Tauroursodeoxycholic acid(TUDCA)improves intestinal barrier function associated with TGR5-MLCK pathway and the alteration of serum metabolites and gut bacteria in weaned piglets

Background:Tauroursodeoxycholic acid(TUDCA),a hydrophilic bile acid,is the main medicinal component of bear bile and is commonly used to treat a variety of hepatobiliary diseases.Meanwhile,TUDCA has been shown to modulate the intestinal barrier function and alleviate DSS-induced colitis in mice.However,the effect of TUDCA on the intestinal barrier of weaned piglets remains largely unclear.Methods:The weaned piglets and porcine IPEC-J2 intestinal epithelial cells were used to investigate the effects of TUDCA on intestinal barrier function in weaned piglets and explore the possible underlying mechanisms.In vivo,72 healthy weaned piglets were randomly allocated into 2 groups according to their gender and body weight,and piglets were fed the basal diet with 0(control,CON)and 200 mg/kg TUDCA for 30 d,respectively.Three female and three male piglets reflecting the average bodyweight were slaughtered in each group and samples were collected.In vitro,IPEC-J2 cells were subjected to 100μmol/L TUDCA to explore the possible underlying mechanisms.Results:Our results demonstrated that dietary TUDCA supplementation significantly reduced the diarrhea incidence of weaned piglets,possibly attributing to the TUDCA-enhanced intestinal barrier function and immunity.In addition,TUDCA supplementation altered serum metabolites and the relative abundance of certain gut bacteria,which might contribute to the improved intestinal barrier function.Furthermore,the in-vitro results showed that TUDCA improved the E.coli-induced epithelial barrier impairment of IPEC-J2 cells and increased Takeda G-coupled protein receptor 5(TGR5)protein expression.However,knockdown of TGR5 and inhibition of myosin light chain kinase(MLCK)pathway abolished the TUDCA-improved epithelial barrier impairment in E.coli-treated IPEC-J2 cells,indicating the involvement of TGR5-MLCK in this process.Conclusions:These findings showed that TUDCA improved intestinal barrier function associated with TGR5-MLCK pathway and the alteration of serum metabolites and gut bacteria in weaned piglets,suggesting the potential application of TUDCA in improving gut health in piglet production.

Efficacy and Safety of Tauroursodeoxycholic Acid in the Treatment of Liver Cirrhosis: A Double-blind Randomized Controlled Trial

No direct comparison of tauroursodeoxycholic acid （TUDCA） and ursodeoxycholic acid （UDCA） has yet been carried out in the treatment of liver cirrhosis in China. We designed a double-blind randomized trial to evaluate the potential therapeutic efficacy of TUDCA in liver cirrhosis, using UDCA as parallel control. The enrolled 23 patients with liver cirrhosis were randomly divided into TUDCA group （n=12） and UDCA group （n=l 1）, and given TUDCA and UDCA respectively at the daily dose of 750 mg, in a randomly assigned sequence for a 6-month period. Clinical, biochemical and histological features, and liver ultrasonographic findings were evaluated before and after the study. Ac- cording to the inclusion criteria, 18 patients were included in the final analysis, including 9 cases in both two groups. Serum ALT, AST and ALP levels in TUDCA group and AST levels in UDCA group were significantly reduced as compared with baseline （P〈0.05）. Serum albumin levels were significantly increased in both TUDCA and UDCA groups （P〈0.05）. Serum markers for liver fibrosis were slightly decreased with the difference being not significant in either group. Only one patient in TUDCA group had significantly histological relief. Both treatments were well tolerated and no patient complained of side effects. It is suggested that TUDCA therapy is safe and appears to be more effective than UDCA in the treatment of liver cirrhosis, particularly in the improvement of the biochemical expression. However, both drugs exert no effect on the serum markers for liver fibrosis during 6-month treatment.

Tauroursodeoxycholic acid:more than just a neuroprotective bile conjugate

Neurological diseases and the neuroinflammatory response：Neurological diseases are usually accompanied by dramatic changes in the tissue homeostasis,inducing a neuroinflammatory environment that leads to the progressive activation of central nervous system（CNS）resident cells.

