Protein Short-Time Diffusion in a Naturally Crowded Environment

Marco Grimaldo; Hender Lopez; Christian Beck; Felix Roosen-Runge; Martine Moulin; Juliette M. Devos; Valerie Laux; Michael Härtlein; Stefano Da Vela; Ralf Schweins; Alessandro Mariani; Fajun Zhang; Jean Louis Barrat; Martin Oettel; V. Trevor Forsyth; Tilo Seydel; Frank Schreiber

doi:10.1021/acs.jpclett.9b00345

Protein Short-Time Diffusion in a Naturally Crowded Environment

Marco Grimaldo, Hender Lopez, Christian Beck, Felix Roosen-Runge, Martine Moulin, Juliette M. Devos, Valerie Laux, Michael Härtlein, Stefano Da Vela, Ralf Schweins, Alessandro Mariani, Fajun Zhang, Jean Louis Barrat, Martin Oettel, V. Trevor Forsyth, Tilo Seydel, Frank Schreiber

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

Abstract

The interior of living cells is a dense and polydisperse suspension of macromolecules. Such a complex system challenges an understanding in terms of colloidal suspensions. As a fundamental test we employ neutron spectroscopy to measure the diffusion of tracer proteins (immunoglobulins) in a cell-like environment (cell lysate) with explicit control over crowding conditions. In combination with Stokesian dynamics simulation, we address protein diffusion on nanosecond time scales where hydrodynamic interactions dominate over negligible protein collisions. We successfully link the experimental results on these complex, flexible molecules with coarse-grained simulations providing a consistent understanding by colloid theories. Both experiments and simulations show that tracers in polydisperse solutions close to the effective particle radius R _eff = R _i ³ ^1/3 diffuse approximately as if the suspension was monodisperse. The simulations further show that macromolecules of sizes R > R _eff (R < R _eff ) are slowed more (less) effectively even at nanosecond time scales, which is highly relevant for a quantitative understanding of cellular processes.

Original language	English
Pages (from-to)	1709-1715
Number of pages	7
Journal	Journal of Physical Chemistry Letters
Volume	10
Issue number	8
DOIs	https://doi.org/10.1021/acs.jpclett.9b00345
Publication status	Published - 18 Apr 2019

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Grimaldo, M., Lopez, H., Beck, C., Roosen-Runge, F., Moulin, M., Devos, J. M., Laux, V., Härtlein, M., Da Vela, S., Schweins, R., Mariani, A., Zhang, F., Barrat, J. L., Oettel, M., Forsyth, V. T., Seydel, T., & Schreiber, F. (2019). Protein Short-Time Diffusion in a Naturally Crowded Environment. Journal of Physical Chemistry Letters, 10(8), 1709-1715. https://doi.org/10.1021/acs.jpclett.9b00345

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title = "Protein Short-Time Diffusion in a Naturally Crowded Environment",

abstract = " The interior of living cells is a dense and polydisperse suspension of macromolecules. Such a complex system challenges an understanding in terms of colloidal suspensions. As a fundamental test we employ neutron spectroscopy to measure the diffusion of tracer proteins (immunoglobulins) in a cell-like environment (cell lysate) with explicit control over crowding conditions. In combination with Stokesian dynamics simulation, we address protein diffusion on nanosecond time scales where hydrodynamic interactions dominate over negligible protein collisions. We successfully link the experimental results on these complex, flexible molecules with coarse-grained simulations providing a consistent understanding by colloid theories. Both experiments and simulations show that tracers in polydisperse solutions close to the effective particle radius R eff = R i 3 1/3 diffuse approximately as if the suspension was monodisperse. The simulations further show that macromolecules of sizes R > R eff (R < R eff ) are slowed more (less) effectively even at nanosecond time scales, which is highly relevant for a quantitative understanding of cellular processes.",

author = "Marco Grimaldo and Hender Lopez and Christian Beck and Felix Roosen-Runge and Martine Moulin and Devos, \{Juliette M.\} and Valerie Laux and Michael H{\"a}rtlein and \{Da Vela\}, Stefano and Ralf Schweins and Alessandro Mariani and Fajun Zhang and Barrat, \{Jean Louis\} and Martin Oettel and Forsyth, \{V. Trevor\} and Tilo Seydel and Frank Schreiber",

