细胞毒药物(Ge mcitabine)治疗人胰腺癌裸鼠胰腺原位移植癌的实验研究

目的 探讨细胞毒药物 (Gemcitabine)对胰腺癌裸鼠原位移植模型 (SOI)生长、转移的抑制作用。方法 SOI模型分为Ⅰ组 (Gemcitabine 10 0mg/kg)、Ⅱ组 (Gemcitabine 5 0mg/kg)和对照组。Gemcitabine于术后第 0 ,3,6 ,9天给药 ,ip ,术后第 10周处死裸鼠 ;并对肿瘤组织的增殖指数 (PI)、凋亡指数 (AI)以及PI/AI进行分析。结果 (1)Ⅰ组能显著抑制胰腺癌生长 ,Ⅱ组则无显著的肿瘤抑制作用 ,但两者对胰腺癌转移和预后均无显著疗效 ;(2 )Ⅰ组可显著降低肿瘤增殖指数 (PI) ,增大凋亡指数 (AI) ,PI/AI显著降低。结论 Gemcitabine单用能有效抑制胰腺癌生长 。

稳定高表达p75NGFR的胰腺原位荷瘤裸鼠模型的建立

由于目前尚无有效的筛查和早期诊断方法，确诊时80％的胰腺癌患者已出现转移，错芝了手术机会，临床上很难获得新鲜的，不同时期的组织标本，更不可能在临床上观察胰腺癌进展过程。

NGAL在原位胰腺癌裸鼠中的表达

目的研究NGAL在原位胰腺癌裸鼠及正常裸鼠中的表达情况。方法构建原位胰腺癌裸鼠模型,采用ELISA、RT-PCR和Western Blot等方法测定原位胰腺癌裸鼠及正常裸鼠NGAL的血清水平及在外周血白细胞中的表达情况。结果原位胰腺癌裸鼠的血清NGAL水平、外周血白细胞NGAL mRNA表达水平及蛋白表达水平均显著高于正常裸鼠(P<0.05)。结论原位胰腺癌裸鼠中NGAL的表达增加,胰腺癌可促进裸鼠的NGAL表达上调。

薏苡仁油对人胰腺癌BxPC-3细胞影响IL-18表达的体外实验研究

目的:研究薏苡仁油对人胰腺癌BxPC-3细胞的增殖影响及相关微环境因素作用,探讨其可能的肿瘤作用机制,为胰腺癌的中西医结合治疗提供实验依据。方法:分组研究,将薏苡仁油作用于人胰腺癌BxPC-3细胞,通过四唑蓝(MTT)法观察细胞增殖状况;收集与MTT法等条件分组培养的细胞培养液上清做IL-18 ELISA。结果:体外培养的BxPC-3细胞经薏苡仁油作用后,增殖受到明显抑制,作用具有浓度依赖性,加药组中以20 mL/L薏苡仁油剂量组的作用最佳,有效作用最佳时间段在36 h左右;薏苡仁油加药组对IL-18的蛋白表达水平显著高于空白对照组(P<0.05),表达水平具有浓度依赖性,48 h达到最高峰值后随即下降。结论:薏苡仁油具有抗人胰腺癌BxPC-3细胞增殖作用,可短暂性上调BxPC-3细胞IL-18的表达。

薏苡仁油对人原位胰腺癌BxPC-3细胞生长及VEGF和bFGF表达的影响

目的研究薏苡仁油(康莱特注射液)体外对人原位胰腺癌BxPC-3细胞生长和血管生长因子的影响,探讨薏苡仁油抗肿瘤作用机制。方法薏苡仁油作用BxPC-3细胞后,经瑞氏染色观察细胞形态,Hoechst 33258荧光染色、DNA梯度电泳观察细胞凋亡;流式细胞仪检测细胞周期的变化;ELISA法检测血管内皮生长因子(VEGF)、成纤维细胞生长因子(bFGF)的变化。结果薏苡仁油(2 mg/mL,20μL/mL)作用于BxPC-3细胞后,瑞氏染色可见细胞出现典型的凋亡小体,Hoechst33258荧光染色可见BxPC-3细胞出现特征性凋亡变化,琼脂糖电泳观察到明显的细胞凋亡特征性DNA梯形条带;细胞周期阻滞在G0/G1期;细胞上清液中VEGF、bFGF的表达水平明显下调。结论薏苡仁油能影响BxPC-3细胞生长周期,导致细胞周期阻滞,下调VEGF和bFGF的表达水平,可能对抑制胰腺癌细胞的扩散产生一定作用。

