Your search keyword '"Alice Y. Guh"' showing total 18 results

1. Carbapenem-Resistant and Extended-Spectrum β-Lactamase–Producing Enterobacterales in Children, United States, 2016–2020

Author

Heather N. Grome, Julian E. Grass, Nadezhda Duffy, Sandra N. Bulens, Uzma Ansari, Davina Campbell, Joseph D. Lutgring, Amy S. Gargis, Thao Masters, Alyssa G. Kent, Susannah L. McKay, Gillian Smith, Lucy E. Wilson, Elisabeth Vaeth, Bailey Evenson, Ghinwa Dumyati, Rebecca Tsay, Erin Phipps, Kristina Flores, Christopher D. Wilson, Christopher A. Czaja, Helen Johnston, Sarah J. Janelle, Ruth Lynfield, Sean O’Malley, Paula Snippes Vagnone, Meghan Maloney, Joelle Nadle, and Alice Y. Guh

Subjects

Enterobacterales, carbapenem-resistant Enterobacterales, extended-spectrum β-lactamase-producing Enterobacterales, antimicrobial resistance, epidemiology, child, Medicine, Infectious and parasitic diseases, RC109-216

Abstract

We conducted surveillance for carbapenem-resistant Enterobacterales (CRE) during 2016–2020 at 10 US sites and extended-spectrum β-lactamase–producing Enterobacterales (ESBL-E) during 2019–2020 at 6 US sites. Among 159 CRE cases in children (median age 5 years), CRE was isolated from urine for 131 (82.4%) and blood from 20 (12.6%). Annual CRE incidence rate (cases/100,000 population) was 0.47–0.87. Among 207 ESBL-E cases in children (median age 6 years), ESBL-E was isolated from urine of 196 (94.7%) and blood of 8 (3.9%). Annual ESBL-E incidence rate was 26.5 in 2019 and 19.63 in 2020. CRE and ESBL-E rates were >2-fold higher among infants than other age groups. Most CRE and ESBL-E cases were healthcare-associated community-onset (68 [43.0%] for CRE vs. 40 [23.7%] for ESBL-E) or community-associated (43 [27.2%] for CRE vs. 109 [64.5%] for ESBL-E). Programs to detect, prevent, and treat multidrug-resistant infections must include pediatric populations (particularly the youngest) and outpatient settings.

Published

2024

2. Informing estimates of probability of Clostridioides difficile infection for testing and treatment: expert consensus from a modified-Delphi procedure

Author

Jonathan D. Baghdadi, Mia Wessel, Erik R. Dubberke, Alison Lydecker, Kimberly C. Claeys, Carolyn Alonso, K.C. Coffey, Michael Durkin, Anne J. Gonzales-Luna, Alice Y. Guh, Jennie H. Kwon, Elise Martin, Preeti Mehrotra, Christopher R. Polage, Michael S. Pulia, Clare Rock, Andrew M. Skinner, Valerie M. Vaughn, Tara Vijayan, Michael E. Yarrington, Daniel J. Morgan, and for the CDC Prevention Epicenters Program

Subjects

Infectious and parasitic diseases, RC109-216, Public aspects of medicine, RA1-1270

Abstract

Abstract Background: Clostridioides difficile infection (CDI) may be misdiagnosed if testing is performed in the absence of signs or symptoms of disease. This study sought to support appropriate testing by estimating the impact of signs, symptoms, and healthcare exposures on pre-test likelihood of CDI. Methods: A panel of fifteen experts in infectious diseases participated in a modified UCLA/RAND Delphi study to estimate likelihood of CDI. Consensus, defined as agreement by >70% of panelists, was assessed via a REDCap survey. Items without consensus were discussed in a virtual meeting followed by a second survey. Results: All fifteen panelists completed both surveys (100% response rate). In the initial survey, consensus was present on 6 of 15 (40%) items related to risk of CDI. After panel discussion and clarification of questions, consensus (>70% agreement) was reached on all remaining items in the second survey. Antibiotics were identified as the primary risk factor for CDI and grouped into three categories: high-risk (likelihood ratio [LR] 7, 93% agreement among panelists in first survey), low-risk (LR 3, 87% agreement in first survey), and minimal-risk (LR 1, 71% agreement in first survey). Other major factors included new or unexplained severe diarrhea (e.g., ≥ 10 liquid bowel movements per day; LR 5, 100% agreement in second survey) and severe immunosuppression (LR 5, 87% agreement in second survey). Conclusion: Infectious disease experts concurred on the importance of signs, symptoms, and healthcare exposures for diagnosing CDI. The resulting risk estimates can be used by clinicians to optimize CDI testing and treatment.

