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5. Estimated COVID-19 vaccine effectiveness against seroconversion from SARS-CoV-2 Infection, March–October, 2021

Author

Plumb, Ian D., Fette, Lida M., Tjaden, Ashley H., Feldstein, Leora, Saydah, Sharon, Ahmed, Amina, Link-Gelles, Ruth, Wierzba, Thomas F., Berry, Andrea A., Friedman-Klabanoff, DeAnna, Larsen, Moira P., Runyon, Michael S., Ward, Lori M., Santos, Roberto P., Ward, Johnathan, Weintraub, William S., Edelstein, Sharon, and Uschner, Diane

Published
2023
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7. Using Randomization Tests to Address Disruptions in Clinical Trials: A Report from the NISS Ingram Olkin Forum Series on Unplanned Clinical Trial Disruptions.

Author

Uschner, Diane, Sverdlov, Oleksandr, Carter, Kerstine, Chipman, Jonathan, Kuznetsova, Olga, Renteria, Jone, Lane, Adam, Barker, Chris, Geller, Nancy, Proschan, Michael, Posch, Martin, Tarima, Sergey, Bretz, Frank, and Rosenberger, William F.

Subjects
*COVID-19 pandemic, *RUSSIAN invasion of Ukraine, 2022-, *EXPERIMENTAL design, *CLINICAL trials, *SENSITIVITY analysis
Abstract

Recent examples for unplanned external events are the global COVID-19 pandemic, the war in Ukraine, or most recently Hurricane Ian in Puerto Rico. Disruptions due to unplanned external events can lead to violation of assumptions in clinical trials. In certain situations, randomization tests can provide nonparametric inference that is robust to violation of the assumptions usually made in clinical trials. The ICH E9 (R1) Addendum on estimands and sensitivity analyses provides a guideline for aligning the trial objectives with strategies to address disruptions in clinical trials. In this article, we embed randomization tests within the estimand framework to allow for inference following disruptions in clinical trials in a way that reflects recent literature. A stylized clinical trial is presented to illustrate the method, and a simulation study highlights situations when a randomization test that is conducted under the intention-to-treat principle can provide unbiased results. [ABSTRACT FROM AUTHOR]

Published
2024
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9. Rejoinder.

Author

Uschner, Diane, Sverdlov, Oleksandr, Carter, Kerstine, Chipman, Jonathan J., Kuznetsova, Olga, Renteria, Jone, Lane, Adam, Barker, Chris, Geller, Nancy L., Proschan, Michael, Posch, Martin, Tarima, Sergey, Bretz, Frank, and Rosenberger, William F.

Subjects
*PATIENT selection, *COVID-19 pandemic, *CONVENIENCE sampling (Statistics), *STATISTICS, *INVESTIGATIONAL therapies, *RANDOMIZATION (Statistics)
Abstract

The article "Rejoinder" responds to comments on the manuscript "Using Randomization Tests to Address Disruptions in Clinical Trials." It highlights the importance of randomization tests in providing valid inference during disruptions, especially in the context of the COVID-19 pandemic. The article discusses the estimand framework and the challenges of generalizability in clinical trials, emphasizing the need for expert knowledge and external sources of information. Randomization tests are presented as a simple and valuable tool for statisticians in the medical and pharmaceutical fields. [Extracted from the article]

Published
2024
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11. Emotional Distress Predicts Reduced Type 2 Diabetes Treatment Adherence in the Glycemia Reduction Approaches in Diabetes: A Comparative Effectiveness Study (GRADE).

Author

Hoogendoorn, Claire J., Krause-Steinrauf, Heidi, Uschner, Diane, Wen, Hui, Presley, Caroline A., Legowski, Elizabeth A., Naik, Aanand D., Golden, Sherita Hill, Arends, Valerie L., Brown-Friday, Janet, Krakoff, Jonathan A., Suratt, Colleen E., Waltje, Andrea H., Cherrington, Andrea L., Gonzalez, Jeffrey S., Crandall, J.P., McKee, M.D., Behringer-Massera, S., Brown-Friday, J., and Xhori, E.

Subjects
TYPE 2 diabetes, PSYCHOLOGICAL distress, PATIENT compliance, COMPARATIVE method, ETHNIC differences, PATIENT satisfaction
Abstract

OBJECTIVE: We examined longitudinal associations between emotional distress (specifically, depressive symptoms and diabetes distress) and medication adherence in Glycemia Reduction Approaches in Diabetes: A Comparative Effectiveness Study (GRADE), a large randomized controlled trial comparing four glucose-lowering medications added to metformin in adults with relatively recent-onset type 2 diabetes mellitus (T2DM). RESEARCH DESIGN AND METHODS: The Emotional Distress Substudy assessed medication adherence, depressive symptoms, and diabetes distress in 1,739 GRADE participants via self-completed questionnaires administered biannually up to 3 years. We examined baseline depressive symptoms and diabetes distress as predictors of medication adherence over 36 months. Bidirectional visit-to-visit relationships were also examined. Treatment satisfaction, beliefs about medication, diabetes care self-efficacy, and perceived control over diabetes were evaluated as mediators of longitudinal associations. RESULTS: At baseline, mean ± SD age of participants (56% of whom were White, 17% Hispanic/Latino, 18% Black, and 66% male) was 58.0 ± 10.2 years, diabetes duration 4.2 ± 2.8 years, HbA1c 7.5% ± 0.5%, and medication adherence 89.9% ± 11.1%. Higher baseline depressive symptoms and diabetes distress were independently associated with lower adherence over 36 months (P < 0.001). Higher depressive symptoms and diabetes distress at one visit predicted lower adherence at the subsequent 6-month visit (P < 0.0001) but not vice versa. Treatment assignment did not moderate relationships. Patient-reported concerns about diabetes medications mediated the largest percentage (11.9%–15.5%) of the longitudinal link between emotional distress and adherence. CONCLUSIONS: Depressive symptoms and diabetes distress both predict lower adherence to glucose-lowering medications over time among adults with T2DM. Addressing emotional distress and concerns about anticipated negative effects of taking these treatments may be important to support diabetes treatment adherence. [ABSTRACT FROM AUTHOR]

Published
2024
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13. Residual [beta] cell function in long-term type 1 diabetes associates with reduced incidence of hypoglycemia

Author

Gubitosi-Klug, Rose A., Braffett, Barbara H., Hitt, Susan, Arends, Valerie, Uschner, Diane, Jones, Kimberly, Diminick, Lisa, Karger, Amy B., Paterson, Andrew D., Roshandel, Delnaz, Marcovina, Santica, Lachin, John M., Steffes, Michael, and Palmer, Jerry P.

