Abstract
We compared optimal antibiotic prescribing before and after implementing an interpretive β-lactamase microbiology comment for Haemophilus influenzae and Moraxella catarrhalis in lower respiratory-tract infections. The postintervention group was associated with 5-fold increased odds of optimal de-escalation (adjusted odds ratio, 5.03; 95% confidence interval, 2.57–9.87).
Lower respiratory-tract infections (LRTIs) are an important target for antimicrobial stewardship programs due to their frequency, diagnostic uncertainty, and association with antibiotic overuse; however, gaps in effective LRTI-targeted stewardship strategies remain. The development of pragmatic and impactful antimicrobial stewardship interventions are needed to improve optimal antibiotic utilization and patient outcomes.
Behavioral interventions such as nudging clinicians with purposeful, interpretative microbiology comments are associated with improved antibiotic prescribing. 3–6 Notably, framing strategies with actionable comments is useful to direct antibiotic selection. 5 In 2 studies utilizing purposeful microbiology report comments, significant improvement was achieved in overall appropriateness of antibiotic use. 3,5,6
The Clinical Laboratory Standards Institute recommends a direct β-lactamase test as a means of rapid identification for ampicillin or amoxicillin resistance. 7 Laboratory reports for Hemophilus influenzae and Moraxella catarrhalis may be perceived as ambiguous to prescribers unfamiliar with the meaning of a positive or negative β-lactamase result. To minimize ambiguity and to assess optimal definitive antibiotic prescribing, we implemented a nudge with an automated, interpretive respiratory culture comment for β-lactamase negative or positive H. influenzae or M. catarrhalis LRTIs. We hypothesized that implementation of a targeted microbiology nudge would be associated with optimal de-escalation in this setting.
Methods
Study design
This before-and-after quasiexperimental study was conducted at Henry Ford Health over 2 periods: a preintervention period before the microbiology comment (from August 20, 2017, to March 19, 2019) and a corresponding postintervention period after the microbiology comment was implemented (from March 21, 2019, to August 20, 2021). Hospitalized patients were included if they were aged ≥18 years and had been prescribed antibiotics for an LRTI with dominant growth of H. influenzae or M. catarrhalis. Respiratory specimens included in the study were sputum, tracheal aspirate, and bronchoalveolar lavage (BAL). Patients were excluded for non-LRTI or polymicrobial infections, receipt of prophylactic antibiotics for opportunistic infections, and documented IgE-mediated β-lactam allergy. Only the index episode of H. influenzae or M. catarrhalis LRTI was included. The study received institutional review board approval with waiver of consent.
Intervention
On March 20, 2019, an automated, interpretive comment on respiratory cultures for β-lactamase negative or positive H. influenzae or M. catarrhalis was implemented. The intervention consisted of appending a new comment for β-lactamase negative H. influenzae or M. catarrhalis stating, “This organism is predictably susceptible to ampicillin or amoxicillin.” For β-lactamase positive H. influenzae or M. catarrhalis, the new comment stated, “This organism is predictably susceptible to ampicillin-sulbactam or amoxicillin-clavulanate.” These results are available within patient culture results in the electronic medical record (EMR). Prior to the intervention, microbiology reports stated the β-lactamase result as either “positive” or “negative” with no interpretation.
Study data and outcome definitions
Patient and infection-related characteristics were manually collected from the EMR using a standardized case report form. Microbiology variables included were infection type, duration of antibiotic therapy, and Clostridioides difficile infection after initial antibiotic therapy until discharge. Identification of M. catarrhalis or H. influenzae from respiratory isolates was determined by the Henry Ford Health centralized clinical microbiology laboratory using BD BBL Cefinase paper disk β-lactamase testing (BD Microbiology Systems, Cockeysville, MD).
