三角帆蚌alpha-2巨球蛋白cDNA全长的克隆及表达特征

alpha-2巨球蛋白是河蚌体内重要的天然免疫因子,参与广泛的免疫防御和调节。通过RACE法克隆了三角帆蚌α2M全长cDNA序列,提交Genbank,获得核苷酸序列登陆号:DQ993157.1。同时,采用生物信息学方法对alpha-2巨球蛋白进行了系统分析。该基因cDNA全长5124bp,其中编码区4836bp,5′端非编码区35bp,3′端非编码区为253bp(含polyA尾31bp),该基因能编码1611个氨基酸,其中前23个氨基酸残基为信号肽序列,成熟蛋白分子量为177571.8u,等电点为5.49。蛋白的不稳定系数为39.53,表明该蛋白是稳定的。在此基础上,以18S作为内标,利用半定量RT-PCR法检测α2M基因在三角帆蚌不同组织和不同生理状态下的表达情况。结果表明,alpha-2巨球蛋白仅在血细胞中有表达,而在外套膜、闭壳肌、肠和性腺中没有表达。经注射大肠杆菌和嗜水气单胞菌12h后,三角帆蚌体内α2M的表达水平都有一定量的升高,证明α2M是三角帆蚌基础免疫系统中的组成部分。本研究丰富了软体动物免疫学研究内容,为三角帆蚌抗病机理提供理论资料。

三角帆蚌alpha-2巨球蛋白活性测定及不同组织的表达

alpha-2巨球蛋白(alpha-2 Macroglobulin,α2M)是一种蛋白酶结合蛋白,是重要的天然免疫因子。利用α2M的作用原理,用三角帆蚌血浆保护胰蛋白酶,后用大豆蛋白酶抑制剂抑制未被保护的胰蛋白酶。利用Na-benzoyl-DL-arg-nine-p-nitroanilide(BAPNA)作为酶底物检测被保护的蛋白酶活性的方法,首次证明了三角帆蚌体内α2M的存在。在此基础上,克隆了α2M基因保守区受体结合区片段,进一步证明了α2M在三角帆蚌体内的存在。同时,还进行了α2M不同组织的表达检测,结果显示,α2M基因在血细胞中有表达,而在外套膜、闭壳肌、肠和性腺中没有表达。

双氢青蒿素对C2株蓝氏贾第鞭毛虫Alpha-7.3giardin基因mRNA表达水平的影响

目的观察双氢青蒿素(dihydroartemisinin,DHA)对C2株蓝氏贾第鞭毛虫(Giardia lamblia)Alpha-7.3giardin(α-贾第素)基因mRNA表达水平的影响,探讨其对蓝氏贾第鞭毛虫骨架蛋白的损伤作用。方法用双氢青蒿素浓度为100μg/mL、200μg/mL的改良TYI-S-33培养基分别培养C2株蓝氏贾第鞭毛虫2h、4h、8h、12h后,以不含药物组为对照,实时荧光定量RT-PCR检测药物作用后Alpha-7.3giardin基因mRNA表达水平的变化。结果双氢青蒿素作用虫体后Alpha-7.3giardin基因mRNA表达水平明显低于对照组,二者有显著性差异。结论双氢青蒿素对C2株蓝氏贾第鞭毛虫Alpha-7.3giardin基因mRNA的表达具有明显的抑制作用,抑制效果与药物浓度和作用时间相关,提示双氢青蒿素对蓝氏贾第鞭毛虫骨架蛋白具有损伤作用。