Subjects
Polypeptides -- Measurement -- Health aspects, Type 1 diabetes -- Complications and side effects -- Physiological aspects, Pancreatic beta cells -- Physiological aspects -- Health aspects, Hypoglycemia -- Risk factors -- Prevention, Health care industry
Abstract

BACKGROUND. We investigated residual [beta] cell function in Diabetes Control and Complications Trial/Epidemiology of Diabetes Interventions and Complications (DCCT/EDIC) study participants with an average 35-year duration of type 1 diabetes mellitus (T1DM). METHODS. Serum C-peptide was measured during a 4-hour mixed-meal tolerance test. Associations with metabolic outcomes and complications were explored among nonresponders (all C-peptide values after meal 0.2), intermediate (>0.03 to RESULTS. Of the 944 participants, 117 (12.4%) were classified as responders. Residual C-peptide concentrations were associated with higher DCCT baseline concentrations of stimulated C-peptide (P value for trend = 0.0001). Residual C- peptide secretion was not associated with current or mean HbA1c, HLA high-risk haplotypes for T1DM, or the current presence of T1DM autoantibodies. The proportion of subjects with a history of severe hypoglycemia was lower with high (27%) and intermediate (48%) residual C-peptide concentrations than with low (74%) and no (70%) residual C-peptide concentrations (P value for trend = 0.0001). Responders and nonresponders demonstrated similar rates of advanced microvascular complications. CONCLUSION. [beta] Cell function can persist in long-duration T1DM. With a peak C-peptide concentration of >0.03 nmol/L, we observed clinically meaningful reductions in the prevalence of severe hypoglycemia. TRIAL REGISTRATION. ClinicalTrials.gov NCT00360815 and NCT00360893. FUNDING. Division of Diabetes Endocrinology and Metabolic Diseases of the National Institute of Diabetes and Digestive and Kidney Diseases (DP3-DK104438, U01 DK094176, and U01 DK094157)., Introduction Insulin secretion declines in most individuals with type 1 diabetes mellitus (T1DM) as duration of diabetes increases, yet residual insulin secretion, as detected by circulating C-peptide after a meal [...]

Published
2021
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15. Association of Obesity and Diabetes With SARS-CoV-2 Infection and Symptoms in the COVID-19 Community Research Partnership.

Author

Mongraw-Chaffin, Morgana, Tjaden, Ashley Hogan, Seals, Austin Lyles, Miller, Kristen, Ahmed, Naheed, Espeland, Mark A., Gibbs, Michael, Thomas, Dorey, Uschner, Diane, Weintraub, William S., and Edelstein, Sharon L.

Abstract

Context: Obesity and diabetes are established risk factors for severe SARS-CoV-2 outcomes, but less is known about their impact on susceptibility to COVID-19 infection and general symptom severity. Objective: We hypothesized that those with obesity or diabetes would be more likely to self-report a positive SARS-CoV-2 test, and, among those with a positive test, have greater symptom severity and duration. Methods: Among 44 430 COVID-19 Community Research Partnership participants, we evaluated the association of self-reported and electronic health record obesity and diabetes with a self-reported positive COVID-19 test at any time. Among the 2663 participants with a self-reported positive COVID-19 test during the study, we evaluated the association of obesity and diabetes with self-report of symptom severity, duration, and hospitalization. Logistic regression models were adjusted for age, sex, race/ethnicity, socioeconomic status, and health care worker status. Results: We found a positive graded association between body mass index (BMI) category and positive COVID-19 test (overweight odds ratio [OR] 1.14 [1.05-1.25]; obesity I OR 1.29 [1.17-2.42]; obesity II OR 1.34 [1.19-1.50]; obesity III OR 1.53 [1.35-1.73]), and a similar but weaker association with COVID-19 symptoms and severity among those with a positive test. Diabetes was associated with COVID-19 infection but not symptoms after adjustment, with some evidence of an interaction between obesity and diabetes. Conclusion: While the limitations of this health system convenience sample include generalizability and selection around test seeking, the strong graded association of BMI and diabetes with self-reported COVID-19 infection suggests that obesity and diabetes may play a role in risk for symptomatic SARS-CoV-2 beyond co-occurrence with socioeconomic factors. [ABSTRACT FROM AUTHOR]

Published
2023
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16. Psychosocial factors predict medication adherence in young adults with youth‐onset type 2 diabetes: Longitudinal results from the TODAY2 iCount study.

Author

Trief, Paula M., Uschner, Diane, Kalichman, Seth, Anderson, Barbara J., Fette, Lida M., Wen, Hui, Bulger, Jane D., and Weinstock, Ruth S.

Subjects
*CLINICAL drug trials, *INSULIN therapy, *DRUG addiction, *THERAPEUTICS, *SUBSTANCE abuse, *ORAL drug administration, *SELF-evaluation, *ATTITUDE (Psychology), *HYPOGLYCEMIC agents, *REGRESSION analysis, *HOUSING stability, *RACE, *TYPE 2 diabetes, *PATIENTS' attitudes, *AGE factors in disease, *PSYCHOSOCIAL factors, *DESCRIPTIVE statistics, *HEALTH attitudes, *RESEARCH funding, *PATIENT compliance, *LOGISTIC regression analysis, *PEOPLE with diabetes, *LONGITUDINAL method, *ADULTS
Abstract

Aim: To identify psychosocial predictors of medication adherence in young adults with youth‐onset type 2 diabetes in the Treatment Options for type 2 Diabetes in Adolescents and Youth (TODAY2) cohort. Methods: Participants (mean age: 26 years) completed validated psychosocial measures. Unannounced telephone pill counts were completed at T1 (baseline) and T2 (follow‐up, approximately 1 year later) to assess adherence to oral hypoglycaemia agents (OHAs). Adherence to insulin was assessed by self‐report. Logistic and linear regressions identified factors that predicted 'low adherence' (<80% of pills/insulin) and per cent adherence, adjusted for potential confounders. Results: Of 171 participants with OHA adherence scores at T1 and T2 (65% women, 43% Hispanic and 35% non‐Hispanic Black), 65.4% were low adherent. After adjustment (including T1 adherence), concerns about diabetes medicines (adverse effects, dependence) at T1 predicted higher odds of being low adherent (categorical) at T2 (p = 0.019). Housing insecurity (p = 0.045) and reporting ≥2 need insecurities (p = 0.027) at T1 predicted lower per cent adherence (continuous) at T2. Of 157 participants with insulin adherence scores at T1 and T2 (69% women, 38% Hispanic and 38% non‐Hispanic Black), 36.3% were low adherent. After adjustment (including T1 adherence), beliefs that medicines are overused predicted higher odds of insulin low adherence at T2 (p = 0.013), and beliefs that medicines are harmful (p = 0.004) and overused (p = 0.010) predicted lower per cent insulin adherence at T2. Conclusions: Suboptimal medication adherence, common in young adults with youth‐onset type 2 diabetes, is predicted by interfering beliefs about medicines and social factors. We must address these beliefs and unmet needs to develop tailored interventions for this vulnerable group. [ABSTRACT FROM AUTHOR]

Published
2023
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17. Characterisation of infection-induced SARS-CoV-2 seroprevalence amongst children and adolescents in North Carolina.

