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. 2024 Oct;154(4):1022-1032.
doi: 10.1016/j.jaci.2024.06.019. Epub 2024 Jul 9.

Nonsense CD247 mutations show dominant-negative features in T-cell receptor expression and function

Alejandro C Briones  1 Rebeca F Megino  1 Ana V Marin  1 Daniel Chacón-Arguedas  1 Elena García-Martinez  2 Héctor Balastegui-Martín  2 Hugh T Reyburn  3 Sarah E Henrickson  4 Carmen Rodríguez-Sainz  2 Elena Seoane-Reula  5 Paloma Sanchez-Mateos  2 Paula P Cardenas  1 Jose R Regueiro  6
Affiliations
Free article

Nonsense CD247 mutations show dominant-negative features in T-cell receptor expression and function

Alejandro C Briones et al. J Allergy Clin Immunol. 2024 Oct.
Free article

Abstract

Background: The invariant TCR ζ/CD247 homodimer is crucial for TCR/CD3 expression and signaling through its 3 immunoreceptor tyrosine-based activation motifs (ITAMs). Homozygous null mutations in CD247 lead to immunodeficiency, while carriers exhibit 50% reduced surface CD3. It is unclear whether carriers of other CD247 variants show dominant-negative effects.

Objective: We sought to analyze and model the potential impact on T-cell receptor (TCR) expression and function of heterozygous nonsense CD247 mutations found in patients with signs of immunodeficiency or autoimmunity.

Methods: Jurkat T cells, either wild-type (WT) or CRISPR/Cas9-edited CD247-deficient (ZKO), were lentivirally transduced with WT CD247 or mutations ablating 1 (Q142X), 2 (Q101X), or 3 (Q70X) ITAMs.

Results: Three patients from unrelated families were studied. Two heterozygous nonsense CD247 mutations were identified (p.Y152X and p.Q101X), which affected ITAM-3 and ITAM-2 and ITAM-3, respectively. Both mutations were associated with low surface CD3 expression and normal intracellular CD247 levels using a transmembrane-specific antibody, but very low intracellular CD247 levels using an ITAM-3-specific one, suggesting the presence of truncated variants in T cells. Transduction of the mutations lacking 1, 2, or 3 ITAMs into ZKO cells could not restore normal surface CD3 expression (only 60%, 22%, and 10%, respectively), whereas in WT cells, normal surface CD3 expression was reduced (to 39%, 19%, and 9% of normal levels), and both effects were dependent on ITAM number. All 6 transfectants showed reduced CD69 induction (25% to 50%), indicating that they were unable to signal downstream properly, neither isolated nor associated with WT CD247.

Conclusions: Our results suggest that CD247 variants lacking ITAMs due to nonsense, but not null, mutations are defective for normal TCR assembly and exert a dominant-negative effect on TCR expression and signaling in vitro. This, in turn, may correlate with clinical features in vivo.

Keywords: CD247; CD3ζ; ITAM; TCR; TCR ζ; autoimmunity; immunodeficiency.

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Conflict of interest statement

Disclosure statement This work was supported by grants from the Ministerio de Economía y Competitividad (MINECO PID2021-125501OB-I00 and RTI2018-095673-B-I00) and Asociación Española Contra el Cáncer (AECC PROYE20084REGU). A.C.B. was supported by Complutense University scholarship (CT27/16 and CT31/21). R.F.M. and D.C.A. were supported by the Spanish Ministry of Science, Innovation and Universities (FPU19/03136 and PRE2019-088150). P.P.C. was supported by Juan de la Cierva-Incorporación fellowship (IJCI-2014-19262). Disclosure of potential conflict of interest: The authors declare that they have no conflicts of interest.

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