Assessing the Impact of Antimicrobial Exposure and Infection Control Measures on the Spread of VRE

• Conditions: Antibiotic Resistant Infection; VRE Infection
• Interventions: Other: Rectal swabs - microbiological analysis; Other: Examination of patient room

• Registration Number: NCT04624464
• Lead Sponsor: University Hospital of Cologne

Brief Summary

The AEGON study is a German multicenter, prospective observational study. The study consists of two parts, which are carried out at all participating study sites and include two different patient cohorts. Part 1 focuses on the collection and analysis of rectal swabs from newly admitted VREf-negative patients at high risk of nosocomial VREf acquisition. Moreover, patients included into this part of the study will undergo in-depth documentation of clinical data if an antibiotic therapy is administered. Initiated antibiotic therapies will then be assessed by an AMS board (Antimicrobial Stewardship Board). In Part 2, environmental investigations will be performed in newly occupied single rooms of previously known VREf-positive patients. In addition, rectal swabs will be collected and data on antibiotic exposure of these patients will be documented in order to correlate the VRE contamination burden of surfaces with the intestinal VREf-load and antibiotic exposure.

Detailed Description

Current studies show that Vancomycin-resistant Enterococci (VRE) have become increasingly widespread throughout Germany in recent years, especially E. faecium (VREf). Healthy individuals can come into contact with VREf in various ways, for example via the food chain, contaminated drinking water or animal contacts. A possibly caused low-grade colonisation of the gastrointestinal tract with VREf (so-called low-level colonisation) can remain undetected during hospital admission using routine screening methods. The AEGON study, based on the use of state-of-the-art molecular diagnostics and comprehensive clinical data collection, will provide a detailed analysis of the factors involved in the rapid spread of VREf. In addition, diagnostic detection limits of common screening methods are determined by the use of additional diagnostics such as enrichment culture or molecular VREf detection.

The study is a German multicenter, prospective observational study and consists of two parts, which are carried out at all participating study sites and include two different patient cohorts. Part 1 focuses on the collection and analysis of rectal swabs from newly admitted VRE-negative patients at high risk of nosocomial VREf acquisition. Moreover, patients included into this part of the study will undergo in-depth documentation of clinical data if an antibiotic therapy is administered. Initiated antibiotic therapies will then be assessed by an AMS board. In Part 2, environmental investigations will be performed in newly occupied single rooms of previously known VREf-positive patients. In addition, rectal swabs will be collected and data on antibiotic exposure of these patients will be documented in order to correlate the VRE contamination burden of surfaces with the intestinal VREf-load and antibiotic exposure. The AEGON study, based on the use of state-of-the-art molecular diagnostics and comprehensive clinical data collection, will provide a detailed analysis of the factors involved in the rapid spread of VREf. In addition, diagnostic detection limits of common screening methods are determined by the use of additional diagnostics such as enrichment culture or molecular VREf detection.

Study Timeline

• Study Start: 2019-01-01
• Study First Submitted: 2020-07-30
• Status Verified: 2020-11
• Study First Submitted QC: 2020-11-05
• Last Update Submitted: 2020-11-05
• Study First Posted: 2020-11-10
• Last Update Posted: 2020-11-10
• Primary Completion: 2020-12-31
• Study Completion: 2020-12-31

Recruitment & Eligibility

• Status: UNKNOWN
• Sex: All
• Target Recruitment: 170

Inclusion Criteria

• ≥ 18 years
• Patients with malignant primary disease and current inpatient admission to a normal ward with expected inpatient stay of at least 15 days
• High risk of exposure to antibiotics during the stay
• Written informed consent of the patient after clarification has been given

Exclusion Criteria

• Already known current or documented past colonisation or infection by VRE
• Simultaneous participation in other studies is only an exclusion criterion if the other study explicitly excludes participation in observational studies or if the other study complicates the interpretation of the endpoints of AEGON (e.g. double-blind study on antibiotic use).

