Effects of tachyplesin and n-sodium butyrate on proliferation and gene expression of human gastric adenocarcinoma cell line BGC-823

瞄准：在增长和人的胃的腺癌房间线 BGC-823 的基因表示上调查 tachyplesin 和 n 钠丁酸盐的效果。方法：BGC-823 房间的增长上的 tachyplesin 和 n 钠丁酸盐的效果与尝试平底锅蓝色染料排除测试被决定并且他染色。房间周期上的 tachyplesin 和 n 钠丁酸盐的效果被流动血细胞计数检测。c-erbB-2， c-myc， p53 和 p16 的蛋白质层次被免疫细胞化学检验。结果：禁止的效果在 2.0 mg/L tachyplesin 和 2.0 mmol/L n 钠丁酸盐处理以后是类似的，细胞的生长的禁止的率分别地是 62.66% 和 60.19% ，并且各自的最大的有丝分裂的索引被 49.35% 和 51.69% 分别地减少。Tachyplesin 和 n 钠丁酸盐处理能显著地在 /G (1 ) 分阶段执行并且减少的 G (0 ) 增加房间的比例在 S 的比例阶段。当表示肿瘤铺平时， oncogene c-erbB-2， c-myc，和 mtp53 蛋白质的表示层次是下面调整的压制或基因 p16 蛋白质在有 tachyplesin 或 n 钠丁酸盐的处理以后是起来调整的。在有 1.0 mmol/L n 钠丁酸盐的联合的 1.0 mg/L tachyplesin 的效果比他们在改变房间周期分发和 c-erbB-2， c-myc， mtp53 和 p16 蛋白质的表示的单个处理显然优异。在联合处理以后的 BGC-823 房间的细胞的生长的禁止的率是 62.29% ，最大的有丝分裂的索引被 51.95% 减少。结论：肿瘤房间的区别 inducer 在肿瘤房间， oncogene 和肿瘤压制的关联词的表示或基因的增长上作为 n 钠丁酸盐有类似的效果的 Tachyplesin。它也在肿瘤房间的区别上有协同的效果。

The Effect of Sodium Nitrite on Induction of Apoptosis in Human Gastric Adenocarcinoma Epithelia (AGS) Cells

To examine the cytocidal effect of sodium nitrite on the cancer cell, we subjected human gastric adenocarcinoma epithelia (AGS) cells to various experimentation following exposure to sodium nitrite, and measured the resulting changes in the levels of cell death, lactate dehydrogenase (LDH) release, and caspase-3, -6, -8, and -9 activities. Our data revealed that, in AGS cells, treatment with ≥6.25 mM sodium nitrite for 8 h resulted in an obvious increase in cell death. LDH release was also markedly increased following sodium nitrite treatment, but at a concentration of ≥6.25 mM for 24 h. This increasing trend showed a positive correlation (r = 0.9564, P < 0.05). In addition, we detected pronounced increases in caspase activities with various concentrations of sodium nitrite: caspase-3 at ≥25 mM for 1 h, ≥12.5 mM for 3 h and 6 h;caspase-9 at 50 mM for 1 h and 3 h, and ≥6.25 mM for 6 h;and caspase-6 at 50 mM for 1 h and 3 h. We did not however, detect any observable increase in the activity of caspase-8 following sodium nitrite treatment at any concentration or for any duration of treatment in this study. This data demonstrates that, in AGS cells, higher concentrations or longer durations of treatment with sodium nitrite could exhibit a cytocidal effect, and that sodium nitrite could induce apoptosis via activation of the caspase-9, caspase-3 cascade (intrinsic pathway) and caspase-6.

