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α-黑素细胞刺激素的特异性受体广泛分布于啮齿动物的组织中。

Specific receptors for alpha-melanocyte-stimulating hormone are widely distributed in tissues of rodents.

作者信息

Tatro J B, Reichlin S

机构信息

Department of Medicine, Tufts University School of Medicine, New England Medical Center, Inc., Boston, Massachusetts 02111.

出版信息

Endocrinology. 1987 Nov;121(5):1900-7. doi: 10.1210/endo-121-5-1900.

Abstract

alpha MSH is known to act on several nonmelanocyte cell types, which has led to recent interest in its regulatory roles in fever, inflammation, immunity, and behavior. To determine its possible sites of action, we examined the distribution of alpha MSH receptors in a variety of tissues in mice and rats. The superpotent and enzymatically resistant alpha MSH analog, Nle4,D-Phe7-alpha MSH (NDP-MSH), was radioiodinated using lactoperoxidase (Enzymobeads) and purified by reverse phase chromatography for use as a tracer. [125I]NDP-MSH exhibited consistent and specific binding to cultured B16 and Cloudman S91 murine melanoma cells, which are highly responsive to alpha MSH. The tracer had full biological activity, as determined by its potency in stimulating melanogenesis in B16 cells. To study receptor distribution in vivo, [125I]NDP-MSH was administered iv to C3H/HeJ (pigmented) mice and Sprague-Dawley (albino) rats. To determine the specificity of tracer uptake by tissues, some animals received a large molar excess of alpha MSH together with [125I]NDP-MSH. Data were expressed as tissue to plasma radioactivity concentration ratios. In mice, specific (i.e. alpha MSH-inhibitable) binding of [125I]NDP-MSH was found in a number of glandular organs, including lacrimal, Harderian, preputial, submandibular, and adrenal glands and pancreas, as well as in brown and white adipose tissues, bladder, duodenum, skin, spleen, and hypothalamus. In rats, results were generally similar; specific tracer uptake was observed in lacrimal, Harderian, preputial, and thyroid glands; pancreas, duodenum, spleen, hypothalamus; and white adipose tissue. These results show that specific receptors for alpha MSH are widely distributed, suggesting that alpha MSH may affect the functions of a number of organs.

摘要

已知α-MSH作用于多种非黑素细胞类型,这使得近来人们对其在发热、炎症、免疫和行为方面的调节作用产生了兴趣。为了确定其可能的作用位点,我们研究了α-MSH受体在小鼠和大鼠多种组织中的分布情况。使用乳过氧化物酶(酶珠)对超强效且酶抗性的α-MSH类似物Nle4,D-Phe7-α-MSH(NDP-MSH)进行放射性碘化,并通过反相色谱法纯化,用作示踪剂。[125I]NDP-MSH与培养的B16和Cloudman S91小鼠黑素瘤细胞表现出一致且特异性的结合,这些细胞对α-MSH高度敏感。根据其刺激B16细胞黑素生成的效力确定,该示踪剂具有完全的生物学活性。为了研究体内受体分布,将[125I]NDP-MSH静脉注射给C3H/HeJ(有色)小鼠和Sprague-Dawley(白化)大鼠。为了确定组织摄取示踪剂的特异性,一些动物在注射[125I]NDP-MSH的同时给予大量摩尔过量的α-MSH。数据以组织与血浆放射性浓度比表示。在小鼠中,在许多腺器官中发现了[125I]NDP-MSH的特异性(即α-MSH可抑制的)结合,包括泪腺、哈德氏腺、包皮腺、下颌下腺、肾上腺和胰腺,以及棕色和白色脂肪组织、膀胱、十二指肠、皮肤、脾脏和下丘脑。在大鼠中,结果总体相似;在泪腺、哈德氏腺、包皮腺和甲状腺;胰腺、十二指肠、脾脏、下丘脑;以及白色脂肪组织中观察到特异性示踪剂摄取。这些结果表明,α-MSH的特异性受体广泛分布,提示α-MSH可能影响许多器官的功能。

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