mainly as a result of delivery of granule proteins into
the target cells. Two types of granule proteins critical for
Fig. 6.11 Functions of Th17 cells. Th17 cells produce the
cytokine interleukin-17 (IL-17), which induces production of
chemokines and other cytokines from various cells, and these
recruit neutrophils (and monocytes, not shown) into the site of
intestinal tract and other tissues. APC, Antigen-presenting cell;
CSFs, colony-stimulating factors; TNF, tumor necrosis factor.
132 CHAPTER 6 Effector Mechanisms of T Cell–Mediated Immunity
killing are granzymes (granule enzymes) and perforin.
Perforin disrupts the integrity of the target cell plasma
enzymes called caspases (cysteine proteases that cleave
proteins after aspartic acid residues) that are present in
the cytosol of target cells and whose major function is to
Activated CTLs also express a membrane protein
activates caspases and induces target cell apoptosis; this
The net result of these effector mechanisms of CTLs
CTLs themselves are not injured during the process
of killing other cells, so each CTL can kill a target cell,
detach, and go on to kill additional targets.
activation of macrophages in infections and in disease
states where excessive activation of CD8+ T cells may
be a feature. It may also play a role in defense against
Although we have described the effector functions of
CD4+ T cells and CD8+ T cells separately, these types
of T lymphocytes may function cooperatively to destroy
intracellular microbes (Fig. 6.13). If microbes are
phagocytosed and remain sequestered in macrophage
vesicles, CD4+ T cells may be adequate to eradicate these
requires destruction of the infected cells by CD8+ CTLs.
RESISTANCE OF PATHOGENIC MICROBES
Different microbes have developed diverse mechanisms to resist T lymphocyte–mediated host
defense (Fig. 6.14). Many intracellular bacteria,
CHAPTER 6 Effector Mechanisms of T Cell–Mediated Immunity 133
such as Mycobacterium tuberculosis, Legionella
pneumophila, and Listeria monocytogenes, inhibit
the fusion of phagosomes with lysosomes or create pores in phagosome membranes, allowing these
organisms to escape into the cytosol. Thus, these
MHC–associated antigen presentation by inhibiting
production or expression of class I molecules, by
blocking transport of antigenic peptides from the
cytosol into the endoplasmic reticulum (ER) and by
removing newly synthesized class I molecules from
result of this defective loading is reduced surface
expression of class I MHC molecules, because empty
class I molecules are unstable and are not expressed
on the cell surface. It is interesting that NK cells
are activated by class I–deficient cells (see Chapter 2). Thus, host defenses have evolved to combat
immune evasion mechanisms of microbes: CTLs
recognize class I MHC–associated viral peptides,
viruses inhibit class I MHC expression, and NK cells
recognize the absence of class I MHC molecules on
cytokines available to trigger cell-mediated immune
inhibitory receptors, including PD-1 (programmed
[cell] death protein 1; see Chapter 9) on CD8+ T cells,
thus inhibiting the effector functions of CTLs. This
phenomenon, in which the T cells mount an initial
chronic antigenic stimulation, as in chronic viral
infections or tumors, and is a mechanism by which
the repeatedly stimulated T cell terminates its own
Fig. 6.13 Cooperation between CD4+ and CD8+ T cells in eradication of intracellular infections. In a
infection. CTL, Cytotoxic T lymphocyte; IFN, interferon.
134 CHAPTER 6 Effector Mechanisms of T Cell–Mediated Immunity
CHAPTER 6 Effector Mechanisms of T Cell–Mediated Immunity 135
response. Still other viruses directly infect and kill
immune cells, the best example being human immunodeficiency virus (HIV), which is able to survive in
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