Large-scale evaluation of outcomes after a genetic diagnosis in children with severe developmental disorders

Genetics in Medicine Open Pub Date : 2024-01-01 DOI:10.1016/j.gimo.2024.101864

Harriet Copeland , Karen J. Low , Sarah L. Wynn , Ayesha Ahmed , Victoria Arthur , Meena Balasubramanian , Katya Bennett , Jonathan Berg , Marta Bertoli , Lisa Bryson , Catrin Bucknall , Jamie Campbell , Kate Chandler , Jaynee Chauhan , Amy Clarkson , Rachel Coles , Hector Conti , Philandra Costello , Tessa Coupar , Amy Craig , Caroline F. Wright

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Abstract

Purpose

We sought to evaluate outcomes for clinical management after a genetic diagnosis from the Deciphering Developmental Disorders study.

Methods

Individuals in the Deciphering Developmental Disorders study who had a pathogenic/likely pathogenic genotype in the DECIPHER database were selected for inclusion (n = 5010). Clinical notes from regional clinical genetics services notes were reviewed to assess predefined clinical outcomes relating to interventions, prenatal choices, and information provision.

Results

Outcomes were recorded for 4237 diagnosed probands (85% of those eligible) from all 24 recruiting centers across the United Kingdom and Ireland. Clinical management was reported to have changed in 28% of affected individuals. Where individual-level interventions were recorded, additional diagnostic or screening tests were started in 903 (21%) probands through referral to a range of different clinical specialties, and stopped or avoided in a further 26 (0.6%). Disease-specific treatment was started in 85 (2%) probands, including seizure-control medications and dietary supplements, and contra-indicated medications were stopped or avoided in a further 20 (0.5%). The option of prenatal/preimplantation genetic testing was discussed with 1204 (28%) families, despite the relatively advanced age of the parents at the time of diagnosis. Importantly, condition-specific information or literature was given to 3214 (76%) families, and 880 (21%) were involved in family support groups. In the most common condition (KBG syndrome; 79 [2%] probands), clinical interventions only partially reflected the temporal development of phenotypes, highlighting the importance of consensus management guidelines and patient support groups.

Conclusion

Our results underscore the importance of achieving a clinico-molecular diagnosis to ensure timely onward referral of patients, enabling appropriate care and anticipatory surveillance, and for accessing relevant patient support groups.

查看原文本刊更多论文

严重发育障碍儿童基因诊断后结果的大规模评估。

目的：我们试图评估来自破译发育障碍研究的基因诊断后的临床管理结果。方法：在破译发育障碍研究中，选择在破译数据库中具有致病/可能致病基因型的个体（n = 5010）纳入研究。来自区域临床遗传学服务记录的临床记录进行了审查，以评估与干预措施、产前选择和信息提供有关的预先确定的临床结果。结果：记录了来自英国和爱尔兰所有24个招募中心的4237名确诊先证患者（85%符合条件的患者）的结果。据报道，28%的受影响个体的临床管理发生了变化。在记录个人水平干预措施的地方，903名先证者（21%）通过转诊到一系列不同的临床专科开始了额外的诊断或筛查测试，另外26名先证者（0.6%）停止或避免了额外的诊断或筛查测试。85名（2%）先证者开始了疾病特异性治疗，包括癫痫控制药物和膳食补充剂，另外20名（0.5%）先证者停止或避免使用禁忌症药物。1204个（28%）家庭讨论了产前/植入前基因检测的选择，尽管诊断时父母的年龄相对较大。重要的是，向3214个（76%）家庭提供了特定疾病的信息或文献，880个（21%）家庭参与了家庭支持小组。在最常见的情况下(KBG综合征；79[2%]先知者)，临床干预仅部分反映了表型的时间发展，强调了共识管理指南和患者支持团体的重要性。结论：我们的研究结果强调了实现临床分子诊断的重要性，以确保患者及时转诊，实现适当的护理和预期监测，并获得相关的患者支持小组。

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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Genetics in Medicine Open

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