Author

Ahmed, Amina, DeWitt, Michael E., Dantuluri, Keerti L., Castri, Paola, Buahin, Asare, LaGarde, William H., Weintraub, William S., Rossman, Whitney, Santos, Roberto P., Gibbs, Michael, and Uschner, Diane

Abstract

Few prospective studies have documented the seropositivity among those children infected with severe acute respiratory syndrome coronavirus 2. From 2 April 2021 to 24 June 2021, we prospectively enrolled children between the ages of 2 and 17 years at three North Carolina healthcare systems. Participants received at least four at-home serological tests detecting the presence of antibodies against, but not differentiating between, the nucleocapsid or spike antigen. A total of 1,058 participants were enrolled in the study, completing 2,709 tests between 1 May 2021 and 31 October 2021. Using multilevel regression with poststratification techniques and considering our assay sensitivity and sensitivity, we estimated that the seroprevalence of infection-induced antibodies among unvaccinated children and adolescents aged 2–17 years in North Carolina increased from 15.2% (95% credible interval, CrI 9.0–22.0) in May 2021 to 54.1% (95% CrI 46.7–61.1) by October 2021, indicating an average infection-to-reported-case ratio of 5. A rapid rise in seropositivity was most pronounced in those unvaccinated children aged 12–17 years, based on our estimates. This study underlines the utility of serial, serological testing to inform a broader understanding of the regional immune landscape and spread of infection. [ABSTRACT FROM AUTHOR]

Published
2023
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18. Association of psychosocial factors with medication adherence in emerging adults with youth‐onset type 2 diabetes: The iCount study.

Author

Trief, Paula M., Kalichman, Seth, Uschner, Diane, Tung, Melinda, Drews, Kimberly L., Anderson, Barbara J., Fette, Lida M., Wen, Hui, Bulger, Jane D., and Weinstock, Ruth S.

Subjects
SOCIAL determinants of health, SELF-management (Psychology), FOOD security, HYPOGLYCEMIC agents, REGRESSION analysis, TYPE 2 diabetes, PSYCHOSOCIAL factors, DRUGS, PATIENT compliance, LOGISTIC regression analysis, ODDS ratio, PEOPLE with diabetes, INSURANCE, PSYCHOLOGICAL distress
Abstract

Aims: To assess associations of psychosocial factors with medication adherence in young adults with youth‐onset type 2 diabetes in the Treatment Options for type 2 Diabetes in Adolescents and Youth (TODAY2) cohort. Methods: Participants (mean age 26 years) completed validated psychosocial measures. Adherence to oral hypoglycemia agents (OHAs) was assessed with 3‐monthly unannounced phone pill counts; insulin adherence by self‐report. Logistic and linear regressions identified factors associated with "low‐adherence" (<80% of pills/insulin) controlling for confounders. Results: Of 212 participants taking OHAs (67% female, 39% Hispanic, 36% non‐Hispanic Black), 69.8% were low‐adherent. After adjustment, beliefs that medicines are necessary was associated with lower odds of low‐adherence (p = 0.040, dichotomous). Less self‐management support (p = 0.008), no healthcare coverage (p = 0.001), ≥1 (p = 0.008)/≥2 (p = 0.045) need insecurities were associated with higher odds of low‐adherence. Factors associated with lower % adherence (continuous) were beliefs that medicines are harmful (p < 0.001)/overused (p = 0.007)/less necessary (p = 0.022), low self‐management support (p = 0.003), food insecurity (p = 0.036), no healthcare coverage (p < 0.001), ≥1 (p = 0.003)/≥2 (p = 0.018) need insecurities. Of 192 taking insulin (69% female, 36% Hispanic, 41% non‐Hispanic Black, 16% non‐Hispanic white), 37.0% were low‐adherent. Beliefs that medicines are overused (p = 0.009), that diabetes is not serious (p = 0.010), low diabetes self‐efficacy (p = 0.035), high distress (p = 0.027), low self‐management support (p = 0.001), food insecurity (p = 0.020), ≥1 (p = 0.011)/≥2 (p = 0.015) insecurities increased odds of insulin low‐adherence. Conclusion s : Poor medication adherence, common in young adults with youth‐onset type 2 diabetes, is associated with interfering beliefs, diabetes distress and social factors. We must address these factors to develop tailored interventions for this vulnerable group. [ABSTRACT FROM AUTHOR]

Published
2022
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19. Self-Reported SARS-CoV-2 Vaccination Is Consistent with Electronic Health Record Data among the COVID-19 Community Research Partnership.

Author

Tjaden, Ashley H., Fette, Lida M., Edelstein, Sharon L., Gibbs, Michael, Hinkelman, Amy N., Runyon, Michael, Santos, Roberto P., Weintraub, William S., Yukich, Joshua, and Uschner, Diane

Subjects
ELECTRONIC health records, VACCINATION, VACCINE effectiveness, SCIENTIFIC community, DATA recorders & recording
Abstract

