| Literature DB >> 23546513 |
Eung-Sam Kim1, Do Soo Jang, Seung Yun Yang, Mi Nam Lee, Kyeong Sik Jin, Hyung Jin Cha, Jin Kon Kim, Young Chul Sung, Kwan Yong Choi.
Abstract
Nanotechnology has been applied to the development of more effective and compatible drug delivery systems for therapeutic proteins. Human growth hormone (hGH) was fused with a hybrid Fc fragment containing partial Fc domains of human IgD and IgG4 to produce a long-acting fusion protein. The fusion protein, hGH-hyFc, resulted in the increase of the hydrodynamic diameter (ca. 11 nm) compared with the diameter (ca. 5 nm) of the recombinant hGH. A diblock copolymer membrane with nanopores (average diameter of 14.3 nm) exhibited a constant release rate of hGH-hyFc. The hGH-hyFc protein released in a controlled manner for one month was found to trigger the phosphorylation of Janus kinase 2 (JAK2) in human B lymphocyte and to exhibit an almost identical circular dichroism spectrum to that of the original hGH-hyFc, suggesting that the released fusion protein should maintain the functional and structural integrity of hGH. Thus, the nanoporous release device could be a potential delivery system for the long-term controlled release of therapeutic proteins fused with the hybrid Fc fragment.Entities:
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Year: 2013 PMID: 23546513 DOI: 10.1039/c3nr00474k
Source DB: PubMed Journal: Nanoscale ISSN: 2040-3364 Impact factor: 7.790