Lefranc Florence, Sadeghi Niloufar, Metens Thierry, Brotchi Jacques, Salmon Isabelle, Kiss Robert
Department of Neurosurgery, Erasmus University Hospital, Brussels, Belgium.
Neurosurgery. 2003 Apr;52(4):881-90; discussion 890-1. doi: 10.1227/01.neu.0000053366.00088.80.
Growth patterns of astrocytic tumors can be modulated in vitro by gastrin. In this study, the influence of gastrin on the in vitro cell cycle kinetics and the in vivo growth features of three experimental malignant gliomas was investigated.
Gastrin-induced influence on overall growth was assayed in vitro by means of the 3-(4,5-dimethylthiazol-2-yl)-2,5-diphenyltetrazolium colorimetric assay for human U373 and rat C6 gliomas and for rat 9L gliosarcoma. Although cell cycle analyses were performed by means of computer-assisted microscope analyses of Feulgen-stained nuclei, the gastrin-induced effects of the levels of expression of cyclins D3 and E, CDK2, CDK4, CDK5, CDK7, p15, p16, E2F1, and E2F2 were assayed by means of quantitative Western blot test. The presence of ribonucleic acids for the CCK(B) and CCK(C) gastrin receptors in the U373, C6, and 9L models was assayed by means of quantitative reverse transcriptase-polymerase chain reaction, and the presence or absence of ribonucleic acids for CCK(A) receptor was checked by means of conventional polymerase chain reaction. The influence of gastrin was also characterized in vivo in terms of the survival periods of conventional rats orthotopically grafted with the C6 and 9L models and nude rats with the U373 model.
Gastrin significantly decreased the overall growth rate in the rat C6 and the human U373 high-grade astrocytic tumor models with either CCK(B) or CCK(C) gastrin receptor but not in the 9L rat gliosarcoma, which had no CCK(B) gastrin receptor (but had CCK(A) receptor) and only weak amounts of CCK(C) receptor. This effect seems to occur via a cytostatic effect; that is, an accumulation of tumor astrocytes occurs in the G(1) cell cycle phase. The cytostatic effect could relate to a gastrin-induced decrease in the amounts of the cyclin D3-CDK4 complex in both C6 and U373 glioma cells. In vivo, gastrin significantly increased the survival periods of C6 and U373 glioma-bearing rats, but not of 9L gliosarcoma-bearing rats.
Gastrin is able to significantly modify the growth levels of a number of experimental gliomas.
胃泌素可在体外调节星形细胞瘤的生长模式。在本研究中,研究了胃泌素对三种实验性恶性胶质瘤体外细胞周期动力学及体内生长特征的影响。
采用3-(4,5-二甲基噻唑-2-基)-2,5-二苯基四氮唑比色法检测胃泌素对人U373、大鼠C6胶质瘤及大鼠9L胶质肉瘤体外总体生长的影响。虽然通过对Feulgen染色细胞核进行计算机辅助显微镜分析来进行细胞周期分析,但通过定量蛋白质免疫印迹试验检测胃泌素对细胞周期蛋白D3和E、细胞周期蛋白依赖性激酶2(CDK2)、CDK4、CDK5、CDK7、p15、p16、E2F1和E2F2表达水平的影响。通过定量逆转录-聚合酶链反应检测U373、C6和9L模型中CCK(B)和CCK(C)胃泌素受体的核糖核酸的存在情况,并通过常规聚合酶链反应检查CCK(A)受体核糖核酸的有无。还通过原位移植C6和9L模型的常规大鼠以及移植U373模型的裸鼠的生存期,在体内表征胃泌素的影响。
胃泌素显著降低了具有CCK(B)或CCK(C)胃泌素受体的大鼠C6和人U373高级别星形细胞瘤模型的总体生长速率,但对不具有CCK(B)胃泌素受体(但具有CCK(A)受体)且仅含有少量CCK(C)受体的9L大鼠胶质肉瘤没有影响。这种作用似乎是通过细胞生长抑制作用发生的;也就是说,肿瘤星形胶质细胞在G(1)细胞周期阶段发生积聚。细胞生长抑制作用可能与胃泌素诱导的C6和U373胶质瘤细胞中细胞周期蛋白D3-CDK4复合物数量减少有关。在体内,胃泌素显著延长了携带C6和U373胶质瘤大鼠的生存期,但对携带9L胶质肉瘤大鼠的生存期没有影响。
胃泌素能够显著改变多种实验性胶质瘤的生长水平。
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