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OBJECTIVE To prepare spider fibroin membrane loaded with Periplaneta americana extract, and investigate its characterization, in vitro drug release property and cytotoxicity. METHODS Using natural spider silk collected from Chilobrachys guangxiensis as raw material, P. americana extract as model drug, the drug-loaded spider fibroin membrane (hereinafter referred to as drug-loaded membrane) was prepared by solvent casting method. The material matrix spider fibroin membrane without P. americana extract (hereinafter referred to as blank membrane) was prepared with same method. The membrane structure was characterized by static water contact angle, Fourier infrared chromatography, X-ray diffraction and scanning electron microscopy from different angles; drug release characteristics in artificial saliva were simulated in vitro to evaluate the drug sustained-release performance. MTT assay was adopted to validate the cytotoxicity of drug-loaded membrane. RESULTS The drug-loaded membrane was prepared, and the static water contact angle was less than 90°, which was less than that of blank membrane. The drug-loaded membrane showed the characteristic absorption peak to polypeptide of P. americana extract at 1 500-1 700 cm-1. X-ray diffraction and scanning electron microscopy also proved that the drug was successfully loaded into the pellicle. The release time of the pellicle in artificial saliva was more than 200 min. The MTT test results showed that the cell proliferation rates of blank membrane and drug-loaded membrane were 84.6% and 79.4% (both greater than 70%), respectively, without significant potential cytotoxicity. CONCLUSIONS Drug-loaded membrane prepared with natural spider silk has a certain sustained-release effect in artificial saliva, which can be further developed as a drug sustained-release carrier with excellent biological characteristics and biocompatibility.
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Objective:To study the clinical features, genetic characteristics and prognosis of neonatal diabetes mellitus (NDM).Methods:From January 2015 to January 2022, neonates with NDM admitted to the Department of Neonatology of our hospital were retrospectively reviewed.Their clinical manifestations, biochemical data, genetic tests, treatments and outcomes were analyzed.Results:A total of 6 cases with NDM were included, with 3 males and 3 females. All 6 cases were full-term infants, 5 were low birth weight infants and 1 had family history of diabetes. High blood glucose were found on 1~11 d (average 4 d) after birth. 3 cases were diagnosed during blood glucose screening for low birth weight and 3 cases were diagnosed due to infection and/or diabetic ketoacidosis. Blood C-peptide levels were below normal range in all 6 cases. Blood insulin levels were decreased in 5 cases and remained at the lower limit of normal range in 1 case. All infants received genetic tests and 4 showed abnormal results, including 2 cases of ABCC8 gene mutation [c.2060C>T (p.T687M), not reported; c.674T>C (p.L225P), reported], 1 case of KCNJ11 gene mutation [c.602G>A (p.Arg201His), not reported] and 1 case of paternal uniparental disomy (UPD)6q24 (reported). All 6 cases were treated with insulin. Glibenclamide was experimented to replace insulin in 3 cases and 1 case was successful. During follow-up (at the age 4 months~5 years old), 4 cases were diagnosed with transient NDM, 1 case with permanent NDM and 1 case died at the age of 4 months without classification. 1 case showed psychomotor and language delay and the others had otherwise normal development.Conclusions:Most NDM infants are low birth weight infants with reduced blood insulin and C-peptide.Transient NDM are common. Proactive genetic testing may help treatment.
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OBJECTIVE:To preliminarily optimize the preparation technology of Ligustrazine pellicle ,and to study its in vitro percutaneous permeation characteristics. METHODS :With the amounts of PVA- 124,ethyl alcohol ,glycerin,tween-80 and azone as factors ,single factor experiment was used to optimize the Ligustrazine pellicle matrix formulation ;modified scoring standard was used to evaluate the film formation time ,film formation ability ,ductility,uniformity and the presence of bubble. On the basis of the optimal matrix formulation ,the pellicle with different loading amount of ligustrazine (300,250,200,150,100,50 mg/mL) was prepared and its maximum loading amount was investigated. HPLC method was adopted to determine the content of ligustrazine,and methodology investigation was conducted. Isolated back skin of rats were collected ,the percutaneous permeation test was conducted for high ,medium and low loading amount (100,75,50 mg/mL)of Ligustrazine pellicle. At 15,30,45,60, 75,90,120,150,180 min,the sample was taken and the permeation rate of ligustrazine was calculated. RESULTS :When the amounts of PVA- 124,ethyl alcohol,glycerin,tween-80 and azone were 2.5 g,7.0 mL,1.97 mL,0.07 mL,0.28 mL(in terms of 50 mL formulation amount ),the optimal matrix formulation of Ligustrazine pellicle was obtained. The maximum drug loading amount of ligustrazine was 100 mg/mL. The linear ranges of ligustrazine was 3.125-100 μg/mL. The specificity,precision, reproducibility,recovery and stability investigation of content determination method of ligustrazine were all in line with the requirements(RSD<2%). The permeation rate of high ,medium and low loading amount of Ligustrazine pellicle were 608.42, 384.19,158.20 μg(/ cm2·h). CONCLUSIONS :According to the optimized formulation ,the prepared Ligustrazine pellicle had a short film forming time ,stable and re liable quality ; the drug-loading amount was up to 100 mg/mL. The pellicle with drug-loading amount of 75 mg/mL had reached the penetration rate range of effective plasma concentration of ligustrazine treatment.
