Publication | Closed Access
A Case of Fulminant Type 1 Diabetes Following Anti-PD1 Immunotherapy in a Genetically Susceptible Patient
40
Citations
14
References
2017
Year
Acute Type 1ImmunologyImmune RegulationPathologyImmunotherapyImmune DysregulationImmune CheckpointType 1Susceptible PatientCancer ResearchAutoimmune DiseaseAnti-pd1 ImmunotherapyFulminant Type 1AutoimmunityImmunologic DiseaseInborn Error Of ImmunityTumor MicroenvironmentDiabetesImmune Checkpoint InhibitorDiabetes MellitusMedicineImmunological Biomarkers
Programmed cell death-1 protein (PD-1) is an immune checkpoint that has gained popularity in the treatment of several advanced cancers. Inhibiting this checkpoint is known to enhance immune response, but is also known to diminish immune tolerance and to increase autoimmune toxicity. We discuss a case of rapid onset fulminant Type 1 diabetes induced by treatment with anti-programmed cell death-1 monoclonal antibody, nivolumab, in a patient with late-stage non-small-cell lung adenocarcinoma. The patient had no history of previous diabetes but did reveal a high-risk genotype for Type 1 diabetes development (DR3-DQ2; DR4-DQ8). This finding supports that acute Type 1 diabetes can be an important adverse effect of immunotherapies targeting T-cell activation regulation. Because of the severity of this adverse effect, physicians should be aware of it, and studies directed to the detection of new biomarkers for early risk stratification (e.g., HLA) should be sought.
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