Pietras Kristian, Pahler Jessica, Bergers Gabriele, Hanahan Douglas
Department of Biochemistry and Biophysics, Diabetes Center and Comprehensive Cancer Center, University of California San Francisco, San Francisco, California, United States ofAmerica.
PLoS Med. 2008 Jan 29;5(1):e19. doi: 10.1371/journal.pmed.0050019.
Important support functions, including promotion of tumor growth, angiogenesis, and invasion, have been attributed to the different cell types populating the tumor stroma, i.e., endothelial cells, cancer-associated fibroblasts, pericytes, and infiltrating inflammatory cells. Fibroblasts have long been recognized inside carcinomas and are increasingly implicated as functional participants. The stroma is prominent in cervical carcinoma, and distinguishable from nonmalignant tissue, suggestive of altered (tumor-promoting) functions. We postulated that pharmacological targeting of putative stromal support functions, in particular those of cancer-associated fibroblasts, could have therapeutic utility, and sought to assess the possibility in a pre-clinical setting.
We used a genetically engineered mouse model of cervical carcinogenesis to investigate platelet-derived growth factor (PDGF) receptor signaling in cancer-associated fibroblasts and pericytes. Pharmacological blockade of PDGF receptor signaling with the clinically approved kinase inhibitor imatinib slowed progression of premalignant cervical lesions in this model, and impaired the growth of preexisting invasive carcinomas. Inhibition of stromal PDGF receptors reduced proliferation and angiogenesis in cervical lesions through a mechanism involving suppression of expression of the angiogenic factor fibroblast growth factor 2 (FGF-2) and the epithelial cell growth factor FGF-7 by cancer-associated fibroblasts. Treatment with neutralizing antibodies to the PDGF receptors recapitulated these effects. A ligand trap for the FGFs impaired the angiogenic phenotype similarly to imatinib. Thus PDGF ligands expressed by cancerous epithelia evidently stimulate PDGFR-expressing stroma to up-regulate FGFs, promoting angiogenesis and epithelial proliferation, elements of a multicellular signaling network that elicits functional capabilities in the tumor microenvironment.
This study illustrates the therapeutic benefits in a mouse model of human cervical cancer of mechanism-based targeting of the stroma, in particular cancer-associated fibroblasts. Drugs aimed at stromal fibroblast signals and effector functions may prove complementary to conventional treatments targeting the overt cancer cells for a range of solid tumors, possibly including cervical carcinoma, the second most common lethal malignancy in women worldwide, for which management remains poor.
肿瘤基质中的不同细胞类型,即内皮细胞、癌症相关成纤维细胞、周细胞和浸润性炎症细胞,具有重要的支持功能,包括促进肿瘤生长、血管生成和侵袭。长期以来,成纤维细胞在癌组织中一直存在,并越来越多地被认为是功能性参与者。基质在宫颈癌中很突出,且与非恶性组织不同,提示其功能发生了改变(促进肿瘤)。我们推测,对假定的基质支持功能进行药理学靶向,特别是对癌症相关成纤维细胞的功能进行靶向,可能具有治疗作用,并试图在临床前环境中评估这种可能性。
我们使用一种基因工程小鼠宫颈癌发生模型,来研究癌症相关成纤维细胞和周细胞中的血小板衍生生长因子(PDGF)受体信号传导。用临床批准的激酶抑制剂伊马替尼对PDGF受体信号进行药理学阻断,减缓了该模型中癌前宫颈病变的进展,并抑制了已存在的浸润性癌的生长。抑制基质PDGF受体会通过一种机制减少宫颈病变中的增殖和血管生成,该机制涉及癌症相关成纤维细胞对血管生成因子成纤维细胞生长因子2(FGF-2)和上皮细胞生长因子FGF-7表达的抑制。用针对PDGF受体的中和抗体进行治疗可重现这些效果。一种FGFs配体陷阱与伊马替尼类似,损害了血管生成表型。因此,癌上皮细胞表达的PDGF配体显然刺激表达PDGFR的基质上调FGFs,促进血管生成和上皮增殖,这是一个多细胞信号网络的组成部分,可引发肿瘤微环境中的功能。
本研究说明了在人类宫颈癌小鼠模型中,基于机制靶向基质,特别是癌症相关成纤维细胞的治疗益处。针对基质成纤维细胞信号和效应功能的药物,可能被证明是针对一系列实体瘤(可能包括宫颈癌,宫颈癌是全球女性中第二常见的致命恶性肿瘤,其治疗效果仍然很差)中明显癌细胞的传统治疗的补充。
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