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OBJECTIVE:To investigate the effects of Periplaneta americana extract on the proliferation and apoptosis of human non-small cell lung cancer A 549 cells as well as its possible mechanism. METHODS :The dry bodies of P. americana were soaked with 90% ethanol and eluted with gradient water-methanol by polyamide column chromatography. The 20%,30%,40%, 50%,60%,70%,80%,90% methanol elution sites (YS-A-H)were obtained. MTT method was used to screen the active site , and the inhibition rate of different doses of active site was detected. Flow cytometry was adopted to detect cell apoptosis ,cell cycle and mitochondrial membrane potential of cells after treated with different doses of active site. RESULTS :Half inhibition concentrations of YS-A-H were (95.25±8.42),(129.93±7.24),(221.28±12.68),(275.39±14.87),(276.76±16.32),(31.90± 5.34),(163.15±6.97),(122.81±8.36)μg/mL,respectively. YS-F had the strongest activity. After treated with 3,9,27,81 μg/mL YS-F for 24,48,72 h,cell proliferation inhibitory rate was increased significantly at different time points ;after treated for 48,72 h,that was significantly higher than same group after treated for 24 h;after 72 h treatment ,that was significantly higher than same group after 48 h treatment (P<0.01). There was no significant effect of 24 h treatment of 3 μg/mL YS-F and 72 h treatment of 9 μg/mL YS-F on the percentage of cells in the late stage of necrosis,24 h treatment of 3 μg/mL YS-F on the percentage of cells in G2/M phase and 48 h treatment of 3 μg/mL YS-F on the reduction rate of mitochondrial membrane potential(P>0.05). The percentage of cells in the early stage of apoptosis ,the late stage of apoptosis and the early stage of necrosis ,the late stage of necrosis,as well as the percentage of cells in the Sub-G 0/G1 and S phase at each time point were significantly increased in other different doses groups ,while the percentage of cells in G 0/G1 and G 2/M phase was decreased significantly (P<0.01). In each dose group,the percentage of cells in the early stage of apoptosis ,the late stage of apoptosis and the early stage of necrosis ,the late stage of necrosis (except for the percentage of cells in the late stage of necrosis treated with YS-F 9 μg/mL for 72 h)and the percentage of cells in Sub-G 0/G1 phase,G2/M phase (except for YS-F 27,81 μg/mL for 48 h)after treated for 48,72 h were significantly higher than same group after 24 h of treatment ;the percentage of cells in G 0/G1 phase,S phase and G 2/M phase (except for YS-F 9 μg/mL for 48 h)after treated for 48,72 h were significantly lower than same group after 24 h of treatment (P<0.01);the percentage of cells in the early stage of apoptosis ,the late stage of apoptosis and the early stage of necrosis ,the late stage of necrosis (except for the percentage of cells in the late stage of apoptosis and early stage of necrosis when treated with YS-F 27 μg/mL for 72 h,the percentage of cells in the late stage of necrosis when treated with YS-F 3,9 μg/mL for 72 h were decreased significantly )and the percentage of cells in S phase (except for YS-F 3 μg/mL for 72 h)and Sub-G 0/G1 phase after treated for 72 h were significantly higher than same group after 48 h of treatment ,while the percentage of cells in G 0/G1 and G 2/M phase were significantly lower than same group after 48 h of treatment (P<0.01). After treated with YS-F 9,27,81 μg/mL for 48 h,the reduction rate of cell mitochondrial membrane potential was increased significantly ;YS-F 27,81 μg/mL groups were significantly higher than YS-F 9 μg/mL group,and YS-F 81 μg/mL group was significantly higher than YS-F 27 μg/mL group. CONCLUSIONS:YS-F can inhibit the proliferation and promote the apoptosis of A 549 cells by preventing cell transformation from S phase to G 2/M phase ,and reducing mitochondrial membrane potential ,in time-dependent or dose-dependent manner.
