Natural killer cells, or NK cells, are a type of cytotoxic lymphocyte critical to the innate immune system. The role NK cells play is analogous to that of cytotoxic T cells in the vertebrate adaptive immune response. NK cells provide rapid responses to viral-infected cells, acting at around 3 days after infection, and respond to tumor formation. Typically, immune cells detect major histocompatibility complex (MHC) presented on infected cell surfaces, triggering cytokine release, causing lysis or apoptosis. NK cells are unique, however, as they have the ability to recognize stressed cells in the absence of antibodies and MHC, allowing for a much faster immune reaction. They were named "natural killers" because of the initial notion that they do not require activation to kill cells that are missing "self" markers of MHC class 1. This role is especially important because harmful cells that are missing MHC I markers cannot be detected and destroyed by other immune cells, such as T lymphocyte cells.
NK cells (belonging to the group of innate lymphoid cells) are defined as large granular lymphocytes (LGL) and constitute the third kind of cells differentiated from the common lymphoid progenitor-generating B and T lymphocytes. NK cells are known to differentiate and mature in the bone marrow, lymph nodes, spleen, tonsils, and thymus, where they then enter into the circulation. NK cells differ from natural killer T cells (NKTs) phenotypically, by origin and by respective effector functions; often, NKT cell activity promotes NK cell activity by secreting interferon gamma. In contrast to NKT cells, NK cells do not express T-cell antigen receptors (TCR) or pan T marker CD3 or surface immunoglobulins (Ig) B cell receptors, but they usually express the surface markers CD16 (FcγRIII) and CD56 in humans, NK1.1 or NK1.2 in C57BL/6 mice. The NKp46 cell surface marker constitutes, at the moment, another NK cell marker of preference being expressed in both humans, several strains of mice (including BALB/c mice) and in three common monkey species.
In addition to the knowledge that natural killer cells are effectors of innate immunity, recent research has uncovered information on both activating and inhibitory NK cell receptors which play important functional roles, including self tolerance and the sustaining of NK cell activity. NK cells also play a role in the adaptive immune response: numerous experiments have demonstrated their ability to readily adjust to the immediate environment and formulate antigen-specific immunological memory, fundamental for responding to secondary infections with the same antigen. The role of NK cells in both the innate and adaptive immune responses is becoming increasingly important in research using NK cell activity as a potential cancer therapy.
NK cell receptors
The HLA ligand for KIR
NK cell receptors can also be differentiated based on function. NK Cells are not a subset of the T lymphocyte family. Natural cytotoxicity receptors directly induce apoptosis after binding to Fas ligand
that directly indicate infection of a cell. The MHC-dependent receptors
(described above) use an alternate pathway to induce apoptosis in
infected cells. Natural killer cell activation is determined by the
balance of inhibitory and activating receptor stimulation. For example,
if the inhibitory receptor signaling is more prominent, then NK cell
activity will be inhibited; similarly, if the activating signal is
dominant, then NK cell activation will result.
Protein structure of NKG2D
NK cell receptor types (with inhibitory, as well as some activating
members) are differentiated by structure, with a few examples to follow:
Protein structure of NKp44
Activating receptors
- Ly49 (homodimers), relatively ancient, C-type lectin family receptors, are of multigenic presence in mice, while humans have only one pseudogenic Ly49, the receptor for classical (polymorphic) MHC I molecules.
- NCR (natural cytotoxicity receptors), a type of type 1 transmembrane proteins of the immunoglobulin superfamily, upon stimulation, mediate NK killing and release of IFNγ. They bind viral ligands such as hemagglutinins and hemagglutinin neuraminidases, some bacterial ligands and cellular ligands related with tumour growth such as PCNA.
- CD16 (FcγIIIA) plays a role in antibody-dependent cell-mediated cytotoxicity; in particular, they bind IgG.
Inhibitory receptors
- Killer-cell immunoglobulin-like receptors (KIRs) belong to a multigene family of more recently evolved Ig-like extracellular domain receptors; they are present in nonhuman primates, and are the main receptors for both classical MHC I (HLA-A, HLA-B, HLA-C) and nonclassical Mamu-G (HLA-G) in primates. Some KIRs are specific for certain HLA subtypes. Most KIRs are inhibitory and dominant. Regular cells express MHC class 1, so are recognised by KIR receptors and NK cell killing is inhibited.
