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Ferretti JJ, Stevens DL, Fischetti VA, editors. Streptococcus pyogenes : Basic Biology to Clinical Manifestations [Internet]. Oklahoma City (OK): University of Oklahoma Health Sciences Center; 2016-.

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Streptococcus pyogenes : Basic Biology to Clinical Manifestations [Internet].

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Severe Group A Streptococcal Infections

, PhD, MD and , PhD.

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Introduction

Life-threatening infections caused by Streptococcus pyogenes (group A streptococcus) include scarlet fever, bacteremia, pneumonia, necrotizing fasciitis, myonecrosis and Streptococcal Toxic Shock Syndrome (StrepTSS). This chapter focuses on the clinical and epidemiological features of these infections, as well as treatment options and bacterial pathogenesis. In brief, such invasive infections can simply be defined as any infection in which S. pyogenes is isolated from a normally sterile body site. Patients with invasive S. pyogenes infections have a relatively low mortality rate, unless they meet the established criteria for StrepTSS.

Patient mortality is also influenced by the site of infection and the patient’s presenting history. For example, in patients with S. pyogenes necrotizing fasciitis/myonecrosis that lacks a discernable portal of bacterial entry, classical cutaneous signs of a necrotizing process are not initially apparent. In the absence of such clinical clues, the correct diagnosis is often missed or delayed until the patient manifests systemic shock and organ failure. This delay results in high morbidity and mortality rates. Interestingly, patients in this “no portal” category frequently develop soft-tissue infection at a site of relatively minor antecedent soft tissue injury (strain, bruise) that did not break the skin. Pain at the time of presentation is often out of proportion to the injury itself, and is an important clinical clue. A molecular mechanism that links injury to secondary S. pyogenes infection has been recently proposed, and is discussed later in this chapter.

Development of severe invasive infections is associated with strains that produce streptococcal pyrogenic exotoxins (Spe)—a family of bacterial superantigens that includes the classical scarlatina toxins SpeA and SpeC, the cysteine proteinase SpeB, and a number of more recently described superantigens (such as mitogenic factor [MF, SpeF] and streptococcal superantigen [SSA]). Superantigens are potent immunostimulators that cause clonal proliferation of T cells and watershed production of pro-inflammatory cytokines that mediate shock and organ failure. This concept, as well as the molecular biology of streptococcal virulence, colonization, and tissue invasion, is discussed in more detail in the section on the pathogenesis of StrepTSS.

Invasive Streptococcal Infections of Skin and Soft Tissues

In the mid-1980s, outbreaks of invasive streptococcal infections, of a frequency and severity not seen in the preceding decades, began to be reported both in the United States and abroad (Hoge, et al., 1993; Martin & Høiby, 1990; Strömberg, Romanus, & Burman, 1991; Demers, et al., 1993). Although certain S. pyogenes M-types (M 1, 3, 11, 12, and 28) account for 50% of the associated isolates (O'Brien, et al., 2002), there has been a definite and consistent tendency for M-types 1 and 3 to be associated with the more life-threatening infections (reviewed in (Wong & Stevens, 2013)). A high proportion of these cases have occurred in adults, and the portal of entry is frequently the skin, mucous membranes, or soft tissues. Invasive infections are often associated with shock and multi-organ failure, features similar to those of severe staphylococcal toxic shock syndrome (StaphTSS) (Silversides, Lappin, & Ferguson, 2010). Thus, the entity attributed to S. pyogenes has been termed StrepTSS. Clinical features of serious streptococcal skin and soft tissue infections and StrepTSS are described below.

Necrotizing Fasciitis (Streptococcal Gangrene)

Necrotizing fasciitis (NF) is an infection of the deeper subcutaneous tissues and fascia that is characterized by extensive and rapidly spreading necrosis (gangrene) of the skin and underlying structures. While necrotizing soft-tissue infections may be caused by multiple aerobic and anaerobic microorganisms and may vary in their clinical manifestations, the present discussion is limited to necrotizing fasciitis caused by S. pyogenes (Bisno & Stevens, 1996), and as described by Meleney in 1924 as hemolytic streptococcal gangrene (Meleney, 1924). Characteristically, streptococcal gangrene begins at a site of trivial or even unapparent trauma or in an operative incision. The initial lesion may appear only as an area of mild erythema, but undergoes a rapid evolution over the next 24–72 hours. The inflammation becomes more pronounced and extensive, the skin becomes dusky and then purplish, and bullae containing yellow or hemorrhagic fluid appear. Bacteremia is frequently present, and metastatic abscesses may occur. By the fourth to fifth day, frank gangrenous changes are evident in the affected skin, followed by extensive sloughing. The process may march inexorably over large body areas unless measures are taken to contain it. The patient with streptococcal gangrene appears perilously ill, with high fever and extreme prostration. Mortality rates are high, even with appropriate treatment (Stevens, 1992).

In modern times, the course of S. pyogenes necrotizing fasciitis appears to be much more fulminant than that described by Meleney. Specifically, ecchymoses and bullae may appear within 2-3 days and deep muscle involvement is more common. In addition, the mortality rate in 1924 was only 20%, despite the lack of antibiotics, IV fluids, ventilators, and dialysis. In contrast, mortality rates of as high as 70–80% have been reported in the current era (reviewed in (Wong & Stevens, 2013)). Given the destruction of multiple layers of soft tissue (epidermis, dermis, subcutaneous tissue, fascia, muscle) in today’s infections, this author believes that “necrotizing soft-tissue infection” is a more accurate term to describe the modern disease.

Successful management of necrotizing fasciitis is dependent on early recognition, yet patients may initially present with cutaneous findings that appear relatively benign (Bisno, Cockerill, & Bermudez, 2000). Fever, when present (Bisno, Cockerill, & Bermudez, 2000), and severe pain are often the earliest manifestations of disease and are important clinical clues that should not be dismissed. In those patients with a defined portal of entry, such as a surgical incision, burn, insect bite or varicella lesion, there is redness of the skin, pain, and swelling. However, in the 50% of patients who develop necrotizing fasciitis/myonecrosis without a defined portal of entry, the infection begins deep in the tissues, frequently at the site of a hematoma, muscle strain, or traumatic joint injury. In these patients, the classical cutaneous signs of inflammation and infection are absent until late in the course. The most important clinical clue in this setting is crescendo pain.

Routine radiographs, computed tomography (CT) scanning, and magnetic resonance imaging (MRI) may show localized swelling of the deep structures, but characteristically do not show frank abscess formation or gas in the tissue—and thus are not definitive procedures. This is particularly problematic in the “no portal” patients who report antecedent trauma, since this history complicates the interpretation of imaging studies, in that clinicians cannot easily distinguish the cause of the deep swelling. In these cases, such studies often delay, rather than facilitate, a diagnosis. Further, patients with prior injury or surgery may have taken non-steroidal anti-inflammatory drugs (NSAIDs) that mask fever and reduce pain. Unexplained tachycardia, a marked left shift, and an elevated creatine phosphokinase level are also important clues to the diagnosis of necrotizing soft-tissue infections, and their presence should prompt surgical inspection of the deep tissues. Gram stains of aspirated fluid will reveal chains of Gram-positive cocci and few, if any, white blood cells. Similarly, a biopsy with frozen section may aid in the diagnosis of NF (Stamenkovic & Lew, 1984; Majeski & Majeski, 1997).

Myositis and Myonecrosis

Strictly speaking, myositis is a localized purulent infection of muscle. Most cases occur in tropical regions where S. aureus is the predominant causative agent; myositis due to S. pyogenes is rare. In contrast, non-purulent soft tissue infection due to S. pyogenes is common in patients with necrotizing fasciitis, myonecrosis, and StrepTSS. Many of these cases occur at sites of blunt, non-penetrating trauma, or arise spontaneously in the soft tissues. Organisms are likely hematogenously translocated from the throat to the deep soft tissues, though antecedent or concomitant streptococcal pharyngitis is not a prerequisite for this infection. Systemic toxicity is also common, and mortality as high as 80% has been reported (Adams, et al., 1985). The destruction of tissue is poorly understood, but infection within the confined muscle compartment may result in pressures that exceed arterial pressure, which necessitate emergent fasciotomy and debridement. In addition, bacterial toxin-induced formation of intravascular aggregates of platelets and leukocytes could obstruct blood flow, which leads to the ischemic necrosis of tissue (Bryant, et al., 2005).

As previously mentioned, there is a great deal of overlap in the clinical features of necrotizing fasciitis and myonecrosis (Stevens, 1992; Adams, Gudmundsson, Yocum, Haselby, Craig, & Sundstrom, 1985), since later in the disease course, both infections frequently destroy all layers of the soft tissues, including muscle. Differentiation of these entities can be made by surgical inspection or biopsy; however, treatment recommendations are the same for both (Stevens, et al., 2014).

Streptococcal Toxic Shock Syndrome

StrepTSS is more fully defined in Table 1 (The Working Group on Severe Streptococcal Infections, 1993), but, simply stated, is any streptococcal infection that is associated with the sudden onset of shock and organ failure. Definite cases are those in which S. pyogenes is isolated from a normally sterile body site. Such cases were first described in the United States and Europe during the mid- to late 1980s (Martin & Høiby, 1990; Stevens, et al., 1989; Francis & Warren, 1988). Since then, reports of StrepTSS in adults and children have emerged worldwide. Most cases have occurred sporadically, though some clusters have been reported. The highest incidence of invasive streptococcal disease occurred in a small Minnesota community, where 26 cases/100,000 population were recorded (Cockerill, et al., 1997). In addition, outbreaks have occurred in closed environments, such as nursing homes (Thigpen, et al., 2007; Hohenboken, Anderson, & Kaplan, 1994; Jordan, Richards, Burton, Thigpen, & Van Beneden, 2007; Harkness, Bentley, Mottley, & Lee, 1992; Ruben, Norden, Heisler, & Korica, 1984) and hospitals (DiPersio, et al., 1996). Secondary cases of StrepTSS are unusual, but transmission to family members (DiPersio, et al., 1996; Gamba, et al., 1997) or health care workers (DiPersio, et al., 1996; Valenzuela, Hooton, Kaplan, & Schlievert, 1991) has been well documented by demonstrating identical pulsed-field gel electrophoresis patterns from cross-infecting strains. Although many of the initial reports described StrepTSS in adults, children are also affected (Cockerill, et al., 1997; Wheeler, Roe, Kaplan, Schlievert, & Todd, 1991; Kiska, et al., 1997; Givner, Abramson, & Wasilauskas, 1991; Brogan, Nizet, Waldhausen, Rubens, & Clarke, 1995; Stockmann, et al., 2012). In 2010, the incidence of invasive infection in children in Utah reached 14 cases/100,000 population (Stockmann, et al., 2012). Thus, persons of all ages can be afflicted and, although some have underlying medical conditions such as diabetes and alcoholism (Francis & Warren, 1988; Wheeler, Roe, Kaplan, Schlievert, & Todd, 1991; Schwartz, Facklam, & Breiman, 1990; Barnham, 1989; Braunstein, 1991; Holm, Norrby, Bergholm, & Norgren, 1992), many have no predisposing medical condition and are not immunocompromised. This contrasts sharply with reviews of S. pyogenes bacteremia from several decades ago (Francis & Warren, 1988; Barnham, 1989; Braunstein, 1991), which found that the disease occurred primarily among the very young, the very old, or patients with predisposing conditions, such as cancer, renal failure, leukemia, severe burns, or iatrogenic immunosuppression.

