• 
<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 
?
    
	
    
		
		
		
	
    

    

    
    
    
    
    
        
    
            
    Anti-hypertensive effects of rosiglitazone on renovascular hypertensive rats: role of oxidative stress and lipid metabolism
    
                
    2015-04-22 07:49:48LIYan李巖GUONan郭楠FUZhenping付振平DONGJirui董繼銳ZHAOJianpu趙劍璞FENGHuihong馮會(huì)紅LIUPinduo劉品多XIAYu夏雨
    
                
    關(guān)鍵詞:李巖夏雨
    
                    
    LI Yan(李巖), GUO Nan(郭楠), FU Zhen-ping(付振平), DONG Ji-rui(董繼銳),ZHAO Jian-pu(趙劍璞), FENG Hui-hong(馮會(huì)紅), LIU Pin-duo(劉品多), XIA Yu(夏雨)
    (School of Life Science, Beijing Institute of Technology, Beijing 100081, China)
    ?
    Anti-hypertensive effects of rosiglitazone on renovascular hypertensive rats: role of oxidative stress and lipid metabolism
    LI Yan(李巖), GUO Nan(郭楠), FU Zhen-ping(付振平), DONG Ji-rui(董繼銳),ZHAO Jian-pu(趙劍璞), FENG Hui-hong(馮會(huì)紅), LIU Pin-duo(劉品多), XIA Yu(夏雨)
    (School of Life Science, Beijing Institute of Technology, Beijing 100081, China)
    This study investigated the anti-hypertensive mechanism of rosiglitazone in renovascular hypertensive rats, and examined its relationship to oxidative stress and lipid metabolism. The renovascular hypertension was induced by stenosis of the left renal artery. Four groups of rats were selected: control, induced untreated, rosiglitazone (20 mg/kg) and captopril (10 mg/kg). After 14 d of administration, compared with induced untreated group, rosiglitazone group reduced the renovascular hypertensive rats’ systolic blood pressure and diastolic blood pressure, and decreased total cholesterol (TCH), triglyceride (TG), angiotensin II (Ang II) and angiotensin receptor (AT1) levels(P<0.05). Meanwhile, rosiglitazone remarkably decreased the levels of malondialdehyde (MDA) and hydrogen peroxide (H2O2) while improved the levels of supperoxide dismutase (SOD) and reduced glutathione (GSH). These results suggested that rosiglitazone could effectively decreased the blood pressure in renovascular hypertensive rats, and this might be performed by regulating the activity of angiotensin and the lipid metabolism and improving the oxidative stress.
    rosiglitazone; renovascular hypertensive rat; lipid metabolism; oxidative stress
    Human hypertension is a slowly-developed disorder, and involves the complex structural and functional alterations of its target organs. Hypertension is manifested by an increased arterial pressure[1]. Epidemiological data revealed that elevation of blood pressure alone in hypertension patients is less than 20%, most hypertension patients is always accompany with other metabolic disorder, such as obesity and lipid abnormality[2]. Chronic kidney artery diseases such as renal artery stenosis generally result in hypertension. Two-kidney, one-clip (2K1C) model in which one of the renal arteries is subjected to artery stenosis by clip placement, is one of the kidney related animal models of hypertension. Kidney ischemia leads to increase in plasma renin and angiotensin activity which successively results in persistent rise in blood pressure[3].
    Thiazolidinediones (TZDs), a class of synthetic insulin-sensitizing agent (e.g., pioglitazone, rosiglitazone) used in the treatment of diabetes mellitus type 2, act by enhancing sensitivity to insulin to lower blood sugar. Overseas study found that in diabetic animals and patients, TZDs can not only lower blood glucose by enhancing insulin sensitivity, but also reduce blood pressure, suggesting that lower blood pressure is associated with enhanced insulin sensitivity[4-5]. As TZDs represented drug, rosiglitazone can improve insulin resistance and have a hypoglycemic effect which may be related to competitive peroxisome proliferator-activated receptor γandregulationofinsulingenetranscriptionreactivity[6-7].Althoughrosiglitazonereducesbloodpressurebyreducingtheroleofinsulinresistancehasbeenconfirmedbyclinicalandanimalstudies[8],itsmechanismremainsunclear.Toinvestigateanti-hypertensivemechanismofrosiglitazone,therenovascularhypertensiveratmodelwasinducedbystenosisoftheleftrenalartery,andangiotensinanditsreceptorlevel,lipidmetabolism,andoxidativestressweredetected.
