Your search keyword '"Pfaff, Emily"' showing total 11 results

1. NSAID use and clinical outcomes in COVID-19 patients: a 38-center retrospective cohort study.

Author

Reese, Justin T, Reese, Justin T, Coleman, Ben, Chan, Lauren, Blau, Hannah, Callahan, Tiffany J, Cappelletti, Luca, Fontana, Tommaso, Bradwell, Katie R, Harris, Nomi L, Casiraghi, Elena, Valentini, Giorgio, Karlebach, Guy, Deer, Rachel, McMurry, Julie A, Haendel, Melissa A, Chute, Christopher G, Pfaff, Emily, Moffitt, Richard, Spratt, Heidi, Singh, Jasvinder A, Mungall, Christopher J, Williams, Andrew E, Robinson, Peter N, Reese, Justin T, Reese, Justin T, Coleman, Ben, Chan, Lauren, Blau, Hannah, Callahan, Tiffany J, Cappelletti, Luca, Fontana, Tommaso, Bradwell, Katie R, Harris, Nomi L, Casiraghi, Elena, Valentini, Giorgio, Karlebach, Guy, Deer, Rachel, McMurry, Julie A, Haendel, Melissa A, Chute, Christopher G, Pfaff, Emily, Moffitt, Richard, Spratt, Heidi, Singh, Jasvinder A, Mungall, Christopher J, Williams, Andrew E, and Robinson, Peter N

Abstract

BackgroundNon-steroidal anti-inflammatory drugs (NSAIDs) are commonly used to reduce pain, fever, and inflammation but have been associated with complications in community-acquired pneumonia. Observations shortly after the start of the COVID-19 pandemic in 2020 suggested that ibuprofen was associated with an increased risk of adverse events in COVID-19 patients, but subsequent observational studies failed to demonstrate increased risk and in one case showed reduced risk associated with NSAID use.MethodsA 38-center retrospective cohort study was performed that leveraged the harmonized, high-granularity electronic health record data of the National COVID Cohort Collaborative. A propensity-matched cohort of 19,746 COVID-19 inpatients was constructed by matching cases (treated with NSAIDs at the time of admission) and 19,746 controls (not treated) from 857,061 patients with COVID-19 available for analysis. The primary outcome of interest was COVID-19 severity in hospitalized patients, which was classified as: moderate, severe, or mortality/hospice. Secondary outcomes were acute kidney injury (AKI), extracorporeal membrane oxygenation (ECMO), invasive ventilation, and all-cause mortality at any time following COVID-19 diagnosis.ResultsLogistic regression showed that NSAID use was not associated with increased COVID-19 severity (OR: 0.57 95% CI: 0.53-0.61). Analysis of secondary outcomes using logistic regression showed that NSAID use was not associated with increased risk of all-cause mortality (OR 0.51 95% CI: 0.47-0.56), invasive ventilation (OR: 0.59 95% CI: 0.55-0.64), AKI (OR: 0.67 95% CI: 0.63-0.72), or ECMO (OR: 0.51 95% CI: 0.36-0.7). In contrast, the odds ratios indicate reduced risk of these outcomes, but our quantitative bias analysis showed E-values of between 1.9 and 3.3 for these associations, indicating that comparatively weak or moderate confounder associations could explain away the observed associations.ConclusionsStudy interpretation is limited by the