Table 1.

Table 1.

Case Definition for the Streptococcal Toxic Shock Syndrome*

The common portals of entry for streptococci include the vagina, pharynx, mucosa, and skin (Stevens, et al., 1989). In other cases, surgical procedures such as suction lipectomy, hysterectomy, vaginal delivery, bunionectomy, reduction mammoplasty, hernia repair, bone pinning, and vasectomy have provided portals for entry. StrepTSS rarely occurs secondary to streptococcal pharyngitis (Herold, 1990; Bradley, Schlievert, & Peterson, 1991; Chapnick, et al., 1992), while viral infections, such as varicella and influenza, have provided portals of entry in other cases (Stevens, et al., 1989; Kiska, et al., 1997; Herold, 1990; Lesko, O'Brien, Schwartz, Vezina, & Mitchell, 2001).

Additional factors increase the risk of invasive S. pyogenes infections. Three studies have demonstrated that a high or increasing prevalence of M-types 1 or 3 strains among throat isolates may signal an increased incidence of StrepTSS in a community (Kiska, et al., 1997; Holm, Norrby, Bergholm, & Norgren, 1992; Sellers, Woods, Morris, & Saffle, 1996). The use of NSAIDs for pain associated with muscle strain, trauma, chickenpox or childbirth may mask the early signs and symptoms of streptococcal infection or possibly predispose patients to more severe infection, such as necrotizing fasciitis or StrepTSS (Stevens, et al., 1989; Stockmann, et al., 2012; Stevens, 1995a; Barnham, 1997).

Pathogenesis of StrepTSS

Colonization and Translocation

The entry of S. pyogenes into the bloodstream and deeper tissues may occur as a result of a breach of an epithelial barrier, or the organism itself may penetrate intact membranes, such as the pharyngeal mucosa. Although bacteremia rarely follows streptococcal pharyngitis, transient bacteremia likely occurs in ~50% of patients who develop invasive infections without a portal of entry. The organism adeptly avoids destruction by the host’s immune system largely because of the anti-phagocytic properties of the M protein (Lancefield, 1933). Adherence of S. pyogenes to pharyngeal mucosal cells is a prerequisite to colonization or infection, and has been related to surface structures, such as lipoteichoic acid and fibronectin-binding proteins. Penetration or translocation of the organism through respiratory epithelial cells has been demonstrated for M-type 1 S. pyogenes. Some have suggested that M-1 strains possessing an invasin (inv+) gene penetrate more efficiently (LaPenta, Rubens, Chi, & Cleary, 1994). If penetration of mucosal barriers occurs readily with these strains, it generally does not result in clinically detectable bacteremia in the vast majority of cases, since the incidence of invasive infection remains generally very low (~3.5 cases/100,000 population) (O'Brien, et al., 2002). Thus, the clearance of S. pyogenes by the human immune system must be highly efficient.

Recent studies have suggested that, following the colonization of mucosa or skin, SpeB attenuates the local host response and limits bacterial exotoxin functionality through its proteolytic activity. Later in the course of the disease, production of SpeB is curtailed by in vivo selection of strains that harbor mutations in covS (control of virulence), the sensory component of a key 2-component regulatory system, CovRS (Aziz, et al., 2004; Kansal, et al., 2010). This results in a stable phase-shift to a SpeB negative phenotype, which allows these particular strains to bind plasminogen, evade the immune system, and switch to an invasive phenotype (Walker, et al., 2007). In addition, streptolysin O (SLO) likely disrupts the local tissue inflammatory response in much the same way as the related toxin, perfringolysin O from Clostridium perfringens, inhibits leukocytosis in gas gangrene (Stevens, Tweten, Awad, Rood, & Bryant, 1997b).

S. pyogenes produces many surface-bound and extracellular virulence factors that contribute to pathogenesis in unique ways (reviewed in (Stevens & Kaplan, 2000)). Temporal and environmental control of virulence factor gene expression depends on multiple complex and interrelated stand-alone or two-component regulatory systems. The most intensively studied of these include Mga (multiple virulence gene regulator of group A streptococcus) (McIver, 2009), Mry (M protein RNA yield) (Perez-Casal & Caparon, 1991), and the two-component regulator CsrRS (capsule synthesis regulator, Response and Sensor components (Levin & Wessels, 1998)) which is alternately known as CovRS (control of virulence (Federle, McIver, & Scott, 1999)). The regulator of proteinase B (RopB) has also been shown to have multiple polymorphisms that control the virulence of S. pyogenes (Carroll, et al., 2011).

The Role of Antecedent Soft-Tissue Injury

A critical role for antecedent soft-tissue injury has been well established for some bacterial infections, such as clostridial myonecrosis, where a deep, penetrating injury interrupts the blood supply and directly introduces organisms (or spores) into devitalized tissues. Though the rate at which S. pyogenes myonecrosis progresses is comparable to that of clostridial gangrene (inches per hour), the types of predisposing injuries are distinctly different. With S. pyogenes infection, a minor muscle strain, sprain, or bruise is often the rule (Adams, et al., 1985; Stevens, et al., 1989). For instance, in our initial report of 20 cases of invasive streptococcal infection, one had a superficial bruise to the hand, and the portal of entry was entirely unknown in the other 7 patients (Stevens, et al., 1989). Thus, 8 of 20 patients (40%) had no known portal of entry, and overall mortality was 30% (Stevens, et al., 1989). Similarly, Adams et al. documented 21 cases of life-threatening S. pyogenes infection, 19 of which lacked an obvious portal of entry and 18 (85.7%) died (Adams, et al., 1985). Finally, a recent case-controlled study found that non-penetrating trauma was significantly associated with S. pyogenes necrotizing fasciitis (Nuwayhid, Aronoff, & Mulla, 2007). In these “no portal” cryptic infections, the correct diagnosis is often delayed until after shock and organ failure manifest (Bisno & Stevens, 1996), which often causes mortality to exceed 70% (Adams, et al., 1985). Survivors undergo emergent amputation or extensive surgical debridement and prolonged hospitalization (Bisno & Stevens, 1996; Stevens, et al., 1989; Schurr, Engelhardt, & Helgerson, 1998). Such findings have prompted several authors to conclude that non-penetrating muscle injury may be a prerequisite for S. pyogenes necrotizing fasciitis or myonecrosis (Adams, et al., 1985; Nuwayhid, Aronoff, & Mulla, 2007).

Our initial studies of this process demonstrated that injury of cultured human skeletal muscle cells increased the binding of S. pyogenes (Bryant, Bayer, Huntington, & Stevens, 2006). While S. pyogenes bind host proteins such as fibronectin, collagen, and laminin (reviewed in (Courtney, Hasty, & Dale, 2002)), multiple lines of evidence suggest that these did not contribute to the initial S. pyogenes/skeletal muscle interaction within the first 24–48 hrs after injury (reviewed in (Bryant, Bayer, Aldape, & Stevens, 2015)), but could contribute at later times in the disease course. Instead, our findings demonstrated that the ubiquitous intermediate filament protein, vimentin, was the principal S. pyogenes adhesin on injured muscle cells (Bryant, Bayer, Huntington, & Stevens, 2006). Though classically an intracellular cytoskeletal protein (reviewed in (Fuchs & Weber, 1994)), our studies clearly demonstrated that injured muscle cells in culture also display vimentin on their surface (Bryant, Bayer, Huntington, & Stevens, 2006)—adding to other reports that describe a cell-surface form of vimentin in platelets, endothelial cells, and lymphocytes (Xu, et al., 2004; Podor, et al., 2002; Boilard, Bourgoin, Bernatchez, & Surette, 2003). Further, S. pyogenes, but not S. aureus, bound soluble vimentin in vitro (authors’ unpublished data) and was associated with vimentin-positive necrotic muscle in a human case of S. pyogenes NF (Bryant, Bayer, Huntington, & Stevens, 2006).

In a murine model of injury-associated cryptogenic S. pyogenes infection (Hamilton, Bayer, Stevens, Lieber, & Bryant, 2008), vimentin expression was significantly increased by 6 hrs, peaked at 48 hrs, and remained elevated over 72 hrs after injury (Hamilton, Bayer, Stevens, Lieber, & Bryant, 2008). Intravenous infusion of M-type 3 S. pyogenes at the peak of vimentin expression resulted in the homing of the organism to the injured site (Hamilton S. M., Bayer, Stevens, Lieber, & Bryant, 2008). Since regenerating muscle cell precursors (satellite cells), but not mature healthy myofibers, express vimentin (Vaittinen, et al., 2001), these results provided the first molecular mechanism to explain the development of severe S. pyogenes soft tissue infections precisely at sites of prior minor muscle trauma.

Mechanisms of Shock and Organ Failure: Cytokine Induction

Within the deeper tissues and bloodstream, the induction of cytokine synthesis plays a critically important role in the production of shock and organ failure. Like the staphylococcal enterotoxins and TSST-1, multiple S. pyogenes exotoxins (such as streptococcal pyrogenic exotoxins [Spe] A, B and C, MF, and SSA (Norrby-Teglund, et al., 1998)) and potentially M protein fragments (Kotb, et al., 1993) act as superantigens to stimulate T-cell responses, through their ability to bind to both the MHC class II complex of antigen-presenting cells and specific Vβ regions of the T-cell receptor (Mollick & Rich, 1991). The net effect is a watershed induction of both monocyte- and lymphocyte-derived cytokines (tumor necrosis factor [TNF] -α, interleukin [IL]-1β, IL-6 and TNF-β, IL-2, interferon-γ, respectively) (Norrby-Teglund, et al., 1998; Kotb, et al., 1993; Hackett & Stevens, 1993; Fast, Schlievert, & Nelson, 1989; Norrby-Teglund, Newton, Kotb, Holm, & Norgren, 1994a; Norrby-Teglund, Norgren, Holm, Andersson, & Andersson, 1994b). Superantigens drive the clonal proliferation of specific Vβ T-cells, in part through induction of IL-2. Thus, it would be expected to find the expansion of superantigen-specific Vβ T-cell clones in an infected individual. However, studies in patients with StrepTSS demonstrate depletion, rather than expansion, of superantigen-specific T-cell subsets (Watanabe-Ohnishi, et al., 1995). This enigma remains to be reconciled.

