Literature DB >> 22124930

A microfluidic system for investigation of extravascular transport and cellular uptake of drugs in tumors.

Nelita T Elliott1, Fan Yuan.   

Abstract

Three-dimensional (3D) tumor models have been established in various microfluidic systems for drug delivery and resistance studies in vitro. However, one of the main drawbacks of these models is non-uniform distribution of cells, leaving regions with very low cell density within the 3D structures. As a result, molecular diffusion in the cell compartments is faster than that observed in solid tumors. To solve this problem, we developed a new technique for preparation of 3D tumor models in vitro. It was based on a microfluidic device containing three parallel channels separated by narrowly spaced posts. Tumor cells were loaded into the central channel at high density. To test the system, B16.F10 melanoma cells were perfusion-cultured overnight and the resulting 3D structure was characterized in terms of viability, density, and morphology of cells as well as transport properties of small fluorescent molecules. Immediately upon loading of tumor cells, the cell density was comparable to those observed in B16.F10 tumor tissues in vivo; and the viability of tumor cells was maintained through the overnight culture. The tumor model displayed low extracellular space and high resistance to diffusion of small molecules. For membrane-permeant molecules (e.g., Hoechst 33342), the rate of interstitial penetration was extremely slow, compared to membrane-impermeant molecules (e.g., sodium fluorescein). This versatile tumor model could be applied to in vitro studies of transport and cellular uptake of drugs and genes.
Copyright © 2011 Wiley Periodicals, Inc.

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Year:  2011        PMID: 22124930      PMCID: PMC4163945          DOI: 10.1002/bit.24397

Source DB:  PubMed          Journal:  Biotechnol Bioeng        ISSN: 0006-3592            Impact factor:   4.530


  50 in total

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2.  Role of necrosis in regulating the growth saturation of multicellular spheroids.

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3.  Penetration of anticancer drugs through solid tissue: a factor that limits the effectiveness of chemotherapy for solid tumors.

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4.  Transition to invasion in breast cancer: a microfluidic in vitro model enables examination of spatial and temporal effects.

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5.  Proliferation behavior of E. coli in a three-dimensional in vitro tumor model.

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7.  Available volume fraction of macromolecules in the extravascular space of a fibrosarcoma: implications for drug delivery.

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Journal:  Cancer Res       Date:  1999-08-15       Impact factor: 12.701

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10.  Pgp and MRP activities using calcein-AM are prognostic factors in adult acute myeloid leukemia patients.

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Review 4.  Microfluidics-assisted in vitro drug screening and carrier production.

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6.  Bioreactor-Based Tumor Tissue Engineering.

Authors:  A E Guller; P N Grebenyuk; A B Shekhter; A V Zvyagin; S M Deyev
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7.  Co-Culture of Tumor Spheroids and Fibroblasts in a Collagen Matrix-Incorporated Microfluidic Chip Mimics Reciprocal Activation in Solid Tumor Microenvironment.

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8.  Lung carcinoma spheroids embedded in a microfluidic platform.

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9.  A Microvascularized Tumor-mimetic Platform for Assessing Anti-cancer Drug Efficacy.

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  10 in total

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