Blocking beta 2-adrenergic receptor inhibits dendrite ramification in a mouse model of Alzheimer's disease

Dendrite ramification affects synaptic strength and plays a crucial role in memory. Previous studies revealed a correlation between beta 2-adrenergic receptor dysfunction and Alzheimer＇s disease （AD）, although the mechanism involved is still poorly understood. The current study investigated the potential effect of the selective β2-adrenergic receptor antagonist, ICI 118551 （ICI）, on Aβ deposits and AD-related cognitive impairment. Morris water maze test results demonstrated that the performance of AD-transgenic （TG） mice treated with ICI （AD-TG/ICI） was significantly poorer compared with NaCl-treated AD-TG mice （AD-TG/NaCl）, suggesting that β2-adrenergic receptor blockage by ICI might reduce the learning and memory abilities of mice. Golgi staining and immunohistochemical staining revealed that blockage of the β2-adrenergic receptor by ICI treatment decreased the number of dendritic branches, and ICI treatment in AD-TG mice decreased the expression of hippocampal synaptophysin and synapsin 1. Western blot assay results showed that the blockage of β2-adrener- gic receptor increased amyloid-β accumulation by downregulating hippocampal a-secretase activity and increasing the phosphorylation of amyloid precursor protein. These findings suggest that blocking the β2-adrenergic receptor inhibits dendrite ramification of hippocampal neurons in a mouse model of AD.

Activation of β_2-Adrenergic Receptor Induced by Three Catecholamine Agonists:a Docking and Molecular Dynamics Study

We studied the activation of β2-adrenergic receptor（β2AR） by norepinephrine, epinephrine and isoprote- renol using docking and molecular dynamics（MD） simulation. The simulation was done on the assumption that β2AR was surrounded with explicit water and infinite lipid bilayer membrane at body temperature. So the result should be close to that under the physiological conditions. We calculated the structure of binding sites in β2AR for the three ac- tivators. We also simulated the change of the conformation ofβ2AR in the transmembrane regions（TMs）, in the mo- lecular switches, and in the conserved DRY（Aspartic acid, Arginine and Tyrosine） motif. This study provides detailed information concerning the structure ofβ2AR during activation process.

Beta-adrenergic receptor polymorphisms: A basis for pharmacogenetics

Aims: Polymorphisms of the β-adrenergic receptor, the frequency of which may differ in ethnic groups, alters β-receptor function. The aim of this study was to elucidate the frequency of β1 and β2-adrenergic receptor polymorphisms in healthy Greeks and to compare with those of Caucasian European (Euro) and African American (AA) origin. Methods: Ninety-nine individuals with a median age of 63 without clinical evidence of any disease were studied. Blood samples were obtained and common β1 and β2-adrenergic receptor polymorphisms that change the en-coded amino acid were determined by pyrosequencing. Results: The most common β1-adrenergic receptor polymorphism in Greeks is nucleotide substitution cytosine for guanine at position 1165 (1165 C/G) resulting in amino acid substitution arginine for glycine at position 389 (389 Arg/Gly) with a minor allele frequency of 28% (Euro 27%, AA 42%);this polymorphism increases the sensitivity of the β1-receptor. The most common β2-adrenergic receptor polymorphism in Greeks is the nucleotide substitution guanine for adenine at position 46 (46 G/A) resulting in amino acid substitution glycine for arginine at position 16 (16 Gly/Arg) with a minor allele frequency of 38% (Euro 41%, AA 50%);this polymerphism facilitates receptor down-regulation during chronic adrenergic stimulation. Conclusion: The most common β1 and β2-adrenergic receptor polymorphisms in the Greek population are similar to those of other European ancestry, and less common than in those of African origin indicating variability in ethnic groups. This information provides insight into common polymorphisms that may assist in optimizing β-antagonist and agonist therapy.

