Riesgo de las enfermedades tromboembólicas venosas de los fármacos oncológicos - page 17

Inmunoterapia

Anticuerpos anti-PD1-PD-L1, CTLA-4

Incidencia de ETV (no incremento de riesgo)

•

Ipilimumab (<1%)

•

Nivolumab

•

Pembrolizumab

Toxicidad cardiológica

No incremento de ETEA

Miocarditis

Evento adverso mediado inmunologicamente

Combinación 0,27% vs 0,06% en monoterapia

Johnson DB et al. N Engl J Med. 2016

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