Published

2022

2. NSAID use and clinical outcomes in COVID-19 patients: a 38-center retrospective cohort study.

Author

Reese, Justin T, Reese, Justin T, Coleman, Ben, Chan, Lauren, Blau, Hannah, Callahan, Tiffany J, Cappelletti, Luca, Fontana, Tommaso, Bradwell, Katie R, Harris, Nomi L, Casiraghi, Elena, Valentini, Giorgio, Karlebach, Guy, Deer, Rachel, McMurry, Julie A, Haendel, Melissa A, Chute, Christopher G, Pfaff, Emily, Moffitt, Richard, Spratt, Heidi, Singh, Jasvinder A, Mungall, Christopher J, Williams, Andrew E, Robinson, Peter N, Reese, Justin T, Reese, Justin T, Coleman, Ben, Chan, Lauren, Blau, Hannah, Callahan, Tiffany J, Cappelletti, Luca, Fontana, Tommaso, Bradwell, Katie R, Harris, Nomi L, Casiraghi, Elena, Valentini, Giorgio, Karlebach, Guy, Deer, Rachel, McMurry, Julie A, Haendel, Melissa A, Chute, Christopher G, Pfaff, Emily, Moffitt, Richard, Spratt, Heidi, Singh, Jasvinder A, Mungall, Christopher J, Williams, Andrew E, and Robinson, Peter N

Abstract

BackgroundNon-steroidal anti-inflammatory drugs (NSAIDs) are commonly used to reduce pain, fever, and inflammation but have been associated with complications in community-acquired pneumonia. Observations shortly after the start of the COVID-19 pandemic in 2020 suggested that ibuprofen was associated with an increased risk of adverse events in COVID-19 patients, but subsequent observational studies failed to demonstrate increased risk and in one case showed reduced risk associated with NSAID use.MethodsA 38-center retrospective cohort study was performed that leveraged the harmonized, high-granularity electronic health record data of the National COVID Cohort Collaborative. A propensity-matched cohort of 19,746 COVID-19 inpatients was constructed by matching cases (treated with NSAIDs at the time of admission) and 19,746 controls (not treated) from 857,061 patients with COVID-19 available for analysis. The primary outcome of interest was COVID-19 severity in hospitalized patients, which was classified as: moderate, severe, or mortality/hospice. Secondary outcomes were acute kidney injury (AKI), extracorporeal membrane oxygenation (ECMO), invasive ventilation, and all-cause mortality at any time following COVID-19 diagnosis.ResultsLogistic regression showed that NSAID use was not associated with increased COVID-19 severity (OR: 0.57 95% CI: 0.53-0.61). Analysis of secondary outcomes using logistic regression showed that NSAID use was not associated with increased risk of all-cause mortality (OR 0.51 95% CI: 0.47-0.56), invasive ventilation (OR: 0.59 95% CI: 0.55-0.64), AKI (OR: 0.67 95% CI: 0.63-0.72), or ECMO (OR: 0.51 95% CI: 0.36-0.7). In contrast, the odds ratios indicate reduced risk of these outcomes, but our quantitative bias analysis showed E-values of between 1.9 and 3.3 for these associations, indicating that comparatively weak or moderate confounder associations could explain away the observed associations.ConclusionsStudy interpretation is limited by the

Published

2022

3. A method for comparing multiple imputation techniques: a case study on the U.S. National COVID Cohort Collaborative

Author

Casiraghi, Elena, Wong, Rachel, Hall, Margaret, Coleman, Ben, Notaro, Marco, Evans, Michael D., Tronieri, Jena S., Blau, Hannah, Laraway, Bryan, Callahan, Tiffany J., Chan, Lauren E., Bramante, Carolyn T., Buse, John B., Moffitt, Richard A., Sturmer, Til, Johnson, Steven G., Shao, Yu Raymond, Reese, Justin, Robinson, Peter N., Paccanaro, Alberto, Valentini, Giorgio, Huling, Jared D., Wilkins, Kenneth, Bennet, Tell, Chute, Christopher, DeWitt, Peter, Gersing, Kenneth, Girvin, Andrew, Haendel, Melissa, Harper, Jeremy, Hajagos, Janos, Hong, Stephanie, Pfaff, Emily, Reusch, Jane, Antoniescu, Corneliu, Robaski, Kimberly, Casiraghi, Elena, Wong, Rachel, Hall, Margaret, Coleman, Ben, Notaro, Marco, Evans, Michael D., Tronieri, Jena S., Blau, Hannah, Laraway, Bryan, Callahan, Tiffany J., Chan, Lauren E., Bramante, Carolyn T., Buse, John B., Moffitt, Richard A., Sturmer, Til, Johnson, Steven G., Shao, Yu Raymond, Reese, Justin, Robinson, Peter N., Paccanaro, Alberto, Valentini, Giorgio, Huling, Jared D., Wilkins, Kenneth, Bennet, Tell, Chute, Christopher, DeWitt, Peter, Gersing, Kenneth, Girvin, Andrew, Haendel, Melissa, Harper, Jeremy, Hajagos, Janos, Hong, Stephanie, Pfaff, Emily, Reusch, Jane, Antoniescu, Corneliu, and Robaski, Kimberly

