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胎儿抗原1(FA1)能否识别具有再生、内分泌和神经内分泌潜能的细胞?对胚胎、胎儿、胎盘组织及母体循环中FA1的研究。

Does fetal antigen 1 (FA1) identify cells with regenerative, endocrine and neuroendocrine potentials? A study of FA1 in embryonic, fetal, and placental tissue and in maternal circulation.

作者信息

Floridon C, Jensen C H, Thorsen P, Nielsen O, Sunde L, Westergaard J G, Thomsen S G, Teisner B

机构信息

Department of Obstetrics and Gynaecology and Institute of Pathology, Odense University Hospital, Denmark.

出版信息

Differentiation. 2000 Aug;66(1):49-59. doi: 10.1046/j.1432-0436.2000.066001049.x.

Abstract

Fetal antigen 1 (FA1) is a circulating EGF multidomain glycoprotein. FA1 and its membrane-associated precursor is defined by the mRNAs referred to as delta-like (dlk), preadipocyte factor 1 (pref-1) or zona glomerulosa-specific factor (ZOG). Using a polyclonal antibody recognising both forms, the localisation of FA1/dlk was analysed in embryonic and fetal tissues between week 5 to 25 of gestation and related to germinal origin and development. FA1 was observed in endodermally derived hepatocytes, glandular cells of the pancreas anlage, and in respiratory epithelial cells. FA1 was also present in mesodermally derived cells of the renal proximal tubules, adrenal cortex, Leydig and Hilus cells of the testes and ovaries, fetal chondroblasts, and skeletal myotubes. Ectodermally derived neuro- and adenohypophysial cells, cells in the floor of the 3rd ventricle and plexus choroideus were also FA1 positive. The number of cells expressing FA1 decreased during fetal development where the expression became restricted to specific functional cells. Epidermis, gut epithelium, gall bladder, blood cells, spleen, thyroid gland, salivary glands, and smooth muscle cells were FA1 negative. Analysis of extra-embryonic tissues from normal and pathological pregnancies revealed FA1 in stromal cells surrounding the blood islands of the yolk sac as well as in placental fibroblasts where the expression was most pronounced in diploid, androgenic complete hydatidiform moles. However, as measured by ELISA, the circulating maternal FA1 levels in complete moles were not different from normal pregnancies. The results presented suggest that FA1 is a growth and/or differentiation factor extensively expressed in immature cells and down-regulated during fetal development. FA1 down-regulation was associated with a shift in the subcellular localisation indicating differential post-translational/post-transcriptional modifications during fetal development. FA1 may be a new marker of cellular subtypes with a regenerative potential and of specific cells with endocrine or neuroendocrine functions.

摘要

胎儿抗原1(FA1)是一种循环的表皮生长因子多结构域糖蛋白。FA1及其膜相关前体由被称为δ样(dlk)、前脂肪细胞因子1(pref-1)或球状带特异性因子(ZOG)的信使核糖核酸所定义。使用一种能识别两种形式的多克隆抗体,在妊娠第5至25周的胚胎和胎儿组织中分析了FA1/dlk的定位,并将其与胚层起源和发育相关联。在由内胚层衍生的肝细胞、胰腺原基的腺细胞以及呼吸上皮细胞中观察到了FA1。FA1也存在于由中胚层衍生的肾近端小管细胞、肾上腺皮质、睾丸和卵巢的间质细胞、睾丸间质细胞和门细胞、胎儿成软骨细胞以及骨骼肌管中。由外胚层衍生的神经垂体和腺垂体细胞、第三脑室底部的细胞以及脉络丛也呈FA1阳性。在胎儿发育过程中,表达FA1的细胞数量减少,其表达局限于特定的功能细胞。表皮、肠道上皮、胆囊、血细胞、脾脏、甲状腺、唾液腺和平滑肌细胞均为FA1阴性。对正常和病理妊娠的胚外组织分析显示,在卵黄囊血岛周围的基质细胞以及胎盘成纤维细胞中存在FA1,其表达在二倍体、雄激素性完全性葡萄胎中最为明显。然而,通过酶联免疫吸附测定法测量,完全性葡萄胎中母体循环中的FA1水平与正常妊娠并无差异。所呈现的结果表明,FA1是一种在未成熟细胞中广泛表达且在胎儿发育过程中下调的生长和/或分化因子。FA1的下调与亚细胞定位的改变相关,这表明在胎儿发育过程中存在不同的翻译后/转录后修饰。FA1可能是具有再生潜能的细胞亚型以及具有内分泌或神经内分泌功能的特定细胞的新标志物。

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