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OBJECTIVE: To systematically evaluate therapeutic efficacy of modified Cangfu daotan decoction (MCDD) combined with chemical medicine versus chemical medicine alone in the treatment of polycystic ovarian syndrome (PCOS), and to provide evidence-based reference for clinical decision. METHODS: Retrieved from PubMed, Embase, Cochrane Library, CJFD, Wanfang database, VIP and CBM, randomized controlled trials (RCTs) about MCDD combined with chemical medicine [ethynestradiol cycloprogesterone (Diane-35), clomiphene, metformin] (trial group) versus chemical medicine alone (control group) in the treatment of PCOS were collected. After data extraction and quality evaluation with Cochrane 5.1.0 bias risk evaluation tool and Jadad scale, Meta-analysis was conducted for total response rate, serum hormone level (FSH, LH, LH/FSH, testosterone), BMI, ovulation rate and physical signs (hirsutism, acne) by using Stata 14.0 software. Trial sequential analysis(TSA)was conducted by using TSA 0.9 software. RESULTS: A total of 20 RCTs were included, involving 1 484 patients. Results of Meta analysis showed that total response rate [RR=1.13,95%CI (1.02,1.24),P<0.05], serum hormone level {FSH [WMD=-0.59,95%CI(-0.98,-0.20),P<0.05],LH [WMD=-0.95,95%CI(-1.41, -0.52),P<0.05],LH/FSH [WMD=-1.04,95%CI(-1.78,-0.33),P<0.05],testosterone [WMD=-0.93,95%CI(-1.38,-0.28),P<0.05]}, BMI [SMD=-1.01,95%CI (-1.76,-0.27),P<0.05], ovulation rate [RR=1.17,95%CI(1.02,1.34),P<0.05] and physical signs {hirsutism [WMD=-0.48,95%CI(-0.86, -0.10),P<0.05], acne [WMD=-1.16,95%CI(-1.56,-0.75),P<0.05]} of trial group were all better than those of control group, with statistical significance. TSA showed that there are reliable evidences for MCDD combined with chemical medicine in the treatment of PCOS. CONCLUSIONS: Versus chemical medicine alone in the treatment of PCOS, MCDD combined with chemical medicine can improve total response rate and ovulation rate, reduce serum hormone levels, BMI and physical signs.
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OBJECTIVE: To study the mechanism of Prunus persica-Carthamus tinctorius couplet medicine in the treatment of osteonecrosis of the femoral head (ONFH). METHODS: The network pharmacology was adopted. The active components of P. persica -C. tinctorius couplet medicine and ONFH target were screened through TCM systematic pharmacological analysis platform target (TCMSP), DRAR-CPI, hnuman gene database (GeneCards) and online medelian inheritance in man (OMIM) using oral availability of compounds (OB)>30% and drug like (DL)>0.18 as standard. Network topology attribute analysis software Cytoscape 3.6.0 was utilized to construct the active components-ONFH targets network. Target protein interaction network was established on the basis of STRING database, and top 5 target proteins in the list of connectivity were screened, and molecular docking server was used to predict the combination activity of active components from P. persica -C. tinctorius couplet medicine. The biological processes of target gene ontology (GO) and metabolic pathways in Kyoto encyclopedia of genes and genomes (KEGG) were enriched and analyzed by DAVID. RESULTS: A total of 44 active components were screened from P. persica -C. tinctorius couplet medicine, including baicalin, quercetin, etc., and 78 targets related to ONFH including VEGF, VEGI, CRP, etc. Through analysis of molecular docking server, binding activity of active components of P. persica -C. tinctorius couplet medicine to target protein was strong. GO and KEGG pathway enrichment analysis showed that biological process of P. persica -C. tinctorius couplet medicine for ONFH was related with negative regulation of apoptosis process and positive regulation of nuclear factor-κB transcription factor, mainly through regulating secretory glycoprotein signaling pathway, melanogenesis signaling pathway, VEGF signaling pathway, signaling pathway of basal cell carcinoma, adenosine-activated protein kinase signaling pathway. CONCLUSIONS: This study preliminarily validates the major targets and pathways of P. persica -C. tinctorius couplet medicine for ONFH, which lay a foundation for further study on their pharmacological action.
