One-way membrane trafficking of SOS in receptor-triggered Ras activation

Sune M. Christensen; Hsiung Lin Tu; Jesse E. Jun; Steven Alvarez; Meredith G. Triplet; Jeffrey S. Iwig; Kamlesh K. Yadav; Dafna Bar-Sagi; Jeroen P. Roose; Jay T. Groves

doi:10.1038/nsmb.3275

One-way membrane trafficking of SOS in receptor-triggered Ras activation

Sune M. Christensen
, Hsiung Lin Tu
, Jesse E. Jun
, Steven Alvarez
, Meredith G. Triplet
, Jeffrey S. Iwig
, Kamlesh K. Yadav
, Dafna Bar-Sagi
, Jeroen P. Roose
, Jay T. Groves

Icahn School of Medicine at Mount Sinai

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

50 Scopus citations

Abstract

SOS is a key activator of the small GTPase Ras. In cells, SOS-Ras signaling is thought to be initiated predominantly by membrane recruitment of SOS via the adaptor Grb2 and balanced by rapidly reversible Grb2-SOS binding kinetics. However, SOS has multiple protein and lipid interactions that provide linkage to the membrane. In reconstituted-membrane experiments, these Grb2-independent interactions were sufficient to retain human SOS on the membrane for many minutes, during which a single SOS molecule could processively activate thousands of Ras molecules. These observations raised questions concerning how receptors maintain control of SOS in cells and how membrane-recruited SOS is ultimately released. We addressed these questions in quantitative assays of reconstituted SOS-deficient chicken B-cell signaling systems combined with single-molecule measurements in supported membranes. These studies revealed an essentially one-way trafficking process in which membrane-recruited SOS remains trapped on the membrane and continuously activates Ras until being actively removed via endocytosis.

Original language	English
Pages (from-to)	838-846
Number of pages	9
Journal	Nature Structural and Molecular Biology
Volume	23
Issue number	9
DOIs	https://doi.org/10.1038/nsmb.3275
State	Published - 1 Sep 2016

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@article{1631566d69fc4696856d91ffd11cd2f4,

title = "One-way membrane trafficking of SOS in receptor-triggered Ras activation",

abstract = "SOS is a key activator of the small GTPase Ras. In cells, SOS-Ras signaling is thought to be initiated predominantly by membrane recruitment of SOS via the adaptor Grb2 and balanced by rapidly reversible Grb2-SOS binding kinetics. However, SOS has multiple protein and lipid interactions that provide linkage to the membrane. In reconstituted-membrane experiments, these Grb2-independent interactions were sufficient to retain human SOS on the membrane for many minutes, during which a single SOS molecule could processively activate thousands of Ras molecules. These observations raised questions concerning how receptors maintain control of SOS in cells and how membrane-recruited SOS is ultimately released. We addressed these questions in quantitative assays of reconstituted SOS-deficient chicken B-cell signaling systems combined with single-molecule measurements in supported membranes. These studies revealed an essentially one-way trafficking process in which membrane-recruited SOS remains trapped on the membrane and continuously activates Ras until being actively removed via endocytosis.",

author = "Christensen, \{Sune M.\} and Tu, \{Hsiung Lin\} and Jun, \{Jesse E.\} and Steven Alvarez and Triplet, \{Meredith G.\} and Iwig, \{Jeffrey S.\} and Yadav, \{Kamlesh K.\} and Dafna Bar-Sagi and Roose, \{Jeroen P.\} and Groves, \{Jay T.\}",

note = "Funding Information: Acknowledgments The authors thank the members of the laboratories of J.P.R., J.T.G., J. Kuriyan, and D.B.-S. for helpful comments and suggestions. The authors thank J. Kuriyan for insightful comments on the manuscript. In addition, the authors thank W.-C. Lin and L. Iversen for assistance with initial SLB experiments. This research was supported by a P01 Program grant from NIH-NIAID (AI091580 - to J.P.R. and J.T.G.). Further support came from R01-CA187318 NIH-NCI and R01-AI104789 (both to J.P.R.) and ARRA stimulus supplement GM078266 (to D.B.-S. and K.K.Y.) as well as a grant from the Danish Council for Independent Research, Natural Sciences (to S.M.C.). We thank T. Kurosaki (RIKEN) for providing wild-type and SOS1-2- DT40 B cells.",

year = "2016",

month = sep,

day = "1",

doi = "10.1038/nsmb.3275",

language = "English",

volume = "23",

pages = "838--846",

journal = "Nature Structural and Molecular Biology",

issn = "1545-9993",

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number = "9",

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T1 - One-way membrane trafficking of SOS in receptor-triggered Ras activation

AU - Christensen, Sune M.

