Dominant-negative mutations in human <i>IL6ST</i> underlie hyper-IgE syndrome

Béziat, Vivien; Sj, Tavernier; Chen, Y-H.; Ma, Chuang; Materna, Marie; Laurence, Arian; Staal, Jens; Aschenbrenner, Dominik; Roels, Lisa; Worley, Lisa; Claes, Kathleen; Gartner, Lisa; La, Kohn; M, De Bruyne; Schmitz-Abe, Klaus; Charbonnier, Louis-Marie; Keleş, Sevgi; Nammour, Justine; Vladikine, Natasha; Renkilaraj, Majistor Raj Luxman Maglorius; Seeleuthner, Yoann; Migaud, Mélanie; Rosain, Jérémie; Jeljeli, Mohamed; Boisson, Bertrand; E, Van Braeckel; Ja, Rosenfeld; Hirata, Dai; Lc, Burrage; Dr, Murdock; Lambrecht, Bart N.; Avettand-Fenoel,; Tp, Vogel; Cr, Esther; Haskoloğlu, Şule; Doğu, Figen; Čižnár, Peter; Boutboul, David; Marie, O; Amourette, Jean; Mn, Lebras; Gauvain, C.; Tchérakian, Colas; İkincioğulları, Aydan; Beyaert, Rudi; Abel, Laurent; Jd, Milner; Grimbacher, Bodo; Lj, Couderc; Mj, Butte; Af, Freeman; Catherinot, Émilie; Fieschi, Claire; Chatila, Talal A.; Sg, Tangye; Uhlig, Holm H.; Haerynck, Filomeen; Casanova, Jean‐Laurent; Puel, Anne

doi:10.1084/jem.20191804

Cited by 77 publications

(91 citation statements)

References 100 publications

(177 reference statements)

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“…Moreover, the viral phenotypes of patient fibroblasts were not rescued by treatment with IFN-a2b or -b, further confirming a complete IFNAR1 deficiency. Complete cytokine receptor deficiency due to the expression at the cell surface of a non-functional receptor has already been documented for IFNGR1, IFNGR2, IL17RA, IL10RA, IL10RB, IL6ST, and IL12RB1, with mutations impairing cytokine binding(56,(74)(75)(76)(77)(78)(79)(80). By contrast to these previous observations, the mutant IFNAR1 reported here is loss-of-function due to the absence of most of its intracellular domain, abolishing its signaling activity.…”

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confidence: 64%

Herpes simplex encephalitis in a patient with a distinctive form of inherited IFNAR1 deficiency

Bastard¹,

Manry²,

Chen³

et al. 2021

Journal of Clinical Investigation

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Inborn errors of TLR3-dependent IFN-a/b-and-l-mediated immunity in the central nervous system (CNS) can underlie herpes simplex virus 1 (HSV-1) encephalitis (HSE). The respective contributions of IFN-a/b and-l are unknown. We report a child homozygous for a genomic deletion of the entire coding sequence and part of the 3'UTR of the last exon of IFNAR1, who died from HSE at the age of two years. An older cousin died following vaccination against measles, mumps and rubella at 12 months of age, and another 17-year-old cousin homozygous for the same variant has had other, less severe viral illnesses. The encoded IFNAR1 protein is expressed on the cell surface but is truncated and cannot interact with the tyrosine kinase TYK2. The patient's fibroblasts and EBV-B cells did not respond to IFN-a2b or IFN-b, in terms of STAT1, STAT2 and STAT3 phosphorylation, or the genome-wide induction of IFN-stimulated genes. The patient's fibroblasts were susceptible to viruses, including HSV-1, even in the presence of exogenous IFN-a2b or IFN-b. HSE is therefore a consequence of inherited complete IFNAR1 deficiency. This viral disease occurred in natural conditions, unlike those previously reported in other patients with IFNAR1 or IFNAR2 deficiency. This experiment of Nature indicates that IFN-a/b are essential for anti-HSV-1 immunity in the CNS.

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contrasting

confidence: 64%

Herpes simplex encephalitis in a patient with a distinctive form of inherited IFNAR1 deficiency

Bastard¹,

Manry²,

Chen³

et al. 2021

Journal of Clinical Investigation

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“…This premise could account for the increased ERK signaling seen in IL6RA mutant mice, perhaps reflecting increased IL11-driven ERK signaling 3 . The idea of diminished interaction of mutant alpha chains with gp130 is suggested further by human genetics: autosomal recessive mutations in gp130 are associated with craniosynostosis, whereas autosomal dominant variation is not 19,20 .…”

Section: Discussionmentioning

confidence: 99%

Similarities and differences between IL11 and IL11RA1 knockout mice for lung fibro-inflammation, fertility and craniosynostosis