Alpha-2-HS糖蛋白遗传多态性的研究进展

Heremans最早发现人类α2-HS-糖蛋白（α2-HS-glycoprotein）,称为α2-Z-球蛋白（α2-Z-globulin）。Schmid及Burg继续研究,将其命名为Baα2-糖蛋白（Baα2-glycoprotein）。Schultze等根据这种蛋白质的电泳迁移率（α2）将其命名为α2-HS-糖蛋白。H与S分别是Heremans与Schmid姓氏的第一个字母。α2HS的分子量是49000道尔顿,由A、B两条多肽链组成,两链以二硫链共价结合。A链含282个氨基酸,有4个连接糖的部位,B链含27个氨基酸,只有1个连接糖的部位,即第6个氨基酸残基丝氨酸;与B链连接的糖侧链由涎酸、半乳糖及N-乙酰胺基半乳糖组成,用神经氨酸酶（ncuraminidase,NANA）脱涎酸,可使α2HS的等电点由pH4.5～5.0提高至pH5.5,最近才报道。α2HS的分离与纯化及其生化特征。

The Predictive Value of Baseline HBs Ag Level and Early Response for HBs Ag Loss in Patients with HBe Ag-positive Chronic Hepatitis B during Pegylated Interferon Alpha-2a Treatment

Objective To explore the predictive value of baseline HBs Ag level and early response for HBs Ag loss in patients with HBe Ag-positive chronic hepatitis B during pegylated interferon alpha-2a treatment. Methods A total of 121 patients with HBe Ag-positive chronic hepatitis B who achieved HBs Ag loss were enrolled; all patients were treated with PEG-IFNα-2a 180 μg/week. Serum HBV DNA and serological indicators （HBs Ag, anti-HBs, HBe Ag, and anti-HBe） were determined before and every 3 months during treatment. Results The median treatment time for HBs Ag loss was 84 weeks （7-273 weeks）, and 74.38% （90 cases） of the patients needed extended treatment （〉 48 weeks）. The correlation between baseline HBs Ag levels and the treatment time of HBs Ag loss was significant （B = 14.465, t = 2.342, P = 0.021）. Baseline HBs Ag levels together with the decline range of HBs Ag at 24 weeks significantly correlated with the treatment time of HBs Ag loss （B = 29.862, t = 4.890, P = 0.000 and B = 27.993, t = 27.993, P = 0.005）. Conclusion Baseline HBs Ag levels and extended therapy are critical steps toward HBs Ag loss. Baseline HBs Ag levels together with early response determined the treatment time of HBs Ag loss in patients with HBe Ag-positive chronic hepatitis B during pegylated interferon alpha-2a treatment.

Alpha-2-macroglobulin as a radioprotective agent: a review

Radiation is an important modality in cancer treatment, and eighty percent of cancer patients need radiotherapy at some point during their clinical management. However, radiation-induced damage to normal tissues restricts the therapeutic doses of radiation that can be delivered to tumours and thereby limits the effectiveness of the treatment. The use of radioprotectors represents an obvious strategy to obtain better tumour control using a higher dose in radiotherapy. However, most of the synthetic radioprotective compounds studied have shown inadequate clinical efficacy owing to their inherent toxicity and high cost. Hence, the development of radioprotective agents with lower toxicity and an extended window of protection has attracted a great deal of attention, and the identification of alternative agents that are less toxic and highly effective is an absolute necessity. Recent studies have shown that alpha-2-macroglobulin（α2M） possesses radioprotective effects. α2M is a tetrameric, disulfide-rich plasma glycoprotein that functions as a nonselective inhibitor of different types of non-specific proteases and as a carrier of cytokines, growth factors, and hormones. α2M induces protein factors whose interplay underlies radioprotection, which supports the idea that α2M is the central effector of natural radioprotection in the rat. Pretreatment with α2M has also induced a significant reduction of irradiation-induced DNA damage and the complete restoration of liver and body weight. Mihailovi？ et al. concluded that the radioprotection provided by α2M was in part mediated through cytoprotection of new blood cells produced in the bone marrow; these authors also indicated that an important aspect of the radioprotective effect of amifostine was the result of the induction of the endogenous cytoprotective capability of α2M. The radioprotective effects of α2M are possibly due to antioxidant, antifibrosis, and anti-inflammatory functions, as well as the maintenance of homeostasis, and enhancement of the DNA repair and cell recovery processes. This review is the first to summarise the observations and elucidate the possible mechanisms responsible for the beneficial effects of α2M. The lacunae in the existing knowledge and directions for future research are also addressed.

