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OBJECTIVE: To investigate the improvement effects of Liqi sanjie granule on liver-qi stagnation model rats. METHODS: According to the weight, totally 80 rats were randomly divided into blank control group (normal saline), model control group (normal saline), Xiaoyao pill control group (positive control a, 750 mg/kg ,calculated by crude drug), Xiaojin pill control group (positive control b, 200 mg/kg, calculated by pill weight), Liqi sanjie pill control group (prototype control, 1 957 mg, calculated by crude drug) and Liqi sanjie granule low-dose, medium-dose and high-dose groups (978.5, 1 957, 3 914 mg/kg, calculated by crude drug), with 10 rats in each group. Each group was given medicine 20 mL/kg intragastrically once a day, for consecutive 21 d. 1 h after per medication, liver-qi stagnation model was established in those groups by binding method except for blank control group. The syrup preference of rats was determined by designing syrup preference test. Rattail suspension test was adopted to determine the hanging immobility time and struggling times of mice. Open-field behavior test was used to determine total behavior score so as to judge the extent of liver-qi stagnation and effect of the drug in rats. RESULTS: Compared with blank control group, hanging immobility time of model control group was significantly prolonged, the syrup preference and the total behavior score of open field test were decreased significantly, with statistical significance (P<0.05 or P<0.01). Compared with model control group, the struggling times of rats were increased significantly in Xiaojin pill control group, Liqi sanjie pill control group and Liqi sanjie granule medium-dose group (P<0.05 or P<0.01); the hanging immobility time of Xiaoyao pill control group, Xiaojin pill control group, Liqi sanjie pill control group, Liqi sanjie granule low-dose and medium-dose groups were shortened significantly; syrup preference and total behavior score of open-field behavior test were increased significantly (P<0.05 or P<0.01). Compared with Liqi sanjie pill control group, the struggling times of rats were decreased significantly and hanging immobility time were prolonged significantly only in Liqi sanjie granule high-dose group (P<0.05 or P<0.01); there was no statistical significance in above indexes of rats in Liqi sanjie granule low-dose and medium-dose groups (P>0.05). CONCLUSIONS: Liqi sanjie granule can significantly improve liver-qi stagnation caused by binding method, and the effects of low-dose and medium-dose Liqi sanjie granule are similar to those of Liqi sanjie pill.
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OBJECTIVE: To study the long-term toxicity of Liqi sanjie extractum in rats after intragastric administration, and to provide reference for safety evaluation before clinical practice. METHODS: A total of 160 rats were randomly divided into control group (normal saline) and Liqi sanjie extractum low-dose, medium-dose and high-dose groups (7.828 0, 15.656 0, 31.312 0 g/kg, calculated by crude drug), with 40 rats in each group. They were given relevant medicine intragastrically once a day from Monday to Saturday. The experimental period was 120 days, and the recovery period was 30 days after the end of the experiment. General information of rats was observed, and body weight and feed consumption of rats were measured once a week. At the 61st day of administration, the end of administration and the end of recovery period, 10, 20 and 10 rats were collected from each group to observe their hematology, blood biochemistry, organ coefficient and histopathology changes. RESULTS: From 61st day to 120th day of administration, the rats of Liqi sanjie extractum high-dose group had hair loss and erection, and recovered after withdrawal of medicine. During medication, the body weight of mice in Liqi sanjie extractum low-dose and medium-dose groups increased faster than control group, while the body weight of rats in Liqi sanjie extractum high-dose group increased slower than control group. Compared with control group, the feed consumption of Liqi sanjie extractum low-dose group increased, while those of Liqi sanjie extractum medium-dose and high-dose groups decreased; the rats were recovered after drug withdrawal. On the 61st day of administration and after the end of administration, some hematological indexes, blood biochemical indexes and organ coefficients of rats in administration group were significantly different from those of control group (P<0.05 or P<0.01). The hematology, blood biochemistry and organ coefficients of rats were basically recovered after the end of the recovery period. The number of erythrocyte, hematocrit, standard deviation of erythrocyte width, albumin, globulin ratio and potassium K+ levels in Liqi sanjie extractum low-dose group were significantly lower than those in control group (P<0.05 or P<0.01). The absolute value of intermediate cells in blood of rats in Liqi sanjie extractum medium-dose group was significantly higher than that of control group (P<0.05), and the mean hemoglobin concentration, K+ and uterine coefficient in blood were significantly lower than those of control group (P<0.05). The number of white blood cells, absolute value of lymphocyte, absolute value of intermediate cells, the percentage of intermediate cells, prothrombin time and spleen coefficient in Liqi sanjie extractum high-dose group were significantly higher than those in the control group (P<0.05 or P<0.01). Mean hemoglobin concentration, granulocyte percentage, albumin, alkaline phosphatase and K+ were significantly lower than those in the control group (P<0.05 or P<0.01). No abnormalities in systemic autopsy and histopathology were noticed in rats. CONCLUSIONS: Long-term intragastric administration of Liqi sanjie extractum can cause certain toxic reactions in rats, and low dose of Liqi sanjie extractum causes less and lighter toxic reactions which can be automatically recovered after drug withdrawal. It can provide reference for the determination of clinical safe dose.
