Development of structural and functional connectivity in the thalamocortical somatosensory pathway in the wallaby.

Neuronal activity is implicated as a driving force in the development of sensory systems. In order for it to play a developmental role, however, the pathways involved must be capable of transmitting this activity. The relationship between afferent arrival, synapse formation and the onset of chemical neurotransmission has been examined using the advantageous model of a marsupial mammal, the wallaby (Macropus eugenii), to determine at what stage activity has the capacity to influence cortical development. It is known that thalamocortical afferents arrive in the somatosensory cortex on postnatal day (P)15 and that their growth cones reach to the base of the compact cell zone of the cortical plate. However, electronmicroscopy showed that thalamocortical synapses were absent at this stage. Glutamatergic responses were recorded in the cortex following stimulation of the thalamus in slices at this time but only in magnesium-free conditions. The responses were mediated entirely by N-methyl-d-aspartate (NMDA) receptors. From P28, responses could be recorded in normal magnesium and comprised a dominant NMDA-mediated component and a non-NMDA mediated component. At this time thalamocortical synapses were first identified and they were in the cortical plate. By P63 the non-NMDA-mediated component had increased relative to the NMDA-mediated component, and by P70 layer IV began to emerge and contained thalamocortical synapses. By P76 a fast non-NMDA-mediated peak dominated the response. This coincides with the appearance of cortical whisker-related patches and the onset in vivo of responses to peripheral stimulation of the whiskers.

Retinocollicular synaptogenesis and synaptic transmission during formation of the visual map in the superior colliculus of the wallaby (Macropus eugenii).

Spontaneous retinal activity has been implicated in the development of the topographic map in the superior colliculus (SC) but a direct demonstration that it reaches the colliculus is lacking. Here we investigate when the retinocollicular projection is capable of transmitting information from the retina in a marsupial mammal, the wallaby (Macropus eugenii). The projection develops postnatally, allowing in vivo analysis throughout development. Quantification of retinocollicular synaptogenesis has been combined with electrophysiology of the development and characteristics of retinocollicular transmission, including in vivo and in vitro recording in the same animals. Prior to postnatal day (P) 12-14 in vitro recording detected only presynaptic activity in retinal axons in the colliculus, in response to stimulation of the optic nerve. Postsynaptic responses, comprising both N-methyl-d-aspartate (NMDA) and non-NMDA responses, were first detected in vitro at P12-14 and retinal synapses were identified. In contrast, postsynaptic responses to optic nerve stimulation could not be detected in vivo until P39, around the time that retinal axons begin arborizing. Around this age density and numbers of total synapses began increasing in the retinorecipient layers of the colliculus. By P55-64, the numbers of retinal synapses had increased significantly and density and numbers of retinal and total synapses continued to increase up to P94-99. During this time the map is undergoing refinement and degenerating axons and synapses were present. The discrepancy between in vitro and in vivo onset of functional connections raises the question of when retinal activity reaches collicular cells in the intact, unanaesthetized animal and this will require investigation.

Developmental onset of functional activity in the wallaby whisker cortex in response to stimulation of the infraorbital nerve.

This study used the extrauterine development of a marsupial wallaby to investigate the onset of functional activity in the somatosensory pathway from the whiskers. In vivo recordings were made from the somatosensory cortex from postnatal day (P) 55 to P138, in response to electrical stimulation of the infraorbital nerve supplying the mystacial whiskers. Current source density analysis was used to localize the responses within the cortical depth. This was correlated with development of cortical lamination and the onset of whisker-related patches, as revealed by cytochrome oxidase. The earliest evoked activity occurred at P61, when layers 5 and 6 are present, but layer 4 has not yet developed. This activity showed no polarity reversal with depth, suggesting activity in thalamocortical afferents. By P72 synaptic responses were detected in developing layer 4 and cytochrome oxidase showed the first hint of segregation into whisker-related patches. These patches were clear by P86. The evoked response at this age showed synaptic activity first in layer 4 and then in deep layer 5/upper layer 6. With maturity, responses became longer lasting with a complex sequence of synaptic activity at different cortical depths. The onset of functional activity is coincident with development of layer 4 and the onset of whisker-related pattern formation. A similar coincidence is seen in the rat, despite the markedly different chronological timetable, suggesting similar developmental mechanisms may operate in both species.

Topography of functional subpopulations of neurons in the superior cervical ganglion of the rat.

