Nogueira A C, Neubert R, Felies A, Jacob-Müller U, Frankus E, Neubert D
University Medical Center, Free University Berlin, Germany.
Life Sci. 1996;58(4):337-48. doi: 10.1016/0024-3205(95)02293-7.
The two thalidomide (Thd) derivatives beta-EM12 and phthalimidophthalimide (Phtpht), which exhibit no obvious teratogenicity, were tested for their ability to induce changes in the pattern of lymphocyte subpopulations, and especially changes in integrin receptors, in marmosets (Callithrix jacchus). Previously, Thd and its highly teratogenic derivative alpha-EM12 had been found to alter the expression of adhesion molecules, such as CD2 (LFA-2) or CD11a/CD18 (LFA-1). None of these typical effects on adhesion receptors were observed following administration of the relatively high daily doses of 50 mg/kg body wt beta-EM12 and Phtpht. Nevertheless, there were some minor effects, such as alterations in the receptor density on peripheral blood mononuclear cells, which were often contrary to the effects induced by Thd. Mainly affected were: CD8 cells, B cells bearing the CD54 receptor and CD4 cells bearing the CD56 (NCAM) surface marker. We observed an increase in the receptor density of CD11c (p150,95) on monocytes with Phtpht but not with beta-EM12. The inability of the two substances with no obvious teratogenic potential to typically modify beta 2-integrin receptors on white blood cells at comparatively high doses is consistent with our hypothesis, that the teratogenicity of Thd may also be linked to alterations in the expression of adhesion molecules.
对两种无明显致畸性的沙利度胺(Thd)衍生物β-EM12和邻苯二甲酰亚胺基邻苯二甲酰亚胺(Phtpht),在狨猴(Callithrix jacchus)中测试了它们诱导淋巴细胞亚群模式变化的能力,特别是整合素受体的变化。此前已发现Thd及其高致畸性衍生物α-EM12可改变黏附分子的表达,如CD2(淋巴细胞功能相关抗原2)或CD11a/CD18(淋巴细胞功能相关抗原1)。给予相对高剂量(50mg/kg体重)的β-EM12和Phtpht后,未观察到这些对黏附受体的典型影响。然而,仍有一些轻微影响,如外周血单个核细胞上受体密度的改变,这些改变往往与Thd诱导的影响相反。主要受影响的是:CD8细胞、带有CD54受体的B细胞以及带有CD56(神经细胞黏附分子)表面标志物的CD4细胞。我们观察到,Phtpht可使单核细胞上CD11c(p150,95)的受体密度增加,而β-EM12则无此作用。这两种无明显致畸潜力的物质在相对高剂量下无法典型地改变白细胞上的β2整合素受体,这与我们的假设一致,即Thd的致畸性可能也与黏附分子表达的改变有关。
