Factor quinolinone inhibitors disrupt spindles and multiple LSF (TFCP2)-protein interactions in mitosis, including with microtubule-associated proteins

Factor quinolinone inhibitors (FQIs), a first-in-class set of small molecule inhibitors targeted to the transcription factor LSF (TFCP2), exhibit promising cancer chemotherapeutic properties. FQI1, the initial lead compound identified, unexpectedly induced a concentration-dependent delay in mitotic...

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Autores principales: Yunes, Sarah A., Willoughby, Jennifer L. S., Kwan, Julian H., Biagi, Jessica M., Pokharel, Niranjana, Chin, Hang Gyeong, York, Emily A., Su, Kuan-Chung, George, Kelly, Shah, Jagesh V., Emili, Andrew, Schaus, Scott E., Hansen, Ulla
Formato: Online Artículo Texto
Lenguaje:English
Publicado: Public Library of Science 2022
Materias:
Research Article
Acceso en línea:https://www.ncbi.nlm.nih.gov/pmc/articles/PMC9200292/
https://www.ncbi.nlm.nih.gov/pubmed/35704642
http://dx.doi.org/10.1371/journal.pone.0268857
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author Yunes, Sarah A.
Willoughby, Jennifer L. S.
Kwan, Julian H.
Biagi, Jessica M.
Pokharel, Niranjana
Chin, Hang Gyeong
York, Emily A.
Su, Kuan-Chung
George, Kelly
Shah, Jagesh V.
Emili, Andrew
Schaus, Scott E.
Hansen, Ulla
author_facet Yunes, Sarah A.
Willoughby, Jennifer L. S.
Kwan, Julian H.
Biagi, Jessica M.
Pokharel, Niranjana
Chin, Hang Gyeong
York, Emily A.
Su, Kuan-Chung
George, Kelly
Shah, Jagesh V.
Emili, Andrew
Schaus, Scott E.
Hansen, Ulla
author_sort Yunes, Sarah A.
collection PubMed
description Factor quinolinone inhibitors (FQIs), a first-in-class set of small molecule inhibitors targeted to the transcription factor LSF (TFCP2), exhibit promising cancer chemotherapeutic properties. FQI1, the initial lead compound identified, unexpectedly induced a concentration-dependent delay in mitotic progression. Here, we show that FQI1 can rapidly and reversibly lead to mitotic arrest, even when added directly to mitotic cells, implying that FQI1-mediated mitotic defects are not transcriptionally based. Furthermore, treatment with FQIs resulted in a striking, concentration-dependent diminishment of spindle microtubules, accompanied by a concentration-dependent increase in multi-aster formation. Aberrant γ-tubulin localization was also observed. These phenotypes suggest that perturbation of spindle microtubules is the primary event leading to the mitotic delays upon FQI1 treatment. Previously, FQIs were shown to specifically inhibit not only LSF DNA-binding activity, which requires LSF oligomerization to tetramers, but also other specific LSF-protein interactions. Other transcription factors participate in mitosis through non-transcriptional means, and we recently reported that LSF directly binds α-tubulin and is present in purified cellular tubulin preparations. Consistent with a microtubule role for LSF, here we show that LSF enhanced the rate of tubulin polymerization in vitro, and FQI1 inhibited such polymerization. To probe whether the FQI1-mediated spindle abnormalities could result from inhibition of mitotic LSF-protein interactions, mass spectrometry was performed using as bait an inducible, tagged form of LSF that is biotinylated by endogenous enzymes. The global proteomics analysis yielded expected associations for a transcription factor, notably with RNA processing machinery, but also to nontranscriptional components. In particular, and consistent with spindle disruption due to FQI treatment, mitotic, FQI1-sensitive interactions were identified between the biotinylated LSF and microtubule-associated proteins that regulate spindle assembly, positioning, and dynamics, as well as centrosome-associated proteins. Probing the mitotic LSF interactome using small molecule inhibitors therefore supported a non-transcriptional role for LSF in mediating progression through mitosis.
