TLR2 and TLR4 mediated host immune responses in major infectious diseases: a review

Mukherjee, Suprabhat; Karmakar, Subhajit; Babu, Santi Prasad Sinha

doi:10.1016/j.bjid.2015.10.011

Abstract

During the course of evolution, multicellular organisms have been orchestrated with an efficient and versatile immune system to counteract diverse group of pathogenic organisms. Pathogen recognition is considered as the most critical step behind eliciting adequate immune response during an infection. Hitherto Toll-like receptors (TLRs), especially the surface ones viz. TLR2 and TLR4 have gained immense importance due to their extreme ability of identifying distinct molecular patterns from invading pathogens. These pattern recognition receptors (PRRs) not only act as innate sensor but also shape and bridge innate and adaptive immune responses. In addition, they also play a pivotal role in regulating the balance between Th1 and Th2 type of response essential for the survivability of the host. In this work, major achievements rather findings made on the typical signalling and immunopathological attributes of TLR2 and TLR4 mediated host response against the major infectious diseases have been reviewed. Infectious diseases like tuberculosis, trypanosomiasis, malaria, and filariasis are still posing myriad threat to mankind. Furthermore, increasing resistance of the causative organisms against available therapeutics is also an emerging problem. Thus, stimulation of host immune response with TLR2 and TLR4 agonist can be the option of choice to treat such diseases in future.

Keywords
Toll like receptor (TLR); Trypanosomiasis; Malaria; Filariasis

Introduction

Antimicrobial inflammatory response primarily onsets through initial sensing of distinct pathogen associated molecular patterns (PAMPs) by pattern recognition receptors (PRRs) of hosts. These receptors serve as crucial innate PRRs that sense microbial or endogenous products released from damaged or dying cells and trigger innate immunity through the activation of intracellular signal transduction pathways.¹1 Kawai T, Akira S. Toll-like receptors and their crosstalk with other innate receptors in infection and immunity. Immunity. 2011; 34:637-50 Amongst the innate immune PRRs, Toll-like receptors (TLRs) have the unique capacity to sense the initial infection and are the most potent inducers of the inflammatory responses.¹1 Kawai T, Akira S. Toll-like receptors and their crosstalk with other innate receptors in infection and immunity. Immunity. 2011; 34:637-50 Depending on their cellular localization or respective PAMPs they identify, TLRs can be divided into two sub groups such as transmembrane (TLR1, TLR2, TLR4, TLR5, TLR6, and TLR11) and intracellular (TLR3, TLR7, TLR8, and TLR9).¹1 Kawai T, Akira S. Toll-like receptors and their crosstalk with other innate receptors in infection and immunity. Immunity. 2011; 34:637-50 These evolutionary conserved type-I transmembrane proteins (TLRs) can recognize ligand from almost all types of pathogenic organisms including viruses, bacteria, fungi, protozoa, helminths, etc. Structurally, TLRs located on cell membranes possesses an extracellular domain containing leucine-rich repeats that recognize distinct PAMPs and a toll-interleukin 1 (IL-1) receptor (TIR) domain required for downstream signalling that guides activation of transcription factor nuclear factor-κB (NF-κB) for inducing pro-inflammatory cytokines and chemokines as well as the up-regulation of co-stimulatory molecules on antigen presenting cells, such as macrophages (MΦs) and dendritic cells (DCs) that in turn sensitize T-cell activation. Inflammation signalled from TLR is a protective measure of the host body to ensure removal of detrimental threats posed by infectious agents as well as to accelerate the healing process. However, the Th1 biased inflammatory consequences orchestrated by TLRs not only involve in eliminating pathogenic infections but also can induce fatal pathological outcomes like septic shock (Fig. 1). Similarly, pathogen modulated TLR signalling develops a Th2 based response beneficial for the pathogen i.e. disease progression (Fig. 1). Thus, an adequate balance between pro- and anti-inflammatory immune responses is of immense importance to restore the normal physiological conditions of the host body during and after a pathogenic infection.²2 Zeytun A, Chaudhary A, Pardington P, Cary R, Gupta G. Induction of cytokines and chemokines by Toll-like receptor signaling strategies for control of inflammation. Crit Rev Immunol. 2010; 30:53-67 Herein, major research findings exploring the role of TLR2 and TLR4 in the induction of host immunity against major parasitic diseases such as tuberculosis, leishmaniasis, malaria, trypanosomiasis, and filariasis have been reviewed.

Fig. 1
Cytokine mediated proinflammatory (Th1) or anti-inflammatory (Th2) polarization of immune cells.

Immunobiology of TLR2 and 4

Since their discovery, TLR2 and 4 have gained much attention due to their extreme ability of identifying diversified array of pathogenic ligands.¹1 Kawai T, Akira S. Toll-like receptors and their crosstalk with other innate receptors in infection and immunity. Immunity. 2011; 34:637-50 Alike Drosophila protein ‘Toll’, mammalian TLR2/4 possesses a cytosolic IL-1 receptor homolog domain but heterologous extracellular leucine-rich repeats.³3 Botos I, Segal D.M, Davies D.R. The structural biology of Toll-like receptors. Structure. 2011; 19:447-59 Interestingly, the mode of signalling is highly similar for e.g. transcription factor ‘Dorsal’ activated by Toll pathway in Drosophila is a functional homologue of NF-κB.⁴4 Valanne S, Wang J.H, Ramet M. The Drosophila Toll signaling pathway. J Immunol. 2011; 186:649-56 The mode of activation of NF-κB or Dorsal also share high degree of similarity in terms of signalling intermediates like protein kinases such as ‘Pelle’ of Drosophila⁵5 Ganesan S, Aggarwal K, Paquette N, Silverman N. NF-kappaB/Rel proteins and the humoral immune responses of Drosophila melanogaster. Curr Top Microbiol Immunol. 2011; 349:25-60 ⁶6 Janeway Jr. C.A, Medzhitov R. Innate immune recognition. Annu Rev Immunol. 2002; 20:197-216 and mammalian IL-1 receptor-associated kinase.⁷7 Maeshima N, Fernandez R.C. Recognition of lipid A variants by the TLR4-MD-2 receptor complex. Front Cell Infect Microbiol. 2013; 3:3 A comparative homology in the signal pathway transduced by Drosophila ‘Toll’ and mammalian “TLR” have been depicted in Fig. 2.

Fig. 2
Signalling homology between the Toll-pathway of Drosophila (left) and mammalian TLR pathway (right) in response to extracellular ligand (s).

The functional features of “Toll signaling” are primarily different from insect to mammals. As obvious, ‘Toll’ receptors in insect (Drosophila) perform developmental roles primarily but it serves as innate immune receptor majorly in mammals. The proteins involved in the dorso-ventral polarity also play crucial role in the antimicrobial response in the fly as well.⁸8 Kimbrell D.A, Beutler B. The evolution and genetics of innate immunity. Nat Rev Genet. 2001; 2:256-67 Interestingly, intermediates of dorso-ventral polarity determining ‘Toll’ pathway of insect share high degree of homology with vertebrate TLRs (specifically TLR4) that performs pattern recognition.⁸8 Kimbrell D.A, Beutler B. The evolution and genetics of innate immunity. Nat Rev Genet. 2001; 2:256-67 Thus, the functional ancestry between development and immune pathway has been emerged as a major question. In particular, the discovery of immune function of ‘Toll’ in Drosophila also suggested towards the fact that the immune function of the Toll gene product was not adapted by the higher animals rather it can be revealed that the coordination and integration and/or cross talk between the intermediates of ‘Toll signaling’ has been improved with the increase in complexity among animals most likely during the course of evolution.⁸8 Kimbrell D.A, Beutler B. The evolution and genetics of innate immunity. Nat Rev Genet. 2001; 2:256-67 In addition, unrelenting selective pressure exerted by the rapidly evolving pathogenic organism also contributed in this adaptive evolution of ‘Toll’ receptor.⁸8 Kimbrell D.A, Beutler B. The evolution and genetics of innate immunity. Nat Rev Genet. 2001; 2:256-67 Particularly for TLR4, evolution of the gene (mostly due to mutation) led to differential expression of TLR4 with different affinity and specificity to its PAMP⁸8 Kimbrell D.A, Beutler B. The evolution and genetics of innate immunity. Nat Rev Genet. 2001; 2:256-67 which may be the reason behind resistance/susceptibility to an infectious disease. However, the exact molecular explanation of the mechanism involved in the introduction of immune functioning in the “Toll pathway” alongside its developmental function or its functional divergence still remains as a shaded area in our understanding.

