The Staphylococcal Superantigen-Like Protein 7 Binds IgA and Complement C5 and Inhibits IgA-FcαRI Binding and Serum Killing of Bacteria

Langley, Ries J.; Wines, Bruce D.; Willoughby, Natasha; Basu, Indira; Proft, Thomas; Fraser, John D.

doi:10.4049/jimmunol.174.5.2926

Cited by 211 publications

(237 citation statements)

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“…Interestingly, the SSL7 ␤-grasp domains extend beyond the end of the Fc and are around the expected position of the tail pieces and J-chain that are responsible for the formation of polymeric IgA. We have demonstrated previously that SSL7 binds with high affinity to IgA found in mucosal secretions (22). The relatively flat topography of the current complex may allow the Fc of dimeric IgA to interact concurrently with both secretory component and SSL7.…”

Section: Resultsmentioning

confidence: 99%

“…Because SSL7 binds serum IgA a role in inhibiting Fc␣RI-mediated effector functions in S. aureus systemic infections is feasible (29,42,43). However, the topography of the SSL7 interaction with Fc may reflect adaptation for its known binding of secretory IgA (22), thereby facilitating mucosal colonization by S. aureus. The existence of functionally equivalent, although unrelated, proteins from group A and group B streptococci (29,30), themselves often mucosal pathogens, suggests the mucosal response is the primary target of these IgA-binding proteins.…”

Section: Discussionmentioning

confidence: 99%

“…Circulating and secreted IgA differ in form and function (41), and SSL7 binds both with high affinity (22). Because SSL7 binds serum IgA a role in inhibiting Fc␣RI-mediated effector functions in S. aureus systemic infections is feasible (29,42,43).…”

Section: Discussionmentioning

confidence: 99%

“…This prototypical member of the SSL family of exotoxins (12) can bind with high affinity by comprehensively shielding both sides of the lower half of the Fc, apparently without blocking the additional components (tailpieces, J-chain, and secretory component) that assemble to form dimeric and secretory IgA (22). The Fc residues recognized by SSL7 occur in all human IgA subclasses and allotypes.…”

Section: Discussionmentioning

confidence: 99%

“…Both SSL5 (21) and SSL11 (M. C. Chung, B.D.W., H. Baker, R. J. Langley, E. N. Baker, and J.D.F., unpublished data) interact with sialyl-Le x and related oligosaccharides, thereby inhibiting key cellular adhesion processes such as neutrophil transmigration. Notably, SSL7 exhibits multiple activities, including the binding of complement component C5 and serum and mucosal forms of IgA, thereby inhibiting both C5 and fragment crystalline (Fc) receptor for IgA (Fc␣RI)-mediated immunity (22,23). Furthermore, SSL7 has been observed to alter cytokine secretion (12) and to bind, and be rapidly internalized by, monocytes and dendritic cells, but the ligands involved are yet to be identified (16,19).…”

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Structural basis for evasion of IgA immunity by Staphylococcus aureus revealed in the complex of SSL7 with Fc of human IgA1

Ramsland

Willoughby

Trist

et al. 2007

Proc. Natl. Acad. Sci. U.S.A.

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104

102

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Infection by Staphylococcus aureus can result in severe conditions such as septicemia, toxic shock, pneumonia, and endocarditis with antibiotic resistance and persistent nasal carriage in normal individuals being key drivers of the medical impact of this virulent pathogen. In both virulent infection and nasal colonization, S. aureus encounters the host immune system and produces a wide array of factors that frustrate host immunity. One in particular, the prototypical staphylococcal superantigen-like protein SSL7, potently binds IgA and C5, thereby inhibiting immune responses dependent on these major immune mediators. We report here the three-dimensional structure of the complex of SSL7 with Fc of human IgA1 at 3.2 Å resolution. Two SSL7 molecules interact with the Fc (one per heavy chain) primarily at the junction between the C␣2 and C␣3 domains. The binding site on each IgA chain is extensive, with SSL7 shielding most of the lateral surface of the C␣3 domain. However, the SSL7 molecules are positioned such that they should allow binding to secretory IgA. The key IgA residues interacting with SSL7 are also bound by the leukocyte IgA receptor, Fc␣RI (CD89), thereby explaining how SSL7 potently inhibits IgAdependent cellular effector functions mediated by Fc␣RI, such as phagocytosis, degranulation, and respiratory burst. Thus, the ability of S. aureus to subvert IgA-mediated immunity is likely to facilitate survival in mucosal environments such as the nasal passage and may contribute to systemic infections.Staphylococcus aureus is an important human pathogen causing conditions ranging from minor superficial skin infections to life-threatening syndromes, including sepsis, toxic shock syndrome, osteomyelitis, pneumonitis, and endocarditis. It is carried without symptoms in at least 20% of individuals (1, 2). The emergence in the 1960s of pandemic penicillin-resistant S. aureus has been followed by a variety of hospital-associated and community-associated methicillin-resistant strains (HA-and CA-MRSA) (2, 3). The increased prevalence of MRSA infections and corresponding rise in life-threatening syndromes have made it imperative to elucidate the mechanisms of pathogenesis for S. aureus. The interaction between S. aureus and the host is complex and is mediated by an array of bacterial proteins that both mediate the various pathologies and modify the immune system of the host (4-10).SSL7 (formerly named SET1) is the first described member of a new family of putative S. aureus toxins, the staphylococcal superantigen-like (SSL) proteins (11, 12), related to the staphylococcal enterotoxins (SEs) or superantigens (13). The SSL proteins have Ϸ30% sequence identity with toxic shock syndrome 1 (TSST-1) and 25% or less identity with other SEs. Despite the sequence differences, the SSL proteins have a typical SE tertiary structure consisting of a distinct oligonucleotide/oligosaccharide binding (OB-fold) linked to a ␤-grasp domain (14 -16).Similar to the se genes, the ssl genes are located in a pathogenicity island (SaPIn2) and ...

