N-terminal site-specific mono-PEGylation of epidermal growth factor

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Purpose. N-terminal site-specific mono-PEGylation of recombinant human epidermal growth factor (EGF) was accomplished using polyethyleneglycol ( PEG) derivatives (Mw = 2000 and 5000) through a reactive terminal aldehyde group. Methods. The site-specific PEG conjugation was conducted at a slightly acidic pH condition (pH 5.5). The mono-PEGylation was targeted to an alpha-amine group at the N-terminal end of EGF to minimize reduction of biologic activity. Tryptic digestion mapping and MALDI-TOF MS techniques were applied to show the occurrence of mono-PEGylation at the N-terminus of EGF. Results. The site-specific mono-PEGylated EGF, when compared with native EGF, fully retained its in vitro biologic activities such as cell proliferation and intracellular signal transduction. This revealed that although a synthetic polymer of a PEG was covalently conjugated to EGF, the internalized complex of PEGylated EGF-receptor within cells did not hamper the intracellular signal transduction events. The PEGylated EGF also exhibited a prolonged circulation in blood stream in vivo and markedly enhanced physical stability when incubated with tissue homogenate. Conclusion. N-terminally mono-PEGylated EGF shows increased physical stability while retaining its biologic activity.
Publisher
KLUWER ACADEMIC/PLENUM PUBL
Issue Date
2003-05
Language
English
Article Type
Article
Keywords

RECEPTOR TYROSINE KINASES; POLYETHYLENE-GLYCOL; DIRECTED MUTAGENESIS; CELLS; ENDOCYTOSIS; EGF; IMMUNOGENICITY; MICROSPHERES; CONJUGATION; STABILITY

Citation

PHARMACEUTICAL RESEARCH, v.20, no.5, pp.818 - 825

ISSN
0724-8741
DOI
10.1023/A:1023402123119
URI
http://hdl.handle.net/10203/13146
Appears in Collection
CH-Journal Papers(저널논문)BS-Journal Papers(저널논문)
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