Direct Measurements on CD24-Mediated Rolling of Human Breast Cancer MCF-7 Cells on E-Selectin

Myung, Ja Hye; Gajjar, Khyati A.; Pearson, Ryan M.; Launiere, Cari; Eddington, David T.; Hong, Seungpyo

doi:10.1021/ac102901e

Cited by 54 publications

(59 citation statements)

References 52 publications

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“…Here, the effect of immobilized surfactant-nanotube complexes on ES-mediated adhesion of tumor cells under flow was assessed. Sialylated carbohydrate ligands are expressed on the surface of many tumor cell types, which can induce rolling tumor cell adhesion on ES (47),(48) . We initially studied COLO 205 colon cancer cell and MCF7 breast cancer cell adhesion to ES on immobilized surfactant-nanotube surfaces, given that they have been shown to interact with ES under physiologically-relevant shear stresses (47),(49),(50) .…”

Section: Resultsmentioning

confidence: 99%

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

Mitchell

Castellanos

King

2015

J. Biomed. Mater. Res.

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The metastatic spread of tumor cells from the primary site to anatomically distant organs leads to a poor patient prognosis. Increasing evidence has linked adhesive interactions between circulating tumor cells (CTCs) and endothelial cells to metastatic dissemination. Microscale biomimetic flow devices hold promise as a diagnostic tool to isolate CTCs and develop metastatic therapies, utilizing E-selectin (ES) to trigger the initial rolling adhesion of tumor cells under flow. To trigger firm adhesion and capture under flow, such devices also typically require antibodies against biomarkers thought to be expressed on CTCs. This approach is challenged by the fact that CTCs are now known to exhibit heterogeneous expression of conventional biomarkers. Here, we describe surfactant-nanotube complexes to enhance ES-mediated capture and isolation of tumor cells without the use of capture antibodies. While the majority of tumor cells exhibited weaker rolling adhesion on halloysite nanotubes (HNT) coated with ES, HNT functionalization with the sodium dodecanoate (NaL) surfactant induced a switch to firm cellular adhesion under flow. Conversely, surfactant-nanotube complexes significantly reduced the number of primary human leukocytes captured via ES-mediated adhesion under flow. The switch in tumor cell adhesion was exploited to capture and isolate tumor cells in the absence of EpCAM antibodies, commonly utilized as the gold standard for CTC isolation. Additionally, HNT-NaL complexes were shown to capture tumor cells with low to negligible EpCAM expression, that are not efficiently captured using conventional approaches.

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Section: Resultsmentioning

confidence: 99%

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

Mitchell

Castellanos

King

2015

J. Biomed. Mater. Res.

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“…Using the parallel flow chamber assay, they confirmed the physiological role of CD24 as a ligand for P-selectin on KS cells in the presence of shear stress. 2 Later, Myung et al 115 reported the role of CD24 on MCF7 breast cancer cells as a ligand for E-selectin under flow by measuring the binding kinetics of CD24 with E-selectin with surface plasmon resonance (SPR). The identification of CD24 as a ligand for both P-and E-selectin may provide better understanding of the adhesion and invasion mechanisms of metastatic breast cancer.…”

Section: Metastatic Cascade: Adhesive Recruitment Of Cancer Cells Viamentioning

confidence: 99%

Glycomechanics of the Metastatic Cascade: Tumor Cell–Endothelial Cell Interactions in the Circulation

2011

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Hydrodynamic shear force plays an important role in the leukocyte adhesion cascade that involves the tethering and rolling of cells along the endothelial layer, their firm adhesion or arrest, and their extravasation or escape from the circulatory system by inducing passive deformation, or cell flattening, and microvilli stretching, as well as regulating the expression, distribution, and conformation of adhesion molecules on leukocytes and the endothelial layer. Similarly, the dissemination of circulating tumor cells (CTCs) from the primary tumor sites is believed to involve tethering, rolling, and firm adhesion steps before their eventual extravasation which leads to secondary tumor sites (metastasis). Of particular importance to both the leukocyte adhesion cascade and the extravasation of CTCs, glycoproteins are involved in all three steps (capture, rolling, and firm adhesion) and consist of a variety of important selectin ligands. This review article provides an overview of glycoprotein glycosylation associated with the abnormal glycan expression on cancer cell surfaces, where well-established and novel selectin ligands that are cancer related are discussed. An overview of computational approaches on the effects of fluid mechanical force on glycoprotein mediated cancer cell rolling and adhesion is presented with a highlight of recent flow-based and selectin-mediated cell capturing/enriching devices. Finally, as an important branch of the glycoprotein family, mucins, specifically MUC1, are discussed in the context of their aberrant expression on cancer cells and their role as cancer cell adhesion molecules. Since metastasis relies heavily on glycoprotein interactions in the bloodstream where the fluid shear stress highly regulates cell adhesion forces, it is important to study and understand the glycomechanics of all relevant glycoproteins (well-established and novel) as they relate to the metastatic cascade.

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“…CD133 function is not clear but its presence on early and undifferentiated cells is suggestive of a growth factor receptor, and the presence of five tyrosine residues on the 50-aa cytoplasmic tail may indicate that the protein is phosphorylated in response to ligand binding and triggers a signal transduction [11]. CD24 is a sialoglycoprotein expressed on mature granulocytes [12], B and T lymphocyte subsets [13,14], normal and cancer stem cells [15,16]. The protein is anchored via a glycosyl phosphatidylinositol to cell surface.…”

Section: Discussionmentioning

confidence: 99%

CD133 and CD24 expression in renal tissue of patients affected by autosomal dominant polcystic kidney disease

Lodi¹,

Ligabue²,

Fabrizio³

et al. 2013

SCD

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Direct Measurements on CD24-Mediated Rolling of Human Breast Cancer MCF-7 Cells on E-Selectin

Cited by 54 publications

References 52 publications

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

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

Glycomechanics of the Metastatic Cascade: Tumor Cell–Endothelial Cell Interactions in the Circulation

CD133 and CD24 expression in renal tissue of patients affected by autosomal dominant polcystic kidney disease

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