1. Stefin B Interacts with Histones and Cathepsin L in the Nucleus
- Author
-
Miha Renko, Katarina Maher, Špela Konjar, Alain Nepveu, Nataša Kopitar-Jerala, Eva Žerovnik, Igor Križaj, Mojca Bencina, Urska Repnik, Boris Turk, and Slavko Čeru
- Subjects
Cathepsin L ,Models, Biological ,Biochemistry ,Cathepsin B ,Histones ,Mice ,Histone H3 ,Cytosol ,Cathepsin O ,Cell Line, Tumor ,Cathepsin L1 ,Fluorescence Resonance Energy Transfer ,medicine ,Animals ,Humans ,Cystatin B ,Molecular Biology ,Cell Nucleus ,biology ,Cell Cycle ,Cell Biology ,Fibroblasts ,Cell cycle ,Molecular biology ,Cell nucleus ,medicine.anatomical_structure ,Gene Expression Regulation ,Enzymology ,biology.protein - Abstract
Stefin B (cystatin B) is an endogenous inhibitor of cysteine proteinases localized in the nucleus and the cytosol. Loss-of-function mutations in the stefin B gene (CSTB) gene were reported in patients with Unverricht-Lundborg disease (EPM1). We have identified an interaction between stefin B and nucleosomes, specifically with histones H2A.Z, H2B, and H3. In synchronized T98G cells, stefin B co-immunoprecipitated with histone H3, predominantly in the G(1) phase of the cell cycle. Stefin B-deficient mouse embryonic fibroblasts entered S phase earlier than wild type mouse embryonic fibroblasts. In contrast, increased expression of stefin B in the nucleus delayed cell cycle progression in T98G cells. The delay in cell cycle progression was associated with the inhibition of cathepsin L in the nucleus, as judged from the decreased cleavage of the CUX1 transcription factor. In vitro, inhibition of cathepsin L by stefin B was potentiated in the presence of histones, whereas histones alone did not affect the cathepsin L activity. Interaction of stefin B with the Met-75 truncated form of cathepsin L in the nucleus was confirmed by fluorescence resonance energy transfer experiments in the living cells. Stefin B could thus play an important role in regulating the proteolytic activity of cathepsin L in the nucleus, protecting substrates such as transcription factors from its proteolytic processing.
- Published
- 2010
- Full Text
- View/download PDF