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Featured researches published by John R. Dunn.


The New England Journal of Medicine | 2015

Burden of Clostridium difficile Infection in the United States

Fernanda C. Lessa; Yi Mu; Wendy Bamberg; Zintars G. Beldavs; Ghinwa Dumyati; John R. Dunn; Monica M. Farley; Stacy M. Holzbauer; James Meek; Erin C. Phipps; Lucy E. Wilson; Lisa G. Winston; Jessica Cohen; Brandi Limbago; Scott K. Fridkin; Dale N. Gerding; L. Clifford McDonald

BACKGROUND The magnitude and scope of Clostridium difficile infection in the United States continue to evolve. METHODS In 2011, we performed active population- and laboratory-based surveillance across 10 geographic areas in the United States to identify cases of C. difficile infection (stool specimens positive for C. difficile on either toxin or molecular assay in residents ≥ 1 year of age). Cases were classified as community-associated or health care-associated. In a sample of cases of C. difficile infection, specimens were cultured and isolates underwent molecular typing. We used regression models to calculate estimates of national incidence and total number of infections, first recurrences, and deaths within 30 days after the diagnosis of C. difficile infection. RESULTS A total of 15,461 cases of C. difficile infection were identified in the 10 geographic areas; 65.8% were health care-associated, but only 24.2% had onset during hospitalization. After adjustment for predictors of disease incidence, the estimated number of incident C. difficile infections in the United States was 453,000 (95% confidence interval [CI], 397,100 to 508,500). The incidence was estimated to be higher among females (rate ratio, 1.26; 95% CI, 1.25 to 1.27), whites (rate ratio, 1.72; 95% CI, 1.56 to 2.0), and persons 65 years of age or older (rate ratio, 8.65; 95% CI, 8.16 to 9.31). The estimated number of first recurrences of C. difficile infection was 83,000 (95% CI, 57,000 to 108,900), and the estimated number of deaths was 29,300 (95% CI, 16,500 to 42,100). The North American pulsed-field gel electrophoresis type 1 (NAP1) strain was more prevalent among health care-associated infections than among community-associated infections (30.7% vs. 18.8%, P<0.001). CONCLUSIONS C. difficile was responsible for almost half a million infections and was associated with approximately 29,000 deaths in 2011. (Funded by the Centers for Disease Control and Prevention.).


JAMA Internal Medicine | 2013

Epidemiology of Community-Associated Clostridium difficile Infection, 2009 Through 2011

Amit S. Chitnis; Stacy M. Holzbauer; Ruth Belflower; Lisa G. Winston; Wendy Bamberg; Carol Lyons; Monica M. Farley; Ghinwa Dumyati; Lucy E. Wilson; Zintars G. Beldavs; John R. Dunn; L. Hannah Gould; Duncan MacCannell; Dale N. Gerding; L. Clifford McDonald; Fernanda C. Lessa

IMPORTANCE Clostridium difficile infection (CDI) has been increasingly reported among healthy individuals in the community. Recent data suggest that community-associated CDI represents one-third of all C difficile cases. The epidemiology and potential sources of C difficile in the community are not fully understood. OBJECTIVES To determine epidemiological and clinical characteristics of community-associated CDI and to explore potential sources of C difficile acquisition in the community. DESIGN AND SETTING Active population-based and laboratory-based CDI surveillance in 8 US states. PARTICIPANTS Medical records were reviewed and interviews performed to assess outpatient, household, and food exposures among patients with community-associated CDI (ie, toxin or molecular assay positive for C difficile and no overnight stay in a health care facility within 12 weeks). Molecular characterization of C difficile isolates was performed. Outpatient health care exposure in the prior 12 weeks among patients with community-associated CDI was a priori categorized into the following 3 levels: no exposure, low-level exposure (ie, outpatient visit with physician or dentist), or high-level exposure (ie, surgery, dialysis, emergency or urgent care visit, inpatient care with no overnight stay, or health care personnel with direct patient care). MAIN OUTCOMES AND MEASURES Prevalence of outpatient health care exposure among patients with community-associated CDI and identification of potential sources of C difficile by level of outpatient health care exposure. RESULTS Of 984 patients with community-associated CDI, 353 (35.9%) did not receive antibiotics, 177 (18.0%) had no outpatient health care exposure, and 400 (40.7%) had low-level outpatient health care exposure. Thirty-one percent of patients without antibiotic exposure received proton pump inhibitors. Patients having CDI with no or low-level outpatient health care exposure were more likely to be exposed to infants younger than 1 year (P = .04) and to household members with active CDI (P = .05) compared with those having high-level outpatient health care exposure. No association between food exposure or animal exposure and level of outpatient health care exposure was observed. North American pulsed-field gel electrophoresis (NAP) 1 was the most common (21.7%) strain isolated; NAP7 and NAP8 were uncommon (6.7%). CONCLUSIONS AND RELEVANCE Most patients with community-associated CDI had recent outpatient health care exposure, and up to 36% would not be prevented by reduction of antibiotic use only. Our data support evaluation of additional strategies, including further examination of C difficile transmission in outpatient and household settings and reduction of proton pump inhibitor use.


