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A systematic literature review and bayesian meta-analysis of oral vancomycin primary prophylaxis for Clostridioides difficile infection in stem cell transplant patients

Published online by Cambridge University Press:  14 October 2025

Erika Viana-Cardenas Open the ORCID record for Erika Viana-Cardenas [Opens in a new window] ,
Eugenia Miranti Open the ORCID record for Eugenia Miranti [Opens in a new window] ,
Wajeeha Tariq ,
Guillermo Rodriguez-Nava ,
Sa Shen ,
Evans Whitaker Open the ORCID record for Evans Whitaker [Opens in a new window] ,
Mingjun Jiang ,
Mindy M. Sampson Open the ORCID record for Mindy M. Sampson [Opens in a new window] ,
Andrew Rezvani  and
Ami S. Bhatt
...Show all authors
Erika Viana-Cardenas*
Affiliation:
Division of Infectious Diseases and Geographic Medicine, Stanford University School of Medicine, Stanford, CA, USA
Eugenia Miranti
Affiliation:
Division of Infectious Diseases and Geographic Medicine, Stanford University School of Medicine, Stanford, CA, USA
Wajeeha Tariq
Affiliation:
Division of Infectious Diseases and Geographic Medicine, Stanford University School of Medicine, Stanford, CA, USA
Guillermo Rodriguez-Nava
Affiliation:
Division of Infectious Diseases and Geographic Medicine, Stanford University School of Medicine, Stanford, CA, USA
Sa Shen
Affiliation:
Quantitative Sciences Unit, Stanford University, Stanford, CA, USA
Evans Whitaker
Affiliation:
Lane Medical Library, Stanford University School of Medicine, Stanford, CA, USA
Mingjun Jiang
Affiliation:
Department Civil and Environmental Engineering, Stanford University, Stanford, CA, USA
Mindy M. Sampson
Affiliation:
Division of Infectious Diseases and Geographic Medicine, Stanford University School of Medicine, Stanford, CA, USA
Andrew Rezvani
Affiliation:
Division of Blood and Marrow Transplantation, Stanford University School of Medicine, Stanford, CA, USA
Ami S. Bhatt
Affiliation:
Department of Medicine (Hematology) and of Genetics, Stanford University School of Medicine, Stanford, CA, USA
Alexandre R. Marra
Affiliation:
Department of Internal Medicine, University of Iowa Carver College of Medicine, Iowa City, IA, USA Faculdade Israelita de Ciências da Saúde Albert Einstein, Hospital Israelita Albert Einstein, São Paulo, SP, Brazil
Jorge L. Salinas
Affiliation:
Division of Infectious Diseases and Geographic Medicine, Stanford University School of Medicine, Stanford, CA, USA
*
Corresponding author: Erika Viana-Cardenas; Email: epviana@stanford.edu

Abstract

Introduction:

Clostridioides difficile infection (CDI) is common among patients undergoing hematopoietic stem cell transplantation (HSCT). Oral vancomycin prophylaxis may effectively prevent CDI in certain populations. We investigated the effectiveness of oral vancomycin primary prophylaxis in preventing CDI in HSCT patients.

Methods:

We searched six databases from inception to March 21, 2025, for studies comparing the incidence of CDI in HSCT patients who received oral vancomycin primary prophylaxis versus those who did not. We built a Bayesian random-effects model for meta-analysis. The primary outcome was the incidence of CDI. Secondary outcomes included incidence of positive vancomycin-resistant Enterococcus cultures, blood stream infections, graft-vs-host disease, and length of hospital stay. We also assessed for heterogeneity and publication bias using Robust Bayesian Meta-Analyses.

Results:

Six studies met inclusion criteria with a total of 1,236 patients. Four of the studies were of fair to good quality. Oral vancomycin primary prophylaxis reduced the incidence of CDI during hospitalization (OR 0.31; 95%CrI 0.16–0.59). Studies were weakly heterogeneous but had strong publication bias. Oral vancomycin primary prophylaxis reduced the odds of CDI by 12% after accounting for publication bias (OR 0.88; 95%CrI 0.32–1.16), although this reduction was not statistically significant. Secondary outcomes were similar in both groups.

Conclusion:

Oral vancomycin primary prophylaxis prevented CDI in HSCT patients without significantly affecting secondary outcomes. However, after controlling for publication bias, these findings were no longer significant. Further studies are needed to provide stronger evidence for or against this intervention, assess long-term safety, and assess potential effects on antimicrobial resistance.

