Journal article

Ro 31-6045, the inactive analogue of the protein kinase C inhibitor Ro 31-8220, blocks in vivo activation of p70(s6k)/p85(s6k): implications for the analysis of S6K signalling

N Marmy-Conus, KM Hannan, RB Pearson

FEBS LETTERS | ELSEVIER SCIENCE BV | Published : 2002

DOI: 10.1016/S0014-5793(02)02738-2

Abstract

The mitogen-stimulated protein kinase p70(s6k)/p85(s6k) (S6K) plays an essential role in cell proliferation and growth, with inhibitors of the S6K signalling pathway showing promise as anti-tumour therapeutics. Here, we report that the bisindolylmaleimide derivative Ro 31-6045, previously reported to be inactive as a kinase inhibitor, inhibited S6K activity in vivo with an IC50=8 microM. Structure/function analysis using mutant forms of S6K indicates that Ro 31-6045 inhibition is independent of the upstream activator mTOR. Ro 31-6045 will prove useful in elucidating the complex activation mechanism of S6K and its independence from mTOR will allow confirmation of functional data obtained usin..

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Keywords

Rapamycin
Protein Kinase C
Protein-Serine-Threonine Kinases
Signal Transduction
Biochemistry & Molecular Biology
P70(s6k)
Translation
Fibroblasts
Purification
Animals
Indoles
Sirolimus
Maleimides
Mtor
Mice, Inbred Balb C
Proto-Oncogene Proteins
Science & Technology
Ro 31-6045
Proto-Oncogene Proteins C-Akt
Enzyme Activation
Cell Biology
Messenger-Rna
Bisindolylmaleimide
Structure-Activity Relationship
Mice
Sulfonamides
Mutagenesis, Site-Directed
Protein Kinases
Kidney
Biophysics
Ribosomal Protein S6 Kinases
P70(s6k)/p85(s6k)
Requirement
Protein Kinase Inhibitor
Cell Line
Tor Serine-Threonine Kinases
Enzyme Inhibitors
Life Sciences & Biomedicine
Family
Transfection
Identification
Phosphorylation Sites
Humans
Protein Kinase Inhibitors
Mechanism
Isoquinolines