Murine intestinal organoids resemble intestinal epithelium in their microRNA profiles

Intestinal organoids were established as an ex vivo model of the intestinal epithelium. We investigated whether organoids resemble the intestinal epithelium in their microRNA (miRNA) profiles. Total RNA samples were obtained from crypt and villus fractions in murine intestine and from cultured organoids. Microarray analysis showed that organoids largely resembled intestinal epithelial cells in their miRNA profiles. In silico prediction followed by qRT-PCR suggested that six genes are regulated by corresponding miRNAs along the crypt-villus axis, suggesting miRNA regulation of epithelial cell renewal in the intestine. However, such expression patterns of miRNAs and their target mRNAs were not reproduced during organoids maturation. This might be due to lack of luminal factors and endocrine, nervous, and immune systems in organoids and different cell populations between in vivo epithelium and organoids. Nevertheless, we propose that intestinal organoids provide a useful in vitro model to investigate miRNA expression in intestinal epithelial cells.     

党参多糖对肠道微生态及肠道疾病作用研究进展

党参为生活中常用的药食两用药材,具有补益作用,其中党参多糖为主要的活性成分之一,具有多种生物活性。近年来,很多学者在研究党参多糖治疗肠道相关疾病方面取得了显著进展。近期研究显示,肠道菌群可能是党参多糖治疗相关肠道疾病的潜在作用靶点。因此,本文就党参多糖对肠道微生物调节及肠道疾病作用的研究进行综述,以期为党参多糖作为益生元微生态制剂的开发和治疗肠道相关疾病提供一些理论依据和试验基础。     

肠道上皮与肠道微生物相互作用的研究现状

肠道上皮是肠上皮细胞及其分泌物有机构成的黏膜界面。随着技术的进步和对肠道菌群作用的逐渐重视,研究者对肠道上皮与肠道微生物相互作用的认识也不断深入。研究表明,肠道上皮调节并维持肠道微生物的定殖与分布,肠道微生物也影响肠道上皮的多种屏障功能,二者通过一系列细胞分子机制紧密联系,共同维持肠道稳态。此外,其过程中产生的宿主-肠道菌群共代谢物被发现可以反映宿主的生理病理状态,作为指标被应用于临床疾病诊断、治疗效果评估和预后推测。本文基于近年的研究,综述了肠道上皮与肠道微生物的相互作用及其细胞分子机制,为进一步研究和临床应用总结了理论基础,并探讨了未来可能的研究方向。     

猪源乳杆菌Lactobacillus reuteri strain DSM和Lactobacillus taiwanensis strain BCRC对肠道炎症的影响

[目的] 旨在以葡聚糖硫酸钠（DSS）诱导小鼠肠炎模型研究猪源乳杆菌Lactobacillus reuteri strain DSM（LR）和Lactobacillus taiwanensis strain BCRC（LT）对肠道炎症的影响。[方法] 选取24只8周龄体重相近的C57BL/6J雄性小鼠,随机分为4组（每组6个重复）：正常对照组、DSS组、LR菌处理组（DSS+LR）和LT菌处理组（DSS+LT）。适应期7 d,试验期16 d,随后处死小鼠并采样。[结果] 与正常对照组相比,DSS组小鼠体重、结肠长度显著降低,疾病活动指数（DAI）显著增加（P<0.05）;与DSS组相比,LR、LT菌处理组小鼠体重下降的程度并没有显著缓解,但是,其DAI评分显著降低;并且,LT菌处理组结肠长度显著增加（P<0.05）。正常对照组和LT菌处理组结肠组织病理学评分显著低于DSS组和LR菌处理组（P<0.05）。结肠髓过氧化物酶（MPO）活性在正常对照组和LT菌处理组也显著低于DSS组（P<0.05）,在LR菌处理组与DSS组无显著差异（P>0.05）。与正常对照组相比,DSS组结肠和血浆的促炎因子TNF-α、IL-1β、IL-6水平显著升高,而抗炎因子IL-10水平显著降低;相比于DSS组,LT菌处理组显著降低了结肠和血浆的TNF-α、IL-1β、IL-6水平,升高了IL-10水平;LR菌处理组显著降低了结肠TNF-α水平、血浆IL-1β水平,升高IL-10水平（P<0.05）。免疫组化和ELISA结果显示,相比于正常对照组,DSS组降低了结肠紧密连接蛋白Claudin-1、Occludin、ZO-1和黏蛋白Muc-2表达水平,而LR或LT菌的处理则上调了DSS影响下的屏障相关蛋白表达。16S rDNA测序技术检测结肠菌群组成,PCoA分析得出,正常对照组和DSS组显著分离,LT处理组菌群组成更接近于正常对照组。门水平上,变形菌门丰度在正常对照组显著低于DSS组（P<0.05）;与DSS组相比,LT菌处理组也能降低变形菌门丰度,但未达显著水平（P>0.05）。属水平上,Muribaculaceae_norank属在正常对照组显著高于其他3组,Bacteroides在正常对照组显著低于其他3组（P<0.05）;与DSS组相比,LR或LT菌的处理增加了Muribaculaceae_norank丰度,降低了Bacteroides菌丰度,但差异不显著（P>0.05）。[结论] 乳杆菌Lactobacillus reuteri和Lactobacillus taiwanensis能增强肠上皮屏障,对DSS引起的肠道炎症起到了一定的缓解作用;其中,Lactobacillus taiwanensis对肠上皮屏障的保护效果更为明显。     

