633. Eravacycline Use in Immunocompromised Patients: Multicenter Evaluation of Clinical and Safety Endpoints

BACKGROUND: Infections caused by multidrug-resistant (MDR) bacteria are an increasingly common public health threat associated with worse outcomes in immunocompromised patients. Eravacycline (ERV) has potent in-vitro activity against MDR Gram-negative and Gram-positive bacteria and has demonstrated...

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Autores principales: Kunz Coyne, Ashlan J, Allosaimy, Sara, Molina, Kyle C, Kang-Birken, Lena, Lagnf, Abdalhamid M, Claeys, Kimberly C, Veve, Michael, King, Madeline, Pullinger, Benjamin, Bouchard, Jeannette, Gore, Tristan, Rojas, Leonar, Tart, Serina, Hobbs, Athena L V, Perkins, Nicholas, Biagi, Mark, Pierce, Michael, Cosimi, Reese, Jones, Bruce M, Truong, James, Andrade, Justin, Huang, Glen, Lucas, Kristen, Morrisette, Taylor, Holger, Dana, Rebold, Nicholas S, Ghali, Amer El, Davis, Susan L, Rybak, Michael J
Formato: Online Artículo Texto
Lenguaje:English
Publicado: Oxford University Press 2022
Materias:
Abstracts
Acceso en línea:https://www.ncbi.nlm.nih.gov/pmc/articles/PMC9752349/
http://dx.doi.org/10.1093/ofid/ofac492.685
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author Kunz Coyne, Ashlan J
Allosaimy, Sara
Molina, Kyle C
Kang-Birken, Lena
Lagnf, Abdalhamid M
Claeys, Kimberly C
Veve, Michael
King, Madeline
Pullinger, Benjamin
Bouchard, Jeannette
Gore, Tristan
Rojas, Leonar
Tart, Serina
Hobbs, Athena L V
Perkins, Nicholas
Biagi, Mark
Pierce, Michael
Cosimi, Reese
Jones, Bruce M
Truong, James
Andrade, Justin
Huang, Glen
Lucas, Kristen
Morrisette, Taylor
Holger, Dana
Rebold, Nicholas S
Ghali, Amer El
Ghali, Amer El
Davis, Susan L
Rybak, Michael J
author_facet Kunz Coyne, Ashlan J
Allosaimy, Sara
Molina, Kyle C
Kang-Birken, Lena
Lagnf, Abdalhamid M
Claeys, Kimberly C
Veve, Michael
King, Madeline
Pullinger, Benjamin
Bouchard, Jeannette
Gore, Tristan
Rojas, Leonar
Tart, Serina
Hobbs, Athena L V
Perkins, Nicholas
Biagi, Mark
Pierce, Michael
Cosimi, Reese
Jones, Bruce M
Truong, James
Andrade, Justin
Huang, Glen
Lucas, Kristen
Morrisette, Taylor
Holger, Dana
Rebold, Nicholas S
Ghali, Amer El
Ghali, Amer El
Davis, Susan L
Rybak, Michael J
author_sort Kunz Coyne, Ashlan J
collection PubMed
description BACKGROUND: Infections caused by multidrug-resistant (MDR) bacteria are an increasingly common public health threat associated with worse outcomes in immunocompromised patients. Eravacycline (ERV) has potent in-vitro activity against MDR Gram-negative and Gram-positive bacteria and has demonstrated non-inferiority to meropenem in the phase III IGNITE4 trial; however, the trial excluded immunocompromised patients. We aimed to evaluate clinical and safety endpoints of immunocompromised patients receiving ERV as definitive therapy. METHODS: Multicenter, retrospective, observational study conducted from October 2018 to April 2022. Adult hospitalized immunocompromised patients treated with ERV for ≥72 hours were included. Immunocompromised patients were defined as having any of the following: chemo or radiation therapy < 30 days of hospital admission, HIV/AIDS with CD4 < 200, chronic steroids ( >40 mg prednisone or equivalent. The primary outcome was 30-day survival. Secondary outcomes were lack of 30-day infection recurrence and drug-related safety events. RESULTS: Overall, 75 immunocompromised patients treated with ERV were included from 17 United States medical centers. Median (IQR) age was 62 (53-70) and 61.6% were male. Hospital length of stay was 28 (13-42) days and 67% were admitted to the intensive care unit. SOFA and APACHE II scores were 3.5 (1-7) and 16 (11-20), respectively. Common infection sources were intra-abdominal (26%) and lower respiratory tract (18%); 24% were bacteremic. Most patients had cultured Enterobacterales (58.7%) and Enterococci (37%) spp. infections. Of those, 21.3% were CRE and 19% were VRE. Infectious diseases consult was obtained in 91.8% of cases. Time elapsed from index culture collection to ERV initiation was 4 (2-8) days and duration of ERV therapy was 7 (4-12) days. In total, 81.3% of immunocompromised patients achieved 30-day survival and 90.7% did not have 30-day infection recurrence. Probable drug-related adverse events occurred in 5.3% of patients (GI 4%, rash 1%). CONCLUSION: A majority of immunocompromised patients receiving ERV as definitive therapy achieved 30-day survival and did not experience infection recurrence. ERV use in immunocompromised subpopulations will benefit from studies tailored to their specific characteristics. DISCLOSURES: Kimberly C. Claeys, PharmD, BioFire Diagnostics: Honoraria Bruce M. Jones, Pharm.D., FIDSA, BCPS, AbbVie: Advisor/Consultant|AbbVie: Honoraria|La Jolla: Honoraria|Melinta: Advisor/Consultant|Paratek: Honoraria|Regeneron: Honoraria.