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doi = "10.1021/acs.jpclett.9b00345",

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Grimaldo, M, Lopez, H, Beck, C, Roosen-Runge, F, Moulin, M, Devos, JM, Laux, V, Härtlein, M, Da Vela, S, Schweins, R, Mariani, A, Zhang, F, Barrat, JL, Oettel, M, Forsyth, VT, Seydel, T & Schreiber, F 2019, 'Protein Short-Time Diffusion in a Naturally Crowded Environment', Journal of Physical Chemistry Letters, vol. 10, no. 8, pp. 1709-1715. https://doi.org/10.1021/acs.jpclett.9b00345

TY - JOUR

T1 - Protein Short-Time Diffusion in a Naturally Crowded Environment

AU - Grimaldo, Marco

AU - Lopez, Hender

AU - Beck, Christian

AU - Roosen-Runge, Felix

AU - Moulin, Martine

AU - Devos, Juliette M.

AU - Laux, Valerie

AU - Härtlein, Michael

AU - Da Vela, Stefano

AU - Schweins, Ralf

AU - Mariani, Alessandro

AU - Zhang, Fajun

AU - Barrat, Jean Louis

AU - Oettel, Martin

AU - Forsyth, V. Trevor

AU - Seydel, Tilo

AU - Schreiber, Frank

PY - 2019/4/18

Y1 - 2019/4/18

N2 - The interior of living cells is a dense and polydisperse suspension of macromolecules. Such a complex system challenges an understanding in terms of colloidal suspensions. As a fundamental test we employ neutron spectroscopy to measure the diffusion of tracer proteins (immunoglobulins) in a cell-like environment (cell lysate) with explicit control over crowding conditions. In combination with Stokesian dynamics simulation, we address protein diffusion on nanosecond time scales where hydrodynamic interactions dominate over negligible protein collisions. We successfully link the experimental results on these complex, flexible molecules with coarse-grained simulations providing a consistent understanding by colloid theories. Both experiments and simulations show that tracers in polydisperse solutions close to the effective particle radius R eff = R i 3 1/3 diffuse approximately as if the suspension was monodisperse. The simulations further show that macromolecules of sizes R > R eff (R < R eff ) are slowed more (less) effectively even at nanosecond time scales, which is highly relevant for a quantitative understanding of cellular processes.

AB - The interior of living cells is a dense and polydisperse suspension of macromolecules. Such a complex system challenges an understanding in terms of colloidal suspensions. As a fundamental test we employ neutron spectroscopy to measure the diffusion of tracer proteins (immunoglobulins) in a cell-like environment (cell lysate) with explicit control over crowding conditions. In combination with Stokesian dynamics simulation, we address protein diffusion on nanosecond time scales where hydrodynamic interactions dominate over negligible protein collisions. We successfully link the experimental results on these complex, flexible molecules with coarse-grained simulations providing a consistent understanding by colloid theories. Both experiments and simulations show that tracers in polydisperse solutions close to the effective particle radius R eff = R i 3 1/3 diffuse approximately as if the suspension was monodisperse. The simulations further show that macromolecules of sizes R > R eff (R < R eff ) are slowed more (less) effectively even at nanosecond time scales, which is highly relevant for a quantitative understanding of cellular processes.

UR - https://www.scopus.com/pages/publications/85064159263

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DO - 10.1021/acs.jpclett.9b00345

M3 - Article

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AN - SCOPUS:85064159263

SN - 1948-7185

VL - 10

SP - 1709

EP - 1715

JO - Journal of Physical Chemistry Letters

JF - Journal of Physical Chemistry Letters

IS - 8

ER -

Protein Short-Time Diffusion in a Naturally Crowded Environment

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