Published

2024

3. Development of a Broth Microdilution Method To Characterize Chlorhexidine MICs among Bacteria Collected from 2005 to 2019 at Three U.S. Sites

Author

Joseph D. Lutgring, Julian E. Grass, David Lonsway, Brian B. Yoo, Erin Epson, Megan Crumpler, Karen Galliher, Kathleen O’Donnell, Matthew Zahn, Eric Evans, Jesse T. Jacob, Alexander Page, Sarah W. Satola, Gillian Smith, Marion Kainer, Daniel Muleta, Christopher D. Wilson, Mary K. Hayden, Sujan Reddy, Christopher A. Elkins, J. Kamile Rasheed, Maria Karlsson, Shelley S. Magill, and Alice Y. Guh

Subjects

broth microdilution, chlorhexidine, susceptibility testing, Microbiology, QR1-502

Abstract

ABSTRACT Chlorhexidine bathing to prevent transmission of multidrug-resistant organisms has been adopted by many U.S. hospitals, but increasing chlorhexidine use has raised concerns about possible emergence of resistance. We sought to establish a broth microdilution method for determining chlorhexidine MICs and then used the method to evaluate chlorhexidine MICs for bacteria that can cause health care-associated infections. We adapted a broth microdilution method for determining chlorhexidine MICs, poured panels, established quality control ranges, and tested Staphylococcus aureus, Escherichia coli, Klebsiella pneumoniae, and Enterobacter cloacae complex isolates collected at three U.S. sites. Chlorhexidine MICs were determined for 535 isolates including 129 S. aureus, 156 E. coli, 142 K. pneumoniae, and 108 E. cloacae complex isolates. The respective MIC distributions for each species ranged from 1 to 8 mg/L (MIC50 = 2 mg/L and MIC90 = 4 mg/L), 1 to 64 mg/L (MIC50 = 2 mg/L and MIC90 = 4 mg/L), 4 to 64 mg/L (MIC50 = 16 mg/L and MIC90 = 32 mg/L), and 1 to >64 mg/L (MIC50 = 16 mg/L and MIC90 = 64 mg/L). We successfully adapted a broth microdilution procedure that several laboratories were able to use to determine the chlorhexidine MICs of bacterial isolates. This method could be used to investigate whether chlorhexidine MICs are increasing. IMPORTANCE Chlorhexidine bathing to prevent transmission of multidrug-resistant organisms and reduce health care-associated infections has been adopted by many hospitals. There is concern about the possible unintended consequences of using this agent widely. One possible unintended consequence is decreased susceptibility to chlorhexidine, but there are not readily available methods to perform this evaluation. We developed a method for chlorhexidine MIC testing that can be used to evaluate for possible unintended consequences.

Published

2023

4. Improved Phenotype-Based Definition for Identifying Carbapenemase Producers among Carbapenem-Resistant Enterobacteriaceae

Author

Nora Chea, Sandra N. Bulens, Thiphasone Kongphet-Tran, Ruth Lynfield, Kristin Shaw, Paula Snippes Vagnone, Marion Kainer, Daniel Muleta, Lucy Wilson, Elisabeth Vaeth, Ghinwa Dumyati, Cathleen Concannon, Erin C. Phipps, Karissa Culbreath, Sarah J. Janelle, Wendy Bamberg, Alice Y. Guh, Brandi M. Limbago, and Alexander J. Kallen

Subjects

carbapenemase, carbapenem-resistant, carbapenemase producers, Enterobacteriaceae, CRE, enterobacteria, Medicine, Infectious and parasitic diseases, RC109-216

