Crystal structure of human vaccinia‐related kinase 1 in complex with AMP‐PNP, a non‐hydrolyzable ATP analog

Ngow, Yeen Shian; Rajan, S. S.; Ye, Hong; Yoon, Ho Sup

doi:10.1002/pro.3552

Cited by 4 publications

(3 citation statements)

References 43 publications

(76 reference statements)

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“…Gly135 interacts with ATP and is required for the kinase activity 30 , and the variant G135R has lost most of its activity, and is also unstable. These two residues, R133 and G135 undergo chemical shift perturbations and affect the DRF motif 53 . It is known that the loss of VRK1 kinase activity by itself makes this protein unstable 13 .…”

Section: Discussionmentioning

confidence: 99%

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VRK1 functional insufficiency due to alterations in protein stability or kinase activity of human VRK1 pathogenic variants implicated in neuromotor syndromes

Martín-Doncel

Rojas

Cantarero

et al. 2019

Sci Rep

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Very rare polymorphisms in the human VRK1 (vaccinia-related kinase 1) gene have been identified in complex neuromotor phenotypes associated to spinal muscular atrophy (SMA), pontocerebellar hypoplasia (PCH), microcephaly, amyotrophic lateral sclerosis (ALS) and distal motor neuron dysfunctions. The mechanisms by which these VRK1 variant proteins contribute to the pathogenesis of these neurological syndromes are unknown. The syndromes are manifested when both of these rare VRK1 polymorphic alleles are implicated, either in homozygosis or compound heterozygosis. In this report, to identify the common underlying pathogenic mechanism of VRK1 polymorphisms, we have studied all human VRK1 variants identified in these neurological phenotypes from a biochemical point of view by molecular modeling, protein stability and kinase activity assays. Molecular modelling predicted that VRK1 variant proteins are either unstable or have an altered kinase activity. The stability and kinase activity of VRK1 pathogenic variants detected two groups. One composed by variants with a reduced protein stability: R133C, R358X, L195V, G135R and R321C. The other group includes VRK1variants with a reduced kinase activity tested on several substrates: histones H3 and H2AX, p53, c-Jun, coilin and 53BP1, a DNA repair protein. VRK1 variants with reduced kinase activity are H119R, R133C, G135R, V236M, R321C and R358X. The common underlying effect of VRK1 pathogenic variants with reduced protein stability or kinase activity is a functional insufficiency of VRK1 in patients with neuromotor developmental syndromes. The G135 variant cause a defective formation of 53BP1 foci in response to DNA damage, and loss Cajal bodies assembled on coilin.

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Section: Discussionmentioning

confidence: 99%

“…Modelling of the human VRK1 pathogenic variant proteins was performed using as reference the published structures 2RSV 29 and 2LAV 30,53 available from the Protein Data Bank. FoldX program 81 (http://foldxsuite.crg.eu/) was used to predict the effect of missense mutations in the structural stability of the VRK kinase (PDB identifier 2LAV).…”

Section: Methodsmentioning

confidence: 99%

VRK1 functional insufficiency due to alterations in protein stability or kinase activity of human VRK1 pathogenic variants implicated in neuromotor syndromes

Martín-Doncel

Rojas

Cantarero

et al. 2019

Sci Rep

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“…Vaccinia-related kinase 1 (VRK1) is a serine/threonine mitotic nuclear kinase that is linked to cell proliferation and regarded as a cancer drug target. , Starting from the bound substrate analogue structure (PDB: 6ac9), we decided to apply our approach toward designing a potential ligand inhibitor. First, we removed the ribose phosphate tail and predicted a fragment to replace it; interestingly, the top solution was an aminotetrahydrofuran ring, with the oxygen atom of the tetrahydrofuran interacting with Lys71 and the charged amino group interacting with Asp197 and Asn182.…”

Section: Resultsmentioning

confidence: 99%

FragExplorer: GRID-Based Fragment Growing and Replacement

Cross

Cruciani

2022

J. Chem. Inf. Model.

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Understanding which chemical modifications can be made to known ligands is a key aspect of structure-based drug design and one that was pioneered by the software GRID. We developed FragExplorer with the explicit aim of showing GRID users which fragments would best match the GRID molecular interaction fields in a protein binding site, given a bound ligand as a starting point. Users can grow ligands or replace existing moieties; the R-Group Exploration mode identifies all potential R-Groups and searches for replacements automatically; the Scaffold Exploration mode does the same for all potential scaffolds. For a ligand with three points of variation, R-Group Exploration will typically explore a chemical space of 10 16 potential molecules; including Scaffold Exploration increases this to 10 22 . FragExplorer was designed to be integrated within an interactive 3D Editor/Designer; therefore, the speed of computation was an important consideration; a typical fragment search takes 20 seconds. In a fragment reprediction test, FragExplorer demonstrates an overall fragment retrieval rate of 55%, increasing to 69% for smaller fragments. At a 90% substructural match, the retrieval rate increases to ∼80%. We also show how the approach could have been used to hop from olmesartan to azilsartan or to optimize a p38 MAP kinase lead to a compound that bears similarity to a known nanomolar inhibitor.

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Nuclear functions regulated by the VRK1 kinase

Lazo

2024

Nucleus

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Crystal structure of human vaccinia‐related kinase 1 in complex with AMP‐PNP, a non‐hydrolyzable ATP analog

Cited by 4 publications

References 43 publications

VRK1 functional insufficiency due to alterations in protein stability or kinase activity of human VRK1 pathogenic variants implicated in neuromotor syndromes

VRK1 functional insufficiency due to alterations in protein stability or kinase activity of human VRK1 pathogenic variants implicated in neuromotor syndromes

FragExplorer: GRID-Based Fragment Growing and Replacement

Nuclear functions regulated by the VRK1 kinase

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