Study & Design

• Study Type: OBSERVATIONAL
• Study Design: Not specified

Arm && Interventions

Group	Intervention	Description
Cohort 1: VRE negative at admission	Rectal swabs - microbiological analysis	150 patients meeting the following inclusion criteria: * ≥ 18 years * Patients with malignant primary disease and current inpatient admission to a normal ward with expected inpatient stay of at least 15 days * High risk of exposure to antibiotics during the stay * Written informed consent of the patient after clarification has been given Exclusion criteria: * Already known current or documented past colonisation or infection by VRE * Simultaneous participation in other studies is only an exclusion criterion if the other study explicitly excludes participation in observational studies or if the other study complicates the interpretation of the endpoints of AEGON (e.g. double-blind study on antibiotic use).
Cohort 2: VRE positive at admission	Examination of patient room	A total 20 known VREf-positive patients meeting the following inclusion criteria: * Intestinal VREf colonization already known at the time of admission (e.g. based on examinations during previous stays or in external facilities) * Accommodation in a single room or alternatively multi-bed room with single occupancy on standard wards * Expected stay of at least 7 days
Cohort 2: VRE positive at admission	Rectal swabs - microbiological analysis	A total 20 known VREf-positive patients meeting the following inclusion criteria: * Intestinal VREf colonization already known at the time of admission (e.g. based on examinations during previous stays or in external facilities) * Accommodation in a single room or alternatively multi-bed room with single occupancy on standard wards * Expected stay of at least 7 days

Primary Outcome Measures

Name	Time	Method
VREf - Patient rooms	Change from baseline spread to spread at 10 weeks.	Primary Outcome for Cohort 2: Description of the spread of VREf in single rooms newly enrolled in known VREf-positive patients
VREf - Intestinal microbiota	Baseline	Primary Outcome for Cohort 1: Rate of VREf intestinal colonization detected by enrichment culture or specific PCR at time of uptake not detected by standard culture methods

Secondary Outcome Measures

Name	Time	Method
Standard culture VREf detection	baseline and every week up to 10 weeks max.	Cohort 1: Quantitative detection limit of standard culture methods for VREf detection compared to enrichment culture and qPCR (quantitative polymerase chain reaction)
Antibiotics	baseline and every week up to 10 weeks max.	Cohort 1: Identification of antibiotic classes that increase the risk of clonal expansion and subsequent domination by VREf. Domination by VREf is defined as the combination of cultural VREf detection from a sample and 16S rRNA (16S ribosomal ribonucleic acid) sequencing of the relative frequency of the Enterococcus genus over 30% as the most abundant genus in the sample.
Inadequately administered antibiotics	baseline and every week up to 10 weeks max.	Cohort 1: Proportion of inadequately administered antibiotics, defined as unnecessary, too long, too broad or too high doses in patients who develop VREf domination (see definition above) compared to patients without VREf acquisition and patients with VREf acquisition but without domination.
Adequate antibiotic	baseline and every week up to 10 weeks max.	Cohort 1: Rate of patients with no or adequate antibiotic therapy compared to patients with inadequate antibiotic therapy who develop a new colonization with VREf during the stay
Influence of antibiotic exposure duration	baseline and every week up to 10 weeks max.	Cohort 1: Influence of antibiotic exposure duration on microbiota
Influence of antibiotic class	baseline and every week up to 10 weeks max.	Cohort 1: Influence of antibiotic class on microbiota
VREf contamination	baseline at least every 72 hours up to max of 20 days.	Cohort 2: Identification of high risk objects and surfaces for VREf contamination in patient rooms with known VREf-positive patients
Correlation of the antibiotic exposure	baseline at least every 72 hours up to max of 20 days.	Cohort 2: Correlation of the antibiotic exposure of already known VREf-positive patients with the contamination load of objects and surfaces in the corresponding patient room.
Contamination load of objects	baseline at least every 72 hours up to max of 20 days.	Cohort 2: Correlation of the relative proportion of enterococci in intestinal microbiota with the contamination load of objects and surfaces in the associated patient room
Cleaning quality	baseline at least every 72 hours up to max of 20 days.	Cohort 2: Correlation of cleaning quality with the contamination load of VREf on objects and surfaces in rooms of known VRE-positive patients

Trial Locations

Locations (1)

University Hospital of Cologne; 🇩🇪 Cologne, NRW, Germany