    1 Materials and methods
    1.1Experimentaldrugs
    RosiglitazonewasfromHenryPharmaceuticalCo.,Ltd.Chengdu(batchnumber: 110901).CaptoprilwasorderedfromNorthChinaPharmaceuticalCo.,Ltd. (batchnumber: 1109002).
    1.2Preparationofhypertensionmodel
    FortymaleSDrats(180-220g)werepurchasedfromthePekingUniversityHealthScienceLaboratoryAnimalScienceMinistry,CertificateofConformitySCXK-(Beijing) 2011-0012.Animalsweremaintainedunder12hlight/darkcyclesatatemperatureofapproximately24±1 ℃withfoodandwateradlibitum.After3days,animalswererandomlydividedintotwogroups,thecontrolgroupandthehypertensionmodelgroup.Leftrenalarterystenosiswasinducedusingthe2K1Cmethodtoestablishhypertensionmodel.Heartrateandbloodpressureinratsafteroperationweredeterminedbythedetector(CODAMonitorTypenoninvasivebloodpressuremeter,USAKentScientificCorporation).Bloodpressurewasmonitoredwiththetailcuffmethodfor4weeks.Ratswithhigherthan160mmHgsystolicbloodpressureswereselectedandrandomlydividedintothreegroups(n=8foreachgroup).Groupinganddosingregimenisasfollows:rosiglitazonegroup: 20mg/kg;captoprilgroup: 10mg/kg;blankgroupandmodelgroupweregivenanequalvolumeofsaline.Ratswereadministratedbyintragastricadministrationonceadayforconsecutive14days.
    1.3 Blood pressure monitoring and sample collection
    Rats’ blood pressures were measured at 0 d, 4 d, 7 d, 10 d, and 14 d respectively after administration. After the last administration, rats were anesthetized with 10% chloral hydrates (300 mg/kg, ip). Abdominal aortic blood samples were used to determine AngII (Beijing Biotechnology Co., Keno spring, lot: 20120501A), serum total cholesterol (kit, TCH, batch number: 2011110012), triglycerides (kit,TG, batch number: 2011110011), superoxide dismutase (kit,SOD, batch number: 20120306), malondialdehyde (kit, MDA, batch number: 20111101), reduced glutathione (kit, GSH, batch number: 20120515) and hydrogen peroxide (kit, H2O2, batch number: 20120511, purchased from Nanjing Jiancheng Bioengineering Institute). Rats were sacrificed to take kidneys for detecting angiotensin II receptor 1 (Angiotensin II type 1 receptor, AT1) (kit, Beijing Keno spring Biotech Co., Ltd., batch number: 20120501A).
    1.4 Statistical analysis
    2 Results and discussion
    2.1 Effect of rosiglitazone on renal vascular hypertension in rats
    Experimental results show that systolic blood pressure and diastolic blood pressureof model group were significantly higher compared with control group, rosiglitazone group and captopril group (P<0.01) on 0 d, suggesting the hypertension model was established successfully; after 14 d administration compared with model group, systolic blood pressure in captopril group and rosiglitazone group were significantly lower, with the average reduction of 20.2% and 30.0%, respectively (P<0.01). And the diastolic blood pressure were also significantly lower with the average reduction of 21.8%, 28.0% respectively (P<0.01). The results shown in Tab.1 and Tab.2 suggest that rosiglitazone has a significant anti-hypertensive effect on renal hypertensive rats.
    Tab.1 Effect of rosiglitazone on systolic blood pressure in renovascular hypertensive rats ±s, n=8, mmHg)
    Compared with control,*P<0.05, **P<0.01; compared with Induced untreated group,#P<0.05,##P<0.01
    Tab.2 Effect of rosiglitazone on diastolic blood pressure in renovascular hypertensive rats ±s, n=8, mmHg)
    Compared with control,*P<0.05, **P<0.01; compared with Induced untreated group,#P<0.05,##P<0.01
    2.2 Effects of rosiglitazone on AngII and AT1in renal hypertensive rats
    Experimental results(Fig.1) showed that: compared with the control group, the contents of Ang II, AT1in model group were significantly increased (P<0.01); compared with induced untreated group, the contents of Ang II, AT1in rosiglitazone group and captopril group were significantly reduced (P<0.01). Thus, the results suggested that rosiglitazone plays an important role of regulating the activity of the renin-angiotensin in vivo.
    2.3 Effect of rosiglitazone on the levels of oxidative stress in renal hypertensive rats