Hydrogen-rich saline protects against intestinal ischemia/reperfusion injury in rats

Hydrogen gas was reported to reduce reactive oxygen species and alleviate cerebral, myocardial and hepatic ischemia/reperfusion (I/R) injuries. This paper studied the effect of hydrogen-rich saline, which was easier for clinical application, on the intestinal I/R injury. Model of intestinal I/R injury was induced in male Sprague-Dawley rats. Physiological saline, hydrogen-rich saline or nitrogen-rich saline (5 ml/kg) was administered via intravenous infusion at 10 min before reperfusion, respectively. The intestine damage was detected microscopically and was assessed by Chiu score system after I/R injury. In addition, serum DAO activity, TNF-α, IL-1β and IL-6 levels, tissue MDA, protein carbonyl and MPO activity were all increased significantly by I/R injury. Hydrogen-rich saline reduced these markers and relieved morphological intestinal injury, while no significant reduction was observed in the nitrogen-rich saline-treated animals. In conclusion, hydrogen-rich saline protected the small intestine against I/R injury, possibly by reduction of inflammation and oxidative stress.     

The role of autophagy in maintaining intestinal mucosal barrier

The intestinal mucosal barrier is the first line to defense against luminal content penetration and performs numerous biological functions. The intestinal epithelium contains a huge surface that is lined by a monolayer of intestinal epithelial cells (IECs). IECs are dominant mediators in maintaining intestinal homeostasis that drive diverse functions including nutrient absorption, physical segregation, secretion of antibacterial peptides, and modulation of immune responses. Autophagy is a cellular self-protection mechanism in response to various stresses, and accumulating studies have revealed its importance in participating physiological processes of IECs. The regulatory effects of autophagy depend on the specific IEC types. This review aims to elucidate the myriad roles of autophagy in regulating the functions of different IECs (stem cells, enterocytes, goblet cells, and Paneth cells), and present the progress of autophagy-targeting therapy in intestinal diseases. Understanding the involved mechanisms can provide new preventive and therapeutic strategies for gastrointestinal dysfunction and diseases.     

胰高血糖素样肽-2对小鼠小肠缺血/再灌注损伤的保护作用

目的:观察胰高血糖素样肽-2(GLP-2)对缺血/再灌注损伤小鼠小肠的保护效应.方法:采用肠缺血/再灌注(I/R)模型,将32只小鼠随机分为4组(n=8)假手术(Sham)组、I/R组、I/R GLP-2保护组和I/R 谷氨酰胺(GLN)阳性对照组.光镜观察小肠黏膜形态学改变.检测小肠绒毛高度和隐窝深度;小肠组织二胺氧化酶(DAO)活性;肠系膜淋巴结(MLN)细菌易位率.结果:与假手术组相比,I/R组部分小肠绒毛坏死脱落,绒毛高度下降,隐窝变浅(P＜0 01);小肠组织DAO活性降低(P＜0.01);MLN细菌易位率增加(P＜0.05).与I/R组比,GLP-2组肠绒毛损害明显减轻,DAO活性回升(P＜0.01),细菌易位率回降(P＜0.05).结论:GLP-2对缺血/再灌注损伤小鼠小肠的形态结构及肠屏障功能具有保护作用.     