Widjaja

Sivakumar

et al. 2020

Preprint

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Genetic loss of function (LOF) in IL11RA infers IL11 signaling as important for fertility, fibrosis, inflammation and craniosynostosis. The impact of genetic LOF in IL11 has not been characterized. We generated IL11-knockout (Il11-/-) mice, which are born in normal Mendelian ratios, have normal hematological profiles and are protected from bleomycin-induced lung fibro-inflammation. Noticeably, baseline IL6 levels in the lungs of Il11-/- mice are lower than those of wild-type mice and are not induced by bleomycin damage, placing IL11 upstream of IL6. Lung fibroblasts from Il11-/- mice are resistant to pro-fibrotic stimulation and show evidence of reduced autocrine IL11 activity. Il11-/- female mice are infertile. Unlike Il11ra1-/- mice, Il11-/- mice do not have a craniosynostosis-like phenotype and exhibit mildly reduced body weights. These data highlight similarities and differences between LOF in IL11 or IL11RA while establishing further the role of IL11 signaling in fibrosis and stromal inflammation.

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“…All 27 patients harbored rare variants in the STAT3 gene: eight in exon 21; eight in exon 13; three in exon 10; two in exon 15, and one each in exon 6,16,17,19,22, and splice site downstream of exon 12 (Figure 1, Supplementary Table 1). Of these, three were picked up by whole exome sequencing, 16 by the 320 gene NGS panel, one by the limited 44 gene NGS panel, and seven by Sanger sequencing for STAT3 gene (Supplementary Table 2).…”

Section: Group I Hies With Rare Variants In Stat3 Genementioning

confidence: 99%

“…TH17 cell numbers were low in 10/11 (90.9%) STAT3 HIES tested. Rare variants observed were 8 in exon 21; 8 in exon 13; 3 in exon 10; 2 in exon 15, and one each in exon 6,16,17,19,22, and splice site downstream of exon 12. Seven variants were novel and included F174S, N567D, L404Sfs * 8, G419 =, M329K, T714I, R518X, and a splice site variant downstream of exon 12.…”

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confidence: 97%

Clinical Profile of Hyper-IgE Syndrome in India

et al. 2021

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Introduction: Hyper-IgE Syndrome (HIES) is a rare inborn error of immunity (IEI) characterized by a constellation of symptoms related to susceptibility to Staphylococcal skin and pulmonary infections, eczema, raised serum IgE (>2,000 IU/ml), craniofacial anomalies, and recurrent bone fractures. Data on HIES from the Indian subcontinent is scarce and restricted to small case series and case reports. This is the first compilation of national data on HIES.Materials and Methods: A total 103 cases clinically diagnosed and treated as HIES were analyzed from nine centers. Cases with clinical and/or molecular diagnosis of DOCK8 deficiency were not included. Patients were divided into two groups: group I for whom a heterozygous rare variant of STAT3 was identified, and group II, with clinical features similar to those of AD STAT3 deficiency, but without any genetic diagnosis.Results: Genetic diagnosis was available in 27 patients (26.2%) and all harbored rare variants in the STAT3 gene. Majority of these STAT3 HIES patients presented with recurrent skin abscesses (77.7%) or pneumonia (62.9%) or both (59.2%). Other features included eczema (37%), candidiasis (55.5%), facial dysmorphism (55.5%), recurrent fractures (11.1%), and retained primary teeth (7.4%). Mycobacterial infections were seen in a significant 18.5%. Mortality was seen in three subjects (11.1%). A similar trend in the clinical presentation was observed when all the 103 patients were analyzed together. Twenty percent of patients without a rare variant in the STAT3 gene had an NIH score of ≥40, whereas, 51.9% of STAT3 HIES subjects had scores below the cut off of ≥40. TH17 cell numbers were low in 10/11 (90.9%) STAT3 HIES tested. Rare variants observed were 8 in exon 21; 8 in exon 13; 3 in exon 10; 2 in exon 15, and one each in exon 6, 16, 17, 19, 22, and splice site downstream of exon 12. Seven variants were novel and included F174S, N567D, L404Sfs*8, G419 =, M329K, T714I, R518X, and a splice site variant downstream of exon 12.Conclusions: The report includes seven novel STAT3 variants, including a rare linker domain nonsense variant and a CC domain variant. Mycobacterial diseases were more frequent, compared to western literature.

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Dominant-negative mutations in human IL6ST underlie hyper-IgE syndrome

Cited by 77 publications

References 100 publications

Herpes simplex encephalitis in a patient with a distinctive form of inherited IFNAR1 deficiency

Herpes simplex encephalitis in a patient with a distinctive form of inherited IFNAR1 deficiency

Similarities and differences between IL11 and IL11RA1 knockout mice for lung fibro-inflammation, fertility and craniosynostosis

Clinical Profile of Hyper-IgE Syndrome in India

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