Effect of a uniform partial denervation of the periphery on the peripheral and central vibrissal system in guinea pigs.

In some rodents, somatotopically organized architectonic patterns corresponding precisely to the arrangement of the vibrissae on the face are found in each of the central stations of the trigeminal (V) pathway. Two lines of evidence indicate that these architectonic patterns reflect the level of peripheral innervation. First, in normal mice, the sizes of the individual units within the cortical representation are proportional to the number of fibers supplying the corresponding vibrissal follicles. Second, complete surgical denervation of groups of vibrissae can severely attenuate the sizes of and alter the patterns of their central representations. However, previous studies in this system do not distinguish the effects of the absolute and the relative levels of peripheral innervation on central representations. To address this question, we have studied guinea pigs in which all vibrissae are partially deafferentated before birth by fetal exposure to antibodies against NGF. This approach reduces the absolute level of peripheral innervation in a graded way, and does so uniformly, without changing the pattern of vibrissal innervation. In the most severely affected animals, only 18% of the normal number of V ganglion neurons survive. The effect of this loss on the V system was assessed by comparing the peripheral and central components of the vibrissal system in normal and NGF-deprived animals. Peripheral fibers from the V ganglion neurons, including those to the vibrissae, are less reduced in number (50%) than expected. The number of peripheral fiber fascicles is also decreased. In contrast, neither the patterns nor the areas of the central representations in medulla and cortex differ from those of normal animals. We conclude that 18% of the normal number of V ganglion cells is sufficient to establish normal central architectonic patterns and the size of the central vibrissal representations is independent of the absolute magnitude of peripheral innervation. These observations are of relevance to understanding the role of NGF on the morphogenesis of central somatosensory pathways, the effects of "mismatches" between peripheral innervation, and the development of projections to central targets in the mammalian brain, and provide new data for understanding competitive interactions in the developing central and peripheral trigeminal system.