Being among the cell surface TLRs, TLR2 and 4 shape pathogen specific innate immunity through distinct ligand binding which in turn develops antigen-specific acquired immunity as well. These two TLRs are the best characterized PRRs which not only identify invading pathogens outside the cell but also intracellular pathogens captured in endosomes or lysosomes.⁹9 Park B.S, Lee J.O. Recognition of lipopolysaccharide pattern by TLR4 complexes. Exp Mol Med. 2013; 45:e66 TLR2 and 4 can sense PAMPs from various infectious micro and macro organisms as summarized in Table 1. The best possible explanation of cell surface TLR activation is the presentation and binding of lipopolysaccharide (LPS) to TLR4. Under pathogenic condition, a soluble plasma protein namely LPS-binding protein (LBP) interacts and binds with LPS.⁹9 Park B.S, Lee J.O. Recognition of lipopolysaccharide pattern by TLR4 complexes. Exp Mol Med. 2013; 45:e66 The entire LPS-LBP complex handed over to glycosyl phosphatidyl inositol linked CD14 firstly and then on to the TLR4-MD2 complex.⁹9 Park B.S, Lee J.O. Recognition of lipopolysaccharide pattern by TLR4 complexes. Exp Mol Med. 2013; 45:e66 TLR4 forms a complex with MD2 on the cell surface which serves as the main LPS-binding component.¹1 Kawai T, Akira S. Toll-like receptors and their crosstalk with other innate receptors in infection and immunity. Immunity. 2011; 34:637-50 Five out of the six lipid chains of LPS occupy the hydrophobic pocket of MD2 and the remaining lipid chain exposed to the surface on MD2 associates with TLR4.¹1 Kawai T, Akira S. Toll-like receptors and their crosstalk with other innate receptors in infection and immunity. Immunity. 2011; 34:637-50 The phosphate groups on sugar moieties also interact with the positively charged residues of TLR4. The multimeric receptor composed of two copies of the TLR4-MD2-LPS complex resulting initiation of signal transduction by recruiting intracellular adaptor molecules such as Myeloid differentiation factor 88 (MyD88), TIR-related adaptor protein inducing interferon (TRIF), TRIF-related adaptor molecule (TRAM), TIR domain containing adaptor protein (TIRAP) or MyD88 adaptor like (MAL), and Sterile-alpha and Armadillo motif-containing protein (SARM). The summary of mode of ligand recognition by TLR4 has been depicted in Fig. 3.

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Table 1
Recognition of ligand and functional immunobiology of different TLRs against array of pathogens.

Fig. 3
Presentation of ligand (LPS) to TLR4 through the coordinated actions of serum LBP, membrane bound CD14 and MD2.

TLR2 forms an m-shaped heterodimers with either TLR1 or TLR6 for recognizing tri- or di-acylated lipopeptides respectively from the pathogens (Gram-negative bacteria, mycoplasma, etc.).³3 Botos I, Segal D.M, Davies D.R. The structural biology of Toll-like receptors. Structure. 2011; 19:447-59 Out of the three lipid chains of tri-acylated ligand (lipopeptide e.g. Pam3CSK4), two interact with TLR2 in the TLR2-TLR1 heterodimer whereas the third chain occupies the hydrophobic channel of TLR1.⁷7 Maeshima N, Fernandez R.C. Recognition of lipid A variants by the TLR4-MD-2 receptor complex. Front Cell Infect Microbiol. 2013; 3:3 An absence of hydrophobic channel in TLR6, TLR2-TLR6 heterodimer cannot recognize triacylated lipopeptides. Other than discrimination between lipoproteins, TLR2 has the ability to act together with co-receptor (CD36) by working with the heterodimer to mediate the sensing of some but not all TLR2 agonists which induces internalization.⁴²42 Oliveira-Nascimento L, Massari P, Wetzler L.M. The role of TLR2 in infection and immunity. Front Immunol. 2012; 3:79 Thus TLR2 is involved in the recognition of a wide range of PAMPs derived from bacteria, fungi, parasites and viruses also. TLR2, together with its co-receptors, TLR1 and TLR6, requires internalization to trigger NF-κB activation in response to Lipoteichoic acid (LTA) and Pam3CSK4 that provides a novel accepting mechanism on how TLRs coordinate ligand recognition and subsequent triggering of a specific signal.⁴³43 Brandt K.J, Fickentscher C, Kruithof E.K, de Moerloose P. TLR2 ligands induce NF-kappaB activation from endosomal compartments of human monocytes. PLoS ONE. 2013; 8:e80743 Despite the expression of TLR2 at the cell surface, the bacterial TLR2 ligands namely Pam3CSK4 and LTA can induce NF-κB-dependent signalling from endosomal compartments reported for human monocytes and for a NF-κB sensitive reporter cell line.⁴³43 Brandt K.J, Fickentscher C, Kruithof E.K, de Moerloose P. TLR2 ligands induce NF-kappaB activation from endosomal compartments of human monocytes. PLoS ONE. 2013; 8:e80743

TLR2 and 4 are expressed in various immune cells including neutrophils, monocytes/MΦs and DCs.⁴⁴44 O’Mahony D.S, Pham U, Iyer R, Hawn T.R, Liles W.C. Differential constitutive and cytokine-modulated expression of human Toll-like receptors in primary neutrophils, monocytes, and macrophages. Int J Med Sci. 2008; 5:1-8 Amongst these, neutrophils first migrate to the site of infection, sense the pathogen and elicit immune response. However, coordinated activation of adaptive response is mediated through binding of specific ligand to monocytes or DCs that are also mediated principally by TLR2 and 4.⁴⁵45 Blasius A.L, Beutler B. Intracellular toll-like receptors. Immunity. 2010; 32:305-15 Moreover, these TLRs are also expressed on classical adaptive immune cells viz. B and T lymphocytes.⁴⁶46 Muzio M, Bosisio D, Polentarutti N, et al. Differential expression and regulation of toll-like receptors (TLR) in human leukocytes selective expression of TLR3 in dendritic cells. J Immunol. 2000; 164:5998-6004

After recognizing PAMPs by the TLR2 and 4 in a particular cell type, cytosolic TIR domain and associated adaptors (MyD88, TRIF, and SARM) are activated that in turn drive activation of the transcription factors such as NF-κB and/or IRF3. Activation of these TLRs triggers two distinct signalling pathways viz. MyD88 dependent and MyD88 independent or TRIF dependent pathway. MyD88, TRIF, TRAM, MAL, and SARM are the five important adaptors of TLR activation. MyD88 is the first amongst the adaptors used by all TLRs except TLR3. Upon TLR activation, MyD88 recruits interleukin 1 receptor associated kinase 4 (IRAK-4) that phosphorylates IRAK1 which in turn activate TNF Receptor-Associated Factor 6 (TRAF6). Both proteins leave the receptor complex and interact with TGF-β-activated kinase 1 (TAK1) and two TAK1 binding proteins TAB1 and TAB2. TAK1 becomes phosphorylated and activates the I-κB kinase (IKK) complex comprising IKKα, IKKβ, and NEMO/IKKγ, and Mitogen-activated protein kinase (MAPK) leading to the activation of NF-κB and c-Jun N-terminal kinases (JNK) signalling pathways respectively for triggering the expression of cytokines (IL-6, IL-12, TNF-α).⁴⁷47 Oeckinghaus A, Hayden M.S, Ghosh S. Crosstalk in NF-kappaB signaling pathways. Nat Immunol. 2011; 12:695-708 I-κB is then phosphorylated allowing NF-κB translocation to the nucleus and induces expression of pro-inflammatory cytokines. TAK1 is also capable of phosphorylating MKK6 and 7 which leads to the activation of p38 and JNK. MAL or TIRAP is the second adaptor that transmits signal from TLR4 and TLR2 by facilitating movement of MyD88 to TLR4 and/or possibly to TLR2 for transcription factor activation like NF-κB, JNK and Extracellular regulated kinases 1(ERK-1).⁴⁸48 Kagan J.C, Medzhitov R. Phosphoinositide-mediated adaptor recruitment controls Toll-like receptor signaling. Cell. 2006; 125:943-55 TRIF is the third adaptor for TLR4 and TLR3 that activates Interferon regulatory factor 3 (IRF3) by activating the kinases TBK1 and the I-κB kinase €. Fourth adaptor is TRAM which is one of the interacting partners of TRIF. TRAM involves in transmitting TLR4 signalling and results in MyD88-independent interferon-β production.⁴⁹49 Babu S, Anuradha R, Kumar N.P, George P.J, Kumaraswami V, Nutman T.B. Filarial lymphatic pathology reflects augmented toll-like receptor-mediated, mitogen-activated protein kinase-mediated proinflammatory cytokine production. Infect Immun. 2011; 79:4600-8 The fifth adaptor is SARM which mainly interact with TRIF and negatively regulate NF-κB and IRF3 activation.⁵⁰50 Carpenter S, O’Neill L.A. How important are Toll-like receptors for antimicrobial responses. Cell Microbiol. 2007; 9:1891-901