Liver as a new target organ in Alzheimer's disease:insight from cholesterol metabolism and its role in amyloid-beta clearance

Alzheimer's disease,the primary cause of dementia,is characterized by neuropathologies,such as amyloid plaques,synaptic and neuronal degeneration,and neurofibrillary tangles.Although amyloid plaques are the primary characteristic of Alzheimer's disease in the central nervous system and peripheral organs,targeting amyloid-beta clearance in the central nervous system has shown limited clinical efficacy in Alzheimer's disease treatment.Metabolic abnormalities are commonly observed in patients with Alzheimer's disease.The liver is the primary peripheral organ involved in amyloid-beta metabolism,playing a crucial role in the pathophysiology of Alzheimer's disease.Notably,impaired cholesterol metabolism in the liver may exacerbate the development of Alzheimer's disease.In this review,we explore the underlying causes of Alzheimer's disease and elucidate the role of the liver in amyloid-beta clearance and cholesterol metabolism.Furthermore,we propose that restoring normal cholesterol metabolism in the liver could represent a promising therapeutic strategy for addressing Alzheimer's disease.

TUDCA通过抑制内质网应激及氧化应激减轻CCl_(4)所致小鼠急性肝损伤

目的:探讨牛磺熊去氧胆酸(TUDCA)对小鼠急性肝损伤的保护机制。方法:采用小鼠腹腔注射四氯化碳(CCl_(4))诱导急性肝损伤动物模型,通过测定血清转氨酶变化及观察肝组织切片HE染色,检测TUDCA对小鼠急性肝损伤的保护效果;采用硫代巴比妥酸(TBA)法检测血清中丙二醛(MDA)的含量及羟胺法检测血清中超氧化物歧化酶(SOD)活性;采用蛋白免疫印迹、PCR等方法检测肝组织中免疫球蛋白重链结合蛋白(Bip)、肌醇需求酶1(IRE1)、c-Jun氨基末端激酶(JNK)蛋白以及X盒结合蛋白1(XBP1)基因转录表达的变化,分析TUDCA对急性肝损伤的保护机制。结果:TUDCA显著保护由CCl_(4)中毒引发的肝组织病变,与单独急性肝损伤相比,TUDCA预处理显著增强肝组织的抗氧化水平,并抑制内质网应激程度。结论:TUDCA通过抑制由CCl_(4)中毒引发的内质网应激和氧化应激,对急性肝组织损伤具有显著保护作用。

Ursodeoxycholic acid improves gastrointestinal motility defects in gallstone patients

AIM: To simultaneously evaluate the presence of defects in gallbladder and gastric emptying, as well as in intestinal transit in gallstone patients (GS) and the effect of chronic ursodeoxycholic acid (UDCA) administration on these parameters and on serum bile acids and clinical outcome in GS and controls (CTR). METHODS: After a standard liquid test meal, gallbla-dder and gastric emptying (by ultrasound), oroileal transit time (OITT) (by an immunoenzymatic technique) and serum bile acids (by HPLC) were evaluated before and after 3 mo of UDCA (12 mg/kg bw/d) or placebo administration in 10 symptomatic GS and 10 matched healthy CTR. RESULTS: OITT was longer in GS than in CTR (P < 0.0001); UDCA significantly reduced OITT in GS (P < 0.0001), but not in CTR. GS had longer gastric half-emptying time (t1/2) than CTR (P < 0.0044) at baseline; after UDCA, t1/2 significantly decreased (P < 0.006) in GS but not in CTR. Placebo administration had no effect on gastric emptying and intestinal transit in both GS and CTR. CONCLUSION: The gallstone patient has simultaneous multiple impairments of gallbladder and gastric emptying, as well as of intestinal transit. UDCA administration restores these defects in GS, without any effect in CTR. These results confirm the pathogenetic role of gastrointestinal motility in gallstone disease and suggest an additional mechanism of action for UDCA in reducing bile cholesterol supersaturation.

