miR-924靶向TGM2抑制胃癌MGC803细胞增殖

探讨miR-924影响胃癌MGC803细胞增殖的分子机制。首先预测靶向结合组织型转谷氨酰胺酶(TGM2)的miRNAs,分析miR-924调控TGM2基因3′-UTR结合位点及两者的靶向结合。然后将miR-924导入MGC803细胞,检测其对TGM2表达及MGC803细胞增殖的影响,以及JAK3、STAT3及其磷酸化蛋白表达情况。发现miR-924与TGM2基因3′UTR的864-871位核苷酸靶向结合,并抑制MGC803细胞中TGM2 mRNA及蛋白质表达(P<0.05)。miR-924高表达后MGC803细胞的生长速度减慢,克隆形成能力降低;JAK3与STAT3蛋白磷酸化水平下调(P<0.05)。由此得出,miR-924通过靶向抑制TGM2表达,下调JAK3/STAT3通路活化,降低MGC803细胞增殖。

Studies on GA_3 Spraying Dosage for eui TGMS Rice Changxuan 3S in Its Hybrid Seed Production

[Objective] Changxuan 3S was thermo-sensitive genicmale sterile（TGMS）rice selected from irradiated seeds of Peiai 64S by 350 Gy^（60）Coγ-ray.The aim of the study was to confirm GA3 spraying dosage of Changxuan 3S with eui gene in its hybrid seed production.[Method] Changxuan 3S possessing eui gene and its parent Peiai 64S were chosen as materials.Comparison studies on sensitivity to GA3 in their hybrid seed production were carried out.[Result] The suitable stage for spraying GA3 in the hybrid seed production of Changxuan 3S was at 10% of panicles headed;The optimal dosage was 90 g/hm2 with 2 split sprayings,the first spraying of 45 g/hm2 at heading of 10% panicles and the second one of 45 g/hm2 on the following day.Under the condition of spraying GA3 at the rate of 90 g/hm2,the panicle neck exsertions of Changxuan 3S was ＋1.78 cm,and exserted stigma rate and seed setting rate of Changxuan 3S were 96.87% and 36.44%,being 21.46% and 16.33% more than those of Peiai 64S,respectively.The theoretical yield of ＂Changxuan 3S/9311＂ reached 2 931.90 kg/hm2,which was increased by 1 259.40 kg/hm2 comparing with ＂Peiai 64S/9311＂.[Conclusion] Compared with Peiai 64S,Changxuan 3S is more sensitive to GA3,which results in no or little using GA3 in seed production of Changxuan 3S.Moreover,Changxuan 3S showed higher yield potential than Peiai 64S.

TGM3在食管鳞状细胞癌发生、发展中的研究进展

食管鳞状细胞癌(esophageal squamous cell carcinoma,ESCC)是具有鳞状细胞分化的恶性上皮性肿瘤,镜下特征性表现为角质细胞样细胞存在细胞间桥和(或)角化。谷氨酰胺转氨酶3(transglutaminase 3,TGM3)是由TGM3基因编码的蛋白酶,属于催化蛋白谷氨酸残基与赖氨酸残基共价交联的谷氨酰胺转氨酶家族。TGM3主要表达于基层上部的复层鳞状上皮,是角质形成细胞末端分化的关键因子。近年有研究发现TGM3分子在ESCC中从食管正常鳞状上皮到癌变的病理过程中出现表达降低的变化,因此,有学者认为其可以作为ESCC预后的分子学标志物。提示TGM3分子与ESCC的发生、发展有十分密切的关系。现就近年对TGM3分子的结构特点、生物学功能及其在ESCC中的作用做一综述。

转谷氨酰胺酶3(TGM3)促进肝细胞肝癌(HCC)增殖侵袭的潜在机制及其临床意义

目的研究转谷氨酰胺酶3(transglutaminase 3,TGM3)在肝细胞肝癌(hepatocellular carcinoma,HCC)发生、发展过程中的作用及其预测HCC预后的临床价值。方法收集复旦大学附属中山医院HCC患者标本和临床资料进行分析,用qRT-PCR和Western blot方法检测28例HCC患者癌和癌旁TGM3表达差异,利用组织芯片染色结果及临床随访资料对92例HCC患者行Kaplan-Meier及Cox回归分析,探究TGM3不同表达水平对患者预后的影响。shRNA下调HCC细胞系Huh7和97H的TGM3表达水平,利用CCK-8法、克隆形成实验、Transwell小室实验、裸鼠皮下成瘤实验分析干扰后细胞增殖、迁移、侵袭及皮下成瘤能力的变化,Westernblot检测PI3K/AKT、MAPK/EPK、NF-κB信号通路、上皮间质转化(epithelial-mesenchymal transition,EMT)及凋亡相关蛋白的变化。结果TGM3在HCC中高表达,Kaplan-Meier生存分析表明TGM3高表达组的中位复发时间和中位生存期均较低表达组显著缩短(15.00个月vs.49.25个月,P<0.05;38.63个月vs.未达到;P<0.05);多因素Cox回归分析发现TGM3表达水平是HCC患者术后复发和死亡的独立预后因素(HR=2.31,P=0.029;HR=2.78,P=0.009)。体内外实验表明TGM3表达下调可以抑制HCC细胞的增殖、侵袭及皮下成瘤能力。TGM3下调使AKT、ERK、p65蛋白磷酸化水平降低,cleavedcaspase3水平增高,EMT相关指标E-钙黏素表达增加,N-钙黏素、纤维连接蛋白及波形蛋白表达下降。结论TGM3可能通过影响多条信号通路和EMT过程促进HCC的增殖和侵袭,并可作为HCC患者潜在的预后指标及治疗靶点。