乌司他丁对犬胰岛的保护作用

目的 判定在机械分离纯化犬胰岛过程中，胰腺原位灌洗时应用乌司他丁（UTI）的保护作用，观察胰岛的获取产量。方法将20只犬随机分为两组，每组10只。HC-A组：胰腺经腹主动脉原位灌洗时用冷HC-A液2500ml；HC-A＋UTI组：胰腺原位灌洗时，HC-A液中加用UTI 10000U／kg。两组均经主胰管用4℃胶原酶V控压灌注，在Ricordi Chamber系统中消化，用Ficoll连续梯度离心纯化。

乌司他丁对犬胰岛的保护作用

目的判定在机械分离纯化犬胰岛过程中,胰腺原位灌洗时应用乌司他丁(UTI)的保护作用,观察胰岛的获取产量。方法将20只犬随机分为两组,每组10只。HC-A组:胰腺经腹主动脉原位灌洗时用冷HC-A液2500ml;HC-A+UTI组:胰腺原位灌洗时,HC-A液中加用UTI10000U/kg。两组均经主胰管用4℃胶原酶V控压灌注,在RicordiChamber系统中消化,用Ficoll连续梯度离心纯化。记录消化时间、胰岛外分泌腺包裹率、胰岛纯度、纯化后胰岛在体外用低糖与高糖刺激下胰岛素分泌量、C-肽的释放量及收获的胰岛当量(IEQ),并对纯化后的胰岛进行光镜及电镜观察。结果HC-A+UTI组与HC-A组在胰腺消化时间、胰岛外分泌腺包裹率、胰岛纯度、纯化后的胰岛在体外经低糖与高糖刺激下胰岛素分泌量、C-肽的释放量以及胰岛的形态和结构上比较,差异均无统计学意义(P>0.05)。HC-A组收获胰岛[(3.42±1.47)×104]IEQ,HC-A+UTI组收获胰岛[(6.17±2.86)×104]IEQ,两组差异有统计学意义(P<0.05)。结论在犬胰岛分离和纯化过程中,胰腺获取原位灌洗液中加用UTI能保护胰腺组织,增加胰岛产量。

Increased expression of neuropeptide Y and its mRNA in STZ-diabetic rats

OBJECTIVE: To study the relationship between neuropeptide Y (NPY) and diabetes by examining the content and distribution of NPY and its mRNA expression in the hypothalamus and pancreas of STZ-diabetic rats. METHODS: Thirty Wistar rats were randomly divided into 3 groups (diabetic group, diabetic insulin treatment group, and control group). After feeding for 24 weeks, the rats were sacrificed. The expression of NPY in the hypothalamus and pancreas was detected with immunohistochemistry and in situ hybridization. RESULTS: (1) The hypothalamic content of NPY and its mRNA were significantly increased in STZ-diabetic rats in comparison with normal controls. Increased expression of NPY mRNA was found only in the arcuate nucleus and not in the paraventricular nucleus in diabetic rats, suggesting that NPY was produced in the arcuate nucleus. (2) The hypothalamic content of NPY and its mRNA in STZ-diabetic rats were visibly reduced after insulin treatment compared with that in untreated diabetic rats. This supports the hypothesis that insulin deficiency in the brain may be responsible for increased hypothalamic NPY gene expression in diabetic rats. (3) The increase of hypothalamic NPY in STZ diabetic rats associated with hyperphagia and polydipsia could be reversed by insulin replacement, suggesting that increased hypothalamic NPY contributes to the pathophysiological progress of the diabetic state. (4) The present study demonstrated for the first time that the content of NPY and its mRNA in the pancreas was increased in STZ-diabetic rats, and that the distribution of NPY-positive cell in islets was changed from the periphery to the whole islet. The content and distribution of NPY and its mRNA in islets were not changed by insulin treatment. CONCLUSION: Increased NPY in the hypothalamus results in hypophagia and polydipsia, while the implication of increased NPY in the pancreas of diabetic rats is not clear.