Toll-Like Receptors

Toll-like receptors ( TLRs ) are homologous to a Drosophila protein called Toll, which was discovered for its role in the development of the fly and later shown to be essential for protecting flies against fungal infections. In vertebrates, there are 10 different TLRs specific for different components of microbes ( Fig. 2.3 ). TLR-2 recognizes several glycolipids and peptidoglycans that are made by gram-positive bacteria and some parasites; TLR-3 is specific for double-stranded RNA, and TLR-7 and TLR-8 are specific for single-stranded RNA; TLR-4 is specific for bacterial LPS (endotoxin), made by gram-negative bacteria; TLR-5 is specific for a bacterial flagellar protein called flagellin; and TLR-9 recognizes unmethylated CpG DNA, which is abundant in microbial genomes. TLRs specific for microbial proteins, lipids, and polysaccharides (many of which are present in bacterial cell walls) are located on cell surfaces, where they recognize these products of extracellular microbes. TLRs that recognize nucleic acids are in endosomes, into which microbes are ingested and where they are digested and their nucleic acids are released.

Specificities of Toll-like receptors.

Different TLRs recognize many different, structurally diverse products of microbes. Plasma membrane TLRs are specific for cell wall components of bacteria, and endosomal TLRs recognize nucleic acids. All TLRs contain a ligand-binding domain composed of leucine-rich motifs and a cytoplasmic signaling, Toll-like interleukin-1 (IL-1) receptor (TIR) domain. ds, Double-stranded; LPS, lipopolysaccharide; ss, single-stranded.

Signals generated by TLRs activate transcription factors that stimulate expression of cytokines and other proteins involved in the inflammatory response and in the antimicrobial functions of activated phagocytes and other cells ( Fig. 2.4 ). Among the most important transcription factors activated by TLR signals are members of the nuclear factor κB (NF-κB) family, which promote expression of various cytokines and endothelial adhesion molecules that play important roles in inflammation, and interferon regulatory factors (IRFs), which stimulate production of the antiviral cytokines, type I interferons.

Signaling functions of toll-like receptors.

TLRs activate similar signaling mechanisms, which involve adaptor proteins and lead to the activation of transcription factors. These transcription factors stimulate the production of proteins that mediate inflammation and antiviral defense. NF-κB, Nuclear factor κB.

Rare autosomal recessive diseases characterized by recurrent infections are caused by mutations affecting TLRs or their signaling molecules, highlighting the importance of these pathways in host defense against microbes. For example, individuals with mutations affecting TLR-3 are susceptible to herpes simplex virus infections, particularly encephalitis, and mutations in MyD88, the adaptor protein downstream of several TLRs, make individuals susceptible to bacterial pneumonias.

NOD-Like Receptors

The NOD-like receptors (NLRs) are a large family of innate receptors that sense DAMPs and PAMPs in the cytosol of cells and initiate signaling events that promote inflammation. All NLRs contain a nucleotide oligomerization domain (NOD, named because of the activity it was originally associated with) but different NLRs have different N-terminal domains. Two important NLRs, NOD1 and NOD2, have N-terminal caspase related domains (CARDs), and are expressed in several cell types including mucosal barrier epithelial cells and phagocytes. NOD1 and NOD2 both recognize peptides derived from bacterial cell wall peptidoglycans, and in response, they generate signals that activate the NF-κB transcription factor, which promotes expression of genes encoding inflammatory proteins. NOD2 is highly expressed in intestinal Paneth cells in the small bowel, where it stimulates expression of antimicrobial substances called defensins in response to pathogens. Some polymorphisms of the NOD2 gene are associated with inflammatory bowel disease, perhaps because these variants have reduced function and allow luminal microbes to penetrate the intestinal wall and trigger inflammation.

Inflammasomes

Inflammasomes are multiprotein complexes that assemble in the cytosol of cells in response to microbes or changes associated with cell injury, and proteolytically generate active forms of the inflammatory cytokines IL-1β and IL-18. IL-1β and IL-18 are synthesized as inactive precursors, which must be cleaved by the enzyme caspase-1 to become active cytokines that are released from the cell and promote inflammation. Inflammasomes are composed of oligomers of a sensor, caspase-1, and an adaptor that links the two. There are many different types of inflammasomes, most of which use 1 of 10 different NLR-family proteins as sensors. These sensors directly recognize microbial products in the cytosol or sense changes in the amount of endogenous molecules or ions in the cytosol that indirectly indicate the presence of infection or cell damage. Some inflammasomes use sensors that are not in the NLR family, such as AIM-family DNA sensors and a protein called pyrin. After recognition of microbial or endogenous ligands, the NLR sensors oligomerize with an adaptor protein and an inactive (pro) form of the enzyme caspase-1 to form the inflammasome, resulting in generation of the active form of caspase-1 ( Fig. 2.5 ). Active caspase-1 cleaves the precursor form of the cytokine interleukin-1β (IL-1β), pro-IL-1β, to generate biologically active IL-1β. As discussed later, IL-1 induces acute inflammation and causes fever.