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OBJECTIVE: To investigate the effects and its mechanism of calcium phosphate bone cement (CPC) loading total flavonoids of Davallia mariesii on osteogenic differentiation of induced membrane in rats. METHODS: Drug-loading CPC and drug-loading polymethyl methacrylate (PMMA) cement were prepared with the contents of Qianggu capsules (total flavonoids of D. mariesii as active ingredient) using CPC and PMMA cement as carrier. Totally 64 male SD rats were randomly divided into drug-loading CPC group, drug-loading PMMA cement group, no-drug CPC group, no-drug PMMA cement group, with 16 rats in each group. The femur of rats was separated and osteotomized to prepare bone defect model, and then the corresponding bone cement was implanted. Four weeks after modeling, the induced membranes of rats were cut and protected. Bone cement was taken out and autogenous cancellous bone was implanted. At the 4th week after modeling, X-ray photographs were taken on the hind limb bones of rats. At the 4th week after modeling and 6th week after bone grafting, induced membranes and new bone were taken from the bone defect area of rats respectively. HE staining was used to observe the morphology of induced membrane, and the width of bone rabecular and the number of osteoblasts of new bone tissue were measured. Immunohistochemistry was used to detect the protein expression of BMP-2 and VEGF in induced membrane. Western blotting assay was used to detect the protein expression of Smad1, Smad4 and Smad7 in new bone. RESULTS: Compared with other 3 groups, the degradation of bone cement in drug-loading CPC group was more obvious in the bone defect areas, which showed that the formation of induced membrane was observed and the bone defect areas were smaller; capillary endothelial cells were abundant and orderly arranged in the induced membranes, and the width of bone trabeculae and the number of osteoblasts in the new bone tissue increased significantly (P<0.05); the protein expression of BMP-2 and VEGF in the induced membrane, the protein expression of Smad1, Smad4 and Smad7 in new bone were increased significantly (P<0.05). CONCLUSIONS: CPC loading total flavonoids of D. mariesii promotes the formation of induced membrane osteoblast in bone defect model rats, which may be associated with regulating osteoblast differentiation by activating BMP-2/Smad pathway; at the same time, it can promote bone healing by promoting the differentiation of vascular endothelial cells, accelerating the formation of capillary network and increasing the expression of vascular endothelial cells.
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OBJECTIVE: To explore potential mechanism of “Astragalus membranaceus-Draba nemorosa” couplet medicine for heart failure. METHODS: By network pharmacology, based on drug-like and oral bioavailability, the active components of “A. membranaceus-D. nemorosa” for chronic heart failure were screened and the targets of treating chronic heart failure were predicted by using TCMSP,GeneCards database, OMIM database and DRAR-CPI. The active component-chronic heart failure target network was established by Cytoscape 3.6.0 software. The protein-protein interaction network was constructed by utilizing STRING database. Then top 5 targets in the list of connectivity were screened and performed a molecular docking in molecular docking server. Finally, GO bioprocess analysis and KEGG pathway enrichment analysis were performed in DAVID database. RESULTS: The study predicted 28 active components in total, including 20 A. membranaceus and 12 D. nemorosa, such as kaempferol and quercetin, there were four components in common. Totally 92 target gene of active components were obtained, including heat shock protein 90α (HSP90AA1), tyrosine protein kinase SRC gene, etc. Results of GO bioprocess analysis showed an association with mitochondrial electron transport, mitochondrial intima, cytoplasmic sol, extracellular body, mitochondrial matrix and drug response. KEGG pathway enrichment analysis showed a link with MAPK signal pathway, TGF signal pathway, PI3K signal pathway, cAMP signal pathway, protein kinase B signal pathway, EPK1 signal pathway and NF-κB signal pathway. CONCLUSIONS: “A. membranaceus-D. nemorosa” couplet medicine exerts therapeutic effects on heart failure from multiple targets as HSP90AA1, SRC and mitochondrial electron transport and MAPK signaling pathway. The study can provide reference for further researches on its material basis and mechanism.
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OBJECTIVE: To study the effects of Tiaopi huxin prescription (TPHXP) on the atherosclerosis (AS) of ApoE-/- mice, and to investigate its mechanism. METHODS: Forty male ApoE-/- mice were divided into blank group, model group, simvastatin group (positive control, 5 mg/kg) and TPHXP low-dose and high-dose groups (50, 150 mg/kg), with 8 mice in each group. Except that blank group was given common diet, other groups were given high-lipid diet to induce AS model. After modeling, administration groups were given relevant medicine intragastrically, and blank group and model group were given constant volume of normal saline intragastrically, once a day, for consecutive 12 weeks. After last medication, the serum levels of TC, TG, LDL-C and HDL-C were determined by spectrophotometry. The serum level of NO was detected by nitrate reduction method. The serum levels of IL-6 and VCAM-1 were determined by ELISA. After separating thoracic aorta, HE staining was used to observe the formation of plaque in the thoracic aorta of mice in each group, and the corrected plaque area was calculated. Western blotting was conducted to determine the expression of NF-κB p65, Cav-1 and eNOS. RESULTS: Compared with blank group, the serum levels of TC, TG, LDL-C, IL-6 and VCAM-1 were increased significantly in model group, while the levels of HDL-C and NO were decreased significantly (P<0.01). The plaque of thoracic aorta was obvious and the corrected plaque area were increased significantly (P<0.01). The relative expression of NF-κB p65 and Cav-1 were increased significantly, while the relative expression of eNOS was decreased significantly (P<0.01). Compared with model group, the serum levels of TC, TG and LDL-C in administration groups, the serum levels of IL-6 and VCAM-1 in simvastatin group and TPHXP high-dose group were decreased significantly, while the serum levels of HDL-C and NO were increased significantly in administration groups (P<0.05 or P<0.01). In administration groups, the plaques of thoracic aorta were reduced and the corrected plaque area was decreased significantly (P<0.05 or P<0.01); the relative expression of NF-κB p65 and Cav-1 were decreased significantly, while the relative expression of eNOS was increased significantly (P<0.05 or P<0.01). CONCLUSIONS: TPHXP can regulate the level of blood lipid, decrease the level of inflammatory factors and inhibit the formation of AS plaque, the mechanism of which may be associated with inhibiting Cav-1/NF-κB pathway.