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Enteroendocrine peptides regulate feeding behavior via controlling intestinal contraction of the silkworm Bombyx mori

机译:肠内分泌肽通过控制蚕Bombyx mori的肠道收缩来调节进食行为

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摘要

Our previous study demonstrated that predominant feeding inhibitory effects were found in the crude extracts of foregut and midgut of the silkworm Bombyx mori larvae. To address the entero-intestinal control crucial for the regulation of insect feeding behavior, the present study identified and functionally characterized feeding inhibitory peptides from the midgut of B. mori larvae. Purification and structural analyses revealed that the predominant inhibitory factors in the crude extracts were allatotropin (AT) and GSRYamide after its C-terminal sequence. In situ hybridization revealed that AT and GSRYamide were expressed in enteroendocrine cells in the posterior and anterior midgut, respectively. Receptor screening using Ca2+-imaging technique showed that the B. mori neuropeptide G protein-coupled receptor (BNGR)-A19 and -A22 acted as GSRYamide receptors and BNGR-A5 acted as an additional AT receptor. Expression analyses of these receptors and the results of the peristaltic motion assay indicated that these peptides participated in the regulation of intestinal contraction. Exposure of pharynx and ileum to AT and GSRYamide inhibited spontaneous contraction in ad libitum-fed larvae, while exposure of pharynx to GSRYamide did not inhibit contraction in non-fed larvae, indicating that the feeding state changed their sensitivity to inhibitory peptides. These different responses corresponded to different expression levels of their receptors in the pharynx. In addition, injection of AT and GSRYamide decreased esophageal contraction frequencies in the melamine-treated transparent larvae. These findings strongly suggest that these peptides exert feeding inhibitory effects by modulating intestinal contraction in response to their feeding state transition, eventually causing feeding termination.
机译:我们以前的研究表明,家蚕Bombyx mori幼虫的前肠和中肠的粗提物中发现了主要的摄食抑制作用。为了解决肠内肠道控制对昆虫摄食行为的调节至关重要的问题,本研究确定了食虫双歧杆菌幼虫中肠的摄食抑制肽并对其功能进行了表征。纯化和结构分析表明,粗提物中的主要抑制因素是C末端序列后的同素异形蛋白(AT)和GSRYamide。原位杂交表明,AT和GSRYamide分别在中肠后肠和前肠肠内分泌细胞中表达。使用Ca 2 + -成像技术进行的受体筛选显示,桑蚕神经肽G蛋白偶联受体(BNGR)-A19和-A22充当GSRYamide受体,BNGR-A5充当另外的AT受体。这些受体的表达分析和蠕动试验的结果表明,这些肽参与了肠收缩的调节。咽和回肠暴露于AT和GSRYamide可抑制随意喂养幼虫的自发收缩,而咽暴露于GSRYamide则不会抑制非喂养幼虫的收缩,这表明摄食状态改变了它们对抑制肽的敏感性。这些不同的反应对应于它们在咽中的受体的不同表达水平。此外,AT和GSRYamide的注射降低了三聚氰胺处理的透明幼虫的食道收缩频率。这些发现强烈暗示这些肽通过响应于其进食状态转变而调节肠收缩来发挥进食抑制作用,最终导致进食终止。

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