(Fig.8).8). Together, these effects create a permissive environment for regeneration at the GSK1120212 lesion site and stimulating glia to generate new progenitors. The similarity to the Fgf-dependent mechanisms evident in zebrafish post-SCI, a proregenerative
model, is striking and suggests that distinct regulation of Fgf signaling mediates the differential regenerative capacity of the two systems. In both cases Inhibitors,research,lifescience,medical the major cell population that responds to the injury by proliferation and migration to the lesion site are the GFAP-positive glial cells. In addition to reactive astrocytes, diverse stem and progenitor cell populations are activated after SCI in rodents (Meletis et al. 2008; Petit et al. 2011). However, these cell populations are non-neurogenic under normal physiological or pathological conditions in the mammalian spinal cord. Inhibitors,research,lifescience,medical As a result, a glial scar composed of dense
processes is formed, which prevents neurite regeneration through the lesion in murine SCI. Our work shows that addition of exogenous Fgf2 after SCI in the mouse spinal cord has several important proregenerative effects. First, reactive proliferating astrocytes dedifferentiate to increase radial glia numbers at the lesion (Yang et al. 2011), second, the existing population of radial glia within the spinal cord start proliferating. In agreement with Inhibitors,research,lifescience,medical this result we show that Pax6-positive, Sox2-positive, and nestin-positive cells in PBS-injected animals remain low within the gray matter after SCI. In contrast, Fgf2-treated mice show a significant increase in cells that colabel with all three markers 2 weeks after injury. The change in marker expression is accompanied by changes in glial Inhibitors,research,lifescience,medical cell morphology and behavior. Fgf2 treatment shifts the glial population from cells with astroglial morphology toward cells with radial Inhibitors,research,lifescience,medical and bipolar morphology. Similarly, Fgf signaling changes glia morphology in the zebrafish spinal cord (Goldshmit et al. 2012) or in mammalian astrocytes in vitro (Imura et al. 2006; Goldshmit et al. 2012; Lichtenstein
et al. 2012). The radial and bipolar glia cells promote the formation of bridges that support axonal regeneration through the lesion. Furthermore, Fgf2 injection increases neurogenesis and neuronal learn more survival consistent with previous reports (Meijs et al. 2004). Importantly, we show functional improvement in behavioral assays 5 weeks post-SCI in Fgf2-treated mice, consistent with other studies in rodents (Lee et al. 1999; Rabchevsky et al. 1999). Figure 8 Model for fibroblast growth factor (Fgf)2-mediating glia bridges after spinal cord injury in mouse. Fgf2 increases neurogenesis and radial/progenitor cell marker expression and mediates polarized morphology of glial cells which form glia bridges that …