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find Keyword "动物" 559 results
  • Influence of Alcohol Intervention on the Outcome of Rats and Mice with Ischemic Stroke: A Systematic Review

    Objective To systematically evaluate the influence of alcohol intervention on the outcome of rats and mice with ischemic stroke. Methods Databases including PubMed, EMbase, BIOSIS and CNKI were electronically searched from establishment dates of databases to June 2012 to retrieve animal experiments on the influence of alcohol intervention on the outcome of rats and mice with ischemic stroke. The relevant studies were identified according to the predefined inclusion and exclusion criteria, the data were extracted, and the quality was evaluated. Then meta-analysis was performed using RevMan 5.1 software. Results Eight studies were included. The results of meta-analysis showed that no significant difference was found between the alcohol intervention group and the control group (MD=−6.98%, 95%CI −20.38% to 6.43%, P=0.31). However, compared with the control group, low dose of acute alcohol intervention (less than 2 g/kg) improved the prognosis of ischemic stroke with a significant difference (MD=−22.83%, 95%CI −38.77% to −6.89%, P=0.005), and highly-concentrated of chronic alcohol intervention worsened the cerebral ischemic damage of rats and mice with a significant difference (MD=24.06%, 95%CI 10.54% to 37.58%, P=0.000 5). Conclusion Low dose of acute alcohol intervention (less than 2 g/kg) could improve the prognosis of rats and mice with ischemic stroke which has the potential neuro-protective effects. However, highly-concentrated chronic alcohol intervention could worsen the cerebral ischemic damage. Due to the limitations of the included studies such as publication bias, the influence of alcohol intervention on the outcome of rats and mice with ischemic stroke could be overestimated.

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  • Adoptive Transfusion of Tolerance Dendritic Cells Prolongs the Survival of Cardiac Allograft: A Systematic Review of 44 Basic Studies in Mice△

    Objective Tolerogenic DCs (Tol-DCs), a group of cells with imDC phenotype, can stably induce T cells low-reactivity and immune tolerance. We systematically reviewed the adoptive transfusion of Tol-DCs induced by different ways to prolong cardiac allograft survival and its possible mechanism. Method MEDLINE (1966 to March 2011), EMbase (1980 to March 2011), and ISI (inception to March 2011) were searched for identification of relevant studies. We used allogeneic heart graft survival time as endpoint outcome to analyze the effect of adoptive transfusion of Tol-DC on cardiac allograft. By integrating studies’ information, we summarized the mechanisms of Tol-DC in prolonging cardiac grafts. Results Four methods were used to induce Tol-DC in all of the 44 included studies including gene-modified, drug-intervened, cytokine-induced, and other-derived (liver-derived amp; spleen-derived) DCs. The results showed that all types of Tol-DC can effectively prolong graft survival, and the average extension of graft survival time for each group was as follows: 22.02 ± 21.9 days (3.2 folds to control group) in the gene modified group, 25.94 ± 16.9 days (4.3 folds) in the drug-intervened groups, 9.00 ± 8.13 days (1.9 folds) in the cytokine-induced group, and 10.69 ± 9.94 days (2.1 folds) in the other-derived group. The main mechanisms of Tol-DCs to prolong graft survival were as follows: a) induceT-cell hyporeactivity (detected by MLR); b) reduce the effect of cytotoxic lymphocyte (CTL); c) promote Th2 differentiation; d) induce Treg; e) induce chimerism. Conclusion For fully MHC mismatched allogeneic heart transplant recipients of inbred mouse, adoptive transfusion of Tol-DC, which can be gene-modified, drug-intervened, cytokine-induced, spleen-derived or liver-derived, can clearly prolong the survival of cardiac allograft or induce immune tolerance. Gene-modified and drug-induced Tol-DC can prolong graft survival most obviously. Having better reliability and stability than drug-induction, gene-modification is the best way to induce Tol-DCs at present. One-time intravenous infusion of 2 × 106 Tol-DC is a simple and feasible way to induce long-term graft survival. Multiple infusions will prolong it but increase the risk and cost. Adoptive transfusion of Tol-DC in conjunction with immunosuppressive agents may also prolong the graft survival time.

    Release date:2016-08-25 02:39 Export PDF Favorites Scan
  • The Need for Systematic Reviews of Animal Studies

    Release date:2016-08-25 03:34 Export PDF Favorites Scan
  • 降钙素原对胰腺炎感染早期预测的研究进展

    急性胰腺炎为急腹症常见疾病,大多为轻症。胰腺坏死超过30%的患者中有30%~40%发生感染,其病情凶险,病死率高。因而早期对急性胰腺炎感染进行预测,识别感染患者并给予早期积极治疗至关重要。近年来降钙素原作为炎症及感染的标志物受到广泛关注,现对降钙素原预测急性胰腺炎感染的动物基础研究、临床研究和抗生素管理方面的研究进行综述。

    Release date:2016-08-26 02:09 Export PDF Favorites Scan
  • YAG Laser Surgery of Lacrimal Passage on Animal

