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Cardiac telocytes — their junctions and functional implications

机译:心肌细胞-它们的连接和功能含义

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Telocytes (TCs) form a cardiac network of interstitial cells. Our previous studies have shown that TCs are involved in heterocellular contacts with cardiomyocytes and cardiac stem/progenitor cells. In addition, TCs frequently establish ‘stromal synapses’ with several types of immunoreactive cells in various organs (www.telocytes.com). Using electron microscopy (EM) and electron microscope tomography (ET), we further investigated the interstitial cell network of TCs and found that TCs form ‘atypical’ junctions with virtually all types of cells in the human heart. EM and ET showed different junction types connecting TCs in a network (puncta adhaerentia minima, processus adhaerentes and manubria adhaerentia). The connections between TCs and cardiomyocytes are ‘dot’ junctions with nanocontacts or asymmetric junctions. Junctions between stem cells and TCs are either ‘stromal synapses’ or adhaerens junctions. An unexpected finding was that TCs have direct cell–cell (nano)contacts with Schwann cells, endothelial cells and pericytes. Therefore, ultrastructural analysis proved that the cardiac TC network could integrate the overall ‘information’ from vascular system (endothelial cells and pericytes), nervous system (Schwann cells), immune system (macrophages, mast cells), interstitium (fibroblasts, extracellular matrix), stem cells/progenitors and working cardiomyocytes. Generally, heterocellular contacts occur by means of minute junctions (point contacts, nanocontacts and planar contacts) and the mean intermembrane distance is within the macromolecular interaction range (10–30 nm). In conclusion, TCs make a network in the myocardial interstitium, which is involved in the long-distance intercellular signaling coordination. This integrated interstitial system appears to be composed of large homotropic zones (TC–TC junctions) and limited (distinct) heterotropic zones (heterocellular junctions of TCs).
机译:telocytes(TCs)形成间质细胞的心脏网络。我们以前的研究表明,TCs参与与心肌细胞和心脏干/祖细胞的异源性接触。此外,TC经常在各种器官中与几种类型的免疫反应细胞建立“基质突触”(www.telocytes.com)。使用电子显微镜(EM)和电子显微镜断层摄影(ET),我们进一步研究了TC的间质细胞网络,发现TC与人心脏中几乎所有类型的细胞形成“非典型”连接。 EM和ET显示了在网络中连接TC的不同结点类型(小突点小突突,突突小突突和Manubria小突突)。 TC和心肌细胞之间的连接是具有纳米接触或不对称连接的“点”连接。干细胞与TC之间的连接点是“基质突触”或adhaerens连接点。一个出乎意料的发现是,TC与雪旺氏细胞,内皮细胞和周细胞有直接的细胞-细胞(纳米)接触。因此,超微结构分析证明了心脏TC网络可以整合来自血管系统(内皮细胞和周细胞),神经系统(Schwann细胞),免疫系统(巨噬细胞,肥大细胞),间质(成纤维细胞,细胞外基质)的整体“信息” ,干细胞/祖细胞和正常的心肌细胞。通常,异质细胞接触通过微小的连接(点接触,纳米接触和平面接触)发生,并且平均膜间距离在大分子相互作用范围内(10–30 nm)。总之,TCs在心肌间质中形成网络,该网络参与长距离细胞间信号协调。这种整合的间隙系统似乎由较大的同质带(TC-TC交界处)和有限的(不同的)异质带(TC的异质细胞交界处)组成。

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