Abstract

Healthcare datasets obtained from Electronic Health Records have proven to be extremely useful to assess associations between patients' predictors and outcomes of interest. However, these datasets often suffer from missing values in a high proportion of cases and the simple removal of these cases may introduce severe bias. For these reasons, several multiple imputation algorithms have been proposed to attempt to recover the missing information. Each algorithm presents strengths and weaknesses, and there is currently no consensus on which multiple imputation algorithms works best in a given scenario. Furthermore, the selection of each algorithm parameters and data-related modelling choices are also both crucial and challenging. In this paper, we propose a novel framework to numerically evaluate strategies for handling missing data in the context of statistical analysis, with a particular focus on multiple imputation techniques. We demonstrate the feasibility of our approach on a large cohort of type-2 diabetes patients provided by the National COVID Cohort Collaborative (N3C) Enclave, where we explored the influence of various patient characteristics on outcomes related to COVID-19. Our analysis included classic multiple imputation techniques as well as simple complete-case Inverse Probability Weighted models. The experiments presented here show that our approach could effectively highlight the most valid and performant missing-data handling strategy for our case study. Moreover, our methodology allowed us to gain an understanding of the behavior of the different models and of how it changed as we modified their parameters. Our method is general and can be applied to different research fields and on datasets containing heterogeneous types.

Published

2022

4. NSAID use and clinical outcomes in COVID-19 patients: A 38-center retrospective cohort study

Author

Reese, Justin T, Reese, Justin T, Coleman, Ben, Chan, Lauren, Blau, Hannah, Callahan, Tiffany J, Cappelletti, Luca, Fontana, Tommaso, Bradwell, Katie Rebecca, Harris, Nomi L, Casiraghi, Elena, Valentini, Giorgio, Karlebach, Guy, Deer, Rachel, McMurry, Julie A, Haendel, Melissa A, Chute, Christopher G, Pfaff, Emily, Moffitt, Richard, Spratt, Heidi, Singh, Jasvinder, Mungall, Christopher J, Williams, Andrew E, Robinson, Peter N, Reese, Justin T, Reese, Justin T, Coleman, Ben, Chan, Lauren, Blau, Hannah, Callahan, Tiffany J, Cappelletti, Luca, Fontana, Tommaso, Bradwell, Katie Rebecca, Harris, Nomi L, Casiraghi, Elena, Valentini, Giorgio, Karlebach, Guy, Deer, Rachel, McMurry, Julie A, Haendel, Melissa A, Chute, Christopher G, Pfaff, Emily, Moffitt, Richard, Spratt, Heidi, Singh, Jasvinder, Mungall, Christopher J, Williams, Andrew E, and Robinson, Peter N

