Family History of Early Infant Death Correlates with Earlier Age at Diagnosis But Not Shorter Time to Diagnosis for Severe Combined Immunodeficiency

Luk, Anderson Dik Wai; Lee, Pamela; Mao, Huawei; Chan, Koon Wing; Chen, Xiang Yuan; Chen, Tong Xin; He, Jian Xin; Kechout, Nadia; Suri, Deepti; Bo, Tao
, 
Yin; Xu, Yong; Jiang, Li; Liew, Woei Kang; Jirapongsananuruk, Orathai; Daengsuwan, Tassalapa; Gupta, Anju; Singh, Surjit; Latiff, Amir Hamzah Abdul; Lee, Acw; Shek, Lynette Pei‐Chi; Nguyen, Thi Van Anh; Chin, Tek Jee; Chien, Yin‐Hsiu; Latiff, Zarina Abdul; Le, Thi Minh Huong; Le, Nguyen Ngoc Quynh; Lee, Bee Wah; Li, Qiang; Raj, Dinesh; Barbouche, Mohamed Ridha; Thong, Meow‐Keong; Ang, Maria Carmen D.; Wang, Xiao Chuan; Xu, Chuanlong; Yu, Hai Guo; Yu, Hsin-Hui; Lee, Tsz Leung; Yau, Felix Yat Sun; Wong, Wilfred Hing Sang; Tu, Wenwei; Yang, Wu; Chong, Patrick Chun Yin; Ho, Marco Hok Kung; Lau, Yu Lung

doi:10.3389/fimmu.2017.00808

Cited by 27 publications

(22 citation statements)

References 66 publications

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“…In conclusion, the diagnosis of disseminated BCG disease should be considered when a BCG vaccinated infant presents with cutaneous papules, pustules, and nodules, especially in infants with immunodeficiency. One study from the Asian Primary Immunodeficiency Network found typical clinical features of SCID, like candidiasis, BCG infections, pneumonia, chronic diarrhea, severe infections, and absolute lymphocyte count below 3 × 109/L were often not recognized by clinicians, thereby prolonging the time to diagnosis . The only solution for early diagnosis of SCID is newborn screening.…”

Section: Discussionmentioning

confidence: 99%

“…One study from the Asian Primary Immunodeficiency Network found typical clinical features of SCID, like candidiasis, BCG infections, pneumonia, chronic diarrhea, severe infections, and absolute lymphocyte count below 3 × 109/L were often not recognized by clinicians, thereby prolonging the time to diagnosis. 11 The F I G U R E 4 Black arrow designates the proband. Sequencing identified de novo compound heterozygous mutation c. 1934 A > G in the JAK3 gene and heterozygous variant c. 1899 C > A in the JAK3 gene carried by both the proband and her mother…”

Section: Discussionmentioning

confidence: 99%

See 1 more Smart Citation

Disseminated Bacille Calmette‐Guérin infection in a patient with severe combined immunodeficiency caused by JAK3 gene mutation

Chen

Zhu

et al. 2019

Pediatric Dermatology

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Bacille Calmette‐Guérin (BCG), a live attenuated vaccine prepared using Mycobacterium bovis, can prevent tuberculosis in children and is routinely administered to infants in China and many other countries. A serious complication following vaccination is disseminated BCG infection. The risk is greatly increased in patients with severe combined immunodeficiency disease (SCID), a syndrome characterized by deficiency of both humoral and cellular immunity. We report a case of disseminated BCG infection in an infant with SCID caused by two novel janus kinase 3 (JAK3) gene mutations.

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Section: Discussionmentioning

confidence: 99%

Section: Discussionmentioning

confidence: 99%

Disseminated Bacille Calmette‐Guérin infection in a patient with severe combined immunodeficiency caused by JAK3 gene mutation

Chen

Zhu

et al. 2019

Pediatric Dermatology

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“…The SCIDX1 patients with IL2RG deficiency are the largest group in the populations with low‐consanguinity rates like European or far east countries (Fischer et al., 2015; Luk et al., 2017), but we found RAG1/2 deficiency (47%) which leads to T‐B‐NK+ phenotype is the most common group in our Turkish SCID cohort. Due to the high consanguineous marriage rates in our country, autosomal‐recessive inherited genes might be the most effected genes among the SCID patients in our cohort.…”

