AI Article Synopsis

  • Human iris patterns show significant variation, which is important for understanding eye diseases, forensics, and neurodevelopment processes.
  • Genome-wide association studies on specific iris traits in Australian individuals of European descent identified links between these traits and certain genes, with significant p-values indicating strong associations.
  • The research implies that genes related to neurodevelopment may also play a role in shaping the structures of the human iris, suggesting a connection between neuronal development and iris pattern formation.

Article Abstract

Human iris patterns are highly variable. The origins of this variation are of interest in the study of iris-related eye diseases and forensics, as well as from an embryological developmental perspective, with regard to their possible relationship to fundamental processes of neurodevelopment. We have performed genome-wide association scans on four iris characteristics (crypt frequency, furrow contractions, presence of peripupillary pigmented ring, and number of nevi) in three Australian samples of European descent. Both the discovery (n = 2121) and replication (n = 499 and 73) samples showed evidence for association between (1) crypt frequency and variants in the axonal guidance gene SEMA3A (p = 6.6 × 10(-11)), (2) furrow contractions and variants within the cytoskeleton gene TRAF3IP1 (p = 2.3 × 10(-12)), and (3) the pigmented ring and variants in the well-known pigmentation gene SLC24A4 (p = 7.6 × 10(-21)). These replicated findings individually accounted for around 1.5%-3% of the variance for these iris characteristics. Because both SEMA3A and TRAFIP1 are implicated in pathways that control neurogenesis, neural migration, and synaptogenesis, we also examined the evidence of enhancement among such genes, finding enrichment for crypts and furrows. These findings suggest that genes involved in normal neuronal pattern development may also influence tissue structures in the human iris.

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Source
http://www.ncbi.nlm.nih.gov/pmc/articles/PMC3155193PMC
http://dx.doi.org/10.1016/j.ajhg.2011.07.011DOI Listing

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