Your search keyword '"Kimberly A. Reske"' showing total 90 results

1. Genomic surveillance of Clostridioides difficile transmission and virulence in a healthcare setting

Author

Erin P. Newcomer, Skye R. S. Fishbein, Kailun Zhang, Tiffany Hink, Kimberly A. Reske, Candice Cass, Zainab H. Iqbal, Emily L. Struttmann, Carey-Ann D. Burnham, Erik R. Dubberke, and Gautam Dantas

Subjects

C. difficile infection, transmission, whole-genome sequencing, virulence factors, pathogens, antibiotic resistance, Microbiology, QR1-502

Abstract

ABSTRACT Clostridioides difficile infection (CDI) is a major cause of healthcare-associated diarrhea, despite the widespread implementation of contact precautions for patients with CDI. Here, we investigate strain contamination in a hospital setting and the genomic determinants of disease outcomes. Across two wards over 6 months, we selectively cultured C. difficile from patients (n = 384) and their environments. Whole-genome sequencing (WGS) of 146 isolates revealed that most C. difficile isolates were from clade 1 (131/146, 89.7%), while only one isolate of the hypervirulent ST1 was recovered. Of culture-positive admissions (n = 79), 19 (24%) patients were colonized with toxigenic C. difficile on admission to the hospital. We defined 25 strain networks at ≤2 core gene single nucleotide polymorphisms; two of these networks contain strains from different patients. Strain networks were temporally linked (P < 0.0001). To understand the genomic correlates of the disease, we conducted WGS on an additional cohort of C. difficile (n = 102 isolates) from the same hospital and confirmed that clade 1 isolates are responsible for most CDI cases. We found that while toxigenic C. difficile isolates are associated with the presence of cdtR, nontoxigenic isolates have an increased abundance of prophages. Our pangenomic analysis of clade 1 isolates suggests that while toxin genes (tcdABER and cdtR) were associated with CDI symptoms, they are dispensable for patient colonization. These data indicate that toxigenic and nontoxigenic C. difficile contamination persist in a hospital setting and highlight further investigation into how accessory genomic repertoires contribute to C. difficile colonization and disease.IMPORTANCEClostridioides difficile infection remains a leading cause of hospital-associated diarrhea, despite increased antibiotic stewardship and transmission prevention strategies. This suggests a changing genomic landscape of C. difficile. Our study provides insight into the nature of prevalent C. difficile strains in a hospital setting and transmission patterns among carriers. Longitudinal sampling of surfaces and patient stool revealed that both toxigenic and nontoxigenic strains of C. difficile clade 1 dominate these two wards. Moreover, quantification of transmission in carriers of these clade 1 isolates underscores the need to revisit infection prevention measures in this patient group. We identified unique genetic signatures associated with virulence in this clade. Our data highlight the complexities of preventing transmission of this pathogen in a hospital setting and the need to investigate the mechanisms of in vivo persistence and virulence of prevalent lineages in the host gut microbiome.

Published

2024

2. Epidemiology of Plasmid Lineages Mediating the Spread of Extended-Spectrum Beta-Lactamases among Clinical Escherichia coli

Author

Bejan Mahmud, Meghan A. Wallace, Kimberly A. Reske, Kelly Alvarado, Carol E. Muenks, David A. Rasmussen, Carey-Ann D. Burnham, Cristina Lanzas, Erik R. Dubberke, and Gautam Dantas

Subjects

Escherichia coli, beta-lactamases, plasmid-mediated resistance, Microbiology, QR1-502

Abstract

ABSTRACT The prevalence of extended-spectrum beta-lactamases (ESBLs) among clinical isolates of Escherichia coli has been increasing, with this spread driven by ESBL-encoding plasmids. However, the epidemiology of ESBL-disseminating plasmids remains understudied, obscuring the roles of individual plasmid lineages in ESBL spread. To address this, we performed an in-depth genomic investigation of 149 clinical ESBL-like E. coli isolates from a tertiary care hospital. We obtained high-quality assemblies for 446 plasmids, revealing an extensive map of plasmid sharing that crosses time, space, and bacterial sequence type boundaries. Through a sequence-based network, we identified specific plasmid lineages that are responsible for the dissemination of major ESBLs. Notably, we demonstrate that IncF plasmids separate into 2 distinct lineages that are enriched for different ESBLs and occupy distinct host ranges. Our work provides a detailed picture of plasmid-mediated spread of ESBLs, demonstrating the extensive sequence diversity within identified lineages, while highlighting the genetic elements that underlie the persistence of these plasmids within the clinical E. coli population. IMPORTANCE The increasing incidence of nosocomial infections with extended-spectrum beta-lactamase (ESBL)-producing Escherichia coli represents a significant threat to public health, given the limited treatment options available for such infections. The rapid ESBL spread is suggested to be driven by localization of the resistance genes on conjugative plasmids. Here, we identify the contributions of different plasmid lineages in the nosocomial spread of ESBLs. We provide further support for plasmid-mediated spread of ESBLs but demonstrate that some ESBL genes rely on dissemination through plasmids more than the others. We identify key plasmid lineages that are enriched in major ESBL genes and highlight the encoded genetic elements that facilitate the transmission and stable maintenance of these plasmid groups within the clinical E. coli population. Overall, our work provides valuable insight into the dissemination of ESBLs through plasmids, furthering our understating of factors underlying the increased prevalence of these genes in nosocomial settings.

Published

2022

3. Microbiota restoration reduces antibiotic-resistant bacteria gut colonization in patients with recurrent Clostridioides difficile infection from the open-label PUNCH CD study

Author

Amy Langdon, Drew J. Schwartz, Christopher Bulow, Xiaoqing Sun, Tiffany Hink, Kimberly A. Reske, Courtney Jones, Carey-Ann D. Burnham, Erik R. Dubberke, Gautam Dantas, and for the CDC Prevention Epicenter Program

Subjects

Fecal microbiota transplantation, Multidrug resistance, Antibiotic resistance, Metagenomics, Microbiome, Clostridioides difficile, Medicine, Genetics, QH426-470

Abstract

Abstract Background Once antibiotic-resistant bacteria become established within the gut microbiota, they can cause infections in the host and be transmitted to other people and the environment. Currently, there are no effective modalities for decreasing or preventing colonization by antibiotic-resistant bacteria. Intestinal microbiota restoration can prevent Clostridioides difficile infection (CDI) recurrences. Another potential application of microbiota restoration is suppression of non-C. difficile multidrug-resistant bacteria and overall decrease in the abundance of antibiotic resistance genes (the resistome) within the gut microbiota. This study characterizes the effects of RBX2660, a microbiota-based investigational therapeutic, on the composition and abundance of the gut microbiota and resistome, as well as multidrug-resistant organism carriage, after delivery to patients suffering from recurrent CDI. Methods An open-label, multi-center clinical trial in 11 centers in the USA for the safety and efficacy of RBX2660 on recurrent CDI was conducted. Fecal specimens from 29 of these subjects with recurrent CDI who received either one (N = 16) or two doses of RBX2660 (N = 13) were analyzed secondarily. Stool samples were collected prior to and at intervals up to 6 months post-therapy and analyzed in three ways: (1) 16S rRNA gene sequencing for microbiota taxonomic composition, (2) whole metagenome shotgun sequencing for functional pathways and antibiotic resistome content, and (3) selective and differential bacterial culturing followed by isolate genome sequencing to longitudinally track multidrug-resistant organisms. Results Successful prevention of CDI recurrence with RBX2660 correlated with taxonomic convergence of patient microbiota to the donor microbiota as measured by weighted UniFrac distance. RBX2660 dramatically reduced the abundance of antibiotic-resistant Enterobacteriaceae in the 2 months after administration. Fecal antibiotic resistance gene carriage decreased in direct relationship to the degree to which donor microbiota engrafted. Conclusions Microbiota-based therapeutics reduce resistance gene abundance and resistant organisms in the recipient gut microbiome. This approach could potentially reduce the risk of infections caused by resistant organisms within the patient and the transfer of resistance genes or pathogens to others. Trial registration ClinicalTrials.gov, NCT01925417 ; registered on August 19, 2013.

Published

2021

4. Impact of investigational microbiota therapeutic RBX2660 on the gut microbiome and resistome revealed by a placebo-controlled clinical trial

Author

Suryang Kwak, JooHee Choi, Tiffany Hink, Kimberly A. Reske, Kenneth Blount, Courtney Jones, Margaret H. Bost, Xiaoqing Sun, Carey-Ann D. Burnham, Erik R. Dubberke, Gautam Dantas, and for the CDC Prevention Epicenter Program

Subjects

Microbiota-based therapy, Placebo, Microbiome, Resistome, Clostridioides difficile infection, Antibiotic-resistant organisms, Microbial ecology, QR100-130

Abstract

Abstract Background Intestinal microbiota restoration can be achieved by complementing a subject’s perturbed microbiota with that of a healthy donor. Recurrent Clostridioides difficile infection (rCDI) is one key application of such treatment. Another emerging application of interest is reducing antibiotic-resistant genes (ARGs) and organisms (AROs). In this study, we investigated fecal specimens from a multicenter, randomized, double-blind, placebo-controlled phase 2b study of microbiota-based investigational drug RBX2660. Patients were administered either placebo, 1 dose of RBX2660 and 1 placebo, or 2 doses of RBX2660 via enema and longitudinally tracked for changes in their microbiome and antibiotic resistome. Results All patients exhibited significant recovery of gut microbiome diversity and a decrease of ARG relative abundance during the first 7 days post-treatment. However, the microbiome and resistome shifts toward average configurations from unperturbed individuals were more significant and longer-lasting in RBX2660 recipients compared to placebo. We quantified microbiome and resistome modification by RBX2660 using a novel “transplantation index” metric. We identified taxonomic and metabolic features distinguishing the baseline microbiome of non-transplanted patients and taxa specifically enriched during the process of transplantation. We elucidated the correlation between resistome and taxonomic transplantations and post-treatment dynamics of patient-specific and RBX2660-specific ARGs. Whole genome sequencing of AROs cultured from RBX2660 product and patient samples indicate ARO eradication in patients via RBX2660 administration, but also, to a lesser extent, introduction of RBX2660-derived AROs. Conclusions Through shotgun metagenomic sequencing, we elucidated the effects of RBX2660 in the microbiome and resistome. Antibiotic discontinuation alone resulted in significant recovery of gut microbial diversity and reduced ARG relative abundance, but RBX2660 administration more rapidly and completely changed the composition of patients’ microbiome, resistome, and ARO colonization by transplanting RBX2660 microbiota into the recipients. Although ARGs and AROs were transmitted through RBX2660, the resistome post-RBX2660 more closely resembled that of the administered product—a proxy for the donor—than an antibiotic perturbed state. Trial registration ClinicalTrials.gov, NCT02299570 . Registered 19 November 2014 Video Abstract

Published

2020

5. Isolation of SARS-CoV-2 in Viral Cell Culture in Immunocompromised Patients With Persistently Positive RT-PCR Results

Author

Abby Sung, Adam L. Bailey, Henry B. Stewart, David McDonald, Meghan A. Wallace, Kate Peacock, Candace Miller, Kimberly A. Reske, Caroline A. O’Neil, Victoria J. Fraser, Michael S. Diamond, Carey-Ann D. Burnham, Hilary M. Babcock, and Jennie H. Kwon

Subjects

COVID-19, SARS-CoV-2, immunocompromised, rituximab, obinutuzumab, laboratory medicine, Microbiology, QR1-502

Abstract

Immunocompromised adults can have prolonged acute respiratory syndrome coronavirus 2 (SARS-CoV-2) positive RT-PCR results, long after the initial diagnosis of coronavirus disease 2019 (COVID-19). This study aimed to determine if SARS-CoV-2 virus can be recovered in viral cell culture from immunocompromised adults with persistently positive SARS-CoV-2 RT-PCR tests. We obtained 20 remnant SARS-CoV-2 PCR positive nasopharyngeal swabs from 20 immunocompromised adults with a positive RT-PCR test ≥14 days after the initial positive test. The patients’ 2nd test samples underwent SARS-CoV-2 antigen testing, and culture with Vero-hACE2-TMPRSS2 cells. Viral RNA and cultivable virus were recovered from the cultured cells after qRT-PCR and plaque assays. Of 20 patients, 10 (50%) had a solid organ transplant and 5 (25%) had a hematologic malignancy. For most patients, RT-PCR Ct values increased over time. There were 2 patients with positive viral cell cultures; one patient had chronic lymphocytic leukemia treated with venetoclax and obinutuzumab who had a low viral titer of 27 PFU/mL. The second patient had marginal zone lymphoma treated with bendamustine and rituximab who had a high viral titer of 2 x 106 PFU/mL. Most samples collected ≥7 days after an initial positive SARS-CoV-2 RT-PCR had negative viral cell cultures. The 2 patients with positive viral cell cultures had hematologic malignancies treated with chemotherapy and B cell depleting therapy. One patient had a high concentration titer of cultivable virus. Further data are needed to determine risk factors for persistent viral shedding and methods to prevent SARS-CoV-2 transmission from immunocompromised hosts.

