C-type lectin receptors in tuberculosis: what we know

Goyal, Surabhi; Klassert, Tilman E.; Slevogt, Hortense

doi:10.1007/s00430-016-0470-1

Cited by 34 publications

(22 citation statements)

References 258 publications

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“…It is part of a large family of C-type lectin (CTL) receptors, which can cross-talk with other pattern recognition receptor (PRRs) (Goyal et al, 2016). CD206 is a calcium-dependent type I transmembrane glycoprotein that contains an extracellular N-terminal cysteine-rich (CR) domain, a fibronectin II (FNII) domain, eight carbohydrate recognition domains (CRDs), a transmembrane domain, and a cytoplasmic tail (Stahl et al, 1980).…”

Section: Introductionmentioning

confidence: 99%

“…The MR is currently recognized as a prototypic PRR expressed on macrophages, some dendritic cells (Sallusto et al, 1995) and other cell types (Stahl and Ezekowitz, 1998), orchestrating innate and adaptive immune communication (He et al, 2007), and is emerging as a critical regulator of health and disease (Lee et al, 2002; Zhang et al, 2012; Hattori et al, 2010; Hattori et al, 2009). Despite its well-known central role in host recognition of a variety of microbes and ability to modulate inflammatory responses, its receptor-specific role in transducing signals to regulate phagocytosis and inflammatory pathways remains in question (Le Cabec et al, 2005; Gazi and Martinez-Pomares, 2009; Goyal et al, 2016; Hoving et al, 2014; Martinez-Pomares, 2012; Sancho and Reis E Sousa, 2012, Taylor et al, 2005; Gordon, 2016). …”

Section: Introductionmentioning

confidence: 99%

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M. tuberculosis -Initiated Human Mannose Receptor Signaling Regulates Macrophage Recognition and Vesicle Trafficking by FcRγ-Chain, Grb2, and SHP-1

et al. 2017

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Summary Despite its prominent role as C-type lectin (CTL) pattern recognition receptor, mannose receptor (MR, CD206)-specific signaling molecules and pathways are unknown. The MR is highly expressed on human macrophages, regulating endocytosis, phagocytosis and immune responses, and mediating Mycobacterium tuberculosis (M.tb) phagocytosis by human macrophages thereby limiting phagosome-lysosome (P-L) fusion. We identified human MR-associated proteins using phosphorylated and non-phosphorylated MR cytoplasmic tail peptides. We found that MR binds FcRγ-chain, which is required for MR plasma membrane localization and M.tb cell association. Additionally, we discovered that MR-mediated M.tb association triggers immediate MR tyrosine residue phosphorylation and Grb2 recruitment, activating the Rac/Pak/Cdc-42 signaling cascade important for M.tb uptake. MR activation subsequently recruits SHP-1 to the M.tb-containing phagosome, where its activity limits PI(3)P generation at the phagosome and M.tb P-L fusion, and promotes M.tb growth. In sum, we identify human MR signaling pathways that temporally regulate phagocytosis and P-L fusion during M.tb infection.

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Section: Introductionmentioning

confidence: 99%

Section: Introductionmentioning

confidence: 99%

M. tuberculosis -Initiated Human Mannose Receptor Signaling Regulates Macrophage Recognition and Vesicle Trafficking by FcRγ-Chain, Grb2, and SHP-1

et al. 2017

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“…In contrast, normal or increased levels of MBL are linked to frequent infection with M. tuberculosis and M. leprae (Garred et al 1994(Garred et al , 1997b, probably through complement-mediated phagocytosis of the pathogen. Up to 30% of healthy individuals have polymorphisms linked to MBL deficiency and these, together with serum levels, have been associated with susceptibility to tuberculosis and other inflammatory diseases in some ethnic populations (Takahashi and Ezekowitz 2005;Thiel et al 2006;Goyal et al 2016).…”

Section: Mblmentioning

confidence: 99%

Collectins: Innate Immune Pattern Recognition Molecules

Murugaiah

Tsolaki

Kishore

2020

Advances in Experimental Medicine and Biology

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Collectins are collagen-containing C-type (calcium-dependent) lectins which are important pathogen pattern recognising innate immune molecules. Their primary structure is characterised by an N-terminal, triple-helical collagenous region made up of Gly-X-Y repeats, an a-helical coiled-coil trimerising neck region, and a Cterminal C-type lectin or carbohydrate recognition domain (CRD). Further oligomerisation of this primary structure can give rise to more complex and multimeric structures that can be seen under electron microscope. Collectins can be found in serum as well as in a range of tissues at the mucosal surfaces. Mannanbinding lectin can activate the complement system while other members of the collectin family are extremely versatile in recognising a diverse range of pathogens via their CRDs and bring about effector functions designed at the clearance of invading pathogens. These mechanisms include opsonisation, enhancement of phagocytosis, triggering superoxidative burst and nitric oxide production. Collectins can also potentiate the adaptive immune response via antigen presenting cells such as macrophages and dendritic cells through modulation of cytokines and chemokines, thus they can act as a link between innate and adaptive immunity. This chapter describes the structure-function relationships of collectins, their diverse functions, and their interaction with viruses, bacteria, fungi and parasites.

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“…Mannose Receptor (MR) also recognizes a number of mycobacterial mannose-containing PAMPs, including ManLAM, higher PIMs, LM, and other mannosylated proteins. MR is predominantly expressed on alveolar macrophages, and its interaction with ManLAM induces production of anti-inflammatory cytokines [34]. More work is still required in understanding downstream signaling of MR.…”

Section: Other Clrsmentioning

confidence: 99%