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1. KIF2C/MCAK a prognostic biomarker and its oncogenic potential in malignant progression, and prognosis of cancer patients: a systematic review and meta-analysis as biomarker.

Author

Kreis, Nina-Naomi, Moon, Ha Hyung, Wordeman, Linda, Louwen, Frank, Solbach, Christine, Yuan, Juping, and Ritter, Andreas

Subjects
TUMOR diagnosis, TUMOR genetics, RESEARCH funding, CELL physiology, TUMOR markers, META-analysis, CANCER patients, SYSTEMATIC reviews, GENE expression, ONCOGENES, CELL death, KINESIN, TUMORS, PROGRESSION-free survival, DISEASE progression, GENOMES, OVERALL survival
Abstract

KIF2C/MCAK (KIF2C) is the most well-characterized member of the kinesin-13 family, which is critical in the regulation of microtubule (MT) dynamics during mitosis, as well as interphase. This systematic review briefly describes the important structural elements of KIF2C, its regulation by multiple molecular mechanisms, and its broad cellular functions. Furthermore, it systematically summarizes its oncogenic potential in malignant progression and performs a meta-analysis of its prognostic value in cancer patients. KIF2C was shown to be involved in multiple crucial cellular processes including cell migration and invasion, DNA repair, senescence induction and immune modulation, which are all known to be critical during the development of malignant tumors. Indeed, an increasing number of publications indicate that KIF2C is aberrantly expressed in multiple cancer entities. Consequently, we have highlighted its involvement in at least five hallmarks of cancer, namely: genome instability, resisting cell death, activating invasion and metastasis, avoiding immune destruction and cellular senescence. This was followed by a systematic search of KIF2C/MCAK's expression in various malignant tumor entities and its correlation with clinicopathologic features. Available data were pooled into multiple weighted meta-analyses for the correlation between KIF2Chigh protein or gene expression and the overall survival in breast cancer, non-small cell lung cancer and hepatocellular carcinoma patients. Furthermore, high expression of KIF2C was correlated to disease-free survival of hepatocellular carcinoma. All meta-analyses showed poor prognosis for cancer patients with KIF2Chigh expression, associated with a decreased overall survival and reduced disease-free survival, indicating KIF2C's oncogenic potential in malignant progression and as a prognostic marker. This work delineated the promising research perspective of KIF2C with modern in vivo and in vitro technologies to further decipher the function of KIF2C in malignant tumor development and progression. This might help to establish KIF2C as a biomarker for the diagnosis or evaluation of at least three cancer entities. [ABSTRACT FROM AUTHOR]

Published
2024
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3. Oxidative stress decreases microtubule growth and stability in ventricular myocytes

Author

Drum, Benjamin ML, Yuan, Can, Li, Lei, Liu, Qinghang, Wordeman, Linda, and Santana, L Fernando

Subjects
1.1 Normal biological development and functioning, Underpinning research, Cardiovascular, Animals, Heart Ventricles, Mice, Microscopy, Fluorescence, Microtubule-Associated Proteins, Microtubules, Myocardial Infarction, Myocytes, Cardiac, Oxidative Stress, Protein Binding, Protein Transport, Tubulin, Microtubule dynamics, Cardiomyocytes, Live imaging, Oxidative stress, Myocardial infarction, Transient outward current, Cardiorespiratory Medicine and Haematology, Medical Physiology, Cardiovascular System & Hematology
Abstract

Microtubules (MTs) have many roles in ventricular myocytes, including structural stability, morphological integrity, and protein trafficking. However, despite their functional importance, dynamic MTs had never been visualized in living adult myocytes. Using adeno-associated viral vectors expressing the MT-associated protein plus end binding protein 3 (EB3) tagged with EGFP, we were able to perform live imaging and thus capture and quantify MT dynamics in ventricular myocytes in real time under physiological conditions. Super-resolution nanoscopy revealed that EB1 associated in puncta along the length of MTs in ventricular myocytes. The vast (~80%) majority of MTs grew perpendicular to T-tubules at a rate of 0.06μm∗s(-1) and growth was preferentially (82%) confined to a single sarcomere. Microtubule catastrophe rate was lower near the Z-line than M-line. Hydrogen peroxide increased the rate of catastrophe of MTs ~7-fold, suggesting that oxidative stress destabilizes these structures in ventricular myocytes. We also quantified MT dynamics after myocardial infarction (MI), a pathological condition associated with increased production of reactive oxygen species (ROS). Our data indicate that the catastrophe rate of MTs increases following MI. This contributed to decreased transient outward K(+) currents by decreasing the surface expression of Kv4.2 and Kv4.3 channels after MI. On the basis of these data, we conclude that, under physiological conditions, MT growth is directionally biased and that increased ROS production during MI disrupts MT dynamics, decreasing K(+) channel trafficking.

