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PLCG2-associated immune dysregulation (PLAID) comprises broad and distinct clinical presentations related to functional classes of genetic variants. | LitMetric

AI Article Synopsis

  • - The study investigates pathogenic variants of the PLCG2 gene, which are linked to two forms of immune dysregulation, PLAID and APLAID, and aims to functionally classify these variants to understand their effects better.
  • - Researchers collected clinical data and performed experiments on PLCG2 variants to assess their impact on B-cell activation and associated immune responses, finding that three-fourths of the variants altered B-cell function.
  • - The findings reveal a new class of PLCG2 mutations leading to immune deficiencies and suggest a distinct phenotypic cluster linked to various immune issues, particularly emphasizing the role of heterozygous variants in this dysregulation.

Article Abstract

Background: Pathogenic variants of phospholipase C gamma 2 (PLCG2) cause 2 related forms of autosomal-dominant immune dysregulation (ID), PLCγ2-associated antibody deficiency and immune dysregulation (PLAID) and autoinflammatory PLAID (APLAID). Since describing these conditions, many PLCG2 variants of uncertain significance have been identified by clinical sequencing of patients with diverse features of ID.

Objective: We sought to functionally classify PLCG2 variants and explore known and novel genotype-function-phenotype relationships.

Methods: Clinical data from patients with PLCG2 variants were obtained via standardized questionnaire. PLCG2 variants were generated by mutagenesis of enhanced green fluorescent protein (EGFP)-PLCG2 plasmid, which was overexpressed in Plcg2-deficient DT-40 B cells. B-cell receptor-induced calcium flux and extracellular signal-regulated kinase phosphorylation were assayed by flow cytometry. In some cases, stimulation-induced calcium flux was also measured in primary patient cells.

Results: Three-fourths of PLCG2 variants produced functional alteration of B-cell activation, in vitro. Thirteen variants led to gain of function (GOF); however, most functional variants defined a new class of PLCG2 mutation, monoallelic loss of function (LOF). Susceptibility to infection and autoinflammation were common with both GOF and LOF variants, whereas a new phenotypic cluster consisting of humoral immune deficiency, autoinflammation, susceptibility to herpesvirus infection, and natural killer cell dysfunction was observed in association with multiple heterozygous LOF variants detected in both familial and sporadic cases. In some cases, PLCG2 variants produced greater effects in natural killer cells than in B cells.

Conclusions: This work expands the genotypic and phenotypic associations with functional variation in PLCG2, including a novel form of ID in carriers of heterozygous loss of PLCG2 function. It also demonstrates the need for more diverse assays for assessing the impact of PLCG2 variants on human disease.

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Source
http://www.ncbi.nlm.nih.gov/pmc/articles/PMC11337301PMC
http://dx.doi.org/10.1016/j.jaci.2023.08.036DOI Listing

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