Introduction: Observational studies of SARS-CoV-2 vaccine effectiveness depend on accurate ascertainment of vaccination receipt, date, and product type. Self-reported vaccine data may be more readily available to and less expensive for researchers than assessing medical records. Methods: We surveyed adult participants in the COVID-19 Community Research Partnership who had an authenticated Electronic Health Record (EHR) (N = 41,484) concerning receipt of SARS-CoV-2 vaccination using a daily survey beginning in December 2020 and a supplemental survey in September–October 2021. We compared self-reported information to that available in the EHR for the following data points: vaccine brand, date of first dose, and number of doses using rates of agreement and Bland–Altman plots for visual assessment. Self-reported data was available immediately following vaccination (in the daily survey) and at a delayed interval (in a secondary supplemental survey). Results: For the date of first vaccine dose, self-reported "immediate" recall was within ±7 days of the date reported in the "delayed" survey for 87.9% of participants. Among the 19.6% of participants with evidence of vaccination in their EHR, 95% self-reported vaccination in one of the two surveys. Self-reported dates were within ±7 days of documented EHR vaccination for 97.6% of the "immediate" surveys and 92.0% of the "delayed" surveys. Self-reported vaccine product details matched those in the EHR for over 98% of participants for both "immediate" and "delayed" surveys. Conclusions: Self-reported dates and product details for COVID-19 vaccination can be a good surrogate when medical records are unavailable in large observational studies. A secondary confirmation of dates for a subset of participants with EHR data will provide internal validity. [ABSTRACT FROM AUTHOR]

Published
2022
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20. Analysis of accumulated SARS-CoV-2 seroconversion in North Carolina: The COVID-19 Community Research Partnership.

Author

Williamson, John C., Wierzba, Thomas F., Santacatterina, Michele, Munawar, Iqra, Seals, Austin L., Pittman Ballard, Christine Ann, Alexander-Miller, Martha, Runyon, Michael S., McCurdy, Lewis H., Gibbs, Michael A., Ahmed, Amina, Lagarde, William H., Maguire, Patrick D., King-Thiele, Robin, Hamrick, Terri, Ihmeidan, Abdalla, Henderson, Shakira, Gallaher, T. Ryan, Uschner, Diane, and Edelstein, Sharon L.

Subjects
MEDICAL personnel, SEROCONVERSION, SCIENTIFIC community, SARS-CoV-2, PROPORTIONAL hazards models, COVID-19, IMMUNOGLOBULIN M, IMMUNOGLOBULIN G
Abstract

Introduction: The COVID-19 Community Research Partnership is a population-based longitudinal syndromic and sero-surveillance study. The study includes over 17,000 participants from six healthcare systems in North Carolina who submitted over 49,000 serology results. The purpose of this study is to use these serology data to estimate the cumulative proportion of the North Carolina population that has either been infected with SARS-CoV-2 or developed a measurable humoral response to vaccination. Methods: Adult community residents were invited to participate in the study between April 2020 and February 2021. Demographic information was collected and daily symptom screen was completed using a secure, HIPAA-compliant, online portal. A portion of participants were mailed kits containing a lateral flow assay to be used in-home to test for presence of anti-SARS-CoV-2 IgM or IgG antibodies. The cumulative proportion of participants who tested positive at least once during the study was estimated. A standard Cox proportional hazards model was constructed to illustrate the probability of seroconversion over time up to December 20, 2020 (before vaccines available). A separate analysis was performed to describe the influence of vaccines through February 15, 2021. Results: 17,688 participants contributed at least one serology result. 68.7% of the population were female, and 72.2% were between 18 and 59 years of age. The average number of serology results submitted per participant was 3.0 (±1.9). By December 20, 2020, the overall probability of seropositivity in the CCRP population was 32.6%. By February 15, 2021 the probability among healthcare workers and non-healthcare workers was 83% and 49%, respectively. An inflection upward in the probability of seropositivity was demonstrated around the end of December, suggesting an influence of vaccinations, especially for healthcare workers. Among healthcare workers, those in the oldest age category (60+ years) were 38% less likely to have seroconverted by February 15, 2021. Conclusions: Results of this study suggest more North Carolina residents may have been infected with SARS-CoV-2 than the number of documented cases as determined by positive RNA or antigen tests. The influence of vaccinations on seropositivity among North Carolina residents is also demonstrated. Additional research is needed to fully characterize the impact of seropositivity on immunity and the ultimate course of the pandemic. [ABSTRACT FROM AUTHOR]

Published
2022
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21. Diabetes Distress in Young Adults With Youth-Onset Type 2 Diabetes: TODAY2 Study Results.

Author

Trief, Paula M., Uschner, Diane, Tung, Melinda, Marcus, Marsha D., Rayas, Maria, MacLeish, Sarah, Farrell, Ryan, Keady, Joyce, Chao, Lily, and Weinstock, Ruth S.

Subjects
*TYPE 2 diabetes, *YOUNG adults, *PSYCHOLOGICAL distress, *DIABETES, *INSULIN therapy, *MENTAL depression, *INSULIN, *RESEARCH funding, *EMOTIONS, *ANXIETY, *LONGITUDINAL method, *DISEASE complications
Abstract

Objective: To assess the prevalence of high diabetes distress and associated factors in the Treatment Options for Type 2 Diabetes in Adolescents and Youth (TODAY2) study cohort of young adults with youth-onset type 2 diabetes.Research Design and Methods: Participants completed the Diabetes Distress Scale (DDS) at end-of-study visits. Factors examined for association with high distress were demographic (sex, race/ethnicity, age, education, income), medical (HbA1c, BMI, complications), psychological (depressive and anxiety symptoms), and social (number in household, offspring, health care coverage, established with diabetes care provider). Univariate logistic regression identified factors associated with high distress that were controlled for in multivariate logistic regressions.Results: Of 438 participants, 66% were female (mean age 26.8 years, 18% non-Hispanic White, 37% non-Hispanic Black, 38% Hispanic). High distress (DDS ≥2) was reported by 105 (24%) participants. Subscales identified 40% with high regimen distress and 29.7% with high emotional burden. A greater percentage of those with high distress were female (P = 0.002), diagnosed with hypertension (P = 0.037) and retinopathy (P = 0.005), treated with insulin, had higher HbA1c, and had moderate to severe depressive and anxiety symptoms (all P < 0.001). In multivariate analyses, female sex (P < 0.001), HbA1c (P < 0.001), anxiety symptoms (P = 0.036), and lack of health care coverage (P = 0.019) were associated with high distress, after controlling for potential confounders. Moderate to severe depressive symptoms were associated with high regimen distress (P = 0.018) and emotional burden (P < 0.001); insulin treatment was associated with high emotional burden (P = 0.027).Conclusions: Future research should identify modifiable factors associated with high diabetes distress in young adults with youth-onset type 2 diabetes that may inform distress interventions with this medically vulnerable group. [ABSTRACT FROM AUTHOR]

Published
2022
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22. Duration of SARS-CoV-2 sero-positivity in a large longitudinal sero-surveillance cohort: the COVID-19 Community Research Partnership.

