A founder <scp>RAB27A</scp> variant causes Griscelli syndrome type 2 with phenotypic heterogeneity in Qatari families

Alsulaiman, Reem; Othman, Amna; El‐Akouri, Karen; Fareed, Shehab; Almulla, Hajer; Sukik, Aseel; Al‐Mureikhi, Mariam; Shahbeck, Noora; Ali, Rehab; Al‐Mesaifri, Fatma; Musa, Sara; Al-Mulla, Mariam; Ibrahim, Khalid; Mohamed, Khalid; Al-Nesef, Maryam Ali; Ehlayel, Mohammad; Ben‐Omran, Tawfeg

doi:10.1002/ajmg.a.61829

Cited by 14 publications

(30 citation statements)

References 39 publications

(40 reference statements)

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“…When the studies on GS2 are examined, it has drawn our attention that genetic mutations are concentrated in some regions. The c.514_518del mutation in Turkey and Iran (11), (current study) the c.C550T mutation in a study by Singh et al in India, and the c.244C > T mutation in a study involving 6 families in Qatar by Al-Sulaiman et al (12), (13). However, predisposing any founder affect based on the findings and literature knowledge is less likely due to the lack of population specific databases.…”

Section: Discussionmentioning

confidence: 64%

Hemophagocytic Lymphohistiocytosis in Children with Griscelli Syndrome Type 2 : Genetic, Laboratory findings and Treatment

Çay

Sezer

Karakulak

et al. 2023

Preprint

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Section: Discussionmentioning

confidence: 64%

Hemophagocytic Lymphohistiocytosis in Children with Griscelli Syndrome Type 2 : Genetic, Laboratory findings and Treatment

Çay

Sezer

Karakulak

et al. 2023

Preprint

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“…RAG1, one of the genes involved in Severe Combined Immunodeficiency (SCID) [25], is also reported in association with refractory status epilepticus [26] and optic neuropathy [27]. Other associations include AIRE with autoimmune cerebellar degeneration [28]; RAB27A with developmental regression and seizures [29]; RTEL1 with microcephaly, developmental delay, spastic diplegia, and cerebellar dysfunction [30]; STAT1 with CNS aneurysms and inflammatory spinal cord lesions [31]; SMARCAL1 with microcephaly, developmental delays, and neuronal migration disorders [32]. TTC7A with perisylvian polymicrogyria, cerebellar hypoplasia and arthrogryposis, severe microcephaly, refractory epilepsy, developmental delay, and hypomyelinating leukodystrophy [33]; and ZAP70 with silent brain infarcts [34].…”

Section: Discussionmentioning

confidence: 99%

Association of rare variants in genes of immune regulation with pediatric autoimmune CNS diseases

et al. 2022

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Background There is a gap in the literature regarding genetic underpinnings of pediatric autoimmune CNS diseases. This study explored rare gene variants implicated in immune dysregulation within these disorders. Methods This was a single-center observational study of children with inflammatory CNS disorder who had genetic testing through next generation focused exome sequencing targeting 155 genes associated with innate or adaptive immunity. For in silico prediction of functional effects of single-nucleotide variants, Polymorphism Phenotyping v2, and Sorting Intolerant from Tolerant were used, and Combined Annotation Dependent Depletion (CADD) scores were calculated. Identified genes were analyzed using Kyoto Encyclopedia of Genes and Genomes (KEGG) pathway analysis. Results Of 54 patients, 42 (77.8%) carried variant(s), among which 12 (22.2%) had 3-8 variants. Eighty-eight unique singlenucleotide variants of 55 genes were identified. The most variants were detected in UNC13D, LRBA, LYST, NOD2, DOCK8, RNASEH2A, STAT5B, and AIRE. The majority of variants (62, 70.4%) had CADD > 10. KEGG pathway analysis revealed seven genes associated with primary immunodeficiency (Benjamini 1.40E − 06), six genes with NOD-like receptor signaling (Benjamini 4.10E − 04), five genes with Inflammatory Bowel Disease (Benjamini 9.80E − 03), and five genes with NF-kappa B signaling pathway (Benjamini 1.90E − 02). Discussion We observed a high rate of identification of rare and low-frequency variants in immune regulatory genes in pediatric neuroinflammatory CNS disorders. We identified 88 unique single-nucleotide variants of 55 genes with pathway analysis revealing an enrichment of NOD2-receptor signaling, consistent with involvement of the pathway within other autoinflammatory conditions and warranting further investigation.

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“…Another case was also diagnosed with HLH with a prior EBV infection and died at the age of 39 years. 11 In a study in Turkey by Cetinkaya et.al, on 28 patients with HLH, the median age of the study population was 23 (4.3 to 117) months at the time of the diagnosis of HLH. In a study in Egypt, 101 patients with HLH were enrolled and the median age at presentation was 13.1 months.…”

Section: Case Presentationmentioning

confidence: 98%

Neonatal Onset of Hemophagocytic Lymphohistiocytosis Due to Prenatal Varicella-Zoster Infection in a Neonate with Griscelli Syndrome Type 2

Nodehi¹,

Faranoush²,

Arshi³

et al. 2022

IJAAI

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Griscelli syndrome (GS) type 2 is an inborn error of the immune system classified as immune dysregulation. This autosomal recessive disease has three types with different genetic causes. In all variants, hypopigmentation is common, but neurological involvement or immunodeficiency varies in severity. The known genetic defects associated with GS include mutations in myosin 5 A (GS type1), guanosine triphosphate binding protein (GS type 2), and human melanophilin (GS type 3). Hemophagocytic lymphohistiocytosis (HLH) is a life-threatening condition and is characterized by severe, ineffective, and uncontrolled inflammatory reactions. A HLH can be classified as primary or secondary, with secondary resulting from autoimmunity, malignancy, spontaneous or infectious causes. Many prenatal infections can cause long-term complications in the fetus, including toxoplasmosis, rubella, cytomegalovirus, herpes simplex, syphilis, parvovirus, and varicella zoster (known as TORCH syndrome). Prenatal infections have been associated with TORCH for a long time, but HLH is a rare complication. The report presents a case of HLH with symptoms of sepsis, organomegaly, and cytopenia from the time of birth. A genetic test confirmed Griscelli Syndrome Type 2, which was diagnosed during an immunologic consultation regarding partial albinism not seen in family members. Prenatal infection was the only approved finding in the investigation into the trigger of HLH in this patient starting in the first days of life. Accordingly, the patient was diagnosed with type 2GS syndrome with neonatal-onset HLH caused by a prenatal infection.

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A founder RAB27A variant causes Griscelli syndrome type 2 with phenotypic heterogeneity in Qatari families

Cited by 14 publications

References 39 publications

Hemophagocytic Lymphohistiocytosis in Children with Griscelli Syndrome Type 2 : Genetic, Laboratory findings and Treatment

Hemophagocytic Lymphohistiocytosis in Children with Griscelli Syndrome Type 2 : Genetic, Laboratory findings and Treatment

Association of rare variants in genes of immune regulation with pediatric autoimmune CNS diseases

Neonatal Onset of Hemophagocytic Lymphohistiocytosis Due to Prenatal Varicella-Zoster Infection in a Neonate with Griscelli Syndrome Type 2

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