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Genetic diagnostic outcomes from a 10-year research programme in autism in Aotearoa New Zealand

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Taylor & Francis Group2025-08-11 更新2026-04-16 收录
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https://tandf.figshare.com/articles/dataset/Genetic_diagnostic_outcomes_from_a_10-year_research_programme_in_autism_in_Aotearoa_New_Zealand/27055669/1
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Autism is a relatively common neurodevelopmental difference with considerable phenotypic heterogeneity impacting cognitive, sensory, and social processing, and often co-occurs with other conditions. Therefore, there is not a one-size-fits-all clinical support pathway for autistic individuals following diagnosis. DNA sequencing technology has enabled the discovery of genes causative of, or associated with, autism. Unsurprisingly, genetic heterogeneity goes hand-in-hand with the phenotypic heterogeneity for this condition; with causative genetic variation ranging from single base pair changes to complex chromosomal rearrangements in more than 100 different genes. This study captures a snapshot (201 individuals) of the autistic population (both clinically referred and self-referred) in Aotearoa New Zealand and documents a decade’s research effort to refine diagnosis using a flexible and customised genome-wide sequencing approach. The diagnostic yield in this phenotypically disparate cohort was 12.9%, with an additional 15.9% of individuals harbouring ‘likely causal’ variants, providing the groundwork to tailor clinical, social, and educational care. Importantly, this study reveals the diagnostic utility of customised genetic screening for autism across a phenotypically diverse autistic population.
提供机构:
Walker, Caroline; Samson, Christopher; Muir, Colette; Lehnert, Klaus; Swan, Brendan; Taylor, Juliet; Love, Donald R.; Jacobsen, Jessie C.; Garton, Alexandra; Monk, Ruth; Hawkins, Victoria; Knowles, Sarah D.; Snell, Russell G.; Lowther, Chelsea; Port, Waiora; Whitford, Whitney; Velzian, Lydia; Poquérusse, Jessie; Moodley, Kriebashne S.; Musgrave, Suzanne M.; Hill, Rosamund; Talkowski, Michael E.
创建时间:
2024-09-18
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