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The Global ETD Search service is a free service for researchers
to find electronic theses and dissertations. This service is
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Networked Digital Library of Theses and Dissertations.
Our metadata is collected from universities around the world. If you manage a university/consortium/country archive and want to be added, details can be found on the NDLTD website.
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Showing 11 to 20 of 34 (0.046 seconds)Spelling suggestions: "subject:"inwebassembly checkpoint"" "subject:"possible.assembly checkpoint""
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Characterizing BUBR1 interactions with MAD2 and p31comet during the Mitotic CheckpointLaBelle, Jenna J. January 2018 (has links)
No description available.
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| 12 |
TRIP13 AAA-ATPase Promotes Spindle Assembly Checkpoint Activation through Coordinating with MAD1 at Unattached KinetochoresArnst, Christopher Edward 04 September 2019 (has links)
No description available.
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| 13 |
Spindle Assembly Checkpoint Stability Depends on Integrity of the Nucleolus and Septins in <i>Saccharomyces cerevisiae</i>Rai, Urvashi 05 June 2017 (has links)
No description available.
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| 14 |
The Regulation of Sororin by PhosphorylationDreier, Megan Renee 26 June 2012 (has links)
No description available.
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| 15 |
How to Assemble a Functional Mitotic Checkpoint ComplexTipton, Aaron R. 20 September 2012 (has links)
No description available.
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| 16 |
Functional interactions between the Arabidopsis homologs of spindle assembly checkpoint proteins MAD1 and MAD2 and the nucleoporin NUADing, Dongfeng January 2011 (has links)
No description available.
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| 17 |
Changes in Kinetochore Structure and Molecular Composition in Response to Mis-attachmentShen, Muyao 18 July 2011 (has links)
Each mitotic chromosome is constituted by two sister chromatids whose correct segregation to the daughter cells is ensured by amphitelic attachment, in which the two sister kinetochores (KTs) are attached to microtubules (MTs) from opposite mitotic spindle poles. KT mis-attachments can occur in early mitosis and cause chromosome mis-segregation and aneuploidy if not corrected. These mis-attachments include monotelic (one attached and one unattached sister KT), syntelic (both sister KTs attached to the same spindle pole), and merotelic (a single KT attached to MTs from opposite spindle poles) attachments. A biochemical pathway named the Spindle Assembly Checkpoint (SAC) is responsible for delaying anaphase onset to allow correction of KT mis-attachments. SAC activation is believed to occur due to KT localization of certain SAC proteins and/or lack of tension, but only monotelic attachment has been proven to activate the SAC. To determine if and how other KT mis-attachments may activate the SAC, we studied how molecular composition and structure of the KT changes in response to different types of attachments. Our data suggest that monotelic attachment is the only type of attachment that can induce a SAC response thanks to the accumulation of the SAC protein Mad2 at the KT. Our data also indicate that structural changes of the KT, measured as intra- or inter-KT stretching, do not directly induce a SAC response. Instead, our findings suggest decreased KT stretching, especially in inter-KT stretching of syntelic chromosomes, may play a key role in bringing MCAK and other KT substrates closer to Aurora B kinase for rapid and efficient correction of KT mis-attachments. / Master of Science
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| 18 |
Involvement of Nlrp5 in the Maintenance of Genome Integrity in Murine OocytesVelummailum, Russanthy 25 August 2011 (has links)
Nlrp5, a maternal-effect gene, is required for embryonic progression and female fertility in mice. Previous work indicated an age-related decline in Nlrp5 transcripts in murine oocytes. As maternal age is associated with increased spindle organization defects, studies in this thesis focused on the analysis of meiotic spindle defects in oocytes of Nlrp5-deficient mice. NALP5 protein showed a novel kinetochore-localization pattern, which was disturbed by spindle poisons. Nlrp5-deficient oocytes displayed a higher frequency of spindle abnormalities and chromosomal misalignment. Upon fertilization, these defects translated into increased incidences of multinucleation. As these phenotypes are associated with deficiencies in genome stability, we examined spindle assembly checkpoint (SAC) components. We found that numerous SAC proteins were dysregulated, implying that NALP5 may be critical in sensing oocyte-related SAC defects. We found that Nlrp5-deficient oocytes may have increased DNA damage. Thus, Nlrp5 may be an integral component responsible for preservation of genome integrity in female gametes.
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| 19 |
Involvement of Nlrp5 in the Maintenance of Genome Integrity in Murine OocytesVelummailum, Russanthy 25 August 2011 (has links)
Nlrp5, a maternal-effect gene, is required for embryonic progression and female fertility in mice. Previous work indicated an age-related decline in Nlrp5 transcripts in murine oocytes. As maternal age is associated with increased spindle organization defects, studies in this thesis focused on the analysis of meiotic spindle defects in oocytes of Nlrp5-deficient mice. NALP5 protein showed a novel kinetochore-localization pattern, which was disturbed by spindle poisons. Nlrp5-deficient oocytes displayed a higher frequency of spindle abnormalities and chromosomal misalignment. Upon fertilization, these defects translated into increased incidences of multinucleation. As these phenotypes are associated with deficiencies in genome stability, we examined spindle assembly checkpoint (SAC) components. We found that numerous SAC proteins were dysregulated, implying that NALP5 may be critical in sensing oocyte-related SAC defects. We found that Nlrp5-deficient oocytes may have increased DNA damage. Thus, Nlrp5 may be an integral component responsible for preservation of genome integrity in female gametes.
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| 20 |
The implication of Kv10.1 in the regulation of G2/M progressionMovsisyan, Naira 16 May 2019 (has links)
No description available.
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