Cargando…
A multicenter characterization of hepatitis associated with immune checkpoint inhibitors
Immune checkpoint inhibitors (ICI) predispose patients to immune-related adverse events (irAEs). Although hepatitis is a potentially lethal toxicity, the timing and outcomes have not been well described. In this retrospective study, patients from six international institutions were included if they...
| Autores principales: | , , , , , , , , , , , , , , , , , , |
|---|---|
| Formato: | Online Artículo Texto |
| Lenguaje: | English |
| Publicado: |
Taylor & Francis
2021
|
| Materias: | |
| Acceso en línea: | https://www.ncbi.nlm.nih.gov/pmc/articles/PMC7889227/ https://www.ncbi.nlm.nih.gov/pubmed/33628621 http://dx.doi.org/10.1080/2162402X.2021.1875639 |
| _version_ | 1783652266594533376 |
|---|---|
| author | Patrinely, J. Randall McGuigan, Ben Chandra, Sunandana Fenton, Sarah E. Chowdhary, Akansha Kennedy, Lucy B. Mooradian, Meghan J. Palmeri, Marisa Portal, Daniella Horst, Sara N. Scoville, Elizabeth A. Long, Georgina V. Shi, Chanjuan Mehnert, Janice M. Sullivan, Ryan J. Salama, April K. Sosman, Jeffrey A. Menzies, Alexander M. Johnson, Douglas B. |
| author_facet | Patrinely, J. Randall McGuigan, Ben Chandra, Sunandana Fenton, Sarah E. Chowdhary, Akansha Kennedy, Lucy B. Mooradian, Meghan J. Palmeri, Marisa Portal, Daniella Horst, Sara N. Scoville, Elizabeth A. Long, Georgina V. Shi, Chanjuan Mehnert, Janice M. Sullivan, Ryan J. Salama, April K. Sosman, Jeffrey A. Menzies, Alexander M. Johnson, Douglas B. |
| author_sort | Patrinely, J. Randall |
| collection | PubMed |
| description | Immune checkpoint inhibitors (ICI) predispose patients to immune-related adverse events (irAEs). Although hepatitis is a potentially lethal toxicity, the timing and outcomes have not been well described. In this retrospective study, patients from six international institutions were included if they were treated with ICIs and developed immune-related hepatitis. Patient and tumor characteristics, and hepatitis management and outcomes were evaluated. Of the 164 patients included, most were male (53.7%) with a median age of 63.0 years. Most patients had melanoma (83.5%) and stage IV disease (86.0%). Median follow-up was 585 days; median OS and PFS were not reached. The initial grade of hepatitis was most often grade 2 (30.5%) or 3 (45.7%) with a median time to onset of 61 days. Patients were most commonly asymptomatic (46.2%), but flu-like symptoms, including fatigue/anorexia (17.1%), nausea/emesis (14.0%), abdominal/back pain (11.6%), and arthralgias/myalgias (8.5%) occurred. Most patients received glucocorticoids (92.1%); the median time to improvement by one grade was 13.0 days, and the median time to complete resolution was 52.0 days. Second-line immunosuppression was required in 37 patients (22.6%), and steroid-dose re-escalation in 45 patients (27.4%). Five patients (3%) died of ICI-hepatitis or complications of hepatitis treatment. Ninety-one patients (58.6%) did not resume ICI; of 66 patients (40 grade 1/2, 26 grade 3/4) that were rechallenged, only 25.8% (n = 17) had recurrence. In this multi-institutional cohort, immune-related hepatitis was associated with excellent outcomes but frequently required therapy discontinuation, high-dose steroids, and second-line immunosuppression. Rechallenge was associated with a modest rate of hepatitis recurrence. |
| format | Online Article Text |
| id | pubmed-7889227 |
| institution | National Center for Biotechnology Information |
| language | English |
| publishDate | 2021 |
| publisher | Taylor & Francis |
| record_format | MEDLINE/PubMed |