TUDCA治疗视网膜色素变性机制的研究进展

牛磺熊去氧胆酸(tauroursodeoxycholic acid,TUDCA)是由牛磺酸连接熊去氧胆酸(ursodeoxycholic acid,UDCA)形成,具有抗炎、抗凋亡、降低胶原细胞激活的作用,而这些作用皆可能成为延缓视网膜色素变性(retinitis pigmentosa,RP)病理过程最关键的环节。研究证明,TUDCA对RP有潜在的治疗价值,本文就TUDCA治疗RP的机制研究进展进行综述。

牛磺熊去氧胆酸干预缺糖缺氧条件下脊髓神经元的凋亡

背景:牛磺熊去氧胆酸是一种亲水性胆汁酸衍生物,在多种神经系统疾病模型中均有神经保护作用,但目前鲜有报道研究牛磺熊去氧胆酸对脊髓损伤的作用。目的:观察缺糖缺氧条件下牛磺熊去氧胆酸对脊髓神经元凋亡的作用,以及对脊髓损伤后小鼠运动功能恢复的影响。方法:①体外实验:从孕13.5 d的C57 BL/6小鼠胚胎中分离提取原代脊髓神经元,培养72 h后,分3组处理:正常组加入Neurobasal完全培养基,置于CO_(2)培养箱(体积分数5%CO_(2)+95%空气)内培养24 h;氧糖剥夺组加入无糖的Neurobasal培养基,置于三气培养箱(体积分数94%N2+5%CO_(2)+1%O_(2))培养12 h,更换为Neurobasal完全培养基后置于CO_(2)培养箱内培养12 h;实验组处理过程大致同氧糖剥夺组,其中在加入无糖Neurobasal培养基的同时加入牛磺熊去氧胆酸。采用TUNEL染色检测细胞凋亡,CCK-8法检测细胞活性,免疫荧光染色检测细胞βⅢ微管蛋白表达。②动物实验:采用随机数字表法将60只C57 BL/6小鼠分为假手术组、脊髓损伤组与实验组,每组20只,脊髓损伤组与实验组采用Allen打击法建立T_(9)-T_(10)脊髓损伤模型,造模后第1天开始,实验组灌胃给予牛磺熊去氧胆酸溶液,假手术组与脊髓损伤组灌胃给予生理盐水,1次/d。连续给药14 d后,采用行为学和组织学方法评估脊髓组织修复情况。结果与结论:①体外实验:TUNEL染色、CCK-8与免疫荧光染色检测显示,氧糖剥夺组细胞凋亡数量高于正常组(P<0.01),细胞活性与βⅢ微管蛋白表达低于正常组(P<0.01);实验组细胞凋亡数量低于氧糖剥夺组(P<0.01),细胞活性与βⅢ微管蛋白表达高于氧糖剥夺组(P<0.01)。②动物实验:旷场实验BBB评分与后肢足迹实验显示,实验组小鼠行走与运动功能恢复程度好于脊髓损伤组。苏木精-伊红染色显示,脊髓损伤组小鼠脊髓损伤部位可见明显畸形和空洞,神经细胞数量明显减少;与脊髓损伤组比较,实验组脊髓损伤病变面积显著减小,脊髓畸形程度更小、空洞更少,神经细胞数量增加。免疫荧光染色显示,脊髓损伤组神经元胞核标记神经元细胞数量少于假手术组(P<0.01),实验组神经元胞核标记神经元细胞数量高于脊髓损伤组(P<0.01)。③结果表明:牛磺熊去氧胆酸能减少缺糖缺氧引起的脊髓神经元凋亡、轴突的丢失,促进脊髓损伤小鼠运动功能的恢复。

