Intestinal permeability of metformin using single-pass intestinal perfusion in rats

瞄准：在老鼠描绘 metformin 的肠的运输和机制并且调查 metformin 是否是为 P-glycoprotein (P-gp ) 的底层。方法：metformin 的有效肠的渗透用单个通行证的肠的灌注(SPIP ) 被调查在男痨牛老鼠的技术。如果 metformin 的肠的运输展出了地点依赖者变化， SPIP 在 metformin ( 50 microg/mL )的一样的集中在三个孤立的肠的片断(十二指肠，空肠和回肠)被执行到测试，并且在 metformin 的三不同集中在一样孤立肠的片断(十二指肠的片断)( 10 ， 50 ， 200 microg/mL )变化如果 metformin 的肠的运输展出了集中依赖者，测试。而且， P-gp 禁止者 verapamil (400 microg/mL ) 在十二指肠片断与 metformin (50 microg/mL ) 被共同酒发现 metformin 的肠吸收是否被沿着胃肠的轨道退出的 P-gp 影响。稳定性研究被进行保证 metformin 的损失能被归因于肠吸收。结果：在在 50 microg/mL 的空肠和回肠的 metformin 的有效渗透价值(P (eff )) 是比在在一样的集中的十二指肠的那些显著地低的。而且，在在高集中(200 microg/mL ) 的十二指肠的 P (eff ) 价值被发现比在低、中等的集中(10 和 50 microg/mL ) 的那些显著地低。而且有 verapamil 的合作灌注没在十二指肠在 50 microg/mL 增加 metformin 的 P (eff ) 价值。结论：Metformin 能从整个肠被吸收，与在十二指肠的主要吸收地点。在十二指肠的这集中依赖者渗透行为显示 metformin 被被动、活跃的调停搬运人的可饱和的机制搬运。P (eff ) 价值不能被合作灌注与 verapamil 增加，显示 metformin 的吸收没被在内脏墙中的 P-gp 高效地搬运。而且 metformin 是既不底层也不 P-gp 的 inducer。基于在现在的学习并且用确定的关系获得的 P (eff ) 价值，为 metformin 吸收的人的部分剂量被估计是 74%-90% 人的肠。

Absorption characteristic of Paeoniflorin-6＇O-benzene sulfonate in an situ single-pass intestinal perfusion model

Aim Paeoniflorin-6＇O-benzene sulfonate （CP-25） was synthesized to improve oral absorption. This study was performed to investigate absorptive behavior and mechanism of CP-25 in intestine. Methods The effects of drug concentration, intestinal segments, gender as well as ATP binding cassette （ABC） transporter inhibitors on absorption of CP-25 were studied in a situ single-pass intestinal perfusion rat model. Meanwhile, Paeoniflorin （Pae） was tested and served as control group. The concentration of tested drugs was measured by HPLC. Results The results showed intestinal absorption of CP-25 was neither segmental dependent changes nor gender difference. Transepithelial transportation would not change with increasing concentrations of CP-25, which suggest a passive transport was the main pattern of CP-25. Additionally, absorption of CP-25 was much better than that of Pae in small intestine. When compared with Pae, CP-25 gave a 1.82-fold permeability rate. Finally, the results indicated Pae was substrate of P-glycoprotein （P-gp） , but was not the substrate of breast cancer resistance protein and muhi- drug resistance associated protein 2. Among the used ABC inhibitors, the absorption rate of Pae could only be in- creased by？ P-gp inhibitor Verapamil and GF120918, while CP-25 had no remarkable alteration. Conclusion CP-25 has better absorptive features than that of Pae, which may be attributed to its lipophicity enhancement and be unaffected by P-gp efflux.

