Introduction
Clostridioides difficile is a spore-forming, gram-positive anaerobic bacteria that causes infections ranging from colonization to fulminant colitis. Reference Kelly, Pothoulakis and Lamont1,Reference Karas, Enoch and Aliyu2 C. difficile infection (CDI) is the most common cause of healthcare-associated infectious diarrhea and causes significant morbidity and mortality resulting in substantial cost to the healthcare system. Reference Guh, Mu and Winston3,Reference Mora Pinzon, Buie and Liou4 Despite resolution after treatment, CDI recurrence is common. Current estimates are that approximately 10%–30% of patients treated for CDI will have at least 1 recurrence. Reference Zilberberg, Shorr, Jesdale, Tjia and Lapane5 Risk for recurrence varies depending on initial treatment selection, administration of other systemic antibiotics, reduced immune response, advancing age, or severe underlying disease. Reference Kociolek, Gerding and Carrico6 Patients with recurrence may require rehospitalization due to the severity of the disease. Reference Benitez, Shehadeh and Kalligeros7 Rehospitalizations are a particular focus of the Centers for Medicare and Medicaid Services (CMS), and improvements in care coordination at discharge are important to prevent recurrence and rehospitalization. 8
Multiple studies have demonstrated the benefit of early patient follow-up after hospitalization in reducing rehospitalization, especially but not exclusively, with regard to heart failure and chronic obstructive pulmonary disease. Reference Anderson, Mills and Willits9 The benefit of follow-up appointments for CDI has not been previously described. Specialty providers, such as infectious diseases (ID) or gastroenterology (GI), are uniquely trained to manage potential complex gastrointestinal infections, such as CDI. Consultations from these providers may occur during hospitalization to provide recommendations regarding initial or discharge management. In conjunction or alternatively, patients may see specialty providers following discharge from the hospital for follow-up and ongoing management of CDI. There is a growing body of evidence that while inpatient evaluation by specialists is critical for patient care for numerous diseases, rehospitalization reduction is strongly influenced by close post-discharge follow-up. Reference Anderson, Mills and Willits9–Reference Goto, Schweizer and Vaughan-Sarrazin13
The purpose of our study was to evaluate critical influences on rehospitalization related to CDI.
Methods
Study design and population
This study was a single-center, retrospective cohort study of patients who tested positive for C. difficile and who were admitted at a 547-bed tertiary academic medical center located outside of Chicago, Illinois, and were subsequently discharged from the hospital from January 1, 2018, through December 31, 2018. Hospital protocol allowed for C. difficile testing of any patient within the first 72 hours of hospitalization with a stool that nursing staff deemed as “loose” without physician review. After 72 hours, testing required an infection control review. The study was reviewed by the Loyola Institution Review Board and deemed exempt (IRB no. 213449).
Study definitions and outcomes
A C. difficile event (CD event) during the index hospitalization was defined as a person having a positive C. difficile polymerase chain reaction (PCR) test (GI panel PCR, FilmArray, Biofire, or C. difficile PCR, Xpert CD assay, Cepheid). For analysis, these events were divided into primary CD event and recurrent CD event. A primary CD event was defined as a positive C. difficile test with no positive C. difficile test within 8 weeks of the index hospitalization. A recurrent CD event was defined as a positive C. difficile test, and the patient had a positive C. difficile test within 2–8 weeks prior to the index event.
The primary outcome was rehospitalization due to a CDI within 60 days of the index hospitalization discharge. CDI was defined as a positive C. difficile PCR within 2–8 weeks of the positive test during the index event with documented evidence of diarrhea and a clinical scenario consistent with a CDI within the electronic medical record (EMR). Patients diagnosed as having C. difficile are at risk for developing a recurrent case up to 8 weeks after completing therapy; thus, rehospitalization within 60 days was selected for the primary endpoint rather than within 30 days because the CMS 30-day hospital readmission metric may fail to capture all patients at risk for developing a subsequent CDI after the index hospitalization. 8,Reference McDonald, Coignard, Dubberke, Song, Horan and Kutty14 The secondary outcomes were rehospitalization due to a CDI within 30 days of discharge and all-cause rehospitalization at 60 days. Patients with planned hospitalizations were excluded from all-cause rehospitalization analysis (ie, chemotherapy, elective surgery [n = 6]). CDI-related rehospitalization was defined as a patient requiring rehospitalization in which CDI was listed as a primary cause of admission in the rehospitalization discharge note.