    Tab.3 showed that, the activity of SOD and GSH in induced untreated group was significantly lower than the control group (P<0.05), and MDA and H2O2content was significantly higher than the control group (P<0.05); SOD and GSH levels in rosiglitazone and captopril group were significantly increased compared with the induced untreated group. The level of MDA and H2O2were significantly reduced (P<0.05). Conclusion can be made that rosiglitazone can regulate SOD, GSH, MDA; H2O2levels, and enhance body’s ability of anti-oxidative stress to mediate the hypertension.
    Fig.1 Effects of rosiglitazone on AngII and AT1 in renal hypertensive rats (compared with control, *P<0.05, **P<0.01; compared with Induced untreated group,#P<0.05,##P<0.01)
    2.4 Effect of rosiglitazone on TCH and TG in renal hypertensive rats
    As shown in Fig.2, TCH and TG serum contents in induced untreated group was significantly increased compared with the control group (P<0.05); Compared with induced untreated group, TCH, TG contents of the rosiglitazone group and captopril group decreased significantly (P<0.01). These results indicated that rosiglitazone had effect on the TCH and TG contents in renal hypertensive rats.
    Tab.3 Effect of rosiglitazone on serum oxidative stress level in renovascular hypertensive rats ±s, n=8)
    compared with control, *P<0.05, **P<0.01; compared with Induced untreated group,#P<0.05,##P<0.01
    Fig.2 Effect of rosiglitazone on TCH and TG in renal hypertensive rats ±s, n=8)(compared with control, *P<0.05, **P<0.01; compared with Induced untreated group,#P<0.05,##P<0.01)
    3 Discussion and conclusions
    In the 2K1C model, renovascular hypertension is featured by elevated AngII expression resulted from ischemia in the clipped kidney and shear stress in the non-clipped kidney, activating rennin-angiotensial-aldosterone system (RAAS), and sustained increase of blood pressure. AngII is the primary effector molecule of the renin-angiotensin system. It is primarily recognized for its role in the regulation of arterial pressure and blood volume[9]. The effects of Ang II on cardiovascular and reproductive functions are mainly mediated through Ang II type 1 (AT1) receptor. Therefore, specific AT1antagonists are potentially useful for treating hypertension and for improving sexual dysfunction in hypertensive patients[10]. Our data suggest that rosiglitazone could decline the AngII content, and decrease the ability of the vasoconstriction. Meanwhile, the expression value of AT1in vivo was also reduced. Thus, rosiglitazone can inhabit RAS in rats, and improved hypertension system.
    In previous studies, Raji et al. have showed a positive correlation between BP values and insulin sensitivity in patients treated with rosiglitazone[11]. Whether oxidative stress and lipid metabolism play roles in mediating the blood pressure in hypertension rat has not been determined. Lipid metabolism disorder can influence the membrane Ca2+transporters involved in the pathogenesis of hypertension through affect lipid structure[12]. Previous studies have found that cholesterol-lowering is beneficial to the reduction of blood pressure. The present study reveals that rosiglitazone can attenuate hypertension by the reduction of TCH and TG in renal vascular hypertension rats.
    Oxidative stress has been implicated in pathophysiological conditions (e.g., cigarette smoking, hypercholesterolemia, diabetes, and hypertension[13-15]) that affect the cardiovascular system[16-18]. Oxidative stress is a major factor in mediating hypertension[10]. In spontaneously hypertensive rats, there is a found of increased level of oxyradical production from xanthine oxidase activity and the formation of lipid peroxide[19]. Level of MDA is an estimate of lipid per oxidation[20]. The results indicate that rosiglitazone could improve the levels of SOD and GSH, decrease the contents of MDA and H2O2, and improve the oxidative stress which maybe the mechanism of contributing to the reduction of blood pressure.
    In conclusion, the present study reveals the potential protective effect of rosiglitazone against the renovascular hypertensive, which seems to be related to down-regulated activity of angiotensin, improved oxidative stress, and attenuation of serum lipid.
