Intermediate vancomycin susceptibility in a community-associated MRSA clone.We describe a case of treatment failure caused by a strain of USA300 community-associated methicillin-resistant Staphylococcus aureus methicillin-resistant Staphylococcus aureus Methicillin-aminoglycoside resistant Staphylococcus aureus, MRSA An organism with multiple antibiotic resistances–eg, aminoglycosides, chloramphenicol, clindamycin, erythromycin, rifampin, tetracycline, (MRSA MRSA Methicillin-resistant Staphylococcus aureus. See MARSA. ) with intermediate susceptibility to vancomycin and reduced susceptibility to daptomycin. The strain was isolated from the bone of a 56-year-old man with lumbar osteomyelitis osteomyelitis (ŏs'tēōmī'əlī`tĭs), infection of the bone and bone marrow. Direct infection of bone usually occurs through open fractures, penetrating wounds, or surgical operations. after a 6-week treatment course of vancomycin for catheter-associated septic thrombophlebitis thrombophlebitis: see phlebitis. . ********** A 56-year-old man with a history of type 2 diabetes type 2 diabetes n. See diabetes mellitus. and chronic kidney disease Chronic kidney disease (CKD), also know as chronic renal disease, is a progressive loss of renal function over a period of months or years through five stages. Each stage is a progression through an abnormally low and progressively worse glomerular filtration rate, which is was seen at San Francisco General Hospital San Francisco General Hospital is the main public hospital in San Francisco, California, and the only Level I Trauma Center serving San Francisco and San Mateo. The hospital budget is for only 302 beds at SFGH. in November 2005 because of hyperkalemia Hyperkalemia Definition The normal concentration of potassium in the serum is in the range of 3.5 to 5.0 mM. Hyperkalemia refers to serum or plasma levels of potassium ions above 5.0 mM. and volume overload. On day 4 of hospitalization, a fever of 39[degrees]C and cellulitis Cellulitis Definition Cellulitis is a spreading bacterial infection just below the skin surface. It is most commonly caused by Streptococcus pyogenes or Staphylococcus aureus. in the right arm associated with a peripheral intravenous line developed. Two blood cultures were drawn, the line was removed, and therapy was initiated with oral cephalexin cephalexin /ceph·a·lex·in/ (-lek´sin) a semisynthetic first-generation cephalosporin, effective against a wide range of gram-positive and a limited range of gram-negative bacteria; used as the base or the hydrochloride salt. . One of the 2 blood cultures subsequently grew methicillin-resistant Staphylococcus aureus (MRSA) that was susceptible to tetracycline tetracycline (tĕ'trəsī`klēn), any of a group of antibiotics produced by bacteria of the genus Streptomyces. They are effective against a wide range of Gram positive and Gram negative bacteria, interfering with protein and trimethoprim-sulfamethoxazole. The patient was treated with oral trimethoprim-sulfamethoxazole and discharged to home to complete a 10-day course. His right upper extremity cellulitis subsequently resolved, but he returned to the hospital in January 2006 with volume over-load and symptoms consistent with uremia uremia (y  rē`mēə), condition resulting from advanced stages of kidney failure in which urea and other nitrogen-containing wastes are found in the blood. . A tunneled
right internal jugular jugular /jug·u·lar/ (jug´u-lar)1. cervical. 2. pertaining to a jugular vein. 3. a jugular vein. jug·u·lar adj. hemodialysis catheter was placed on January 11, hemodialysis was initiated, and he was discharged to home. On February 20, he was seen in the emergency department of another facility with nausea and altered mental status. He was afebrile afebrile /afe·brile/ (a-feb´ril) without fever. a·feb·rile adj. Apyretic. afebrile without fever. afebrile adjective Feverless but hypotensive hypotensive /hy·po·ten·sive/ (-ten´siv) marked by low blood pressure or serving to reduce blood pressure. hy·po·ten·sive adj. 1. Of or characterized by low blood pressure. 