首页> 美国卫生研究院文献>Cell Stress Chaperones >Retinoid- and sodium-butyrate– induced decrease in heat shock protein 70 membrane-positive tumor cells is associated with reduced sensitivity to natural killer cell lysis growth delay and altered growth morphology

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Retinoid- and sodium-butyrate– induced decrease in heat shock protein 70 membrane-positive tumor cells is associated with reduced sensitivity to natural killer cell lysis growth delay and altered growth morphology

机译：类维生素A和丁酸钠引起的热休克蛋白70膜阳性肿瘤细胞减少与对自然杀伤细胞裂解生长延迟和生长形态改变的敏感性降低有关

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Human tumors frequently present heat shock protein 70 (Hsp70) on their cell membranes, whereas corresponding normal tissues fail to do so. Therefore, an Hsp70 membrane-positive phenotype provided a tumor-specific marker. Moreover, membrane-bound Hsp70 provides a target structure for the cytolytic attack mediated by natural killer (NK) cells. Vitamin A derivatives 13-cis retinoic acid (13-RA) and all-trans retinoic acid (ATRA) and sodium-butyrate (SBU) are known for their redifferentiating capacity. Therefore, we asked the question whether loss in tumorigenicity might be associated with a reduced Hsp70 membrane expression. For our studies we used epithelial colon (CX+/CX−) and thyroid (ML-1) cancer cells, with initially different Hsp70 cell surface expression pattern. After treatment up to 7 weeks with freshly prepared 13-RA, ATRA, and SBU at nonlethal concentrations of 10 μM, 1 μM, and 0.5 mM, respectively, growth morphology, Hsp70 levels, and sensitivity toward Hsp70-specific NK cells were compared with that of untreated tumor cells. Significant growth delay was determined in CX+ tumor cells after 6 weeks treatment with 13-RA. Concomitantly, growth morphology changed from spheroid cell clusters to monolayers. Despite a weak increase in cytosolic Hsp70, the percentage of Hsp70 membrane-positive cells dropped significantly after repeated treatments with 13-RA and ATRA in CX+ and ML-1 but not in CX− tumor cells. Similar results were observed with SBU. Functionally, the decrease in Hsp70 membrane-positive CX+ and ML-1 cells correlated with a reduced sensitivity to lysis mediated by NK cells. In summary, redifferentiating agents predominantly affected Hsp70 membrane-positive tumors. The decrease in Hsp70 membrane positivity correlated with a lower sensitivity to NK lysis, growth delay, and altered growth morphology.

机译：人类肿瘤经常在其细胞膜上出现热激蛋白70（Hsp70），而相应的正常组织却没有这样做。因此，Hsp70膜阳性表型提供了肿瘤特异性标志物。此外，膜结合的Hsp70为自然杀伤（NK）细胞介导的溶细胞攻击提供了目标结构。维生素A衍生物13-顺式视黄酸（13-RA）和全反式视黄酸（ATRA）和丁酸钠（SBU）以其再分化能力而闻名。因此，我们提出了一个问题，即致癌性的丧失是否可能与Hsp70膜表达降低有关。在我们的研究中，我们使用了上皮结肠（CX + / CX-）和甲状腺（ML-1）癌细胞，它们最初具有不同的Hsp70细胞表面表达模式。在分别用非致死浓度分别为10μM，1μM和0.5 mM的新鲜制备的13-RA，ATRA和SBU处理长达7周后，将生长形态，Hsp70水平和对Hsp70特异性NK细胞的敏感性进行了比较。未经治疗的肿瘤细胞在用13-RA治疗6周后，在CX +肿瘤细胞中确定了显着的生长延迟。同时，生长形态从球状细胞簇变为单层。尽管胞质中Hsp70的增加微弱，但在CX +和ML-1中反复用13-RA和ATRA处理后，Hsp70膜阳性细胞的百分比显着下降，但在CX-肿瘤细胞中没有下降。使用SBU观察到相似的结果。从功能上讲，Hsp70膜阳性CX +和ML-1细胞的减少与对NK细胞介导的裂解敏感性降低有关。总之，再分化剂主要影响Hsp70膜阳性肿瘤。 Hsp70膜阳性的减少与对NK裂解，生长延迟和生长形态改变的敏感性降低有关。

