Immunological and molecular study in children with combined immunodeficiency.

IF 2.6 Q2 ALLERGY European annals of allergy and clinical immunology Pub Date : 2024-07-01 Epub Date: 2023-02-14 DOI:10.23822/EurAnnACI.1764-1489.286
S Kholoussi, A Ramadan, N Kholoussi, E A Ashaat, A G Fayez, H A Raouf, I Helwa, N N Esmaiel, R Ghorab, A M Abo-Shanab
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Abstract

Summary: Background. Severe combined immunodeficiency (SCID) is a form of immunodeficiencies (PID), caused by molecular defects. These defects can restrict the development and function of lymphocytes. Early diagnosis and treatment of SCID can lead to disease-free survival. This study aims to investigate some of the possible underlying genetic defects in a group of Egyptian infants and children with clinical and immunological profiles suggestive of SCID. Methods. This study included eighty patients who showed clinical warning signs of immunodeficiency. Subjects were thoroughly examined clinically. Laboratory evaluation included immunoglobulins serum levels and flow cytometric assessment of immune cells. This testing showed an altered immune profile in thirty patients. They had decreased T and/or B lymphocytes or natural killer cells. DNA extraction was done for those cases. The coding regions of the RAG1 gene and RAG2 gene was investigated for hot spot mutations by sequencing technique guided by the patient clinical evaluation, inheritance pattern, immunophenotyping by flow cytometric analysis of lymphocyte subsets, and serum immunoglobulins level detection. Results. Results showed novel and previously reported variants (mutation, polymorphism), they were found in 18 cases which include variants in the RAG1 gene (E880K, A960A, H249R, S913R, K820R, V782G), and variants in the RAG2 gene (P501T, L514M, rs10836573, cDNA.2129A>T). Conclusions. To evaluate SCID patients completely, mutation gene analysis is highly required and recommended.

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联合免疫缺陷儿童的免疫学和分子研究
摘要:背景。严重联合免疫缺陷症(SCID)是免疫缺陷病(PID)的一种形式,由分子缺陷引起。这些缺陷会限制淋巴细胞的发育和功能。早期诊断和治疗 SCID 可使患者无病存活。研究目的本研究旨在调查一组临床和免疫学特征提示存在 SCID 的埃及婴幼儿可能存在的潜在遗传缺陷。研究方法。本研究包括 80 名出现免疫缺陷临床警示症状的患者。对受试者进行了全面的临床检查。实验室评估包括免疫球蛋白血清水平和免疫细胞流式细胞术评估。检测结果显示,30 名患者的免疫特征发生了改变。他们的 T 和/或 B 淋巴细胞或自然杀伤细胞减少。对这些病例进行了 DNA 提取。在患者临床评估、遗传模式、淋巴细胞亚群流式细胞分析免疫分型和血清免疫球蛋白水平检测的指导下,通过测序技术对 RAG1 基因和 RAG2 基因的编码区进行了热点突变研究。结果显示结果显示,18个病例中发现了新的和以前报道过的变异(突变、多态性),其中包括RAG1基因变异(E880K、A960A、H249R、S913R、K820R、V782G)和RAG2基因变异(P501T、L514M、rs10836573、cDNA.2129A>T)。结论为了全面评估 SCID 患者,我们强烈建议进行基因突变分析。
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