    [1] Yu Tingting, Guo Kun, Chen Hanchun, et al. Effect of traditional Chinese medicine Xin-Ji-Er-Kang formula on 2K1C hypertension rats: role of oxidative stress and endothelial dysfunction[J].BMC Complementary and Alternative Medicine,2013,13:173-183.
    [2] Pistrosch F, Passauer J, Herbrig K, et al. Effect of thiazolidinedione treatment on proteinuria and renal hemodynamic in type 2 diabetic patients with overt nephropathy [J]. Hormone and Metabolic Research, 2012, 44(12):914-918.
    [3] Basile D P, Donohoe D L, Phillips S A, et al. Enhanced skeletal musclearteriolar reactivity to ANGII after recovery from ischemic acute renalailure [J]. Am J Physiol Regul Integr Comp Physiol2005,289:1770-1776.
    [4] Yoshimoto T, Naruse M, Shizume H, et al. Vasculo-protective of insulin sensitizing agent pioglitazone in neointinmal thickening and hypertensive vascular hepertrophy [J]. Atherosclerosis, 1999, 145:333-340.
    [5] Walker A B, Chattington P D, Buckingham R E, et al. The thiazolidinedione rosiglitazone (BRL-49653) lowers blood preasure and protects against impairment of endothelial function in Zucker fatty rats [J]. Diabetes, 1999, 48:1448-1450.
    [6] Chen Junqun, Huang Qiren. PPARγand insulin resistance[J]. National Medical Frontiers of China, 2011,20:12-13
    [7] El-Gowelli H M, Abd-Elrahman K S, Saad E I, et al. PPAR gamma dependence of cyclosporine-isoprenaline renovascular interaction: roles of nitric oxide synthase and heme oxygenase [J]. Journal of Cardiovascular Pharmacology, 2011, 58(2):173-180.
    [8] Reaven G M. Banting Lecture 1998. Role of insulin resistance in human disease [J]. Diabetes, 1988, 37(12):1595-1607.
    [9] Kim S, Iwao H. Molecular and cellular mechanisms of angiotensinII-mediated cardiovascular and renal diseases [J]. Pharmacol Reviews, 2000, 52:11-34.
    [10] Karin Viana Weissheimer, Celso Rodrigues Franci, Aldo Bolten Lucion, et al. The role of AT1 receptor-mediated reproductive function in renovascular hypertension in male rats [J]. Hormones and Behavior 2012,62: 43-49.
    [11] Annaaswamy Raji, Ellen W Seely, Shannon A Bekins, et al. Rosiglitazone improves insulin sensitivity and lowers blood pressure in hypertensive patients [J]. Diabetes Care, 2003, 26: 172-178.
    [12] Xu Dingli. Hypertension and lipid metabolism disorder [J].Chin J Cardiol, 2006, 34:36-39.
    [13] Steinberg D, Witztum J L. Is the oxidative modification hypothesis relevant to human atherosclerosis? [J].Circulation, 2002, 105:2107-2111.
    [14] Chilsom G M, Steimberg D. The oxidative modification hypothesis of atherogenesis: an overview [J]. Free Radic Biol Med, 2000, 28:1815-1826.
    [15] Cai H, Harrison D G. Endothelial dysfunction in cardiovascular disease: the role of oxidant stress [J]. Circ Res, 2000, 87:840-844.
    [16] Denner L A, Rodriguez-Rivera J, Haidacher S J, et al. Cognitive enhancement with rosiglitazone links the hippocampal PPARgamma and ERK MAPK signaling pathways [J]. The Journal of Neuroscien, 2012, 32(47):16725-16735.
    [17] Dong J, Wong S L, Lau C W, et al. Calcitriol protects renovascular function in hypertension by down-regulating angiotensin II type 1 receptors and reducing oxidative stress [J]. European Heart Journal, 2012, 33(23):2980-2990.
    [18] da Costa C A, de Oliveira P R B, de Bem G F, et al. Euterpe oleracea Mart.-derived polyphenols prevent endothelial dysfunction and vascular structural changes in renovascular hypertensive rats: role of oxidative stress[J]. Naunyn-Schmiedeberg’s Arch Pharmacol, 2012, 385:1199-1209.
    [19] Suzuki H, Delano F A, Parks D A, et al. Xanthine oxidase activity associated with arterial blood pressure in spontaneously hypertensive rats [J]. Proc Natl Acad Sci USA, 1998, 95:4754-4759.
    [20] Varga E,Bodi A,F(xiàn)erdinandy P. The protective effect of EGb in isolated ischemic/reperfused rat hearts: a link between cardiac function and nitric oxide production [J]. Cardiovasc Pharmacol, 2001, 34(5):711.
    (Edited by Wang Yuxia)
    10.15918/j.jbit1004-0579.201524.0321
    R 977 Document code: A Article ID: 1004- 0579(2015)03- 0422- 05
    Received 2014- 01- 07
    E-mail: leeyan@bit.edu.cn
    