Author

The COVID-19 Community Research Partnership Study Group, Herrington, David M., Sanders, John W., Wierzba, Thomas F., Alexander-Miller, Martha, Espeland, Mark, Bertoni, Alain G., Mathews, Allison, Seals, Austin L., Munawar, Iqra, Runyon, Michael S., McCurdy, Lewis H., Gibbs, Michael A., Kotloff, Karen, Friedman-Klabanoff, DeAnna, Weintraub, William, Correa, Adolfo, Uschner, Diane, Edelstein, Sharon, and Santacatterina, Michele

Subjects
COVID-19, SARS-CoV-2, MEDICAL personnel, COVID-19 pandemic, SCIENTIFIC community, INFECTION
Abstract

Background: Estimating population prevalence and incidence of prior SARS-CoV-2 infection is essential to formulate public health recommendations concerning the COVID-19 pandemic. However, interpreting estimates based on sero-surveillance requires an understanding of the duration of elevated antibodies following SARS-CoV-2 infection, especially in the large number of people with pauci-symptomatic or asymptomatic disease.Methods: We examined > 30,000 serology assays for SARS-CoV-2 specific IgG and IgM assays acquired longitudinally in 11,468 adults between April and November 2020 in the COVID-19 Community Research Partnership.Results: Among participants with serologic evidence for infection but few or no symptoms or clinical disease, roughly 50% sero-reverted in 30 days of their initial positive test. Sero-reversion occurred more quickly for IgM than IgG and for antibodies targeting nucleocapsid protein compared with spike proteins, but was not associated with age, sex, race/ethnicity, or healthcare worker status.Conclusions: The short duration of antibody response suggests that the true population prevalence of prior SARS-CoV-2 infection may be significantly higher than presumed based on earlier sero-surveillance studies. The impact of the large number of minimally symptomatic COVID-19 cases with only a brief antibody response on population immunity remains to be determined. [ABSTRACT FROM AUTHOR]

Published
2021
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23. A roadmap to using randomization in clinical trials.

Author

Berger, Vance W., Bour, Louis Joseph, Carter, Kerstine, Chipman, Jonathan J., Everett, Colin C., Heussen, Nicole, Hewitt, Catherine, Hilgers, Ralf-Dieter, Luo, Yuqun Abigail, Renteria, Jone, Ryeznik, Yevgen, Sverdlov, Oleksandr, Uschner, Diane, for the Randomization Innovative Design Scientific Working Group, Beckman, Robert A, and Randomization Innovative Design Scientific Working Group

Subjects
CLINICAL trials, FALSE positive error, MEDICAL research personnel, MEASUREMENT errors, INFERENTIAL statistics
Abstract

Background: Randomization is the foundation of any clinical trial involving treatment comparison. It helps mitigate selection bias, promotes similarity of treatment groups with respect to important known and unknown confounders, and contributes to the validity of statistical tests. Various restricted randomization procedures with different probabilistic structures and different statistical properties are available. The goal of this paper is to present a systematic roadmap for the choice and application of a restricted randomization procedure in a clinical trial.Methods: We survey available restricted randomization procedures for sequential allocation of subjects in a randomized, comparative, parallel group clinical trial with equal (1:1) allocation. We explore statistical properties of these procedures, including balance/randomness tradeoff, type I error rate and power. We perform head-to-head comparisons of different procedures through simulation under various experimental scenarios, including cases when common model assumptions are violated. We also provide some real-life clinical trial examples to illustrate the thinking process for selecting a randomization procedure for implementation in practice.Results: Restricted randomization procedures targeting 1:1 allocation vary in the degree of balance/randomness they induce, and more importantly, they vary in terms of validity and efficiency of statistical inference when common model assumptions are violated (e.g. when outcomes are affected by a linear time trend; measurement error distribution is misspecified; or selection bias is introduced in the experiment). Some procedures are more robust than others. Covariate-adjusted analysis may be essential to ensure validity of the results. Special considerations are required when selecting a randomization procedure for a clinical trial with very small sample size.Conclusions: The choice of randomization design, data analytic technique (parametric or nonparametric), and analysis strategy (randomization-based or population model-based) are all very important considerations. Randomization-based tests are robust and valid alternatives to likelihood-based tests and should be considered more frequently by clinical investigators. [ABSTRACT FROM AUTHOR]

Published
2021
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25. The assessment of bias in randomized controlled clinical trials

Author

Uschner, Diane, Hilgers, Ralf-Dieter, and Willmes-von Hinckeldey, Klaus

Subjects
clinical trials, imbalance, open source, R software package, multi-arm trial, selection bias, ddc:610, randomization, chronological bias, time trend
Abstract

Dissertation, RWTH Aachen University, 2018; Aachen 1 Online-Ressource : Illustrationen (2018). = Dissertation, RWTH Aachen University, 2018, In controlled clinical trials, randomization is the key technique to ensure the comparability of two or more treatment groups. However, selection bias and time trends can lead to covariate imbalances that can influence the results of a clinical trial despite randomization. The unified assessment of selection bias and time trends is the objective of this thesis.Within the scope of this thesis, a sequence based approach for the assessment of selection bias and time trend was developed, and an explicit form for the influence of selection bias on the type-I-error rate in multi-arm trials was derived. A bias adjusted test was proposed and its power was investigated via simulations. The main result is the randomizeR software package in R that unifies the assessment of randomization procedures with respect to their susceptibility to selection and chronological bias. The sequence based approach allows the graphical presentation of the differences of the randomization procedures based on the type I and II error probabilities. For certain randomization procedures, the selection bias adjusted test can detect the treatment effect without substantial loss of power. In total, researchers are supported in choosing a randomization procedure that isleast susceptible to bias given the clinical scenario of the specific trial., Published by Aachen

Published
2018
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26. Randomization‐based inference in the presence of selection bias.

Author

Uschner, Diane

Subjects
*FALSE positive error, *MONTE Carlo method, *ERROR probability, *STATISTICAL models
Abstract

For the analysis of clinical trials, the study participants are usually assumed to be representative sample of a target population. This assumption is rarely fulfilled in clinical trials, and particularly not if the sample size is small. In addition, covariate imbalances may affect the trial. Randomization tests provide a nonparametric analysis method of the treatment effect that does not rely on population‐based assumptions. We propose a nonparametric statistical model that yields a formal basis for randomization tests. We adapt the model for the presence of covariate imbalance in the form of selection bias and investigate the effects of bias on the rejection probability of the randomization test using Monte Carlo simulations. Finally, we show that ancillary statistics can be used to control for the influence of bias. We show that covariate imbalance leads to an inflation of the type I error probability. The proposed nonparametric model allows for the use of ancillary statistics that yield an unbiased adjusted randomization test. [ABSTRACT FROM AUTHOR]

Published
2021
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27. Randomization tests for multiarmed randomized clinical trials.

