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1.
本试验旨在研究发酵前后芹菜汁的主要功能成分变化和芹菜发酵液对葡聚糖硫酸钠(DSS)诱导的小鼠溃疡性结肠炎(UC)的防治及免疫调节作用。选取50只4周龄雄性C57BL/6小鼠随机分为空白组、模型组及低、中、高浓度芹菜发酵液组,每组10只。按10 μL/g BW的剂量标准给空白组和模型组小鼠灌胃无菌生理盐水,其他组小鼠则灌胃不同浓度的芹菜发酵液,持续7 d。从第8天开始,除空白组自由饮用无菌水外,其余组连续7 d自由饮用3% DSS溶液;在此过程,每日称量体重,进行疾病活动指数(DAI)评分。在第14天,通过摘眼球取血法获得全血,随后脱颈处死小鼠,解剖取出结肠组织测量长度并通过苏木素-伊红(HE)染色法制作病理切片,进行病理学分析。以流式细胞仪分选技术检测外周血中CD4+/CD8+T淋巴细胞比值,以酶联免疫吸附法(ELISA)检测血清中肿瘤坏死因子-α(TNF-α)、白细胞介素-6(IL-6)、γ-干扰素(IFN-γ)和IL-10的含量。结果表明:①芹菜汁经发酵后,总酸、总糖、总多酚、类黄酮、维生素C和超氧化物歧化酶(SOD)等多种活性成分的含量均显著增加(P<0.05)。②与模型组相比,芹菜发酵液高浓度组能减少DSS引起的小鼠体重损失(P<0.01)、结肠缩短(P<0.01)和DAI降低(P<0.05)。③组织病理学分析结果表明,各发酵液组的UC症状均得到不同程度改善,肠腺结构相对完整,杯状细胞轻微减少,仅有少量淋巴细胞和中性粒细胞浸入。④流式细胞仪分析结果显示,相较于模型组,发酵液组全血CD4+/CD8+T淋巴细胞比值极显著升高(P<0.01)。⑤ELISA检测结果显示,与模型组相比,芹菜发酵液组的IL-6、TNF-α和IFN-γ含量极显著下调(P<0.01),IL-10的含量极显著上调(P<0.01)。综上,芹菜汁经发酵后主要功能活性成分均得到显著提高,并且发酵芹菜液对DSS诱导的小鼠UC具有一定的防治和免疫调节作用,其作用机制可能与维持外周血中CD4+与CD8+T淋巴细胞平衡,以及抑制促炎症因子(TNF-α、IL-6和IFN-γ)表达,促进抗炎症因子(IL-10)表达有关。 相似文献
2.
Deborah C. Silverstein DVM DACVECC Janet Aldrich DVM Steve C. Haskins DVM MS DACVECC DACVA Kenneth J. Drobatz DVM MSCE DACVECC DACVIM Larry D. Cowgill DVM PhD DACVIM 《Journal of Veterinary Emergency and Critical Care》2005,15(3):185-192
Objective: To determine the continuous changes in blood volume in response to fluid administration using an in‐line hematocrit monitor. Design: Prospective study. Setting: Research laboratory. Animals: Four healthy dogs. Interventions: Each dog received intravenous boluses of 80 mL/kg of 0.9% saline (S), 4 mL/kg of 7.5% saline (HS), 20 mL/kg of dextran 70 (D), 20 mL/kg of hetastarch (HES), or no fluids (control, C) on separate occasions. Fluids were administered at 150 mL/min in the S, D, and HES groups, and at 1 mL/kg/min in the HS group. Measurements and main results: Blood volume changes were measured every 20 seconds for 240 minutes using an in‐line hematocrit monitor. There was a rapid rise in blood volume during all infusions. Immediately after the administration of crystalloid fluids, the rapid rise in blood volume ceased. Subsequently, there was a steep decline in blood volume for 10 minutes, and a slower decline thereafter. In contrast, the rise in blood volume continued for at least 10 minutes after the infusion of the colloids was complete, and a plateau was observed for the remainder of the experiment. The blood volume effect, as measured by area under the curve, was significantly greater in the saline group than the other groups during the infusion time and for the 0–240 minutes time period. The areas under the curve for the two colloid solutions were not significantly different from each other during any time periods. The percent increase in blood volume immediately following the infusions was 76.4±10.0 in the S group, 17.1±3.2 in the HS group, 23.0±10.5 in the D group, and 27.2±6.4 in the HES group. At 30 minutes from the start of the infusion, the mean percent increases in blood volumes were 35.2±9.3 in the S group, 12.3±0.9 in the HS group, 35.9±7.3 in the D group, and 36.8±6.5 in the HES group. At 240 h post‐infusion, the mean percent increases in blood volume were 18.0±9.7 in the S group, 2.9±6.1 in the HS group, 25.6±16.1 in the D group, and 26.6±8.6 in the HES group. The