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乳腺中的分化与癌症:揭示一种古老的二分法。

Differentiation and cancer in the mammary gland: shedding light on an old dichotomy.

作者信息

Petersen O W, Rønnov-Jessen L, Weaver V M, Bissell M J

机构信息

Structural Cell Biology Unit, Panum Institute, Copenhagen, Denmark.

出版信息

Adv Cancer Res. 1998;75:135-61. doi: 10.1016/s0065-230x(08)60741-1.

Abstract

In this brief review, the development of breast cancer is discussed from the vantage of phenotypic differentiation, similar to what has been considered over the years for leukemias and melanomas, both of which express easily visible differentiation markers (Hart and Easty, 1991; Clarke et al., 1995; Lynch, 1995; Sachs, 1996; Sledge, 1996). The review is divided into a theoretical background for human breast differentiation and a discussion of recent experimental results in our laboratories with differentiation of breast epithelial cells. In the theoretical background, in situ markers of differentiation of normal breast and carcinomas are discussed with emphasis on their possible implications for tumor therapy. So far, most of the emphasis regarding differentiation therapy of tumors has been focused on the possible action of soluble factors, such as colony-stimulating factors in leukemias and retinoic acids in solid tumors (Lotan, 1996; Sachs, 1996). However, an emerging and promising new avenue in this area appears to point to additional factors, such as the cellular form and extracellular matrix (ECM) (Bissel et al., 1982; Bissel and Barcellos-Hoff, 1987; Ingber, 1992). The recent interest in these parameters has evolved along with an increasing understanding of the molecular composition of the ECM, and of the molecular basis of the classical findings that normal cell--in contrast to tumor cells--are anchorage dependent for survival and growth (Folkman and Moscona, 1978; Hannigan et al., 1996). We now know that this is the case for epithelial as well as fibroblastic cells, and that interaction with ECM is crucial for such regulation. Indeed, ECM and integrins are emerging as the central regulators of differentiation, apoptosis, and cancer (Boudreau et al., 1995; Boudreau and Bissel, 1996; Werb et al., 1996; Bissell, 1997; Weaver, et al., 1997). In the experimental part, we elaborate on our own recent experiments with functional culture models of the human breast, with particular emphasis on how "normal" and cancer cells could be defined within a reconstituted ECM. Special attention is given to integrins, the prominent ECM receptors. We further discuss a number of recent experimental results, all of which point to the same conclusion: namely that phenotypic reversion toward a more normal state for epithelial tumors is no longer an elusive goal. Thus "therapy by differentiation" could be broadened to include not only blood-borne tumors, but also solid tumors of epithelial origin.

摘要

在这篇简短的综述中,我们从表型分化的角度探讨了乳腺癌的发展,这类似于多年来对白血病和黑色素瘤的研究,白血病和黑色素瘤都表达易于观察到的分化标志物(哈特和伊斯蒂,1991;克拉克等人,1995;林奇,1995;萨克斯,1996;斯莱奇,1996)。综述分为人类乳腺分化的理论背景以及我们实验室中乳腺上皮细胞分化的最新实验结果讨论两部分。在理论背景部分,我们讨论了正常乳腺和癌组织的原位分化标志物,并重点阐述了它们对肿瘤治疗的潜在意义。到目前为止,肿瘤分化治疗的大部分研究重点都集中在可溶性因子的可能作用上,比如白血病中的集落刺激因子和实体瘤中的视黄酸(洛坦,1996;萨克斯,1996)。然而,该领域一个新兴且有前景的新方向似乎指向了其他因素,比如细胞形态和细胞外基质(ECM)(比塞尔等人,1982;比塞尔和巴塞洛斯 - 霍夫,1987;英格伯,1992)。随着对ECM分子组成以及正常细胞(与肿瘤细胞不同)依赖锚定进行存活和生长这一经典发现的分子基础的理解不断加深,人们对这些参数的兴趣日益浓厚(福克曼和莫斯科纳,1978;汉尼根等人,1996)。我们现在知道上皮细胞和成纤维细胞都是如此,并且与ECM的相互作用对于这种调节至关重要。事实上,ECM和整合素正逐渐成为分化、细胞凋亡和癌症的核心调节因子(布德罗等人,1995;布德罗和比塞尔,1996;韦布等人,1996;比塞尔,1997;韦弗等人,1997)。在实验部分,我们详细阐述了我们自己最近关于人乳腺功能培养模型的实验,特别强调了在重构的ECM中如何定义“正常”细胞和癌细胞。我们特别关注了整合素,即突出的ECM受体。我们还进一步讨论了一些最近的实验结果,所有这些结果都指向同一个结论:即上皮性肿瘤向更正常状态的表型逆转不再是一个难以实现的目标。因此,“分化治疗”可以扩展到不仅包括血源性肿瘤,还包括上皮起源的实体瘤。

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