Published

2022

6. Predictors of humoral response to SARS-CoV-2 mRNA vaccine BNT162b2 in patients receiving maintenance dialysis

Author

Tingting Li, Sumanth Gandra, Kimberly A. Reske, Margaret A. Olsen, Silvana Bommarito, Candace Miller, Karl G. Hock, Claire A. Ballman, Christina Su, Na Le Dang, Jennie H. Kwon, David K. Warren, Victoria J. Fraser, Christopher W. Farnsworth, and for the Centers for Disease Control and Prevention Epicenters Program

Subjects

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

Abstract

Abstract Objective: Patients on dialysis are at high risk for severe COVID-19 and associated morbidity and mortality. We examined the humoral response to SARS-CoV-2 mRNA vaccine BNT162b2 in a maintenance dialysis population. Design: Single-center cohort study. Setting and participants: Adult maintenance dialysis patients at 3 outpatient dialysis units of a large academic center. Methods: Participants were vaccinated with 2 doses of BNT162b2, 3 weeks apart. We assessed anti–SARS-CoV-2 spike antibodies (anti-S) ∼4–7 weeks after the second dose and evaluated risk factors associated with insufficient response. Definitions of antibody response are as follows: nonresponse (anti-S level,

Published

2022

7. Longitudinal analysis of risk factors associated with severe acute respiratory coronavirus virus 2 (SARS-CoV-2) infection among hemodialysis patients and healthcare personnel in outpatient hemodialysis centers

Author

Sumanth Gandra, Tingting Li, Kimberly A. Reske, Kate Peacock, Karl G. Hock, Silvana Bommarito, Candace Miller, Henry Stewart, Na Le Dang, Christopher W. Farnsworth, Margaret A. Olsen, Jennie H. Kwon, David K. Warren, Victoria J. Fraser, and for the CDC Prevention Epicenters Program

Subjects

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

Abstract

In this prospective, longitudinal study, we examined the risk factors for severe acute respiratory coronavirus virus 2 (SARS-CoV-2) infection among a cohort of chronic hemodialysis (HD) patients and healthcare personnel (HCPs) over a 6-month period. The risk of SARS-CoV-2 infection among HD patients and HCPs was consistently associated with a household member having SARS-CoV-2 infection.

Published

2022

8. Microbiology Clinical Culture Diagnostic Yields and Antimicrobial Resistance Proportions before and during the COVID-19 Pandemic in an Indian Community Hospital and Two US Community Hospitals

Author

Sumanth Gandra, Gerardo Alvarez-Uria, Dustin Stwalley, Katelin B. Nickel, Kimberly A. Reske, Jennie H. Kwon, Erik R. Dubberke, Margaret A. Olsen, and Jason P. Burnham

Subjects

COVID-19, microbiology, antimicrobial resistance, Therapeutics. Pharmacology, RM1-950

Abstract

Studies comparing the impact of the COVID-19 pandemic on diagnostic microbiology culture yields and antimicrobial resistance proportions in low-to-middle-income and high-income countries are lacking. A retrospective study using blood, respiratory, and urine microbiology data from a community hospital in India and two community hospitals (Hospitals A and B) in St. Louis, MO, USA was performed. We compared the proportion of cultures positive for selected multi-drug-resistant organisms (MDROs) listed on the WHO’s priority pathogen list both before the COVID-19 pandemic (January 2017–December 2019) and early in the COVID-19 pandemic (April 2020–October 2020). The proportion of blood cultures contaminated with coagulase-negative Staphylococcus (CONS) was significantly higher during the pandemic in all three hospitals. In the Indian hospital, the proportion of carbapenem-resistant (CR) Klebsiella pneumoniae in respiratory cultures was significantly higher during the pandemic period, as was the proportion of CR Escherichia coli in urine cultures. In the US hospitals, the proportion of methicillin-resistant Staphylococcus aureus in blood cultures was significantly higher during the pandemic period in Hospital A, while no significant increase in the proportion of Gram-negative MDROs was observed. Continuity of antimicrobial stewardship activities and better infection prevention measures are critical to optimize outcomes and minimize the burden of antimicrobial resistance among COVID-19 patients.

Published

2023

9. Randomized Controlled Trial of Oral Vancomycin Treatment in Clostridioides difficile-Colonized Patients

Author

Skye R. S. Fishbein, Tiffany Hink, Kimberly A. Reske, Candice Cass, Emily Struttmann, Zainab Hassan Iqbal, Sondra Seiler, Jennie H. Kwon, Carey-Ann D. Burnham, Gautam Dantas, and Erik R. Dubberke

Subjects

Microbiology, QR1-502

Abstract

A gold standard diagnostic for Clostridioides difficile

Published

2021

10. Comparative Genomics of Antibiotic-Resistant Uropathogens Implicates Three Routes for Recurrence of Urinary Tract Infections

Author

Robert Thänert, Kimberly A. Reske, Tiffany Hink, Meghan A. Wallace, Bin Wang, Drew J. Schwartz, Sondra Seiler, Candice Cass, Carey-Ann D. Burnham, Erik R. Dubberke, Jennie H. Kwon, and Gautam Dantas

Subjects

antibiotic resistance, clonal tracking, comparative genomics, recurrence, urinary tract infection, Microbiology, QR1-502

Abstract

ABSTRACT The rise of antimicrobial resistance in uropathogens has complicated the management of urinary tract infections (UTIs), particularly in patients who are afflicted by recurrent episodes of UTIs. Antimicrobial-resistant (AR) uropathogens persistently colonizing individuals at asymptomatic time points have been implicated in the pathophysiology of UTIs. The dynamics of uropathogen persistence following the resolution of symptomatic disease are, however, mostly unclear. To further our understanding, we determined longitudinal AR uropathogen carriage and clonal persistence of uropathogenic Escherichia coli, Proteus mirabilis, and Klebsiella pneumoniae isolates in the intestinal and urinary tracts of patients affected by recurrent and nonrecurrent UTIs. Clonal tracking of isolates in consecutively collected urine and fecal specimens indicated repeated transmission of uropathogens between the urinary tract and their intestinal reservoir. Our results further implicate three independent routes of recurrence of UTIs: (i) following an intestinal bloom of uropathogenic bacteria and subsequent bladder colonization, (ii) reinfection of the urinary tract from an external source, and (iii) bacterial persistence within the urinary tract. Taken together, our observation of clonal persistence following UTIs and uropathogen transmission between the intestinal and urinary tracts warrants further investigations into the connection between the intestinal microbiome and recurrent UTIs. IMPORTANCE The increasing antimicrobial resistance of uropathogens is challenging the continued efficacy of empiric antibiotic therapy for UTIs, which are among the most frequent bacterial infections worldwide. It has been suggested that drug-resistant uropathogens could persist in the intestine after the resolution of UTI and cause recurrences following periurethral contamination. A better understanding of the transmission dynamics between the intestinal and urinary tracts, combined with phenotypic characterization of the uropathogen populations in both habitats, could inform prudent therapies designed to overcome the rising resistance of uropathogens. Here, we integrate genomic surveillance with clinical microbiology to show that drug-resistant clones persist within and are readily transmitted between the intestinal and urinary tracts of patients affected by recurrent and nonrecurrent UTIs. Thus, our results advocate for understanding persistent intestinal uropathogen colonization as part of the pathophysiology of UTIs, particularly in patients affected by recurrent episodes of symptomatic disease.

Published

2019

11. Impact of Amoxicillin-Clavulanate followed by Autologous Fecal Microbiota Transplantation on Fecal Microbiome Structure and Metabolic Potential

Author

Christopher Bulow, Amy Langdon, Tiffany Hink, Meghan Wallace, Kimberly A. Reske, Sanket Patel, Xiaoqing Sun, Sondra Seiler, Susan Jones, Jennie H. Kwon, Carey-Ann D. Burnham, Gautam Dantas, and Erik R. Dubberke

Subjects

antimicrobial resistance, fecal microbiota transplantation, metagenomics, microbiome, multidrug resistance, Microbiology, QR1-502

Abstract

ABSTRACT Strategies to prevent multidrug-resistant organism (MDRO) infections are scarce, but autologous fecal microbiota transplantation (autoFMT) may limit gastrointestinal MDRO expansion. AutoFMT involves banking one’s feces during a healthy state for later use in restoring gut microbiota following perturbation. This pilot study evaluated the effect of autoFMT on gastrointestinal microbiome taxonomic composition, resistance gene content, and metabolic capacity after exposure to amoxicillin-clavulanic acid (Amox-Clav). Ten healthy participants were enrolled. All received 5 days of Amox-Clav. Half were randomized to autoFMT, derived from stool collected pre-antimicrobial exposure, by enema, and half to saline enema. Participants submitted stool samples pre- and post-Amox-Clav and enema and during a 90-day follow-up period. Shotgun metagenomic sequencing revealed taxonomic composition, resistance gene content, and metabolic capacity. Amox-Clav significantly altered gut taxonomic composition in all participants (n = 10, P 0.05, compared to enrollment). Alterations to microbial metabolic capacity occurred following antimicrobial exposure even in participants without substantial taxonomic disruption, potentially creating open niches for pathogen colonization. Our findings suggest that metabolic potential is an important consideration for complete assessment of antimicrobial impact on the microbiome. AutoFMT was well tolerated and may have contributed to phylogenetic recovery. (This study has been registered at ClinicalTrials.gov under identifier NCT02046525.) IMPORTANCE The spread of multidrug resistance among pathogenic organisms threatens the efficacy of antimicrobial treatment options. The human gut serves as a reservoir for many drug-resistant organisms and their resistance genes, and perturbation of the gut microbiome by antimicrobial exposure can open metabolic niches to resistant pathogens. Once established in the gut, antimicrobial-resistant bacteria can persist even after antimicrobial exposure ceases. Strategies to prevent multidrug-resistant organism (MDRO) infections are scarce, but autologous fecal microbiota transplantation (autoFMT) may limit gastrointestinal MDRO expansion. AutoFMT involves banking one’s feces during a healthy state for later use in restoring gut microbiota following perturbation. This pilot study evaluated the effect of amoxicillin-clavulanic acid (Amox-Clav) exposure and autoFMT on gastrointestinal microbiome taxonomic composition, resistance gene content, and metabolic capacity. Importantly, we found that metabolic capacity was perturbed even in cases where gross phylogeny remained unchanged and that autoFMT was safe and well tolerated.

Published

2018

12. Attributable Outcomes of Endemic Clostridium difficile–associated Disease in Nonsurgical Patients

Author

Erik R. Dubberke, Anne M. Butler, Kimberly A. Reske, Denis Agniel, Margaret A. Olsen, Gina D’Angelo, L. Clifford McDonald, and Victoria J. Fraser

Subjects

Clostridium difficile, attributable mortality, outcomes, healthcare epidemiology, hospital-associated infections, research, Medicine, Infectious and parasitic diseases, RC109-216

Abstract

Data are limited on the attributable outcomes of Clostridium difficile–associated disease (CDAD), particularly in CDAD-endemic settings. We conducted a retrospective cohort study of nonsurgical inpatients admitted for >48 hours in 2003 (N = 18,050). The adjusted hazard ratios for readmission (hazard ratio 2.19, 95% confidence interval [CI] 1.87–2.55) and deaths within 180 days (hazard ratio 1.23, 95% CI 1.03–1.46) were significantly different among CDAD case-patients and noncase patients. In a propensity score matched-pairs analysis that used a nested subset of the cohort (N = 706), attributable length of stay attributable to CDAD was 2.8 days, attributable readmission at 180 days was 19.3%, and attributable death at 180 days was 5.7%. CDAD patients were significantly more likely than controls to be discharged to a long-term-care facility or outside hospital. Even in a nonoutbreak setting, CDAD had a statistically significant negative impact on patient illness and death, and the impact of CDAD persisted beyond hospital discharge.

Published

2008

13. Multi-omics investigation of Clostridioides difficile-colonized patients reveals pathogen and commensal correlates of C. difficile pathogenesis

Author

Skye RS Fishbein, John I Robinson, Tiffany Hink, Kimberly A Reske, Erin P Newcomer, Carey-Ann D Burnham, Jeffrey P Henderson, Erik R Dubberke, and Gautam Dantas

Subjects

Clostridioides difficile, gut microbiome, colonization resistance, Medicine, Science, Biology (General), QH301-705.5

Abstract

Clostridioides difficile infection (CDI) imposes a substantial burden on the health care system in the United States. Understanding the biological basis for the spectrum of C. difficile-related disease manifestations is imperative to improving treatment and prevention of CDI. Here, we investigate the correlates of asymptomatic C. difficile colonization using a multi-omics approach. We compared the fecal microbiome and metabolome profiles of patients with CDI versus asymptomatically colonized patients, integrating clinical and pathogen factors into our analysis. We found that CDI patients were more likely to be colonized by strains with the binary toxin (CDT) locus or strains of ribotype 027, which are often hypervirulent. We find that microbiomes of asymptomatically colonized patients are significantly enriched for species in the class Clostridia relative to those of symptomatic patients. Relative to CDI microbiomes, asymptomatically colonized patient microbiomes were enriched with sucrose degradation pathways encoded by commensal Clostridia, in addition to glycoside hydrolases putatively involved in starch and sucrose degradation. Fecal metabolomics corroborates the carbohydrate degradation signature: we identify carbohydrate compounds enriched in asymptomatically colonized patients relative to CDI patients. Further, we reveal that across C. difficile isolates, the carbohydrates sucrose, rhamnose, and lactulose do not serve as robust growth substrates in vitro, consistent with their enriched detection in our metagenomic and metabolite profiling of asymptomatically colonized individuals. We conclude that pathogen genetic variation may be strongly related to disease outcome. More interestingly, we hypothesize that in asymptomatically colonized individuals, carbohydrate metabolism by other commensal Clostridia may prevent CDI by inhibiting C. difficile proliferation. These insights into C. difficile colonization and putative commensal competition suggest novel avenues to develop probiotic or prebiotic therapeutics against CDI.