- CD94/NKG2 (heterodimers), a C-type lectin family receptor, is conserved in both rodents and primates and identifies nonclassical (also nonpolymorphic) MHC I molecules such as HLA-E. Expression of HLA-E at the cell surface is dependent on the presence of nonamer peptide epitope derived from the signal sequence of classical MHC class I molecules, which is generated by the sequential action of signal peptide peptidase and the proteasome. Though indirect, this is a way to survey the levels of classical (polymorphic) HLA molecules.
- ILT or LIR (immunoglobulin-like receptor) — are recently discovered members of the Ig receptor family.
- Ly49 (homodimers) have both activating and inhibitory isoforms. They are highly polymorphic on the population level; though they are structurally unrelated to KIRs, they are the functional homologues of KIRs in mice, including the expression pattern. Ly49s are receptor for classical (polymorphic) MHC I molecules.
Function
Cytolytic granule mediated cell apoptosis
NK cells are cytotoxic; small granules in their cytoplasm contain proteins such as perforin and proteases known as granzymes. Upon release in close proximity to a cell slated for killing, perforin forms pores in the cell membrane
of the target cell, creating an aqueous channel through which the
granzymes and associated molecules can enter, inducing either apoptosis or osmotic cell lysis. The distinction between apoptosis and cell lysis is important in immunology: lysing a virus-infected cell could potentially only release the virions, whereas apoptosis leads to destruction of the virus inside. α-defensins,
antimicrobial molecules, are also secreted by NK cells, and directly
kill bacteria by disrupting their cell walls in a manner analogous to
that of neutrophils.
Antibody-dependent cell-mediated cytotoxicity
Infected cells are routinely opsonized with antibodies for detection by immune cells. Antibodies that bind to antigens can be recognised by FcϒRIII (CD16) receptors expressed on NK cells, resulting in NK activation, release of cytolytic granules and consequent cell apoptosis. This is a major killing mechanism of some monoclonal antibodies like rituximab (Rituxan), ofatumumab (Azzera),
and others. The contribution of antibody-dependent cell-mediated
cytotoxicity to tumor cell killing can be measured with a specific test
that uses NK-92
that has been transfected with a high-affinity FcR. Results are
compared to the "wild type" NK-92 that does not express the FcR.
Cytokine-induced NK and Cytotoxic T lymphocyte (CTL) activation
Cytokines play a crucial role in NK cell activation. As these are stress molecules released by cells upon viral infection, they serve to signal to the NK cell the presence of viral pathogens in the affected area. Cytokines involved in NK activation include IL-12, IL-15, IL-18, IL-2, and CCL5.
NK cells are activated in response to interferons or macrophage-derived
cytokines. They serve to contain viral infections while the adaptive
immune response generates antigen-specific cytotoxic T cells
that can clear the infection. NK cells work to control viral infections
by secreting IFNγ and TNFα. IFNγ activates macrophages for phagocytosis
and lysis, and TNFα acts to promote direct NK tumor cell killing.
Patients deficient in NK cells prove to be highly susceptible to early
phases of herpes virus infection.
Missing 'self' hypothesis
Schematic diagram indicating the complementary activities of cytotoxic T cells and NK cells
For NK cells to defend the body against viruses and other pathogens,
they require mechanisms that enable the determination of whether a cell
is infected or not. The exact mechanisms remain the subject of current
investigation, but recognition of an "altered self" state is thought to
be involved. To control their cytotoxic activity, NK cells possess two
types of surface receptors: activating receptors and inhibitory receptors, including killer-cell immunoglobulin-like receptors. Most of these receptors are not unique to NK cells and can be present in some T cell subsets, as well.
