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Cho, Moo J.; Scieszka, Jeffrey F.; Cramer, Clay T.; Thompson, David P.; Vidmar, Thomas J.

doi:10.1023/a:1015859921397

Pharmaceutical Research

1989

DOI: 10.1023/a:1015859921397

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Moo J. Cho

Jeffrey F. Scieszka

Clay T. Cramer

et al.

Abstract: Targeted drug delivery to peripheral blood neutrophils (PMNs) should be of therapeutic potential in various disease states. In addition, substances taken up by PMNs in the circulation may be delivered to an extravascular site via the naturally occurring cell infiltration. The present study employs an in vitro chemotaxis model to test whether particulate drug carriers such as liposomes can be transported across a cellular barrier by migrating PMNs. The system contained 10(7) human PMNs/ml, 0.3-micron liposomes … Show more

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Cited by 10 publications

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In vivo behaviour of long‐circulating liposomes in blood vessels in hamster inflammation and septic shock models—use of intravital fluorescence microscopy

Devoisselle¹,

Bégu²,

Tourné-Péteilh³

et al. 2001

Luminescence

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This study aimed to observe liposome uptake by leukocytes in vivo. The study was performed on skin by using a dorsal skin-fold chamber implanted in golden hamsters using intravital microscopy. 5 and 6-CF-encapsulated polyethylene glycolated liposomes were injected intravenously. The skin microcirculation was observed with an intravital Eclipse E800 Nikon microscope (using x40, x80 magnification) fitted with a Xenon light source and an epifluorescence assembly (excitation, 470 nm, FWHM 40 nm; emission, 540 nm, FWHM 40 nm). An ultra-high sensitivity videocamera mounted on the microscope projected the image onto a monitor, and the images (720 x 576 pixels) were recorded for playback analysis with a digital video cassette recorder. An acute inflammatory response was obtained by removing one complete layer of skin and the underlying fascia and avascular tissue on the opposing side of the flap corresponding to an area equivalent to the window aperture. Using this model and set-up, leukocyte rolling and adhesion were easily observed and the entry of PEGylated liposomes into hamster blood leukocytes was studied for a period of 6 h. PEGylated liposomes were clearly identified alone inside the blood flow and inside the leukocytes as soon as the inflammatory reaction appeared. This study shows for the first time that blood leukocytes in their natural milieu of whole blood are capable of interacting with, and taking up, liposomes. This observation is in accordance with previous in vitro studies.

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In vivo behaviour of long‐circulating liposomes in blood vessels in hamster inflammation and septic shock models—use of intravital fluorescence microscopy

Devoisselle¹,

Bégu²,

Tourné-Péteilh³

et al. 2001

Luminescence

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show abstract

Impact of membrane properties on uptake and transcytosis of colloidal nanocarriers across an epithelial cell barrier model

Orthmann

Zeisig

Koklic

et al. 2010

Journal of Pharmaceutical Sciences

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T lymphocytes increase the synthesis of esterified cholesterol in human monocyte-derived macrophages by activation of the scavenger pathway

Kotake

Oikawa

Naito

et al. 1992

Biochimica et Biophysica Acta (BBA) - Molecular Basis of Diseas

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Untitled

Cited by 10 publications

References 10 publications

In vivo behaviour of long‐circulating liposomes in blood vessels in hamster inflammation and septic shock models—use of intravital fluorescence microscopy

In vivo behaviour of long‐circulating liposomes in blood vessels in hamster inflammation and septic shock models—use of intravital fluorescence microscopy

Impact of membrane properties on uptake and transcytosis of colloidal nanocarriers across an epithelial cell barrier model

T lymphocytes increase the synthesis of esterified cholesterol in human monocyte-derived macrophages by activation of the scavenger pathway

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