Among the 4 alleles of SpeA, alleles 2 and 3 are most common and have the highest affinity for MHC class II on antigen presenting cells (Kline & Collins, 1996). Some clinical studies have suggested that variations in human leukocyte antigen (HLA) haplotype may result in a predisposition to worse outcomes in some patients with StrepTSS (Kotb, et al., 2002). Finally, a lack of anti-SpeA antibodies is a predisposing factor for development of StrepTSS (Mascini, et al., 2000).

Other streptococcal virulence factors can also induce mononuclear cell pro-inflammatory cytokine production. Specifically, SpeB releases active IL-1β from preformed intracellular pools (Kapur, Majesky, Li, Black, & Musser, 1993). SLO also stimulates mononuclear cells to produce TNF-α and IL-1β and, in the presence of SpeA, has synergistic effects on IL-1β production (Hackett & Stevens, 1992). Heat-killed S. pyogenes, as well as isolated peptidoglycan and lipoteichoic acid, are also potent inducers of TNF-α and IL-1β (Hackett, Ferretti, & Stevens, 1994; Müller-Alouf, et al., 1994).

Recent evidence suggests that cardiomyocyte-derived cytokines are produced following direct S. pyogenes stimulation and after exposure to S. pyogenes-activated inflammatory cells (Li, et al., 2011). In addition, viable S. pyogenes induced the production of cardiomyocyte-derived stimulator/s that boosts macrophage production of matrix metalloproteinase-9, pro-inflammatory cytokines (IL-1β, IL-6) and cardiodepressant factors (iNOS) (Li, Bryant, Parimon, & Stevens, 2012). These locally produced, cardiomyocyte-derived cytokines (termed “cardiokines”) may mediate cardiac contractile dysfunction observed in some patients with StrepTSS who develop a unique and reversible form of cardiomyopathy that is characterized by global hypokinesia and reduced cardiac index (Stevens, Shelly, Stiller, Villasenor-Sierra, & Bryant, 2008).

Other non-cytokine-mediated mechanisms of shock may also play a role in this process. For example, SpeB has been shown to release bradykinin from a high-molecular-weight kininogen (Herwald, Collin, Müller-Esterl, & Björck, 1996). Bradykinin is a potent vasodilator of systemic and pulmonary vasculature and could be at least partially responsible for the early hypotension observed in StrepTSS (Stevens, et al., 1996). Finally, recent studies demonstrated that SLO, through its ability to form membrane pores, is the major S. pyogenes exotoxin responsible for direct cardiomyocyte contractile dysfunction (Bolz, et al., 2015). Within minutes of exposure, SLO disrupted the normal contraction response of isolated murine cardiac cells to electrical pacing. Later, SLO induced spontaneous, non-paced contractions that were characterized by hyper-augmented contractile force. These effects were mediated by an influx of calcium through SLO-induced membrane pores. Upon removal of SLO, normal electrical pacing resumed, which suggests that membrane lesions were repaired and normal intracellular calcium levels were restored. These observations are consistent with the clinical observation that cardiomyopathy is a reversible condition in patients who survive StrepTSS (Stevens, Shelly, Stiller, Villasenor-Sierra, & Bryant, 2008).

There are likely many streptococcal and host factors that contribute to the shock and organ failure characteristic of StrepTSS. Experimental evidence suggests that TNF plays a central role in this process. Specifically, high levels of TNFα were observed in a baboon model of S. pyogenes bacteremia when profound hypotension was manifest (Stevens, et al., 1996); administration of a neutralizing anti-TNFα antibody restored normal blood pressure and reduced mortality by 50% (Stevens, et al., 1996). Diffuse capillary leaking also contributes to hypotension in StrepTSS and is likely attributable to cytokines and other mediators, though it may also be related to circulating M protein-fibrinogen complexes (Herwald, et al., 2004).

NSAIDs and Severe S. pyogenes Infection

In 1985, a report by Brun-Buisson and colleagues suggested a possible association between NSAID use and development of severe S. pyogenes necrotizing fasciitis (Brun-Buisson, et al., 1985). These authors identified 6 previously healthy individuals with no underlying conditions in whom NF either developed spontaneously (2/6) or following minor non-penetrating trauma (4/6). All had received at least one NSAID in the 4–10 days prior to hospitalization. One patient died; survivors underwent multiple surgeries and prolonged hospitalization. The authors concluded that NSAIDs contributed to the development and/or extension of the disease process. Following this report, other case series and retrospective studies appeared in the literature concerning this possible association (reviewed in (Bryant, Bayer, Aldape, & Stevens, 2015)).

In 1995, Stevens proposed that NSAIDs, through their ability to interrupt the negative feedback loop that limits production of TNFα, may predispose individuals to more severe S. pyogenes infections (Stevens, 1995a). Others argued that NSAIDs merely mask the signs and symptoms of developing infections, such that diagnosis and antibiotic treatment are delayed. In an effort to examine a potential cause/effect relationship, Aronoff and Bloch reviewed the available published reports through 2002 (Aronoff & Bloch, 2003) and concluded that because most studies lacked appropriate control groups or had other significant limitations, the data did not support a causal role for NSAIDs in the development of S. pyogenes NF or to a worsening of the infection once established. However, their work suggested that further investigations were warranted.

Since then, additional reports have emerged that lend support to an association between NSAIDs and S. pyogenes, including one from the United Kingdom that demonstrated that NSAID use was independently associated with a 3-fold increased risk for development of StrepTSS (Lamagni, et al., 2008), a second multicentre prospective study in France (Dubos, Hue, Grandbastien, Catteau, & Martinot, 2008), and a nested case-controlled study in the UK by Mikaeloff et al. (Mikaeloff, Kezouh, & Suissa, 2008) that each found that NSAID use was independently associated with severe secondary complications in children with varicella infections.

Experimental evidence that directly addresses this issue is limited. Guibal et al. challenged rabbits with a combination of viable S. pyogenes plus S. aureus alpha toxin and treated them immediately thereafter with diclofenac (Guibal, et al., 1998). This relatively COX-2-selective NSAID (Süleyman, Demircan, & Karagöz, 2007) limited the extent of necrotizing fasciitis and lowered the bacterial numbers in the tissues (Guibal, et al., 1998). The authors concluded that any NSAID-induced increase in severity of NF in humans is likely due to the therapeutic delay induced by the misleading clinical effects of the NSAID, and not to any inhibition of antibacterial defenses (Guibal, et al., 1998). Goldmann et al. showed that a highly COX-2-selective NSAID (NS-398), delivered 2 hr before and again 2 hr after intravenous S. pyogenes challenge, significantly but transiently delayed the mortality of mice (Goldmann, et al., 2010). Our studies of NSAIDs in experimental S. pyogenes myonecrosis demonstrated that a highly COX-2-selective NSAID (SC-236), given 1 hr after IM challenge and continuing every 12 hr for 3 days, showed no benefit in either survival or disease severity (Hamilton, Bayer, Stevens, & Bryant, 2014). Together, these limited data suggest that COX-2-selective NSAIDs provide little to no benefit in S. pyogenes infections.

In striking contrast to the results with highly COX-selective NSAIDs, our studies of experimental S. pyogenes myonecrosis (Hamilton, Bayer, Stevens, & Bryant, 2014) and those of Weng et al. (Weng, Chen, Toh, & Tang, 2011) clearly demonstrate that different non-selective NSAIDs each accelerated the disease course, worsened outcomes, and reduced antibiotic efficacy. Of note, one non-selective NSAID, ketorolac tromethamine, also significantly augmented S. pyogenes infection of experimentally injured muscles in the above-mentioned murine model of cryptogenic S. pyogenes infection (Hamilton, Bayer, Stevens, Lieber, & Bryant, 2008).

As a result, a preponderance of clinical evidence and some experimental data suggest that non-selective NSAIDs do more than merely mask the signs and symptoms of developing S. pyogenes infection.

Clinical Manifestations and Stages of Infection

The first phase of StrepTSS begins with an influenza-like prodrome that is characterized by fever, chills, myalgias, nausea, vomiting, and diarrhea that precedes hypotension by 24–48 hours (Stevens, et al., 1989). Confusion and/or combativeness is present in 55% of patients. Where there is a defined portal of entry, early cutaneous evidence of streptococcal infection may be present. In contrast, in patients without a portal of entry (~50% of cases) and who subsequently develop necrotizing infection, increasingly severe pain is the most common symptom. Such pain is so severe as to prompt patients to seek medical care and, interestingly, often precedes cutaneous evidence of localized infection by 12-24 hours (Stevens, et al., 1989). In both children (Kiska, et al., 1997) and adults (Stevens, et al., 1989), the soft tissues are the most common primary site of infection. In the remaining cases, pneumonia, meningitis, endophthalmitis, peritonitis, myocarditis, joint infection, and intrauterine infection have been described.

Phase 2 of StrepTSS is characterized by tachycardia, tachypnea, increasing pain and persistent fever (Stevens, 1995b). In children with varicella infection, toxicity or persistence of fever longer than 4 days should also prompt careful evaluation. Many patients are seen in emergency departments at this stage and frequently sent home on one or two occasions with mistaken diagnoses, such as deep vein thrombophlebitis, muscle strain, viral gastroenteritis, dehydration, or sprained ankle (Bisno, Cockerill, & Bermudez, 2000). High fever and excruciating pain, particularly in individuals with no risk factors for deep vein thrombosis, should arouse suspicion of a deep-seated infection. The laboratory tests described later are helpful, and CT and MRI may be useful to define the level of tissue involvement but are not specific.

In Phase 3 of StrepTSS, the sudden onset of shock and organ failure are manifested. Many patients are in florid shock at the time of admission or within hours thereafter. Clinical evidence of necrotizing fasciitis is frequently a late finding, often occurring after hypotension is present. The appearance of purple bullae and dusky-appearing skin is a bad prognostic sign and should prompt emergent surgical exploration. In modern cases, the progression of necrotizing fasciitis from red skin to purple bullae may occur within a 24-hour period, whereas that described by Meleney in 1924 took 7-10 days (Meleney, 1924). In addition, the rapidity with which shock and multi-organ failure can progress is impressive, and many patients die within 24-48 hours of hospitalization (Stevens, et al., 1989).

Laboratory tests should be performed in patients with aggressive soft tissue infections or patients with severe pain and fever who appear toxic. The serum creatinine measurement is particularly useful because renal impairment (creatinine level more than twice normal) is apparent even during phase 2, before hypotension is apparent. In addition, creatine phosphokinase levels in serum are markedly elevated in those with necrotizing fasciitis and myonecrosis. The white blood count is usually normal or modestly elevated at admission but with a profound left shift that includes myelocytes and metamyelocytes. Finally, serum albumin and calcium levels are usually low on admission and drop precipitously as a diffuse capillary leak syndrome develops. Thrombocytopenia does not develop until later in the course but is the earliest sign of disseminated coagulopathy. Profound metabolic acidosis develops early in phase 3, and serum bicarbonate, lactate, and blood gas pH determinations are crucial tests to follow therapeutic progress. Because the acute respiratory distress syndrome (ARDS) develops in 55% of patients with StrepTSS, pulse oximetry and, later, blood gas levels are necessary to evaluate the need for intubation and ventilation.

