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配体密度和降解性对水凝胶诱导乳腺癌休眠和激活的影响。

The Influence of Ligand Density and Degradability on Hydrogel Induced Breast Cancer Dormancy and Reactivation.

机构信息

Department of Biomedical Engineering, University of Delaware, 590 Avenue 1743, Biomedical Engineering, Newark, DE, 19713, USA.

出版信息

Adv Healthc Mater. 2021 Jun;10(11):e2002227. doi: 10.1002/adhm.202002227. Epub 2021 Apr 30.

Abstract

The role of hydrogel properties in regulating the phenotype of triple negative metastatic breast cancer is investigated using four cell lines: the MDA-MB-231 parental line and three organotropic sublines BoM-1833 (bone-tropic), LM2-4175 (lung-tropic), and BrM2a-831 (brain-tropic). Each line is encapsulated and cultured for 15 days in three poly(ethylene glycol) (PEG)-based hydrogel formulations composed of proteolytically degradable PEG, integrin-ligating RGDS, and the non-degradable crosslinker N-vinyl pyrrolidone. Dormancy-associated metrics including viable cell density, proliferation, metabolism, apoptosis, chemoresistance, phosphorylated-ERK and -p38, and morphological characteristics are quantified. A multimetric classification approach is implemented to categorize each hydrogel-induced phenotype as: 1) growth, 2) balanced tumor dormancy, 3) balanced cellular dormancy, or 4) restricted survival, cellular dormancy. Hydrogels with high adhesivity and degradability promote growth. Hydrogels with no adhesivity, but high degradability, induce restricted survival, cellular dormancy in the parental line and balanced cellular dormancy in the organotropic lines. Hydrogels with reduced adhesivity and degradability induce balanced cellular dormancy in the parental and lung-tropic lines and balanced tumor mass dormancy in bone- and brain-tropic lines. The ability to induce escape from dormancy via dynamic incorporation of RGDS is also presented. These results demonstrate that ECM properties and organ-tropism synergistically regulate cancer cell phenotype and dormancy.

摘要

研究了水凝胶性质在调节三阴性转移性乳腺癌表型中的作用,使用了四种细胞系:MDA-MB-231 亲本系和三种器官趋向性亚系 BoM-1833(骨趋向性)、LM2-4175(肺趋向性)和 BrM2a-831(脑趋向性)。将每条线分别包裹并在三种基于聚乙二醇(PEG)的水凝胶制剂中培养 15 天,这三种制剂由可酶解的 PEG、整合素结合 RGDS 和不可降解的交联剂 N-乙烯基吡咯烷酮组成。休眠相关的指标,包括活细胞密度、增殖、代谢、凋亡、化学抗性、磷酸化-ERK 和 -p38 以及形态特征都被定量。实施了一种多指标分类方法,将每种水凝胶诱导的表型归类为:1)生长,2)平衡肿瘤休眠,3)平衡细胞休眠,或 4)限制生存、细胞休眠。高黏附性和可降解性的水凝胶促进生长。无黏附性但可降解性高的水凝胶在亲本系中诱导限制生存、细胞休眠,在器官趋向性系中诱导平衡细胞休眠。降低黏附性和可降解性的水凝胶在亲本和肺趋向性系中诱导平衡细胞休眠,在骨和脑趋向性系中诱导平衡肿瘤质量休眠。还展示了通过动态掺入 RGDS 诱导逃避休眠的能力。这些结果表明,细胞外基质特性和器官趋向性协同调节癌细胞表型和休眠。

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