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T helper cell

April 10, 2024

"Th2" redirects here. For the professional wrestling tag team, see The Hybrid 2.

The T helper cells (Th cells), also known as CD4+ cells or CD4-positive cells, are a type of T cell that play an important role in the adaptive immune system. They aid the activity of other immune cells by releasing cytokines. They are considered essential in B cell antibody class switching, breaking cross-tolerance in dendritic cells, in the activation and growth of cytotoxic T cells, and in maximizing bactericidal activity of phagocytes such as macrophages and neutrophils. CD4+ cells are mature Th cells that express the surface protein CD4. Genetic variation in regulatory elements expressed by CD4+ cells determines susceptibility to a broad class of autoimmune diseases.[1]

Activation of macrophage or B cell by T helper cell

Structure and function edit

Th cells contain and release cytokines to aid other immune cells. Cytokines are small protein mediators that alter the behavior of target cells that express receptors for those cytokines. These cells help polarize the immune response depending on the nature of the immunological insult (for example; virus vs. extracellular bacterium vs. intracellular bacterium vs. helminth vs. fungus vs. protist).[citation needed]

Mature Th cells express the surface protein CD4 and are referred to as CD4+ T cells. CD4+ T cells are generally treated as having a pre-defined role as helper T cells within the immune system. For example, when an antigen-presenting cell displays a peptide antigen on MHC class II proteins, a CD4+ cell will aid those cells through a combination of cell to cell interactions (e.g. CD40 (protein) and CD40L) and through cytokines.

Th cells are not a monolithic immunological entity because they are diverse in terms of function and their interaction with partner cells. In general, mature naive T cells are stimulated by professional antigen presenting cells to acquire an effector module. These are defined by the presence of a lineage-determining (or lineage-specifying) transcription factor (also called master regulator, though the term has been criticized for being too reductive).[2] The loss of function in a lineage specifying transcription factor results in the absence of the corresponding class of helper T cell which can be devastating for the health of the host.

Activation of naive helper T cells edit

 
T-cell dependent B-cell activation, showing TH2-cell (left) B-cell (right) and several interaction molecules self-made according to Janeway et al, Immunologie (Berlin, 2002)

Following Development in the thymus, these cells (termed recent thymic emigrants (RTE)) egress from the thymus and home to secondary lymphoid organs (SLO; spleen and lymph nodes). Of note, only a very small minority of T cells egresses from the thymus (estimates commonly range from 1–5% but some experts feel even this is generous).[3] Maturation of RTE in SLO results in the generation of mature naive T cells (naïve meaning they have never been exposed to the antigen that they are programmed to respond to), but naive T cells now lack or have downregulated (reduced) expression of the RTE-related surface markers, such as CD31, PTK7, Complement Receptor 1 and 2 (CR1, CR2) and the production of interleukin 8 (IL-8).[4][5] Like all T cells, they express the T cell receptor-CD3 complex. The T cell receptor (TCR) consists of both constant and variable regions. The variable region determines what antigen the T cell can respond to. CD4+ T cells have TCRs with an affinity for Class II MHC, and CD4 is involved in determining MHC affinity during maturation in the thymus. Class II MHC proteins are generally only found on the surface of professional antigen-presenting cells (APCs). Professional antigen-presenting cells are primarily dendritic cells, macrophages and B cells, although dendritic cells are the only cell group that expresses MHC Class II constitutively (at all times). Some APCs also bind native (or unprocessed) antigens to their surface, such as follicular dendritic cells (these are not the same type of cells as the dendritic cells of the immune system but rather have a non-hematopoietic origin, and in general lack MHC Class II, meaning they are not true professional antigen-presenting cells; however, follicular dendritic cells may acquire MHC Class II proteins via exosomes that become attached to them[6]). T cells require antigens to be processed into short fragments which form linear epitopes on MHC Class II (in the case of helper T cells because they express CD4) or MHC class I (in the case of cytotoxic T cells which express CD8). MHC Class II binding pockets are flexible with respect to the length of the peptides they hold. Generally, there are 9 core amino acid residues with several flanking amino acids which form a length of about 12–16 amino acids total[7] but have been known to hold as many as 25 amino acids.[8] By comparison, MHC Class I proteins are usually 9-10 peptides long.[9] The activation of naive T cells is commonly explained in terms of the 3-signal model, elaborated upon below.[10]

Activation (signal 1) edit

 
Antigen presentation stimulates naïve CD8+ and CD4+ T cells to become mature "cytotoxic" CD8+ cells and "helper" CD4+ cells respectively .

During an immune response, professional antigen-presenting cells (APCs) endocytose antigens (typically bacteria or viruses), which undergo processing, then travel from the infection site to the lymph nodes. Typically, the APC responsible is a dendritic cell. If the antigen expresses appropriate molecular patterns (sometimes known as signal 0), it can induce maturation of the dendritic cell which results in enhanced expression of costimulatory molecules needed to activate T cells (see signal 2)[11] and MHC Class II.[12] Once at the lymph nodes, the APCs begin to present antigen peptides that are bound to Class II MHC, allowing CD4+ T cells that express the specific TCRs against the peptide/MHC complex to activate.[citation needed]

When a Th cell encounters and recognizes the antigen on an APC, the TCR-CD3 complex binds strongly to the peptide-MHC complex present on the surface of professional APCs. CD4, a co-receptor of the TCR complex, also binds to a different section of the MHC molecule. It is estimated that approximately 50 of these interactions are required for the activation of a helper T cell and assemblies known as microclusters have been observed forming between the TCR-CD3-CD4 complexes of the T cell and the MHC Class II proteins of the dendritic cell at the zone of contact. When these all come together, the CD4 is able to recruit a kinase called Lck which phosphorylates immunoreceptor tyrosine-based activation motifs (ITAMs) present on the CD3 gamma, delta, epsilon, and zeta chains. The protein ZAP-70 can bind these phosphorylated ITAMs via its SH2 domain and then itself becomes phosphorylated, wherein it orchestrates the downstream signaling required for T cell activation. Lck activation is controlled by the opposing actions of CD45 and Csk.[13] CD45 activates Lck by dephosphorylating a tyrosine in its C-terminal tail, while Csk phosphorylates Lck at that site. The loss of CD45 produces a form of SCID because failure to activate Lck prevents appropriate T cell signaling. Memory T cells also make use of this pathway and have higher levels of Lck expressed and the function of Csk is inhibited in these cells.[14]

The binding of the antigen-MHC to the TCR complex and CD4 may also help the APC and the Th cell adhere during Th cell activation, but the integrin protein LFA-1 on the T cell and ICAM on the APC are the primary molecules of adhesion in this cell interaction.[citation needed]

It is unknown what role the relatively bulky extracellular region of CD45 plays during cell interactions, but CD45 has various isoforms that change in size depending on the Th cell's activation and maturation status. For example, CD45 shortens in length following Th activation (CD45RA+ to CD45RO+), but whether this change in length influences activation is unknown. It has been proposed that the larger CD45RA may decrease the accessibility of the T cell receptor for the antigen-MHC molecule, thereby necessitating an increase in the affinity (and specificity) of the T cell for activation. However, once the activation has occurred, CD45 shortens, allowing easier interactions and activation as an effector T helper cell.[citation needed]