The inhibitory receptors recognize MHC class I alleles,
which could explain why NK cells preferentially kill cells that possess
low levels of MHC class I molecules. This mode of NK cell target
interaction is known as "missing-self recognition", a term coined by Klas Kärre
and co-workers in the late 90s. MHC class I molecules are the main
mechanism by which cells display viral or tumor antigens to cytotoxic T
cells. A common evolutionary adaptation to this is seen in both
intracellular microbes
and tumors: the chronic down-regulation of MHC I molecules, which makes
affected cells invisible to T cells, allowing them to evade T
cell-mediated immunity. NK cells apparently evolved as an evolutionary
response to this adaptation (the loss of the MHC eliminates CD4/CD8
action, so another immune cell evolved to fulfill the function).
Tumor cell surveillance
Natural killer cells often lack antigen-specific cell surface receptors, so are part of innate immunity, i.e.
able to react immediately with no prior exposure to the pathogen. In
both mice and humans, NKs can be seen to play a role in tumor
immunosurveillance by directly inducing the death of tumor cells (NKs
act as cytolytic effector lymphocytes), even in the absence of surface
adhesion molecules and antigenic peptides. This role of NK cells is
critical to immune success particularly because T cells are unable to
recognize pathogens in the absence of surface antigens. Tumor cell detection results in activation of NK cells and consequent cytokine production and release.
If tumor cells do not cause inflammation, they will also be
regarded as self and will not induce a T cell response. A number of
cytokines are produced by NKs, including tumor necrosis factor α (TNFα), IFNγ, and interleukin (IL-10).
TNFα and IL-10 act as proinflammatory and immunosuppressors,
respectively. The activation of NK cells and subsequent production of
cytolytic effector cells impacts macrophages, dendritic cells, and neutrophils,
which subsequently enables antigen-specific T and B cell responses.
Instead of acting via antigen-specific receptors, lysis of tumor cells
by NK cells is mediated by alternative receptors, including NKG2D, NKp44, NKp46, NKp30, and DNAM. NKG2D is a disulfide-linked homodimer which recognizes a number of ligands, including ULBP and MICA,
which are typically expressed on tumor cells. The role of dendritic
cell—NK cell interface in immunobiology have been studied and defined as
critical for the comprehension of the complex immune system.
NK cells, along with macrophages and several other cell types, express the Fc receptor (FcR) molecule (FC-gamma-RIII = CD16), an activating biochemical receptor that binds the Fc portion of IgG class antibodies. This allows NK cells to target cells against which a humoral response has been gone through and to lyse
cells through antibody-dependant cytotoxicity (ADCC). This response
depends on the affinity of the Fc receptor expressed on NK cells, which
can have high, intermediate, and low affinity for the Fc portion of the
antibody. This affinity is determined by the amino acid in position 158
of the protein, which can be phenylalanine (F allele) or valine (V
allele). Individuals with high-affinity FcRgammRIII (158 V/V allele)
respond better to antibody therapy. This has been shown for lymphoma
patients who received the antibody Rituxan. Patients who express the 158
V/V allele had a better antitumor response. Only 15–25% of the
population expresses the 158 V/V allele. To determine the ADCC
contribution of monoclonal antibodies, NK-92 cells (a "pure" NK cell
line) has been transfected with the gene for the high-affinity FcR.
Adaptive features of NK cells—"memory-like", "adaptive" and memory NK cells
The ability to generate memory cells following a primary infection
and the consequent rapid immune activation and response to succeeding
infections by the same antigen is fundamental to the role that T and B
cells play in the adaptive immune response. For many years, NK cells
have been considered to be a part of the innate immune system. However,
recently increasing evidence suggests that NK cells can display several
features that are usually attributed to adaptive immune cells (e.g. T
cell responses) such as dynamic expansion and contraction of subsets,
increased longevity and a form of immunological memory, characterized by
a more potent response upon secondary challenge with the same antigen.
In mice, the majority of research was carried out with murine
cytomegalovirus (MCMV) and in models of hapten-hypersensitivity
reactions. Especially, in the MCMV model, protective memory functions of
MCMV-induced NK cells were discovered
and direct recognition of the MCMV-ligand m157 by the receptor Ly49 was
demonstrated to be crucial for the generation of adaptive NK cell
responses.
