies. However, there is a lack of clear guidance for determining the sample size needed for phylogenetic studies, which are becoming an essential part of studying pathogen transmission. We introduce a statistical framework for determining the number of true infector-infectee transmission pairs identified by a phylogenetic study, given the size and population coverage of that study.

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  • Cholera outbreaks in West Africa are not well understood, and genomic surveillance could help identify transmission patterns to improve control measures.
  • Researchers sequenced 46 cholera isolates from Nigeria, Cameroon, and Niger to explore the relationships between strains circulating in those countries.
  • Analysis showed that a specific T12 lineage of the cholera bacterium has been continuously transmitted in West Africa since 2009, even during periods without reported cases; this study models future coordinated surveillance efforts.
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The early COVID-19 pandemic was characterized by rapid global spread. In Maryland and Washington, DC, United States, more than 2500 cases were reported within 3 weeks of the first COVID-19 detection in March 2020. We aimed to use genomic sequencing to understand the initial spread of SARS-CoV-2 - the virus that causes COVID-19 - in the region.

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  • Cholera epidemics in South Sudan (2014-2017) were influenced by civil unrest, flooding, and population displacement, resulting in three waves with varying spatial spread.
  • The study employed epidemiological methods and genomic sequencing to analyze the progression of cholera, explore the impact of vaccination campaigns, and examine the relationship between rainfall and disease transmission.
  • Findings revealed that earlier epidemics were geographically limited, while the last wave spread significantly, with close genetic ties to cholera strains in neighboring countries, and highlighted the role of population movement in the distribution of cases.
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  • Positive COVID-19 tests can occur even after negative results, and prolonged viral RNA shedding has been linked to infectiousness, particularly in symptomatic individuals.
  • A study using over 29,000 specimens found that virus growth in culture was more likely with lower cycle threshold (Ct) values, specifically a mean Ct of 18.8, indicating active infection.
  • Whole-genome sequencing confirmed that patients often carried the same virus over time, and high Ct values (greater than 29.5) were generally associated with non-infectious positivity.
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Background: The early COVID-19 pandemic has been characterized by rapid global spread. In the United States National Capital Region, over 2,000 cases were reported within three weeks of its first detection in March 2020. We aimed to use genomic sequencing to understand the initial spread of SARS-CoV-2, the virus that causes COVID-19, in the region.

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Unusually large outbreaks of mumps across the United States in 2016 and 2017 raised questions about the extent of mumps circulation and the relationship between these and prior outbreaks. We paired epidemiological data from public health investigations with analysis of mumps virus whole genome sequences from 201 infected individuals, focusing on Massachusetts university communities. Our analysis suggests continuous, undetected circulation of mumps locally and nationally, including multiple independent introductions into Massachusetts and into individual communities.

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Metagenomic sequencing has the potential to transform microbial detection and characterization, but new tools are needed to improve its sensitivity. Here we present CATCH, a computational method to enhance nucleic acid capture for enrichment of diverse microbial taxa. CATCH designs optimal probe sets, with a specified number of oligonucleotides, that achieve full coverage of, and scale well with, known sequence diversity.

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During 2018, an unusual increase in Lassa fever cases occurred in Nigeria, raising concern among national and international public health agencies. We analyzed 220 Lassa virus genomes from infected patients, including 129 from the 2017-2018 transmission season, to understand the viral populations underpinning the increase. A total of 14 initial genomes from 2018 samples were generated at Redeemer's University in Nigeria, and the findings were shared with the Nigerian Center for Disease Control in real time.

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In one patient over time, we found that concentration of Ebola virus RNA in semen during recovery is remarkably higher than blood at peak illness. Virus in semen is replication-competent with no change in viral genome over time. Presence of sense RNA suggests replication in cells present in semen.

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Although the recent Zika virus (ZIKV) epidemic in the Americas and its link to birth defects have attracted a great deal of attention, much remains unknown about ZIKV disease epidemiology and ZIKV evolution, in part owing to a lack of genomic data. Here we address this gap in knowledge by using multiple sequencing approaches to generate 110 ZIKV genomes from clinical and mosquito samples from 10 countries and territories, greatly expanding the observed viral genetic diversity from this outbreak. We analysed the timing and patterns of introductions into distinct geographic regions; our phylogenetic evidence suggests rapid expansion of the outbreak in Brazil and multiple introductions of outbreak strains into Puerto Rico, Honduras, Colombia, other Caribbean islands, and the continental United States.

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Article Synopsis
  • Zika virus (ZIKV) has sparked a significant epidemic, particularly linked to serious birth defects, with local transmission first reported in the U.S. in July 2016.
  • Researchers tracked the virus's introduction in Florida through genome sequencing of infected patients and mosquitoes, identifying at least 4 to potentially 40 separate introductions before local transmission began in spring 2016.
  • The study highlights that most ZIKV cases in Florida were connected to the Caribbean, supported by data on high traffic and infection rates from that region to Miami, enhancing understanding of how ZIKV spreads to new areas.
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The 2013-2016 West African epidemic caused by the Ebola virus was of unprecedented magnitude, duration and impact. Here we reconstruct the dispersal, proliferation and decline of Ebola virus throughout the region by analysing 1,610 Ebola virus genomes, which represent over 5% of the known cases. We test the association of geography, climate and demography with viral movement among administrative regions, inferring a classic 'gravity' model, with intense dispersal between larger and closer populations.

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Genomic analysis is a powerful tool for understanding viral disease outbreaks. Sequencing of viral samples is now easier and cheaper than ever before and can supplement epidemiological methods by providing nucleotide-level resolution of outbreak-causing pathogens. In this review, we describe methods used to answer crucial questions about outbreaks, such as how they began and how a disease is transmitted.

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