Adverse events (AEs). Measurement time: up to 30 days after the last dose of treatment received and up to a maximum of 24 months - Occurrence of any AE in the subject (yes/no). - Description of the AE (Name of the adverse event). - Duration of the AE (Difference in dates between the start and end of the event) - Intensity of the AE (Mild, Moderate, Severe, Life-threatening or disabling AE, Fatal AE) - Severity of the AE (Serious, Not serious) - Attitude towards the study treatment (no change in dose, temporary or permanent interruption of the study treatment) - Outcome of the AE (recovered/resolved, improving/in resolution, persistent/unresolved, with sequelae requiring treatment) -Causality (1.Definite, 2.Very Probable, 3.Probable, 4.Possible, 5.Not related, 6.Unknown) -Antibodies against the monoclonal antibody Anti-PD1 2C12 (yes/no). Measurement time: prior to the start of treatment and every six weeks while the treatment is maintained. Pharmacokinetic parameters (values ​​estimated using the Monolix system, SAEM algorithm combined with Monte Carlo code with a sparse data design in blocks of 3, with 4 repetitions per block where each patient will have 4 extractions). Measurement time: baseline (first hour before infusion), end of infusion (at 60 minutes), after infusion at 6 hours, 24 hours, 48 ​​hours, 168 hours (one week), 336 hours (two weeks), 504 hours (three weeks, coincides with the baseline sample of the next cycle): - Area under the curve (AUC) - Maximum concentration (Cmax) - Time to maximum concentration (Tmax) - Minimum concentration - Elimination half-life (t1/2) - Plasma clearance (CL) - Volume of distribution (Vd) Overall Survival (OS) (Time from the date of patient inclusion in the study until death, regardless of cause, or until the date of last news). Measurement time: 24 months. Progression-free survival (PFS) (Time from patient inclusion date to the date considered disease progression or death from any cause). Measurement time: 24 months.