Immobilized surfactant-nanotube complexes support selectin-mediated capture of viable circulating tumor cells in the absence of capture antibodies

Mitchell, Michael J.; Castellanos, Carlos Alberto Hoyos; King, Michael R.

doi:10.1002/jbm.a.35445

Cited by 26 publications

(18 citation statements)

References 67 publications

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“…Various receptor-ligand bond formations (via a family of selectin adhesion molecules) and hydrodynamic interactions have previously been modeled for leukocytes-endothelium adhesion [26,65,19,23]. Recent experiments in microfluidic devices have also reported either selectin-mediated [40] or platelet-enhanced [37] adhesive capture of tumor cells. Moreover, cell rolling along the endothelium that was observed in in vitro experiments and modeled in silico in the case of leukocytes [3,19,25,38] has also been postulated to work in the case of circulating tumor cells [37,67].…”

Section: Circulating Tumor Cell Adhesion and Rolling On The Endothmentioning

confidence: 99%

Circulating Tumor Cells: When a Solid Tumor Meets a Fluid Microenvironment

Rejniak

2016

Advances in Experimental Medicine and Biology

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Solid tumor dissemination from the primary site to the sites of metastasis involves tumor cell transport through the blood or lymph circulation systems. Once the tumor cells enter the bloodstream, they encounter a new hostile microenvironment. The cells must withstand hemodynamic forces and overcome the effects of fluid shear. The cells are exposed to immunological signaling insults from leukocytes, to collisions with erythrocytes, and to interactions with platelets or macrophages. Finally, the cells need to attach to the blood vessel walls and extravasate to the surrounding stroma to form tumor metastases. Although only a small fraction of invasive cells is able to complete the metastatic process, most cancer-related deaths are the result of tumor metastasis. Thus, investigating the intracellular properties of circulating tumor cells and the extracellular conditions that allow the tumor cells to survive and thrive in this microenvironment is of vital interest. In this chapter, we discuss the intravascular microenvironment that the circulating tumor cells must endure. We summarize the current experimental and computational literature on tumor cells in the circulation system. We also illustrate various aspects of the intravascular transport of circulating tumor cells using a mathematical model based on immersed boundary principles.

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Section: Circulating Tumor Cell Adhesion and Rolling On The Endothmentioning

confidence: 99%

Circulating Tumor Cells: When a Solid Tumor Meets a Fluid Microenvironment

Rejniak

2016

Advances in Experimental Medicine and Biology

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“…Biodegradable particles such as PLGA are particularly advantageous for in vivo administration, where the material can degrade in a safe manner3839. PLGA particles functionalized with an epithelial cell adhesion molecule (EpCAM)-targeting antibody, which binds to EpCAM expressed on tumour cells of epithelial origin40, were bound to the tumour cell surface with minimal effects on cell viability under shear and static conditions (Supplementary Fig. 10a).…”

Section: Resultsmentioning

confidence: 99%

Polymeric mechanical amplifiers of immune cytokine-mediated apoptosis

et al. 2017

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Physical forces affect tumour growth, progression and metastasis. Here, we develop polymeric mechanical amplifiers that exploit in vitro and in vivo physical forces to increase immune cytokine-mediated tumour cell apoptosis. Mechanical amplifiers, consisting of biodegradable polymeric particles tethered to the tumour cell surface via polyethylene glycol linkers, increase the apoptotic effect of an immune cytokine on tumour cells under fluid shear exposure by as much as 50% compared with treatment under static conditions. We show that targeted polymeric particles delivered to tumour cells in vivo amplify the apoptotic effect of a subsequent treatment of immune cytokine, reduce circulating tumour cells in blood and overall tumour cell burden by over 90% and reduce solid tumour growth in combination with the antioxidant resveratrol. The work introduces a potentially new application for a broad range of micro- and nanoparticles to maximize receptor-mediated signalling and function in the presence of physical forces.

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“…3B) is a microfluidic technology that uses magnetic affinity-based CTC isolation. 82,155 Blood is first incubated in a static, diffusion-limited environment with Ab-coated magnetic microbeads. The, the iChip uses several concepts to isolate CTCs: 107 (i) the blood is “debulked” by deterministic lateral displacement, 109 a hydrodynamic technique that depletes cells smaller than 8 μm (monocytes, lymphocytes, RBCs, and platelets) and cells larger than 30 μm; 50,107 (ii) the remaining cells are aligned into a single line by inertial focusing; 107,110 and (iii) a magnetic field is applied to separate labelled cells from non-labelled cells.…”

Section: Magnetic Affinity-selection – From Cellsearch™ To Microflmentioning

confidence: 99%

“…Electrostatic or hydrophobic interactions selectively bind cancer cells versus neutrophils and were suggested to be associated with an extracellular matrix specific to cancer cells. 155 In another example, the halloysite nanotubes were coated with liposomes containing doxorubicin, which were functionalized with E-selectin to cause liposomal-CTC binding and selective chemotherapy delivery to the CTCs. 156 …”

Section: Microfluidic-based Biological Ctc Selectionmentioning

confidence: 99%

Materials and microfluidics: enabling the efficient isolation and analysis of circulating tumour cells

et al. 2017

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We present a critical review of microfluidic technologies and material effects on the analyses of circulating tumour cells (CTCs) selected from the peripheral blood of cancer patients. CTCs are a minimally invasive source of clinical information that can be used to prognose patient outcome, monitor minimal residual disease, assess tumour resistance to therapeutic agents, and potentially screen individuals for the early diagnosis of cancer. The performance of CTC isolation technologies depends on microfluidic architectures, the underyling principles of isolation, and the choice of materials. In this review, we present a critical review of the fundamental principles used in these technologies and discuss their performance. We also give context to how CTC isolation technologies enable downstream analysis of selected CTCs in terms of detecting genetic mutations and gene expression that could be used to gain information that may affect patient outcome.

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Immobilized surfactant-nanotube complexes support selectin-mediated capture of viable circulating tumor cells in the absence of capture antibodies

Cited by 26 publications

References 67 publications

Circulating Tumor Cells: When a Solid Tumor Meets a Fluid Microenvironment

Circulating Tumor Cells: When a Solid Tumor Meets a Fluid Microenvironment

Polymeric mechanical amplifiers of immune cytokine-mediated apoptosis

Materials and microfluidics: enabling the efficient isolation and analysis of circulating tumour cells

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