Bacterial killing by complement requires membrane attack complex formation via surface‐bound C5 convertases

Heesterbeek, Dani A. C.; Bardoel, Bart W.; Parsons, Edward S.; Bennett, Isabel; Ruyken, Maartje; Doorduijn, Dennis J.; Gorham, Ronald D.; Berends, Evelien T.M.; Pyne, Alice L. B.; Hoogenboom, Bart W.; Rooijakkers, Suzan H. M.

doi:10.15252/embj.201899852

Cited by 84 publications

(154 citation statements)

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“…[36] In general, monomers of the MACPF/CDC protein family first bind to a specific target on the target surface via a membrane-binding domain. Our recent report, describing how surface-bound C5 convertases are essential to properly insert MAC pores into target bacteria, [22] supports this hypothesis. [37] After binding to the membrane, these monomers homo-oligomerize and form a "prepore" that does not yet permeate the membrane.…”

Section: The Assembly Of the Mac Porementioning

confidence: 57%

“…These C5 convertases, which are multimeric, enzymatic complexes that cleave C5 into C5a and C5b, are covalently linked to the bacterial surface when the complement system is activated. [22,29,49] In contrast to convertase-generated MAC pores, pores that were generated from preassembled C5b6 were sensitive to trypsin and not visible by AFM, suggesting that these pores were not stably inserted into the bacterial OM. Local MAC assembly by C5 convertases is crucial to efficiently insert MAC pores into the bacterial OM.…”

Section: Bacterial Killing By the Mac Requires Local Mac Assembly Bymentioning

confidence: 99%

“…Since this composite cell envelope of Gram-negative bacteria spans over 30 nm (as shown in Figure 2A), [19] it seems physically impossible for the MAC (that has a transmembrane domain of ≈5 nm [29] ) to damage the full cell envelope. B) Schematic overview of how local MAC assembly damages the cell envelope of Gramnegative bacteria, explained using the recently developed assay for measuring cell envelope integrity in Heesterbeek et al [22] When the MAC is locally generated by surface-bound C5 convertases, these pores are stably inserted into the bacterial OM and permeate the OM leading to leakage of periplasmic proteins (as depicted by the absence of red periplasmic content). Moreover, as Gram-negative bacteria are metabolically active, an active cellular process could also be involved in bacterial killing by MAC pores.…”

Section: Functional Insights Into How Mac Pores Kill Gram-negative Bamentioning

confidence: 99%

“…[22] In order to efficiently kill a bacterium, the MAC needs to be generated by surface-bound C5 convertases. [22] In order to efficiently kill a bacterium, the MAC needs to be generated by surface-bound C5 convertases.…”

Section: Bacterial Killing By the Mac Requires Local Mac Assembly Bymentioning

confidence: 99%

“…[16][17][18] However, the exact molecular mechanism by which MAC pores kill Gram-negative bacteria remains largely unknown. [22] This review provides an overview of these recent structural findings on how MAC pores assemble and summarizes these recent functional studies on bacteria. [19] Several hypotheses on how MAC pores could permeate the complex cell envelope of Gram-negative bacteria in order to kill the bacterium have previously been reviewed.…”

Section: Introductionmentioning

confidence: 99%

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How the Membrane Attack Complex Damages the Bacterial Cell Envelope and Kills Gram‐Negative Bacteria

2019

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The human immune system can directly lyse invading micro-organisms and aberrant host cells by generating pores in the cell envelope, called membrane attack complexes (MACs). Recent studies using single-particle cryoelectron microscopy have revealed that the MAC is an asymmetric, flexible pore and have provided a structural basis on how the MAC ruptures single lipid membranes. Despite these insights, it remains unclear how the MAC ruptures the composite cell envelope of Gram-negative bacteria. Recent functional studies on Gram-negative bacteria elucidate that local assembly of MAC pores by surface-bound C5 convertase enzymes is essential to stably insert these pores into the bacterial outer membrane (OM). These convertase-generated MAC pores can subsequently efficiently damage the bacterial inner membrane (IM), which is essential for bacterial killing. This review summarizes these recent insights of MAC assembly and discusses how MAC pores kill Gramnegative bacteria. Furthermore, this review elaborates on how MAC-dependent OM damage could lead to IM destabilization, which is currently not well understood. A better understanding on how MAC pores kill bacteria could facilitate the future development of novel strategies to treat infections with Gram-negative bacteria.