The inflammasome.

Shown is the activation of the NLRP3 inflammasome, which processes pro–interleukin-1β (pro–IL-1β) to active IL-1. The synthesis of pro–IL-1β is induced by various PAMPs or DAMPs through pattern recognition receptor signaling. Subsequent production of biologically active IL-1β is mediated by the inflammasome. The inflammasome also stimulates production of active IL-18, which is closely related to IL-1 (not shown). Other forms of the inflammasome exist which contain sensors other than NLRP3, including NLRP1, NLRC4, or AIM2. ATP, Adenosine triphosphate; NLRP3, NOD-like receptor family, pyrin domain containing 3; TLRs, Toll-like receptors.

One of the best characterized inflammasomes uses NLRP3 (NOD-like receptor family, pyrin domain containing 3) as a sensor. The NLRP3 inflammasome is expressed in innate immune cells including macrophages and neutrophils, as well as keratinocytes in the skin and other cells. A wide variety of stimuli induce formation of the NLRP3 inflammasome, including crystalline substances such as uric acid (a by-product of DNA breakdown, indicating nuclear damage) and cholesterol crystals, extracellular adenosine triphosphate (ATP) (an indicator of mitochondrial damage) binding to cell surface purinoceptors, reduced intracellular potassium ion (K ⁺ ) concentration (which indicates plasma membrane damage), and reactive oxygen species. Thus, the inflammasome reacts to injury affecting various cellular components. How NLRP3 recognizes such diverse types of cellular stress or damage is not clearly understood. Inflammasome activation is tightly controlled by posttranslational modifications such as ubiquitination and phosphorylation, which block inflammasome assembly or activation, and some micro-RNAs, which inhibit NLRP3 messenger RNA.

Inflammasome activation also causes an inflammatory form of programmed cell death of macrophages and DCs called pyroptosis , characterized by swelling of cells, loss of plasma membrane integrity, and release of inflammatory cytokines. Activated caspase-1 cleaves a protein called gasdermin D. The N-terminal fragment of gasdermin D oligomerizes and forms a channel in the plasma membrane that initially allows the egress of mature IL-1β, and eventually permits the influx of ions, followed by cell swelling and pyroptosis.

The inflammasome is important not only for host defense but also because of its role in several diseases. Gain-of-function mutations in NLRP3, and less frequently, loss-of-function mutations in regulators of inflammasome activation, are the cause of autoinflammatory syndromes , characterized by uncontrolled and spontaneous inflammation. IL-1 antagonists are effective treatments for these diseases. The common joint disease gout is caused by deposition of urate crystals and subsequent inflammation mediated by inflammasome recognition of the crystals and IL-1β production. The inflammasome may also contribute to atherosclerosis, in which inflammation caused by cholesterol crystals may play a role.

Cytosolic RNA and DNA Sensors

The innate immune system includes several cytosolic proteins that recognize microbial RNA or DNA and respond by generating signals that lead to the production of inflammatory and antiviral cytokines.

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  The RIG-like receptors (RLRs) are cytosolic proteins that sense viral RNA and induce the production of the antiviral type I IFNs. RLRs recognize features of viral RNAs not typical of mammalian RNA, such as dsRNA that is longer than dsRNA that may be formed transiently in normal cells, or RNA with a 5′ triphosphate moiety not present in mammalian host cell cytosolic RNA. (Host RNAs are modified and have a 5’ 7methyl-guanosine “cap.”) RLRs are expressed in many cell types that are susceptible to infection by RNA viruses. After binding viral RNAs, RLRs interact with a mitochondrial membrane protein called mitochondrial antiviral-signaling (MAVS), which is required to initiate signaling events that activate transcription factors that induce the production of type I IFNs.

  
  
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  Cytosolic DNA sensors (CDSs) include several structurally related proteins that recognize microbial double-stranded (ds) DNA in the cytosol and activate signaling pathways that initiate antimicrobial responses, including type 1 IFN production and autophagy. DNA may be released into the cytosol from various intracellular microbes. Since mammalian DNA is not normally in the cytosol, the innate cytosolic DNA sensors will see only microbial DNA.

Most innate cytosolic DNA sensors engage the stimulator of IFN genes ( STING ) pathway to induce type 1 IFN production ( Fig. 2.6 ). In this pathway, cytosolic dsDNA binds to the enzyme cyclic GMP-AMP synthase (cGAS), which activates the production of a cyclic dinucleotide signaling molecule called cyclic GMP-AMP (cGAMP), which binds to an endoplasmic reticulum membrane adaptor protein called stimulator of interferon gene (STING). In addition, bacteria themselves produce other cyclic dinucleotides that also bind to STING. Upon binding these cyclic dinucleotides, STING initiates signaling events that lead to transcriptional activation and expression of type I IFN genes. STING also stimulates autophagy, a mechanism by which cells degrade their own organelles in lysosomes. Autophagy is used in innate immunity to deliver cytosolic microbes to the lysosome, where they are killed by proteolytic enzymes. Other cytosolic DNA sensors besides cGAS can also activate STING.

