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诱导性早熟对雌性 Wistar 大鼠颅骨生长的影响。

Effects of induced precocious puberty on cranial growth in female Wistar rats.

机构信息

Department of Odontopediatrics and Orthodontics, Federal University of Rio Grande do Sul (UFRGS) Dental School, Brazil.

出版信息

Eur J Orthod. 2012 Apr;34(2):133-40. doi: 10.1093/ejo/cjq130. Epub 2011 Aug 1.

Abstract

This investigation examined the effects of pharmacologically induced precocious puberty on cranial growth in Wistar rats. Forty-eight female newborn Wistar rats were divided into two groups: a control group (C) and an experimental group (E), with four subgroups of six animals each. The time interval from birth until sacrifice differed between the subgroups, and was set at 30, 60, 90, and 120 days. An intramuscular single dose (300 μg) of steroid hormone danazol was administered on day 5 after birth, as a means of inducing precocious puberty. Alizarin (2 mg/100 g) was administered to three animals in each subgroup three days prior to sacrifice. Body mass and dates corresponding to the beginning of the oestrous cycle were recorded. Craniometric measurements were undertaken. Histological analysis using light and fluorescence microscopy was then carried out to qualitatively and quantitatively evaluate the spheno-occipital synchondrosis and to visualize bone deposition patterns. The results were analysed with a Student's t-test and analysis of variance. Precocious puberty was effectively induced and differences between groups denoted an earlier maturation in the experimental rats. In qualitative analysis, a significant increase of total synchondrosis width was noted only in group E60, in comparison with C60, and an increase in the E90 subgroup cortical bone width compared with the C90 subgroup. Histomorphometrically, a statistical difference between total width values of subgroups E60 (434.3 μm) and C60 (323.5 μm) was detected. However, body mass and macroscopic measurements did not show statistically significant differences. An appropriate model for studying bone growth associated with precocious puberty in Wistar female rats was not achieved using steroid hormone danazol, when evaluated at 30 day intervals.

摘要

本研究旨在探讨药物诱导性早熟对 Wistar 大鼠颅面生长的影响。48 只新生雌性 Wistar 大鼠被随机分为两组:对照组(C)和实验组(E),每组又分为 4 个亚组,每组 6 只。不同亚组的大鼠从出生到处死的时间间隔不同,分别为 30、60、90 和 120 天。在出生后第 5 天,实验组大鼠肌肉注射单剂量(300μg)类固醇激素丹那唑,以诱导性早熟。在处死前 3 天,每个亚组的 3 只大鼠经尾静脉注射茜素红(2mg/100g)。记录大鼠体重和动情周期开始的日期。进行颅测量。然后通过光镜和荧光显微镜对组织学进行分析,以定性和定量评估蝶枕缝的融合,并观察骨沉积模式。使用学生 t 检验和方差分析对结果进行分析。性早熟被有效诱导,实验组与对照组之间的差异表明实验组大鼠成熟更早。在定性分析中,仅在 E60 组中观察到总缝宽度显著增加,与 C60 组相比;E90 组皮质骨宽度与 C90 组相比也有所增加。组织形态计量学分析显示,E60 组(434.3μm)和 C60 组(323.5μm)的总宽度值存在统计学差异。然而,体重和宏观测量值无统计学差异。使用丹那唑作为类固醇激素未能成功建立一个研究 Wistar 雌性大鼠性早熟相关骨生长的合适模型,从 30 天的时间间隔评估。

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