Activation of IRF3 and NF-κB are the principal targets of TRIF-dependent pathway.⁵¹51 Iwanaszko M, Kimmel M. NF-kappaB and IRF pathways cross-regulation on target genes promoter level. BMC Genomics. 2015; 16:307 TRIF recruits TRAF6 and activates TAK1 for NF-κB activation through ubiquitination dependent mechanisms similar to those of the MyD88 dependent pathway.⁴⁵45 Blasius A.L, Beutler B. Intracellular toll-like receptors. Immunity. 2010; 32:305-15 TRIF forms a multiprotein signalling complex along with TRAF6, TNFR-associated death domain (TRADD), Pellino-1 and Receptor-interacting protein1 (RIP1) required for the activation of TAK1, which further activates NF-κB and MAPK.¹1 Kawai T, Akira S. Toll-like receptors and their crosstalk with other innate receptors in infection and immunity. Immunity. 2011; 34:637-50 In addition to NF-κB activation, the TRIF-dependent pathway also leads to IRF3 activation and interferon-β transcription.⁵²52 Tamassia N, Bazzoni F, Le Moigne V, et al. IFN-beta expression is directly activated in human neutrophils transfected with plasmid DNA and is further increased via TLR-4-mediated signaling. J Immunol. 2012; 189:1500-9 TRIF recruits another signalling complex involving the non-canonical IKKs, TBK1 and IKKi (IKK¿), which catalyze the phosphorylation of IRF3 and induce nuclear translocation to mediate transcription of target genes.⁵³53 Kawai T, Akira S. Regulation of innate immune signalling pathways by the tripartite motif (TRIM) family proteins. EMBO Mol Med. 2011; 3:513-27 TRAF3 is also incorporated into the MyD88 complex during signalling. Degradation of TRAF3 results in the translocation of the membrane proximal signalling complex to the cytoplasm leading to TAK1 activation that phosphorylates the IKK complex to mediate NF-κB activation.⁵⁴54 Kawasaki T, Kawai T. Toll-like receptor signaling pathways. Front Immunol. 2014; 5:461 The mechanism of signalling induced from TLR-ligand interface to mediate inflammatory response has been presented in Fig. 4.

Fig. 4
Signalling pathways and their crosstalk in response to specific ligand from pathogen.

Involvement of TLR2 and TLR4 in infectious diseases

Diseases caused by parasites/microbes are just not the burden for mankind; they are economically considered as biohazards. Major infectious diseases like tuberculosis (TB), malaria, leishmaniasis, trypanosomiasis, and filariasis are the deadliest for the extent of harm they result. In this section, current scenario of the diseases of our interests has been presented with up-to-date information.

Tuberculosis

Tuberculosis (TB) caused by the intracellular bacterium Mycobacterium tuberculosis, capable of surviving within host mononuclear cells, remains one of the world's deadliest communicable diseases. TB is a major public health problem causing 10 million new infected cases diagnosed each year whereas deaths of 2 million victims.⁵⁵55 Kleinnijenhuis J, Oosting M, Joosten L.A, Netea M.G, Van Crevel R. Innate immune recognition of Mycobacterium tuberculosis. Clin Dev Immunol. 2011; 2011:405310 In 2013, an estimated 9.0 million people developed TB and 1.5 million died from the disease worldwide (WHO, 2014). TLR2 and 4 significantly contribute in the typical immune response in TB and their interaction with Mycobacterium tuberculosis believed to be the principal event. The decision behind progression or elimination depends what type of microbacterial ligand binds to these receptors.⁵⁶56 Stenger S, Modlin R.L. Control of Mycobacterium tuberculosis through mammalian Toll-like receptors. Curr Opin Immunol. 2002; 14:452-7 In general, mycobacteria have adopted sophisticated evasion strategy to bypass MΦs through alternative activation whereas elimination of mycobacterial infection is predominantly occurring by classically activated MΦs.⁵⁷57 Rocha-Ramirez L.M, Estrada-Garcia I, Lopez-Marin L.M, et al. Mycobacterium tuberculosis lipids regulate cytokines, TLR-2/4 and MHC class II expression in human macrophages. Tuberculosis (Edinb). 2008; 88:212-20 Kusner⁵⁸58 Kusner D.J. Mechanisms of mycobacterial persistence in tuberculosis. Clin Immunol. 2005; 114:239-47 has reported a 19 kDa mycobacterial secretary lipoprotein that activates murine and human MΦs to secrete TNF-α and nitric oxide (NO) via interaction with TLR2, but not TLR4. Mycobacterial glycolipids like lipoarabinomannan (LAM), lipomannans (LM), phosphatidylinositol mannosides (PIM2, PIM6), and a 19-kDa lipoprotein, are the mycobacterial PAMPs believed to cause MΦ activation via the TLR2 activating innate pathway by regulating tumour necrosis factor (TNF-α) and IL-10 secretion reported for human monocyte-derived MΦs.⁵⁷57 Rocha-Ramirez L.M, Estrada-Garcia I, Lopez-Marin L.M, et al. Mycobacterium tuberculosis lipids regulate cytokines, TLR-2/4 and MHC class II expression in human macrophages. Tuberculosis (Edinb). 2008; 88:212-20 The interaction of MΦs with M. tuberculosis through TLRs is critical in defining the cytokine profile that may or may not control disease progression. This interaction promotes the synthesis of antibacterial molecules (e.g., NO) and several cytokines, including TNF-α, interleukin-6 (IL-6), IL-1β, and IL-12.⁵⁷57 Rocha-Ramirez L.M, Estrada-Garcia I, Lopez-Marin L.M, et al. Mycobacterium tuberculosis lipids regulate cytokines, TLR-2/4 and MHC class II expression in human macrophages. Tuberculosis (Edinb). 2008; 88:212-20 In DCs, the engagement of TLR2 with these PAMPs induces the secretion of anti-inflammatory cytokines such as IL-10, a cytokine that promotes disease progression, by mechanisms that limit the inflammatory response.⁵⁷57 Rocha-Ramirez L.M, Estrada-Garcia I, Lopez-Marin L.M, et al. Mycobacterium tuberculosis lipids regulate cytokines, TLR-2/4 and MHC class II expression in human macrophages. Tuberculosis (Edinb). 2008; 88:212-20 Along with cytokine expression TLR2 activation leads to NO dependent and independent killing of intracellular M. tuberculosis in mouse and human MΦs respectively.⁵⁹59 Herbst S, Schaible U.E, Schneider B.E. Interferon gamma activated macrophages kill mycobacteria by nitric oxide induced apoptosis. PLoS ONE. 2011; 6:e19105 Apoptosis by infected host cells is also mediated by TLR2 mediated pathway involving MyD88, Fas-Associated protein with Death Domain (FADD) and caspase-8 in which MyD88 associates with FADD via their respective death domains.⁶⁰60 Aliprantis A.O, Yang R.B, Weiss D.S, Godowski P, Zychlinsky A. The apoptotic signaling pathway activated by Toll-like receptor-2. EMBO J. 2000; 19:3325-36 A scheme on TB induced TLR activation has been shown in Fig. 5.

Fig. 5
Recognition of ligand and onset of inflammatory response against bacteria, protozoan and nematode parasites.