Data collection
The EMR was manually chart reviewed for all patients who tested positive for C. difficile to extract data pertaining to demographics, white blood cell (WBC) count (cells/mL), creatinine (mg/dL), temperature (Celsius), Charlson Comorbidity Index (CCI) Reference Charlson, Pompei, Ales and MacKenzie15 , use of proton pump inhibitors (PPI) or histamine receptor type 2 antagonist (H2RA), immunosuppressed status, admitting physician service, ID or GI inpatient consultation, post-discharge clinical follow-up, systemic antibiotic exposures up to 60 days after hospital discharge, and CDI treatment.
Variable definitions
CDI treatment was defined as the receipt of antibiotics directed toward C. difficile for >48 hours. In patients that received CDI treatment, the variable was subdivided into treatment with a standard 10-day oral vancomycin regimen, an oral vancomycin taper regimen, a 10–14-day metronidazole regimen, and “other” regimens. Other regimens included fidaxomicin treatment (n = 1) and other nonstandard treatment regimens as defined by the IDSA/SHEA 2021 guidelines. Reference Johnson, Lavergne and Skinner16 Immunosuppressed was defined as a patient having a current diagnosis of solid organ malignancy, uncontrolled human immunodeficiency virus (HIV) (CD4 <200 and not currently on HIV therapy), autoimmune disease, history of organ transplantation, lymphoma, leukemia, multiple myeloma, or receipt of medications with known immunocompromising effects such as long-term steroids (eg, 20 mg of prednisone [or equivalent] for ≥20 days) for any reason not listed above. Post-discharge clinical follow-up addressing C. difficile was defined as any clinical follow-up within 60 days of discharge (ie, primary care provider or specialist) after the index hospitalization with EMR documentation by the provider addressing C. difficile. Exposure to systemic antibiotics was defined as antibiotic use that was not for CDI. Post-hospitalization data was collected up to 60 days after discharge from the hospital or until the patient was hospitalized for any cause.
Patient exclusions
Individuals were excluded from analysis if they died or entered hospice during hospitalization, were lost to follow-up immediately upon discharge (defined as no record of any further care in the EMR up to 90 days after hospital discharge), or were placed on long-term C. difficile suppression beyond the study period, the CDI treatment regimen prescribed during the index event was completed less than 14 days prior to the end of the study period (60 days from patient discharge), the patient died prior to completing CDI therapy, or CDI therapy was completed >30 days prior to discharge from the hospital during the index event. Exclusion criteria were selected to reduce potential confounding for patients in which CDI could not be reasonably assessed. To assess for selection bias, baseline demographics of excluded patients were assessed separately (data not shown).
Statistical analysis
All statistical analyses were conducted using R v4.3.1. Significance was defined as a p-value of ≤ 0.05, and all tests were two-tailed. Fisher exact test and χ Reference Karas, Enoch and Aliyu2 test were used to assess for differences in proportions across categorical variables for individuals who developed a CDI within 60 days of the index hospital discharge and individuals who did not develop a CDI. The normality of continuous variables was determined by the Kolmogorov–Smirnov method. Wilcoxon signed-rank test was used to compare nonparametric variables, and the Student t test was used to compare parametric variables. Nonparametric variables were reported as median with interquartile range (IQR), and parametric variables were reported as mean with 95% CI.
Time-to-event methods were utilized to assess the effect of key variables on 60-day CDI-related rehospitalization for patients who developed CDI after the index hospitalization discharge (n = 68). Kaplan–Meier method was used to determine the unadjusted relationship between both systemic antibiotic exposure within 60 days of hospital discharge and time to rehospitalization as well as post-discharge clinical follow-up and time to rehospitalization. Individuals were censored on the day that they died, entered hospice, were lost to follow-up, or were rehospitalized for any cause. Log-rank test was used to assess the difference between the survival curves.
Cox proportional hazard regression methods were utilized to estimate the crude and adjusted hazard ratios (cHR and aHR) reported with 95% CI for variables that were determined to reasonably affect rehospitalization related to CDI in patients who developed a CDI. Time-zero for the Cox proportional hazard model was defined as the day of index hospitalization discharge.
