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Increasing the bulk of the 1TEL–target linker and retaining the 10×His tag in a 1TEL–CMG2-vWa construct improves crystal order and diffraction limits

TELSAM-fusion crystallization has the potential to become a revolutionary tool for the facile crystallization of proteins. TELSAM fusion can increase the crystallization rate and enable crystallization at low protein concentrations, in some cases with minimal crystal contacts [Nawarathnage et al. (2...

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Autores principales: Gajjar, Parag L., Pedroza Romo, Maria J., Litchfield, Celeste M., Callahan, Miles, Redd, Nathan, Nawarathnage, Supeshala, Soleimani, Sara, Averett, Jacob, Wilson, Elijah, Lewis, Andrew, Stewart, Cameron, Tseng, Yi-Jie, Doukov, Tzanko, Lebedev, Andrey, Moody, James D.
Formato: Online Artículo Texto
Lenguaje:English
Publicado: International Union of Crystallography 2023
Materias:
Acceso en línea:https://www.ncbi.nlm.nih.gov/pmc/articles/PMC10565734/
https://www.ncbi.nlm.nih.gov/pubmed/37747038
http://dx.doi.org/10.1107/S2059798323007246
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author Gajjar, Parag L.
Pedroza Romo, Maria J.
Litchfield, Celeste M.
Callahan, Miles
Redd, Nathan
Nawarathnage, Supeshala
Soleimani, Sara
Averett, Jacob
Wilson, Elijah
Lewis, Andrew
Stewart, Cameron
Tseng, Yi-Jie
Doukov, Tzanko
Lebedev, Andrey
Moody, James D.
author_facet Gajjar, Parag L.
Pedroza Romo, Maria J.
Litchfield, Celeste M.
Callahan, Miles
Redd, Nathan
Nawarathnage, Supeshala
Soleimani, Sara
Averett, Jacob
Wilson, Elijah
Lewis, Andrew
Stewart, Cameron
Tseng, Yi-Jie
Doukov, Tzanko
Lebedev, Andrey
Moody, James D.
author_sort Gajjar, Parag L.
collection PubMed
description TELSAM-fusion crystallization has the potential to become a revolutionary tool for the facile crystallization of proteins. TELSAM fusion can increase the crystallization rate and enable crystallization at low protein concentrations, in some cases with minimal crystal contacts [Nawarathnage et al. (2022 ▸), Open Biol. 12, 210271]. Here, requirements for the linker composition between 1TEL and a fused CMG2 vWa domain were investigated. Ala-Ala, Ala-Val, Thr-Val and Thr-Thr linkers were evaluated, comparing metrics for crystallization propensity and crystal order. The effect on crystallization of removing or retaining the purification tag was then tested. It was discovered that increasing the linker bulk and retaining the 10×His purification tag improved the diffraction resolution, likely by decreasing the number of possible vWa-domain orientations in the crystal. Additionally, it was discovered that some vWa-domain binding modes are correlated with scrambling of the 1TEL polymer orientation in crystals and an effective mitigation strategy for this pathology is presented.
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spelling pubmed-105657342023-10-12 Increasing the bulk of the 1TEL–target linker and retaining the 10×His tag in a 1TEL–CMG2-vWa construct improves crystal order and diffraction limits Gajjar, Parag L. Pedroza Romo, Maria J. Litchfield, Celeste M. Callahan, Miles Redd, Nathan Nawarathnage, Supeshala Soleimani, Sara Averett, Jacob Wilson, Elijah Lewis, Andrew Stewart, Cameron Tseng, Yi-Jie Doukov, Tzanko Lebedev, Andrey Moody, James D. Acta Crystallogr D Struct Biol Research Papers TELSAM-fusion crystallization has the potential to become a revolutionary tool for the facile crystallization of proteins. TELSAM fusion can increase the crystallization rate and enable crystallization at low protein concentrations, in some cases with minimal crystal contacts [Nawarathnage et al. (2022 ▸), Open Biol. 12, 210271]. Here, requirements for the linker composition between 1TEL and a fused CMG2 vWa domain were investigated. Ala-Ala, Ala-Val, Thr-Val and Thr-Thr linkers were evaluated, comparing metrics for crystallization propensity and crystal order. The effect on crystallization of removing or retaining the purification tag was then tested. It was discovered that increasing the linker bulk and retaining the 10×His purification tag improved the diffraction resolution, likely by decreasing the number of possible vWa-domain orientations in the crystal. Additionally, it was discovered that some vWa-domain binding modes are correlated with scrambling of the 1TEL polymer orientation in crystals and an effective mitigation strategy for this pathology is presented. International Union of Crystallography 2023-09-25 /pmc/articles/PMC10565734/ /pubmed/37747038 http://dx.doi.org/10.1107/S2059798323007246 Text en © Parag L. Gajjar et al. 2023 https://creativecommons.org/licenses/by/4.0/This is an open-access article distributed under the terms of the Creative Commons Attribution (CC-BY) Licence, which permits unrestricted use, distribution, and reproduction in any medium, provided the original authors and source are cited.
spellingShingle Research Papers
Gajjar, Parag L.
Pedroza Romo, Maria J.
Litchfield, Celeste M.
Callahan, Miles
Redd, Nathan
Nawarathnage, Supeshala
Soleimani, Sara
Averett, Jacob
Wilson, Elijah
Lewis, Andrew
Stewart, Cameron
Tseng, Yi-Jie
Doukov, Tzanko
Lebedev, Andrey
Moody, James D.
Increasing the bulk of the 1TEL–target linker and retaining the 10×His tag in a 1TEL–CMG2-vWa construct improves crystal order and diffraction limits
title Increasing the bulk of the 1TEL–target linker and retaining the 10×His tag in a 1TEL–CMG2-vWa construct improves crystal order and diffraction limits
title_full Increasing the bulk of the 1TEL–target linker and retaining the 10×His tag in a 1TEL–CMG2-vWa construct improves crystal order and diffraction limits
title_fullStr Increasing the bulk of the 1TEL–target linker and retaining the 10×His tag in a 1TEL–CMG2-vWa construct improves crystal order and diffraction limits
title_full_unstemmed Increasing the bulk of the 1TEL–target linker and retaining the 10×His tag in a 1TEL–CMG2-vWa construct improves crystal order and diffraction limits
title_short Increasing the bulk of the 1TEL–target linker and retaining the 10×His tag in a 1TEL–CMG2-vWa construct improves crystal order and diffraction limits
title_sort increasing the bulk of the 1tel–target linker and retaining the 10×his tag in a 1tel–cmg2-vwa construct improves crystal order and diffraction limits
topic Research Papers
url https://www.ncbi.nlm.nih.gov/pmc/articles/PMC10565734/
https://www.ncbi.nlm.nih.gov/pubmed/37747038
http://dx.doi.org/10.1107/S2059798323007246
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