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Tissue-engineered 3D cancer-in-bone modeling: silk and PUR protocols

机译:组织工程的3D骨癌建模:丝绸和PUR协议

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摘要

Cancers that metastasize or grow in the bone marrow are typically considered incurable and cause extensive damage to the bone and bone marrow. The bone is a complex, dynamic, three-dimensional (3D) environment composed of a plethora of cells that may contribute to, or constrain, the growth of tumor cells and development of bone disease. The development of safe and effective drugs is currently hampered by pre-clinical two-dimensional (2D) models whose poor predictive power does not accurately predict the success or failure of therapeutics. These inadequate models often result in drugs proceeding through extensive pre-clinical studies only to fail clinically. Consistently, 3D co-culture systems prove superior to 2D mono-cultures in modeling in vivo cell phenotypes, disease progression and response to therapeutics. As a complex, multicellular, multidimensional bone microenvironment, 3D models allow for more accurate predictions of tumor growth, cell–cell and cell–matrix interactions, and resulting therapeutic responses. In this review we will discuss various 3D models available and describe step-by-step protocols for two of the most well-established 3D culture models for studying tumor-induced bone disease.
机译:通常认为,在骨髓中转移或生长的癌症是无法治愈的,会对骨骼和骨髓造成广泛的损害。骨骼是由许多细胞组成的复杂,动态的三维(3D)环境,这些细胞可能有助于或限制肿瘤细胞的生长和骨骼疾病的发展。目前,临床前二维(2D)模型阻碍了安全有效药物的开发,该模型的不良预测能力无法准确预测治疗的成功或失败。这些不足的模型通常会导致药物经过广泛的临床前研究而只能在临床上失败。一致地,在建模体内细胞表型,疾病进展和对治疗的反应方面,证明3D共培养系统优于2D单培养。作为复杂的,多细胞,多维的骨骼微环境,3D模型可以更准确地预测肿瘤的生长,细胞间以及细胞基质间的相互作用以及由此产生的治疗反应。在这篇综述中,我们将讨论各种可用的3D模型,并描述用于研究肿瘤引起的骨病的两个最完善的3D培养模型的分步方案。

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