Altered profiles of nuclear matrix proteins during the differentiation of human gastric mucous adenocarcinoma MGc80-3 cells

AIM: To find and identify specific nuclear matrix proteins associated with proliferation and differentiation of carcinoma cells, which will be potential markers for cancer diagnosis and targets in cancer therapy.METHODS: Nuclear matrix proteins were selectively extracted from MGc80-3 cells treated with or without hexamethylamine bisacetamide (HMBA), and subjected to 2-D gel electrophoresis. The resulted protein patterns were analyzed by Melanie software. Spots of nuclear matrix proteins differentially expressed were excised and subjected to in situ digestion with trypsin. Peptide masses were obtained by matrix-assisted laser-desorption/ionization time of flight mass spectrometry (MALDI-TOF-MS) analysis and submitted for database searching using Mascot tool.RESULTS: The MGc80-3 cells were induced into differentiation by HMBA. There were 22 protein spots which changed remarkably in the nuclear matrix, from differentiation of MGc80-3 cells compared to control.Eleven of which were identified. Seven proteins -actin, prohibitin, porin 31HL, heterogeneous nuclear ribonucleoprotein A2/B1, vimentin, ATP synthase, and heatshock protein 60 were downregulated, whereas three proteins - heat shock protein gp96, heat shock protein 90-beta, and valosin-containing protein were upregulated,and the oxygen-regulated protein was only found in the differentiated MGc80-3 cells.CONCLUSION: The induced differentiation of carcinoma cells is accompanied by the changes of nuclear matrix proteins. Further characterization of those proteins will show the mechanism of cellular proliferation and differentiation, as well as cancer differentiation.

Effects of Spinach Powder Fat-Soluble Extract on Proliferation of Human Gastric Adenocarcinoma Cells

Four kinds of assays were used to study the effect of a fat-soluble extract of spinach powder (SPFE) on the proliferation of human gastric adenocareinoma cell line (SGC-7901) in vitro.These studies included: (Ⅰ) cell growth assay, (Ⅱ) colony forming assay, (Ⅲ) MTT colorimetric assay, and (Ⅳ) 3H-TdR incorporation assay. The concentrations of SPFE expressed as the level of β-carotene in the medium were 2×10-8, 2×10-7 and 2×10-6 mol/L β-carotene in assays (Ⅰ)～(Ⅲ), but 4×10- 8, 4×10-7 and 4×10-6 mol/L β-caretene in assay (Ⅳ) respectively. The results indicated that SPFE inhibited the prolifendion and colony forming ability of SGC-7901 cells. And in MTT assay, SPFE inhibited the viability of SGC7901 cells, but no inhibitory effect of SPFE was observed on the viability of lymphocytes in peripheral blood of healthy people. Finally, in the 3H-TdR incorporation test, both SPFE and β-carotene showed significant inhibitory effects on DNA synthesis in SGC-7901 cells, but SPFE was more effective than β-carotene.

CHEMOSENSITIVITY OF MGc80-3 HUMAN GASTRIC ADENOCARCINOMA CELLS AND ITS CLINICAL SIGNIFICANCE

In the present study, the chemosensitivity of MGc80-3 human gastric adenocarcinoma cells was determined by means of colony-forming assay and the in vitro activities of 10 anticancer drugs were examined on the basis of the clinically achievable peak plasma drug concentration. The results showed that MGc80-3 cells were most sensitive to mitomyc'n C, adriamycin and 5-fluorouracil, being consistent with the response noted in clinical gastric cancer. This cell line may retain its original drug sensitivity and may be useful in screening for new compounds with activity against this disease.

Inhibitory effects of dobutamine on human gastric adenocarcinoma

AIM:To explore the inhibitory effects of dobutamine on gastric adenocarcinoma cells.METHODS:Dobutamine was used to treat gastric adenocarcinoma cells(SGC-7901)and cell viability was determined by the 3-(4,5-dimethylthiazol-2-yl)-2,5-diphenyltetrazolium bromide(MTT)assay.The effects of dobutamine combined with cisplatin on cell viability were also analyzed.Cell migration was studied using the wound healing assay,and cell proliferation was analyzed using the colony formation assay.A cell invasion assay was carried out using Transwell cell culture chambers.The cell cycle and cell apoptosis were analyzed by flow cytometry.Western blot and immunocytochemistry were performed to determine the expression of Yes-associated protein(YAP)in treated cells.RESULTS:Dobutamine significantly inhibited cell growth,migration,cell colony formation,and cell invasion into Matrigel.Dobutamine also arrested the cell cycle at G1/S phase,and increased the rate of apoptosis of gastric adenocarcinoma cells.The expression ofYAP was detected mainly in the nucleus in the absence of dobutamine.However,reduced expression of phosphorylated YAP was mainly found in the cytosol following treatment with dobutamine.CONCLUSION:Dobutamine has significant inhibitory effects on gastric adenocarcinoma cells and may be used in neoadjuvant therapy not only for gastric cancer,but also for other tumors.

