β-Dystroglycan as a Target for MMP-9, in Response to Enhanced Neuronal Activity

Michaluk, Piotr; Kolodziej, Lukasz; Mioduszewska, Barbara; Wilczyński, Grzegorz M.; Dzwonek, Joanna; Jaworski, Jacek; Górecki, Dariusz C.; Ottersen, Ole Petter; Kaczmarek, Leszek

doi:10.1074/jbc.m700641200

Cited by 170 publications

(197 citation statements)

References 42 publications

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“…However, its fairly low enzymatic efficiency under our conditions might indicate that this event is finely modulated by conformational changes of b-DG. The recent discovery of a b-DG processing carried out by MMP-9 in response to enhanced neuronal activity (23,24) would strengthen the hypothesis that MMP-9 cooperates with the DG complex in the signal transduction.…”

Section: Discussionmentioning

confidence: 86%

“…Interestingly, b-DG has been proposed to be the first substrate digested by MMP-9 in response to enhanced neuronal activity, playing a role in synaptic plasticity, learning and memory (23,24). These data suggest that modulating the a-DG/b-DG interaction may have a precise functional role and that MMP-9 may be involved in this physiological process.…”

Section: Introductionmentioning

confidence: 88%

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Enzymatic processing of β‐dystroglycan recombinant ectodomain by MMP‐9: Identification of the main cleavage site

et al. 2009

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SummaryDystroglycan (DG) is a membrane receptor belonging to the complex of glycoproteins associated to dystrophin. DG is formed by two subunits, a-DG, a highly glycosylated extracellular matrix protein, and b-DG, a transmembrane protein. The two DG subunits interact through the C-terminal domain of a-DG and the N-terminal extracellular domain of b-DG in a noncovalent way. Such interaction is crucial to maintain the integrity of the plasma membrane. In some pathological conditions, the interaction between the two DG subunits may be disrupted by the proteolytic activity of gelatinases (i.e. MMP-9 and/or MMP-2) that removes a portion or the whole b-DG ectodomain producing a 30 kDa truncated form of b-DG. However, the molecular mechanism underlying this event is still unknown. In this study, we carried out proteolysis of the recombinant extracellular domain of b-DG, b-DG(654-750) with human MMP-9, characterizing the catalytic parameters of its cleavage. Furthermore, using a combined approach based on SDS-PAGE, MALDI-TOF and HPLC-ESI-IT mass spectrometry, we were able to identify one main MMP-9 cleavage site that is localized between the amino acids His-715 and Leu-716 of b-DG, and we analysed the proteolytic fragments of b-DG(654-750) produced by MMP-9 enzymatic activity.

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Section: Discussionmentioning

confidence: 86%

Section: Introductionmentioning

confidence: 88%

Enzymatic processing of β‐dystroglycan recombinant ectodomain by MMP‐9: Identification of the main cleavage site

et al. 2009

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“…On the other hand, some of our findings are not consistent with previous reports. For instance, a prominent increase in MMP-9 mRNA levels was observed in rats 2 h after a single 50 mg/kg PTZ dose (Rylski et al, 2009), and MMP-9 activity increased as early as 5 min after bicuculline treatment in mouse cortical cultures (Michaluk et al, 2007). More detailed examination of temporal changes and species differences in MMP-9 expression after single and repeated PTZ injection may help explain these discrepant results.…”

Section: Discussionmentioning

confidence: 87%

“…Repeated PTZ treatment increased protein and mRNA levels of BDNF in the hippocampi of kindled mice as described below, whereas protein levels of other substrates for MMP, such as laminin (Gu et al, 2005), ␤-dystroglycan (Michaluk et al, 2007), and NCAM (Hübschmann et al, 2005), did not change (Table 1). In fully kindled …”

Section: Mmp-9 Contributed To Ptz-induced Development Of Kindled Seizurementioning

confidence: 99%

Matrix Metalloproteinase-9 Contributes to Kindled Seizure Development in Pentylenetetrazole-Treated Mice by Converting Pro-BDNF to Mature BDNF in the Hippocampus

Mizoguchi¹,

Nakade²,

Terabe³

et al. 2011

J. Neurosci.

172

142

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(Ϫ/Ϫ) mice compared with wild-type mice, an observation that was accompanied by decreased hippocampal levels of mature brain-derived neurotrophic factor. Microinjecting the BDNF scavenger TrkB-Fc into the right ventricle before each PTZ treatment significantly suppressed the development of kindling in wild-type mice, whereas no effect was observed in MMP-9 (Ϫ/Ϫ) mice. On the other hand, bilateral injections of pro-BDNF into the hippocampal dentate gyrus significantly enhanced kindling in wild-type mice but not MMP-9 (Ϫ/Ϫ) mice. These findings suggest that MMP-9 is involved in the progression of behavioral phenotypes in kindled mice because of conversion of pro-BDNF to mature BDNF in the hippocampus.

