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前脂肪酶在大鼠胃中产生——肠抑胃肽的一种新来源。

Procolipase is produced in the rat stomach--a novel source of enterostatin.

作者信息

Sörhede M, Mulder H, Mei J, Sundler F, Erlanson-Albertsson C

机构信息

Department of Cell and Molecular Biology, University of Lund, Sweden.

出版信息

Biochim Biophys Acta. 1996 Jun 11;1301(3):207-12. doi: 10.1016/0005-2760(96)00034-3.

Abstract

Procolipase was identified in the stomach by in situ hybridisation. A strong autoradiographic labelling of chief cells was seen in the fundus region, declining more distally and being almost absent in antrum. There was no labelling seen in the intestine. Colipase activity was estimated in rat gastric juice following pentagastrin stimulation and was found to average 2 microM. Furthermore, enterostatin, the N-terminal pentapeptide of procolipase, has been identified in the rat gut and pancreas. Extracts from gastric mucosa, intestinal mucosa and pancreas were purified by gel filtration (Sephadex G25), ion-exchange chromatography (CM-Sepharose) and HPLC (C18 reverse phase). Using an ELISA assay with antibodies directed against enterostatin, two forms of the peptide were identified both in the gut and in the pancreas, with the amino-acid sequences APGPR and VPGPR, respectively. APGPR was found to be the predominant form of enterostatin, whereas only a small amount had the structure VPGPR. Enterostatin in the form of APGPR, when injected intracerebroventricularly in female Sprague-Dawley rats, significantly reduced high-fat food intake in a two-choice situation of low-fat (14% fat by energy) and high-fat (38% fat) food. It is concluded that procolipase is produced in the stomach and secreted into the gastric juice. This is also a novel source of enterostatin.

摘要

通过原位杂交在胃中鉴定出前膦脂酶。在胃底部区域可见主细胞有强烈的放射自显影标记,向远端逐渐减弱,在胃窦几乎不存在。在肠道中未观察到标记。在五肽胃泌素刺激后,对大鼠胃液中的膦脂酶活性进行了估计,发现平均为2微摩尔。此外,前膦脂酶的N端五肽肠抑素已在大鼠肠道和胰腺中被鉴定出来。胃黏膜、肠黏膜和胰腺的提取物通过凝胶过滤(葡聚糖G25)、离子交换色谱(CM-琼脂糖)和高效液相色谱(C18反相)进行纯化。使用针对肠抑素的抗体进行酶联免疫吸附测定,在肠道和胰腺中均鉴定出两种形式的该肽,其氨基酸序列分别为APGPR和VPGPR。发现APGPR是肠抑素的主要形式,而只有少量具有VPGPR结构。当以APGPR形式的肠抑素经脑室内注射到雌性斯普拉格-道利大鼠体内时,在低脂(能量的14%为脂肪)和高脂(38%为脂肪)食物的二选一情况下,显著降低了高脂肪食物的摄入量。结论是前膦脂酶在胃中产生并分泌到胃液中。这也是肠抑素的一个新来源。

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