Section: Discussionmentioning

confidence: 45%

Mutational landscape of severe combined immunodeficiency patients from Turkey

Fırtına

et al. 2020

Int J Immunogenetics

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Severe combined immunodeficiency (SCID) has a diverse genetic aetiology, where a clinical phenotype, caused by single and/or multiple gene variants, can give rise to multiple presentations. The advent of next‐generation sequencing (NGS) has recently enabled rapid identification of the molecular aetiology of SCID, which is crucial for prognosis and treatment strategies. We sought to identify the genetic aetiology of various phenotypes of SCIDs and assessed both clinical and immunologic characteristics associated with gene variants. An amplicon‐based targeted NGS panel, which contained 18 most common SCID‐related genes, was contumely made to screen the patients (n = 38) with typical SCID, atypical SCID or OMENN syndrome. Allelic segregations were confirmed for the detected gene variants within the families. In total, 24 disease‐causing variants (17 known and 7 novel) were identified in 23 patients in 9 different SCID genes: RAG1 (n = 5), RAG2 (n = 2), ADA (n = 3), DCLRE1C (n = 2), NHEJ1 (n = 2), CD3E (n = 2), IL2RG (n = 3), JAK3 (n = 4) and IL7R (n = 1). The overall success rate of our custom‐made NGS panel was 60% (39.3% for NK+ SCID and 100% for NK− SCID). Incidence of autosomal‐recessive inherited genes is more frequently found in our cohort than the previously reported populations probably due to the high consanguineous marriages in Turkey. In conclusion, the custom‐made sequencing panel was able to identify and confirm the previously known and novel disease‐causing variants with high accuracy.

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“…The R328X mutation was first reported in 2017 in a cohort of 147 Asiatic SCID patients , but detailed clinical and immunological information has only been described recently in two patients with the same mutation . Lim et al reported the R328X mutation in a 16‐year‐old Kurdish boy with chronic airway hypersensitivity and recurrent sinopulmonary infections and Tanita et al described the same mutation in a 21‐year‐old Japanese male with recurrent respiratory infections, EBV‐associated leiomyoma during childhood and invasive Haemophilus influenzae infection .…”

Section: Discussionmentioning

confidence: 99%

“…Until very recently, mutations in exon 8 have been described only in association with the typical X-SCID phenotype [28], thus suggesting a critical role on the C-terminal part of the cytoplasmic domain of γ c for correct signal transmission. Up to the present, two case reports and a cohort study have reported a hypomorphic mutation located in exon 8 (c.C982T/ p.328X) [19,21,29].…”

Section: Introductionmentioning

confidence: 90%

The IL-2RG R328X nonsense mutation allows partial STAT-5 phosphorylation and defines a critical region involved in the leaky-SCID phenotype

Arcas-García

García-Prat

Magallón-Lorenz

et al. 2020

Clinical and Experimental Immunology

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Summary In addition to their detection in typical X‐linked severe combined immunodeficiency, hypomorphic mutations in the interleukin (IL)‐2 receptor common gamma chain gene (IL2RG) have been described in patients with atypical clinical and immunological phenotypes. In this leaky clinical phenotype the diagnosis is often delayed, limiting prompt therapy in these patients. Here, we report the biochemical and functional characterization of a nonsense mutation in exon 8 (p.R328X) of IL2RG in two siblings: a 4‐year‐old boy with lethal Epstein–Barr virus‐related lymphoma and his asymptomatic 8‐month‐old brother with a TlowB+natural killer (NK)+ immunophenotype, dysgammaglobulinemia, abnormal lymphocyte proliferation and reduced levels of T cell receptor excision circles. After confirming normal IL‐2RG expression (CD132) on T lymphocytes, signal transducer and activator of transcription‐1 (STAT‐5) phosphorylation was examined to evaluate the functionality of the common gamma chain (γc), which showed partially preserved function. Co‐immunoprecipitation experiments were performed to assess the interaction capacity of the R328X mutant with Janus kinase (JAK)3, concluding that R328X impairs JAK3 binding to γc. Here, we describe how the R328X mutation in IL‐2RG may allow partial phosphorylation of STAT‐5 through a JAK3‐independent pathway. We identified a region of three amino acids in the γc intracellular domain that may be critical for receptor stabilization and allow this alternative signaling. Identification of the functional consequences of pathogenic IL2RG variants at the cellular level is important to enable clearer understanding of partial defects leading to leaky phenotypes.

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Family History of Early Infant Death Correlates with Earlier Age at Diagnosis But Not Shorter Time to Diagnosis for Severe Combined Immunodeficiency

Cited by 27 publications

References 66 publications

Disseminated Bacille Calmette‐Guérin infection in a patient with severe combined immunodeficiency caused by JAK3 gene mutation

Disseminated Bacille Calmette‐Guérin infection in a patient with severe combined immunodeficiency caused by JAK3 gene mutation

Mutational landscape of severe combined immunodeficiency patients from Turkey

The IL-2RG R328X nonsense mutation allows partial STAT-5 phosphorylation and defines a critical region involved in the leaky-SCID phenotype

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