人肠道类器官作为上小肠离子转运生理和病理生理学的模型
Human Enteroids as a Model of Upper Small Intestinal Ion Transport Physiology and Pathophysiology.
作者信息
Foulke-Abel Jennifer, In Julie, Yin Jianyi, Zachos Nicholas C, Kovbasnjuk Olga, Estes Mary K, de Jonge Hugo, Donowitz Mark
机构信息
Department of Medicine, Division of Gastroenterology, Johns Hopkins University School of Medicine, Baltimore, Maryland.
Department of Molecular Virology and Microbiology, Baylor College of Medicine, Houston, Texas.
出版信息
Gastroenterology. 2016 Mar;150(3):638-649.e8. doi: 10.1053/j.gastro.2015.11.047. Epub 2015 Dec 8.
BACKGROUND & AIMS: Human intestinal crypt-derived enteroids are a model of intestinal ion transport that require validation by comparison with cell culture and animal models. We used human small intestinal enteroids to study neutral Na(+) absorption and stimulated fluid and anion secretion under basal and regulated conditions in undifferentiated and differentiated cultures to show their functional relevance to ion transport physiology and pathophysiology.
METHODS
Human intestinal tissue specimens were obtained from an endoscopic biopsy or surgical resections performed at Johns Hopkins Hospital. Crypts were isolated, enteroids were propagated in culture, induced to undergo differentiation, and transduced with lentiviral vectors. Crypt markers, surface cell enzymes, and membrane ion transporters were characterized using quantitative reverse-transcription polymerase chain reaction, immunoblot, or immunofluorescence analyses. We used multiphoton and time-lapse confocal microscopy to monitor intracellular pH and luminal dilatation in enteroids under basal and regulated conditions.
RESULTS
Enteroids differentiated upon withdrawal of WNT3A, yielding decreased crypt markers and increased villus-like characteristics. Na(+)/H(+) exchanger 3 activity was similar in undifferentiated and differentiated enteroids, and was affected by known inhibitors, second messengers, and bacterial enterotoxins. Forskolin-induced swelling was completely dependent on cystic fibrosis transmembrane conductance regulator and partially dependent on Na(+)/H(+) exchanger 3 and Na(+)/K(+)/2Cl(-) cotransporter 1 inhibition in undifferentiated and differentiated enteroids. Increases in cyclic adenosine monophosphate with forskolin caused enteroid intracellular acidification in HCO3(-)-free buffer. Cyclic adenosine monophosphate-induced enteroid intracellular pH acidification as part of duodenal HCO3(-) secretion appears to require cystic fibrosis transmembrane conductance regulator and electrogenic Na(+)/HCO3(-) cotransporter 1.
CONCLUSIONS
Undifferentiated or crypt-like, and differentiated or villus-like, human enteroids represent distinct points along the crypt-villus axis; they can be used to characterize electrolyte transport processes along the vertical axis of the small intestine. The duodenal enteroid model showed that electrogenic Na(+)/HCO3(-) cotransporter 1 might be a target in the intestinal mucosa for treatment of secretory diarrheas.
背景与目的
人肠道隐窝来源的肠类器官是一种肠道离子转运模型,需要通过与细胞培养和动物模型比较来进行验证。我们使用人小肠肠类器官研究未分化和分化培养物在基础和调节条件下的中性钠吸收以及刺激的液体和阴离子分泌,以显示它们与离子转输生理学和病理生理学的功能相关性。
方法
人肠道组织标本取自约翰霍普金斯医院进行的内镜活检或手术切除。分离隐窝,在培养中培养肠类器官,诱导其分化,并用慢病毒载体进行转导。使用定量逆转录聚合酶链反应、免疫印迹或免疫荧光分析对隐窝标志物、表面细胞酶和膜离子转运体进行表征。我们使用多光子和延时共聚焦显微镜监测基础和调节条件下肠类器官内的细胞内pH值和管腔扩张。
结果
在撤除WNT3A后,肠类器官发生分化,隐窝标志物减少,绒毛样特征增加。未分化和分化的肠类器官中钠/氢交换体3的活性相似,且受到已知抑制剂、第二信使和细菌肠毒素的影响。在未分化和分化的肠类器官中,福司可林诱导的肿胀完全依赖于囊性纤维化跨膜传导调节因子,部分依赖于钠/氢交换体3和钠/钾/2氯协同转运体1的抑制。在无HCO3(-)的缓冲液中,福司可林使环磷酸腺苷增加导致肠类器官细胞内酸化。作为十二指肠HCO3(-)分泌的一部分,环磷酸腺苷诱导的肠类器官细胞内pH酸化似乎需要囊性纤维化跨膜传导调节因子和电中性钠/碳酸氢根协同转运体1。
结论
未分化或隐窝样以及分化或绒毛样的人肠类器官代表沿隐窝 - 绒毛轴的不同点;它们可用于表征沿小肠垂直轴的电解质转运过程。十二指肠肠类器官模型表明,电中性钠/碳酸氢根协同转运体1可能是肠黏膜治疗分泌性腹泻的一个靶点。
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