Vibrio parahaemolyticus

Vibrio parahaemolyticus is a halophilic gram-negative rod. The organisms are found in waters along the entire coastline of the United States. Generally, the incidence of clinical disease is greatest in the warm summer months when the organism is commonly found in zooplankton. V. parahaemolyticus absorbs onto chitin and to minute crustacean copepods that feed on sediment. It has been postulated that unusual warm coastal currents (such as El Niño) may contribute to increased proliferation of Vibrio species. The optimal growth temperature of V. parahaemolyticus is 35° to 37° C (95° to 98.6° F); under ideal conditions, the generation time has been estimated at less than 10 minutes, with explosive population growth from 10 to 10⁶ organisms in 3 to 4 hours.

Extraintestinal wound infections are most common in persons who suffer chronic liver disease or immunosuppression. Although more than 95% of V. parahaemolyticus strains associated with human illness are positive, the relationship to pathogenicity of the Kanagawa reaction (production of a cell-free hemolysin on high salt-mannitol [Wagatsuma] agar), caused by a heat-stable direct hemolysin, is not yet clear. Furthermore, most marine strains are not Kanagawa positive. Virulence factors include proteases, beta-hemolysins (thermostable direct hemolysin [tdh] and tdh-related hemolysin [trh]), adhesins, and the expression of virulence genes, including the toxR operons.^12,164 Some primary soft tissue infections previously attributed to V. parahaemolyticus may theoretically be attributed to misidentified V. vulnificus. Panophthalmitis requiring enucleation occurred in a man who suffered a corneal laceration.¹⁷³

Vibrio vulnificus

Vibrio vulnificus (formerly known as a “lactose [fermenting]-positive” vibrio) is a halophilic gram-negative bacillus. V. vulnificus (Latin for “wounding”) is found in virtually all U.S. coastal waters and has been reported to cause infection worldwide.¹¹ It prefers salinity of 0.7% to 1.6%; although it prefers a habitat of warm (at least 20° C [68° F]) seawater, it can be found in much colder water. It does not appear to be associated with fecal contamination of seawater. It has been shown to exist in Chesapeake Bay with bacterial counts comparable with those reported from the Gulf of Mexico.²⁰³ A series of nine cases of Vibrio infection, in most cases of the species vulnificus, was reported associated with finning injury of the hands.⁴⁷

V. vulnificus may or may not have an acidic polysaccharide capsule (opaque colony), which confers protection against bactericidal activity of human serum and phagocytosis and thus renders the organism more virulent in animals. At extremely low frequency, some strains can shift between unencapsulated (avirulent; translucent colony) and capsulated (virulent) serotypes. The encapsulated isolates show exquisite (positive) sensitivity to iron. Virulent isolates can use 100% but not 30% saturated (normal for humans) transferrin as an iron source, as well as iron in hemoglobin and hemoglobin–haptoglobin complexes. V. vulnificus exhibits enhanced growth and virulence in the presence of increased serum iron concentration or saturated transferrin-binding sites.² V. vulnificus is classified into three biotypes: biotype 1 is pathogenic for humans and biotype 2 is pathogenic for fish.^48,49 Biotype 3 causes soft-tissue infections and septicemia following contact with fish from freshwater ponds; it was first noted in Israel. Within biotype 1, various genetically distinct subgroups identified by randomly amplified polymorphic deoxyribonucleic acid (DNA) polymerase chain reaction (PCR) appear to be especially virulent.⁸ Furthermore, complete genomic sequencing of V. vulnificus YJ016, a biotype 1 strain, reveals gene clusters related to pathogenicity (cell adhesion, colonization, cytotoxicity, and tissue destruction), including capsular polysaccharide, siderophore biosynthesis and transport, and heme receptor and transport.⁴⁹ In vivo antigen technology can identify virulence genes produced and expressed in humans.⁹³ The ability of biotype 1 to multiply and produce a toxic metalloprotease in human serum may be a prominent virulence factor.¹⁹⁶