牛磺熊去氧胆酸通过抑制内质网应激诱导的凋亡促进类鼻疽菌的清除

目的 拟通过类鼻疽菌感染RAW264.7巨噬细胞模型,探讨牛磺熊去氧胆酸(tauroursodeoxycholic acid,TUDCA)促进类鼻疽菌胞内清除的作用机制。方法 类鼻疽菌感染RAW264.7细胞后8 h,设置未感染组和类鼻疽菌感染组,在不同浓度TUDCA处理条件下,采用流式细胞仪检测类鼻疽菌诱导细胞凋亡的情况;同时使用另外一种内质网应激抑制剂4-PBA,通过Annexin-V/PI双染法和MTT细胞增殖实验分别检测类鼻疽菌感染对宿主细胞凋亡和增殖的影响;进一步使用siRNA干扰内质网应激关键基因CHOP,设置siC对照组和siCHOP干扰组,通过Western blot和流式细胞仪检测类鼻疽菌感染后Caspase-3、Caspase-12等细胞凋亡相关蛋白的表达水平及细胞凋亡情况;通过细菌胞内生存实验分析TUDCA通过抑制内质网应激减少其诱导的细胞凋亡、增强巨噬细胞对类鼻疽菌胞内清除作用的机制。结果 在不同浓度TUDCA处理下,100μmol/L或200μmol/L TUDCA可明显减少类鼻疽菌感染诱导的RAW264.7细胞凋亡数量(P<0.05)。分别使用两种内质网应激抑制剂TUDCA和4-PBA均可降低类鼻疽菌感染诱导的细胞凋亡(P<0.05)。在siC对照组,相较于未感染时类鼻疽菌感染后Caspase-3和Caspase-12表达明显增加。在siCHOP干扰组,细胞凋亡相关蛋白的表达显著低于siC对照组,TUDCA处理后细胞凋亡相关蛋白表达水平与未加TUDCA药物相比无明显差异。流式细胞仪检测结果也显示,TUDCA能够减少类鼻疽菌感染后诱导的细胞凋亡(P<0.05),但在siCHOP干扰组中,TUDCA对类鼻疽菌感染诱导的凋亡无明显改变。细菌胞内生存计数结果显示,在siC对照组加入TUDCA能够增加宿主细胞对类鼻疽菌的清除(P<0.05),而在siCHOP干扰组中TUDCA的处理对类鼻疽菌胞内增殖无明显影响。结论 在类鼻疽菌感染RAW264.7细胞模型中,TUDCA能够通过抑制巨噬细胞内质网应激诱导的凋亡,促进巨噬细胞对类鼻疽菌的胞内清除。

牛磺熊去氧胆酸通过调节内质网应激抑制转化生长因子β1所诱导的心肌成纤维细胞纤维化

目的探讨牛磺熊去氧胆酸(TUDCA)对转化生长因子β1(TGF-β1)所诱导的心肌成纤维细胞(CFs)活化的作用及相关机制,为TUDCA治疗糖尿病心肌纤维化提供新的治疗目标。方法提取原代SD乳鼠CFs和心肌细胞,通过免疫荧光法鉴定CFs的纯度。分别将高糖培养下的CFs用不同时间的TGF-β1干预,用Western blot检测内质网应激(ERS)通路相关蛋白和纤维化指标的表达,探讨TGF-β1对CFs活化及ERS相关通路的影响。用Western blot检测CFs和心肌细胞内同型半胱氨酸内质网应激泛素样结构域1(Herpud1)的表达情况。通过沉默Herpud1的表达及用Transwell和Western blot检测沉默Herpud1后CFs纤维化指标的表达,探讨Herpud1在TGF-β1诱导的CFs活化中的作用。用CCK-8检测不同浓度的TUDCA处理下CFs的活力。用免疫荧光和Western blot检测TUDCA对TGF-β1诱导的CFs中Herpud1、葡萄糖调节蛋白78(GRP78)、转录激活因子6(ATF6)、α-平滑肌肌动蛋白(α-SMA)、波形蛋白(Vimentin)和Ⅰ型胶原蛋白(CollagenⅠ)表达的影响。为进一步明确Herpud1在TUDCA抑制CFs活化中的作用,用Western blot检测过表达Herpud1后相关蛋白的表达情况。结果在成功构建CFs纤维化模型的基础上,TGF-β1能够诱导CFs活化及ERS通路相关蛋白的表达;Herpud1在CFs中的表达高于心肌细胞;敲除Herpud1可抑制TGF-β1所诱导的CFs活化;TUDCA能显著降低TGF-β1诱导的CFs中GRP78、ATF6、α-SMA、Vimentin和CollagenⅠ的表达水平;此外,过表达Herpud1还可逆转TUDCA对TGF-β1诱导的CFs活化的抑制。结论下调Herpud1基因的表达是TUDCA抑制TGF-β1诱导的CFs纤维化的机制之一。