Management

Source Control

Prompt and aggressive surgical exploration and debridement of suspected deep-seated streptococcal infection are mandatory. Emergent surgical consultation should be sought in patients with extreme pain and fever or who are toxic. Surgical inspection provides samples for etiologic determination and allows assessment of the extent of necrosis. CT and MRI are helpful to locate the primary site of infection, but because S. pyogenes do not elaborate gas in the tissues or form frank abscesses, radiologist interpretations are frequently not definitive. Once necrosis is established, extensive debridement is necessary, since shock and organ failure continue to progress if devitalized tissue remains. While necrosis of the fascia may be present, it is important to recognize that global necrosis of muscle, skin, fascia and sub-cutaneous tissue is commonly present.

Fluid Resuscitation

Because of intractable hypotension and diffuse capillary leak, massive amounts of IV fluids (10 to 20 L/day) in an adult may be required. If several liters of crystalloid intravenous fluid challenge do not rapidly improve blood pressure (mean arterial pressure to more than 60 mm Hg) or tissue perfusion, then invasive monitoring or echocardiography is indicated. If despite adequate crystalloid administration, hypotension persists, the serum albumin concentration and hematocrit should be checked because capillary leak contributes to profoundly low albumin levels (< 2 g/dL) and because hemolysins produced by S. pyogenes can cause dramatic drops in circulating red cell mass. Thus, transfusion with packed red blood cells, with or without albumin, may be useful to improve blood pressure and preserve tissue perfusion.

Antimicrobial Treatment

Prompt antimicrobial therapy is mandatory, and empirical broad-spectrum coverage for septic shock should be initially instituted. Once the etiology of S. pyogenes is confirmed, high-dose penicillin and clindamycin should be given (Stevens, et al., 2014). This recommendation is based on the following: (1) all strains of S. pyogenes remain sensitive to penicillin; (2) resistance to clindamycin has only rarely been reported and erythromycin resistance among S. pyogenes is currently <5% in the United States, though some locales have reported higher rates; (3) clindamycin is more efficacious in experimental models of necrotizing fasciitis and myonecrosis; (4) penicillin-binding proteins are not expressed during stationary-phase growth of S. pyogenes, and thus penicillin is ineffective in severe deep infections in which large numbers of bacteria are present; (5) clindamycin suppresses S. pyogenes exotoxin and M protein production; (6) clindamycin has a much longer half-life and post-antibiotic effect; (7) no antagonistic effects between penicillin and clindamycin were found when used together in vitro at clinically relevant concentrations (Stevens, Madaras-Kelly, & Richards, 1998); and (8) clindamycin suppresses pro-inflammatory cytokine production by human mononuclear cells (Stevens, Bryant, & Hackett, 1995; Stevens, Hackett, & Bryant, 1997a). When combined, these facts have resulted in the current (2014) recommendation by the Infectious Disease Society of America to use clindamycin as the main antibiotic to treat invasive S. pyogenes infections (Stevens, et al., 2014); penicillin is included in this recommendation, largely due to the potential for clindamycin resistance.

Management in the Intensive Care Unit

In patients with persistent hypotension, monitoring of cardiac outputs, pulmonary artery occlusion pressure, and mean arterial pressure is important. Intubation and ventilator support are usually required because of the high incidence of ARDS (55%) in patients with StrepTSS. Vasopressors such as dopamine are used frequently, although no controlled trials have been performed in StrepTSS. In patients with intractable hypotension, high doses of dopamine, epinephrine, or phenylephrine have been used, but caution should be exercised in those with evidence of disseminated intravascular coagulation (DIC) and in particular in those with cold, cyanotic digits. Symmetrical gangrene involving all fingers and toes, the tip of the nose, and the breast areola has been described. In addition, amputation of 1–4 extremities has been observed (Stevens & Bryant, 2015). In these cases, both excessive vasopressors and DIC are likely to contribute to symmetrical gangrene.

Dialysis and Hemoperfusion

Dialysis and/or hemoperfusion may be necessary because more than 50% of patients develop acute renal failure. Both techniques may also non-specifically reduce the concentrations of circulating toxins. A Swedish study of severe S. pyogenes infection suggested that plasma exchange might be a beneficial adjunct to treatment of patients who fail conventional treatment (Stegmayr, et al., 1992). Finally, a polystyrene superantigen absorbing device (SAAD) was developed in Japan and was shown to be highly efficacious in absorbing both streptococcal pyrogenic exotoxin A and staphylococcal toxic shock syndrome toxin 1 (TSST-1) from plasma and, when used extra-corporeally in animals infused with TSST-1 and lipopolysaccharide (LPS), mortality was reduced from 100% to 50% (Miwa, Fukuyama, Ida, Igarashi, & Uchiyama, 2003).

Intravenous Immune Globulin

The rationale for the use of intravenous immune globulin (IVIG) in the treatment of StrepTSS is based on the data implicating extracellular toxins as mediators of shock and organ failure. This concept was demonstrated as early as 1924, when George and Gladys Dick showed that convalescent sera from scarlet fever patients neutralized scarlatina toxins in vitro and, when passively administered, attenuated the course of severe scarlet fever in humans (Dick & Dick, 1925). Anti-scarlatina toxin horse serum became commercially available in the United States shortly thereafter, but because of the new widespread availability of penicillin and the decline in the severity of scarlet fever, it was never used.

Several reports have described the successful use of IVIG in patients with StrepTSS (Lamothe, D'Amico, Ghosn, Tremblay, Braidy, & Patenaude, 1995; Barry, Hudgins, Donta, & Pesanti, 1992; Stevens, 1998). The largest treatment study (15 patients) showed a significant reduction in mortality with IVIG, as compared with matched historical controls (Kaul, et al., 1999). However, the mortality rate of 70% in the control group was among the highest ever reported, whereas mortality in the IVIG group (30%) was similar to that of some series that did not use IVIG (Stevens, et al., 1989). A double-blind clinical trial was undertaken in northern Europe that compared IVIG with albumin in patients with StrepTSS. All patients received clindamycin. The mortality rate in the IVIG group was 16%, whereas that in the albumin group was 32% (Darenberg, et al., 2003). Unfortunately, the study was stopped because of low enrollment, and only seven or eight patients with proven S. pyogenes infections were in each group. Thus, the differences were not significant. A retrospective study in patients with StrepTSS has also shown no benefit of IVIG on mortality (Beaulieu, McGeer, & Muller, 2008). It is hoped that further double-blind studies with sufficient numbers of cases will resolve the continuing dilemma regarding the potential efficacy of IVIG (Stevens, 2003). It is clear that if IVIG were to be used, it should be given early and probably more than one dose should be given, because batches of IVIG have variable neutralizing activity against streptococcal exotoxins (Norrby-Teglund, et al., 1998; Norrby-Teglund, et al., 1996).

Hyperbaric Oxygen

There have been no comparative trials describing the efficacy of hyperbaric oxygen treatment in StrepTSS, although some state that such treatment reduces mortality and the need for further debridements (Riseman, et al., 1990). Certainly, use of this modality should not delay (or be used in preference to) surgical debridement, when the latter is indicated.

Bacteremia

Group A streptococcal bacteremia has been relatively uncommon in the antibiotic era (Weinstein, Reller, Murphy, & Lichtenstein, 1983). Before the mid-1980s, bacteremia predominantly occurred at the extremes of life and was usually community-acquired. Occasional cases were seen in young and middle-aged adults, and were associated with surgical wound infections and endometritis.

During the past decade, however, there has been an increase in the number of reported cases of S. pyogenes bacteremia, which reflects the changing epidemiology and clinical patterns of invasive streptococcal infection, as noted earlier. Many of the patients were previously healthy adults between the ages of 20 and 50 years. There has also been an apparent increase in cases associated with parenteral injection of illicit drugs (Stevens, et al., 1989; Braunstein, 1991), as well as nosocomial outbreaks in nursing homes (Thigpen, et al., 2007; Hohenboken, Anderson, & Kaplan, 1994; Jordan, Richards, Burton, Thigpen, & Van Beneden, 2007; Harkness, Bentley, Mottley, & Lee, 1992; Ruben, Norden, Heisler, & Korica, 1984).

Bacteremia in children may emanate from an upper respiratory infection, but it is more commonly associated with cutaneous foci, including burns and varicella (Valenzuela, Hooton, Kaplan, & Schlievert, 1991). Older patients with streptococcal bacteremia present with a variety of chronic illnesses; their relation to the bacteremia is often unclear. Diabetes mellitus and peripheral vascular disease do appear to be predisposing factors in older adults, and, as in children, the portal of entry is usually the skin. Malignancy and immunosuppression are risk factors in both age groups (Stevens, 1992; Duma, Weinberg, Medrek, & Kunz, 1969). Although S. pyogenes bacteremia may be transient and relatively benign at times (Dan, Maximova, Siegman-Igra, Gutman, & Rotmensch, 1990), it is more often fulminant. The onset is abrupt, with chills, high fever, and prostration. Rarely, patients may present with acute abdominal pain (Dan, Maximova, Siegman-Igra, Gutman, & Rotmensch, 1990; Ispahani, Donald, & Aveline, 1988). Mortality in five modern series (Francis & Warren, 1988; Dan, Maximova, Siegman-Igra, Gutman, & Rotmensch, 1990; Ispahani, Donald, & Aveline, 1988; Bucher, et al., 1992; Burkert & Watanakunakorn, 1992) has ranged from 27% to 38%.

Other Streptococcal Infections

Infection Associated with Pregnancy

S. pyogenes infection associated with pregnancy (also referred to as puerperal sepsis, childbed fever, or postpartum infection) was first described by Semmelweis in the 1850s and remains an important cause of maternal and infant mortality worldwide (reviewed in (Hamilton, Stevens, & Bryant, 2013)). Unlike in Semmelweis’ era, only 14% of modern-day S. pyogenes postpartum infections in developed countries are nosocomially acquired. Rather, the majority occur after hospital discharge. Nearly 20 percent of cases of S. pyogenes infection occur during the third trimester, prior to the onset of labor or rupture of membranes (Hamilton, Stevens, & Bryant, 2013).

Patients with S. pyogenes puerperal sepsis typically present with fever, abdominal pain, and hypotension without tachycardia or leukocytosis. About 220 cases occur annually in the United States, for an overall rate of 6 cases per 100,000 live births (Chuang, Van Beneden, Beall, & Schuchat, 2002). In 2002, the case fatality rate was about 3.5 percent. Maternal mortality is highest when infection develops within four days of delivery or during the late third trimester (Hamilton, Stevens, & Bryant, 2013).