Published

2022

14. SARS-CoV-2 Infection Risk Factors among Maintenance Hemodialysis Patients and Health Care Personnel In Outpatient Hemodialysis Centers

Author

Christopher W Farnsworth, Jennie H. Kwon, Tingting Li, Victoria J. Fraser, Karl G. Hock, Candace Miller, Na Le Dang, David K. Warren, Sumanth Gandra, Kimberly A. Reske, and Margaret A. Olsen

Subjects

medicine.medical_specialty, Infection risk, viruses, medicine.medical_treatment, Severe acute respiratory syndrome coronavirus 2 (SARS-CoV-2), 030232 urology & nephrology, 030204 cardiovascular system & hematology, Brief Communication, 03 medical and health sciences, 0302 clinical medicine, Renal Dialysis, Risk Factors, Outpatients, Health care, medicine, Humans, Infection control, skin and connective tissue diseases, SARS-CoV-2, business.industry, fungi, COVID-19, General Medicine, Maintenance hemodialysis, respiratory tract diseases, body regions, Increased risk, Emergency medicine, Hemodialysis, business, Delivery of Health Care

Abstract

Key Points Increased risk of SARS-CoV-2 infection was associated with community prevalence. Increased risk of SARS-CoV-2 infection was associated with exposure to infected family members and personal infection prevention measures

Published

2021

15. A randomized controlled trial of Lactobacillus rhamnosus GG on antimicrobial-resistant organism colonization

Author

Erik R. Dubberke, Victoria J. Fraser, Cdc Prevention Epicenter Program, Carey-Ann D. Burnham, Sondra Seiler, Adriana M Rauseo, Tiffany Hink, Kimberly A. Reske, and Kerry M. Bommarito

Subjects

Microbiology (medical), medicine.medical_specialty, Epidemiology, medicine.drug_class, Antibiotics, Placebo, Gastroenterology, law.invention, 03 medical and health sciences, Probiotic, 0302 clinical medicine, Randomized controlled trial, Lactobacillus rhamnosus, law, Internal medicine, medicine, Ingestion, Colonization, 030212 general & internal medicine, 0303 health sciences, biology, 030306 microbiology, business.industry, Antimicrobial, biology.organism_classification, Infectious Diseases, business

Abstract

Objective:Alteration of the colonic microbiota following antimicrobial exposure allows colonization by antimicrobial-resistant organisms (AROs). Ingestion of a probiotic, such as Lactobacillus rhamnosus GG (LGG), could prevent colonization or infection with AROs by promoting healthy colonic microbiota. The purpose of this trial was to determine the effect of LGG administration on ARO colonization in hospitalized patients receiving antibiotics.Design:Prospective, double-blinded, randomized controlled trial of LGG versus placebo among patients receiving broad-spectrum antibiotics.Setting:Tertiary care center.Patients:In total, 88 inpatients receiving broad-spectrum antibiotics were enrolled.Intervention:Patients were randomized to receive 1 capsule containing 1×1010 cells of LGG twice daily (n = 44) or placebo (n = 44), stratified by ward type. Stool or rectal-swab specimens were collected for culture at enrollment, during admission, and at discharge. Using selective media, specimens were cultured for Clostridioides difficile, vancomycin-resistant Enterococcus spp (VRE), and antibiotic-resistant gram-negative bacteria. The primary outcome was any ARO acquisition. Secondary outcomes included loss of any ARO if colonized at enrollment, and acquisition or loss of individual ARO.Results:ARO colonization prevalence at study enrollment was similar (LGG 39% vs placebo 39%). We detected no difference in any ARO acquisition (LGG 30% vs placebo 33%; OR,1.19; 95% CI, 0.38–3.75) nor for any individual ARO acquisition. There was no difference in the loss of any ARO (LGG 18% vs placebo 24%; OR, 1.44; 95% CI, 0.27–7.68) nor for any individual ARO.Conclusion:LGG administration neither prevented acquisition of ARO nor accelerated loss of ARO colonization.

Published

2021

16. Using Appropriate Functional Forms for Continuous Variables and Improving Predictive Accuracy in Developing the Risk Model of Clostridium Difficile Infection

Author

Kimberly A. Reske, Yan Yan, Erik R. Dubberke, Graham A. Colditz, and Victoria J. Fraser

Subjects

0301 basic medicine, Regression analysis, Wald test, Regression, 03 medical and health sciences, Spline (mathematics), 030104 developmental biology, 0302 clinical medicine, Vuong's closeness test, 030220 oncology & carcinogenesis, Statistics, Predictive modelling, Parametric statistics, Mathematics, Statistical hypothesis testing

Abstract

Simple parametric functional forms, if appropriate, are preferred over more complicated functional forms in clinical prediction models. In this paper, we illustrate our practical approach to obtaining the appropriate functional forms for continuous variables in developing a clinical prediction model for risk of Clostridium dicile infection. First, we used a nonpara- metric regression smoother to establish the reference curve. Then, we used regression spline function-restricted cubic spline (RCS) and simple para- metric forms to approximate the reference curve. Based on the shape of the reference curve, the model t information (AIC), and the formal statistical test (Vuong test), we selected the simple parametric forms to replace the more elaborated RCS functions. Finally, we rened the simple parametric forms in the multiple variable regression model using the Wald test and the likelihood-ratio test. In addition, we compared the calibration and discrim- ination aspects between the model with appropriate functional forms and the model with simple linear terms. The calibration 2 (8.4 versus 10) and calibration plot, the area under ROC curve (0.88 vs 0.84,p < 0:05), and inte- grated discrimination improvement (0.0072, p < 0:001) indicated the model with appropriate forms was better calibrated and had higher discrimination ability.

Published

2021

17. Strategies to prevent adverse outcomes following Clostridioides difficile infection in the elderly

Author

Margaret A. Olsen, Adriana M Rauseo, Erik R. Dubberke, and Kimberly A. Reske

Subjects

0301 basic medicine, Microbiology (medical), medicine.medical_specialty, genetic structures, Adverse outcomes, business.industry, Transmission (medicine), 030106 microbiology, Microbiology, 03 medical and health sciences, 0302 clinical medicine, Infectious Diseases, Susceptible individual, Supportive psychotherapy, Virology, Epidemiology, medicine, Antimicrobial stewardship, Infection control, 030212 general & internal medicine, Intensive care medicine, business, Clostridioides

Abstract

Introduction: Clostridioides difficile remains the most common cause of healthcare-associated infections in the US, and it disproportionately affects the elderly. Older patients are more susceptible and have a greater risk of adverse outcomes from C. difficile infection (CDI), despite advances in treatment and prevention.Areas covered: The epidemiology and pathogenesis of CDI, as well as risk factors in the aging host, will be reviewed. The importance of antimicrobial stewardship and infection prevention in order to avoid acquisition and transmission will be discussed, as well as strategies to prevent adverse outcomes and recurrent CDI, through optimization of CDI treatment s,election.Expert opinion: Appropriate CDI-prevention strategies to avoid adverse outcomes in this susceptible population involve antimicrobial stewardship and methods to prevent C. difficile transmission in healthcare settings. Management strategies to prevent adverse outcomes include initiation of supportive therapy and proper selection of CDI specific treatments. Many patients may also benefit from adjunctive therapies or additional procedures.

Published

2020

18. Assessment of antibiotic-resistant organism transmission among rooms of hospitalized patients, healthcare personnel, and the hospital environment utilizing surrogate markers and selective bacterial cultures

Author

Carey-Ann D. Burnham, Caroline A O'Neil, Tiffany Hink, Jennie H. Kwon, Erik R. Dubberke, Victoria J. Fraser, Stephen Y. Liang, Sondra Seiler, Candice Cass, Kimberly A. Reske, and Meghan A. Wallace

Subjects

Microbiology (medical), medicine.medical_specialty, Microbiological culture, Patients, Epidemiology, Hospitalized patients, Health Personnel, media_common.quotation_subject, education, Pilot Projects, Article, 03 medical and health sciences, 0302 clinical medicine, Hygiene, Drug Resistance, Multiple, Bacterial, Internal medicine, medicine, Humans, Bacteriophages, Hand Hygiene, In patient, 030212 general & internal medicine, media_common, Patient isolation, Academic Medical Centers, Cross Infection, 0303 health sciences, 030306 microbiology, Transmission (medicine), business.industry, Hospitals, Antibiotic resistant organism, Hospitalization, Infectious Diseases, Contact precautions, Equipment Contamination, Guideline Adherence, business

Abstract

Objective:To assess potential transmission of antibiotic-resistant organisms (AROs) using surrogate markers and bacterial cultures.Design:Pilot study.Setting:A 1,260-bed tertiary-care academic medical center.Participants:The study included 25 patients (17 of whom were on contact precautions for AROs) and 77 healthcare personnel (HCP).Methods:Fluorescent powder (FP) and MS2 bacteriophage were applied in patient rooms. HCP visits to each room were observed for 2–4 hours; hand hygiene (HH) compliance was recorded. Surfaces inside and outside the room and HCP skin and clothing were assessed for fluorescence, and swabs were collected for MS2 detection by polymerase chain reaction (PCR) and selective bacterial cultures.Results:Transfer of FP was observed for 20 rooms (80%) and 26 HCP (34%). Transfer of MS2 was detected for 10 rooms (40%) and 15 HCP (19%). Bacterial cultures were positive for 1 room and 8 HCP (10%). Interactions with patients on contact precautions resulted in fewer FP detections than interactions with patients not on precautions (P < .001); MS2 detections did not differ by patient isolation status. Fluorescent powder detections did not differ by HCP type, but MS2 was recovered more frequently from physicians than from nurses (P = .03). Overall, HH compliance was better among HCP caring for patients on contact precautions than among HCP caring for patients not on precautions (P = .003), among nurses than among other nonphysician HCP at room entry (P = .002), and among nurses than among physicians at room exit (P = .03). Moreover, HCP who performed HH prior to assessment had fewer fluorescence detections (P = .008).Conclusions:Contact precautions were associated with greater HCP HH compliance and reduced detection of FP and MS2.

Published

2020

19. Author response: Multi-omics investigation of Clostridioides difficile-colonized patients reveals pathogen and commensal correlates of C. difficile pathogenesis

Author

Skye RS Fishbein, John I Robinson, Tiffany Hink, Kimberly A Reske, Erin P Newcomer, Carey-Ann D Burnham, Jeffrey P Henderson, Erik R Dubberke, and Gautam Dantas

Published

2022

20. Alternative Causes of Infectious Diarrhea in Patients with Negative Tests for Clostridoides Difficile

Author

Caroline A O'Neil, Rachel E Bosserman, Carey-Ann D. Burnham, Erik R. Dubberke, Tiffany Hink, Jennie H. Kwon, and Kimberly A. Reske

Subjects

Diarrhea, medicine.medical_specialty, Salmonella, Adolescent, business.industry, Clostridioides difficile, Norovirus, General Medicine, Articles, medicine.disease_cause, Gastroenterology, Immunoenzyme Techniques, Feces, Rotavirus, Internal medicine, medicine, Humans, In patient, Have Diarrhea, medicine.symptom, Enteropathogenic Escherichia coli, business

Abstract

Background Hospitalized patients with diarrhea who have a negative Clostridoides difficile (C. difficile) test are not routinely evaluated for alternative causes of infectious diarrhea. This study assessed for potential infectious causes of diarrhea in hospitalized patients with an order for repeat C. difficile toxin enzyme immunoassay (tEIA) testing after an initial tEIA test was negative. Methods For patients age ≥18 years who had a second C. difficile tEIA test ordered within 96 h after a negative tEIA test, remnant fecal specimens from the first (negative) tEIA test were evaluated using the BioFire FilmArray Gastrointestinal Panel PCR, C. difficile toxigenic culture, and culture on a blood agar plate (BAP) to identify other potential causes of infectious diarrhea. Growth of organisms on the BAP was also used to assess potential disruptions in the gastrointestinal microbiota. Results Among 84 remnant specimens, toxigenic C. difficile was identified in 9 (11%) by culture or PCR, while potential alternative causes of infectious diarrhea, including norovirus, rotavirus, enteropathogenic Escherichia coli, and Salmonella, were identified in 11 specimens (13%) by PCR. For the majority of patients, no infectious cause of diarrhea was identified, but 84% exhibited disrupted gastrointestinal microbiota, which may contribute to diarrhea. Conclusions When a hospitalized patient has a negative C. difficile tEIA test but continues to have diarrhea, alternative infectious and noninfectious causes of diarrhea should be considered. If the patient has clinical signs and symptoms suggestive of infection or risk factors for gastrointestinal infection, laboratory testing for other etiologic agents may be appropriate.