In humans, most studies have focused on the expansion of an NK cell subset carrying the activating receptor NKG2C. Such expansions were observed primarily in response to human cytomegalovirus (HCMV), but also in other infections including Hantavirus, Chikungunya virus, HIV, or viral hepatitis.
However, whether these virus infections trigger the expansion of
adaptive NKG2C+ NK cells or whether other infections result in
re-activation of latent HCMV (as suggested for hepatitis ), remains a field of study. Notably, further insights into the biology of adaptive NK cells are hampered by the fact that a direct viral ligand for NKG2C has not yet been identified.
NK cell function in pregnancy
As the majority of pregnancies involve two parents who are not tissue-matched, successful pregnancy requires the mother's immune system to be suppressed. NK cells are thought to be an important cell type in this process. These cells are known as "uterine NK cells" (uNK cells) and they differ from peripheral NK cells. They are in the CD56bright NK cell subset, potent at cytokine secretion, but with low cytotoxic ability and relatively similar to peripheral CD56bright NK cells, with a slightly different receptor profile. These uNK cells are the most abundant leukocytes present in utero in early pregnancy, representing about 70% of leukocytes here, but from where they originate remains controversial.
These NK cells have the ability to elicit cell cytotoxicity in vitro, but at a lower level than peripheral NK cells, despite containing perforin. Lack of cytotoxicity in vivo may be due to the presence of ligands for their inhibitory receptors. Trophoblast cells downregulate HLA-A and HLA-B to defend against cytotoxic T cell-mediated
death. This would normally trigger NK cells by missing self
recognition; however, these cells survive. The selective retention of HLA-E (which is a ligand for NK cell inhibitory receptor NKG2A) and HLA-G (which is a ligand for NK cell inhibitory receptor KIR2DL4) by the trophoblast is thought to defend it against NK cell-mediated death.
Uterine NK cells have shown no significant difference in women with recurrent miscarriage
compared with controls. However, higher peripheral NK cell percentages
occur in women with recurrent miscarriages than in control groups.
NK cells secrete a high level of cytokines which help mediate their function. Some important cytokines they secrete include TNF-α, IL-10, IFN-γ, and TGF-β, among others. For example, IFN-γ dilates and thins the walls of maternal spiral arteries to enhance blood flow to the implantation site.
NK cell evasion by tumor cells
By
shedding decoy NKG2D soluble ligands, tumor cells may avoid immune
responses. These soluble NKG2D ligands bind to NK cell NKG2D receptors,
activating a false NK response and consequently creating competition
for the receptor site. This method of evasion occurs in prostate cancer.
In addition, prostate cancer tumors can evade CD8 cell recognition due
to their ability to downregulate expression of MHC class 1 molecules.
This example of immune evasion actually highlights NK cells' importance
in tumor surveillance and response, as CD8 cells can consequently only
act on tumor cells in response to NK-initiated cytokine production
(adaptive immune response).
History
In
early experiments on cell-mediated cytotoxicity against tumor target
cells, both in cancer patients and animal models, investigators
consistently observed what was termed a "natural" reactivity; that is, a
certain population of cells seemed to be able to lyse tumor cells
without having been previously sensitized to them. The first published
study to assert that untreated lymphoid cells were able to confer a
natural immunity to tumors was performed by Dr. Henry Smith at the
University of Leeds School of Medicine in 1966,
leading to the conclusion that the "phenomenon appear[ed] to be an
expression of defense mechanisms to tumor growth present in normal
mice." Other researchers had also made similar observations, but as
these discoveries were inconsistent with the established model at the
time, many initially considered these observations to be artifacts.
By 1973, 'natural killing' activity was established across a wide
variety of species, and the existence of a separate lineage of cells
possessing this ability was postulated. The discovery that a unique type
of lymphocyte was responsible for “natural” or spontaneous cytotoxicity
was made in the early 1970s by doctoral student Rolf Kiessling and
postdoctoral fellow Hugh Pross, in the mouse, and by Hugh Pross and doctoral student Mikael Jondal in the human. The mouse and human work was carried out under the supervision of professors Eva Klein
and Hans Wigzell, respectively, of the Karolinska Institute, Stockholm.
