Effect of Clinically Used Microtubule Targeting Drugs on Viral Infection and Transport Function

Oliva, M.A.; Tosat‐Bitrián, Carlota; Barrado-Gil, Lucía; Bonato, Francesca; Galindo, Inmaculada; Garaigorta, Urtzi; Álvarez-Bernad, Beatriz; París-Ogáyar, Rebeca; Lucena‐Agell, Daniel; Giménez-Abián, Juan F.; García-Dorival, Isabel; Urquiza, Jesús; Gastaminza, Pablo; Díaz, J. Fernando; Palomo, Valle; Alonso, Covadonga

doi:10.3390/ijms23073448

Cited by 9 publications

(10 citation statements)

References 90 publications

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“…Noticeably, we have found that PM534 is also effective in tumor cells that upregulate tubulin βIII isotype, as it is not affected by the Cys239 to Ser239 change in the colchicine binding site. This is a known resistance mechanism emerging as a feature of aggressive and treatment-refractory cancers. ,, Notice that some of the compounds that bind deeper in the CBD are more selective for certain tubulin isotypes or bind preferentially to tubulins of other species . This ability to choose isotypes comes from some residues within the domain, like βC241 (in central hinge helix H7) and βI318 (pharmacophore center I), which are often involved in protein–drug interactions and are changed in the βIII-tubulin isotype to βS241 and βV318, respectively.…”

Section: Discussionmentioning

confidence: 99%

“… 41 , 45 , 50 Notice that some of the compounds that bind deeper in the CBD are more selective for certain tubulin isotypes 51 or bind preferentially to tubulins of other species. 52 This ability to choose isotypes comes from some residues within the domain, like βC241 (in central hinge helix H7) and βI318 (pharmacophore center I), which are often involved in protein–drug interactions and are changed in the βIII-tubulin isotype to βS241 and βV318, respectively. PM534 does not interact with βC241, although it can establish hydrophobic contacts with βI318, which could work against overexpression of the tubulin isotype βIII.…”

Section: Discussionmentioning

confidence: 99%

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PM534, an Optimized Target-Protein Interaction Strategy through the Colchicine Site of Tubulin

Lucena-Agell,

Guillén,

Matesanz

et al. 2024

J. Med. Chem.

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Targeting microtubules is the most effective wide-spectrum pharmacological strategy in antitumoral chemotherapy, and current research focuses on reducing main drawbacks: neurotoxicity and resistance. PM534 is a novel synthetic compound derived from the Structure−Activity-Relationship study on the natural molecule PM742, isolated from the sponge of the order Lithistida, family Theonellidae, genus Discodermia (du Bocage 1869). PM534 targets the entire colchicine binding domain of tubulin, covering four of the five centers of the pharmacophore model. Its nanomolar affinity and high retention time modulate a strikingly high antitumor activity that efficiently overrides two resistance mechanisms in cells (detoxification pumps and tubulin βIII isotype overexpression). Furthermore, PM534 induces significant inhibition of tumor growth in mouse xenograft models of human non-small cell lung cancer. Our results present PM534, a highly effective new compound in the preclinical evaluation that is currently in its first human Phase I clinical trial.

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Section: Discussionmentioning

confidence: 99%

Section: Discussionmentioning

confidence: 99%

PM534, an Optimized Target-Protein Interaction Strategy through the Colchicine Site of Tubulin

Lucena-Agell,

Guillén,

Matesanz

et al. 2024

J. Med. Chem.

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“…Our theoretical and numerical predictions thus present numerous possibilities for superradiance- and subradiance-enabled metabolic regulation, communication, and control in and between cells (see Table S3) and with external agents that interact with the cytoskeleton at various stages of cellular growth and replication . We complement the theory and computation with experimental measurements of fluorescence QY in tubulin and MTs, which point to a significant increase from the former to the latter, in line with the numerical predictions.…”

Section: Discussionmentioning

confidence: 99%

Ultraviolet Superradiance from Mega-Networks of Tryptophan in Biological Architectures