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spelling pubmed-92002922022-06-16 Factor quinolinone inhibitors disrupt spindles and multiple LSF (TFCP2)-protein interactions in mitosis, including with microtubule-associated proteins Yunes, Sarah A. Willoughby, Jennifer L. S. Kwan, Julian H. Biagi, Jessica M. Pokharel, Niranjana Chin, Hang Gyeong York, Emily A. Su, Kuan-Chung George, Kelly Shah, Jagesh V. Emili, Andrew Schaus, Scott E. Hansen, Ulla PLoS One Research Article Factor quinolinone inhibitors (FQIs), a first-in-class set of small molecule inhibitors targeted to the transcription factor LSF (TFCP2), exhibit promising cancer chemotherapeutic properties. FQI1, the initial lead compound identified, unexpectedly induced a concentration-dependent delay in mitotic progression. Here, we show that FQI1 can rapidly and reversibly lead to mitotic arrest, even when added directly to mitotic cells, implying that FQI1-mediated mitotic defects are not transcriptionally based. Furthermore, treatment with FQIs resulted in a striking, concentration-dependent diminishment of spindle microtubules, accompanied by a concentration-dependent increase in multi-aster formation. Aberrant γ-tubulin localization was also observed. These phenotypes suggest that perturbation of spindle microtubules is the primary event leading to the mitotic delays upon FQI1 treatment. Previously, FQIs were shown to specifically inhibit not only LSF DNA-binding activity, which requires LSF oligomerization to tetramers, but also other specific LSF-protein interactions. Other transcription factors participate in mitosis through non-transcriptional means, and we recently reported that LSF directly binds α-tubulin and is present in purified cellular tubulin preparations. Consistent with a microtubule role for LSF, here we show that LSF enhanced the rate of tubulin polymerization in vitro, and FQI1 inhibited such polymerization. To probe whether the FQI1-mediated spindle abnormalities could result from inhibition of mitotic LSF-protein interactions, mass spectrometry was performed using as bait an inducible, tagged form of LSF that is biotinylated by endogenous enzymes. The global proteomics analysis yielded expected associations for a transcription factor, notably with RNA processing machinery, but also to nontranscriptional components. In particular, and consistent with spindle disruption due to FQI treatment, mitotic, FQI1-sensitive interactions were identified between the biotinylated LSF and microtubule-associated proteins that regulate spindle assembly, positioning, and dynamics, as well as centrosome-associated proteins. Probing the mitotic LSF interactome using small molecule inhibitors therefore supported a non-transcriptional role for LSF in mediating progression through mitosis. Public Library of Science 2022-06-15 /pmc/articles/PMC9200292/ /pubmed/35704642 http://dx.doi.org/10.1371/journal.pone.0268857 Text en © 2022 Yunes et al https://creativecommons.org/licenses/by/4.0/This is an open access article distributed under the terms of the Creative Commons Attribution License (https://creativecommons.org/licenses/by/4.0/) , which permits unrestricted use, distribution, and reproduction in any medium, provided the original author and source are credited.
spellingShingle Research Article
Yunes, Sarah A.
Willoughby, Jennifer L. S.
Kwan, Julian H.
Biagi, Jessica M.
Pokharel, Niranjana
Chin, Hang Gyeong
York, Emily A.
Su, Kuan-Chung
George, Kelly
Shah, Jagesh V.
Emili, Andrew
Schaus, Scott E.
Hansen, Ulla
Factor quinolinone inhibitors disrupt spindles and multiple LSF (TFCP2)-protein interactions in mitosis, including with microtubule-associated proteins
title Factor quinolinone inhibitors disrupt spindles and multiple LSF (TFCP2)-protein interactions in mitosis, including with microtubule-associated proteins
title_full Factor quinolinone inhibitors disrupt spindles and multiple LSF (TFCP2)-protein interactions in mitosis, including with microtubule-associated proteins
title_fullStr Factor quinolinone inhibitors disrupt spindles and multiple LSF (TFCP2)-protein interactions in mitosis, including with microtubule-associated proteins
title_full_unstemmed Factor quinolinone inhibitors disrupt spindles and multiple LSF (TFCP2)-protein interactions in mitosis, including with microtubule-associated proteins
title_short Factor quinolinone inhibitors disrupt spindles and multiple LSF (TFCP2)-protein interactions in mitosis, including with microtubule-associated proteins
title_sort factor quinolinone inhibitors disrupt spindles and multiple lsf (tfcp2)-protein interactions in mitosis, including with microtubule-associated proteins
topic Research Article
url https://www.ncbi.nlm.nih.gov/pmc/articles/PMC9200292/
https://www.ncbi.nlm.nih.gov/pubmed/35704642
http://dx.doi.org/10.1371/journal.pone.0268857
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