Effects ofβ_2-Adrenergic Antagonist on Cytosolic Ca^(2+) in Ventricular Myocytes from Infarcted Rat Heart

Objectives To investigate the effects of β2-adrenergic antagonist on cytosolic Ca^2 ＋ （[Ca^2＋ ]i） in ventricular myocytes from infarcted rat heart. Methods A ligature was placed around left anterior descending coronary artery of rat hearts. Rats in the control group were sham-operated. Cardiomyocytes were dissociated at two, four, eight weeks after myocardial infarction （MI） and [Ca^2＋]i was measured via fura-2 fluorescence. The response of cardiomyocytes to isoproterenol in presence or absence of betal-adrenergic antagonist atenolol, beta2-adrenergic antagonist ICI118, 551 or non-selective β1, 2- adrenergic antagonists propranolol was examined. Results The followings were found that ICI 118, 551 had no significant effects on the rise of [Ca^2＋]i induced by isoproterenol in normal ventricular myocytes （P 〉 0.05）, ICI118, 551 only significantly attenuated the rise of [Ca^2＋]i induced by isoproterenol at four weeks and eight weeks after MI （24.5%±5.7% vs 57.8% ± 13.2%, P〈 0.01; 12.2%±7.9% vs 44.6%±11.3%, P〈 0.01）. Atenolol had suppressive effects only in the control group and the post-MI group of two weeks （P 〈 0.05）, and propranolol had suppressive effects in the control and all the three post-MI groups （P 〈 0.01）. Conclusions Beta2-adrenergic antagonist ICI118, 551 may exert negative effects on Ca^2＋ overload initiated by sympathetic stimulation after MI.

Prognostic Value of Promoter Hypermethylation of Retinoic Acid Receptor Beta (RARB) and CDKN2 (p16/MTS1) in Prostate Cancer

Objective: The molecular mechanism of prostate cancer is poorly understood. The aim of the study was to investigate the prevalence and prognostic value of promoter hypermethylation of retinoic acid receptor beta (RARB) and p16 among benign prostatic hyperplasia (BPH) and prostate cancer patients. Methods: In this case-control study, 63 patients were included in three groups; 21 with BPH as the control group, 21 with prostate cancer and good prognostic factors (based on prostate-specific antigen, Gleason score and stage) as good prognosis group, and 21 with prostate cancer and poor prognostic features as poor prognosis group. The prostate biopsy specimen of each individual was examined for hypermethylation of RARB and p16 promoters by methylation specific PCR (MSPCR). Results: Seven (33.3%) patients with good prognosis and 15 (71.4%) patients with poor prognosis were positive for RARB methylation, which were significantly higher than controls (P <0.0001). p16 promoter methylation was shown in 19.0% and 47.6% patients with good and poor prognosis, respectively. The RARB and p16 promoter methylation in the poor prognosis group was significantly higher than that in the good prognosis group (P =0.02 for RARB and P<0.0001 for p16). Conclusion: Hypermethylation of RARB and p16 promoters may predict prognosis in prostate cancer.

