Benefits and constrains of covalency : the role of loop length in protein stability and ligand binding

Linse, Sara; Thulin, Eva; Nilsson, Hanna; Stigler, Johannes

Benefits and constrains of covalency : the role of loop length in protein stability and ligand binding

Mark

Linse, Sara ^LU ; Thulin, Eva ^LU ; Nilsson, Hanna ^LU and Stigler, Johannes (2020) In Scientific Reports 10(1).

Abstract: Protein folding is governed by non-covalent interactions under the benefits and constraints of the covalent linkage of the backbone chain. In the current work we investigate the influence of loop length variation on the free energies of folding and ligand binding in a small globular single-domain protein containing two EF-hand subdomains—calbindin D_9k. We introduce a linker extension between the subdomains and vary its length between 1 to 16 glycine residues. We find a close to linear relationship between the linker length and the free energy of folding of the Ca²⁺-free protein. In contrast, the linker length has only a marginal effect on the Ca²⁺ affinity and cooperativity. The variant with a... (More); Protein folding is governed by non-covalent interactions under the benefits and constraints of the covalent linkage of the backbone chain. In the current work we investigate the influence of loop length variation on the free energies of folding and ligand binding in a small globular single-domain protein containing two EF-hand subdomains—calbindin D_9k. We introduce a linker extension between the subdomains and vary its length between 1 to 16 glycine residues. We find a close to linear relationship between the linker length and the free energy of folding of the Ca²⁺-free protein. In contrast, the linker length has only a marginal effect on the Ca²⁺ affinity and cooperativity. The variant with a single-glycine extension displays slightly increased Ca²⁺ affinity, suggesting that the slightly extended linker allows optimized packing of the Ca²⁺-bound state. For the extreme case of disconnected subdomains, Ca²⁺ binding becomes coupled to folding and assembly. Still, a high affinity between the EF-hands causes the non-covalent pair to retain a relatively high apparent Ca²⁺ affinity. Our results imply that loop length variation could be an evolutionary option for modulating properties such as protein stability and turnover without compromising the energetics of the specific function of the protein.
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Please use this url to cite or link to this publication: https://lup.lub.lu.se/record/3b2997e2-2659-468a-a38c-05a412fe49f7

author

Linse, Sara ^LU ; Thulin, Eva ^LU ; Nilsson, Hanna ^LU and Stigler, Johannes

organization

publishing date

2020

type

Contribution to journal

publication status

published

subject

Biochemistry and Molecular Biology

in

Scientific Reports

volume

10

issue

1

article number

20108

publisher

Nature Publishing Group

external identifiers

scopus:85096214463
pmid:33208843

ISSN

2045-2322

DOI

10.1038/s41598-020-76598-x

language

English

LU publication?

yes

id

3b2997e2-2659-468a-a38c-05a412fe49f7

date added to LUP

2021-01-15 11:12:36

date last changed

2024-06-14 08:55:53

@article{3b2997e2-2659-468a-a38c-05a412fe49f7,
  abstract     = {{<p>Protein folding is governed by non-covalent interactions under the benefits and constraints of the covalent linkage of the backbone chain. In the current work we investigate the influence of loop length variation on the free energies of folding and ligand binding in a small globular single-domain protein containing two EF-hand subdomains—calbindin D<sub>9k</sub>. We introduce a linker extension between the subdomains and vary its length between 1 to 16 glycine residues. We find a close to linear relationship between the linker length and the free energy of folding of the Ca<sup>2+</sup>-free protein. In contrast, the linker length has only a marginal effect on the Ca<sup>2+</sup> affinity and cooperativity. The variant with a single-glycine extension displays slightly increased Ca<sup>2+</sup> affinity, suggesting that the slightly extended linker allows optimized packing of the Ca<sup>2+</sup>-bound state. For the extreme case of disconnected subdomains, Ca<sup>2+</sup> binding becomes coupled to folding and assembly. Still, a high affinity between the EF-hands causes the non-covalent pair to retain a relatively high apparent Ca<sup>2+</sup> affinity. Our results imply that loop length variation could be an evolutionary option for modulating properties such as protein stability and turnover without compromising the energetics of the specific function of the protein.</p>}},
  author       = {{Linse, Sara and Thulin, Eva and Nilsson, Hanna and Stigler, Johannes}},
  issn         = {{2045-2322}},
  language     = {{eng}},
  number       = {{1}},
  publisher    = {{Nature Publishing Group}},
  series       = {{Scientific Reports}},
  title        = {{Benefits and constrains of covalency : the role of loop length in protein stability and ligand binding}},
  url          = {{http://dx.doi.org/10.1038/s41598-020-76598-x}},
  doi          = {{10.1038/s41598-020-76598-x}},
  volume       = {{10}},
  year         = {{2020}},
}

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Benefits and constrains of covalency : the role of loop length in protein stability and ligand binding