Malaria

Malaria is a mosquito borne infectious disease of humans and other animals caused by parasitic protozoan of genus Plasmodium (WHO, 2014) causing huge number of death each year.⁶¹61 Caraballo H, King K. Emergency department management of mosquito-borne illness: malaria, dengue, and West Nile virus. Emerg Med Pract. 2014; 16:1-23 The host response during malaria infection, expresses high levels of many proinflammatory cytokines, including TNF-α, IL-1, IL-6, IL-12 and IFN-γ that have important roles in controlling parasite growth.⁶²62 Punsawad C. Effect of malaria components on blood mononuclear cells involved in immune response. Asian Pac J Trop Biomed. 2013; 3:751-6 Such types of responses are primarily originated from interaction of malarial surface molecules and TLRs of host immune cells. Till date, search for TLR activating PAMPs from malarial parasites have been the major highlighted objective for last few decades. In this connection, a glycolipid moiety, glycosyl phosphatidyl inositol (GPI) from P. falciparum has been reported to be a ligand of both TLR2 (heterodimeric form with TLR1 and TLR6) and TLR4.⁶³63 Gun S.Y, Claser C, Tan K.S, Renia L. Interferons and interferon regulatory factors in malaria. Mediators Inflamm. 2014; 2014:243713 Malarial GPI is structurally dissimilar than human and comprises a conserved ethanolamine phosphate-substituted oligosaccharide moiety, EtN-P-6Mana1-2Mana1-6Mana1-4GlcN, linked to phosphatidylinositol by a (1-6)-glycosidic bond.²⁹29 Gowda D.C. TLR-mediated cell signaling by malaria GPIs. Trends Parasitol. 2007; 23:596-604 The covalently linked fatty-acyl moieties of GPIs display a specific pattern for recognition by TLR2 and the co-receptors. This malarial ligand from infected erythrocytes interact with the mentioned TLRs located on MΦs or DCs and contribute to the immunopathology of the infection by inducing the expression of proinflammatory cytokines, such as TNF-α, IL-6 and IL-1. In addition, GPI anchored proteins, merozoite surface protein 1 (MSP1) and MSP2, two major asexual blood stage surface antigens, have endotoxin activity that indeed results in decreasing frequency of the parasitic load from host.⁶³63 Gun S.Y, Claser C, Tan K.S, Renia L. Interferons and interferon regulatory factors in malaria. Mediators Inflamm. 2014; 2014:243713 Moreover, such immunostimulatory host response by these surface proteins are induced through their binding to TLR4 and activation of immune signalling leading to release of cytokines from MΦs or DCs. P. falciparum GPI-induced MΦ activation is typically CD36 dependent transmits through MAPK, namely extracellular signal regulated kinase (ERK), p38 and c-Jun N-terminal kinase (JNK) pathways as well as through the Nuclear factor- kappa B (NF-κB).²⁹29 Gowda D.C. TLR-mediated cell signaling by malaria GPIs. Trends Parasitol. 2007; 23:596-604 In addition, studies using inhibitors of p38 activity and ERK1/2 activation indicated towards significant crosstalk among the GPI activated MAPK pathways represents redundant and overlapping functions in the initiation and regulation of innate immune responses.²⁹29 Gowda D.C. TLR-mediated cell signaling by malaria GPIs. Trends Parasitol. 2007; 23:596-604 Activation of TLR4/MyD88 dependent signalling pathway during the malarial infection results in the excessive proinflammatory cytokine production responsible for the several symptoms of the diseases.²⁹29 Gowda D.C. TLR-mediated cell signaling by malaria GPIs. Trends Parasitol. 2007; 23:596-604 This adaptor protein plays a more prominent role in pathogenesis, rather than in protection. A scheme on malaria induced TLR activation has been shown in Fig. 5.

In particular, reactive oxygen and nitrogen radicals produced by the malaria sensitized MΦs guides immune system by TNF-α, IL-12, and IFN-γ to kill these parasites through the induction of apoptosis.²⁹29 Gowda D.C. TLR-mediated cell signaling by malaria GPIs. Trends Parasitol. 2007; 23:596-604 These proinflammatory cytokines facilitate parasite-specific adaptive immunity for efficient parasite clearance to sustained and effective protection against disease pathology. However, overwhelmed proinflammatory response often results in fatal outcomes.²⁹29 Gowda D.C. TLR-mediated cell signaling by malaria GPIs. Trends Parasitol. 2007; 23:596-604 On other side, cell-mediated adaptive immune responses and the modulation of humoral responses by the induction of antibody isotype switching occur mainly by the involvement of IL-12.²⁹29 Gowda D.C. TLR-mediated cell signaling by malaria GPIs. Trends Parasitol. 2007; 23:596-604 Generally, a gradual down-regulation of proinflammatory cytokine production occurs with a parallel increase in the expression of anti-inflammatory cytokines (IL-10) when the parasite burden starts declining during malaria infection.²⁹29 Gowda D.C. TLR-mediated cell signaling by malaria GPIs. Trends Parasitol. 2007; 23:596-604 However this balance is required for fighting against the infection while escaping pathogenesis might not always be reached, contributing to medical situations.

Leishmaniasis

Leishmaniasis is caused by a protozoa parasite and transmitted to humans by the bite of infected female phlebotomus sandflies. This disease is the second-largest parasitic killer in the world (after malaria), responsible for an estimated 200,000–400,000 infections each year worldwide (WHO, 2015). The anti-leishmanial host response typically depends on the quality of the adaptive immune response primarily induced from host-parasite interaction. Especially, interaction between leishmanial parasite and innate immune receptors rather TLRs results generation of inflammatory mediators to deprive parasite burden and develops efficient adaptive responses. Lipophosphoglycan (LPG), the major identified ligand from these parasites, has been reported to induce inflammation through TLR2 and 4.⁶⁴64 Silvestre R, Silva A.M, Cordeiro-da-Silva A, Ouaissi A. The contribution of Toll-like receptor 2 to the innate recognition of a Leishmania infantum silent information regulator 2 protein. Immunology. 2009; 128:484-99 ⁶⁵65 Faria M.S, Reis F.C, Lima A.P. Toll-like receptors in leishmania infections guardians or promoters?. J Parasitol Res. 2012; 2012:930257 LPG occurs both in the parasite surface as well as in the secretory form and these two forms are structurally similar but differ in the average number of phosphorylated oligosaccharide repeat units present and in the sugar types present in the glycan. Up-regulation and activation of TLR2 on human Natural killer (NK) cells by LPG of L. major results enhancement of TNF-α and IFN-γ. However, interaction of LPGs with the TLRs is also influenced by the structural diversity of the phosphoglycan. Likewise, LPG of L. major, L. mexicana, L. aethiopica, and L. tropica were reported as classical TLR2 ligand of MΦs whereas performance of L. tropica LPG is not so much satisfactory.⁶⁵65 Faria M.S, Reis F.C, Lima A.P. Toll-like receptors in leishmania infections guardians or promoters?. J Parasitol Res. 2012; 2012:930257 Study on the induction of TNF-α in MΦ by L. major LPG showed need of a lipid anchor and a functional MyD88 adaptor.⁶⁵65 Faria M.S, Reis F.C, Lima A.P. Toll-like receptors in leishmania infections guardians or promoters?. J Parasitol Res. 2012; 2012:930257 Such MyD88-dependent pathways are particularly important in developing protective IL-12-mediated Th1 response against the parasite.⁶⁵65 Faria M.S, Reis F.C, Lima A.P. Toll-like receptors in leishmania infections guardians or promoters?. J Parasitol Res. 2012; 2012:930257 The L. infantum protein related to the silent information regulator 2 (SIR2) family has been reported for stimulating the proliferation of activated B lymphocytes, overexpression of major histocompatibility complex- (MHC) II and the co-stimulatory molecules CD40 and CD86 as well as maturation of DCs accompanied by the secretion of IL-12 and TNF-α are principally governed through TLR2.⁶⁴64 Silvestre R, Silva A.M, Cordeiro-da-Silva A, Ouaissi A. The contribution of Toll-like receptor 2 to the innate recognition of a Leishmania infantum silent information regulator 2 protein. Immunology. 2009; 128:484-99 In spite of its proinflammatory activity, LPG has been shown to inhibit the progression of inflammatory signalling originated from TLR2/TLR4 by inducing the expression of suppressors of the cytokine signalling (SOCS) family proteins viz. SOCS-1 and SOCS-3.⁶⁵65 Faria M.S, Reis F.C, Lima A.P. Toll-like receptors in leishmania infections guardians or promoters?. J Parasitol Res. 2012; 2012:930257 ⁶⁶66 de Veer M.J, Curtis J.M, Baldwin T.M, et al. MyD88 is essential for clearance of Leishmania major possible role for lipophosphoglycan and Toll-like receptor 2 signaling. Eur J Immunol. 2003; 33:2822-31 Another exciting fact about LPG is that production of ROS is induced through the interaction between membrane LPG and immune cell TLR-2 leading to the differentiation of Th2 subsets whereas Th1-promoting cytokines are reported to be induced solely by soluble LPG.⁶⁵65 Faria M.S, Reis F.C, Lima A.P. Toll-like receptors in leishmania infections guardians or promoters?. J Parasitol Res. 2012; 2012:930257 LPG potentiated inflammatory responses through TLR2 stimulation and IL-12 expression followed by Th1 responses in mice was also reported after treating with synthetic oligosaccharide analogues of LPG glycan structure indicating the importance of glycan in the immunostimulatory activity of LPG.⁶⁵65 Faria M.S, Reis F.C, Lima A.P. Toll-like receptors in leishmania infections guardians or promoters?. J Parasitol Res. 2012; 2012:930257 Interestingly, parasites also use the same ligand as well as the TLRs to supress the immune cell activation required for parasites’ benefit i.e. disease progression. Faria et al.⁶⁵65 Faria M.S, Reis F.C, Lima A.P. Toll-like receptors in leishmania infections guardians or promoters?. J Parasitol Res. 2012; 2012:930257 reported L. donovani infected human THP1-derived MΦs showed suppression in the TLR2 stimulated IL-12 release with increased production of IL-10 resulted from the inhibition of MAPKp38 phosphorylation and activating ERK1/2 phosphorylation. In addition, L. donovani, L. mexicana, and L. major have been reported to exploit the MΦ tyrosine phosphatase SHP-1 to inactivate kinases (e.g. IRAK) involved in TLR signalling.³²32 Abu-Dayyeh I, Shio M.T, Sato S, Akira S, Cousineau B, Olivier M. Leishmania-induced IRAK-1 inactivation is mediated by SHP-1 interacting with an evolutionarily conserved KTIM motif. PLoS Negl Trop Dis. 2008; 2:e305 A graphical summary on leishmanial parasite induced TLR activation is shown in Fig. 5.