The variables that were deemed to reasonably affect rehospitalization related to CDI included during the index hospitalization were (1) age ≥65 years old, (2) a stratified CCI (CCI: ≤1, 2–3, and ≥4), (3) serum WBC (cells/mL), (4) serum creatinine (mg/dL), (5) immunosuppressed status, (6) index case classified as recurrent CD event, (7) inpatient admitting service (medical service), (8) treatment of C. difficile, (9) ID consultation while inpatient, (10) GI consultation while inpatient, (11) in-person post-discharge clinical follow-up appointment for C. difficile after index event, and (12) receipt of systemic antibiotics prior to rehospitalization or up to the end of 60-day study period in patients not rehospitalized.
The multivariable model included all variables that were significant in univariate analysis. Additionally, we included the stratified CCI variable due to a known risk of all-cause rehospitalization associated with a higher CCI and because multiple components of the CCI are known risk factors for CDI (ie, age, immunosuppression, renal disease). Reference Wei, Sun, Chen, Meng and Wu17,Reference McDonald, Gerding and Johnson18 To reduce the potential for multicollinearity with CCI, the variables age ≥65, serum creatinine, and immunosuppressed status were excluded from the multivariable model. The remaining variables were added in a stepwise fashion and compared by –2 log-likelihood comparison. The model that provided the best fit was chosen as the final model. Model assumptions were assessed via Schoenfeld residuals and log-log plots.
Results
From January 1, 2018, to December 31, 2018, we identified 559 individual cases of a positive C. difficile test during that hospitalization (Figure 1). Among these 559 cases, 33 were excluded as the individuals either died or were enrolled in hospice prior to discharge. Another 85 cases were excluded as the individuals were lost to follow-up immediately on hospital discharge. Another 33 were excluded as they were placed on long-term CDI suppression with vancomycin, a treatment course beyond the study period, died prior to completing CDI therapy or had completed CDI therapy >30 days prior to hospital discharge. After exclusion, there were 408 index cases available for review (Figure 1).
Demographics
Of the 408 cases included for analysis, 51.2% (209 of 408) were female, and the median age was 63 (IQR: 51–72). Prior to the index event, 16.9% (69 of 408) of individuals with a case had been diagnosed as having CDI within the past 6 months, and 45.8% (187 of 408) were classified as immunosuppressed (Table 1). Primary CD events accounted for 85.8% (350 of 408) of cases, and 14.2% (58 of 408) of the index cases were classified as recurrent CD events (Table 1).
No, number; %, percent; IQR, interquartile range; CDI, C. difficile infection; PPI, proton pump inhibitor; H2A, Histamine Type-2 Receptor Antagonist; WBC, white blood cell; †severe CDI defined as WBC >15,000 cells/mL or creatinine ≥1.5 mg/dl.
All-cause rehospitalization
Among all cases, 46.1% (188 of 408) of individuals were rehospitalized for any reason within 60 days. The median time to rehospitalization for all patients was 23 days (IQR: 12–36). Among the study population, there were multiple reasons for rehospitalization. After excluding planned rehospitalization within 60 days of discharge (n = 6), the most common reason for rehospitalization at 60 days was CDI (49 of 182 [26.9%]) (Figure 2).
Patients with CDI after discharge
For the entire study population, 68 of 408 (16.7%) had a CDI within 60 days of hospital discharge, and 49 of 68 (72.1%), or 12.2% (49 of 408), were rehospitalized within 60 days for the management of CDI. Among the 68 patients who developed CDI post-hospitalization, 64.7% (44 of 68) developed CDI within 30 days of discharge, and 72.3% (32 of 44) were rehospitalized for the management of CDI. Of 24 patients who developed a CDI between days 31 and 60, 70.8% (17 of 24) were rehospitalized for the management of CDI within 60 days of discharge.
