• 
<tr id="yyy80"></tr>
    • <sup id="yyy80"></sup>
  • 

    <tfoot id="yyy80"><noscript id="yyy80"></noscript></tfoot>
  • 
99热精品在线国产_美女午夜性视频免费_国产精品国产高清国产av_av欧美777_自拍偷自拍亚洲精品老妇_亚洲熟女精品中文字幕_www日本黄色视频网_国产精品野战在线观看 
?
    
	
    
		
		
		
	
    

    

    
    
    
    
    
        
    
            
    Oatp and Mrp mRNA expression of liver transporters in spontaneously hypertensive rats
    
                
    2017-11-28 05:45:09,,,,,
    
                
    關(guān)鍵詞:轉(zhuǎn)運(yùn)體外排自發(fā)性
    
                    
     , , , , , 
    (Key Laboratory of Basic Pharmacology of Ministry of Education and Joint International Research Laboratory of Ethnomedicine of Ministry of Education,Zunyi Medical University,Zunyi Guizhou 563099,China)
    基礎(chǔ)醫(yī)學(xué)研究
    OatpandMrpmRNAexpressionoflivertransportersinspontaneouslyhypertensiverats
    YueYun,WuYuting,FuShu,QianZhiqiang,LiYeli,YangDanli
    (Key Laboratory of Basic Pharmacology of Ministry of Education and Joint International Research Laboratory of Ethnomedicine of Ministry of Education,Zunyi Medical University,Zunyi Guizhou 563099,China)
    ObjectiveTo investigate the effects of spontaneous hypertension on the mRNA expression of organic anion transporting polypeptides (Oatps) and multidrug resistance-associated proteins (Mrps) of hepatic tissue in spontaneously hypertensive rats (SHR).MethodsFourteen weeks old male SHR were the SHR group (SHR,n=10).The same aged male homologous Kyoto rats (WKY) were the WKY group (WKY,n=10).Rats were routine fed for 12 weeks.The mRNA expression of the major uptake transporter Oatp1a1,Oatp1a4,Oatp1a5 and Oatp1b2 as well as the main efflux transporters Mrp1,Mrp2,Mrp3 and Mrp4 were detected by Real time RT-PCR.The weight change of rats in each group were recorded every two weeks.Blood pressure change was detected in rats with Scientific CODA Kent system.ResultsCompared with the WKY group,the blood pressure in SHR group was significantly increased (Plt;0.05).The mRNA expression of Oatp1a1,Oatp1a4,Oatp1a5,Oatp1b2,Mrp2 and Mrp4 were up-regulated (Plt;0.01) and the mRNA expression of Mrp3 was down-regulated (Plt;0.01) in SHR group.However,the mRNA expression of Mrp1 did not changed significantly (Pgt;0.05).Among four Oatps,the mRNA expression of Oatp1b2 was the highest (32.77% or 79.59% of β-actin) in WKY or SHR groups,and Oatp1a5 was the lowest (0.0033% or 0.0092% of β-actin) in WKY or SHR groups.Among four Mrps,the mRNA expression of Mrp2 was the highest (22.46% or 61.04% of β-actin) in WKY or SHR groups.ConclusionThe mRNA expression of Oatp1a1,Oatp1a4,Oatp1a5,Oatp1b2,Mrp2,Mrp3 and Mrp4 in the main liver transporters of rats were significantly affected by hypertension.However,hypertension has no significant effect on the mRNA expression of Mrp1.
    Organic anion transporting polypeptides; multidrug resistance-associated protein; spontaneous hypertension rat
    Liver transporters mediate drug uptake and efflux,which play an important role in endogenous and exogenous substances,drug transport and drug-drug interactions[1].And its functional inhibition or deletion is an important factor in the interaction between drug metabolism and disease[2].
    Organic anion transporting polypeptides (Oatps/OATPs) are an intake transporter,which belongs to the superfamily of solute carriers (SLC)[1,3].There coding genes are collectively referred as SLCO genes[3].It is an important cell membrane intake protein in animals and human,and has great influence on the absorption,distribution and elimination of internal and external substances,especially drugs[1,3].Humans are represented in OATPs,and rodents are represented in Oatps.Multidrug resistance-associated proteins (Mrps) are the major efflux transporters in liver that mediate the efflux of drugs and metabolites in hepatic[1].Multidrug resistance associated protein responsible for the removal of xenobiotics,and the conjugates and products of oxidative are excreted in two ways:(1) hepatic parenchymal sinusoidal cells,such as Mrp1,Mrp3 and Mrp4; (2) microscopic cells,such as Mrp2[1].
    Transporters are important transmembrane proteins that mediate the cellular entry and exit of a wide range of substrates throughout the body and then play vital roles in human pathology,physiology,pharmacology and toxicology.Transporters mediate the absorption,distribution,metabolism and excretion of the drug invivoand thereby further influencing the invivoprocess of the drug[1].Drug efficacy,drug interactions,adverse drug reactions,and drug detoxification are closely related to transporters[4].The changes of the transporters are involved in the invivobehaviour of commonly used antihypertensive drugs.Whether the hypertension affects the liver transporters is not clear.For now,there are few reports on this research at home and abroad.And,our team has made some progress in the study of spontaneously hypertensive rats.Because of this background,we expected to explore whether hypertension has effects on liver transporters.So that we observe the change of genes related to hepatic organic anion transporters (Oatp1a1,Oatp1a4,Oatp1a5,Oatp1b2) and multidrug resistance-associated proteins (Mrp1,Mrp2,Mrp3,Mrp4).
    1 Materials and Methods
    1.1 Animals 14 weeks old male SHR and WKY(260~300 g) were from the SPF-grade.These rats were purchased from Beijing Weitong Lihua Experimental Animal Technology Co.,Ltd.License number is SCXK (Beijing) 2012-0001.
    1.2 Experimental protocol 14 weeks old SHR were the SHR group (SHR,n=10).The same aged made were the WKY group (WKY,n=10).These rats were routine fed for 12 weeks.
