Utilizing Genomically Targeted Molecular Data to Improve Patient-Specific Outcomes in Autism Spectrum Disorder |
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Authors: | Sharon Hausman-Cohen William LaValley Heather Way Emily Gutierrez Jordan Reeder |
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Affiliation: | 1.IntellxxDNA, Austin, TX 78731, USA;2.LaValley MD Protocols, Austin, TX 78759, USA;3.The Australian Center for Genomic Analysis, Kenmore, QLD 4069, Australia;4.Neuronutrition Associates, Austin, TX 78730, USA; |
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Abstract: | Molecular biology combined with genomics can be a powerful tool for developing potential intervention strategies for improving outcomes in children with autism spectrum disorders (ASD). Monogenic etiologies rarely cause autism. Instead, ASD is more frequently due to many polygenic contributing factors interacting with each other, combined with the epigenetic effects of diet, lifestyle, and environment. One limitation of genomics has been identifying ways of responding to each identified gene variant to translate the information to something clinically useful. This paper will illustrate how understanding the function of a gene and the effects of a reported variant on a molecular level can be used to develop actionable and targeted potential interventions for a gene variant or combinations of variants. For illustrative purposes, this communication highlights a specific genomic variant, SHANK3. The steps involved in developing molecularly genomically targeted actionable interventions will be demonstrated. Cases will be shared to support the efficacy of this strategy and to show how clinicians utilized these targeted interventions to improve ASD-related symptoms significantly. The presented approach demonstrates the utility of genomics as a part of clinical decision-making. |
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Keywords: | autism spectrum disorder (ASD) clinical decision support tool (CDS tool) SHANK3 (SH3 and multiple ankyrin repeat domains 3) genomics molecular biology variant SNP (small nucleic polymorphism) personalized medicine glutamate PMS (Phelan-McDermid syndrome) PDD (pervasive developmental disorder) |
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