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OBJECTIVE: To investigate the acute toxicity, long-term toxicity, skin irritation and anaphylaxis of Bee venom (BV) plastics, and to evaluate its preclinical safety. METHODS: The acute toxicity of BV plastics to rats was investigated after administration of high-dose, medium-dose and low-dose (144, 96, 48 mg/kg) of BV plastics. The long-term toxicity of BV plastics was investigated by continuous administration of high-dose, medium-dose and low-dose (72, 48, 24 mg/kg) of BV plastics for 28 days. The irritation of intact and damaged skin in rabbits with 8 mg/kg BV plastics was investigated by using the self-control method of left and right homologous body. The skin anaphylaxis of guinea pig were investigated after sensitized with 15 mg/kg BV plastics on the left back (on 0, 7th, 14th day) and stimulated with 15 mg/kg BV plastics on the right back. RESULTS: During the acute toxicity experiment with BV plastic,the weight of rats and the changes of viscera were normal,and there was no relevant toxic reaction. Long-term toxicity test results showed that no significant pathological changes were observed at 24 h after the last administration; the spleen index of rats in BV low-dose group, testicular index in middle-dose group and epididymis index in high-dose and middle-dose groups were significantly increased, while PT in plasma of rats in BV medium-dose and low-dose groups was significantly prolonged (P<0.05). There were no abnormal changes in organ appearance, other organ index, coagulation index and blood biochemical index. All above indexes became normal at the end of 2-week recovery period. Skin irritation test showed that BV plastics could cause slight erythema and obvious scab on the skin of rabbits which along with little irritation on intact or damaged skin. Skin anaphylaxis test showed that BV plastics produced mild erythema in the skin of guinea pigs, belonging to light allergy. CONCLUSIONS: No acute or long-term toxicity is observed after transdermal administration of BV plastics, which is safe and only causes mild irritation and irritability to skin, indicating there is good safety of the plastic under experiment doses.
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OBJECTIVE: To observe improvement effects of fingolimod on middle cerebral artery occlusion/reperfusion (MCAO/R) injury model rats. METHODS: Male SD rats were randomly divided into sham operation group, model group and fingolimod low-dose, medium-dose and high-dose groups (0.5, 1, 2 mg/kg), with 8 rats in each group. Except for sham operation group, MCAO/R injury model was induced by suture-occluded method in other groups. Administration groups were given relevant medicine intragastrically after reperfusion [1 h after reperfusion (1st day), 22.5 h after reperfusion (2nd day), and then every 24 h until 142.5 h of reperfusion (7th day)]. Sham operation group and model group were given constant volume of normal saline intragastrically, once a day, for consecutive 7 d. The scores of neurological deficit and balance beam test, the times of memory error [work memory error (WME), reference memory error (RME) and total error] were recorded in each group. The contents of serum inflammatory cytokines (IL-6, IL-8, IL-10, TNF-α) were determined by ELISA, and triphenyl tetrazolium chloride staining method was used to detect the rate of cerebral infarction. RESULTS: Compared with sham operation group, neurological deficit scores (at different time points of 1st-7th day after administration), balance beam test scores (2nd, 4th, 7th day after administration), times of memory error (2nd, 4th, 7th day after administration), the contents of serum inflammatory cytokines and the rate of cerebral infarction were increased significantly in model group (P<0.05 or P<0.01). Compared with model group, neurological deficit scores (low-dose group at different time points of 3rd-7th day, medium-dose and high-dose groups at different time points of 2nd-7th day after administration), balance beam test scores (low-dose group at 7th day, medium-dose group at 4th and 7th day, high-dose group at 2nd, 4th, 7th day), RME times and total error times (low-dose group at 4th and 7th day, medium-dose group and high-dose group at 2nd, 4th, 7th day after administration), WME times (administrations groups at 7th day after administration), serum contents of IL-6, IL-8 and IL-10 (administrations groups), serum contents of TNF-α (medium-dose and high-does groups) and cerebral infarction rate (medium-dose and high-dose groups) were all decreased significantly (P<0.05 or P<0.01). CONCLUSIONS: Intragastric administration of fingolimod can significantly reduce neurological deficit score, balance beam test score and the times of memory error in MCAO/R injury model rats, and has a protective effect on cerebral tissue and memory function. These effects may be related to the down-regulation of inflammatory cytokines such as IL-6 and TNF-α by fingolimod.