    1.3 Total RNA isolation and real-time RT-PCR analysis Total RNA was isolated from liver tissue of rats by RNAiso Plus (TaKaRa Biotechnology) and then purified of it.Then the mRNA expressions of Oatp1a1,Oatp1a4,Oatp1a5,Oatp1b2,Mrp1,Mrp2,Mrp3 and Mrp4 were detected by Real time RT-PCR.The gene sequences of rat Oatps and Mrps were accessed from GenBank (Table 1).
    The composition of the reaction system:SYBR?GREEN PCR Master Mix 7.5 μl,Upstream and downstream primer mixture 0.5 μl,0.1% DEPC water 4.0 μl,The diluted cDNA samples 3.0 μl,The total volume of the reaction was 15 μl.The process of reaction:Stage 1:Pre-degeneration,95 °C 30min.Stage 2:PCR reaction,55 °C 5 sec; 60 °C 45 sec,40 Cycles.Stage 3:Analysis of melting curve,Starting at 55 °C and decreasing by 0.5 °C in every 5 sec,80 Cycles.The relative expressions of genes were calculated by the 2-△△Ctmethod and normalized to the house-keeping gene β-actin.And the relative transcript levels were calculated as percentage of β-actin.
    Tab1PrimerpairsusedinRealtimeRT-PCR
    GeneGenBankaccessionNo.Forwardprimer(5'-3')Reverseprimer(5'-3')β-actinOatp1a1Oatp1a4NM-031144NM_017111NM_131906AGCCATGTACGTAGCCATCCCCTGTGACAATGCAGCAGTTCCTAGGCATAGGCATTTGGAACCCTCATA-GATGGGCACAGGCTGCAATC-CTGAAACACCATCAACCAAAG-CACAAAGCAGOatp1a5Oatp1b2Mrp1Mrp2Mrp3Mrp4AF041105NM_03165NM_022281.2NM_012833.2NM_080581.1NM_133411.1GCAGGATGATGTGGATGGAAC-TAACAACATGCTTCGTGGGATAGGATTGTGTATGCCCCTCCCAATCTCTTGCGCTCACAGAAGATCCCCATTCATCAACCTGCTTGCACTGTTCTCACCATTGCGCATGTA-AATCGGATTG-CAGGAGCATGGAAGT-GTGCCCTTCTTTGAGGAAG-TAGGGC-CCAAAGGAAACTG-GAATACGCCG-CATTCAGTTTGAT-GCGGGAGTCTTTTTGCT-GTTTCGGT-GAGGG
    1.4 Rat weight and blood pressure detection The body weight changes of the rats in each group were recorded every two weeks using an electronic scale (Beijing Sartorius Electronics Co.,Ltd.).Then,the blood pressure change was detected in the rats with Scientific CODA Kent system (Kent Scientific,USA).
    1.5 Statistical analysis All data were described using mean±SEM.The software SPSS18.0 was used for statistical analysis.Two independent samples were determined by two-tailed independent samplest-test.WhenPlt;0.05 orPlt;0.01 the difference was considered statistically significant.
    2 Results
    2.1 Changes of body weight in rats The body weight changes (Fig1) were increased with age in each group,but there was no statistically difference between WKY group and SHR group (Pgt;0.05).
    Fig 1 Changes of body weight of rats in each group(±SEM,n=6)
    2.2 Changes of blood pressure in rats The blood pressure was increased with age in SHR group (Fig 2).Compared with the WKY group,the blood pressure of SHR group (Fig 2) was significantly raised (Plt;0.05).
    #Plt;0.05 vs WKY. Fig 2 Changes of blood pressure of rats in each group(±SEM,n=6)
    2.3 Changes of Oatp1a1,Oatp1a4,Oatp1a5 and Oatp1b2 mRNA levels in liver tissues Among four Oatps,the mRNA expression of Oatp1b2 (Fig 3) was the highest (32.77% or 79.59% of β-actin) in WKY or SHR groups,and Oatp1a5 (Fig 3) was the lowest (0.0033% or 0.0092% of β-actin) in WKY or SHR groups.Compared with WKY group,the mRNA levels of Oatp1a1,Oatp1a4,Oatp1a5 and Oatp1b2 (Fig 3,4) were significantly up-regulated (Plt;0.01) in SHR.
    ##Plt;0.01 vs WKY. Fig 3 Changes of mRNA expression of Oatp1a1,Oatp1a4 ,Oatp1a5 and Oatp1b2 in liver(±SEM,n=4)
    ##Plt;0.01 vs WKY Fig 4 Changes of mRNA expression of Oatp1a1,Oatp1a4 ,Oatp1a5 and Oatp1b2 in liver(±SEM,n=4)
    2.4 Changes of Mrp1,Mrp2,Mrp3 and Mrp4 mRNA levels in liver tissues Among four Mrps,the mRNA expression of Mrp2 (Fig 5) was the highest (22.46% or 61.04% of β-actin) in WKY or SHR groups.Compared with the WKY group,the mRNA expression of Mrp2 and Mrp4 (Fig 5,6) were up-regulated (Plt;0.01) in spontaneously hypertensive rats,and the mRNA expression of Mrp3 (Fig 5,6) was down-regulated (Plt;0.01).However,the mRNA expression of Mrp1 (Fig 5,6) did not changed significantly (Pgt;0.05).
    ##Plt;0.01 vs WKY. Fig 5 Changes of mRNA expression of Mrp1,Mrp2,Mrp3 and Mrp4 in liver(±SEM,n=4)
    ##Plt;0.01 vs WKY. Fig 6 Changes of mRNA expression of Mrp1,Mrp2,Mrp3 and Mrp4 in liver(±SEM,n=4)
    3 Discussion
    The liver is one of the major detoxification organs,which is of vital importance for the transport,metabolism,elimination and redistribution of drugs.The changes of transporters in the liver can significantly affect the treatment of endogenous and exogenous compounds.At present,there are few reports about the changes of liver transporters in spontaneously hypertensive rats at home and abroad,and this research provides a theoretical basis for it.
    OATPs/Oatps,mainly the endogenous and exogenous substances,especially have significant effects on absorption,distribution and elimination of drugs[3].In Oatps,Oatp1a1,Oatp1a4 and Oatp1b2 are the main hepatic uptake transporters[5].Oatps are a non-Na+-dependent solute carrier,which mediates the transfer of organic cationic drugs[6].The current research considered that Oatps mainly mediated the transfer of drugs from blood into hepatocytes[7].In the liver,the functions of rat liver Oatp1a1,Oatp1a4,Oatp1a5 and Oatp1b2 are similar to human OATP1A2,OATP1B1 and OATP1B3[1].