Published
2016

4. A mitotic kinase scaffold depleted in testicular seminomas impacts spindle orientation in germ line stem cells.

Author

Hehnly, Heidi, Canton, David, Bucko, Paula, Langeberg, Lorene K, Ogier, Leah, Gelman, Irwin, Santana, L Fernando, Wordeman, Linda, and Scott, John D

Subjects
Germ Cells, Stem Cells, Animals, Mice, Knockout, Humans, Mice, Seminoma, Protein-Serine-Threonine Kinases, Cell Cycle Proteins, Proto-Oncogene Proteins, Cell Division, A Kinase Anchor Proteins, Spindle Apparatus, Aurora Kinase A, biochemistry, cell biology, cell regulation, human, mitotic spindle, mouse, protein kinase, signal transduction, testicular cancer, Knockout, Biochemistry and Cell Biology
Abstract

Correct orientation of the mitotic spindle in stem cells underlies organogenesis. Spindle abnormalities correlate with cancer progression in germ line-derived tumors. We discover a macromolecular complex between the scaffolding protein Gravin/AKAP12 and the mitotic kinases, Aurora A and Plk1, that is down regulated in human seminoma. Depletion of Gravin correlates with an increased mitotic index and disorganization of seminiferous tubules. Biochemical, super-resolution imaging, and enzymology approaches establish that this Gravin scaffold accumulates at the mother spindle pole during metaphase. Manipulating elements of the Gravin-Aurora A-Plk1 axis prompts mitotic delay and prevents appropriate assembly of astral microtubules to promote spindle misorientation. These pathological responses are conserved in seminiferous tubules from Gravin(-/-) mice where an overabundance of Oct3/4 positive germ line stem cells displays randomized orientation of mitotic spindles. Thus, we propose that Gravin-mediated recruitment of Aurora A and Plk1 to the mother (oldest) spindle pole contributes to the fidelity of symmetric cell division.

Published
2015

7. De novo design of self-assembling helical protein filaments

Author

Shen, Hao, Fallas, Jorge A., Lynch, Eric, Sheffler, William, Parry, Bradley, Jannetty, Nicholas, Decarreau, Justin, Wagenbach, Michael, Vicente, Juan Jesus, Chen, Jiajun, Wang, Lei, Dowling, Quinton, Oberdorfer, Gustav, Stewart, Lance, Wordeman, Linda, De Yoreo, James, Jacobs-Wagner, Christine, Kollman, Justin, and Baker, David

Published
2018

12. Cooperation of the Dam1 and Ndc80 kinetochore complexes enhances microtubule coupling and is regulated by aurora B

Author

Tien, Jerry F, Umbreit, Neil T, Gestaut, Daniel R, Franck, Andrew D, Cooper, Jeremy, Wordeman, Linda, Gonen, Tamir, Asbury, Charles L, and Davis, Trisha N

Subjects
Biochemistry and Cell Biology, Biological Sciences, Genetics, 1.1 Normal biological development and functioning, Underpinning research, Generic health relevance, Aurora Kinases, Cell Cycle Proteins, Green Fluorescent Proteins, Kinetochores, Microtubule-Associated Proteins, Microtubules, Nuclear Proteins, Protein Serine-Threonine Kinases, Saccharomyces cerevisiae, Saccharomyces cerevisiae Proteins, Spindle Apparatus, Medical and Health Sciences, Developmental Biology, Biological sciences, Biomedical and clinical sciences
Abstract