熊胆粉及其活性成分治疗神经系统疾病作用机制研究进展

熊胆粉活性成分熊去氧胆酸(ursodesxycholic acid, UDCA)、牛磺熊去氧胆酸(tauroursodeoxycholic acid, TUDCA)在不同的神经系统疾病动物模型中具有神经保护作用。其中UDCA、TUDCA可通过抑制丝裂原活化蛋白激酶(mitogen-activated protein kinase, MAPK)信号通路中细胞外调节蛋白激酶(extracellular regulated protein kinase, ERK)、c-Jun氨基末端激酶(c-Jun N-terminal kinasa, JNK)、p38 MAPK的磷酸化发挥抗神经炎症的作用;UDCA通过激活单磷酸腺苷活化蛋白激酶(AMP-activated protein kinase, AMPK)/雷帕霉素靶蛋白(mechanistic target of rapamycin, mTOR)和抑癌基因诱导的假定激酶蛋白1(PTEN induced putative kinase 1,PINK1)/RBR E3泛素蛋白连接酶(RBR E3 ubiquitin-protein ligase, Parkin)信号通路,抑制小鼠帕金森病(parkinson’s disease, PD)中神经细胞凋亡,增加线粒体自噬起到改善线粒体功能障碍和神经保护的作用。熊胆粉、TUDCA通过上调G蛋白偶联受体(G protein-coupled bile acid receptor 5,TGR5)的表达抑制蛋白激酶B(protein kinase B, Akt)/核因子-κB(nuclear factor-κB,NF-κB)信号通路的激活及调控巨噬细胞的分化,减轻神经炎症反应,保护神经细胞;TUDCA下调蛋白激酶R样内质网激酶(protrin kinase R-like ER kinase, PERK)/PERK-真核细胞起始因子2α(eukaryotic initiation factor 2α,eIF2α)/转录激活因子4(activating transcription factor 4,ATF4)/C/EBP同源蛋白(C/EBP-homologous protein, CHOP)信号通路的表达,上调CIBZ基因的表达,激活核因子E2相关因子2(nuclear factor-erythroid 2 related factor 2,Nrf2)/NADPH醌氧化还原酶1(NADPH quinone oxidoreductase 1,NQO1)、TGR5/去乙酰化酶3(recombinant sirtuin 3)等信号通路,抑制内质网应激、氧化应激所引起的神经细胞调亡,TUDCA通过调节细胞自噬和能量代谢抑制细胞凋亡发挥神经保护作用。现将近年来对熊胆粉、UDCA、TUDCA治疗神经系统病作用机制进行综述,为熊胆粉及其活性成分的临床运用提供参考。

傅里叶变换红外光谱结合化学计量学快速预测熊胆粉中牛磺熊去氧胆酸与牛磺鹅去氧胆酸含量

目的:建立用于熊胆粉中牛磺熊去氧胆酸(TUDCA)及牛磺鹅去氧胆酸(TCDCA)含量预测的傅里叶变换红外光谱预测模型,对熊胆粉进行快速质量评价。方法:以高效液相色谱法测定的98批熊胆粉中TUDCA及TCDCA含量为化学参考值;采集样品的红外光谱,筛选最佳光谱预处理方法、光谱波段及主因子个数,建立TUDCA和TCDCA含量预测的偏最小二乘回归模型。结果:熊胆粉中TUDCA和TCDCA红外定量分析模型的校正集相关系数(R2)分别为0.9446和0.9382,校正集均方根误差(RMSEC)依次为0.9551%和1.2854%,验证集R2分别为0.9121和0.8410,验证集均方根误差(RMSEP)依次为1.3058%和1.8748%。配对t检验结果表明预测值与实测值之间无显著性差异。结论:所建立的2个PLSR模型稳定,预测结果准确,可用于熊胆粉中TUDCA及TCDCA的快速定量分析。