    Oatp1a1 is mainly distributed in liver and kidney[1].Rat Oatp1a1 is the first cloned member of the OATP/Oatp gene family,which expresses in liver and kidney and has extensive substrate specificity[8].In our study,the mRNA expression of Oatp1a1 was up-regulated in spontaneously hypertensive rats.Oatp1a4 mainly distributes in the retina,brain,lung and liver,and it expresses highly in the liver[9],which is a specific liver uptake transporter.Oatp1a4 can also cause PFOS sulfation[10],and it can be inhibited by amiodarone[6],thus affecting the uptake of digoxin[6].Our study showed that the mRNA expression of Oatp1a4 was raised in spontaneously hypertensive rat livers.Oatp1a5 major distributes in the lung,brain,intestine and liver tissues[11],which is inhibited by a series of Chinese herbs[12].In addition,Oatp1a5 has a wide range of substrate properties in the liver and is closely related to the low substrate of Oatp[13],and plays an important role in the liver[13].In our research,the mRNA expression of Oatp1a5 was increased in spontaneously hypertensive rat livers.Rat Oatp1b2 is homologous with mouse Oatp1b2,human OATP1B1 and OATP1B3,which plays an important role in the liver intake of drugs,poisons and environmental chemicals[7,14],and it is also the transporters of sodium[13-14].Rat Oatp1b2 is an enzyme resistant inducer[9],which plays an important role in the maintenance of endogenous substances.In our study,we found that the mRNA expression of Oatp1b2 was also increased in spontaneously hypertensive rat livers.It is speculated that hypertension could affect the mRNA expressions of the major hepatic uptakes transporters Oatp1a1,Oatp1a4,Oatp1a5 and Oatp1b2,in which the mRNA expressions of Oatp1a1,Oatp1a4,Oatp1a5 and Oatp1b2 were up-regulated in spontaneously hypertensive rats.Among four Oatps,the mRNA expression of Oatp1b2 (Fig 4) was the highest (32.77% of β-actin),and Oatp1a5 (Fig 4) was the lowest (0.0033% of β-actin) in WKY,which is consistent with the literature[9].In our study,it is interesting to find that the mRNA expression of Oatp1b2 (Fig 4) was the highest (79.59% of β-actin) and Oatp1a5 (Fig 4) was the lowest (0.0092% of β-actin) in SHR which is alike to in WKY.
    Mrps are the major efflux transporter in the liver that mediate the efflux of drugs and metabolites in the liver[1].
    MRP1 has little or no immune reactivity in normal human liver,but the expression of MRP1 is increased in primary biliary cirrhosis,chronic hepatitis C virus infection and compliant cell necrosis[15].The expression of Mrp1 is also increased in many liver diseases[15].However,in our research,the mRNA expression of Mrp1 in spontaneously hypertensive rat livers was not significantly different.Mrp2 exists in the apical cell membrane,which promotes the elimination of many exogenous substances,the translocation of endogenous and exogenous organic detoxification substances through bile[16].The anomaly expression of Mrp2 in liver diseases has been extensively documented,such as cholestasis,hepatitis,fibrosis,cirrhosis,and liver cancer[17].Studies have found that the mRNA expression increased of Mrp2 could enhance the efflux function of liver cells,reduce the accumulation of toxic components in intrahepatic bile,promote the metabolism of bile acids and reduce the damage to the hepatic[18].In our research,the mRNA expression level of Mrp2 in spontaneously hypertensive rat livers was increased.Mrp3 is a basal efflux pump for the transport of bilirubin glucuronide,which together with Mrp2 regulates conjugated hyperbilirubinemia[19].Normal hepatocytes mainly express MRP2,but the expression of MRP3 is very low or even not expressed.However,under certain pathological conditions,the expression of MRP2 was decreased,while the expression of MRP3 was increased dramatically.The opposite expression patterns of MRP2 and MRP3 were often accompanied in the above diseases[20].In our study,the mRNA expression of Mrp3 in spontaneously hypertensive rat livers was decreased,and the mRNA expression of Mrp2 was increased,thereby,it was speculated that the opposite expression changes of Mrp2 and Mrp3 were also associated with the phenomenon of coupling in hypertension.Mrp4 is a general efflux transporter for drugs and poisons[21].In the model of Mrp4 knoct out in rats with cholestasis,the extent of liver damage was found to be significantly more severe than that in the wild-type rat cholestasis SHR[22],indicated that the Mrp4 gene had a protective effect on the liver.In fact,the mRNA expression of Mrp4 was significantly increased in human advanced hepatocellular carcinoma in various etiology (HCV infection,alcoholic liver disease and primary sclerosing cholangitis)[23].Our research showed that the mRNA expression of Mrp4 was increased.It is speculated that the mRNA expressions of Mrp2,Mrp3 and Mrp4 were influenced by hypertension,but it had no effect on the mRNA expression of Mrp1.At the same time,it is interesting to show that the mRNA expression of Mrp2 among four Mrps was the highest in both WKY and SHR in our study,which should be further evaluated.This suggests that Mrp2 play an important role,and hypertension may affect the expression of Mrp2.
    As result,the mRNA expressions of liver transporter Oatp1a1,Oatp1a4,Oatp1a5,Oatp1b2,Mrp2 and Mrp4 in spontaneous hypertensive rats were significantly higher than the WKY group,whereas the mRNA expression of Mrp3 was decreased significantly,and the mRNA expression of Mrp1 had no evident change.It gives us some hints for future study,we plan to do more further research for Oatps (Oatp1a4,Oatp1b2) and Mrp2 protein expression.
    [1] Klaassen C D,Aleksunes L M.Xenobiotic,bile acid,and cholesterol transporters:function and regulation[J].Pharmacological Reviews,2010,62(1):1-96.
    [2] 張愛(ài)杰,劉克辛.肝臟轉(zhuǎn)運(yùn)體介導(dǎo)藥物相互作用的研究進(jìn)展[J].世界華人消化雜志,2012,20(28):2655-2660.
