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建立癌基因与肿瘤血管生成之间的联系。

Establishing a link between oncogenes and tumor angiogenesis.

作者信息

Kerbel R S, Viloria-Petit A, Okada F, Rak J

机构信息

Division of Cancer Biology Research, Sunnybrook Health Science Centre, Toronto, Ontario, Canada.

出版信息

Mol Med. 1998 May;4(5):286-95.

Abstract

We have tried to stress that mutant oncogenes or overexpressed, nonmutated proto-oncogenes, in addition to their direct affect on promoting aberrant tumor cell proliferation (and survival), may possess a crucial indirect means of stimulating tumor cell growth through regulation of angiogenesis. This effect would never be observed in tissue culture studies of oncogene function using pure cultures of tumor cells, which probably helps explain why the pro-angiogenic function of oncogenes has not been appreciated until only relatively recently. Indeed, the very first indication of a possible contributory role of oncogenes, such as ras and myc, to tumor angiogenesis was first reported by Thompson et al. in 1989, who used reconstituted organ cultures of the mouse prostate gland for their studies (69). This potentially important contribution of oncogenes to tumor growth and development may prove to have an impact on how various signal transduction inhibitors that are now in early phase clinical trials, e.g., monoclonal neutralizing antibodies to the human EGF receptor (70), function in vivo as anti-tumor agents.

摘要

我们一直强调,突变的癌基因或过度表达的非突变原癌基因,除了直接影响促进异常肿瘤细胞增殖(和存活)外,可能还拥有一种关键的间接方式,即通过调节血管生成来刺激肿瘤细胞生长。在使用肿瘤细胞纯培养物进行的癌基因功能组织培养研究中,永远不会观察到这种效应,这可能有助于解释为什么直到最近人们才认识到癌基因的促血管生成功能。事实上,1989年汤普森等人首次报道了癌基因(如ras和myc)可能对肿瘤血管生成起作用的迹象,他们使用小鼠前列腺的重组器官培养物进行研究(69)。癌基因对肿瘤生长和发展的这一潜在重要贡献,可能会对目前处于早期临床试验阶段的各种信号转导抑制剂(例如针对人表皮生长因子受体的单克隆中和抗体,70)在体内作为抗肿瘤药物的作用方式产生影响。

https://cdn.ncbi.nlm.nih.gov/pmc/blobs/4f6f/2230380/bf8abc594876/molmed00017-0015-a.jpg

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