What question did this study set out to answer?

To determine the frequency and impact of bacteremia related to peripheral intravenous catheters (PIV) in hospitalized patients.

January 14, 2026Open Access

P-1032. Vein Attempts & IV League Hazards: Rethinking Peripheral IV and Bacteremia Risk

Key Points

To determine the frequency and impact of bacteremia related to peripheral intravenous catheters (PIV) in hospitalized patients.
Retrospective analysis of blood cultures positive for bacteria obtained at a teaching hospital.
Frequency of PIV starts and associated complications was tracked using hospital census data and safety reporting systems.
Infectious diseases providers reviewed cases of Staphylococcus aureus bacteremia to identify sources.
7477 PIV starts resulted in 28 bacteremias, equating to a rate of 3.7 bacteremias per 1,000 PIV starts.
21% of PIV-related bacteremia cases were caused by MRSA, contributing to hospital-onset infections.
PIV-related bacteremia was associated with a mean of 17.2 extra hospital days and 21.3 additional days of antibiotic therapy.

Abstract

Abstract Background Peripheral intravenous catheters (PIV) are the most common invasive devices in hospitalized patients, yet data pertaining to serious complications from PIV are scarce. After noticing an apparent uptick in such complications, we sought to determine the frequency and impact of PIV-related bacteremia from 01/01/2023 to 04/15/2025 at a 528-bed teaching hospital in upstate New York.Table 1Characteristics of Peripheral Intravenous Catheter Associated Bacteremia (n = 28)Table 2Barriers to Best Practices for Insertion and Maintenance of Peripheral Intravenous Catheters Methods All blood cultures positive /= 48 hrs. post admission were obtained via laboratory information system query. Number of PIV starts was obtained from census data. All patients with Staphlococcus aureus bacteremia (SaB) are routinely seen by infectious diseases providers who identify the source of all bacteremia. During mandatory reporting of hospital onset methicillin resistant SaB, the source of the bacteremia is also routinely identified. PIV-related adverse events were obtained from a virtual private network service (Safe Connect® McAfee) used to report serious safety-related issues, and via notifications from staff. Records of patients with proven PIV-driven bacteremia were retrospectively reviewed. Results 7477 PIV starts led to 28 bacteremias for a rate of 3.7 bacteremias/1,000 starts. 1534 positive blood cultures from 1017 unique patients were obtained. 2.8% (28/1017) of all hospital onset (HO) bacteremia had PIV as a definite source. Five species accounted for all PIV-driven bacteremia (PIV-B), 71% (n=20) were SaB (Table 1). 21% (6/28) of PIV-B were caused by MRSA. 25 HO-MRSA occurred. 24% 6/25 of HO MRSA had PIV as the source of the bacteremia. PIV-B was associated with the excess costs seen in Table 1, including a mean of 17.2 extra days of stay and 21.3 extra antibiotic days of therapy. PIV-B was also associated with endocarditis and central nervous system involvement. 21% of PIV-B were fatal. Conclusion The morbidity, mortality and avoidable costs associated with PIV-B are substantial. Our findings highlight the criticality of using well-known best practices for insertion and maintenance. Barriers to those practices appear in Table 2. Disclosures All Authors: No reported disclosures

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Cite This Study

Dahiya et al. (Thu,) studied this question.

synapsesocial.com/papers/6966f2e313bf7a6f02c002aa https://doi.org/https://doi.org/10.1093/ofid/ofaf695.1228

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