Combination Therapy with Pegylated Interferon alpha-2b and Adefovir Dipivoxil in HBeAg-positive Chronic Hepatitis B versus Interferon Alone: A Prospective, Randomized Study

Currently available monotherapies of oral nucleoside/nucleotide analogs or interferon are unable to achieve a sustained and effective response in most of patients with chronic hepatitis B（CHB）. The objective of the present study was to compare the efficacy and safety of pegylated interferon（Peg-IFN） alpha-2b plus adefovir dipivoxil combination therapy versus Peg-IFN alpha-2b alone. Sixty-one HBeAg-positive chronic hepatitis B patients were randomized to receive Peg-IFN alpha-2b alone（1.5 μg/kg once weekly） or Peg-IFN alpha-2b plus adefovir（10 mg daily） for up to 52 weeks. Efficacy and safety analyses were performed on all participants who received at least one dose of study medication. The rate of HBeAg seroconversion and undetectable HBV-DNA were evaluated after 52 weeks of therapy. At the end of treatment, 11 of 30（36.7%） patients receiving combination therapy achieved HBeAg seroconversion versus 8 of 31（25.8%） in the monotherapy group（P=0.36）. In contrast, the percentage of patients with undetectable serum HBV DNA was significantly higher in the combination group than in the monotherapy group（76.7% vs. 29.0%, P〈0.001）. Thyroid dysfunction was more frequent in the combination group than in the monotherapy group（P〈0.05）. In HBeAg-positive CHB, combination of Peg-IFN alpha-2b and adefovir for 52 weeks resulted, at the end of treatment, in a higher virological response but without significant impact on the rate of HBeAg seroconversion and possibly an adverse effect on thyroid function.

Treatment of Hepatitis C with Pegylated Interferon Alpha-2a and Ribavirin:Experience from Benin

Background: Viral hepatitis C (HCV) is common in Benin. Untreated, it can be complicated by cirrhosis and hepatocarcinoma, which are sources of death. The objectives of this work were twofold: 1) to evaluate the effectiveness and safety of treatment with classic dual interferon pegylated alpha-2a (IFN) and ribavirin therapy in Benin, and 2) to present problems related to financial accessibility to this treatment. Methods: This was a cross-sectional, descriptive and analytical study, with a retrospective collection of data from November 1, 2010 to December 31, 2015 and prospective collection from January 1, 2016 to July 31, 2016 (7 months). We included all patients treated with IFN + ribavirin for hepatitis C at CNHU/HKM. Sustained virological response (SVR) was defined as undetectable viral load C 6 months after stopping treatment. Safety was appreciated by the search for clinical and hematological adverse effects. Results: One hundred and six patients were followed for HCV, of whom 58 (54.7%) undergoing treatment (26 under standard dual therapy and 32 under direct-acting antivirals). Of the 26 patients under-conventional dual therapy, 12 (46.1%) were genotype 1, 13 (50%) genotype 2 and one (3.9%) genotype 4. In conventional dual therapy, SVR was achieved in 15 (57.7%) patients, including the genotype 4 patient, 4 out of 12 (33.3%) genotype 1 patients, and 10 out of 13 (76.9%) for genotype 2 patients. The most common side effects with this treatment were severe asthenia (23 cases), flu-like symptoms (22 cases), weight loss (21 cases) and neutropenia (22 cases), anemia and thrombocytopenia (20 of 26 cases). The overall cost of treatment per patient was 11,800,624 FCFA for genotypes 1 and 4;and 7,835,048 FCFA for genotype 2. Conclusion: The treatment of HCV with IFN + ribavirin in Benin is effective for genotype 2. But its adverse effects are manifold and its cost is high. The switch to direct-acting antivirals (more effective, better tolerated and less expensive) was therefore necessary.