Abstract

BACKGROUND: Non-steroidal anti-inflammatory drugs (NSAIDs) are commonly used to reduce pain, fever, and inflammation but have been associated with complications in community-acquired pneumonia. Observations shortly after the start of the COVID-19 pandemic in 2020 suggested that ibuprofen was associated with an increased risk of adverse events in COVID-19 patients, but subsequent observational studies failed to demonstrate increased risk and in one case showed reduced risk associated with NSAID use. METHODS: A 38-center retrospective cohort study was performed that leveraged the harmonized, high-granularity electronic health record data of the National COVID Cohort Collaborative. A propensity-matched cohort of COVID-19 inpatients was constructed by matching cases (treated with NSAIDs) and controls (not treated) from 857,061 patients with COVID-19. The primary outcome of interest was COVID-19 severity in hospitalized patients, which was classified as: moderate, severe, or mortality/hospice. Secondary outcomes were acute kidney injury (AKI), extracorporeal membrane oxygenation (ECMO), invasive ventilation, and all-cause mortality at any time following COVID-19 diagnosis. RESULTS: Logistic regression showed that NSAID use was not associated with increased COVID-19 severity (OR: 0.57 95% CI: 0.53-0.61). Analysis of secondary outcomes using logistic regression showed that NSAID use was not associated with increased risk of all-cause mortality (OR 0.51 95% CI: 0.47-0.56), invasive ventilation (OR: 0.59 95% CI: 0.55-0.64), AKI (OR: 0.67 95% CI: 0.63-0.72), or ECMO (OR: 0.51 95% CI: 0.36-0.7). In contrast, the odds ratios indicate reduced risk of these outcomes, but our quantitative bias analysis showed E-values of between 1.9 and 3.3 for these associations, indicating that comparatively weak or moderate confounder associations could explain away the observed associations. CONCLUSIONS: Study interpretation is limited by the observational design. Recording of NSAID use may ha

Published

2021

5. The National COVID Cohort Collaborative (N3C): Rationale, design, infrastructure, and deployment.

Author

Haendel, Melissa A, Haendel, Melissa A, Chute, Christopher G, Bennett, Tellen D, Eichmann, David A, Guinney, Justin, Kibbe, Warren A, Payne, Philip RO, Pfaff, Emily R, Robinson, Peter N, Saltz, Joel H, Spratt, Heidi, Suver, Christine, Wilbanks, John, Wilcox, Adam B, Williams, Andrew E, Wu, Chunlei, Blacketer, Clair, Bradford, Robert L, Cimino, James J, Clark, Marshall, Colmenares, Evan W, Francis, Patricia A, Gabriel, Davera, Graves, Alexis, Hemadri, Raju, Hong, Stephanie S, Hripscak, George, Jiao, Dazhi, Klann, Jeffrey G, Kostka, Kristin, Lee, Adam M, Lehmann, Harold P, Lingrey, Lora, Miller, Robert T, Morris, Michele, Murphy, Shawn N, Natarajan, Karthik, Palchuk, Matvey B, Sheikh, Usman, Solbrig, Harold, Visweswaran, Shyam, Walden, Anita, Walters, Kellie M, Weber, Griffin M, Zhang, Xiaohan Tanner, Zhu, Richard L, Amor, Benjamin, Girvin, Andrew T, Manna, Amin, Qureshi, Nabeel, Kurilla, Michael G, Michael, Sam G, Portilla, Lili M, Rutter, Joni L, Austin, Christopher P, Gersing, Ken R, N3C Consortium, Haendel, Melissa A, Haendel, Melissa A, Chute, Christopher G, Bennett, Tellen D, Eichmann, David A, Guinney, Justin, Kibbe, Warren A, Payne, Philip RO, Pfaff, Emily R, Robinson, Peter N, Saltz, Joel H, Spratt, Heidi, Suver, Christine, Wilbanks, John, Wilcox, Adam B, Williams, Andrew E, Wu, Chunlei, Blacketer, Clair, Bradford, Robert L, Cimino, James J, Clark, Marshall, Colmenares, Evan W, Francis, Patricia A, Gabriel, Davera, Graves, Alexis, Hemadri, Raju, Hong, Stephanie S, Hripscak, George, Jiao, Dazhi, Klann, Jeffrey G, Kostka, Kristin, Lee, Adam M, Lehmann, Harold P, Lingrey, Lora, Miller, Robert T, Morris, Michele, Murphy, Shawn N, Natarajan, Karthik, Palchuk, Matvey B, Sheikh, Usman, Solbrig, Harold, Visweswaran, Shyam, Walden, Anita, Walters, Kellie M, Weber, Griffin M, Zhang, Xiaohan Tanner, Zhu, Richard L, Amor, Benjamin, Girvin, Andrew T, Manna, Amin, Qureshi, Nabeel, Kurilla, Michael G, Michael, Sam G, Portilla, Lili M, Rutter, Joni L, Austin, Christopher P, Gersing, Ken R, and N3C Consortium