C group had a mean percent change in blood volume of ?3.7±3.4 at the end of the experiment. Conclusions: This study indicates that the rapid administration of saline at clinically relevant doses leads to the largest immediate increase in blood volume, although this change is transient because of rapid redistribution of the fluid. Despite a brief increase in blood volume that was almost 3 times the volume administered, hypertonic saline led to the smallest increase in blood volume post‐infusion. The synthetic colloid solutions increased the blood volume by an amount greater than that infused and the effect was sustained for a longer period of time than seen following crystalloid administration, but the maximum increase in blood volume was significantly less than saline. The measurement of continuous changes in blood volume, using an in‐line hematocrit monitor, was a useful means of assessing the dynamic effects of fluid administration in dogs in a research setting. 相似文献
3.
Objective To evaluate and compare coagulation variables following the administration of oxypolygelatin and dextran 70 to clinically healthy dogs. Study design Randomized cross‐over experimental study. Animals A total of eight healthy adult female Beagles aged 2–4 years old and weighing 11.8 ± 2.7 kg. Methods The dogs received a 15‐minute intravenous (IV) infusion of 5 mL kg?1 oxypolygelatin or 10 mL kg?1 6% dextran 70. Before (PRE) and at 2, 5, and 24 hours after administration, packed cell volume (PCV), total solids concentration (TS), prothrombin time (PT), activated partial thromboplastin time (APTT), fibrinogen concentration (FIB), platelet numbers (Plat), factor VIII coagulant activity (VIII:C), von Willebrand factor antigen concentration (vWf:Ag) and platelet function and buccal mucosal bleeding time (BMBT) were measured. Platelet function was assessed using aggregation and by measuring ATP release from aggregating platelets over 6 minutes, with 20, 10, and 5 µm ADP and 5 and 10 µg of collagen mL?1 as platelet activation agonists. Results All baseline values were within our normal ranges, except for one dog that had low vWf:Ag PRE values prior to both dextran and oxypolygelatin administration. Following dextran and oxypolygelatin administration, the PCV and TP were significantly (p < 0.05) decreased. Plat, FIB, and vWf:Ag decreased, while BMBT and VIII:C increased following dextran administration. Dextran also caused a significant decrease in platelet aggregation in response to ADP. Oxypolygelatin caused a significant decrease in vWf:Ag, Plat, and FIB compared to PRE values. The total amount of ATP released, standardized to platelet number, did not vary significantly for either group at any sampling time from PRE values. No significant changes from PRE values were noted at any time in either group for PT or APTT. Conclusion At the doses administered, both dextran and oxypolygelatin can interfere with hemostatic variables in healthy dogs, but dextran's effect is more profound and prolonged when compared to oxypolygelatin. Clinical relevance Oxypolygelatin causes fewer hemostatic abnormalities when compared to dextran, making it a superior colloid for administration at the doses tested. 相似文献
4.