Abstract

Preventing transmission of carbapenemase-producing, carbapenem-resistant Enterobacteriaceae (CP-CRE) is a public health priority. A phenotype-based definition that reliably identifies CP-CRE while minimizing misclassification of non–CP-CRE could help prevention efforts. To assess possible definitions, we evaluated enterobacterial isolates that had been tested and deemed nonsusceptible to >1 carbapenem at US Emerging Infections Program sites. We determined the number of non-CP isolates that met (false positives) and CP isolates that did not meet (false negatives) the Centers for Disease Control and Prevention CRE definition in use during our study: 30% (94/312) of CRE had carbapenemase genes, and 21% (14/67) of Klebsiella pneumoniae carbapenemase–producing Klebsiella isolates had been misclassified as non-CP. A new definition requiring resistance to 1 carbapenem rarely missed CP strains, but 55% of results were false positive; adding the modified Hodge test to the definition decreased false positives to 12%. This definition should be considered for use in carbapenemase-producing CRE surveillance and prevention.

Published

2015

5. Endophthalmitis Outbreak Associated with Repackaged Bevacizumab

Author

Laura S. Edison, Hope O. Dishman, Melissa Tobin-D’Angelo, C. Richard Allen, Alice Y. Guh, and Cherie L. Drenzek

Subjects

Gram-positive bacterial infections, disease outbreaks, drug compounding, drug contamination, endophthalmitis, eye infections, Medicine, Infectious and parasitic diseases, RC109-216

Published

2015

6. Evaluation of viral co-infections among patients with community-associated Clostridioides difficile infection.

Author

Lauren Korhonen, Jessica Cohen, Nicole Gregoricus, Monica M Farley, Rebecca Perlmutter, Stacy M Holzbauer, Ghinwa Dumyati, Zintars Beldavs, Ashley Paulick, Jan Vinjé, Brandi M Limbago, Fernanda C Lessa, and Alice Y Guh

Subjects

Medicine, Science

Abstract

We assessed viral co-infections in 155 patients with community-associated Clostridioides difficile infection in five U.S. sites during December 2012-February 2013. Eighteen patients (12%) tested positive for norovirus (n = 10), adenovirus (n = 4), rotavirus (n = 3), or sapovirus (n = 1). Co-infected patients were more likely than non-co-infected patients to have nausea or vomiting (56% vs 31%; p = 0.04), suggesting that viral co-pathogens contributed to symptoms in some patients. There were no significant differences in prior healthcare or medication exposures or in CDI complications.

Published

2020

7. Reply to Gonzales-Luna et al

Author

Amy S Gargis, Maria Karlsson, J Kamile Rasheed, Alyssa G Kent, Susannah L McKay, Ashley L Paulick, Karen F Anderson, Michelle Adamczyk, Davina Campbell, Lauren C Korhonen, Gillian McAllister, Nicholas Vlachos, Alison L Halpin, Joseph D Lutgring, Alice Y Guh, L Clifford McDonald, and Christopher A Elkins

Subjects

Microbiology (medical), Infectious Diseases

Published

2023

8. Comparison of the Risk of Recurrent Clostridioides Difficile Infections Among Patients in 2018 Versus 2013

Author

Alice Y Guh, Sarah H Yi, James Baggs, Lisa Winston, Erin Parker, Helen Johnston, Elizabeth Basiliere, Danyel Olson, Scott K Fridkin, Nirja Mehta, Lucy Wilson, Rebecca Perlmutter, Stacy M Holzbauer, Paige D’Heilly, Erin C Phipps, Kristina G Flores, Ghinwa K Dumyati, Trupti Hatwar, Rebecca Pierce, Valerie L S Ocampo, Christopher D Wilson, Jasmine J Watkins, Lauren Korhonen, Ashley Paulick, Michelle Adamczyk, Dale N Gerding, and Sujan C Reddy

Subjects

Infectious Diseases, Oncology, Brief Report

Abstract

Among persons with an initial Clostridioides difficile infection (CDI) across 10 US sites in 2018 compared with 2013, 18.3% versus 21.1% had ≥1 recurrent CDI (rCDI) within 180 days. We observed a 16% lower adjusted risk of rCDI in 2018 versus 2013 (P

