Your search keyword '"Boutros J"' showing total 2 results

1. Whole‐exome sequencing of T‐B+ severe combined immunodeficiency in Egyptian infants, JAK3 predominance and novel variants.

Author

El Hawary, R., Meshaal, S., Mauracher, A.A., Opitz, L., Abd Elaziz, D., Lotfy, S., Eldash, A., Boutros, J., Galal, N., Pachlopnik Schmid, J., and Elmarsafy, A.

Subjects

SEVERE combined immunodeficiency, GENETIC counseling, HUMAN chromosome abnormality diagnosis, DIAGNOSIS, MOLECULAR diagnosis, INFANTS

Abstract

Summary: Severe combined immunodeficiency (SCID) is fatal if not treated with immune reconstitution. In Egypt, T‐B+ SCID accounts for 38·5% of SCID diagnoses. An accurate genetic diagnosis is essential for choosing appropriate treatment modalities and for offering genetic counseling to the patient's family. The objectives of this study were to describe the clinical, immunological and molecular characteristics of a cohort of twenty Egyptian patients with T‐B+ SCID. The initial diagnosis (based on clinical features and flow cytometry) was followed by molecular investigation (whole‐exome sequencing). All patients had the classic clinical picture for SCID, including failure to thrive (n = 20), oral candidiasis (n = 17), persistent diarrhea (n = 14), pneumonia (n = 13), napkin dermatitis (n = 10), skin rash (n = 7), otitis media (n = 3) and meningitis (n = 2). The onset of manifestations was at the age of 2·4 ± 1·6 months and diagnosis at the age of 6·7 ± ·5 months, giving a diagnostic delay of 4·3 months. JAK3 gene variants were most frequent (n = 12) with three novel variants identified, followed by IL2Rγ variants (n = 6) with two novel variants. IL7Rα and CD3ε variants were found once, with a novel variant each. T‐B+NK− SCID accounted for approximately 90% of the Egyptian patients with T‐B+SCID. Of these T‐B+NK− SCID cases, 60% were autosomal recessive syndromes caused by JAK3 mutations and 30% were X‐linked syndromes. It might be useful to sequence the JAK3 gene (i.e. targeted Sanger sequencing) in all T‐B+ SCID patients, especially after X‐linked SCID has been ruled out. Hence, no more than 10% of T‐B+ SCID patients might require next‐generation for a molecular diagnosis. [ABSTRACT FROM AUTHOR]

Published

2021

2. Phenotypical heterogeneity in RAG‐deficient patients from a highly consanguineous population.

Author

Meshaal, S. S., El Hawary, R. E., Abd Elaziz, D. S., Eldash, A., Alkady, R., Lotfy, S., Mauracher, A. A., Opitz, L., Pachlopnik Schmid, J., van der Burg, M., Chou, J., Galal, N. M., Boutros, J. A., Geha, R., and Elmarsafy, A. M.

Subjects

SEVERE combined immunodeficiency, GENETIC regulation, B cells, CONSANGUINITY, POPULATION

Abstract

Summary: Mutations affecting recombination activation genes RAG1 and RAG2 are associated with variable phenotypes, depending on the residual recombinase activity. The aim of this study is to describe a variety of clinical phenotypes in RAG‐deficient patients from the highly consanguineous Egyptian population. Thirty‐one patients with RAG mutations (from 28 families) were included from 2013 to 2017. On the basis of clinical, immunological and genetic data, patients were subdivided into three groups; classical T–B– severe combined immunodeficiency (SCID), Omenn syndrome (OS) and atypical SCID. Nineteen patients presented with typical T–B–SCID; among these, five patients carried a homozygous RAG2 mutation G35V and five others carried two homozygous RAG2 mutations (T215I and R229Q) that were detected together. Four novel mutations were reported in the T–B–SCID group; three in RAG1 (A565P, N591Pfs*14 and K621E) and one in RAG2 (F29S). Seven patients presented with OS and a novel RAG2 mutation (C419W) was documented in one patient. The atypical SCID group comprised five patients. Two had normal B cell counts; one had a previously undescribed RAG2 mutation (V327D). The other three patients presented with autoimmune cytopaenias and features of combined immunodeficiency and were diagnosed at a relatively late age and with a substantial diagnostic delay; one patient had a novel RAG1 mutation (C335R). PID disorders are frequent among Egyptian children because of the high consanguinity. RAG mutations stand behind several variable phenotypes, including classical SCID, OS, atypical SCID with autoimmunity and T–B+ CID. RAG1/2 mutations stand behind variable clinical phenotypes.‎ The different phenotypes extend to include T–B+SCID and combined immunodeficiency ‎with granuloma and/or autoimmunity.‎ The genotype–phenotype correlation is not absolute and is affected by epigenetics, early ‎exposure to infections and other environmental factors. [ABSTRACT FROM AUTHOR]

Published

2019