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Section: Resultsmentioning

confidence: 99%

Section: Discussionmentioning

confidence: 99%

Section: Discussionmentioning

confidence: 99%

Section: Discussionmentioning

confidence: 99%

mentioning

confidence: 99%

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Structural basis for evasion of IgA immunity by Staphylococcus aureus revealed in the complex of SSL7 with Fc of human IgA1

Ramsland

Willoughby

Trist

et al. 2007

Proc. Natl. Acad. Sci. U.S.A.

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104

102

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Staphylococcal superantigen‐like proteins interact with human MAP kinase signaling protein ERK2

Dutta

Mukherjee

et al. 2019

FEBS Letters

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This study aimed to identify the intracellular binding partner of a unique class of staphylococcal secreted exotoxins called superantigen‐like proteins (SSL) from human macrophage and keratinocyte cell lysates. Here, we report that SSL1 specifically binds to human extracellular signal‐regulated kinase 2 (hERK2), an important stress‐activated kinase in mitogen‐activated protein kinase signaling pathways. Western blot and in vitro binding studies with recombinant hERK2 confirmed the binding interaction of SSL1, SSL7, and SSL10 with hERK2. Moreover, the SSLs‐hERK2 interaction was validated biochemically by ELISA. Our finding shows that SSLs play a novel role by binding with host cell MAP kinase signaling pathway protein. Understanding the SSL‐hERK2 interaction will also provide a basis for designing SSL‐based peptide inhibitors of hERK2 in cancer therapy.

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Immune Defence: Microbial Interference

Merino

2010

Encyclopedia of Life Sciences

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The immune system controls the host–microbe interactions, the outcome of which can range from symbiotic coexistence with commensally microbiota, to mild asymptomatic infections, to highly virulent infectious diseases. This control is achieved by two defence mechanisms: the innate immune defence, which consists in a nonspecific mechanism, and the adaptive immunity defence, acquired over time following infections or vaccination. Despite the sophisticated immune system, extracellular and intracellular pathogens have developed numerous, and often ingenious strategies, to evade, interfere or eradicate the effectiveness of host immune defences. Although the strategies used by viral and bacterial pathogens are numerous, there are several general mechanisms shared between these microbial pathogens. The success of each pathogen depends on the coordinated activities of its virulence factors to overcome host barriers to colonisation and its ability to mount an effective anti‐immune response within the infected host, which can ultimately result in acute disease or chronic infection. Key Concepts: Immunoglobulin proteases cleave antibodies rendering them nonfunctional and leading to deficiencies in the immune system. Complement regulators prevent complement activation and cell destruction. Interference with major histocompatibility complexes overcomes T‐cell recognition. Microbial interference with cytokines modulates intracellular signalling critical to the regulation, proliferation and differentiation of lymphocytes, which drive inflammation. Intracellular resistance allows microorganisms to circumvent humoral defence mechanisms and spread within the host. Immunosuppresion reduces T or B lymphocytes’ defence.

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The Staphylococcal Superantigen-Like Protein 7 Binds IgA and Complement C5 and Inhibits IgA-FcαRI Binding and Serum Killing of Bacteria

Cited by 211 publications

References 34 publications

Structural basis for evasion of IgA immunity by Staphylococcus aureus revealed in the complex of SSL7 with Fc of human IgA1

Structural basis for evasion of IgA immunity by Staphylococcus aureus revealed in the complex of SSL7 with Fc of human IgA1

Staphylococcal superantigen‐like proteins interact with human MAP kinase signaling protein ERK2

Immune Defence: Microbial Interference

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