{"title":"维甲酸对人神经母细胞瘤细胞分化、增殖和粘附的影响。","authors":"A Voigt, P Hartmann, F Zintl","doi":"10.3109/15419060009109023","DOIUrl":null,"url":null,"abstract":"<p><p>Because of the known property of spontaneous regression in stage IVS of neuroblastoma all attempts are made to elucidate whether differentiation inducers possibly could be applied for neuroblastoma therapy. Here we examined the influence of retinoic acid (RA) in vitro on differentiation, proliferation and adhesion of 10 permanent and 4 primary cell lines as well as of several SCID-mouse tumour transplants. In general, after RA treatment morphologically different cell types which are characteristic for neuroblastoma cells have changed. N (neuronal)-type cells prolonged their neuronal processes, whereas S (epithelial, substrate-adherent, Schwann cell-like)-type cells lost their adherence to substratum and became apoptotic. Additionally, the reactions of all neuroblastoma cell lines with monoclonal antibodies against beta-tubulin (for neuronal cells) and glial fibrillary acidic protein (for epithelial cells) were determined. The anti-proliferative effect of all-trans-RA as well as 13-cis-RA was more profound in S-type cells (up to 40% in primary cell lines). To elucidate the role of adhesion molecules during neuronal cell differentiation, we have analysed the adhesion of neuroblastoma cells on poly-D-lysin-precoated plates under RA influence. While N-type cells displayed an increased adhesion, all S-type cell lines as well as all primary cell lines exhibited a reduced adhesion (IMR-5 and IMR-32: p < 0.001; JW, SR and PM: p < 0.05). RA treatment increased predominantly the tested antigens (HCAM, ICAM-1, NCAM, PECAM-1, VCAM-1, cadherin, FGF-R, IGF-R, NGF-R, TGF-beta/1, NF200, NF160, NF68, NSE, HLA-ABC) in all cell lines independently of their phenotypes (TGF-beta/1: p < 0.001; NF68: p < 0.01; PECAM-1 and NGF-R: p < 0.05). In recultured SCID-mouse-passaged tumour cells antigens were down-regulated (FGF-R: p < 0.01), but increased again after RA influence (TGF-beta/1: p < 0.05). In summary, the RA differentiation model demonstrates the possibility to interfere in cell adhesion and to diminish growth potential both in N-type as well as S-type neuroblastoma cells.</p>","PeriodicalId":79325,"journal":{"name":"Cell adhesion and communication","volume":"7 5","pages":"423-40"},"PeriodicalIF":0.0000,"publicationDate":"2000-05-01","publicationTypes":"Journal Article","fieldsOfStudy":null,"isOpenAccess":false,"openAccessPdf":"https://sci-hub-pdf.com/10.3109/15419060009109023","citationCount":"48","resultStr":"{\"title\":\"Differentiation, proliferation and adhesion of human neuroblastoma cells after treatment with retinoic acid.\",\"authors\":\"A Voigt, P Hartmann, F Zintl\",\"doi\":\"10.3109/15419060009109023\",\"DOIUrl\":null,\"url\":null,\"abstract\":\"<p><p>Because of the known property of spontaneous regression in stage IVS of neuroblastoma all attempts are made to elucidate whether differentiation inducers possibly could be applied for neuroblastoma therapy. Here we examined the influence of retinoic acid (RA) in vitro on differentiation, proliferation and adhesion of 10 permanent and 4 primary cell lines as well as of several SCID-mouse tumour transplants. In general, after RA treatment morphologically different cell types which are characteristic for neuroblastoma cells have changed. N (neuronal)-type cells prolonged their neuronal processes, whereas S (epithelial, substrate-adherent, Schwann cell-like)-type cells lost their adherence to substratum and became apoptotic. Additionally, the reactions of all neuroblastoma cell lines with monoclonal antibodies against beta-tubulin (for neuronal cells) and glial fibrillary acidic protein (for epithelial cells) were determined. The anti-proliferative effect of all-trans-RA as well as 13-cis-RA was more profound in S-type cells (up to 40% in primary cell