Developmental anatomy of the thalamus, perinatal lesions, and neurological development

Publication date

2025-01

Authors

Govaert, Paul
Arena, Roberta
Dudink, JeroenISNI 0000000387693657
Steggerda, Sylke
Agut, Thais
Marissens, Gertjan
Hoebeek, Freek E
eurUS.brain group

Editors

Advisors

Supervisors

Document Type

Article

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License

taverne

Abstract

The thalamic nuclei develop before a viable preterm age. GABAergic neuronal migration is especially active in the third trimester. Thalamic axons meet cortical axons during subplate activation and create the definitive cortical plate in the second and third trimesters. Default higher-order cortical driver connections to the thalamus are then replaced by the maturing sensory networks, in a process that is driven by first-order thalamic neurons. Surface electroencephalographic activity, generated first in the subplate and later in the cortical plate, gradually show oscillations based on the interaction of the cortex with thalamus, which is controlled by the thalamic reticular nucleus. In viable newborn infants, in addition to sensorimotor networks, the thalamus already contributes to visual, auditory, and pain processing, and to arousal and sleep. Isolated thalamic lesions may present as clinical seizures. In addition to asphyxia and stroke, infection and network injury are also common. Cranial ultrasound can be used to classify neonatal thalamic injuries based on functional parcelling of the mature thalamus. We provide ample illustration and a detailed description of the impact of neonatal focal thalamic injury on neurological development, and discuss the potential for neuroprotection based on thalamocortical plasticity.

Keywords

Humans, Thalamus/diagnostic imaging, Infant, Newborn, Taverne, Pediatrics, Perinatology, and Child Health, Developmental Neuroscience, Clinical Neurology, Journal Article, Review

Citation

Govaert, P, Arena, R, Dudink, J, Steggerda, S, Agut, T, Marissens, G, Hoebeek, F & eurUS.brain group 2025, 'Developmental anatomy of the thalamus, perinatal lesions, and neurological development', Developmental Medicine and Child Neurology, vol. 67, no. 1, pp. 15-34. https://doi.org/10.1111/dmcn.15992