Meningitis and Endocarditis

Although endocarditis caused by S. pyogenes was relatively common in the pre-antibiotic era, it is now rarely seen (Ramirez, Naragi, & McCulley, 1984; Baddour, 1998). Meningitis caused by S. pyogenes usually follows upper respiratory infection, including sinusitis or otitis (van de Beek, et al., 2002), or neurosurgical conditions (Sommer, et al., 1999). It is clinically indistinguishable from other forms of acute pyogenic meningeal infection (Murphy, 1983).

Pneumonia

Pneumonia caused by S. pyogenes is frequently associated with antecedent viral infections such as influenza, measles, or varicella, or with chronic pulmonary disease. Numerous epidemics have been described in military recruit populations (Basiliere, Bistrong, & Spence, 1968; Crum, et al., 2005). An increased number of cases has been reported over the past few years in association with the resurgence of invasive streptococcal infections. In one-third or fewer of the cases, there was a history of preceding streptococcal upper respiratory infection. The onset is typically abrupt and the disease is characterized by chills, fever, dyspnea, cough productive of blood-streaked sputum, pleuritic chest pain, and, in more severe cases, cyanosis. The pulmonary picture is that of bronchopneumonia, with consolidation being uncommon. Empyema develops in 30–40% of cases, tends to appear early in the disease, and typically consists of copious amounts of thin serosanguinus fluid. Bacteremia occurs in 10-15% of cases. Complications include mediastinitis, pericarditis, pneumothorax, and bronchiectasis, and the clinical course of the disease is often prolonged. Mortality has generally been low with penicillin therapy and adequate drainage of empyema, which perhaps reflects its occurrence in healthy military recruits. However, in a recent Canadian report of 222 cases of community-acquired pneumonia among adults (with a median age of 56 years), the case-fatality rate was 38% (Muller, et al., 2003). Interestingly, a recent review of the 1918 pandemic of influenza has demonstrated that the major cause of death was secondary bacterial pneumonia (Morens, Taubenberger, & Fauci, 2008). While S. pneumoniae was the most common etiologic agent, S. pyogenes was second, followed by S. aureus. Among patients with pneumonia with empyema, S. pyogenes was first. Investigators have demonstrated in a mouse model that a non-lethal influenza infection greatly enhanced the severity and mortality of secondary respiratory infection with S. pyogenes (Okamoto, et al., 2003).

Prophylaxis for, and Risk of, Secondary StrepTSS

StrepTSS is most commonly community-acquired and sporadic in nature, yet clusters of invasive cases have been described in nursing homes (Thigpen, et al., 2007; Hohenboken, Anderson, & Kaplan, 1994; Jordan, Richards, Burton, Thigpen, & Van Beneden, 2007; Harkness, Bentley, Mottley, & Lee, 1992; Ruben, Norden, Heisler, & Korica, 1984), families (DiPersio, et al., 1996; Gamba, et al., 1997), and hospital workers (Valenzuela, Hooton, Kaplan, & Schlievert, 1991; Kakis, et al., 2002). In San Francisco, 23 hospital workers became colonized or infected with S. pyogenes as a result of contact from a single case of StrepTSS (Kakis, et al., 2002). This example, as well as many historical studies in schools, military posts, and nursing homes, has taught us that S. pyogenes is highly contagious. Fortunately, mere contact or colonization is usually not sufficient to cause a secondary case of invasive S. pyogenes infection. Epidemiologic studies by the Centers for Disease Control and Prevention found one secondary case of invasive infection among more than 1500 contacts (Prevention of Invasive Group A Streptococcal Infections Workshop Participants, 2002). This would extrapolate to 66/100,000 population/year for secondary cases (Robinson, et al., 2003). As noted, the current incidence of primary cases of invasive S. pyogenes infections in the United States is 3.5/100,000 population/year. Thus, the risk to contacts is roughly 20 times greater than that for the general population, but still remains very low. Given the relative infrequency of these infections and the lack of a clearly effective chemoprophylactic regimen, routine screening for and prophylaxis against streptococcal infection are not recommended for household contacts of index patients (Prevention of Invasive Group A Streptococcal Infections Workshop Participants, 2002). In deciding who should receive prophylaxis, the clinician needs to consider the duration and intimacy of contact and underlying host factors of individual contacts. Specifically, contacts with open wounds, who have had recent surgery or childbirth, who have concurrent viral infections such as varicella or influenza, or those with immunodeficiency diseases should receive prophylaxis. In a multicenter study of adults aged 18–45 years, human immunodeficiency virus infection and injecting drug use were independently associated with an increased risk of invasive S. pyogenes disease. In those aged 45 years of age or older, diabetes, cardiac disease, cancer, and corticosteroid use were significant risk factors (Factor, et al., 2003). Moreover, persons aged 65 years or older are at an increased risk of mortality, should they contract invasive disease. Thus, it may be prudent to initiate prophylaxis in households with older adults or those with the above-mentioned risk factors.

As there is a present lack of firm data on which to base antimicrobial prophylaxis, it seems reasonable to choose those agents that have achieved highest rates of pharyngeal eradication in asymptomatic individuals; among these are penicillin, clindamycin, and azithromycin. Specific regimens have been published elsewhere (Prevention of Invasive Group A Streptococcal Infections Workshop Participants, 2002).