Survival (signal 2) edit

Having received the first TCR/CD3 signal, the naïve T cell must activate a second independent biochemical pathway, known as Signal 2. This verification step is a protective measure to ensure that a T cell is responding to a foreign antigen. If this second signal is not present during initial antigen exposure, the T cell presumes that it is auto-reactive. This results in the cell becoming anergic (anergy is generated from the unprotected biochemical changes of Signal 1). Anergic cells will not respond to any antigen in the future, even if both signals are present later on. These cells are generally believed to circulate throughout the body with no value until they undergo apoptosis.[15]

The second signal involves an interaction between CD28 on the CD4+ T cell and the proteins CD80 (B7.1) or CD86 (B7.2) on the professional APCs. Both CD80 and CD86 activate the CD28 receptor. These proteins are also known as co-stimulatory molecules.[citation needed]

Although the verification stage is necessary for the activation of naïve helper T cells, the importance of this stage is best demonstrated during the similar activation mechanism of CD8+ cytotoxic T cells. As naïve CD8+ T cells have no true bias towards foreign sources, these T cells must rely on the activation of CD28 for confirmation that they recognise a foreign antigen (as CD80/CD86 is only expressed by active APC's). CD28 plays an important role in decreasing the risk of T cell auto-immunity against host antigens.[citation needed]

Once the naïve T cell has both pathways activated, the biochemical changes induced by Signal 1 are altered, allowing the cell to activate instead of undergoing anergy. The second signal is then obsolete; only the first signal is necessary for future activation. This is also true for memory T cells, which is one example of learned immunity. Faster responses occur upon reinfection because memory T cells have already undergone confirmation and can produce effector cells much sooner.[citation needed]

Differentiation (signal 3) edit

Once the two-signal activation is complete the T helper cell (Th) then allows itself to proliferate. It achieves this by releasing a potent T cell growth factor called interleukin 2 (IL-2) which acts upon itself in an autocrine fashion. Activated T cells also produce the alpha sub-unit of the IL-2 receptor (CD25 or IL-2R), enabling a fully functional receptor that can bind with IL-2, which in turn activates the T cell's proliferation pathways.[citation needed]

The autocrine or paracrine secretion of IL-2 can bind to that same Th cell or neighboring Th's via the IL-2R thus driving proliferation and clonal expansion. The Th cells receiving both signals of activation and proliferation will then become Th0 (T helper 0) cells that secrete IL-2, IL-4 and interferon gamma (IFN-γ). The Th0 cells will then differentiate into Th1 or Th2 cells depending on cytokine environment. IFN-γ drives Th1 cell production while IL-10 and IL-4 inhibit Th1 cell production. Conversely, IL-4 drives Th2 cell production and IFN-γ inhibits Th2 cells. These cytokines are pleiotropic and carry out many other functions of the immune response.[citation needed]

Effector function edit

In 1991, three groups reported discovering CD154, which is the molecular basis of T cell helper function. Seth Lederman at Columbia University generated a murine monoclonal antibody, 5c8 that inhibited contact-dependent T cell helper function in human cells which characterized the 32 kDa surface protein transiently expressed on CD4+ T cells.[16] Richard Armitage at Immunex cloned a cDNA encoding CD154 by screening an expression library with CD40-Ig.[17] Randolph Noelle at Dartmouth Medical School generated an antibody that bound a 39 kDa protein on murine T cells and inhibited helper function.[18]

Determination of the effector T cell response edit

Helper T cells are capable of influencing a variety of immune cells, and the T cell response generated (including the extracellular signals such as cytokines) can be essential for a successful outcome from infection. In order to be effective, helper T cells must determine which cytokines will allow the immune system to be most useful or beneficial for the host. Understanding exactly how helper T cells respond to immune challenges is currently of major interest in immunology, because such knowledge may be very useful in the treatment of disease and in increasing the effectiveness of vaccination.[citation needed]

Th1/Th2 model edit

Proliferating helper T cells that develop into effector T cells differentiate into two major subtypes of cells known as Th1 and Th2 cells (also known as Type 1 and Type 2 helper T cells, respectively).

Th1 helper cells lead to an increased cell-mediated response (primarily by macrophages and cytotoxic T cells),[19] typically against intracellular bacteria and protozoa. They are triggered by the polarising cytokine IL-12 and their effector cytokines are IFN-γ and IL-2. The main effector cells of Th1 immunity are macrophages as well as CD8 T cells, IgG B cells, and IFN-γ CD4 T cells. The key Th1 transcription factors are STAT4 and T-bet. IFN-γ secreted by CD4 T cells can activate macrophages to phagocytose and digest intracellular bacteria and protozoa. In addition, IFN-γ can activate iNOS (inducible nitric oxide synthase) to produce nitric oxide free radicals to directly kill intracellular bacteria and protozoa. Th1 overactivation against autoantigens will cause Type IV or delayed-type hypersensitivity reaction. Tuberculin reaction and Type 1 diabetes belong to this category of autoimmunity.[20]

Th2 helper cells lead to a humoral immune response,[19] typically against extracellular parasites such as helminths. They are triggered by the polarising cytokines IL-4 and IL-2, and their effector cytokines are IL-4, IL-5, IL-9, IL-10, IL-13 and IL-25. The main effector cells are eosinophils, basophils, and mast cells as well as B cells, and IL-4/IL-5 CD4 T cells. The key Th2 transcription factors are STAT6 and GATA3.[21] IL-4 is the positive feedback cytokine for Th2 cells differentiation. Besides, IL-4 stimulates B-cells to produce IgE antibodies, which in turn stimulate mast cells to release histamine, serotonin, and leukotriene to cause broncho-constriction, intestinal peristalsis, gastric fluid acidification to expel helminths. IL-5 from CD4 T cells will activate eosinophils to attack helminths. IL-10 suppresses Th1 cells differentiation and function of dendritic cells. Th2 overactivation against antigen will cause Type I hypersensitivity which is an allergic reaction mediated by IgE. Allergic rhinitis, atopic dermatitis, and asthma belong to this category of overactivation .[20] In addition to expressing different cytokines, Th2 cells also differ from Th1 cells in their cell surface glycans (oligosaccharides), which makes them less susceptible to some inducers of cell death.[22][23]

