Guided Antitumoural Drugs: (Imidazol-2-ylidene)(L)gold(I) Complexes Seeking Cellular Targets Controlled by the Nature of Ligand L

Three [1,3-diethyl-4-(p-methoxyphenyl)-5-(3,4,5-trimethoxyphenyl)imidazol-2-ylidene](L)gold(I) complexes, 4 a (L=Cl), 5 a (L=PPh₃), and 6 a (L=same N-heterocyclic carbene (NHC)), and their fluorescent [4-(anthracen-9-yl)-1,3-diethyl-5-phenylimidazol-2-ylidene](L)gold(I) analogues, 4 b , 5 b , and 6 b , respectively, were studied for their localisation and effects in cancer cells. Despite their identical NHC ligands, the last three accumulated in different compartments of melanoma cells, namely, the nucleus ( 4 b ), mitochondria ( 5 b ), or lysosomes ( 6 b ). Ligand L was also more decisive for the site of accumulation than the NHC ligand because the couples 4 a / 4 b , 5 a / 5 b , and 6 a / 6 b , carrying different NHC ligands, afforded similar results in cytotoxicity tests, and tests on targets typically found at their sites of accumulation, such as DNA in nuclei, reactive oxygen species and thioredoxin reductase in mitochondria, and lysosomal membranes. Regardless of the site of accumulation, cancer cell apoptosis was eventually induced. The concept of guiding a bioactive complex fragment to a particular subcellular target by secondary ligand L could reduce unwanted side effects.     

右半结肠癌完全结肠系膜切除术清扫肠系膜根部淋巴结效果观察

目的 探讨右半结肠癌行完全结肠系膜切除术（CME）清扫肠系膜根部淋巴结的临床疗效。方法 以2010年12月 至2012 年12 月行CME 的57 例右半结肠癌患者作为观察组,同期接受传统结肠癌根治术的99 例右半结肠癌患者作为对照组,对两组患者的淋巴结清扫数量、平均出血量、手术时间、住院时间、术后排气、排便时间、手术并发症、2年局部复发率及生存率等情况进行比较,初步评价CME 清扫肠系膜根部淋巴结的临床效果。结果 CME 组与对照组总淋巴结清扫数量分别为（22.6±2.8）、（14.6±2.7）枚,CME 组淋巴结清扫数量明显多于对照组（P＜0.05）;CME 组平均出血量为（167.4±20.8）ml,对照组为（205.4±19.3）ml,CME 组出血量少于对照组（P＜0.05）;两组的手术时间、住院时间、术后排气、排便时间比较差异均无统计学意义（均P＞0.05）;CME 组手术并发症发生率与对照组比较差异无统计学意义（P ＞0.05）;Ⅲ期患者CME 组2 年局部复发率38.2％、生存率88.2％,对照组分别为64.8％和68.5％,两组差异有统计学意义（均P＜0.05）。结论 右半结肠癌患者采用CME 清扫肠系膜根部 淋巴结是安全和有效的。     

去甲斑蝥素对人胰腺癌PANC-1 细胞凋亡作用的研究

目的 探讨去甲斑蝥素对人胰腺癌PANC-1细胞凋亡的作用及其机制。方法 将PANC-1 细胞株随机分为处理组 和对照组,处理组加入不同浓度的去甲斑蝥素培养24h后,CCK-8 法检测细胞增殖情况;流式细胞术分析细胞的凋亡情况;免疫印迹法检测细胞内质网应激和凋亡相关蛋白的表达;荧光定量PCR 技术检测细胞内质网应激和凋亡相关蛋白mRNA表达。结果 不同浓度去甲斑蝥素处理PANC-1细胞24h后,与对照组相比,能降低细胞的存活率并诱导其凋亡。与对照组相比,处理组中内质网应激和凋亡相关蛋白的表达水平均上调（均P＜0.05）,同时其mRNA 的表达水平亦均上调（均P＜0.05）。结论 去甲斑蝥素能明显抑制人胰腺癌PANC-1 细胞的生长并诱导其凋亡,并且具有浓度依赖性,这一作用可能是通过内质网应激介导的凋亡途径实现的。     