1,25(OH)_(2)D_(3)及VDR敲除对山羊附睾头上皮细胞β防御素家族表达的影响

旨在研究1,25(OH)_(2)D_(3)是否通过VDR途径调节山羊附睾头上皮细胞β防御素基因表达。本试验选取3只6月龄太行黑山羊,分别采集附睾头组织。采用差速贴壁法分离山羊附睾头上皮细胞,用细胞免疫荧光鉴定上皮细胞纯度。添加100 nmol·L^(-1)1,25(OH)_(2)D_(3)处理附睾头上皮细胞以及筛选出敲除效率最高的pCas9/gRNA1质粒载体进行细胞转染,同时设置阴性对照组和空白对照组,每组3个重复孔。附睾头上皮细胞经1,25(OH)_(2)D_(3)处理以及VDR基因敲除后,分别用qRT-PCR检测VDR和17种β防御素基因的表达,用Western blot检测VDR蛋白和3种β防御素蛋白的表达。结果表明,1,25(OH)_(2)D_(3)能极显著提高VDR、gBD124、gBD126和gBD104a的mRNA和蛋白表达(P<0.01),同时极显著提高gBD104、gBD 109tr1、gBD 109tr2、gBD113、gBD116、gBD120、gBD 121以及gBD 123基因的表达(P<0.01),显著提高gBD106、gBD127、gBD 129以及gBD 134基因的表达(P<0.05),而对gBD 110like和gBD 128基因没有显著影响(P>0.05);3个基因敲除载体进行细胞转染后,pCas9-VDR-V1组VDR蛋白表达极显著降低(P<0.01)。VDR基因敲除极显著降低gBD124的mRNA和蛋白表达(P<0.01),显著降低gBD126和gBD104a的mRNA和蛋白表达(P<0.05),同时VDR基因敲除组gBD 109tr1、gBD 109tr2、gBD116、gBD123、gBD127、gBD 128以及gBD 134基因的表达极显著低于其他组(P<0.01),VDR基因敲除组gBD104、gBD106、gBD 120以及gBD 129基因的表达显著低于其他组(P<0.05),而对gBD121、gBD 110like以及gBD 113的相对表达则无显著影响(P>0.05)。综上所述,1,25(OH)_(2)D_(3)可以上调VDR和部分β防御素表达;VDR基因敲除后降低部分β防御素表达,结果表明1,25(OH)_(2)D_(3)通过上调VD/VDR信号通路关键基因VDR的表达调控山羊附睾头上皮细胞部分β防御素表达。

高分辨率CT评分联合血清sTREM-1、HBD-2对老年肺结核患者的预后价值

目的探讨高分辨率CT(HRCT)评分与血清可溶性髓系细胞触发受体-1(sTREM-1)、β-防御素2(HBD-2)联合检测对老年肺结核患者预后的预测价值。方法纳入该院2021年5月至2023年5月收治的132例老年肺结核患者作为研究组,根据预后分为预后良好组96例和预后不良组36例。选取同期行HRCT检查的130例体检健康者作为对照组。采用酶联免疫吸附试验检测血清sTREM-1、HBD-2水平,采用受试者工作特征(ROC)曲线分析HRCT评分及血清sTREM-1、HBD-2水平对老年肺结核患者预后不良的预测价值,采用多因素Logistic回归分析老年肺结核患者预后不良的影响因素。结果研究组HRCT评分及血清sTREM-1、HBD-2水平均高于对照组(P<0.05)。治疗前及治疗后2、6个月,预后良好组HRCT评分及血清sTREM-1、HBD-2水平呈下降趋势(P<0.05),即存在时间效应。治疗后2、6个月,预后不良组HRCT评分及血清sTREM-1、HBD-2水平高于预后良好组(P<0.05),时间和分组因素存在交互效应。HRCT评分及血清sTREM-1、HBD-2水平单独及联合预测老年肺结核患者预后不良的曲线下面积(AUC)分别为0.847、0.743、0.810、0.954。HRCT评分、sTREM-1、HBD-2是老年肺结核患者预后不良的影响因素(P<0.05)。结论HRCT评分联合血清sTREM-1、HBD-2有望作为预测老年肺结核患者预后不良的标志物。

β-2 Adrenergic receptor gene polymorphism and response to propranolol in cirrhosis

AIM: To evaluate the association of β-2 adrenergic receptor(β2-AR) gene polymorphism with response of variceal pressure to propranolol in cirrhosis.METHODS: Sixty-four non-related cirrhotic patients participated in this study and accepted variceal pressure measurement before and after propranolol administration. Polymorphism of the β 2-AR gene was determined by directly sequencing of the polymerase chain reaction products from the DNA samples that were prepared from the patients.RESULTS: The prevalence of Gly16-Glu/Gln27 and Arg16-Gln27 homozygotes, and compound heterozygotes was 29.7%, 10.9%, and 59.4%, respectively.Patients with cirrhosis with Gly16-Glu/Gln27 homozygotes had a greater decrease of variceal pressure after propranolol administration than those with Arg16-Gln27 homozygotes or with compound heterozygotes(22.4% ± 2.1%, 13.1% ± 2.7% and 12.5% ± 3.1%,respectively, P < 0.01).CONCLUSION: The variceal pressure response to propranolol was associated with polymorphism of β 2-AR gene. Patients with the Gly16-Glu/Gln27 homozygotes probably benefit from propranolol therapy.