 
Th1/Th2 Model for helper T cells. An antigen is ingested and processed by an APC. It presents fragments from it to T cells. The upper, Th0, is a T helper cell. The fragment is presented to it by MHC2.[24] IFN-γ, interferon γ; TGF-β, transforming growth factor β; mø, macrophage; IL-2, interleukin 2; IL-4, interleukin 4
Th1/Th2 dichotomy
Type 1/ Th1 Type 2/ Th2[20]
Main partner cell type Macrophage, CD8+ T cell B-cell, eosinophil, mast cell
Cytokines produced Interferon gamma (IFNγ) and TNF-β. Interleukin 2 and interleukin 10 production has been reported in activated Th1 cell.[25] Interleukin 4, interleukin 5, interleukin 6, interleukin 9, interleukin 10, interleukin 13
Immune stimulation promoted Cellular immune system. Maximizes the killing efficacy of the macrophages and the proliferation of cytotoxic CD8+ T cells. Also promotes the production of IgG, an opsonizing antibody. Humoral immune system. Stimulates B-cells into proliferation, to induce B-cell antibody class switching, and to increase neutralizing antibody production (IgG, IgM and IgA as well as IgE antibodies).
Other functions The Type 1 cytokine IFNγ increases the production of interleukin 12 by dendritic cells and macrophages, and via positive feedback, IL-12 stimulates the production of IFNγ in helper T cells, thereby promoting the Th1 profile. IFNγ also inhibits the production of cytokines such as interleukin 4, an important cytokine associated with the Type 2 response, and thus it also acts to preserve its own response. The Type 2 response promotes its own profile using two different cytokines. Interleukin 4 acts on helper T cells to promote the production of Th2 cytokines (including itself; it is auto-regulatory), while interleukin 10 (IL-10) inhibits a variety of cytokines including interleukin 2 and IFNγ in helper T cells and IL-12 in dendritic cells and macrophages. The combined action of these two cytokines suggests that once the T cell has decided to produce these cytokines, that decision is preserved (and also encourages other T cells to do the same).

While we know about the types of cytokine patterns helper T cells tend to produce, we understand less about how the patterns themselves are decided. Various evidence suggests that the type of APC presenting the antigen to the T cell has a major influence on its profile. Other evidence suggests that the concentration of antigen presented to the T cell during primary activation influences its choice. The presence of some cytokines (such as the ones mentioned above) will also influence the response that will eventually be generated, but our understanding is nowhere near complete.

Th17 helper cells edit

Main article: T helper 17 cell

Th17 helper cells are a subset of T helper cells developmentally distinct from Th1 and Th2 lineages. Th17 cells produce interleukin 17 (IL-17), a pro-inflammatory substance, as well as interleukins 21 and 22.[26] This means that Th17 cells are especially good at fighting extracellular pathogens[26] and fungi, particularly during mucocutaneous immunity against Candida spp.[27]

THαβ helper cells edit

THαβ helper cells provide the host immunity against viruses. Their differentiation is triggered by IFN α/β or IL-10. Their key effector cytokine is IL-10. Their main effector cells are NK cells as well as CD8 T cells, IgG B cells, and IL-10 CD4 T cells. The key THαβ transcription factors are STAT1 and STAT3 as well as IRFs. IL-10 from CD4 T cells activate NK cells' ADCC to apoptose virus-infected cells and to induce host as well as viral DNA fragmentation. IFN alpha/beta can suppress transcription to avoid virus replication and transmission. Overactivation of THαβ against autoantigen will cause type 2 antibody-dependent cytotoxic hypersensitivity. Myasthenia gravis or Graves' disease belong to this category.[28]

Limitations to the Th1/Th2 model edit

The interactions between cytokines from the Th1/Th2 model can be more complicated in some animals. For example, the Th2 cytokine IL-10 inhibits cytokine production of both Th subsets in humans. Human IL-10 (hIL-10) suppresses the proliferation and cytokine production of all T cells and the activity of macrophages, but continues to stimulate plasma cells, ensuring that antibody production still occurs. As such, hIL-10 is not believed to truly promote the Th2 response in humans, but acts to prevent over-stimulation of helper T cells while still maximising the production of antibodies.[citation needed]

There are also other types of T cells that can influence the expression and activation of helper T cells, such as natural regulatory T cells, along with less common cytokine profiles such as the Th3 subset of helper T cells. Terms such as "regulatory" and "suppression" have become ambiguous after the discovery that helper CD4+ T cells are also capable of regulating (and suppressing) their own responses outside of dedicated regulatory T cells.[citation needed]

One major difference between regulatory T cells and effector T cells is that regulatory T cells typically serve to modulate and deactivate the immune response, while effector T cell groups usually begin with immune-promoting cytokines and then switch to inhibitory cytokines later in their life cycle. The latter is a feature of Th3 cells, which transform into a regulatory subset after its initial activation and cytokine production.[citation needed]

Both regulatory T cells and Th3 cells produce the cytokine transforming growth factor-beta (TGF-β) and IL-10. Both cytokines are inhibitory to helper T cells; TGF-β suppresses the activity of most of the immune system. There is evidence to suggest that TGF-β may not suppress activated Th2 cells as effectively as it might suppress naive cells, but it is not typically considered a Th2 cytokine.[citation needed]

The novel characterisation of another T helper subtype, T helper 17 cells (Th17)[29] has cast further doubt on the basic Th1/Th2 model. These IL-17 producing cells were initially described as a pathogenic population implicated in autoimmunity but are now thought to have their own distinct effector and regulatory functions. Of note, some evidence suggest that functional plasticity is an intrinsic capacity of T helper cells. Indeed, a study in mice demonstrated that Th17 cells transform into Th1 cells in vivo.[30] A subsequent study furthermore showed that extensive T helper cell plasticity is also prominent in humans.[31]

Many of the cytokines in this article are also expressed by other immune cells (see individual cytokines for details), and it is becoming clear that while the original Th1/Th2 model is enlightening and gives insight into the functions of helper T cells, it is far too simple to define its entire role or actions. Some immunologists question the model completely, as some in vivo studies suggest that individual helper T cells usually do not match the specific cytokine profiles of the Th model, and many cells express cytokines from both profiles.[32] That said, the Th model has still played an important part in developing our understanding of the roles and behaviour of helper T cells and the cytokines they produce during an immune response.

Studies by Stockinger et al. revealed that another T helper subset may exist. Th9 cells are claimed to be an IL9 (interleukin 9)–producing T cell subset focused on defending helminth infections.[33]

Memory T cell edit

Main article: Memory T cell

Historically, memory T cells were thought to belong to either the effector or central memory subtypes, each with their own distinguishing set of cell surface markers.[34] Central memory T cells reside in the lymph nodes while effector memory T cells lack the C-C chemokine receptor type 7 (CCR7) and L-selectin (CD62L) receptors, which prevents them from trafficking to the lymph nodes.

Additional populations of memory T cells are now known to exist. These include tissue-resident memory T (Trm) cells and virtual memory T cells.[35] The single unifying theme for all memory T cell subtypes is that they are long-lived and can expand quickly to large numbers of effector T cells upon encountering their cognate antigen. By this mechanism they provide the immune system with "memory" against previously encountered pathogens.

Role in disease edit

Considering the diverse and important role helper T cells play in the immune system, it is not surprising that these cells often influence the immune response against disease. They also occasionally generate non-beneficial responses. Very rarely, the helper T cell response could lead to the death of the host.[citation needed]

Antitumor immunity edit

Main article: CD4+ T cells and antitumor immunity

Hypersensitivity edit

The immune system must achieve a balance of sensitivity in order to respond to foreign antigens without responding to the antigens of the host itself. When the immune system responds to very low levels of antigen that it usually shouldn't respond to, a hypersensitivity response occurs. Hypersensitivity is believed to be the cause of allergy and some auto-immune disease.

