4.0 Article

Ri sk factors and prognostic significance of infection of totally implantable vascular access port in solid tumor patients: A prospective cohort study

Journal

INFECTIOUS DISEASES NOW
Volume 53, Issue 8, Pages -

Publisher

ELSEVIER FRANCE-EDITIONS SCIENTIFIQUES MEDICALES ELSEVIER
DOI: 10.1016/j.idnow.2023.104766

Keywords

Infection; Mortality; Risk factors; Solid tumor; Totally Implantable Vascular Access Port

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This study aimed to investigate the risk factors for TIVAP-related infection (TIVAP-RI) and its impact on patient prognosis in adult patients with solid tumors. The results showed that TIVAP insertion was associated with a low infection rate and did not affect one-year mortality. Additionally, young age, impaired health status, TIVAP insertion within one month of initiating chemotherapy, and TIVAP insertion in an irradiated area were identified as newly reported preventable risk factors for TIVAP-RI.
Objectives: Totally implantable venous access ports (TIVAP) are devices mainly used to deliver antineoplastic chemotherapies, of which the insertion may be complicated by TIVAP-related infection (TIVAPRI). This study aims to provide data on the risk factors for TIVAP-RI and its influence on patient prognosis. Patients and methods: Prospective observational study including adult patients with solid tumors, in whom a TIVAP was inserted to deliver antineoplastic chemotherapy between January 2018 and October 2019. Factors associated with TIVAP-RI and one-year mortality were determined using multiple logistic regressions. Results: More than a thousand (1014) patients were included, among whom 48 (4.7%) presented with TIVAP-RI. Gram-positive cocci and Gram-negative bacilli represented 51% and 41% of the pathogens isolated, respectively. Young age (odds ratio [OR] 0.67; 95% Confidence Interval [0.53-0.83] per 10-year increase), WHO performance status > 1 (OR 3.24 [1.52-7.79]), chemotherapy administration in the month before TIVAP placement (OR 2.26 [1.17-4.26]), and radiation therapy of the homolateral chest wall (OR 3.28 [1.51-6.67]) were independently associated with TIVAP-RI occurrence. During the year following TIVAP insertion, 287 (28%) patients died. TIVAP-RI was not associated with one-year mortality (OR 1.56 [0.75-3.19]). Conclusion: TIVAP insertion in adult patients with solid tumors is associated with a low infection rate, which did not influence one-year mortality. In addition to young age and impaired health status, TIVAP insertion in the month following initiation of the antineoplastic chemotherapy and TIVAP insertion in an irradiated area are two newly reported preventable TIVAP-RI risk factors.

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