牛磺熊去氧胆酸减轻重症急性胰腺炎诱导的模型大鼠肝损伤

目的探讨牛磺熊去氧胆酸(TUDCA)经蛋白激酶R样内质网激酶(PERK)通路对重症急性胰腺炎(SAP)大鼠肝损伤的作用及机制。方法将30只SD大鼠随机分为3组(每组10只):假手术组(SO组)、重症急性胰腺炎组(SAP组)和牛磺熊去氧胆酸组(TUDCA组)。通过逆行胰胆管注射5%牛磺胆酸钠(STC)溶液(1 mL/kg)建立SAP大鼠模型。造模前,TUDCA组大鼠连续3 d经腹腔注射TUDCA溶液(400 mg/kg·d-1),SAP组和SO组大鼠经腹腔注射等体积的0.9%氯化钠溶液。造模后12 h处死大鼠,采集静脉血及部分胰腺及肝组织,使用全自动生化仪检测淀粉酶(AMY)、谷草转氨酶(AST)和谷丙转氨酶(ALT)水平;酶联免疫吸附检测试剂盒(ELISA)检测白细胞介素-6(IL-6)的表达;苏木精-伊红(HE)染色观察胰腺及肝脏组织病理学的变化;原位末端脱氧核苷酸转移酶标记法(TUNEL)观察肝细胞凋亡情况;Western blot测定肝脏组织大鼠葡萄糖调节蛋白78(GRP78)、蛋白激酶R样内质网激酶(PERK)、C/EBP同源蛋白(CHOP)、核因子-κB p65(NF-κB p65)和半胱天冬酶-3(caspase-3)蛋白的表达。结果与SO组比较,SAP组大鼠血清AMY、AST、ALT及IL-6表达上升(P<0.05);胰腺和肝脏组织坏死及肝细胞凋亡程度增加;肝脏GRP78、PERK、CHOP、NF-κB p65及caspase-3蛋白水平升高(P<0.05)。与SAP组比较,TUDCA组大鼠血清AMY、AST、ALT及IL-6表达下降(P<0.05);胰腺和肝脏组织坏死及肝细胞凋亡程度降低;肝脏GRP78、PERK、CHOP、NF-κB p65和caspase-3蛋白水平降低(P<0.05)。结论TUDCA可能通过抑制PERK信号通路,减少内质网应激(ERS)的发生,减轻炎性反应及细胞凋亡,对重症急性胰腺炎诱导的大鼠肝损伤起保护作用。

高效液相色谱法测定肝胆双清口服液中3种成分含量

目的 建立测定肝胆双清口服液中牛磺熊去氧胆酸、牛磺鹅去氧胆酸和特女贞苷含量的高效液相色谱法。方法 牛磺熊去氧胆酸和牛磺鹅去氧胆酸的含量测定,色谱柱为Agilent Extend-C_(18)柱(150 mm×4.6 mm,3.5μm),流动相为0.02 mol/L磷酸二氢钠溶液(用三乙胺调pH至6.0)-乙腈(梯度洗脱),流速为1 mL/min,检测波长为205 nm,柱温为40℃,进样量为10μL;特女贞苷的含量测定,色谱柱为Thermo Acclaim^(TM)120A C_(18)柱(250 mm×4.6 mm,5μm),流动相为乙腈-水(梯度洗脱),流速为1 mL/min,检测波长为224 nm,柱温为40℃,进样量为10μL。结果 牛磺熊去氧胆酸、牛磺鹅去氧胆酸和特女贞苷的质量浓度分别在0.040 0~1.000 5 mg/mL、0.031 0~0.776 0 mg/mL、0.029 3~0.731 5 mg/mL范围内与峰面积线性关系良好(r=0.999 9,n=6);精密度、稳定性、重复性试验结果的RSD均小于2.0%(n=6);加样回收率分别为98.49%,99.49%,99.78%,RSD分别为3.04%,2.20%,1.15%(n=6)。3批样品中3种成分的含量分别为0.323 1~0.325 8 mg/mL、0.285 8~0.287 6 mg/mL、0.268 8~0.305 5 mg/mL。结论 所建立的方法操作简便快速、重复性好、结果准确,可用于肝胆双清口服液中牛磺熊去氧胆酸、牛磺鹅去氧胆酸和特女贞苷的含量测定。

柱前衍生化-HPLC法测定牛磺熊去氧胆酸中牛磺酸的残留量

建立了测定牛磺熊去氧胆酸(TUDCA)原料药中牛磺酸残留量的柱前衍生化高效液相色谱(HPLC)分析方法。样品用芴甲氧羰酰氯(FMOC-Cl)进行柱前衍生,产物用C18反相色谱柱进行HPLC分离,以柠檬酸-柠檬酸钠缓冲液(A)与甲醇-乙腈-柠檬酸-柠檬酸钠缓冲液(B)为流动相梯度洗脱,检测波长264 nm。该方法能使痕量牛磺酸与牛磺熊去氧胆酸及其有关物质达到基线分离,牛磺酸峰面积与浓度在0.31~41μg/mL范围内线性关系较好,相关系数r为0.9995,检出限为0.1μg/mL,加标回收率在98.8%~100.5%之间。已用于实际样品的分析。该方法灵敏度高,重现性好,适用于牛磺熊去氧胆酸中牛磺酸的残留量的测定。