Absorption characteristics of the total alkaloids from Mahonia bealei in an in situ single-pass intestinal perfusion assay

AIM: To investigate the absorption characteristics of the total alkaloids from Mahoniae Caulis(TAMC) through the administration of monterpene absorption enhancers or protein inhibitors. METHOD: The absorption behavior was investigated in an in situ single-pass intestinal perfusion(SPIP) assay in rats. RESULTS: The intestinal absorption of TAMC was much more than that of a single compound or a mixture of compounds(jatrorrhizine, palmatine, and berberine). Promotion of absorption by the bicyclic monoterpenoids(borneol or camphor) was higher than by the monocyclic monoterpenes(menthol or menthone), and promotion by compounds with a hydroxyl group(borneol or menthol) was higher than those with a carbonyl group(camphor or menthone). The apparent permeability coefficient(Papp) of TAMC was increased to 1.8-fold by verapamil, while it was reduced to one half by thiamine. The absorption rate constant(Ka) and Papp of TAMC were unchanged by probenecid and pantoprazole. CONCLUSION: The intestinal absorption characteristics of TAMC might be passive transport, and the intestinum tenue was the best absorptive site. In addition, TAMC might be likely a substrate of P-glycoprotein(P-gp) and organic cation transporters(OCT), rather than multidrug resistance protein(MRP) and breast cancer resistance protein(BCRP). Compared with a single compound and a mixture of compounds, TAMC was able to be absorbed in the blood circulation effectively.

Intestinal injury can be reduced by intra-arterial postischemic perfusion with hypertonic saline

AIM:To investigate the effect of local intestinal perfusion with hypertonic saline(HTS) on intestinal ischemia-reperfusion injury(IRI) in bothex vivo andin vivo rat models.METHODS:All experiments were performed on male Wistar rats anesthetized with pentobarbital sodium given intraperitoneally at a dose of 60 mg/kg.Ex vivo vascularly perfused rat intestine was subjected to 60-min ischemia and either 30-min reperfusion with isotonic buffer(controls),or 5 min with HTS of 365 or 415 mOsm/L osmolarity(HTS 365mOsm or HTS 415mOsm,respectively) followed by 25-min reperfusion with isotonic buffer.The vascular intestinal perfusate flow(IPF) rate was determined by collection of the effluent from the portal vein in a calibrated tube.Spontaneous intestinal contraction rate was monitored throughout.Irreversible intestinal injury or area of necrosis(AN) was evaluated histochemically using 2.3.5-triphenyltetrazolium chloride staining.In vivo,30-min ischemia was followed by either 30-min blood perfusion or 5-min reperfusion with HTS 365mOsm through the superior mesenteric artery(SMA) followed by 25-min blood perfusion.Arterial blood pressure(BP) was measured in the common carotid artery using a miniature pressure transducer.Histological injury was evaluated in both preparations using the Chui score.RESULTS:Ex vivo,intestinal IRI resulted in a reduction in the IPF rate during reperfusion(P < 0.05 vs sham).The postischemic recovery of the IPF rate did not differ between the controls and the HTS 365mOsm group.In the HTS 415mOsm group,postischemic IPF rates were lower than in the controls and the HTS 365mOsm group(P < 0.05).The intestinal contraction rate was similar at baseline in all groups.An increase in this parameter was observed during the first 10 min of reperfusion in the control group as compared to the sham-treated group,but no such increase was seen in the HTS 365mOsm group.In controls,AN averaged 14.8% ± 5.07% of the total tissue volume.Administration of HTS 365mOsm for 5 min after 60-min ischemia resulted in decrease in AN(5.1% ± 1.20% vs controls,P < 0.01).However,perfusion of the intestine with the HTS of greater osmolarity(HTS 415mOsm) failed to protect the intestine from irreversible injury.The Chiu score was lower in the HTS 365mOsm group in comparison with controls(2.4 ± 0.54 vs 3.2 ± 0.44,P = 0.042),while intestinal perfusion with HTS 415mOsm failed to improve the Chiu score.Intestinal reperfusion with HTS 365mOsm in the in vivo series secured rapid recovery of BP after its transient fall,whereas in the controls no recovery was seen.The Chiu score was lower in the HTS 365mOsm group vs controls(3.1 ± 0.26 and 3.8 ± 0.22,P = 0.0079 respectively,),although the magnitude of the effect was lower than in the ex vivo series.CONCLUSION:Brief intestinal postischemic perfusion with HTS 365mOsm through the SMA followed by blood flow restoration is a protective procedure that could be used for the prevention of intestinal IRI.

