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胚胎发育早期血清素合成减少会改变随后产前应激对成年雄性和雌性大鼠福尔马林试验中持续性疼痛的影响。

Reduced serotonin synthesis during early embryogeny changes effect of subsequent prenatal stress on persistent pain in the formalin test in adult male and female rats.

作者信息

Butkevich Irina Pavlovna, Mikhailenko Victor Anatol'evich, Vershinina Elena Andreevna, Khozhai Ludmila Ivanovna, Grigorev Igor'Pavlovich, Otellin Vladimir Alexandrovich

机构信息

Laboratory of Ontogenesis of Nervous System, IP Pavlov Institute of Physiology of the Russian Academy of Sciences, Nab. Makarova, 6. 199034, St. Petersburg, Russia.

出版信息

Brain Res. 2005 May 3;1042(2):144-59. doi: 10.1016/j.brainres.2005.02.022.

Abstract

The considerable evidence supporting a role for serotonin (5-HT) in the embryonic formation of CNS, mediation of prenatal stress, and pain processing is reviewed. Long-term influences of prenatal 5-HT depletion as well as its combination with prenatal stress effects on tonic nociceptive system in 90-day-old Wistar rats were studied in the formalin test. Pregnant dams were injected with para-chlorophenylalanine (pCPA, 400 mg/kg/2 ml, ip), producing 5-HT depletion during the early period of fetal serotonergic system development. The adult offspring from pCPA-treated dams revealed changes in behavioral indices of persistent pain (flexing + shaking and licking) in the formalin test (2.5%, 50 microl) that were accompanied by irreversible morphological alterations in the dorsal raphe nuclei. In the other series of experiments, the role of 5-HT in the mediation of prenatal stress on the behavioral indices of persistent pain was investigated in the adult offspring from dams with 5-HT depletion followed by restraint stress. Stress during the last embryonic week caused much more increase in flexing + shaking and licking in the second tonic phase of the response to formalin in offspring from pCPA- than saline-treated (control) dams. The former was characterized by alterations in the durations of the interphase, the second phase, and the whole behavioral response too. In offspring from pCPA-treated dams, sex dimorphism was revealed in tonic pain evaluated by licking. Together with our previous results in juvenile rats demonstrating the necessity of definite level of prenatal 5-HT for normal development of tonic nociceptive system, the present pioneering findings obtained in adult rats indicate that prenatal 5-HT depletion causes long-term morphological abnormalities in the dorsal raphe nuclei accompanied by alterations in behavioral indices of tonic pain. Early prenatal 5-HT depletion increases vulnerability of tonic nociceptive circuits to the following prenatal stress.

摘要

本文综述了大量证据,支持血清素(5-羟色胺,5-HT)在中枢神经系统胚胎形成、产前应激介导和疼痛处理中的作用。在福尔马林试验中,研究了产前5-HT耗竭及其与产前应激对90日龄Wistar大鼠紧张性伤害感受系统的长期影响。在胎儿血清素能系统发育早期,给怀孕母鼠注射对氯苯丙氨酸(pCPA,400mg/kg/2ml,腹腔注射),造成5-HT耗竭。来自pCPA处理母鼠的成年后代在福尔马林试验(2.5%,50微升)中表现出持续性疼痛行为指标(屈曲+颤抖和舔舐)的变化,同时中缝背核出现不可逆的形态改变。在另一系列实验中,研究了5-HT在产前应激介导对5-HT耗竭后再施加束缚应激的母鼠成年后代持续性疼痛行为指标中的作用。胚胎期最后一周的应激导致pCPA处理组母鼠后代在福尔马林反应的第二个紧张期比生理盐水处理(对照)组母鼠后代的屈曲+颤抖和舔舐行为增加更多。前者还表现为间期、第二阶段和整个行为反应持续时间的改变。在pCPA处理母鼠的后代中,通过舔舐评估的紧张性疼痛存在性别差异。结合我们之前在幼鼠身上的研究结果,即产前5-HT达到一定水平对紧张性伤害感受系统的正常发育是必要的,目前在成年大鼠中获得的开创性发现表明,产前5-HT耗竭会导致中缝背核长期形态异常,并伴有紧张性疼痛行为指标的改变。产前早期5-HT耗竭会增加紧张性伤害感受回路对后续产前应激的易感性。

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