Criswell K A, Loch-Caruso R, Stuenkel E L
Department of Environmental and Industrial Health, University of Michigan, Ann Arbor 48109-2029.
Toxicol Appl Pharmacol. 1995 Feb;130(2):280-93. doi: 10.1006/taap.1995.1033.
The ability of environmental contaminants to modulate gap junctional communication between uterine smooth muscle cells is generally unknown, despite recognition that myometrial gap junctions may play a role in synchronizing uterine contractions during parturition. The present study tested the hypothesis that the organochlorine pesticide lindane (gamma-hexachlorocyclohexane) inhibits gap junctional communication in myometrial myocytes due to the release of phosphoinositide-dependent second messengers. The effect on gap junctional communication by lindane was tested in cultured rat myometrial smooth muscle cells by monitoring transfer of the fluorescent dye Lucifer yellow. A rapid, concentration-dependent, but reversible inhibition of dye transfer was noted with 4-min exposures, and inhibition was complete with 10 microM lindane. Lindane also stimulated the production of the Ca(2+)-releasing species inositol 1,4,5-trisphosphate which peaked at 5 min (100 pmol/mg protein) and remained elevated after a 15-min exposure. To examine the possible inhibitory role of Ca2+ on gap junctions, the Ca2+ ionophore 4-br-A23187 was used. Although A23187 also inhibited gap junctional communication, inhibition was not complete even at concentrations that appeared cytotoxic (70% inhibition at 2 microM A23187). Cells were then loaded with the Ca2+ chelator BAPTA-AM, which blocked the lindane-induced rise in calcium, and dye transfer experiments with lindane were repeated in Ca(2+)-free medium. Inhibition of dye transfer was still complete under these conditions, showing that increased intracellular calcium was not required for lindane-induced inhibition of gap junctional communication. Subsequently, 10 microM lindane was shown to produce a sustained increase in protein kinase C (PKC) activity (31, 17, and 15 pmol of PKC peptide phosphorylated/min/mg protein for 2-, 5-, and 10-min exposures, respectively). Known activators of PKC, 12-O-tetradecanoylphorbol 13-acetate (TPA) and 1,2-dioctanoyl-sn-glycerol, abolished gap junctional communication at nanomolar concentrations. Although use of the PKC inhibitor staurosporine failed to reverse lindane's inhibitory action, depletion of PKC activity through prolonged exposure to TPA partially reversed lindane's effect. This suggests that PKC activation potentiates but does not solely mediate lindane's inhibitory action on gap junctional communication.
尽管人们认识到子宫肌层间隙连接可能在分娩期间子宫收缩同步化中发挥作用,但环境污染物调节子宫平滑肌细胞间间隙连接通讯的能力总体上仍不清楚。本研究检验了以下假设:有机氯农药林丹(γ-六氯环己烷)由于磷酸肌醇依赖性第二信使的释放而抑制子宫肌层肌细胞中的间隙连接通讯。通过监测荧光染料路西法黄的转移,在培养的大鼠子宫肌层平滑肌细胞中测试了林丹对间隙连接通讯的影响。在4分钟的暴露时间内,观察到染料转移受到快速、浓度依赖性但可逆的抑制,在10微摩尔林丹作用下抑制作用完全。林丹还刺激了钙释放物质肌醇1,4,5-三磷酸的产生,其在5分钟时达到峰值(100皮摩尔/毫克蛋白质),在暴露15分钟后仍保持升高。为了研究钙离子对间隙连接可能的抑制作用,使用了钙离子载体4-溴-A23187。尽管A23187也抑制间隙连接通讯,但即使在出现细胞毒性的浓度下(2微摩尔A23187时70%的抑制率)抑制也不完全。然后用钙离子螯合剂BAPTA-AM处理细胞,其阻断了林丹诱导的钙离子升高,并在无钙培养基中重复了林丹的染料转移实验。在这些条件下,染料转移的抑制仍然完全,表明林丹诱导的间隙连接通讯抑制不需要细胞内钙离子增加。随后,显示10微摩尔林丹使蛋白激酶C(PKC)活性持续增加(分别在暴露2、5和10分钟时,PKC肽磷酸化的量为31、17和15皮摩尔/分钟/毫克蛋白质)。已知的PKC激活剂12-O-十四烷酰佛波醇13-乙酸酯(TPA)和1,2-二辛酰-sn-甘油在纳摩尔浓度下消除了间隙连接通讯。尽管使用PKC抑制剂星形孢菌素未能逆转林丹的抑制作用,但通过长时间暴露于TPA使PKC活性耗竭部分逆转了林丹的作用。这表明PKC激活增强但并非单独介导林丹对间隙连接通讯的抑制作用。