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spelling pubmed-97523492022-12-16 633. Eravacycline Use in Immunocompromised Patients: Multicenter Evaluation of Clinical and Safety Endpoints Kunz Coyne, Ashlan J Allosaimy, Sara Molina, Kyle C Kang-Birken, Lena Lagnf, Abdalhamid M Claeys, Kimberly C Veve, Michael King, Madeline Pullinger, Benjamin Bouchard, Jeannette Gore, Tristan Rojas, Leonar Tart, Serina Hobbs, Athena L V Perkins, Nicholas Biagi, Mark Pierce, Michael Cosimi, Reese Jones, Bruce M Truong, James Andrade, Justin Huang, Glen Lucas, Kristen Morrisette, Taylor Holger, Dana Rebold, Nicholas S Ghali, Amer El Ghali, Amer El Davis, Susan L Rybak, Michael J Open Forum Infect Dis Abstracts BACKGROUND: Infections caused by multidrug-resistant (MDR) bacteria are an increasingly common public health threat associated with worse outcomes in immunocompromised patients. Eravacycline (ERV) has potent in-vitro activity against MDR Gram-negative and Gram-positive bacteria and has demonstrated non-inferiority to meropenem in the phase III IGNITE4 trial; however, the trial excluded immunocompromised patients. We aimed to evaluate clinical and safety endpoints of immunocompromised patients receiving ERV as definitive therapy. METHODS: Multicenter, retrospective, observational study conducted from October 2018 to April 2022. Adult hospitalized immunocompromised patients treated with ERV for ≥72 hours were included. Immunocompromised patients were defined as having any of the following: chemo or radiation therapy < 30 days of hospital admission, HIV/AIDS with CD4 < 200, chronic steroids ( >40 mg prednisone or equivalent. The primary outcome was 30-day survival. Secondary outcomes were lack of 30-day infection recurrence and drug-related safety events. RESULTS: Overall, 75 immunocompromised patients treated with ERV were included from 17 United States medical centers. Median (IQR) age was 62 (53-70) and 61.6% were male. Hospital length of stay was 28 (13-42) days and 67% were admitted to the intensive care unit. SOFA and APACHE II scores were 3.5 (1-7) and 16 (11-20), respectively. Common infection sources were intra-abdominal (26%) and lower respiratory tract (18%); 24% were bacteremic. Most patients had cultured Enterobacterales (58.7%) and Enterococci (37%) spp. infections. Of those, 21.3% were CRE and 19% were VRE. Infectious diseases consult was obtained in 91.8% of cases. Time elapsed from index culture collection to ERV initiation was 4 (2-8) days and duration of ERV therapy was 7 (4-12) days. In total, 81.3% of immunocompromised patients achieved 30-day survival and 90.7% did not have 30-day infection recurrence. Probable drug-related adverse events occurred in 5.3% of patients (GI 4%, rash 1%). CONCLUSION: A majority of immunocompromised patients receiving ERV as definitive therapy achieved 30-day survival and did not experience infection recurrence. ERV use in immunocompromised subpopulations will benefit from studies tailored to their specific characteristics. DISCLOSURES: Kimberly C. Claeys, PharmD, BioFire Diagnostics: Honoraria Bruce M. Jones, Pharm.D., FIDSA, BCPS, AbbVie: Advisor/Consultant|AbbVie: Honoraria|La Jolla: Honoraria|Melinta: Advisor/Consultant|Paratek: Honoraria|Regeneron: Honoraria. Oxford University Press 2022-12-15 /pmc/articles/PMC9752349/ http://dx.doi.org/10.1093/ofid/ofac492.685 Text en © The Author(s) 2022. Published by Oxford University Press on behalf of Infectious Diseases Society of America. https://creativecommons.org/licenses/by/4.0/This is an Open Access article distributed under the terms of the Creative Commons Attribution License (https://creativecommons.org/licenses/by/4.0/), which permits unrestricted reuse, distribution, and reproduction in any medium, provided the original work is properly cited.
spellingShingle Abstracts
Kunz Coyne, Ashlan J
Allosaimy, Sara
Molina, Kyle C
Kang-Birken, Lena
Lagnf, Abdalhamid M
Claeys, Kimberly C
Veve, Michael
King, Madeline
Pullinger, Benjamin
Bouchard, Jeannette
Gore, Tristan
Rojas, Leonar
Tart, Serina
Hobbs, Athena L V
Perkins, Nicholas
Biagi, Mark
Pierce, Michael
Cosimi, Reese
Jones, Bruce M
Truong, James
Andrade, Justin
Huang, Glen
Lucas, Kristen
Morrisette, Taylor
Holger, Dana
Rebold, Nicholas S
Ghali, Amer El
Ghali, Amer El
Davis, Susan L
Rybak, Michael J
633. Eravacycline Use in Immunocompromised Patients: Multicenter Evaluation of Clinical and Safety Endpoints
title 633. Eravacycline Use in Immunocompromised Patients: Multicenter Evaluation of Clinical and Safety Endpoints
title_full 633. Eravacycline Use in Immunocompromised Patients: Multicenter Evaluation of Clinical and Safety Endpoints
title_fullStr 633. Eravacycline Use in Immunocompromised Patients: Multicenter Evaluation of Clinical and Safety Endpoints
title_full_unstemmed 633. Eravacycline Use in Immunocompromised Patients: Multicenter Evaluation of Clinical and Safety Endpoints
title_short 633. Eravacycline Use in Immunocompromised Patients: Multicenter Evaluation of Clinical and Safety Endpoints
title_sort 633. eravacycline use in immunocompromised patients: multicenter evaluation of clinical and safety endpoints
topic Abstracts
url https://www.ncbi.nlm.nih.gov/pmc/articles/PMC9752349/
http://dx.doi.org/10.1093/ofid/ofac492.685
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