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Discovery and mechanisms of host defense to oncogenesis: targeting the beta-defensin-1 peptide as a natural tumor inhibitor

机译:宿主防御的发现和机制致癌:靶向β-防御素-1肽作为天然肿瘤抑制剂

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摘要

Human beta-defensin-1 (hBD-1) is one of a number of small cationic host-defense peptides. Besides its well-known broad-spectrum antimicrobial function, hBD-1 has recently been identified as a chromosome 8p tumor-suppressor gene. The role of hBD-1 in modulating the host immune response to oncogenesis, associated with cell signaling and potential therapeutic applications, has become increasingly appreciated over time. In this study, multiple approaches were used to illustrate hBD-1 anti-tumor activities. Results demonstrate that hBD-1 peptide alters human epidermal growth factor receptor 2 (HER2) signal transduction and represses retroviral-mediated transgene expression in cancer cells. Loss of orthologous murine defense-1 (mBD1) in mice enhances nickel sulfate-induced leiomyosarcoma and causes mouse kidney cells to exhibit increased susceptibility to HPV-16 E6/7-induced neoplastic transformation. Furthermore, for the first time, a novel function of the urine-derived hBD-1 peptide was discovered to suppress bladder cancer growth and this may lead to future applications in the treatment of malignancy.
机译:人β-Defensin-1(HBD-1)是许多小阳离子宿主防御肽之一。除了其众所周知的广谱抗微生物功能外,HBD-1最近已被鉴定为染色体8P肿瘤抑制基因。 HBD-1在调节与细胞信号传导和潜在治疗应用相关的宿主免疫应答的宿主免疫应答的作用变得越来越感谢。在该研究中,使用多种方法来说明HBD-1抗肿瘤活性。结果表明,HBD-1肽改变人表皮生长因子受体2(HER2)信号转导并抑制癌细胞中的逆转录病毒介导的转基因表达。小鼠中的正交鼠防御-1(MBD1)的丧失增强了硫酸镍诱导的平滑肌肉瘤,并使小鼠肾细胞表现出对HPV-16 E6 / 7诱导的肿瘤转化的增加。此外,首次发现尿液衍生的HBD-1肽的新功能以抑制膀胱癌的生长,这可能导致未来的应用治疗恶性肿瘤。

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