Effect of Hypoxia on the Expression of a Subset of Proliferation Related Genes in IRE1 Knockdown U87 Glioma Cells

We have studied the expression of a subset of genes encoding important tumor growth related factors in U87 glioma cells with IRE1 (inositol requiring enzyme-1) knockdown as well as their hypoxic regulation. It was shown that the expression levels of activating transcription factor 6 (ATF6), clusterin (CLU), adhesion G protein-coupled receptor E5 (ADGRE5), transglutaminase?2, C polypeptide (TGM2), leukemia inhibitory factor (LIF), phosphoserine aminotransferase 1 (PSAT1), glyoxalase I (GLO1) and tetraspanin 13 (TSPAN13) are significantly down-regulated in glioma cells with the knockdown of IRE1 signaling enzyme. It was also shown that in glioma cells subjected to hypoxia, the expression levels of PSAT1, TSPAN13, EIF2AK3, and TGM2 genes were up-regulated, whereas the expression of ATF6 gene was down-regulated. At the same time, the expression levels of LIF, CLU, and ADGRE5 genes did not change in response to hypoxic treatment.?Furthermore, inhibition of IRE1, a key effector of an unfolded protein response pathway, modified the effect of hypoxia on the expression of most studied genes. Present study demonstrates that IRE1 knockdown down-regulated the expression of most studied genes and modified their hypoxic regulation and that these changes possibly contributed to the suppression of glioma growth in cells without IRE1 signaling enzyme function.

富水岩溶越江盾构隧道注浆材料试验与应用研究

考虑传统材料难以同时满足富水岩溶充填注浆与后续盾构掘进要求,研制一种环保型可控膏状注浆材料(TGM)。通过大样本室内试验,测试TGM材料的主要性能参数及其在岩溶水下浆材的特性,最后将研究成果成功应用于长沙地铁3号线水下岩溶越江盾构隧道注浆工程。研究结果表明:研制的TGM材料具有凝结时间快、屈服应力增长迅速、流动度高、析水率低、结石体收缩率小以及早期强度起效快,后期强度适中等特点;当注浆材料黏土原浆相对密度为1.30,水固比1∶1,添加剂a掺量1%,添加剂b掺量0.15%时,TGM材料的主要性能最优;岩溶水流速低于1 m/s,留存率可达75%以上,岩溶水养护条件下结石体完全压滤后12 h抗压强度可达2MPa,90 d抗压强度8 MPa,渗透系数低至10-7 cm/s,微观结构显示内部呈明显的块团状稳定结构。通过现场注浆应用表明,TGM材料能有效填充水下岩溶,浆液与岩溶充填物胶结紧密,渗透系数降至4.7×10^(-5) cm/s,后续盾构掘进过程无异常突变情况,盾构机姿态可控,注浆与掘进效果达到预期。可以预见,TGM是一种比较理想的水下岩溶越江盾构隧道注浆材料。

表皮型转谷氨酰胺酶在喉癌组织中的表达及临床意义

目的:探讨表皮型转谷氨酰胺酶(TGM3)在喉癌组织中的表达及其与各临床病理因素的关系。方法:采用流式细胞术检测50例喉癌组织和50例相应癌旁组织中的TGM3的表达,并以20例非喉癌患者喉部正常黏膜组织作对照。结果:①喉癌组织中TGM3蛋白的表达量及阳性表达率均明显低于癌旁组织及正常喉黏膜组织(P<0.05),癌旁组织及正常喉黏膜组织的表达无差别(P>0.05)。②TGM3蛋白的表达与喉癌组织中的淋巴结转移、临床分期、分化程度有相关性(P<0.05);与临床分型、肿瘤大小、年龄和性别无相关性(P>0.05)。结论:TGM3蛋白的低表达可促进喉癌的发生和发展,其蛋白检测可作为判断喉癌分化、浸润、转移、分期的重要指标。