牛磺熊去氧胆酸与熊去氧胆酸对预防保胆术后结石复发的临床研究

目的：评价牛磺熊去氧胆酸（ TUDCA）与熊去氧胆酸（ UDCA）对保胆取石术后患者预防胆囊结石复发的差异性及其临床价值。方法2010年10月～2011年12月，我院内镜微创保胆手术成功的313例胆囊结石按病历号奇偶分为TUDCA组（n＝161）和UDCA组（n＝152），术后2周TUDCA组口服牛磺熊去氧胆酸胶囊（商品名：滔罗特，意大利贝斯迪大药厂生产，进口批文号：H20070200、H20110233）500 mg，每晚1次，连续服用5天后，停药10天，15天为一周期；UDCA组口服熊去氧胆酸胶囊（商品名：优思弗，德国Dr．Falk药厂生产，进口批文号H20050181）500 mg，每晚1次。两组服药疗程均为180天。两组术后护理、饮食等均相同。术后定期随访及复查B超，观察记录胆囊结石复发、胆囊壁厚度变化以及胆囊收缩率。结果2组随访时间12～30个月，TUDCA组和UDCA组2年胆囊结石复发率分别为3．7％和12．4％（log-rank χ2＝5．304，P＝0．021）。结论内镜微创保胆取石术后口服TUDCA预防胆囊结石的复发效果优于UDCA。

牛磺熊去氧胆酸溶解胆囊胆固醇结石有效性和安全性——随机、双盲、安慰剂对照、多中心临床研究

目的 评价牛磺熊去氧胆酸胶囊(滔罗特Taurolite)对胆囊胆固醇结石的溶石效果与安全性. 方法 2003年10月～2004年12月,对滔罗特胶囊(含牛磺熊去氧胆酸250 mg)进行随机双盲、安慰剂对照、多中心的临床研究.受试者为体检查出,无症状或仅有轻度饭后上腹饱胀不适,结石＜2 cm,胆囊有功能的胆固醇结石患者.所有符合入选条件的患者填写知情同意书后随机分入试验组与对照组,进入4个月的双盲期.试验组应用滔罗特胶囊1粒/次,3次/日,对照组应用安慰剂胶囊1粒/次,3次/日.每2个月复查B超,口服胆囊造影(OCG),血常规与肝肾功能检查,以对滔罗特有效性和安全性进行评估.4个月时揭盲,对照组终止试验,试验组继续服药2个月(疗程6个月).疗效评估按国际统一标准:全溶(complete dissolution,CD),OCG示结石充盈缺损全部消失,B超示胆囊无异常回声;大部分溶(greater part dissolution,GPD),OCG和B超示结石的数目或直径或总体积减少50%以上;部分溶(partial dissolution,PD),OCG和B超示结石的数目或直径或总体积减少＜50%;无效(no change,NC),OCG和B超均示结石的数目或直径或总体积没有明显的变化.CD+GPD为显效,CD+GPD+PD为有效. 结果 两中心共纳入123例受试者,其中试验组64例,对照组59例.试验期间脱落和退出试验11例(8.9%),其中试验组2例,对照组9例.112例完成疗程和观察,其中试验组62例,对照组50例.①滔罗特4个月时显效率27.4%(17/62),有效率56.5%(35/62);6个月时显效率41.9%(26/62),有效率67.7%(42/62).对照组4例(8.0%)有溶石反应,46例无效.2组疗效差异有显著性(χ2＝28.678,P=0.000).②试验期间无严重不良事件发生,2组在试验期间共出现不良反应4例,试验组3例(4.8%,3/62),对照组1例(2.0%,1/50).2例与服用药物有关,药物不良反应发生率1.8%(2/112).③试验组服药前与服药后2、4个月后血常规与肝肾功能7项生化指标(ALT、AST、ALP、Tbil、ALB、Cr、BUN)的变化比较均无显著性差异(P＞0.05).血常规与肝肾功能7项生化指标的变化与服用滔罗特无关.④试验组与对照组比较,服药2、4个月时血常规与肝肾功能7项生化指标均无显著性差异(P＞0.05).血常规与肝肾功能7项生化指标的变化与服用滔罗特无关. 结论 滔罗特为治疗胆囊胆固醇结石安全有效的药物.

