The Asparaginyl Endopeptidase Legumain Is Essential for Functional Recovery after Spinal Cord Injury in Adult Zebrafish

Ma, Liping; Shen, Yan‐Qin; Khatri, Harsh P.; Schachner, Melitta

doi:10.1371/journal.pone.0095098

Cited by 19 publications

(16 citation statements)

References 53 publications

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“…In fish, ependymin is involved in memory formation (61) and was shown to promote neurite outgrowth of retinal ganglion cells (62). We further identified legumain, which was demonstrated to be essential for recovery after spinal cord injury in adult zebrafish (63). Because CNS regeneration is superior in fish as compared with mammals, legumain detection might shed new light into mammalian nerve regeneration and will have to be examined functionally in subsequent follow‐up studies.…”

Section: Discussionmentioning

confidence: 99%

Secretome analysis of nerve repair mediating Schwann cells reveals Smad‐dependent trophism

et al. 2018

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Schwann cells promote nerve regeneration by adaptation of a regenerative phenotype referred to as repair mediating Schwann cell. Down‐regulation of myelin proteins, myelin clearance, formation of Bungner's bands, and secretion of trophic factors characterize this cell type. We have previously shown that the sphingosine‐1‐phosphate receptor agonist Fingolimod/FTY720P promotes the generation of this particular Schwann cell phenotype by activation of dedifferentiation markers and concomitant release of trophic factors resulting in enhanced neurite growth of dorsal root ganglion neurons. Despite its biomedical relevance, a detailed characterization of the corresponding Schwann cell secretóme is lacking, and the impact of FTY720P on enhancing neurite growth is not defined. Here, we applied a label‐free quantitative mass spectrometry approach to characterize the secretomes derived from primary neonatal and adult rat Schwann cells in response to FTY720P. We identified a large proportion of secreted proteins with a high overlap between the neonatal and adult Schwann cells, which can be associated with biologic processes such as development, axon growth, and regeneration. Moreover, FTY720P‐treated Schwann cells release proteins downstream of Smad signaling known to support neurite growth. Our results therefore uncover a network of trophic factors involved in glial‐mediated repair of the peripheral nervous system.—Schira, J., Heinen, A., Poschmann, G., Ziegler, B., Hartung, H.‐P., Stühler, K., Küry, P. Secretome analysis of nerve repair mediating Schwann cells reveals Smad‐dependent trophism. FASEB J. 33, 4703–4715 (2019). http://www.fasebj.org

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Section: Discussionmentioning

confidence: 99%

Secretome analysis of nerve repair mediating Schwann cells reveals Smad‐dependent trophism

et al. 2018

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“…The expression of AEP was increased in neurons of regenerative nuclei during the phase of axon regrowth/sprouting. Reducing the expression of AEP impaired axonal regeneration and locomotor recovery 24 .…”

Section: Introductionmentioning

confidence: 99%

Asparagine endopeptidase is an innovative therapeutic target for neurodegenerative diseases

Zhang

Xie

2016

Expert Opinion on Therapeutic Targets

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Introduction Asparagine endopeptidase (AEP) is a pH-dependent endolysosomal cysteine protease that cleaves its substrates after asparagine residues. Our most recent study identifies that it possesses the delta-secretase activity, and that it is implicated in numerous neurological diseases such as Alzheimer’s disease (AD) and stroke. Accumulating evidence supports that the inhibition of AEP exhibits beneficial effects for treating these devastating diseases. Areas covered Based on recent evidence, it is clear that AEP cleaves its substrate, such as amyloid precursor protein (APP), tau and SET, and plays a critical role in neuronal cell death in various neurodegenerative diseases and stroke. In this article, the basic biology of AEP, its knockout phenotypes in mouse models, its substrates in neurodegenerative diseases, and its small peptidyl inhibitors and prodrugs are discussed. In addition, we discuss the potential of AEP as a novel therapeutic target for neurodegenerative diseases. Expert opinion AEP plays a unique role in numerous biological processes, depending on both pH and context. Most striking is our most recent finding; that AEP is activated in an age-dependent manner and simultaneously cleaves both APP and tau, thereby unifying both major pathological events in AD. Thus, AEP acts as an innovative trigger for neurodegenerative diseases. Inhibition of AEP will provide a disease-modifying treatment for neurodegenerative diseases including AD.

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“…We also stained some preparations for HuC/D (elav3) expressed in neurons, neurofilament (NF), synaptic vesicle antigen 2 (SV2), glial fibrillary acidic protein (GFAP), and choline acetyltransferase (ChAT). We examined spinal cord histology for each of these lines at the three regions considered for studies carried on adult zebrafish: the 8th (V8), the 15th (V15), and the 24th vertebrae (V24) (Becker et al, ; Bormann et al, ; Schweitzer et al, ; Reimer et al, ; Hui et al, ; Gabriel et al, ; Guo et al, ; Kyriakatos et al, ; Yu et al, ; Ausborn et al, ; Dias et al, ; Fang et al, ; Goldshmit et al, ; Kuscha et al,; Lin et al, ; Ma et al, ; Ogai et al, ; Ampatzis et al, ; Yu and Schachner, ; Liu et al, ; Vajn et al, ).…”

Section: Introductionmentioning

confidence: 99%

Neuronal labeling patterns in the spinal cord of adult transgenic Zebrafish

Stil

Drapeau

2015

Developmental Neurobiology

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We describe neuronal patterns in the spinal cord of adult zebrafish. We studied the distribution of cells and processes in the three spinal regions reported in the literature: the 8th vertebra used as a transection injury site, the 15th vertebra mainly used for motor cell recordings and also for crush injury, and the 24th vertebra used to record motor nerve activity. We used well-known transgenic lines in which expression of green fluorescent protein (GFP) is driven by promoters to hb9 and isl1 in motoneurons, alx/chx10 and evx1 interneurons, ngn1 in sensory neurons and olig2 in oligodendrocytes, as well as antibodies for neurons (HuC/D, NF and SV2) and glia (GFAP). In isl1:GFP fish, GFP-positive processes are retained in the upper part of ventral horns and two subsets of cell bodies are observed. The pattern of the transgene in hb9:GFP adults is more diffuse and fibers are present broadly through the adult spinal cord. In alx/chx10 and evx1 lines we respectively observed two and three different GFP-positive populations. Finally, the ngn1:GFP transgene identifies dorsal root ganglion and some cells in dorsal horns. Interestingly some GFP positive fibers in ngn1:GFP fish are located around Mauthner axons and their density seems to be related to a rostrocaudal gradient. Many other cell types have been described in embryos and need to be studied in adults. Our findings provide a reference for further studies on spinal cytoarchitecture. Combined with physiological, histological and pathological/traumatic approaches, these studies will help clarify the operation of spinal locomotor circuits of adult zebrafish.

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The Asparaginyl Endopeptidase Legumain Is Essential for Functional Recovery after Spinal Cord Injury in Adult Zebrafish

Cited by 19 publications

References 53 publications

Secretome analysis of nerve repair mediating Schwann cells reveals Smad‐dependent trophism

Secretome analysis of nerve repair mediating Schwann cells reveals Smad‐dependent trophism

Asparagine endopeptidase is an innovative therapeutic target for neurodegenerative diseases

Neuronal labeling patterns in the spinal cord of adult transgenic Zebrafish

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