Infection worsens rapidly after the initiation of symptoms and has been noted most frequently in men older than age 40 years with preexisting hepatic dysfunction (particularly cirrhosis), end-stage renal impairment, leukopenia, or impaired immunity (malignancy, leukemia, hypogammaglobulinemia, human immunodeficiency virus [HIV] infection, diabetes, bone marrow suppression, long-term corticosteroids), although it has been reported in young, previously healthy individuals.* One case followed application of fish blood by a healer as a traditional remedy to a chronic leg ulcer in an obese patient suffering from recurrent erysipelas.¹⁷⁴ Preexisting liver disease is a predictor of death, with 50% of such individuals in one series succumbing to the illness.⁸⁰ Persons with high serum iron levels (from chronic cirrhosis, hepatitis, thalassemia major, hemochromatosis, multiple transfusions [such as are given for aplastic anemia]) or achlorhydria (low gastric acid; may be iatrogenically induced with H₂ blockers) may be at greater risk for fulminant bacteremia.^2,168,183 This has been attributed in part to the protective effect of gastric acid, the iron requirement of the organism, and the effects of liver disease (decreased polymorphonuclear leukocyte and macrophage activity, flawed opsonization, and shunting of portal blood around the liver). It has been proposed that an effective host response against V. vulnificus and similar iron-sensitive pathogens (e.g., Listeria monocytogenes, Klebsiella spp., and Yersinia spp.) is in part augmented by hepcidin, a cysteine-rich cationic antimicrobial peptide central to iron metabolism.^8,195 V. vulnificus produces a siderophore (vulnibactin) and a protease that may enhance pathogenicity.² Other pathogenicity factors may be the polysaccharide capsule, hemolysin, type IV pili and other proteases, including a serine protease and a 45-kDa metalloprotease regulated through quorum sensing at a lower temperature than core body temperature.^124,194

The syndrome consists of flu-like malaise, fever, vomiting, diarrhea, chills, hypotension, and early skin vesiculation that evolve into necrotizing dermatitis and fasciitis, with vasculitis and myositis (Figures 79-1 and 79-2).²⁰⁴ Hematogenous seeding of vibrios to secondary cutaneous lesions is probable. Primary wound infections (approximately 30% of cases) rapidly show marked edema, with erythema, vesicles, and hemorrhagic or contused-appearing bullae, progressing to necrosis. This may require radical surgical debridement or amputation. Up to 25% of these victims may have sepsis. When V. vulnificus is recovered from the blood of a victim with sepsis attributable to a wound infection, the case fatality rate may exceed 30%.⁸⁰ Extracellular elastin-lysing proteases elaborated by the organism, as well as a potent collagenase, probably contribute to the rapid invasion of healthy tissue. V. vulnificus also produces a cytotoxin-hemolysin and phospholipases. Cytolysin produced by most pathogenic strains of V. vulnificus is extremely toxic to mice when injected IV and results in severe perivascular edema and neutrophil infiltration in lung tissues.^89,135 The precise roles of these and other factors (pili, mucinase, chondroitinase, hyaluronidase) in the in vivo pathogenicity of the organism have yet to be determined. Bleeding complications (which may include gastrointestinal hemorrhage and disseminated intravascular coagulation) are common and may be attributed in part to thrombocytopenia. Gastroenteritis is more common (15% to 20%) with the septicemic presentation than with primary wound infection and may exist as an isolated entity (approximately 10% of cases), although it is debated that illness has been erroneously attributed to the asymptomatically carried organism. Vibrio vulnificus endometritis has been reported after an episode of intercourse in the waters of Galveston Bay, Texas.¹⁷⁸ Other presentations of V. vulnificus infections have included meningitis, necrotizing fasciitis following lightning strike in a windsurfer, spontaneous bacterial peritonitis, corneal ulcers, epiglottitis, and infections of the testes, spleen, and heart valves.¹⁸⁵

FIGURE 79-1 Ecthyma gangrenosum associated with Vibrio vulnificus sepsis.