Human papillomavirus DNA and P16～(INK4A) expression in concurrent esophageal and gastric cardia cancers

AIM:To investigate the relationship between human papillomavirus (HPV) infection and concurrent esophagus and gastric cardia cancer from the same patient (CC) and examine the significance of P16 INK4A protein expression.METHODS:Polymerase chain reaction was used to detect the presence of HPV type16 (HPV16).The expression of P16 INK4A protein was detected using immunohistochemistry.RESULTS:Among the CC specimens,HPV16-DNA was found in eight cases of esophageal squamous cell carcinoma (ESCC) and five cases of gastric cardia adenocarcinoma (GCA),respectively (47% vs 29%),and two of both ESCC and GCA.P16 INK4A was highly expressed in both ESCC and GCA.In the HPV-associated positive CC,higher P16 INK4A expression was observed in the GCA than in the ESCC (75% vs 25%,P < 0.05).CONCLUSION:HPV16 as a correlated risk factor may play an important role in the development of ESCC and GCA.P16 INK4A may be a screening index in the HPVassociated carcinoma of gastric cardia.

组蛋白乙酰化对A549和BEAS-2B细胞哮喘易感基因ADAM33的影响

目的:研究丁酸钠、曲古抑菌素A(trichostatin A,TSA)及腺病毒E1A相关的300 kD蛋白(adenoviral E1A binding protein of 300 kD,P300)介导的组蛋白乙酰化在人非小细胞肺癌A549细胞及人支气管上皮BEAS-2B细胞中对哮喘易感的解整合素金属蛋白酶33(a disintegrin and metalloproteinase 33,ADAM33)基因表达的影响。方法:将A549细胞及BEAS-2B细胞分别分为丁酸钠对照组(双蒸水处理)和1、2.5、5 mmol/L丁酸钠组,TSA对照组(0.1%二甲基亚砜处理)和0.2、0.4、0.8μmol/L TSA组,按照组别分别予以相应处理;另将BEAS-2B细胞分为对照组(转染P300突变质粒)和P300组(转染P300表达质粒);采用双荧光素酶报告基因法分析ADAM33启动子活性的变化,实时荧光定量PCR(quantitative real time-PCR,qRT-PCR)检测ADAM33 mRNA表达,蛋白质印迹法检测ADAM33蛋白表达。结果:在人非小细胞肺癌A549细胞中,与对照组相比,1 mmol/L丁酸钠组及0.2μmol/L TSA组ADAM33基因启动子活性明显降低(P<0.01);在BEAS-2B细胞中,与对照组相比,1 mmol/L丁酸钠组及0.2μmol/L TSA组ADAM33基因启动子活性、mRNA及蛋白相对表达水平明显降低(P<0.05或P<0.01)。加大丁酸钠、TSA药物浓度,ADAM33表达无显著差异。在人支气管上皮BEAS-2B细胞中,与对照组相比,P300组ADAM33启动子活性、mRNA和蛋白相对表达水平明显降低(P<0.05)。结论:丁酸钠、TSA通过组蛋白乙酰化降低人非小细胞肺癌A549细胞和人支气管上皮BEAS-2B细胞中ADAM33表达,P300通过组蛋白乙酰化降低人支气管上皮BEAS-2B细胞中ADAM33表达。

非人乳头状瘤病毒相关型宫颈腺癌临床病理分析(附9例)

