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.
Genetic diagnostic outcomes from a 10-year research programme in autism in Aotearoa New Zealand.
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作者:Musgrave Suzanne M, Taylor Juliet, Whitford Whitney, Garton Alexandra, Poquérusse Jessie, Hawkins Victoria, Port Waiora, Moodley Kriebashne S, Monk Ruth, Knowles Sarah D, Walker Caroline, Samson Christopher, Velzian Lydia, Swan Brendan, Love Donald R, Hill Rosamund, Muir Colette, Talkowski Michael E, Lowther Chelsea, Snell Russell G, Lehnert Klaus, Jacobsen Jessie C
| 期刊: | J R Soc N Z | 影响因子: | 0.000 |
| 时间: | 2025 | 起止号: | 2024 Sep 18; 55(6):2464-2480 |
| doi: | 10.1080/03036758.2024.2394128 | ||
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