Kiessling’s research involved the well-characterized ability of T
lymphocytes to lyse tumor cells against which they had been previously
immunized. Pross and Jondal were studying cell-mediated cytotoxicity in
normal human blood and the effect of the removal of various
receptor-bearing cells on this cytotoxicity. Later that same year, Ronald Herberman published similar data with respect to the unique nature of the mouse effector cell.
The human data were confirmed, for the most part, by West et al. using similar techniques and the same erythroleukemic target cell line, K562. K562 is highly sensitive to lysis by human NK cells and, over the decades, the K562 51chromium-release assay has become the most commonly used assay to detect human NK functional activity. Its almost universal use has meant that experimental data can be compared easily by different laboratories around the world.
Using discontinuous density centrifugation, and later monoclonal antibodies,
natural killing ability was mapped to the subset of large, granular
lymphocytes known today as NK cells. The demonstration that density
gradient-isolated large granular lymphocytes were responsible for human
NK activity, made by Timonen and Saksela in 1980, was the first time that NK cells had been visualized microscopically, and was a major breakthrough in the field.
New findings
Anticancer therapy
Since
NK cells recognize target cells when they express nonself HLA antigens
(but not self), autologous (patients' own) NK cell infusions have not
shown any antitumor effects. Instead, investigators are working on using
allogeneic cells from peripheral blood, which requires that all T cells
be removed before infusion into the patients to remove the risk of graft versus host disease,
which can be fatal. This can be achieved using an immunomagnetic column
(CliniMACS). In addition, because of the limited number of NK cells in
blood (only 10% of lymphocytes are NK cells), their number needs to be
expanded in culture. This can take a few weeks and the yield is
donor-dependent. A simpler way to obtain high numbers of pure NK cells
is to expand NK-92 cells whose cells continuously grow in culture and
can be expanded to clinical grade numbers in bags or bioreactors.
Clinical studies have shown it to be well tolerated and some antitumor
responses have been seen in patients with lung cancer, melanoma, and
lymphoma.
Infusions of T cells engineered to express a chimeric antigen
receptor that recognizes an antigen molecule on leukemia cells could
induce remissions in patients with advanced leukemia. Logistical
challenges are present for expanding T cells and investigators are
working on applying the same technology to peripheral blood NK cells and
NK-92.
In a study at Boston Children's Hospital, in coordination with Dana-Farber Cancer Institute, in which immunocompromised mice had contracted lymphomas from EBV infection, an NK-activating receptor called NKG2D was fused with a stimulatory Fc
portion of the EBV antibody. The NKG2D-Fc fusion proved capable of
reducing tumor growth and prolonging survival of the recipients. In a
transplantation model of LMP1-fueled lymphomas, the NKG2D-Fc fusion
proved capable of reducing tumor growth and prolonging survival of the
recipients.
Innate resistance to HIV
Recent
research suggests specific KIR-MHC class I gene interactions might
control innate genetic resistance to certain viral infections, including
HIV and its consequent development of AIDS. Certain HLA allotypes have been found to determine the progression of HIV to AIDS; an example is the HLA-B57
and HLA-B27 alleles, which have been found to delay progression from
HIV to AIDS. This is evident because patients expressing these HLA
alleles are observed to have lower viral loads and a more gradual
decline in CD4+ T
cells numbers. Despite considerable research and data collected
measuring the genetic correlation of HLA alleles and KIR allotypes, a
firm conclusion has not yet been drawn as to what combination provides
decreased HIV and AIDS susceptibility.
NK cells can impose immune pressure on HIV, which had previously been described only for T cells and antibodies. HIV mutates to avoid NK cell activity.
Tissue-resident NK cells
Most
of our current knowledge is derived from investigations of mouse
splenic and human peripheral blood NK cells. However, in recent years
tissue-resident NK cell populations have been described.
These specialized NK-cell subsets can play a role in organ homeostasis.
For example, NK cells are enriched in the human liver with a specific
phenotype and take part in the control of liver fibrosis.
