Staphylococcus aureus Aggregation and Coagulation Mechanisms, and Their Function in Host–Pathogen Interactions

Crosby, Heidi A.; Kwieciński, Jakub; Horswill, Alexander R.

doi:10.1016/bs.aambs.2016.07.018

Cited by 121 publications

(113 citation statements)

References 223 publications

(300 reference statements)

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“…S. aureus expresses a range of host matrix binding proteins on its surface in addition to albumin-binding activities (48)(49)(50). One of the albumin-binding proteins, Ebh, has been shown to contribute to survival in blood and the overall pathogenesis of staphylococcal infections (49).…”

Section: Resultsmentioning

confidence: 99%

The Antistaphylococcal Lysin, CF-301, Activates Key Host Factors in Human Blood To Potentiate Methicillin-ResistantStaphylococcus aureusBacteriolysis

Sauve

Raz

Abdelhady

et al. 2019

Antimicrob Agents Chemother

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Bacteriophage-derived lysins are cell-wall-hydrolytic enzymes that represent a potential new class of antibacterial therapeutics in development to address burgeoning antimicrobial resistance. CF-301, the lead compound in this class, is in clinical development as an adjunctive treatment to potentially improve clinical cure rates of Staphylococcus aureus bacteremia and infective endocarditis (IE) when used in addition to antibiotics. In order to profile the activity of CF-301 in a clinically relevant milieu, we assessed its in vitro activity in human blood versus in a conventional testing medium (cation-adjusted Mueller-Hinton broth [caMHB]). CF-301 exhibited substantially greater potency (32 to Ն100-fold) in human blood versus caMHB in three standard microbiologic testing formats (e.g., broth dilution MICs, checkerboard synergy, and time-kill assays). We demonstrated that CF-301 acted synergistically with two key human blood factors, human serum lysozyme (HuLYZ) and human serum albumin (HSA), which normally have no nascent antistaphylococcal activity, against a prototypic methicillin-resistant S. aureus (MRSA) strain (MW2). Similar in vitro enhancement of CF-301 activity was also observed in rabbit, horse, and dog (but not rat or mouse) blood. Two well-established MRSA IE models in rabbit and rat were used to validate these findings in vivo by demonstrating comparable synergistic efficacy with standard-of-care anti-MRSA antibiotics at Ͼ100-fold lower lysin doses in the rabbit than in the rat model. The unique properties of CF-301 that enable bactericidal potentiation of antimicrobial activity via activation of "latent" host factors in human blood may have important therapeutic implications for durable improvements in clinical outcomes of serious antibiotic-resistant staphylococcal infections.

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Section: Resultsmentioning

confidence: 99%

The Antistaphylococcal Lysin, CF-301, Activates Key Host Factors in Human Blood To Potentiate Methicillin-ResistantStaphylococcus aureusBacteriolysis

Sauve

Raz

Abdelhady

et al. 2019

Antimicrob Agents Chemother

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“…It has been reported that some of the cell surface proteins of S. aureus bind and aggregate following interaction with extracellular matrix proteins in the blood (42,43). We previously analyzed the properties of CBPpositive S. mutans strain binding to type I, III, and IV collagens, since these collagen types are major components of cardiovascular tissues (11).…”

Section: Discussionmentioning

confidence: 99%

Contribution of Streptococcus mutans Strains with Collagen-Binding Proteins in the Presence of Serum to the Pathogenesis of Infective Endocarditis