Abstract

ObjectiveCoronavirus disease 2019 (COVID-19) poses societal challenges that require expeditious data and knowledge sharing. Though organizational clinical data are abundant, these are largely inaccessible to outside researchers. Statistical, machine learning, and causal analyses are most successful with large-scale data beyond what is available in any given organization. Here, we introduce the National COVID Cohort Collaborative (N3C), an open science community focused on analyzing patient-level data from many centers.Materials and methodsThe Clinical and Translational Science Award Program and scientific community created N3C to overcome technical, regulatory, policy, and governance barriers to sharing and harmonizing individual-level clinical data. We developed solutions to extract, aggregate, and harmonize data across organizations and data models, and created a secure data enclave to enable efficient, transparent, and reproducible collaborative analytics.ResultsOrganized in inclusive workstreams, we created legal agreements and governance for organizations and researchers; data extraction scripts to identify and ingest positive, negative, and possible COVID-19 cases; a data quality assurance and harmonization pipeline to create a single harmonized dataset; population of the secure data enclave with data, machine learning, and statistical analytics tools; dissemination mechanisms; and a synthetic data pilot to democratize data access.ConclusionsThe N3C has demonstrated that a multisite collaborative learning health network can overcome barriers to rapidly build a scalable infrastructure incorporating multiorganizational clinical data for COVID-19 analytics. We expect this effort to save lives by enabling rapid collaboration among clinicians, researchers, and data scientists to identify treatments and specialized care and thereby reduce the immediate and long-term impacts of COVID-19.

Published

2021

6. An Open Natural Language Processing Development Framework for EHR-based Clinical Research: A case demonstration using the National COVID Cohort Collaborative (N3C)

Author

Liu, Sijia, Wen, Andrew, Wang, Liwei, He, Huan, Fu, Sunyang, Miller, Robert, Williams, Andrew, Harris, Daniel, Kavuluru, Ramakanth, Liu, Mei, Abu-el-rub, Noor, Schutte, Dalton, Zhang, Rui, Rouhizadeh, Masoud, Osborne, John D., He, Yongqun, Topaloglu, Umit, Hong, Stephanie S, Saltz, Joel H, Schaffter, Thomas, Pfaff, Emily, Chute, Christopher G., Duong, Tim, Haendel, Melissa A., Fuentes, Rafael, Szolovits, Peter, Xu, Hua, Liu, Hongfang, Collaborative, National COVID Cohort, Processing, Natural Language, Subgroup, Liu, Sijia, Wen, Andrew, Wang, Liwei, He, Huan, Fu, Sunyang, Miller, Robert, Williams, Andrew, Harris, Daniel, Kavuluru, Ramakanth, Liu, Mei, Abu-el-rub, Noor, Schutte, Dalton, Zhang, Rui, Rouhizadeh, Masoud, Osborne, John D., He, Yongqun, Topaloglu, Umit, Hong, Stephanie S, Saltz, Joel H, Schaffter, Thomas, Pfaff, Emily, Chute, Christopher G., Duong, Tim, Haendel, Melissa A., Fuentes, Rafael, Szolovits, Peter, Xu, Hua, Liu, Hongfang, Collaborative, National COVID Cohort, Processing, Natural Language, and Subgroup

