Pharmacology - Chemotherapy agents (MOA, Alkalating, antimetabolites, topoisomerase, antimitotic )

00:14:22
https://www.youtube.com/watch?v=t7QDJOXeux4

Résumé

TLDRThe video explains cancer treatment types, focusing on chemotherapy agents and their mechanisms. It outlines the cell cycle phases (G1, S, G2, M) and the importance of checkpoints in preventing abnormalities. Different chemotherapy classes are discussed: alkylating agents (e.g., cyclophosphamide), antimetabolites (e.g., methotrexate), anti-tumor antibiotics (e.g., doxorubicin), topoisomerase inhibitors (e.g., etoposide), and anti-microtubule agents (e.g., taxanes). Each class targets specific cell cycle phases to minimize side effects. The video emphasizes the need to understand chemotherapy's side effects, which are covered in another video.

A retenir

  • 🎯 Cancer treatment types: surgical, radiation, chemotherapy, biologic therapy
  • 🔬 Goal: Eradicate cancer
  • 🔄 Cell cycle phases: G1, S, G2, M
  • 🛑 Checkpoints prevent abnormalities
  • 🧬 Alkylating agents bind to DNA, causing cross-links
  • 💊 Antimetabolites disrupt DNA/RNA metabolism
  • 🔗 Topoisomerase maintains DNA structure
  • 🚫 Anti-microtubule agents disrupt M phase
  • ⚠️ Side effects of chemotherapy are significant
  • 📚 Further details on side effects in another video

Chronologie

  • 00:00:00 - 00:05:00

    Cancer treatment is categorized into four main types: surgical, radiation therapy, chemotherapy, and biologic therapy, with the primary goal being the eradication of cancer. Each treatment type has potential side effects, and chemotherapy agents are discussed in detail, focusing on their mechanisms of action and how they target different phases of the cell cycle. The cell cycle consists of four phases: G1, S, G2, and M, with checkpoints ensuring no abnormalities occur before progression. Understanding the cell cycle is crucial for comprehending how chemotherapy drugs work, as they target specific phases to disrupt cancer cell growth.

  • 00:05:00 - 00:14:22

    Chemotherapy agents are classified into several categories based on their mechanisms of action. Alkylating agents, such as cyclophosphamide and cisplatin, bind to DNA, causing cross-linking that halts cell division. Antimetabolites disrupt DNA and RNA metabolism, affecting the S phase, with drugs like methotrexate inhibiting key enzymes in nucleotide synthesis. Anti-tumor antibiotics, including anthracyclines, inhibit topoisomerase and helicase, leading to DNA replication issues. Topoisomerase inhibitors target the enzymes responsible for DNA topology, while anti-microtubule agents disrupt the M phase, causing cell arrest. Hormonal agents are also significant but are not covered in detail here. Understanding these mechanisms is essential for recognizing the potential side effects of chemotherapy.

Carte mentale

Vidéo Q&R

  • What are the main types of cancer treatment?

    The main types of cancer treatment are surgical, radiation, chemotherapy, and biologic therapy.

  • What is the goal of cancer treatment?

    The goal of cancer treatment is to eradicate the cancer.

  • What are the phases of the cell cycle?

    The cell cycle has four phases: G1 (growth), S (DNA replication), G2 (preparation for mitosis), and M (mitosis).

  • What are alkylating agents?

    Alkylating agents are chemotherapy drugs that bind to DNA, forming cross-links that prevent normal replication.

  • What do antimetabolites do?

    Antimetabolites disrupt DNA and RNA metabolism, affecting the S phase of the cell cycle.

  • What is the role of topoisomerase in DNA replication?

    Topoisomerase helps relax supercoils in DNA, facilitating proper replication.

  • What are anti-microtubule agents?

    Anti-microtubule agents disrupt the M phase of the cell cycle, leading to cell arrest.

  • What are some examples of chemotherapy agents?

    Examples include cyclophosphamide (alkylating agent), methotrexate (antimetabolite), doxorubicin (anti-tumor antibiotic), and etoposide (topoisomerase inhibitor).

  • What are the side effects of chemotherapy?

    Chemotherapy can cause various side effects, which are discussed in a separate video.

  • What is the significance of cell cycle checkpoints?

    Cell cycle checkpoints ensure there are no abnormalities or damage before the cell progresses to the next phase.