Association of β3 Adrenergic Receptor and Peroxisome Proliferator-activated Receptor Gamma 2 Polymorphisms With Insulin Sensitivity:A Twin Study

Objective To study the effect of β3 adrenergic receptor （β3AR） Trp64Arg and peroxisome proliferator activated receptor gamma 2 （PPAR72） Prol2Ala polymorphisms on insulin resistance. Methods One hundred and eight dizygotic twin pairs were enrolled in this study. Microsatellite polymorphism was used to diagnose zygosity of twins. Insulin sensitivity was estimated with logarithm transformed homeostasis model assessment （HOMA）. PCR-RFLP analysis was performed to detect the variants. As a supplement to the sib-pair method, identity by state （IBS） was used to analyze the association of polymorphisms with insulin sensitivity. Results The genotype frequencies of Trp64Trg, Trp64Arg, and Arg64Arg were 72.3%, 23.8%, and 3.9%, respectively, while the genotype frequencies of Pro12Pro, Pro12Ala, and Ala12Ala were 89.9%, 9.6%, and 0.5%, respectively. For β3AR Trp64Arg the interclass co-twin correlations of Waist-to-hip ratio （WHR）, blood glucose （GLU）, and insulin （INS）, homeostasis model assessment insulin resistance index （HOMA-IR） of the twin pairs sharing 2 alleles of IBS were greater than those sharing 0-1 allele of IBS, and HOMA4R had statistic significance. For PPAR3t2 Prol2Ala most traits of twin pairs sharing 2 alleles of IBS had greater correlations and statistic significance in body mass index （BMI）, WHR, percent of body fat （PBF） and GLU, but there were low correlations of either insulin or HOMA-IR of twin pairs sharing 1 or 2 alleles of IBS. The combined effects of the two variations showed less squared significant twin-pair differences of INS and HOMA-IR among twins sharing 4 alleles of IBS. Condusions β3AR Trp64Arg and PPAR）,2 Pro 12Ala polymorphisms might be associated with insulin resistance and obesity, and there might be slight synergistic effects between this two gene loci, and further studies are necessary to confirm this finding.

B2 adrenergic receptors and morphological changes of the enteric nervous system in colorectal adenocarcinoma

AIM To study the morphology of the enteric nervous system and the expression of beta-2 adrenergic(B2A) receptors in primary colorectal cancer.METHODS In this study, we included forty-eight patients with primary colorectal cancer and nine patients for control tissue from the excision of a colonic segment for benign conditions. We determined the clinicopathological features and evaluated the immunohistochemical expression pattern of B2 A receptors as well as the morphological changes of the enteric nervous system(ENS). In order to assess statistical differences, we used the student t-test for comparing the means of two groups and one-way analysis of variance with Bonferroni's post hoc analysis for comparing the means of more than two groups. Correlations were assessed using the Pearson's correlation coefficient.RESULTS B2 A receptors were significantly associated with tumor grading, tumor size, tumor invasion, lymph node metastasis(P < 0.05), while there were no statistically significant associations with gender, CRC location and gross appearance(P > 0.05). We observed, on one hand, a decrease of the relative area for both Auerbach and Meissner plexuses with the increase of the tumor grading, and on the other hand, an increase of the relative area of other nervous elements not in the Meissner plexus or in the Auerbach plexus with the tumor grading. For G1 tumors we found that epithelial B2 A area showed an inverse correlation with the Auerbach plexus areas [r(14) =-0.531, P < 0.05], while for G2 tumors, epithelial B2 A areas showed an indirect variation with both the Auerbach plexus areas [r(14) =-0.453, P < 0.05] and the Meissner areas [r(14) =-0.825, P < 0.01]. For G3 tumors, the inverse dependence increased for both Auerbach [r(14) =-0.587, P < 0.05] and Meissner [r(14) =-0.934, P < 0.05] plexuses.CONCLUSION B2 A receptors play an important role in colorectal carcinogenesis and can be utilized as prognostic factors. Furthermore, study of the ENS in colorectal cancer may lead to targeted molecular therapies.

