在小鼠输卵管中,电慢波依赖于细胞外和细胞内的钙源。
Electrical slow waves in the mouse oviduct are dependent on extracellular and intracellular calcium sources.
机构信息
Dept. of Physiology and Cell Biology, University of Nevada School of Medicine, Reno, NV 89557, USA.
出版信息
Am J Physiol Cell Physiol. 2011 Dec;301(6):C1458-69. doi: 10.1152/ajpcell.00293.2011. Epub 2011 Aug 31.
Spontaneous contractions of the myosalpinx are critical for oocyte transport along the oviduct. Slow waves, the electrical events that underlie myosalpinx contractions, are generated by a specialized network of pacemaker cells called oviduct interstitial cells of Cajal (ICC-OVI). The ionic basis of oviduct pacemaker activity is unknown. Intracellular recordings and Ca(2+) imaging were performed to examine the role of extracellular and intracellular Ca(2+) sources in slow wave generation. RT-PCR was performed to determine the transcriptional expression of Ca(2+) channels. Molecular studies revealed most isoforms of L- and T-type calcium channels (Cav1.2,1.3,1.4,3.1,3.2,3.3) were expressed in myosalpinx. Reduction of extracellular Ca(2+) concentration (Ca(2+)) resulted in the abolition of slow waves and myosalpinx contractions without significantly affecting resting membrane potential (RMP). Spontaneous Ca(2+) waves spread through ICC-OVI cells at a similar frequency to slow waves and were inhibited by reduced Ca(2+). Nifedipine depolarized RMP and inhibited slow waves; however, pacemaker activity returned when the membrane was repolarized with reduced extracellular K(+) concentration (K(+)). Ni(2+) also depolarized RMP but failed to block slow waves. The importance of ryanodine and inositol 1,4,5 trisphosphate-sensitive stores were examined using ryanodine, tetracaine, caffeine, and 2-aminoethyl diphenylborinate. Results suggest that although both stores are involved in regulation of slow wave frequency, neither are exclusively essential. The sarco/endoplasmic reticulum Ca(2+)-ATPase (SERCA) pump inhibitor cyclopiazonic acid inhibited pacemaker activity and Ca(2+) waves suggesting that a functional SERCA pump is necessary for pacemaker activity. In conclusion, results from this study suggest that slow wave generation in the oviduct is voltage dependent, occurs in a membrane potential window, and is dependent on extracellular calcium and functional SERCA pumps.
输卵管肌层的自发性收缩对于卵子沿输卵管的运输至关重要。慢波是输卵管肌层收缩的电活动基础,由称为输卵管间质细胞 Cajal(ICC-OVI)的特殊起搏细胞网络产生。输卵管起搏活动的离子基础尚不清楚。进行了细胞内记录和 Ca(2+)成像,以检查细胞外和细胞内 Ca(2+)源在慢波产生中的作用。进行 RT-PCR 以确定 Ca(2+)通道的转录表达。分子研究表明,大多数 L-和 T-型钙通道(Cav1.2、1.3、1.4、3.1、3.2、3.3)同工型在输卵管肌层中表达。降低细胞外 Ca(2+)浓度(Ca(2+))导致慢波和输卵管肌层收缩的消除,而对静息膜电位(RMP)没有明显影响。自发 Ca(2+)波以与慢波相似的频率在 ICC-OVI 细胞中传播,并被降低的Ca(2+)抑制。硝苯地平使 RMP 去极化并抑制慢波;然而,当用降低的细胞外 K(+)浓度(K(+))使膜复极化时,起搏活动恢复。Ni(2+)也使 RMP 去极化,但不能阻断慢波。使用瑞诺定、三甲卡因、咖啡因和 2-氨基乙基二苯基硼酸盐检查了ryanodine 和肌醇 1,4,5 三磷酸敏感储存库的重要性。结果表明,尽管这两种储存库都参与了慢波频率的调节,但都不是必不可少的。肌浆/内质网 Ca(2+) -ATP 酶(SERCA)泵抑制剂环匹阿尼酸抑制起搏活动和 Ca(2+)波,表明功能性 SERCA 泵对于起搏活动是必需的。总之,本研究结果表明,输卵管中的慢波产生是电压依赖性的,发生在膜电位窗口中,并且依赖于细胞外钙和功能性 SERCA 泵。
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