TY - JOUR
T1 - Ceramide is responsible for the failure of compensatory nerve sprouting in apolipoprotein e knock-out mice
AU - Maysinger, Dusica
AU - Holmes, Michael
AU - Han, Xianlin
AU - Epand, Richard M.
AU - Pertens, Evi
AU - Foerster, Anne
AU - Barlas, Cia
AU - Holtzman, David M.
AU - Diamond, Jack
PY - 2008/7/30
Y1 - 2008/7/30
N2 - Apolipoprotein E (apoE) is a key transporter of the cholesterol and phospholipids required formembranesynthesis and nerve growth.We now report a virtual absence in apoE knock-out (KO) mice of normal nerve growth factor (NGF)-driven compensatory sprouting of undamaged cutaneous nociceptive nerves. In contrast, NGF-independent regeneration of crushed axons was unaffected. Essentially similar results came from aged wild-type mice. In apoE KO mice, the endogenous sprouting stimulus was suspect, because NGF administration induced normal sprouting; nevertheless, NGF increased normally in denervated skin, transported normally in the axons, and led to phosphorylation of trkA, erk1, and erk2. However, sprouting was restored in apoE KO mice (although not in aged mice) by fumonisin B1, an inhibitor of ceramide synthesis.Ashotgun analysis revealed a wide array of changes in individual ceramide species inDRGneurons of apoE KO mice, and the changes for ceramide species OH_N15:0 made it a candidate inhibitor of sprouting (increased in apoE KO mice and normalized by fumonisin B1). Nevertheless, the unknown effects of individual ceramide species on sprouting, as well as the variability of their changed levels in apoE KO mice and how these were affected by fumonisin B1, support a different conclusion. We suggest that absence of apoE expression alters the balance among ceramide species to one that collectively inhibits compensatory sprouting, whereas fumonisin B1 establishes a new balance that allows sprouting. Nontoxic ceramide modulators might usefully promote sprouting and circuitry repair in neurodegenerative disorders in which ceramide species are perturbed, adding to the benefits of reducing ceramideinduced neuronal apoptosis.
AB - Apolipoprotein E (apoE) is a key transporter of the cholesterol and phospholipids required formembranesynthesis and nerve growth.We now report a virtual absence in apoE knock-out (KO) mice of normal nerve growth factor (NGF)-driven compensatory sprouting of undamaged cutaneous nociceptive nerves. In contrast, NGF-independent regeneration of crushed axons was unaffected. Essentially similar results came from aged wild-type mice. In apoE KO mice, the endogenous sprouting stimulus was suspect, because NGF administration induced normal sprouting; nevertheless, NGF increased normally in denervated skin, transported normally in the axons, and led to phosphorylation of trkA, erk1, and erk2. However, sprouting was restored in apoE KO mice (although not in aged mice) by fumonisin B1, an inhibitor of ceramide synthesis.Ashotgun analysis revealed a wide array of changes in individual ceramide species inDRGneurons of apoE KO mice, and the changes for ceramide species OH_N15:0 made it a candidate inhibitor of sprouting (increased in apoE KO mice and normalized by fumonisin B1). Nevertheless, the unknown effects of individual ceramide species on sprouting, as well as the variability of their changed levels in apoE KO mice and how these were affected by fumonisin B1, support a different conclusion. We suggest that absence of apoE expression alters the balance among ceramide species to one that collectively inhibits compensatory sprouting, whereas fumonisin B1 establishes a new balance that allows sprouting. Nontoxic ceramide modulators might usefully promote sprouting and circuitry repair in neurodegenerative disorders in which ceramide species are perturbed, adding to the benefits of reducing ceramideinduced neuronal apoptosis.
KW - Aging
KW - Alzheimer's disease
KW - ApoE
KW - Axonal regeneration
KW - Ceramide
KW - Cutaneous nerve
KW - NGF
KW - Nerve growth factor
KW - Nerve sprouting
UR - http://www.scopus.com/inward/record.url?scp=50349083801&partnerID=8YFLogxK
U2 - 10.1523/JNEUROSCI.1461-08.2008
DO - 10.1523/JNEUROSCI.1461-08.2008
M3 - Article
C2 - 18667621
AN - SCOPUS:50349083801
SN - 0270-6474
VL - 28
SP - 7891
EP - 7899
JO - Journal of Neuroscience
JF - Journal of Neuroscience
IS - 31
ER -