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  • 00:00:05
    cancer treatment is divided into four
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    main types surgical radiation therapy
  • 00:00:11
    chemotherapy and biologic therapy now
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    the goal of cancer treatment is to
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    eradicate the cancer every cancer
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    treatment has the potential to cause
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    harm and treatment may be given that
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    produces toxicity with really no benefit
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    in this video we're gonna talk about
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    chemotherapy agents and their mechanism
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    of action chemotherapy agents have
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    different mechanism action and target
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    different parts of the cell cycle
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    combinations of these chemotherapy
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    agents are preferred because different
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    mechanism action means that they work on
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    different parts of the cell cycle which
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    means that overall less side effects in
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    order to understand how chemotherapy
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    drugs chemotherapy agents work we
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    firstly have to revise the cell cycle
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    the cell cycle has four phases the
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    growth one phase or the g1 phase where
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    the organelles duplicate the S phase
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    which is where the DNA basically
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    replication occurs the growth 2 phase is
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    when the cell prepares itself for the M
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    phase which is mitosis where the cell
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    divides into two identical daughter
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    cells then the cell cycle will repeat
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    itself we can further explore mitosis
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    mitosis has other phases the prophase is
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    where the centrosome duplicates and form
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    these microtubules in metaphase the
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    chromosomes the DNA really align in the
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    middle of the cell and the microtubules
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    that were formed from the centrosome
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    attach to the centromeres which are the
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    center points of the chromosomes in
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    anaphase the chromosomes are separated
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    and reach either end of the cell in
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    chilla phase the cell membrane
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    constricts ready to separate and then a
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    new nuclear membrane
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    is being formed the cell cycle is a
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    continuous process and so you have
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    checkpoints during the cell cycle to
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    make sure that there are no
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    abnormalities in the cell before it
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    progresses to each phase these
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    checkpoints include the g1 checkpoint
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    the g2 checkpoint and the M phase
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    checkpoint one thing these checkpoints
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    look at is whether there are
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    abnormalities damage or mutations to the
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    DNA for example DNA is a double helix
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    structure composed of four nucleotides
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    after the g1 phase where the organelles
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    are duplicate comes the S phase now in
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    the S phase DNA becomes replicated now
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    let's revise this process during
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    replication the DNA strand is separated
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    by an enzyme called helicase during the
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    unwinding of DNA tension can occur
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    distally the tensions are these coils
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    that are being formed the cells have a
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    normal biological mechanism to fix these
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    coils and super coils that are being
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    formed this mechanism is an enzyme
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    called topoisomerase here topoisomerase
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    to fixes these super coils reducing the
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    tension in the DNA strand and we'll talk
