Your search keyword '"Moutinho Santos"' showing total 4 results

1. A tumor suppressor role of the Bub3 spindle checkpoint protein after apoptosis inhibition

Author

Claudio E. Sunkel, Sara Morais da Silva, Tatiana Moutinho-Santos, Morais da Silva, Sara [0000-0001-8337-9893], Moutinho-Santos, Tatiana [0000-0002-9880-9507], Sunkel, Claudio E [0000-0002-2963-9380], and Apollo - University of Cambridge Repository

Subjects

Cell cycle checkpoint, BUB3, Aneuploidy, Apoptosis, Cell Cycle Proteins, Biology, medicine.disease_cause, 03 medical and health sciences, 0302 clinical medicine, Report, medicine, Animals, Drosophila Proteins, Kinetochores, Mitosis, Research Articles, 030304 developmental biology, 0303 health sciences, Kinetochore, Tumor Suppressor Proteins, fungi, Cell Biology, medicine.disease, 3. Good health, Cell biology, Transplantation, Spindle checkpoint, Cell Transformation, Neoplastic, Drosophila melanogaster, Imaginal Discs, Gene Knockdown Techniques, 030220 oncology & carcinogenesis, Mad2 Proteins, Carcinogenesis

Abstract

The loss of the spindle checkpoint protein Bub3 is sufficient to induce aneuploidy and drive tumorigenesis when apoptosis is compromised., Most solid tumors contain aneuploid cells, indicating that the mitotic checkpoint is permissive to the proliferation of chromosomally aberrant cells. However, mutated or altered expression of mitotic checkpoint genes accounts for a minor proportion of human tumors. We describe a Drosophila melanogaster tumorigenesis model derived from knocking down spindle assembly checkpoint (SAC) genes and preventing apoptosis in wing imaginal discs. Bub3-deficient tumors that were also deficient in apoptosis displayed neoplastic growth, chromosomal aneuploidy, and high proliferative potential after transplantation into adult flies. Inducing aneuploidy by knocking down CENP-E and preventing apoptosis does not induce tumorigenesis, indicating that aneuploidy is not sufficient for hyperplasia. In this system, the aneuploidy caused by a deficient SAC is not driving tumorigenesis because preventing Bub3 from binding to the kinetochore does not cause hyperproliferation. Our data suggest that Bub3 has a nonkinetochore-dependent function that is consistent with its role as a tumor suppressor.

Published

2013

2. A tumor suppressor role of the Bub3 spindle checkpoint protein after apoptosis inhibition

Author

Morais da Silva, Sara, primary, Moutinho-Santos, Tatiana, additional, and Sunkel, Claudio E., additional

Published

2013

3. A tumor suppressor role of the Bub3 spindle checkpoint protein after apoptosis inhibition.

Author

da Silva, Sara Morais, Moutinho-Santos, Tatiana, and Sunkel, Claudio E.

Subjects

*TUMORS, *ANEUPLOIDY, *DROSOPHILA melanogaster, *CARCINOGENESIS, *CELL proliferation

Abstract

Most solid tumors contain aneuploid cells, indicating that the mitotic checkpoint is permissive to the proliferation of chromosomally aberrant cells. However, mutated or altered expression of mitotic checkpoint genes accounts for a minor proportion of human tumors. We describe a Drosophila melanogaster tumorigenesis model derived from knocking down spindle assembly checkpoint (SAC) genes and preventing apoptosis in wing imaginal discs. Bub3-deficient tumors that were also deficient in apoptosis displayed neoplastic growth, chromosomal aneuploidy, and high proliferative potential after transplantation into adult flies. Inducing aneuploidy by knocking down CENP-E and preventing apoptosis does not induce tumorigenesis, indicating that aneuploidy is not sufficient for hyperplasia. In this system, the aneuploidy caused by a deficient SAC is not driving tumorigenesis because preventing Bub3 from binding to the kinetochore does not cause hyperproliferation. Our data suggest that Bub3 has a nonkinetochore-dependent function that is consistent with its role as a tumor suppressor. [ABSTRACT FROM AUTHOR]

Published

2013

4. CLASP2 binding to curved microtubule tips promotes flux and stabilizes kinetochore attachments.

Author

Girão, Hugo, Naoyuki Okada, Rodrigues, Tony A., Silva, Alexandra O., Figueiredo, Ana C., Garcia, Zaira, Moutinho-Santos, Tatiana, Ikuko Hayashi, Azevedo, Jorge E., Macedo-Ribeiro, Sandra, and Maiato, Helder

Subjects

*MICROTUBULES, *KINETOCHORE, *CHROMOSOME segregation, *TUBULINS, *FLUX (Energy), *MITOSIS

Abstract

CLASPs are conserved microtubule plus-end-tracking proteins that suppress microtubule catastrophes and independently localize to kinetochores during mitosis. Thus, CLASPs are ideally positioned to regulate kinetochore-microtubule dynamics required for chromosome segregation fidelity, but the underlying mechanism remains unknown. Here, we found that human CLASP2 exists predominantly as a monomer in solution, but it can self-associate through its C-terminal kinetochore-binding domain. Kinetochore localization was independent of self-association, and driving monomeric CLASP2 to kinetochores fully rescued normal kinetochore-microtubule dynamics, while partially sustaining mitosis. CLASP2 kinetochore localization, recognition of growing microtubule plus-ends through EB-protein interaction, and the ability to associate with curved microtubule protofilaments through TOG2 and TOG3 domains independently sustained normal spindle length, timely spindle assembly checkpoint satisfaction, chromosome congression, and faithful segregation. Measurements of kinetochore-microtubule half-life and poleward flux revealed that CLASP2 regulates kinetochore-microtubule dynamics by integrating distinctive microtubulebinding properties at the kinetochore-microtubule interface. We propose that kinetochore CLASP2 suppresses microtubule depolymerization and detachment by binding to curved protofilaments at microtubule plus-ends. [ABSTRACT FROM AUTHOR]

Published

2020