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OBJECTIVE: To study the improvement effects of Bee venom(BV) plastics on experimental cerebral thrombosis in rats. METHODS: Totally 96 SD rats were randomly divided into sham operation group (normal saline), model group (plastics blank matrix), Nimodipine group (positive drug, 4.00 mg/kg) and BV plastics low-dose, medium-dose, high-dose groups (1.67, 3.33, 6.67 mg/kg), with 16 rats in each group. Rats in sham operation group and Nimodipine group were given medicine intragastrically, while rats in model group and BV plastics groups were given medicine by transdermal smearing. After 5 days of continuous administration, the experimental cerebral thrombosis model was established by ligating the right external carotid artery and pterygomandibular artery, and injecting compound thrombus inducer into the internal carotid artery. The wet mass ratio of right brain to left brain was measured to investigate the degree of brain edema on the infarcted side. The content of Evans blue (EB) in the left and right hemispheres of rats was determined by ultraviolet spectrophotometry to investigate the cerebral vascular permeability. Blood rheology and coagulation function indicators of rats were measured. The pathological changes of brain tissue in rats were observed by HE staining, and the number of survival neuron cells was counted. RESULTS: Compared with the indexes of sham operation group, the cerebral thrombosis model was established successfully. Compared with model group, the area of blue staining in the right brain (infarcted side) of rats in BV plastics groups was significantly reduced, and the right brain/left brain wet mass ratio and the content of EB in the right brain tissue were significantly reduced (P<0.05 or P<0.01). The whole blood viscosity and Casson viscosity of rats in BV plastics groups, and the plasma viscosity of rats in BV plastics medium-dose and high-dose groups decreased significantly (P<0.01). PT and APTT of rats were prolonged significantly in BV plastics medium-dose group (P<0.01). The pathological changes of brain tissue in rats in BV plastics groups were significantly alleviated. The arrangement of neuron cells was more orderly, the shape and structure of cells were clear, the nucleolus was clear, the membrane was intact, and the number of survival neuron cells was significantly increased (P<0.01). CONCLUSIONS: BV plastics can alleviate brain edema, inhibit cerebral vascular permeability, improve hemorheology and coagulation function indicators of rats after the formation of cerebral thrombosis, and alleviate nerve cell injury after ischemia.
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Objective To study the association between leptomeningeal anastomosis (LMA) collateral circulation and cerebral infarction in patients with middle cerebral artery (MCA) M1-segment stenosis by observing the compensatory characteristics of LMA collateral circulation.Methods One hundred and fourteen MCA M1-segment stenosis patients were divided into cerebral infarction group (n=68) and cerebral infarction-free group (n=46).The hemilateral phenomenon of homolateral anterior cerebral artery (ACA) stenosis and posterior cerebral artery stenosis was assessed and its effect on the incidence of cerebral infarction was studied according to its magnetic resonance angiography.Results The ACA score and MCA stenosis severity were significantly different between cerebral infarction group and cerebral infarction-free group (P<0.05).Multivariate logistic regression analysis showed that low ACA score and MCA M1-segment stenosis were two independent risk factors for cerebral infarction (OR =0.390,95% CI:0.154-0.987;OR =2.421,95%CI:1.324-4.428,P<0.01).Conclusion The incidence of cerebral infarction is low in MCA M1-segment stenosis patients with good ACA collateral circulation.
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Diabetes,so-called“emaciation-thirst disease”in traditional Chinese medicine(TCM),is a prevalent chronic dis?ease with complicated etiology,incurable and multiple complications,as well as extremely high morbidity and mortality. TCM pays at?tention to tackling the problem in the treatment of emaciation-thirst disease,and many prescriptions are single animal medicine or con?tain animal-original drug;animal-original drugs possess stasis and other unique characteristics and therapeutic effects. Based on the current anti-diabetic drugs,the review gives an in-depth summary and analysis on the single animal-original drugs derived from the complexes of TCM in the treatment of diabetes according to their mechanism of action,with the aim to provide reference for developing new animal-original drugs to treat diabetes.
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Medical insects are an important part of traditional Chinese medicine, their biomedical research and development of insects are gaining attention. The research and application of insect sex pheromone in this area also draws great attention. Currently, in-sect sex pheromone is mainly used for pest control in agroforestry. The review briefly describes the chemical constituents, release, and application of insect sex pheromones;meanwhile, the application of insect sex pheromone and its uses in mass trapping, mating disrup-tion, and pest control, in the insect resources development are preliminarily discussed.
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The recent research progress of the utilization of natural drugs for the treatment of liver fibrosis in China and other countries was reviewed. Forty reported remedies were summarized and classified into 3 categories, that is, the single herbal drugs (rhizome, leaf, fruit, bark, peel, flower, whole plants, and oil), traditional Chinese medicine prescriptions and animal drugs. The future directions of the R&D of new natural drugs against liver fibrosis were discussed and some suggestions were provided.