CHOP-like Regimen in Combination with Rituximab and Peginterferon Alpha-2b in Newly-diagnosed Diffuse Large B-cell Non-Hodgkin＇s Lymphoma： Experience in a Chinese Center

OBJECTIVE To evaluate the efficacy of rituximab combined with CHOP-like regimen with or without IFN in patients newly diagnosed diffuse large B-cell Non-Hodgkin＇s lymphoma （DLBCL）.METHODS From January 2003 to July 2008, 51 patients received CHOP-like chemotherapy （cyclophosphamide 750 mg/m2, epirubicin 80 mg/m2, vindesine 2.8 mg/m2 on day 1, and prednisolone 100 mg/day on day 1 to day 5）. Thirty-one patients received CHOPR-like treatment （rituximab 375 mg/m2 1 day before CHOP-like chemotherapy）. Twenty patients received CHOP-like regimen in combination with peginterferon （pegIFN） （1μg/kg on day 5） and rituximab （on day 6）.RESULTS -The CR （complete remission） rate in the CHOPR-like （with or without pegIFN） group and in the CHOP-like group was 78.4% and 45.1% （P = 0.005）, respectively. The estimated mean time of overall survival （OS） in the CHOPR-like group and CHOP- like group was 58.7 ± 2.8 and 36.4 ±3.4 months, respectively （P = 0.002）. The rates of CR and OR （overall remission） in CHOPR- like with IFN arm were 85.0% and 95.0%, and the rates of those in CHOPR-like without IFN arm were 74.2% and 87.0% （P 〉 0.05）. The estimated mean time of 4-year-PFS （progression- free survival） in CHOPR-like with IFN arm and in CHOPR-like without IFN arm was 62.9 ±3.0 months and 51.0 ± 4.6 months （P = 0.092）, respectively. In the CHOPR-like with IFN arm, no patient relapsed after achieving CR, while the estimated rate of 4-year- DFS （disease-free survival） in the patients who reached CR in the CHOPR-like without IFN arm was （63.4 ± 19.3）% （P = 0.061）. CONCLUSION Rituximab combined with CHOP-like chemotherapy improved the prognosis of DLBCL patients. The IFN may help to improve the quality and duration of response of DLBCL patients treated with rituximab and CHOP-like regimen.

Pain-Relief Effects of Aroma Touch Therapy with <i>Citrus junos</i>Oil Evaluated by Quantitative EEG Occipital Alpha-2 Rhythm Powers

Aroma touch therapy is widely used in clinical fields for alleviating pain-related symptoms;however, few studies have reported the pain-relief mechanisms. The present study aimed to elucidate the analgesic effects of aroma touch therapy with Citrus junos oil based on the quantitative evaluation of deep brain network (DBN) activity using electroencephalogram (EEG) occipital alpha-2 rhythm (10-13 Hz) powers. Experimental investigations were performed with 13 healthy volunteers using the cold pressor task for simulating chronic pain in three different sessions: a baseline session with no therapies, a control session with a touch therapy, and an aroma touch therapy. We have found for the first time that the interviewed pain ratings represented by Numeric Rating Scale (NRS) scores were strongly correlated with a DBN activity index, which was derived from the slow fluctuation components of occipital EEG alpha-2 rhythm powers. The correlation was characterized by a V-shaped curve in the DBN activity index versus the pain rating, i.e., the NRS score, which provided the complete analgesic states (NRS = 0) for some subjects under aroma touch therapy at an appropriate DBN activity index. Such analgesic states were not so strongly correlated with emotional valence. In conclusion, aroma touch therapy may directly modulate DBN activity so that pain-induced outcomes are minimized.