Published

2022

9. Reference Susceptibility Testing and Genomic Surveillance of Clostridioides difficile, United States, 2012-17

Author

Amy S, Gargis, Maria, Karlsson, Ashley L, Paulick, Karen F, Anderson, Michelle, Adamczyk, Nicholas, Vlachos, Alyssa G, Kent, Gillian A, McAllister, Susannah L, McKay, Alison L, Halpin, Valerie, Albrecht, Davina, Campbell, Lauren, Korhonen, Christopher A, Elkins, J Kamile, Rasheed, Alice Y, Guh, L Clifford, McDonald, Joseph D, Lutgring, and Lisa, Winston

Subjects

Microbiology (medical), Infectious Diseases

Abstract

Background Antimicrobial susceptibility testing (AST) is not routinely performed for Clostridioides difficile and data evaluating minimum inhibitory concentrations (MICs) are limited. We performed AST and whole genome sequencing (WGS) for 593 C. difficile isolates collected between 2012 and 2017 through the Centers for Disease Control and Prevention's Emerging Infections Program. Methods MICs to 6 antimicrobial agents (ceftriaxone, clindamycin, meropenem, metronidazole, moxifloxacin, and vancomycin) were determined using the reference agar dilution method according to Clinical and Laboratory Standards Institute guidelines. Whole genome sequencing was performed on all isolates to detect the presence of genes or mutations previously associated with resistance. Results Among all isolates, 98.5% displayed a vancomycin MIC ≤2 μg/mL and 97.3% displayed a metronidazole MIC ≤2 μg/mL. Ribotype 027 (RT027) isolates displayed higher vancomycin MICs (MIC50: 2 μg/mL; MIC90: 2 μg/mL) than non-RT027 isolates (MIC50: 0.5 μg/mL; MIC90: 1 μg/mL) (P < .01). No vanA/B genes were detected. RT027 isolates also showed higher MICs to clindamycin and moxifloxacin and were more likely to harbor associated resistance genes or mutations. Conclusions Elevated MICs to antibiotics used for treatment of C. difficile infection were rare, and there was no increase in MICs over time. The lack of vanA/B genes or mutations consistently associated with elevated vancomycin MICs suggests there are multifactorial mechanisms of resistance. Ongoing surveillance of C. difficile using reference AST and WGS to monitor MIC trends and the presence of antibiotic resistance mechanisms is essential.

Published

2022

10. Correction for Paulick et al., 'Characterization of Clostridioides difficile Isolates Available through the CDCFDA Antibiotic Resistance Isolate Bank'

Author

Ashley, Paulick, Michelle, Adamczyk, Karen, Anderson, Nick, Vlachos, María-José, Machado, Gillian, McAllister, Lauren, Korhonen, Alice Y, Guh, Alison Laufer, Halpin, J Kamile, Rasheed, Maria, Karlsson, Joseph D, Lutgring, and Amy S, Gargis

Subjects

Immunology and Microbiology (miscellaneous), Culture Collections/Mutant Libraries, Genetics, Molecular Biology

Abstract

Thirty Clostridioides difficile isolates collected in 2016 through the Centers for Disease Control and Prevention Emerging Infections Program were selected for reference antimicrobial susceptibility testing and whole-genome sequencing. Here, we present the genetic characteristics of these isolates and announce their availability in the CDC & FDA Antibiotic Resistance Isolate Bank.

Published

2022

11. Reported cases of multisystem inflammatory syndrome in children aged 12-20 years in the USA who received a COVID-19 vaccine, December, 2020, through August, 2021: a surveillance investigation

Author

Anna R Yousaf, Margaret M Cortese, Allan W Taylor, Karen R Broder, Matthew E Oster, Joshua M Wong, Alice Y Guh, David W McCormick, Satoshi Kamidani, Elizabeth P Schlaudecker, Kathryn M Edwards, C Buddy Creech, Mary A Staat, Ermias D Belay, Paige Marquez, John R Su, Mark B Salzman, Deborah Thompson, Angela P Campbell, Oidda Museru, Leigh M. Howard, Monica Parise, John J. Openshaw, Chloe LeMarchand, Lauren E. Finn, Moon Kim, Kiran V. Raman, Kenneth K. Komatsu, Bryce L. Spiker, Cole P. Burkholder, Sean M. Lang, and Jonathan H. Soslow

Subjects

Male, Young Adult, COVID-19 Vaccines, Adolescent, SARS-CoV-2, Pediatrics, Perinatology and Child Health, Developmental and Educational Psychology, COVID-19, Humans, Female, Child, Systemic Inflammatory Response Syndrome, United States

