Frontiers in Immunology (Sep 2018)

Increased Risk for Malignancies in 131 Affected CTLA4 Mutation Carriers

  • David Egg,
  • Charlotte Schwab,
  • Annemarie Gabrysch,
  • Peter D. Arkwright,
  • Edmund Cheesman,
  • Lisa Giulino-Roth,
  • Olaf Neth,
  • Scott Snapper,
  • Satoshi Okada,
  • Michel Moutschen,
  • Philippe Delvenne,
  • Ann-Christin Pecher,
  • Daniel Wolff,
  • Yae-Jean Kim,
  • Suranjith Seneviratne,
  • Kyoung-Mee Kim,
  • Ji-Man Kang,
  • Samar Ojaimi,
  • Catriona McLean,
  • Klaus Warnatz,
  • Maximilian Seidl,
  • Bodo Grimbacher

DOI
https://doi.org/10.3389/fimmu.2018.02012
Journal volume & issue
Vol. 9

Abstract

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Background: Cytotoxic T-lymphocyte-associated antigen 4 (CTLA-4) is a negative immune regulator on the surface of T cells. In humans, heterozygous germline mutations in CTLA4 can cause an immune dysregulation syndrome. The phenotype comprises a broad spectrum of autoinflammatory, autoimmune, and immunodeficient features. An increased frequency of malignancies in primary immunodeficiencies is known, but their incidence in CTLA-4 insufficiency is unknown.Methods: Clinical manifestations and details of the clinical history were assessed in a worldwide cohort of 184 CTLA4 mutation carriers. Whenever a malignancy was reported, a malignancy-specific questionnaire was filled.Results: Among the 184 CTLA4 mutation carriers, 131 were considered affected, indicating a penetrance of 71.2%. We documented 17 malignancies, which amounts to a cancer prevalence of 12.9% in affected CTLA4 mutation carriers. There were ten lymphomas, five gastric cancers, one multiple myeloma, and one metastatic melanoma. Seven lymphomas and three gastric cancers were EBV-associated.Conclusion: Our findings demonstrate an elevated cancer risk for patients with CTLA-4 insufficiency. As more than half of the cancers were EBV-associated, the failure to control oncogenic viruses seems to be part of the CTLA-4-insufficient phenotype. Hence, lymphoproliferation and EBV viral load in blood should be carefully monitored, especially when immunosuppressing affected CTLA4 mutation carriers.

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