| spelling | pubmed-78892272021-02-23 A multicenter characterization of hepatitis associated with immune checkpoint inhibitors Patrinely, J. Randall McGuigan, Ben Chandra, Sunandana Fenton, Sarah E. Chowdhary, Akansha Kennedy, Lucy B. Mooradian, Meghan J. Palmeri, Marisa Portal, Daniella Horst, Sara N. Scoville, Elizabeth A. Long, Georgina V. Shi, Chanjuan Mehnert, Janice M. Sullivan, Ryan J. Salama, April K. Sosman, Jeffrey A. Menzies, Alexander M. Johnson, Douglas B. Oncoimmunology Original Research Immune checkpoint inhibitors (ICI) predispose patients to immune-related adverse events (irAEs). Although hepatitis is a potentially lethal toxicity, the timing and outcomes have not been well described. In this retrospective study, patients from six international institutions were included if they were treated with ICIs and developed immune-related hepatitis. Patient and tumor characteristics, and hepatitis management and outcomes were evaluated. Of the 164 patients included, most were male (53.7%) with a median age of 63.0 years. Most patients had melanoma (83.5%) and stage IV disease (86.0%). Median follow-up was 585 days; median OS and PFS were not reached. The initial grade of hepatitis was most often grade 2 (30.5%) or 3 (45.7%) with a median time to onset of 61 days. Patients were most commonly asymptomatic (46.2%), but flu-like symptoms, including fatigue/anorexia (17.1%), nausea/emesis (14.0%), abdominal/back pain (11.6%), and arthralgias/myalgias (8.5%) occurred. Most patients received glucocorticoids (92.1%); the median time to improvement by one grade was 13.0 days, and the median time to complete resolution was 52.0 days. Second-line immunosuppression was required in 37 patients (22.6%), and steroid-dose re-escalation in 45 patients (27.4%). Five patients (3%) died of ICI-hepatitis or complications of hepatitis treatment. Ninety-one patients (58.6%) did not resume ICI; of 66 patients (40 grade 1/2, 26 grade 3/4) that were rechallenged, only 25.8% (n = 17) had recurrence. In this multi-institutional cohort, immune-related hepatitis was associated with excellent outcomes but frequently required therapy discontinuation, high-dose steroids, and second-line immunosuppression. Rechallenge was associated with a modest rate of hepatitis recurrence. Taylor & Francis 2021-02-08 /pmc/articles/PMC7889227/ /pubmed/33628621 http://dx.doi.org/10.1080/2162402X.2021.1875639 Text en © 2021 The Author(s). Published with license by Taylor & Francis Group, LLC. https://creativecommons.org/licenses/by-nc/4.0/This is an Open Access article distributed under the terms of the Creative Commons Attribution-NonCommercial License (http://creativecommons.org/licenses/by-nc/4.0/ (https://creativecommons.org/licenses/by-nc/4.0/) ), which permits unrestricted non-commercial use, distribution, and reproduction in any medium, provided the original work is properly cited. |
| spellingShingle | Original Research Patrinely, J. Randall McGuigan, Ben Chandra, Sunandana Fenton, Sarah E. Chowdhary, Akansha Kennedy, Lucy B. Mooradian, Meghan J. Palmeri, Marisa Portal, Daniella Horst, Sara N. Scoville, Elizabeth A. Long, Georgina V. Shi, Chanjuan Mehnert, Janice M. Sullivan, Ryan J. Salama, April K. Sosman, Jeffrey A. Menzies, Alexander M. Johnson, Douglas B. A multicenter characterization of hepatitis associated with immune checkpoint inhibitors |
| title | A multicenter characterization of hepatitis associated with immune checkpoint inhibitors |
| title_full | A multicenter characterization of hepatitis associated with immune checkpoint inhibitors |
| title_fullStr | A multicenter characterization of hepatitis associated with immune checkpoint inhibitors |
| title_full_unstemmed | A multicenter characterization of hepatitis associated with immune checkpoint inhibitors |
| title_short | A multicenter characterization of hepatitis associated with immune checkpoint inhibitors |
| title_sort | multicenter characterization of hepatitis associated with immune checkpoint inhibitors |
| topic | Original Research |