Abstract

Multisystem inflammatory syndrome in children (MIS-C) is a hyperinflammatory condition associated with antecedent SARS-CoV-2 infection. In the USA, reporting of MIS-C after vaccination is required under COVID-19 vaccine emergency use authorisations. We aimed to investigate reports of individuals aged 12-20 years with MIS-C after COVID-19 vaccination reported to passive surveillance systems or through clinician outreach to the US Centers for Disease Control and Prevention (CDC).In this surveillance activity, we investigated potential cases of MIS-C after COVID-19 vaccination reported to CDC's MIS-C national surveillance system, the Vaccine Adverse Event Reporting System (co-administered by CDC and the US Food and Drug Administration), and CDC's Clinical Immunization Safety Assessment Project. A multidisciplinary team adjudicated cases by use of the CDC MIS-C definition. Any positive SARS-CoV-2 serology test satisfied case criteria; although anti-nucleocapsid antibodies indicate previous SARS-CoV-2 infection, anti-spike protein antibodies indicate either past or recent infection or COVID-19 vaccination. We describe the demographic and clinical features of cases, stratified by laboratory evidence of SARS-CoV-2 infection. To calculate the reporting rate of MIS-C, we divided the count of all individuals meeting the MIS-C case definition, and of those without evidence of SARS-CoV-2 infection, by the number of individuals aged 12-20 years in the USA who received one or more COVID-19 vaccine doses up to Aug 31, 2021, obtained from CDC national vaccine surveillance data.Using surveillance results from Dec 14, 2020, to Aug 31, 2021, we identified 21 individuals with MIS-C after COVID-19 vaccination. Of these 21 individuals, median age was 16 years (range 12-20); 13 (62%) were male and eight (38%) were female. All 21 were hospitalised: 12 (57%) were admitted to an intensive care unit and all were discharged home. 15 (71%) of 21 individuals had laboratory evidence of past or recent SARS-CoV-2 infection, and six (29%) did not. As of Aug 31, 2021, 21 335 331 individuals aged 12-20 years had received one or more doses of a COVID-19 vaccine, making the overall reporting rate for MIS-C after vaccination 1·0 case per million individuals receiving one or more doses in this age group. The reporting rate in only those without evidence of SARS-CoV-2 infection was 0·3 cases per million vaccinated individuals.Here, we describe a small number of individuals with MIS-C who had received one or more doses of a COVID-19 vaccine before illness onset; the contribution of vaccination to these illnesses is unknown. Our findings suggest that MIS-C after COVID-19 vaccination is rare. Continued reporting of potential cases and surveillance for MIS-C illnesses after COVID-19 vaccination is warranted.US Centers for Disease Control and Prevention.

Published

2022

12. Associations of facility-level antibiotic use and hospital-onset

Author

Sophia V, Kazakova, James, Baggs, Sarah H, Yi, Sujan C, Reddy, Kelly M, Hatfield, Alice Y, Guh, John A, Jernigan, and L Clifford, McDonald

Subjects

Cross Infection, Clostridioides difficile, Clostridium Infections, Humans, Hospitals, Anti-Bacterial Agents

Abstract

Previously reported associations between hospital-level antibiotic use and hospital-onset

Published

2021

13. Updated Recommendations from the Advisory Committee on Immunization Practices for Use of the Janssen (JohnsonJohnson) COVID-19 Vaccine After Reports of Thrombosis with Thrombocytopenia Syndrome Among Vaccine Recipients - United States, April 2021

Author

Jessica R, MacNeil, John R, Su, Karen R, Broder, Alice Y, Guh, Julia W, Gargano, Megan, Wallace, Stephen C, Hadler, Heather M, Scobie, Amy E, Blain, Danielle, Moulia, Matthew F, Daley, Veronica V, McNally, José R, Romero, H Keipp, Talbot, Grace M, Lee, Beth P, Bell, and Sara E, Oliver