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OBJECTIVE: To study the dose-time-effect relationship of Tibetan medicine Rannasangpei in cerebral ischemic- reperfusion injury model rats with intragastric administration. METHODS: The rats were randomly divided into sham operation group (normal saline, 10 mL/kg), model control group (normal saline, 10 mL/kg), positive control group (nimodipine, 30 mg/kg), Rannasangpei different dose groups (0.52, 1.04, 2.08, 4.17, 8.33, 16.67, 33.34, 66.68, 133.36, 266.72 and 533.44 mg/kg), with 18 rats in each group. Each group was given relevant medicine intragastrically once; 25 min after intragastric administration, cerebral ischemic-reperfusion injury model was established with suture-occluded method in those groups except for sham operation group. 24, 48, 72 h after cerebral ischemia, neuroethology of rats were graded in each group. The rate of cerebral infraction was detected to evaluate the optimal effective time, the optimal dose (Dmax) and maximal effect (the rate of minimum cerebral infraction, Emax) of Ratnasampil at different periods of cerebral ischemia. Dose-time-effect relationship of Rannasangpei dose with the rate of cerebral infraction was fitted with Thermo Kinetica 5.1 software. The area under curve (AUClast) and retention dose (MRTlast) of dose-effect curve were calculated, and detect the levels of SOD and MDA. RESULTS: Compared with sham operation group, the neurobehavior of model group was significantly abnormal (P<0.05 or P<0.01), and the rate of cerebral infarction was significantly increased (P<0.01); the level of SOD was decreased significantly (P<0.01, 48 h), and the level MDA was increased significantly (P<0.05, 48 h). Compared with model control group, there was no significant change in neurobehavioral abnormalities in the nimodipine group (P>0.05), and the rate of cerebral infraction was decreased significantly (P<0.01, 24, 48 h). The level of SOD in rats were increased significantly (P<0.01, 48 h), while the level MDA decreased significantly (P<0.05, 48 h). Rannasangpei 2.08-33.34 mg/kg could significantly improved neurobehavioral abnormalities (P<0.05, 24 h); 24 h after cerebral ischemia, the rate of cerebral infraction was decreased significantly in Rannasangpei 4.17-133.36 mg/kg group (the lowest is 33.34 mg/kg group, P<0.05 or P<0.01). The level of SOD in rats were increased significantly in 33.34-533.44 mg/kg groups (P<0.05). the level MDA was decreased significantly in 0.52-2.08, 8.33, 33.34, 266.72 and 533.44 mg/kg groups (P<0.05). Dmax was 33.34 mg/kg, Emax was 3.02%, AUClast was 5 141.76 mg/kg and MRTlast was 329.161 mg/kg. 48 h after cerebral ischemia, the rate of cerebral infraction was decreased significantly in Rannasangpei 2.08-133.36 mg/kg groups (the lowest is 66.68 mg/kg group, P<0.05 or P<0.01), while the level of SOD was increased significantly in 1.04-533.44(except for 4.17)mg/kg groups (P<0.05). The level of MDA was decreased significantly in 16.67-66.68, 533.44 mg/kg groups (P<0.05), Dmax was 66.68 mg/kg, Emax was 2.13%, AUClast was 5 219.36 mg/kg and MRTlast was 340.521 mg/kg. 72 h after cerebral ischemia, the rate of cerebral infraction and the level of MDA had no significant decreased in Rannasangpei groups (P>0.05), and the levels of SOD had no significant increase (except for 0.52 mg/kg group, P>0.05). CONCLUSIONS: The optimal effective time of Rannasangpei for the treatment of cerebral ischemia-reperfusion injury in rats is 48 h, and the Dmax is 66.68 mg/kg. The improvement mechanism may be related to increase the level of SOD and decrease the level of MDA.
