Disinhibition of Cathepsin C Caused by Cystatin F Deficiency Aggravates the Demyelination in a Cuprizone Model

Liang, Jianying; Li, Ning; Zhang, Yanli; Hou, Changyi; Yang, Xin; Shimizu, Takahiro; Wang, Xiaoyu; Ikenaka, Kazuhiro; Fan, Kai; Ma, Jin

doi:10.3389/fnmol.2016.00152

Cited by 29 publications

(31 citation statements)

References 45 publications

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“…Selective inactivated BMDC A 2A Rs or activated non-BMDC A 2A Rs led to systemic inflammatory response, and increased the expression of CF, accordingly activated microglia, whereas selective reconstitution reversed the above phenomenon. CF, a potent endogenous cysteine protease inhibitor, was substantially up-regulated in regions of white matter rarefaction that occurred in various demyelinating diseases of the CNS [32,33]. In this study, we found that BMDC A 2A Rs suppressed CF-mediated microglia activated and non-BMDC A 2A Rs promoted CF-mediated microglia activated, which was consistent with our previous research [16].…”

Section: Discussionsupporting

confidence: 92%

Adenosine A2A Receptors in Bone Marrow-Derived Cells Attenuate Cognitive Impairment in Mice After Chronic Hypoperfusion White Matter Injury

Ran

Yuan

Huang

et al. 2020

Transl. Stroke Res.

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The mechanism of cognitive dysfunction caused by ischemic white matter lesions is unclear. To explore the effect and mechanism of different cell-derived adenosine A2A receptor (A2AR) in cognitive impairment caused by chronic hypoperfusion white matter lesions (CHWMLs), we destroyed the bone marrow hematopoietic capacity of the recipient mice using radiation irradiation followed by establishing the selectively inactivated or reconstituted A2AR models with the transplanting bone marrow from global A2AR gene knockout or wild-type mice into wild-type or gene knockout mice, respectively. Then Morris Water Maze (MWM), ELISA, immunohistochemistry, and Bielschowsky silver staining were used to assess the effect and mechanism of the cognitive function in chronic cerebral blood flow hypoperfusion (CCH) model. Selectively reconstructing bone marrow-derived cells (BMDCs) A2AR (WT → KO group) and activated total adenosine A2AR with CGS21680 (CCH + CGS group) improved the cognitive related index. Activation of BMDC A2AR suppressed expression of inflammatory cytokines in peripheral blood and reduced the number of activated microglia cells co-localized with cystatin F in local brain, consequently inhibited white matter lesions. On the contrary, selective inactivation of adenosine A2AR (KO → WT group) and activation of non-BMDC A2AR with CGS21680 (KO → WT + CGS group) served the opposite effects. These results suggested that BMDC A2AR could inhibit white matter lesions and attenuate cognitive impairment after CHWMLs, whereas non-BMDC A2ARs aggravate cognitive impairment. The systemic inflammatory response and local activated microglia with cystatin F high expression were involved in the process of cognitive function recovery with BMDC A2AR. The overall trend is that BMDC A2ARs play a leading role.

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Section: Discussionsupporting

confidence: 92%

Adenosine A2A Receptors in Bone Marrow-Derived Cells Attenuate Cognitive Impairment in Mice After Chronic Hypoperfusion White Matter Injury

Ran

Yuan

Huang

et al. 2020

Transl. Stroke Res.

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“…Cystatin F is also implicated in several pathological processes. It has been suggested to play a role in multiple sclerosis during the acute phase of demyelination ( 29 , 30 ), in polycythemia vera, a myeloproliferative disorder characterized by an increased proliferation of cells of myeloid lineages ( 31 ) and in chronic fatigue syndrome ( 32 ). Higher expression of the inhibitor correlates with the inflammatory processes associated with lung disorders ( 33 ).…”

