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Your search keyword '"Robertson, Holly"' showing total 7 results
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7 results on '"Robertson, Holly"'

1. Rationale and Design of the Aspirin Dosing—A Patient-Centric Trial Assessing Benefits and Long-term Effectiveness (ADAPTABLE) Trial

Author

Marquis-Gravel, Guillaume, Roe, Matthew T., Robertson, Holly R., Harrington, Robert A., Pencina, Michael J., Berdan, Lisa G., Hammill, Bradley G., Faulkner, Madelaine, Muñoz, Daniel, Fonarow, Gregg C., Nallamothu, Brahmajee K., Fintel, Dan J., Ford, Daniel E., Zhou, Li, Daugherty, Sarah E., Nauman, Elizabeth, Kraschnewski, Jennifer, Ahmad, Faraz S., Benziger, Catherine P., Haynes, Kevin, Merritt, J. Greg, Metkus, Thomas, Kripalani, Sunil, Gupta, Kamal, Shah, Raj C., McClay, James C., Re, Richard N., Geary, Carol, Lampert, Brent C., Bradley, Steven M., Jain, Sandeep K., Seifein, Hani, Whittle, Jeff, Roger, Véronique L., Effron, Mark B., Alvarado, Giselle, Goldberg, Ythan H., VanWormer, Jeffrey L., Girotra, Saket, Farrehi, Peter, McTigue, Kathleen M., Rothman, Russell, Hernandez, Adrian F., and Jones, W. Schuyler

Abstract

IMPORTANCE: Determining the right dosage of aspirin for the secondary prevention treatment of atherosclerotic cardiovascular disease (ASCVD) remains an unanswered and critical question. OBJECTIVE: To report the rationale and design for a randomized clinical trial to determine the optimal dosage of aspirin to be used for secondary prevention of ASCVD, using an innovative research method. DESIGN, SETTING, AND PARTICIPANTS: This pragmatic, open-label, patient-centered, randomized clinical trial is being conducted in 15 000 patients within the National Patient-Centered Clinical Research Network (PCORnet), a distributed research network of partners including clinical research networks, health plan research networks, and patient-powered research networks across the United States. Patients with established ASCVD treated in routine clinical practice within the network are eligible. Patient recruitment began in April 2016. Enrollment was completed in June 2019. Final follow-up is expected to be completed by June 2020. INTERVENTIONS: Participants are randomized on a web platform in a 1:1 fashion to either 81 mg or 325 mg of aspirin daily. MAIN OUTCOMES AND MEASURES: The primary efficacy end point is the composite of all-cause mortality, hospitalization for nonfatal myocardial infarction, or hospitalization for a nonfatal stroke. The primary safety end point is hospitalization for major bleeding associated with a blood-product transfusion. End points are captured through regular queries of the health systems’ common data model within the structure of PCORnet’s distributed data environment. CONCLUSIONS AND RELEVANCE: As a pragmatic study and the first interventional trial conducted within the PCORnet electronic data infrastructure, this trial is testing several unique and innovative operational approaches that have the potential to disrupt and transform the conduct of future patient-centered randomized clinical trials by evaluating treatments integrated in clinical practice while at the same time determining the optimal dosage of aspirin for secondary prevention of ASCVD. TRIAL REGISTRATION: ClinicalTrials.gov Identifier: NCT02697916

Published
2020
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2. Validation of a claims-based algorithm identifying eligible study subjects in the ADAPTABLE pragmatic clinical trial

Author

Fishman, Ezra, Barron, John, Dinh, Jade, Jones, W. Schuyler, Marshall, Amanda, Merkh, Rebecca, Robertson, Holly, and Haynes, Kevin

Abstract

Validate an algorithm that uses administrative claims data to identify eligible study subjects for the ADAPTABLE (Aspirin Dosing: A Patient-centric Trial Assessing Benefits and Long-Term Effectiveness) pragmatic clinical trial (PCT).

Published
2018
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3. Striatal Magnetic Resonance Spectroscopy Abnormalities in Young Adult Sapap3Knockout Mice

Author

Mintzopoulos, Dionyssios, Gillis, Timothy E., Robertson, Holly R., Dalia, Triana, Feng, Guoping, Rauch, Scott L., and Kaufman, Marc J.

Abstract

Obsessive-compulsive disorder (OCD) is a debilitating condition with lifetime prevalence of 1% to 3%. OCD typically arises in youth, but delays in diagnosis impede optimal treatment and developmental studies of the disorder. Research using genetically modified rodents may provide models of etiology that enable earlier detection and intervention. The Sapap3knockout (KO) transgenic mouse was developed as an animal model of obsessive-compulsive and related disorders. KO mice exhibit compulsive self-grooming behavior analogous to behaviors found in people with obsessive-compulsive and related disorders. Striatal hyperactivity has been reported in these mice and in humans with OCD.

Published
2016
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4. Validation of Cardiovascular End Points Ascertainment Leveraging Multisource Electronic Health Records Harmonized Into a Common Data Model in the ADAPTABLE Randomized Clinical Trial.