Published

2021

21. Assessment of dental health care personnel protocol deviations and self-contamination during personal protective equipment donning and doffing

Author

Kimberly A. Reske, Daniel Park, Tracey Habrock Bach, Henry B. Stewart, Lucy C. Vogt, Olivia G. Arter, Daniel Stoeckel, Heidi M. Steinkamp, Stephen Y. Liang, Michael J. Durkin, and Jennie H. Kwon

Subjects

SARS-CoV-2, Health Personnel, Humans, COVID-19, Personal Protective Equipment, Delivery of Health Care, General Dentistry

Abstract

Dental health care personnel (DHCP) may be at increased risk of exposure to severe acute respiratory syndrome coronavirus 2, the virus that causes COVID-19, as well as other clinically important pathogens. Proper use of personal protective equipment (PPE) reduces occupational exposure to pathogens. The authors performed an assessment of PPE donning and doffing practices among DHCP, using a fluorescent marker as a surrogate for pathogen transmission.Participants donned PPE (that is, disposable gown, gloves, face mask, and eye protection) and the fluorescent marker was applied to their palms and abdomen. DHCP then doffed PPE according to their usual practices. The donning and doffing processes were video recorded, areas of fluorescence were noted, and protocol deviations were assessed. Statistical analyses included frequency, type, and descriptions of protocol deviations and factors associated with fluorescence.Seventy DHCP were enrolled. The donning and doffing steps with the highest frequency of protocol deviations were hand hygiene (66% of donning and 78% of doffing observations involved a deviation) and disposable gown use (63% of donning and 60% of doffing observations involved a deviation). Fluorescence was detected on 69% of DHCP after doffing, most frequently on hands. An increasing number of protocol deviations was significantly associated with increased risk of fluorescence. DHCP with a gown doffing deviation, excluding doffing out of order, were more likely to have fluorescence detected.DHCP self-contamination was common with both donning and doffing PPE.Proper use of PPE is an important component of occupational health.

Published

2022

22. Multi-omics investigation of Clostridioides difficile-colonized patients reveals protective commensal carbohydrate metabolism

Author

Erin P. Newcomer, Carey-Ann D. Burnham, Kimberly A. Reske, Tiffany Hink, Gautam Dantas, Jeffrey P. Henderson, Skye R. S. Fishbein, John I. Robinson, and Eric R. Dubberke

Subjects

genetic structures, biology, Rhamnose, Prebiotic, medicine.medical_treatment, Disease, biology.organism_classification, Asymptomatic, Microbiology, law.invention, Clostridia, chemistry.chemical_compound, Probiotic, chemistry, law, medicine, Metabolome, Microbiome, medicine.symptom

Abstract

Clostridioides difficile infection (CDI) imposes a substantial burden on the health care system in the United States. Understanding the biological basis for the spectrum of C. difficile-related disease manifestations is imperative to improving treatment and prevention of CDI. Here, we investigate the correlates of asymptomatic C. difficile colonization using a multi-omics approach, comparing the fecal microbiome and metabolome profiles of patients with CDI versus asymptomatically-colonized patients. We find that microbiomes of asymptomatic patients are significantly enriched for species in the class Clostridia relative to those of symptomatic patients. Asymptomatic patient microbiomes were enriched with fucose, rhamnose, and sucrose degradation pathways relative to CDI patient microbiomes. Fecal metabolomics corroborates this result: we identify carbohydrate compounds enriched in asymptomatic patients relative to CDI patients, and correlated with a number of commensal Clostridia. Further, we reveal that across C. difficile isolates, the carbohydrates rhamnose and lactulose do not serve as robust growth substrates in vitro, corroborating their enriched detection in our metagenomic and metabolite profiling of asymptomatic individuals. We conclude that in asymptomatically-colonized individuals, carbohydrate metabolism by other commensal Clostridia may prevent CDI by inhibiting C. difficile proliferation. These insights into C. difficile colonization and putative commensal competition suggest novel avenues to develop probiotic or prebiotic therapeutics against CDI.

Published

2021

23. Persisting uropathogenic Escherichia coli lineages show signatures of niche-specific within-host adaptation mediated by mobile genetic elements

Author

Robert Thänert, JooHee Choi, Kimberly A. Reske, Tiffany Hink, Anna Thänert, Meghan A. Wallace, Bin Wang, Sondra Seiler, Candice Cass, Margaret H. Bost, Emily L. Struttmann, Zainab Hassan Iqbal, Steven R. Sax, Victoria J. Fraser, Arthur W. Baker, Katherine R. Foy, Brett Williams, Ben Xu, Pam Capocci-Tolomeo, Ebbing Lautenbach, Carey-Ann D. Burnham, Erik R. Dubberke, Jennie H. Kwon, and Gautam Dantas

Subjects

Interspersed Repetitive Sequences, Escherichia coli Proteins, Virology, Urinary Tract Infections, Humans, Uropathogenic Escherichia coli, Parasitology, Host Adaptation, Microbiology, Escherichia coli Infections

Abstract

Large-scale genomic studies have identified within-host adaptation as a hallmark of bacterial infections. However, the impact of physiological, metabolic, and immunological differences between distinct niches on the pathoadaptation of opportunistic pathogens remains elusive. Here, we profile the within-host adaptation and evolutionary trajectories of 976 isolates representing 119 lineages of uropathogenic Escherichia coli (UPEC) sampled longitudinally from both the gastrointestinal and urinary tracts of 123 patients with urinary tract infections. We show that lineages persisting in both niches within a patient exhibit increased allelic diversity. Habitat-specific selection results in niche-specific adaptive mutations and genes, putatively mediating fitness in either environment. Within-lineage inter-habitat genomic plasticity mediated by mobile genetic elements (MGEs) provides the opportunistic pathogen with a mechanism to adapt to the physiological conditions of either habitat, and reduced MGE richness is associated with recurrence in gut-adapted UPEC lineages. Collectively, our results establish niche-specific adaptation as a driver of UPEC within-host evolution.

Published

2022

24. A randomized controlled trial of

Author

Adriana M, Rauseo, Tiffany, Hink, Kimberly A, Reske, Sondra M, Seiler, Kerry M, Bommarito, Victoria J, Fraser, Carey-Ann D, Burnham, and Erik R, Dubberke

Subjects

Lacticaseibacillus rhamnosus, Probiotics, Humans, Prospective Studies, Anti-Bacterial Agents, Vancomycin-Resistant Enterococci

Abstract

Alteration of the colonic microbiota following antimicrobial exposure allows colonization by antimicrobial-resistant organisms (AROs). Ingestion of a probiotic, such as Lactobacillus rhamnosus GG (LGG), could prevent colonization or infection with AROs by promoting healthy colonic microbiota. The purpose of this trial was to determine the effect of LGG administration on ARO colonization in hospitalized patients receiving antibiotics.Prospective, double-blinded, randomized controlled trial of LGG versus placebo among patients receiving broad-spectrum antibiotics.Tertiary care center.In total, 88 inpatients receiving broad-spectrum antibiotics were enrolled.Patients were randomized to receive 1 capsule containing 1×1010 cells of LGG twice daily (n = 44) or placebo (n = 44), stratified by ward type. Stool or rectal-swab specimens were collected for culture at enrollment, during admission, and at discharge. Using selective media, specimens were cultured for Clostridioides difficile, vancomycin-resistant Enterococcus spp (VRE), and antibiotic-resistant gram-negative bacteria. The primary outcome was any ARO acquisition. Secondary outcomes included loss of any ARO if colonized at enrollment, and acquisition or loss of individual ARO.ARO colonization prevalence at study enrollment was similar (LGG 39% vs placebo 39%). We detected no difference in any ARO acquisition (LGG 30% vs placebo 33%; OR,1.19; 95% CI, 0.38-3.75) nor for any individual ARO acquisition. There was no difference in the loss of any ARO (LGG 18% vs placebo 24%; OR, 1.44; 95% CI, 0.27-7.68) nor for any individual ARO.LGG administration neither prevented acquisition of ARO nor accelerated loss of ARO colonization.

Published

2021

25. The Role of Diagnostic Stewardship in

Author

Frances J, Boly, Kimberly A, Reske, and Jennie H, Kwon

Subjects

genetic structures, Article

Abstract

PURPOSE OF REVIEW: Accurate and timely diagnosis of Clostridioides difficile infection (CDI) is imperative to prevent C. difficile transmission and reduce morbidity and mortality due to CDI, but CDI laboratory diagnostics are complex. The purpose of this article is to review the role of laboratory tests in the diagnosis of CDI, and the role of diagnostic stewardship in optimization of C. difficile testing. RECENT FINDINGS: Results from C. difficile diagnostic tests should be interpreted with an understanding of the strengths and limitations inherent in each testing approach. Use of highly sensitive molecular diagnostic tests without accounting for clinical signs and symptoms may lead to over-diagnosis of CDI and increased facility CDI rates. Current guidelines recommend a two-step, algorithmic approach for testing. Diagnostic stewardship interventions, such as education, order sets, order search menus, reflex orders, hard and soft stop alerts, electronic references, feedback and benchmarking, decision algorithms, and predictive analytics may help improve use of C. difficile laboratory tests and CDI diagnosis. The diagnostic stewardship approaches with the highest reported success rates include computerized clinical decision support (CCDS) interventions, face-to-face feedback, and real-time evaluations. SUMMARY: CDI is a clinical diagnosis supported by laboratory findings. Together, clinical evaluation combined with diagnostic stewardship can optimize the accurate diagnosis of CDI.

Published

2021

26. Randomized Controlled Trial of Oral Vancomycin Treatment in Clostridioides difficile-Colonized Patients

Author

Candice Cass, Gautam Dantas, Zainab Hassan Iqbal, Skye R. S. Fishbein, Kimberly A. Reske, Emily Struttmann, Jennie H. Kwon, Sondra Seiler, Erik R. Dubberke, Carey-Ann D. Burnham, and Tiffany Hink

Subjects

Diarrhea, 0301 basic medicine, medicine.medical_specialty, medicine.drug_class, 030106 microbiology, Antibiotics, Population, Context (language use), Placebo, Microbiology, Host-Microbe Biology, law.invention, 03 medical and health sciences, Clostridioides, Randomized controlled trial, Vancomycin, law, Internal medicine, medicine, Humans, Prospective Studies, education, Molecular Biology, Feces, education.field_of_study, Clostridioides difficile, Transmission (medicine), business.industry, Editor's Pick, vancomycin-resistant enterococci, QR1-502, 030104 developmental biology, C. difficile, business, Research Article, medicine.drug

Abstract

A gold standard diagnostic for Clostridioides difficile infection (CDI) does not exist. An area of controversy is how to manage patients whose stool tests positive by nucleic acid amplification tests but negative by toxin enzyme immunoassay., Clostridioides difficile infection (CDI) is most commonly diagnosed using nucleic acid amplification tests (NAAT); the low positive predictive value of these assays results in patients colonized with C. difficile unnecessarily receiving CDI treatment antibiotics. The risks and benefits of antibiotic treatment in individuals with such cases are unknown. Fecal samples of NAAT-positive, toxin enzyme immunoassay (EIA)-negative patients were collected before, during, and after randomization to vancomycin (n = 8) or placebo (n = 7). C. difficile and antibiotic-resistant organisms (AROs) were selectively cultured from fecal and environmental samples. Shotgun metagenomics and comparative isolate genomics were used to understand the impact of oral vancomycin on the microbiome and environmental contamination. Overall, 80% of placebo patients and 71% of vancomycin patients were colonized with C. difficile posttreatment. One person randomized to placebo subsequently received treatment for CDI. In the vancomycin-treated group, beta-diversity (P = 0.0059) and macrolide-lincosamide-streptogramin (MLS) resistance genes (P = 0.037) increased after treatment; C. difficile and vancomycin-resistant enterococci (VRE) environmental contamination was found in 53% of patients and 26% of patients, respectively. We found that vancomycin alters the gut microbiota, does not permanently clear C. difficile, and is associated with VRE colonization/environmental contamination. (This study has been registered at ClinicalTrials.gov under registration no. NCT03388268.) IMPORTANCE A gold standard diagnostic for Clostridioides difficile infection (CDI) does not exist. An area of controversy is how to manage patients whose stool tests positive by nucleic acid amplification tests but negative by toxin enzyme immunoassay. Existing data suggest most of these patients do not have CDI, but most are treated with oral vancomycin. Potential benefits to treatment include a decreased risk for adverse outcomes if the patient does have CDI and the potential to decrease C. difficile shedding/transmission. However, oral vancomycin perturbs the intestinal microbiota and promotes antibiotic-resistant organism colonization/transmission. We conducted a double-blinded randomized controlled trial to assess the risk-benefit of oral vancomycin treatment in this population. Oral vancomycin did not result in long-term clearance of C. difficile, perturbed the microbiota, and was associated with colonization/shedding of vancomycin-resistant enterococci. This work underscores the need to better understand this population of patients in the context of C. difficile/ARO-related outcomes and transmission.