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    about topoisomerase later on now there
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    are four types of nucleotides as
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    mentioned in DNA these nucleotides can
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    be divided into two groups pyrimidine
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    and purine pyrimidine includes thymine
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    and cytosine and purines include adenine
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    and guanine so what happens is a
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    double-stranded DNA gets unwind by
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    helicase into two separate strips
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    another enzyme called DNA polymerase
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    will create a new strand on both strips
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    the new strand following the helicase is
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    the leading strand the lagging strand is
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    the Strand that is created in segments
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    chemotherapy agents target different
  • 00:04:32
    parts of the cell cycle as mentioned
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    because of this they are grouped into
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    different classes let's take a look at
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    the different classes one at a time
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    first let's begin with alkylating agents
  • 00:04:45
    the oldest anti-cancer cytotoxic s-- now
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    these agents are antiproliferative drugs
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    they work by binding covalently via
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    alkyl groups to DNA they then form cross
  • 00:04:58
    links and thought to arrest the cell
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    cycle in the g1 or the S phase of the
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    cell cycle
  • 00:05:04
    now the alkylating agents actually bind
  • 00:05:07
    to the nucleotide guanine once bound
  • 00:05:10
    they form cross linkage of DNA strands
  • 00:05:13
    broken or cross-linked DNA is
  • 00:05:18
    intrinsically unable to complete normal
  • 00:05:21
    replication or cell division so they
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    undergo cell arrest they stop because
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    they're in cell arrest the cell will
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    then either be repaired so it can
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    proceed progress through the cell cycle
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    or this cell will undergo apoptosis
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    basically dying examples of drugs in the
  • 00:05:43
    class of alkylating agents include
  • 00:05:45
    nitrogen mustards such as
  • 00:05:47
    cyclophosphamide and there's also
  • 00:05:50
    cisplatin now cisplatin
  • 00:05:52
    is an interesting drug it is one of the
  • 00:05:55
    most active anti-cancer drugs and used
  • 00:05:57
    on many types of cancers but also come
  • 00:06:01
    with many toxicities it is it is
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    actually its own class but has similar
  • 00:06:06
    mechanism of action to alkylating agents
  • 00:06:09
    and so it is put in this category the
  • 00:06:12
    next class of chemotherapy agents are
  • 00:06:14
    the anti metabolites or the
  • 00:06:16
    antimetabolites these guys interfere
  • 00:06:19
    with normal cell metabolism of nucleic
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    acids so really they disrupt DNA RNA
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    metabolism production interrupting the S
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    phase of the cell cycle we will focus on
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    DNA metabolism here and the four
  • 00:06:34
    nucleotides for DNA are thymine cytosine
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    adenine and guanine of which thymine is
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    strictly DNA
  • 00:06:42
    I mean the DNA nucleotide is made after
  • 00:06:45
    a series of reactions one important
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    reaction is from D UMP to D TMP this
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    reaction is carried out by an enzyme
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    called fireman delayed synthase for D
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    UMP to convert to dtmp requires a
  • 00:07:05
    co-current reaction which phiman delayed
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    synthase also carries out this is the
  • 00:07:12
    conversion between methylene
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    tetrahydrofolate to dihydrofolate so
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    Thermolite synthase catalyzes methylene
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    tetrahydrofolate and D UMP to form
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    dihydrofolate and the TMP dihydrofolate
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    is converted to tetrahydrofolate by
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    another important enzyme dihydrofolate
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    reductase
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    tetrahydrofolate becomes methyl
  • 00:07:43
    tetrahydrofolate once again so this
  • 00:07:47
    whole reaction involving these two
  • 00:07:49
    enzymes thermo delayed synthase and
  • 00:07:51
    dihydrofolate reductase it's important
  • 00:07:53
    in order to make DNA by interrupting any
  • 00:07:57
    of these two enzymes you are essentially
  • 00:07:59
    disrupting thymine thymidine synthesis
  • 00:08:02
    and thus DNA synthesis a few
  • 00:08:08
    chemotherapy agents work here
  • 00:08:10