Risk of CDI-related rehospitalization for patients with CDI after discharge
The Kaplan–Meier results reveal the CDI-related rehospitalization rate was lower in individuals who had post-discharge follow-up addressing the previous positive C. difficile test and was higher among individuals who were exposed to systemic antibiotics (Figure 3). Univariate Cox proportional hazard results revealed multiple factors that could have affected the rate of rehospitalization among individuals who developed a CDI (n = 68). There was an increased rate of rehospitalization among persons who had either been admitted to a medical service (cHR: 3.35; 95% CI, 1.20–9.35), who were treated with metronidazole (cHR: 4.65; 95% CI, 1.37–15.80), or who were exposed to systemic antibiotics up to 60 days from index hospitalization discharge (cHR: 1.92; 95% CI, 1.06–3.44). Inversely, the rate of CDI-associated rehospitalization decreased in individuals who received a post-discharge hospital follow-up addressing CDI management in the clinic (cHR: 0.49; 95% CI, 0.28–0.88) (Table 2).
No, number; %, percent; CI, confidence interval; ID, infectious diseases; GI, gastrointestinal; CDI, C. difficile infection; WBC, white blood cell count.
Antimicrobial dosing: metronidazole: 500 mg 3 times daily for 10–14 days; standard vancomycin regimen: 125 mg 4 times daily for 10–14 days; vancomycin Taper: 125 mg 4 times day for 10–14 days followed by vancomycin taper/pulse regimen that varied in duration by provider.
† Indication that variable was not included in final model; REF, reference group used for comparison under variable header.
After adjustment, rehospitalization rates for CDI remained increased for patients admitted to a medical service (aHR: 3.15; 95% CI, 1.09–9.14) and for patients who were exposed to systemic antibiotics (aHR: 2.78; 95% CI, 1.36–5.64). As with the univariate analysis, patients who had a post-discharge clinical follow-up in which C. difficile was addressed had a decreased rate of CDI rehospitalization (aHR: 0.53; 95% CI, 0.28–0.98) (Table 2).
Discussion
Rehospitalization is an important healthcare concern and should be a priority of hospital leadership. 8 Prior studies have evaluated the impact of post-discharge follow-up on reducing rehospitalizations following disease states other than CDI. However, there is a paucity of data evaluating the impact of post-discharge follow-up after CDI on rehospitalizations. Reference Anderson, Mills and Willits9 Approximately 16% of individuals included in our study developed a CDI after hospital discharge, which is consistent with estimates previously published in the literature. Reference Zilberberg, Shorr, Jesdale, Tjia and Lapane5 The most common cause for rehospitalization was CDI, and most of the patients who developed a CDI following discharge were rehospitalized. Together, these data highlight CDI as an area for focus to reduce overall rehospitalizations.
Although only 12% of all index CD events were rehospitalized for CDI following discharge, we believe targeting post-discharge follow-up is one potential strategy to reduce CDI-related rehospitalizations. Current estimates indicate that the average rehospitalization cost is $15,200 per patient. Reference Weiss and Jiang19 Within our study, 118 patients had an unplanned rehospitalization within 30 days, and 182 patients had an unplanned rehospitalization within 60 days, which would result in approximately $1.8 million and $2.7 million in rehospitalization cost within 30 and 60 days of discharge, respectively. Thirty-day rehospitalization is a particular priority of CMS and, as such, is a focus of many hospitals’ leadership. 8 Given the age and co-morbid medical conditions found in persons typically diagnosed as having CDI, they are a population at high risk for hospitalization at baseline. Reference McDonald, Gerding and Johnson18 However, CDI can significantly affect multiple systems. Given the significant volume depletion and extracellular fluid contraction often associated with CDI diarrhea, an associated impact could be found on persons with co-morbidities such as heart failure or cirrhosis. Reference Miller20,Reference Aithal, Palaniyappan and China21 These persons are often sensitive to volume shifts and would likely require close follow-up for these non-CDI-related issues. Additionally, hospitalization increases the risk of non-CDI-related infections. Although many hospitals have implemented infection control practices to minimize these risks, hospitalization places persons at risk for subsequent infections including infection due to multidrug-resistant organisms, sepsis, urinary tract infections, and pneumonia. Reference Boev and Hospital-Acquired Infections22,Reference Olsen, Keller, Stwalley, Yu and Dubberke23 Moreover, these subsequent infections continue to increase the risk of subsequent development of a CDI likely because of additional systemic antibiotic exposures. Reference Kociolek, Gerding and Carrico6 Within our study, we found that the 2nd most common cause of rehospitalization was another infectious etiology. Our study was unable to capture if these cases went on to develop a further CDI, but given that our data reveal an increased rate of rehospitalization related to CDI with systemic antibiotics, these individuals were at increased risk. Further study is required to determine which systemic antibiotics increase the risk of rehospitalization.