(Courtesy Edward J. Bottone, MD, Department of Microbiology, Mt Sinai Hospital, NY.)

FIGURE 79-2 Torso of a victim with Vibrio vulnificus sepsis.

The explosive nature of the syndrome can lead to gram-negative sepsis and death, reportedly in up to 50% of cases. The mortality rate may be as high as 90% in victims who become hypotensive within 12 hours of initial examination by a physician. For wound infections from all Vibrio species, the organism may only be recovered from blood specimens in less than 20% of victims.⁸⁰ Appropriate antibiotics should be administered as soon as the infection is suspected (see later). In one report, V. vulnificus sepsis was treated with antibiotic therapy, debridement of necrotic tissues, and direct hemoperfusion using polymyxin B immobilized fiber, which served as an artificial reticuloendothelial system and removed endotoxin from the circulating blood.¹⁵³ In an immunocompetent victim who acquired a V. vulnificus hand infection from peeling shrimp, treatment with oral ciprofloxacin was successful. In a series of seven patients treated for primary skin and soft tissue infections secondary to V. vulnificus, prompt operative exploration and debridement were correlated with a decrease in the intensive care unit and hospital length of stay, particularly if the surgery occurred within 72 hours from the time of infection.⁷⁷ The authors noted that all patients had necrosis of underlying subcutaneous tissue, whereas some did not demonstrate skin necrosis.

Vibrio mimicus

Vibrio mimicus is a motile, nonhalophilic, gram-negative, oxidase-positive rod with a single flagellum. It can be distinguished from V. cholerae by its inability to ferment sucrose, inability to metabolize acetylmethyl carbonyl, sensitivity to polymyxin, and negative lipase test. An ear infection may follow exposure to ocean water. Isolates are sensitive to tetracycline. Physicians who collect stool samples for culture to identify suspected V. mimicus must alert the laboratory to use appropriate culture media (thiosulfate–citrate–bile salts–sucrose [TCBS] agar).

Vibrio alginolyticus

Vibrio alginolyticus, found in seawater, has been implicated in soft tissue infections (e.g., those caused by coral cuts or surfing scrapes), sinusitis, and otitis, particularly after previous ear infections or a tympanic membrane perforation. Although bacteremia has been reported in immunosuppressed patients and patients with burns, V. alginolyticus does not generally carry the virulent potential of V. vulnificus.¹¹⁹ Typical symptoms include cellulitis, with seropurulent exudate. Its distinguishing microbiologic features are stated to be sucrose and lactose fermentation, growth in 1% tryptone broth plus 10% NaCL, positive Voges–Proskauer reaction, negative urease reaction, and susceptibility to vibriostatic compound O/129. However, because these indices may vary, identification may be difficult. Antibiotic resistance may be a feature of V. alginolyticus infection.

Photobacterium damsela

Photobacterium (formerly Vibrio or Listonella) damsela, formerly enteric group EF-5 and so-named because it is pathogenic for the damselfish, causes wound infections similar to those attributed to vibrios. Rapidly progressive infection leading to muscle necrosis and fasciitis or to sepsis and death may transpire in an immunosuppressed victim or person with normal immunity.^66,68,175 This may be related to an extracellular cytolysin (damselysin) or other unidentified enzymes or virulence factors.

Vibrio cholerae

Vibrio cholerae is associated with severe gastroenteritis (see Chapter 68). With regard to tissue infection, a case of necrotizing fasciitis and septic shock caused by V. cholerae non-O1 (not agglutinated in cholera polyvalent O1 antiserum) acquired in San Diego, California, has been described.¹⁹² The victim suffered from preexisting diabetes mellitus complicated by chronic plantar ulceration of the affected limb. V. cholerae may cause severe disease signs in Japanese sweetfish (ko-ayu or Plecoglossus altivelis), certain shrimp (e.g., Penaeus monodon), and ornamental fish in India.^13,76,171