The coupling of kinetochores to dynamic spindle microtubules is crucial for chromosome positioning and segregation, error correction, and cell cycle progression. How these fundamental attachments are made and persist under tensile forces from the spindle remain important questions. As microtubule-binding elements, the budding yeast Ndc80 and Dam1 kinetochore complexes are essential and not redundant, but their distinct contributions are unknown. In this study, we show that the Dam1 complex is a processivity factor for the Ndc80 complex, enhancing the ability of the Ndc80 complex to form load-bearing attachments to and track with dynamic microtubule tips in vitro. Moreover, the interaction between the Ndc80 and Dam1 complexes is abolished when the Dam1 complex is phosphorylated by the yeast aurora B kinase Ipl1. This provides evidence for a mechanism by which aurora B resets aberrant kinetochore-microtubule attachments. We propose that the action of the Dam1 complex as a processivity factor in kinetochore-microtubule attachment is regulated by conserved signals for error correction.

Published
2010

13. A Standardized Kinesin Nomenclature

Author

Lawrence, Carolyn J., Dawe, R. Kelly, Christie, Karen R., Cleveland, Don W., Dawson, Scott C., Endow, Sharyn A., Goodson, Holly V., Hirokawa, Nobutaka, Howard, Jonathon, Malmberg, Russell L., McIntosh, J. Richard, Miki, Harukata, Mitchison, Timothy J., Okada, Yasushi, Saxton, William M., Schliwa, Manfred, Scholey, Jonathan M., Vale, Ronald D., Walczak, Claire E., and Wordeman, Linda

Published
2004

17. Movie S1 from ST-11: A New Brain-Penetrant Microtubule-Destabilizing Agent with Therapeutic Potential for Glioblastoma Multiforme

Author

Cherry, Allison E., primary, Haas, Brian R., primary, Naydenov, Alipi V., primary, Fung, Susan, primary, Xu, Cong, primary, Swinney, Katie, primary, Wagenbach, Michael, primary, Freeling, Jennifer, primary, Canton, David A., primary, Coy, Jonathan, primary, Horne, Eric A., primary, Rickman, Barry, primary, Vicente, Juan Jesus, primary, Scott, John D., primary, Ho, Rodney J.Y., primary, Liggitt, Denny, primary, Wordeman, Linda, primary, and Stella, Nephi, primary

Published
2023
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18. Data from ST-11: A New Brain-Penetrant Microtubule-Destabilizing Agent with Therapeutic Potential for Glioblastoma Multiforme

Author

Cherry, Allison E., primary, Haas, Brian R., primary, Naydenov, Alipi V., primary, Fung, Susan, primary, Xu, Cong, primary, Swinney, Katie, primary, Wagenbach, Michael, primary, Freeling, Jennifer, primary, Canton, David A., primary, Coy, Jonathan, primary, Horne, Eric A., primary, Rickman, Barry, primary, Vicente, Juan Jesus, primary, Scott, John D., primary, Ho, Rodney J.Y., primary, Liggitt, Denny, primary, Wordeman, Linda, primary, and Stella, Nephi, primary

Published
2023
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19. Supplemental Figures S1-S7; Supplemental Materials and Methods; and Supplemental Table S1 from ST-11: A New Brain-Penetrant Microtubule-Destabilizing Agent with Therapeutic Potential for Glioblastoma Multiforme

Author

Cherry, Allison E., primary, Haas, Brian R., primary, Naydenov, Alipi V., primary, Fung, Susan, primary, Xu, Cong, primary, Swinney, Katie, primary, Wagenbach, Michael, primary, Freeling, Jennifer, primary, Canton, David A., primary, Coy, Jonathan, primary, Horne, Eric A., primary, Rickman, Barry, primary, Vicente, Juan Jesus, primary, Scott, John D., primary, Ho, Rodney J.Y., primary, Liggitt, Denny, primary, Wordeman, Linda, primary, and Stella, Nephi, primary

Published
2023
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40. Non-enzymatic activity of the α-tubulin acetyltransferase αTAT1 limits synaptic bouton growth in neurons

Author

Coombes, Courtney E., Saunders, Harriet A. J., Mannava, Anirudh G., Johnson-Schlitz, Dena M., Reid, Taylor A., Parmar, Sneha, McClellan, Mark, Yan, Connie, Rogers, Stephen L., Parrish, Jay Z., Wagenbach, Michael, Wordeman, Linda, Wildonger, Jill, and Gardner, Melissa K.

