Hostname: page-component-78c5997874-s2hrs Total loading time: 0 Render date: 2024-11-19T08:23:44.007Z Has data issue: false hasContentIssue false

Satellite glial cells: more than just ‘rings around the neuron’

Published online by Cambridge University Press:  06 July 2010

Menachem Hanani
Affiliation:
Hadassah-Hebrew University Medical Center, Jerusalem 91240, Israel
Rights & Permissions [Opens in a new window]

Abstract

Type
Editorial
Copyright
Copyright © Cambridge University Press 2010

When most neuroscientists discuss peripheral glia, it is usually about Scwhann cells. However, the peripheral nervous system includes a large number of ganglia – sensory and autonomic – which contain specialized glial cells termed ‘satellite glial cells’ (SGCs). (The enteric nervous system has its own specialized glial cells.) SGCs surround the neurons and form a tight envelope around them. In tissue sections SGCs appear like a ring around the neuron, which is mostly very thin and occasionally can even be invisible under the light microscope. These cells could be regarded as a special type of Schwann cells, but their development, and especially their unique organization with respect to the neurons, make them a distinct cell type. The collection of articles in this issue is not meant to be the definitive word on SGCs. We are currently several years away from having a comprehensive understanding of these cells. Rather, these articles can serve as an introduction to this topic and for pointing to potentially important research directions.

In the first article Pannese (Reference Pannese2010) describes the ultrastructure of SGCs. That this article will open this issue is appropriate at least for two reasons. First, Prof. Pannese has pioneered the research on SGCs, and his first article on this topic appeared over 50 years ago (Pannese, Reference Pannese1956). His 1981 monograph on SGCs is a must reading for anyone interested in this field, and is a classic of beauty, precision and clarity (Pannese, Reference Pannese1981). Second, structure is the best way to approach any study in biology because structure gives us important clues on function. Pannese's article emphasizes the unique arrangement of SGC as a tight sheath around the neurons, which results in the formation of a discrete unit consisting of a neuronal cell body and the SGCs surrounding it. This organization distinguishes SGCs from Scwhann cells and astrocytes, and has obvious functional implications, because even if the molecular and pharmacological properties of SGCs were similar to those of these other cell types, the functions of SGCs are very likely to be unique due to this special arrangement. Pannese also highlights the striking morphological changes that SGCs undergo after nerve injury, which include hypertrophy and the formation of bridges with other SGCs, which contain numerous newly formed gap junctions. Obviously, SGCs can sense injury-related changes in sensory neurons.

Garrett and Durham (Reference Garrett and Durham2010) investigated the postnatal temporal and spatial morphological changes in trigeminal ganglia that lead to formation of neuron–SGC units described by Pannese. They found that the expression of the inwardly rectifying K+ channel Kir4.1, the vesicle docking protein SNAP-25 and the neuropeptide CGRP correlate with the formation of these units.

Thippeswamy and his co-workers (e.g. Thippeswamy and Morris, Reference Thippeswamy and Morris1997) were among the first to report the presence of two-way neuron–SGC chemical signaling, which involves the secretion nitric oxide (NO) from neurons. This NO stimulates SGCs to produce growth factors that have a neuroprotective influence. In their article, Bradman et al. (Reference Bradman, Arora, Morris and Thippeswamy2010) summarize their own work and that of others that demonstrate the NO-dependent bidirectional communications between neurons and SGCs.

Ng et al. (Reference Ng, Wong and Wise2010) report that SGC–neuron interactions include influence on neurite retraction in a subpopulation of dorsal root ganglia (DRG) neurons in culture. This work suggests that non-neuronal cells (presumably SGCs) can control neuronal characteristics in sensory ganglia.

The pharmacology of SGCs is just beginning to be unraveled. Currently, the only thoroughly characterized receptor type in these cells is the purinergic P2, which responds to ATP and related nucleotides. Villa et al. (Reference Villa, Fumagalli, Verderio, Abbracchio and Ceruti2010) review the available information of the response of SGCs to ATP, and conclude that these cells display a variety of P2 receptors. It appears that SGCs can respond to ATP via both P2Y (metabotropic) and P2X (ionotropic) receptors, with the PY2 being dominant. Interestingly, there is evidence for plasticity of P2 receptors under injury.

Calcium waves have been proposed as an important means for information transmission in the astrocyte network, and are mediated by ATP release and subsequent activation of P2 purinergic receptors, and also by gap junctions. Because SGCs have P2 receptors and are also coupled by gap junctions, they have the potential to sustain calcium waves. This is now demonstrated by Suadicani et al. (Reference Suadicani, Cherkas, Zuckerman, Smith, Spray and Hanani2010) and serves as another evidence for the similarity between SGCs and astrocytes. This article also provides evidence that SGCs can release ATP, which is one of the main ‘gliotransmitters’.

Gu et al. (Reference Gu, Chen, Zhang, Li, Wang and Huang2010) summarize a series of studies done by L.Y. Huang and her co-workers. This series started with an innovative work showing that somata of sensory neurons can release substance P by Ca2+-dependent exocytosis (Huang and Neher, Reference Huang and Neher1996). Later work by Huang's group showed that these neurons can also release ATP, to which SGCs respond by releasing ATP and the cytokine TNFα. These mediators, in turn, act on the neurons, causing profound functional changes in them. Thus, there is an elaborate bidrectional communication between these two cell types, which can have far-reaching implications for signaling in sensory ganglia.