Section: Introductionmentioning

confidence: 99%

Cystatin F Affects Natural Killer Cell Cytotoxicity

et al. 2017

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Cystatin F is a cysteine peptidase inhibitor which, unlike other cystatin family members, is targeted to endosomal/lysosomal compartments. It is synthesized as an inactive disulfide-linked dimer which is then converted to an active monomer by proteolytic cleavage of 15 N-terminal residues. Cystatin F has been suggested to regulate the cytotoxicity of natural killer (NK) cells by inhibiting the major granzyme convertases, cathepsins C and H. To test this hypothesis, we prepared variants of cystatin F and analyzed their uptake, subcellular trafficking, and peptidase inhibition, as well as their impact on the cytotoxicity of NK-92 cells and primary NK cells. The N-glycosylation pattern is responsible for the secretion, uptake, and subcellular sorting of cystatin F in HeLa and Hek293 cells, whereas the legumain binding site had no effect on these processes. Active, N-terminally truncated, monomeric cystatin F can also be internalized by recipient cells and targeted to endo/lysosomes, affecting also cells lacking the activating peptidase. Cystatin F mutants capable of cell internalization and trafficking through the endo/lysosomal pathway significantly decreased cathepsin C and H activities, both in situ, following transfection and in trans, using conditioned media. Further, incubation of IL-2 stimulated NK-92 and primary NK cells with full-length and N-terminally truncated cystatin F mutants led to suppression of their granule-mediated cytotoxicity. This effect was most significant with the N-terminally truncated mutants. These results suggest that cystatin F can be an important mediator within tumor microenvironment affecting the cytotoxicity of NK cells and consequently antitumor immune response.

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“…We discovered that the Plp1 ‐over‐expressing mouse line ( Plp 4e/− ) and cuprizone mouse model showed worsened symptoms in our previous studies when CysF expression was eliminated, indicating that CysF has supporting role in the demyelinating mouse models which do not show hematopoietic cell infiltration in the lesions (Liang et al . ; Shimizu et al . ).…”

Section: Resultsmentioning

confidence: 99%

“…These results are consistent with previous data using Plp 4e/− and cuprizone model mice (Liang et al . ; Shimizu et al . ), suggesting that CatC plays a role during the early stage of inflammatory demyelinating disease.…”

Section: Resultsmentioning

confidence: 99%

“…A similar result was found in a cuprizone‐induced demyelination model, where the absence of the CysF gene and the resulting disinhibition of CatC aggravated the demyelination (Liang et al . ). CatC activity can be regulated by various mechanisms and is involved in inflammatory responses (Conus and Simon ); for example, the absence of the CysF gene increases the activity of CatC and enhances demyelination.…”

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confidence: 97%

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Cathepsin C modulates myelin oligodendrocyte glycoprotein‐induced experimental autoimmune encephalomyelitis

Durose

Shimizu

et al. 2018

Journal of Neurochemistry

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Multiple sclerosis (MS) is an autoimmune disease characterized by immune-mediated inflammation, which attacks the myelin sheath. MS pursues a relapsing and remitting course with varying intervals between symptoms. The main clinical pathological features include inflammation, myelin sheath destruction and plaque formation in the central nervous system (CNS). We previously reported that cystatin F (CysF) expression is induced in demyelinating lesions that are accompanied by active remyelination (referred to as shadow plaques) but is down-regulated in chronic demyelinated lesions (plaques) in the spinal cord of MS patients and in several murine models of demyelinating disease. CysF is a cathepsin protease inhibitor whose major target is cathepsin C (CatC), which is co-expressed in demyelinating regions in Plp mice, a model of chronic demyelination. Here, we report the time course of CatC and CysF expression and describe the symptoms in a mouse experimental autoimmune encephalomyelitis (EAE) model using CatC knockdown (KD) and CatC over-expression (OE) mice. In myelin oligodendrocyte glycoprotein (MOG)-EAE, CatC positive cells were found to infiltrate the CNS at an early stage prior to any clinical signs, in comparison to WT mice. CysF expression was not observed at this early stage, but appeared later within shadow plaques. CatC expression was found in chronic demyelinated lesions but was not associated with CysF expression, and CatCKD EAE mouse showed delayed demyelination. Whereas, CatCOE in microglia significantly increased severity of demyelination in the MOG-EAE model. Thus, these results demonstrate that CatC plays a major role in MOG-EAE.

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Disinhibition of Cathepsin C Caused by Cystatin F Deficiency Aggravates the Demyelination in a Cuprizone Model

Cited by 29 publications

References 45 publications

Adenosine A2A Receptors in Bone Marrow-Derived Cells Attenuate Cognitive Impairment in Mice After Chronic Hypoperfusion White Matter Injury

Adenosine A2A Receptors in Bone Marrow-Derived Cells Attenuate Cognitive Impairment in Mice After Chronic Hypoperfusion White Matter Injury

Cystatin F Affects Natural Killer Cell Cytotoxicity

Cathepsin C modulates myelin oligodendrocyte glycoprotein‐induced experimental autoimmune encephalomyelitis

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