In vitro stimulation of prolactin release by vasoactive intestinal peptide

The effect of vasoactive intestinal peptide (VIP) on anterior pituitary hormone release was examined in a variety of in vitro preparations. Synthetic VIP was capable of stimulating increased prolactin (PRL) release from male rat hemipituitaries in doses as low as 10⁻⁹ M only when the enzyme inhibitor bacitracin was present in the incubation medium. Natural porcine VIP was similarly capable of stimulating PRL release, but only at higher doses (10⁻⁶ M). Additionally, synthetic VIP was capable of stimulating PRL release from dispersed anterior pituitary cells harvested from adult male and lactating female rats and from an enriched population of lactotrophs obtained by unit gravity sedimentation of similar dispersed cells from infantile female rats. No effect of VIP on luteinizing hormone, growth hormone or thyroid stimulating hormone release was seen. These findings taken in concert with the presence of VIP in the hypothalamus, pituitary and hypophyseal portal plasma of the rat suggest a physiological role for VIP in the control of PRL secretion.     

Gastric and intestinal release of vasoactive intestinal polypeptide in the milk-fed lamb

Vasoactive intestinal polypeptide (VIP) has been proposed as the neurotransmitter of the atropine-resistant relaxation of gastric structures in the lamb. To examine this proposal VIP concentrations in plasma from arterial, gastric venous and intestinal venous blood were measured in healthy conscious lambs before, during and after teasing with, and sucking of milk. Basal arterial plasma VIP concentrations were undetectable (less than 3 pmol/l) and remained so during and after feeding. Before feeding VIP was detected in only 2 of 12 gastric venous plasma samples (5 and 13 pmol/l). During teasing with food there were increments in VIP of 19 +/- 4 pmol/l and during feeding of 27 +/- 5 pmol/l. VIP concentration in gastric venous plasma rapidly returned to fasting levels after cessation of sucking. In contrast VIP in the intestinal venous plasma did not rise during teasing or upon commencement of sucking but a peak increment of 34 +/- 6 pmol/l occurred at 5 min after cessation of feeding. The results are consistent with the hypotheses that VIP is released in anticipation of and during sucking from inhibitory neurones involved in relaxation of gastric structures and that intestinal release of VIP is a consequence of entry of digesta into the small intestine.     

猕猴发育过程中肠肝组织血管活性肠肽及其受体的变化

本文旨在探讨猕猴发育过程中血管活性肠肽(vasoactive intestinal polypeptide,VIP)及其受体在肠肝组织的变化。通过手术途径获得胚胎6月、新生2 d、新生45 d和成年猕猴的回肠、肝脏、门静脉和外周血等标本,应用放射免疫分析法测定各标本中的VIP含量;通过免疫组化方法观察VIP在肠、肝组织内的分布;利用原位杂交法检测VIP受体1(VIP receptor 1,VIPR1)的表达。结果显示:(1)胚胎6月的猕猴小肠VIP含量为(20．7±14．3)ng／mg蛋白;小肠绒毛根部及黏膜下层可见少量的VIP阳性染色颗粒;在发育过程中,小肠VIP含量逐渐增加,成年期时达(514．8±49．2)ng／mg蛋白,较胚胎6月显著增加(P<0．01)。(2)成年猕猴小肠VIP主要分布于绒毛隐窝部、黏膜下层神经及环、纵行肌间神经丛及环行肌,在发育过程中相应部位的VIPR1表达逐渐上调。(3)肝脏在发育过程中VIP及VIPR1含量逐渐降低。(4)发育的各个时期,小肠组织的VIP含量均明显高于肝脏组织,门静脉VIP水平也始终高于外周血。结果提示,小肠绒毛隐窝部、黏膜下层神经及环、纵行肌间神经内VIP及VIPR1含量足在出生以后才迅速增加的;不论是在胚胎还是成年期,VIP均不在肝中代谢和分解,VIPR1仅见于胚胎肝脏血管。     

肠道菌群对耐碳青霉烯类肠杆菌科细菌定殖抗性的研究进展

耐碳青霉烯类肠杆菌科细菌(carbapenem-resistant Enterobacteriaceae,CRE)在肠腔中定殖通常先于或并存于CRE的感染。正常情况下,定殖的CRE、肠道菌群和宿主相互作用,处于稳定平衡的状态,当肠道菌群出现失调时,肠道正常菌群失去对定殖CRE的抵抗力,增加CRE感染的风险。大量研究表明通过肠道共生菌群对CRE的定殖抗性不仅可以预防感染,而且也可以降低医疗环境中患者间相互传播的风险。本文就CRE的流行现状、肠杆菌科细菌定殖机制以及肠道共生菌群对CRE定殖抗性机制作一综述,以期为CRE感染的防控工作提供新思路和新方法。     