    these include five floral uracil which
  • 00:08:13
    inhibits the mid-late synthase and also
  • 00:08:16
    specific time a delayed synthesis
  • 00:08:18
    inhibitors a very common drug used in
  • 00:08:21
    rheumatoid arthritis also is a
  • 00:08:23
    chemotherapy drug and an ectopic
  • 00:08:26
    pregnancy drug this drug is methotrexate
  • 00:08:29
    and it works by inhibiting
  • 00:08:31
    dihydrofolate reductase other
  • 00:08:34
    chemotherapy agents that work
  • 00:08:36
    specifically on disrupting purine
  • 00:08:38
    metabolism and synthesis include or
  • 00:08:41
    CAPTA purine and theö guanine here in
  • 00:08:45
    summary antimetabolites work by
  • 00:08:49
    disrupting DNA RNA metabolism and
  • 00:08:53
    production and thus it will disrupt
  • 00:08:56
    cancer cells from progressing through
  • 00:08:58
    the cell cycle
  • 00:09:00
    the next class are anti-tumor
  • 00:09:04
    antibiotics main ones include a group
  • 00:09:07
    called anthracyclines these antibiotics
  • 00:09:10
    have several mechanism of action but
  • 00:09:13
    their specific mechanism action is
  • 00:09:16
    unclear
  • 00:09:19
    one effect is at these anti-tumor
  • 00:09:22
    antibiotics inhibits topoisomerase to
  • 00:09:25
    remember topoisomerase are important
  • 00:09:28
    enzymes in maintaining the structure
  • 00:09:30
    that topology of DNA topoisomerase to
  • 00:09:33
    remember relaxes super coils by breaking
  • 00:09:36
    two DNA strands unwinding it relaxing it
  • 00:09:40
    and then attaching it back together once
  • 00:09:42
    it's unwound and so by inhibiting
  • 00:09:46
    topoisomerase DNA doesn't relax and so
  • 00:09:49
    replication becomes hard with the super
  • 00:09:50
    coils or maybe the topoisomerase breaks
  • 00:09:55
    the DNA strand but then can't really
  • 00:09:56
    attach it back together
  • 00:09:58
    either way DNA replication is inhibited
  • 00:10:00
    and the cell doesn't progress through
  • 00:10:02
    the cell cycle another way antibiotics
  • 00:10:06
    work is by inhibiting helicase the
  • 00:10:08
    enzyme which unwinds the DNA by
  • 00:10:11
    inhibiting this enzyme you inhibit DNA
  • 00:10:13
    replication finally antibiotics such as
  • 00:10:16
    anthracyclines induce reactive oxygen
  • 00:10:18
    species formation causing destruction of
  • 00:10:21
    the cell and triggering apoptosis
  • 00:10:25
    examples of anthracyclines include
  • 00:10:27
    doxorubicin and donor ribbon
  • 00:10:32
    the next class of chemotherapy drugs are
  • 00:10:35
    the topoisomerase inhibitors
  • 00:10:37
    topoisomerase remember our essential
  • 00:10:40
    enzymes in regulating the topology of
  • 00:10:42
    DNA helix there are two types of
  • 00:10:45
    topoisomerase there's top are summaries
  • 00:10:47
    one and there's topoisomerase to which
  • 00:10:50
    we have already talked about
  • 00:10:52
    topoisomerase one cleaves only one
  • 00:10:56
    strand of the DNA and relaxes DNA coil
  • 00:11:00
    during replication example is here is a
  • 00:11:04
    DNA double helix the top where somewhere
  • 00:11:06
    is one will click one strand
  • 00:11:11
    and then unwind it and attach it causing
  • 00:11:16
    one less coil topoisomerase to as
  • 00:11:20
    mentioned cleaves two strands of the DNA
  • 00:11:23
    helix and relaxes supercoils during DNA
  • 00:11:26
    replication which again we've already
  • 00:11:29
    talked about topoisomerase one
  • 00:11:32
    inhibitors inhibit topoisomerase one and
  • 00:11:36
    thus inhibits the relaxation of DNA and
  • 00:11:39
    thus potentially inhibits proper DNA
  • 00:11:43
    replication example of this chemotherapy
  • 00:11:47
    agent is cam 2 thus in topoisomerase two
  • 00:11:52
    inhibitors we already talked about and
  • 00:11:54
    include etoposide
  • 00:12:03
    you
  • 00:12:05
    the next chemotherapy class work on the
  • 00:12:09
    M phase of the cell cycle and are called
  • 00:12:11
    the anti microtubule agents these guys
  • 00:12:14
    disrupt the M phase of the cell cycle
  • 00:12:17
    leading to cell arrest which then will
  • 00:12:20
    lead to apoptosis these are the taxanes
  • 00:12:23
    and the vinca alkaloids let's just
  • 00:12:26
    quickly recap the M phase to understand
  • 00:12:29
    how these anti microtubule agents work
  • 00:12:33
    the M phase consists of the prophase
  • 00:12:36
    metaphase anaphase and telophase during
  • 00:12:40
    early mitosis microtubules are extending
  • 00:12:44
    from the centrosomes and attach to the
  • 00:12:46
    centromeres of the chromosome the
  • 00:12:49
    microtubules allow for the separation of
  • 00:12:53
    duplicated DNA into either side of the
  • 00:12:56
    cell before the microtubules start
  • 00:12:59
    degrading and breaking down vinca
  • 00:13:03
    alkaloids inhibit microtubule assembly
  • 00:13:06
    or formation and so are known as
  • 00:13:10
    microtubule destabilizes without no
  • 00:13:15
    microtubules forming this will disrupt
  • 00:13:17
    the M phase causing cell arrest
  • 00:13:24
    the other group of anti microtubules are
  • 00:13:27
    the taxanes these guys bind to and
  • 00:13:30
    stabilize the microtubules that are
  • 00:13:33
    already formed in the M phase and so
  • 00:13:36
    these guys are called the microtubule
  • 00:13:38
    stabilizers they basically inhibit the
  • 00:13:42
    breakdown of the microtubules once they
  • 00:13:45
    are formed and so you don't complete the
  • 00:13:47
    M phase of the cell cycle which means
  • 00:13:49
    you get M phase arrest you get cell
  • 00:13:52
    arrest the other important class of
  • 00:13:55
    chemotherapy agents are the hormonal
  • 00:13:57
    agents which are not discussed here
  • 00:13:59
    because there are many times hopefully a
  • 00:14:02
    separate video will look into this thank
  • 00:14:04
    you for watching I hope this helped
  • 00:14:07
    thank you for watching finally it's very
  • 00:14:09
    important to understand the side effects
  • 00:14:12
    of chemotherapy agents I have a separate
  • 00:14:14
    video on that which looks at the side
  • 00:14:16
    effects the acute side effects of
  • 00:14:18
    chemotherapy agents thank you for
  • 00:14:20
    watching
Tags
  • cancer treatment
  • chemotherapy
  • cell cycle
  • alkylating agents
  • antimetabolites
  • anti-tumor antibiotics
  • topoisomerase inhibitors
  • anti-microtubule agents
  • side effects
  • mechanism of action