Scribd Logo
Upload

Welcome to Scribd!

  • 99 views

    ABBAS BAB 2 Innate Immunity

    Uploaded by

    Aulia Ayu Puspita
    - Innate immunity is the first line of defense against microbes and exists before microbes arrive. Its components include epithelial barriers, leukocytes (neutrophils, macrophages, NK cells), circulating effector proteins (complement, collectins, pentraxins), and cytokines. - Innate immune cells recognize pathogens through pattern recognition receptors (PRRs) like Toll-like receptors (TLRs) that detect pathogen-associated molecular patterns (PAMPs) shared by microbes. - Activation of innate immunity stimulates adaptive immune responses through upregulation of costimulatory molecules and cytokine production to provide signals needed for lymphocyte activation.

    Copyright:

    © All Rights Reserved
    Download as PPT, PDF, TXT or read online from Scribd

    ABBAS BAB 2 Innate Immunity

    Uploaded by

    Aulia Ayu Puspita
    99 views28 pages
    - Innate immunity is the first line of defense against microbes and exists before microbes arrive. Its components include epithelial barriers, leukocytes (neutrophils, macrophages, NK cells), circulating effector proteins (complement, collectins, pentraxins), and cytokines. - Innate immune cells recognize pathogens through pattern recognition receptors (PRRs) like Toll-like receptors (TLRs) that detect pathogen-associated molecular patterns (PAMPs) shared by microbes. - Activation of innate immunity stimulates adaptive immune responses through upregulation of costimulatory molecules and cytokine production to provide signals needed for lymphocyte activation.

    Original Description:

    ABBAS BAB 2

    Copyright

    © © All Rights Reserved

    Available Formats

    PPT, PDF, TXT or read online from Scribd

    Did you find this document useful?

    Is this content inappropriate?

    - Innate immunity is the first line of defense against microbes and exists before microbes arrive. Its components include epithelial barriers, leukocytes (neutrophils, macrophages, NK cells), circulating effector proteins (complement, collectins, pentraxins), and cytokines. - Innate immune cells recognize pathogens through pattern recognition receptors (PRRs) like Toll-like receptors (TLRs) that detect pathogen-associated molecular patterns (PAMPs) shared by microbes. - Activation of innate immunity stimulates adaptive immune responses through upregulation of costimulatory molecules and cytokine production to provide signals needed for lymphocyte activation.

    Copyright:

    © All Rights Reserved
    Download as PPT, PDF, TXT or read online from Scribd
    Download as ppt, pdf, or txt
    99 views28 pages

    ABBAS BAB 2 Innate Immunity

    Uploaded by

    Aulia Ayu Puspita
    - Innate immunity is the first line of defense against microbes and exists before microbes arrive. Its components include epithelial barriers, leukocytes (neutrophils, macrophages, NK cells), circulating effector proteins (complement, collectins, pentraxins), and cytokines. - Innate immune cells recognize pathogens through pattern recognition receptors (PRRs) like Toll-like receptors (TLRs) that detect pathogen-associated molecular patterns (PAMPs) shared by microbes. - Activation of innate immunity stimulates adaptive immune responses through upregulation of costimulatory molecules and cytokine production to provide signals needed for lymphocyte activation.

    Copyright:

    © All Rights Reserved
    Download as PPT, PDF, TXT or read online from Scribd
    Download as ppt, pdf, or txt
    of 28

    BAB 2

    INNATE IMMUNITY
    Features of Innate Immune recognation.
    Components of the Innate Immune system
    Role of Innate Immunity in stimulating
    Adaptive Immune Responses
    Summary.

    Specificity of Innate and Adaptive Immunity

    Innate Immunity

    Adaptive immunity

    SPECIFICITY
    Greater diversity

    Limited diversity

    RECEPTORS

    NONCLONAL DISTRIBUTION

    CLONAL DISTRIBUTION

    Toll-like Receptors (TLRs)

    Figure 2-1 Cellular locations of pattern


    recognition molecules of the innate immune
    system. Some pattern recognition molecules of
    the TLR family (see Fig. 2-7), such as TLRs 2, 4,
    and 5, are expressed on the cell surface, where
    they may bind extracellular pathogen-associated
    molecular patterns. Other TLRs are expressed
    on endosomal membranes, such as TLRs 3, 7,
    8, and 9, all of which can recognize nucleic
    acids of microbes that have been phagocytosed
    by cells. Cells also contain cytoplasmic sensors
    of microbial infection (discussed later in the
    chapter), including the NLR family of proteins,
    which recognize bacterial peptidoglycans, and a
    subset of CARD family of proteins, which bind
    viral RNA

    TOLL-LIKE RECEPTOR
    STRUCTURE AND
    SIGNALING PATHWAYS

    Figure 2-2 Mammalian TLRs: specificities,


    basic signaling mechanisms, and cellular
    responses.
    Ligands for TLRs are shown together with
    dimers of the TLRs that specially bind them.
    Note that some TLRs are expressed in
    endosomes and some on the cell surface (see
    Fig. 2-7). The basic steps in TLR signaling,
    illustrated only for TLR3 and TLR4, are
    applicable to all TLRs. Further details about
    the signaling pathways are described in Box 21.

    Components of the Innate Immune System


    Figure 2-3 Epithelial
    barriers.
    Epithelia at the portals of
    entry of microbes provide
    physical barriers,
    produce antimicrobial
    substances, and harbor
    intraepithelial
    lymphocytes that are
    believed to kill microbes
    and infected cells.

    Figure 2-4 Morphology of neutrophils. The light micrograph of a


    blood neutrophil shows the multilobed nucleus, because of which
    these cells are also called polymorphonuclear leukocytes, and the faint
    cytoplasmic granules

    Figure 2-5 Maturation of mononuclear phagocytes. Mononuclear


    phagocytes develop in the bone marrow, circulate in the blood as
    monocytes, and are resident in all tissues of the body as
    macrophages. They may differentiate into specialized forms in
    particular tissues. CNS, central nervous system

    blood monocytes

    blood monocytes

    Tissue macrophage

    Figure 2-6 Morphology of mononuclear phagocytes. A. Light micrograph of a monocyte in a peripheral blood
    smear. B. Electron micrograph of a peripheral blood monocyte. (Courtesy of Dr. Noel Weidner, Department of
    Pathology, University of California, San Diego.) C. Electron micrograph of an activated tissue macrophage
    showing numerous phagocytic vacuoles and cytoplasmic organelles. (From Fawcett DW. Bloom & Fawcett's
    Textbook of Histology, 12th ed. Chapman & Hall, 1994. With kind permission of Springer Science and Business
    Media.)

    RECRUITMENT OF LEUCOCYTES

    Figure 2-7 Recruitment of leukocytes. At sites of infection, macrophages that have encountered microbes
    produce cytokines (such as TNF and IL-1) that activate the endothelial cells of nearby venules to produce
    selectins, ligands for integrins, and chemokines. Selectins mediate weak tethering and rolling of blood
    leukocytes, such as neutrophils on the endothelium; integrins mediate firm adhesion of neutrophils; and
    chemokines increase the affinity of neutrophil integrins and stimulate the migration of the cells through the
    endothelium to the site of infection. Blood neutrophils, monocytes, and activated T lymphocytes use essentially
    the same mechanisms to migrate to sites of infection

    Phagocytosis of Microbes

    Figure 2-8 Phagocytosis and intracellular destruction of microbes. Microbes may be ingested by different membrane receptors of phagocytes;
    some directly bind microbes, and others bind opsonized microbes. (Note that the Mac-1 integrin binds microbes opsonized with complement proteins,
    not shown.) The microbes are internalized into phagosomes, which fuse with lysosomes to form phagolysosomes, where the microbes are killed by
    reactive oxygen and nitrogen intermediates and proteolytic enzymes. NO, nitric oxide; ROS, reactive oxygen species

    Other Functions of
    Activated Macrophages
    Figure 2-9 Effector functions of
    macrophages. Macrophages are
    activated by microbial products such as
    LPS and by NK cell-derived IFN-
    (described later in the chapter). The
    process of macrophage activation leads to
    the activation of transcription factors, the
    transcription of various genes, and the
    synthesis of proteins that mediate the
    functions of these cells. In adaptive cellmediated immunity, macrophages are
    activated by stimuli from T lymphocytes
    (CD40 ligand and IFN-) and respond in
    essentially the same way (see Chapter 13,
    Fig. 13-14).

    Figure 2-10 Activating and inhibitory receptors of


    NK cells.
    A. Activating receptors of NK cells recognize ligands
    on target cells and activate protein tyrosine kinase
    (PTK), whose activity is inhibited by inhibitory
    receptors that recognize class I MHC molecules and
    activate protein tyrosine phosphatase (PTP). NK cells
    do not efficiently kill class I MHC-expressing healthy
    cells. B. If a virus infection or other stress inhibits
    class I MHC expression on infected cells, and
    induces expression of additional activating ligands,
    the NK cell inhibitory receptor is not engaged and the
    activating receptor functions unopposed to trigger
    responses of NK cells, such as killing of target cells
    and cytokine secretion.

    COMPONENTS OF INNATE IMMUNITY


    BARRIERS
    Epithelial layers
    Defensins/cathelicidin
    Intraepithelial lymphocytes

    Prevent microbial entry


    Microbial killing
    Microbial Killing

    CIRCULATING EFFECTOR CELLS.


    Neutrophils
    Early phagocytosisand killing of microbes.
    Macrophages
    Efficient phagocytosis and killing of microbes,
    secretion of cytokines that stimulate inflamation.
    NK cells
    Lysis of infected cells, activation of macrophage

    COMPONENTS OF INNATE IMMUNITY


    CIRCULATING EFFECTOR PROTEINS
    Complement
    Killing of microbes, opsonization of microbes,
    activation of leukocytes
    Mannose-binding
    Opsonization of microbes, activation of complement
    Lectin (collectin)
    (lectin pathway)
    C-reactive protein
    Opsonization of microbes, activation of complement
    (pentraxin)
    CYTOKINES
    TNF,IL-1, chemokines
    INF-,-
    INF-
    IL-12
    IL-15
    IL-10, TGF

    inflammation
    Resitance to viral infection
    Marophage activation
    INF production by NK cells and T cells
    Proliferation of NK cells.
    Control of inlammation.

    INHIBITORY AND ACTIVATING


    RECEPTORS OF NK CELLS

    Figure 2-11 Functions of NK


    cells.
    A. NK cells recognize ligands on
    infected cells or cells undergoing
    other types of stress, and kill the
    host cells. In this way, NK cells
    eliminate reservoirs of infection
    as well as dysfunctional cells. B.
    NK cells respond to IL-12
    produced by macrophages and
    secrete IFN-, which activates
    the macrophages to kill
    phagocytosed microbes.

    The Complement System

    Figure 2-12 Pathways of complement activation. The activation of the complement system may be initiated by three
    distinct pathways, all of which lead to the production of C3b (the early steps). C3b initiates the late steps of
    complement activation, culminating in the production of peptides that stimulate inflammation (C5a) and polymerized
    C9, which forms the membrane attack complex, so called because it creates holes in plasma membranes. The
    principal functions of major proteins produced at different steps are shown. The activation, functions, and regulation of
    the complement system are discussed in much more detail in Chapter 14.

    Role of Innate Immunity in Stimulating


    Adaptive Immune Responses
    Figure 2-13 Stimulation of adaptive immunity by
    innate immune responses.
    Antigen recognition by lymphocytes provides signal
    1 for the activation of the lymphocytes, and
    molecules induced on host cells during innate
    immune responses to microbes provide signal 2.
    In this illustration, the lymphocytes are B cells, but
    the same principles apply to T lymphocytes. The
    nature of second signals differs for B and T cells
    and is described in later chapters.

    RINGKASAN
    Imunitas innate garis pertahanan pertama
    terhadap mikroba. Exist sebelum mikroba
    datang.
    Komponen imunitas innate adalah
    pertahanan epitel, leukosit (neutr, makrofag
    dan sel NK), protein efektor dalam sirkulasi
    (komplemen, kollektin, pentraksin) dan
    sitokin (TNF, IL-1, kemokin, IL-2, INF tipe 1
    dan INF

    RINGKASAN
    Menggunakan reseptor untuk mengenal PAMPs
    (pathogen associated molecular pattern) pada
    mikroba, dimiliki bersama oleh mikroba dan tak
    ada dalam sel mamalia.
    PAMP sangat penting untuk kehidupan mikroba
    sehingga sukar untuk mutasi (menghentikan
    ekspressinya agar selamat dari respon Imun
    innate).
    TLRs adl reseptor terpenting karena dapat
    mengenal variasi yang luas dari ligand( asam
    nukleak mikroba, KH, glikolipid dan protein)

    RINGKASAN
    Makrofag mengenal dan berespon terhadap
    mikroba melalui banyak reseptor (TLRs, Ctype lectins, scavenger receptors danN-formyl
    Met-Leu-Pe receptors).
    Netrofil dan makrofag membunuh mikroba yg
    difagositosis dengan ROS, Nitric Oxide dan
    lisozim dalam fagolisosom.
    Makrofag menghasilkan sitokin untuk inflamasi
    (proinflamasi) dan tissue remodeling pada
    daerah infeksi.

    RINGKASAN
    Neutropil dan monosit (prekursor makrofag
    jaringan) berpindah dari sirkulasi ke daerah
    inflamasi selama respon imun innate.
    Sitokin yang dihasilkan didaerah infeksi (IL-1
    dan TNF) akibat stimulasi produk mikroba akan
    memicu ekspressi molekul adesi pada endotel
    vena yang akan memediasi perlekatan leukosit
    pada endotel untuk selanjutnya migrasi ke
    daerah infeksi.

    RINGKASAN
    Tahapan migrasi mulai dari perlekatan
    lemah dengan molekul adesi (endothelial
    selectin ..leucocyte-selectin ligands )
    disusul perlekatan kuat (leucocyte
    integrin, chemokines) kemudian
    diapedesis (keluar dari sirkulasi)
    Kemokin mengantar leukosit sejak keluar
    dari sirkulai menuju ke daerah infeksi.

    RINGKASAN
    Sel NK adalah limposit yg bekerja untuk kuman
    intraseluler dengan membunuh sel yang
    mengandung mikroba dan menghasilkan INF
    yang memicu aktipasi makrofag.
    Pengenalan sel terinfeksi oleh Sel NK diatur
    melalui kombinasi reseptor aktipasi dan
    inhibisi. Reseptor inhibisi mengenal molekul
    MHC I agar tidak membunuh sel normal tetapi
    membunuh sel terinfeksi karena molekul MHC I
    berkurang.

    RINGKASAN
    Sistem komplemen diaktifkan oleh mikroba dan
    produk dari aktipasi komplemen akan
    meningkatkan fagositosis dan pembunuhan
    mikroba oleh makrofag dan stimulasi inflamasi.
    Effektor molekul dalam plasma seperti
    pentraksins (CRP), kollektin dan fikolin mengikat
    ligan mikroba dan mempercepat pemersihan
    mikroba melalui mekanisme yg tergantung
    komplemen atau tidak.

    RINGKASAN
    Sitokin pada imun innate bekerja untuk
    rekrut dan aktipasi leukosit (TNF,IL-1,
    kemokin), meningkatkan eliminasi mikroba
    oleh fagosit (INF), stimulasi respon sel NK
    dan limposit T (IL-2)
    Pada infeksi berat, produksi berlebihan
    sitokin membahayakan penderita bisa
    menyebabkan kematian.

    RINGKASAN
    Molekul yang dihasilkan oleh imun innate
    memicu imun adaptif dan mempengaruhi
    responnya.
    Makrofag yg diaktifasi oleh mikroba dan
    INF mengeluarkan molekul assessori
    yang meningkatkan aktipasi sel T

    You might also like