Chemotherapeutics and CAR-T Cell-Based Immunotherapeutics Screening on a 3D Bioprinted Vascularized Breast Tumor Model

被引:26
|
作者
Dey, Madhuri [1 ,2 ]
Kim, Myoung Hwan [2 ,3 ]
Dogan, Mikail [4 ]
Nagamine, Momoka [1 ,2 ]
Kozhaya, Lina [4 ]
Celik, Nazmiye [2 ,5 ]
Unutmaz, Derya [4 ,6 ]
Ozbolat, Ibrahim T. [2 ,3 ,5 ,7 ,8 ,9 ,10 ]
机构
[1] Penn State Univ, Dept Chem, University Pk, PA 16802 USA
[2] Penn State Univ, Huck Inst Life Sci, University Pk, PA 16802 USA
[3] Penn State Univ, Biomed Engn Dept, University Pk, PA 16802 USA
[4] Jackson Lab Genom Med, Farmington, CT 06032 USA
[5] Penn State Univ, Engn Sci & Mech Dept, University Pk, PA 16802 USA
[6] Univ Connecticut, Hlth Ctr, Farmington, CT 06032 USA
[7] Penn State Univ, Mat Res Inst, University Pk, PA 16802 USA
[8] Penn State Univ, Canc Inst, Hershey, PA 17033 USA
[9] Penn State Univ, Neurosurg Dept, Hershey, PA 17033 USA
[10] Cukurova Univ, Dept Med Oncol, TR-01330 Adana, Turkey
关键词
bioprinting; cancer; CAR-T immunotherapy; tumor models; CANCER; INTERLEUKIN-6;
D O I
10.1002/adfm.202203966
中图分类号
O6 [化学];
学科分类号
0703 ;
摘要
Despite substantial advancements in development of cancer treatments, lack of standardized and physiologically-relevant in vitro testing platforms limit the early screening of anticancer agents. A major barrier is the complex interplay between the tumor microenvironment and immune response. To tackle this, a dynamic-flow based 3D bioprinted multi-scale vascularized breast tumor model, responding to chemo and immunotherapeutics is developed. Heterotypic tumors are precisely bioprinted at pre-defined distances from a perfused vasculature, exhibit tumor angiogenesis and cancer cell invasion into the perfused vasculature. Bioprinted tumors treated with varying dosages of doxorubicin for 72 h portray a dose-dependent drug response behavior. More importantly, a cell based immune therapy approach is explored by perfusing HER2-targeting chimeric antigen receptor (CAR) modified CD8(+) T cells for 24 or 72 h. Extensive CAR-T cell recruitment to the endothelium, substantial T cell activation and infiltration to the tumor site, resulted in up to approximate to 70% reduction in tumor volumes. The presented platform paves the way for a robust, precisely fabricated, and physiologically-relevant tumor model for future translation of anti-cancer therapies to personalized medicine.
引用
收藏
页数:15
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