Primary study on correlation betweenβ_2-adrenoceptor haplotypes and asthma in children of Han nationality in Chongqing

Objective:To investigatethecorrelationbetweenβ 2 -adrenergicreceptors(β 2 -AR)haplotypesandasthmaof Hannationalitychildrenin Chongqingregion.Methods:PCRandrestrictionfragmentanalysiswereusedto study16,27lociof theβ 2 -ARpolymorphismin76unrelatedasthmaticchildrenandin100healthychildrenandadultsof Hannationali-ty as control.A statisticalanalysisof thecorrelationbetweenglycine(Gly)16allele,Gly16/glutamine(Gln)27haplotype andasthmaticclinicalstatuswas carriedout.Results:Therewas no significantincreaseof thefrequencyof Gly16and Gln27alleleintheasthmaticgroupas comparedwiththecontrolgroup(P>0.05).Therewasa significantincreaseof the frequencyof Gly16alleleandGly16/Gln27haplotypein severeasthmaticcasesthanin themildandmoderateasthmatic ones(P<0.01,0.05).Conclusion:Itis consideredthatasthmais notcausedby GlyandGlnallelesofβ 2 -ARpolymor-phisms.Gly16alleleandGly16/Gln27haplotypearepossiblycorrelatedwiththeseverityof theclinicalmanifestationsin thechildrenof HannationalityinChongqing.

长链非编码RNA alpha-2-巨球蛋白反义RNA 1靶向微小RNA-106b-5p调控氧化型低密度脂蛋白诱导的人脑微血管内皮细胞损伤

目的探讨长链非编码RNA(lncRNA)alpha-2-巨球蛋白反义RNA 1(A2M-AS1)靶向微小RNA(miR)-106b-5p对氧化型低密度脂蛋白(ox-LDL)诱导的人脑微血管内皮细胞损伤的影响。方法用ox-LDL诱导人脑微血管内皮细胞设为ox-LDL组,正常培养细胞为对照(Ctrl)组;A2M-AS1过表达(pcDNA-A2M-AS1组)、空载体(pcDNA组)、miR-106b-5p抑制剂(anti-miR-106b-5p组)、阴性对照(anti-miR-NC组)、pcDNA-A2M-AS1与对照mimic NC(miR-NC组)、pcDNA-A2M-AS1与miR-106b-5p模拟物(miR-106b-5p mimics组)转染细胞后加ox-LDL处理,n=9;Real-time PCR检测A2M-AS1与miR-106b-5p表达;试剂盒检测丙二醛(MDA)、超氧化物歧化酶(SOD)和过氧化氢酶(CAT)水平;流式细胞术及TUNEL法检测细胞凋亡;双荧光素酶报告基因实验检测A2M-AS1与miR-106b-5p靶向关系;Western blotting检测Bcl-2和Bax蛋白表达量。结果与Ctrl组比较,ox-LDL组A2M-AS1表达水平、SOD和CAT活性、Bcl-2蛋白水平降低,miR-106b-5p表达水平、MDA水平、凋亡率、Bax蛋白水平升高(P<0.05);过表达A2M-AS1或干扰miR-106b-5p降低ox-LDL诱导细胞后MDA水平、凋亡率与Bax蛋白水平,升高SOD、CAT活性和Bcl-2蛋白水平(P<0.05);A2M-AS1靶向miR-106b-5p;上调miR-106b-5p逆转过表达lncRNA A2M-AS1对ox-LDL诱导的人脑微血管内皮细胞损伤的作用。结论A2M-AS1通过靶向miR-106b-5p减轻ox-LDL诱导的人脑微血管内皮细胞损伤。