AU - Tu, Hsiung Lin

AU - Jun, Jesse E.

AU - Alvarez, Steven

AU - Triplet, Meredith G.

AU - Iwig, Jeffrey S.

AU - Yadav, Kamlesh K.

AU - Bar-Sagi, Dafna

AU - Roose, Jeroen P.

AU - Groves, Jay T.

N1 - Funding Information: Acknowledgments The authors thank the members of the laboratories of J.P.R., J.T.G., J. Kuriyan, and D.B.-S. for helpful comments and suggestions. The authors thank J. Kuriyan for insightful comments on the manuscript. In addition, the authors thank W.-C. Lin and L. Iversen for assistance with initial SLB experiments. This research was supported by a P01 Program grant from NIH-NIAID (AI091580 - to J.P.R. and J.T.G.). Further support came from R01-CA187318 NIH-NCI and R01-AI104789 (both to J.P.R.) and ARRA stimulus supplement GM078266 (to D.B.-S. and K.K.Y.) as well as a grant from the Danish Council for Independent Research, Natural Sciences (to S.M.C.). We thank T. Kurosaki (RIKEN) for providing wild-type and SOS1-2- DT40 B cells.

PY - 2016/9/1

Y1 - 2016/9/1

N2 - SOS is a key activator of the small GTPase Ras. In cells, SOS-Ras signaling is thought to be initiated predominantly by membrane recruitment of SOS via the adaptor Grb2 and balanced by rapidly reversible Grb2-SOS binding kinetics. However, SOS has multiple protein and lipid interactions that provide linkage to the membrane. In reconstituted-membrane experiments, these Grb2-independent interactions were sufficient to retain human SOS on the membrane for many minutes, during which a single SOS molecule could processively activate thousands of Ras molecules. These observations raised questions concerning how receptors maintain control of SOS in cells and how membrane-recruited SOS is ultimately released. We addressed these questions in quantitative assays of reconstituted SOS-deficient chicken B-cell signaling systems combined with single-molecule measurements in supported membranes. These studies revealed an essentially one-way trafficking process in which membrane-recruited SOS remains trapped on the membrane and continuously activates Ras until being actively removed via endocytosis.

AB - SOS is a key activator of the small GTPase Ras. In cells, SOS-Ras signaling is thought to be initiated predominantly by membrane recruitment of SOS via the adaptor Grb2 and balanced by rapidly reversible Grb2-SOS binding kinetics. However, SOS has multiple protein and lipid interactions that provide linkage to the membrane. In reconstituted-membrane experiments, these Grb2-independent interactions were sufficient to retain human SOS on the membrane for many minutes, during which a single SOS molecule could processively activate thousands of Ras molecules. These observations raised questions concerning how receptors maintain control of SOS in cells and how membrane-recruited SOS is ultimately released. We addressed these questions in quantitative assays of reconstituted SOS-deficient chicken B-cell signaling systems combined with single-molecule measurements in supported membranes. These studies revealed an essentially one-way trafficking process in which membrane-recruited SOS remains trapped on the membrane and continuously activates Ras until being actively removed via endocytosis.

UR - https://www.scopus.com/pages/publications/84981287700

U2 - 10.1038/nsmb.3275

DO - 10.1038/nsmb.3275

M3 - Article

C2 - 27501536

AN - SCOPUS:84981287700

SN - 1545-9993

VL - 23

SP - 838

EP - 846

JO - Nature Structural and Molecular Biology

JF - Nature Structural and Molecular Biology

IS - 9

ER -

One-way membrane trafficking of SOS in receptor-triggered Ras activation

Abstract

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