The preparation of Garcinia Glycosides solid dispersion and intestinal absorption by rat in situ single pass intestinal perfusion

Garcinia Glycosides is a candidate drug obtained by structural modification of Gambogic Acid (GA), which was acquired through High Throughput Screening(HTS). As Garcinia Glycosides is an effective but insoluble anti-tumor drug, the aim of this study was to obtain a solid dispersion form Garcinia Glycosides by using solvent-melt method so that improve the solubility and dissolution rate. The solid dispersion was characterized by High Performance Liquid Chromatography (HPLC), infrared spectroscopy and evaluated the intestinal absorption of the drug by rat in situ single pass intestinal perfusion. The results showed the increase of solubility, dissolution velocity and absorption compared to other forms. This indicated that solid dispersion could greatly improve the relative bioavailability of Garcinia Glycosides in vivo.

Motility patterns of ex vivo intestine segments depend on perfusion mode

AIM:To evaluate and characterize motility patterns from small intestinal gut segments depending on different perfusion media and pressures.METHODS:Experiments were carried out in a custom designed perfusion chamber system to validate and standardise the perfusion technique used.The perfusion chamber was built with a transparent front wall allowing for optical motility recordings and a custom made fastener to hold the intestinal segments.Experiments with different perfusion and storage media combined with different luminal pressures were carried out to evaluate the effects on rat small intestine motility.Software tools which enable thevisualization and characterization of intestinal motility in response to different stimuli were used to evaluate the videotaped experiments.The data collected was presented in so called heatmaps thus providing a concise overview of form and strength of contractility patterns.Furthermore,the effect of different storage media on tissue quality was evaluated.HaematoxylinEosin stainings were used to compare tissue quality depending on storage and perfusion mode.RESULTS:Intestinal motility is characterized by different repetitive motility patterns,depending on the actual situation of the gut.Different motility patterns could be recorded and characterized depending on the perfusion pressure and media used.We were able to describe at least three different repetitive patterns of intestinal motility in vitro.Patterns with an oral,anal and oro-anal propagation direction could be recorded.Each type of pattern finalized its movement with or without a subsequent distension of the wavefront.Motility patterns could clearly be distinguished in heatmap diagrams.Furthermore undirected motility could be observed.The quantity of the different patterns varies and is highly dependent on the perfusion medium used.Tissue preservation varies depending on the perfusion medium utilized,therefore media with a simple composition as Tyrode solution can only be recommended for short time experiments.The more complex media,MEM-HEPES medium and especially AQIXRS-I tissue preservation reagent preserved the tissue much better during perfusion.CONCLUSION:Perfusion media have to be carefully chosen considering type and duration of the experiments.If excellent tissue quality is required,complex media are favorable.Perfusion pressure is also of great importance due to the fact that a minimum amount of luminal pressure seems to be necessary to trigger intestinal contractions.

Absorption of Curcumin Monophosphate in Rat Intestinal Circulation

[Objectives] This study aimed to study the absorption of curcumin monophosphate, a derivative of curcumin, in the small intestine of rats. [Methods] In situ recirculation perfusion technique was used to study the absorption of curcumin monophosphate in intestinal circulation of rats, and the content of curcumin monophosphate in intestinal circulation solution was determined by high-performance liquid chromatography/ultraviolet detector(HPLC/UV). [Results] The established HPLC/UV method has good specificity. Linear regression was conducted between the peak area of curcumin monophosphate(A) and the concentration of curcumin monophosphate(C). The established standard curve equation was y=30.07x+102.48(R^2=0.999 0), indicating that curcumin monophosphate has good linearity in the range of 1.25-100.00 μg/mL. After excluding the degradation of the drug and the loss of sampling, within the first 2 h of the experiment, the drug absorption in the small intestine of rat was 1.39 mg, accounting for 97.2% of the total drug absorption during the 5-h experimental period, and the absorption rate was 53.9%.[Conclusions] Curcumin monophosphate has a good absorption in the small intestine of rats.

