Tyrosine hydroxylase expression and neuronal loss in the male and female adolescent ventral tegmental area.

Neurosci Lett

Department of Psychology: Neural and Cognitive Sciences Program, Bowling Green State University, Bowling Green, OH 43403, United States; John Paul Scott Center for Neuroscience, Mind and Behavior, Bowling Green State University, Bowling Green, OH 43403, United States. Electronic address:

Published: October 2024

AI Article Synopsis

  • Adolescence is a key developmental phase marked by significant changes in behavior and brain structure, but there's less research on how development progresses during this period.
  • The study focuses on the ventral tegmental area (VTA) in rats, examining neuron numbers and expressions of a specific enzyme, tyrosine hydroxylase, at different stages: pre-pubertal, recently post-pubertal, and young adulthood.
  • Results indicate a decline in dopamine neuron numbers from early adolescence to young adulthood, with notable changes in males post-puberty, suggesting that brain development during adolescence may be linked to psychiatric disorders related to dopamine.

Article Abstract

Adolescence is a critical period of development characterized by numerous behavioral and neuroanatomical changes. While studies of adolescent neurodevelopment typically compare adolescent age groups with young adults, there are fewer studies that assess developmental trajectories within the adolescent period. In the adolescent prefrontal cortex, some maturational changes take place linearly/chronologically, while others are associated specifically with pubertal onset. The adolescent ventral tegmental area (VTA), a primary source of forebrain dopamine, is relatively understudied during this period. In the present study, dopamine neuron number, total neuron number and tyrosine hydroxylase expression are assessed in the male and female rat VTA at three timepoints: postnatal day(P) 30 (pre-pubertal), P40 (post-pubertal for females, pre-pubertal for males) and P60 (post-pubertal). There was a non-significant trend for a reduction in total VTA neuron number between P30 and P60, but there was a significant reduction in dopamine neuron number across age. The expression of tyrosine hydroxylase did not change with age. However, in a second cohort of subjects, brain tissue was collected pre-pubertal, from recently post-pubertal males and females, and young adults. In this cohort, there was a sex-specific and transient decrease in tyrosine hydroxylase expression in recently post-pubertal males. These results suggest a selective pruning of VTA dopamine cells between early adolescence and young adulthood, while pubertal onset may coincide with a rapid maturation of these neurons. These findings may have implications for psychiatric disorders associated with dopamine dysfunction that tend to manifest during adolescence.

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Source
http://dx.doi.org/10.1016/j.neulet.2024.137961DOI Listing

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