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降钙素基因相关肽系统在调节猪炎症子宫收缩功能中的作用。

Involvement of the calcitonin gene-related peptide system in the modulation of inflamed uterus contractile function in pigs.

机构信息

Division of Reproductive Biology, Institute of Animal Reproduction and Food Research of the Polish Academy of Sciences, Tuwima 10, 10-078, Olsztyn, Poland.

Department of Clinical Physiology, Faculty of Veterinary Medicine, University of Warmia and Mazury, Oczapowskiego 13, 10-718, Olsztyn, Poland.

出版信息

Sci Rep. 2022 Nov 9;12(1):19146. doi: 10.1038/s41598-022-23867-6.

Abstract

This study analyzed severe acute endometritis action on myometrial density and distribution of protein gene product (PGP)9.5- and calcitonin gene-related peptide (CGRP)-like immunoreactive nerve fibers and calcitonin receptor-like receptor (CLR) expression, and on CGRP receptor (CGRPR) participation in uterine contractility in pigs. E. coli suspension (E. coli group) or saline (SAL group) were injected into the uteri, or only laparotomy was performed (CON group). In the E. coli group myometrium, a lack of significant changes in PGP9.5 and CGRP innervation patterns and increased CLR protein level were revealed. In all groups, compared to the pretreatment period, human αCGRP increased amplitude in the myometrium, while reducing it in endometrium/myometrium. In the E. coli group endometrium/myometrium, human αCGRP lowered amplitude vs other groups. Human αCGRP reduced frequency in CON and SAL groups and enhanced it in the E. coli group endometrium/myometrium. The frequency in E. coli group increased vs other groups. CGRPR antagonist, human αCGRP8-37, reversed (CON, SAL groups) and eliminated (E. coli group) the rise in human αCGRP-induced myometrial amplitude. In endometrium/myometrium, human αCGRP8-37 abolished (CON group) and reversed (SAL group) a decrease in frequency, and reduced the rise in frequency (E. coli group) caused by human αCGRP. Collectively, in the myometrium, endometritis did not change PGP9.5 and CGRP innervation patterns and enhanced CLR protein level. CGRPR also mediated in CGRP action on inflamed uterus contractility.

摘要

本研究分析了严重急性子宫内膜炎对猪子宫肌层密度和蛋白基因产物(PGP)9.5 和降钙素基因相关肽(CGRP)样免疫反应性神经纤维及降钙素受体样受体(CLR)表达的影响,以及 CGRP 受体(CGRPR)在子宫收缩中的参与作用。将大肠杆菌悬浮液(大肠杆菌组)或生理盐水(SAL 组)注入子宫,或仅行剖腹术(CON 组)。在大肠杆菌组的子宫肌层中,发现 PGP9.5 和 CGRP 神经支配模式无明显变化,CLR 蛋白水平升高。在所有组中,与预处理期相比,人 αCGRP 增加了子宫肌层的振幅,而降低了子宫内膜/子宫肌层的振幅。在大肠杆菌组的子宫内膜/子宫肌层中,人 αCGRP 降低了与其他组相比的振幅。人 αCGRP 在 CON 和 SAL 组中降低了频率,而在大肠杆菌组的子宫内膜/子宫肌层中增强了频率。大肠杆菌组的频率高于其他组。CGRPR 拮抗剂人 αCGRP8-37 逆转(CON、SAL 组)和消除(大肠杆菌组)了人 αCGRP 引起的子宫肌层振幅升高。在子宫内膜/子宫肌层中,人 αCGRP8-37 消除了(CON 组)和逆转了(SAL 组)频率的降低,并降低了人 αCGRP 引起的频率升高(大肠杆菌组)。总之,在子宫肌层中,子宫内膜炎并未改变 PGP9.5 和 CGRP 神经支配模式,并增强了 CLR 蛋白水平。CGRPR 也介导了 CGRP 对炎症子宫收缩的作用。

https://cdn.ncbi.nlm.nih.gov/pmc/blobs/0b7c/9646719/eefbedfc4162/41598_2022_23867_Fig1_HTML.jpg

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