Development of a novel DDS for site-specific PEGylated proteins

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作者
Yasuo Yoshioka
Shin-ichi Tsunoda
Yasuo Tsutsumi
机构
[1] Osaka University,Department of Toxicology and Safety Science, Graduate School of Pharmaceutical Sciences
[2] Osaka University,The Center for Advanced Medical Engineering and Informatics
[3] National Institute of Biomedical Innovation,Laboratory of Biopharmaceutical Research
[4] Osaka University,Department of Biomedical Innovation, Graduate school of Pharmaceutical Sciences
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关键词
Lysine Residue; Maleic Anhydride; Polymer Carrier; Polymeric Modifier; Bioactive Protein;
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摘要
Because of the shifted focus in life science research from genome analyses to genetic and protein function analyses, we now know functions of numerous proteins. These analyses, including those of newly identified proteins, are expected to contribute to the identification of proteins of therapeutic value in various diseases. Consequently, pharmacoproteomic-based drug discovery and development of protein therapies attracted a great deal of attention in recent years. Clinical applications of most of these proteins are, however, limited because of their unexpectedly low therapeutic effects, resulting from the proteolytic degradation in vivo followed by rapid removal from the circulatory system. Therefore, frequent administration of excessively high dose of a protein is required to observe its therapeutic effect in vivo. This often results in impaired homeostasis in vivo and leads to severe adverse effects. To overcome these problems, we have devised a method for chemical modification of proteins with polyethylene glycol (PEGylation) and other water-soluble polymers. In addition, we have established a method for creating functional mutant proteins (muteins) with desired properties, and developed a site-specific polymer-conjugation method to further improve their therapeutic potency. In this review, we are introducing our original protein-drug innovation system mentioned above.
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