The primary outcome was optimal de-escalation, defined as definitive therapy with ampicillin or amoxicillin for β-lactamase–negative isolates and amoxicillin-clavulanate or ampicillin-sulbactam for β-lactamase–positive isolates. Secondary outcomes included de-escalation based on specimen type, clinical success, duration of treatment in days, time to de-escalation in days, and continuation of broad-spectrum antibiotics after final microbiology results. Clinical success was defined as improvement in signs and symptoms of infection without need for further antibiotics after completion of the index course. A nonequivalent dependent variable of deep-vein thrombosis (DVT) prophylaxis was used to evaluate overall quality of medication management over the study period to assess maturation.
Statistical analyses
A sample size of 201 patients was calculated using the following assumptions: (1) 2-sided α of 0.05; (2) β of 0.8; and (3) and anticipated effect size of 30% change in optimal de-escalation after comment implementation. 3
In bivariate analysis, continuous data were analyzed using the Mann-Whitney U test; categorical data were compared using the χ2 or Fisher exact test. Stratified analyses by organism and infection type were performed to assess the impact of effect modifiers. To determine patients with the greatest likelihood of receiving optimal antibiotic de-escalation, variables associated with the outcome (P < .20) from bivariate analysis were entered into a multivariable model using a backward, stepwise approach. All statistical tests were performed using SPSS software (SPSS Statistics for Windows version 26.0, Armonk, NY; IBM Corp).
Results
In total, 201 patients were included: 100 in the preintervention group, 101 in the postintervention group. Baseline characteristics are presented in Table 1. The overall organism distribution was 159 (79%) H. influenzae and 49 (24%) M. catarrhalis; 7 cultures grew both organisms with the same β-lactamase result.
Table 1.
Baseline and Infection Characteristics of Patients With Haemophilus influenzae or Moraxella catarrhalis Lower Respiratory Tract Infections Before and After Implementation of an Interpretive β-lactamase Comment
| Baseline Characteristics | Before the Intervention (n = 100), No. (%) |
After the Intervention (n = 101), No. (%) |
P Value |
|---|---|---|---|
| Age, median years (IQR) | 63 (42–84) | 63 (46–80) | .40 |
| Sex, male | 61 (61) | 65 (64) | .62 |
| PWID | 7 (7) | 5 (5) | .54 |
| β-lactam allergy (non-IgE mediated) |
4 (4) | 7 (7) | .36 |
| Infection characteristics | |||
| CAP | 63 (63) | 74 (73) | .12 |
| HAP | 20 (20) | 15 (15) | .34 |
| VAP | 17 (17) | 12 (12) | .30 |
| H. influenzae | 81 (81) | 78 (77) | .51 |
| M. catarrhalis | 24 (24) | 25 (25) | .90 |
| Positive β-lactamase | 46 (46) | 52 (52) | .44 |
| ID consult | 16 (16) | 18 (18) | .73 |
| Antibiotic duration >7 days | 36 (36) | 33 (33) | .62 |
| Severity of illness | |||
| CCI, median (IQR) | 4 (3–8) | 4 (2–6) | .12 |
| WBC >12 or <4 per µL | 55 (55) | 50 (50) | .44 |
| Heart rate >90 bpm | 49 (49) | 46 (46) | .62 |
| RR >20 bpm or pCO2 <32 | 46 (46) | 36 (36) | .22 |
| Temperature >38.3°C | 17 (17) | 20 (20) | .61 |
| Pressors at time of culture collection | 27 (27) | 27 (27) | 1.0 |
| Ventilated at time of culture collection | 57 (57) | 55 (55) | .72 |
Note. PWID, persons who inject drugs; CAP, community-acquired pneumonia; HAP, hospital-acquired pneumonia; VAP, ventilator-associated pneumonia; ID, infectious diseases; CCI, Charlson comorbidity index; WBC, white blood cell; RR, respiratory rate.