Proteoglycolipid complex (P8) composed of acysteine and serine metalloprotease, host-derived Apolipoprotein E (ApoE), and four glycolipids has been reported as another potential TLR4 ligand of Leishmania detected in L. pifanoi amastigotes that influence phagocytosis through TLR activation.⁶⁵65 Faria M.S, Reis F.C, Lima A.P. Toll-like receptors in leishmania infections guardians or promoters?. J Parasitol Res. 2012; 2012:930257 Activated TLR4 at the parasitophorous vacuole affects the microenvironment surrounding the parasite for its control. Particularly for the neutrophils, TLR4 induces IRAK4 for exocytosis of neutrophil secretory granules.⁶⁵65 Faria M.S, Reis F.C, Lima A.P. Toll-like receptors in leishmania infections guardians or promoters?. J Parasitol Res. 2012; 2012:930257 Mechanistically, P8 sensitized MΦs induce proinflammatory cytokines viz. IL-1β and TNF-α through TLR4, MD2, CD14, and MyD88.⁶⁵65 Faria M.S, Reis F.C, Lima A.P. Toll-like receptors in leishmania infections guardians or promoters?. J Parasitol Res. 2012; 2012:930257 In addition, metacyclic promastigotes have been reported to induce phosphorylation of the MAP kinases such as ERK, p38, and JNK through TLR4 in L. mexicana.⁶⁷67 Shweash M, Adrienne McGachy H, Schroeder J, et al. Leishmania mexicana promastigotes inhibit macrophage IL-12 production via TLR-4 dependent COX-2, iNOS and arginase-1 expression. Mol Immunol. 2011; 48:1800-8 During such course of inflammation of MΦ, iNOS, Cyclooxygenase-2 (COX-2), Prostaglandin E2 (PGE2), NO and arginase-1 are been the mediators.⁶⁷67 Shweash M, Adrienne McGachy H, Schroeder J, et al. Leishmania mexicana promastigotes inhibit macrophage IL-12 production via TLR-4 dependent COX-2, iNOS and arginase-1 expression. Mol Immunol. 2011; 48:1800-8

Trypanosomiasis (Chagas disease)

Chagas disease or American trypanosomiasis, is a tropical parasitic disease caused by the protozoan Trypanosoma cruzi (CDC, 2015) and transmitted by insects vector like Triatominae or kissing bugs. In Latin America it causes a health threat for an estimated 10 million people and more than 25 million people are at risk. Typical immunity against Chagas disease is principally mediated by innate recognition through TLRs. Although studied less, TLRs have been characterized as crucial determinants in evoking anti- T. cruzi immune response in which both TLR2 and TLR4 are the key mediators.⁶⁸68 Rodrigues M.M, Oliveira A.C, Bellio M. The immune response to Trypanosoma cruzi role of Toll-like receptors and perspectives for vaccine development. J Parasitol Res. 2012; 2012:507874 In particular, these receptors mediate internalization of trypanosomatid through phagocytosis required for initiating the immune response by phagosomal maturation to kill the parasite followed by antigen presentation.⁶⁹69 Ramasawmy R, Cunha-Neto E, Fae K.C, et al. Heterozygosity for the S180L variant of MAL/TIRAP, a gene expressing an adaptor protein in the Toll-like receptor pathway, is associated with lower risk of developing chronic Chagas cardiomyopathy. J Infect Dis. 2009; 199:1838-45 Researchers have demonstrated fusion of early endosomes, and phagocytosis induced by trypomastigotes in MΦs by ligation of guanine phosphonucleotide- binding proteins Ras-related protein- (Rab-) 5 solely through TLR2.⁶⁹69 Ramasawmy R, Cunha-Neto E, Fae K.C, et al. Heterozygosity for the S180L variant of MAL/TIRAP, a gene expressing an adaptor protein in the Toll-like receptor pathway, is associated with lower risk of developing chronic Chagas cardiomyopathy. J Infect Dis. 2009; 199:1838-45 TLR2 activation has been reported to proceed via MyD88-dependent pathway.⁶⁹69 Ramasawmy R, Cunha-Neto E, Fae K.C, et al. Heterozygosity for the S180L variant of MAL/TIRAP, a gene expressing an adaptor protein in the Toll-like receptor pathway, is associated with lower risk of developing chronic Chagas cardiomyopathy. J Infect Dis. 2009; 199:1838-45 Secretion of chemokines signalled from TLR2 activation further recruit leukocytes to control the infection in a broad way.²⁸28 Coelho P.S, Klein A, Talvani A, et al. Glycosylphosphatidylinositol-anchored mucin-like glycoproteins isolated from Trypanosoma cruzi trypomastigotes induce in vivo leukocyte recruitment dependent on MCP-1 production by IFN-gamma-primed-macrophages. J Leukoc Biol. 2002; 71:837-44 In particular, TLR2 signalling is targeted by the trypanosomatids to hinder the immune response induced by the parasite.

However, TLR activation resulted from immune cells-T. cruzi interaction may also contribute to the disease pathology as well.⁶⁹69 Ramasawmy R, Cunha-Neto E, Fae K.C, et al. Heterozygosity for the S180L variant of MAL/TIRAP, a gene expressing an adaptor protein in the Toll-like receptor pathway, is associated with lower risk of developing chronic Chagas cardiomyopathy. J Infect Dis. 2009; 199:1838-45 Involvement of TLR activation in the immunopathology of chronic Chagas’ cardiopathy has been reported to be due to a single-nucleotide polymorphism in the genes coding for the signalling proteins of TLR signalling and leads to differential susceptibility to Chagas disease.⁶⁹69 Ramasawmy R, Cunha-Neto E, Fae K.C, et al. Heterozygosity for the S180L variant of MAL/TIRAP, a gene expressing an adaptor protein in the Toll-like receptor pathway, is associated with lower risk of developing chronic Chagas cardiomyopathy. J Infect Dis. 2009; 199:1838-45 For example, T. cruzi-infected individuals have heterozygous MAL/TIRAP S180L variant shows poorer signal transduction after binding of the trypanosomal ligand to TLR2 or TLR4 resulting in lesser chance of developing chronic Chagas’ cardiomyopathy.⁶⁹69 Ramasawmy R, Cunha-Neto E, Fae K.C, et al. Heterozygosity for the S180L variant of MAL/TIRAP, a gene expressing an adaptor protein in the Toll-like receptor pathway, is associated with lower risk of developing chronic Chagas cardiomyopathy. J Infect Dis. 2009; 199:1838-45 A summary on trypanosomatid induced TLR activation has been shown in Fig. 5.