藤黄酸诱导肺癌细胞H1975凋亡的机制研究

目的 研究藤黄酸（GA）诱导人肺癌细胞H1975凋亡的分子机制,探讨氧自由基（ROS）和JNK信号通路在GA杀伤 肺癌细胞中的作用。方法 以人肺癌细胞H1975为研究对象,MTT法测定GA抑制细胞增殖的作用,Annexin V/PI 双染法测定细胞凋亡率,DCFH-DA 法测定ROS 含量,JC-1探针染色分析线粒体膜电位（MMP）,Western blot检测JNK 信号通路的激活和线粒体凋亡途径相关蛋白表达的变化。结果 GA 呈剂量依赖性抑制H1975细胞的增殖,各实验组细胞存活率与空白对照组比较,均有统计学差异（P＜0.05 或0.01）。1、2.5 和5滋mol/L GA 作用24h 后,细胞凋亡率分别为25.2%、51.8%和75.1%,剪切型凋亡相关蛋白cleaved caspase-9、cleaved caspase-3 和cleaved PARP 的表达随GA 浓度增高而显著增加,与空白对照组比较,均有统计学差异（P＜0.05或0.01）。GA 作用2h 后H1975细胞ROS 含量显著升高,磷酸化JNK（p-JNK）表达上调（P＜0.05或0.01）。GA 作用16h后各实验组细胞MMP 均明显降低（均P＜0.05）。GA 作用24h后实验组细胞线粒体凋亡途径相关蛋白Bax、Bak、Bik表达增加,而抗凋亡蛋白Bcl-2表达与空白对照组相比明显下降（P＜0.05 或0.01）。结论 GA 具有诱导H1975 细胞凋亡的作用,其可能机制是上调细胞内ROS含量,激活JNK 信号通路,进而引起MMP 降低和线粒体凋亡途径激活。     

Knockdown of 14-3-3ζ enhances radiosensitivity and radio-induced apoptosis in CD133+ liver cancer stem cells

14-3-3ζ is related to many cancer survival cellular processes. In a previous study, we showed that silencing 14-3-3ζ decreases the resistance of hepatocellular carcinoma (HCC) to chemotherapy. In this study, we investigated whether silencing 14-3-3ζ affects the radioresistance of cancer stem-like cells (CSCs) in HCC. Knockdown of 14-3-3ζ decreased cell viability and the number of spheres by reducing radioresistance in CSCs after γ-irradiation (IR). Furthermore, the levels of pro-apoptotic proteins were upregulated in CSCs via silencing 14-3-3ζ after IR. These results suggest that 14-3-3ζ knockdown enhances radio-induced apoptosis by reducing radioresistance in liver CSCs.     

Design of Enzymatically Cleavable Prodrugs of a Potent Platinum‐Containing Anticancer Agent

Using a versatile synthetic approach, a new class of potential ester prodrugs of highly potent, but systemically too toxic, platinum–acridine anticancer agents was generated. The new hybrids contain a hydroxyl group, which has been masked with a cleavable lipophilic acyl moiety. Both butanoic (butyric) and bulkier 2‐propanepentanoic (valproic) esters were introduced. The goals of this design were to improve the drug‐like properties (e.g., logD) and to reduce the systemic toxicity of the pharmacophore. Two distinct pathways by which the target compounds undergo effective ester hydrolysis, the proposed activating step, have been confirmed: platinum‐assisted, self‐immolative ester cleavage in a low‐chloride environment (LC‐ESMS, NMR spectroscopy) and enzymatic cleavage by human carboxylesterase‐2 (hCES‐2) (LC‐ESMS). The valproic acid ester derivatives are the first example of a metal‐containing agent cleavable by the prodrug‐converting enzyme. They show excellent chemical stability and reduced systemic toxicity. Preliminary results from screening in lung adenocarcinoma cell lines (A549, NCI‐H1435) suggest that the mechanism of the valproic esters may involve intracellular deesterification.     