| url | https://www.ncbi.nlm.nih.gov/pmc/articles/PMC7889227/ https://www.ncbi.nlm.nih.gov/pubmed/33628621 http://dx.doi.org/10.1080/2162402X.2021.1875639 |
| work_keys_str_mv | AT patrinelyjrandall amulticentercharacterizationofhepatitisassociatedwithimmunecheckpointinhibitors AT mcguiganben amulticentercharacterizationofhepatitisassociatedwithimmunecheckpointinhibitors AT chandrasunandana amulticentercharacterizationofhepatitisassociatedwithimmunecheckpointinhibitors AT fentonsarahe amulticentercharacterizationofhepatitisassociatedwithimmunecheckpointinhibitors AT chowdharyakansha amulticentercharacterizationofhepatitisassociatedwithimmunecheckpointinhibitors AT kennedylucyb amulticentercharacterizationofhepatitisassociatedwithimmunecheckpointinhibitors AT mooradianmeghanj amulticentercharacterizationofhepatitisassociatedwithimmunecheckpointinhibitors AT palmerimarisa amulticentercharacterizationofhepatitisassociatedwithimmunecheckpointinhibitors AT portaldaniella amulticentercharacterizationofhepatitisassociatedwithimmunecheckpointinhibitors AT horstsaran amulticentercharacterizationofhepatitisassociatedwithimmunecheckpointinhibitors AT scovilleelizabetha amulticentercharacterizationofhepatitisassociatedwithimmunecheckpointinhibitors AT longgeorginav amulticentercharacterizationofhepatitisassociatedwithimmunecheckpointinhibitors AT shichanjuan amulticentercharacterizationofhepatitisassociatedwithimmunecheckpointinhibitors AT mehnertjanicem amulticentercharacterizationofhepatitisassociatedwithimmunecheckpointinhibitors AT sullivanryanj amulticentercharacterizationofhepatitisassociatedwithimmunecheckpointinhibitors AT salamaaprilk amulticentercharacterizationofhepatitisassociatedwithimmunecheckpointinhibitors AT sosmanjeffreya amulticentercharacterizationofhepatitisassociatedwithimmunecheckpointinhibitors AT menziesalexanderm amulticentercharacterizationofhepatitisassociatedwithimmunecheckpointinhibitors AT johnsondouglasb amulticentercharacterizationofhepatitisassociatedwithimmunecheckpointinhibitors AT patrinelyjrandall multicentercharacterizationofhepatitisassociatedwithimmunecheckpointinhibitors AT mcguiganben multicentercharacterizationofhepatitisassociatedwithimmunecheckpointinhibitors AT chandrasunandana multicentercharacterizationofhepatitisassociatedwithimmunecheckpointinhibitors AT fentonsarahe multicentercharacterizationofhepatitisassociatedwithimmunecheckpointinhibitors AT chowdharyakansha multicentercharacterizationofhepatitisassociatedwithimmunecheckpointinhibitors AT kennedylucyb multicentercharacterizationofhepatitisassociatedwithimmunecheckpointinhibitors AT mooradianmeghanj multicentercharacterizationofhepatitisassociatedwithimmunecheckpointinhibitors AT palmerimarisa multicentercharacterizationofhepatitisassociatedwithimmunecheckpointinhibitors AT portaldaniella multicentercharacterizationofhepatitisassociatedwithimmunecheckpointinhibitors AT horstsaran multicentercharacterizationofhepatitisassociatedwithimmunecheckpointinhibitors AT scovilleelizabetha multicentercharacterizationofhepatitisassociatedwithimmunecheckpointinhibitors AT longgeorginav multicentercharacterizationofhepatitisassociatedwithimmunecheckpointinhibitors AT shichanjuan multicentercharacterizationofhepatitisassociatedwithimmunecheckpointinhibitors AT mehnertjanicem multicentercharacterizationofhepatitisassociatedwithimmunecheckpointinhibitors AT sullivanryanj multicentercharacterizationofhepatitisassociatedwithimmunecheckpointinhibitors AT salamaaprilk multicentercharacterizationofhepatitisassociatedwithimmunecheckpointinhibitors AT sosmanjeffreya multicentercharacterizationofhepatitisassociatedwithimmunecheckpointinhibitors AT menziesalexanderm multicentercharacterizationofhepatitisassociatedwithimmunecheckpointinhibitors AT johnsondouglasb multicentercharacterizationofhepatitisassociatedwithimmunecheckpointinhibitors |