    [3] Obaidat A,Roth M,Hagenbuch B.The expression and function of organic anion transporting polypeptides in normal tissues and in cancer[J].Annu Rev Pharm- acol Toxicol,2012,52(1):135-151.
    [4] 劉克辛.轉(zhuǎn)運(yùn)體介導(dǎo)的藥物相互作用與臨床安全用藥[J].大連醫(yī)科大學(xué)學(xué)報(bào),2012,34(1) :1-8.
    [5] Cheng X,Maher J,Chen C,et al.Tissue distribution and ontogeny of mouse organic anion transporting polypeptides (Oatps) [J].Drug Metabolism and Disposition,2005,33(7):1062-1073.
    [6] Funakoshi S,Murakami T,Yumoto R,et al.Role of organic anion transporting polypeptide 2 in pharmacokinetics of digoxin and beta-methyldigoxin in rats[J].J Pharm Sci,2005,94(6):1196-1203.
    [7] Evers R,Chu X Y.Role of the murine organic anion-transporting polypeptide 1b2 (Oatp1b2) in drug disposition and hepatotoxicity[J].Mol Pharmacol,2008,74(2):309-311.
    [8] Jacquemin E,Hagenbuch B,Stieger B,et al .Expression cloning of a rat liver Na+-independent organic anion transporter[J].Proc Natl Acad,1994,91(1):133-137.
    [9] Li N,Hartley D P,Cherrington N J,et al.Tissue expression,ontogeny,and induci-ibility of rat organic anion transporting polypeptide 4[J].J Pharmacol Exp Ther,2002,301(2):551-560.
    [10]Yu W G,Liu W,Liu L,et al.Perfluorooctane sulfonate increased hepatic expression of OAPT2 and MRP2 in rats[J].Arch Toxicol,2011,85(6):613-621.
    [11]Walters H C,Craddock A L,Fusegawa H,et al.Expression,transport properties,and chromosomal location of organic anion transporter subtype 3[J].Am J Physiol Gastrointest Liver Physiol,2000,279(6):1188-1200.
    [12]Ismair M G,Stanca C,Ha H R,et al.Interactions of glycyrrhizin with organic anion transporting polypeptides of rat and human liver[J].Hepatol Res,2003,26(4):343-347.
    [13]Cattori V,Van Montfoort J E,Stieger B,et al.Localization of organic anion transporting polypeptide 4 (Oatp4) in rat liver and comparison of its substrate specificity with Oatp1,Oatp2 and Oatp3[J].Pflugers Arch,2001,443(2):188-195.
    [14]Csanaky I L,Lu H,Zhang Y,et al.Organic anion-transporting polypeptide 1b2 (Oatp1b2) is important for the hepatic uptake of unconjugated bile acids:Studies in Oatp1b2-null mice[J].Hepatology,2011,53(1):272-281.
    [15]Ros J E,Libbrecht L,Geuken M,et al.High expression of MDR1,MRP1,and MRP3 in the hepatic progenitor cell compartment and hepatocytes in severe human liver disease[J].Journal of Pathology,2003,200(5):553-560.
    [16]Jemnitz K,Heredi-Szabo K,Janossy J,et al.ABCC2/Abcc2:a multispecific transporter with dominant excretory functions[J].Drug Metabolism Reviews,2010,42(3):402-436.
    [17]Dzierlenga A L,Clarke J D,Klein D M,et al.Biliary elimination of pemetrexed is dependent on mrp2 in rats:potential mechanism of variable response in nonalcoholic steatohepatitis[J].Journal of Pharmacology amp; Experimental Therapeutics,2016,358(2):246-253.
    [18]牛璐,金晶,陳攀,等.黃芩素對(duì)膽汁外排轉(zhuǎn)運(yùn)體MRP2和BSEP的影響[J].中國(guó)藥理學(xué)通報(bào),2015,31(1):147-148.
    [19]Lw V D S,Verkade H J,Kuipers F,et al.New insights in the biology of ABC transporters ABCC2 and ABCC3:impact on drug disposition[J].Expert Opinion on Drug Metabolism amp; Toxicology,2015,11(2):273-293.
    [20]Keitel V,Burdelski M,Warskulat U,et al.Expression and localization of hepatobiliary transport proteins in progressive familial intrahepatic cholestasis[J].Hepatology,2005,41(5):1160-1172.
    [21]Russel F G,Koenderink J B,Masereeuw R.Multidrug resistance protein 4 (MRP4/ABCC4):a versatile efflux transporter for drugs and signalling molecules[J].Trends in Pharmacological Sciences,2008,29(4):200-207.
    [22]Chai J,Luo D,Wu X,et al.Changes of organic anion transporter MRP4 and related nuclear receptors in human obstructive cholestasis[J].Journal of Gastrointestinal Surgery,2011,15(6):996-1004.
    [23]Chen H L,Liu Y J,Chen H L,et al.Expression of hepatocyte transporters and nuclear receptors in children with early and late-stage biliary atresia[J].Pediatr Res,2008,63(6):667-673.
    [收稿2017-05-07;修回2017-08-12]
    (編輯:譚秀榮)
    國(guó)家自然科學(xué)基金資助項(xiàng)目(NO :81241142)。
    楊丹莉,女,博士,教授,碩士生導(dǎo)師,研究方向:心血管藥理學(xué)、抗炎免疫藥理學(xué),E-mail:zmuyangdanli@foxmail.com。
    自發(fā)性高血壓大鼠肝臟轉(zhuǎn)運(yùn)體Oatp及Mrp mRNA水平的變化
    岳 云,吳雨婷,付 舒,錢志強(qiáng),李葉麗,楊丹莉
    (遵義醫(yī)學(xué)院 基礎(chǔ)藥理教育部重點(diǎn)實(shí)驗(yàn)室暨特色民族藥教育部國(guó)際合作聯(lián)合實(shí)驗(yàn)室,貴州 遵義 563099)
    目的探討高血壓對(duì)大鼠有機(jī)陰離子轉(zhuǎn)運(yùn)多肽(organic anion transporting polypeptides,OATPs/Oatps)及多藥耐藥相關(guān)蛋白(multidrug resistance-associated protein,Mrps)mRNA水平的影響。方法14周齡的雄性自發(fā)性高血壓大鼠(Spontaneous Hypertension Rat,SHR)為SHR組(SHR,n=10),同源正常的京都大鼠(Wistar-Kyoto rat,WKY)為WKY組(WKY,n=10)。常規(guī)飼養(yǎng)12周。每?jī)芍苡涗浉鹘M大鼠體重變化、Kent Scientific CODA系統(tǒng)檢測(cè)大鼠血壓變化。Real time RT-PCR檢測(cè)大鼠肝臟組織中的主要攝取性轉(zhuǎn)運(yùn)體Oatp1a1、Oatp1a4、Oatp1a5、Oatp1b2 及主要外排型轉(zhuǎn)運(yùn)體Mrp1、Mrp2、Mrp3、Mrp4 mRNA的水平。結(jié)果與WKY組相比,SHR組大鼠血壓明顯上升(Plt;0.05),SHR組大鼠肝臟轉(zhuǎn)運(yùn)體Oatp1a1、Oatp1a4、Oatp1a5、Oatp1b2、Mrp2及Mrp4 mRNA的表達(dá)量顯著增高(Plt;0.01),而Mrp3 mRNA的表達(dá)量顯著降低(Plt;0.01),Mrp1 mRNA的表達(dá)量無(wú)明顯變化(Pgt;0.05)。4種OATP中,Oatp1b2 mRNA在WKY(32.77% of f'-actin)及SHR(79.59% of f'-actin)中表達(dá)均最高,Oatpla5 mRNA在WKY(0.0033% of f'-actin )及SHR(0.009 2% of f'-actin)中表達(dá)均最低。4種Mrp中Mrp2 mRNA在WKY(22.46% of f'-actin)及SHR(61.04% of f'-actin)中表達(dá)均最高。結(jié)論高血壓對(duì)大鼠肝臟主要攝取性轉(zhuǎn)運(yùn)體Oatp1a1、Oatp1a4、Oatp1a5、Oatp1b2及主要外排型轉(zhuǎn)運(yùn)體Mrp2、Mrp3、Mrp4 mRNA的表達(dá)有影響,而對(duì)Mrp1 mRNA的表達(dá)無(wú)影響。
    有機(jī)陰離子轉(zhuǎn)運(yùn)多肽;多藥耐藥相關(guān)蛋白;自發(fā)性高血壓大鼠
    R969.1
    A
    1000-2715(2017)05-0469-06
    