Published

2021

27. Acute and persistent effects of commonly used antibiotics on the gut microbiome and resistome in healthy adults

Author

Winston E. Anthony, Bin Wang, Kimberley V. Sukhum, Alaric W. D’Souza, Tiffany Hink, Candice Cass, Sondra Seiler, Kimberly A. Reske, Christopher Coon, Erik R. Dubberke, Carey-Ann D. Burnham, Gautam Dantas, and Jennie H. Kwon

Subjects

Adult, Bacteria, Microbiota, Humans, Symbiosis, General Biochemistry, Genetics and Molecular Biology, Anti-Bacterial Agents, Gastrointestinal Microbiome

Abstract

Antibiotics are deployed against bacterial pathogens, but their targeting of conserved microbial processes means they also collaterally perturb the commensal microbiome. To understand acute and persistent effects of antibiotics on the gut microbiota of healthy adult volunteers, we quantify microbiome dynamics before, during, and 6 months after exposure to 4 commonly used antibiotic regimens. We observe an acute decrease in species richness and culturable bacteria after antibiotics, with most healthy adult microbiomes returning to pre-treatment species richness after 2 months, but with an altered taxonomy, resistome, and metabolic output, as well as an increased antibiotic resistance burden. Azithromycin delays the recovery of species richness, resulting in greater compositional distance. A subset of volunteers experience a persistent reduction in microbiome diversity after antibiotics and share compositional similarities with patients hospitalized in intensive care units. These results improve our quantitative understanding of the impact of antibiotics on commensal microbiome dynamics, resilience, and recovery.

Published

2022

28. The effect of microbiota-based investigational drug RBX2660 on the gut microbiome and resistome revealed by a placebo-controlled clinical trial

Author

Margaret H. Bost, Gautam Dantas, Kenneth Blount, Tiffany Hink, Kimberly A. Reske, JooHee Choi, Suryang Kwak, Courtney Jones, Erik R. Dubberke, Carey-Ann D. Burnham, and Xiaoqing Sun

Subjects

Clinical trial, Investigational drug, business.industry, Medicine, Pharmacology, business, Placebo, Gut microbiome, Resistome

Abstract

Background. Intestinal microbiota restoration can be achieved by replacing a subject’s perturbed microbiota with that of a healthy donor. Recurrent Clostridioides difficile infection (rCDI) is one key application of such treatment. Another emerging application of interest is depletion of antibiotic resistant genes (ARGs) and organisms (AROs). In this study, we investigated fecal specimens from a multicenter, randomized, double-blind, placebo-controlled phase 2b study of microbiota-based investigational drug RBX2660. Patients were administered either placebo, 1 dose of RBX2660 and 1 placebo, or 2 doses of RBX2660 via enema and longitudinally tracked for changes in their microbiome and antibiotic resistome. Results. All patients exhibited significant recovery of gut microbiome diversity and a decrease of ARG abundance during the first 7 days post-treatment. However, the microbiome and resistome shifts towards healthier configurations were more significant and longer-lasting in RBX2660 recipients compared to placebo. We quantified microbiome and resistome modification by RBX2660 using a novel ‘transplantation index’ metric. We identified taxonomic and metabolic features distinguishing the baseline microbiome of non-transplanted patients and taxa specifically enriched during the process of transplantation. We elucidated the correlation between resistome and taxonomic transplantations and post-treatment dynamics of patient-specific and RBX2660-specific ARGs. Whole genome sequencing of AROs cultured from RBX2660 product and patient samples indicate ARO eradication in patients via RBX2660 administration, but also, to a lesser extent, introduction of RBX2660-derived AROs. Conclusions. Through shotgun metagenomic sequencing, we elucidated the effects of RBX2660 in the microbiome and resistome. Antibiotic discontinuation alone resulted in significant recovery of gut microbial diversity and reduced ARG abundance, but RBX2660 administration more rapidly and completely changed the composition of patients’ microbiome, resistome, and ARO colonization by transplanting RBX2660 microbiota into the recipients. Although ARGs and AROs were transmitted through RBX2660, the resistome post-RBX2660 more closely resembled that of the administered product—a proxy for the donor—than an antibiotic perturbed state.

Published

2020

29. The Role of Diagnostic Stewardship in Clostridioides difficile Testing: Challenges and Opportunities

Author

Jennie H. Kwon, Kimberly A. Reske, and Frances Boly

Subjects

0301 basic medicine, medicine.medical_specialty, genetic structures, business.industry, 030106 microbiology, Psychological intervention, Signs and symptoms, Predictive analytics, Clinical decision support system, Highly sensitive, 03 medical and health sciences, 0302 clinical medicine, Infectious Diseases, Clinical diagnosis, medicine, 030212 general & internal medicine, Stewardship, Intensive care medicine, business, Clostridioides

Abstract

Accurate and timely diagnosis of Clostridioides difficile infection (CDI) is imperative to prevent C. difficile transmission and reduce morbidity and mortality due to CDI, but CDI laboratory diagnostics are complex. The purpose of this article is to review the role of laboratory tests in the diagnosis of CDI and the role of diagnostic stewardship in optimization of C. difficile testing. Results from C. difficile diagnostic tests should be interpreted with an understanding of the strengths and limitations inherent in each testing approach. Use of highly sensitive molecular diagnostic tests without accounting for clinical signs and symptoms may lead to over-diagnosis of CDI and increased facility CDI rates. Current guidelines recommend a two-step, algorithmic approach for testing. Diagnostic stewardship interventions, such as education, order sets, order search menus, reflex orders, hard and soft stop alerts, electronic references, feedback and benchmarking, decision algorithms, and predictive analytics, may help improve use of C. difficile laboratory tests and CDI diagnosis. The diagnostic stewardship approaches with the highest reported success rates include computerized clinical decision support (CCDS) interventions, face-to-face feedback, and real-time evaluations. CDI is a clinical diagnosis supported by laboratory findings. Together, clinical evaluation combined with diagnostic stewardship can optimize the accurate diagnosis of CDI.

Published

2020

30. Microbiome Restoration by RBX2660 Does Not Preclude Recurrence of Multidrug-Resistant Urinary Tract Infection Following Subsequent Antibiotic Exposure: A Case Report

Author

Eric C. Keen, Erik R. Dubberke, Preston Tasoff, Tiffany Hink, Kimberly A. Reske, Gautam Dantas, Carey-Ann D. Burnham, and Jennie H. Kwon

Subjects

0301 basic medicine, antibiotic resistance, medicine.drug_class, Urinary system, 030106 microbiology, Antibiotics, microbiome, Disease, fecal microbiota transplant, 03 medical and health sciences, 0302 clinical medicine, Antibiotic resistance, Brief Report (Fast track - FIDSA members only), medicine, 030212 general & internal medicine, Microbiome, microbial restoration therapy, business.industry, Antibiotic exposure, 3. Good health, Multiple drug resistance, Infectious Diseases, Carriage, Oncology, Immunology, business, urinary tract infection, human activities

Abstract

A 62-year-old woman received RBX2660, an investigational microbiome restoration therapeutic, for recurrent multidrug-resistant (MDR) urinary tract infection (UTI). RBX2660 increased gut microbiome diversity but did not eliminate uropathogen carriage, and MDR UTI recurred after subsequent antibiotic exposure. Thus, restoration of microbiome diversity does not preclude disease recurrence by residual MDR pathogens.

Published

2020

31. Strategies to prevent adverse outcomes following

Author

Adriana M, Rauseo, Margaret A, Olsen, Kimberly A, Reske, and Erik R, Dubberke

Subjects

Antimicrobial Stewardship, Cross Infection, Clostridioides difficile, Risk Factors, Clostridium Infections, Animals, Humans, Aged, Anti-Bacterial Agents

Published

2020

32. Clostridium difficile colonization among patients with clinically significant diarrhea and no identifiable cause of diarrhea

Author

Jahnavi Bongu, Jeffrey P. Henderson, Carey-Ann D. Burnham, Jennie H. Kwon, Candice Cass, Kimberly A. Reske, Tiffany Hink, and Erik R. Dubberke

Subjects

Diarrhea, 0301 basic medicine, Microbiology (medical), medicine.medical_specialty, Epidemiology, Bacterial Toxins, 030106 microbiology, Stool specimen, Article, Immunoenzyme Techniques, Enterotoxins, Feces, 03 medical and health sciences, 0302 clinical medicine, Chart review, Internal medicine, Prevalence, Humans, Medicine, Colonization, 030212 general & internal medicine, Retrospective Studies, Missouri, Clostridioides difficile, business.industry, Retrospective cohort study, Guideline, Clostridium difficile, Laboratories, Hospital, Clinical microbiology, Infectious Diseases, Clostridium Infections, medicine.symptom, business

Abstract

ObjectiveTo determine the prevalence of Clostridium difficile colonization among patients who meet the 2017 IDSA/SHEA C. difficile infection (CDI) Clinical Guideline Update criteria for the preferred patient population for C. difficile testing.DesignRetrospective cohort.SettingTertiary-care hospital in St. Louis, Missouri.PatientsPatients whose diarrheal stool samples were submitted to the hospital’s clinical microbiology laboratory for C. difficile testing (toxin EIA) from August 2014 to September 2016.InterventionsElectronic and manual chart review were used to determine whether patients tested for C. difficile toxin had clinically significant diarrhea and/or any alternate cause for diarrhea. Toxigenic C. difficile culture was performed on all stool specimens from patients with clinically significant diarrhea and no known alternate cause for their diarrhea.ResultsA total of 8,931 patients with stool specimens submitted were evaluated: 570 stool specimens were EIA positive (+) and 8,361 stool specimens were EIA negative (−). Among the EIA+stool specimens, 107 (19% of total) were deemed eligible for culture. Among the EIA− stool specimens, 515 (6%) were eligible for culture. One EIA+stool specimen (1%) was toxigenic culture negative. Among the EIA− stool specimens that underwent culture, toxigenic C. difficile was isolated from 63 (12%).ConclusionsMost patients tested for C. difficile do not have clinically significant diarrhea and/or potential alternate causes for diarrhea. The prevalence of toxigenic C. difficile colonization among EIA− patients who met the IDSA/SHEA CDI guideline criteria for preferred patient population for C. difficile testing was 12%.

Published

2018

33. Assessment of Healthcare Worker Protocol Deviations and Self-Contamination During Personal Protective Equipment Donning and Doffing

Author

Carey-Ann D. Burnham, Candice Cass, Erik R. Dubberke, Meghan A. Wallace, Angela Shupe, Tiffany Hink, Victoria J. Fraser, Stephen Y. Liang, Kimberly A. Reske, Sondra Seiler, and Jennie H. Kwon

Subjects

Adult, Male, Microbiology (medical), medicine.medical_specialty, Respiratory Protective Device, Ultraviolet Rays, Epidemiology, Health Personnel, Video Recording, Pilot Projects, Protocol Deviation, 030501 epidemiology, Tertiary Care Centers, 03 medical and health sciences, Health personnel, 0302 clinical medicine, Protective Clothing, Humans, Medicine, Infection control, 030212 general & internal medicine, Respiratory Protective Devices, Personal Protective Equipment, Personal protective equipment, Levivirus, Video recording, Infection Control, Missouri, Reverse Transcriptase Polymerase Chain Reaction, business.industry, Guideline adherence, Healthcare worker, Middle Aged, Infectious Diseases, Emergency medicine, Female, Guideline Adherence, Gloves, Protective, 0305 other medical science, business

Abstract

OBJECTIVETo evaluate healthcare worker (HCW) risk of self-contamination when donning and doffing personal protective equipment (PPE) using fluorescence and MS2 bacteriophage.DESIGNProspective pilot study.SETTINGTertiary-care hospital.PARTICIPANTSA total of 36 HCWs were included in this study: 18 donned/doffed contact precaution (CP) PPE and 18 donned/doffed Ebola virus disease (EVD) PPE.INTERVENTIONSHCWs donned PPE according to standard protocols. Fluorescent liquid and MS2 bacteriophage were applied to HCWs. HCWs then doffed their PPE. After doffing, HCWs were scanned for fluorescence and swabbed for MS2. MS2 detection was performed using reverse transcriptase PCR. The donning and doffing processes were videotaped, and protocol deviations were recorded.RESULTSOverall, 27% of EVD PPE HCWs and 50% of CP PPE HCWs made ≥1 protocol deviation while donning, and 100% of EVD PPE HCWs and 67% of CP PPE HCWs made ≥1 protocol deviation while doffing (P=.02). The median number of doffing protocol deviations among EVD PPE HCWs was 4, versus 1 among CP PPE HCWs. Also, 15 EVD PPE protocol deviations were committed by doffing assistants and/or trained observers. Fluorescence was detected on 8 EVD PPE HCWs (44%) and 5 CP PPE HCWs (28%), most commonly on hands. MS2 was recovered from 2 EVD PPE HCWs (11%) and 3 CP PPE HCWs (17%).CONCLUSIONSProtocol deviations were common during both EVD and CP PPE doffing, and some deviations during EVD PPE doffing were committed by the HCW doffing assistant and/or the trained observer. Self-contamination was common. PPE donning/doffing are complex and deserve additional study.Infect Control Hosp Epidemiol 2017;38:1077–1083

Published

2017

34. Evaluation of Correlation between Pretest Probability for Clostridium difficile Infection and Clostridium difficile Enzyme Immunoassay Results

Author

Carey-Ann D. Burnham, Jennie H. Kwon, Kimberly A. Reske, Erik R. Dubberke, and Tiffany Hink

Subjects

Adult, Diarrhea, Male, 0301 basic medicine, Microbiology (medical), medicine.medical_specialty, genetic structures, Bacterial Toxins, 030106 microbiology, Decision Support Techniques, Immunoenzyme Techniques, Correlation, Feces, Young Adult, 03 medical and health sciences, 0302 clinical medicine, Risk Factors, Internal medicine, medicine, Humans, Prospective Studies, 030212 general & internal medicine, Aged, Aged, 80 and over, medicine.diagnostic_test, Clostridioides difficile, business.industry, Bacteriology, Middle Aged, Clostridium difficile, Pre- and post-test probability, Log-rank test, Clinical diagnosis, Immunoassay, Clostridium Infections, Female, medicine.symptom, business, Clinical evaluation

Abstract

The objective of this study was to evaluate the clinical characteristics and outcomes of hospitalized patients tested for Clostridium difficile and determine the correlation between pretest probability for C. difficile infection (CDI) and assay results. Patients with testing ordered for C. difficile were enrolled and assigned a high, medium, or low pretest probability of CDI based on clinical evaluation, laboratory, and imaging results. Stool was tested for C. difficile by toxin enzyme immunoassay (EIA) and toxigenic culture (TC). Chi-square analyses and the log rank test were utilized. Among the 111 patients enrolled, stool samples from nine were TC positive and four were EIA positive. Sixty-one (55%) patients had clinically significant diarrhea, 19 (17%) patients did not, and clinically significant diarrhea could not be determined for 31 (28%) patients. Seventy-two (65%) patients were assessed as having a low pretest probability of having CDI, 34 (31%) as having a medium probability, and 5 (5%) as having a high probability. None of the patients with low pretest probabilities had a positive EIA, but four were TC positive. None of the seven patients with a positive TC but a negative index EIA developed CDI within 30 days after the index test or died within 90 days after the index toxin EIA date. Pretest probability for CDI should be considered prior to ordering C. difficile testing and must be taken into account when interpreting test results. CDI is a clinical diagnosis supported by laboratory data, and the detection of toxigenic C. difficile in stool does not necessarily confirm the diagnosis of CDI.

