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      Is less really more: Does a prefrontal efficiency genotype actually confer better performance when working memory becomes difficult?

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          Abstract

          Perhaps the most widely studied effect to emerge from the combination of neuroimaging and human genetics is the association of the COMT-Val 108/158Met polymorphism with prefrontal activity during working memory. COMT-Val is a putative risk factor in schizophrenia, which is characterized by disordered prefrontal function. Work in healthy populations has sought to characterize mechanisms by which the valine (Val) allele may lead to disadvantaged prefrontal cognition. Lower activity in methionine (Met) carriers has been interpreted as advantageous neural efficiency. Notably, however, studies reporting COMT effects on neural efficiency have generally not reported working memory performance effects. Those studies have employed relatively low/easy working memory loads. Higher loads are known to elicit individual differences in working memory performance that are not visible at lower loads. If COMT-Met confers greater neural efficiency when working memory is easy, a reasonable prediction is that Met carriers will be better able to cope with increasing demand for neural resources when working memory becomes difficult. To our knowledge, this prediction has thus far gone untested. Here, we tested performance on three working memory tasks. Performance on each task was measured at multiple levels of load/difficulty, including loads more demanding than those used in prior studies. We found no genotype-by-load interactions or main effects of COMT genotype on accuracy or reaction time. Indeed, even testing for performance differences at each load of each task failed to find a single significant effect of COMT genotype. Thus, even if COMT genotype has the effects on prefrontal efficiency that prior work has suggested, such effects may not directly impact high-load working memory ability. The present findings accord with previous evidence that behavioral effects of COMT are small or nonexistent and, more broadly, with a growing consensus that substantial effects on phenotype will not emerge from candidate gene studies.

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          Author and article information

          Journal
          0100725
          3187
          Cortex
          Cortex
          Cortex; a journal devoted to the study of the nervous system and behavior
          0010-9452
          1973-8102
          22 January 2020
          14 November 2015
          January 2016
          18 February 2020
          : 74
          : 79-95
          Affiliations
          [a ]Department of Psychology, Georgetown University, United States
          [b ]Clinical Brain Disorders Branch, National Institute of Mental Health, United States
          Author notes
          [* ] Corresponding author. Department of Psychology, Georgetown University, 302C White-Gravenor Hall, 3700 O Street, NW, Box 571001, Washington, DC 20057, United States. aeg58@ 123456Georgetown.edu (A.E. Green).
          Article
          PMC7028246 PMC7028246 7028246 nihpa1068713
          10.1016/j.cortex.2015.10.025
          7028246
          26649915
          d7bdca0e-1ac3-4afc-bb14-0af16912607f
          History
          Categories
          Article

          DLPFC,Dopamine,Neural efficiency,Working memory,COMT
          DLPFC, Dopamine, Neural efficiency, Working memory, COMT

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