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子宫肌层间质细胞与子宫肌收缩的协调性。

Myometrial interstitial cells and the coordination of myometrial contractility.

机构信息

Perinatal Research Group, 10 floor, St Luc University Hospital, Brussels, Belgium.

出版信息

J Cell Mol Med. 2009 Oct;13(10):4268-82. doi: 10.1111/j.1582-4934.2009.00894.x. Epub 2009 Sep 2.

Abstract

A strict regulation of contractility in the uterus and fallopian tube is essential for various reproductive functions. The uterus contributes, through either increased contractility or periods of relative quiescence, to: (i) expulsion of menstrual debris, (ii) sperm transport, (iii) adequate embryo placement during implantation, (iv) enlarging its capacity during pregnancy and (v) parturition. The dominant cell population of the uterine wall consists of smooth muscle cells that contain the contractile apparatus responsible for the generation of contractile force. Recent interest has focused on a new population of cells located throughout the myometrium on the borders of smooth muscle bundles. These cells are similar to interstitial cells of Cajal (ICC) in the gut that are responsible for the generation of electrical slow waves that control peristalsis. A precise role for myometrial Cajal-like interstitial cells (m-ICLC) has not been identified. m-ICLC express the c-kit receptor, involved in creating and maintaining the ICC phenotype in the gastrointestinal tract. However, both acute and prolonged inhibition of this receptor with the c-kit antagonist imatinib mesylate does not appear to affect the spontaneous contractility of myometrium. Calcium imaging of live tissue slices suggests that contractile signalling starts on the borders of smooth muscle bundles where m-ICLC are located and recently the possible role of extracellular ATP signalling from m-ICLC has been studied. This manuscript reviews the evidence regarding tissue-level signalling in the myometrium with a particular emphasis on the anatomical and possible functional aspects of m-ICLC as new elements of the contractile mechanisms in the uterus.

摘要

子宫和输卵管的收缩严格调节对于各种生殖功能至关重要。子宫通过增加收缩或相对静止期来贡献:(i)排出月经碎片,(ii)精子运输,(iii)在着床期间适当放置胚胎,(iv)在怀孕时扩大其容量和(v)分娩。子宫壁的主要细胞群体由平滑肌细胞组成,这些细胞含有负责产生收缩力的收缩装置。最近的兴趣集中在位于平滑肌束边界处的整个子宫肌层中的新细胞群体上。这些细胞类似于胃肠道中的 Cajal 间质细胞(ICC),负责产生控制蠕动的电慢波。子宫平滑肌样间质细胞(m-ICLC)的确切作用尚未确定。m-ICLC 表达 c-kit 受体,该受体参与在胃肠道中创建和维持 ICC 表型。然而,用 c-kit 拮抗剂伊马替尼甲磺酸盐急性和长期抑制该受体似乎并不影响子宫平滑肌的自发性收缩性。活组织切片的钙成像表明,收缩信号起始于位于 m-ICLC 的平滑肌束边界处,最近研究了 m-ICLC 细胞外 ATP 信号传递的可能作用。本文综述了关于子宫肌层组织水平信号的证据,特别强调了 m-ICLC 的解剖学和可能的功能方面,作为子宫收缩机制的新元素。

https://cdn.ncbi.nlm.nih.gov/pmc/blobs/5251/4496132/5b2f3c6c88a8/jcmm0013-4268-f1.jpg

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