Author

Wang, Yanying, Rosenberger, William F., and Uschner, Diane

Subjects
CLINICAL trials, FALSE positive error, MONTE Carlo method, STATISTICAL power analysis, ERROR rates
Abstract

We examine the use of randomization-based inference for analyzing multiarmed randomized clinical trials, including the application of conditional randomization tests to multiple comparisons. The view is taken that the linkage of the statistical test to the experimental design (randomization procedure) should be recognized. A selected collection of randomization procedures generalized to multiarmed treatment allocation is summarized, and generalizations for two randomization procedures that heretofore were designed for only two treatments are developed. We explain the process of computing the randomization test and conditional randomization test via Monte Carlo simulation, developing an efficient algorithm that makes multiple comparisons possible that would not be possible using a standard algorithm, demonstrate the preservation of type I error rate, and explore the relationship of statistical power to the randomization procedure in the presence of a time trend and outliers. We distinguish between the interpretation of the p-value in the randomization test and in the population test and verify that the randomization test can be approximated by the population test on some occasions. Data from two multiarmed clinical trials from the literature are reanalyzed to illustrate the methodology. [ABSTRACT FROM AUTHOR]

Published
2020
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28. Guideline adherence in acute coronary syndromes between telemedically supported paramedics and conventional on-scene physician care: A longitudinal pre–post intervention cohort study.

Author

Bergrath, Sebastian, Müller, Michael, Rossaint, Rolf, Beckers, Stefan K, Uschner, Diane, and Brokmann, Jörg C

Subjects
CHI-squared test, ELECTROCARDIOGRAPHY, EMERGENCY medical services, EMERGENCY medicine, FISHER exact test, LONGITUDINAL method, MEDICAL consultation, MEDICAL protocols, STATISTICS, T-test (Statistics), TELEMEDICINE, LOGISTIC regression analysis, DATA analysis, PRE-tests & post-tests, RETROSPECTIVE studies, DATA analysis software, ACUTE coronary syndrome, DESCRIPTIVE statistics
Abstract

Health informatics applications reduce time intervals in acute coronary syndromes, but their impact on guideline adherence is unknown. This pre–post intervention study compared guideline adherence between telemedically supported (n = 101, April 2014–July 2015) and conventional on-scene care (n = 120, January 2014–March 2014) in acute coronary syndrome. A multivariate logistic regression was performed for dependent variables: adverse events 0 versus 0, p = NA; electrocardiogram 101 versus 120, p = NA; acetylic salicylic acid 91 versus 102, p = 0.21; heparin 92 versus 112, p = 0.99; morphine 96 versus 107, p = 0.33; oxygen 83 versus 102, p = 0.92; glyceroltrinitrate 55 versus 90, p = 0.038; correct destination: 100 versus 119, p = 1.0. The time from ambulance arrival to hospital arrival was prolonged with telemedicine: 48.7 ± 11 min versus 35.5 ± 8.1 min, p < 0.001. Guideline adherence showed no differences except for glyceroltrinitrate. Prolonged time requirements are critical, though explainable. However, this approach enables a timely and high-quality backup strategy if only paramedics are on-scene. [ABSTRACT FROM AUTHOR]

Published
2019
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30. Randomization: The forgotten component of the randomized clinical trial.

Author

Rosenberger, William F., Uschner, Diane, and Wang, Yanying

Subjects
*CLINICAL trials, *STATISTICAL sampling, *STATISTICS, *DATA analysis
Abstract

"…The customary test for an observed difference…is based on an enumeration of the probabilities, on the initial hypothesis that two treatments do not differ in their effects,…of all the various results which would occur if the trial were repeated indefinitely with different random samples of the same size as those actually used." -Peter Armitage ("Sequential tests in prophylactic and therapeutic trials" in Quarterly Journal of Medicine, 1954;23(91):255-274). Randomization has been the hallmark of the clinical trial since Sir Bradford Hill adopted it in the 1946 streptomycin trial. An exploration of the early literature yields three rationales, ie, (i) the incorporation of randomization provides unpredictability in treatment assignments, thereby mitigating selection bias; (ii) randomization tends to ensure similarity in the treatment groups on known and unknown confounders (at least asymptotically); and (iii) the act of randomization itself provides a basis for inference when random sampling is not conducted from a population model. Of these three, rationale (iii) is often forgotten, ignored, or left untaught. Today, randomization is a rote exercise, scarcely considered in protocols or medical journal articles. Yet, the literature of the last century is rich with statistical articles on randomization methods and their consequences, authored by some of the pioneers of the biostatistics and statistics world. In this paper, we review some of this literature and describe very simple methods to rectify some of the oversight. We describe how randomization-based inference can be used for virtually any outcome of interest in a clinical trial. Special mention is made of nonstandard clinical trials situations. [ABSTRACT FROM AUTHOR]

Published
2019
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31. The impact of selection bias in randomized multi-arm parallel group clinical trials.

Author

Uschner, Diane, Hilgers, Ralf-Dieter, and Heussen, Nicole

Subjects
*CLINICAL trials, *SELECTION bias (Statistics), *THERAPEUTICS, *PROBABILITY theory, *ERROR analysis in mathematics, *STATISTICS
Abstract

The impact of selection bias on the results of clinical trials has been analyzed extensively for trials of two treatments, yet its impact in multi-arm trials is still unknown. In this paper, we investigate selection bias in multi-arm trials by its impact on the type I error probability. We propose two models for selection bias, so-called biasing policies, that both extend the classic guessing strategy by Blackwell and Hodges. We derive the distribution of the F-test statistic under the misspecified outcome model and provide a formula for the type I error probability under selection bias. We apply the presented approach to quantify the influence of selection bias in multi-arm trials with increasing number of treatment groups using a permuted block design for different assumptions and different biasing strategies. Our results confirm previous findings that smaller block sizes lead to a higher proportion of sequences with inflated type I error probability. Astonishingly, our results also show that the proportion of sequences with inflated type I error probability remains constant when the number of treatment groups is increased. Realizing that the impact of selection bias cannot be completely eliminated, we propose a bias adjusted statistical model and show that the power of the statistical test is only slightly deflated for larger block sizes. [ABSTRACT FROM AUTHOR]

Published
2018
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32. ERDO - a framework to select an appropriate randomization procedure for clinical trials.

