Multidomain assembled states of Hck tyrosine kinase in solution

Yang, Sichun; Blachowicz, Lydia; Makowski, Lee; Roux, Benoı̂t

doi:10.1073/pnas.1004569107

Cited by 194 publications

(202 citation statements)

References 33 publications

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“…Activation of the enzyme is induced by Tyr dephosphorylation and other modifications, which release intramolecular contacts and lead to a largely disassembled and more disordered active state. Recent SAXS experiments 26 showed an ensemble of distinct closed and open structures in both the inactive and active states ( Figure 2D), therefore signaling due to dephosphorylation is best described as a shift in the conformational ensemble. 26 In a way similar to the case of interdomain allostery, Hck also represents a combination of traditional and novel types of allostery, because shifts in the population are converted to structure-based signal propagation in the catalytic domain (Table 2).…”

Section: Autoinhibitionmentioning

confidence: 99%

“…24 It also became clear that allosteric coupling might occur without a discernible conformational change, by way of altering the dynamics of the protein only 6,21,25 ( Figure 1C) to favor a particular downstream binding/catalytic event. By combining elements of classical cooperativity (subunit interactions) and conformational coupling augmented by structural disorder (novel allostery), recently it was also reported that domaindomain interactions enabled by a disordered linker 13,26 might permit the formation of an energetic pathway traversing separate domains through their interface (Figure1D).…”

Section: Structural and Dynamic Basis Of Allosterymentioning

confidence: 99%

“…It is rather common that even in the naïve state, besides the inactive conformation (e.g. the autoinhibited closed conformation of Hck, 26 and Vav 106 ) the activated state must also be present, as demanded by local accessibility to the input signal (e.g. a post-translational modification or an incoming binding partner).…”

Section: Structural Characterizationmentioning

confidence: 99%

“…26 Like all kinases in the Src-family, Hck is a multidomain allosteric enzyme with and N-terminal SH4 domain, a unique domain, SH3 and SH2 domains, and a catalytic domain, all connected by flexible linkers. Inactive Hck is dominated by a closed (assembled) conformation maintained by intramolecular interactions between a Cterminal pTyr residue and the SH2 domain, and the Pro-rich linker and the SH3 domain ( Figure 2D).…”

Section: Autoinhibitionmentioning

confidence: 99%

See 3 more Smart Citations

Multisteric Regulation by Structural Disorder in Modular Signaling Proteins: An Extension of the Concept of Allostery

2013

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Section: Autoinhibitionmentioning

confidence: 99%

Section: Structural and Dynamic Basis Of Allosterymentioning

confidence: 99%

Section: Structural Characterizationmentioning

confidence: 99%

Section: Autoinhibitionmentioning

confidence: 99%

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Multisteric Regulation by Structural Disorder in Modular Signaling Proteins: An Extension of the Concept of Allostery

2013

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“…These developments have generated an interest in developing new methods to make optimal use of the available experimental data. From the initial emphasis on the determination of the native structures of proteins, the focus is increasingly shifting toward generating conformational ensembles representing their conformational fluctuations (2)(3)(4). In this context, problems with overfitting are systematically addressed (5), and in general efforts are made to implement the structural restraints as conservatively as possible, for instance by using the maximum entropy principle (6)(7)(8)(9).…”

mentioning

confidence: 99%

Equilibrium simulations of proteins using molecular fragment replacement and NMR chemical shifts

Boomsma

Tian

Frellsen

et al. 2014

Proc. Natl. Acad. Sci. U.S.A.

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Methods of protein structure determination based on NMR chemical shifts are becoming increasingly common. The most widely used approaches adopt the molecular fragment replacement strategy, in which structural fragments are repeatedly reassembled into different complete conformations in molecular simulations. Although these approaches are effective in generating individual structures consistent with the chemical shift data, they do not enable the sampling of the conformational space of proteins with correct statistical weights. Here, we present a method of molecular fragment replacement that makes it possible to perform equilibrium simulations of proteins, and hence to determine their free energy landscapes. This strategy is based on the encoding of the chemical shift information in a probabilistic model in Markov chain Monte Carlo simulations. First, we demonstrate that with this approach it is possible to fold proteins to their native states starting from extended structures. Second, we show that the method satisfies the detailed balance condition and hence it can be used to carry out an equilibrium sampling from the Boltzmann distribution corresponding to the force field used in the simulations. Third, by comparing the results of simulations carried out with and without chemical shift restraints we describe quantitatively the effects that these restraints have on the free energy landscapes of proteins. Taken together, these results demonstrate that the molecular fragment replacement strategy can be used in combination with chemical shift information to characterize not only the native structures of proteins but also their conformational fluctuations.

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Application of Small‐Angle X‐Ray Scattering in Studies of Biological Macromolecules

Gräwert¹,

Svergun²

2019

Encyclopedia of Analytical Chemistry

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Biological small‐angle X‐ray scattering (SAXS) allows one to study overall structures and structural transitions of many biological macromolecules in solution, under close to native conditions. Sample preparation for SAXS is straightforward with no crystallization, labelling or immobilization needed, thus significantly reducing the risk of preparation artefacts. The size range of objects that can be studied spans from small peptides like insulin or nucleic acid aptamers up to megadalton‐size multi subunit complexes and viruses. With a single measurement being performed in sub‐second time scale at modern synchrotron facilities it is possible to study rapid kinetics or decaying samples. SAXS data give insights into size, shape, oligomeric composition and flexibility of the probed macromolecules and complexes. SAXS is useful as a standalone technique but also as a complementary method that profits from the availability of experimental or predicted high resolution models of the studied objects or their fragments and funnels them together with scattering data in powerful hybrid method approaches. Thanks to all these advantages and constant new developments, the use of SAXS to address challenging biological questions is steadily increasing. Here, we review the latest developments providing insights into the wide range of applications that benefit from SAXS.

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Multidomain assembled states of Hck tyrosine kinase in solution

Cited by 194 publications

References 33 publications

Multisteric Regulation by Structural Disorder in Modular Signaling Proteins: An Extension of the Concept of Allostery

Multisteric Regulation by Structural Disorder in Modular Signaling Proteins: An Extension of the Concept of Allostery

Equilibrium simulations of proteins using molecular fragment replacement and NMR chemical shifts

Application of Small‐Angle X‐Ray Scattering in Studies of Biological Macromolecules

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