抗菌肽与肠道健康研究新进展

抗菌肽是生物体内诱导产生的一类具有抗菌作用的生物活性肽,在机体抵抗病原入侵方面起着重要作用。近年来,肠道微生态研究炙手可热,抗菌肽与肠道健康的研究正广泛开展。相关研究结果表明,抗菌肽表达水平的高低可以用来评估机体肠道健康状态,从而监测抗菌肽表达水平来建立一种疾病预防和治疗过程中的辅助诊断手段。本文围绕抗菌肽对肠道菌群结构和免疫影响两方面的最新研究进展进行归纳与分析,旨在为临床诊断与治疗提供参考。     

肠粘膜上皮细胞在天然免疫中的作用

粘膜免疫是机体防御系统的主要成分。致病性细菌侵入机体后,首先遭遇到天然免疫的抵抗,随后产生获得性免疫,两共同执行机体的防御功能,消灭入侵细菌。最近的研究表明上皮细胞对细菌感染有重要的免疫调节作用,在天然免疫与获得性免疫防御机制中起重要作用。本重点介绍肠上皮细胞在天然免疫中的作用。     

Successful implementation of intestinal endoscopy in non‐human primates prompts the possibility of achieving AIDS longitudinal intestinal research

HIV infection induces pathological changes in the intestinal mucosa. Here, a successful endoscopy was performed on the colon of a Chinese rhesus macaque by using Olympus CV170 gastroscope. The stability on postoperative recovery and the integrity of biopsy tissue implied a possibility of achieving AIDS longitudinal intestinal research on macaques.     

猪小肠微生物对不同蛋白源的体外发酵特性比较

【目的】采用体外发酵技术比较小肠微生物对不同蛋白源的发酵规律。【方法】以成年猪的十二指肠、空肠和回肠内容物为接种物,以豆粕、菜粕或鱼粉水解物上清液为氮源底物,于发酵的0、4、8、12 h分别测定发酵液p H、微生物蛋白、氨氮和挥发性脂肪酸含量,同时提取细菌DNA并进行定量分析。【结果】添加含氮底物的空肠组和回肠组氨氮浓度和菌体蛋白浓度均相对增加,尤其是酶解菜粕组菌体蛋白合成量较高;十二指肠组菌体蛋白浓度以及氨氮含量不断减少。各发酵组乳酸和挥发酸快速积累,4–8 h积累量最大;8 h后空肠组和回肠组乳酸和挥发酸含量相对稳定,而十二指肠组后期丙酸含量增加约2 mmol/L,并伴随着乳酸含量的相对减少。同时,各组中总细菌、拟杆菌门、厚壁菌门和乳酸杆菌数量相对增加,且略高于无氮组,但不同蛋白源组间无显著差异。【结论】在体外培养条件下,空肠和回肠微生物具有相似的发酵规律,均能快速利用培养液中的含氮物质合成菌体蛋白;十二指肠微生物具有较强的产挥发酸能力,能够转化乳酸并大量产生丁酸和丙酸,这有利于宿主营养功能和肠道健康。     

益生菌调控肠道屏障功能预防家禽球虫病的研究进展

球虫病给养禽业带来巨大经济损失,人们对绿色健康食品的迫切需求使球虫病的防控面临新的挑战.伴随世界"禁抗"进程的不断推进,家禽养殖业亟需一种安全有效的新型抗球虫方法.益生菌可竞争性排斥病原菌定殖以防止球虫病继发感染,可刺激宿主抗菌肽、黏蛋白和紧密连接蛋白的分泌以抵御球虫入侵,还可激活免疫反应以增强机体抗球虫感染的能力.本...     

发育过程中肝脏血管活性肠肽及其受体量的变化

已有的研究观察到,胚胎肝脏中血管活性肠肽(vasoactiveintestinalpolypeptide,VIP)及其受体(vasoactiveintesti-nalpolypeptidereceptor,VIPR)与造血干细胞生长和肝脏发育有关。本研究旨在了解发育过程中肝VIP及VIPR量的动态变化。采用放射免疫分析法、生物分子相互作用系统和RT-PCR等技术检测了各发育阶段大鼠肝组织VIP浓度、VIP受体结合量及VIP受体表达亚型,实验观察到胎鼠和新生鼠肝脏VIP浓度显著低于未成年鼠及成年鼠肝脏VIP浓度(P<0.05)。发育尚未成熟时(胎鼠、新生鼠、未成年鼠),肝VIPR表达均明显高于成年鼠(P<0.05),表明大鼠在发育过程中肝脏VIP与VIP受体量呈相反的变化趋势。大鼠发育各时期,肝脏均表达VIPR-1。这些结果部分解释了肝脏发育、肝脏造血转移等重要生理现象。