    
                        
    猜你喜歡
    
                        
    李巖夏雨
    
                        
    求MDS 碼權(quán)多項(xiàng)式的組合方法
    李巖國(guó)畫選
    人生之感悟
    夏雨
    再論李巖其人
    文史哲(2020年5期)2020-09-22 08:47:20
    重溫《甲申三百年祭》增強(qiáng)執(zhí)政憂患意識(shí)
    大東方(2017年10期)2017-05-30 10:48:04
    夏雨
    李巖繪畫作品選登
    那一夜(短篇小說(shuō))
    夏雨
    
                    
    
            
    
        
    
        
        
    
    
    

    










а√天堂www在线а√下载|
可以在线观看的亚洲视频|
久久久久久久精品吃奶|
哪里可以看免费的av片|
有码 亚洲区|
狠狠狠狠99中文字幕|
99久久精品国产亚洲精品|
亚洲三级黄色毛片|
国产老妇女一区|
色在线成人网|
我的女老师完整版在线观看|
or卡值多少钱|
99在线视频只有这里精品首页|
日本三级黄在线观看|
伊人久久精品亚洲午夜|
亚洲成人精品中文字幕电影|
少妇裸体淫交视频免费看高清|
欧美xxxx性猛交bbbb|
怎么达到女性高潮|
亚洲电影在线观看av|
久久婷婷人人爽人人干人人爱|
精品免费久久久久久久清纯|
欧美丝袜亚洲另类
|
看黄色毛片网站|
av在线蜜桃|
精品乱码久久久久久99久播|
中亚洲国语对白在线视频|
亚洲av不卡在线观看|
国产精品亚洲美女久久久|
国产精品久久久久久亚洲av鲁大|
欧美性感艳星|
一级av片app|
色综合婷婷激情|
日本免费一区二区三区高清不卡|
欧美日韩中文字幕国产精品一区二区三区|
一级黄片播放器|
成人欧美大片|
久久欧美精品欧美久久欧美|
麻豆国产97在线/欧美|
国产精品嫩草影院av在线观看
|
日韩欧美国产在线观看|
九九在线视频观看精品|
免费高清视频大片|
国产人妻一区二区三区在|
精品一区二区三区av网在线观看|
精品一区二区三区视频在线观看免费|
国产欧美日韩精品亚洲av|
高清毛片免费观看视频网站|
亚洲欧美日韩高清在线视频|
国产午夜福利久久久久久|
avwww免费|
欧美zozozo另类|
亚洲精品456在线播放app
|
日韩成人在线观看一区二区三区|
两个人视频免费观看高清|
久久草成人影院|
欧美绝顶高潮抽搐喷水|
久久国产乱子免费精品|
老鸭窝网址在线观看|
内地一区二区视频在线|
久久精品91蜜桃|
最新中文字幕久久久久|
www.www免费av|
久久久久精品国产欧美久久久|
一个人看的www免费观看视频|
在线观看一区二区三区|
天天躁日日操中文字幕|
国产在线精品亚洲第一网站|
久久久久精品国产欧美久久久|
国产黄片美女视频|
深夜精品福利|
18禁黄网站禁片午夜丰满|
成人精品一区二区免费|
亚洲自拍偷在线|
国内毛片毛片毛片毛片毛片|
特大巨黑吊av在线直播|
欧美区成人在线视频|
国产精品久久久久久精品电影|
精品久久久久久久末码|
欧美一级a爱片免费观看看|
久久香蕉精品热|
丰满人妻一区二区三区视频av|
成人无遮挡网站|
av黄色大香蕉|
熟女电影av网|
九九热线精品视视频播放|
99热6这里只有精品|
日韩欧美在线乱码|
美女免费视频网站|
欧美zozozo另类|
淫妇啪啪啪对白视频|
亚洲 欧美 日韩 在线 免费|
波多野结衣高清作品|
久久午夜亚洲精品久久|
中文字幕av在线有码专区|
神马国产精品三级电影在线观看|
狠狠狠狠99中文字幕|
99热这里只有精品一区|
国产精品一区二区三区四区免费观看
|
少妇裸体淫交视频免费看高清|
国产精品伦人一区二区|
久久久久国产精品人妻aⅴ院|
eeuss影院久久|
丝袜美腿在线中文|
亚洲欧美日韩高清在线视频|
国产午夜精品久久久久久一区二区三区
|
婷婷亚洲欧美|
九九久久精品国产亚洲av麻豆|
日韩av在线大香蕉|
亚洲成人久久爱视频|
久久精品国产亚洲av天美|
婷婷精品国产亚洲av|
久久久久久久久大av|
日本一二三区视频观看|
小蜜桃在线观看免费完整版高清|
色噜噜av男人的天堂激情|
亚洲av熟女|
亚洲欧美激情综合另类|
尤物成人国产欧美一区二区三区|
午夜久久久久精精品|
久久久精品大字幕|
国产精品98久久久久久宅男小说|
最新中文字幕久久久久|
久久久久久久精品吃奶|