Published

2017

35. The Gut Microbiome and Resistome of Healthy Volunteers are Restructured After Short Courses of Antibiotics

Author

Kimberly A. Reske, Sondra Seiler, Carey-Ann D. Burnham, Erik R. Dubberke, Bin Wang, Gautam Dantas, Jennie H. Kwon, Candice Cass, Winston E. Anthony, Christopher Coon, Kimberley V. Sukhum, Alaric W. D’Souza, Tiffany Hink, and Sherry Sun

Subjects

Microbiology (medical), Alternative respiration, biology, Epidemiology, Firmicutes, medicine.drug_class, Antibiotics, biology.organism_classification, Cefpodoxime, Microbiology, Resistome, Infectious Diseases, Antibiotic resistance, medicine, Microbiome, Bacteroides, medicine.drug

Abstract

Background: Antimicrobial exposure is a significant risk factor for the development of antibiotic-resistant organisms (ARO); however, the depth and duration of this impact is not well described. The study goal is to define impact of antibiotics on the gut microbiome of healthy volunteers (HVs). Methods: HVs were randomized to receive either 5 days of levofloxacin (LVX), azithromycin (AZM), cefpodoxime (CPD), or AZM + CPD (Fig. 1). Stool samples were collected at 15 time points per patient before, during, and after antibiotics. Remnant stool samples from the microbiology laboratory were collected from patients admitted to the medical intensive care unit (MICU) as a comparison of the microbiome in a critically ill state. DNA was extracted from samples and was submitted for shotgun sequencing. Relative abundance, resistome, and metabolic pathway abundance of bacterial taxa were determined and statistical analysis conducted in R software. Results: In total, 289 stool specimens from 20 HVs, and 26 remnant stool specimens were obtained from patients admitted from the MICU (Fig. 1). Community diversity and richness decreased in the first week post-ABX for all HVs (P < .01). Linear discriminant analysis identified Bacteroides and Clostridium as taxonomic groups enriched after CPD, while AZM and LVX produced a relative abundance increase in diverse Firmicutes spp. Longitudinal tracking confirmed that after all antibiotics except LVX, HV microbiomes lost species diversity and shifted toward a state similar to that observed in MICU patients (Fig. 2). The gut microbiome of most HVs exhibited resiliency and returned to a higher diversity level similar to their starting point; however, 10% of HVs did not. Moreover, antibiotic-specific increases in resistance markers reveal innate resistance to β-lactams and macrolides within the gut microbiome of the HVs. Finally, HV microbiomes, which shifted toward a MICU-like taxonomic state, also clustered with microbial metabolic profiles from MICU patients.The HV microbial metabolic profiles were significantly enriched for important biosynthesis pathways producing chorismate and polysaccharides. MICU patient gut microbiomes were enriched for fatty acid regulation and quinolone biosynthesis, and for many degradation pathways important for different aspects of antibiotic resistance such as membrane integrity, alternative respiration, and antibiotic inactivation. Conclusions: Short courses of antibiotics can cause acute and chronic microbiome disruptions in HVs, as evidenced by decreased microbiome diversity and increases in specific innate resistance elements. These data support the need for antimicrobial stewardship to support rationale antibiotic use to prevent gut microbiome disruptions.Funding: CDC BAA 200-2016-91962Disclosures: None

Published

2020

36. Metabolomic networks connect host-microbiome processes to human Clostridioides difficile infections

Author

Erik R. Dubberke, William Weir, Kimberly A. Reske, Carey-Ann D. Burnham, Jennie H. Kwon, John I. Robinson, Tiffany Hink, Jan R. Crowley, Peter J. Mucha, and Jeffrey P. Henderson

Subjects

0301 basic medicine, genetic structures, medicine.drug_class, Asymptomatic, Microbiology, 03 medical and health sciences, 0302 clinical medicine, medicine, Humans, Colonization, Microbiome, Feces, biology, Bile acid, Clostridioides difficile, Microbiota, General Medicine, biology.organism_classification, Diarrhea, 030104 developmental biology, 030220 oncology & carcinogenesis, Clostridium Infections, medicine.symptom, Leucine, Bacteria, Research Article

Abstract

Clostridioides difficile infection (CDI) accounts for a substantial proportion of deaths attributable to antibiotic-resistant bacteria in the United States. Although C. difficile can be an asymptomatic colonizer, its pathogenic potential is most commonly manifested in patients with antibiotic-modified intestinal microbiomes. In a cohort of 186 hospitalized patients, we showed that host and microbe-associated shifts in fecal metabolomes had the potential to distinguish patients with CDI from those with non-C. difficile diarrhea and C. difficile colonization. Patients with CDI exhibited a chemical signature of Stickland amino acid fermentation that was distinct from those of uncolonized controls. This signature suggested that C. difficile preferentially catabolizes branched chain amino acids during CDI. Unexpectedly, we also identified a series of noncanonical, unsaturated bile acids that were depleted in patients with CDI. These bile acids may derive from an extended host-microbiome dehydroxylation network in uninfected patients. Bile acid composition and leucine fermentation defined a prototype metabolomic model with potential to distinguish clinical CDI from asymptomatic C. difficile colonization.

Published

2019

37. Impact of Amoxicillin-Clavulanate followed by Autologous Fecal Microbiota Transplantation on Fecal Microbiome Structure and Metabolic Potential

Author

Kimberly A. Reske, Carey-Ann D. Burnham, Christopher Bulow, Jennie H. Kwon, Sanket Patel, Erik R. Dubberke, Susan R. Jones, Gautam Dantas, Sondra Seiler, Xiaoqing Sun, Meghan A. Wallace, Amy Langdon, and Tiffany Hink

Subjects

0301 basic medicine, Adult, Male, lcsh:QR1-502, microbiome, Enema, Biology, Gut flora, Amoxicillin-Potassium Clavulanate Combination, Microbiology, lcsh:Microbiology, Host-Microbe Biology, 03 medical and health sciences, Young Adult, 0302 clinical medicine, Antibiotic resistance, multidrug resistance, Humans, Microbiome, antimicrobial resistance, Molecular Biology, Feces, metagenomics, Microbiota, Gastrointestinal Microbiome, fecal microbiota transplantation, Middle Aged, Antimicrobial, biology.organism_classification, Editor's Pick, Healthy Volunteers, QR1-502, 3. Good health, Anti-Bacterial Agents, Multiple drug resistance, 030104 developmental biology, Metabolism, Treatment Outcome, 030211 gastroenterology & hepatology, Female, beta-Lactamase Inhibitors, Autologous Fecal Microbiota Transplantation, Research Article

Abstract

The spread of multidrug resistance among pathogenic organisms threatens the efficacy of antimicrobial treatment options. The human gut serves as a reservoir for many drug-resistant organisms and their resistance genes, and perturbation of the gut microbiome by antimicrobial exposure can open metabolic niches to resistant pathogens. Once established in the gut, antimicrobial-resistant bacteria can persist even after antimicrobial exposure ceases. Strategies to prevent multidrug-resistant organism (MDRO) infections are scarce, but autologous fecal microbiota transplantation (autoFMT) may limit gastrointestinal MDRO expansion. AutoFMT involves banking one’s feces during a healthy state for later use in restoring gut microbiota following perturbation. This pilot study evaluated the effect of amoxicillin-clavulanic acid (Amox-Clav) exposure and autoFMT on gastrointestinal microbiome taxonomic composition, resistance gene content, and metabolic capacity. Importantly, we found that metabolic capacity was perturbed even in cases where gross phylogeny remained unchanged and that autoFMT was safe and well tolerated., Strategies to prevent multidrug-resistant organism (MDRO) infections are scarce, but autologous fecal microbiota transplantation (autoFMT) may limit gastrointestinal MDRO expansion. AutoFMT involves banking one’s feces during a healthy state for later use in restoring gut microbiota following perturbation. This pilot study evaluated the effect of autoFMT on gastrointestinal microbiome taxonomic composition, resistance gene content, and metabolic capacity after exposure to amoxicillin-clavulanic acid (Amox-Clav). Ten healthy participants were enrolled. All received 5 days of Amox-Clav. Half were randomized to autoFMT, derived from stool collected pre-antimicrobial exposure, by enema, and half to saline enema. Participants submitted stool samples pre- and post-Amox-Clav and enema and during a 90-day follow-up period. Shotgun metagenomic sequencing revealed taxonomic composition, resistance gene content, and metabolic capacity. Amox-Clav significantly altered gut taxonomic composition in all participants (n = 10, P 0.05, compared to enrollment). Alterations to microbial metabolic capacity occurred following antimicrobial exposure even in participants without substantial taxonomic disruption, potentially creating open niches for pathogen colonization. Our findings suggest that metabolic potential is an important consideration for complete assessment of antimicrobial impact on the microbiome. AutoFMT was well tolerated and may have contributed to phylogenetic recovery. (This study has been registered at ClinicalTrials.gov under identifier NCT02046525.) IMPORTANCE The spread of multidrug resistance among pathogenic organisms threatens the efficacy of antimicrobial treatment options. The human gut serves as a reservoir for many drug-resistant organisms and their resistance genes, and perturbation of the gut microbiome by antimicrobial exposure can open metabolic niches to resistant pathogens. Once established in the gut, antimicrobial-resistant bacteria can persist even after antimicrobial exposure ceases. Strategies to prevent multidrug-resistant organism (MDRO) infections are scarce, but autologous fecal microbiota transplantation (autoFMT) may limit gastrointestinal MDRO expansion. AutoFMT involves banking one’s feces during a healthy state for later use in restoring gut microbiota following perturbation. This pilot study evaluated the effect of amoxicillin-clavulanic acid (Amox-Clav) exposure and autoFMT on gastrointestinal microbiome taxonomic composition, resistance gene content, and metabolic capacity. Importantly, we found that metabolic capacity was perturbed even in cases where gross phylogeny remained unchanged and that autoFMT was safe and well tolerated.

Published

2018

38. 2847. Comparative Genomics and Clonal Tracking of Multi-drug-Resistant Uropathogens Implicates the Fecal Microbiome as a Potential Reservoir for Recurrent Urinary Tract Infections

Author

Gautam Dantas, Robert Thänert, Drew J. Schwartz, Sondra Seiler, Meghan A. Wallace, Bin Wang, Kimberly A. Reske, Candice Cass, Erik R. Dubberke, Tiffany Hink, Carey-Ann D. Burnham, and Jennie H. Kwon

Subjects

Comparative genomics, Gastrointestinal tract, biology, business.industry, Klebsiella pneumoniae, Urinary system, Genomics, Bacteriuria, medicine.disease, biology.organism_classification, Microbiology, Abstracts, Infectious Diseases, Oral Abstracts, Oncology, medicine, Microbiome, business, Feces

Abstract

Background Multi-drug-resistant organisms (MDRO) have complicated the treatment of urinary tract infections (UTIs), especially in patients with recurrent UTIs (rUTI). The objective of this pilot prospective cohort study is to determine the role of the fecal microbiome in rUTIs. Methods Stool and urine specimens were prospectively collected from patients with MDRO UTIs at 6 time points during and after the UTI, and with any rUTI. Specimens underwent semi-quantitative culture on differential and selective media for MDROs, and isolates underwent phenotypic susceptibility testing and whole-genome sequencing. Comparative genomics and clonal tracking were used to detect clonal uropathogen strains in the urinary and gastrointestinal tracts. Resistance genes, resistance-plasmids, and virulence genes of MDROs were characterized in silico. Results A total of 110 isolates (95 Escherichia coli, 2 Klebsiella pneumoniae, 13 Proteus mirabilis) were cultured from the urine and stool of 15 patients (7 non-rUTI, 8 rUTI). Clonal uropathogens were isolated between the urinary tract and their intestinal reservoir (Figure 1). Integration of clonality information with semiquantitative culturing implicated three potential routes for recurrence of UTIs: (i) bladder colonization following an intestinal bloom of uropathogens, (ii) reinfection from an external source, and (III) bacterial persistence within the urinary tract (Figures 2 and 3). Antibiotic susceptibility testing and genomic profiling indicated that antibiotic-resistant uropathogen populations colonizing the urinary tract and intestinal reservoir at symptomatic and asymptomatic timepoints have similar resistance profiles that are largely determined via a pool of shared resistance plasmids (Figure 3). Conclusion This study provides the first time-resolved analysis of uropathogen persistence following UTIs, showing that clonal antibiotic-resistant uropathogens can be detected in both the urine and stool at varying time points post-initial infection. The study implicates 3 potential routes of rUTI, including uropathogen persistence within the gut microbiota, reinfection from an external source, and persistent bacteriuria. Study findings could be utilized to inform future diagnostics and therapies for treatment of rUTIs. Disclosures Carey-Ann Burnham, PhD, BioFire: Research Grant; bioMerieux: Research Grant; Cepheid: Research Grant; Luminex: Research Grant.

