Non-glycosylated IGF2 prohormones are more mitogenic than native IGF2

Author:

Potalitsyn PavloORCID,Mrázková Lucie,Selicharová Irena,Tencerová MichaelaORCID,Ferenčáková Michaela,Chrudinová Martina,Turnovská Tereza,Brzozowski Andrzej MarekORCID,Marek Aleš,Kaminský Jakub,Jiráček JiříORCID,Žáková LenkaORCID

Abstract

AbstractInsulin-like Growth Factor-2 (IGF2) is important for the regulation of human embryonic growth and development, and for adults’ physiology. Incorrect processing of the IGF2 precursor, pro-IGF2(156), leads to the formation of two IGF2 proforms, big-IGF2(87) and big-IGF2(104). Unprocessed and mainly non-glycosylated IGF2 proforms are found at abnormally high levels in certain diseases, but their mode of action is still unclear. Here, we found that pro-IGF2(156) has the lowest ability to form its inactivating complexes with IGF-Binding Proteins and has higher proliferative properties in cells than IGF2 and other IGF prohormones. We also showed that big-IGF2(104) has a seven-fold higher binding affinity for the IGF2 receptor than IGF2, and that pro-IGF2(87) binds and activates specific receptors and stimulates cell growth similarly to the mature IGF2. The properties of these pro-IGF2 forms, especially of pro-IGF2(156) and big-IGF2(104), indicate them as hormones that may be associated with human diseases related to the accumulation of IGF-2 proforms in the circulation.

Funder

Grantová Agentura České Republiky

RCUK | Biotechnology and Biological Sciences Research Council

RCUK | Medical Research Council

Publisher

Springer Science and Business Media LLC

Subject

General Agricultural and Biological Sciences,General Biochemistry, Genetics and Molecular Biology,Medicine (miscellaneous)

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