Selective Uptake of Cylindrical Poly(2‐Oxazoline) Brush‐AntiDEC205 Antibody‐OVA Antigen Conjugates into DEC‐Positive Dendritic Cells and Subsequent T‐Cell Activation

To achieve specific cell targeting by various receptors for oligosaccharides or antibodies, a carrier must not be taken up by any of the very many different cells and needs functional groups prone to clean conjugation chemistry to derive well‐defined structures with a high biological specificity. A polymeric nanocarrier is presented that consists of a cylindrical brush polymer with poly‐2‐oxazoline side chains carrying an azide functional group on each of the many side chain ends. After click conjugation of dye and an anti‐DEC205 antibody to the periphery of the cylindrical brush polymer, antibody‐mediated specific binding and uptake into DEC205⁺‐positive mouse bone marrow‐derived dendritic cells (BMDC) was observed, whereas binding and uptake by DEC205^? negative BMDC and non‐DC was essentially absent. Additional conjugation of an antigen peptide yielded a multifunctional polymer structure with a much stronger antigen‐specific T‐cell stimulatory capacity of pretreated BMDC than application of antigen or polymer–antigen conjugate.     

Reinforcement of electrospun polycaprolacton scaffold using KIT-6 to improve mechanical and biological performance

Electrospinning has been extensively accepted as one of most important techniques for fabrication of scaffolds for bone tissue engineering. Polycaprolactone is one of the most applied electro-spinned scaffolds. Since low mechanical strength of polycaprolactone scaffold leads to the limitation of its applications, composition of polycaprolactone with ceramic particles is of great interest. Several studies have been conducted on fabrication and characterization of polycaprolactone nanocomposite scaffolds, but none of these researches has used mesoporous silica particles (KIT-6). In this project, a high-strength and bioactive nanocomposite scaffold has been developed which consists of polycaprolactone and mesoporous silica particles. Results showed that increase of KIT-6 particles percentages up to 5% leads to the enhancement of tensile strength of scaffold from 1.8 ± 0.2 to 2.9 ± 1.0 MPa. Although wettability of scaffolds in presence of particles was totally lower than pure PCL scaffold, but increase of particles percentages led to enhancement of wettability and water absorption of scaffolds. On the other hand presence of KIT-6 particles increased specific surface area and also bioactivity of scaffold was increased by enhancement of ion exchange between surface and simulated body fluid. Finally it was concluded that PCL-KIT-6 scaffolds are a suitable candidate for application in tissue engineering.     

An Activatable Polymeric Reporter for Near-Infrared Fluorescent and Photoacoustic Imaging of Invasive Cancer

Discriminative detection of invasive and noninvasive breast cancers is crucial for their effective treatment and prognosis. However, activatable probes able to do so in vivo are rare. Herein, we report an activatable polymeric reporter (P-Dex) that specifically turns on near-infrared (NIR) fluorescent and photoacoustic (PA) signals in response to the urokinase-type plasminogen activator (uPA) overexpressed in invasive breast cancer. P-Dex has a renal-clearable dextran backbone that is linked with a NIR dye caged with an uPA-cleavable peptide substrate. Such a molecular design allows P-Dex to passively target tumors, activate NIR fluorescence and PA signals to effectively distinguish invasive MDA-MB-231 breast cancer from noninvasive MCF-7 breast cancer, and ultimately undergo renal clearance to minimize the toxicity potential. Thus, this polymeric reporter holds great promise for the early detection of malignant breast cancer.     

新型丁烯内酯衍生物的设计合成及诱导胃癌细胞凋亡研究

开发了一条合成天然产物Uncinine的新方法,基于此设计合成了一系列新型的丁烯内酯衍生物.通过噻唑蓝(MTT)法评价了目标化合物对胃癌细胞的增殖抑制活性,分析了其构效关系.其中,3-吗啉甲基-4-(4-叔丁基苯基)亚基丁烯内酯(9l)对MGC803的IC50为2.9μmol/L,对胃癌细胞MGC803、HGC27以及SGC7901具有明显的选择性增殖抑制作用,而对正常的胃粘膜上皮细胞GES1具有较小的毒性.初步的作用机制研究表明,化合物9l诱导胃癌细胞MGC803凋亡依赖Caspase 9/3激活.