Phelps C J
Department of Structural and Cellular Biology, Tulane University School of Medicine, New Orleans, Louisiana 70112-2699, USA.
Endocrinology. 2004 Dec;145(12):5656-64. doi: 10.1210/en.2004-0931. Epub 2004 Sep 2.
Both Snell (Pit-1(dw) or (dwj), dw/dw) and Ames (Prophet of Pit-1(df), df/df) dwarf mice fail to produce prolactin (PRL) as well as GH due to deficient transcription factor Pit-1 activity and have reduced numbers of hypothalamic PRL-inhibiting area A12 tuberoinfundibular dopaminergic (TIDA) neurons. It has been reported that the TIDA deficit in Ames dwarf mice develops postnatally as a reduction in number after an initial increase that is comparable to that of normal siblings. The present study was designed to characterize A12 TIDA neuronal development in the Snell dwarf (dw/dw) compared with littermate normal mice. Brains of normal (DW/?) and dw(j)/dw(j) mice were examined at 7, 14, 21, 30, and > or = 60 postnatal days (d) by catecholamine fluorescence and quantification of neuron number after tyrosine hydroxylase immunostaining in dopaminergic (DA) areas A12, A13 (medial zona incerta), and A14 (periventricular nucleus). Fluorescence was less in dw/dw than in DW/? A12 perikarya and median eminence but was not reduced in other DA areas, such as substantia nigra, at all ages; A12 fluorescence was virtually absent in Snell dwarf adults. Numbers of TIDA neurons were comparable in normal and Snell dwarf mice at 7 d. In normal (DW/?) mice, A12 neurons increased in number to adult levels at 14 d and were significantly higher than in Snell dwarf (dw/dw) mice at 14 d (P < 0.05) and at subsequent ages (P < 0.01). In Snell dwarf mice, numbers of A12 neurons did not differ at 7, 14, and 21 d, decreased at 30 d (P < 0.05), and reached, at 60 d, 23% of the population in normal sibling mice (P < 0.01 compared with earlier ages). Neuron numbers in nonhypophysiotropic DA area A13 did not vary with age or phenotype. In A14, cell number was higher in both phenotypes at 14 d (P < 0.05 for DW/?; P < 0.01 for dw/dw); neuron number was lower in dw/dw than in DW/? mice at 30 d (P < 0.05) and 60 d (P < 0.01). Thus, compared with normal mice of the same strain, the A12 deficit is more severe in Snell (dw/dw) than in Ames (df/df) dwarf hypothalamus (48% of DF/?), as previously reported, and develops as a decline from the population present at 7 d rather than first increasing. A reduction in A14 neuron number also occurs in the Snell dwarf. Treatment of DW/dw- and dw/dw-containing litters with ovine PRL (50 mug/d, ip), beginning at 12 or 7 d and continuing until 42 d, resulted in TIDA neuron numbers in Snell dwarfs that were lower than those in normal siblings (P < 0.01 for both) but were higher than in untreated adult dwarfs and comparable to the TIDA population size in dwarfs at 7 d, indicating that PRL maintained this maximal number and prevented TIDA neuron dedifferentiation, which occurs in dwarf postnatal development.
斯内尔(Pit-1(dw) 或 (dwj),dw/dw)和阿梅斯(Pit-1 先知 (df),df/df)侏儒小鼠由于转录因子 Pit-1 活性不足,无法产生催乳素(PRL)和生长激素(GH),并且下丘脑催乳素抑制区 A12 结节漏斗多巴胺能(TIDA)神经元数量减少。据报道,阿梅斯侏儒小鼠的 TIDA 缺陷在出生后发展,最初数量增加后数量减少,这一增加幅度与正常同窝小鼠相当。本研究旨在比较斯内尔侏儒(dw/dw)与同窝正常小鼠中 A12 TIDA 神经元的发育情况。通过儿茶酚胺荧光法以及对多巴胺能(DA)区域 A12、A13(内侧未定带)和 A14(室周核)中酪氨酸羟化酶免疫染色后的神经元数量进行定量,在出生后第 7、14、21、30 天以及≥60 天检查正常(DW/?)和 dw(j)/dw(j) 小鼠的大脑。dw/dw 小鼠 A12 核周体和正中隆起处的荧光低于 DW/? 小鼠,但在所有年龄段,其他 DA 区域如黑质的荧光并未降低;在斯内尔侏儒成年小鼠中,A12 几乎没有荧光。在出生后第 7 天,正常小鼠和斯内尔侏儒小鼠的 TIDA 神经元数量相当。在正常(DW/?)小鼠中,A12 神经元数量在出生后第 14 天增加至成年水平,且在第 14 天以及随后各年龄段均显著高于斯内尔侏儒(dw/dw)小鼠(第 14 天 P < 0.05,其他年龄段 P < 0.01)。在斯内尔侏儒小鼠中,A12 神经元数量在第 7、14 和 21 天没有差异,在第 30 天减少(P < 0.05),在第 60 天降至正常同窝小鼠数量的 23%(与早期相比 P < 0.01)。非促垂体 DA 区域 A13 的神经元数量不随年龄或表型变化。在 A14 区域,两种表型在第 14 天的细胞数量均较高(DW/? 小鼠 P < 0.05;dw/dw 小鼠 P < 0.01);在第 30 天和第 60 天,dw/dw 小鼠的神经元数量低于 DW/? 小鼠(P < 0.05)。因此,与同品系正常小鼠相比,如先前报道,斯内尔(dw/dw)侏儒下丘脑的 A12 缺陷比阿梅斯(df/df)侏儒更严重(为 DF/? 的 48%),并且是从出生后第 7 天的数量开始下降,而不是先增加。在斯内尔侏儒小鼠中,A14 神经元数量也减少。从出生后第 12 天或第 7 天开始,每天腹腔注射羊 PRL(50 μg/d),持续至第 42 天,对含有 DW/dw 和 dw/dw 的同窝小鼠进行处理,结果显示斯内尔侏儒小鼠的 TIDA 神经元数量低于正常同窝小鼠(两者均 P < 0.01),但高于未处理的成年侏儒小鼠,且与侏儒小鼠出生后第 7 天的 TIDA 神经元数量相当,这表明 PRL 维持了这一最大数量,并防止了侏儒出生后发育过程中发生的 TIDA 神经元去分化。