Abstract

While we pay attention to the latest advances in clinical natural language processing (NLP), we can notice some resistance in the clinical and translational research community to adopt NLP models due to limited transparency, interpretability, and usability. In this study, we proposed an open natural language processing development framework. We evaluated it through the implementation of NLP algorithms for the National COVID Cohort Collaborative (N3C). Based on the interests in information extraction from COVID-19 related clinical notes, our work includes 1) an open data annotation process using COVID-19 signs and symptoms as the use case, 2) a community-driven ruleset composing platform, and 3) a synthetic text data generation workflow to generate texts for information extraction tasks without involving human subjects. The corpora were derived from texts from three different institutions (Mayo Clinic, University of Kentucky, University of Minnesota). The gold standard annotations were tested with a single institution's (Mayo) ruleset. This resulted in performances of 0.876, 0.706, and 0.694 in F-scores for Mayo, Minnesota, and Kentucky test datasets, respectively. The study as a consortium effort of the N3C NLP subgroup demonstrates the feasibility of creating a federated NLP algorithm development and benchmarking platform to enhance multi-institution clinical NLP study and adoption. Although we use COVID-19 as a use case in this effort, our framework is general enough to be applied to other domains of interest in clinical NLP., Comment: update on contents

Published

2021

7. Enabling Longitudinal Exploratory Analysis of Clinical COVID Data

Author

Borland, David, Brain, Irena, Fecho, Karamarie, Pfaff, Emily, Xu, Hao, Champion, James, Bizon, Chris, Gotz, David, Borland, David, Brain, Irena, Fecho, Karamarie, Pfaff, Emily, Xu, Hao, Champion, James, Bizon, Chris, and Gotz, David

Abstract

As the COVID-19 pandemic continues to impact the world, data is being gathered and analyzed to better understand the disease. Recognizing the potential for visual analytics technologies to support exploratory analysis and hypothesis generation from longitudinal clinical data, a team of collaborators worked to apply existing event sequence visual analytics technologies to a longitudinal clinical data from a cohort of 998 patients with high rates of COVID-19 infection. This paper describes the initial steps toward this goal, including: (1) the data transformation and processing work required to prepare the data for visual analysis, (2) initial findings and observations, and (3) qualitative feedback and lessons learned which highlight key features as well as limitations to address in future work., Comment: To Appear in Proceedings of Visual Analytics in Healthcare 2021

Published

2021

8. Electronic Medical Record Search Engine (EMERSE): An Information Retrieval Tool for Supporting Cancer Research.

Author

Hanauer, David A, Hanauer, David A, Barnholtz-Sloan, Jill S, Beno, Mark F, Del Fiol, Guilherme, Durbin, Eric B, Gologorskaya, Oksana, Harris, Daniel, Harnett, Brett, Kawamoto, Kensaku, May, Benjamin, Meeks, Eric, Pfaff, Emily, Weiss, Janie, Zheng, Kai, Hanauer, David A, Hanauer, David A, Barnholtz-Sloan, Jill S, Beno, Mark F, Del Fiol, Guilherme, Durbin, Eric B, Gologorskaya, Oksana, Harris, Daniel, Harnett, Brett, Kawamoto, Kensaku, May, Benjamin, Meeks, Eric, Pfaff, Emily, Weiss, Janie, and Zheng, Kai

Abstract

PurposeThe Electronic Medical Record Search Engine (EMERSE) is a software tool built to aid research spanning cohort discovery, population health, and data abstraction for clinical trials. EMERSE is now live at three academic medical centers, with additional sites currently working on implementation. In this report, we describe how EMERSE has been used to support cancer research based on a variety of metrics.MethodsWe identified peer-reviewed publications that used EMERSE through online searches as well as through direct e-mails to users based on audit logs. These logs were also used to summarize use at each of the three sites. Search terms for two of the sites were characterized using the natural language processing tool MetaMap to determine to which semantic types the terms could be mapped.ResultsWe identified a total of 326 peer-reviewed publications that used EMERSE through August 2019, although this is likely an underestimation of the true total based on the use log analysis. Oncology-related research comprised nearly one third (n = 105; 32.2%) of all research output. The use logs showed that EMERSE had been used by multiple people at each site (nearly 3,500 across all three) who had collectively logged into the system > 100,000 times. Many user-entered search queries could not be mapped to a semantic type, but the most common semantic type for terms that did match was "disease or syndrome," followed by "pharmacologic substance."ConclusionEMERSE has been shown to be a valuable tool for supporting cancer research. It has been successfully deployed at other sites, despite some implementation challenges unique to each deployment environment.