Published

2019

39. Impact of Clostridium difficile recurrence on hospital readmissions

Author

Margaret A. Olsen, Marya D. Zilberberg, Kimberly A. Reske, Yan Yan, and Erik R. Dubberke

Subjects

medicine.medical_specialty, Pediatrics, genetic structures, Epidemiology, Patient Readmission, Recurrence, Vancomycin, Chart review, Internal medicine, Humans, Medicine, Retrospective Studies, Clostridioides difficile, business.industry, Health Policy, Medical record, Linezolid, Public Health, Environmental and Occupational Health, Retrospective cohort study, Tertiary care hospital, Clostridium difficile, Clostridium difficile infections, Anti-Bacterial Agents, Cephalosporins, Intensive Care Units, Aminoglycosides, Infectious Diseases, Carbapenems, Multivariate Analysis, Cohort, Clostridium Infections, Regression Analysis, business, Fluoroquinolones

Abstract

The impact of recurrent Clostridium difficile infections (CDIs) on hospital readmissions is unknown. The objective of this study was to determine whether recurrent CDI was independently associated with the number of hospital readmissions and days readmitted.We performed a retrospective cohort study at an academic, urban, tertiary care hospital. Data were collected from electronic medical records and supplemented with chart review. CDI patients were followed for 180 days to ascertain the number of hospital readmissions and total days readmitted. Univariate and multivariable negative binomial regression models were used to evaluate factors, including CDI recurrence, associated with hospital readmissions.The study included 3,950 patients with CDI from 2003-2009, including 413 patients with recurrent CDI. Recurrent CDI patients were significantly more likely to have at least 1 readmission (85% vs 41%; P.001) and had more days readmitted (mean = 18.6 vs 7.6; P.001) than patients without recurrent CDI. In multivariable analysis, recurrent CDI was independently associated with number of readmissions (rate ratio = 2.54; 95% confidence interval [CI], 2.21-2.91) and days readmitted (rate ratio = 3.97; 95% CI, 3.11-5.08) after adjustment for demographics, comorbidities, and medications.Recurrent CDI patients are significantly more likely than patients without a recurrence to be readmitted and spend increased time readmitted to the hospital.

Published

2015

40. An Evaluation of the Prevalence of Vancomycin-Resistant Enterococci (VRE) and Methicillin-Resistant Staphylococcus aureus (MRSA) in Hospital Food

Author

Sondra Seiler, Carey-Ann D. Burnham, Meghan A. Wallace, Kerry M. Bommarito, Jennie H. Kwon, Tiffany Hink, Kimberly A. Reske, and Erik R. Dubberke

Subjects

0301 basic medicine, Microbiology (medical), Adult, Male, Methicillin-Resistant Staphylococcus aureus, medicine.medical_specialty, Epidemiology, Hospitalized patients, 030106 microbiology, Staphylococcal infections, medicine.disease_cause, Article, Vancomycin-Resistant Enterococci, Interviews as Topic, Tertiary Care Centers, 03 medical and health sciences, Young Adult, Food Service, Hospital, Internal medicine, mental disorders, medicine, Prevalence, Food microbiology, Humans, Prospective Studies, Prospective cohort study, Gram-positive bacterial infections, Gram-Positive Bacterial Infections, Aged, Aged, 80 and over, Missouri, business.industry, digestive, oral, and skin physiology, biochemical phenomena, metabolism, and nutrition, Middle Aged, Staphylococcal Infections, medicine.disease, bacterial infections and mycoses, Methicillin-resistant Staphylococcus aureus, Hospitals, 030104 developmental biology, Infectious Diseases, Food Microbiology, business

Abstract

This prospective cohort study evaluated the presence of MRSA and VRE in the food of hospitalized patients. 149 patients were enrolled and 910 food specimens cultured; 3.2% were positive for MRSA and 2.4% positive for VRE, from a variety of food types.

Published

2017

41. Development and validation of a recurrentClostridium difficilerisk-prediction model

Author

Erik R. Dubberke, Yan Yan, Margaret A. Olsen, Kimberly A. Reske, and Marya D. Zilberberg

Subjects

medicine.medical_specialty, Multivariate analysis, Leadership and Management, business.industry, Health Policy, Retrospective cohort study, General Medicine, Assessment and Diagnosis, Clostridium difficile, Logistic regression, Intensive care unit, Hospital medicine, law.invention, law, Internal medicine, Medicine, Fundamentals and skills, Young adult, business, Intensive care medicine, Care Planning, Cohort study

Abstract

BACKGROUND Recurrent Clostridium difficile infection (rCDI) affects 10% to 25% of patients with initial CDI (iCDI). Initiation of new therapies that reduce recurrences rests on identifying patients at high risk for rCDI at iCDI onset. OBJECTIVE To develop a predictive model for rCDI based on factors present at iCDI onset. DESIGN Retrospective cohort study. SETTING Large urban academic medical center. PATIENTS All adult patients with an inpatient iCDI from January 1, 2003 to December 31, 2009. INTERVENTION None. MEASUREMENTS Positive toxin assay for C difficile with no C difficile infection in the previous 60 days constituted iCDI. Repeat positive toxin within 42 days of stopping iCDI treatment defined rCDI. Three demographic, 13 chronic, and 12 acute disease characteristics, and 7 processes of care prior to or at the onset of iCDI, were assessed for association with rCDI. A logistic regression model to identify predictors for rCDI was developed and cross-validated. RESULTS Among the 4196 patients enrolled, 425 (10.1%) developed rCDI. Six factors (case status as community-onset healthcare-associated, ≥2 hospitalizations in the prior 60 days, new gastric acid suppression, fluoroquinolone and high-risk antibiotic use at the onset of iCDI, age) predicted rCDI in multivariate analyses, whereas intensive care unit stay appeared protective. The model achieved moderate discrimination (C statistic 0.643) and calibration (Brier score 0.089). Its negative predictive value was 90% or higher across a wide range of risk. CONCLUSIONS Among patients hospitalized with rCDI, multiple factors present at the onset of iCDI increased the risk for rCDI. Recognizing patients at high-risk for rCDI can help clinicians tailor early treatment and prevention. Journal of Hospital Medicine 2014;9:418–423. © 2014 Society of Hospital Medicine

Published

2014

42. 1773. Impact of Antibiotics Used to Treat Community Acquired Pneumonia on the Gut Microbiome and Resistome in Healthy Volunteers

Author

Sondra Seiler, Bin Wang, Winston E. Anthony, Gautam Dantas, Erik R. Dubberke, Candice Cass, Tiffany Hink, Kimberly A. Reske, Carey-Ann D. Burnham, and Jennie H. Kwon

Subjects

medicine.medical_specialty, business.industry, medicine.drug_class, Antibiotics, medicine.disease, Gut microbiome, Resistome, Abstracts, Infectious Diseases, Oncology, Community-acquired pneumonia, A. Oral Abstracts, Internal medicine, Healthy volunteers, Medicine, business

Abstract

Background Antibiotics (ABX) are frequently inappropriately used to treat nonbacterial causes of respiratory illnesses. The goal of this prospective cohort study was to characterize the impact of ABX used to treat community-acquired pneumonia (CAP) on the fecal microbiome and resistome in healthy volunteers (HV). Methods Twenty HVs were randomized to receive 5 days of levofloxacin (LV), azithromycin (AZ), cefpodoxime (CF), or AZ+CF. Stool was collected before, during, and after ABX, then underwent microbiologic culture and shotgun sequencing. DNA was extracted, then sequenced using the Illumina NextSeq platform. Relative abundance of bacterial taxa was estimated by MetaPhlAn and antibiotic resistance gene (ARG) composition by ShortBRED. Analysis was in R. Results The mean HV age was 37 (range 24–59) and 10 were female. Species diversity measured via Shannon Index and richness were significantly lower in samples taken from all HVs 3 days post-ABX (P < 0.01 for all). While nonmetric multidimensional scaling (NDMS) ordination shows high interpatient dissimilarity (Bray–Curtis) for most samples, the post-ABX intrapatient dissimilarity varies by ABX. The AZ group exhibited chronic alterations in taxa dissimilarity and the CF group had increases in dissimilarity directly post-ABX. The CF+AZ group displayed both acute and persistent perturbations (Figure 1). Although there was no significant change in ARG richness post-ABX, there was a significant increase in overall ARG abundance across all samples (P < 0.003). Within each ABX, there were unique changes in ARG abundance, and groups with CF had increases in ARG abundance (Figure 2). Conclusion ABX used to treat CAP can cause acute microbiome disruptions, as evidenced by decreased microbiome species diversity and richness, and an increase in ARG abundance post-ABX. The duration of this impact is variable. To prevent microbiome disruptions, measures to prevent inappropriate ABX use via ABX stewardship are necessary. Disclosures E. R. Dubberke, Rebiotix: Consultant and Investigator, Consulting fee and Research support. Pfizer: Consultant and Grant Investigator, Consulting fee and Research grant. Synthetic biologics: Consultant, Consulting fee. Merck: Consultant and Investigator, Consulting fee and Research support. Valneva: Consultant, Consulting fee. Achaogen: Consultant, Consulting fee. Alere: webinar, Speaker honorarium. Biofire: webinar, Speaker honorarium.

Published

2018

43. Clostridioides (Clostridium) difficile infection burden in Japan: A multicenter prospective study

Author

Makoto Nakamura, Kuniko Yokote, Hidetaka Kitazono, Yasuaki Tagashira, Kimberly A. Reske, Sayuri Morita, Kayoko Toimoto, Daisuke Suzuki, Tatsuyuki Watanabe, Takuya Watanabe, Hideaki Kato, Nobuaki Mori, Erik R. Dubberke, Akiko Higuchi, Takao Toyokawa, Fumi Masumoto, Cedric Mahé, Kei Moriya, Hitoshi Honda, Tetsuya Kikuchi, Tatsuya Bando, Saeko Kashiwagura, Kei Kasahara, Margaret A. Olsen, Junko Ogawa, Hisashi Kume, Yousuke Shimizu, Katsuyuki Kojima, Hideaki Ishikawa, Tadashi Fukuda, Hideo Morikawa, Kayoko Tadera, Izumi Yokomaku, Mitsutoshi Senoh, Seigo Kitada, Hiroko Horiuchi, Hiroko Miyazato, Haruko Saito, Masahisa Honda, Mika Nakama, Hiroshi Chiba, Haru Kato, Harumi Tominaga, Jun-ichi Yoshida, Ichiro Yoshikawa, Yasuhiro Norisue, Saori Ishiguro, and Naoto Hosokawa

Subjects

medicine.medical_specialty, genetic structures, Erythromycin, Microbial Sensitivity Tests, Ribotyping, Microbiology, 03 medical and health sciences, Japan, Internal medicine, medicine, Humans, Public Health Surveillance, Geography, Medical, Prospective cohort study, Retrospective Studies, 030304 developmental biology, 0303 health sciences, Clostridioides difficile, 030306 microbiology, business.industry, Incidence, Incidence (epidemiology), Clindamycin, Retrospective cohort study, Clostridium difficile, Gatifloxacin, Anti-Bacterial Agents, Molecular Typing, Diarrhea, Infectious Diseases, Clostridium Infections, medicine.symptom, business, medicine.drug

Abstract

Clostridioides (Clostridium) difficile is the leading cause of healthcare-associated infectious diarrhea in the developed world. Retrospective studies have shown a lower incidence of C. difficile infection (CDI) in Japan than in Europe or North America. Prospective studies are needed to determine if this is due lack of testing for C. difficile or a true difference in CDI epidemiology. A prospective cohort study of CDI was conducted from May 2014 to May 2015 at 12 medical facilities (20 wards) in Japan. Patients with at least three diarrheal bowel movements (Bristol stool grade 6–7) in the preceding 24 h were enrolled. CDI was defined by positive result on enzyme immunoassay for toxins A/B, nucleic acid amplification test for the toxin B gene or toxigenic culture. C. difficile isolates were subjected to PCR-ribotyping (RT), slpA-sequence typing (slpA-ST), and antimicrobial susceptibility testing. The overall incidence of CDI was 7.4/10,000 patient-days (PD). The incidence was highest in the five ICU wards (22.2 CDI/10,000 PD; range: 13.9–75.5/10,000 PD). The testing frequency and CDI incidence rate were highly correlated (R2 = 0.91). Of the 146 isolates, RT018/018″ was dominant (29%), followed by types 014 (23%), 002 (12%), and 369 (11%). Among the 15 non-ICU wards, two had high CDI incidence rates (13.0 and 15.9 CDI/10,000 PD), with clusters of RT018/slpA-ST smz-02 and 018”/smz-01, respectively. Three non-RT027 or 078 binary toxin-positive isolates were found. All RT018/018” isolates were resistant to moxifloxacin, gatifloxacin, clindamycin, and erythromycin. This study identified a higher CDI incidence in Japanese hospitals than previously reported by actively identifying and testing patients with clinically significant diarrhea. This suggests numerous patients with CDI are being overlooked due to inadequate diagnostic testing in Japan.