    
                        
    猜你喜歡
    
                        
    轉(zhuǎn)運(yùn)體外排自發(fā)性
    
                        
    轉(zhuǎn)運(yùn)體的研究進(jìn)展及在中藥研究上的應(yīng)用
    自發(fā)性冠狀動(dòng)脈螺旋夾層1例
    膠東國(guó)際機(jī)場(chǎng)1、4號(hào)外排渠開(kāi)挖支護(hù)方案研究
    大腸桿菌ABC轉(zhuǎn)運(yùn)體研究進(jìn)展
    高尿酸血癥治療藥物及其作用靶點(diǎn)研究進(jìn)展
    外排體促進(jìn)骨再生的研究進(jìn)展
    三排式吻合器中的雙吻合釘推進(jìn)器對(duì)
    4例自發(fā)性腎破裂患者的護(hù)理
    自發(fā)性乙狀結(jié)腸穿孔7例診治體會(huì)
    RNA干擾技術(shù)在藥物轉(zhuǎn)運(yùn)體研究中的應(yīng)用
    
                    
    
            
    
        
    
        
        
    
    
    

    










一级黄色大片毛片|
丝袜美足系列|
国产成人免费无遮挡视频|
一级毛片电影观看|
中文字幕最新亚洲高清|
日韩一卡2卡3卡4卡2021年|
十分钟在线观看高清视频www|
99久久精品国产亚洲精品|
亚洲成a人片在线一区二区|
国产区一区二久久|
精品午夜福利视频在线观看一区
|
亚洲天堂av无毛|
黄色片一级片一级黄色片|
久久精品国产亚洲av高清一级|
国产成人精品久久二区二区91|
成在线人永久免费视频|
精品久久久久久久毛片微露脸|
叶爱在线成人免费视频播放|
久久久国产精品麻豆|
69av精品久久久久久
|
色婷婷久久久亚洲欧美|
老司机深夜福利视频在线观看|
a级毛片黄视频|
久热爱精品视频在线9|
五月天丁香电影|
成人特级黄色片久久久久久久
|
日韩精品免费视频一区二区三区|
久久精品国产a三级三级三级|
黄网站色视频无遮挡免费观看|
动漫黄色视频在线观看|
黄色 视频免费看|
99国产极品粉嫩在线观看|
久久久精品区二区三区|
日韩欧美一区视频在线观看|
国产精品久久久av美女十八|
久久久久久久国产电影|
精品亚洲成国产av|
亚洲 国产 在线|
亚洲熟女毛片儿|
777久久人妻少妇嫩草av网站|
亚洲 国产 在线|
tube8黄色片|
国产淫语在线视频|
深夜精品福利|
日韩欧美三级三区|
搡老岳熟女国产|
国产日韩欧美亚洲二区|
免费在线观看视频国产中文字幕亚洲|
久久精品国产综合久久久|
午夜91福利影院|
国产精品免费视频内射|
国产欧美日韩一区二区三区在线|
亚洲全国av大片|
老司机靠b影院|
国产精品影院久久|
欧美在线黄色|
日韩欧美一区视频在线观看|
亚洲,欧美精品.|
国产av精品麻豆|
午夜福利免费观看在线|
国产人伦9x9x在线观看|
国产色视频综合|
午夜精品久久久久久毛片777|
久久免费观看电影|
一级毛片电影观看|
高潮久久久久久久久久久不卡|
欧美人与性动交α欧美软件|
avwww免费|
亚洲欧美一区二区三区黑人|
午夜成年电影在线免费观看|
女同久久另类99精品国产91|
男女床上黄色一级片免费看|
一进一出抽搐动态|
国产成人精品久久二区二区免费|
久久精品国产a三级三级三级|
国产精品.久久久|
成人黄色视频免费在线看|
丰满迷人的少妇在线观看|
国产精品亚洲一级av第二区|
一二三四社区在线视频社区8|
国产黄频视频在线观看|
免费一级毛片在线播放高清视频
|
交换朋友夫妻互换小说|
多毛熟女@视频|
成年人午夜在线观看视频|
亚洲欧美色中文字幕在线|
性色av乱码一区二区三区2|
十分钟在线观看高清视频www|
av电影中文网址|
亚洲欧美激情在线|
80岁老熟妇乱子伦牲交|
这个男人来自地球电影免费观看|
人人妻人人添人人爽欧美一区卜|
欧美亚洲日本最大视频资源|
久久久久久久久久久久大奶|
svipshipincom国产片|
国产精品1区2区在线观看.
|
亚洲精品国产精品久久久不卡|
别揉我奶头~嗯~啊~动态视频|
国产成人av激情在线播放|
日韩中文字幕欧美一区二区|
黄色视频不卡|
99国产精品一区二区蜜桃av
|
交换朋友夫妻互换小说|
波多野结衣一区麻豆|
99久久精品国产亚洲精品|
国产成人欧美在线观看
|
精品第一国产精品|
一区二区三区国产精品乱码|
日韩免费av在线播放|
19禁男女啪啪无遮挡网站|
在线观看免费日韩欧美大片|
国产成人免费无遮挡视频|
www.自偷自拍.com|
国产亚洲精品久久久久5区|