Wound Infections Caused by Aeromonas Species

Aeromonas hydrophila (Latin for “gas producing” and “water loving”) is a gram-negative, facultatively anaerobic, polarly flagellated, non–spore-forming, and motile rod member of the family Vibrionaceae that commonly inhabits soil, freshwater streams, and lakes.^3,14,103,188 Aeromonas species are widely distributed and found at wide ranges of temperature and pH. Five species (A. hydrophila, A. sobria, A. schubertii, A. veronii, and A. caviae) of the 9 that have been recovered from clinical material have been linked with human disease; there are 13 or more distinct genotypes.¹ A. hydrophila is pathogenic to amphibians, reptiles, and fish. Soft tissue and gastroenteric infections predominate in humans. Virulence factors elaborated by Aeromonas species include hemolysin, cytotoxin, enterotoxin, cholera toxin–like factor, and hemagglutinins.^27,187 Aeromonas species are sometimes misidentified as members of the genus Vibrio by commonly used screening tests.¹

A wound, particularly of the puncture variety, immersed in contaminated water may become cellulitic within 24 hours, with erythema, edema, and a purulent discharge.^156,201 The lower extremity is most frequently involved. This usually occurs from stepping on a foreign object or being punctured underwater. The appearance may be indistinguishable from a typical streptococcal cellulitis, with localized pain, lymphangitis, fever, and chills. Untreated or managed with antibiotics to which the organism is not susceptible, this may rarely progress to a severe gas-forming soft tissue reaction, bulla formation, necrotizing myositis, or osteomyelitis. Appearance similar to ecthyma gangrenosum caused by Pseudomonas aeruginosa has been reported in Aeromonas septicemia.

Fever, hypotension, jaundice, and chills are common manifestations of septicemia.⁹⁶ Additional clinical manifestations include abdominal pain or tenderness, altered consciousness, acute renal failure, bacteremic pneumonia, and coagulopathy.⁹⁰ In a manner analogous to the pathogenicity of virulent Vibrio species, the chronically ill or immunocompromised host (e.g., chronic liver disease, neoplasm, diabetes, uremia, corticosteroid therapy, extensive burns) is probably at greater risk of a severe infection or complication, such as meningitis, endocarditis, or septicemia. Freshwater aspiration may result in A. hydrophila pneumonitis and bacteremia. Infection has followed the bite of an alligator. A 15-year-old boy suffered an A. hydrophila wound infection after a bite from his pet piranha. For unknown reasons, there is a marked preponderance of male victims. This may represent the phenotypic variation of critical bacterial adhesins or may simply reflect activity patterns of male humans. Corneal ulcer caused by A. sobria was reported after abrasion by a freshwater reed.⁴⁴

Because of the microbiologic similarity of Aeromonas on biochemical testing to members of the Enterobacteriaceae family, such as E. coli or Serratia species, it is important to alert the laboratory to the clinical setting. In the microbiology laboratory, Aeromonas species may be identified on the basis of positive oxidase reaction, no growth on TCBS agar, growth on MacConkey agar, and resistance to the vibriostatic compound O/129.⁹⁶

Gram’s stain of the purulent discharge may demonstrate gram-negative bacilli, singly, paired, or in short chains. Given the appropriate clinical setting (after a wound acquired in the freshwater environment), this should not be casually attributed to contamination.⁸⁹ A. hydrophila is generally sensitive to chloramphenicol, aztreonam, gentamicin, amikacin, tobramycin, trimethoprim–sulfamethoxazole, cefotaxime, cefuroxime, moxalactam, imipenem, ceftazidime, ciprofloxacin, and norfloxacin. In one case, culture of a severe wound infection demonstrated the presence of two species, A. hydrophila and A. sobria. Notably, the latter was resistant to tetracycline in vitro. For a severe infection, initial therapy that includes an aminoglycoside provides coverage against concomitant Pseudomonas or Serratia infection. As has been demonstrated with Vibrio species, the first-generation cephalosporins, penicillin, ampicillin, and ampicillin-sulbactam are not efficacious, perhaps because of the production of a β-lactamase by the organism. Aeromonas species are capable of producing chromosomally encoded β-lactamases induced by β-lactam antibiotics. This leads to resistance to penicillins, cephalosporins, and monobactams. The β-lactamase inhibitors, such as clavulanate, are not effective against these β-lactamases, so that amoxicillin-clavulanate may not kill Aeromonas.¹³⁶ The optimal therapy for invasive infections caused by cefotaxime-resistant A. hydrophila is not known, but a recent study of in vitro and in vivo (mice) activities of fluoroquinolones suggest that ciprofloxacin may be as effective as cefotaxime–minocycline.⁹⁵ In this study, ciprofloxacin and levofloxacin showed greater activity than did gatifloxacin, moxifloxacin, and lomefloxacin.