Hypersensitivity reactions can be divided into four types:

  • Type 1 hypersensitivity includes common immune disorders such as asthma, allergic rhinitis (hay fever), eczema, urticaria (hives) and anaphylaxis. These reactions all involve IgE antibodies, which require a Th2 response during helper T cell development. Preventive treatments, such as corticosteroids and montelukast, focus on suppressing mast cells or other allergic cells; T cells do not play a primary role during the actual inflammatory response. It's important to note that the numeral allocation of hypersensitivity "types" does not correlate (and is completely unrelated) to the "response" in the Th model.
  • Type 2 and Type 3 hypersensitivity both involve complications from auto-immune or low affinity antibodies. In both of these reactions, T cells may play an accomplice role in generating these auto-specific antibodies, although some of these reactions under Type 2 hypersensitivity would be considered normal in a healthy immune system (for example, Rhesus factor reactions during child-birth is a normal immune response against child antigens). The understanding of the role of helper T cells in these responses is limited but it is generally thought that Th2 cytokines would promote such disorders. For example, studies have suggested that lupus (SLE) and other auto-immune diseases of similar nature can be linked to the production of Th2 cytokines.
  • Type 4 hypersensitivity, also known as delayed type hypersensitivity, are caused via the over-stimulation of immune cells, commonly lymphocytes and macrophages, resulting in chronic inflammation and cytokine release. Antibodies do not play a direct role in this allergy type. T cells play an important role in this hypersensitivity, as they activate against the stimulus itself and promote the activation of other cells; particularly macrophages via Th1 cytokines.

Other cellular hypersensitivities include cytotoxic T cell mediated auto-immune disease, and a similar phenomenon; transplant rejection. Helper T cells are required to fuel the development of these diseases. In order to create sufficient auto-reactive killer T cells, interleukin-2 must be produced, and this is supplied by CD4+ T cells. CD4+ T cells can also stimulate cells such as natural killer cells and macrophages via cytokines such as interferon-gamma, encouraging these cytotoxic cells to kill host cells in certain circumstances.

The mechanism that killer T cells use during auto-immunity is almost identical to their response against viruses, and some viruses have been accused of causing auto-immune diseases such as Type 1 diabetes mellitus. Cellular auto-immune disease occurs because the host antigen recognition systems fail, and the immune system believes, by mistake, that a host antigen is foreign. As a result, the CD8+ T cells treat the host cell presenting that antigen as infected, and go on to destroy all host cells (or in the case of transplant rejection, transplant organ) that express that antigen.

Some of this section is a simplification. Many auto-immune diseases are more complex. A well-known example is rheumatoid arthritis, where both antibodies and immune cells are known to play a role in the pathology. Generally the immunology of most auto-immune diseases is not well understood.

HIV infection edit

Perhaps the best example of the importance of CD4+ T cells is demonstrated with human immunodeficiency virus (HIV) infection. HIV mainly targets lymphoid CD4+ T cells, but can infect other cells that express CD4 such as macrophages and dendritic cells (both groups express CD4 at low levels).[citation needed]

It has been proposed that during the non-symptomatic phase of HIV infection, the virus has a relatively low affinity towards T cells (and has a higher affinity for macrophages), resulting in a slow kill rate of CD4+ T cells by the immune system.[citation needed] This is initially compensated for via the production of new helper T cells from the thymus (originally from the bone marrow). Once the virus becomes lymphotropic (or T-tropic) however, it begins to infect CD4+ T cells far more efficiently (likely due to a change in the co-receptors it binds to during infection), and the immune system is overwhelmed. Studies suggest that only ~5% of the lymphoid-derived CD4 T cells targeted by HIV are permissive and become productively infected with the virus. More than 95% of the CD4 T cells that die are resting and are unable to support productive infection. These cells undergo abortive infection with HIV.[36] Cell death is triggered when the host cell detects HIV foreign DNA intermediates and initiates a suicidal death pathway in an attempt to protect the host, leading to caspase-1 activation in inflammasomes, thus causing pyroptosis (a highly inflammatory form of programmed cell death).[37][38][39]

At this point chronic inflammation ensues, and functional CD4+ T cell levels begin to decrease, eventually to a point where the CD4+ T cell population is too small to recognize the full range of antigens that could potentially be detected. The depletion of CD4 T cells and the development of chronic inflammation are signature processes in HIV pathogenesis that propel progression to acquired immune deficiency syndrome (AIDS). CD4 T cell depleted to the cell count of less than 200cell/μL in blood during AIDS allows various pathogens to escape T cell recognition, thus allowing opportunistic infections that would normally elicit a helper T cell response to bypass the immune system.[40] While these complete bypass situations only occur when the helper T cell response is absolutely necessary for infection clearance, most infections increase in severity and/or duration because the immune system's helper T cells provide less efficient immune response.

Two components of the immune system are particularly affected in AIDS, due to its CD4+ T cell dependency:

  1. CD8+ T cells are not stimulated as effectively during the AIDS stage of HIV infection, making AIDS patients very susceptible to most viruses, including HIV itself. This decline in killing of CD4+ T cells results in the virus being produced for a longer period (the infected CD4+ T cells are not killed as quickly), increasing the proliferation of the virus, and accelerating the development of the disease.
  2. Antibody class switching declines significantly once helper T cell function fails. The immune system loses its ability to improve the affinity of their antibodies, and are unable to generate B cells that can produce antibody groups such as IgG and IgA. These effects are primarily due to the loss of any helper T cell that can interact with the B lymphocyte correctly. Another symptom of AIDS is the reduction in antibody levels due to a decrease in Th2 cytokines (and less interactions by helper T cells). All of these complications result in an increased susceptibility to aggressive bacterial infections, especially in areas of the body not accessible by IgM antibodies.

If the patient does not respond to (or does not receive) HIV treatment they will succumb usually to either cancers or infections; the immune system finally reaches a point where it is no longer coordinated or stimulated enough to deal with the disease.

Inhibition of CD4 T-cell expansion during HIV infection may occur due to microbial translocation in an IL-10-dependent way. Triggering PD-1 expressed on activated monocytes by its ligand PD-L1, induces IL-10 production which inhibits CD4 T-cell function.[41]

COVID-19 edit

In coronavirus disease 2019 (COVID-19) B cell, natural killer cell, and total lymphocyte counts decline, but both CD4+ and CD8+ cells decline to a far greater extent.[42] Indicating that SARS-Cov-2 attacks the CD4+ cells during infection. Low CD4+ predicted greater likelihood of intensive care unit admission, and CD4+ cell count was the only parameter that predicted length of time for viral RNA clearance.[42] Despite the reduced levels of CD4+, COVID-19 patients with severe disease had higher levels of Th1 CD4+ cells than patients with moderate disease.[43]

See also edit

References edit

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Further reading edit

  • Doitsh G, Greene WC (March 2016). "Dissecting How CD4 T Cells Are Lost During HIV Infection". Cell Host & Microbe. 19 (3): 280–291. doi:10.1016/j.chom.2016.02.012. PMC 4835240. PMID 26962940.
  • Kanno Y, Vahedi G, Hirahara K, Singleton K, O'Shea JJ (2012). "Transcriptional and epigenetic control of T helper cell specification: molecular mechanisms underlying commitment and plasticity". Annual Review of Immunology. 30: 707–731. doi:10.1146/annurev-immunol-020711-075058. PMC 3314163. PMID 22224760.