The Journal of Infectious Diseases | 2006

Immunogenicity and Reactogenicity of 1 versus 2 Doses of Trivalent Inactivated Influenza Vaccine in Vaccine-Naive 5–8-Year-Old Children

Kathleen M. Neuzil; Lisa A. Jackson; Jennifer C. Nelson; Alexander Klimov; Nancy J. Cox; Carolyn B. Bridges; John R. Dunn; Frank DeStefano; David K. Shay

BACKGROUND Two doses of trivalent inactivated influenza vaccine (TIV) are recommended for children <9 years old receiving vaccine for the first time, but compliance is suboptimal. This study assessed the need for a second dose of TIV in this age group. METHODS In this prospective, open-label study, 232 influenza vaccine-naive 5-8-year-olds enrolled in a health maintenance organization received 2 doses of TIV in fall 2004. Serum for antibody titer measurement was obtained at 3 time points (n = 222). Parents completed diaries for 5 days. RESULTS Both doses of vaccine were well tolerated. The strongest predictor of a protective antibody response (> or =1 : 40) after 1 dose of TIV was baseline seropositive status. In multivariate analysis adjusting for age, sex, and baseline serostatus, the proportion of children with protective antibody responses was significantly higher after 2 doses than after 1 dose of TIV for each antigen (P < .001, for A/H1N1; P = .01, for A/H3N2; P < .001, for B). Age and sex were not independently predictive of a protective antibody response. Over one-third of children had antibody responses <1:40 for the type B vaccine component, even after 2 doses. CONCLUSIONS The present study supports the need for 2 doses of TIV in 5-8-year-olds receiving TIV for the first time. Efforts to increase compliance with the 2-dose recommendation are warranted.


Pediatrics | 2014

Clostridium difficile Infection Among Children Across Diverse US Geographic Locations

Joyanna Wendt; Jessica Cohen; Yi Mu; Ghinwa Dumyati; John R. Dunn; Stacy M. Holzbauer; Lisa G. Winston; Helen Johnston; James Meek; Monica M. Farley; Lucy E. Wilson; Erin C. Phipps; Zintars G. Beldavs; Dale N. Gerding; L. Clifford McDonald; Carolyn V. Gould; Fernanda C. Lessa

OBJECTIVE: Little is known about the epidemiology of Clostridium difficile infection (CDI) among children, particularly children ≤3 years of age in whom colonization is common but pathogenicity uncertain. We sought to describe pediatric CDI incidence, clinical presentation, and outcomes across age groups. METHODS: Data from an active population- and laboratory-based CDI surveillance in 10 US geographic areas during 2010–2011 were used to identify cases (ie, residents with C difficile–positive stool without a positive test in the previous 8 weeks). Community-associated (CA) cases had stool collected as outpatients or ≤3 days after hospital admission and no overnight health care facility stay in the previous 12 weeks. A convenience sample of CA cases were interviewed. Demographic, exposure, and clinical data for cases aged 1 to 17 years were compared across 4 age groups: 1 year, 2 to 3 years, 4 to 9 years, and 10 to 17 years. RESULTS: Of 944 pediatric CDI cases identified, 71% were CA. CDI incidence per 100 000 children was highest among 1-year-old (66.3) and white (23.9) cases. The proportion of cases with documented diarrhea (72%) or severe disease (8%) was similar across age groups; no cases died. Among the 84 cases interviewed who reported diarrhea on the day of stool collection, 73% received antibiotics during the previous 12 weeks. CONCLUSIONS: Similar disease severity across age groups suggests an etiologic role for C difficile in the high rates of CDI observed in younger children. Prevention efforts to reduce unnecessary antimicrobial use among young children in outpatient settings should be prioritized.