目的:探讨非人乳头状瘤病毒(human papillomavirus,HPV)相关型宫颈腺癌临床病理学特征、鉴别诊断、分子特征及治疗和预后。方法:回顾性分析9例非HPV相关型宫颈腺癌的临床特征、病理学形态、免疫表型及治疗和预后,并复习相关文献。结果:患者均为女性,年龄18~57岁,平均45岁。4例宫颈透明细胞癌,5例宫颈胃型腺癌。3例宫颈透明细胞癌临床表现为异常子宫出血,1例年轻患者表现为宫颈赘生物。病理组织学特征表现为小管状、微囊型、乳头状或呈实性生长方式,肿瘤细胞内含透亮、富于糖原的细胞质,细胞核大,核仁明显,呈靴钉样外观,可见致密的嗜酸性间质和玻璃样变小体。免疫组化HNF1-β、Napsin-A、PAX8阳性,Ki-67增殖指数较高(60%~80%),ER、PR、p16阴性;3例宫颈胃型腺癌表现为阴道排液,1例因盆腔包块入院检查发现,1例体检发现。影像学对宫颈胃型腺癌具有特征性,2例胃型腺癌磁共振成像(magnetic resonance imaging,MRI)示宫颈囊实性肿块。病理组织学特征表现为肿瘤性黏液腺体不规则浸润性生长,超出正常宫颈内膜腺体的位置,腺体形态不规则、大小不一,经常成角或囊状,有一些伴有腔内乳头,往往腺体紧邻厚壁血管,间质反应一般轻微或无。肿瘤细胞边界较为清晰,胞浆透明至嗜酸性,内含丰富的黏液,细胞核可有异型性,核分裂象较为罕见。宫颈胃型腺癌表达MUC6、CEA,60%病例p53表现为突变型,p16阴性,宫颈胃型腺癌阿利辛蓝-过碘酸雪夫染色(Alcian blue Periodic acid-Schiff,AB-PAS)呈PAS阳性。所有9例患者HPV检测均为阴性。结论:宫颈透明细胞癌和胃型腺癌均为非HPV相关型宫颈腺癌,临床少见,恶性度高,具有一定的组织形态及免疫组化特征,联合运用一组免疫组化标记物有助于该类疾病的诊断。

七方胃痛颗粒对人胃腺癌细胞的抑制作用及可能机制

目的探讨七方胃痛颗粒对人胃腺癌细胞的抑制作用及可能机制。方法用生理盐水将七方胃痛颗粒稀释并配制成浓度为2 g/mL的七方胃痛颗粒混悬溶液,对20只SD大鼠连续灌胃5 d后获取七方胃痛颗粒含药血清。将AGS细胞分为空白对照组、顺铂组、10%含药血清组、20%含药血清组、30%含药血清组,各组细胞给予相应药物干预48 h。采用流式细胞仪检测细胞周期及凋亡情况,采用Western blot检测人表皮生长因子受体(HER)信号通路相关蛋白及其下游磷脂酰肌醇3-激酶(PI3K)/蛋白激酶B(AKT)信号通路相关蛋白的表达水平,采用实时荧光定量PCR检测上述蛋白对应基因的mRNA表达水平。结果与空白对照组相比,20%含药血清组AGS细胞的中晚期凋亡率升高,30%含药血清组AGS细胞的中晚期凋亡率及总凋亡率升高,4个给药组AGS细胞的G_(0)/G_(1)期比例提高,S期比例降低(均P<0.05)。与空白对照组比较,10%含药血清组AGS细胞的HER4蛋白表达水平下降,20%含药血清组AGS细胞的表皮生长因子受体(EGFR)、HER4蛋白表达水平均下降,顺铂组和30%含药血清组AGS细胞的EGFR、HER2、HER3、HER4、AKT、PI3K蛋白表达水平均下降(均P<0.05)。与空白对照组比较,4个给药组AGS细胞的EGFR、HER2、HER3、HER4、PI3K、AKT的mRNA表达水平下降(均P<0.05)。结论七方胃痛颗粒能促使AGS细胞发生中晚期凋亡,使细胞周期阻滞在G_(0)/G_(1)期,其可能通过抑制HER信号通路及下游PI3K/AKT信号通路的激活,起到抑制AGS细胞增殖的作用。