References

  • Adams E. M., Gudmundsson S., Yocum D. E., Haselby R. C., Craig W. A., Sundstrom W. R. Streptococcal myositis. Archives of Internal Medicine. 1985;145(6):1020–1023. [PubMed: 3890787]
  • Aronoff D. M., Bloch K. C. Assessing the relationship between the use of nonsteroidal antiinflammatory drugs and necrotizing fasciitis caused by group A streptococcus. Medicine (Baltimore). 2003;82(4):225–235. [PubMed: 12861100]
  • Aziz R. K., Pabst M. J., Jeng A., Kansal R., Low D. E., Nizet V., et al. Invasive M1T1 group A Streptococcus undergoes a phase-shift in vivo to prevent proteolytic degradation of multiple virulence factors by SpeB. Molecular Microbiology. 2004;51(1):123–134. [PubMed: 14651616]
  • Baddour L. M. Infective endocarditis caused by beta-hemolytic streptococci. Clinical Infectious Diseases. 1998;26(1):66–71. [PubMed: 9455511]
  • Barnham M. Invasive streptococcal infections in the era before the acquired immune deficiency syndrome: A 10 years' compilation of patients with streptococcal bacteraemia in North Yorkshire. The Journal of Infection. 1989;18(3):231–248. [PubMed: 2663996]
  • Barnham M. Nonsteroidal antiinflammatory drugs: concurrent or causative drugs in serious infection? Clinical Infectious Diseases. 1997;25(5):1272–1273. [PubMed: 9402413]
  • Barry W., Hudgins L., Donta S. T., Pesanti E. L. Intravenous immunoglobulin therapy for toxic shock syndrome. JAMA. 1992;267(24):3315–3316. [PubMed: 1597914]
  • Basiliere J. L., Bistrong H. W., Spence W. F. Streptococcal pneumonia. Recent outbreaks in military recruit populations. The American Journal of Medicine. 1968;44(4):580–589. [PubMed: 5642716]
  • Beaulieu, A., McGeer, A., & Muller, M. P. (2008). Intravenous immunoglobulin for group A streptococcal toxic shock syndrome: A reassessment of efficacy. The 48th Annual Interscience Conference on Antimicrobial Agents and Chemotherapy and the Infectious Diseases Society of America 46th Annual Meeting. Washington, DC: The American Society for Microbiology.
  • Bisno A. L., Stevens D. L. Streptococcal infections in skin and soft tissues. The New England Journal of Medicine. 1996;334:240–245. [PubMed: 8532002]
  • Bisno A. L., Cockerill F. R., Bermudez C. T. The initial outpatient-physician encounter in group A streptococcal necrotizing fasciitis. Clinical Infectious Diseases. 2000;31(2):607–608. [PubMed: 10987730]
  • Boilard E., Bourgoin S. G., Bernatchez C., Surette M. E. Identification of an autoantigen on the surface of apoptotic human T cells as a new protein interacting with inflammatory group IIA phospholipase A2. Blood. 2003;102(8):2901–2909. [PubMed: 12829607]
  • Bolz D. D., Li Z., McIndoo E. R., Tweten R. K., Bryant A. E., Stevens D. L. Cardiac myocyte dysfunction induced by streptolysin O is membrane pore and calcium dependent. Shock. 2015;43(2):178–184. [PMC free article: PMC4297253] [PubMed: 25243426]
  • Bradley J. S., Schlievert P. M., Peterson B. M. Toxic shock-like syndrome: a complication of strep throat. The Pediatric Infectious Disease Journal. 1991;10(10):790. [PubMed: 1945587]
  • Braunstein H. Characteristics of group A streptococcal bacteremia in patients at the San Bernardino County Medical Center. Reviews of Infectious Diseases. 1991;13(1):8–11. [PubMed: 2017638]
  • Brogan T. V., Nizet V., Waldhausen J. H., Rubens C. E., Clarke W. R. Group A streptococcal necrotizing fasciitis complicating primary varicella: a series of fourteen patients. The Pediatric Infectious Disease Journal. 1995;14(7):588–594. [PubMed: 7567287]
  • Brun-Buisson C. J., Saada M., Trunet P., Rapin M., Roujeau J. C., Revuz J. Haemolytic streptococcal gangrene and non-steroidal anti-inflammatory drugs. British Medical Journal (Clinical Research Edition). 1985;290(6484):1786. [PMC free article: PMC1415937] [PubMed: 3924256]
  • Bryant A. E., Bayer C. R., Aldape M. J., Stevens D. L. The roles of injury and nonsteroidal anti-inflammatory drugs in the development and outcomes of severe group A streptococcal soft tissue infections. Current Opinion in Infectious Diseases. 2015;28(3):231–239. [PMC free article: PMC4775098] [PubMed: 25918957]
  • Bryant A. E., Bayer C. R., Chen R. Y., Guth P. H., Wallace R. J., Stevens D. L. Vascular dysfunction and ischemic destruction of tissue in Streptococcus pyogenes infection: the role of streptolysin O-induced platelet/neutrophil complexes. The Journal of Infectious Diseases. 2005;192(6):1014–1022. [PubMed: 16107954]
  • Bryant A. E., Bayer C. R., Huntington J. D., Stevens D. L. Group A streptococcal myonecrosis: increased vimentin expression after skeletal-muscle injury mediates the binding of Streptococcus pyogenes. The Journal of Infectious Diseases. 2006;193(12):1685–1692. [PubMed: 16703512]
  • Bucher A., Martin P. R., Høiby E. A., Halstensen A., Odegaard A., Hellum K. B., et al. Spectrum of disease in bacteraemic patients during a Streptococcus pyogenes serotype M-1 epidemic in Norway in 1988. European Journal of Clinical Microbiology & Infectious Diseases. 1992;11(5):416–426. [PubMed: 1425712]
  • Burkert T., Watanakunakorn C. Group A streptococcal bacteremia in a community teaching hospital--1980-1989. Clinical Infectious Diseases. 1992;14(1):29–37. [PubMed: 1571444]
  • Carroll R. K., Shelburne S. A., Olsen R. J., Suber B., Sahasrabhojane P., Kumaraswami M., et al. Naturally occurring single amino acid replacements in a regulatory protein alter streptococcal gene expression and virulence in mice. The Journal of Clinical Investigation. 2011;121(5):1956–1968. [PMC free article: PMC3083769] [PubMed: 21490401]
  • Chapnick E. K., Gradon D. J., Lutwick L. I., Kim J., Levi M., Kim M. H., et al. Streptococcal toxic shock syndrome due to noninvasive pharyngitis. Clinical Infectious Diseases. 1992;14(5):1074–1077. [PubMed: 1600009]
  • Chuang I., Van Beneden C., Beall B., Schuchat A. Population-based surveillance for postpartum invasive group a streptococcus infections, 1995-2000. Clinical Infectious Diseases. 2002;35(6):665–670. [PubMed: 12203162]
  • Cockerill F. R., MacDonald K. L., Thompson R. L., Roberson F., Kohner P. C., Besser-Wiek J., et al. An outbreak of invasive Group A streptococcal disease associated with high carriage rates of the invasive clone among school-aged children. JAMA. 1997;277(1):38–43. [PubMed: 8980208]
  • Courtney H. S., Hasty D. L., Dale J. B. Molecular mechanisms of adhesion, colonization, and invasion of group A streptococci. Annals of Medicine. 2002;34(2):77–87. [PubMed: 12108578]
  • Crum N. F., Russell K. L., Kaplan E. L., Wallace M. R., Wu J., Ashtari P., et al. Pneumonia outbreak associated with Group A Streptococcus species at a military training facility. Clinical Infectious Diseases. 2005;40(4):511–518. [PubMed: 15712072]
  • Dan M., Maximova S., Siegman-Igra Y., Gutman R., Rotmensch H. H. Varied presentations of sporadic group A streptococcal bacteremia: clinical experience and attempt at classification. Reviews of Infectious Diseases. 1990;12(3):537–542. [PubMed: 2193356]
  • Darenberg J., Ihendyane N., Sjölin J., Aufwerber E., Haidl S., Follin P., et al. Intravenous immunoglobulin G therapy in streptococcal toxic shock syndrome: a European randomized, double-blind, placebo-controlled trial. Clinical Infectious Diseases. 2003;37(3):333–340. [PubMed: 12884156]
  • Demers B., Simor A. E., Vellend H., Schlievert P. M., Byrne S., Jamieson F., et al. Severe invasive group A streptococcal infections in Ontario, Canada: 1987-1991. Clinical Infectious Diseases. 1993;16(6):792–800. [PubMed: 8329511]
  • Dick G. F., Dick G. H. Therapeutic results with concentrated scarlet fever antitoxin. JAMA. 1925;84(11):803–805.
  • DiPersio J. R., File T. M., Stevens D. L., Gardner W. G., Petropoulos G., Dinsa K. Spread of serious disease-producing M3 clones of group A streptococcus among family members and health care workers. Clinical Infectious Diseases. 1996;22(3):490–495. [PubMed: 8852968]
  • Dubos F., Hue V., Grandbastien B., Catteau B., Martinot A. Bacterial skin infections in children hospitalized with varicella: a possible negative impact of non-steroidal anti-inflammatory drugs? Acta Dermato-Venereologica. 2008;88(1):26–30. [PubMed: 18176746]
  • Duma R. J., Weinberg A. N., Medrek T. F., Kunz L. J. Streptococcal Infections. A Bacteriologic and Clinical Study of Streptococcal Bacteremia. Medicine. 1969;48(2):87–128.
  • Factor S. H., Levine O. S., Schwartz B., Harrison L. H., Farley M. M., McGeer A., et al. Invasive group A streptococcal disease: risk factors for adults. Emerging Infectious Diseases. 2003;9(8):970–977. [PMC free article: PMC3020599] [PubMed: 12967496]
  • Fast D. J., Schlievert P. M., Nelson R. D. Toxic shock syndrome-associated staphylococcal and streptococcal pyrogenic toxins are potent inducers of tumor necrosis factor production. Infection and Immunity. 1989;57(1):291–294. [PMC free article: PMC313091] [PubMed: 2642470]
  • Federle M. J., McIver K. S., Scott J. R. A response regulator that represses transcription of several virulence operons in the group A streptococcus. Journal of Bacteriology. 1999;181(12):3649–3657. [PMC free article: PMC93840] [PubMed: 10368137]
  • Francis J., Warren R. E. Streptococcus pyogenes bacteraemia in Cambridge - A review of 67 episodes. The Quarterly Journal of Medicine. 1988;68(256):603–613. [PubMed: 3076677]
  • Fuchs E., Weber K. Intermediate filaments: structure, dynamics, function, and disease. Annual Review of Biochemistry. 1994;63:345–382. [PubMed: 7979242]
  • Gamba M. A., Martinelli M., Schaad H. J., Streuli R. A., DiPersio J., Matter L., et al. Familial transmission of a serious disease-producing group A streptococcus clone: Case reports and review. Clinical Infectious Diseases. 1997;24(6):1118–1121. [PubMed: 9195067]
  • Givner L. B., Abramson J. S., Wasilauskas B. Apparent increase in the incidence of invasive group A beta-hemolytic streptococcal disease in children. The Journal of Pediatrics. 1991;118(3):341–346. [PubMed: 1999773]
  • Goldmann O., Hertzén E., Hecht A., Schmidt H., Lehne S., Norrby-Teglund A., et al. Inducible cyclooxygenase released prostaglandin E2 modulates the severity of infection caused by Streptococcus pyogenes. Journal of Immunology. 2010;185(4):2372–2381. [PubMed: 20644176]
  • Guibal F., Muffat-Joly M., Terris B., Garry L., Morel P., Carbon C. Effects of diclofenac on experimental streptococcal necrotizing fasciitis (NF) in rabbit. Archives of Dermatological Research. 1998;290(11):628–633. [PubMed: 9860284]
  • Hackett S. P., Stevens D. L. Streptococcal toxic shock syndrome: synthesis of tumor necrosis factor and interleukin-1 by monocytes stimulated with pyrogenic exotoxin A and streptolysin O. The Journal of Infectious Diseases. 1992;165(5):879–885. [PubMed: 1569337]
  • Hackett S. P., Stevens D. L. Superantigens associated with staphylococcal and streptococcal toxic shock syndromes are potent inducers of tumor necrosis factor beta synthesis. The Journal of Infectious Diseases. 1993;168(1):232–235. [PubMed: 8515117]
  • Hackett, S., Ferretti, J. J., & Stevens, D. L. (1994). Cytokine induction by viable group A streptococci: suppression by streptolysin O. The 94th Annual Meeting of the American Society for Microbiology (p. 73). Las Vegas: American Society for Microbiology.
