Downregulation of matrix metalloproteinase-9 mRNA by valproic acid plays a role in inhibiting the shedding of MHC class I-related molecules A and B on the surface of human osteosarcoma cells

Yamanegi, Koji; Yamane, Junko; Kobayashi, Kenta; Ohyama, Hideki; Nakasho, Keiji; Yamada, Naoko; Hara, Masaki; Fukunaga, Satoru; Futani, Hiroyuki; Okamura, Haruki; Terada, Nobuyuki

doi:10.3892/or.2012.1981

Cited by 23 publications

(13 citation statements)

References 23 publications

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“…Soluble TL1AL72-L251 acts mainly in a paracrine manner to influence cells in the immune system, whereas the TL1AV84-L251 fragment acts via the autocrine pathway to induce the inhibition of the proliferation and apoptosis of endothelial cells (31). Our previous report indicated that VPA-treated OS cells do not exhibit increased ADAM17 gene transcription (32). Hence, the increase in the expression of soluble VEGI induced by HDAC inhibitors may involve a different mechanism of action than that mediating the shedding of membrane-bound VEGI.…”

Section: Discussionmentioning

confidence: 96%

Sodium valproate, a histone deacetylase inhibitor, modulates the vascular endothelial growth inhibitor-mediated cell death in human osteosarcoma and vascular endothelial cells

Yamanegi

Kawabe

Futani

et al. 2015

International Journal of Oncology

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The level of vascular endothelial growth inhibitor (VEGI) has been reported to be negatively associated with neovascularization in malignant tumors. The soluble form of VEGI is a potent anti-angiogenic factor due to its effects in inhibiting endothelial cell proliferation. This inhibition is mediated by death receptor 3 (DR3), which contains a death domain in its cytoplasmic tail capable of inducing apoptosis that can be subsequently blocked by decoy receptor 3 (DcR3). We investigated the effects of sodium valproate (VPA) and trichostatin A (TSA), histone deacetylase inhibitors, on the expression of VEGI and its related receptors in human osteosarcoma (OS) cell lines and human microvascular endothelial (HMVE) cells. Consequently, treatment with VPA and TSA increased the VEGI and DR3 expression levels without inducing DcR3 production in the OS cell lines. In contrast, the effect on the HMVE cells was limited, with no evidence of growth inhibition or an increase in the DR3 and DcR3 expression. However, VPA-induced soluble VEGI in the OS cell culture medium markedly inhibited the vascular tube formation of HMVE cells, while VEGI overexpression resulted in enhanced OS cell death. Taken together, the HDAC inhibitor has anti-angiogenesis and antitumor activities that mediate soluble VEGI/DR3-induced apoptosis via both autocrine and paracrine pathways. This study indicates that the HDAC inhibitor may be exploited as a therapeutic strategy modulating the soluble VEGI/DR3 pathway in osteosarcoma patients.

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Section: Discussionmentioning

confidence: 96%

Sodium valproate, a histone deacetylase inhibitor, modulates the vascular endothelial growth inhibitor-mediated cell death in human osteosarcoma and vascular endothelial cells

Yamanegi

Kawabe

Futani

et al. 2015

International Journal of Oncology

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“…Valproate treatment in osteosarcoma cells downregulates MMP9 expression and thereby enhances the expression of MICA and MICB ligands on the cell surface while downregulating the release of soluble forms of these ligands 79 . Moreover, the hypomethylating reagent hydralazine reduces the release of soluble form of MICA and MICB in conjunction with enhanced surface expression of these ligands 80 .…”

Section: Mechanisms Involved In the Secretion Of Snkg2dlmentioning

confidence: 99%

Secretory pathways generating immunosuppressive NKG2D ligands: New targets for therapeutic intervention

2014

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Natural Killer Group 2 member D (NKG2D) activating receptor, present on the surface of various immune cells, plays an important role in activating the anticancer immune response by their interaction with stress-inducible NKG2D ligands (NKG2DL) on transformed cells. However, cancer cells have developed numerous mechanisms to evade the immune system via the downregulation of NKG2DL from the cell surface, including the release of NKG2DL from the cell surface in a soluble form. Here, we review the mechanisms involved in the production of soluble NKG2DL (sNKG2DL) and the potential therapeutic strategies aiming to block the release of these immunosuppressive ligands. Therapeutically enabling the NKG2D-NKG2DL interaction would promote immunorecognition of malignant cells, thus abrogating disease progression.

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“…Our data collectively indicate that the release of sMICA is associated with tumor progression and metastasis in RCC. Shedding of NKG2D ligands, in particular MICA, from the cell surface represents a mechanism by which tumors escape NKG2D-mediated immunosurveillance (Kohga et al, 2012;Yamanegi et al, 2012). The production of sMICA has been found to impair NKG2D expression and NK cytotoxicity (Raffaghello et al, 2004).…”

Section: Discussionmentioning

confidence: 99%

Clinical Significance of Soluble Major Histocompatibility Complex Class I Chain-related A in Renal Cell Carcinoma Patients

Qiu

Zhao²,

Gang³

et al. 2013

Asian Pacific Journal of Cancer Prevention

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Downregulation of matrix metalloproteinase-9 mRNA by valproic acid plays a role in inhibiting the shedding of MHC class I-related molecules A and B on the surface of human osteosarcoma cells

Cited by 23 publications

References 23 publications

Sodium valproate, a histone deacetylase inhibitor, modulates the vascular endothelial growth inhibitor-mediated cell death in human osteosarcoma and vascular endothelial cells

Sodium valproate, a histone deacetylase inhibitor, modulates the vascular endothelial growth inhibitor-mediated cell death in human osteosarcoma and vascular endothelial cells

Secretory pathways generating immunosuppressive NKG2D ligands: New targets for therapeutic intervention

Clinical Significance of Soluble Major Histocompatibility Complex Class I Chain-related A in Renal Cell Carcinoma Patients

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