在体单向肠灌流模型测定甘草素的药物渗透性及生物药剂学分类预测

目的测定不同浓度甘草素在大鼠不同肠段的渗透性,初步探讨甘草素在肠道中的吸收机制,并对甘草素进行生物药剂学分类预测。方法参考2020年版《中国药典》中关于溶解度定义,考察甘草素在pH 1.2、4.0、6.8、7.4的缓冲液和水中的平衡溶解度来评价甘草素的溶解性,采用在体单向肠灌流模型测定甘草素在25、50、75μg·mL^(-1)对大鼠十二指肠、结肠、空肠、回肠的渗透性;结合溶解性和渗透性结果预测甘草素生物药剂学分类。结果甘草素在不同pH下和水中平衡溶解度都低于100μg·mL^(-1),溶解度为不溶或几乎不溶,亲脂性不强,甘草素在大鼠不同肠段下的渗透性都大于1.2×10^(-3)cm·min^(-1),为易吸收药物。结论甘草素在大鼠肠吸收中存在自身吸收抑制,存在吸收饱和特性,可能有主动转运或扩散等转运机制参与,预测甘草素为生物药剂学Ⅱ类药物,为低溶解度,高渗透性药物。

基于在体单向肠灌流模型探究去氢骆驼蓬碱衍生物HM-Y-A的肠吸收特性

目的考察去氢骆驼蓬碱衍生物(HM-Y-A)在小肠不同肠段、不同条件下的吸收特性,探究HM-Y-A的吸收机制。方法采用大鼠在体单向肠灌流模型结合HPLC测定法,考察不同肠段、不同药物浓度、不同pH值及P-糖蛋白抑制剂对HM-Y-A吸收参数(K_(a)和P_(app))的影响。结果HM-Y-A在小肠各段均有吸收,最佳吸收肠段是十二指肠和空肠;随着药物浓度升高,吸收参数K_(a)和P_(app)不断降低,低浓度与中、高浓度间差异具有统计学意义(P<0.05);在pH 6.4和7.4时K_(a)和P_(app)显著增高(P<0.05);加入P-糖蛋白抑制剂前后,吸收参数差异无统计学意义。结论HM-Y-A在小肠全段均有吸收,在十二指肠和空肠吸收较好;吸收机制可能以主动吸收或促进扩散为主;药物在偏碱性条件下吸收较好;HM-Y-A可能不是P-gp的底物。

Comparison of intestinal absorption characteristics between rhubarb traditional Chinese medicine preparation and activity ingredients using in situ and in vitro model

Objective: The intestinal absorption characteristics of active ingredients are very important for oral administration of traditional Chinese medicine(TCM) to achieve the desired therapeutic effect.However, a deeper understanding about active ingredients absorption characteristics is still lack. The aim of this study was to investigate the absorption properties and mechanism of rhubarb active ingredients in TCM preparation and pure form.Methods: The intestinal absorption behavior of active ingredients in Shenkang extract(SKE) and rhubarb anthraquinone ingredients(RAI) were investigated by in situ single-pass intestinal perfusion model. And the bidirectional transport characteristics of these active ingredients were assessed by in vitro Caco-2 cell monolayer model.Results: In situ experiment on Sprague-Dawley rats, the effective permeability coefficient values of aloeemodin, emodin and chrysophanol in RAI were higher than those in SKE, and the value of rhein in RAI was lower than that in SKE. But the easily absorbed segments of intestine were consistent for all ingredients,whether in SKE or in RAI. In vitro experiment, the apparent permeability coefficient values of rhein, emodin and chrysophanol in RAI were higher than those in SKE, and this value of aloe-emodin in RAI was lower than that in SKE. But their efflux ratio(ER) values in SKE and RAI were all similar.Conclusion: Four rhubarb anthraquinone ingredients in SKE and RAI have similar absorption mechanism and different absorption behavior, and the microenvironment of the study models influenced their absorption behavior. The results may provide an aid for understanding of the absorption characteristics of the TCM active ingredients in complex environments and the complementarities of different research models.

不同链长油相葛根素W/O型微乳在体肠吸收的研究

目的研究不同链长油相对葛根素W/O型微乳口服吸收的影响。方法采用在体单向肠灌流法考察不同链长油相葛根素W/O型微乳的肠吸收行为。以吸收速率常数(K_(a))和表观吸收系数(P_(app))为评价指标,分析不同链长油相对葛根素W/O型微乳在大鼠不同肠段的吸收特性。结果葛根素W/O型微乳在大鼠整个肠段的吸收均显著高于葛根素混悬液,不同链长油相W/O型微乳的肠吸收有差异。此外,葛根素W/O型微乳在大鼠整个肠段的肠吸收与微乳的油相链长在一定程度上成正相关,其中长链油微乳肠吸收最佳。结论长链油微乳能增强葛根素的肠吸收,从而进一步提高葛根素的口服生物利用度。

