Abstract

Cancers are among the leading causes of death around the world with an estimated mortality of close to 10 million in 2015, among which a total of 1,658,370 new cancer cases and 589,430 cancer deaths are projected to occur in the US alone. Particularly, breast cancer is one of the prevailing cancers among the Americans: about 1 in 8 (12%) women in the US is likely to develop invasive breast cancer during their lifetime. In 2015, estimated new cases of invasive breast cancer of 231,480 (80% invasive ductal carcinomas [IDCs]) and carcinoma in situ of 60,290 (>85% ductal carcinoma in situ [DCIS]) will be diagnosed in US women, leading to a death toll of about 40,290. Although tremendous improvements in breast cancer survival have been achieved, current drug administration procedures relying on chemotherapy followed by radiographic scans often lead to disparity in cancer care, which is largely caused by the variance in drug responses arose from intratumor heterogeneity. For example, when a presumably effective drug is administered, it requires lengthy follow-ups before the ineffectiveness of the drug and progression of the disease can be revealed. The patient will then receive an alternative drug for treatment, leading to i) accumulated systemic toxicity towards healthy organs; ii) impaired time responsiveness to the cancer which may have further progressed, rendering treatment more difficult; and iii) high cost of the treatment plan. The goal of this proposal is to tackle the aforementioned challenges by engineering and validating a multi- component ductal-carcinoma-on-a-chip platform, which recapitulates the biology and physiology of the tumor in vivo through i) construction of 3D vascularized stroma embedding perfusable, interconnected microvessels; ii) introduction of basement membrane-coated duct-like structures via bioprinting; iii) induction of progression, invasion, and angiogenesis of ductal carcinoma on the chip that recapitulates such processes in vivo; iv) establishment of a sensor-integrated platform for anti-cancer drug screening; and v) extension to a tumor-and- multi-organ-on-a-chip platform for proof-of-concept investigation of systemic drug effect. The efficacy of this platform will be validated in animal (mouse) patients. This innovative platform is expected to be clinically transformative in the future in building personalized chips through application of patient-derived cells.

Public Health Relevance

While breast cancer is one of the prevailing cancers among the Americans, a significant portion of the patients with breast cancers is diagnosed as ductal carcinomas. The drug administration process for breast cancer patients is time-consuming and often inefficient, largely due to intratumor heterogeneity and systemic side effects, which often lead to differential responses towards anti-cancer drugs. In order to tackle this issue, a microfluidic platform will be engineered to recapitulate the microenvironment of ductal carcinoma and its progression, invasion, and angiogenesis. Biosensors will be integrated to probe its responses to various anti- cancer drugs. Such platform, when fabricated using patients' own biopsied tumor cells and combined with a multi-organ platform, will ultimately enable personalized screening of anti-cancer drugs for individual patients.

  Funding Agency

Agency
National Institute of Health (NIH)
Institute
National Cancer Institute (NCI)
Type
Career Transition Award (K99)
Project #
5K99CA201603-02
Application #
9274241
Study Section
Subcommittee I - Transistion to Independence (NCI)
Program Officer
Radaev, Sergey
Project Start
2016-05-16
Project End
2018-04-30
Budget Start
2017-05-01
Budget End
2018-04-30
Support Year
2
Fiscal Year
2017
Total Cost
Indirect Cost

  Institution

Name
Brigham and Women's Hospital
Department
Type
DUNS #
030811269
City
Boston
State
MA
Country
United States
Zip Code
02115

  Publications

Miri, Amir K; Hosseinabadi, Hossein Goodarzi; Cecen, Berivan et al. (2018) Permeability mapping of gelatin methacryloyl hydrogels. Acta Biomater 77:38-47
Zhang, Yu Shrike; Oklu, Rahmi; Dokmeci, Mehmet Remzi et al. (2018) Three-Dimensional Bioprinting Strategies for Tissue Engineering. Cold Spring Harb Perspect Med 8:
Miri, Amir K; Nieto, Daniel; Iglesias, Luis et al. (2018) Microfluidics-Enabled Multimaterial Maskless Stereolithographic Bioprinting. Adv Mater 30:e1800242
Liu, Wanjun; Zhong, Zhe; Hu, Ning et al. (2018) Coaxial extrusion bioprinting of 3D microfibrous constructs with cell-favorable gelatin methacryloyl microenvironments. Biofabrication 10:024102
Lobo, Anderson Oliveira; Afewerki, Samson; de Paula, Mirian Michele Machado et al. (2018) Electrospun nanofiber blend with improved mechanical and biological performance. Int J Nanomedicine 13:7891-7903
Rocca, Marco; Fragasso, Alessio; Liu, Wanjun et al. (2018) Embedded Multimaterial Extrusion Bioprinting. SLAS Technol 23:154-163
Shin, Su Ryon; Migliori, Bianca; Miccoli, Beatrice et al. (2018) Electrically Driven Microengineered Bioinspired Soft Robots. Adv Mater 30:
Rosellini, Elisabetta; Zhang, Yu Shrike; Migliori, Bianca et al. (2018) Protein/polysaccharide-based scaffolds mimicking native extracellular matrix for cardiac tissue engineering applications. J Biomed Mater Res A 106:769-781
Zhang, Yu Shrike; Yao, Junjie (2018) Imaging Biomaterial-Tissue Interactions. Trends Biotechnol 36:403-414
Zhang, Yu Shrike; Pi, Qingmeng; van Genderen, Anne Metje (2017) Microfluidic Bioprinting for Engineering Vascularized Tissues and Organoids. J Vis Exp :

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