Case Report: Characterizing the Role of the STXBP2-R190C Monoallelic Mutation Found in a Patient With Hemophagocytic Syndrome and Langerhans Cell Histiocytosis

Viñas-Giménez, Laura; Rincón, Rafael Gómez-Ferrer; Colobran, Roger; Cruz, Xavier de la; Celis, Verónica; Dapena, José Luís; Alsina, Laia; Sayós, Joan; Martínez-Gallo, Mónica

doi:10.3389/fimmu.2021.723836

Cited by 4 publications

(1 citation statement)

References 12 publications

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“…Case reports of other STXBP2 monoallelic mutations have shown similar decreases in NK function and degranulation. A patient with an STXBP2 (c.568C > T, p.Arg190Cys) mutation developed sHLH in the setting of Langerhans cell histiocytosis; NK cell lysis was found to be decreased, improving with sHLH therapies and CD107a expression was significantly lower than controls [30]. A different study noted that patients with STXBP2 (c.194G > A, p.Arg65Gln) and STXBP2 (c.193C > T/p.Arg65Trp) monoallelic mutations again showed decreased degranulation and cytotoxic activity with interference in membrane fusion and SNARE-complex assembly [29].…”

Section: Css/hlh/mas Systemmentioning

confidence: 96%

A Rare STXBP2 Mutation in Severe COVID-19 and Secondary Cytokine Storm Syndrome

Reiff

Zhang

Smitherman

et al. 2022

Life

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Background: Primary (familial) hemophagocytic lymphohistiocytosis (pHLH) is a potentially lethal syndrome of infancy, caused by genetic defects in natural killer (NK) cell and CD8 T cell cytotoxicity, leading to hyperinflammation, elevated cytokine levels, and a disorganized immune response resulting in multi-organ system failure and frequently death. Secondary HLH (sHLH) can be triggered in the setting of malignances, diseases of chronic immune system activation, or by infectious etiologies. While pHLH is usually a result of homozygous gene mutations, monoallelic hypomorphic and dominant-negative mutations in pHLH genes have been implicated in sHLH. Coronavirus disease 2019 (COVID-19) has been an omnipresent viral infection since its arrival, and severe cases can present with cytokine storm and have clinical features and laboratory findings consistent with sHLH. Herein, we report an adolescent with severe COVID-19, decreased NK cell function, and features of sHLH. Her genetic evaluation identified a monoallelic missense mutation in the pHLH gene STXBP2, and NK cell assays of her blood showed decreased cytolysis and degranulation ex vivo. Methods: Patient data was extracted through an electronic medical record review. Using a lentiviral approach, the patient’s STXBP2 mutation and wild-type (WT) STXBP2 were separately transduced into the NK-92 human NK cell line. The WT and mutant STXBP2 transduced NK-92 cells were stimulated with NK-sensitive K562 erythroleukemia target cells in vitro, and NK cell degranulation and cytolysis were measured via CD107a expression and Live/Dead near-IR dye, respectively. Results: Compared to WT STXBP2, the patient’s STXBP2 mutation caused significantly decreased NK cell cytolysis and associated degranulation in vitro. Conclusion: These findings add weight to the hypothesis that some severe cases of COVID-19 may be accompanied by sHLH and hyperinflammation, especially in the setting of heterozygous pHLH genetic mutations. This has implications both diagnostically and therapeutically for severe COVID-19.

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Section: Css/hlh/mas Systemmentioning

confidence: 96%