全杜仲胶囊对自发性高血压大鼠肠壁微血流灌注的影响

目的 探讨全杜仲胶囊(QDZJN)和松脂醇二葡萄糖苷(PDG)对自发性高血压大鼠(SHRs)肠壁微循环血流灌注及其频谱特征的影响。方法 将SHRs随机分为SHR,SHR+QDZJN,SHR+PDG(L),SHR+PDG (M)和SHR+PDG (H)组。对照组为Wistar-kyoto(WKY)鼠。各组分别接受QDZJN或纯净水(对照组和SHR组)灌胃2个月。手术暴露大鼠小肠,激光多普勒血流探测仪(LDF)和血流成像仪(LDPI)检测并比较各组大鼠肠壁微血流灌注水平。小波分析比较各组肠壁内皮源性频段幅值。结果 与对照组相比,SHRs肠壁血流灌注水平显著降低(P<0.001)。QDZJN和各剂量PDG治疗2个月后,SHRs肠壁血流灌注水平显著升高(P<0.001)。SHRs组肠壁微血流灌注一氧化氮(NO)依赖和非依赖性内皮细胞源频段振幅均显著低于对照组(P<0.01)。QDZJN和PDG治疗可显著提高内皮细胞源频段幅值(NO依赖:P<0.0001;NO非依赖:P<0.01)。结论 QDZJN和PDG治疗2个月可显著改善SHRs肠壁的微血流动力学和内皮功能障碍。

他克莫司对肝移植急性排斥反应大鼠肠道菌群的影响

目的探讨他克莫司对心脏死亡器官捐献(donation after cardiac death,DCD)供肝移植后急性排斥反应大鼠肠道菌群的影响。方法构建稳定运行的常温机械灌注(normothermic machine perfusion,NMP)系统。夹闭Lewis大鼠胸主动脉30 min获取DCD肝脏,以棕色挪威大鼠(BN)为受体,建立原位肝移植急性排斥反应模型。根据对肝脏的不同处理方法,将BN大鼠分为以下3组:假手术(Sham)组、单纯NMP(NMP)组及NMP联合术后他克莫司(FMP)组,每组6只,术后14 d收集血液、肝脏和肠道内容物样本。血液标本检测肝功能,HE染色观察肝脏组织学变化并计算排斥活动指数(rejection activity index,RAI),16 SrDNA检测肠道内容物,观察各组肠道菌群结构、多样性及功能变化。结果FMP组(中位生存期>60 d)大鼠存活时间较NMP组(中位生存期为16.5 d)延长,肝功能和肝组织病理较NMP组显著改善(P<0.05)。计算RAI结果显示,FMP组(2.00±1.23)显著低于NMP组(7.60±1.14)(P<0.05)。与NMP组相比,FMP组肠道菌群丰度下降,两组在物种之间有明显差异,FMP组富含厚壁菌门、阿克曼菌科和毛螺菌科,且富集其他聚糖降解和鞘脂代谢通路。结论他克莫司能够改善DCD供肝移植后急性排斥反应大鼠肝损伤,同时调节肠道菌群结构和代谢途径。

基于寡肽转运蛋白的氟苯尼考肠吸收特性研究

本研究旨在考察氟苯尼考(florfenicol,FF)在不同浓度下的肠吸收特性,探究寡肽转运蛋白对氟苯尼考肠吸收的影响。采用高效液相色谱法测定灌流样品中氟苯尼考的含量,建立大鼠在体肠循环灌流模型,考察不同浓度药物对氟苯尼考吸收速率的影响;以寡肽转运蛋白1(oligopeptide transporter 1,PepT1)的典型底物甘氨酰肌氨酸来考察PepT1对氟苯尼考吸收的影响,计算氟苯尼考的药物吸收速率常数(Ka)及有效渗透系数(P_(eff))。结果表明,所建立的FF含量测定方法准确度、精密度均符合检测要求。FF低(50μg·mL^(-1))、中(75μg·mL^(-1))、高(100μg·mL^(-1))3个浓度下的Ka(μg·h^(-1)·cm^(-2)值分别为1.48±0.02、1.73±0.14、1.90±0.07,低浓度与中高浓度组间均具有显著性差异(P<0.05);有效渗透系数P_(eff)(×10^(2)cm·h^(-1))分别为84.12±2.40、101.28±4.57、110.64±5.70,3个组别均具有显著性差异(P<0.05),FF跨肠道吸收的Ka与P_(eff)在试验所用浓度范围内随浓度增加而增加。添加高浓度(100μg·mL^(-1))甘氨酰肌氨酸(GlySar)后,P_(eff)(×10^(2)cm·h^(-1))值为97.2±5.30,与未添加组相比具有显著性差异,加入PepT1典型底物后,氟苯尼考的吸收显著性下降。结果说明,氟苯尼考的吸收方式不是只有简单扩散,PepT1可能作为主动转运蛋白参与了氟苯尼考的跨肠道吸收过程。