牛磺熊去氧胆酸治疗非酒精性脂肪肝疗效观察

目的比较牛磺熊去氧胆酸(TUDCA)与熊去氧胆酸(UDCA)治疗非酒精性脂肪肝的临床疗效。方法 58例非酒精性脂肪肝患者被随机分为两组,28例对照组采用UDCA联合多烯磷脂酰胆碱治疗,30例观察组采用TUDCA联合多烯磷脂酰胆碱治疗,两组疗程均为8w。结果在治疗结束时,观察组患者血清ALT(45.3±18.7)U/L对(67.4±20.3)U/L和TG(1.3±0.6)mmol/L对(2.4±0.7)mmol/L改善明显好于对照组(P<0.05)。结论 TUDCA治疗NAFLD疗效明显优于UDCA,可显著改善患者肝功能和血脂水平。

牛磺熊脱氧胆酸在棕榈酸诱导的INS-1细胞凋亡中的作用

为观察牛磺熊脱氧胆酸(Tauroursodeoxycholic acid,TUDCA)对棕榈酸(Palmitate)诱导的INS-1细胞凋亡的影响,分别用不同浓度棕榈酸(0.25mmol·L-1、0.5mmol·L-1、1.0mmol·L-1),棕榈酸(0.5mmol·L-1)+不同浓度TUDCA(25μmol·L-1、50μmol·L-1、100μmol·L-1)培养INS-1细胞12h,用MTT法检测细胞毒性作用,流式细胞术检测细胞凋亡,RT-PCR技术检测凋亡相关基因Bax/Bcl-2的表达.结果表明,与空白对照组比较,棕榈酸组(浓度≥0.5mmol·L-1)INS-1细胞凋亡率显著上升(p<0.05);加TUDCA培养组,当浓度≥50μmol·L-1时,与棕榈酸组相比,INS-1细胞凋亡率显著下降(p<0.05),呈剂量-效应关系.此外,棕榈酸组(浓度≥0.5mmol·L-1)INS-1细胞凋亡相关基因Bax表达显著上升(p<0.05),Bcl-2则明显下降;加TUDCA后,Bax基因表达显著下降(p<0.05),而Bcl-2则明显上升(p<0.05),并呈剂量-效应关系.以上结果表明,TUDCA能够减少游离脂肪酸引起的INS-1细胞凋亡,对INS-1细胞发挥保护作用.而凋亡促进基因Bax的表达下调,凋亡抑制基因Bcl-2的表达上调可能是其作用机制之一.

牛黄熊脱氧胆酸抑制TNF-α刺激3T3-L1细胞脂肪分解

目的探讨牛黄熊脱氧胆酸(tauroursodeoxycholic acid,TUDCA)对TNF-α刺激3T3-L1细胞脂肪分解及其可能的机制。方法以3T3-L1前脂肪细胞经1-甲基-3-异丁基-黄嘌呤、地塞米松、胰岛素诱导分化成3T3-L1脂肪细胞,设:①对照组;②TNF-α(50 ng/ml)组;③TUDCA(1 mmol/L)+TNF-α(50 ng/ml)组;④TUDCA组(1 mmol/L)。通过油红O染色观察脂滴形态变化并测定培养基中甘油含量作为评价脂肪分解的指标,同时用Western blot检测脂滴包被蛋白perilipinA蛋白表达。结果 TNF-α可以显著刺激3T3-L1细胞脂肪分解,包括功能学显示甘油释放量显著增加[(2.784±0.104)mmol/L,P<0.01],形态学显示脂滴碎裂;TUDCA可以明显抑制TNF-α刺激的3T3-L1细胞脂肪分解,包括阻止脂滴形态的改变,逆转甘油的释放[(1.718±0.085)mmol/L,P<0.01]。通过Western blot检测结果显示TNF-α可以下调perilipin A蛋白表达[(0.227±0.004),P<0.01],而TUDCA可以阻断TNF-α对perilipin A蛋白表达的下调作用[(0.705±0.066),P<0.01]。结论 TUDCA可能通过阻止perilipin A蛋白下调而抑制TNF-α诱发脂肪分解,通过减少游离脂肪酸FFA,从而对胰岛素抵抗、糖尿病等具有一定的改善作用。