Emerging Infectious Diseases | 2009

Rickettsia parkeri in Amblyomma americanum ticks, Tennessee and Georgia, USA.

Sara B. Cohen; Michael J. Yabsley; Laurel E. Garrison; James D. Freye; Brett G. Dunlap; John R. Dunn; Daniel G. Mead; Timothy F. Jones; Abelardo Moncayo

To determine the geographic distribution of the newly recognized human pathogen Rickettsia parkeri, we looked for this organism in ticks from Tennessee and Georgia, USA. Using PCR and sequence analysis, we identified R. parkeri in 2 Amblyomma americanum ticks. This rickettsiosis may be underdiagnosed in the eastern United States.


Open Forum Infectious Diseases | 2016

Burden of Nursing Home-Onset Clostridium difficile Infection in the United States: Estimates of Incidence and Patient Outcomes

Jennifer C. Hunter; Yi Mu; Ghinwa Dumyati; Monica M. Farley; Lisa G. Winston; Helen Johnston; James Meek; Rebecca Perlmutter; Stacy M. Holzbauer; Zintars G. Beldavs; Erin C. Phipps; John R. Dunn; Jessica Cohen; Johannetsy J. Avillan; Nimalie D. Stone; Dale N. Gerding; L. Clifford McDonald; Fernanda C. Lessa

Background. Approximately 4 million Americans receive nursing home (NH) care annually. Nursing home residents commonly have risk factors for Clostridium difficile infection (CDI), including advanced age and antibiotic exposures. We estimated national incidence of NH-onset (NHO) CDI and patient outcomes. Methods. We identified NHO-CDI cases from population-based surveillance of 10 geographic areas in the United States. Cases were defined by C difficile-positive stool collected in an NH (or from NH residents in outpatient settings or ≤3 days after hospital admission) without a positive stool in the prior 8 weeks. Medical records were reviewed on a sample of cases. Incidence was estimated using regression models accounting for age and laboratory testing method; sampling weights were applied to estimate hospitalizations, recurrences, and deaths. Results. A total of 3503 NHO-CDI cases were identified. Among 262 sampled cases, median age was 82 years, 76% received antibiotics in the 12 weeks prior to the C difficile-positive specimen, and 57% were discharged from a hospital in the month before specimen collection. After adjusting for age and testing method, the 2012 national estimate for NHO-CDI incidence was 112 800 cases (95% confidence interval [CI], 93 400–131 800); 31 400 (28%) were hospitalized within 7 days after a positive specimen (95% CI, 25 500–37 300), 20 900 (19%) recurred within 14–60 days (95% CI, 14 600–27 100), and 8700 (8%) died within 30 days (95% CI, 6600–10 700). Conclusions. Nursing home onset CDI is associated with substantial morbidity and mortality. Strategies focused on infection prevention in NHs and appropriate antibiotic use in both NHs and acute care settings may decrease the burden of NHO CDI.