Subjects

Adult, Male, COVID-19 Vaccines, Adolescent, United States Food and Drug Administration, Advisory Committees, COVID-19, Thrombosis, Middle Aged, Risk Assessment, Thrombocytopenia, United States, Safety-Based Drug Withdrawals, Young Adult, Practice Guidelines as Topic, Adverse Drug Reaction Reporting Systems, Humans, Female, Full Report, Centers for Disease Control and Prevention, U.S, Drug Approval, Drug Labeling

Abstract

On February 27, 2021, the Food and Drug Administration (FDA) issued an Emergency Use Authorization (EUA) for the Janssen COVID-19 (Ad.26.COV2.S) vaccine (Janssen Biotech, Inc., a Janssen Pharmaceutical company, JohnsonJohnson; New Brunswick, New Jersey), and on February 28, 2021, the Advisory Committee on Immunization Practices (ACIP) issued interim recommendations for its use in persons aged ≥18 years (1,2). On April 13, 2021, CDC and FDA recommended a pause in the use of the Janssen COVID-19 vaccine after reports of six U.S. cases of cerebral venous sinus thrombosis (CVST) with thrombocytopenia, a rare thromboembolic syndrome, among Janssen COVID-19 vaccine recipients (3). Two emergency ACIP meetings were rapidly convened to review reported cases of thrombosis with thrombocytopenia syndrome (TTS) and to consider updated recommendations for use of the Janssen COVID-19 vaccine in the United States. On April 23, 2021, after a discussion of the benefits and risks of resuming vaccination, ACIP reaffirmed its interim recommendation for use of the Janssen COVID-19 vaccine in all persons aged ≥18 years under the FDA's EUA, which now includes a warning that rare clotting events might occur after vaccination, primarily among women aged 18-49 years. Patient and provider education about the risk for TTS with the Janssen COVID-19 vaccine, especially among women aged50 years, as well as the availability of alternative COVID-19 vaccines, is required to guide vaccine decision-making and ensure early recognition and clinical management of TTS.

Published

2021

14. Prescriber perceptions of fluoroquinolones, extended-spectrum cephalosporins, and

Author

Julia E, Szymczak, Brandi M, Muller, Nikitha Shankar, Shakamuri, Keith W, Hamilton, Jeffrey S, Gerber, Maryrose, Laguio-Vila, Ghinwa K, Dumyati, Scott K, Fridkin, Alice Y, Guh, Sujan C, Reddy, and Ebbing, Lautenbach

Subjects

Cross Infection, Clostridioides, Clostridioides difficile, Clostridium Infections, Humans, Perception, Anti-Bacterial Agents, Cephalosporins, Fluoroquinolones

Abstract

Fluoroquinolones (FQs) and extended-spectrum cephalosporins (ESCs) are associated with higher risk of Clostridioides difficile infection (CDI). Decreasing the unnecessary use of FQs and ESCs is a goal of antimicrobial stewardship. Understanding how prescribers perceive the risks and benefits of FQs and ESCs is needed.We conducted interviews with clinicians from 4 hospitals. Interviews elicited respondent perceptions about the risk of ESCs, FQs, and CDI. Interviews were audio recorded, transcribed, and analyzed using a flexible coding approach.Interviews were conducted with 64 respondents (38 physicians, 7 nurses, 6 advance practice providers, and 13 pharmacists). ESCs and FQs were perceived to have many benefits, including infrequent dosing, breadth of coverage, and greater patient adherence after hospital discharge. Prescribers stated that it was easy to make decisions about these drugs, so they were especially appealing to use in the context of time pressures. They described having difficulty discontinuing these drugs when prescribed by others due to inertia and fear. Prescribers were skeptical about targeting specific drugs as a stewardship approach and felt that the risk of a negative outcome from under treatment of a suspected bacterial infection was a higher priority than the prevention of CDI.Prescribers in this study perceived many advantages to using ESCs and FQs, especially under conditions of time pressure and uncertainty. In making decisions about these drugs, prescribers balance risk and benefit, and they believed that the risk of CDI was acceptable in compared with the risk of undertreatment.