Filariasis

Lymphatic filariasis, a vector borne neglected tropical disease, mainly caused by three species of nematode parasites- Wuchereria bancrofti, Brugia malayi, and B. timori is considered to be a major public health burden (WHO, 2015). Pathological manifestations of this disease mainly include lymphedema, elephantiasis and rarely a greater degree of neurological manifestation.⁷⁰70 Mukherjee S, Sinha Babu S.P. Neurofilariasis. Neurology in tropics. Asia Pacific: Elsevier; 2015. Recent studies also showed existence of co-infection of filarial parasite with bacteria (TB),⁴⁹49 Babu S, Anuradha R, Kumar N.P, George P.J, Kumaraswami V, Nutman T.B. Filarial lymphatic pathology reflects augmented toll-like receptor-mediated, mitogen-activated protein kinase-mediated proinflammatory cytokine production. Infect Immun. 2011; 79:4600-8 malaria ⁴⁹49 Babu S, Anuradha R, Kumar N.P, George P.J, Kumaraswami V, Nutman T.B. Filarial lymphatic pathology reflects augmented toll-like receptor-mediated, mitogen-activated protein kinase-mediated proinflammatory cytokine production. Infect Immun. 2011; 79:4600-8 ⁷¹71 Hoerauf A, Satoguina J, Saeftel M, Specht S. Immunomodulation by filarial nematodes. Parasite Immunol. 2005; 27:417-29 and opportunistic yeast.⁷²72 Mukherjee S, Mukherjee N, Saini P, Gayen P, Roy P, Sinha Babu S.P. Molecular evidence on the occurrence of co-infection with Pichia guilliermondii and Wuchereria bancrofti in two filarial endemic districts of India. Infect Dis Poverty. 2014; 3:13 In general, the immunoresponse in filariasis is complicated and unresolved especially the involvement and functional role played by TLR2 and TLR4.⁴⁹49 Babu S, Anuradha R, Kumar N.P, George P.J, Kumaraswami V, Nutman T.B. Filarial lymphatic pathology reflects augmented toll-like receptor-mediated, mitogen-activated protein kinase-mediated proinflammatory cytokine production. Infect Immun. 2011; 79:4600-8 Filarial intracellular symbiotic bacterium, Wolbachia has been reported to cause inflammation through its lipopolysaccharide (of outer membrane) after binding with TLR4. TLR2 and TLR4 are also capable to bind other Wolbachial products like Wolbachia surface protein (WSP) and induce inflammatory response by secreting pro-inflammatory cytokines from MΦs and DCs.¹³13 Brattig N.W, Bazzocchi C, Kirschning C.J, et al. The major surface protein of Wolbachia endosymbionts in filarial nematodes elicits immune responses through TLR2 and TLR4. J Immunol. 2004; 173:437-45 Such proinflammatory responses are of immense importance to eliminate the infection from host. However, filarial nematodes also target TLR2 and TLR4, especially TLR4, for modulating host immune response. A phosphorylcholine- conjugated glycoprotein molecule namely ES-62 binds TLR4 and create anti-inflammatory/Th2 biased immune response to prolong survivability of the parasite inside host.³⁶36 Goodridge H.S, Marshall F.A, Else K.J, et al. Immunomodulation via novel use of TLR4 by the filarial nematode phosphorylcholine-containing secreted product, ES-62. J Immunol. 2005; 174:284-93 In chronic infection, filarial nematode induces apoptotic death of T cells for down regulating host response and interestingly the process is also operative through TLR4.⁷³73 Babu S, Nutman T.B. Immunopathogenesis of lymphatic filarial disease. Semin Immunopathol. 2012; 34:847-61 Live microfilarae of B. malayi have been reported to modulate TLR4 expression in monocyte derived human DCs (mhDCs) to induce an immunosuppressive environment in host through interference of MyD88-dependent suppression of NF-κB signalling to hinder production of proinflammatory cytokines and type-1 interferons. In addition to such inhibitory effect of microfilarae over DCs, these also results partial inhibition of the function of human Langerhans cells (LCs) and prevent proliferation of CD4+ T cells.⁷⁴74 Venugopal P.G, Nutman T.B, Semnani R.T. Activation and regulation of toll-like receptors (TLRs) by helminth parasites. Immunol Res. 2009; 43:252-63 Interestingly, TLR2 and TLR4 have been reported to be expressed on circulating B cells during helminthic infection that uphold and maintain Th2 type-immune responses to make “worm favourable” conditions.⁷⁵75 Ludwig-Portugall I, Layland L.E. TLRs, Treg, and B Cells, an Interplay of Regulation during Helminth Infection. Front Immunol. 2012; 3:8 These specialized B cell subsets are known as regulatory B cells (Breg) and their immunosuppressive function is also regulated through TLR4.⁷⁵75 Ludwig-Portugall I, Layland L.E. TLRs, Treg, and B Cells, an Interplay of Regulation during Helminth Infection. Front Immunol. 2012; 3:8 TLR4 on these cells trigger induction of IL-10 secretion from B cell through Myd88-dependent pathway.⁷⁶76 Yanaba K, Bouaziz J.D, Matsushita T, Tsubata T, Tedder T.F. The development and function of regulatory B cells expressing IL-10 (B10 cells) requires antigen receptor diversity and TLR signals. J Immunol. 2009; 182:7459-72 Particularly in filariasis, Breg cells are responsible for the induction as well as maintenance of hypo-responsive immune status with elevated levels of Treg, IL-10 and filarial-specific IgG4.⁷⁵75 Ludwig-Portugall I, Layland L.E. TLRs, Treg, and B Cells, an Interplay of Regulation during Helminth Infection. Front Immunol. 2012; 3:8 This Breg mediated responses is recompensing as patients remain asymptomatic due to devoid of excessive immunopathology.⁷⁵75 Ludwig-Portugall I, Layland L.E. TLRs, Treg, and B Cells, an Interplay of Regulation during Helminth Infection. Front Immunol. 2012; 3:8 However, this typical Th2 environment by Breg results secondary infections by bacteria and/or fungi due to lack of protective immune cells repertoires in filarial subjects.⁷⁵75 Ludwig-Portugall I, Layland L.E. TLRs, Treg, and B Cells, an Interplay of Regulation during Helminth Infection. Front Immunol. 2012; 3:8 A probable mechanism of TLR activation by filarial parasites has been shown in Fig. 5.

Conclusion and future prospects

Studies on the recognition of infectious pathogens through TLRs have significantly contributed to our understanding of the underlying mechanisms of innate immune defense against the deadliest parasites. In this review, we have put forward the findings made on the role played by two crucial members of the TLR family viz. TLR2 and TLR4 against the most threatening infectious diseases. We have discussed different previously reported findings on types of pathogenic ligand alongside the mechanism of action of inflammatory cascade originated from TLR4 and TLR2 in tuberculosis, malaria, leishmaniasis, filariasis, and trypanosomiasis. Interesting outcomes achieved in the experimental vaccine adjuvants and/or immunotherapy against active leishmaniasis promises for effective future applications as well as opens new possibilities regarding the use of TLR based immunotherapeutic control strategies for malaria or other diseases. Similarly, immunomodulatory TLR4 ligand from filarial parasites has also shown to control allergic reaction by inhibiting proinflammatory mediators and this strategy could be used effectively to combat inflammatory pathology of malaria or other disease to reduce mortality. Similarly, TLR4 has been emerged as a target of therapeutics for immunopharmacological control of infectious and/or inflammatory diseases.⁷⁷77 Mukherjee N, Mukherjee S, Saini P, Roy P, Sinha Babu S.P. Phenolics and terpenoids the promising new search for anthelmintics: a critical review. Mini Rev Med Chem. 2015;

However, many questions remain to be answered for this aspect. Thus more concluding information rather inferences are need to be gathered through population based studies. Similarly, there is a need to search for other microbial ligands for a same microbe/parasite as well as interplay between the TLRs and obviously the signalling crosstalk. From immunological perspectives, study of mechanism of parasite/microbe induced polarization of major antigen presenting cells may offer us new target for developing therapeutic strategy to restore Th1 (to eliminate infection) or Th2 biased (to protect host from overt inflammation) immune response.

Conflicts of interest

The authors declare no conflicts of interest.

Acknowledgement

SM acknowledges University Grants Commission for the award of his Senior Research Fellowship.

