Microtubule Inhibitors Mechanism of Action
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🔬 Understanding Microtubules:
Microtubules are dynamic protein structures essential for various cellular processes, especially cell division. Imagine them as the intricate scaffolding that guides the construction of new cells. Microtubule inhibitors disrupt this process, exerting a potent anti-cancer effect.
Vinca alkaloids, such as vincristine and vinblastine, exert their effects on cells by interfering with microtubule dynamics, which are crucial for cell division and various other cellular processes. Microtubules are dynamic protein structures formed by the polymerization of tubulin protein subunits, and they play a vital role in maintaining cell shape, intracellular transport, and segregation of chromosomes during cell division. The molecular mechanism of vinca alkaloids involves their interaction with microtubules, leading to disruption of these processes. Here's a breakdown of the mechanism:
1. Microtubule Disruption:
Vinca alkaloids bind to the β-tubulin subunits of microtubules, specifically at a site on the tubulin molecule called the vinca-binding domain. This binding prevents the assembly of tubulin subunits into microtubules and interferes with the stability of existing microtubules. As a result, microtubules become shorter and less organized.
2. Mitotic Arrest:
During cell division (mitosis), microtubules are responsible for capturing and segregating chromosomes into daughter cells. By disrupting microtubule dynamics, vinca alkaloids prevent the proper formation of the mitotic spindle, which is essential for chromosome segregation. This leads to a delay or arrest of cells in the metaphase stage of mitosis.
3. Inhibition of Cell Division:
Due to the disruption of microtubule dynamics and the mitotic spindle, cells treated with vinca alkaloids cannot complete the process of cell division. This results in the inhibition of cell proliferation. This effect is particularly pronounced in rapidly dividing cells, such as cancer cells, making vinca alkaloids valuable chemotherapy agents.
4. Induction of Apoptosis:
In addition to the mitotic arrest, vinca alkaloids can trigger a pathway leading to apoptosis, or programmed cell death. Cells that are unable to progress through mitosis due to microtubule disruption may activate cell death pathways to eliminate themselves, preventing the formation of abnormal or non-viable daughter cells.
Overall, the disruption of microtubule dynamics and the consequent effects on mitosis and cell division are key to the therapeutic action of vinca alkaloids. However, it's worth noting that while these alkaloids target rapidly dividing cells like cancer cells, they can also affect normal cells that undergo rapid division, leading to potential side effects commonly associated with chemotherapy.
Taxanes, such as paclitaxel and docetaxel, are chemotherapy drugs that work by targeting microtubules, which are crucial structures for various cellular processes, particularly cell division. Taxanes exert their effects by stabilizing microtubules, leading to disruptions in the normal dynamics of these structures. Here's how taxanes work at a molecular level:
1. Microtubule Stabilization:
Taxanes bind to a specific site on the β-tubulin subunit of microtubules. This binding promotes and stabilizes the assembly of tubulin subunits into microtubules, preventing their disassembly. Normally, microtubules undergo dynamic instability, a process involving continuous cycles of growth and shrinkage. Taxanes freeze microtubules in a polymerized state, making them more resistant to disassembly.
2. Formation of Aberrant Microtubule Bundles:
Due to the stabilization caused by taxanes, microtubules become locked in a stable polymerized state. This results in the formation of bundles of microtubules within the cell. These bundles are structurally different from the dynamic and organized microtubules required for normal cell division processes.
3. Mitotic Arrest and Cellular Effects:
As microtubules are essential for proper chromosome segregation during cell division (mitosis), the abnormal microtubule bundles formed by taxanes disrupt the mitotic spindle formation. This disruption leads to mitotic arrest, where cells are unable to progress through the stages of mitosis. This mitotic arrest triggers a signaling cascade that eventually leads to programmed cell death, or apoptosis.
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Have questions or topics you'd like us to cover? Leave a comment below, and don't forget to hit the like button if you found this video insightful.
[Disclaimer: This video is intended for educational purposes only. Consult a healthcare professional for personalized medical advice.]
