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孕期酒精暴露会延缓胎儿C57BL小鼠中血清素神经元的迁移和发育。

Prenatal alcohol exposure retards the migration and development of serotonin neurons in fetal C57BL mice.

作者信息

Zhou F C, Sari Y, Zhang J K, Goodlett C R, Li T

机构信息

Department of Anatomy and Cell Biology, Indiana University School of Medicine, Indianapolis, IN 46202, USA.

出版信息

Brain Res Dev Brain Res. 2001 Feb 28;126(2):147-55. doi: 10.1016/s0165-3806(00)00144-9.

Abstract

Incomplete neural tube fusion (iNTF), induced by alcohol, in midline floor and roof plates was found in our recent study. In this study, serotonin (5-HT) neurons, known to be born entirely in the midline raphe at brainstem, were examined during their development with fetal alcohol exposure. Weight-matched C57BL mice pregnant dams were divided into three groups on E8: one received ethanol via a chocolate Sustacal liquid diet providing 20% ethanol-derived calories as the sole source of nutrients (ALC); the second received an isocaloric Sustacal liquid diet and was pair-fed to individual dams in the ethanol-fed group (PF); the third was fed ad lib rat chow (Chow). Fetal brains were obtained on E15 and were processed for immunostaining of 5-HT and its trophic factor, S100 beta. The ascending 5-HT neurons, in normal development, appear bilaterally near midline on E12, and by E15, as seen in chow and PF groups, migrate from the midline germinal zone laterally and dorsally to their final position with rich fibers. In contrast, in the E15 ALC group, many 5-HT-im neurons were found remaining in the midline germinal region or had migrated, but with under-differentiated, sparse fibers. There were 20--30% fewer 5-HT-im neurons in ALC as compared to PF and Chow. In addition, the number of S100 beta cells was less in ALC as compared with PF and Chow groups. No difference was found between PF and Chow in number of 5-HT-im or S100 beta-im cells. The 5-HT neurons found compromised in migration and differentiation may, in part, stem from failure of access to floor plate or midline tissue induction and the insufficient support by S100 beta. As 5-HT neurons have been implicated for signaling brain maturation, fewer 5-HT neurons may have lasting effects on the development of brain or, if persistent in the adult, profoundly affect adult brain function.

摘要

我们最近的研究发现,酒精会导致神经管融合不完全(iNTF),出现在中线的底板和顶板中。在这项研究中,对已知完全在脑干中线缝核中产生的血清素(5-HT)神经元在其发育过程中进行了胎儿酒精暴露检查。体重匹配的C57BL小鼠怀孕母鼠在胚胎第8天(E8)被分为三组:一组通过巧克力Sustacal液体饮食接受乙醇,该饮食提供20%乙醇衍生热量作为唯一营养来源(ALC组);第二组接受等热量的Sustacal液体饮食,并与乙醇喂养组的个体母鼠进行配对喂养(PF组);第三组自由采食大鼠饲料(Chow组)。在胚胎第15天(E15)获取胎儿大脑,并进行5-HT及其营养因子S100β的免疫染色处理。在正常发育过程中,上升的5-HT神经元在E12时双侧出现在中线附近,到E15时,如在Chow组和PF组中所见,从中线生发区向外侧和背侧迁移至其最终位置,伴有丰富的纤维。相比之下,在E15的ALC组中,发现许多5-HT免疫反应性神经元仍留在中线生发区域,或者已经迁移,但纤维分化不足且稀疏。与PF组和Chow组相比,ALC组中5-HT免疫反应性神经元减少了20%-30%。此外,与PF组和Chow组相比,ALC组中S100β细胞数量更少。PF组和Chow组在5-HT免疫反应性或S100β免疫反应性细胞数量上没有差异。发现迁移和分化受损的5-HT神经元可能部分源于无法接触底板或中线组织诱导以及S100β支持不足。由于5-HT神经元与大脑成熟信号有关,较少的5-HT神经元可能对大脑发育产生持久影响,或者如果在成年期持续存在,会深刻影响成年大脑功能。

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