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Topological control of cytokine receptor signaling induces differential effects in hematopoiesis.


ABSTRACT: Although tunable signaling by G protein-coupled receptors can be exploited through medicinal chemistry, a comparable pharmacological approach has been lacking for the modulation of signaling through dimeric receptors, such as those for cytokines. We present a strategy to modulate cytokine receptor signaling output by use of a series of designed C2-symmetric cytokine mimetics, based on the designed ankyrin repeat protein (DARPin) scaffold, that can systematically control erythropoietin receptor (EpoR) dimerization orientation and distance between monomers. We sampled a range of EpoR geometries by varying intermonomer angle and distance, corroborated by several ligand-EpoR complex crystal structures. Across the range, we observed full, partial, and biased agonism as well as stage-selective effects on hematopoiesis. This surrogate ligand strategy opens access to pharmacological modulation of therapeutically important cytokine and growth factor receptor systems.

SUBMITTER: Mohan K 

PROVIDER: S-EPMC7274355 | biostudies-literature | 2019 May

REPOSITORIES: biostudies-literature

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Topological control of cytokine receptor signaling induces differential effects in hematopoiesis.

Mohan Kritika K   Ueda George G   Kim Ah Ram AR   Jude Kevin M KM   Fallas Jorge A JA   Guo Yu Y   Hafer Maximillian M   Miao Yi Y   Saxton Robert A RA   Saxton Robert A RA   Piehler Jacob J   Sankaran Vijay G VG   Baker David D   Garcia K Christopher KC  

Science (New York, N.Y.) 20190523 6442


Although tunable signaling by G protein-coupled receptors can be exploited through medicinal chemistry, a comparable pharmacological approach has been lacking for the modulation of signaling through dimeric receptors, such as those for cytokines. We present a strategy to modulate cytokine receptor signaling output by use of a series of designed C2-symmetric cytokine mimetics, based on the designed ankyrin repeat protein (DARPin) scaffold, that can systematically control erythropoietin receptor (  ...[more]

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