Jiro Sonoda Yuki Seki Atsushi Hakura Satoru Hosokawa 《Journal of toxicologic pathology》2015,28(2):109-120
Benzo[a]pyrene (BP) is mutagenic but noncarcinogenic in the murine colon. Recently, we reported rapid induction of colonic tumors by treatment of CD2F1 mice with BP (125 mg/kg for 5 days) followed by a colitis inducer, dextran sulfate sodium (DSS) (4% in drinking water for 1 or 2 weeks). However, there are no reports on detailed time course and histopathological features of colonic proliferative lesions in this model. Here, we show the detailed time course of colonic dysplasia, adenoma and adenocarcinoma induced by treatment with BP, DSS, and a combination of the two (BP/DSS). In the colon of mice exposed to BP/DSS, 14.6 dysplastic foci per mouse were present one week after DSS treatment (week 4). The number of dysplastic foci decreased with time to 3.1 at week 9 and thereafter remained almost constant. At week 4, 1.5 adenocarcinomas were also observed, with a marked increase in numbers with time, reaching 29.3 at week 14. In contrast, the number of dysplastic foci induced by DSS alone showed a time course similar to that following BP/DSS treatment; however, only a few tumors appeared. Neither dysplastic foci nor neoplastic lesions were induced by BP only. In mice exposed to BP/DSS, β-catenin was demonstrated immunohistochemically in the nucleus and/or cytoplasm of the tumor cells, and this translocation from the cell membrane was evident in subsets of dysplastic foci. In dysplastic foci induced by DSS alone, β-catenin was absent in the nucleus/cytoplasm. These finding suggest that aberrant β-catenin accumulation in dysplastic foci is associated with tumor progression in this BP/DSS model. 相似文献
5.
KANG Jing-jing ZHAO De-ming TENG Ke-dao JIAO Xi-lan WANG Ping-li SUN Zhe NI Pei-pei WANG Zhi-feng ZHANG Rui YANG Yu-rong LIANG Hong-de 《农业科学学报》2014,13(4):858-869
Ulcerative colitis (UC) is a lifelong illness with profound emotional and social impacts, and could cause serious damage to large intestine, especially in colon. However, the pathogenesis of UC remained unclear. The present study attempts to find out the role of matrix metalloproteinases-7 (MMP-7) and lysozyme in the pathogenesis of UC through a mice model induced by dextran sulfate sodium (DSS). The UC model was evaluated both by disease activity index (DAI) and the intestinal histopathology. The results show that there is a high correlation between the DAI score and the pathological changes of colon. Interleukin-6 (IL-6) serum levels and large intestinal fluids levels in UC mice are always higher than that of the control groups, which might be associated with the degree of the inflammation damage in the colon. The change tendency of the MMP-7 mRNA and protein expressions are both up-regulated firstly and then down-regulated from 1 to 5 d in the colon, but only the MMP-7 protein is up-regulated at 7 d again. The up-regulated MMP-7 levels in the early stage of UC may play a protective role through the activated defensins, while the down-regulated levels in the mid-later stage of UC may be connected with the severe lesions in the colon. However, the up-regulated MMP-7 levels in the later stage of UC in the colon may also contribute to the tissue repair or be served as a marker to CRC (colorectal cancer). The distribution of lysozyme protein indicates that there may be Paneth-like cells in the colon. Both the changes of MMP-7 and lysozyme in the small intestine may play a protective role for the safe environment of the whole gut, especially to the colon of UC. 相似文献
6.
将右旋糖酐侧链进行功能化修饰,制备了一种富含醛基的改性多糖.利用这种改性多糖作为还原剂和稳定剂合成银纳米粒子,并研究了该银纳米粒子与阿霉素的相互作用及其共振光散射光谱.研究表明,体系的lg(ΔIRLS)值与阿霉素的浓度在一定范围内呈线性关系,线性方程为lg(ΔIRLS)=0.874 4+0.704 7c,线性范围为1.36×10-6~4.08×10-6mol/L,检出限(3σ)为1.30×10-7mol/L. 相似文献
7.