久久久久性生活片|
日本在线视频免费播放|
99久久99久久久精品蜜桃|
h日本视频在线播放|
五月伊人婷婷丁香|
嫩草影院精品99|
欧美激情在线99|
亚洲成a人片在线一区二区|
国产av麻豆久久久久久久|
亚洲精品在线美女|
中文字幕人成人乱码亚洲影|
超碰av人人做人人爽久久|
国产精华一区二区三区|
免费在线观看亚洲国产|
日本一本二区三区精品|
日韩中文字幕欧美一区二区|
亚洲av.av天堂|
亚洲国产精品成人综合色|
一进一出抽搐动态|
看黄色毛片网站|
亚洲专区中文字幕在线|
国产精品一及|
欧美在线一区亚洲|
最新在线观看一区二区三区|
日日夜夜操网爽|
久久精品91蜜桃|
欧美黄色片欧美黄色片|
一边摸一边抽搐一进一小说|
午夜福利成人在线免费观看|
国产精品乱码一区二三区的特点|
91字幕亚洲|
国产三级黄色录像|
亚洲最大成人手机在线|
亚洲精品乱码久久久v下载方式|
日韩国内少妇激情av|
日韩精品青青久久久久久|
日韩欧美一区二区三区在线观看|
亚洲七黄色美女视频|
三级毛片av免费|
中文在线观看免费www的网站|
91狼人影院|
国产爱豆传媒在线观看|
久久婷婷人人爽人人干人人爱|
国产精品女同一区二区软件
|
夜夜爽天天搞|
久久久久性生活片|
亚洲在线观看片|
看十八女毛片水多多多|
av中文乱码字幕在线|
亚洲熟妇中文字幕五十中出|
女人十人毛片免费观看3o分钟|
国产麻豆成人av免费视频|
亚洲人成网站高清观看|
久久国产精品影院|
热99在线观看视频|
欧美日韩福利视频一区二区|
亚洲经典国产精华液单
|
韩国av一区二区三区四区|
深夜a级毛片|
成人无遮挡网站|
精品久久久久久久人妻蜜臀av|
av国产免费在线观看|
一本久久中文字幕|
免费av观看视频|
亚洲美女视频黄频|
国产精品嫩草影院av在线观看
|
三级男女做爰猛烈吃奶摸视频|
国产成年人精品一区二区|
99在线人妻在线中文字幕|
亚洲成a人片在线一区二区|
av福利片在线观看|
精品久久国产蜜桃|
别揉我奶头 嗯啊视频|
麻豆久久精品国产亚洲av|
在线观看美女被高潮喷水网站
|
欧美bdsm另类|
午夜精品久久久久久毛片777|
日本熟妇午夜|
色综合亚洲欧美另类图片|
午夜激情欧美在线|
亚洲 欧美 日韩 在线 免费|
91久久精品国产一区二区成人|
亚洲在线自拍视频|
avwww免费|
亚洲成人久久爱视频|
看十八女毛片水多多多|
极品教师在线免费播放|
色尼玛亚洲综合影院|
国内少妇人妻偷人精品xxx网站|
69人妻影院|
亚洲欧美日韩高清在线视频|
黄色女人牲交|
成人鲁丝片一二三区免费|
动漫黄色视频在线观看|
亚洲aⅴ乱码一区二区在线播放|
亚洲在线观看片|
一级a爱片免费观看的视频|
精品欧美国产一区二区三|
国产免费男女视频|
免费高清视频大片|
www.熟女人妻精品国产|
午夜福利18|
免费观看的影片在线观看|
91九色精品人成在线观看|
久久99热这里只有精品18|
国产成人aa在线观看|
免费无遮挡裸体视频|
九九热线精品视视频播放|
99久久成人亚洲精品观看|
午夜福利在线在线|
1024手机看黄色片|
免费av不卡在线播放|
国产精品自产拍在线观看55亚洲|
av黄色大香蕉|
一区福利在线观看|
国产69精品久久久久777片|
日韩中文字幕欧美一区二区|
嫩草影院入口|
亚洲va日本ⅴa欧美va伊人久久|
亚洲18禁久久av|
亚洲av电影不卡..在线观看|
神马国产精品三级电影在线观看|
在现免费观看毛片|
又紧又爽又黄一区二区|
亚洲国产精品成人综合色|
亚洲中文日韩欧美视频|
欧美精品国产亚洲|
午夜久久久久精精品|
亚洲欧美日韩无卡精品|
99热6这里只有精品|
成人特级黄色片久久久久久久|
欧美一区二区亚洲|
在线国产一区二区在线|
变态另类丝袜制服|
99久久成人亚洲精品观看|
亚洲成人精品中文字幕电影|
国内精品久久久久久久电影|
悠悠久久av|
69av精品久久久久久|
天堂av国产一区二区熟女人妻|
国产蜜桃级精品一区二区三区|
色视频www国产|
每晚都被弄得嗷嗷叫到高潮|
99riav亚洲国产免费|
特级一级黄色大片|
露出奶头的视频|
国产高清三级在线|
国产蜜桃级精品一区二区三区|
欧美丝袜亚洲另类
|
长腿黑丝高跟|
天堂影院成人在线观看|
在线观看一区二区三区|
婷婷丁香在线五月|
91av网一区二区|
国产成人aa在线观看|
亚洲成人免费电影在线观看|
亚洲精品影视一区二区三区av|
免费av观看视频|
国产欧美日韩精品亚洲av|
国产av一区在线观看免费|
美女大奶头视频|
久9热在线精品视频|
亚洲av二区三区四区|
欧美一区二区亚洲|
韩国av一区二区三区四区|
九色成人免费人妻av|