Author

Hilgers, Ralf-Dieter, Uschner, Diane, Rosenberger, William F., and Heussen, Nicole

Subjects
*RANDOMIZED controlled trials, *CLINICAL medicine research, *CLINICAL trials, *EXTENSIONS, *PHARMACEUTICAL industry, *ALGORITHMS, *CASE studies, *RESEARCH bias
Abstract

Background: Randomization is considered to be a key feature to protect against bias in randomized clinical trials. Randomization induces comparability with respect to known and unknown covariates, mitigates selection bias, and provides a basis for inference. Although various randomization procedures have been proposed, no single procedure performs uniformly best. In the design phase of a clinical trial, the scientist has to decide which randomization procedure to use, taking into account the practical setting of the trial with respect to the potential of bias. Less emphasis has been placed on this important design decision than on analysis, and less support has been available to guide the scientist in making this decision.Methods: We propose a framework that weights the properties of the randomization procedure with respect to practical needs of the research question to be answered by the clinical trial. In particular, the framework assesses the impact of chronological and selection bias on the probability of a type I error. The framework is applied to a case study with a 2-arm parallel group, single center randomized clinical trial with continuous endpoint, with no-interim analysis, 1:1 allocation and no adaptation in the randomization process.Results: In so doing, we derive scientific arguments for the selection of an appropriate randomization procedure and develop a template which is illustrated in parallel by a case study. Possible extensions are discussed.Conclusion: The proposed ERDO framework guides the investigator through a template for the choice of a randomization procedure, and provides easy to use tools for the assessment. The barriers for the thorough reporting and assessment of randomization procedures could be further reduced in the future when regulators and pharmaceutical companies employ similar, standardized frameworks for the choice of a randomization procedure. [ABSTRACT FROM AUTHOR]

Published
2017
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33. Romantic Comedies and Responsive Adaptive Randomization in Clinical Trials.

Author

Jiang, Yunyun and Uschner, Diane

Subjects
*PERSISTENT fetal circulation syndrome, *CLINICAL trials
Abstract

Like his contemporary Sir R.A. Fisher, he argued that a control group was necessary and that patients must be allocated at random to the groups - treatment/therapy and control - to ensure that patients treated with streptomycin were truly comparable to control subjects. The state of equipoise justifies the fact that some patients will receive the worse treatment, given that determining which treatment constitutes the worse treatment is the goal of the investigation. Response-adaptive randomization (RAR), also known as outcome-adaptive randomization, has gained increasing attention in recent decades, mainly because of its potential ethical benefit. Thompson, et al., defined a BRAR randomization scheme as a function of the posterior predictive probability that one treatment is better than the other, i.e., SB I j i sb = Pr( I p i SB I j i sb > I p i SB I k i sb | I Data i , I j i I k i ) I j i , I k i = 1, 2, ..., I m i , where I p i SB I j i sb and I p i SB I k i sb are the posterior probability of success for I j i th and I k i th arm respectively, and I m i is the number of treatment arms. [Extracted from the article]

Published
2019
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34. 42-LB: Medication Adherence in Young Adults with Youth-Onset Type 2 Diabetes: The iCount Study.

Author

TRIEF, PAULA M., USCHNER, DIANE, TUNG, MELINDA, DREWS, KIMBERLY, KALICHMAN, SETH, ANDERSON, BARBARA, BULGER, JANE D., and WEINSTOCK, RUTH S.

Abstract

Background: Medication adherence is poor in young adults (YAs) with youth-onset type 2 diabetes (T2D). Little is known about intrapersonal factors that may relate to adherence. Aims: To assess associations of intrapersonal factors to medication adherence in Treatment Options for Adolescents and Youth (TODAY2) YAs. Methods: Validated measures (attitudes, beliefs, self-efficacy, distress, depression, anxiety) and insulin use surveys, were completed at a TODAY2 visit. Adherence to oral hypoglycemia agents (OHAs) was assessed with 3 monthly unannounced phone pill counts. Those taking ≥ 80% of pills/insulin classified "high-adherent;" < 80% of pills/insulin, "low-adherent." If taking none, reasons were queried and adjudicated (no need vs. low-adherent). Logistic regressions assessed factors associated with OHA/insulin adherence controlling for gender, race/ethnicity, education, duration, healthcare coverage, and HbA1c. Results: Of 381 YAs in iCount (mean age 26 yrs, 68% female, 20% non-Hispanic white, 38% non-Hispanic Black, 36% Hispanic, 64.9% <$25k income, mean HbA1c 9.4%), 224 were taking OHAs. As 12 lacked adherence scores, 212 were in OHA analyses; 70.0% were low-adherent to OHAs. Negative beliefs about medicines were associated with low OHA adherence in univariate, but not multivariate analyses. No measured intrapersonal factor was associated with OHA adherence. Of 192 in insulin analyses, 37.0% were low-adherent to insulin. Low insulin adherence was associated with less belief in seriousness of T2D (p=0.036), more concern that medications are overused (p=0.005) and diabetes distress (p=0.020). Insulin adherence did not relate to other diabetes attitudes or beliefs, depressive symptoms or anxiety. Limitations: small N with high depressive/anxiety symptoms; self-reported insulin use. Conclusion: Poor medication adherence is common in YAs with youth-onset T2D. More needs to be learned about factors associated with adherence to develop tailored, effective interventions. Disclosure: P. M. Trief: None. D. Uschner: None. M. Tung: None. K. Drews: None. S. Kalichman: None. B. Anderson: None. J. D. Bulger: None. R. S. Weinstock: Research Support; Self; Boehringer Ingelheim International GmbH, Diasome Pharmaceuticals, Inc., Eli Lilly and Company, Insulet Corporation, Kowa Research Institute, Inc., Medtronic, Tolerion, Inc. Funding: National Institute of Diabetes and Digestive and Kidney Diseases (1RO1DK110456-01A1; U01DK61230) [ABSTRACT FROM AUTHOR]

Published
2021
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35. 554-P: Diabetes Distress in Young Adults with Youth-Onset Type 2 Diabetes: TODAY Study Results.