Information

Type
Original Article
Information
Antimicrobial Stewardship & Healthcare Epidemiology , Volume 5 , Issue 1 , 2025 , e265
Creative Commons
Creative Common License - CCCreative Common License - BY
This is an Open Access article, distributed under the terms of the Creative Commons Attribution licence (https://creativecommons.org/licenses/by/4.0/), which permits unrestricted re-use, distribution and reproduction, provided the original article is properly cited.
Copyright
© The Author(s), 2025. Published by Cambridge University Press on behalf of The Society for Healthcare Epidemiology of America

Introduction

Clostridioides difficile infection (CDI) is common and consequential among patients undergoing hematopoietic stem cell transplantation (HSCT), particularly allogeneic hematopoietic stem cell transplant recipients. Reference Misch and Safdar1 Estimates of incidence of CDI in the first-year posttransplant range from ∼15–30%. Reference Bhutani, Jaiyeoba and Kim2,Reference Ramanathan, Kim and He3 The development of CDI in this population has been associated with an increased risk of graft-versus-host disease (GVHD) and mortality. Reference Alonso, Treadway and Hanna4,Reference Chakrabarti, Lees, Jones and Milligan5 Colonization with C. difficile is also prevalent among HSCT patients, with rates ranging from 9.3% to 29%. Reference Cannon, Musuuza and Barker6Reference Bruminhent, Wang and Hu8 Colonization is associated with a higher risk for progression to CDI—which may be mitigated by providing prophylaxis to colonized patients. Reference Turner, Grambow and Polage9

Several studies have indicated that oral vancomycin prophylaxis may effectively prevent CDI, particularly when used as secondary prophylaxis. Reference Johnson, Brown and Priest10Reference Caroff, Menchaca and Zhang12 There is great interest in whether oral vancomycin may also prevent CDI in the HSCT population, given their particularly high rates of CDI. However, there is also concern that oral vancomycin prophylaxis might lead to deleterious secondary outcomes such as vancomycin-resistant Enterococcus infection. To date, observational studies have not identified an impact of oral vancomycin prophylaxis on vancomycin-resistant Enterococcus infection rate. Reference Stevens, Khader and Echevarria13Reference Salgado, Giannetta and Farr17 In the immunocompromised HSCT population, there is the additional risk for GVHD and in increased risk for bloodstream infection. Reference Poutsiaka, Munson, Price, Chan and Snydman18 Both could potentially be the result of alterations in the microbiome by oral vancomycin prophylaxis.

We aimed to investigate the effectiveness of oral vancomycin primary prophylaxis in preventing CDI in HSCT patients. By analyzing data from multiple studies, we sought to 1) provide a clearer understanding of the impact of oral vancomycin prophylaxis on CDI incidence, and 2) explore the impact of oral vancomycin prophylaxis on GVHD, vancomycin-resistant Enterococcus infection risk, bloodstream infection risk, and length of hospital stay. Our findings will contribute to the growing body of evidence evaluating the use of vancomycin as a prophylactic measure in the high-risk HSCT population.

Methods

Systematic literature review and search strategy

This systematic literature review was carried out following the guidelines set forth by the Preferred Reporting Items for Systematic Reviews and Meta-Analyses (PRISMA), Reference Liberati, Altman and Tetzlaff19 and the Bayesian Analysis Reporting Guidelines (BARG). Reference Kruschke20 The review was registered with the International Prospective Register of Systematic Reviews (PROSPERO) on March 21, 2025 (CRD420251016925), with its protocol included. Approval from the Institutional Review Board was not necessary for this study and no patient informed consent was required either.

Our search strategy was developed in March 2025 with the assistance of a health sciences librarian. We explored Embase, PubMed, Scopus, Web of Science, Cochrane, and CINAHL. The literature search included manuscripts published from the inception of each database up to May 21, 2025. The detailed search strategy is available in the Supplementary Table 1.

Studies were included if they evaluated the incidence of CDI in patients who received oral vancomycin prophylaxis compared to those who did not. CDI was defined as detection of a positive nucleic acid amplification testing (NAAT) and/or reflex to toxin enzyme-linked immunosorbent assay for C. difficile, ideally in a two-step testing, in patients with new onset diarrhea (24 h or less). Reference Turner, Grambow and Polage9 Primary prophylaxis was defined as the use of a drug to prevent disease in at-risk individuals with no prior history, while secondary prophylaxis aimed to prevent the recurrence of a disease in patients who have already experienced it. The intervention was defined as providing oral Vancomycin 125 mg twice daily, starting on the day of inpatient admission and continued until discharge. We excluded comments or reviews, studies that focused on secondary CDI, studies without a comparable control group, studies where controls received a different intervention (other than standard of care), pilot studies, and studies that used the same hospital population of an already included study.