ADRB2基因调控区多态性对SABA治疗儿童哮喘急性发作疗效的影响

目的探究ADRB2基因调控区多态性对短效β2受体激动剂(SABA)治疗儿童哮喘急性发作疗效的影响。方法选取2016年10月-2020年10月就诊于中国人民解放军北部战区总医院的急性轻中度发作且接受SABA治疗7 d的支气管哮喘患儿127例,检测其基因型分布,比较不同基因型患儿治疗后肺功能指标的改善情况和疗效,并考察基因多态性高阶交互作用对疗效的影响。结果127例患儿中,rs2895795位点TT、TA、AA型分别有80、44、3例,rs11168070位点CC、CG、GG型分别有93、32、2例,rs12654778位点GG、GA、AA型分别有41、64、22例,均符合Hardy-Weinberg平衡(P>0.05)。治疗后,rs2895795位点TA型患儿的最高呼气流量占预计值百分比(PEF%pred)、用力呼气75%肺活量时的瞬间流量占预计值百分比(FEF75%pred)改善率均显著低于TT型(P<0.05);rs11168070位点CG型患儿的PEF%pred、FEF75%pred改善率均显著低于CC型(P<0.05);rs12654778位点GA、AA型患儿的PEF%pred改善率均显著低于GG型(P<0.05)。各位点不同基因型患儿治疗前后呼出气一氧化氮差值比较,差异均无统计学意义(P>0.05)。rs2895795位点TT型患儿的显效比例是TA+AA型患儿的2.358倍(P<0.05),ADRB2基因多态性高阶交互作用对哮喘患儿的疗效没有明显影响(P>0.05)。结论支气管哮喘患儿ADRB2基因调控区多态性与SABA用于哮喘患儿急性发作的疗效相关,rs2895795、rs11168070、rs12654778位点野生型患儿的肺功能改善更明显,且rs2895795位点TT型患儿接受SABA治疗的效果更好。

广西黑衣壮族ADRB2基因、IL-4R基因多态性与儿童哮喘发病的关联研究

目的探讨β2肾上腺素受体(ADRB2)基因rs1042713、白细胞介素4受体(IL-4R)基因rs1801275位点的多态性与儿童哮喘的相关性。方法采用临床病例对照法,选取黑衣壮中年龄<16岁的儿童200例。其中哮喘组100例,健康组100例。采用聚合酶连接酶链式反应(PCR-LCR chain reaction)检测ADRB2基因rs1042713、IL-4R基因rs1801275位点多态性,并分析其检测结果。结果(1)ADRB2基因rs1042713、IL-4R基因rs1801275位点均检测出AA、AG、GG三种基因型;(2)ADRB2基因rs1042713、IL-4R基因rs1801275位点基因型在哮喘组与健康组中差异有统计学意义(P<0.05);(3)ADRB2基因rs1042713位点基因型AA、AG+AA和等位基因A可能增加哮喘发病风险,GG+AG可降低哮喘发病风险。IL-4R基因rs1801275位点AG、AG+GG和等位基因G可降低哮喘发病风险,相较杂合子AG,纯合子AA+GG能增加哮喘发病风险。结论(1)广西黑衣壮儿童中存在ADRB2基因rs1042713、IL-4R基因rs1801275位点多态性;(2)ADRB2基因rs1042713、IL-4R基因rs1801275位点可能是广西黑衣壮儿童哮喘发病的相关因子。

Inhibiting 5-hydroxytryptamine receptor 3 alleviates pathological changes of a mouse model of Alzheimer's disease

