A Unique Heterozygous CARD11 Mutation Combines Pathogenic Features of Both Gain- and Loss-of-Function Patients in a Four-Generation Family

Marylin Desjardins,Batsukh Dorjbal,Julie Niemela,Angela Wang,Swadhinya Arjunaraja,Janani Sundaresan,Jeffrey R Stinson,Pamela Angelus,Andrew L Snow,Mark Raffeld,Helen F Matthews,Bruce D Mazer,Helen C Su

doi:10.3389/fimmu.2018.02944

Abstract

CARD11 is a lymphocyte-specific scaffold molecule required for proper activation of B- and T-cells in response to antigen. Germline gain-of-function (GOF) mutations in the CARD11 gene cause a unique B cell lymphoproliferative disorder known as B cell Expansion with NF-κB and T cell Anergy (BENTA). In contrast, patients carrying loss-of-function (LOF), dominant negative (DN) CARD11 mutations present with severe atopic disease. Interestingly, both GOF and DN CARD11 variants cause primary immunodeficiency, with recurrent bacterial and viral infections, likely resulting from impaired adaptive immune responses. This report describes a unique four-generation family harboring a novel heterozygous germline indel mutation in CARD11 (c.701-713delinsT), leading to one altered amino acid and a deletion of 4 others (p.His234_Lys238delinsLeu). Strikingly, affected members exhibit both moderate B cell lymphocytosis and atopic dermatitis/allergies. Ectopic expression of this CARD11 variant stimulated constitutive NF-κB activity in T cell lines, similar to other BENTA patient mutations. However, unlike other GOF mutants, this variant significantly impeded the ability of wild-type CARD11 to induce NF-κB activation following antigen receptor ligation. Patient lymphocytes display marked intrinsic defects in B cell differentiation and reduced T cell responsiveness in vitro. Collectively, these data imply that a single heterozygous CARD11 mutation can convey both GOF and DN signaling effects, manifesting in a blended BENTA phenotype with atopic features. Our findings further emphasize the importance of balanced CARD11 signaling for normal immune responses.

Highlights

BENTA disease [B cell Expansion with nuclear factor kappa B (NF-κB) and T cell Anergy] is a rare immunodeficiency disorder that presents with splenomegaly and unusual peripheral blood lymphocytosis comprised of naïve and immature B cells [1, 2]
BENTA is caused by germline, heterozygous GOF mutations in CARD11, which encodes a large multi-domain scaffold molecule best known for connecting antigen receptor (AgR) ligation to NF-κB activation in B and T lymphocytes
Small reactive lymphocytes were present on the peripheral blood smear

Summary

Introduction

BENTA disease [B cell Expansion with nuclear factor kappa B (NF-κB) and T cell Anergy] is a rare immunodeficiency disorder that presents with splenomegaly and unusual peripheral blood lymphocytosis comprised of naïve and immature B cells [1, 2]. Similar to somatic GOF mutations typically found in the coiled-coil (CC) domain of CARD11 and associated with diffuse large B-cell lymphoma [3], BENTA CARD11 mutants spontaneously aggregate to form active signaling clusters with BCL-10 and MALT1 (CBM complex), resulting in constitutive NF-κB activation without requiring B or T cell receptor interaction [4]. Mildly anergic T cell responses may explain increased susceptibility to certain viral infections [e.g., molluscum contagiousum, EpsteinBarr virus (EBV)]. Together, these immune abnormalities increase patients’ susceptibility to viral and bacterial infections, including chronic EBV infection, and may to contribute to a higher potential risk of B-cell malignancy [9]

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Discussion

Conclusion