亚洲第一欧美日韩一区二区三区
|
国产一区二区三区在线臀色熟女
|
免费日韩欧美在线观看|
精品一品国产午夜福利视频|
亚洲熟女精品中文字幕|
美女福利国产在线|
国产精品麻豆人妻色哟哟久久|
狠狠狠狠99中文字幕|
亚洲国产欧美在线一区|
亚洲中文字幕日韩|
精品久久久久久久毛片微露脸|
女人精品久久久久毛片|
九色亚洲精品在线播放|
十八禁网站免费在线|
午夜精品久久久久久毛片777|
在线观看免费高清a一片|
99国产极品粉嫩在线观看|
大陆偷拍与自拍|
精品欧美一区二区三区在线|
天堂俺去俺来也www色官网|
免费在线观看完整版高清|
免费人妻精品一区二区三区视频|
精品少妇内射三级|
免费少妇av软件|
1024视频免费在线观看|
最新美女视频免费是黄的|
中文字幕精品免费在线观看视频|
国产主播在线观看一区二区|
国产欧美日韩一区二区精品|
真人做人爱边吃奶动态|
免费看a级黄色片|
啦啦啦中文免费视频观看日本|
亚洲五月色婷婷综合|
丁香欧美五月|
一区二区三区精品91|
天堂8中文在线网|
久久久久久人人人人人|
精品免费久久久久久久清纯
|
国产精品免费大片|
精品国产国语对白av|
在线观看www视频免费|
91字幕亚洲|
两个人免费观看高清视频|
一本一本久久a久久精品综合妖精|
精品国内亚洲2022精品成人
|
91字幕亚洲|
中文字幕另类日韩欧美亚洲嫩草|
黄色a级毛片大全视频|
狠狠精品人妻久久久久久综合|
日韩视频一区二区在线观看|
欧美精品av麻豆av|
日韩免费av在线播放|
中文字幕另类日韩欧美亚洲嫩草|
两个人看的免费小视频|
波多野结衣av一区二区av|
久久久久久久久久久久大奶|
久久 成人 亚洲|
免费黄频网站在线观看国产|
久久九九热精品免费|
大片免费播放器 马上看|
久久国产精品男人的天堂亚洲|
一级片免费观看大全|
久久影院123|
悠悠久久av|
久久中文字幕一级|
黑人欧美特级aaaaaa片|
波多野结衣av一区二区av|
av超薄肉色丝袜交足视频|
久久人人爽av亚洲精品天堂|
新久久久久国产一级毛片|
精品福利永久在线观看|
成人精品一区二区免费|
另类亚洲欧美激情|
午夜精品久久久久久毛片777|
搡老熟女国产l中国老女人|
亚洲国产看品久久|
中文字幕人妻熟女乱码|
精品福利观看|
国产精品二区激情视频|
老司机午夜福利在线观看视频
|
亚洲欧美一区二区三区黑人|
精品国内亚洲2022精品成人
|
一进一出好大好爽视频|
国产区一区二久久|
婷婷成人精品国产|
纵有疾风起免费观看全集完整版|
亚洲精品国产色婷婷电影|
午夜视频精品福利|
久久天躁狠狠躁夜夜2o2o|
精品国内亚洲2022精品成人
|
他把我摸到了高潮在线观看
|
丁香欧美五月|
91国产中文字幕|
亚洲av片天天在线观看|
kizo精华|
亚洲国产av影院在线观看|
亚洲色图av天堂|
亚洲成av片中文字幕在线观看|
e午夜精品久久久久久久|
欧美日韩精品网址|
免费高清在线观看日韩|
成人18禁高潮啪啪吃奶动态图|
久久人人97超碰香蕉20202|
狠狠狠狠99中文字幕|
黄色a级毛片大全视频|
亚洲美女黄片视频|
大香蕉久久成人网|
热99国产精品久久久久久7|
亚洲成人国产一区在线观看|
99热网站在线观看|
每晚都被弄得嗷嗷叫到高潮|
久久免费观看电影|
xxxhd国产人妻xxx|
亚洲精品在线美女|
1024香蕉在线观看|
久久久久久久精品吃奶|
日韩一卡2卡3卡4卡2021年|
伦理电影免费视频|
老司机亚洲免费影院|
伊人久久大香线蕉亚洲五|
日本精品一区二区三区蜜桃|
电影成人av|
美女扒开内裤让男人捅视频|
精品国产乱子伦一区二区三区|
9热在线视频观看99|
国产野战对白在线观看|
久久精品人人爽人人爽视色|
男人操女人黄网站|
欧美久久黑人一区二区|
亚洲av成人不卡在线观看播放网|
久久久久国内视频|
我要看黄色一级片免费的|
黄片小视频在线播放|
日本撒尿小便嘘嘘汇集6|
国产精品98久久久久久宅男小说|
欧美日韩亚洲综合一区二区三区_|
久久人妻av系列|
亚洲美女黄片视频|
免费在线观看黄色视频的|
激情在线观看视频在线高清
|
最黄视频免费看|
国产成+人综合+亚洲专区|
午夜福利,免费看|
最新在线观看一区二区三区|
免费在线观看影片大全网站|
亚洲精华国产精华精|
色综合婷婷激情|
少妇被粗大的猛进出69影院|
中文字幕色久视频|
国产在线一区二区三区精|
亚洲一区二区三区欧美精品|
国产精品久久久久成人av|
99在线人妻在线中文字幕
|
水蜜桃什么品种好|
国产伦人伦偷精品视频|
男男h啪啪无遮挡|
久久中文看片网|
成人国语在线视频|
好男人电影高清在线观看|
1024视频免费在线观看|
欧美激情久久久久久爽电影
|
十八禁网站网址无遮挡|
av一本久久久久|
亚洲精品在线观看二区|
汤姆久久久久久久影院中文字幕|
老司机在亚洲福利影院|
