BACKGROUND:As a multifunctional histone acetyltransferase,E1A binding protein P300(EP300)is widely involved in biological processes such as gene expression regulation,cell growth and differentiation,and has been associated with a variety of inflammatory and immune-related diseases.However,its specific role in the pathogenesis of allergic rhinitis is unclear.OBJECTIVE:To explore the changes in gene expression related to allergic rhinitis,analyze its association with programmed cell death,and search for potential biomarkers and therapeutic targets.METHODS:(1)Gene expression data of patients with allergic rhinitis and the control group were collected from the GSE51392,GSE43523 and GSE206149 datasets.Differentially expressed genes were screened and weighted gene co-expression network analysis was performed.(2)From March 2022 to May 2024,10 patients with allergic rhinitis who underwent vidian neurectomy and 10 healthy controls were recruited from the Fifth Affiliated Hospital of Xinjiang Medical University.Blood and nasal mucosal tissue samples were collected from the patients before and after surgery.(3)A rat model of allergic rhinitis was established and EP300 was knocked down.The rats were divided into control group,model group,model+shEP300-NC group,and model+shEP300 group.ELISA,hematoxylin-eosin staining,RT-qPCR and western blot assay were used to detect the levels of inflammatory factors,pathological changes in nasal mucosal tissues,and the expression of related genes and proteins.RESULTS AND CONCLUSION:(1)A total of 43 intersection genes were identified between allergic rhinitis and the control group.Weighted gene co-expression network analysis revealed that the Green module was strongly correlated with allergic rhinitis.Through intersection analysis with genes related to programmed cell death and common differentially expressed genes,the key gene EP300 was obtained.(2)Compared with the preoperative status of patients with allergic rhinitis,the levels of interleukin-4,interleukin-5,interleukin-13,EP300,LC3B,Beclin1,cleaved-Caspase were significantly decreased,while the expressions of p62 and Bcl2 in nasal mucous tissue were significantly increased after surgery.(3)Compared with the control group,the levels of interleukin-4,interleukin-5,interleukin-13,EP300,LC3B,Beclin1,and cleaved-Caspase were significantly increased,while the expressions of p62 and Bcl2 in nasal mucous tissue were significantly decreased in the model group.Compared with the model group,the above indicators had opposite changes.To conclude,EP300 can participate in allergic rhinitis by regulating inflammation,autophagy and apoptosis.

BACKGROUND:As a multifunctional histone acetyltransferase,E1A binding protein P300(EP300)is widely involved in biological processes such as gene expression regulation,cell growth and differentiation,and has been associated with a variety of inflammatory and immune-related diseases.However,its specific role in the pathogenesis of allergic rhinitis is unclear.OBJECTIVE:To explore the changes in gene expression related to allergic rhinitis,analyze its association with programmed cell death,and search for potential biomarkers and therapeutic targets.METHODS:(1)Gene expression data of patients with allergic rhinitis and the control group were collected from the GSE51392,GSE43523 and GSE206149 datasets.Differentially expressed genes were screened and weighted gene co-expression network analysis was performed.(2)From March 2022 to May 2024,10 patients with allergic rhinitis who underwent vidian neurectomy and 10 healthy controls were recruited from the Fifth Affiliated Hospital of Xinjiang Medical University.Blood and nasal mucosal tissue samples were collected from the patients before and after surgery.(3)A rat model of allergic rhinitis was established and EP300 was knocked down.The rats were divided into control group,model group,model+shEP300-NC group,and model+shEP300 group.ELISA,hematoxylin-eosin staining,RT-qPCR and western blot assay were used to detect the levels of inflammatory factors,pathological changes in nasal mucosal tissues,and the expression of related genes and proteins.RESULTS AND CONCLUSION:(1)A total of 43 intersection genes were identified between allergic rhinitis and the control group.Weighted gene co-expression network analysis revealed that the Green module was strongly correlated with allergic rhinitis.Through intersection analysis with genes related to programmed cell death and common differentially expressed genes,the key gene EP300 was obtained.(2)Compared with the preoperative status of patients with allergic rhinitis,the levels of interleukin-4,interleukin-5,interleukin-13,EP300,LC3B,Beclin1,cleaved-Caspase were significantly decreased,while the expressions of p62 and Bcl2 in nasal mucous tissue were significantly increased after surgery.(3)Compared with the control group,the levels of interleukin-4,interleukin-5,interleukin-13,EP300,LC3B,Beclin1,and cleaved-Caspase were significantly increased,while the expressions of p62 and Bcl2 in nasal mucous tissue were significantly decreased in the model group.Compared with the model group,the above indicators had opposite changes.To conclude,EP300 can participate in allergic rhinitis by regulating inflammation,autophagy and apoptosis.