Author

Marquis-Gravel, Guillaume, Hammill, Bradley G. DrPH, Mulder, Hillary MS, Roe, Matthew T. MHS, Robertson, Holly R., Wruck, Lisa M., Sharlow, Amber CCRA, Harris, Debra F. BA, Pohlman, F. Will, Hernandez, Adrian F. MHS, Jones, W. Schuyler, Hammill, Bradley G, Mulder, Hillary, Roe, Matthew T, Sharlow, Amber, Harris, Debra F, and Hernandez, Adrian F

Subjects
MYOCARDIAL infarction treatment, STROKE treatment, MYOCARDIAL infarction diagnosis, STROKE diagnosis, HEMORRHAGE diagnosis, RESEARCH, STROKE, RESEARCH methodology, MYOCARDIAL infarction, EVALUATION research, COMPARATIVE studies, RANDOMIZED controlled trials, ASPIRIN, PLATELET aggregation inhibitors, HEMORRHAGE
Abstract

Background: The ADAPTABLE trial (Aspirin Dosing: A Patient-Centric Trial Assessing Benefits and Long-Term Effectiveness) is the first randomized trial conducted within the National Patient-Centered Clinical Research Network to use the electronic health record data formatted into a common data model as the primary source of end point ascertainment, without confirmation by standard adjudication. The objective of this prespecified study is to assess the validity of nonfatal end points captured from the National Patient-Centered Clinical Research Network, using traditional blinded adjudication as the gold standard.Methods: A total of 15 076 participants with established atherosclerotic cardiovascular disease were randomized to two doses of aspirin (81 mg and 325 mg once daily). Nonfatal end points (hospitalization for nonfatal myocardial infarction, nonfatal stroke, and major bleeding requiring transfusion of blood products) were captured with the use of programming algorithms applied to National Patient-Centered Clinical Research Network data. A random subset of end points was independently reviewed by a disease-specific expert adjudicator. The positive predictive value of the programming algorithms were calculated separately for end points listed as primary and as nonprimary diagnoses.Results: A total of 225 end points were identified (91 myocardial infarction events, 89 stroke events, and 45 bleeding events), including 142 (63%) that were listed as primary diagnoses. Complete source documents were missing for 14% of events. The positive predictive value were 90%, 72%, and 93% for hospitalizations for myocardial infarction, stroke, and major bleeding, respectively, as compared to adjudication. When only primary diagnoses were considered, positive predictive value were 93%, 91%, and 97%, respectively. When only nonprimary diagnoses were considered, positive predictive value were 82%, 36%, and 71%.Conclusions: As compared with blinded adjudication, clinical end point ascertainment from queries of the National Patient-Centered Clinical Research Network distributed harmonized data was valid to identify hospitalizations for myocardial infarction in ADAPTABLE. The proportion of contradicted events was high for hospitalizations for bleeding and strokes when nonprimary diagnoses were analyzed, but not when only primary diagnoses were considered. [ABSTRACT FROM AUTHOR]

Published
2021
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5. Computable Phenotype Implementation for a National, Multicenter Pragmatic Clinical Trial: Lessons Learned From ADAPTABLE.

Author

Ahmad, Faraz S., Ricket, Iben M., Hammill, Bradley G., Eskenazi, Lisa, Robertson, Holly R., Curtis, Lesley H., Dobi, Cecilia D., Girotra, Saket, Haynes, Kevin, Kizer, Jorge R., Kripalani, Sunil, Roe, Mathew T., Roumie, Christianne L., Waitman, Russ, Jones, W. Schuyler, and Weiner, Mark G.

Subjects
CARDIOVASCULAR disease diagnosis, RESEARCH, PATIENT selection, CARDIOVASCULAR diseases, MEDICAL cooperation, RANDOMIZED controlled trials, ASPIRIN, PLATELET aggregation inhibitors, ALGORITHMS, PHENOTYPES, DATA mining
Abstract

Background: Many large-scale cardiovascular clinical trials are plagued with escalating costs and low enrollment. Implementing a computable phenotype, which is a set of executable algorithms, to identify a group of clinical characteristics derivable from electronic health records or administrative claims records, is essential to successful recruitment in large-scale pragmatic clinical trials. This methods paper provides an overview of the development and implementation of a computable phenotype in ADAPTABLE (Aspirin Dosing: a Patient-Centric Trial Assessing Benefits and Long-Term Effectiveness)-a pragmatic, randomized, open-label clinical trial testing the optimal dose of aspirin for secondary prevention of atherosclerotic cardiovascular disease events.Methods and Results: A multidisciplinary team developed and tested the computable phenotype to identify adults ≥18 years of age with a history of atherosclerotic cardiovascular disease without safety concerns around using aspirin and meeting trial eligibility criteria. Using the computable phenotype, investigators identified over 650 000 potentially eligible patients from the 40 participating sites from Patient-Centered Outcomes Research Network-a network of Clinical Data Research Networks, Patient-Powered Research Networks, and Health Plan Research Networks. Leveraging diverse recruitment methods, sites enrolled 15 076 participants from April 2016 to June 2019. During the process of developing and implementing the ADAPTABLE computable phenotype, several key lessons were learned. The accuracy and utility of a computable phenotype are dependent on the quality of the source data, which can be variable even with a common data model. Local validation and modification were required based on site factors, such as recruitment strategies, data quality, and local coding patterns. Sustained collaboration among a diverse team of researchers is needed during computable phenotype development and implementation.Conclusions: The ADAPTABLE computable phenotype served as an efficient method to recruit patients in a multisite pragmatic clinical trial. This process of development and implementation will be informative for future large-scale, pragmatic clinical trials. Registration: URL: https://www.clinicaltrials.gov; Unique identifier: NCT02697916. [ABSTRACT FROM AUTHOR]

Published
2020
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