    目的:本文观察了三只做了泪道激光手术的狗泪小管组织,目的是为了解激光术后是否泪道会遗留瘢痕或狭窄。方法:三只成年狗用激光分别点击了泪小点,泪小管,泪囊。30天内取材。结果:泪道上皮及管道未见损害。结论:泪道YAG激光只要掌握能量和点击次数,术后不会遗留瘢痕。

    Release date:2016-09-08 10:14 Export PDF Favorites Scan
  • Establishment of Lung Injury Model Caused by Severe Acute Pancreatitis in Rats with Ligated Pancreatic Duct

    Objective To establish a stable and reliable lung injury model caused by severe acute pancreatitis(SAP)in rats, which is helpful to study the acute lung injury (ALI)and acute respiratory distress syndrome (ARDS) induced by SAP.Methods Sixty Sprague-Dawley rats were randomized into ligature group (n=20), traditional group (n=20),and sham operation group (n=20). SAP model was established through retrograde injection of 5% taurocholic acid. After injection, the pancreatic duct of rats was ligated in ligature group, but not in traditional group. The lung damage and edema at 24 h after operaton and natural course of rats were observed.Results The ALI model of rats induced by SAP was established successfully in ligature group. The rats died of acute respiratory failure within 48 h in ligature group, the mortality was significantly higher than that in traditional group (100% vs.20%),P<0.05. Pleural effusion occurred in four rats in ligature group, while no pleural effusion was found in rats in other two groups. The volume of ascites of rats in ligature group was (21.15±5.33) ml, which was more than that in traditional group 〔(7.75±2.66) ml〕,P<0.05, while no ascites was found in rats in sham operation group. The level of serum amylase of rats in ligature group was (2 470.70±399.73) U/L,which was significantly higher than that in traditional group 〔(1 528.40±289.54) U/L〕 and sham operation group 〔(831.10±93.26) U/L〕,P<0.001. The level of serum albumin of rats in ligature group was (6.90±1.66)g/L, which was significantly lower than that in traditional group 〔(13.10±0.99) g/L〕 and sham operation group 〔(16.20±0.92) g/L〕,P<0.001.The lung wet-to-dry weight ratio (W/D) of rats in ligature group was 6.50±0.23, which was greater than that in traditional group (4.92±0.18) and sham operation group (4.61±0.16), P<0.001. The score of lung histopathologic of rats in ligature group was 29.25±1.07, which was significantly higher than that in traditional group (12.65±1.98) and sham operation group (0),P<0.001. The score of pancreas histopathologic of rats in ligature group was 15.95±0.15,which was significantly higher than that in traditional group (13.75±0.66) and sham operation group (0.13±0.29),P<0.001. Under transmission electron microscope, basement membrane of pulmonary capillary of rats in ligation group was destructive, the nuclei was dissolved, endothelial pinocytotic vesicles was functional active, and tight junctions between capillary endothelial cells were blurred and even ruptured. Moreover, tight junctions between alveolar epithelial cells were destructive. Pathological changes of lung ultrastructure of rats in ligation group were more severe than that in traditional group, while no pathological change of lung ultrastructure was observed in rats in sham operation group. Conclusions Injury process and pathogenesis of ALI or ARDS clinically caused by acute gallstone pancreatitis can be reproduced in this animal model, which is suitable to explore the related mechanisms of ALI caused by SAP and provides good animal model for the study of ALI caused by SAP.

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  • Preparation and Evaluation of Chronic Hindlimb Ischemia of Lewis Rat

    Objective To establish chronic hindlimb ischemia model with suture-occluded method in rats, and then compare the effects of chronic hindlimb ischemia model with acute ischemia model. Methods Models of chronic hindlimb ischemia were established by using suture-occluded femoral artery method. The laser Doppler blood flow analysis and angiography were performed on day 7, 14, 28, 42, and 49 after operation, and then the rats were sacrificed after angiography, respectively, the quadriceps and gastrocnemius of contralateral and ipsilateral (surgical side) were gotten, which were tested by HE staining and α-actin immunohistochemistry staining, and then calculate arteriolar density. Results There were no lameness and limb necrosis after operation in chronic hindlimb ischemia models. Laser Doppler analysis found that chronic hindlimb ischemia models were still maintained in ischemia state on day 49 after operation compared with acute ischemic models. The resluts of HE staining showed no acute necrosis and muscle fibrosis in chronic hindlimb ischemia model group. Chronic hindlimb ischemia models after operation did not appear obvious lameness and limb necrosis. The arteriolar density of quadriceps femoris on day 7 after operation in chronic hindlimb ischemia models were less than that in acute hindlimb ischemia models (0.015 2 vs. 0.036 4). Conclusions Compared with the commonly used acute ischemic models, the duration of arterial limb ischemia in chronic hindlimb ischemia rats, which were established by suture-occluded method, is longer and less likely to be affected by the compensatory mechanisms. So suture-occluded method can provide a new animal hindlimb ischemia model for further study of ischemia angiogenesis mechanism and treatment of severe lower extremity ischemia.