This study describes the distribution patterns of neurons in the rat SCG that project to a number of spatially separated and functionally different target tissues. Fluorescent dyes were used to label retrogradely neurons that project to the pineal gland, iris, nictitating membrane, Müller's smooth muscle of the eyelid, submaxillary gland, thyroid gland, tongue, buccal mucosa, and skin in several areas of head and neck. The numbers of neurons in the various subpopulations were quantified and, in several instances, postganglionic nerve transection was used to correlate the topography of subpopulations with the exit site/s of their projections from the ganglion. Individual neurons were found to have very limited projection fields and contralateral innervation of bilateral targets appeared to be minimal. Neurons with specific functions or projection fields were not highly localised within the SCG, but there was a general rostrocaudal organisation of neurons with respect to the position of their targets along the rostrocaudal axis of the body and this was correlated with the exist sites of the neurons from the ganglion.

The impact of sexual dimorphism on neuron numbers in the superior cervical ganglion of the rat.

Other workers have reported a sexual dimorphism in the number of neurons that project from the rat superior cervical ganglion (SCG) via the internal carotid nerve (ICN). We have re-examined this situation by comparing ganglionic neuron numbers as well as the number of neurons labelled retrogradely from the iris and the pineal gland, in age-matched adult male and female rats. No significant dimorphism was seen in total cell numbers or in the cell populations supplying iris or pineal gland, although there was a trend towards more neurons in male animals. From evaluation of our results and the published data, we suggest that the variation in absolute numbers of neurons counted in the SCG is so wide, within genders, that any impact of gender differences on cell numbers is of little significance.

Effects of very early monocular and binocular enucleation on primary visual centers in the tammar wallaby (Macropus eugenii).

The role of retinal afferents and their binocular interactions in the development of mammalian primary visual centers has been studied in the marsupial wallaby. Monocular and binocular enucleation was performed prior to any retinal innervation of the visual centers. After monocular enucleation retinal projections were traced by horseradish peroxidase histochemistry and compared with those in normal animals and those during development. The topography of retinal projections to the superior colliculus and the dorsal lateral geniculate nucleus after monocular enucleation was determined by making retinal lesions and tracing the remaining projections with horseradish peroxidase. The position and nature of the filling defects in terminal label were compared with controls with similarly placed lesions. The superior colliculus and dorsal lateral geniculate nucleus ipsilateral to the remaining eye were shrunken. Projections to the ipsilateral superior colliculus, ipsilateral accessory optic nuclei, and ipsilateral suprachiasmatic nucleus, although enlarged, never approached the density contralaterally, as was also the case during normal development. The expanded projection in the ipsilateral superior colliculus came primarily from temporal and ventral retina. In the dorsal lateral geniculate nucleus, terminal bands and cellular laminae, although not identical to normal, did develop. During normal development overlap of afferents from the two eyes occurs in the binocular region. The decrease in volume of the nucleus ipsilateral to the remaining eye after monocular enucleation suggests that the monocular region disappears in the absence of appropriate input and the binocular region survives. Contralaterally there was no decrease in volume, compatible with this idea. The topography of retinal projections supports this interpretation. It was normal contralaterally while ipsilaterally it was appropriate for the normal binocular region. There was an expansion of the projection along the lines of projection in what would normally be binocular regions of the nucleus, where retinal afferents failed to segregate in the absence of binocular competition. After binocular enucleation the alpha and beta segments of the dorsal lateral geniculate nucleus were still recognizable but cell-sparse zones were absent, as was the characteristic orientation of primary dendrites of geniculocortical cells. There are rigid developmental constraints operating on the innervation of territory by retinal afferents from the two eyes, and many features of the mature pattern arise without binocular interactions during development.

Retinal projections to the superior colliculus and dorsal lateral geniculate nucleus in the tammar wallaby (Macropus eugenii): I. Normal topography.

The topography of retinal projections to the superior colliculus and dorsal lateral geniculate nucleus of a wallaby, the tammar (Macropus eugenii), was investigated by an anatomical method. Small laser lesions were made in the retinas of experimental animals, and the remaining retinal projections were visualized by means of horseradish-peroxidase histochemistry. The position of each lesion was correlated with the position of the filling defects in the terminal label. The whole of the retina projects to the contralateral superior colliculus. The nasal retina is represented caudally, and the temporal retina rostrally. The ventral retina is represented medially, and the dorsal retina laterally. There is a projection to the ipsilateral superior colliculus, but it is patchy and its topography could not be determined by this method. The retinotopic map in the contralateral dorsal lateral geniculate nucleus has the nasal retina represented rostrally and the temporal retina caudally in the nucleus. The dorsal retina is represented ventrally, and the ventral retina is represented dorsally. It appears that the whole of the retina projects contralaterally, and in addition the temporal retina projects ipsilaterally. The maps of visual space through the two eyes were shown to be in topographic register in the binocular region by making a deposit of HRP in the visual cortex. This resulted in a column of retrogradely labeled cells in the nucleus. This column crossed the laminae, which are innervated by the ipsilateral and contralateral eye at right angles.