The article by Ohara et al. (Reference Ohara, Vit, Bhargava and Jasmin2010) describes how recent progress in the understanding of the properties of SGCs can help in developing pain therapies. It has been shown previously that nerve damage increases gap junction-mediated coupling between SGCs, which may contribute to chronic pain (Hanani et al., Reference Hanani, Huang, Cherkas, Ledda and Pannese2002). Here, Ohara et al. (Reference Ohara, Vit, Bhargava and Jasmin2010) demonstrate that knocking down the gap junction protein connexin 43 reduced pain in a rat model. They further report that SGCs can be exploited in other ways for pain therapeutic purposes.

Dubový et al. (Reference Dubový, Klusáková, Svíženská and Brázda2010) describe molecular changes that take place in SGCs in DRG following unilateral sciatic nerve injury, which induces neuropathic pain. They observed an increase in the level of the proinflammatory cytokine IL-6 and its receptor (IL-6R) in SGCs in the ipsilateral DRG. Interestingly, SGCs in the contralateral DRG also displayed augmented IL-6 (but not IL-6R). These findings indicate that SGCs in ganglia affected by the injury and also in ganglia not affected by it become activated by the injury. This suggests that SGCs are sensitive to both local signals and to systemic ones.

As mentioned above, SGCs are present not only in sensory ganglia. In fact, there is a large population of these cells in all sympathetic and parasympathetic ganglia, which are part of the peripheral autonomic nervous system. However, research on SGCs in these ganglia has lagged behind that on SGCs in sensory ganglia. The article by Hanani et al. (Reference Hanani, Caspi and Belzer2010) highlights some similarities between SGCs in sympathetic ganglia and those in sensory ganglia. Because neurons in autonomic ganglia (unlike neurons in sensory ganglia) receive synapses, SGCs in these ganglia are likely to possess some special characteristics. The potential influence of SGCs on synaptic transmission in autonomic ganglia is a promising avenue for future research.

I wish to thank the Chief Editor of Neuron Glia Biology Dr. Douglas Fields for his support throughout all the stages of the preparation of this special issue. Many thanks are due to the authors for their contributions and to the reviewers for valuable comments on the articles.

References

REFERENCES

Bradman, M.J., Arora, D.K., Morris, R. and Thippeswamy, T. (2010) How do the satellite glia cells of the dorsal root ganglia respond to stressed neurons? – nitric oxide saga from embryonic development to axonal injury in adulthood. Neuron Glia Biology.CrossRefGoogle ScholarPubMed
Dubový, P., Klusáková, I., Svíženská, I. and Brázda, V. (2010) Satellite glial cells express IL-6 and corresponding signal-transducing receptors in the dorsal root ganglia of rat neuropathic pain model. Neuron Glia Biology.CrossRefGoogle ScholarPubMed
Garrett, F.G. and Durham, P.L. (2010) Development of functional units within trigeminal ganglia correlates with increased expression of proteins involved in neuron-glia interactions. Neuron Glia Biology.Google Scholar
Gu, Y., Chen, Y., Zhang, X., Li, G.E., Wang, C.Y. and Huang, L.-Y.M. (2010) Neuronal soma-satellite glial cell interactions in sensory ganglia and the participation of purinergic receptors. Neuron Glia Biology.CrossRefGoogle ScholarPubMed
Hanani, M., Caspi, A. and Belzer, V. (2010) Peripheral inflammation augments gap junction-mediated coupling among satellite glial cells in mouse sympathetic ganglia. Neuron Glia Biology.Google Scholar
Hanani, M., Huang, T.Y., Cherkas, P.S., Ledda, M. and Pannese, E. (2002) Glial cell plasticity in sensory ganglia induced by nerve damage. Neuroscience 114, 279283.CrossRefGoogle ScholarPubMed
Huang, L.Y. and Neher, E. (1996) Ca2 +-dependent exocytosis in the somata of dorsal root ganglion neurons. Neuron 17, 135145.Google Scholar
Ng, K.-Y., Wong, Y.H. and Wise, H. (2010) The role of glial cells in influencing neurite extension by dorsal root ganglion cells. Neuron Glia Biology.Google Scholar
Ohara, P.T., Vit, J.-P., Bhargava, A. and Jasmin, L. (2010) Can satellite glial cells be therapeutic targets for pain control? Neuron Glia Biology.Google Scholar
Pannese, E. (1956) Research on the morphology of the perineuronal satellite cells in the spinal and sympathetic ganglia of mammals. I. Phase-contrast findings. Bollettino Societa Italiana Biologia Sperimentale 32, 7274.Google Scholar
Pannese, E. (1981) The satellite cells of the sensory ganglia. Advances in Anatomy Embryology and Cell Biology 65, 1111.Google Scholar
Pannese, E. (2010) The structure of the perineuronal sheath of satellite glial cells (SGCs) in sensory ganglia. Neuron Glia Biology.Google Scholar
Suadicani, S.O., Cherkas, P.S., Zuckerman, J., Smith, D.N., Spray, D.C. and Hanani, M. (2010) Bidirectional calcium signaling between satellite glial cells and neurons in cultured mouse trigeminal ganglia. Neuron Glia Biology.CrossRefGoogle ScholarPubMed
Thippeswamy, T. and Morris, R. (1997) Cyclic guanosine 3′,5′-monophosphate-mediated neuroprotection by nitric oxide in dissociated cultures of rat dorsal root ganglion neurones. Brain Research 774, 116122.CrossRefGoogle ScholarPubMed
Villa, G., Fumagalli, M., Verderio, C., Abbracchio, M.P. and Ceruti, S. (2010) Expression and contribution of satellite glial cells purinoceptors to pain transmission in sensory ganglia: an update. Neuron Glia Biology.CrossRefGoogle ScholarPubMed