1
These authors contributed equally to this work.

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Publication Dates

Publication in this collection
Mar-Apr 2016

History

Received
31 Aug 2015
Accepted
16 Oct 2015

This is an open-access article distributed under the terms of the Creative Commons Attribution License, which permits unrestricted use, distribution, and reproduction in any medium, provided the original work is properly cited.

[1] 1
These authors contributed equally to this work.

Organism	Ligand(s)	Targeted receptor	Localization of ligands	Effector function
Bacteria
Gram-negative bacteria	Lipopolysaccharide (LPS)	TLR4	Outer membrane	Induces proinflammatory response¹⁰10 Aderem A, Ulevitch R.J. Toll-like receptors in the induction of the innate immune response. Nature. 2000; 406:782-7
Gram-positive bacteria	Peptidoglycans	TLR2	Cell wall	Enhances inflammatory response¹⁰10 Aderem A, Ulevitch R.J. Toll-like receptors in the induction of the innate immune response. Nature. 2000; 406:782-7
Streptococcus B	Lipoteichoic acid	TLR2	Protoplast membranes	Initiates inflammatory response¹⁰10 Aderem A, Ulevitch R.J. Toll-like receptors in the induction of the innate immune response. Nature. 2000; 406:782-7
Staphylococcus aureus	Phenol soluble modulin(PMS)	TLR2	Extracellular	Inhibit proinflammatory cytokines TNF, IL-12 and IL-6¹¹11 Schreiner J, Kretschmer D, Klenk J, et al. Staphylococcus aureus phenol-soluble modulin peptides modulate dendritic cell functions and increase in vitro priming of regulatory T cells. J Immunol. 2013; 190:3417-26
Trepanema maltophilum	Glycolipids	TLR2	Outer membrane surface	Including the pro-inflammatory cytokines interleukin (IL)-1, IL-6, and tumour necrosis factor (TNF)-α¹²12 Opitz B, Schroder N.W, Spreitzer I, et al. Toll-like receptor-2 mediates Treponema glycolipid and lipoteichoic acid-induced NF-kappaB translocation. J Biol Chem. 2001; 276:22041-7
Wolbachia	Wolbachia surface protein (WSP)	TLR2	Membrane surface	Induces TNF-α, IL-12, and IL-8¹³13 Brattig N.W, Bazzocchi C, Kirschning C.J, et al. The major surface protein of Wolbachia endosymbionts in filarial nematodes elicits immune responses through TLR2 and TLR4. J Immunol. 2004; 173:437-45
Wolbachia	Wolbachial liporotein	TLR2	Bacterial membranes	Induces TNF-α production and up-regulates surface markers of human lymphatic endothelium¹³13 Brattig N.W, Bazzocchi C, Kirschning C.J, et al. The major surface protein of Wolbachia endosymbionts in filarial nematodes elicits immune responses through TLR2 and TLR4. J Immunol. 2004; 173:437-45
Borrelia burgdorferi	Outer surface protein A lipoprotein (OspAL)	TLR2	Outer membrane surface	Induces the inflammatory response & down-regulate the cell response to flagellin¹⁴14 Bulut Y, Faure E, Thomas L, Equils O, Arditi M. Cooperation of Toll-like receptor 2 and 6 for cellular activation by soluble tuberculosis factor and Borrelia burgdorferi outer surface protein A lipoprotein role of Toll-interacting protein and IL-1 receptor signaling molecules in Toll-like receptor 2 signaling. J Immunol. 2001; 167:987-94 ¹⁵15 Cabral E.S, Gelderblom H, Hornung R.L, Munson P.J, Martin R, Marques A.R. Borrelia burgdorferi lipoprotein-mediated TLR2 stimulation causes the down-regulation of TLR5 in human monocytes. J Infect Dis. 2006; 193:849-59
Staphylococcus epidermidis	PSM	TLR2	Bacterial cell surface	Induce cytokine release¹⁶16 Strunk T, Power Coombs M.R, Currie A.J, et al. TLR2 mediates recognition of live Staphylococcus epidermidis and clearance of bacteremia. PLoS ONE. 2010; 5:e10111
Mycobacterium tuberculosis	19 kDa lipoprotein	TLR2	Cell wall	Induces apoptosis and inhibits IFN-γ induced expression of several immune function genes¹⁷17 Pennini M.E, Pai R.K, Schultz D.C, Boom W.H, Harding C.V. Mycobacterium tuberculosis 19-kDa lipoprotein inhibits IFN-gamma-induced chromatin remodeling of MHC2TA by TLR2 and MAPK signaling. J Immunol. 2006; 176:4323-30
Pseudomonas aeruginosa	LPS	TLR4, TLR2	Outer membrane	Induces TNF-α and IL-6¹⁸18 McIsaac S.M, Stadnyk A.W, Lin T.J. Toll-like receptors in the host defense against Pseudomonas aeruginosa respiratory infection and cystic fibrosis. J Leukoc Biol. 2012; 92:977-85
Pseudomonas aeruginosa	Lipoprotein (OprI)	TLR2, TLR4	Outer membrane	Modulate allergen-specific Th2 effector cells¹⁹19 Revets H, Pynaert G, Grooten J, De Baetselier P. Lipoprotein I, a TLR2/4 ligand modulates Th2-driven allergic immune responses. J Immunol. 2005; 174:1097-103

Virus
Measles	Hemagglutinin (HA)	TLR2	Cytoplasm	Suppresses IL-12 production²⁰20 Hahm B, Cho J.H, Oldstone M.B. Measles virus-dendritic cell interaction via SLAM inhibits innate immunity selective signaling through TLR4 but not other TLRs mediates suppression of IL-12 synthesis. Virology. 2007; 358:251-7
Herpes	Herpes Simplex Virus (HSV)	TLR2	Golgi complex	TNF-αand the IFN-stimulated gene CXCL9²¹21 Sorensen L.N, Reinert L.S, Malmgaard L, Bartholdy C, Thomsen A.R, Paludan S.R. TLR2 and TLR9 synergistically control herpes simplex virus infection in the brain. J Immunol. 2008; 181:8604-12
Respiratory syncytial virus (RSV)	F protein	TLR4	Membrane of the endoplasmic reticulum (ER)	Inflammatory cytokines (TNF-α, IL-6, etc.), type-1 interferons²²22 Uematsu S, Akira S. Toll-Like receptors (TLRs) and their ligands. Handb Exp Pharmacol. 2008; 1-20
Mouse mammary tumour virus (MMTV)	Envelope protein	TLR4	Nucleolus	Inflammatory cytokines (TNF-α, IL-6, etc.), type-1 interferons²²22 Uematsu S, Akira S. Toll-Like receptors (TLRs) and their ligands. Handb Exp Pharmacol. 2008; 1-20

Fungi
Saccharomyces cerevisiae	Zymosan	TLR2	Cell wall	Inflammatory cytokines (TNF-α, IL-6, etc.), type-1 interferons²²22 Uematsu S, Akira S. Toll-Like receptors (TLRs) and their ligands. Handb Exp Pharmacol. 2008; 1-20
Saccharomyces cerevisiae	Mannan	TLR4	Cell wall	Triggers TNF-α production²³23 Tada H, Nemoto E, Shimauchi H, et al. Saccharomyces cerevisiae- and Candida albicans-derived mannan induced production of tumor necrosis factor alpha by human monocytes in a CD14- and Toll-like receptor 4-dependent manner. Microbiol Immunol. 2002; 46:503-12
Candida albicans	Mannan	TLR4	Cell wall	Induces secrction of tumour necrosis factor(TNF)-α²³23 Tada H, Nemoto E, Shimauchi H, et al. Saccharomyces cerevisiae- and Candida albicans-derived mannan induced production of tumor necrosis factor alpha by human monocytes in a CD14- and Toll-like receptor 4-dependent manner. Microbiol Immunol. 2002; 46:503-12
Candida albicans	Phospholipomannan	TLR2	Cell wall	Stimulate tumour necrosis factor (TNF)-α production²⁴24 Jouault T, Ibata-Ombetta S, Takeuchi O, et al. Candida albicans phospholipomannan is sensed through toll-like receptors. J Infect Dis. 2003; 188:165-72
Cryptococcus neoformans	Glucuronoxylomannan (GXM)	TLR4	Capsule	Up-regulation of FasL²⁵25 Monari C, Pericolini E, Bistoni G, Casadevall A, Kozel T.R, Vecchiarelli A. Cryptococcus neoformans capsular glucuronoxylomannan induces expression of fas ligand in macrophages. J Immunol. 2005; 174:3461-8
Aspergillus fumigatus	Galactomannan	TLR4	Hyphae/Mycelium	Downregulates the IL-6 and TNF-α production²⁶26 Chai L.Y, Kullberg B.J, Vonk A.G, et al. Modulation of Toll-like receptor 2 (TLR2) and TLR4 responses by Aspergillus fumigatus. Infect Immun. 2009; 77:2184-92

