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Synergy of matrix stiffness and EGFR inhibition in apoptosis of pancreatic tumor cells in 3D

机译:基质刚度和EGFR抑制在3D胰腺癌细胞凋亡中的协同作用

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This study highlights the importance of using a 3D matrix to study the effect of therapeutic drugs on pancreatic cancer cell survival. An EGFR peptide inhibitor, NYQQN, was found to be effective only in cell-responsive and stiffer matrices. Furthermore, the effective peptide dosage on inducing cell death was lower for cells encapsulated in a stiffer matrix than that used in a conventional 2D culture (i.e., 2 mM in 3D vs. 4 mM in 2D). In summary, this gel platform provides a highly tunable synthetic tumor microenvironment with precise controls over matrix properties for in vitro cancer cell research.
机译:这项研究强调了使用3D矩阵研究治疗药物对胰腺癌细胞存活的影响的重要性。发现EGFR肽抑制剂NYQQN仅对细胞反应性强的基质有效。此外,封装在较硬基质中的细胞诱导细胞死亡的有效肽剂量要比常规2D培养所用的有效肽剂量低(即3D中的2 mM与2D中的4 mM)。总之,该凝胶平台提供了高度可调节的合成肿瘤微环境,可精确控制体外癌细胞研究的基质特性。

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