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期刊名称 Cell Stress Chaperones
作者
Mathias Gehrmann; Johann Schönberger; Tanja Zilch; Lydia Rossbacher; Gerald Thonigs; Christoph Eilles; Gabriele Multhoff;
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年(卷),期 2005(10),2
年度 2005
页码 136–146
总页数 11
原文格式 PDF
正文语种
中图分类细胞生物学;
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专利

1. Dual function of membrane-bound heat shock protein 70 (Hsp70), Bag-4, and Hsp40: protection against radiation-induced effects and target structure for natural killer cells. [J] . Gehrmann M, Marienhagen J, Eichholtz Wirth H, Cell death and differentiation . 2005,第1期

机译：膜结合热休克蛋白70（Hsp70），Bag-4和Hsp40的双重功能：防止辐射诱导的效应和天然杀伤细胞的靶结构。
2. Targeting the testis-specific heat-shock protein 70-2 (HSP70-2) reduces cellular growth, migration, and invasion in renal cell carcinoma cells [J] . Singh Swarnendra, Suri Anil Tumour biology : . 2014,第12期

机译：靶向睾丸特异性热休克蛋白70-2（HSP70-2）可减少肾癌细胞中的细胞生长，迁移和侵袭
3. P67. Targeted natural killer (NK) cell based adoptive immunotherapy for the treatment of patients with non-small cell lung cancer (NSCLC) after radiochemotherapy (RCT) – clinical application of NK cells activated by heat shock protein 70 (Hsp70) [J] . HM Specht, J Pelzel, H Hautmann, Journal for ImmunoTherapy of Cancer . 2014,第S2期

机译：P67。基于靶向自然杀伤（NK）细胞的过继免疫疗法，用于治疗放化疗（RCT）后的非小细胞肺癌（NSCLC）患者–热休克蛋白70（Hsp70）激活的NK细胞的临床应用
4. 7.7: Presentation session: Poster session and reception: “Modeling the effect of melanoma tumor cell growth in the presence of natural killer cells” [C] . Wells Ann Proceedings of the 2010 Biomedical Sciences and Engineering Conference . 2010

机译：7.7：演讲环节：海报环节和接待：“在自然杀伤细胞的存在下模拟黑素瘤肿瘤细胞生长的效果”
5. Inhibition of heat-induced apoptosis in human tumor cells by heat shock protein 70 occurs upstream of mitochondrial membrane permeabilization through suppression ofc-Jun N-terminal kinase activity. [D] . Lachapelle, Guillaume. 2008

机译：通过抑制c-Jun N端激酶活性，热激蛋白70抑制人肿瘤细胞中的热诱导细胞凋亡发生在线粒体膜通透性的上游。
6. Inhibition of tumor growth in mice with severe combined immunodeficiency is mediated by heat shock protein 70 (Hsp70)-peptide–activated CD94 positive natural killer cells [O] . Christian Moser, Christin Schmidbauer, Ulrich Gürtler, 2002

机译：具有热休克蛋白70（Hsp70）-肽激活的CD94阳性自然杀伤细胞介导对具有严重联合免疫缺陷的小鼠的肿瘤生长的抑制
7. Retinoid- and sodium-butyrate– induced decrease in heat shock protein 70 membrane-positive tumor cells is associated with reduced sensitivity to natural killer cell lysis, growth delay, and altered growth morphology [O] . Gehrmann, Mathias, Schönberger, Johann, Zilch, Tanja, 2005

机译：类维生素A和丁酸钠引起的热休克蛋白70膜阳性肿瘤细胞减少与对自然杀伤细胞裂解的敏感性降低，生长延迟和生长形态改变有关

Retinoid- and sodium-butyrate– induced decrease in heat shock protein 70 membrane-positive tumor cells is associated with reduced sensitivity to natural killer cell lysis growth delay and altered growth morphology

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