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“…Generally, MMPs cleave a potentially large number of extracellular matrix proteins and other cell-surface or cell-adhesion molecules (Sternlicht and Werb 2001), many of which are expressed in hippocampus and are involved in synaptic plasticity and/or memory (Strekalova et al 2002;Dityatev and Schachner 2003). A recent study (Michaluk et al 2007) has identified ␤-dystroglycan (␤-dg) as an activity-dependent target of MMP-9 cleavage in cultured cortical neurons. ␤-dg is a transmembrane protein that links, via association with ␣-dystroglycan, proteins of the extracellular matrix with the actin cytoskeleton (Higginson and Winder 2005).…”

Section: Discussionmentioning

confidence: 99%

The extracellular protease matrix metalloproteinase-9 is activated by inhibitory avoidance learning and required for long-term memory

Nagy¹,

Bozdagi²,

Huntley³

2007

Learn. Mem.

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Matrix metalloproteinases (MMPs) are a family of extracellularly acting proteolytic enzymes with well-recognized roles in plasticity and remodeling of synaptic circuits during brain development and following brain injury. However, it is now becoming increasingly apparent that MMPs also function in normal, nonpathological synaptic plasticity of the kind that may underlie learning and memory. Here, we extend this idea by investigating the role and regulation of MMP-9 in an inhibitory avoidance (IA) learning and memory task. We demonstrate that following IA training, protein levels and proteolytic activity of MMP-9 become elevated in hippocampus by 6 h, peak at 12-24 h, then decline to baseline values by ∼72 h. When MMP function is abrogated by intrahippocampal infusion of a potent gelatinase (MMP-2 and MMP-9) inhibitor 3.5 h following IA training, a time prior to the onset of training-induced elevation in levels, IA memory retention is significantly diminished when tested 1-3 d later. Animals impaired at 3 d exhibit robust IA memory when retrained, suggesting that such impairment is not likely attributed to toxic or other deleterious effects that permanently disrupt hippocampal function. In anesthetized adult rats, the effective distance over which synaptic plasticity is impaired by a single intrahippocampal infusion of the MMP inhibitor of the kind that blocks IA memory is ∼1200 µm. Taken together, these data suggest that IA training induces a slowly emerging, but subsequently protracted period of MMP-mediated proteolysis critical for enabling long-lasting synaptic modification that underlies long-term memory consolidation.New information is learned and remembered through functional and structural modifications of synaptic connections (Bliss and Collingridge 1993;Rogan et al. 1997;Rioult-Pedotti et al. 1998Jorntell and Hansel 2006;Pastalkova et al. 2006;Whitlock et al. 2006). Several kinds of learning and memory tasks have been shown to drive changes in neurotransmitter receptor function and/or localization (Cammarota et al. 1995;Bevilaqua et al. 2005;Rumpel et al. 2005;Whitlock et al. 2006), as well as induce over time changes in synapse number or morphology (O'Malley et al. 2000;Geinisman et al. 2001;Eyre et al. 2003;Leuner et al. 2003;Maviel et al. 2004;Lamprecht et al. 2006;Rekart et al. 2007). These observations suggest that there must be learninginduced cellular mechanisms for coordinating functional and structural remodeling of synaptic connectivity to enable longterm memory, but there is little known about the molecules that could fulfill such a role.Learning-related, regulated extracellular proteolysis could be one mechanism for coordinating functional and structural synaptic plasticity, thereby enabling memory (Huang et al. 1996;Madani et al. 1999;Calabresi et al. 2000;Pawlak et al. 2002;Tamura et al. 2006). It is well-recognized that extracellular matrix (ECM) proteins as well synaptic cell adhesion molecules contribute to both functional and structural aspects of synaptic plasticity, are modified by l...

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β-Dystroglycan as a Target for MMP-9, in Response to Enhanced Neuronal Activity

Cited by 170 publications

References 42 publications

Enzymatic processing of β‐dystroglycan recombinant ectodomain by MMP‐9: Identification of the main cleavage site

Enzymatic processing of β‐dystroglycan recombinant ectodomain by MMP‐9: Identification of the main cleavage site

Matrix Metalloproteinase-9 Contributes to Kindled Seizure Development in Pentylenetetrazole-Treated Mice by Converting Pro-BDNF to Mature BDNF in the Hippocampus

The extracellular protease matrix metalloproteinase-9 is activated by inhibitory avoidance learning and required for long-term memory

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