1) "Cancer Signaling Pathways and Targeted Therapies"
- https://www.udemy.com/course/cancer-b...
🔬 Understanding Microtubules:
Microtubules are dynamic protein structures essential for various cellular processes, especially cell division. Imagine them as the intricate scaffolding that guides the construction of new cells. Microtubule inhibitors disrupt this process, exerting a potent anti-cancer effect.
Vinca alkaloids, such as vincristine and vinblastine, exert their effects on cells by interfering with microtubule dynamics, which are crucial for cell division and various other cellular processes. Microtubules are dynamic protein structures formed by the polymerization of tubulin protein subunits, and they play a vital role in maintaining cell shape, intracellular transport, and segregation of chromosomes during cell division. The molecular mechanism of vinca alkaloids involves their interaction with microtubules, leading to disruption of these processes. Here's a breakdown of the mechanism:
1. Microtubule Disruption:
Vinca alkaloids bind to the β-tubulin subunits of microtubules, specifically at a site on the tubulin molecule called the vinca-binding domain. This binding prevents the assembly of tubulin subunits into microtubules and interferes with the stability of existing microtubules. As a result, microtubules become shorter and less organized.
2. Mitotic Arrest:
During cell division (mitosis), microtubules are responsible for capturing and segregating chromosomes into daughter cells. By disrupting microtubule dynamics, vinca alkaloids prevent the proper formation of the mitotic spindle, which is essential for chromosome segregation. This leads to a delay or arrest of cells in the metaphase stage of mitosis.
3. Inhibition of Cell Division:
Due to the disruption of microtubule dynamics and the mitotic spindle, cells treated with vinca alkaloids cannot complete the process of cell division. This results in the inhibition of cell proliferation. This effect is particularly pronounced in rapidly dividing cells, such as cancer cells, making vinca alkaloids valuable chemotherapy agents.
4. Induction of Apoptosis:
In addition to the mitotic arrest, vinca alkaloids can trigger a pathway leading to apoptosis, or programmed cell death. Cells that are unable to progress through mitosis due to microtubule disruption may activate cell death pathways to eliminate themselves, preventing the formation of abnormal or non-viable daughter cells.
Overall, the disruption of microtubule dynamics and the consequent effects on mitosis and cell division are key to the therapeutic action of vinca alkaloids. However, it's worth noting that while these alkaloids target rapidly dividing cells like cancer cells, they can also affect normal cells that undergo rapid division, leading to potential side effects commonly associated with chemotherapy.
Taxanes, such as paclitaxel and docetaxel, are chemotherapy drugs that work by targeting microtubules, which are crucial structures for various cellular processes, particularly cell division. Taxanes exert their effects by stabilizing microtubules, leading to disruptions in the normal dynamics of these structures. Here's how taxanes work at a molecular level:
1. Microtubule Stabilization:
Taxanes bind to a specific site on the β-tubulin subunit of microtubules. This binding promotes and stabilizes the assembly of tubulin subunits into microtubules, preventing their disassembly. Normally, microtubules undergo dynamic instability, a process involving continuous cycles of growth and shrinkage. Taxanes freeze microtubules in a polymerized state, making them more resistant to disassembly.
2. Formation of Aberrant Microtubule Bundles:
Due to the stabilization caused by taxanes, microtubules become locked in a stable polymerized state. This results in the formation of bundles of microtubules within the cell. These bundles are structurally different from the dynamic and organized microtubules required for normal cell division processes.
3. Mitotic Arrest and Cellular Effects:
As microtubules are essential for proper chromosome segregation during cell division (mitosis), the abnormal microtubule bundles formed by taxanes disrupt the mitotic spindle formation. This disruption leads to mitotic arrest, where cells are unable to progress through the stages of mitosis. This mitotic arrest triggers a signaling cascade that eventually leads to programmed cell death, or apoptosis.
📣 Connect with Us:
Have questions or topics you'd like us to cover? Leave a comment below, and don't forget to hit the like button if you found this video insightful.
[Disclaimer: This video is intended for educational purposes only. Consult a healthcare professional for personalized medical advice.]
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