Department of Biological and Agricultural Engineering, Louisiana State University, Baton Rouge, Louisiana, USA.
Department of Chemistry, Louisiana State University, Baton Rouge, Louisiana, USA.
Tissue Eng Part A. 2021 Apr;27(7-8):500-511. doi: 10.1089/ten.TEA.2020.0364.
The development of resistance to therapy is a significant obstacle to effective therapeutic regimens. Evaluating the effects of oncology drugs in the laboratory setting is limited by the lack of translational models that accurately recapitulate cell-microenvironment interactions present in tumors. Acquisition of resistance to therapy is facilitated, in part, by the composition of the tumor extracellular matrix (ECM), with the primary current model using collagen I (COL I). Here we seek to identify the prevalence of COL I-enhanced expression in the triple-negative breast cancer (TNBC) subtype. Furthermore, we identify if methods of response to therapy are altered depending on matrix composition. We demonstrated that collagen content varies in patient tumor samples across subtypes, with COL I expression dramatically increased in typically less aggressive estrogen receptor (ER)-positive(ER)/progesterone receptor (PGR)-positive (PGR) cancers irrespective of patient age or race. These findings are of significance considering how frequently COL I is implicated in tumor progression. analyses of ER and ER-negative (ER) cell lines were used to determine the effects of ECM content (collagen I, collagen IV, fibronectin, and laminin) on proliferation, cellular phenotype, and survival. Neither ER nor ER cells demonstrated significant increases in proliferation when cultured on these ECM substrates. ER cells cultured on these substrates were sensitized to both chemotherapy and targeted therapy. In addition, MDA-MB-231 cells expressed different morphologies, binding affinities, and stiffness across these substrates. We also demonstrated that ECM composition significantly alters transcription of senescence-associated pathways across ER and ER cell lines. Together, these results suggest that complex matrix composites should be incorporated into tumor models, especially for the drug-resistant TNBC subtype. Impact statement The importance of tumor extracellular matrix (ECM) in disease progression is often inadequately represented in models of breast cancer that rely heavily on collagen I and Matrigel. Through immunohistochemistry analysis of patient breast tumors, we show a wide variation in collagen content based on subtype, specifically a repression of fibril collagens in the receptor negative subtype, irrespective of age and race. We also demonstrated that tumor ECM composition alters cellular elasticity and oncogenic pathway activation demonstrating that physiologically relevant three-dimensional models of breast cancer should include an ECM that is subtype specific.
治疗耐药性的发展是有效治疗方案的重大障碍。在实验室环境中评估肿瘤药物的效果受到缺乏准确再现肿瘤中细胞-微环境相互作用的转化模型的限制。治疗耐药性的获得部分受到肿瘤细胞外基质 (ECM) 的组成的促进,目前主要的模型使用胶原 I (COL I)。在这里,我们试图确定三阴性乳腺癌 (TNBC) 亚型中 COL I 增强表达的普遍性。此外,我们确定治疗反应方法是否因基质组成而异。我们证明胶原含量在患者肿瘤样本中因亚型而异,COL I 表达在通常侵袭性较低的雌激素受体 (ER) 阳性 (ER)/孕激素受体 (PGR) 阳性 (PGR) 癌症中显著增加,而与患者年龄或种族无关。考虑到 COL I 经常参与肿瘤进展,这些发现具有重要意义。我们对 ER 和 ER 阴性 (ER) 细胞系进行了 分析,以确定细胞外基质 (胶原 I、胶原 IV、纤连蛋白和层粘连蛋白) 含量对增殖、细胞表型和存活的影响。当在这些 ECM 底物上培养时,ER 或 ER 细胞均未显示出显著的增殖增加。在这些底物上培养的 ER 细胞对化疗和靶向治疗均敏感。此外,MDA-MB-231 细胞在这些底物上表现出不同的形态、结合亲和力和刚度。我们还证明,ECM 组成会显著改变 ER 和 ER 细胞系中与衰老相关的途径的转录。总之,这些结果表明,复杂的基质复合材料应纳入肿瘤模型,特别是对于耐药性 TNBC 亚型。影响说明肿瘤细胞外基质 (ECM) 在疾病进展中的重要性在严重依赖胶原 I 和 Matrigel 的乳腺癌模型中经常被低估。通过对患者乳腺癌肿瘤的免疫组织化学分析,我们显示出基于亚型的胶原含量广泛变化,具体表现为受体阴性亚型中纤维胶原的抑制,而与年龄和种族无关。我们还证明,肿瘤 ECM 组成会改变细胞弹性和致癌途径激活,这表明乳腺癌的生理相关三维模型应包括特定于亚型的 ECM。