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Animals , Humans , Biological Products , Therapeutic Uses , Biomedical Research , Methods , China , Drugs, Chinese Herbal , Therapeutic Uses , Liver Cirrhosis , Drug Therapy , Medicine, Chinese Traditional , Methods , PhytotherapyABSTRACT
Objective: To study the apoptosis of T lymphocyte subsets of peripheral blood in systemic lupus erythematosus(SLE)and the correlated pathogenesis.Methods: The percentages of T lymphocyte subsets,the positive expression rates of Fas/FasL on T lymphocyte subsets,and the apoptosis of T lymphocyte subsets were determined by three-colorflow cytometry.The level of serum IL-10 was analyzed by ABCELISA.IL-10 antibody and FasL antibody were added respectively into the 48 hours' culture of 10 SLE patients' PBMCs in vitro,whose serum IL-10 significantly increased, and then, the changes of T lymphocyte subsets of SLE PBMCs were determined by three-colodlow cytometry.Results: 1)In SLE, mainly in hyperactive SLE, the apoptesis of CD4~+ T lymphocytes increased significantly(P<0.05),and the ratio of CD4~+/CD8~+ decreased compared with normal controls,and the abnormal apoptesis of CD4~+ T lymphocytes had a positive correlation with the increased expression rates of Fas/FasL on CD4~+ and CD8~+ T lymphocytes(P<0.05).2)The serum IL-10 level increased significantly in SLE (P<0.01), expecially in hyperactive SLE, and serum IL-10 had a positive correlation with the level of serum anti-dsDNA antibodies, CD4~+/CD8 + ratio, and the positive expression rate of FasL on CD4 * T lymphocytes(P<0.05).3)According to a tracking experiment on two different groups of SLE patients,we found that:with the stabilization of the illness,the level of serum IL-10 decreased significantly, the positive expression rate of Fas/FasL on T lymphocytes,particularly on CD4~+ T lymphocytes, reduced evidently,and the apoptosis of CD4~+ T lymphocytes decreased(P<0.05).Conclusion: The abnormal activities of T lymphocytes, particularly of CD4~+ T lymphocytes from patients with SLE,which lead to AICD,cause the percentage of CD4~+ T lymphocytes and the ratio of CD4~+/CD8~+ to decrease,disorder immune response, and accelerate the process of SLE.As a key factor in modulating the positive expression rate of Fas/FasL on CD4~+ T lymphocytes,IL-10 plays an important role in causing SLE.
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Objective Effects of Weiyanxiao on basal gastric- acid secretion in anesthetized rats were investigated.Methods pH value of gastric perfusate in rat models of gastric perfusion were detected with a precise acidity meter to evaluated the effects of Weiyanxiao on basal gastric- acid secretion and gastrin- induced acid secretion.Results Small- dose Weiyanxiao (12.3 g/kg) had no significant influence on basal gastric- acid secretion and has slight inhibition on high- level gastric- acid secretion induced by gastrin ;large- dose Weiyanxiao (24.6g/kg) could restrain basal gastric- acid secretion (P
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Objective To observe the clinical effect of Chi nese herbs Biejia Ruangan pill(BRP)on fibrosis in chronic hepatic B.Methods Ninety -eight patients with liver fibrosis of chronic hepatitis B were ra ndomly divided into two groups of BRP ,treatment group and co ntrol group,in which clinical manif estation scoring,liver function an d serum marker of hepatic fibrosis were obse rved.Results BRP could obviously improve the clin ical manifestation scoring,liver function and serum marker of hepatic fibrosis as compared with the contro l group.Conclusion Chinese herbs BRP could treat liver fibrosis of chronic hepatitis B effectively.
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Objective:To study the apoptosis of T lymphocyte subsets of peripheral blood in systemic lupus erythematosus(SLE) and the correlated pathogenesis.Methods:The percentages of T lymphocyte subsets,the positive expression rates of Fas/FasL on T lymphocyte subsets,and the apoptosis of T lymphocyte subsets were determined by three-colorflow cytometry.The level of serum IL-10 was analyzed by ABC-ELISA.IL-10 antibody and FasL antibody were added respectively into the 48 hours' culture of 10 SLE patients' PBMCs in vitro,whose serum IL-10 significantly increased,and then,the changes of T lymphocyte subsets of SLE PBMCs were determined by three-colorflow cytometry.Results:1) In SLE,mainly in hyperactive SLE,the apoptosis of CD4+ T lymphocytes increased significantly(P