Compartmentalization of the Cell Membrane

Alf Honigmann; Arnd Pralle

doi:10.1016/j.jmb.2016.09.022

Compartmentalization of the Cell Membrane

Alf Honigmann
, Arnd Pralle

Physics

Max Planck Institute of Molecular Cell Biology and Genetics

Research output: Contribution to journal › Review article › peer-review

72 Scopus citations

Abstract

Many cell-membrane-associated processes require transient spatiotemporal separation of components on scales ranging from a couple of molecules to micrometers in size. Understanding these processes mechanistically involves understanding how lipids and proteins self-organize and interact with the cell cortex. Here, we review recent advances in dissecting the mechanisms of cell membrane compartmentalization. We introduce the challenges in studying cell membrane organization, the current understanding of how complex membranes self-organize to form transient domains, and the role of protein scaffolds in membrane organization. We discuss the formation of signaling domains as an important example of transient membrane compartmentalization. We conclude by pointing to the current limitations of measuring membrane organization in living cells and the steps that are required to advance the field.

Original language	English
Pages (from-to)	4739-4748
Number of pages	10
Journal	Journal of Molecular Biology
Volume	428
Issue number	24
DOIs	https://doi.org/10.1016/j.jmb.2016.09.022
State	Published - Dec 4 2016

Keywords

cell membrane ultrastructure
cortical actin
lipid raft
nano cluster
network

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10.1016/j.jmb.2016.09.022

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abstract = "Many cell-membrane-associated processes require transient spatiotemporal separation of components on scales ranging from a couple of molecules to micrometers in size. Understanding these processes mechanistically involves understanding how lipids and proteins self-organize and interact with the cell cortex. Here, we review recent advances in dissecting the mechanisms of cell membrane compartmentalization. We introduce the challenges in studying cell membrane organization, the current understanding of how complex membranes self-organize to form transient domains, and the role of protein scaffolds in membrane organization. We discuss the formation of signaling domains as an important example of transient membrane compartmentalization. We conclude by pointing to the current limitations of measuring membrane organization in living cells and the steps that are required to advance the field.",

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N2 - Many cell-membrane-associated processes require transient spatiotemporal separation of components on scales ranging from a couple of molecules to micrometers in size. Understanding these processes mechanistically involves understanding how lipids and proteins self-organize and interact with the cell cortex. Here, we review recent advances in dissecting the mechanisms of cell membrane compartmentalization. We introduce the challenges in studying cell membrane organization, the current understanding of how complex membranes self-organize to form transient domains, and the role of protein scaffolds in membrane organization. We discuss the formation of signaling domains as an important example of transient membrane compartmentalization. We conclude by pointing to the current limitations of measuring membrane organization in living cells and the steps that are required to advance the field.

AB - Many cell-membrane-associated processes require transient spatiotemporal separation of components on scales ranging from a couple of molecules to micrometers in size. Understanding these processes mechanistically involves understanding how lipids and proteins self-organize and interact with the cell cortex. Here, we review recent advances in dissecting the mechanisms of cell membrane compartmentalization. We introduce the challenges in studying cell membrane organization, the current understanding of how complex membranes self-organize to form transient domains, and the role of protein scaffolds in membrane organization. We discuss the formation of signaling domains as an important example of transient membrane compartmentalization. We conclude by pointing to the current limitations of measuring membrane organization in living cells and the steps that are required to advance the field.

KW - cell membrane ultrastructure

KW - cortical actin

KW - lipid raft

KW - nano cluster

KW - network

UR - https://www.scopus.com/pages/publications/84998885574

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DO - 10.1016/j.jmb.2016.09.022

M3 - Review article

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VL - 428

SP - 4739

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JO - Journal of Molecular Biology

JF - Journal of Molecular Biology

IS - 24

ER -

Compartmentalization of the Cell Membrane

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Keywords

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