Protozoa
Trypanosoma cruzi	GPI anchor	TLR2	Outer leaflet of the lipid bilayer	Proinflammatory cytokine release, interleukin12 (IL-12), nitric oxide (NO) and tumour necrosis factor (TNF) production²⁷27 Aoki M.P, Carrera-Silva E.A, Cuervo H, Fresno M, Girones N, Gea S. Nonimmune cells contribute to crosstalk between immune cells and inflammatory mediators in the innate response to Trypanosoma cruzi infection. J Parasitol Res. 2012; 2012:737324 Cytokine induction
Trypanosoma cruzi	Glycoinositolphospholipids	TLR4	Outer leaflet of the membrane	Induces IL12, TNF-α, and nitric oxide (NO) production²⁸28 Coelho P.S, Klein A, Talvani A, et al. Glycosylphosphatidylinositol-anchored mucin-like glycoproteins isolated from Trypanosoma cruzi trypomastigotes induce in vivo leukocyte recruitment dependent on MCP-1 production by IFN-gamma-primed-macrophages. J Leukoc Biol. 2002; 71:837-44
Plasmodium falciprum	GPI anchor	TLR2, TLR4	Cell membrane	Induces TNF-αand reduced IL-10 production²⁹29 Gowda D.C. TLR-mediated cell signaling by malaria GPIs. Trends Parasitol. 2007; 23:596-604
Toxoplasma gondii	GPI anchors	TLR2, TLR4	Microneme	Induces TNF-α production²²22 Uematsu S, Akira S. Toll-Like receptors (TLRs) and their ligands. Handb Exp Pharmacol. 2008; 1-20
Leishmania donovani	Galbetal 1, 4Manalpha-po(4)-containing phosphoglycans	TLR2	Surface	Induces nitric oxide (NO) and proinflammatory Cytokines³⁰30 Flandin J.F, Chano F, Descoteaux A. RNA interference reveals a role for TLR2 and TLR3 in the recognition of Leishmania donovani promastigotes by interferon-gamma-primed macrophages. Eur J Immunol. 2006; 36:411-20
Leishmania major	Lipophosphoglycan (LPG)	TLR2, TLR4	Entire surface of the parasite	Induces IL-12, TNF-α, IFN-γ, NO production³¹31 Faria M.S, Calegari-Silva T.C, de Carvalho Vivarini A, Mottram J.C, Lopes U.G, Lima A.P. Role of protein kinase R in the killing of Leishmania major by macrophages in response to neutrophil elastase and TLR4 via TNFalpha and IFNbeta. FASEB J. 2014; 28:3050-63
Leishmania major	Ecotin-like serine peptidase inhibitor	TLR2, TLR4	Cytosol	Up-regulation of proinflammatory cytokines³¹31 Faria M.S, Calegari-Silva T.C, de Carvalho Vivarini A, Mottram J.C, Lopes U.G, Lima A.P. Role of protein kinase R in the killing of Leishmania major by macrophages in response to neutrophil elastase and TLR4 via TNFalpha and IFNbeta. FASEB J. 2014; 28:3050-63
Leishmana sp.	SHP-1	TLR2	Nuclear envelope	Inhibition of pro inflammatory gene expression³²32 Abu-Dayyeh I, Shio M.T, Sato S, Akira S, Cousineau B, Olivier M. Leishmania-induced IRAK-1 inactivation is mediated by SHP-1 interacting with an evolutionarily conserved KTIM motif. PLoS Negl Trop Dis. 2008; 2:e305
Leishmania mexicana	SHP-1	TLR2	Nuclear envelope	Block IFN-γmediated nitric oxide (NO) production in macrophages³³33 Abu-Dayyeh I, Hassani K, Westra E.R, Mottram J.C, Olivier M. Comparative study of the ability of Leishmania mexicana promastigotes and amastigotes to alter macrophage signaling and functions. Infect Immun. 2010; 78:2438-45
Entamoeba histolytica	Lipopeptidophosphoglycans (LPPG)	TLR2, TLR4	Cell surface of the trophozoites	Leads to TNF-α, IL-12, IL-10, and nitric oxide release in phagocytes³⁴34 Wong-Baeza I, Alcantara-Hernandez M, Mancilla-Herrera I, et al. The role of lipopeptidophosphoglycan in the immune response to Entamoeba histolytica. J Biomed Biotechnol. 2010; 2010:254521

Nematode
Filarial nematode	Lacto-N-fucopentaose III (LNFPIII)	TLR4	Surface	Promote type 2 responses³⁵35 Diaz A, Allen J.E. Mapping immune response profiles the emerging scenario from helminth immunology. Eur J Immunol. 2007; 37:3319-26
Acanthocheilonema Viteae	Phosphatidyl Choline moiety (ES-62)	TLR4	Surface	Blockade of IL-12 and TNF-α Production³⁶36 Goodridge H.S, Marshall F.A, Else K.J, et al. Immunomodulation via novel use of TLR4 by the filarial nematode phosphorylcholine-containing secreted product, ES-62. J Immunol. 2005; 174:284-93
Ascaris lumbricoides	phospholipids	TLR2	Muscle, cuticle	Induces Th2 response³⁷37 van Riet E, Everts B, Retra K, et al. Combined TLR2 and TLR4 ligation in the context of bacterial or helminth extracts in human monocyte derived dendritic cells molecular correlates for Th1/Th2 polarization. BMC Immunol. 2009; 10:9

Trematode
Schistosoma mansoni	Lysophosphatidylserine (lyso-PS)	TLR2	Tegumental surface membrane	Induce the development of IL-10-producing regulatory T cells³⁸38 van der Kleij D, Latz E, Brouwers J.F, et al. A novel host-parasite lipid cross-talk. Schistosomal lyso-phosphatidylserine activates toll-like receptor 2 and affects immune polarization. J Biol Chem. 2002; 277:48122-9
Schistosoma mansoni	Glycolipid (LFNPIII)	TLR2	Surface membrane	Induction of Treg& IL-10³⁵35 Diaz A, Allen J.E. Mapping immune response profiles the emerging scenario from helminth immunology. Eur J Immunol. 2007; 37:3319-26
Schistosoma mansoni	Schistosoma soluble egg antigen (SEA)	TLR2	Egg and adult tegument	Up-regulation of OX40L in DC and block the Th2 response³⁵35 Diaz A, Allen J.E. Mapping immune response profiles the emerging scenario from helminth immunology. Eur J Immunol. 2007; 37:3319-26
Schistosoma mansoni	Lysophosphatidylserine [LPhS (SWA)]	TLR2	Surface membrane	Generation of IL-10-producing Treg cells³⁵35 Diaz A, Allen J.E. Mapping immune response profiles the emerging scenario from helminth immunology. Eur J Immunol. 2007; 37:3319-26
Schistosoma japonicum	HSP60 (SjHSP60)-derived peptide SJMHE1	TLR2	Surface membrane	InducesTreg with immunosuppressive activity³⁹39 Wang X, Zhou S, Chi Y, et al. CD4+CD25+ Treg induction by an HSP60-derived peptide SJMHE1 from Schistosoma japonicum is TLR2 dependent. Eur J Immunol. 2009; 39:3052-65

Cestode
Taenia crassiceps	Taeniacrassiceps excreted/secreted antigens (TcES)	TLR4	Excretory or secretory products	Impaired pro-inflammatory cytokine production and increased Th2 biasing ability of dendritic cells⁴⁰40 Terrazas C.A, Gomez-Garcia L, Terrazas L.I. Impaired pro-inflammatory cytokine production and increased Th2-biasing ability of dendritic cells exposed to Taenia excreted/secreted antigens: a critical role for carbohydrates but not for STAT6 signaling. Int J Parasitol. 2010; 40:1051-62
Taenia solium	N-linkedglycans	TLR2	Membrane surface	Diminish the production of proinflammatory cytokines⁴¹41 Johnston M.J, MacDonald J.A, McKay D.M. Parasitic helminths a pharmacopeia of anti-inflammatory molecules. Parasitology. 2009; 136:125-47

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