When accounting for only CDI-related rehospitalization at 30 and 60 days post-discharge, this would equate to $486,400 and $729,600 per current rehospitalization cost estimates. Reference Weiss and Jiang19 Within our study, we found a hazard reduction of 47% for rehospitalization for persons who had post-discharge follow-up for CDI at 60 days. This would indicate a significant amount of savings for a hospital.
These data further show the need for a reduction in rehospitalizations related to CDI in patients initially hospitalized with a CD event. Given the increased rate of rehospitalization due to recurrence in those who received systemic antibiotics within 60 days after discharge, ensuring coordination of multispecialty care and communication may prove beneficial. Comprehensive transitions of care should be further studied, particularly in those individuals discharged from the hospital following a CD event. We believe that the key components that warrant the most attention in future studies are the benefit of discharge planning in patients with positive C. difficile testing, including a timely post-hospitalization clinic appointment, providing C. difficile medication instructions (if indicated), symptoms of C. difficile to monitor for, and a point of contact if they have questions. Additionally, studying the impact of reviewing antibiotics prior to discharge in this population and ensuring dedicated follow-up to confirm continued resolution would provide context into possible interventions.
Our study is not without limitations. As a retrospective study, there is the possibility of unmeasured confounding. However, a robust chart review and the interconnection of multiple EMRs from multiple hospitals allowed us to collect additional data to reduce potential confounding. Individuals were included with a positive PCR test, regardless of toxin testing, thus potentially including individuals who were colonized. However, recent data have revealed that persons who are colonized may also be at increased risk for developing a true CDI when exposed to systemic antibiotics. Reference Miles-Jay, Snitkin and Lin24,Reference Crobach, Hornung and Verduin25 Additionally, strain typing data were not available; thus, we cannot account for the potential impact of outbreak strains with increased risk for CDI recurrence. At the time these data were collected, vancomycin was the preferred treatment option. As fidaxomicin is now the recommended treatment for persons with primary CDI and recurrent CDI, this treatment may affect recurrence rates and thus affect the number of persons rehospitalized for CDI. Reference Johnson, Lavergne and Skinner16 Lastly, our determination of hospital follow-up is reliant on narrative documentation and may not fully capture conversations between patients and providers.
Conclusions
There are numerous facets that could affect rehospitalization related to CDI. These data indicate that dedicated hospital follow-up and antimicrobial stewardship could reduce CDI-associated rehospitalizations. Further study is required to assess these critical steps within patient transitions of care addressing C. difficile that is detected during hospitalization and how to best prevent rehospitalization.
Acknowledgments
We would like to thank Erik Dubberke and L. Clifford McDonald for reviewing the manuscript and providing feedback.
Author contributions
E. N. D., S. J., and A. M .S. conceptualized the research question. E. N. D. and A. M. S. contributed to data collection and curation. E. N .D., S. J., L. H. D., and A. M. S. contributed to the methodology design and wrote the original draft. A. M. S. and S. J. provided supervision. All authors contributed to reviewing and editing the manuscript.
Financial support
A. M. S. and S. J. receive funding through the US Veteran Affairs. This work was supported in part by the National Center for Advancing Translational Sciences of the National Institutes of Health (NIH) that funds the Institute for Translational Medicine (grant no. 5KL2TR002387 to AS) and the US Department of Veterans Affairs Biomedical Laboratory Research and Development Service (grant no. IK2BX005609 to AS). The content is solely the responsibility of the authors and does not necessarily represent the official views of the NIH, the US Veterans Affairs, or the US Government.
Competing interests
S. J. has served as a consultant for Acurx Pharmaceuticals, Inc., Bio-K+ International, and Ferring Pharmaceuticals. L. H. D. has served as a consultant for Ferring Pharmaceuticals. A. M. S. has served as a consultant for Bio-K+ International, Ferring Pharmaceuticals, and Recursion Pharmaceuticals. S. J. and A. M. S. have previously received research funding from Paratek Pharmaceuticals (paid to institution). E. N. D. has no disclosures.