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Chunk #26 — HIGHLIGHTS

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The Collaborative Study on the Genetics of Alcoholism: Overview.
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Individual reviews in this issue provide detailed illustrations of the ways in which COGA data have contributed towards advancing our understanding of the etiology, course and consequences of AUD, and pathways from onset to remission and relapse. COGA's intergenerational design has, in addition to identifying genetic risk factors, contributed to our understanding of the role of social genetic mechanisms 50 , 52 , 64 , 65 , 66 in the interplay between genetic liability and the socio‐environmental milieu (e.g., References 40, 48, 67, 68). Diversity in the data have driven gene discoveries within our dataset (e.g., Reference 44) and in collaboration with others (e.g., References 5, 55, 69). Our ability to develop iPSCs from individuals with different genetic loading is producing insights into properties of cells derived from persons with archival electrophysiological and behavioral phenotyping, and how the cells differentially respond to ethanol exposure. A notable contribution of COGA's family design has been to disentangle antecedents of, and predisposition to AUD from its sequelae. By characterizing brain and behavior in offspring from families enriched for AUD liability—both genetic and environmental—prior