Emerging Concepts in Myeloid Cell Biology after Spinal Cord Injury

Hawthorne, Alicia L.; Popovich, Phillip G.

doi:10.1007/s13311-011-0032-6

Cited by 83 publications

(63 citation statements)

References 111 publications

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“…This is due, in part, to the release of numerous mediators from microglia and macrophages that exert cytotoxic effects on CNS cells that can lead to demyelination and neuronal loss Hawthorne and Popovich 2011;Ren and Young 2013). Nevertheless, these cells also produce a variety of factors that promote cell survival and tissue healing, and under certain circumstances, may lead to protective effects in the injured CNS Popovich and Longbrake 2008).…”

Section: Discussionmentioning

confidence: 99%

IL-4 drives microglia and macrophages toward a phenotype conducive for tissue repair and functional recovery after spinal cord injury

Francos-Quijorna

Amo-Aparicio

Martínez-Muriana

2016

Glia

156

135

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"This is the peer reviewed version of the following article: Francos-Quijorna I, Amo-Aparicio J, Martinez-Muriana A, López-Vales R. IL-4 drives microglia and macrophages toward a phenotype conducive for tissue repair andfunctional recovery after spinal cord injury. Glia. 2016 Dec;64(12):2079-2092 ABSTRACTMacrophages and microglia play a key role in the maintenance of nervous system homeostasis.However, upon different challenges, they can adopt several phenotypes, which may lead to divergent effects on tissue repair. After spinal cord injury (SCI), microglia and macrophages show predominantly pro-inflammatory activation and contribute to tissue damage. However, the factors that hamper their conversion to an anti-inflammatory state after SCI, or to other protective phenotypes, are poorly understood. Here, we show that IL-4 protein levels are undetectable in the spinal cord after contusion injury, which likely favors microglia and macrophages to remain in a pro-inflammatory state. We also demonstrate that a single delayed intraspinal injection of IL-4, 48hours after SCI, induces increased expression of M2 marker in microglia and macrophages. We also show that delayed injection of IL-4 leads to the appearance of resolution-phase macrophages, and that IL-4 enhances resolution of inflammation after SCI. Interestingly, we provide clear evidence that delayed administration of IL-4 markedly improves functional outcomes and reduces tissue damage after contusion injury. It is possible that these improvements are mediated by the presence of macrophages with M2 markers and resolution-phase macrophages. These data suggest that therapies aimed at increasing IL-4 levels could be valuable for the treatment of acute SCI, for which there are currently no effective treatments.

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Section: Discussionmentioning

confidence: 99%

IL-4 drives microglia and macrophages toward a phenotype conducive for tissue repair and functional recovery after spinal cord injury

Francos-Quijorna

Amo-Aparicio

Martínez-Muriana

2016

Glia

156

135

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“…Chemokine gradients are argued to persist indefinitely or to reoccur periodically, in order to explain the observation of infiltrated for long periods, namely about 6 weeks for neutrophils and over 6 months for monocytes, in the lesioned spinal cord, despite their short lifespan of roughly 5 days and 2 months, respectively (Pillay et al 2010;Hawthorne and Popovich 2011). The rapid and transient induction of several chemokines, for example, CCL2, CCL21 and CXCL10, in neurons has recently been shown to precede the induction of these chemokines in astrocytes, although the latter are considered the major source of chemokines after CNS injury (de Haas et al 2007).…”

Section: Altered Chemokine Expression Following Cns Injurymentioning

confidence: 99%

Chemokines in CNS injury and repair

2012

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Recruitment of inflammatory cells is known to drive the secondary damage cascades that are common to injuries of the central nervous system (CNS). Cell activation and infiltration to the injury site is orchestrated by changes in the expression of chemokines, the chemoattractive cytokines. Reducing the numbers of recruited inflammatory cells by the blocking of the action of chemokines has turned out be a promising approach to diminish neuroinflammation and to improve tissue preservation and neovascularization. In addition, several chemokines have been shown to be essential for stem/progenitor cell attraction, their survival, differentiation and cytokine production. Thus, chemokines might indirectly participate in remyelination, neovascularization and neuroprotection, which are important prerequisites for CNS repair after trauma. Moreover, CXCL12 promotes neurite outgrowth in the presence of growth inhibitory CNS myelin and enhances axonal sprouting after spinal cord injury (SCI). Here, we review current knowledge about the exciting functions of chemokines in CNS trauma, including SCI, traumatic brain injury and stroke. We identify common principles of chemokine action and discuss the potentials and challenges of therapeutic interventions with chemokines.

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“…In cases of MS or other demyelinating conditions, it has been shown that there exists a subset of microglia at the site of demyelination that can recruit oligodendrocyte precursor cells and phagocytose damaged neurons (Olah et al, 2011). In SCI, cells of the myeloid origin have been shown to play a role in intraspinal trafficking past the injury (Hawthorne and Popovich, 2011).…”

Section: Microglia In Disease and Agingmentioning

confidence: 99%

Impact of Prenatal Immune System Disturbances on Brain Development

Madhusudan

Vogel

Knuesel

2012

J Neuroimmune Pharmacol

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As research into various aging-associated neurodegenerative disorders reveals their immense pathophysiological complexity, the focus is currently shifting from studying changes in an advanced disease state to investigations involving pre-symptomatic periods, possible aberrations in early life, and even abnormalities in brain development. Recent studies on the etiology of schizophrenia and autism spectrum disorders revealed a profound impact of neurodevelopmental disturbances on disease predisposition, onset and progression. Here, we discuss how a prenatal immune challenge can affect the developing brain-with a selective focus on the impact on microglia, the brain's immune cells-and the implications for brain aging and its associated risk of developing Alzheimer's disease. ABSTRACTAs research into various aging-associated neurodegenerative disorders reveals their immense

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Emerging Concepts in Myeloid Cell Biology after Spinal Cord Injury

Cited by 83 publications

References 111 publications

IL-4 drives microglia and macrophages toward a phenotype conducive for tissue repair and functional recovery after spinal cord injury

IL-4 drives microglia and macrophages toward a phenotype conducive for tissue repair and functional recovery after spinal cord injury

Chemokines in CNS injury and repair

Impact of Prenatal Immune System Disturbances on Brain Development

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