Published

2020

15. Trends in U.S. Burden of

Author

Alice Y, Guh, Yi, Mu, Lisa G, Winston, Helen, Johnston, Danyel, Olson, Monica M, Farley, Lucy E, Wilson, Stacy M, Holzbauer, Erin C, Phipps, Ghinwa K, Dumyati, Zintars G, Beldavs, Marion A, Kainer, Maria, Karlsson, Dale N, Gerding, and L Clifford, McDonald

Subjects

Community-Acquired Infections, Hospitalization, Cross Infection, Treatment Outcome, Clostridioides difficile, Recurrence, Incidence, Population Surveillance, Clostridium Infections, Humans, Hospital Mortality, United States, Article

Abstract

BACKGROUND: Efforts to prevent Clostridioides difficile infection continue to expand across the health care spectrum in the United States. Whether these efforts are reducing the national burden of C. difficile infection is unclear. METHODS: The Emerging Infections Program identified cases of C. difficile infection (stool specimens positive for C. difficile in a person ≥1 year of age with no positive test in the previous 8 weeks) in 10 U.S. sites. We used case and census sampling weights to estimate the national burden of C. difficile infection, first recurrences, hospitalizations, and in-hospital deaths from 2011 through 2017. Health care–associated infections were defined as those with onset in a health care facility or associated with recent admission to a health care facility; all others were classified as community-associated infections. For trend analyses, we used weighted random-intercept models with negative binomial distribution and logistic-regression models to adjust for the higher sensitivity of nucleic acid amplification tests (NAATs) as compared with other test types. RESULTS: The number of cases of C. difficile infection in the 10 U.S. sites was 15,461 in 2011 (10,177 health care–associated and 5284 community-associated cases) and 15,512 in 2017 (7973 health care–associated and 7539 community-associated cases). The estimated national burden of C. difficile infection was 476,400 cases (95% confidence interval [CI], 419,900 to 532,900) in 2011 and 462,100 cases (95% CI, 428,600 to 495,600) in 2017. With accounting for NAAT use, the adjusted estimate of the total burden of C. difficile infection decreased by 24% (95% CI, 6 to 36) from 2011 through 2017; the adjusted estimate of the national burden of health care–associated C. difficile infection decreased by 36% (95% CI, 24 to 54), whereas the adjusted estimate of the national burden of community-associated C. difficile infection was unchanged. The adjusted estimate of the burden of hospitalizations for C. difficile infection decreased by 24% (95% CI, 0 to 48), whereas the adjusted estimates of the burden of first recurrences and in-hospital deaths did not change significantly. CONCLUSIONS: The estimated national burden of C. difficile infection and associated hospitalizations decreased from 2011 through 2017, owing to a decline in health care–associated infections. (Funded by the Centers for Disease Control and Prevention.)

Published

2020

16. Web Exclusive. Annals On Call - C difficile: The Most Common Health Care-Associated Infection in the United States

Author

Robert M, Centor, Alice Y, Guh, and Preeta K, Kutty

Published

2019

17. Outbreak Investigations

Author

Alison Laufer Halpin, Alice Y. Guh, and Alexander J. Kallen

Published

2018

18. Using PCR-based detection and genotyping to trace Streptococcus salivarius meningitis outbreak strain to oral flora of radiology physician assistant.

Author

Velusamy Srinivasan, Robert E Gertz, Patricia L Shewmaker, Sarah Patrick, Amit S Chitnis, Heather O'Connell, Isaac Benowitz, Priti Patel, Alice Y Guh, Judith Noble-Wang, George Turabelidze, and Bernard Beall

Subjects

Medicine, Science

Abstract

We recently investigated three cases of bacterial meningitis that were reported from a midwestern radiology clinic where facemasks were not worn during spinal injection of contrast agent during myelography procedures. Using pulsed field gel electrophoresis we linked a case strain of S. salivarius to an oral specimen of a radiology physician assistant (RPA). We also used a real-time PCR assay to detect S. salivarius DNA within a culture-negative cerebrospinal fluid (CSF) specimen. Here we extend this investigation through using a nested PCR/sequencing strategy to link the culture-negative CSF specimen to the case strain. We also provide validation of the real-time PCR assay used, demonstrating that it is not solely specific for Streptococcus salivarius, but is also highly sensitive for detection of the closely related oral species Streptococcus vestibularis. Through using multilocus sequence typing and 16S rDNA sequencing we further strengthen the link between the CSF case isolate and the RPA carriage isolate. We also demonstrate that the newly characterized strains from this study are distinct from previously characterized S. salivarius strains associated with carriage and meningitis.

Published

2012