The Journal of Infectious Diseases | 2016

Whole-Genome Sequencing: Opportunities and Challenges for Public Health, Food-borne Outbreak Investigations, and the Global Food Supply

John R. Dunn

nue in the food industry are substantial. Globally the burden is even higher, and multinational outbreaks due to the global movement of contaminated foods are being described increasingly. The global food supply links nations and economies, emphasizing the need to view food safety with an integrated farm-to-fork lens. As predicted, advances in molecular techniques and information management have been transformative for food-borne disease investigation [2]. Almost 2 decades have passed since the Centers for Disease Control and Prevention (CDC) launched a national molecular subtyping system known as PulseNet, and since that time it has become an indispensable laboratory surveillance system for detection of multijurisdictional food-borne outbreaks. With PulseNet, public health authorities developed a unique system able to link bacterial isolates that could identify food-borne outbreaks dispersed far and wide geographically with only a few cases. Notable examples of PulseNet’s impact include elucidation of the association of Escherichia coli O157 and ground beef [3], as well as numerous produce-associated outbreaks [4,5].Not only food-borne disease investigations have been enhanced; investigations related to direct animal contact have improved as well [6, 7]. Indeed, PulseNet has facilitated more cluster evaluations, faster outbreak investigations, and timelier regulatory interventions and has undoubtedly prevented many illnesses


Clinical Infectious Diseases | 2018

Impact of Culture-Independent Diagnostic Testing on Recovery of Enteric Bacterial Infections

Aamer Imdad; Fiona Retzer; Linda S Thomas; Marcy McMillian; Katie Garman; Peter F. Rebeiro; Stephen A. Deppen; John R. Dunn; Amy M. Woron

Background Culture-independent diagnostic tests (CIDTs) are increasingly used to identify enteric pathogens. However, foodborne illness surveillance systems have relied upon culture confirmation to estimate disease burden and identify outbreaks through molecular subtyping. This study examined the impacts of CIDT and estimated costs for culture verification of Shigella, Salmonella, Shiga toxin-producing Escherichia coli (STEC), and Campylobacter at the Tennessee Department of Health Public Health Laboratory (PHL). Methods This observational study included laboratory and epidemiological surveillance data collected between years 2013-2016 from patients with the reported enteric illness. We calculated pathogen recovery at PHL based on initial diagnostic test type reported at the clinical laboratory. Adjusted prevalence ratios (PRs) and 95% confidence intervals (CIs) were estimated with modified Poisson regression. Estimates of cost were calculated for pathogen recovery from CIDT-positive specimens compared to recovery from culture-derived isolates. Results During the study period, PHL received 5553 specimens from clinical laboratories from patients with the enteric illness. Pathogen recovery was 57% (984/1713) from referred CIDT-positive stool specimens and 95% (3662/3840) from culture-derived isolates (PR, 0.61 [95% CI, .56-.66]). Pathogen recovery from CIDT-positive specimens varied based on pathogen type: Salmonella (72%), Shigella (64%), STEC (57%), and Campylobacter (26%). Compared to stool culture-derived isolates, the cost to recover pathogens from 100 CIDT-positive specimens was higher for Shigella (US


Pediatrics | 2016

Safety and immunogenicity of sequential rotavirus vaccine schedules

Romina Libster; Monica M. McNeal; Emmanuel B. Walter; Andi L. Shane; Patricia L. Winokur; Gretchen A. Cress; Andrea A. Berry; Karen L. Kotloff; Kwabena O. Sarpong; Christine B. Turley; Christopher J. Harrison; Barbara Pahud; Jyothi Marbin; John R. Dunn; Jill El-Khorazaty; Jill Barrett; Kathryn M. Edwards

6192), Salmonella (US


Journal of the Pediatric Infectious Diseases Society | 2018

Evaluating Previous Antibiotic Use as a Risk Factor for Acute Gastroenteritis Among Children in Davidson County, Tennessee, 2014–2015

Jonathan M Kolsin; Benjamin A. Lopman; Daniel C. Payne; Mary E. Wikswo; John R. Dunn; Natasha Halasa; Aron J Hall

18373), and STEC (US

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Fernanda C. Lessa

Centers for Disease Control and Prevention

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Ghinwa Dumyati

University of Rochester Medical Center

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L. Clifford McDonald

Centers for Disease Control and Prevention

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Dale N. Gerding

Loyola University Chicago

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Erin C. Phipps

University of New Mexico

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Jessica Cohen

Centers for Disease Control and Prevention

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