Vaccinia-related kinase 1 (VRK1) confers resistance to DNA-damaging agents in human breast cancer by affecting DNA damage response

Salzano, Marcella; Vázquez-Cedeira, Marta; Sanz-García, Marta; Valbuena, Alberto; Blanco, Sandra; Fernández, Isabel F.; Lazo, Pedro A.

doi:10.18632/oncotarget.1678

Cited by 48 publications

(59 citation statements)

References 52 publications

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“…Such an effect has already been identified in response to doxorubicin. 54 Alternatively, high VRK1 levels should make cells more resistant to treatment, and this has been reported in breast cancer, 54 in which VRK1 identifies a subgroup within estrogen receptor positive cases that presents a poorer prognosis. 64,65 The structure of VRK1 indicates that any specific inhibitor will have no crossinhibitory effect on other kinases due its very low promiscuity index 55,56 and, therefore, makes VRK1 a very good candidate for development of highly specific inhibitors that may be useful in treatment of some tumors.…”

Section: Discussionmentioning

confidence: 99%

VRK1 chromatin kinase phosphorylates H2AX and is required for foci formation induced by DNA damage

et al. 2015

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All types of DNA damage cause a local alteration and relaxation of chromatin structure. Sensing and reacting to this initial chromatin alteration is a necessary trigger for any type of DNA damage response (DDR). In this context, chromatin kinases are likely candidates to participate in detection and reaction to a locally altered chromatin as a consequence of DNA damage and, thus, initiate the appropriate cellular response. In this work, we demonstrate that VRK1 is a nucleosomal chromatin kinase and that its depletion causes loss of histones H3 and H4 acetylation, which are required for chromatin relaxation, both in basal conditions and after DNA damage, independently of ATM. Moreover, VRK1 directly and stably interacts with histones H2AX and H3 in basal conditions. In response to DNA damage induced by ionizing radiation, histone H2AX is phosphorylated in Ser139 by VRK1. The phosphorylation of H2AX and the formation of gH2AX foci induced by ionizing radiation (IR), are prevented by VRK1 depletion and are rescued by kinase-active, but not kinase-dead, VRK1. In conclusion, we found that VRK1 is a novel chromatin component that reacts to its alterations and participates very early in DDR, functioning by itself or in cooperation with ATM.

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Section: Discussionmentioning

confidence: 99%

VRK1 chromatin kinase phosphorylates H2AX and is required for foci formation induced by DNA damage

et al. 2015

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“…VRK1 is discovered as an early response gene and is one of the important factors for the initiation of cell division process, reflected on its overexpression in many cancerous tissues . Recent studies have shown direct correlation of poor clinical outcomes of breast cancer patients was associated with high expression levels of VRK1 suggesting it as a promising cancer drug target . VRK1 can phosphorylate itself (auto‐phosphorylate) as well as its interacting substrate proteins.…”

Section: Introductionmentioning

confidence: 99%

“…16 Recent studies have shown direct correlation of poor clinical outcomes of breast cancer patients was associated with high expression levels of VRK1 17 suggesting it as a promising cancer drug target. [16][17][18][19] VRK1 can phosphorylate itself (auto-phosphorylate) as well as its interacting substrate proteins. During mitosis, VRK1 can phosphorylate (a) barrierto-autointegration factor (BAF) to regulate the morphology of nuclear envelope 20 ; (b) H3's N-terminal tail H-15 N TROSY spectra of VRK1 in free state (red) with that of VRK1 in the presence of AMP-PNP at a molar ratio of 1:5 (VRK1: AMP-PNP; blue).…”

Section: Introductionmentioning

confidence: 99%

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

Ngow

Rajan

et al. 2018

Protein Science

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Vaccinia‐related kinase 1 (VRK1), a serine/threonine mitotic kinase, is widely over‐expressed in dividing cells and regarded as a cancer drug target primarily due to its function as an early response gene in cell proliferation. However, the mechanism of VRK1 phosphorylation and substrate activation is not well understood. More importantly even the molecular basis of VRK1 interaction with its cofactor, adenosine triphosphate (ATP), is unavailable to‐date. As designing specific inhibitors remains to be the major challenge in kinase research, such a molecular understanding will enable us to design ATP‐competitive specific inhibitors of VRK1. Here we report the molecular characterization of VRK1 in complex with AMP‐PNP, a non‐hydrolyzable ATP‐analog, using NMR titration followed by the co‐crystal structure determined upto 2.07 Å resolution. We also carried out the structural comparison of the AMP‐PNP bound‐form with its apo and inhibitor‐bound counterparts, which has enabled us to present our rationale toward designing VRK1‐specific inhibitors.

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“…Por lo tanto, el desarrollo de inhibidores de diferentes componentes de la respuesta al daño en el ADN pueda tener un gran potencial para la sensibilización de las células a los tratamientos, en particular aquellos tipos de cáncer más radio o quimioresistentes (Curtin, 2012;Martin, 2001). Se ha demostrado que células de cáncer de mama positivas para el receptor de estrógenos muestran altos niveles proteicos de VRK1, lo que puede contribuir a la resistencia de este tipo de tumores (Salzano et al, 2014). De tal manera, proponemos a VRK1 como una diana de inhibición ya que hemos demostrado que esta quinasa tiene un papel importante en la modulación de la respuesta al daño en el ADN a diferentes niveles en la vía de señalización, de tal forma que un tratamiento combinado puede ser una alternativa a producir lesiones sin que estas puedan ser reparadas, por ejemplo la inhibición de ATM con inhibidores específicos como KU55933 o CGK733, junto con el tratamiento con doxorubicina, incrementaron los niveles de apoptosis en células cancerosas (Khalil HS, 2012).…”

Section: Rnf8unclassified

Implicación de las quinasas humanas VRK1 y VRK2 en las rutas de respuesta a daño genético y apoptosis

Carmona¹

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Vaccinia-related kinase 1 (VRK1) confers resistance to DNA-damaging agents in human breast cancer by affecting DNA damage response

Cited by 48 publications

References 52 publications

VRK1 chromatin kinase phosphorylates H2AX and is required for foci formation induced by DNA damage

VRK1 chromatin kinase phosphorylates H2AX and is required for foci formation induced by DNA damage

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

Implicación de las quinasas humanas VRK1 y VRK2 en las rutas de respuesta a daño genético y apoptosis

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