Literature DB >> 26158500

A microengineered pathophysiological model of early-stage breast cancer.

Yoonseok Choi1, Eunjeh Hyun, Jeongyun Seo, Cassidy Blundell, Hee Chan Kim, Eunhee Lee, Su Hyun Lee, Aree Moon, Woo Kyung Moon, Dongeun Huh.   

Abstract

A mounting body of evidence in cancer research suggests that the local microenvironment of tumor cells has a profound influence on cancer progression and metastasis. In vitro studies on the tumor microenvironment and its pharmacological modulation, however, are often hampered by the technical challenges associated with creating physiological cell culture environments that integrate cancer cells with the key components of their native niche such as neighboring cells and extracellular matrix (ECM) to mimic complex microarchitecture of cancerous tissue. Using early-stage breast cancer as a model disease, here we describe a biomimetic microengineering strategy to reconstitute three-dimensional (3D) structural organization and microenvironment of breast tumors in human cell-based in vitro models. Specifically, we developed a microsystem that enabled co-culture of breast tumor spheroids with human mammary ductal epithelial cells and mammary fibroblasts in a compartmentalized 3D microfluidic device to replicate microarchitecture of breast ductal carcinoma in situ (DCIS). We also explored the potential of this breast cancer-on-a-chip system as a drug screening platform by evaluating the efficacy and toxicity of an anticancer drug (paclitaxel). Our microengineered disease model represents the first critical step towards recapitulating pathophysiological complexity of breast cancer, and may serve as an enabling tool to systematically examine the contribution of the breast cancer microenvironment to the progression of DCIS to an invasive form of the disease.

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Year:  2015        PMID: 26158500      PMCID: PMC4524879          DOI: 10.1039/c5lc00514k

Source DB:  PubMed          Journal:  Lab Chip        ISSN: 1473-0189            Impact factor:   6.799


  22 in total

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2.  Postpartum mammary gland involution drives progression of ductal carcinoma in situ through collagen and COX-2.

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Review 3.  Organs-on-chips at the frontiers of drug discovery.

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Review 4.  Building risk-on-a-chip models to improve breast cancer risk assessment and prevention.

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Journal:  Integr Biol (Camb)       Date:  2013-09       Impact factor: 2.192

5.  Endometase/matrilysin-2 in human breast ductal carcinoma in situ and its inhibition by tissue inhibitors of metalloproteinases-2 and -4: a putative role in the initiation of breast cancer invasion.

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6.  Extracellular matrix heterogeneity regulates three-dimensional morphologies of breast adenocarcinoma cell invasion.

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8.  Silencing of HSulf-2 expression in MCF10DCIS.com cells attenuate ductal carcinoma in situ progression to invasive ductal carcinoma in vivo.

Authors:  Ashwani Khurana; Hiedi McKean; Hyunseok Kim; Sung-Hoon Kim; Jacie mcguire; Lewis R Roberts; Matthew P Goetz; Viji Shridhar
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10.  A multifunctional 3D co-culture system for studies of mammary tissue morphogenesis and stem cell biology.

Authors:  Jonathan J Campbell; Natalia Davidenko; Maria M Caffarel; Ruth E Cameron; Christine J Watson
Journal:  PLoS One       Date:  2011-09-30       Impact factor: 3.240

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  67 in total

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2.  Sacrificial Bioprinting of a Mammary Ductal Carcinoma Model.

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3.  Transitions from mono- to co- to tri-culture uniquely affect gene expression in breast cancer, stromal, and immune compartments.

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Review 4.  Tumour-on-a-chip: microfluidic models of tumour morphology, growth and microenvironment.

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Review 5.  Heralding a new paradigm in 3D tumor modeling.

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6.  Developmentally inspired human 'organs on chips'.

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Journal:  Development       Date:  2018-05-18       Impact factor: 6.868

7.  Native extracellular matrix-derived semipermeable, optically transparent, and inexpensive membrane inserts for microfluidic cell culture.

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Review 8.  Multiorgan Microphysiological Systems for Drug Development: Strategies, Advances, and Challenges.

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Review 10.  Studying Adipose Tissue in the Breast Tumor Microenvironment In Vitro: Progress and Opportunities.

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