Published

2020

9. Electronic Medical Record Search Engine (EMERSE): An Information Retrieval Tool for Supporting Cancer Research.

Author

Hanauer, David A, Hanauer, David A, Barnholtz-Sloan, Jill S, Beno, Mark F, Del Fiol, Guilherme, Durbin, Eric B, Gologorskaya, Oksana, Harris, Daniel, Harnett, Brett, Kawamoto, Kensaku, May, Benjamin, Meeks, Eric, Pfaff, Emily, Weiss, Janie, Zheng, Kai, Hanauer, David A, Hanauer, David A, Barnholtz-Sloan, Jill S, Beno, Mark F, Del Fiol, Guilherme, Durbin, Eric B, Gologorskaya, Oksana, Harris, Daniel, Harnett, Brett, Kawamoto, Kensaku, May, Benjamin, Meeks, Eric, Pfaff, Emily, Weiss, Janie, and Zheng, Kai

Abstract

PurposeThe Electronic Medical Record Search Engine (EMERSE) is a software tool built to aid research spanning cohort discovery, population health, and data abstraction for clinical trials. EMERSE is now live at three academic medical centers, with additional sites currently working on implementation. In this report, we describe how EMERSE has been used to support cancer research based on a variety of metrics.MethodsWe identified peer-reviewed publications that used EMERSE through online searches as well as through direct e-mails to users based on audit logs. These logs were also used to summarize use at each of the three sites. Search terms for two of the sites were characterized using the natural language processing tool MetaMap to determine to which semantic types the terms could be mapped.ResultsWe identified a total of 326 peer-reviewed publications that used EMERSE through August 2019, although this is likely an underestimation of the true total based on the use log analysis. Oncology-related research comprised nearly one third (n = 105; 32.2%) of all research output. The use logs showed that EMERSE had been used by multiple people at each site (nearly 3,500 across all three) who had collectively logged into the system > 100,000 times. Many user-entered search queries could not be mapped to a semantic type, but the most common semantic type for terms that did match was "disease or syndrome," followed by "pharmacologic substance."ConclusionEMERSE has been shown to be a valuable tool for supporting cancer research. It has been successfully deployed at other sites, despite some implementation challenges unique to each deployment environment.

Published

2020

10. Semantic integration of clinical laboratory tests from electronic health records for deep phenotyping and biomarker discovery.

Author

Zhang, Xingmin Aaron, Zhang, Xingmin Aaron, Yates, Amy, Vasilevsky, Nicole, Gourdine, JP, Callahan, Tiffany J, Carmody, Leigh C, Danis, Daniel, Joachimiak, Marcin P, Ravanmehr, Vida, Pfaff, Emily R, Champion, James, Robasky, Kimberly, Xu, Hao, Fecho, Karamarie, Walton, Nephi A, Zhu, Richard L, Ramsdill, Justin, Mungall, Christopher J, Köhler, Sebastian, Haendel, Melissa A, McDonald, Clement J, Vreeman, Daniel J, Peden, David B, Bennett, Tellen D, Feinstein, James A, Martin, Blake, Stefanski, Adrianne L, Hunter, Lawrence E, Chute, Christopher G, Robinson, Peter N, Zhang, Xingmin Aaron, Zhang, Xingmin Aaron, Yates, Amy, Vasilevsky, Nicole, Gourdine, JP, Callahan, Tiffany J, Carmody, Leigh C, Danis, Daniel, Joachimiak, Marcin P, Ravanmehr, Vida, Pfaff, Emily R, Champion, James, Robasky, Kimberly, Xu, Hao, Fecho, Karamarie, Walton, Nephi A, Zhu, Richard L, Ramsdill, Justin, Mungall, Christopher J, Köhler, Sebastian, Haendel, Melissa A, McDonald, Clement J, Vreeman, Daniel J, Peden, David B, Bennett, Tellen D, Feinstein, James A, Martin, Blake, Stefanski, Adrianne L, Hunter, Lawrence E, Chute, Christopher G, and Robinson, Peter N