We identified a total of 164 studies from our literature search. After removing duplicates, 132 studies were screened using title and abstract by two independent reviewers (WT and EV). From this initial review, 23 full-text studies were independently assessed (WT and EV). Discrepancies were resolved through discussion or consultation with a third reviewer (EM). Ultimately, six studies met inclusion criteria and were included in this systematic review.

Data abstraction form and quality assessment

Two independent reviewers (WT, EM) abstracted data for each article using a standardized abstraction form. We recorded data regarding authors, publication year, study period, design, population selection, setting, inclusion and exclusion criteria of each study, studied groups, prophylaxis regimen, CDI diagnostic criteria, number of participants, total number of participants receiving the intervention, number of CDI per group, and secondary outcomes analyzed. Our primary outcome was the incidence of CDI in patients who received oral vancomycin prophylaxis and those who did not. Our secondary outcomes were bloodstream infections, vancomycin-resistant Enterococcus cultures, GVHD, and length of hospital stay.

We used the Downs and Black scale to assess quality of studies, which is specifically designed for randomized and non-randomized studies. Reference Downs and Black21 All questions of the original published scale were answered for each reviewed paper and the total score calculated. We adapted question 27 of the Downs and Black scale replacing the multiple-choices options with a yes/no answer. The maximum possible score was 28. Downs and Black score ranges were given corresponding quality levels: excellent (26–28); good (20–25); fair (15–19); and poor (≤14). The reviewers (WT, EM, EV) performed the quality analysis independently and inconsistencies were resolved by discussion.

Statistical analysis

Effect sizes and their standard errors were calculated from the sample sizes and reported cases for each study using the metafor package in R (version 4.8-0). The meta-analysis was conducted with the bayesmeta package version 3.4, employing Bayesian random-effects models. Reference Röver22 The Bayesian approach is especially useful to account for between-study heterogeneity. Additionally, unlike frequentist methods, it does not require a larger number of studies and directly provides credible intervals for the pooled mean effect. Half-normal prior was applied for both the overall effect and heterogeneity parameters. Heterogeneity is calculated using tau (τ), an estimate of the amount of true variability between the effect sizes of the included studies in a random-effects meta-analysis model. Results were summarized by reporting the posterior mean as an odds ratio (OR), along with 95% credible intervals (95% CrI) for the overall effect size and the tau statistic to quantify heterogeneity among the studies. And the prediction describes the consistency of data and model by comparing the actual data to data sets predicted via the posterior distribution. Reference Röver22

The potential for publication bias was assessed using funnel plot, Egger’s test, and the Robust Bayesian Meta-Analyses (RoBMA) package version 3.4.0. Reference Maier, Bartoš and Wagenmakers23 RoBMA results use Bayes factors (BF), a continuous measure of evidence in favor of the presence or absence of effect, heterogeneity, and publication bias. Bayes factor values above 10 indicate very strong evidence, from 3 to 10 moderate evidence, and from 1 to 3 weak evidence and <1 no evidence. Reference Wagenmakers and Lee24 Sensitivity analyses assessed the robustness of findings by excluding studies with unpublished full-text manuscripts. All analyses were performed using R version 2024.12.0 + 467.

Results

Study characteristics

From the 164 studies identified on the search strategy, a total of six met inclusion criteria to be in this systematic literature review and meta-analysis (Figure 1 and Table 1). Of them, four were studies published in full-text, Reference Altemeier and Konrardy25Reference Williams, Atienza and Franzen28 and two were published abstracts. Reference Ogawa, Wright and Luk29,Reference Vartanov, Shestovska and Hamby30 Five of them were conducted in academic medical centers, and one in a community hospital. Reference Williams, Atienza and Franzen28 All were conducted in the United States. Studies were performed between January 2012 and May 2023, and their duration varied from 11 to 120 months. In all six studies, patients received oral vancomycin 125 mg twice daily, starting on the day of inpatient admission and continued until discharge.

Figure 1. Literature search for studies published up to March 21, 2025, that evaluated the impact of oral Vancomycin prophylaxis for Clostridioides difficile infection in stem cell transplant patients.

