http://dbkgroup.org/Papers/davey_kell_micrev96.pdf

Flow cytometry and cell sorting of heterogeneous microbial populations: the importance of single-cell analyses.

Purpose: The purpose of this study was to determine whether hyperthermic exposure would accelerate drug release from thermosensitive sterically stabilized liposomes and enhance their extravasation in tumor tissues. Materials and Methods: In vivo fluorescence video microscopy was used to measure the extravasation of liposomes, as well as release of their contents, in a rat skin flap window chamber containing a vascularized mammary adenocarcinoma under defined thermal conditions (34°, 42°, and 45°C). Images of tissue areas containing multiple blood vessels were recorded via a SIT camera immediately before, and for upto 2 h after i.v. injection of two liposome populations with identical lipid composition: one liposome preparation was surface labeled with Rhodamine-PE (Rh-PE) and the other contained either Doxorubicin (Dox) or calcein at self-quenching concentrations. The light intensity of the entire tissue area was measured at 34°C (the physiological temperature of the skin) for 1 h, and at 42° or 45°C for a second hour. These measurements were then used to calculate the fluorescent light intensity arising from each tracer (liposome surface label and the released contents) inside the vessel and in the interstitial region. Results: The calculated intensity of Rh-PE for the thermosensitive liposomes in the interstitial space (which represents the amout of extravasated liposomes) was low during the first hour, while temperature was maintained at 34°C and increased to 47 times its level before heating, when the tumor was heated at 42° or 45° C for 1 h. The calculated intensity of the liposome contents (Dox) in the interstitial space was negligible at 34°C, and increased by 38- and 76-fold, when the tumor was heated at 42° and 45° C for 1 h, respectively. Similar values were obtained when calcein was encapsulated in liposomes instead of Dox. A similar increase in liposome extravasation was seen with nonthermosensitive liposomes, but negligible release of Dox occurred when the window chamber was heated to 45°C for 1 h. Extravasation of liposomes continued after heating was stopped, but content release stopped after removal of heat. Release of Dox from extravasated liposomes was also seen if heating was applied 24 h after liposome administration, but no further enhancement of liposome extravasation occurred in this case. Conclusions: Our data suggest that hyperthermia can be used to selectively enhance both the delivery and the rate of release of drugs from thermosensitive liposomes to targeted tissues.

Thermosensitive liposomes: extravasation and release of contents in tumor microvascular networks.

Partly PEGylated polyamidoamine dendrimer for tumor-selective targeting of doxorubicin: the effects of PEGylation degree and drug conjugation style.

The removal of the indigo carmine dye from aqueous solutions using cross-linked chitosan: evaluation of adsorption thermodynamics using a full factorial design.

Chromatographic behavior of epirubicin and its analogues on high-purity silica in hydrophilic interaction chromatography.

Solid-phase extraction and optimized separation of doxorubicin, epirubicin and their metabolites using reversed-phase high-performance liquid chromatography.

Optimised separation of E- and Z- isomers of tamoxifen, and its principal metabolites using reversed-phase high performance liquid chromatography.

A high wavelength fluorescent probe, Nile Red, was added to four proteins, viz., bovine albumin, alpha 1-acid glycoprotein, beta-lactoglobulin and ovomucoid. Nile Red showed an enhancement in fluorescence and a shift in emission wavelength, suggesting it was bonding hydrophobically to these proteins. Drug displacement of Nile Red from alpha 1-acid glycoprotein was achieved with both D,L-propranolol and flufenamic acid, showing that the binding site is less electrostatic and more hydrophobic in nature. In order to monitor these interactions, a simple spectrofluorimeter was constructed from solid-state components; the sensitivity of this instrument compared well with that of standard laboratory spectrofluorimeters.

Novel instrumentation and biomedical applications of very near-infrared fluorescence

Methods for liquid chromatographic analysis of tamoxifen, tamoxifen metabolites and their geometric isomers in biological samples

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Solid-phase extraction and optimized separation of doxorubicin, epirubicin and their metabolites using reversed-phase high-performance liquid chromatography.

Optimised separation of E- and Z- isomers of tamoxifen, and its principal metabolites using reversed-phase high performance liquid chromatography.

Novel instrumentation and biomedical applications of very near-infrared fluorescence

Methods for liquid chromatographic analysis of tamoxifen, tamoxifen metabolites and their geometric isomers in biological samples