芍药苷及芍药苷磷脂复合物胶束在体肠吸收对比分析

目的比较芍药苷(PF)和芍药苷磷脂复合物(PF-PLC)胶束的肠吸收特点,探讨磷脂复合物胶束提高芍药苷生物利用度的作用机制。方法采用大鼠在体单向肠灌流模型,以吸收速率常数(K_(a))和有效渗透系数(P_(eff))为指标,通过超高效液相色谱(UPLC)测定不同浓度芍药苷原料药和芍药苷磷脂复合物胶束在十二指肠中的肠吸收情况。同时,在灌流液中添加维拉帕米,考察P-糖蛋白(P-gp)抑制剂对芍药苷原料药和芍药苷磷脂复合物胶束肠吸收的影响。结果芍药苷磷脂复合物胶束浓度的提高可显著增加芍药苷的肠道吸收(P<0.001,P<0.05)。在灌流液中加入维拉帕米后发现,与单纯芍药苷组比较,芍药苷+维拉帕米组的吸收速率常数和有效渗透系数值虽有增加的趋势,但无明显统计学差异;与芍药苷磷脂复合物胶束组比较,芍药苷磷脂复合物胶束+维拉帕米组差异也无统计学意义。结论大鼠在体单向肠灌流实验结果显示芍药苷磷脂复合物胶束的吸收主要是被动转运途径,且磷脂复合物胶束的形成显著改善了芍药苷在十二指肠的吸收。维拉帕米的加入对芍药苷磷脂复合物胶束的吸收无显著影响,即芍药苷磷脂复合物胶束的吸收不受外排转运体的影响,这可能是生物利用度提高的原因之一。

酚妥拉明对肠缺血再灌注损伤小鼠肠黏膜屏障及组织灌注的影响

目的:探讨酚妥拉明(Regitine)对肠缺血再灌注(Ⅱ/R)损伤小鼠肠黏膜屏障和组织灌注的保护作用。方法:采用夹闭肠系膜上动脉方法建立Ⅱ/R模型,将32只小鼠随机分为四组:对照组、Ⅱ/R组(肠缺血再灌注)、Regitine组(Ⅱ/R+酚妥拉明肠系膜根部注射)和Regitineⅳ组(Ⅱ/R+酚妥拉明尾静脉注射),每组8只。观察各组肠道炎症因子(IL-6、TNF-α)、血清肠损伤标记物水平(D-lactate、I-FABP),肠道血流灌注指数、平均动脉压(MAP)、血清血管内皮损伤标记物(Syndecan-1),组织病理评分、肠黏膜屏障通透性(FD4)、紧密连接蛋白(Claudin-1、Occludin)表达变化,肠组织细胞凋亡(TUNEL)、线粒体自噬水平(p62、mito-LC3、Tim23)以及细胞色素C(Cyt-c)泄露水平。结果:与Ⅱ/R组相比,Regitine组和Regitineⅳ组小鼠肠道IL-6、TNF-α、血清D-lactate、I-FABP、Syndecan-1、FD4、组织病理评分、肠组织TUNEL以及Cyt-c泄露减少(P<0.05),肠道血流灌注指数、紧密连接蛋白表达、线粒体自噬水平升高,差别具有统计学意义(P<0.05);与Regitineⅳ组相比,Regitine组肠道IL-6、血清D-lactate、I-FABP、FD4水平、肠组织TUNEL及Cyt-c泄露水平降低(P<0.05),同时肠道血流灌注指数、MAP、Occludin表达、线粒体自噬水平升高(P<0.05)。结论:酚妥拉明对Ⅱ/R小鼠肠黏膜屏障和组织灌注具有一定的保护作用,肠系膜根部局部给药效果优于尾静脉全身给药,该发现有望为保护Ⅱ/R后肠黏膜屏障功能和组织灌注提供新的治疗思路。