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  • Dynamically Observed Histopathologic Changes of Acute Rejection in Rat Orthotopic Liver Transplantation Model after Tacrolimus Discontinued 

    Objective To observe the dynamic histopathologic changes of acute rejection in rat orthotopic liver transplantation (OLT) model after tacrolimus discontinued and provide some prediction and evaluation data for clinical acute rejection after liver transplantation. Methods Kamada two-cuff technique was used to establish 60 rat OLT model, and male DA rats, male Lewis rats were used as donors and recipients respectively. Therapeutic amount of tacrolimus (0.05 mg/kg, twice per day, continued for 8 d, 1 d before operation and 7 d after operation, intragastric administrated) was administrated to recipients, then continuously half dose was decreased every day beginning from day 8 after operation and tacrolimus administration was stopped on day 13. Liver tissues were collected on day 7, 14, 21, and 28 after liver transplantation. Histopathologic changes and rejection activity index (RAI) of liver tissues were observed, survival time of recipients was calculated. Results Owing to protection effects of tacrolimus, liver tissues displayed no significant histopathologic changes of acute rejection in 7 d after OLT, while typical acute rejection histopathologic changes began to be observed on day 14 after OLT due to tacrolimus discontinuation. On day 14, 21, and 28, RAI were 3.7±0.9, 6.3±0.9, and 8.1±0.7 respectively. Survival time of recipients was (20.85±0.71) d with a median of 21 d. Conclusion Acute rejection could be induced in rat OLT model after tacrolimus discontinuation, and data collected from this model shows some extent of predictive value and assessment value for clinical liver acute rejection.

    Release date:2016-09-08 10:49 Export PDF Favorites Scan
  • Discussion and Experiences in Establishing Rat Models of Cavernous Transformation of Portal Vein

    Objective To explore adaptive condition of preparation of animal model and afford reliable and stable model animal for further research on clinical diagnosis and treatment of cavernous transformation of portal vein (CTPV) by establishment of animal model by partial portal vein stenosis. Methods According to different straight blunttip needles used, 80 healthy Sprague-Dawley rats were randomly averagely divided into 4 groups: sham operation group, gauge 19 (19G) group, gauge 21 (21G) group and gauge 23 (23G) group. Six weeks after model making, pressure measurement and angiography of portal vein and pathological examination of portal vein and its surrounding tissues were used to evaluate portal hypertension and CTPV. Results Six weeks after model making no rat died in sham operation group, while the numbers of died rats in 19G group, 21G group and 23G group were 2, 4 and 16, respectively. No portal hypertension was displayed in sham operation group and 19G group 6 weeks after model making. Portography showed that the portal vein seemed smooth without variceal and dilatation in sham operation group and 19G group. Pathological examination demonstrated that the portal vein walls were not enlarged, endothelial cells were smooth. The smooth muscles of middle membrane were not thickened and adventitia was intact. Portal pressure increased and CTPV formed in 21G group and 23G group 6 weeks after model making. Portography showed that collateral circulation formed around portal vein in 21G group and 23G group. The vessel lumens with different size and irregular shapes were displayed by pathological examination. Within the narrow fibrous septum between there were the lumens the fat cells, scattered lymphocytes and mast cells, etc. The portal vein walls were enlarged notably, endothelial cells were damaged, the smooth muscle of middle membrane were thickened, thrombosis were formed. Conclusion Establishment of CTPV animal models by partial portal vein stenosis is a reliable method. 21G blund-tip needles fits well in the preparation of CTPV, which is reliable and stable with lower mortality.

    Release date:2016-09-08 10:50 Export PDF Favorites Scan
  • Reproduction and Evaluation of Hepatic VX2 Tumor Model in Rabbits

    Objective To establish the model of hepatic VX2 tumor in rabbits and to offer the experimental evidences for the application of the model. Methods The hepatoma model was reproduced with VX2 cell lines in rabbits. The method to reproduce the model was improved. The changes of liver function (ALT, AST and TB) were determined at a different phase. Tumor’s growth and metastases, pathological changes, images and spontaneous survival time of the animal were observed. Results The tumors could grow up to 1.5-2.0 cm in diameter in 3 weeks after implanting. The successful rate of implantation was 100%. Nodular enhanced echo was found in the liver by color ultrasound. CT scans showed the low density foci in liver, while enhanced CT scans demonstrated asymmetrical intensification in the foci. Macroscopic observation showed that the tumors were grayish white in color and felt harder, necrotic foci was present in the center of tumor. Observation with light microscope showed that the tumor cells’ nucleoplasm proportion was great, tumor cells arranged irregularly, and the tumors displayed invasive growth and no obvious envelope around them. Animals’ spontaneous survival time was 40-53 days. The cause for their death was multiple system organ failure. Conclusion In pathological morphology, pathological process and prognosis, the hepaticVX2 tumors in rabbits are similar to human hepatocarcinoma. It has such characteristics as easy reproduction, short growth period, high success rate, high stability and so on. The model is an ideal hepatoma model in animals.

    Release date:2016-08-28 04:43 Export PDF Favorites Scan
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