ERK1/2介导去甲肾上腺素对内皮祖细胞的功能调节

目的探讨去甲肾上腺素(NE)对内皮祖细胞(EPCs)增殖和迁移能力的调节作用及其分子机制。方法将培养的健康成人外周血EPCs用不同浓度的NE、肾上腺素能受体拮抗剂或MAPK信号通道阻滞剂干预,检测EPCs的增殖和迁移能力,以及ERK1/2信号通路的激活情况。结果 NE浓度依赖性地(0.01、0.1、1、10μmol/L)促进EPCs增殖,与对照组比较EPCs分别增加(48.3±23.3)%、(70.5±35.6)%、(82.4±14.9)%和(100.3±48.1)%。α受体拮抗剂酚妥拉明、选择性β2肾上腺能受体拮抗剂I127、JNK抑制剂SP600125和ERK1/2抑制剂A6355能够阻断NE的促增殖作用;而β1受体拮抗剂美托洛尔和p38抑制剂PD169318不能阻断NE的刺激效应。10μmol/L NE促进EPCs的迁移(P<0.05),10μmol/L酚妥拉明和10μmol/L I127能够阻断这种作用,但美托洛尔不能。NE能够浓度依赖性(0.1、1、10μmol/L)地激活EPCs内的ERK1/2,酚妥拉明和I127能够阻断ERK1/2激活(P<0.05),而美托洛尔不能。结论 NE可能通过α和β2肾上腺能受体激活ERK1/2促进EPCs的迁移和增殖。

三七皂甙单体Rb_1对心肌细胞Ca^（2＋）内流作用的研究

应用Ｆｕｒａ－２荧光技术及放射配基结合实验探讨三七皂甙单体Ｒｂ１对心肌细胞胞外Ｃａ２＋内流的作用。０．０４ｍｍｏｌ·Ｌ－１Ｒｂ１可以抑制高钾引起的大鼠心肌细胞胞浆Ｃａ２＋浓度的升高，且呈浓度依赖性；可以完全阻断高钾基础上的异丙肾上腺素的作用。其作用与钙通道拮抗剂维拉帕米类似。Ｒｂ１对大鼠心肌细胞膜上β受体亲和力和受体数均无明显影响。结果提示：Ｒｂ１对心肌细胞电压依赖性钙通道开放引起的胞内钙升高有抑制作用；对β受体相关联的钙通道开放引起的胞浆Ｃａ２＋升高也有抑制作用。而不影响β受体本身。

β_2-肾上腺素能受体激动剂福莫特罗的合成工艺研究

设计了一条合成新型 β2 肾上腺素能受体激动剂福莫特罗的新路线 ,该路线较文献路线简捷方便 ,且后处理简单 ,由原料 1 (4 苄氧基 3 硝基苯基 ) 2 溴乙酮出发 ,总收率为 13 4% .适于实验室制备和工业化生产 .

大鼠主动脉α_1肾上腺素能受体激活引起Ca^（2＋）内流的特性

在大鼠主动脉平滑肌标本上，０．５μｍｏｌ．Ｌ－１硝苯吡啶能完全阻断由１００ｍｍｏｌ·Ｌ－１ＫＣｌ引起的血管收缩和４５Ｃａ内流；并部分抑制苯肾上腺素引起的血管收缩效应和４５Ｃａ内流；６ｍｍｏｌ·Ｌ－１普鲁卡因能完全阻断无钙Ｋｒｅｂｓ液中苯肾上腺素引起的血管收缩和４５Ｃａ外溢，且部分阻断正常Ｋｒｅｂｓ液中苯肾上腺素引起的血管收缩和４５Ｃａ内流；０．５μｍｏｌ·Ｌ－１硝苯吡啶和６ｍｍｏｌ·Ｌ－１普鲁卡因合用能阻断苯肾上腺素引起的Ｃａ２＋内流。提示：α１受体兴奋后引起的细胞外Ｃａ２＋内流可分为硝苯吡啶敏感和不敏感两部分，而后者受细胞内Ｃａ２＋释放调节。

