Separation of fast from slow anabolism by site-specific PEGylation of insulin-like growth factor I (IGF-I).

نویسندگان

  • Friedrich Metzger
  • Waseem Sajid
  • Stefanie Saenger
  • Christian Staudenmaier
  • Chris van der Poel
  • Bettina Sobottka
  • Angelika Schuler
  • Mandy Sawitzky
  • Raphael Poirier
  • Dietrich Tuerck
  • Eginhard Schick
  • Andreas Schaubmar
  • Friederike Hesse
  • Kurt Amrein
  • Hansruedi Loetscher
  • Gordon S Lynch
  • Andreas Hoeflich
  • Pierre De Meyts
  • Hans-Joachim Schoenfeld
چکیده

Insulin-like growth factor I (IGF-I) has important anabolic and homeostatic functions in tissues like skeletal muscle, and a decline in circulating levels is linked with catabolic conditions. Whereas IGF-I therapies for musculoskeletal disorders have been postulated, dosing issues and disruptions of the homeostasis have so far precluded clinical application. We have developed a novel IGF-I variant by site-specific addition of polyethylene glycol (PEG) to lysine 68 (PEG-IGF-I). In vitro, this modification decreased the affinity for the IGF-I and insulin receptors, presumably through decreased association rates, and slowed down the association to IGF-I-binding proteins, selectively limiting fast but maintaining sustained anabolic activity. Desirable in vivo effects of PEG-IGF-I included increased half-life and recruitment of IGF-binding proteins, thereby reducing risk of hypoglycemia. PEG-IGF-I was equipotent to IGF-I in ameliorating contraction-induced muscle injury in vivo without affecting muscle metabolism as IGF-I did. The data provide an important step in understanding the differences of IGF-I and insulin receptor contribution to the in vivo activity of IGF-I. In addition, PEG-IGF-I presents an innovative concept for IGF-I therapy in diseases with indicated muscle dysfunction.

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عنوان ژورنال:
  • The Journal of biological chemistry

دوره 286 22  شماره 

صفحات  -

تاریخ انتشار 2011