首页> 外文期刊>Journal of Endodontics: Official Journal of American Association of Endodontists >Regulation of matrix metalloproteinase-2 production by cytokines and pharmacological agents in human pulp cell cultures.
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Regulation of matrix metalloproteinase-2 production by cytokines and pharmacological agents in human pulp cell cultures.

机译:在人类牙髓细胞培养物中细胞因子和药理剂对基质金属蛋白酶2产生的调节。

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Type IV matrix metalloproteinases (MMPs) are members of the family of MMPs and are thought to play an important role in degradation of extracellular components. Human pulp cells can secrete and produce these enzymes. Recent evidence shows that MMPs may play a role in pulpal inflammation. To date little is known regarding the regulation of MMPs in human pulp cell cultures. The purpose of this study was to determine the effects of cytokines (interleukin-1 and transforming growth factor-beta (TGF-beta), protein synthesis inhibitor cycloheximide (CD), and protein kinase C inhibitors (H7 and Go6976) on the secretion and production of MMPs by human pulp cell cultures using gelatin zymography. The main gelatinase secreted by human pulp cells migrated at 72 kDa and represented MMP-2. Minor gelatinolytic bands were also observed at 92 kDa regions that correspond to MMP-9. After an 8-day culture period TGF-beta, CD, H7, and Go6976 were found to depress MMP-2 production. The inhibition decreased in an order of CD > H7 > TGF-beta > Go6976. IL-1 was found to elevate MMP-2 production. Human pulp cells, however treated with either cytokines or pharmacological agents had no effect on the pattern of MMP-9 produced or secreted in either cell extracts or conditioned medium fractions. These observations suggest that the cytokines and pharmacological agents can regulate MMP-2 produced by human pulp cells. Inflammatory cytokines stimulate the production of elevated levels of MMP-2 and MMP-2 might play a role in pulpal inflammation. In addition agents that target protein synthesis or the protein kinase C pathway in human pulp cells inhibit MMP-2 production, and such inhibition may contribute to the pathogenesis of pulpal inflammation. Such inhibition might contribute to therapeutic efficacy.
机译:IV型基质金属蛋白酶(MMP)是MMP家族的成员,被认为在细胞外成分的降解中起重要作用。人牙髓细胞可以分泌并产生这些酶。最近的证据表明,MMP可能在牙髓炎症中起作用。迄今为止,关于人类浆细胞培养物中MMP的调控知之甚少。这项研究的目的是确定细胞因子(白介素-1和转化生长因子-β(TGF-β),蛋白质合成抑制剂环己酰亚胺(CD)和蛋白质激酶C抑制剂(H7和Go6976)对分泌和分泌的影响。用明胶酶谱法检测人牙髓细胞培养的MMPs,人牙髓细胞分泌的主要明胶酶以72kDa迁移并代表MMP-2,在与MMP-9对应的92kDa区域也观察到较小的明胶分解带。日培养期发现TGF-β,CD,H7和Go6976抑制MMP-2的产生,抑制作用以CD> H7>TGF-β> Go6976的顺序降低,IL-1被发现升高MMP-2。人牙髓细胞,无论用细胞因子或药理剂处理,对细胞提取物或条件培养基组分中产生或分泌的MMP-9的模式都没有影响,这些发现表明细胞因子和药理剂可以调节MMP。 -2由人类牙髓细胞产生。炎性细胞因子刺激产生高水平的MMP-2,而MMP-2可能在牙髓炎症中起作用。另外,靶向人牙髓细胞中蛋白质合成或蛋白激酶C途径的药物可抑制MMP-2的产生,并且这种抑制作用可能有助于牙髓炎症的发病机理。这种抑制可能有助于治疗功效。

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