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Immune-related Adverse Events from Immune Checkpoint Inhibitor Therapy

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43 Table 6. Renal Toxicities Nephritis and Renal Dysfunction — Diagnosis and Monitoring Clinical Presentation* and Diagnosis: Definite ICPi-RELATED nephritis/acute kidney injury (AKI): • Kidney biopsy-confirmed diagnosis compatible with ICPi-Nephritis/AKI, and after clinical review of risk factors. † Probable ICPi-RELATED nephritis/acute renal failure: BOTH of the following: • Sustained increase in serum creatinine ≥50% on at least two consecutive values or need for renal replacement therapy (RRT), after clinical review of risk factors. † • Absence of an alternative plausible etiolog y. AND at least one of the following: • Sterile pyuria (≥5 WBCs/hpf ) • Concomitant or recent extrarenal irAE-eosinophilia (≥500 cells per µL) Possible ICPi-RELATED Nephritis/Acute Renal Failure: BOTH of the following: • Increase in serum creatinine ≥50% • Need for RRT nephritis/AKI is not readily attributable to alternative causes * Adapted from Gupta, 2020. † Risk factors include prior or concomitant nephrotoxic agent(s) use, prior or concomitant extrarenal irAEs. Monitoring • Monitor patients for elevated serum creatinine prior to every dose. • Routine urinalysis is not necessary, other than to rule out urinary tract infections (UTIs), etc. • For any suspected immune-mediated adverse reactions, exclude other causes (see below). • For suspected renal irAE obtain urinalysis, consider referral to nephrolog y. • For patients receiving combination therapy with immune checkpoint inhibitors and other agents, assess the potential contribution of the non-iCPI treatment to the renal failure. • Assess for concomitant medications, prescribed and OTC, herbals, vitamins, nephrotoxic agents, or contrast media. • If no potential alternative cause of AKI identified, then one can assume it is ICPi related and should forego biopsy. • Swift treatment of autoimmune component is important.

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