Extracellular amyloid beta(Aβ) plaques are main pathological feature of Alzheimer’s disease.However,the specific type of neuro ns that produce Aβ peptides in the initial stage of Alzheimer’s disease are unknown.In this study,we found that 5-hydroxytryptamin receptor 3A subunit(HTR3A) was highly expressed in the brain tissue of transgenic amyloid precursor protein and presenilin-1 mice(an Alzheimer’s disease model) and patients with Alzheimer’s disease.To investigate whether HTR3A-positive interneurons are associated with the production of Aβ plaques,we performed double immunostaining and found that HTR3A-positive interneurons were clustered around Aβ plaques in the mouse model.Some amyloid precursor protein-positive or β-site amyloid precursor protein cleaving enzyme-1-positive neurites near Aβ plaques were co-localized with HTR3A interneurons.These results suggest that HTR3A-positive interneurons may partially contribute to the generation of Aβ peptides.We treated 5.0-5.5-month-old model mice with tro pisetron,a HTR3 antagonist,for 8 consecutive weeks.We found that the cognitive deficit of mice was partially reversed,Aβ plaques and neuroinflammation we re remarkably reduced,the expression of HTR3 was remarkably decreased and the calcineurin/nuclear factor of activated T-cell 4 signaling pathway was inhibited in treated model mice.These findings suggest that HTR3A interneurons partly contribute to generation of Aβ peptide at the initial stage of Alzheimer’s disease and inhibiting HTR3 partly reve rses the pathological changes of Alzheimer’s disease.

Jueming Prescription(决明方) Reduces Body Weight by Increasing the mRNA Expressions of Beta3-Adrenergic Receptor and Uncoupling Protein-2 in Adipose Tissue of Diet-Induced Obese Rats

Objective： To investigate the antiobesity effect of Jueming Prescription （决明方, JMP）, a Chinese herbal medicine formula, and its influence on mRNA expressions of beta3 adrenergic receptor （beta3-AR） and uncoupling protein-2 （UCP-2） in adipose tissue of diet-induced obese rats. Methods： Fifty male Sprague-Dawley rats were randomly divided into the normal control group （n=8） that was on a standard chow diet, and the obese model group （n=42） that was on a diet of high fat chow. Two weeks after the high fat diet, 29 obese rats in the obese model group were further randomly divided into 3 groups： the untreated obese model group （n=9）, the met＇formin group （n=10, mefformin 300 mg-kg-1.day-1）, and the JMP group （n=10, JMP 4 g.kg-1.dayl）. After 8-week treatment, body weight, wet weight of visceral fat, and percentage of body fat （PBF） were measured. The levels of fasting blood glucose, serum lipids, and insulin were assessed, and insulin sensitivity index （ISI） was calculated. The adipose tissue section was stained with hematoxylin-Eosin, and the cellular diameter and quantity of adipocytes were evaluated by light microscopy. The mRNA expressions of beta3-AR and UCP-2 from the pet-renal fat tissue were determined by real-time reverse transcription polymerase chain reaction （RT-PCR）. Results： Compared with the obese model group, treatment with JMP resulted in significantly lower body weight, wet weight of visceral fat, PBF, and diameter of adipocytes, and significantly higher level of high-density lipoprotein cholesterol, ISI （all P〈0.01）, JMP increased the mRNA expressions of beta3-AR and UCP-2 from pedrenal fat tissue （P〈0.05, P〈0.01）. Conclusions： JMP could reduce body weight and adipocyte size; and the effect was associated with the up-regulation of beta3-AR and UCP-2 expressions in the adipose tissue and improvement of insulin sensitivity.