99久久成人亚洲精品观看|
亚洲精品成人久久久久久|
18禁黄网站禁片午夜丰满|
动漫黄色视频在线观看|
美女cb高潮喷水在线观看|
亚洲最大成人中文|
亚洲av第一区精品v没综合|
国产激情偷乱视频一区二区|
国产av不卡久久|
中文在线观看免费www的网站|
欧美bdsm另类|
成人亚洲精品av一区二区|
久久欧美精品欧美久久欧美|
中文字幕精品亚洲无线码一区|
午夜福利在线观看免费完整高清在
|
日本在线视频免费播放|
久久精品夜夜夜夜夜久久蜜豆|
亚洲一区高清亚洲精品|
av天堂在线播放|
麻豆国产av国片精品|
欧美日韩综合久久久久久
|
亚洲成av人片免费观看|
久久香蕉精品热|
男女视频在线观看网站免费|
看十八女毛片水多多多|
男女视频在线观看网站免费|
精品福利观看|
中亚洲国语对白在线视频|
少妇熟女aⅴ在线视频|
最近视频中文字幕2019在线8|
精品国内亚洲2022精品成人|
91麻豆精品激情在线观看国产|
色视频www国产|
亚洲av成人不卡在线观看播放网|
99在线视频只有这里精品首页|
夜夜看夜夜爽夜夜摸|
亚洲精华国产精华精|
亚洲最大成人中文|
欧美zozozo另类|
一个人看视频在线观看www免费|
中文字幕熟女人妻在线|
看黄色毛片网站|
麻豆国产97在线/欧美|
亚洲在线自拍视频|
国产欧美日韩精品亚洲av|
观看免费一级毛片|
深夜精品福利|
怎么达到女性高潮|
床上黄色一级片|
国内精品久久久久精免费|
一进一出好大好爽视频|
国产 一区 欧美 日韩|
黄色女人牲交|
日本在线视频免费播放|
91麻豆精品激情在线观看国产|
亚洲不卡免费看|
18禁黄网站禁片免费观看直播|
亚洲成a人片在线一区二区|
97碰自拍视频|
xxxwww97欧美|
午夜影院日韩av|
少妇人妻精品综合一区二区
|
亚洲精华国产精华精|
99国产精品一区二区三区|
亚洲av一区综合|
国产午夜精品论理片|
or卡值多少钱|
欧美+日韩+精品|
黄色视频,在线免费观看|
看免费av毛片|
天堂动漫精品|
脱女人内裤的视频|
丰满乱子伦码专区|
亚洲国产日韩欧美精品在线观看|
黄色视频,在线免费观看|
netflix在线观看网站|
色综合站精品国产|
小蜜桃在线观看免费完整版高清|
АⅤ资源中文在线天堂|
成人精品一区二区免费|
黄色视频,在线免费观看|
中文资源天堂在线|
亚洲七黄色美女视频|
757午夜福利合集在线观看|
一夜夜www|
特级一级黄色大片|
丝袜美腿在线中文|
欧美激情久久久久久爽电影|
国产精品久久视频播放|
国产精品1区2区在线观看.|
日本免费a在线|
中文资源天堂在线|
69人妻影院|
国内精品一区二区在线观看|
精品久久久久久久末码|
久久精品91蜜桃|
最后的刺客免费高清国语|
日本成人三级电影网站|
一本久久中文字幕|
1000部很黄的大片|
中文字幕精品亚洲无线码一区|
人人妻,人人澡人人爽秒播|
欧美色欧美亚洲另类二区|
最好的美女福利视频网|
中出人妻视频一区二区|
久久亚洲精品不卡|
真实男女啪啪啪动态图|
一二三四社区在线视频社区8|
中文字幕久久专区|
国产三级黄色录像|
一本综合久久免费|
亚洲国产精品成人综合色|
免费av不卡在线播放|
日韩高清综合在线|
色哟哟哟哟哟哟|
99在线视频只有这里精品首页|
成人毛片a级毛片在线播放|
欧美xxxx性猛交bbbb|
日本五十路高清|
美女高潮的动态|
精品久久久久久,|
特大巨黑吊av在线直播|
亚洲激情在线av|
国产 一区 欧美 日韩|
亚洲18禁久久av|
丁香六月欧美|
国产精品自产拍在线观看55亚洲|
欧美精品啪啪一区二区三区|
国模一区二区三区四区视频|
成年女人看的毛片在线观看|
成人性生交大片免费视频hd|
国产精品久久久久久亚洲av鲁大|
国产精品久久久久久久久免
|
国产亚洲欧美98|
美女免费视频网站|
av黄色大香蕉|
九色成人免费人妻av|
国产精品人妻久久久久久|
深爱激情五月婷婷|
国产精品一区二区三区四区免费观看
|
婷婷色综合大香蕉|
级片在线观看|
99在线人妻在线中文字幕|
中文字幕高清在线视频|
91在线精品国自产拍蜜月|
国产白丝娇喘喷水9色精品|
在线观看午夜福利视频|
国内精品美女久久久久久|
精品人妻熟女av久视频|
少妇人妻一区二区三区视频|
黄色丝袜av网址大全|
欧美黄色片欧美黄色片|
久久久久久久久中文|
午夜亚洲福利在线播放|
久久国产精品影院|
国产真实乱freesex|
97碰自拍视频|
老司机福利观看|
免费av毛片视频|
欧美一级a爱片免费观看看|
丰满乱子伦码专区|
黄色配什么色好看|
男插女下体视频免费在线播放|
国产高潮美女av|
97超级碰碰碰精品色视频在线观看|
