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C Delgado

Researcher at Royal Free Hospital

Publications -  11
Citations -  1535

C Delgado is an academic researcher from Royal Free Hospital. The author has contributed to research in topics: PEG ratio & Polyethylene glycol. The author has an hindex of 8, co-authored 11 publications receiving 1516 citations.

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Journal Article

The uses and properties of PEG-linked proteins.

TL;DR: PEG-modified cytokines have been constructed and one of the conjugates, PEG- modified granulocyte-macrophage colony-stimulating factor, showed dissociation of two biological properties, which may open new horizons to the application of PEGylation technology.
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Influence of surface hydrophilicity of liposomes on their interaction with plasma protein and clearance from the circulation: studies with poly(ethylene glycol)-coated vesicles.

TL;DR: Preformed liposomes which quantitatively retain aqueous markers were covalenty coupled via dipalmitoylphosphatidyl-ethanolamine, to the hydrophilic polymer, monomethoxypoly(ethylene glycol) (MPEG 5000), and it is suggested that the polymer acts as a surface barrier to plasma factors which otherwise bind to liposome in the blood and accelerate vesicle removal.
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Polyethylene Glycol Modification: Relevance of Improved Methodology to Tumour Targeting

TL;DR: Studies investigating the underlying principles of tumour targeting suggest that current views concerning the optimisation of PEGylated vehicles for tumour localisation need to be re-examined.
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Enhanced tumour specificity of an anti-carcinoembrionic antigen Fab' fragment by poly(ethylene glycol) (PEG) modification.

TL;DR: PEG-F9 emerges as a new generation antibody with potential advantages for both radioimmunotherapy and tumour imaging, since there was a reduction in antigen binding and optimisation of PEGylation might further improve tumour specificity.
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Analytical partitioning of poly(ethylene glycol)-modified proteins.

TL;DR: Although somewhat simplistic, 'weight fraction' based analysis of partition data appears robust enough to accommodate laboratory to laboratory variation in protein, polymer and phase system type and facilitates comparisons between partition data involving disparate polymer-protein conjugates.