Matrix metalloproteinase activity stimulates N-cadherin shedding and the soluble N-cadherin ectodomain promotes classical microglial activation

Conant, Katherine; Daniele, Stefano G.; Bozzelli, P. Lorenzo; Abdi, Tsion; Edwards, Amanda A.; Szklarczyk, Arek; Olchefske, India; Ottenheimer, David J.; Maguire‐Zeiss, Kathleen A.

doi:10.1186/s12974-017-0827-4

Cited by 21 publications

(20 citation statements)

References 78 publications

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“…The FGF-1 may interact with the fourth extracellular domain (EC4) of N-cadherin based on the fact that transfer of EC4 domain from N-cadherin onto E-cadherin reconstituted the invasive function of N-cadherin [ 21 ]. Other authors suggest the role of the cytoplasmic domain of N-cadherin [ 35 , 36 ] and soluble N-cadherin domain in regulating cell migration [ 37 ].…”

Section: Discussionmentioning

confidence: 99%

The inhibition of invasion of human melanoma cells through N-cadherin knock-down

Ciołczyk-Wierzbicka

Laidler

2018

Med Oncol

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N-cadherin seems to promote cell migration and invasion in many types of cancers. The object of this study is recognition of the possible role of N-cadherin and selected downstream protein kinases: PI3K, ERK1/2, and mTOR in cell invasion in malignant melanoma. Melanoma cells were transfected with the small interfering RNA (siRNA) that targets human N–cadherin gene (CDH2). Inhibitors LY294002 (PI3K), U0126 (ERK1/2), and everolimus (mTOR) were used to inhibit selected kinases of signalling pathways. In vitro cell invasion was studied using Matrigel and an analysis of matrix metalloproteinases MMP-2 and MMP-9 activity by gelatinase zymogram assay. Treatment of melanoma cell with either siRNA against N-cadherin or protein kinase inhibitors led to significantly decreased MMPs expression and activity, as well as diminished invasion. Both the current and the former results suggest that activation of PI3/AKT, mTOR, and ERK kinase, following N-cadherin expression, contributes not only to increased proliferation but also invasive potential of melanoma cells. The results also indicate that N-cadherin, as well as the studied kinases, should be considered as a potential target in melanoma therapy.

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Section: Discussionmentioning

confidence: 99%

The inhibition of invasion of human melanoma cells through N-cadherin knock-down

Ciołczyk-Wierzbicka

Laidler

2018

Med Oncol

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“…Proteolytic processing is an important transduction mechanism for type I classical cadherins, such as N-cad and epithelial cadherin (Marambaud et al, 2002;Maretzky et al, 2005;Reiss et al, 2005;Symowicz et al, 2007;Jang et al, 2011;Conant et al, 2017). ICD cleavage and subsequent nuclear translocation might also be a general characteristic of Pcdh-dependent signaling, as multiple studies have shown nuclear ICD localization for several Pcdhs (e.g., PcdhγC3, PcdhγC5, Pcdhα4, and Pcdh1α).…”

Section: Proteolytic Processing Of Pcdhs As a Potential Signaling Mecmentioning

confidence: 99%

Protocadherins at the Crossroad of Signaling Pathways

Pancho

Aerts

Mitsogiannis

et al. 2020

Front. Mol. Neurosci.

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Protocadherins (Pcdhs) are cell adhesion molecules that belong to the cadherin superfamily, and are subdivided into clustered (cPcdhs) and non-clustered Pcdhs (ncPcdhs) in vertebrates. In this review, we summarize their discovery, expression mechanisms, and roles in neuronal development and cancer, thereby highlighting the context-dependent nature of their actions. We furthermore provide an extensive overview of current structural knowledge, and its implications concerning extracellular interactions between cPcdhs, ncPcdhs, and classical cadherins. Next, we survey the known molecular action mechanisms of Pcdhs, emphasizing the regulatory functions of proteolytic processing and domain shedding. In addition, we outline the importance of Pcdh intracellular domains in the regulation of downstream signaling cascades, and we describe putative Pcdh interactions with intracellular molecules including components of the WAVE complex, the Wnt pathway, and apoptotic cascades. Our overview combines molecular interaction data from different contexts, such as neural development and cancer. This comprehensive approach reveals potential common Pcdh signaling hubs, and points out future directions for research. Functional studies of such key factors within the context of neural development might yield innovative insights into the molecular etiology of Pcdh-related neurodevelopmental disorders.

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“…The increased levels of MMP substrate cleavage fragments provide evidence for a role of aberrant MMP activity in the context of impaired cognition. We have previously shown that the MMP-cleaved ectodomain of the adhesion molecule N-cadherin promotes microglial activation (Conant et al, 2017) which may reflect an alternate pathway whereby HIV promotes MMPdependent gliosis.…”

Section: Discussionmentioning

confidence: 97%

HIV‐1 Tat promotes astrocytic release of CCL2 through MMP/PAR‐1 signaling

Bozzelli

Yin

Avdoshina

et al. 2019

Glia

Self Cite

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The HIV‐1 protein Tat is continually released by HIV‐infected cells despite effective combination antiretroviral therapies (cART). Tat promotes neurotoxicity through enhanced expression of proinflammatory molecules from resident and infiltrating immune cells. These molecules include matrix metalloproteinases (MMPs), which are pathologically elevated in HIV, and are known to drive central nervous system (CNS) injury in varied disease settings. A subset of MMPs can activate G‐protein coupled protease‐activated receptor 1 (PAR‐1), a receptor that is highly expressed on astrocytes. Although PAR‐1 expression is increased in HIV‐associated neurocognitive disorder (HAND), its role in HAND pathogenesis remains understudied. Herein, we explored Tat's ability to induce expression of the PAR‐1 agonists MMP‐3 and MMP‐13. We also investigated MMP/PAR‐1‐mediated release of CCL2, a chemokine that drives CNS entry of HIV infected monocytes and remains a significant correlate of cognitive dysfunction in the era of cART. Tat exposure significantly increased the expression of MMP‐3 and MMP‐13. These PAR‐1 agonists both stimulated the release of astrocytic CCL2, and both genetic knock‐out and pharmacological inhibition of PAR‐1 reduced CCL2 release. Moreover, in HIV‐infected post‐mortem brain tissue, within‐sample analyses revealed a correlation between levels of PAR‐1‐activating MMPs, PAR‐1, and CCL2. Collectively, these findings identify MMP/PAR‐1 signaling to be involved in the release of CCL2, which may underlie Tat‐induced neuroinflammation.

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Matrix metalloproteinase activity stimulates N-cadherin shedding and the soluble N-cadherin ectodomain promotes classical microglial activation

Cited by 21 publications

References 78 publications

The inhibition of invasion of human melanoma cells through N-cadherin knock-down

The inhibition of invasion of human melanoma cells through N-cadherin knock-down

Protocadherins at the Crossroad of Signaling Pathways

HIV‐1 Tat promotes astrocytic release of CCL2 through MMP/PAR‐1 signaling

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