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Objective To analyze the occurrence rate of gastrointestinal and pulmonary infection and hospital acquired pneumonia (HAP)in severe craniocerebral injuries in my hospital using proton pump inhibitors (PPIs) ,discuss the right way to use PPIs for severe craniocerebral injuries .Methods The case histories of 141 severe craniocerebral injuries in my hospital from 2011 to 2012 were looked up ,and divided into three groups as follows :the group that never used PPIs(17 cases) ,the group that used PPIs for a long time (59 cases) ,and the group that used PPIs for a short time (65 cases) ,and the risks of getting infected using PPIs were analyzed in those three groups above .Results The patients in PPIs group had a higher risk of gastrointestinal tract infection and HAP ,especially who were treated with PPIs more than 9 days .Adjusted by GCS score ,using PPIs for a long time was a risk factor in different multivariate logistic .Conclusion Using PPIs for a long time might be a risk factor of gastro‐intestinal tract infection and HAP .Therefore ,apart from considering the state of illness ,more attention should be paid to the u‐sing time w hen use PPIs .
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Aim To investigate the effect and mecha-nism of quercetin combined with cisplatin on prolifera-tion and apoptosis of human osteosarcoma cell line MG-63 . Methods MG-63 cells were treated with quercetin alone or combined with cisplatin. Cellular morphologic changes were observed under inverted phase contrast microscope. The effects of proliferation inhibition were assayed by CCK-8 method. The combination effect was judged through Chou-Talaly analysis. The apoptosis ra-tios of cells were analyzed by flow cytometry. The gene expression of Bcl-2 and caspase-3 was detected by RT-PCR assay. The protein expression of Bcl-2 and caspase-3 was measured by Western blot assay. Re-sults Quercetin alone or combined with cisplatin could inhibit the proliferation, but induce the apoptosis of MG-63 cells. Combination of quercetin and cisplatin revealed a synergistic effect on cell proliferation and apoptosis as it reduced the expression of Bcl-2 but en-hanced that of caspase-3 at both gene and protein lev-els. Conclusion Synergistic effect of quercetin com-bined with cisplatin on cell proliferation and apoptosis of MG-63 cells is possibly due to reduction of Bcl-2 and enhancement of caspase-3 expression.
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Objective To explore the speech respiratory characteristics of 7-15 years old children with spastic cerebral palsy and the differences between ordinary children and children with cerebral palsy.Methods The maximum phonation time (MPT) and maximum counting ability (MCA) of 90 ordinary children and 58 children with cerebral palsy aged 7-15 years were measured and a comparison between the 2 groups were conducted.Results (1) Age has significant effects on MPT and MCA of the ordinary children (P <0.05).The MPT and MCA of the ordinary children at the age of 7 ~9 years and 10 ~ 12 years are lower than the ones at the age of 13 ~ 15 years.Age has almost no effects on MPT and MCA of children with cerebral palsy(P >0.05) ; (2)Sex has no significant effects on MPT and MCA of ordinary children and children with cerebral palsy (P >0.05) ; (3) The MPT and MCA of children with cerebral palsy are significantly lower than those of ordinary children (P <0.05).Conclusions The MPT and MCA of ordinary children are increased with the growth of age,especially after the age of 13 years,but the children with spastic cerebral palsy do not show that kind of trend and demonstrate a state of retardation of speech respiratory function.Compared with ordinary children,the children with spastic cerebral palsy are easier to suffer from insufficient respiratory support and poor respiratory-phonatory coordination.
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<p><b>OBJECTIVE</b>To present the authors' experience with percutaneous dilatational tracheostomy (PDT), with special attention to early and late complications, outcomes, and primary disease influence.</p><p><b>METHODS</b>Between November 2000 and May 2001, 22 PDTs were performed with the aid of dilatating forceps in 21 neurosurgical coma patients. A Seldinger wire was introduced through a cannula into the trachea serving as a guide. The guidewire was threaded through the clamped guidewire dilating forceps and the forceps was advanced through the tracheal wall. The trachea was dilated by opening forceps. The guidewire was then threaded through the obturator of the tracheostomy tube and both were advanced into the trachea. Demographic data, patient disease variables and patient anatomical features, as well as perioperative and late complications were recorded prospectively.</p><p><b>RESULTS</b>Completion of the procedure consumed 4 - 16 minutes (mean, 12 minutes). The procedure caused complications in 3 operations: 2 cases of stomal bleeding, 1 of intratracheal bleeding, but there was no severe tracheal injury or mediastinal emphysema. Furthermore, none of the cases required intervention due to complications. All patients were followed up for 1 to 6 months. Tracheostomy tubes were removed in 16 patients. All cervical incisions were closed with cosmetic demand. Two patients with tracheostomy tubes were retained for primary diseases. Causes of death in 3 others were unrelated to the PDT. No patient developed tracheomalacia or tracheal stenosis as a late complication.</p><p><b>CONCLUSIONS</b>Percutaneous dilatational tracheostomy is a fast, safe and simple procedure for neurosurgical coma patients and can be safely performed by neurosurgeons.</p>