External links edit

 
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April 10, 2024
helper, cell, redirects, here, professional, wrestling, team, hybrid, cells, also, known, cells, positive, cells, type, cell, that, play, important, role, adaptive, immune, system, they, activity, other, immune, cells, releasing, cytokines, they, considered, e. Th2 redirects here For the professional wrestling tag team see The Hybrid 2 The T helper cells Th cells also known as CD4 cells or CD4 positive cells are a type of T cell that play an important role in the adaptive immune system They aid the activity of other immune cells by releasing cytokines They are considered essential in B cell antibody class switching breaking cross tolerance in dendritic cells in the activation and growth of cytotoxic T cells and in maximizing bactericidal activity of phagocytes such as macrophages and neutrophils CD4 cells are mature Th cells that express the surface protein CD4 Genetic variation in regulatory elements expressed by CD4 cells determines susceptibility to a broad class of autoimmune diseases 1 Activation of macrophage or B cell by T helper cell Contents 1 Structure and function 2 Activation of naive helper T cells 2 1 Activation signal 1 2 2 Survival signal 2 2 3 Differentiation signal 3 3 Effector function 4 Determination of the effector T cell response 4 1 Th1 Th2 model 4 2 Th17 helper cells 4 3 THab helper cells 4 4 Limitations to the Th1 Th2 model 5 Memory T cell 6 Role in disease 6 1 Antitumor immunity 6 2 Hypersensitivity 6 3 HIV infection 6 4 COVID 19 7 See also 8 References 9 Further reading 10 External linksStructure and function editTh cells contain and release cytokines to aid other immune cells Cytokines are small protein mediators that alter the behavior of target cells that express receptors for those cytokines These cells help polarize the immune response depending on the nature of the immunological insult for example virus vs extracellular bacterium vs intracellular bacterium vs helminth vs fungus vs protist citation needed Mature Th cells express the surface protein CD4 and are referred to as CD4 T cells CD4 T cells are generally treated as having a pre defined role as helper T cells within the immune system For example when an antigen presenting cell displays a peptide antigen on MHC class II proteins a CD4 cell will aid those cells through a combination of cell to cell interactions e g CD40 protein and CD40L and through cytokines Th cells are not a monolithic immunological entity because they are diverse in terms of function and their interaction with partner cells In general mature naive T cells are stimulated by professional antigen presenting cells to acquire an effector module These are defined by the presence of a lineage determining or lineage specifying transcription factor also called master regulator though the term has been criticized for being too reductive 2 The loss of function in a lineage specifying transcription factor results in the absence of the corresponding class of helper T cell which can be devastating for the health of the host Activation of naive helper T cells edit nbsp T cell dependent B cell activation showing TH2 cell left B cell right and several interaction molecules self made according to Janeway et al Immunologie Berlin 2002 Following Development in the thymus these cells termed recent thymic emigrants RTE egress from the thymus and home to secondary lymphoid organs SLO spleen and lymph nodes Of note only a very small minority of T cells egresses from the thymus estimates commonly range from 1 5 but some experts feel even this is generous 3 Maturation of RTE in SLO results in the generation of mature naive T cells naive meaning they have never been exposed to the antigen that they are programmed to respond to but naive T cells now lack or have downregulated reduced expression of the RTE related surface markers such as CD31 PTK7 Complement Receptor 1 and 2 CR1 CR2 and the production of interleukin 8 IL 8 4 5 Like all T cells they express the T cell receptor CD3 complex The T cell receptor TCR consists of both constant and variable regions The variable region determines what antigen the T cell can respond to CD4 T cells have TCRs with an affinity for Class II MHC and CD4 is involved in determining MHC affinity during maturation in the thymus Class II MHC proteins are generally only found on the surface of professional antigen presenting cells APCs Professional antigen presenting cells are primarily dendritic cells macrophages and B cells although dendritic cells are the only cell group that expresses MHC Class II constitutively at all times Some APCs also bind native or unprocessed antigens to their surface such as follicular dendritic cells these are not the same type of cells as the dendritic cells of the immune system but rather have a non hematopoietic origin and in general lack MHC Class II meaning they are not true professional antigen presenting cells however follicular dendritic cells may acquire MHC Class II proteins via exosomes that become attached to them 6 T cells require antigens to be processed into short fragments which form linear epitopes on MHC Class II in the case of helper T cells because they express CD4 or MHC class I in the case of cytotoxic T cells which express CD8 MHC Class II binding pockets are flexible with respect to the length of the peptides they hold Generally there are 9 core amino acid residues with several flanking amino acids which form a length of about 12 16 amino acids total 7 but have been known to hold as many as 25 amino acids 8 By comparison MHC Class I proteins are usually 9 10 peptides long 9 The activation of naive T cells is commonly explained in terms of the 3 signal model elaborated upon below 10 Activation signal 1 edit nbsp Antigen presentation stimulates naive CD8 and CD4 T cells to become mature cytotoxic CD8 cells and helper CD4 cells respectively During an immune response professional antigen presenting cells APCs endocytose antigens typically bacteria or viruses which undergo processing then travel from the infection site to the lymph nodes Typically the APC responsible is a dendritic cell If the antigen expresses appropriate molecular patterns sometimes known as signal 0 it can induce maturation of the dendritic cell which results in enhanced expression of costimulatory molecules needed to activate T cells see signal 2 11 and MHC Class II 12 Once at the lymph nodes the APCs begin to present antigen peptides that are bound to Class II MHC allowing CD4 T cells that express the specific TCRs against the peptide MHC complex to activate citation needed When a Th cell encounters and recognizes the antigen on an APC the TCR CD3 complex binds strongly to the peptide MHC complex present on the surface of professional APCs CD4 a co receptor of the TCR complex also binds to a different section of the MHC molecule It is estimated that approximately 50 of these interactions are required for the activation of a helper T cell and assemblies known as microclusters have been observed forming between the TCR CD3 CD4 complexes of the T cell and the MHC Class II proteins of the dendritic cell at the zone of contact When these all come together the CD4 is able to recruit a kinase called Lck which phosphorylates immunoreceptor tyrosine based activation motifs ITAMs present on the CD3 gamma delta epsilon and zeta chains The protein ZAP 70 can bind these phosphorylated ITAMs via its SH2 domain and then itself becomes phosphorylated wherein it orchestrates the downstream signaling required for T cell activation Lck activation is controlled by the opposing actions of CD45 and Csk 13 CD45 activates Lck by dephosphorylating a tyrosine in its C terminal tail while Csk phosphorylates Lck at that site The loss of CD45 produces a form of SCID because failure to activate Lck prevents appropriate T cell signaling Memory T cells also make use of this pathway and have higher levels of Lck expressed and the function of Csk is inhibited in these cells 14 The binding of the antigen MHC to the TCR complex and CD4 may also help the APC and the Th cell adhere during Th cell activation but the integrin protein LFA 1 on the T cell and ICAM on the APC are the primary molecules of adhesion in this cell