三氧化二砷(As_2O_3)诱导人胃腺癌SGC7901细胞程序化死亡并降低c-myc基因的表达

目的：探讨Ａｓ２Ｏ３对胃腺癌ＳＧＣ７９０１细胞系的生物学效应及机制。方法：通过ＭＴＴ还原法检测Ａｓ２Ｏ３对该细胞系存活率的影响，从光学显微镜形态观察，流式细胞仪分析，ＤＮＡ凝胶电泳，细胞凋亡原位检测（ＴＵＮＥＬ）进行细胞凋亡的检测。半定量ＲＴＰＣＲ检测基因表达。结果：Ａｓ２Ｏ３处理ＳＧＣ７９０１细胞后，细胞的存活率明显降低，光学显微镜下可见到明显的凋亡细胞，流式细胞仪测定细胞周期的Ｇ１期前有亚２倍体的凋亡峰，ＤＮＡ凝胶电泳显示出典型的凋亡特征：ＤＮＡ有规律断裂形成的梯状图谱，细胞凋亡原位检测发现ＤＮＡ的断裂，并降低细胞ｃｍｙｃ基因的表达。结论：Ａｓ２Ｏ３能诱导人胃腺癌ＳＧＣ７９０１细胞程序化死亡并可能通过降低ｃｍｙｃ基因的表达。

中国鲎素和正丁酸钠对人胃腺癌BGC-823细胞形态与超微结构的影响

目的以正丁酸钠为平行对照,比较观察鲎素和癌细胞诱导分化物对人胃癌细胞形态与超微结构变化的影响。方法采用光镜、扫描电镜与透射电镜,观察经2.0 mg/L鲎素、2.0 mmol/L正丁酸钠和1.0 mg/L鲎素+1.0 mmol/L正丁酸钠组合处理的人胃腺癌BGC-823细胞。结果光镜观察显示,鲎素和正丁酸钠以及鲎素+正丁酸钠处理的BGC-823细胞形态均较为一致,细胞体积增大、趋于扁平铺展状态,细胞核质比例减小,细胞核形状较圆整,核仁数量减少。扫描与透射电镜观察可见经鲎素、正丁酸钠及其组合处理的BGC-823细胞均出现细胞表面微绒毛稀少,细胞边缘丝状伪足减少,片状伪足增多;细胞核形态较规则,核内异染色质减少,常染色质增多:细胞质内线粒体增多,结构较为一致,高尔基复合体呈较为典型发达状态,并出现粗面内质网增多和多聚核糖体减少等变化。结论鲎素具有与正丁酸钠等诱导分化物相似的改变人胃癌细胞形态与超微结构恶性表型特征的作用,和与诱导分化物协同加成的诱导分化效果。

β-紫罗兰酮抑制SGC-7901细胞潜在的转移作用

目的观察β紫罗兰酮对人胃腺癌细胞(SGC7901)潜在转移的影响。方法采用细胞生长曲线,酶谱法和RTPCR技术,我们检查了不同浓度(25、50、100和200μmolL)β紫罗兰酮对SGC7901细胞生长,IV明胶酶的活性(MMP2和MMP9),nm23H1基因和金属蛋白酶抑制剂(TIMP1和TIMP2)在SGC7901细胞表达情况。β紫罗兰酮处理时间为24小时和48小时。结果β紫罗兰酮可抑制SGC7901细胞增殖。用不同浓度的β紫罗兰酮处理SGC7901细胞8天的抑制率分别为25.93%、28.21%、74.36%和90.11%。β紫罗兰酮作用于SGC7901细胞的IC50值为89μmolL。β紫罗兰酮不影响SGC7901细胞的基质金属蛋白酶2(MMP2)和基质金属蛋白酶9(MMP9)的活性。然而,β紫罗兰酮可明显地促进nm23H1基因、TIMP1和TIMP2的表达,呈现剂量-反应关系。结论β紫罗兰酮可抑制SGC7901细胞的生长和增殖。可能通过上调nm23H1,TIMP1和TIMP2来影响SGC7901细胞潜在的转移。然而,β紫罗兰酮对SGC7901细胞的IV型明胶酶活性没有影响,因而,β紫罗兰酮抑制SGC7901细胞的转移需要进一步研究。

