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利什曼原虫鞘脂对肿瘤生长的抗肿瘤作用及其对血管生成事件和炎症反应的调节

Antineoplastic impact of leishmanial sphingolipid in tumour growth with regulation of angiogenic event and inflammatory response.

作者信息

Das Subhadip, Chatterjee Nabanita, Bose Dipayan, Banerjee Somenath, Jha Tarun, Das Saha Krishna

机构信息

Cancer Biology & Inflammatory Disorder Division, CSIR-Indian Institute of Chemical Biology, 4 Raja S.C. Mullick Road, Kolkata, 700032, West Bengal, India.

出版信息

Apoptosis. 2015 Jun;20(6):869-82. doi: 10.1007/s10495-015-1121-5.

Abstract

Very often conventional therapy, i.e. chemotherapeutic treatment, develops resistance in cancer cells and fails to be effective against disease states. An alternative strategy or a new entity may resolve the problem. Interestingly, the microbial world has begun to be explored in medicinal research as a potential new source to deliver bio-active molecules such as sphingolipids for efficacious cancer treatment. A sphingolipid of microbial origin, especially from Leishmania donovani (LSPL), is a novel entity which may exert anti-cancer activity by regulating cellular growth. The present study reveals that among a range of cancer cells evaluated, LSPL-1 (a component of LSPL) reduces cell viability, annexin exposures and arrests cell cycle in B16F10 cells in a concentration and time dependent manner. Flowcytometric analysis showed that it alters mitochondrial membrane potential and generates a number of ROS positive melanoma cells. It activates p53 at serine anchor region via up-regulation of p21 subunit along with PUMA and NOXA. It also exerts activity in vivo by reducing tumor micro vessel and mitotic index while simultaneously improving the survival rate. The inflammatory responses including elevated level of cytokine-chemokine and increased expression of PCNA and F480 are subdued by LSPL-1 treatment in tumour bearing mice. Besides, it reduces the metastatic outburst of angiogenic factors like VEGF, Ang-2, and CD34 through the involvement of several growth promoting factors. These findings indicate that LSPL-1 may be explored as a potent entity against melanoma growth and the associated angiogenic promotion.

摘要

通常情况下,传统疗法,即化疗,会使癌细胞产生耐药性,对疾病状态无效。一种替代策略或新的药物可能会解决这个问题。有趣的是,微生物界已开始在医学研究中被探索,作为一种潜在的新来源,用于提供生物活性分子,如鞘脂,以有效治疗癌症。一种源自微生物的鞘脂,特别是来自杜氏利什曼原虫的鞘脂(LSPL),是一种新型药物,它可能通过调节细胞生长发挥抗癌活性。本研究表明,在一系列评估的癌细胞中,LSPL-1(LSPL的一种成分)以浓度和时间依赖的方式降低B16F10细胞的细胞活力、膜联蛋白暴露并使细胞周期停滞。流式细胞术分析表明,它改变线粒体膜电位并产生大量ROS阳性黑色素瘤细胞。它通过上调p21亚基以及PUMA和NOXA在丝氨酸锚定区域激活p53。它还通过减少肿瘤微血管和有丝分裂指数,同时提高存活率在体内发挥作用。LSPL-1处理可抑制荷瘤小鼠的炎症反应,包括细胞因子趋化因子水平升高以及PCNA和F480表达增加。此外,它通过多种生长促进因子的参与减少血管生成因子如VEGF、Ang-2和CD34的转移爆发。这些发现表明,LSPL-1可能被开发为一种对抗黑色素瘤生长及相关血管生成促进的有效药物。

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