Author

TRIEF, PAULA M., WEINSTOCK, RUTH S., USCHNER, DIANE, TUNG, MELINDA, CHAO, LILY, FARRELL, RYAN M., KEADY, JOYCE, MACLEISH, SARAH A., MARCUS, MARSHA D., and RAYAS, MARIA S.

Abstract

Aims: Diabetes distress (DD) is associated with poor health outcomes. Little is known about level of DD in young adults (YAs) with youth-onset type 2 diabetes (T2D) or individual factors associated with DD. Aims were to assess level of DD, and factors associated with high DD, in the Treatment Options for type 2 Diabetes in Adolescents and Youth (TODAY2) cohort. Methods: YAs completed the Diabetes Distress Scale (DDS), PHQ-9 (depressive symptoms) and GAD7 (anxiety), at the end-of-study visit. Factors that may relate to DD were demographics (sex, race/ethnicity, age, education, income), medical history (HbA1c, BMI, complications), and social/economic factors (# persons in household, parent status, healthcare coverage, access to diabetes care provider). Univariate logistic regressions found factors associated with high DD. Multivariate regression controlled for sex, HbA1c, healthcare coverage, anxiety, depressive symptoms and retinopathy. Results: Of 457 YAs, mean age=26.7 yrs, 65% were female, 20% non-Hispanic white, 38% non-Hispanic Black, 20% Hispanic, 62% <$25K income. High DD (DDS ≥2) was reported by 108 (23.6%). Subscales found 39.8% with high "regimen distress," 29.8% with high "emotional burden" (29.8%). Unadjusted results: Sex (p=0.001), HbA1c (p<0.0001), no healthcare coverage (p=0.043), hypertension (p=0.036) and retinopathy (p=0.005) were associated with DD. Moderate-severe depressive symptoms (PHQ-9 ≥10) and anxiety (GAD≥5) were also associated with DD (p<0.0001). In multivariate analyses, female sex, anxiety, HbA1c (p<0.0001 for all), and no healthcare coverage (p=0.022) remained associated with DD. Individual microvascular complications, BMI, depressive symptoms, race/ethnicity, age, education, income, # persons in household, or having a diabetes care provider did not relate to adjusted DD. Conclusion: In young adults with youth-onset T2D, high DD was significantly more likely in females, and those with anxiety, high HbA1c, and without healthcare coverage. Disclosure: P. M. Trief: None. M. S. Rayas: Research Support; Self; National Center for Advancing Translational Sciences. R. S. Weinstock: Research Support; Self; Boehringer Ingelheim International GmbH, Diasome Pharmaceuticals, Inc., Eli Lilly and Company, Insulet Corporation, Kowa Research Institute, Inc., Medtronic, Tolerion, Inc. D. Uschner: None. M. Tung: None. L. Chao: None. R. M. Farrell: Stock/Shareholder; Self; Tandem Diabetes Care. J. Keady: None. S. A. Macleish: Advisory Panel; Self; Insulet Corporation. M. D. Marcus: Advisory Panel; Self; Weight Watchers International, Inc. Funding: National Institute of Diabetes and Digestive and Kidney Diseases (U01DK61212, U01DK61230, U01DK61239, U01DK61242, U01DK61254) [ABSTRACT FROM AUTHOR]

Published
2021
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37. Association of Obesity and Diabetes with SARS-Cov-2 Infection and Symptoms in the COVID-19 Community Research Partnership.

Author

Mongraw-Chaffin M, Tjaden AH, Seals AL, Miller K, Ahmed N, Espeland MA, Gibbs M, Thomas D, Uschner D, Weintraub WS, and Edelstein SL

Abstract

Objective: Obesity and diabetes are established risk factors for severe SARS-CoV-2 outcomes, but less is known about their impact on susceptibility to COVID-19 infection and general symptom severity. We hypothesized that those with obesity or diabetes would be more likely to self-report a positive SARS-CoV-2 test, and among those with a positive test, have greater symptom severity and duration., Methods: Among 44,430 COVID-19 Community Research Partnership participants, we evaluated the association of self-reported and electronic health record obesity and diabetes with a self-reported positive COVID-19 test at any time. Among the 2,663 participants with a self-reported positive COVID-19 test during the study, we evaluated the association of obesity and diabetes with self-report of symptom severity, duration, and hospitalization. Logistic regression models were adjusted for age, sex, race/ethnicity, socioeconomic status, and healthcare worker status., Results: We found a positive graded association between Body Mass Index (BMI) category and positive COVID-19 test (Overweight OR = 1.14 [1.05-1.25]; Obesity I OR = 1.29 [1.17-2.42]; Obesity II OR = 1.34 [1.19-1.50]; Obesity III OR = 1.53 [1.35-1.73]), and a similar but weaker association with COVID-19 symptoms and severity among those with a positive test. Diabetes was associated with COVID-19 infection but not symptoms after adjustment, with some evidence of an interaction between obesity and diabetes., Conclusions: While the limitations of this health system convenience sample include generalizability and selection around test-seeking, the strong graded association of BMI and diabetes with self-reported COVID-19 infection suggests that obesity and diabetes may play a role in risk for symptomatic SARS-CoV-2 beyond co-occurrence with socioeconomic factors., (© The Author(s) 2022. Published by Oxford University Press on behalf of the Endocrine Society. All rights reserved. For permissions, please e-mail: journals.permissions@oup.com.)

Published
2022
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38. Breakthrough SARS-CoV-2 Infections after Vaccination in North Carolina.

Author

Uschner D, Bott M, Lagarde WH, Keating J, Tapp H, Berry AA, Seals AL, Munawar I, Schieffelin J, Yukich J, Santacatterina M, Gunaratne M, Fette LM, Burke B, Strylewicz G, Edelstein SL, Ahmed A, Miller K, Sanders JW, Herrington D, Weintraub WS, Runyon MS, and On Behalf Of The Covid-Community Research Partnership

Abstract

We characterize the overall incidence and risk factors for breakthrough infection among fully vaccinated participants in the North Carolina COVID-19 Community Research Partnership cohort. Among 15,808 eligible participants, 638 reported a positive SARS-CoV-2 test after vaccination. Factors associated with a lower risk of breakthrough in the time-to-event analysis included older age, prior SARS-CovV-2 infection, higher rates of face mask use, and receipt of a booster vaccination. Higher rates of breakthrough were reported by participants vaccinated with BNT162b2 or Ad26.COV2.S compared to mRNA-1273, in suburban or rural counties compared to urban counties, and during circulation of the Delta and Omicron variants.

Published
2022
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