lines). To elucidate the role of adhesion molecules during neuronal cell differentiation, we have analysed the adhesion of neuroblastoma cells on poly-D-lysin-precoated plates under RA influence. While N-type cells displayed an increased adhesion, all S-type cell lines as well as all primary cell lines exhibited a reduced adhesion (IMR-5 and IMR-32: p < 0.001; JW, SR and PM: p < 0.05). RA treatment increased predominantly the tested antigens (HCAM, ICAM-1, NCAM, PECAM-1, VCAM-1, cadherin, FGF-R, IGF-R, NGF-R, TGF-beta/1, NF200, NF160, NF68, NSE, HLA-ABC) in all cell lines independently of their phenotypes (TGF-beta/1: p < 0.001; NF68: p < 0.01; PECAM-1 and NGF-R: p < 0.05). In recultured SCID-mouse-passaged tumour cells antigens were down-regulated (FGF-R: p < 0.01), but increased again after RA influence (TGF-beta/1: p < 0.05). 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引用次数: 48
摘要
由于已知的神经母细胞瘤IVS期自发消退的特性,所有的尝试都是为了阐明分化诱导剂是否可能应用于神经母细胞瘤治疗。我们在体外研究了维甲酸(RA)对10个永久细胞系和4个原代细胞系以及几种scid小鼠肿瘤移植的分化、增殖和粘附的影响。一般来说,在RA治疗后,神经母细胞瘤细胞的形态学特征发生了变化。N(神经元)型细胞延长其神经元过程,而S(上皮、底物粘附、雪旺细胞样)型细胞失去对底物的粘附并发生凋亡。此外,测定了所有神经母细胞瘤细胞系对β -微管蛋白(用于神经元细胞)和胶质原纤维酸性蛋白(用于上皮细胞)单克隆抗体的反应。all-trans-RA和13-顺式ra的抗增殖作用在s型细胞中更为明显(在原代细胞系中高达40%)。为了阐明粘附分子在神经细胞分化过程中的作用,我们分析了RA影响下神经母细胞瘤细胞在聚d -溶素预涂覆板上的粘附。虽然n型细胞表现出增加的粘附,但所有s型细胞系和所有原代细胞系都表现出降低的粘附(IMR-5和IMR-32: p < 0.001;JW、SR、PM: p < 0.05)。RA处理显著增加了所有细胞系中检测抗原(HCAM、ICAM-1、NCAM、PECAM-1、VCAM-1、cadherin、FGF-R、IGF-R、NGF-R、tgf - β /1、NF200、NF160、NF68、NSE、HLA-ABC),与表型无关(tgf - β /1: p < 0.001;NF68: p < 0.01;PECAM-1和NGF-R: p < 0.05)。再培养scid小鼠传代肿瘤细胞抗原下调(FGF-R: p < 0.01),但RA影响后抗原再次升高(tgf - β /1: p < 0.05)。综上所述,RA分化模型显示了在n型和s型神经母细胞瘤细胞中干扰细胞粘附和降低生长潜力的可能性。
Differentiation, proliferation and adhesion of human neuroblastoma cells after treatment with retinoic acid.
Because of the known property of spontaneous regression in stage IVS of neuroblastoma all attempts are made to elucidate whether differentiation inducers possibly could be applied for neuroblastoma therapy. Here we examined the influence of retinoic acid (RA) in vitro on differentiation, proliferation and adhesion of 10 permanent and 4 primary cell lines as well as of several SCID-mouse tumour transplants. In general, after RA treatment morphologically different cell types which are characteristic for neuroblastoma cells have changed. N (neuronal)-type cells prolonged their neuronal processes, whereas S (epithelial, substrate-adherent, Schwann cell-like)-type cells lost their adherence to substratum and became apoptotic. Additionally, the reactions of all neuroblastoma cell lines with monoclonal antibodies against beta-tubulin (for neuronal cells) and glial fibrillary acidic protein (for epithelial cells) were determined. The anti-proliferative effect of all-trans-RA as well as 13-cis-RA was more profound in S-type cells (up to 40% in primary cell lines). To elucidate the role of adhesion molecules during neuronal cell differentiation, we have analysed the adhesion of neuroblastoma cells on poly-D-lysin-precoated plates under RA influence. While N-type cells displayed an increased adhesion, all S-type cell lines as well as all primary cell lines exhibited a reduced adhesion (IMR-5 and IMR-32: p < 0.001; JW, SR and PM: p < 0.05). RA treatment increased predominantly the tested antigens (HCAM, ICAM-1, NCAM, PECAM-1, VCAM-1, cadherin, FGF-R, IGF-R, NGF-R, TGF-beta/1, NF200, NF160, NF68, NSE, HLA-ABC) in all cell lines independently of their phenotypes (TGF-beta/1: p < 0.001; NF68: p < 0.01; PECAM-1 and NGF-R: p < 0.05). In recultured SCID-mouse-passaged tumour cells antigens were down-regulated (FGF-R: p < 0.01), but increased again after RA influence (TGF-beta/1: p < 0.05). In summary, the RA differentiation model demonstrates the possibility to interfere in cell adhesion and to diminish growth potential both in N-type as well as S-type neuroblastoma cells.
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