Babcock,

Montes-Cabrera,

Oberhofer

et al. 2024

J. Phys. Chem. B

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Networks of tryptophan (Trp)�an aromatic amino acid with strong fluorescence response�are ubiquitous in biological systems, forming diverse architectures in transmembrane proteins, cytoskeletal filaments, subneuronal elements, photoreceptor complexes, virion capsids, and other cellular structures. We analyze the cooperative effects induced by ultraviolet (UV) excitation of several biologically relevant Trp mega-networks, thus giving insights into novel mechanisms for cellular signaling and control. Our theoretical analysis in the single-excitation manifold predicts the formation of strongly superradiant states due to collective interactions among organized arrangements of up to >10 5 Trp UV-excited transition dipoles in microtubule architectures, which leads to an enhancement of the fluorescence quantum yield (QY) that is confirmed by our experiments. We demonstrate the observed consequences of this superradiant behavior in the fluorescence QY for hierarchically organized tubulin structures, which increases in different geometric regimes at thermal equilibrium before saturation, highlighting the effect's persistence in the presence of disorder. Our work thus showcases the many orders of magnitude across which the brightest (hundreds of femtoseconds) and darkest (tens of seconds) states can coexist in these Trp lattices.

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“…Peptidic probes combined a cell penetrating region and a kinesin binding domain and were labelled at the N -termini with Cy5 to provide a fluorescent kinesin binding peptide. Their synthesis and labelling has been previously described ( Oliva et al, 2022 ).…”

Section: Methodsmentioning

confidence: 99%

TTBK1 and CK1 inhibitors restore TDP-43 pathology and avoid disease propagation in lymphoblast from Alzheimer’s disease patients

Martínez-González

Cuevas

Tosat‐Bitrián

et al. 2023

Front. Mol. Neurosci.

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IntroductionTDP-43 proteinopathy in Alzheimer’s disease (AD) patients is recently emerging as a relevant pathomolecular event that may have been overlooked. Recent results in immortalized lymphocytes from AD patients have shown not only an increase of post-translational modifications in TDP-43, such as hyperphosphorylation and fragmentation, but also its prionic behaviour and cell-to-cell disease transmission. With the main goal to advance therapeutic interventions, we present in this work different kinase inhibitors with potential to restore this pathological mechanism.MethodologyWe have used immortalized lymphocytes from healthy controls and AD severe patients to evaluate the correction of TDP-43 pathology after the treatment with previously synthetized TTBK1 and CK1 inhibitors. Moreover we used the conditioned mediums of these cells to perform different disease propagation experiments.ResultsTDP-43 pathology observed in lymphoblasts from severe AD patients is reduced after the treatment with TTBK1 and CK1 inhibitors (decreasing phosphorylation and increasing nuclear localisation), Furthermore, the significant increase in TDP-43 phosphorylation, cytoplasmic accumulation and aberrant F-actin protrusions (TNT-like structures) observed in control cells growing in CM from AD lymphoblasts were abolished when the CM from AD lymphoblasts treated with previously reported TTBK1 and CK1 inhibitors were used. In addition, the cytosolic transport mediated by molecular motors of the receptor cells was altered with the induced TDP-43 pathology, but it was not produced with the abovementioned pretreated CMs.ConclusionTTBK1 and CK1 inhibitors, specially VNG1.47 and IGS2.7 compounds, restore TDP-43 pathology and avoid cell-to-cell propagation in immortalized lymphocytes from AD patients, being excellent candidates for the future therapy of this prevalent and devastating disease.

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Effect of Clinically Used Microtubule Targeting Drugs on Viral Infection and Transport Function

Cited by 9 publications

References 90 publications

PM534, an Optimized Target-Protein Interaction Strategy through the Colchicine Site of Tubulin

PM534, an Optimized Target-Protein Interaction Strategy through the Colchicine Site of Tubulin

Ultraviolet Superradiance from Mega-Networks of Tryptophan in Biological Architectures

TTBK1 and CK1 inhibitors restore TDP-43 pathology and avoid disease propagation in lymphoblast from Alzheimer’s disease patients

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