Cbl promotes clustering of endocytic adaptor proteins

Daniela Jozic; Nayra Cárdenes; Yonathan Lissanu Deribe; Gabriel Moncalián; Daniela Hoeller; Yvonne Groemping; Ivan Dikic; Katrin Rittinger; Jerónimo Bravo

doi:10.1038/nsmb1000

Cbl promotes clustering of endocytic adaptor proteins

Daniela Jozic, Nayra Cárdenes, Yonathan Lissanu Deribe, Gabriel Moncalián, Daniela Hoeller, Yvonne Groemping, Ivan Dikic, Katrin Rittinger, Jerónimo Bravo

Research output: Contribution to journal › Article › peer-review

54 Scopus citations

Abstract

The ubiquitin ligases c-Cbl and Cbl-b play a crucial role in receptor downregulation by mediating multiple monoubiquitination of receptors and promoting their sorting for lysosomal degradation. Their function is modulated through interactions with regulatory proteins including CIN85 and PIX, which recognize a proline-arginine motif in Cbl and thus promote or inhibit receptor endocytosis. We report the structures of SH3 domains of CIN85 and β-PIX in complex with a proline-arginine peptide from Cbl-b. Both structures reveal a heterotrimeric complex containing two SH3 domains held together by a single peptide. Trimerization also occurs in solution and is facilitated by the pseudo-symmetrical peptide sequence. Moreover, ternary complexes of CIN85 and Cbl are formed in vivo and are important for the ability of Cbl to promote epidermal growth factor receptor (EGFR) downregulation. These results provide molecular explanations for a novel mechanism by which Cbl controls receptor downregulation.

Original language	English (US)
Pages (from-to)	972-979
Number of pages	8
Journal	Nature Structural and Molecular Biology
Volume	12
Issue number	11
DOIs	https://doi.org/10.1038/nsmb1000
State	Published - Nov 29 2005
Externally published	Yes

ASJC Scopus subject areas

Structural Biology
Molecular Biology

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@article{d1d4997758b74ec2b751ca94f8ab6795,

title = "Cbl promotes clustering of endocytic adaptor proteins",

abstract = "The ubiquitin ligases c-Cbl and Cbl-b play a crucial role in receptor downregulation by mediating multiple monoubiquitination of receptors and promoting their sorting for lysosomal degradation. Their function is modulated through interactions with regulatory proteins including CIN85 and PIX, which recognize a proline-arginine motif in Cbl and thus promote or inhibit receptor endocytosis. We report the structures of SH3 domains of CIN85 and β-PIX in complex with a proline-arginine peptide from Cbl-b. Both structures reveal a heterotrimeric complex containing two SH3 domains held together by a single peptide. Trimerization also occurs in solution and is facilitated by the pseudo-symmetrical peptide sequence. Moreover, ternary complexes of CIN85 and Cbl are formed in vivo and are important for the ability of Cbl to promote epidermal growth factor receptor (EGFR) downregulation. These results provide molecular explanations for a novel mechanism by which Cbl controls receptor downregulation.",

author = "Daniela Jozic and Nayra C{\'a}rdenes and Deribe, {Yonathan Lissanu} and Gabriel Moncali{\'a}n and Daniela Hoeller and Yvonne Groemping and Ivan Dikic and Katrin Rittinger and Jer{\'o}nimo Bravo",

note = "Funding Information: The b-PIX-SH3 plasmid was a gift of E. Manser (Institute of Molecular and Cell Biology, Singapore). We are grateful to S. Howell and L. Haire (National Institute for Medical Research, London) for mass spectrometry; P. Fletcher (National Institute for Medical Research, London) and W. Mawby (University of Bristol, Bristol, UK) for peptide synthesis; J. Nicholson and R. Kehoe at Daresbury Laboratory for beamline assistance; A. Albert for help in data collection and M. Ortiz for help with CIN85A structure refinement. Research on CIN85 was supported by grant SAF2003-03860 of the Ministerio de Ciencia y Tecnolog{\'i}a, Spain, and N.C. received a fellowship from the Ram{\'o}n Areces Foundation. D.J. and K.R. are funded by the Medical Research Council, UK. Work by Y.L.D, D.H. and I.D. is supported by grants from Deutsche Forschungsgemeinschaft, Germany.",

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doi = "10.1038/nsmb1000",

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T1 - Cbl promotes clustering of endocytic adaptor proteins

AU - Jozic, Daniela

AU - Cárdenes, Nayra

AU - Deribe, Yonathan Lissanu

AU - Moncalián, Gabriel

AU - Hoeller, Daniela

AU - Groemping, Yvonne

AU - Dikic, Ivan

AU - Rittinger, Katrin

AU - Bravo, Jerónimo

N1 - Funding Information: The b-PIX-SH3 plasmid was a gift of E. Manser (Institute of Molecular and Cell Biology, Singapore). We are grateful to S. Howell and L. Haire (National Institute for Medical Research, London) for mass spectrometry; P. Fletcher (National Institute for Medical Research, London) and W. Mawby (University of Bristol, Bristol, UK) for peptide synthesis; J. Nicholson and R. Kehoe at Daresbury Laboratory for beamline assistance; A. Albert for help in data collection and M. Ortiz for help with CIN85A structure refinement. Research on CIN85 was supported by grant SAF2003-03860 of the Ministerio de Ciencia y Tecnología, Spain, and N.C. received a fellowship from the Ramón Areces Foundation. D.J. and K.R. are funded by the Medical Research Council, UK. Work by Y.L.D, D.H. and I.D. is supported by grants from Deutsche Forschungsgemeinschaft, Germany.

PY - 2005/11/29

Y1 - 2005/11/29

N2 - The ubiquitin ligases c-Cbl and Cbl-b play a crucial role in receptor downregulation by mediating multiple monoubiquitination of receptors and promoting their sorting for lysosomal degradation. Their function is modulated through interactions with regulatory proteins including CIN85 and PIX, which recognize a proline-arginine motif in Cbl and thus promote or inhibit receptor endocytosis. We report the structures of SH3 domains of CIN85 and β-PIX in complex with a proline-arginine peptide from Cbl-b. Both structures reveal a heterotrimeric complex containing two SH3 domains held together by a single peptide. Trimerization also occurs in solution and is facilitated by the pseudo-symmetrical peptide sequence. Moreover, ternary complexes of CIN85 and Cbl are formed in vivo and are important for the ability of Cbl to promote epidermal growth factor receptor (EGFR) downregulation. These results provide molecular explanations for a novel mechanism by which Cbl controls receptor downregulation.

AB - The ubiquitin ligases c-Cbl and Cbl-b play a crucial role in receptor downregulation by mediating multiple monoubiquitination of receptors and promoting their sorting for lysosomal degradation. Their function is modulated through interactions with regulatory proteins including CIN85 and PIX, which recognize a proline-arginine motif in Cbl and thus promote or inhibit receptor endocytosis. We report the structures of SH3 domains of CIN85 and β-PIX in complex with a proline-arginine peptide from Cbl-b. Both structures reveal a heterotrimeric complex containing two SH3 domains held together by a single peptide. Trimerization also occurs in solution and is facilitated by the pseudo-symmetrical peptide sequence. Moreover, ternary complexes of CIN85 and Cbl are formed in vivo and are important for the ability of Cbl to promote epidermal growth factor receptor (EGFR) downregulation. These results provide molecular explanations for a novel mechanism by which Cbl controls receptor downregulation.

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JF - Nature Structural and Molecular Biology

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ER -

Cbl promotes clustering of endocytic adaptor proteins

Abstract

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