  • Hamilton S. M., Bayer C. R., Stevens D. L., Bryant A. E. Effects of selective and nonselective nonsteroidal anti-inflammatory drugs on antibiotic efficacy of experimental group A streptococcal myonecrosis. The Journal of Infectious Diseases. 2014;209(9):1429–1435. [PMC free article: PMC3982845] [PubMed: 24218498]
  • Hamilton S. M., Bayer C. R., Stevens D. L., Lieber R. L., Bryant A. E. Muscle injury, vimentin expression, and nonsteroidal anti-inflammatory drugs predispose to cryptic group A streptococcal necrotizing infection. The Journal of Infectious Diseases. 2008;198(11):1692–1698. [PubMed: 18939933]
  • Hamilton S. M., Stevens D. L., Bryant A. E. Pregnancy-related group a streptococcal infections: temporal relationships between bacterial acquisition, infection onset, clinical findings, and outcome. Clinical Infectious Diseases. 2013;57(6):870–876. [PMC free article: PMC3749745] [PubMed: 23645851]
  • Harkness G. A., Bentley D. W., Mottley M., Lee J. Streptococcus pyogenes outbreak in a long-term care facility. American Journal of Infection Control. 1992;20(3):142–148. [PubMed: 1636935]
  • Herold A. H. Group A beta-hemolytic streptococcal toxic shock from a mild pharyngitis. The Journal of Family Practice. 1990;31(5):549–551. [PubMed: 2230679]
  • Herwald H., Collin M., Müller-Esterl W., Björck L. Streptococcal cysteine proteinase releases kinins: a novel virulence mechanism. The Journal of Experimental Medicine. 1996;184(2):665–673. [PMC free article: PMC2192748] [PubMed: 8760820]
  • Herwald H., Cramer H., Mörgelin M., Russell W., Sollenberg U., Norrby-Teglund A., et al. M protein, a classical bacterial virulence determinant, forms complexes with fibrinogen that induce vascular leakage. Cell. 2004;116(3):367–379. [PubMed: 15016372]
  • Hoge C. W., Schwartz B., Talkington D. F., Breiman R. F., MacNeill E. M., Englender S. J. The changing epidemiology of invasive group A streptococcal infections and the emergence of streptococcal toxic shock-like syndrome. JAMA. 1993;269(3):384–389. [PubMed: 8418346]
  • Hohenboken, J. J., Anderson, F., & Kaplan, E. L. (1994). Invasive group A streptococcal (GAS) serotype M-1 outbreak in a long-term care facility (LTCF) with mortality. Program & Abstracts of the Interscience Conference on Antimicrobial Agents and Chemotherapy (p. 192). Orlando: American Society for Microbiology.
  • Holm S. E., Norrby A., Bergholm A. M., Norgren M. Aspects of pathogenesis of serious group A streptococcal infections in Sweden, 1988-1989. The Journal of Infectious Diseases. 1992;166(1):31–37. [PubMed: 1607705]
  • Ispahani P., Donald F. E., Aveline A. J. Streptococcus pyogenes bacteremia: an old enemy subdued, but not defeated. The Journal of Infection. 1988;16(1):37–46. [PubMed: 3284952]
  • Jordan H. T., Richards C. L., Burton D. C., Thigpen M. C., Van Beneden C. A. roup a streptococcal disease in long-term care facilities: descriptive epidemiology and potential control measures. Clinical Infectious Diseases. 2007;45(6):742–752. [PubMed: 17712760]
  • Kakis A., Gibbs L., Equia J., Kimura J., Vogelei D., Troup N., et al. An outbreak of group A streptococcal infection among health care workers. Clinical Infectious Diseases. 2002;35(11):1353–1359. [PubMed: 12439798]
  • Kansal R. G., Datta V., Aziz R. K., Abdeltawab N. F., Rowe S., Kotb M. Dissection of the molecular basis for hypervirulence of an in vivo-selected phenotype of the widely disseminated M1T1 strain of group A Streptococcus bacteria. The Journal of Infectious Diseases. 2010;201(6):855–865. [PubMed: 20151844]
  • Kapur V., Majesky M. W., Li L. L., Black R. A., Musser J. M. Cleavage of Interleukin 1b (IL-1b) precursor to produce active IL-1b by a conserved extracellular cysteine protease from Streptococcus pyogenes. Proceedings of the National Academy of Sciences of the United States of America. 1993;90(16):7676–7680. [PMC free article: PMC47205] [PubMed: 7689226]
  • Kaul R., McGeer A., Norrby-Teglund A., Kotb M., Schwartz B., O'Rourke K., et al. Intravenous immunoglobulin therapy for streptococcal toxic shock syndrome - A comparative observational study. Clinical Infectious Diseases. 1999;28(4):800–807. [PubMed: 10825042]
  • Kiska D. L., Thiede B., Caracciolo J., Jordan M., Johnson D., Kaplan E. L., et al. Invasive group A streptococcal infections in North Carolina: Epidemiology, clinical features, and genetic and serotype analysis of causative organisms. The Journal of Infectious Diseases. 1997;176(4):992–1000. [PubMed: 9333158]
  • Kline J. B., Collins C. M. Analysis of the superantigenic activity of mutant and allelic forms of streptococcal pyrogenic exotoxin A. Infection and Immunity. 1996;64(3):861–869. [PMC free article: PMC173849] [PubMed: 8641793]
  • Kotb M., Norrby-Teglund A., McGeer A., El-Sherbini H., Dorak M. T., Khurshid A., et al. An immunogenetic and molecular basis for differences in outcomes of invasive group A streptococcal infections. Nature Medicine. 2002;8(12):1398–1404. [PubMed: 12436116]
  • Kotb M., Ohnishi H., Majumdar G., Hackett S., Bryant A., Higgins G., et al. Temporal relationship of cytokine release by peripheral blood mononuclear cells stimulated by the streptococcal superantigen pepM5. Infection and Immunity. 1993;61(4):1194–1201. [PMC free article: PMC281348] [PubMed: 8454323]
  • Lamagni T. L., Neal S., Keshishian C., Alhaddad N., George R., Duckworth G., et al. Severe Streptococcus pyogenes Infections, United Kingdom, 2003-2004. Emerging Infectious Diseases. 2008;14(2):202–209. [PMC free article: PMC2600190] [PubMed: 18258111]
  • Lamothe F., D'Amico P., Ghosn P., Tremblay C., Braidy J., Patenaude J. V. Clinical usefulness of intravenous human immunoglobulins in invasive group A streptococcal infections: case report and review. Clinical Infectious Diseases. 1995;21(6):1469–1470. [PubMed: 8749635]
  • Lancefield R. C. A serological differentiation of human and other groups of hemolytic streptococci. The Journal of Experimental Medicine. 1933;57(4):571–595. [PMC free article: PMC2132252] [PubMed: 19870148]
  • LaPenta D., Rubens C., Chi E., Cleary P. P. Group A streptococci efficiently invade human respiratory epithelial cells. Proceedings of the National Academy of Sciences of the United States of America. 1994;91(25):12115–12119. [PMC free article: PMC45387] [PubMed: 7991594]
  • Lesko S. M., O'Brien K. L., Schwartz B., Vezina R., Mitchell A. A. Invasive group A streptococcal infection and nonsteroidal antiinflammatory drug use among children with primary varicella. Pediatrics. 2001;107(5):1108–1115. [PubMed: 11331694]
  • Levin J. C., Wessels M. R. Identification of csrR/csrS, a genetic locus that regulates hyaluronic acid capsule synthesis in group A streptococcus. Molecular Microbiology. 1998;30(1):209–219. [PubMed: 9786197]
  • Li Z., Bryant A. E., Hamilton S. M., Bayer C. R., Ma Y., Stevens D. L. Do cardiomyocytes mount an immune response to Group A Streptococcus? Cytokine. 2011;54(3):258–265. [PMC free article: PMC3086889] [PubMed: 21377378]
  • Li Z., Bryant A. E., Parimon T., Stevens D. L. Cardiac dysfunction in StrepTSS: group A streptococcus disrupts the directional cardiomyocyte-to-macrophage crosstalk that maintains macrophage quiescence. Cytokine. 2012;59(1):191–194. [PubMed: 22534112]
  • Majeski J., Majeski E. Necrotizing fasciitis: improved survival with early recognition by tissue biopsy and aggressive surgical treatment. Southern Medical Journal. 1997;90(11):1065–1068. [PubMed: 9386043]
  • Martin P. R., Høiby E. A. Streptococcal serogroup A epidemic in Norway 1987-1988. Scandinavian Journal of Infectious Diseases. 1990;22(4):421–429. [PubMed: 2218404]
  • Mascini E. M., Jansze M., Schellekens J. F., Musser J. M., Faber J. A., Verhoef-Verhage L. A., et al. Invasive group A streptococcal disease in the Netherlands: Evidence for a protective role of anti-exotoxin A antibodies. The Journal of Infectious Diseases. 2000;181(2):631–638. [PubMed: 10669348]
  • McIver K. S. Stand-alone response regulators controlling global virulence networks in streptococcus pyogenes. Contributions to Microbiology. 2009;16:103–119. [PubMed: 19494581]
  • Meleney F. L. Hemolytic Streptococcus Gangrene. Archives of Surgery. 1924;9(2):317–364.
  • Mikaeloff Y., Kezouh A., Suissa S. Nonsteroidal anti-inflammatory drug use and the risk of severe skin and soft tissue complications in patients with varicella or zoster disease. British Journal of Clinical Pharmacology. 2008;65(2):203–209. [PMC free article: PMC2291221] [PubMed: 18251759]
  • Miwa K., Fukuyama M., Ida N., Igarashi H., Uchiyama T. Preparation of a superantigen-adsorbing device and its superantigen removal efficacies in vitro and in vivo. International Journal of Infectious Diseases. 2003;7(1):21–26. [PubMed: 12718806]
  • Mollick J. A., Rich R. R. Characterization of a superantigen from a pathogenic strain of Streptococcus pyogenes. Clinical Research. 1991;39(2):213A.
  • Morens D. M., Taubenberger J. K., Fauci A. S. Predominant role of bacterial pneumonia as a cause of death in pandemic influenza: implications for pandemic influenza preparedness. The Journal of Infectious Diseases. 2008;198(7):962–970. [PMC free article: PMC2599911] [PubMed: 18710327]
  • Muller M. P., Low D. E., Green K. A., Simor A. E., Loeb M., Gregson D., et al. Clinical and epidemiologic features of Group A streptococcal pneumonia in Ontario, Canada. Archives of Internal Medicine. 2003;163(4):467–472. [PubMed: 12588207]
  • Müller-Alouf H., Alouf J. E., Gerlach D., Ozegowski J. H., Fitting C., Cavaillon J. M. Comparative study of cytokine release by human peripheral blood mononuclear cells stimulated with Streptococcus pyogenes superantigenic erythrogenic toxins, heat-killed streptococci and lipopolysaccharide. Infection and Immunity. 1994;62(11):4915–4921. [PMC free article: PMC303207] [PubMed: 7927772]
  • Murphy D. J. Group A streptococcal meningitis. Pediatrics. 1983;71(1):1–5. [PubMed: 6336834]
  • Norrby-Teglund A., Basma H., Andersson J., McGeer A., Low D. E., Kotb M. Varying titers of neutralizing antibodies to streptococcal superantigens in different preparations of normal polyspecific immunoglobulin G: implications for therapeutic efficacy. Clinical Infectious Diseases. 1998;26(3):631–638. [PubMed: 9524835]
  • Norrby-Teglund A., Kaul R., Low D. E., McGeer A., Andersson J., Andersson U., et al. Evidence for the presence of streptococcal-superantigen-neutralizing antibodies in normal polyspecific immunoglobulin G. Infection and Immunity. 1996;64(12):5395–5398. [PMC free article: PMC174535] [PubMed: 8945593]
  • Norrby-Teglund A., Newton D., Kotb M., Holm S. E., Norgren M. Superantigenic properties of the group A streptococcal exotoxin SpeF (MF). Infection and Immunity. 1994a;62(12):5227–5233. [PMC free article: PMC303258] [PubMed: 7960098]
  • Norrby-Teglund A., Norgren M., Holm S. E., Andersson U., Andersson J. Similar cytokine induction profiles of a novel streptococcal exotoxin, MF, and pyrogenic exotoxins A and B. Infection and Immunity. 1994b;62(9):3731–3738. [PMC free article: PMC303024] [PubMed: 8063387]