Cytosolic DNA sensors and the STING pathway.

Cytoplasmic microbial dsDNA activates the enzyme cGAS, which catalyzes the synthesis of cyclic GMP-AMP (cGAMP) from ATP and GTP. cGAMP binds to STING in the endoplasmic reticulum membrane, and then STING recruits and activates the kinase TBK1, which phosphorylates IRF3. Phospo-IRF3 moves to the nucleus, where it induces type I IFN gene expression. The bacterial second messenger molecules cyclic di-GMP (c-di-GMP) and cyclic di-AMP (c-di-AMP) are directly sensed by STING. STING also stimulates autophagy and lysosomal degradation of pathogens associated with cytoplasmic organelles. cGAS, Cyclic GMP-AMP synthase; IFN, interferon; IRF3, interferon regulatory factor 3.

Other Cellular Receptors of Innate Immunity

Many other receptor types are involved in innate immune responses to microbes (see Fig. 2.2 ).

Some lectins (carbohydrate-recognizing proteins) in the plasma membrane are receptors specific for fungal glucans (these receptors are called dectins) or for terminal mannose residues (called mannose receptors); they are involved in the phagocytosis of fungi and bacteria and in inflammatory responses to these pathogens. A cell surface receptor expressed mainly on phagocytes, called formyl peptide receptor 1, recognizes polypeptides with an N-terminal formylmethionine, which is a specific feature of bacterial proteins. Signaling by this receptor promotes the migration as well as the antimicrobial activities of the phagocytes.

Although our emphasis thus far has been on cellular receptors, the innate immune system also contains several circulating molecules that recognize and provide defense against microbes, as discussed later.

Epithelial Barriers

The major interfaces between the body and the external environment—the skin, gastrointestinal tract, respiratory tract, and genitourinary tract—are protected by layers of epithelial cells that provide physical and chemical barriers against infection ( Fig. 2.7 ). Microbes come into contact with vertebrate hosts mainly at these interfaces by external physical contact, ingestion, inhalation, and sexual activity. All these portals of entry are lined by continuous epithelia consisting of tightly adherent cells that form a mechanical barrier against microbes. Keratin on the surface of the skin and mucus secreted by mucosal epithelial cells prevent most microbes from interacting with and infecting or getting through the epithelia. Epithelial cells also produce antimicrobial peptides including defensins and cathelicidins, which kill bacteria and some viruses by disrupting their outer membranes. Thus, antimicrobial peptides provide a chemical barrier against infection. In addition, epithelia contain lymphocytes called intraepithelial T lymphocytes that belong to the T cell lineage but express antigen receptors of limited diversity. Some of these T cells express receptors composed of two chains, γ and δ, that are similar but not identical to the αβ T cell receptors expressed on the majority of T lymphocytes (see Chapters 4 and 5). Intraepithelial lymphocytes often recognize microbial lipids and other structures. Intraepithelial T lymphocytes presumably react against infectious agents that attempt to breach the epithelia, but the specificity and functions of these cells are poorly understood.

Functions of epithelia in innate immunity.

Epithelia present at the portals of entry of microbes provide physical barriers formed by keratin (in the skin) or secreted mucus (in the gastrointestinal, bronchopulmonary, and genitourinary systems) and by tight junctions between epithelial cells. Epithelia also produce antimicrobial substances (e.g., defensins) and harbor lymphocytes that kill microbes and infected cells.

Phagocytes: Neutrophils and Monocytes/Macrophages

The two types of circulating phagocytes, neutrophils and monocytes, are blood cells that are recruited to sites of infection, where they recognize and ingest microbes for intracellular killing ( Fig. 2.8 ).

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  Neutrophils , also called polymorphonuclear leukocytes (PMNs), are the most abundant leukocytes in the blood, numbering 4,000 to 10,000 per μL ( Fig. 2.9A ). In response to certain bacterial and fungal infections, the production of neutrophils from the bone marrow increases rapidly, and their numbers in the blood may rise up to 10 times the normal. The production of neutrophils is stimulated by cytokines, known as colony-stimulating factors (CSFs), which are secreted by many cell types in response to infections and act on hematopoietic cells to stimulate proliferation and maturation of neutrophil precursors. Neutrophils are the first and most numerous cell type to respond to most infections, particularly bacterial and fungal infections, and thus are the dominant cells of acute inflammation, as discussed later. Neutrophils ingest microbes in the circulation, and they rapidly enter extravascular tissues at sites of infection, where they also phagocytose (ingest) and destroy microbes. Neutrophils express receptors for products of complement activation and for antibodies that coat microbes. These receptors enhance phagocytosis of antibody- and complement-coated microbes and also transduce activating signals that enhance the ability of the neutrophils to kill ingested microbes. The process of phagocytosis and intracellular destruction of microbes is described later. Neutrophils are also recruited to sites of tissue damage in the absence of infection, where they initiate the clearance of cell debris. Neutrophils live for only several hours in tissues, so they are the early responders, but they do not provide prolonged defense.

  
  

  
  

  
  

  

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