腹腔热灌注化疗对结直肠癌患者术后肠黏膜屏障功能及康复效果影响

目的探讨腹腔热灌注化疗对结直肠癌患者术后肠黏膜屏障功能及康复效果影响。方法选取2020年1月—2022年12月本院收治的35例结直肠癌患者为研究对象,按照随机数字表法分为观察组(n=18)和对照组(n=17)。所有患者均行结直肠癌根治术,观察组给予腹腔热灌注化疗,对照组术后则不开展腹腔热灌注化疗。比较两组围手术期相关指标、化疗前后胃肠功能、生存质量水平和术后腹胀发生率。结果与对照组相比较,观察组肠鸣音恢复、首次排气、首次排便时间均较短,差异有统计学意义(P<0.05);术后观察组首次大便性状评分明显低于对照组,差异有统计学意义(P<0.05);观察组术后发生腹胀、恶心呕吐率明显低于对照组,差异有统计学意义(P<0.05);术后两组MTL、GAS水平降低,ORTC QLQ-C30评分提升,且与对照组相比较,观察组MTL、GAS水平下降幅度较小,ORTC QLQ-C30评分较高,差异有统计学意义(P<0.05)。结论结直肠癌患者术后应用腹腔热灌注化疗,能有效改善患者的肠黏膜屏障功能,促进胃肠功能的恢复,同时也有利于提高患者生活质量水平。

丹酚酸B大鼠在体肠吸收研究

目的:研究丹酚酸B在大鼠小肠的吸收情况。方法:采用在体单向灌流法进行小肠吸收实验,利用HPLC法测定灌流液中丹酚酸B的浓度。结果:丹酚酸B浓度为24.63μg·mL-1时,在十二指肠、空肠、回肠段的吸收速率常数(Ka)和表观吸收系数(Papp)无显著性差异(P>0.05)。与12.54μg·mL-1浓度比较,48.12μg·mL-1浓度时Sal B在空肠的Ka和Papp均显著降低[Ka:(2.13±0.50)×10-2vs(3.10±0.42)×10-2min-1,P<0.05;Papp:(2.07±0.49)×10-3vs(3.10±0.51)×10-3cm.min-1,P<0.05]。结论:丹酚酸B的小肠吸收存在高浓度饱和现象,且在全肠道吸收良好,且在小肠内无特定吸收部位,提示该药物适合制成日服2次的缓控释制剂。

大鼠在体肠灌流模型中补骨脂素的吸收研究

目的:研究补骨脂素在大鼠小肠的吸收特性及其机制,探讨其在临床上血药浓度差异较大的原因。方法:采用改良大鼠在体单向肠灌流模型,通过颈静脉插管补充血液、肠系膜静脉插管采集血样,同时收集灌流流出液,以反相高效液相色谱法测定补骨脂素含量,计算其通透率。结果:补骨脂素在大鼠小肠内通透率较高,吸收较好。不同浓度的补骨脂素灌流时均以约30%的比例吸收入血,且通透率Plumen,Pblood在所测浓度范围内基本保持不变。结论:补骨脂素在大鼠小肠的转运机制为被动转运,不受P-糖蛋白的影响,临床上血药浓度个体差异大可能与肝脏的首过效应有关,而非小肠吸收代谢所致。

隐丹参酮在小肠吸收机制的实验研究

目的 研究隐丹参酮在大鼠小肠的吸收机制。方法 用大鼠在体一过式肠灌流方法,通过肠系膜静脉插管采集血样,同时收集灌流流出液,以高效液相色谱法测定样品中隐丹参酮含量,计算其通透率。结果 隐丹参酮在大鼠小肠的肠管通透率(Plumen)和血管通透率(Pblood)随浓度的增加而下降;加入P-糖蛋白抑制剂维拉帕米后其通透率增高。结论 隐丹参酮在大鼠小肠的转运机制可能为主动转运,隐丹参酮可能为P-糖蛋白底物。