  • Nuwayhid Z. B., Aronoff D. M., Mulla Z. D. Blunt trauma as a risk factor for group A streptococcal necrotizing fasciitis. Annals of Epidemiology. 2007;17(11):878–881. [PMC free article: PMC4029051] [PubMed: 17697787]
  • O'Brien K. L., Beall B., Barrett N. L., Ciselak P. R., Reingold A., Farley M. M., et al. Epidemiology of invasive group a streptococcus disease in the United States, 1995-1999. Clinical Infectious Diseases. 2002;35(3):268–276. [PubMed: 12115092]
  • Okamoto S., Kawabata S., Nakagawa I., Okuno Y., Goto T., Sano K., et al. Influenza A virus-infected hosts boost an invasive type of Streptococcus pyogenes infection in mice. Journal of Virology. 2003;77(7):4104–4112. [PMC free article: PMC150641] [PubMed: 12634369]
  • Perez-Casal J., Caparon M. G. Mry, a trans-acting positive regulator of the M protein gene of Streptococcus pyogenes with similarity to the receptor proteins of two-component regulatory systems. Journal of Bacteriology. 1991;173(8):2617–2624. [PMC free article: PMC207828] [PubMed: 1849511]
  • Podor T. J., Singh D., Chindemi P., Foulon D. M., McKelvie R., Weitz J. I., et al. Vimentin exposed on activated platelets and platelet microparticles localizes vitronectin and plasminogen activator inhibitor complexes on their surface. The Journal of Biological Chemistry. 2002;277(9):7529–7539. [PubMed: 11744725]
  • Prevention of Invasive Group A Streptococcal Infections Workshop Participants. (2002). Prevention of invasive group A streptococcal disease among household contacts of case patients and among postpartum and postsurgical patients: Recommendations from the Centers for Disease Control and Prevention. Clinical Infectious Diseases, 35(8), 950-959. [PubMed: 12355382]
  • Ramirez C. A., Naragi S., McCulley D. J. Group A beta-hemolytic streptococcus endocarditis. American Heart Journal. 1984;108(5):1383–1386. [PubMed: 6496302]
  • Riseman J. A., Zamboni W. A., Curtis A., Graham D. R., Konrad H. R., Ross D. S. Hyperbaric oxygen therapy for necrotizing fasciitis reduces mortality and the need for debridements. Surgery. 1990;108(5):847–850. [PubMed: 2237764]
  • Robinson K. A., Rothrock G., Phan Q., Sayler B., Stefonek K., Van Beneden C., et al. Risk for severe group A streptococcal disease among patients' household contacts. Emerging Infectious Diseases. 2003;9(4):443–447. [PMC free article: PMC2957982] [PubMed: 12702224]
  • Ruben F. L., Norden C. W., Heisler B., Korica Y. An outbreak of Streptococcus pyogenes infections in a nursing home. Annals of Internal Medicine. 1984;101(4):494–496. [PubMed: 6383164]
  • Schurr M., Engelhardt S., Helgerson R. Limb salvage for streptococcal gangrene of the extremity. American Journal of Surgery. 1998;175(3):213–217. [PubMed: 9560122]
  • Schwartz B., Facklam R. R., Breiman R. F. Changing epidemiology of Group A streptococcal infection in the USA. Lancet. 1990;336(8724):1167–1171. [PubMed: 1978035]
  • Sellers B. J., Woods M. L., Morris S. E., Saffle J. R. Necrotizing group A streptococcal infections associated with streptococcal toxic shock syndrome. American Journal of Surgery. 1996;172(5):523–527. [PubMed: 8942557]
  • Silversides J. A., Lappin E., Ferguson A. J. Staphylococcal toxic shock syndrome: mechanisms and management. Current Infectious Disease Reports. 2010;12(5):392–400. [PubMed: 21308522]
  • Sommer R., Rohner P., Garbino J., Auckenthaler R., Malinverni R., Lew D., et al. Group A beta-hemolytic streptococcus meningitis: clinical and microbiological features of nine cases. Clinical Infectious Diseases. 1999;29(4):929–931. [PubMed: 10589913]
  • Stamenkovic I., Lew P. D. Early recognition of potentially fatal necrotizing faciitis. The New England Journal of Medicine. 1984;310(26):1689–1693. [PubMed: 6727947]
  • Stegmayr B., Björck S., Holm S., Nisell J., Rydvall A., Settergren B. Septic shock induced by group A streptococcal infections: clinical and therapeutic aspects. Scandinavian Journal of Infectious Diseases. 1992;24(5):589–597. [PubMed: 1465576]
  • Stevens D. L. Invasive group A streptococcus infections. Clinical Infectious Diseases. 1992;14(1):2–11. [PubMed: 1571429]
  • Stevens D. L. Could nonsteroidal anti-inflammatory drugs (NSAIDs) enhance the progression of bacterial infections to toxic shock syndrome? Clinical Infectious Diseases. 1995a;21(4):977–980. [PubMed: 8645850]
  • Stevens D. L. Streptococcal toxic shock syndrome: Spectrum of disease, pathogenesis and new concepts in treatment. Emerging Infectious Diseases. 1995b;1(3):69–78. [PMC free article: PMC2626872] [PubMed: 8903167]
  • Stevens D. L. Editorial response: Rationale for the use of intravenous gamma globulin in the treatment of streptococcal toxic shock syndrome. Clinical Infectious Diseases. 1998;26:639–641. [PubMed: 9524836]
  • Stevens D. L. Dilemmas in the treatment of invasive Streptococcus pyogenes infections. Clinical Infectious Diseases. 2003;37:341–343. [PubMed: 12884157]
  • Stevens, D. L., & Bryant, A. E. (2015). Unpublished research.
  • Stevens, D. L., & Kaplan, E. L. (Eds.). (2000). Streptococcal Infections: Clinical Aspects, Microbiology, and Molecular Pathogenesis. New York: Oxford University Press.
  • Stevens D. L., Bisno A. L., Chambers H. F., Dellinger E. P., Goldstein E. J., Gorbach S. L., et al. Practice guidelines for the diagnosis and management of skin and soft tissue infections: 2014 update by the Infectious Diseases Society of America. Clinical Infectious Diseases. 2014;59(2):e10–e52. [PubMed: 24973422]
  • Stevens D. L., Bryant A. E., Hackett S. P. Antibiotic effects on bacterial viability, toxin production, and host response. Clinical Infectious Diseases. 1995;20 Suppl 2:S154–S157. [PubMed: 7548539]
  • Stevens D. L., Bryant A. E., Hackett S. P., Chang A., Peer G., Kosanke S., et al. Group A streptococcal bacteremia: The role of tumor necrosis factor in shock and organ failure. The Journal of Infectious Diseases. 1996;173(3):619–626. [PubMed: 8627025]
  • Stevens, D. L., Hackett, S. P., & Bryant, A. E. (1997a). Suppression of mononuclear cell synthesis of tumor necrosis factor by azithromycin. The Annual Meeting of the Infectious Diseases Society of America (p. 181). San Francisco: The Infectious Diseases Society of America.
  • Stevens D. L., Madaras-Kelly K. J., Richards D. M. In vitro antimicrobial effects of various combinations of penicillin and clindamycin against four strains of Streptococcus pyogenes. Antimicrobial Agents and Chemotherapy. 1998;42(5):1266–1268. [PMC free article: PMC105799] [PubMed: 9593164]
  • Stevens, D. L., Shelly, M., Stiller, R., Villasenor-Sierra, A., & Bryant, A. E. (2008). Acute reversible cardiomyopathy in patients with streptococcal toxic shock syndrome. Proceedings of the XVIIth Lancefield International Symposium on Streptococci and Streptococcal Diseases (p. 179). Porto Heli: FEMS.
  • Stevens D. L., Tanner M. H., Winship J., Swarts R., Reis K. M., Schlievert P. M., et al. Reappearance of scarlet fever toxin A among streptococci in the Rocky Mountain West: Severe group A streptococcal infections associated with a toxic shock-like syndrome. The New England Journal of Medicine. 1989;321(1):1–7. [PubMed: 2659990]
  • Stevens D. L., Tweten R. K., Awad M. M., Rood J. I., Bryant A. E. Clostridial gas gangrene: Evidence that alpha and theta toxins differentially modulate the immune response and induce acute tissue necrosis. The Journal of Infectious Diseases. 1997b;176(1):189–195. [PubMed: 9207366]
  • Stockmann C., Ampofo K., Hersh A. L., Blaschke A. J., Kendall B. A., Korgenski K., et al. Evolving epidemiologic characteristics of invasive group a streptococcal disease in Utah, 2002-2010. Clinical Infectious Diseases. 2012;55(4):479–487. [PMC free article: PMC3520385] [PubMed: 22534148]
  • Strömberg A., Romanus V., Burman L. G. Outbreak of group A streptococcal bacteremia in Sweden: An epidemiologic and clinical study. The Journal of Infectious Diseases. 1991;164(3):595–598. [PubMed: 1869845]
  • Süleyman H., Demircan B., Karagöz Y. Anti-inflammatory and side effects of cyclooxygenase inhibitors. Pharmacological Reports. 2007;59(3):247–258. [PubMed: 17652824]
  • The Working Group on Severe Streptococcal Infections. Defining the group A streptococcal toxic shock syndrome: rationale and consensus definition. JAMA. 1993;269(3):390–391. [PubMed: 8418347]
  • Thigpen M. C., Richards C. L., Lynfield R., Barrett N. L., Harrison L. H., Arnold K. E., et al. Invasive group A streptococcal infection in older adults in long-term care facilities and the community, United States, 1998-2003. Emerging Infectious Diseases. 2007;13(12):1852–1859. [PMC free article: PMC2876747] [PubMed: 18258035]
  • Vaittinen S., Lukka R., Sahlgren C., Hurme T., Rantanen J., Lendahl U., et al. The expression of intermediate filament protein nestin as related to vimentin and desmin in regenerating skeletal muscle. Journal of Neuropathology and Experimental Neurology. 2001;60(6):588–597. [PubMed: 11398835]
  • Valenzuela T. D., Hooton T. M., Kaplan E. L., Schlievert P. Transmission of 'toxic strep' syndrome from an infected child to a firefighter during CPR. Annals of Emergency Medicine. 1991;20(1):90–92. [PubMed: 1984738]
  • van de Beek D., de Gans J., Spanjaard L., Sela S., Vermeulen M., Dankert J. Group a streptococcal meningitis in adults: report of 41 cases and a review of the literature. Clinical Infectious Diseases. 2002;34(9):e32–e36. [PubMed: 11941569]
  • Walker M. J., Hollands A., Sanderson-Smith M. L., Cole J. N., Kirk J. K., Henningham A., et al. DNase Sda1 provides selection pressure for a switch to invasive group A streptococcal infection. Nature Medicine. 2007;13(8):981–985. [PubMed: 17632528]
  • Watanabe-Ohnishi R., Low D. E., McGeer A., Stevens D. L., Schlievert P. M., Newton D., et al. Selective depletion of V beta-bearing T cells in patients with severe invasive group A streptococcal infections and streptococcal toxic shock syndrome. Ontario Streptococcal Study Project. The Journal of Infectious Diseases. 1995;171(1):74–84. [PubMed: 7798684]
  • Weinstein M. P., Reller L. B., Murphy J. R., Lichtenstein K. A. The clinical significance of positive blood cultures: a comprehensive analysis of 500 episodes of bacteremia and fungemia in adults. I. Laboratory and epidemiologic observations. Reviews of Infectious Diseases. 1983;5(1):35–53. [PubMed: 6828811]
  • Weng T. C., Chen C. C., Toh H. S., Tang H. J. Ibuprofen worsens Streptococcus pyogenes soft tissue infections in mice. Journal of Microbiology, Immunology, and Infection. 2011;44(6):418–423. [PubMed: 21697021]
  • Wheeler M. C., Roe M. H., Kaplan E. L., Schlievert P. M., Todd J. K. Outbreak of group A streptococcus septicemia in children. Clinical, epidemiologic, and microbiological correlates. JAMA. 1991;266(4):533–537. [PubMed: 2061980]
  • Wong C. J., Stevens D. L. Serious group a streptococcal infections. The Medical Clinics of North America. 2013;97(4):721–736. [PubMed: 23809722]
  • Xu B., deWaal R. M., Mor-Vaknin N., Hibbard C., Markovitz D. M., Kahn M. L. The endothelial cell-specific antibody PAL-E identifies a secreted form of vimentin in the blood vasculature. Molecular and Cellular Biology. 2004;24(20):9198–9206. [PMC free article: PMC517872] [PubMed: 15456890]
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