Table 1. Summary of study characteristics

Abbreviations: AlloHCT, allogenic hematopoietic stem cell transplantation; AutoHSCT, autologous hematopoietic stem cell transplantation; CAR T-cell therapy, chimeric antigen receptor T-cell therapy; CDI, Clostridioides difficile infection; EIA, enzyme immunoassay; GVHD, graft-versus-host disease; HSCT, hematopoietic stem cell transplantation; OVP, oral vancomycin prophylaxis; PCR, polymerase chain reaction; N/A, Not available; VRE, vancomycin-resistant Enterococci.

All included studies were quasi-experimental: they conducted retrospective chart reviews, gathering data from both control and intervention populations before and after implementing the intervention. The intervention group included all patients admitted to the Bone Marrow Transplant unit after the implementation of oral vancomycin prophylaxis for HSCT. By contrast, the control group consisted of all patients from the same unit who underwent stem cell transplantation before the prophylaxis was introduced and did not receive this treatment.

All six studies reported the total number of participants (n = 1,236) with and without CDI as their primary outcome. The definition of CDI was explicitly discussed in five studies, while one study did not provide this information. Reference Ogawa, Wright and Luk29 Four studies employed a two-step diagnostic algorithm that combined immunoassay and NAAT for diagnosis, whereas one study utilized only NAAT. Reference Altemeier and Konrardy25 Two studies specified that testing was conducted for patients exhibiting clinical symptoms, defined as having more than three unformed stools within a 24-hour period, Reference Altemeier and Konrardy25,Reference Williams, Atienza and Franzen28 while one study indicated that testing was performed based on compatible clinical presentations. Reference Reitmeyer, Rana and Awad27 Notably, none of the studies assessed C. difficile colonization at baseline.

Outcomes

A Bayesian meta-analysis was conducted to estimate the pooled mean effect of the intervention across the six studies. Unadjusted analysis showed that oral vancomycin prophylaxis was associated with a reduced incidence of CDI, with a mean OR of .31 (95% CrI: .16 – .59), see Figure 2. A sensitivity analysis including only the four studies published in full text yielded similar results (mean OR: .24; 95% CrI: .11 – .56), see Figure 3.

Figure 2. Forest plot of unadjusted Clostridioides difficile infection risk in stem cell transplant patients: impact of oral Vancomycin primary prophylaxis.

Figure 3. Forest plot of unadjusted Clostridioides difficile infection risk in stem cell transplant patients: impact of oral Vancomycin primary prophylaxis, full-text published studies only.

Further analysis was conducted to estimate the overall mean effects of secondary outcomes across the studies, including bloodstream infections (OR 1.10; 95% CrI .65 – 1.81), positive vancomycin-resistant Enterococcus cultures (OR .75; 95% CrI .31 – 1.78), GVHD (OR 1.21; 95% CrI .59 – 2.47), and length of hospital stay (OR .90; 95% CrI .29 – 2.72). However, none of these assessments demonstrated a statistically significant effect (details available in the Supplementary Section).

A variety of secondary outcomes were studied: Four studies reported on bloodstream infections, Reference Altemeier and Konrardy25Reference Reitmeyer, Rana and Awad27,Reference Vartanov, Shestovska and Hamby30 while four also examined vancomycin-resistant Enterococcus isolated from any clinical culture. Reference Altemeier and Konrardy25Reference Reitmeyer, Rana and Awad27,Reference Ogawa, Wright and Luk29 Three studies focused on GVHD. Reference Altemeier and Konrardy25,Reference Ganetsky, Han and Hughes26,Reference Ogawa, Wright and Luk29 Lengths of hospital stay were reported in days by five studies; among these, two provided estimates of variability, Reference Reitmeyer, Rana and Awad27,Reference Williams, Atienza and Franzen28 two did not report variability estimates, Reference Altemeier and Konrardy25,Reference Ganetsky, Han and Hughes26 and one study stratified length of stay by transplant type, including its variance. Reference Vartanov, Shestovska and Hamby30 The remaining study did not mention length of hospitalization. Reference Ogawa, Wright and Luk29 Additionally, only two studies reported the use of systemic antibiotics during hospitalization, Reference Ganetsky, Han and Hughes26,Reference Williams, Atienza and Franzen28 and two studies assessed event-free survival at one year. Reference Altemeier and Konrardy25,Reference Ganetsky, Han and Hughes26 One study reported allergic reactions to vancomycin, Reference Reitmeyer, Rana and Awad27 and one study mentioned that patients with prior allergic reactions were excluded. Reference Ganetsky, Han and Hughes26