To summarize Professor TU Jinwen's clinical experience in the treatment of severe influenza based on the “heat toxin theory”. He believed that “heat toxin” is the main disease mechanism of severe influenza， emphasized the pathogenesis process that toxin enters with the pathogenic qi， heat generates by the toxin， and changes initiate from the toxin， and proposed simultaneous treatment of warmth and toxin and combination of multiple methods as the treatment principles. Syndrome differentiation in clinic should combine with wei-qi-ying-blood. The disease in the early stage located in wei （defensive） and qi level， treated by clearing heat and resolving toxins， releasing the exterior and expelling pathogen， harmonizing the exterior and interior， dredging the bowels with diarrhea， and combining other methods to get rid of the heat and toxin， and modified Self-Prescribed Tuire No. 1 Formula （自拟退热1号方） is recommended； the disease in progression stage located in ying-blood， treated by relieving heat and resolving toxins， and clearing the ying level and cool the blood， with prescriptions as modified Self-Prescribed Tuire No. 1 Formula plus Qingying Decoction （清营汤）， or Xijiao Dihuang Decoction （犀角地黄汤）； the disease in the late stage with of yin fluid consumption， and heat toxin in the blood level， treated by eliminating heat and resolving toxins， and enriching yin and cooling the blood， with prescriptions as modified Shashen Maidong Decoction （沙参麦冬汤） and Zhuye Shigao Decoction （竹叶石膏汤）. At the same time， it is emphasised that heat-clearing and fire-draining method and harmonising methods are important， and that dispelling pathogen should not injure healthy qi， and that the selection of prescriptions and medicines need consider syndrome differentiation and treatment.

目的：分析Claudin-2蛋白在食管鳞癌（esophageal squamous cell carcinomas，ESCC）组织中的表达及其与患者临床病理特征、5年生存率的关系，探索其对ESCC细胞KYSE450的增殖、迁移和侵袭的影响。方法：选取河南省肿瘤医院2010至2013年间初治的ESCC患者手术切除肿瘤组织52例及其中20例对应的癌旁组织标本，采用免疫组化和WB法检测Claudin-2的表达并分析其与患者临床病理特征和5年生存率的关系。WB法检测ESCC细胞（KYSE450、KYSE150、KYSE510、KYSE140）和人永生化食管上皮细胞SHEE中Claudin-2的表达，构建Claudin-2 shRNA慢病毒载体并转染KYSE450细胞构建敲低Claudin-2表达的细胞系，进一步通过克隆形成实验、细胞划痕实验及Transwell实验检测敲低Claudin-2对KYSE450细胞增殖、迁移和侵袭的影响。结果：ESCC组织中Claudin-2阳性率显著高于癌旁组织（P<0.05），ESCC组织中Claudin-2的表达与淋巴结转移有关（P<0.05）。Claudin-2表达阳性患者5年生存率显著低于阴性者（P<0.05）。成功构建敲低Claudin-2表达的KYSE450细胞系。sh-Claudin-2组细胞的克隆形成数、伤口愈合率和侵袭细胞数均显著低于sh-NT组和对照组（P<0.05）。结论：ESCC组织中Claudin-2的表达高于癌旁组织，且与患者5年生存率呈负相关，Claudin-2能够增强KYSE450细胞的增殖、迁移和侵袭能力。

Objective:To systematically evaluate the influence of the implementation of essential drug policy ( EDP) on prescrip-tion use rate of antibiotics in primary hospitals. Methods:Based on CNKI, Wanfang and VIP of China journal databases, all litera-tures were adopted including the data of the prescription use rate of antibiotics in primary hospitals. RevMan5. 3 and Stata 12. 0 soft-ware were used to conduct the Meta analysis. Results:Totally 43 literatures were included in the study according to the evaluation se-lection criteria. After the implementation of EDP, the prescription use rate of antibiotics in primary hospitals was decreased, and com-pared with that before the implementation of EDP, the risk difference value was significant [RD= -0. 03,95%CI( -0. 04,-0. 03), P<0. 000 01], while the use rate was still high (46. 16%). The result of Egger’s test indicated the publication bias of the 43 litera-tures was not significant (P=0. 571). However, there was high heterogeneity(I2 =94%,P<0. 000 01)among the different studies. Based on the classification of hospital type and different areas, the results of sub-group analysis showed the differences of study methods in the literatures and regional implementation measures of EDP contributed to the high heterogeneity among the different studies. Con-clusion:In order to reduce the heterogeneity of studies, a unified evaluation criteria for the research quality of the cross-section survey should be established. And special policies related to EDP should be taken to effectively decrease the use rate of antibiotics in primary hospitals.

OBJECTIVE:To investigate the permeability of lomefloxacin through blood-pancreatic barrier in rats.METHO-DS:Lomefloxacin(20mg/kg body weight) was injected through caudal vein.At the given time points,the samples were collected.The concentrations of lomefloxacin in the serum,pancreatic tissue and liver tissue were measured by HPLC.RESULTS:The concentration-time profiles of lomefloxacin could be described as two-compartment model in rats.The peak concentrations in serum,pancreatic tissue and liver tissue were 65.550?g/ml,48.801?g/g and 84.121?g/g at 5 min post-injection respectively.Then the concentrations decreased quickly in all of them.Concentrations in pancreatic tissue were higher than those in serum at 10 min and even at 480 min post-injection.The permeation ratio (PR) through blood-pancreatic barrier was 0.744 at 5 min and rose to 3.817 at 480min.CONCLUSION:After intravenous injection,lomefloxacin can permeate blood-pancreatic barrier satisfactory,therefore it is worthy of being recommended for prevention and treatment of pancreatic infections.