interaction citation needed It is unknown what role the relatively bulky extracellular region of CD45 plays during cell interactions but CD45 has various isoforms that change in size depending on the Th cell s activation and maturation status For example CD45 shortens in length following Th activation CD45RA to CD45RO but whether this change in length influences activation is unknown It has been proposed that the larger CD45RA may decrease the accessibility of the T cell receptor for the antigen MHC molecule thereby necessitating an increase in the affinity and specificity of the T cell for activation However once the activation has occurred CD45 shortens allowing easier interactions and activation as an effector T helper cell citation needed Survival signal 2 edit Having received the first TCR CD3 signal the naive T cell must activate a second independent biochemical pathway known as Signal 2 This verification step is a protective measure to ensure that a T cell is responding to a foreign antigen If this second signal is not present during initial antigen exposure the T cell presumes that it is auto reactive This results in the cell becoming anergic anergy is generated from the unprotected biochemical changes of Signal 1 Anergic cells will not respond to any antigen in the future even if both signals are present later on These cells are generally believed to circulate throughout the body with no value until they undergo apoptosis 15 The second signal involves an interaction between CD28 on the CD4 T cell and the proteins CD80 B7 1 or CD86 B7 2 on the professional APCs Both CD80 and CD86 activate the CD28 receptor These proteins are also known as co stimulatory molecules citation needed Although the verification stage is necessary for the activation of naive helper T cells the importance of this stage is best demonstrated during the similar activation mechanism of CD8 cytotoxic T cells As naive CD8 T cells have no true bias towards foreign sources these T cells must rely on the activation of CD28 for confirmation that they recognise a foreign antigen as CD80 CD86 is only expressed by active APC s CD28 plays an important role in decreasing the risk of T cell auto immunity against host antigens citation needed Once the naive T cell has both pathways activated the biochemical changes induced by Signal 1 are altered allowing the cell to activate instead of undergoing anergy The second signal is then obsolete only the first signal is necessary for future activation This is also true for memory T cells which is one example of learned immunity Faster responses occur upon reinfection because memory T cells have already undergone confirmation and can produce effector cells much sooner citation needed Differentiation signal 3 edit Once the two signal activation is complete the T helper cell Th then allows itself to proliferate It achieves this by releasing a potent T cell growth factor called interleukin 2 IL 2 which acts upon itself in an autocrine fashion Activated T cells also produce the alpha sub unit of the IL 2 receptor CD25 or IL 2R enabling a fully functional receptor that can bind with IL 2 which in turn activates the T cell s proliferation pathways citation needed The autocrine or paracrine secretion of IL 2 can bind to that same Th cell or neighboring Th s via the IL 2R thus driving proliferation and clonal expansion The Th cells receiving both signals of activation and proliferation will then become Th0 T helper 0 cells that secrete IL 2 IL 4 and interferon gamma IFN g The Th0 cells will then differentiate into Th1 or Th2 cells depending on cytokine environment IFN g drives Th1 cell production while IL 10 and IL 4 inhibit Th1 cell production Conversely IL 4 drives Th2 cell production and IFN g inhibits Th2 cells These cytokines are pleiotropic and carry out many other functions of the immune response citation needed Effector function editIn 1991 three groups reported discovering CD154 which is the molecular basis of T cell helper function Seth Lederman at Columbia University generated a murine monoclonal antibody 5c8 that inhibited contact dependent T cell helper function in human cells which characterized the 32 kDa surface protein transiently expressed on CD4 T cells 16 Richard Armitage at Immunex cloned a cDNA encoding CD154 by screening an expression library with CD40 Ig 17 Randolph Noelle at Dartmouth Medical School generated an antibody that bound a 39 kDa protein on murine T cells and inhibited helper function 18 Determination of the effector T cell response editHelper T cells are capable of influencing a variety of immune cells and the T cell response generated including the extracellular signals such as cytokines can be essential for a successful outcome from infection In order to be effective helper T cells must determine which cytokines will allow the immune system to be most useful or beneficial for the host Understanding exactly how helper T cells respond to immune challenges is currently of major interest in immunology because such knowledge may be very useful in the treatment of disease and in increasing the effectiveness of vaccination citation needed Th1 Th2 model edit Proliferating helper T cells that develop into effector T cells differentiate into two major subtypes of cells known as Th1 and Th2 cells also known as Type 1 and Type 2 helper T cells respectively Th1 helper cells lead to an increased cell mediated response primarily by macrophages and cytotoxic T cells 19 typically against intracellular bacteria and protozoa They are triggered by the polarising cytokine IL 12 and their effector cytokines are IFN g and IL 2 The main effector cells of Th1 immunity are macrophages as well as CD8 T cells IgG B cells and IFN g CD4 T cells The key Th1 transcription factors are STAT4 and T bet IFN g secreted by CD4 T cells can activate macrophages to phagocytose and digest intracellular bacteria and protozoa In addition IFN g can activate iNOS inducible nitric oxide synthase to produce nitric oxide free radicals to directly kill intracellular bacteria and protozoa Th1 overactivation against autoantigens will cause Type IV or delayed type hypersensitivity reaction Tuberculin reaction and Type 1 diabetes belong to this category of autoimmunity 20 Th2 helper cells lead to a humoral immune response 19 typically against extracellular parasites such as helminths They are triggered by the polarising cytokines IL 4 and IL 2 and their effector cytokines are IL 4 IL 5 IL 9 IL 10 IL 13 and IL 25 The main effector cells are eosinophils basophils and mast cells as well as B cells and IL 4 IL 5 CD4 T cells The key Th2 transcription factors are STAT6 and GATA3 21 IL 4 is the positive feedback cytokine for Th2 cells differentiation Besides IL 4 stimulates B cells to produce IgE antibodies which in turn stimulate mast cells to release histamine serotonin and leukotriene to cause broncho constriction intestinal peristalsis gastric fluid acidification to expel helminths IL 5 from CD4 T cells will activate eosinophils to attack helminths IL 10 suppresses Th1 cells differentiation and function of dendritic cells Th2 overactivation against antigen will cause Type I hypersensitivity which is an allergic reaction mediated by IgE Allergic rhinitis atopic dermatitis and asthma belong to this category of overactivation 20 In addition to expressing different cytokines Th2 cells also differ from Th1 cells in their cell surface glycans oligosaccharides which makes them less susceptible to some inducers of cell death 22 23 nbsp Th1 Th2 Model for helper T cells An antigen is ingested and processed by an APC It presents fragments from it to T cells The upper Th0 is a T helper cell The fragment is presented to it by MHC2 24 IFN g interferon g TGF b transforming growth factor b mo macrophage IL 2 interleukin 2 IL 4 interleukin 4Th1 Th2 dichotomy Type 1 Th1 Type 2 Th2 20 Main partner cell type Macrophage CD8 T cell B cell eosinophil mast cellCytokines produced Interferon gamma IFNg and TNF b Interleukin 2 and interleukin 10 production has been reported in activated Th1 cell 25 Interleukin 4 interleukin 5 interleukin 6 interleukin 9 interleukin 10 interleukin 13Immune stimulation promoted Cellular immune system Maximizes the killing efficacy of the macrophages and the proliferation