The primary outcome of optimal de-escalation occurred in 19 patients (19%) in the preintervention group and 51 patients (51%) in the postintervention group (P < .001). The proportions of patients who received DVT prophylaxis, the nonequivalent dependent variable, in the preintervention and postintervention groups were 93 (93%) and 82 (81%) (P = .013). After adjusting for persons who inject drugs (PWID), hospital-acquired pneumonia (HAP), and patients with sputum cultures, the β-lactamase comment was associated with a 5-fold increased odds of optimal de-escalation (adjOR, 5.03; 95% CI, 2.57–9.87) (Table 2). In total, optimal de-escalation occurred in 50 patients (50%) with sputum, 39 (39%) with tracheal aspirate, and 11 (11%) with BAL cultures (P = .07). The median time to de-escalation, in days, was 1 (IQR, 0–2) day in the preintervention group and 0 (IQR, 0–1) days in the postintervention group (P < .001). The total median duration of antibiotic therapy was 7 days (IQR, 6–8) in the preintervention group and 7 days (IQR, 6–10) in the postintervention group (P = .28).
Table 2.
Variables Associated With Optimal De-escalation
| Variable | Optimal De-escalation, No. (%) | Unadjusted OR (95% CI) |
P Value | Adjusted OR (95% CI) |
|---|---|---|---|---|
| Postintervention β-lactamase nudge | 51 (73) | 4.35 (2.31–8.20) | <.001 | 5.03 (2.57–9.87) |
| PWID | 1 (1) | 0.16 (0.02–1.25) | .06 | 0.15 (0.02–1.22) |
| HAP | 16 (23) | 1.75 (0.83–3.66) | .137 | 2.17 (0.96–4.92) |
| Sputum sample | 35 (50) | 0.58 (0.32–1.04) | .067 | 0.48 (0.25–0.92) |
| Receipt of vasopressor therapy | 20 (29) | 1.16 (0.61–2.23) | .65 | Not tested |
| ID consultation | 13 (19) | 1.20 (0.56–2.56) | .65 | Not tested |
Note. PWID, persons who inject drugs; HAP, hospital-acquired pneumonia; ID, infectious diseases; OR, odds ratio; CI, confidence interval.
Hosmer Lemeshow goodness of fit, 0.727.
In total, 79 patients (79%) met the definition of clinical success in the preintervention group, compared to 81 patients (81%) in the postintervention group (P = .54). All-cause, in-hospital mortality occurred in 15 patients (15%) in the preintervention group and 9 patients (9%) in the postintervention group (P = .18). C. difficile infection occurred in 4 patients (4%) in the preintervention group and 2 patients (2%) in the postintervention group (P = .45).
Discussion
Optimal de-escalation significantly improved after implementation of an interpretive β-lactamase comment, with no negative impact on patient outcomes. Our findings suggest that prescribers may be unfamiliar with the meaning of β-lactamase results for M. catarrhalis and H. influenzae and that they are more likely to act in response to a purposeful comment. This unfamiliarity could be related to the misconception that all β-lactamase–producing organisms reflect resistance requiring broad-spectrum antibiotic therapy (ie, carbapenem). These data add to the body of literature on nudging providers into action using a framing microbiology comment. 3–6
This study had several limitations. This study may have been subject to maturation bias and/or regression to the mean. To evaluate for maturation, we used a nonequivalent dependent variable of DVT prophylaxis to assess quality of medication management, which was not improved in the intervention group. LRTI specimen quality can also be considered a limitation because this could influence prescriber comfort with de-escalation. The capacity of an institution to adopt microbiology-culture comment nudges may be a limiting factor in generalizability to other centers without advanced microbiology services.
Microbiology nudges are pragmatic, sustainable stewardship interventions that can be reproduced in most settings without substantial resources. 3,10 An interpretative β-lactamase comment for M. catarrhalis and H. influenzae was associated with improved definitive therapy prescribing. This study supports nudging within the EMR to positively influence antibiotic prescribing.
Acknowledgments
The authors report no notable acknowledgements related to this study.
Financial support
No financial support was utilized to conduct this study.
Conflict of interest
All authors report no conflicts of interest relevant to this article.
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