Toxicity of immune checkpoint inhibitors and tyrosine kinase inhibitor combinations in solid tumours: a systematic review and meta-analysis

被引:4
作者
O'Reilly, David [1 ,2 ,3 ]
O'Leary, Caroline L. [1 ]
Reilly, Aislinn [1 ]
Teo, Min Yuen [4 ]
O'Kane, Grainne [5 ]
Hendriks, Lizza [6 ]
Bennett, Kathleen [7 ]
Naidoo, Jarushka [1 ,2 ,8 ]
机构
[1] Beaumont Hosp, Med Oncol, Dublin, Ireland
[2] RCSI Univ Med & Hlth Sci, Sch Hlth Sci, Dept Med, Dublin, Ireland
[3] Bon Secours Hosp, Med Oncol, Dublin, Ireland
[4] Mem Sloan Kettering Canc Ctr, Dept Med, New York, NY USA
[5] Trinity Coll Dublin, Trinity St Jamess Canc Inst, HOPE Directorate, Dublin, Ireland
[6] Maastricht Univ, Med Ctr, Dept Pulm Dis, GROW Sch Oncol & Dev Biol, Maastricht, Netherlands
[7] RCSI Univ Med & Hlth Sci, Data Sci Ctr, Sch Populat Hlth, Dublin, Ireland
[8] Johns Hopkins Univ, Thorac Oncol, Sidney Kimmel Comprehens Canc Ctr, Baltimore, MD USA
来源
FRONTIERS IN ONCOLOGY | 2024年 / 14卷
关键词
tyrosine kinase inhibitors; immunotherapy; toxicity; immune related adverse events; immune checkpoint blockade; LENVATINIB PLUS PEMBROLIZUMAB; LUNG-CANCER; ADVANCED NSCLC; ATEZOLIZUMAB; CHEMOTHERAPY; THERAPY; MODELS; TRIAL;
D O I
10.3389/fonc.2024.1380453
中图分类号
R73 [肿瘤学];
学科分类号
100214 ;
摘要
The combination of immune checkpoint inhibitors (ICIs) and tyrosine kinase inhibitors (TKIs) can be associated with significant toxicity. We performed a systematic review and meta-analysis of the toxicity of combination treatment of ICIs with TKIs (ICI + TKI) in clinical trials with solid organ malignancies. Our primary endpoint explored the incidence of grade 3 - 5 (G3-5) treatment-related toxicity and our secondary endpoints included the incidence of toxicity by treatment type, disease type and studies with run-in strategies. A total of 9750 abstracts were identified, of which 72 eligible studies were included. The most common disease types were non-small cell lung cancer (n=8, 11.1%), renal cell carcinoma (n=10, 13.8%) and hepatobiliary cancers (n=10, 13.8%). The overall incidence of G3-5 toxicity was 56% (95% CI = 50% - 61%). The most common TKIs combined with ICIs in this analysis were multi-targeted TKIs (n = 52, 72%), VEGF specific (n = 9, 12.5%), or oncogene-targeting TKIs (EGFR, ALK, BRAF, MEK) (n =11, 15.3%). Oncogene-targeted TKIs were associated a higher incidence of rashes and immune related adverse events (irAEs) and lower incidence of hypertension. In studies which used a TKI 'run-in' to mitigate toxicity, the pooled estimate of G3-5 toxicity was 71% (95% CI 57-81%). Almost half of studies (48%) omitted the incidence of G3-5 irAEs. Our work suggests that the majority of patients who receive ICI-TKI combinations will experience high grade toxicity (G3-G5) and that toxicity may be specific to TKI partner (Oncogene targeted TKIs: Rash, irAEs; VEGF/Multitargeted: Hypertension). These data did not suggest that a TKI 'run-in' was associated with a lower incidence of G3-5 toxicity. Reporting of irAEs was inconsistent supporting the need for harmonisation of adverse event reporting to include onset, duration and treatment. Systematic review registration: https://www.crd.york.ac.uk/prospero/, identifier CRD42022367416.
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页数:13
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