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PMID:22084075

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Citation

Means, CK, Lygren, B, Langeberg, LK, Jain, A, Dixon, RE, Vega, AL, Gold, MG, Petrosyan, S, Taylor, SS, Murphy, AN, Ha, T, Santana, LF, Tasken, K and Scott, JD (2011) An entirely specific type I A-kinase anchoring protein that can sequester two molecules of protein kinase A at mitochondria. Proc. Natl. Acad. Sci. U.S.A. 108:E1227-35

Abstract

A-kinase anchoring proteins (AKAPs) tether the cAMP-dependent protein kinase (PKA) to intracellular sites where they preferentially phosphorylate target substrates. Most AKAPs exhibit nanomolar affinity for the regulatory (RII) subunit of the type II PKA holoenzyme, whereas dual-specificity anchoring proteins also bind the type I (RI) regulatory subunit of PKA with 10-100-fold lower affinity. A range of cellular, biochemical, biophysical, and genetic approaches comprehensively establish that sphingosine kinase interacting protein (SKIP) is a truly type I-specific AKAP. Mapping studies located anchoring sites between residues 925-949 and 1,140-1,175 of SKIP that bind RI with dissociation constants of 73 and 774 nM, respectively. Molecular modeling and site-directed mutagenesis approaches identify Phe 929 and Tyr 1,151 as RI-selective binding determinants in each anchoring site. SKIP complexes exist in different states of RI-occupancy as single-molecule pull-down photobleaching experiments show that 41 ± 10% of SKIP sequesters two YFP-RI dimers, whereas 59 ± 10% of the anchoring protein binds a single YFP-RI dimer. Imaging, proteomic analysis, and subcellular fractionation experiments reveal that SKIP is enriched at the inner mitochondrial membrane where it associates with a prominent PKA substrate, the coiled-coil helix protein ChChd3.

Links

PubMed PMC3228425 Online version:10.1073/pnas.1107182108

Keywords

A Kinase Anchor Proteins/genetics; A Kinase Anchor Proteins/metabolism; Adaptor Proteins, Signal Transducing/genetics; Adaptor Proteins, Signal Transducing/metabolism; Analysis of Variance; Animals; Blotting, Western; Cell Line; Cloning, Molecular; Cyclic AMP-Dependent Protein Kinases/metabolism; Humans; Immunoprecipitation; Mass Spectrometry; Mice; Mitochondria/metabolism; Mitochondrial Proteins/metabolism; Models, Molecular; Mutagenesis, Site-Directed; Protein Binding/genetics; Protein Conformation; Surface Plasmon Resonance; Transfection

Significance

Annotations

Gene product Qualifier GO Term Evidence Code with/from Aspect Extension Notes Status

MOUSE:PACR

enables

GO:0005515: protein binding

ECO:0000353: physical interaction evidence used in manual assertion

PR:Q6NSW3

F

Seeded From UniProt

complete

MOUSE:SPKAP

located_in

GO:0030018: Z disc

ECO:0000314: direct assay evidence used in manual assertion

C

  • part_of:(CL:0000746)

Seeded From UniProt

complete

MOUSE:SPKAP

located_in

GO:0005739: mitochondrion

ECO:0000314: direct assay evidence used in manual assertion

C

  • part_of:(CL:0000746)

Seeded From UniProt

complete

MOUSE:SPKAP

enables

GO:0051018: protein kinase A binding

ECO:0000353: physical interaction evidence used in manual assertion

PR:P70205

F

  • occurs_in:(CL:0000057)

Seeded From UniProt

complete


See also

References

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