Abstract

Electronic Health Record (EHR) systems typically define laboratory test results using the Laboratory Observation Identifier Names and Codes (LOINC) and can transmit them using Fast Healthcare Interoperability Resource (FHIR) standards. LOINC has not yet been semantically integrated with computational resources for phenotype analysis. Here, we provide a method for mapping LOINC-encoded laboratory test results transmitted in FHIR standards to Human Phenotype Ontology (HPO) terms. We annotated the medical implications of 2923 commonly used laboratory tests with HPO terms. Using these annotations, our software assesses laboratory test results and converts each result into an HPO term. We validated our approach with EHR data from 15,681 patients with respiratory complaints and identified known biomarkers for asthma. Finally, we provide a freely available SMART on FHIR application that can be used within EHR systems. Our approach allows readily available laboratory tests in EHR to be reused for deep phenotyping and exploits the hierarchical structure of HPO to integrate distinct tests that have comparable medical interpretations for association studies.

Published

2019

11. Semantic integration of clinical laboratory tests from electronic health records for deep phenotyping and biomarker discovery.

Author

Zhang, Xingmin Aaron, Zhang, Xingmin Aaron, Yates, Amy, Vasilevsky, Nicole, Gourdine, JP, Callahan, Tiffany J, Carmody, Leigh C, Danis, Daniel, Joachimiak, Marcin P, Ravanmehr, Vida, Pfaff, Emily R, Champion, James, Robasky, Kimberly, Xu, Hao, Fecho, Karamarie, Walton, Nephi A, Zhu, Richard L, Ramsdill, Justin, Mungall, Christopher J, Köhler, Sebastian, Haendel, Melissa A, McDonald, Clement J, Vreeman, Daniel J, Peden, David B, Bennett, Tellen D, Feinstein, James A, Martin, Blake, Stefanski, Adrianne L, Hunter, Lawrence E, Chute, Christopher G, Robinson, Peter N, Zhang, Xingmin Aaron, Zhang, Xingmin Aaron, Yates, Amy, Vasilevsky, Nicole, Gourdine, JP, Callahan, Tiffany J, Carmody, Leigh C, Danis, Daniel, Joachimiak, Marcin P, Ravanmehr, Vida, Pfaff, Emily R, Champion, James, Robasky, Kimberly, Xu, Hao, Fecho, Karamarie, Walton, Nephi A, Zhu, Richard L, Ramsdill, Justin, Mungall, Christopher J, Köhler, Sebastian, Haendel, Melissa A, McDonald, Clement J, Vreeman, Daniel J, Peden, David B, Bennett, Tellen D, Feinstein, James A, Martin, Blake, Stefanski, Adrianne L, Hunter, Lawrence E, Chute, Christopher G, and Robinson, Peter N

Abstract

Electronic Health Record (EHR) systems typically define laboratory test results using the Laboratory Observation Identifier Names and Codes (LOINC) and can transmit them using Fast Healthcare Interoperability Resource (FHIR) standards. LOINC has not yet been semantically integrated with computational resources for phenotype analysis. Here, we provide a method for mapping LOINC-encoded laboratory test results transmitted in FHIR standards to Human Phenotype Ontology (HPO) terms. We annotated the medical implications of 2923 commonly used laboratory tests with HPO terms. Using these annotations, our software assesses laboratory test results and converts each result into an HPO term. We validated our approach with EHR data from 15,681 patients with respiratory complaints and identified known biomarkers for asthma. Finally, we provide a freely available SMART on FHIR application that can be used within EHR systems. Our approach allows readily available laboratory tests in EHR to be reused for deep phenotyping and exploits the hierarchical structure of HPO to integrate distinct tests that have comparable medical interpretations for association studies.

Published

2019