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      Development of rostral prefrontal cortex and cognitive and behavioural disorders.

      Developmental Medicine and Child Neurology
      Adolescent, Cell Count, Child, Child Behavior Disorders, diagnosis, epidemiology, Child, Preschool, Cognition Disorders, Dendrites, physiology, Humans, Intelligence, Magnetic Resonance Imaging, Memory Disorders, Prefrontal Cortex, pathology, Severity of Illness Index, Synapses

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          Abstract

          Information on the development and functions of rostral prefrontal cortex (PFC), or Brodmann area 10, has been gathered from different fields, from anatomical development to functional neuroimaging in adults, and put forward in relation to three particular cognitive and behavioural disorders. Rostral PFC is larger and has a lower cell density in humans than in other primates. It also has a large number of dendritic spines per cell and numerous connections to the supramodal cortex. These characteristics suggest that rostral PFC is likely to support processes of integration or coordination of inputs that are particularly developed in humans. The development of rostral PFC is prolonged, with decreases in grey matter and synaptic density continuing into adolescence. Functions attributed to rostral PFC, such as prospective memory, seem similarly to follow a prolonged development until adulthood. Neuroimaging studies have generally found a reduced recruitment of rostral PFC, for example in tasks requiring response inhibition, in adults compared with children or adolescents, which is consistent with maturation of grey matter. The examples of autism, attention-deficit-hyperactivity disorder, and schizophrenia show that rostral PFC could be affected in several disorders as a result of the susceptibility of its prolonged maturation to developmental abnormalities.

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