of cytotoxic CD8 T cells Also promotes the production of IgG an opsonizing antibody Humoral immune system Stimulates B cells into proliferation to induce B cell antibody class switching and to increase neutralizing antibody production IgG IgM and IgA as well as IgE antibodies Other functions The Type 1 cytokine IFNg increases the production of interleukin 12 by dendritic cells and macrophages and via positive feedback IL 12 stimulates the production of IFNg in helper T cells thereby promoting the Th1 profile IFNg also inhibits the production of cytokines such as interleukin 4 an important cytokine associated with the Type 2 response and thus it also acts to preserve its own response The Type 2 response promotes its own profile using two different cytokines Interleukin 4 acts on helper T cells to promote the production of Th2 cytokines including itself it is auto regulatory while interleukin 10 IL 10 inhibits a variety of cytokines including interleukin 2 and IFNg in helper T cells and IL 12 in dendritic cells and macrophages The combined action of these two cytokines suggests that once the T cell has decided to produce these cytokines that decision is preserved and also encourages other T cells to do the same While we know about the types of cytokine patterns helper T cells tend to produce we understand less about how the patterns themselves are decided Various evidence suggests that the type of APC presenting the antigen to the T cell has a major influence on its profile Other evidence suggests that the concentration of antigen presented to the T cell during primary activation influences its choice The presence of some cytokines such as the ones mentioned above will also influence the response that will eventually be generated but our understanding is nowhere near complete Th17 helper cells edit Main article T helper 17 cell Th17 helper cells are a subset of T helper cells developmentally distinct from Th1 and Th2 lineages Th17 cells produce interleukin 17 IL 17 a pro inflammatory substance as well as interleukins 21 and 22 26 This means that Th17 cells are especially good at fighting extracellular pathogens 26 and fungi particularly during mucocutaneous immunity against Candida spp 27 THab helper cells edit THab helper cells provide the host immunity against viruses Their differentiation is triggered by IFN a b or IL 10 Their key effector cytokine is IL 10 Their main effector cells are NK cells as well as CD8 T cells IgG B cells and IL 10 CD4 T cells The key THab transcription factors are STAT1 and STAT3 as well as IRFs IL 10 from CD4 T cells activate NK cells ADCC to apoptose virus infected cells and to induce host as well as viral DNA fragmentation IFN alpha beta can suppress transcription to avoid virus replication and transmission Overactivation of THab against autoantigen will cause type 2 antibody dependent cytotoxic hypersensitivity Myasthenia gravis or Graves disease belong to this category 28 Limitations to the Th1 Th2 model edit The interactions between cytokines from the Th1 Th2 model can be more complicated in some animals For example the Th2 cytokine IL 10 inhibits cytokine production of both Th subsets in humans Human IL 10 hIL 10 suppresses the proliferation and cytokine production of all T cells and the activity of macrophages but continues to stimulate plasma cells ensuring that antibody production still occurs As such hIL 10 is not believed to truly promote the Th2 response in humans but acts to prevent over stimulation of helper T cells while still maximising the production of antibodies citation needed There are also other types of T cells that can influence the expression and activation of helper T cells such as natural regulatory T cells along with less common cytokine profiles such as the Th3 subset of helper T cells Terms such as regulatory and suppression have become ambiguous after the discovery that helper CD4 T cells are also capable of regulating and suppressing their own responses outside of dedicated regulatory T cells citation needed One major difference between regulatory T cells and effector T cells is that regulatory T cells typically serve to modulate and deactivate the immune response while effector T cell groups usually begin with immune promoting cytokines and then switch to inhibitory cytokines later in their life cycle The latter is a feature of Th3 cells which transform into a regulatory subset after its initial activation and cytokine production citation needed Both regulatory T cells and Th3 cells produce the cytokine transforming growth factor beta TGF b and IL 10 Both cytokines are inhibitory to helper T cells TGF b suppresses the activity of most of the immune system There is evidence to suggest that TGF b may not suppress activated Th2 cells as effectively as it might suppress naive cells but it is not typically considered a Th2 cytokine citation needed The novel characterisation of another T helper subtype T helper 17 cells Th17 29 has cast further doubt on the basic Th1 Th2 model These IL 17 producing cells were initially described as a pathogenic population implicated in autoimmunity but are now thought to have their own distinct effector and regulatory functions Of note some evidence suggest that functional plasticity is an intrinsic capacity of T helper cells Indeed a study in mice demonstrated that Th17 cells transform into Th1 cells in vivo 30 A subsequent study furthermore showed that extensive T helper cell plasticity is also prominent in humans 31 Many of the cytokines in this article are also expressed by other immune cells see individual cytokines for details and it is becoming clear that while the original Th1 Th2 model is enlightening and gives insight into the functions of helper T cells it is far too simple to define its entire role or actions Some immunologists question the model completely as some in vivo studies suggest that individual helper T cells usually do not match the specific cytokine profiles of the Th model and many cells express cytokines from both profiles 32 That said the Th model has still played an important part in developing our understanding of the roles and behaviour of helper T cells and the cytokines they produce during an immune response Studies by Stockinger et al revealed that another T helper subset may exist Th9 cells are claimed to be an IL9 interleukin 9 producing T cell subset focused on defending helminth infections 33 Memory T cell editMain article Memory T cell Historically memory T cells were thought to belong to either the effector or central memory subtypes each with their own distinguishing set of cell surface markers 34 Central memory T cells reside in the lymph nodes while effector memory T cells lack the C C chemokine receptor type 7 CCR7 and L selectin CD62L receptors which prevents them from trafficking to the lymph nodes Additional populations of memory T cells are now known to exist These include tissue resident memory T Trm cells and virtual memory T cells 35 The single unifying theme for all memory T cell subtypes is that they are long lived and can expand quickly to large numbers of effector T cells upon encountering their cognate antigen By this mechanism they provide the immune system with memory against previously encountered pathogens Role in disease editConsidering the diverse and important role helper T cells play in the immune system it is not surprising that these cells often influence the immune response against disease They also occasionally generate non beneficial responses Very rarely the helper T cell response could lead to the death of the host citation needed Antitumor immunity edit Main article CD4 T cells and antitumor immunity Hypersensitivity edit The immune system must achieve a balance of sensitivity in order to respond to foreign antigens without responding to the antigens of the host itself When the immune system responds to very low levels of antigen that it usually shouldn t respond to a hypersensitivity response occurs Hypersensitivity is believed to be the cause of allergy and some auto immune disease Hypersensitivity reactions can be divided into four types Type 1 hypersensitivity includes common immune disorders such as asthma allergic rhinitis hay fever eczema urticaria hives and anaphylaxis These reactions all