Cellular Distribution of Gangliosides in the Developing Mouse Cerebellum: Analysis Using the Staggerer Mutant

Abstract

The distribution of cerebellar gangliosides was studied in staggerer (sg/sg) mutant mice, where the majority of granule cells die after completing their migration across the molecular layer. In addition, the external granule cell layer in (sg/sg) mice persists longer than in normal mice. Moreover, in the sg/sg cerebellum, Purkinje cells are significantly reduced in number, and almost none have tertiary branchlet spines. The loss of Purkinje cells and granule cells in sg/sg mice is accompanied by an early-onset reactive gliosis that continues through adulthood. By correlating changes in ganglioside composition with the well-documented histological events of cerebellar development in normal and sg/sg mice, we obtained strong evidence for a nonrandom cellular distribution of gangliosides. The sharpest reduction in the G_D1a content of sg/sg cerebellum occurred after 15 days of age, coincident with granule cell loss. G_T1a, on the other hand, was significantly reduced from 15 through 150 days in the sg/sg mice. G_D3 is a major ganglioside of the undifferentiated granule cell, but it becomes rapidly displaced by the more complex gangliosides with the onset of granule cell maturation. In the sg/sg mice, G_D3 persisted at abnormally high levels from 15 to 28 days and then accumulated through adulthood. These findings, and those from other cerebellar mouse mutants, suggest that G_D1a is enriched in granule cells and that G_T1a is enriched in Purkinje cells. Our findings also suggest that G_T1a is more concentrated in branchlet spines than in other regions of the Purkinje cell membrane. G_T1b appears to be enriched in both granule cells and Purkinje cells, whereas G_M1 appears to be enriched in myelin. Furthermore, the apparent persistence of the embryonic ganglioside G_D3 in sg/sg mice results from an early-onset reactive gliosis, together with a partial retardation in granule cell maturation. The accumulation of G_D3 beyond 28 days reflects the continued accretion of G_D3 in reactive glia.