Initial therapy of a severe soft tissue infection related to Aeromonas should include aggressive wound debridement to mitigate the potentially invasive nature of the organism. In one case of severe cellulitis unresponsive to debridement, fasciotomy, and antibiotic therapy, treatment with hyperbaric oxygen was felt to contribute to successful infection control.¹¹⁸

Curiously, medicinal leeches can harbor Aeromonas in their gut flora; soft tissue infections related to this phenomenon have been reported.¹⁶⁵ The genus Plesiomonas also belongs to the family Vibrionaceae; it has been definitively linked with aquarium-associated infection complicated by watery diarrhea and fever.

Infections Caused by a Fish Pathogen, Streptococcus iniae

Streptococcus iniae is a pathogen of fish, noted to cause subcutaneous abscesses in Amazon freshwater dolphins (Mammalia: Inia geoffrensis) kept in captivity.¹⁹⁷ Epizootic fatal meningoencephalitis in fish species caused by streptococci has been observed in outbreaks affecting tilapia, yellowtail, rainbow trout, and coho salmon. S. iniae has emerged as a serious pathogen of farmed barramundi in Australia.²⁹ Persons who handle these fish are at risk for bacteremic illness, which can manifest as cellulitis or sepsis. Endocarditis, meningitis, and arthritis have been noted to accompany S. iniae infection.

The tilapia (Oreochromis and Tilapia species) are also known as St. Peter’s fish or Hawaiian sunfish. The surfaces of these commonly aquacultured fishes may be colonized with S. iniae. Persons of Asian descent have been identified as prone to infection, probably because they often prepare this fish with the intent to dine. Typically, the victim recalls puncturing the skin of the hand with a fin, bone, or implement of preparation. Cellulitis with lymphangitis and fever is common, without skin necrosis or bulla formation.¹⁹⁷

In culture, S. iniae shows β-hemolysis. However, it may appear to be α-hemolytic because the narrow zone of β-hemolysis is ringed by more prominent zone of α-hemolysis. Therefore, it may be misidentified as a viridans streptococcus and thus considered a contaminant. A reasonable approach to antibiotic therapy includes penicillin, cefazolin, ceftriaxone, erythromycin, clindamycin, or trimethoprim–sulfamethoxazole. In one series, ciprofloxacin showed slightly less efficacy in vitro.

A General Approach to Antibiotic Therapy

Management of freshwater-acquired infections should include therapy against Aeromonas species. First-generation cephalosporins provide inadequate coverage against growth of freshwater bacteria. Third-generation cephalosporins provide excellent coverage, whereas second-generation products are less effective. Ceftriaxone may not be efficacious against Aeromonas species. Ciprofloxacin, imipenem, ceftazidime, gentamicin, and trimethoprim–sulfamethoxazole are reasonable antibiotics against gram-negative microorganisms. Trimethoprim or ampicillin alone may be inefficacious.

Whether to begin antimicrobial therapy before establishment of a wound infection is controversial. Pending a prospective evaluation of prophylactic antibiotics in freshwater-acquired wounds, the following recommendations are based on the potentially serious nature of soft tissue infections caused by Aeromonas species: