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Biology 151 Lec 9
                          T-cells and B-cells



                                         Parungao-Balolong 2011
Thursday, February 10, 2011
WHAT YOU NEED TO KNOW

                 Recall: Immune Response
                 T- Cell Maturation,
                 Activation and
                 Differentiation
                 B-Cell Generation, Activation
                 and Differentiation

                                       Parungao-Balolong 2011
Thursday, February 10, 2011
recall:
                  Immune response
                (Adaptive immunity)


                              Parungao-Balolong 2011
Thursday, February 10, 2011
Parungao-Balolong 2011
Thursday, February 10, 2011
1. Complement
      System                                      2. Phagocytes




                                                                  “T suppressor cells: prevent overreaction of the
                                                                    system = Inhibit B-lymphocyte production”




                              3. Lymphocytes: T and B Cells                       Parungao-Balolong 2011
Thursday, February 10, 2011
Parungao-Balolong 2011
Thursday, February 10, 2011
the lymphocytes :
                                t-cells


                                        Parungao-Balolong 2011
Thursday, February 10, 2011
T CELLS
      arise in the bone marrow BUT migrate to the thymus gland to mature

      cannot recognize antigen alone, T-cell receptors can recognize only antigen
      bound to cell-membrane proteins (MHC molecules)

            CD4-TH; CD8-TC

      TYPES:

            Helper T cells, Cytotoxic T cells, Suppressor T cells

      CRUCIAL STEPS:

            a naive T cell encounters antigen combined with a MHC molecule on a cell

            T cell proliferates

            differentiates into memory T cells and various effector T cells

                                                                       Parungao-Balolong 2011
Thursday, February 10, 2011
NOTE:
         THE ATTRIBUTE THAT DISTINGUISH
         ANTIGEN RECOGNITION BY MOST
          T-CELLS FROM RECOGNITION BY
            B-CELLS IS MHC RESTRICTION!



                               Parungao-Balolong 2011
Thursday, February 10, 2011
the lymphocytes:
                                   b-cells


                                           Parungao-Balolong 2011
Thursday, February 10, 2011
the b cells
                              B lymphocytes mature
                              within the bone marrow;
                              when they leave it, each
                              expresses a unique antigen-
                              binding receptor on its
                              membrane
                              Plasma cells live for only a
                              few days, they secrete
                              enormous amounts of
                              antibody (2000/sec)

                                          Parungao-Balolong 2011
Thursday, February 10, 2011
receptors
      T-cell receptors (TCRs) and B-cell receptors (BCRs)
       have different structures thus they bind to different
      molecular structures and have different genetic codes
                                              Parungao-Balolong 2011
Thursday, February 10, 2011
comparing notes...
             T-cell receptors (TCRs) enable the cell to bind to and, if additional
             signals are present, to be activated by and respond to an epitope
             presented by APCs

             There are two types of T cells and thus two types of TCRs: CD8 and CD4

                   CD8 T cells destroy the cells they bind to, such as virus cells.

                   CD4 T cells group together to cause inflammation, which isolates an
                   infected area so it can heal = helps build immunities

             B-cell receptors (BCRs) enable the cell to bind to and, if additional
             signals are present, to be activated by and respond to an epitope on
             molecules of a soluble antigen

                   B cells bind to these toxins and digest them into smaller pieces

                   the response ends with descendants of the B cell secreting
                   antibodies (via the plasma cells)
                                                                      Parungao-Balolong 2011
Thursday, February 10, 2011
development &
                               maturation


                                         Parungao-Balolong 2011
Thursday, February 10, 2011
T cells versus B cells




                                            Parungao-Balolong 2011
Thursday, February 10, 2011
T
                                           -
                                           C
   Experiment!
                                           E
                                           L
                                           L


                              Parungao-Balolong 2011
Thursday, February 10, 2011
T
                                                                                            -
                                                                                            C
                                                                                            E
                                                                                            L
                                                                                            L
             In the thymus, developing T cells, known as thymocytes, proliferate and differentiate
             along developmental pathways that generate functionally distinct subpopulations of
             mature T cells

             Aside from being the main source of all T cells, it is where T cells diversify and then
             are shaped into an effective primary T-cell repertoire by an extraordinary pair of
             selection processes (+ and - SELECTION)                         Parungao-Balolong 2011
Thursday, February 10, 2011
POSITIVE AND
        NEGATIVE SELECTION
   •       positive selection, permits the survival of
           only those T cells whose TCRs are capable of
           recognizing self-MHC molecules

         •       It is thus responsible for the creation of
                 a self-MHC-restricted repertoire
                 of T cells

                 Cells that fail positive selection are
                 eliminated within the thymus by apoptosis

   •       negative selection, eliminates T cells that
           react too strongly with self-MHC or with
           self-MHC plus self- peptides

         •       bearing high-affinity receptors for self-
                 MHC molecules alone or self-antigen
                 presented by self-MHC, which results in
                 self-tolerance

         •       It is an extremely important factor in
                 generating a primary T-cell
                 repertoire that is self-tolerant             Parungao-Balolong 2011
Thursday, February 10, 2011
B
                                                                                     -
                                                                                     C
                                                                                     E
                                                                                     L
                                                                                     L
            B cells develop in bone marrow and undergo antigen-
            induced activation and differentiation in the periphery

            Activated B cells can give rise to antibody-secreting plasma
            cells or memory B cells                                        Parungao-Balolong 2011
Thursday, February 10, 2011
B CELL MATURATION
  AND DEVELOPMENT


      • During B-cell development,
              sequential Ig-gene
              rearrangements transform a
              pro-B cell into an immature
              B cell expressing mIgM with
              a single antigenic specificity

      • Further development yields
              mature naive B cells
              expressing both mIgM and
              mIgD

                                               Parungao-Balolong 2011
Thursday, February 10, 2011
B CELL MATURATION
  AND DEVELOPMENT
      •       When a self-reactive BCR is
              expressed in the bone marrow,
              negative selection of the self-
              reactive immature B cells
              occurs

      •       The selected cells are deleted
              by apoptosis or undergo
              receptor editing to produce
              non-self-reactive mIg

      •       B cells reactive with self-
              antigens encountered in the
              periphery are rendered
              anergic
                                                Parungao-Balolong 2011
Thursday, February 10, 2011
activation &
                              DIFFERENTIATION


                                          Parungao-Balolong 2011
Thursday, February 10, 2011
t CELL ACTIVATION
                                    TH-cell activation is initiated
                                    by interaction of the TCR- CD3
                                    complex with a peptide-MHC
                                    complex on an antigen-
                                    presenting cell

                                    Activation also requires the
                                    activity of accessory
                                    molecules, including the
                                    coreceptors CD4 and CD8

                                    Many different intracellular
                                    signal-transduction pathways
                                    are activated by the
                                    engagement of the TCR
                                             Parungao-Balolong 2011
Thursday, February 10, 2011
Parungao-Balolong 2011
Thursday, February 10, 2011
SIGNALS FOR ACTIVATION
     •       In addition to the signals
             mediated by the T-cell receptor
             and its associated accessory
             molecules (signal 1), activation
             of the TH cell requires a co-
             stimulatory signal (signal 2)
             provided by the antigen-
             presenting cell

     •        The co-stimulatory signal is
             commonly induced by
             interaction between molecules
             of the B7 family on the
             membrane of the APC with
             CD28 on the TH cell

     •       Engagement of CTLA-4, a close
             relative of CD28, by B7 inhibits
             T-cell activation                  Parungao-Balolong 2011
Thursday, February 10, 2011
SIGNALS FOR ACTIVATION
     •       TCR engagement with antigenic peptide-MHC may induce activation or
             clonal anergy

     •       The presence or absence of the co-stimulatory signal (signal 2) determines
             whether activation results in clonal expansion or clonal anergy




                                                                  Parungao-Balolong 2011
Thursday, February 10, 2011
Parungao-Balolong 2011
Thursday, February 10, 2011
Parungao-Balolong 2011
Thursday, February 10, 2011
DIFFERENTIATION IN T-CELLS
       •      Naive T cells are resting cells (G0) that
              have not encountered antigen.
              Activation of naive cells leads to the
              generation of effector and memory T
              cells

       •      Memory T cells, which are more easily
              activated than naive cells, are
              responsible for secondary responses

       •      Effector cells are short lived and
              perform helper, cytotoxic, or delayed-
              type hypersensitivity functions.

       •      The T-cell repertoire is shaped by
              apoptosis in the thymus and periphery

       •      gamma delta T cells are not MHC
              restricted
                                                          Parungao-Balolong 2011
Thursday, February 10, 2011
B CELL ACTIVATION




                                      Parungao-Balolong 2011
Thursday, February 10, 2011
B CELL ACTIVATION
        B-cells are activated when antigen
        binds to receptors on the B-cell surface,
        followed by a co-stimulatory signal,
        usually provided by a helper T-cell.

        Antigens that require co-stimulation by
        a T-cell to activate a B-cell are T-
        dependent antigens and are usually
        proteins

        In order for the helper T-cell to stimulate
        the B-cell both must be activated - this
        usually requires that the B-cell
        internalize the antigen, process it, and
        then present it on the cell surface
        bound to a class II HLA molecule

        The HLA-antigen complex is recognized
        by a receptor on the surface of the T-
        cell (the T-cell receptor, or TCR)
                                                      Parungao-Balolong 2011
Thursday, February 10, 2011
B CELL ACTIVATION
               The B-cell expresses an activation receptor on its surface (CD40) that binds
               to a complementary ligand (CD154) on the surface of the helper T-cell

               This interaction will co-stimulate the B-cell, activating it to clonally proliferate

               In addition, the helper T-cell will secrete interleukins that will promote growth
               and antibody production by the activated B-cell

               The helper T-cell would normally have been activated by interaction with a
               macrophage or dendritic cell but the B-cell can act as an antigen presenting
               cell as well

               The B-cell can express B7 proteins on its surface which will bind to CD28 on
               the surface of the helper T-cell

               The combination of TCR-HLA/antigen binding and B7-CD28 binding will
               activate the T-cell
                                                                            Parungao-Balolong 2011
Thursday, February 10, 2011
Parungao-Balolong 2011
Thursday, February 10, 2011
Parungao-Balolong 2011
Thursday, February 10, 2011
Parungao-Balolong 2011
Thursday, February 10, 2011
END OF FIRST EXAM
                            COVERAGE


                                     Parungao-Balolong 2011
Thursday, February 10, 2011

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T cells and b-cells

  • 1. Biology 151 Lec 9 T-cells and B-cells Parungao-Balolong 2011 Thursday, February 10, 2011
  • 2. WHAT YOU NEED TO KNOW Recall: Immune Response T- Cell Maturation, Activation and Differentiation B-Cell Generation, Activation and Differentiation Parungao-Balolong 2011 Thursday, February 10, 2011
  • 3. recall: Immune response (Adaptive immunity) Parungao-Balolong 2011 Thursday, February 10, 2011
  • 5. 1. Complement System 2. Phagocytes “T suppressor cells: prevent overreaction of the system = Inhibit B-lymphocyte production” 3. Lymphocytes: T and B Cells Parungao-Balolong 2011 Thursday, February 10, 2011
  • 7. the lymphocytes : t-cells Parungao-Balolong 2011 Thursday, February 10, 2011
  • 8. T CELLS arise in the bone marrow BUT migrate to the thymus gland to mature cannot recognize antigen alone, T-cell receptors can recognize only antigen bound to cell-membrane proteins (MHC molecules) CD4-TH; CD8-TC TYPES: Helper T cells, Cytotoxic T cells, Suppressor T cells CRUCIAL STEPS: a naive T cell encounters antigen combined with a MHC molecule on a cell T cell proliferates differentiates into memory T cells and various effector T cells Parungao-Balolong 2011 Thursday, February 10, 2011
  • 9. NOTE: THE ATTRIBUTE THAT DISTINGUISH ANTIGEN RECOGNITION BY MOST T-CELLS FROM RECOGNITION BY B-CELLS IS MHC RESTRICTION! Parungao-Balolong 2011 Thursday, February 10, 2011
  • 10. the lymphocytes: b-cells Parungao-Balolong 2011 Thursday, February 10, 2011
  • 11. the b cells B lymphocytes mature within the bone marrow; when they leave it, each expresses a unique antigen- binding receptor on its membrane Plasma cells live for only a few days, they secrete enormous amounts of antibody (2000/sec) Parungao-Balolong 2011 Thursday, February 10, 2011
  • 12. receptors T-cell receptors (TCRs) and B-cell receptors (BCRs) have different structures thus they bind to different molecular structures and have different genetic codes Parungao-Balolong 2011 Thursday, February 10, 2011
  • 13. comparing notes... T-cell receptors (TCRs) enable the cell to bind to and, if additional signals are present, to be activated by and respond to an epitope presented by APCs There are two types of T cells and thus two types of TCRs: CD8 and CD4 CD8 T cells destroy the cells they bind to, such as virus cells. CD4 T cells group together to cause inflammation, which isolates an infected area so it can heal = helps build immunities B-cell receptors (BCRs) enable the cell to bind to and, if additional signals are present, to be activated by and respond to an epitope on molecules of a soluble antigen B cells bind to these toxins and digest them into smaller pieces the response ends with descendants of the B cell secreting antibodies (via the plasma cells) Parungao-Balolong 2011 Thursday, February 10, 2011
  • 14. development & maturation Parungao-Balolong 2011 Thursday, February 10, 2011
  • 15. T cells versus B cells Parungao-Balolong 2011 Thursday, February 10, 2011
  • 16. T - C Experiment! E L L Parungao-Balolong 2011 Thursday, February 10, 2011
  • 17. T - C E L L In the thymus, developing T cells, known as thymocytes, proliferate and differentiate along developmental pathways that generate functionally distinct subpopulations of mature T cells Aside from being the main source of all T cells, it is where T cells diversify and then are shaped into an effective primary T-cell repertoire by an extraordinary pair of selection processes (+ and - SELECTION) Parungao-Balolong 2011 Thursday, February 10, 2011
  • 18. POSITIVE AND NEGATIVE SELECTION • positive selection, permits the survival of only those T cells whose TCRs are capable of recognizing self-MHC molecules • It is thus responsible for the creation of a self-MHC-restricted repertoire of T cells Cells that fail positive selection are eliminated within the thymus by apoptosis • negative selection, eliminates T cells that react too strongly with self-MHC or with self-MHC plus self- peptides • bearing high-afnity receptors for self- MHC molecules alone or self-antigen presented by self-MHC, which results in self-tolerance • It is an extremely important factor in generating a primary T-cell repertoire that is self-tolerant Parungao-Balolong 2011 Thursday, February 10, 2011
  • 19. B - C E L L B cells develop in bone marrow and undergo antigen- induced activation and differentiation in the periphery Activated B cells can give rise to antibody-secreting plasma cells or memory B cells Parungao-Balolong 2011 Thursday, February 10, 2011
  • 20. B CELL MATURATION AND DEVELOPMENT • During B-cell development, sequential Ig-gene rearrangements transform a pro-B cell into an immature B cell expressing mIgM with a single antigenic specificity • Further development yields mature naive B cells expressing both mIgM and mIgD Parungao-Balolong 2011 Thursday, February 10, 2011
  • 21. B CELL MATURATION AND DEVELOPMENT • When a self-reactive BCR is expressed in the bone marrow, negative selection of the self- reactive immature B cells occurs • The selected cells are deleted by apoptosis or undergo receptor editing to produce non-self-reactive mIg • B cells reactive with self- antigens encountered in the periphery are rendered anergic Parungao-Balolong 2011 Thursday, February 10, 2011
  • 22. activation & DIFFERENTIATION Parungao-Balolong 2011 Thursday, February 10, 2011
  • 23. t CELL ACTIVATION TH-cell activation is initiated by interaction of the TCR- CD3 complex with a peptide-MHC complex on an antigen- presenting cell Activation also requires the activity of accessory molecules, including the coreceptors CD4 and CD8 Many different intracellular signal-transduction pathways are activated by the engagement of the TCR Parungao-Balolong 2011 Thursday, February 10, 2011
  • 25. SIGNALS FOR ACTIVATION • In addition to the signals mediated by the T-cell receptor and its associated accessory molecules (signal 1), activation of the TH cell requires a co- stimulatory signal (signal 2) provided by the antigen- presenting cell • The co-stimulatory signal is commonly induced by interaction between molecules of the B7 family on the membrane of the APC with CD28 on the TH cell • Engagement of CTLA-4, a close relative of CD28, by B7 inhibits T-cell activation Parungao-Balolong 2011 Thursday, February 10, 2011
  • 26. SIGNALS FOR ACTIVATION • TCR engagement with antigenic peptide-MHC may induce activation or clonal anergy • The presence or absence of the co-stimulatory signal (signal 2) determines whether activation results in clonal expansion or clonal anergy Parungao-Balolong 2011 Thursday, February 10, 2011
  • 29. DIFFERENTIATION IN T-CELLS • Naive T cells are resting cells (G0) that have not encountered antigen. Activation of naive cells leads to the generation of effector and memory T cells • Memory T cells, which are more easily activated than naive cells, are responsible for secondary responses • Effector cells are short lived and perform helper, cytotoxic, or delayed- type hypersensitivity functions. • The T-cell repertoire is shaped by apoptosis in the thymus and periphery • gamma delta T cells are not MHC restricted Parungao-Balolong 2011 Thursday, February 10, 2011
  • 30. B CELL ACTIVATION Parungao-Balolong 2011 Thursday, February 10, 2011
  • 31. B CELL ACTIVATION B-cells are activated when antigen binds to receptors on the B-cell surface, followed by a co-stimulatory signal, usually provided by a helper T-cell. Antigens that require co-stimulation by a T-cell to activate a B-cell are T- dependent antigens and are usually proteins In order for the helper T-cell to stimulate the B-cell both must be activated - this usually requires that the B-cell internalize the antigen, process it, and then present it on the cell surface bound to a class II HLA molecule The HLA-antigen complex is recognized by a receptor on the surface of the T- cell (the T-cell receptor, or TCR) Parungao-Balolong 2011 Thursday, February 10, 2011
  • 32. B CELL ACTIVATION The B-cell expresses an activation receptor on its surface (CD40) that binds to a complementary ligand (CD154) on the surface of the helper T-cell This interaction will co-stimulate the B-cell, activating it to clonally proliferate In addition, the helper T-cell will secrete interleukins that will promote growth and antibody production by the activated B-cell The helper T-cell would normally have been activated by interaction with a macrophage or dendritic cell but the B-cell can act as an antigen presenting cell as well The B-cell can express B7 proteins on its surface which will bind to CD28 on the surface of the helper T-cell The combination of TCR-HLA/antigen binding and B7-CD28 binding will activate the T-cell Parungao-Balolong 2011 Thursday, February 10, 2011
  • 36. END OF FIRST EXAM COVERAGE Parungao-Balolong 2011 Thursday, February 10, 2011