4-((4-((2-取代苯氧基)乙基)-1-哌嗪)-甲基)-1,2-二氢喹啉-2-酮类化合物的合成及体外α-受体拮抗活性

目的 研究DDPH类似物 1,2 二氢喹啉 2 酮类化合物的合成及其体外α 受体拮抗活性。方法 通过酰化、溴代、环合和取代反应等合成目的物 ;推测了异常中间体 3 溴 4 溴甲基 1,2 二氢喹啉 2 酮 (5 )和 3 溴 4 甲基 1,2 二氢喹啉 2 酮 (6 )的生成机理 ;测定目的物的体外α 受体拮抗活性。结果 设计、合成了 12个新化合物II1～ 6和IV1～ 6,其中 6个目的物 1,2 二氢喹啉 2 酮类 (IV1～ 6)的结构经IR ,1 HNMR ,MS和HRMS确证 ;IV3 ,IV4和IV6对兔主动脉环抑制作用较明显。结论 化合物IV3 ,IV4和IV6显示了一定的抑制活性 ,值得进一步研究。

α_2肾上腺素受体与镜像痛调制

镜像痛为躯体一侧组织或神经损伤时产生疼痛及痛敏,在对侧对应区域亦产生疼痛及痛敏的现象。α2肾上腺素受体(alpha-2 adrenergicreceptor,α2-AR)在痛觉调制过程中起着重要作用,在镜像痛研究显示α2-AR激动剂亦可减缓镜像痛敏。现就镜像痛的发生机制结合最新的研究进展,探讨α2-AR参与镜像痛调控的可能机制。α2-AR在镜像痛的调制方面或具重要作用。

呋塞米对α_1肾上腺素受体亚型引起的Ca^(2+)内流的影响

目的 探讨Cl-通道开放在不同α1肾上腺素受体亚型引起的Ca2 +内流中的作用。方法 采用Fura 2 /AM荧光分光光度法 ,测定胞浆游离Ca2 +浓度 ,观察Cl-通道阻断剂呋塞米 ,钙通道阻断剂SK&F96 36 5和硝苯地平对不同α1肾上腺素受体亚型 (α1A、α1B AR)引起的Ca2 +内流的影响 ,并加以比较。结果 2 5 ,5和 10 μmol·L-1呋塞米呈浓度依赖性地抑制了α1A和α1B AR亚型引起的Ca2 +内流 ;对α1A AR引起的Ca2 +内流的抑制率分别为 8 3 %± 6 1% ,2 3 8%±14 8%和 40 7%± 19 3% ,对α1B AR引起的Ca2 +内流的抑制率分别为 12 0 %± 5 4% ,19 2 %± 4 9%和 31 9%±4 9%。α1A AR引起的Ca2 +内流被最大抑制浓度 ( 2 0 μmol·L-1)的SK&F96 36 5抑制后 ,不能被 10 μmol·L-1呋塞米进一步抑制 ;而α1B AR引起的Ca2 +内流被 2 0 μmol·L-1SK&F96 36 5抑制后 ,仍能被 10 μmol·L-1呋塞米进一步抑制 ,抑制率为 6 6 %± 3 2 %。结论 参与α1A和α1B AR引起的Ca2

Ca^(2+)运动对α_1-肾上腺素受体引起内源性ClC-3氯通道表达的作用

目的 研究Ca2 +运动对α1 肾上腺素受体引起ClC 3氯通道表达的作用。方法 在A10细胞上 ,用RT PCR和Westernblot检测ClC 3mRNA和蛋白质表达情况。结果 苯肾上腺素 ( 10 μmol·L-1)和thapsigargin( 0 1μmol·L-1)可促进ClC 3mRNA和蛋白质的表达 ;SK&F963 65 ( 10 μmol·L-1)和genistein( 10 μmol·L-1)可抑制苯肾上腺素引起的ClC 3的表达 ,nifedipine( 10 μmol·L-1)无此作用。结论 在A10细胞上 ,通过钙池操纵性Ca2 +通道 (SOCC)的Ca2 +内流参与了α1 肾上腺素受体引起的内源性ClC 3氯通道的表达 ,而通过电压依赖性Ca2 +通道 (VDCC)的Ca2 +内流可能与此无关。蛋白酪氨酸激酶参与了ClC