Neurodevelopmental outcomes in two cases of artemis deficiency

LymphoSign Journal Pub Date : 2024-01-10 DOI:10.14785/lymphosign-2023-0011

Angela Hu, Omar Almatrafi, Vy HD Kim, Donna Wall, R. Brager

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Abstract

Background: Severe Combined Immunodeficiency (SCID) is a category of inborn errors of immunity where there is impaired T and B cell development and/or function. Artemis SCID (Art-SCID) is characterized by dysfunctional Artemis protein, which is crucial for V(D)J recombination in T and B cell maturation. Art-SCID is fatal without management, and current definitive treatment involves hematopoietic stem cell transplantation (HSCT) or gene therapy. As the prognosis and survival of SCID patients improves, current research has begun unveiling long-term complications and morbidities. Previous literature has reported neurodevelopmental abnormalities in SCID patients, such as developmental delay and Autism Spectrum Disorder (ASD). However, it remains unknown whether these neurodevelopmental differences are linked to the SCID mutation, an adverse outcome of treatment and hospitalization, or comorbid social isolation and psychosocial challenges. Aims: In this case series, we discuss two cases of Art-SCID which presented with neurodevelopmental deficits following successful HSCT. Results: In both cases, SCID was detected on Newborn Screening (NBS), and Art-SCID was confirmed with genetic testing. Both patients were successfully treated with HSCT at 80 days of life, and followed up clinically well, with robust cell counts. Both patients later presented in toddlerhood with developmental, speech and language delay, however only one patient met diagnostic criteria for ASD. Conclusion: The definitive relationship between SCID, HSCT, and neurodevelopmental outcomes remain unclear, and warrants further study to allow for early intervention. We are currently working with colleagues across the country to further investigate and define this complex relationship. Statement of Novelty: We are investigating the complex relationship between SCID, HSCT, and potential neurodevelopmental outcomes. We present two cases of patients with Artemis SCID who were successfully treated with HSCT, and later presented in toddlerhood with developmental, speech, and language delay.

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两例青蒿素缺乏症患者的神经发育结果

背景：严重联合免疫缺陷症（SCID）是一类先天性免疫缺陷，T 细胞和 B 细胞发育和/或功能受损。Artemis SCID（Art-SCID）的特点是Artemis蛋白功能障碍，该蛋白对T细胞和B细胞成熟过程中的V(D)J重组至关重要。Art-SCID不经治疗是致命的，目前的确切治疗方法包括造血干细胞移植（HSCT）或基因治疗。随着SCID患者预后和存活率的提高，目前的研究已开始揭示长期并发症和发病率。以往的文献报道了SCID患者的神经发育异常，如发育迟缓和自闭症谱系障碍（ASD）。然而，这些神经发育异常是否与 SCID 基因突变、治疗和住院的不良后果或合并的社会隔离和社会心理挑战有关，目前仍不得而知。目的：在本病例系列中，我们讨论了两例成功造血干细胞移植后出现神经发育缺陷的Art-SCID病例。结果两例患者均在新生儿筛查（NBS）中发现SCID，并通过基因检测确诊为Art-SCID。两名患者均在出生后80天成功接受了造血干细胞移植治疗，临床随访情况良好，细胞计数强劲。两名患者在幼儿期均出现发育、言语和语言障碍，但只有一名患者符合 ASD 诊断标准。结论SCID、造血干细胞移植和神经发育结果之间的明确关系仍不清楚，需要进一步研究，以便及早干预。目前，我们正与全国各地的同行合作，进一步研究和界定这种复杂的关系。新颖性声明：我们正在研究 SCID、造血干细胞移植和潜在神经发育结果之间的复杂关系。我们介绍了两例阿特米斯 SCID 患者，他们成功接受了造血干细胞移植治疗，后来在幼儿期出现了发育、言语和语言发育迟缓。

本文章由计算机程序翻译，如有差异，请以英文原文为准。

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LymphoSign Journal

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