Taylor R G, Fuller P J
Department of Surgery, Royal Childrens Hospital, Parkville, Victoria, Australia.
Baillieres Clin Endocrinol Metab. 1994 Jan;8(1):165-83. doi: 10.1016/s0950-351x(05)80230-7.
After the loss of small bowel through disease or surgery the residual bowel adapts by increasing its functional capacity. This process of adaptation involves dilatation, hypertrophy and mucosal hyperplasia, particularly distal to the area of bowel loss or disease. The response of the residual bowel is mediated by a complex interplay of factors including luminal nutrition, pancreaticobiliary secretions, luminal or local growth factors and also humoral or endocrine factors. The experimental model commonly used to characterize the adaptive response, massive small bowel resection (MSBR), involves 80% resection of the small bowel in the rat. Of the various putative humoral factors, most work has focused on the products of the ileal L cells: enteroglucagon and peptide YY. Plasma levels of both hormones are increased after MSBR and indeed their mRNA levels are also increased as a result of an increase in the amount of message per L cell. Whilst PYY probably serves as an 'ileal brake' to slow the movement of the luminal contents and hence increase their mucosal contact time, the role of the enteroglucagon is unresolved. The molecular cloning of the proglucagon gene has revealed, firstly, that there are a number of biologically active peptides which derive from the propeptide and, secondly, that tissue-specific differential processing occurs. Most studies do not clearly define which of these products of proglucagon is being measured and is termed as glucagon-like or enteroglucagon immunoreactivity. The insulin-like growth factors (IGF) have a potent mitogenic action on the bowel. Their role after MSBR is likely to be largely paracrine. Though IGF-I mRNA levels do not increase after MSBR, the precipitous and early fall in ileal IGF-binding protein-3 (IGFBP-3) mRNA levels suggests a fall in IGFBP-3 levels may increase local IGF-I bioactivity. Polyamine synthesis is a critical component of the adaptive response, although the stimulus to their dramatic increase in synthesis after MSBR remains to be elucidated. Other humoral factors such as cholecystokinin, neurotensin and bombesin probably have minor indirect roles in the adaptive response. Components of the epidermal growth factor/transforming growth factor alpha response pathway family of growth factors may be involved as paracrine regulators. There is thus strong evidence that humoral factors play an important role in intestinal adaptation; characterization of the nature of the humoral factors and their relationship with other influences such as luminal nutrition and pancreatic biliary secretions may facilitate the development of new therapeutic strategies for the short bowel syndromes.
由于疾病或手术导致小肠缺失后,残余肠段会通过增加其功能能力来进行适应。这种适应过程包括扩张、肥大和黏膜增生,尤其是在肠缺失或疾病区域的远端。残余肠段的反应是由多种因素复杂相互作用介导的,这些因素包括腔内营养、胰胆分泌、腔内或局部生长因子以及体液或内分泌因子。常用于表征适应性反应的实验模型是大鼠的大规模小肠切除术(MSBR),即切除大鼠80%的小肠。在各种假定的体液因子中,大多数研究都集中在回肠L细胞的产物:肠高血糖素和肽YY上。MSBR后这两种激素的血浆水平都会升高,实际上它们的mRNA水平也会因每个L细胞中信息数量的增加而升高。虽然PYY可能作为一种“回肠刹车”来减缓腔内内容物的移动,从而增加它们与黏膜的接触时间,但肠高血糖素的作用仍未明确。胰高血糖素原基因的分子克隆首先揭示,有许多生物活性肽源自该前体肽,其次,存在组织特异性的差异加工。大多数研究没有明确界定所检测的这些胰高血糖素原产物中哪一种被称为胰高血糖素样或肠高血糖素免疫反应性。胰岛素样生长因子(IGF)对肠道有强大的促有丝分裂作用。它们在MSBR后的作用可能主要是旁分泌。虽然MSBR后IGF-I mRNA水平没有增加,但回肠IGF结合蛋白-3(IGFBP-3)mRNA水平的急剧早期下降表明IGFBP-3水平的下降可能会增加局部IGF-I的生物活性。多胺合成是适应性反应的关键组成部分,尽管MSBR后刺激其合成急剧增加的因素仍有待阐明。其他体液因子如胆囊收缩素、神经降压素和蛙皮素可能在适应性反应中起次要的间接作用。表皮生长因子/转化生长因子α反应途径家族的生长因子成分可能作为旁分泌调节因子参与其中。因此,有强有力的证据表明体液因子在肠道适应中起重要作用;表征体液因子的性质及其与腔内营养和胰胆分泌等其他影响因素的关系,可能有助于开发针对短肠综合征的新治疗策略。
