Fc fusion to Glucagon-like peptide-1 inhibits degradation by human DPP-IV, increasing its half-life in serum and inducing a potent activity for human GLP-1 receptor activation
The short in vivo half-life of GLP-1 prevents it from being used clinically. This short half-life occurs because GLP-1 is rapidly degraded by dipeptidyl peptidases such as DPP-IV. To overcome this obstacle, a GLP-1/Fc was constructed and evaluated to determine if it was degraded by DPP-IV and in serum. When the degradation of GLP-1/Fc by human DPP-IV and rabbit serum was compared with that of GLP-1 it was found to be reduced by approximately 5- and 4-fold, respectively. Furthermore, GLP-1/Fc showed a potent activity for human GLP-1 receptor activation (EC(50) approximately 6 nM). Taken together, these results indicate that GLP-1/Fc may have an extended half-life in vivo that occurs as a result of inhibition of degradation by human DPP-IV. Due to the extended half life, GLP-1/Fc may be useful for clinical treatments. [BMB reports 2009; 42(4): 212-216]
- Issue Date
- 2009
- Language
- English
- Article Type
- Article
- Keywords
PROTEIN-KINASE-B; BETA-CELLS; INDUCED APOPTOSIS; GROWTH-FACTOR; DB/DB MICE; EXPRESSION; PROLIFERATION; INS-1
- Citation
BMB REPORTS, v.42, no.4, pp.212 - 216
- ISSN
- 1976-6696
- Appears in Collection
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