丁酸钠对人结肠癌细胞株HCT-116细胞凋亡及基质相互作用分子和Orai1蛋白活性的影响

目的研究丁酸钠诱导结肠癌细胞株HCT-116细胞凋亡机制。方法 hoechst 33342和AnnexinV+PI检测丁酸钠诱导结肠癌细胞HCT-116的凋亡作用;免疫荧光法检测丁酸钠对基质相互作用分子(STIMl)和钙离子通道Orail蛋白在细胞内定位的影响;免疫印迹法检测STIMl和Orail蛋白表达量的变化。结果丁酸钠可诱导结肠癌细胞HCT-116凋亡、STIMl移位并与Orail具有共定位现象。结论丁酸钠可通过调节STIM1和Orail在结肠癌细胞中的定位而促发细胞凋亡。

丁酸钠诱导高转移人肺癌细胞恶性表型逆转和抑制侵袭作用的研究

本文作者选用丁酸钠处理克隆化高转移人肺巨细胞癌（PGCL3）细胞，发现肿瘤细胞在形态、增殖速度、分裂指数、软琼脂集落形成能力和凝集反应等方面均出现向正常细胞表型逆转，证明丁酸钠具有抑制PGCL3细胞增殖及诱导分化的作用。我们还进行了反映肿瘤细胞浸润和转移能力的粘附、运动和降解侵袭实验，结果显示丁酸钠对PGCL3细胞的上述三种能力都有明显的抑制作用，表明丁酸钠在诱导PGCL3细胞向成熟方向分化的同时，还使PGCL3细胞的侵袭能力减弱。

蛇葡萄素钠联合卡铂对人肺腺癌GLC-82细胞增殖及凋亡的影响

目的探讨蛇葡萄素钠(AMP-Na)单用及其与卡铂(CBP)合用对人肺腺癌GLC-82细胞增殖的抑制作用及可能的机制。方法四甲基偶氮唑盐(MTT)比色法测定两药单用及合用对GLC-82细胞的体外杀伤活性;透射电子显微镜(TEM)观察GLC-82细胞超微结构的变化;流式细胞仪(FCM)检测GLC-82细胞凋亡和caspase-3的表达。结果对于GLC-82细胞,AMP-Na与CBP合用,CBP的IC50由(17.10±4.78)mg·L-1降低到<3.12 mg·L-1(P<0.01),表明Amp-Na对卡铂抑制GLC-82细胞增殖的作用具有协同效应(CDI<1)。TEM及FCM检测结果表明,单用AMP-Na及与卡铂合用均可诱导GLC-82细胞凋亡、坏死,两药合用后坏死率由(2.56±0.41)%升高到(71.83±5.43)%(P<0.01)。AMP-Na单用及与卡铂合用作用于GLC-82细胞48 h后,caspase-3的表达均明显增高。结论AMP-Na和CBP具有协同诱导GLC-82细胞凋亡的作用,机制可能与激活细胞内caspase-3介导的信号转导通路相关。

封闭内源性miR-23a对人胃腺癌细胞系MGC803增殖及侵袭的影响

目的设计并合成miR-23aASO(ASO-23a),封闭内源性miR-23a的功能后,检测人胃腺癌细胞系MGC803增殖及侵袭能力的改变。方法首先设计并合成ASO-23a,经脂质体方法转染MGC803细胞,实时定量PCR检测转染细胞MGC803中miR-23a的表达水平;经MTT实验、平板克隆形成实验、软琼脂克隆形成实验、TUNEL实验及transwell实验-观察细胞内源性miR-23a功能被封闭后对MGC803细胞增殖、凋亡及侵袭能力的影响。结果实时定量PCR结果表明ASO-23a能够有效封闭细胞中内源性miR-23a;MTT、平板克隆形成及软琼脂克隆形成实验结果显示,封闭内源性miR-23a后可抑制MGC803细胞活性;TUNEL实验结果显示,ASO-23a可以促进MGC803细胞凋亡的发生;Transwell实验结果显示,ASO-23a可以抑制MGC803细胞的侵袭能力。结论设计并合成的.ASO-23a在人胃腺癌细胞系MGC803中有效封闭内源性miR-23a,能够抑制细胞活性及侵袭能力,并能促进细胞凋亡的发生。