雌激素受体β基因沉默对人成骨细胞转化生长因子β1和骨形态发生蛋白2表达的影响

背景:雌激素受体β基因参与骨代谢的研究较少,其对骨代谢的具体调节机制仍不清楚。目的:分析雌激素受体β基因沉默对人成骨细胞转化生长因子β1和骨形态发生蛋白2表达的影响。方法:实验分3组:空白对照组(即h FOB 1.19,未感染任何反转录病毒)、阴性对照组(即含无效干扰片断雌激素受体β-sh RNA-nc)、最佳RNAi组(即ERβ-sh RNA-3)。将前期最佳RNAi组的雌激素受体β-sh RNA反转录病毒载体感染人成骨细胞,通过抗性筛选并扩大培养,利用MTT法检测雌激素受体β稳定抑制后对细胞增殖的影响;随后在雌激素干预下,通过Western blot技术检测雌激素受体β蛋白表达的稳定抑制效率,并使用半定量RT-PCR和Western blot技术检测雌激素受体β稳定抑制后对转化生长因子β1和骨形态发生蛋白2表达的影响。结果与结论:(1)成功筛选出稳定感染ERβ-shR NA-3反转录病毒载体的人成骨细胞,MTT法检测显示雌激素受体β稳定抑制后对细胞的增殖没有明显影响(P>0.05);(2)在雌激素干预下,雌激素受体β蛋白的抑制率为(93.11±0.57)%(P<0.05),且雌激素受体β稳定抑制后对转化生长因子β1 mR NA和蛋白的上调率分别为(26.65±3.81)%和(23.79±3.76)%,骨形态发生蛋白2 mR NA和蛋白的上调率分别为(16.62±1.71)%和(18.08±3.20)%(均P<0.05);(3)结果提示雌激素受体β可能通过调控转化生长因子β1和骨形态发生蛋白2的表达在骨代谢中发挥作用。

β2肾上腺素能受体在乳腺癌细胞中的表达及对侵袭能力的影响

目的:探讨β2肾上腺素能受体(β2 adrenergic receptor,β2-AR)在人乳腺癌细胞株中的表达以及对乳腺癌细胞侵袭能力的影响。方法:RT-PCR法检测10种乳腺癌细胞株及正常乳腺上皮细胞中β2-AR的表达;用脂质体转染法将β2-AR基因转入乳腺癌细胞MDA-MB-435;用细胞侵袭实验(Transwell)检测亲本细胞及转染细胞的侵袭能力。结果:β2-AR在正常乳腺上皮细胞HBL-100及乳腺癌细胞BT-549、HCC1937、BCaP-37中表达;在乳腺癌细胞MDA-MB-435、MDA-MB-435HM、MCF-7、T47D中基本无表达;在乳腺癌细胞MDA-MB-231、MDA-MB-231HM、MDA-MB-468中高表达。细胞侵袭实验证实表达β2-AR蛋白的MDA-MB-231及稳定转染β2-AR基因的细胞克隆MDA-MB-435β2-AR可由β2-AR受体激动剂去甲肾上腺素趋化而定向迁移及侵袭。结论:β2-AR在多种乳腺癌细胞株中表达;转染β2-AR可使乳腺癌细胞的侵袭能力增强。

骨碎补总黄酮对去卵巢骨质疏松模型大鼠血清中瘦素、白细胞介素6、前列腺素E_2及骨组织中β_2-肾上腺素受体的影响

目的:观察骨碎补总黄酮对去卵巢骨质疏松(OP)模型大鼠血清中瘦素(LEP)、白细胞介素6(IL-6)、前列腺素E_2(PGE_2)及骨组织中β_2-肾上腺素受体(ADRB2)的影响。方法:采用双侧卵巢切除法复制OP大鼠模型;造模12周后以双能X线法检测骨矿物质密度(BMD),确定OP模型是否复制成功;用药12周后应用酶联免疫法检测血清中LEP、IL-6和PGE_2的浓度,免疫组化法检测大鼠骨组织中ADRB2的表达。结果:造模12周后,模型组与假手术组相比,多个部位BMD显著下降(P<0.01),提示OP模型复制成功。用药12周后模型组LEP、IL-6和PGE_2较假手术组均有显著增高(P<0.05);骨碎补总黄酮组LEP和IL-6较模型组有明显降低(P<0.01),PGE_2无显著差异(P>0.05);模型组ADRB2表达与假手术组和给药组间比较有显著差异(P<0.05),假手术组和给药组间比较无显著差异(P>0.05)。结论:去卵巢OP大鼠血清LEP、IL-6、PGE_2和骨组织ADRB2表达升高;而骨碎补总黄酮能降低去卵巢OP大鼠血清中LEP、IL-6水平和骨组织ADRB2表达,抑制骨吸收,这可能是骨碎补总黄酮防治OP的作用机制之一。

