Immune checkpoint inhibitors linked to increased major cardiac events in the real world | Đa khoa

Treatment with immune checkpoint inhibitors (ICIs) in real-world settings is associated with a higher incidence of adverse cardiovascular events than traditionally reported in clinical trials, a retrospective cohort study has shown. Patients at risk include those with a history of cardiovascular disease (CVD), especially a history of heart failure (HF) or valvular heart disease (VHD).

“In rare cases, ICIs cause immune-mediated myocarditis. However, the true incidence of other major adverse cardiovascular events [MACEs; ie, acute coronary syndrome (ACS), HF, stroke, and transient ischaemic attack (TIA)] after ICI treatment remains unknown, because late-occurring side effects are rarely reported in prospective clinical trials … and current literature on cardiovascular toxicity of ICIs consists mainly of case series,” wrote the researchers. [J Clin Oncol 2022:doi:10.1200/JCO.21.01808]

To identify the incidence and risk factors of MACEs in ICI-treated patients, 672 cancer patients treated with ICIs (full ICI cohort; mean age, 64.8 years; male, 64.7 percent; history of CVD, 20.5 percent) were included in the study.

During a median follow-up of 13 months, MACEs occurred in 10.3 percent of ICI-treated cancer patients, with a median time to event of 5 months and a high total mortality rate of 54.9 percent, but a low cardiovascular death rate of 1.9 percent.

“A history of HF or VHD increased the vulnerability of ICI-treated patients to MACE,” highlighted the researchers. History of HF was associated with a twofold higher risk of MACEs (HR, 2.27; 95 percent CI, 1.03–5.04; p=0.043), while history of VHD was associated with a threefold higher risk of MACEs (HR, 3.01; 95 percent CI, 1.05–8.66; p=0.041), according to multivariable analysis.

In secondary outcome analysis, smoking history (HR, 5.18; 95 percent CI, 1.09–24.70; p=0.039) and previous treatment with VEGF inhibitors (HR, 3.74; 95 percent CI, 1.29–10.88; p=0.016) were independently associated with ACS. Furthermore, history of HF and VHD were both associated with a threefold higher risk of HF (history of HF: HR, 3.42; 95 percent CI, 1.48–7.92; p=0.004) (history of VHD: HR, 3.76; 95 percent CI, 1.26–11.22; p=0.017).

After adjusting for age (± 5 years), sex, and history of CVD, the incidence of MACEs in the ICI cohort (n=421; mean age, 65.4 years; male, 70.8 percent; history of CVD, 22.8 percent) was compared with the incidence in two matched cohorts, including cancer patients without exposure to ICIs (positive controls; n=396) and individuals without a history of cancer (negative controls; n=399).

“In patients treated with ICIs, incidence rates of MACEs were significantly [higher than] both control groups,” reported the researchers.

Results of the study showed a significantly lower risk of MACEs in the non-ICI group (HR, 0.61; 95 percent CI, 0.38–0.99; p=0.047) and in individuals without a history of cancer (HR, 0.24; 95 percent CI, 0.15–0.037; p<0.001). “This suggests a potential harmful effect of ICI treatment besides the underlying risk profile,” the researchers noted. “A modest, although statistically nonsignificant overweight of HF events [was] likely responsible for these findings.”

“Our data highlight the clinical relevance of cardiovascular work-up in patients with cancer before exposure to ICI treatment, particularly in those with pre-existing CVD,” recommended the researchers. “A routine thorough cardiovascular history, electrocardiography, and echocardiography might identify patients who need regular cardiovascular follow-up during and after ICI treatment.”