幽门螺杆菌与胃上皮细胞不同作用时间点蛋白质组的差异分析

目的:分析幽门螺杆菌(Hpylori)与人胃腺癌上皮细胞(humangastric adenocarcinoma epithelial,AGS)的相互作用蛋白质组学差异.方法:采用双向凝胶电泳分离Hpylori26695株与AGS细胞相互作用0.5、2、4h时间点的细胞和黏附菌的全蛋白样品,考马斯亮兰染色,ImageMster2D图像分析软件比较分析,识别差异蛋白,将差异蛋白点进行胶内酶解,经基质辅助电离解析飞行时间质谱(MALDI-TOF-TOF/MS)获得肽质量指纹图谱(PMF),通过搜寻蛋白质数据库完成对差异蛋白的鉴定.结果:对0.5、2、4h时间点图谱差异蛋白点分析共发现主要差异蛋白点66个,对其中34个(共对应16种蛋白)最终完成准确鉴定,2h后8种蛋白开始上调,其中2种是细胞来源,6种Hpylori来源;4h时4种细胞来源蛋白下调,并有4种新的蛋白开始被观察到.在共感染的早期,细胞的琥珀酸脱氢酶、Hpylori的抗氧化酶类、黏附素以及HSP60表达上调.感染晚期主要是细胞来源的亲环素A、新生多肽相关复合物α多肽开始表达,Hpylori来源的尿素酶、非血红素铁蛋白等蛋白明显出现在黏附菌成分中.结论:Hpylori与AGS细胞相互作用过程中,细菌和细胞蛋白表达均存在明显时序性变化,早期相互作用则主要表现为以与黏附等有关的蛋白表达变化,后期向有利细菌存活和增殖的方向发展,并呈现出与免疫逃逸和病理损伤相关的变化.

菠菜粉脂溶性粗提物对人胃癌细胞的体外抑制作用

目的：以体外培养的人胃腺癌细胞株ＳＧＣ－７９０１为材料，观察菠菜粉脂溶性粗提物（ＳＰＦＥ）对人胃癌细胞体外增殖和功能的影响。方法：在３Ｈ－ＴｄＲ掺入实验中ＳＰＦＥ的剂量（以培养液中β－胡萝卜素浓度计）为４×１０－８、４×１０－７、４×１０－６ｍｏｌ／Ｌ；在其它三个实验中为２×１０－８、２×１０－７、２×１０－６ｍｏｌ／Ｌ。结果：１．生长曲线实验中，ＳＰＦＥ在中、高剂量组对人胃癌细胞的增殖有显著的抑制作用，且随剂量增加，抑制作用有增强趋势；２．集落形成实验中，ＳＰＦＥ各剂量组均抑制了胃癌细胞的集落形成（Ｐ＜０．０１），抑制作用呈剂量－反应关系；３．甲基噻唑基四唑（ＭＴＴ）实验中，ＳＰＦＥ各剂量组在抑制胃癌细胞活性和功能的同时，对正常人外周血淋巴细胞却没有影响（Ｐ＞０．０５）；４．对３Ｈ－ＴｄＲ掺入胃癌细胞量的测定表明，ＳＰＦＥ各剂量组和同剂量的β－胡萝卜素对胃癌细胞的ＤＮＡ合成均有抑制作用（Ｐ＜０．０５），但菠菜ＳＰＦＥ的抑制作用显著较β－胡萝卜素强（Ｐ＜０．０５）。

正丁酸钠诱导人肝癌细胞表型分化的观察

目的 探讨ＳＢ对人肝癌细胞的诱导分化作用。方法 以０－２ｍｍｏｌＬ的ＳＢ作用于培养的人肝癌细胞ＧＨＣ－ ３，作用３０ 天后恢复正常培养，观察癌细胞表型的变化。结果 人肝癌细胞生长抑制；ＳＢ作用３０ 天细胞形态由多角型转变为棱形，ＣｏｎＡ凝集现象消失，琼脂集落形成率下降；染色体主流范围变窄，二倍体及亚二倍体比例升高；３Ｈ－ ＴｄＲ 掺入率、细胞ＤＮＡ含量下降与对照比较有显著差异（ Ｐ＜ ０－０１） ；并观察到，上述细胞再经不含ＳＢ 的正常培液继续培养三代后该细胞表型未发生明显改变。结论 人肝癌细胞在低剂量丁酸钠持续作用下，某些恶性表型可发生部分逆转，且这些改变在恢复正常培养后可保持相对稳定。