亚洲精品一区av在线观看|
中出人妻视频一区二区|
丰满人妻一区二区三区视频av|
成人一区二区视频在线观看|
制服丝袜大香蕉在线|
又黄又爽又免费观看的视频|
男人的好看免费观看在线视频|
国产野战对白在线观看|
午夜免费激情av|
国产毛片a区久久久久|
日本免费a在线|
丁香六月欧美|
日韩欧美一区二区三区在线观看|
中出人妻视频一区二区|
国产野战对白在线观看|
99热这里只有是精品在线观看
|
免费在线观看亚洲国产|
日本免费一区二区三区高清不卡|
日韩有码中文字幕|
一区二区三区激情视频|
色精品久久人妻99蜜桃|
国产精品亚洲美女久久久|
观看美女的网站|
中文资源天堂在线|
亚洲av美国av|
丰满人妻熟妇乱又伦精品不卡|
久久国产乱子免费精品|
免费在线观看亚洲国产|
欧美一区二区精品小视频在线|
美女cb高潮喷水在线观看|
在线a可以看的网站|
啪啪无遮挡十八禁网站|
两性午夜刺激爽爽歪歪视频在线观看|
久久久久久大精品|
麻豆一二三区av精品|
欧美精品国产亚洲|
亚洲av成人精品一区久久|
久久精品国产清高在天天线|
婷婷丁香在线五月|
av国产免费在线观看|
亚洲精品456在线播放app
|
中文字幕人成人乱码亚洲影|
国产单亲对白刺激|
亚洲乱码一区二区免费版|
99热这里只有是精品在线观看
|
免费在线观看成人毛片|
亚洲国产精品999在线|
精品久久久久久成人av|
有码 亚洲区|
天天一区二区日本电影三级|
亚洲av免费高清在线观看|
国产野战对白在线观看|
老女人水多毛片|
亚洲最大成人av|
老熟妇乱子伦视频在线观看|
真人一进一出gif抽搐免费|
人人妻人人澡欧美一区二区|
乱码一卡2卡4卡精品|
or卡值多少钱|
麻豆成人av在线观看|
18禁黄网站禁片午夜丰满|
久久精品久久久久久噜噜老黄
|
国产白丝娇喘喷水9色精品|
免费人成视频x8x8入口观看|
国产老妇女一区|
无人区码免费观看不卡|
人人妻人人澡欧美一区二区|
久久草成人影院|
少妇丰满av|
欧美最黄视频在线播放免费|
99国产精品一区二区蜜桃av|
每晚都被弄得嗷嗷叫到高潮|
色av中文字幕|
精品久久国产蜜桃|
精品福利观看|
午夜激情福利司机影院|
国产精品久久久久久精品电影|
天堂av国产一区二区熟女人妻|
69av精品久久久久久|
一进一出抽搐gif免费好疼|
成熟少妇高潮喷水视频|
有码 亚洲区|
99久久九九国产精品国产免费|
精品欧美国产一区二区三|
亚洲精品日韩av片在线观看|
日韩大尺度精品在线看网址|
欧美激情在线99|
久久久久久九九精品二区国产|
一卡2卡三卡四卡精品乱码亚洲|
免费高清视频大片|
国产精品国产高清国产av|
亚洲国产色片|
久久精品夜夜夜夜夜久久蜜豆|
国产激情偷乱视频一区二区|
亚洲精品影视一区二区三区av|
亚洲精品亚洲一区二区|
欧美国产日韩亚洲一区|
亚洲狠狠婷婷综合久久图片|
av天堂中文字幕网|
99久久精品国产亚洲精品|
国产精品,欧美在线|
国产亚洲精品综合一区在线观看|
亚洲无线观看免费|
俺也久久电影网|
欧美日本亚洲视频在线播放|
国产 一区 欧美 日韩|
国产精品女同一区二区软件
|
亚洲熟妇中文字幕五十中出|
欧美日韩瑟瑟在线播放|
可以在线观看的亚洲视频|
九九久久精品国产亚洲av麻豆|
欧美高清成人免费视频www|
日韩高清综合在线|
色在线成人网|
免费在线观看日本一区|
亚洲七黄色美女视频|
两个人的视频大全免费|
国产精品久久电影中文字幕|
a级毛片a级免费在线|
熟女电影av网|
国产v大片淫在线免费观看|
麻豆国产97在线/欧美|
亚洲精品一卡2卡三卡4卡5卡|
99热6这里只有精品|
黄片小视频在线播放|
欧美乱色亚洲激情|
国产真实乱freesex|
久久精品国产亚洲av香蕉五月|
国产亚洲精品av在线|
一本久久中文字幕|
亚洲成人中文字幕在线播放|
日日摸夜夜添夜夜添小说|
欧美xxxx黑人xx丫x性爽|
亚洲乱码一区二区免费版|
国产色婷婷99|
欧美在线一区亚洲|
好男人电影高清在线观看|
精品人妻一区二区三区麻豆
|
波多野结衣高清无吗|
真实男女啪啪啪动态图|
一区二区三区四区激情视频
|
成人亚洲精品av一区二区|
欧美性猛交黑人性爽|
国产精品亚洲一级av第二区|
欧美丝袜亚洲另类
|
国产淫片久久久久久久久
|
久久久国产成人精品二区|
长腿黑丝高跟|
在线观看66精品国产|
欧美中文日本在线观看视频|
国产一区二区在线av高清观看|
日本成人三级电影网站|
成年女人毛片免费观看观看9|
亚洲国产欧美人成|
亚洲中文字幕日韩|
色av中文字幕|
亚洲性夜色夜夜综合|
免费在线观看影片大全网站|
国内久久婷婷六月综合欲色啪|
美女xxoo啪啪120秒动态图
|