Abbott B D, Birnbaum L S
National Toxicology Program, National Institute of Environmental Health Sciences, Research Triangle Park, North Carolina 27709.
Toxicol Appl Pharmacol. 1990 Dec;106(3):418-32. doi: 10.1016/0041-008x(90)90337-t.
2,3,7,8-Tetrachlorodibenzo-p-dioxin (TCDD) is teratogenic in mice, inducing cleft palate and hydronephrosis at doses which are not overtly maternally toxic or embryotoxic. After TCDD exposure the palatal shelves of normal size come into contact, but fail to fuse due to altered differentiation of the medial epithelial cells. These cells continue to express EGF receptors, proliferate, and differentiate into an oral-like stratified squamous epithelium. The present study examines the effect of TCDD on the expression of growth factors which are believed to regulate differentiation and proliferation in the palate. This study also examined the combined effect of TCDD and retinoic acid (RA), since in teratology studies coadministration of these agents results in an enhancement of cleft palate incidence. Embryos were exposed in vivo on Gestation Day (GD) 10 or 12 to TCDD ot TCDD + RA and the palatal shelves were dissected on GD 14-16. Growth factor expression was determined immunohistochemically using antibodies to TGF-alpha, EGF, TGF-beta 1, or TGF-beta 2. The growth factors displayed specific spatial and temporal expression in the palatal shelves. TCDD reduced the expression of TGF-alpha, EGF, and TGF-beta 1 in epithelial and mesenchymal cells. The degree of reduction was generally greater after exposure on GD 10 to TCDD alone or in combination with RA when compared to that on GD 12. The abnormal proliferation and differentiation of TCDD-exposed medial cells may be a response to reduced expression of EGF and TGF-alpha. Low levels of these factors may be related to the previously observed elevated levels of EGF receptors in medial cells. In other systems, low levels of ligand have resulted in upregulation of the EGF receptor. Continued proliferation and altered differentiation could also be attributable to decreased levels of TGF-beta 1, a factor inhibitory to epithelial proliferation. Since TGF-beta 1 stimulates mesenchymal growth and TGF-alpha and EGF stimulate epithelial proliferation, the formation of small shelves after exposure to TCDD + RA on GD 10 may be due to the severe reduction in these factors. Only a slight to moderate reduction in growth factor expression occurs after exposure to TCDD + RA on GD 12 and in this case shelves of normal size form. Since TCDD and RA appear to act in part through pathways that involve TGF-beta 1, in vitro experiments were designed to examine the involvement of TGF-beta 1 in TCDD teratogenicity.(ABSTRACT TRUNCATED AT 400 WORDS)
2,3,7,8-四氯二苯并对二恶英(TCDD)对小鼠具有致畸性,在不会明显导致母体毒性或胚胎毒性的剂量下可诱发腭裂和肾积水。TCDD暴露后,正常大小的腭突会接触,但由于内侧上皮细胞分化改变而无法融合。这些细胞继续表达表皮生长因子(EGF)受体,增殖并分化为类似口腔的复层鳞状上皮。本研究考察了TCDD对据信可调节腭部分化和增殖的生长因子表达的影响。本研究还考察了TCDD与视黄酸(RA)的联合作用,因为在致畸学研究中,同时给予这些药物会导致腭裂发生率增加。在妊娠第10天或第12天,将胚胎在体内暴露于TCDD或TCDD + RA,在妊娠第14 - 16天解剖腭突。使用针对转化生长因子-α(TGF-α)、EGF、转化生长因子-β1(TGF-β1)或转化生长因子-β2(TGF-β2)的抗体,通过免疫组织化学法测定生长因子表达。这些生长因子在腭突中呈现出特定的时空表达。TCDD降低了上皮细胞和间充质细胞中TGF-α、EGF和TGF-β1的表达。与妊娠第12天暴露相比,妊娠第10天单独暴露于TCDD或与RA联合暴露后,这些因子的降低程度通常更大。TCDD暴露的内侧细胞异常增殖和分化可能是对EGF和TGF-α表达降低的一种反应。这些因子的低水平可能与之前观察到的内侧细胞中EGF受体水平升高有关。在其他系统中,配体水平低会导致EGF受体上调。持续增殖和分化改变也可能归因于TGF-β1水平降低,TGF-β1是一种抑制上皮增殖的因子。由于TGF-β1刺激间充质生长,而TGF-α和EGF刺激上皮增殖,妊娠第10天暴露于TCDD + RA后小腭突的形成可能是由于这些因子的严重减少。妊娠第12天暴露于TCDD + RA后,生长因子表达仅出现轻微至中度降低,在这种情况下会形成正常大小的腭突。由于TCDD和RA似乎部分通过涉及TGF-β1的途径起作用,因此设计了体外实验来考察TGF-β1在TCDD致畸性中的作用。(摘要截短于400字)