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Section: The Assembly Of the Mac Porementioning

confidence: 57%

Section: Bacterial Killing By the Mac Requires Local Mac Assembly Bymentioning

confidence: 99%

Section: Functional Insights Into How Mac Pores Kill Gram-negative Bamentioning

confidence: 99%

Section: Bacterial Killing By the Mac Requires Local Mac Assembly Bymentioning

confidence: 99%

Section: Introductionmentioning

confidence: 99%

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How the Membrane Attack Complex Damages the Bacterial Cell Envelope and Kills Gram‐Negative Bacteria

2019

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Complement evasion by the human respiratory tract pathogens Haemophilus influenzae and Moraxella catarrhalis

Riesbeck

2020

FEBS Letters

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All infective bacterial species need to conquer the innate immune system in order to colonize and survive in their hosts. The human respiratory pathogens Haemophilus influenzae and Moraxella catarrhalis are no exceptions and have developed sophisticated mechanisms to evade complement-mediated killing. Both bacterial species carry lipooligosaccharides preventing complement attacks and attract and utilize host complement regulators C4b binding protein and factor H to inhibit the classical and alternative pathways of complement activation, respectively. In addition, the regulator of the terminal pathway of complement activation, vitronectin, is hijacked by both bacteria. An array of different outer membrane proteins (OMP) in H. influenzae and M. catarrhalis simultaneously binds complement regulators, but also plasminogen. Several of the bacterial complement-binding proteins are important adhesins and contain highly conserved regions for interactions with the host. Thus, some of the OMP are viable targets for new therapeutics, including vaccines aimed at preventing respiratory tract diseases such as otitis media in children and exacerbations in patients suffering from chronic obstructive pulmonary disease.

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Streptococci and the complement system: interplay during infection, inflammation and autoimmunity

et al. 2020

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Streptococci are a broad group of Gram-positive bacteria. This genus includes various human pathogens causing significant morbidity and mortality. Two of the most important human pathogens are Streptococcus pneumoniae (pneumococcus) and Streptococcus pyogenes (group A streptococcus or GAS). Streptococcal pathogens have evolved to express virulence factors that enable them to evade complement-mediated attack. These include factor Hbinding M (S. pyogenes) and pneumococcal surface protein C (PspC) (S. pneumoniae) proteins. In addition, S. pyogenes and S. pneumoniae express cytolysins (streptolysin and pneumolysin), which are able to destroy host cells. Sometimes, the interplay between streptococci, the complement, and antistreptococcal immunity may lead to an excessive inflammatory response or autoimmune disease. Understanding the fundamental role of the complement system in microbial clearance and the bacterial escape mechanisms is of paramount importance for understanding microbial virulence, in general, and, the conversion of commensals to pathogens, more specifically. Such insights may help to identify novel antibiotic and vaccine targets in bacterial pathogens to counter their growing resistance to commonly used antibiotics.

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Bacterial killing by complement requires membrane attack complex formation via surface‐bound C5 convertases

Cited by 84 publications

References 64 publications

How the Membrane Attack Complex Damages the Bacterial Cell Envelope and Kills Gram‐Negative Bacteria

How the Membrane Attack Complex Damages the Bacterial Cell Envelope and Kills Gram‐Negative Bacteria

Complement evasion by the human respiratory tract pathogens Haemophilus influenzae and Moraxella catarrhalis

Streptococci and the complement system: interplay during infection, inflammation and autoimmunity

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