β_2肾上腺素能受体基因与小儿哮喘的关系

目的 :探讨β2 肾上腺素能受体 (β2 AR)基因与小儿哮喘的关系。方法 :采用聚合酶链反应 (PCR)技术扩增β2 AR 5′端基因片段 ,对 6 5例哮喘患儿和 2 0例正常对照进行分析。结果 :哮喘组中 2 2例及对照组中 6例存在β2 AR基因片段的缺失 ,缺失率分别为 33.8% (2 2 / 6 5 )和 30 % (6 / 2 0 ) ,哮喘组与对照组相比差异无显著性 ,但哮喘组中重度与轻度、中度比较 β2 AR基因缺失率高。结论 :β2 AR基因片段的缺失与哮喘发病无关 ,但与重度哮喘患者的发病有关。

Β_2肾上腺素受体拮抗剂对大鼠心肌梗死后心肌细胞胞浆游离CA^(2+)浓度的影响

目的:观察Β2肾上腺素受体拮抗剂对心肌梗死后心肌细胞胞浆游离CA2+浓度([CA2+]I)的影响。方法:结扎冠状动脉,复制大鼠心肌梗死模型。随机分为心肌梗死后2、4、8周组,正常对照组作假手术。分离大鼠心肌细胞,每组大鼠制备20份样品,再随机分为4小组,分别给予Β2受体拮抗剂ICI118,551、Β1受体拮抗剂阿替洛尔、非选择性Β受体拮抗剂普萘洛尔后,用FURA-2荧光技术测定心肌细胞[C2+]I。结果:心肌梗死后4、8周,ICI118, 551组心肌细胞[CA2+]I增幅显著低于异丙肾上腺素组(24．5％±5．7％ VS 57．8％±13．2％,P<0．01;12．2％±7．9％ VS 44．6％±11．3%, P<0．01);正常对照组和心肌梗死后2周,上述两组心肌细胞[CA2+]I增幅无显著差异(P> 0．05)。正常对照组和心肌梗死后2周,阿替洛尔组心肌细胞[CA2+]I增幅显著低于异丙肾上腺素组(P<0．05);正常对照组及心肌梗死后2、4、8周,普萘洛尔组心肌细胞[CA2+]I增幅均显著低于异丙肾上腺素组(P<0．05)。结论:Β2 受体拮抗剂对于有效抑制心肌梗死后交感神经激动引起的心肌细胞内钙超载可能起重要作用。

心脏β_2,α_1及AT_1受体自身抗体与原发性高血压的相关性(英文)

目的研究受体与自身抗体在高血压发病中的作用机制,探讨抗G-蛋白偶联家族中β2,α1及AT1受体的自身抗体在原发性高血压病程进展中的分布情况。方法应用酶联免疫吸附测定(ELISA)技术,以细胞外第二环表位肽段的合成肽作为抗原,检测50例高血压心脏病、40例单纯高血压和40例正常人血清中抗G-蛋白偶联家族中β2、α1和AT1受体的自身抗体。结果高血压心脏病患者血清中抗G-蛋白偶联型β2、α1和AT1受体自身抗体的阳性率明显高于单纯高血压和正常对照组(χ2=3.85～13.5,P<0.05);高血压心脏病自身抗体阳性的平均几何抗体滴度与单纯性高血压比较无明显差异(t=1.41～1.88,P>0.05),但两组阳性抗体的平均几何滴度均明显高于正常对照组(t=2.51～6.61,P<0.05);高血压心脏病抗β2受体自身抗体阳性患者,其中81%的患者同时具有α1受体的自身抗体;76%的患者同时具有AT1受体的自身抗体;52%的患者存在上述3种受体的自身抗体。结论抗G-蛋白偶联型β2,α1和AT1受体的自身抗体参与原发性高血压的病理生理过程,可能与心肌和血管重构有关。通过检测抗G-蛋白偶联家族中与心血管疾病相关的自身抗体,可能对预测高血压病程及心肌和血管病变程度有一定的参考价值,也可能为临床选择联合降压治疗提供参考依据。