国产亚洲精品久久久久5区|
av国产精品久久久久影院|
国产精品久久久人人做人人爽|
99热国产这里只有精品6|
国产精品亚洲一级av第二区|
老鸭窝网址在线观看|
精品国产国语对白av|
亚洲久久久国产精品|
免费久久久久久久精品成人欧美视频|
亚洲欧美色中文字幕在线|
18禁黄网站禁片午夜丰满|
久久国产精品影院|
最近最新中文字幕大全免费视频|
日韩免费高清中文字幕av|
国产在线视频一区二区|
午夜激情久久久久久久|
丝袜喷水一区|
操美女的视频在线观看|
亚洲 国产 在线|
久久性视频一级片|
午夜两性在线视频|
久久免费观看电影|
色老头精品视频在线观看|
日韩熟女老妇一区二区性免费视频|
高清在线国产一区|
国产精品久久久av美女十八|
一区二区av电影网|
亚洲专区中文字幕在线|
男人操女人黄网站|
在线观看免费视频日本深夜|
亚洲av欧美aⅴ国产|
一本综合久久免费|
亚洲人成77777在线视频|
久久人人爽av亚洲精品天堂|
久久亚洲精品不卡|
一级片'在线观看视频|
乱人伦中国视频|
制服诱惑二区|
欧美日韩黄片免|
中国美女看黄片|
国产老妇伦熟女老妇高清|
亚洲av电影在线进入|
一级毛片女人18水好多|
午夜福利欧美成人|
亚洲综合色网址|
亚洲少妇的诱惑av|
国产一区二区在线观看av|
老汉色∧v一级毛片|
日韩人妻精品一区2区三区|
老司机深夜福利视频在线观看|
国产成人精品在线电影|
国产成人免费无遮挡视频|
久久狼人影院|
两性夫妻黄色片|
十八禁人妻一区二区|
亚洲天堂av无毛|
搡老熟女国产l中国老女人|
avwww免费|
一区二区av电影网|
丰满少妇做爰视频|
日韩欧美一区二区三区在线观看
|
99国产精品免费福利视频|
十分钟在线观看高清视频www|
一二三四在线观看免费中文在|
亚洲中文av在线|
婷婷丁香在线五月|
国产一区二区三区视频了|
99精国产麻豆久久婷婷|
av一本久久久久|
国产男靠女视频免费网站|
a在线观看视频网站|
亚洲av片天天在线观看|
人妻 亚洲 视频|
在线观看免费午夜福利视频|
亚洲午夜精品一区,二区,三区|
日韩欧美三级三区|
两人在一起打扑克的视频|
99国产精品一区二区三区|
国产主播在线观看一区二区|
黄片大片在线免费观看|
王馨瑶露胸无遮挡在线观看|
天天影视国产精品|
日本av免费视频播放|
一本大道久久a久久精品|
国产91精品成人一区二区三区
|
一边摸一边做爽爽视频免费|
国产精品.久久久|
午夜激情久久久久久久|
在线观看www视频免费|
大陆偷拍与自拍|
国产人伦9x9x在线观看|
欧美+亚洲+日韩+国产|
久久久久久久精品吃奶|
色视频在线一区二区三区|
国产在线一区二区三区精|
中亚洲国语对白在线视频|
亚洲成人手机|
另类亚洲欧美激情|
两人在一起打扑克的视频|
亚洲五月色婷婷综合|
日韩欧美免费精品|
两人在一起打扑克的视频|
少妇的丰满在线观看|
国产成人av激情在线播放|
少妇精品久久久久久久|
成人亚洲精品一区在线观看|
色视频在线一区二区三区|
亚洲国产毛片av蜜桃av|
中文欧美无线码|
国产老妇伦熟女老妇高清|
国产午夜精品久久久久久|
夜夜夜夜夜久久久久|
欧美日韩亚洲高清精品|
亚洲国产精品一区二区三区在线|
9色porny在线观看|
国产精品久久久av美女十八|
欧美精品一区二区免费开放|
色播在线永久视频|
80岁老熟妇乱子伦牲交|
国产麻豆69|
女同久久另类99精品国产91|
99国产综合亚洲精品|
久久国产精品人妻蜜桃|
tube8黄色片|
别揉我奶头~嗯~啊~动态视频|
a级毛片黄视频|
成人亚洲精品一区在线观看|
免费av中文字幕在线|
伊人久久大香线蕉亚洲五|
1024视频免费在线观看|
无限看片的www在线观看|
精品人妻熟女毛片av久久网站|
色综合欧美亚洲国产小说|
人人妻,人人澡人人爽秒播|
精品一区二区三区四区五区乱码|
午夜福利视频在线观看免费|
法律面前人人平等表现在哪些方面|
人妻 亚洲 视频|
欧美精品av麻豆av|
日韩三级视频一区二区三区|
精品卡一卡二卡四卡免费|
叶爱在线成人免费视频播放|
久久久久网色|
最新的欧美精品一区二区|
麻豆乱淫一区二区|
午夜精品久久久久久毛片777|
黑人巨大精品欧美一区二区蜜桃|
国产成人欧美在线观看
|
国产在线免费精品|
丰满少妇做爰视频|
国产成人精品久久二区二区91|
精品福利观看|
久久性视频一级片|
亚洲全国av大片|
99热网站在线观看|
久久狼人影院|
天堂8中文在线网|
岛国毛片在线播放|
国产亚洲精品一区二区www
|
麻豆成人av在线观看|
一区二区三区精品91|
久久人妻av系列|
一区福利在线观看|
av一本久久久久|
www.999成人在线观看|
黄色毛片三级朝国网站|
久久中文字幕人妻熟女|
亚洲色图av天堂|
欧美亚洲 丝袜 人妻 在线|
九色亚洲精品在线播放|