involve IgE antibodies which require a Th2 response during helper T cell development Preventive treatments such as corticosteroids and montelukast focus on suppressing mast cells or other allergic cells T cells do not play a primary role during the actual inflammatory response It s important to note that the numeral allocation of hypersensitivity types does not correlate and is completely unrelated to the response in the Th model Type 2 and Type 3 hypersensitivity both involve complications from auto immune or low affinity antibodies In both of these reactions T cells may play an accomplice role in generating these auto specific antibodies although some of these reactions under Type 2 hypersensitivity would be considered normal in a healthy immune system for example Rhesus factor reactions during child birth is a normal immune response against child antigens The understanding of the role of helper T cells in these responses is limited but it is generally thought that Th2 cytokines would promote such disorders For example studies have suggested that lupus SLE and other auto immune diseases of similar nature can be linked to the production of Th2 cytokines Type 4 hypersensitivity also known as delayed type hypersensitivity are caused via the over stimulation of immune cells commonly lymphocytes and macrophages resulting in chronic inflammation and cytokine release Antibodies do not play a direct role in this allergy type T cells play an important role in this hypersensitivity as they activate against the stimulus itself and promote the activation of other cells particularly macrophages via Th1 cytokines Other cellular hypersensitivities include cytotoxic T cell mediated auto immune disease and a similar phenomenon transplant rejection Helper T cells are required to fuel the development of these diseases In order to create sufficient auto reactive killer T cells interleukin 2 must be produced and this is supplied by CD4 T cells CD4 T cells can also stimulate cells such as natural killer cells and macrophages via cytokines such as interferon gamma encouraging these cytotoxic cells to kill host cells in certain circumstances The mechanism that killer T cells use during auto immunity is almost identical to their response against viruses and some viruses have been accused of causing auto immune diseases such as Type 1 diabetes mellitus Cellular auto immune disease occurs because the host antigen recognition systems fail and the immune system believes by mistake that a host antigen is foreign As a result the CD8 T cells treat the host cell presenting that antigen as infected and go on to destroy all host cells or in the case of transplant rejection transplant organ that express that antigen Some of this section is a simplification Many auto immune diseases are more complex A well known example is rheumatoid arthritis where both antibodies and immune cells are known to play a role in the pathology Generally the immunology of most auto immune diseases is not well understood HIV infection edit Perhaps the best example of the importance of CD4 T cells is demonstrated with human immunodeficiency virus HIV infection HIV mainly targets lymphoid CD4 T cells but can infect other cells that express CD4 such as macrophages and dendritic cells both groups express CD4 at low levels citation needed It has been proposed that during the non symptomatic phase of HIV infection the virus has a relatively low affinity towards T cells and has a higher affinity for macrophages resulting in a slow kill rate of CD4 T cells by the immune system citation needed This is initially compensated for via the production of new helper T cells from the thymus originally from the bone marrow Once the virus becomes lymphotropic or T tropic however it begins to infect CD4 T cells far more efficiently likely due to a change in the co receptors it binds to during infection and the immune system is overwhelmed Studies suggest that only 5 of the lymphoid derived CD4 T cells targeted by HIV are permissive and become productively infected with the virus More than 95 of the CD4 T cells that die are resting and are unable to support productive infection These cells undergo abortive infection with HIV 36 Cell death is triggered when the host cell detects HIV foreign DNA intermediates and initiates a suicidal death pathway in an attempt to protect the host leading to caspase 1 activation in inflammasomes thus causing pyroptosis a highly inflammatory form of programmed cell death 37 38 39 At this point chronic inflammation ensues and functional CD4 T cell levels begin to decrease eventually to a point where the CD4 T cell population is too small to recognize the full range of antigens that could potentially be detected The depletion of CD4 T cells and the development of chronic inflammation are signature processes in HIV pathogenesis that propel progression to acquired immune deficiency syndrome AIDS CD4 T cell depleted to the cell count of less than 200cell mL in blood during AIDS allows various pathogens to escape T cell recognition thus allowing opportunistic infections that would normally elicit a helper T cell response to bypass the immune system 40 While these complete bypass situations only occur when the helper T cell response is absolutely necessary for infection clearance most infections increase in severity and or duration because the immune system s helper T cells provide less efficient immune response Two components of the immune system are particularly affected in AIDS due to its CD4 T cell dependency CD8 T cells are not stimulated as effectively during the AIDS stage of HIV infection making AIDS patients very susceptible to most viruses including HIV itself This decline in killing of CD4 T cells results in the virus being produced for a longer period the infected CD4 T cells are not killed as quickly increasing the proliferation of the virus and accelerating the development of the disease Antibody class switching declines significantly once helper T cell function fails The immune system loses its ability to improve the affinity of their antibodies and are unable to generate B cells that can produce antibody groups such as IgG and IgA These effects are primarily due to the loss of any helper T cell that can interact with the B lymphocyte correctly Another symptom of AIDS is the reduction in antibody levels due to a decrease in Th2 cytokines and less interactions by helper T cells All of these complications result in an increased susceptibility to aggressive bacterial infections especially in areas of the body not accessible by IgM antibodies If the patient does not respond to or does not receive HIV treatment they will succumb usually to either cancers or infections the immune system finally reaches a point where it is no longer coordinated or stimulated enough to deal with the disease Inhibition of CD4 T cell expansion during HIV infection may occur due to microbial translocation in an IL 10 dependent way Triggering PD 1 expressed on activated monocytes by its ligand PD L1 induces IL 10 production which inhibits CD4 T cell function 41 COVID 19 edit In coronavirus disease 2019 COVID 19 B cell natural killer cell and total lymphocyte counts decline but both CD4 and CD8 cells decline to a far greater extent 42 Indicating that SARS Cov 2 attacks the CD4 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2020 COVID 19 poses a riddle for the immune system Nature 584 7821 345 346 doi 10 1038 d41586 020 02379 1 PMID 32807916 Further reading editDoitsh G Greene WC March 2016 Dissecting How CD4 T Cells Are Lost During HIV Infection Cell Host amp Microbe 19 3 280 291 doi 10 1016 j chom 2016 02 012 PMC 4835240 PMID 26962940 Kanno Y Vahedi G Hirahara K Singleton K O Shea JJ 2012 Transcriptional and epigenetic control of T helper cell specification molecular mechanisms underlying commitment and plasticity Annual Review of Immunology 30 707 731 doi 10 1146 annurev immunol 020711 075058 PMC 3314163 PMID 22224760 External links edit nbsp Wikimedia Commons has media related to T helper cell T cell Group T Cells Cardiff University Retrieved from https en wikipedia org w index php title T helper cell amp oldid 1216761326, wikipedia, wiki, book, books, library,

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