本文报道新型高效皮肤渗透促进剂氮酮(Azone)对右旋糖酐铁的透皮吸收促进作用及其对防治仔猪缺铁性贫血的意义. 相似文献
8.
A set of experiments was carried out in order to approach the complex nature of L. monocytogenes infections from different aspects. Experiment 1 showed that Listeria are able to gain admission to body by numerous ways and both subcutaneous and oral entry can lead to fatal septicemia. It also gave slight support to the theory of direct neural transmission of Listeria to the brain and indicated the possibility that intestinal absorption after oral exposition at least partly occurs via lymphatic vessels. No inflammatory reaction could be caused to mice by ocular flushing with Listeria suspension.The second trial proved that there are vast differences in the animal pathogenecity of Listeria strains — even among those of the same serotype. In experiment 3A the abolishing effect of dextran sulfate on the early resistance of mice to Listeria was confirmed and it turned out that cortisone at a therapeutic dose level did not bring about that phenomenon. Levamisole granted no conspicuous enhancement of resistance in this acute challenge; however, the results of the immunity test (3B) suggested that levamisole may be beneficial during the induction phase. On the other hand, starvation appeared to impair long-term immunity. Likewise, in experiment 4 starved mice were quite susceptible to acute challenge with Listeria. Raised ambient temperature, on the contrary, prominently increased the survival rate of the animals.Owing to the fairly small number of animals these results should be regarded as preliminary starting points to further studies. 相似文献
9.
为提高大豆分离蛋白的表面活性,试验采用过氧乙酸控制性的打开蛋白质的二硫键,并在此基础上加入葡聚糖进行复合修饰。结果表明:随着二硫键断开程度的增加,接枝度明显提升,褐变度与其有相同的变化趋势。当二硫键断开率为46%时,表面活性最理想。其中乳化性和乳化稳定性提高107.56%和175%;起泡性和起泡稳定性提高83.63%和105%;荧光图谱表明随着二硫键断开率的增加,荧光强度出现先升高后降低的趋势,而糖基化复合产物荧光强度依次降低;SDS-PAGE进一步证实,在糖基化过程中7S亚基最先消失,二硫键断开后,可以加速11S酸性亚基与葡聚糖发生糖基化反应。 相似文献
10.
Camila Trevisan Pereira Fabio Luiz Navarro Marques Jamie Williams Benedicto Wlademir De Martin Pedro Primo Bombonato 《Veterinary radiology & ultrasound》2008,49(5):487-491
Lymphoscintigraphy is the technique of choice for sentinel lymph node detection in women with early breast cancer, but there is limited information evaluating the value of this technique in animals. We investigated mammary lymphatic drainage in 25 young female mongrel dogs by intramammary injection of 18.5 MBq of 99mTc-dextran (70,000 Da). Lymph node anatomical referencing was obtained using an external marker, bone scintigraphy, or scintiscanning the body contour. Cranial and caudal thoracic mammary glands drained into the cranial sternal lymph node and axillary lymph center. The cranial thoracic mammary gland also drained into the superficial cervical lymph node in two of five animals. The cranial abdominal gland was drained by the axillary lymph center. The caudal abdominal mammary gland was drained by the superficial inguinal lymph node in all animals and simultaneously by medial iliac lymph nodes in four of five animals. In one dog, this mammary gland was also drained by the mediastinal and the superficial cervical lymph nodes. The inguinal mammary gland was drained by superficial inguinal lymph nodes and simultaneously via the medial iliac lymph node in one animal. Lymphatic communications between lymph nodes were identified in 11 of 25 (44%) animals. 99mTc-dextran mammary lymphoscintigraphy was easy and rapid to perform and may provide valuable information for further studies. 相似文献