国产熟女午夜一区二区三区|
av天堂在线播放|
欧美一级毛片孕妇|
91麻豆精品激情在线观看国产
|
www.熟女人妻精品国产|
亚洲精品美女久久久久99蜜臀|
日日夜夜操网爽|
国产男女超爽视频在线观看|
国产老妇伦熟女老妇高清|
久久精品91无色码中文字幕|
欧美亚洲日本最大视频资源|
99久久精品国产亚洲精品|
av在线播放免费不卡|
正在播放国产对白刺激|
日韩三级视频一区二区三区|
国产在视频线精品|
色精品久久人妻99蜜桃|
成人av一区二区三区在线看|
日韩中文字幕视频在线看片|
国产精品国产av在线观看|
精品少妇久久久久久888优播|
人人妻人人澡人人爽人人夜夜|
久久精品国产综合久久久|
国产成人精品在线电影|
91精品国产国语对白视频|
成人亚洲精品一区在线观看|
欧美精品啪啪一区二区三区|
国产黄色免费在线视频|
日韩免费av在线播放|
18禁裸乳无遮挡动漫免费视频|
一区二区日韩欧美中文字幕|
免费在线观看日本一区|
91av网站免费观看|
国产精品亚洲一级av第二区|
bbb黄色大片|
国产精品麻豆人妻色哟哟久久|
久久久精品94久久精品|
国产欧美亚洲国产|
无限看片的www在线观看|
夜夜爽天天搞|
999精品在线视频|
无人区码免费观看不卡
|
久久久久久久久免费视频了|
午夜福利在线免费观看网站|
亚洲午夜精品一区,二区,三区|
久久精品亚洲av国产电影网|
国产精品影院久久|
国产男女内射视频|
十八禁网站网址无遮挡|
国产成+人综合+亚洲专区|
一级片免费观看大全|
亚洲国产欧美日韩在线播放|
日韩大片免费观看网站|
日韩欧美一区视频在线观看|
国产精品电影一区二区三区
|
老司机午夜福利在线观看视频
|
午夜激情久久久久久久|
欧美黑人欧美精品刺激|
91九色精品人成在线观看|
老鸭窝网址在线观看|
老司机靠b影院|
桃花免费在线播放|
亚洲成人国产一区在线观看|
午夜福利视频精品|
亚洲欧美一区二区三区黑人|
老汉色∧v一级毛片|
成年女人毛片免费观看观看9
|
叶爱在线成人免费视频播放|
亚洲成人免费电影在线观看|
夜夜夜夜夜久久久久|
亚洲成人国产一区在线观看|
美国免费a级毛片|
亚洲一区二区三区欧美精品|
精品人妻1区二区|
一级毛片电影观看|
久久国产精品大桥未久av|
久热爱精品视频在线9|
一区二区av电影网|
一进一出好大好爽视频|
在线观看舔阴道视频|
久久免费观看电影|
国产在线一区二区三区精|
国产高清videossex|
国产男女超爽视频在线观看|
午夜两性在线视频|
一本色道久久久久久精品综合|
美女高潮喷水抽搐中文字幕|
高清欧美精品videossex|
久久九九热精品免费|
国产成人系列免费观看|
免费在线观看日本一区|
精品福利永久在线观看|
www.自偷自拍.com|
国产精品一区二区在线不卡|
丝袜美腿诱惑在线|
欧美日韩黄片免|
大码成人一级视频|
岛国毛片在线播放|
亚洲精品一卡2卡三卡4卡5卡|
国产精品秋霞免费鲁丝片|
一进一出好大好爽视频|
一本久久精品|
日本av免费视频播放|
美女午夜性视频免费|
国产成人免费无遮挡视频|
久久人妻熟女aⅴ|
黄色视频在线播放观看不卡|
亚洲一区二区三区欧美精品|
久久这里只有精品19|
久久久久久久大尺度免费视频|
精品熟女少妇八av免费久了|
www.自偷自拍.com|
av片东京热男人的天堂|
欧美精品高潮呻吟av久久|
午夜久久久在线观看|
亚洲第一青青草原|
久久青草综合色|
国产亚洲欧美在线一区二区|
精品国产国语对白av|
免费观看av网站的网址|
久久精品亚洲熟妇少妇任你|
午夜福利免费观看在线|
窝窝影院91人妻|
亚洲美女黄片视频|
日本撒尿小便嘘嘘汇集6|
国产亚洲精品第一综合不卡|
国产成人av教育|
免费看a级黄色片|
国产一区二区在线观看av|
亚洲国产毛片av蜜桃av|
av又黄又爽大尺度在线免费看|
成年动漫av网址|
可以免费在线观看a视频的电影网站|
免费看a级黄色片|
老司机午夜福利在线观看视频
|
午夜日韩欧美国产|
欧美激情极品国产一区二区三区|
色综合欧美亚洲国产小说|
日韩欧美一区二区三区在线观看
|
亚洲人成伊人成综合网2020|
国产精品一区二区精品视频观看|
18禁美女被吸乳视频|
丁香六月欧美|
亚洲熟妇熟女久久|
大片免费播放器 马上看|
露出奶头的视频|
咕卡用的链子|
国产在线视频一区二区|
我的亚洲天堂|
成人亚洲精品一区在线观看|
在线观看免费高清a一片|
久久久国产精品麻豆|
国产成+人综合+亚洲专区|
日韩视频一区二区在线观看|
不卡av一区二区三区|
满18在线观看网站|
国产日韩欧美视频二区|
嫁个100分男人电影在线观看|
亚洲精品一卡2卡三卡4卡5卡|
亚洲国产精品一区二区三区在线|
午夜福利影视在线免费观看|
欧美精品一区二区大全|
欧美国产精品va在线观看不卡|
色精品久久人妻99蜜桃|