Subjects
Drosophila melanogaster, nervous system, Acetyltransferases, Larva, fungi, Neuromuscular Junction, Presynaptic Terminals, Animals, Article
Abstract

Neuronal axons terminate as synaptic boutons that form stable yet plastic connections with their targets. Synaptic bouton development relies on an underlying network of both long-lived and dynamic microtubules that provide structural stability for the boutons while also allowing for their growth and remodeling. However, a molecular-scale mechanism that explains how neurons appropriately balance these two microtubule populations remains a mystery. We hypothesized that α-tubulin acetyltransferase (αTAT), which both stabilizes long-lived microtubules against mechanical stress via acetylation and has been implicated in promoting microtubule dynamics, could play a role in this process. Using the Drosophila neuromuscular junction as a model, we found that non-enzymatic dαTAT activity limits the growth of synaptic boutons by affecting dynamic, but not stable, microtubules. Loss of dαTAT results in the formation of ectopic boutons. These ectopic boutons can be similarly suppressed by resupplying enzyme-inactive dαTAT or by treatment with a low concentration of the microtubule-targeting agent vinblastine, which acts to suppress microtubule dynamics. Biophysical reconstitution experiments revealed that non-enzymatic αTAT1 activity destabilizes dynamic microtubules but does not substantially impact the stability of long-lived microtubules. Further, during microtubule growth, non-enzymatic αTAT1 activity results in increasingly extended tip structures, consistent with an increased rate of acceleration of catastrophe frequency with microtubule age, perhaps via tip structure remodeling. Through these mechanisms, αTAT enriches for stable microtubules at the expense of dynamic ones. We propose that the specific suppression of dynamic microtubules by non-enzymatic αTAT activity regulates the remodeling of microtubule networks during synaptic bouton development.

Published
2020

41. A brain-penetrant microtubule-targeting agent that disrupts hallmarks of glioma tumorigenesis

Author

Horne, Eric A, primary, Diaz, Philippe, additional, Cimino, Patrick J, additional, Jung, Erik, additional, Xu, Cong, additional, Hamel, Ernest, additional, Wagenbach, Michael, additional, Kumasaka, Debra, additional, Wageling, Nicholas B, additional, Azorín, Daniel D, additional, Winkler, Frank, additional, Wordeman, Linda G, additional, Holland, Eric C, additional, and Stella, Nephi, additional

Published
2020
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43. EXTH-53. A BRAIN-PENETRANT MICROTUBULE-TARGETING AGENT THAT DISRUPTS HALLMARKS OF GLIOMA TUMORIGENESIS

Author

Horne, Eric, primary, Vicente Ruiz, Juan J, additional, Cimino, Patrick, additional, Jung, Erik, additional, Xu, Cong, additional, Diaz, Philippe, additional, Hamel, Ernest, additional, Kumasaka, Debra K, additional, Wagenbach, Michael J, additional, Winkler, Frank, additional, Wordeman, Linda G, additional, Holland, Eric, additional, and Stella, Nephi, additional

Published
2020
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48. Non-enzymatic Activity of the α-Tubulin Acetyltransferase αTAT Limits Synaptic Bouton Growth in Neurons

Author

Coombes, Courtney E., primary, Saunders, Harriet A.J., additional, Mannava, Anirudh G., additional, Johnson-Schlitz, Dena M., additional, Reid, Taylor A., additional, Parmar, Sneha, additional, McClellan, Mark, additional, Yan, Connie, additional, Rogers, Stephen L., additional, Parrish, Jay Z., additional, Wagenbach, Michael, additional, Wordeman, Linda, additional, Wildonger, Jill, additional, and Gardner, Melissa K., additional

Published
2020
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50. Subcellular drug targeting illuminates local kinase action

Author

Bucko, Paula J, primary, Lombard, Chloe K, additional, Rathbun, Lindsay, additional, Garcia, Irvin, additional, Bhat, Akansha, additional, Wordeman, Linda, additional, Smith, F Donelson, additional, Maly, Dustin J, additional, Hehnly, Heidi, additional, and Scott, John D, additional

Published
2019
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