Quality assessment scores

In terms of quality assessment scores, one study was classified as good quality, Reference Reitmeyer, Rana and Awad27 while three studies were rated as fair quality, Reference Altemeier and Konrardy25,Reference Ganetsky, Han and Hughes26,Reference Williams, Atienza and Franzen28 all of which were published in full text. By contrast, the two studies published only as abstracts were deemed poor quality according to the Downs and Black quality assessment tool (see Supplementary Table 2). Reference Ogawa, Wright and Luk29,Reference Vartanov, Shestovska and Hamby30

In-depth assessment of publication bias

The potential for publication bias was assessed using three methods. The funnel plot exhibited significant asymmetry, with a noticeable concentration of studies reporting protective effect sizes and a lack of smaller studies with opposing or null results. This pattern suggests the potential presence of publication bias, indicating that studies with less favorable outcomes may be underrepresented in the literature. Egger’s test confirmed this asymmetry (P = .001). Furthermore, RoBMA, a robust Bayesian model-averaged meta-regression analysis, found weak evidence of heterogeneity among the studies (BF = .68); and a strong suggestion of publication bias (BF = 97.70). We also employed RoBMA to simultaneously account for effect size, heterogeneity, and publication bias to estimate the overall effect of oral vancomycin prophylaxis. The RoBMA model found that the association between oral vancomycin prophylaxis and the incidence of CDI was statistically nonsignificant, with an OR of .88 (95% CrI: .32 – 1.16), therefore confirming the strong presence of publication bias, see Figure 4. A RoBMA sensitivity analysis including only the four studies published in full text yielded similar results (heterogeneity BF = .77 and publication bias BF = 12.25), see Figure 5.

Figure 4. Forest plot of RoBMA-adjusted Clostridioides difficile infection risk in stem cell transplant patients: impact of oral Vancomycin primary prophylaxis.

Figure 5. Forest plot of RoBMA-adjusted Clostridioides difficile infection risk in stem cell transplant patients: impact of oral Vancomycin primary prophylaxis, full-text published studies only.

Discussion

This is one of the first meta-analyses addressing the use of oral vancomycin as primary prophylaxis specifically in the HSCT patient population. Oral vancomycin primary prophylaxis appeared to protect against the incidence of CDI. All secondary outcomes were no different after implementation of vancomycin prophylaxis (eg, vancomycin-resistant Enterococcus, GVHD). However, inherent characteristics of the included studies (eg, publication bias) prevented us from more strongly concluding that oral vancomycin should be used in this patient population.

We found that oral vancomycin primary prophylaxis is associated with preventing CDI in HSCT patients. While a meta-analysis of general inpatient populations found primary oral vancomycin prophylaxis ineffective, Reference Tariq, Laguio-Vila, Tahir, Orenstein, Pardi and Khanna31 two meta-analysis including immunocompromised transplant patients showed it to be beneficial. Reference Maraolo, Mazzitelli and Zappulo32,Reference Babar, El Kurdi and El Iskandarani33 The American College of Gastroenterology endorses oral vancomycin secondary prophylaxis, Reference Kelly, Fischer and Allegretti34 but the Infectious Disease Society of America’s latest guidelines do not address CDI prophylaxis. Reference Johnson, Lavergne and Skinner35 Furthermore, the European Society of Clinical Microbiology and Infectious Diseases do not recommend the routine use of oral vancomycin prophylaxis. Reference Van Prehn, Reigadas and Vogelzang36 Our meta-analysis uniquely examines the HSCT population without known history of prior CDI, providing new insights into the efficacy of oral vancomycin prophylaxis in this high-risk group.

Oral vancomycin as primary prophylaxis did not change the incidence of vancomycin-resistant Enterococcus or bloodstream infections in this population. It is a rational choice for CDI prophylaxis due to its strong efficacy against C. difficile, minimal long-term systemic adverse effects, and cost-effectiveness. Reference Garey37 However, it alters the gut microbiome, Reference Nazzal, Soiefer and Chang38 potentially increasing the risk of colonization by vancomycin-resistant Enterococcus and other multidrug-resistant organisms. While studies in this meta-analysis showed no impact on vancomycin-resistant Enterococcus positivity during transplant hospitalization, other studies also found no significant differences in infection rates with or without oral vancomycin secondary prophylaxis. Reference Tariq, Laguio-Vila, Tahir, Orenstein, Pardi and Khanna31Reference Babar, El Kurdi and El Iskandarani33 Consequently, the long-term effects of oral vancomycin on the colonization of vancomycin-resistant Enterococcus or other multidrug-resistant organisms remain uncertain.