Published

2019

44. Performance of laboratory tests for detection for Clostridioides difficile: A multicenter prospective study in Japan

Author

Takuya Watanabe, Hisashi Kume, Hideaki Kato, Kimberly A. Reske, Sayuri Morita, Hitoshi Honda, Cedric Mahé, Kei Moriya, Daisuke Suzuki, Kei Kasahara, Katsuyuki Kojima, Seigo Kitada, Tatsuya Bando, Erik R. Dubberke, Hideo Morikawa, Yasuaki Tagashira, Naoto Hosokawa, Haruko Saito, Kayoko Tadera, Masahisa Honda, Haru Kato, Harumi Tominaga, Makoto Nakamura, Kuniko Yokote, Akiko Higuchi, Tatsuyuki Watanabe, Kayoko Toimoto, Saeko Kashiwagura, Yasuhiro Norisue, Tadashi Fukuda, Ichiro Yoshikawa, Hideaki Ishikawa, Mika Nakama, Yousuke Shimizu, Tetsuya Kikuchi, Saori Ishiguro, Junko Ogawa, Hiroshi Chiba, Hiroko Miyazato, Hiroko Horiuchi, Jun-ichi Yoshida, Hidetaka Kitazono, Nobuaki Mori, Takao Toyokawa, Fumi Masumoto, Izumi Yokomaku, Mitsutoshi Senoh, and Margaret A. Olsen

Subjects

Male, medicine.medical_specialty, Bacterial Toxins, Clostridium difficile toxin B, Polymerase Chain Reaction, Ribotyping, Sensitivity and Specificity, Microbiology, Gastroenterology, 03 medical and health sciences, Japan, Internal medicine, medicine, Humans, In patient, Prospective Studies, Prospective cohort study, 030304 developmental biology, Bacteriological Techniques, 0303 health sciences, Clostridioides difficile, 030306 microbiology, business.industry, Gold standard (test), Predictive value, Diarrhea, Infectious Diseases, Clostridium Infections, Female, Enzyme immunoassays, medicine.symptom, business, Clostridioides

Abstract

Background The optimal and practical laboratory diagnostic approach for detection of Clostridioides difficile to aid in the diagnosis of C. difficile infection (CDI) is controversial. A two-step algorithm with initial detection of glutamate dehydrogenase (GDH) or nucleic acid amplification test (NAAT) alone are recommended as a predominant method for C. difficile detection in developed countries. The aim of this study was to compare the performance of enzyme immunoassays (EIA) detecting toxins A and B, NAAT detecting the toxin B gene, and GDH compared to toxigenic culture (TC) for C. difficile as the gold standard, in patients prospectively and actively assessed with clinically significant diarrhea in 12 medical facilities in Japan. Methods A total of 650 stool specimens were collected from 566 patients with at least three diarrheal bowel movements (Bristol stool grade 6–7) in the preceding 24 h. EIA and GDH were performed at each hospital, and NAAT and toxigenic C. difficile culture with enriched media were performed at the National Institute of Infectious Diseases. All C. difficile isolates recovered were analyzed by PCR-ribotyping. Results Compared to TC, the sensitivity, specificity, positive predictive value (PPV) and negative predictive value (NPV) of EIA were 41%, 96%, 75% and 84%, respectively, and for NAAT were 74%, 98%, 91%, and 92%, respectively. In 439 specimens tested with GDH, the sensitivity, specificity, PPV, and NPV were 73%, 87%, 65%, and 91%, and for an algorithm (GDH plus toxin EIA, arbitrated by NAAT) were 71%, 96%, 85%, and 91%, respectively. Among 157 isolates recovered, 75% of isolates corresponded to one of PCR-ribotypes (RTs) 002, 014, 018/018”, and 369; RT027 was not isolated. No clear differences in the sensitivities of any of EIA, NAAT and GDH for four predominant RTs were found. Conclusion The analytical sensitivities of NAAT and GDH-algorithm to detect toxigenic C. difficile in this study were lower than most previous reports. This study also found low PPV of EIAs. The optimal method to detect C. difficile or its toxins to assist in the diagnosis of CDI needs further investigation.

Published

2019

45. 2570. A Randomized Controlled Trial of Lactobacillus rhamnosus GG on Multidrug-Resistant Organism (MDRO) Colonization

Author

Kerry M. Bommarito, Carey-Ann D. Burnham, Tiffany Hink, Erik R. Dubberke, Kimberly A. Reske, Sondra Seiler, Adriana M Rauseo, and Victoria J. Fraser

Subjects

biology, business.industry, Multidrug resistant organism, biology.organism_classification, Antimicrobial, Microbiology, law.invention, Abstracts, Infectious Diseases, Oncology, Lactobacillus rhamnosus, Randomized controlled trial, law, Poster Abstracts, Ingestion, Medicine, Colonization, business

Abstract

Background MDRO present a greater threat to public health than ever before, and antimicrobial options are decreasing. Altered colonic microbiota following antimicrobial exposure allows for subsequent colonization by MDRO. Ingestion of prophylactic Lactobacillus rhamnosus GG (LGG) could be an approach to prevent the spread of, and subsequent infection due to MDRO, by promoting a healthy bacterial milieu within the colon. Methods This is a prospective, double-blinded, randomized clinical trial in which a total of 87 subjects on broad-spectrum antibiotics were randomized to receive LGG twice daily (n = 43) vs placebo (n = 44). Stool or rectal swab specimens were collected for culture at enrollment, every 3 days during admission, and at discharge. Selective media were used to detect the following MDRO: Clostridioides difficile (CD), vancomycin-resistant Enterococcus (VRE), and antibiotic-resistant Gram-negatives (GN). The primary outcome was MDRO acquisition. Secondary outcomes included analysis for loss of any MDRO if colonized at enrollment, and acquisition or loss of individual MDRO. Results Subjects in both groups had similar prevalence of colonization with any MDRO at study enrollment (LGG 40% vs. placebo 39%), with similar colonization prevalence for individual MDRO (Figure 1). There was no difference in any MDRO acquisition (LGG 27%, placebo 33%, OR 1.36, 95% CI 0.42–4.41) or any individual MDRO acquisition (Figure 2). There was also no difference in loss of any MDRO (LGG 18%, placebo 24%, OR 1.44, 95% CI 0.27–7.68) or any individual MDRO (Figure 2). Conclusion LGG administration did not prevent acquisition of MDRO or accelerate loss of MDRO colonization. Disclosures All authors: No reported disclosures.

Published

2019

46. Risk for

Author

Erik R, Dubberke, Kimberly A, Reske, Margaret A, Olsen, Kerry M, Bommarito, Sondra, Seiler, Fernanda P, Silveira, Tom M, Chiller, John, DiPersio, and Victoria J, Fraser

Subjects

genetic structures, Infectious Disease

Abstract

Background Clostridium difficile infection (CDI) is a frequent cause of diarrhea among allogeneic hematopoietic cell transplant (HCT) recipients. It is unknown whether risk factors for CDI vary by time posttransplant. Methods We performed a 3-year prospective cohort study of CDI in allogeneic HCT recipients. Participants were enrolled during their transplant hospitalizations. Clinical assessments were performed weekly during hospitalizations and for 12 weeks posttransplant, and monthly for 30 months thereafter. Data were collected through patient interviews and chart review, and included CDI diagnosis, demographics, transplant characteristics, medications, infections, and outcomes. CDI cases were included if they occurred within 1 year of HCT and were stratified by time from transplant. Multivariable logistic regression was used to determine risk factors for CDI. Results One hundred eighty-seven allogeneic HCT recipients were enrolled, including 63 (34%) patients who developed CDI. 38 (60%) CDI cases occurred during the preengraftment period (days 0-30 post-HCT) and 25 (40%) postengraftment (day >30). Lack of any preexisting comorbid disease was significantly associated with lower risk of CDI preengraftment (odds ratio [OR], 0.3; 95% confidence interval [CI], 0.1-0.9). Relapsed underlying disease (OR, 6.7; 95% CI, 1.3-33.1), receipt of any high-risk antimicrobials (OR, 11.8; 95% CI, 2.9-47.8), and graft-versus-host disease (OR, 7.8; 95% CI, 2.0-30.2) were significant independent risk factors for CDI postengraftment. Conclusions A large portion of CDI cases occurred during the postengraftment period in allogeneic HCT recipients, suggesting that surveillance for CDI should continue beyond the transplant hospitalization and preengraftment period. Patients with continued high underlying severity of illness were at increased risk of CDI postengraftment.

Published

2016

47. An Evaluation of Food as a Potential Source for Clostridium difficile Acquisition in Hospitalized Patients

Author

Carey-Ann D. Burnham, Jennie H. Kwon, Sondra Seiler, Tiffany Hink, Kerry M. Bommarito, Kimberly A. Reske, Cristina Lanzas, and Erik R. Dubberke

Subjects

0301 basic medicine, Microbiology (medical), Adult, Male, medicine.medical_specialty, Epidemiology, Hospitalized patients, 030106 microbiology, Article, 03 medical and health sciences, Feces, Young Adult, 0302 clinical medicine, Internal medicine, medicine, Food microbiology, Humans, Potential source, 030212 general & internal medicine, Prospective Studies, Young adult, Prospective cohort study, Enterocolitis, Pseudomembranous, Aged, Aged, 80 and over, Meal, Academic Medical Centers, Cross Infection, Inpatients, Missouri, business.industry, Clostridioides difficile, Clostridium difficile, Middle Aged, Hospitalization, Infectious Diseases, Food Microbiology, Female, business

Abstract

OBJECTIVETo determine whetherClostridium difficileis present in the food of hospitalized patients and to estimate the risk of subsequent colonization associated withC. difficilein food.METHODSThis was a prospective cohort study of inpatients at a university-affiliated tertiary care center, May 9, 2011–July 12, 2012. Enrolled patients submitted a portion of food from each meal. Patient stool specimens and/or rectal swabs were collected at enrollment, every 3 days thereafter, and at discharge, and were cultured forC. difficile. Clinical data were reviewed for evidence of infection due toC. difficile.A stochastic, discrete event model was developed to predict exposure toC. difficilefrom food, and the estimated number of new colonization events from food exposures per 1,000 admissions was determined.RESULTSA total of 149 patients were enrolled and 910 food specimens were obtained. Two food specimens from 2 patients were positive forC. difficile(0.2% of food samples; 1.3% of patients). Neither of the 2 patients was colonized at baseline withC. difficile. Discharge colonization status was available for 1 of the 2 patients and was negative. Neither was diagnosed withC. difficileinfection while hospitalized or during the year before or after study enrollment. Stochastic modeling indicated contaminated hospital food would be responsible for less than 1 newly colonized patient per 1,000 hospital admissions.CONCLUSIONSThe recovery ofC. difficilefrom the food of hospitalized patients was rare. Modeling suggests hospital food is unlikely to be a source ofC. difficileacquisition.Infect Control Hosp Epidemiol2016;1401–1407

Published

2016

48. Epidemiology of Clostridium difficile Infections in Japan

Author

Yasuaki Tagashira, Mitsutoshi Senoh, Margaret A. Olsen, Erik R. Dubberke, Hitoshi Honda, Kimberly A. Reske, Haru Kato, and Tadashi Fukuda

Subjects

medicine.medical_specialty, business.industry, 030503 health policy & services, Clostridium difficile infections, Surgery, 03 medical and health sciences, 0302 clinical medicine, Infectious Diseases, Oncology, Internal medicine, Epidemiology, medicine, 030212 general & internal medicine, 0305 other medical science, business

Published

2016

49. Effect of an Electronic Hard-Stop Intervention to Prevent Repeat Clostridium difficile Toxin Testing on Test Utilization and Clinical Outcomes

Author

Erik R. Dubberke, Carey-Ann D. Burnham, Jennie H. Kwon, Ronald Jackups, Kimberly A. Reske, and Tiffany Hink

Subjects

medicine.medical_specialty, Infectious Diseases, Oncology, business.industry, Intervention (counseling), medicine, Clostridium difficile toxin A, Intensive care medicine, business, Test (assessment)

Published

2016

50. Quantitative Responses of Taxonomic Composition and Resistance Gene Abundance in the Gut Microbiota to Fecal Microbiota Transplantation

Author

Courtney Jones, Tiffany Hink, Xiaoqing Sun, Carey-Ann D. Burnham, Gautam Dantas, Amy Langdon, Kimberly A. Reske, Christopher Bulow, and Erik R. Dubberke

Subjects

Taxonomic composition, Infectious Diseases, Oncology, Resistance (ecology), Abundance (ecology), Fecal bacteriotherapy, Biology, Gut flora, biology.organism_classification, Gene, Microbiology

Published

2016