Changes of nerve growth factor synthesis in nonneuronal cells in response to sciatic nerve transection.

Heumann, Rolf; Korsching, Sigrun I.; Bandtlow, Christine E.; Thoenen, H.

doi:10.1083/jcb.104.6.1623

Cited by 987 publications

(429 citation statements)

References 34 publications

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“…Indeed, the local administration of CNTF after transection of the facial nerve in newborn rats virtually completely prevented the degeneration of the motoneuron cell bodies (93). Moreover, in adult animals, in spite of the reduction of the CNTF mRNA after transection of the sciatic nerve, the CNTF -assigned biological activity in the peripheral part of the sciatic nerve undergoing Wallerian degeneration was still about 1000 times higher than the amount of " reactively" enhanced synthesis of NGF by non neuronal sciatic cells 1 week after lesion (35,97,98). Certainly, CNTF is not the sole factor responsible for motoneuron regeneration in peripheral nerves.…”

Section: Thoenen Hughes and Sendtnermentioning

confidence: 94%

“…The cloning of CNTF was the prerequisite for producing large quantities of recombinant CNTF (49,59,100) and for the determination of its developmental expression and cellular localization (20,27,86,94,97,100,101). These investigations demonstrated that CNTF is expressed postnatally in myelinating Schwann cells (27,86,97,100,101) and a subpopulation of type I astrocytes (20,101) in the CNS, that CNTF is a cytosolic molecule, and that the biological activity, e.g., in the adult sciatic nerve, is more than 10,000 _ times higher than that of (retrogradely) transported NGF in the rat sciatic nerve (35,97,98).…”

Section: Thoenen Hughes and Sendtnermentioning

confidence: 98%

See 1 more Smart Citation

Trophic Support of Motoneurons: Physiological, Pathophysiological, and Therapeutic Implications

Thoenen¹,

Hughes²,

Sendtner³

1993

Experimental Neurology

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Section: Thoenen Hughes and Sendtnermentioning

confidence: 94%

Section: Thoenen Hughes and Sendtnermentioning

confidence: 98%

Trophic Support of Motoneurons: Physiological, Pathophysiological, and Therapeutic Implications

Thoenen¹,

Hughes²,

Sendtner³

1993

Experimental Neurology

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“…NGF levels were increased (Heumann et al 1987) and NT-3 levels were decreased (Cai et al 1998) following sciatic crush injury. In addition, total neurotrophic support appears to be more important in the survival and maintenance of peripheral neurons than the influence of any one neurotrophin (Zhou et al 1999).…”

Section: Ngf and Nt-3 Protein In Peripheral Tissues Following Denervamentioning

confidence: 95%

Regulation of NGF and NT-3 protein expression in peripheral targets by sympathetic input

2007

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Nerve growth factor (NGF) and neurotrophin-3 (NT-3) are target-derived proteins that regulate innervating sympathetic neurons. Here, we used western blot analysis to investigate changes in NGF and NT-3 protein in several peripheral tissues following loss of sympathetic input. Following removal of the superior cervical ganglion (SCG), large molecular weight (MW) NGF species, including proNGF-A, were increased in distal intracranial SCG targets, such as pineal gland and extracerebral blood vessels (bv). Mature NGF was a minor species in these tissues and unchanged following sympathectomy. Large MW NGF species also were increased when sympathectomy was followed by in vivo NGF administration. Mature NT-3, which was abundant in controls, was significantly decreased in these targets following sympathetic denervation. The decrease in mature NT-3 was enhanced following NGF administration. The trigeminal ganglion, which provides sensory input to these targets, showed increased NGF, but decreased NT-3, in these treatments, demonstrating that decreased NT-3 at the targets did not result from enhanced NT-3 uptake. Unlike pineal gland and extracerebral bv, the external carotid artery, an extracranial proximal SCG target, showed no change in NGF following denervation, and mature NT-3 was significantly increased. Following NGF administration, NT-3 was significantly decreased. We provide evidence for sympathetic regulation of NGF and NT-3 in peripheral targets and that elevated NGF can depress NT-3. The differential response in distal and proximal adult targets is consistent with the idea that neurons innervating proximal and distal targets may serve different roles in regulating neurotrophin protein. In addition, we conclude that previous ELISA results showing increased NGF protein following sympathetic denervation may have resulted from increases in large MW species, rather than an increase in mature NGF.

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“…This is reflected by the high ratio of NGF to mRNA NGF , in contrast to densely innervated peripheral organs, which bave NGF levels similar to those in the sciatic nerve . Tbe high NGF levels in the sciatic nerve result predominantly from NGF transported retrogradely from peripheral target tissues (Korsching and Thoenen , 1983b;Heumann et al, 1987). However, after transection of the sciatic nerve, local synthesis by nonneuronal cells increases up to 15-fold both proximally and distally to tbe transection site.…”

Section: Nonneuronal Ceusmentioning

confidence: 99%

“…However, the amount of tissue is too small to replace fully the interrupted supply from the periphery. In situ bybridization experiments demonstrated that after transection, all nonneuronal cells expressed mRNA NGF , and not just those ensheathing the NGF-responsive neurons Heumann et al , 1987). When pieces of rat sciatic were brought ioto culture, the mRNA NGF levels first increased to a maximum after 8 hr, and then dropped to lower levels between 12 and 24 hr, just as they do in vivo (Heumann er al.…”

Section: Nonneuronal Ceusmentioning

confidence: 99%

Nerve growth factor: Cellular localization and regulation of synthesis

et al. 1988

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SUMMARY1. The role of nerve growth facta T (NGF) as aretrograde messenger between peripheral target tissues and innervating sympathetic and neural crest·derived sensory neurons is supported by the observations that (a) the interruption of retrograde axonal transport has the same effects as the neutralization of endogenous NGF by anti-NGF antibodies and (b) the dose correlation between tbe density of innervation by fibers of NGF-responsive neurons and the levels of NGF and mRNA NGF in their target organs.2. In situ hybridization experiments have demonstrated that a great variety of cells in the projection fi eld or NGP-responsive neurons is synthesizing NGF, among them epithelial cells, smooth musd e cells, tibroblasts, and Schwann cells.3. The temporal correlation between the growth of trigeminal sensory tibers ioto the whisker pad of the mouse and the commencement of NGF synthesis initially suggested a causal relationsh ip between these two events. However, in chick embryos rendered aneural by prior removal of the neural tube or the neural crest, it was shown that the onsel of NGF synthesis in the periphery is independent of neurons, and is controlled by an endogenous "dock" whose regulatory mechanism remains to be established. 4. A comparison between NGF synthesis in the nonneuronal cells of the newborn rat sciatic nerve and that in the adult sciatic nerve after lesion provided evidence for the important regulatory role played by a secretory product of I Max-Planck.Instilute Cor Psychialry, Oeparlmeol of Neu rochemi$uy, 0-8033 Marti nsricd, FRQ. 2To whom oorrespondence should be addressed.

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Changes of nerve growth factor synthesis in nonneuronal cells in response to sciatic nerve transection.

Cited by 987 publications

References 34 publications

Trophic Support of Motoneurons: Physiological, Pathophysiological, and Therapeutic Implications

Trophic Support of Motoneurons: Physiological, Pathophysiological, and Therapeutic Implications

Regulation of NGF and NT-3 protein expression in peripheral targets by sympathetic input

Nerve growth factor: Cellular localization and regulation of synthesis

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