Similarly, we found no significant differences in the length of hospitalization or the incidence of GVHD between HSCT patients who received primary prophylaxis and those who did not. Despite the established association between prolonged hospital stays with increased incidence of CDI, Reference Alonso, Treadway and Hanna4 the length of hospital stay remained consistent before and after the implementation of oral vancomycin prophylaxis. Although it has been hypothesized that CDI may trigger gastrointestinal GVHD, Reference Trifilio, Pi and Mehta39 the reduced incidence of CDI in the prophylaxis group did not translate into a measurable impact on GVHD rates. Notably, these secondary outcomes were not evaluated in previous studies with similar objectives.

Our analysis revealed a significant publication bias, prompting us to conduct a robust Bayesian model-averaged meta-analysis. While meta-analyses are valuable tools for integrating data and informing decision-making in evidence-based medicine, publication bias remains a major limitation, Reference Kicinski, Springate and Kontopantelis40 as it can lead to an overestimation of intervention effects. To address this issue, we employed a statistical method that tests and adjusts for effect size, heterogeneity, and publication bias. Reference Maier, Bartoš and Wagenmakers23 RoBMA is an innovative methodological approach that integrates these factors into an adjusted model, which is relatively new in this field. Although our unadjusted analysis indicated a significant association between oral vancomycin prophylaxis and reduced odds of CDI, the publication bias-adjusted model revealed a nonsignificant effect of primary prophylaxis. This underscores the urgent need for randomized controlled trials to provide more robust evidence regarding this association.

This systematic review has additional limitations that should be considered when interpreting the findings. First, all included studies were observational in nature, which may introduce biases, including confounding factors that could influence the estimated impact of oral vancomycin prophylaxis on the incidence of CDI. Additionally, variability in patient populations and diagnostic protocols for CDI across the studies may limit the generalizability of the results. The quality assessment of the included studies identified several methodological weaknesses. Furthermore, the limited number of studies and the small sample sizes within each study included in the meta-analysis may restrict statistical power and the ability to detect subtle differences in outcomes.

In conclusion, this systematic review and Bayesian meta-analysis indicate that there is weak evidence in favor of primary oral vancomycin prophylaxis in preventing CDI in patients undergoing HSCT, and the current data show no immediate indications of harm. Given the heightened vulnerability of this patient population to CDI and the potential complications that can arise, such as GVHD and non-relapse mortality, oral vancomycin prophylaxis emerges as a potential intervention that merits further investigation. Nonetheless, critical questions remain regarding its long-term safety, potential effects on antimicrobial resistance, influence on the gut microbiome, and its efficacy in patients with a history of CDI or colonization. Addressing these questions in future research will be essential to fully elucidate the benefits and risks of oral vancomycin prophylaxis in this high-risk population.

Supplementary material

The supplementary material for this article can be found at https://doi.org/10.1017/ash.2025.10179.

Financial support

None reported.

Competing interests

All authors report no conflicts of interest relevant to this article.

Authorship and manuscript preparation

Conceptualization, J.S. and E.V.; search strategy, E.W.; literature review, W.T. and E.V.; data analysis, E.V., methodological guidance, S.S.; writing—original draft, E.V. and E.M.; writing—reviewing and editing, J.S., A.R.M., G.R.N. M.S., A.B., and A.R.

We would like to express our gratitude to Evans Whitaker, librarian at the Stanford Lane Medical Library, for his invaluable assistance in defining our search strategy. We also extend our appreciation to Sa Shen from the Quantitative Studies Unit for her expert guidance on the statistical methods employed in this study.

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Figure 0

Figure 1. Literature search for studies published up to March 21, 2025, that evaluated the impact of oral Vancomycin prophylaxis for Clostridioides difficile infection in stem cell transplant patients.

Figure 1

Table 1. Summary of study characteristics

Figure 2

Figure 2. Forest plot of unadjusted Clostridioides difficile infection risk in stem cell transplant patients: impact of oral Vancomycin primary prophylaxis.

Figure 3

Figure 3. Forest plot of unadjusted Clostridioides difficile infection risk in stem cell transplant patients: impact of oral Vancomycin primary prophylaxis, full-text published studies only.

Figure 4

Figure 4. Forest plot of RoBMA-adjusted Clostridioides difficile infection risk in stem cell transplant patients: impact of oral Vancomycin primary prophylaxis.

Figure 5

Figure 5. Forest plot of RoBMA-adjusted Clostridioides difficile infection risk in stem cell transplant patients: impact of oral Vancomycin primary prophylaxis, full-text published studies only.

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