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Graphene oxide induces apoptotic cell death in endothelial cells by activating autophagy via calcium-dependent phosphorylation of c-Jun N-terminal kinases

机译:通过通过C-JUM N-末端激酶的钙依赖性磷酸化激活自噬诱导内皮细胞中的氧化烯氧化物在内皮细胞中诱导凋亡细胞死亡

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摘要

Despite the rapid expansion of the biomedical applications of graphene oxide (GO), safety issues related to GO, particularly with regard to its effects on vascular endothelial cells (ECs), have been poorly evaluated. To explore possible GO-mediated vasculature cytotoxicity and determine lateral GO size relevance, we constructed four types of GO: micrometer-sized GO (MGO; 1089.9 +/- 135.3 nm), submicrometer-sized GO (SGO; 390.2 +/- 51.4 nm), nanometer-sized GO (NGO; 65.5 +/- 16.3 nm), and graphene quantum dots (GQDs). All types but GQD showed a significant decrease in cellular viability in a dose-dependent manner. Notably, SGO or NGO, but not MGO, potently induced apoptosis while causing no detectable necrosis. Subsequently, SGO or NGO markedly induced autophagy through a process dependent on the c-Jun N-terminal kinase (JNK)-mediated phosphorylation of B-cell lymphoma 2 (Bcl-2), leading to the dissociation of Beclin-1 from the Beclin-1-Bcl-2 complex. Autophagy suppression attenuated the SGO- or NGO-induced apoptotic cell death of ECs, suggesting that SGO- or NGO-induced cytotoxicity is associated with autophagy. Moreover, SGO or NGO significantly induced increased intracellular calcium ion (Ca2+) levels. Intracellular Ca2+ chelation with BAPTA-AM significantly attenuated microtubule-associated protein 1A/1B-light chain 3-II accumulation and JNK phosphorylation, resulting in reduced autophagy. Furthermore, we found that SGO or NGO induced Ca2+ release from the endoplasmic reticulum through the PLC beta 3/IP3/IP3R signaling axis. These results elucidate the mechanism underlying the size-dependent cytotoxicity of GOs in the vasculature and may facilitate the development of a safer biomedical application of GOs.
机译:尽管石墨烯氧化物(GO)的生物医学应用的快速扩张,但与其相关的安全问题,特别是关于其对血管内皮细胞(ECS)的影响,这一直很差。为了探索可能的血管系统细胞毒性并确定横向转向尺寸相关性,我们构建了四种类型的GO:微米尺寸的GO(MgO; 1089.9 +/-135.3 NM),子微米计大小的GO(Sgo; 390.2 +/- 51.4 nm ),纳米大小的GO(非政府组织; 65.5 +/- 16.3nm)和石墨烯量子点(GQDS)。所有类型但GQD以剂量依赖性方式显示细胞活力显着降低。值得注意的是,SgO或非政府组织,但不是MgO,似乎诱导的细胞凋亡,同时导致没有可检测的坏死。随后,SgO或Nogs通过依赖于C-JUN N-末端激酶(JNK)介导的B细胞淋巴瘤2(BCL-2)的磷酸化的方法明显诱导自噬,从而导致BECLIN-1从BENGLIN的解离-1-bcl-2复合物。自噬抑制减弱了ECS的Sgo或Ngo诱导的凋亡细胞死亡,表明SgO或NGO诱导的细胞毒性与自噬相关。此外,Sgo或非政府组织显着诱导细胞内钙离子(CA2 +)水平增加。细胞内Ca2 +螯合与Bapta-Am显着减弱的微管相关蛋白质1a / 1b-轻链3-II积累和JNK磷酸化,导致自噬减少。此外,我们发现SgO或NGO诱导Ca2 +通过PLCβ3/ IP3 / IP3R信号轴从内质网释放。这些结果阐明了脉管系统中GOS的大小依赖性细胞毒性的机制,并且可以促进GOS的更安全的生物医学应用。

著录项

  • 来源
    《Acta biomaterialia》 |2016年第null期|共13页
  • 作者单位

    Korea Res Inst Biosci &

    Biotechnol Biotherapeut Translat Res Ctr 125 Gwahak Ro Daejeon 305806;

    Catholic Univ Korea Coll Med Dept Obstet &

    Gynecol Seoul South Korea;

    Univ Sci &

    Technol Korea Res Inst Biosci &

    Biotechnol Harzards Monitoring BNT Res Ctr Major;

    Korea Res Inst Biosci &

    Biotechnol Biotherapeut Translat Res Ctr 125 Gwahak Ro Daejeon 305806;

    Korea Res Inst Biosci &

    Biotechnol Biotherapeut Translat Res Ctr 125 Gwahak Ro Daejeon 305806;

    Korea Res Inst Biosci &

    Biotechnol Biotherapeut Translat Res Ctr 125 Gwahak Ro Daejeon 305806;

    Korea Res Inst Biosci &

    Biotechnol Biotherapeut Translat Res Ctr 125 Gwahak Ro Daejeon 305806;

    Univ Sci &

    Technol Korea Res Inst Biosci &

    Biotechnol Harzards Monitoring BNT Res Ctr Major;

    Korea Res Inst Biosci &

    Biotechnol Biotherapeut Translat Res Ctr 125 Gwahak Ro Daejeon 305806;

    Korea Res Inst Biosci &

    Biotechnol Biotherapeut Translat Res Ctr 125 Gwahak Ro Daejeon 305806;

    Korea Res Inst Biosci &

    Biotechnol Biotherapeut Translat Res Ctr 125 Gwahak Ro Daejeon 305806;

    Korea Res Inst Biosci &

    Biotechnol Biotherapeut Translat Res Ctr 125 Gwahak Ro Daejeon 305806;

    Korea Res Inst Stand &

    Sci Ctr Nanosafety Metrol Daejeon South Korea;

    Korea Res Inst Biosci &

    Biotechnol Biotherapeut Translat Res Ctr 125 Gwahak Ro Daejeon 305806;

    Korea Res Inst Biosci &

    Biotechnol Biotherapeut Translat Res Ctr 125 Gwahak Ro Daejeon 305806;

    Korea Res Inst Biosci &

    Biotechnol Biotherapeut Translat Res Ctr 125 Gwahak Ro Daejeon 305806;

    Korea Res Inst Biosci &

    Biotechnol Biotherapeut Translat Res Ctr 125 Gwahak Ro Daejeon 305806;

  • 收录信息
  • 原文格式 PDF
  • 正文语种 eng
  • 中图分类 普通生物学;
  • 关键词

    Graphene oxide; Cytotoxicity; Autophagy; Calcium ion; Endothelial cell;

    机译:氧化石墨烯;细胞毒性;自噬;钙离子;内皮细胞;

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