et al. 2017

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Streptococcus mutans, a major pathogen of dental caries, is considered one of the causative agents of infective endocarditis (IE). Recently, bacterial DNA encoding 120-kDa cell surface collagen-binding proteins (CBPs) has frequently been detected from S. mutans-positive IE patients. In addition, some of the CBP-positive S. mutans strains lacked a 190-kDa protein antigen (PA), whose absence strengthened the adhesion to and invasion of endothelial cells. The interaction between pathogenic bacteria and serum or plasma is considered an important virulence factor in developing systemic diseases; thus, we decided to analyze the pathogenesis of IE induced by S. mutans strains with different patterns of CBP and PA expression by focusing on the interaction with serum or plasma. CBP-positive (CBP ϩ )/PA-negative (PA Ϫ ) strains showed prominent aggregation in the presence of human serum or plasma, which was significantly greater than that with CBP ϩ /PA-positive (PA ϩ ) and CBP-negative (CBP Ϫ )/PAϩ strains. Aggregation of CBP ϩ /PA Ϫ strains was also observed in the presence of a high concentration of type IV collagen, a major extracellular matrix protein in serum. In addition, aggregation of CBP ϩ /PA Ϫ strains was drastically reduced when serum complement was inactivated. Furthermore, an ex vivo adherence model and an in vivo rat model of IE showed that extirpated heart valves infected with CBP ϩ /PA Ϫ strains displayed prominent bacterial mass formation, which was not observed following infection with CBP ϩ /PA ϩ and CBP Ϫ /PA ϩ strains. These results suggest that CBP ϩ /PA Ϫ S. mutans strains utilize serum to contribute to their pathogenicity in IE. KEYWORDS Streptococcus mutans, blood, infective endocarditisG ram-positive cocci, such as Staphylococcus aureus and viridans group streptococci, are major pathogens in infective endocarditis (IE) (1, 2). One of the important steps for the pathogenesis of IE is invasion of pathogenic bacteria into the bloodstream (1). Viridans group streptococci invade the bloodstream following professional dental treatment as well as routine daily oral care (3, 4) and are associated with a risk for IE in subjects with underlying heart disorders, though these bacteria are predominantly phagocytosed and eliminated in healthy humans (5).Streptococcus mutans, classified as a viridans group streptococcus, is a major pathogen of dental caries and is occasionally isolated from the blood of IE patients (6). In 1993, approximately 10 to 20% of S. mutans strains were demonstrated to possess collagen-binding activity, which was regarded to be advantageous for binding to collagenous tissue, such as dentin (7). Thereafter, 120-kDa collagen-binding proteins (CBPs), which were classified as Cnm and Cbm, were identified on the cell surfaces of some S. mutans strains in 2004 and 2012, respectively (8, 9).

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“…Bacteria in different growth modes have distinctly different characteristics. Planktonic refers to free living bacterial cells, which can occur in two forms: as single bacterial cells or in clusters known as planktonic aggregates (Crosby et al 2016). Clinically, this planktonic mode generally refers to bacteria that gain entrance to the human body in the bloodstream and cause bacteremia, which results in acute infections often effectively treated by the host immune system and antibiotics (Stewart and Costerton 2001;Brady et al 2018).…”

Section: Bacteriamentioning

confidence: 99%

Sonobactericide: An Emerging Treatment Strategy for Bacterial Infections

Lattwein

Shekhar

Kouijzer

et al. 2020

Ultrasound in Medicine & Biology

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Ultrasound has been developed as both a diagnostic tool and a potent promoter of beneficial bioeffects for the treatment of chronic bacterial infections. Bacterial infections, especially those involving biofilm on implants, indwelling catheters and heart valves, affect millions of people each year, and many deaths occur as a consequence. Exposure of microbubbles or droplets to ultrasound can directly affect bacteria and enhance the efficacy of antibiotics or other therapeutics, which we have termed sonobactericide. This review summarizes investigations that have provided evidence for ultrasound-activated microbubble or droplet treatment of bacteria and biofilm. In particular, we review the types of bacteria and therapeutics used for treatment and the in vitro and pre-clinical experimental setups employed in sonobactericide research. Mechanisms for ultrasound enhancement of sonobactericide, with a special emphasis on acoustic cavitation and radiation force, are reviewed, and the potential for clinical translation is discussed. (

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Staphylococcus aureus Aggregation and Coagulation Mechanisms, and Their Function in Host–Pathogen Interactions

Cited by 121 publications

References 223 publications

The Antistaphylococcal Lysin, CF-301, Activates Key Host Factors in Human Blood To Potentiate Methicillin-ResistantStaphylococcus aureusBacteriolysis

The Antistaphylococcal Lysin, CF-301, Activates Key Host Factors in Human Blood To Potentiate Methicillin-ResistantStaphylococcus aureusBacteriolysis

Contribution of Streptococcus mutans Strains with Collagen-Binding Proteins in the Presence of Serum to the Pathogenesis of Infective Endocarditis

Sonobactericide: An Emerging Treatment Strategy for Bacterial Infections

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