2. , and tenderness at the entrance site of the hemodialysis catheter was noted. Two blood cultures were positive for MRSA. The patient's catheter was removed, and intravenous vancomycin was started. Transthoracic transthoracic /trans·tho·rac·ic/ (-thah-ras´ik) through the thoracic cavity or across the chest wall. trans·tho·rac·ic adj. Across or through the thoracic cavity or chest wall. and subsequent transesophageal echocardiograms were negative for endocarditis endocarditis (ĕn'dōkärdī`tĭs), bacterial or fungal infection of the endocardium (inner lining of the heart) that can be either acute or subacute. , but evidence of thrombosis in the superior vena cava superior vena cava n. Abbr. SVC A large vein formed by the union of the two brachiocephalic veins and the azygos vein that receives blood from the head, neck, upper limbs, and chest, and empties into the right atrium of the heart. was seen. Multiple blood cultures were positive for MRSA through March 1, after which they became negative. The vancomycin MIC for serial isolates remained unchanged. The patient was treated with vancomycin for a 6-week course, beginning March 1. Anticoagulation with coumadin was also initiated. After clearance of his blood cultures, a right subclavian subclavian /sub·cla·vi·an/ (sub-kla´ve-an) below the clavicle. Subclavian Located beneath the collarbone (clavicle). tunneled hemodialysis catheter and a left upper extremity arteriovenous fistula were placed. Vancomycin trough levels were assayed on multiple occasions during the 6-week course; all were [greater than or equal to]20 [micro]g/mL. On April 24, the patient was seen by his primary care provider for worsening bilateral knee and back pain and difficulty walking. A lumbar spine radiograph radiograph /ra·dio·graph/ (-graf?) the film produced by radiography. ra·di·o·graph n. demonstrated cortical irregularity A defect, failure, or mistake in a legal proceeding or lawsuit; a departure from a prescribed rule or regulation. An irregularity is not an unlawful act, however, in certain instances, it is sufficiently serious to render a lawsuit invalid. at L4-L5, indicative of discitis. He was admitted to the hospital, and vancomycin was initiated. Magnetic resonance imaging magnetic resonance imaging (MRI), noninvasive diagnostic technique that uses nuclear magnetic resonance to produce cross-sectional images of organs and other internal body structures. of the lumbar spine on April 25 demonstrated findings consistent with osteomyelitis and discitis at L4-L5. A needle biopsy of the L4-L5 lesion was performed on April 27. That evening, the patient was noted to be febrile febrile /feb·rile/ (feb´ril) pertaining to or characterized by fever. feb·rile adj. Of, relating to, or characterized by fever; feverish. and had an episode of emesis emesis /em·e·sis/ (em´e-sis) vomiting. em·e·sis n. pl. em·e·ses The act or process of vomiting. Emesis The medical term for vomiting. . Later in the evening, he was apneic and without a pulse, with fixed and dilated dilated a state of dilatation. dilated cardiomyopathy see congestive cardiomyopathy. dilated pupil syndrome see feline dysautonomia (Key-Gaskell syndrome). pupils. Cardiopulmonary resuscitation was performed. When neurologic function did not return during the next 4 days, supportive care was withdrawn, and the patient died May 1. Multiple blood cultures from this hospitalization remained negative, but results of a culture of lumbar fluid from a biopsy specimen on April 27 were positive for a vancomycin-intermediate S. aureus The aureus (pl. aurei) was a gold coin of ancient Rome valued at 25 silver denarii. The aureus was regularly issued from the 1st century BC to the beginning of the 4th century AD, when it was replaced by the solidus. (VISA) isolate, with a vancomycin MIC of 8 [micro]g/mL. The antimicrobial susceptibility profiles of the blood isolates from November and February and the lumbar isolate from April are shown in the Table. All MIC susceptibilities were determined by broth microdilution methods per Clinical and Laboratory Standards Institute guidelines. The November and April isolates were tested with MicroScan overnight panels (Dade Behring, Deerfield, IL, USA); the February isolate was tested by using a noncommercial tray. Confirmatory testing of the vancomycin MIC of the April isolate was determined by E-test, which returned an MIC of 6 [micro]g/mL initially and 4 gg/mL on repeat testing. The isolate also grew on vancomycin (6 [micro]g/mL) agar screen plates. Susceptibilities to daptomycin, linezolid, and tigecycline were performed on the February and April isolates by E-test. Notably, the daptomycin MIC of the April isolate was reproducibly 2 [micro]g/mL, an increase from 1 [micro]g/mL for the February isolate. On blood agar plate, the April lumbar isolate was noted to be weakly [beta]-hemolytic with small colony size. With multiple subcultures in the absence of vancomycin this morphotype reverted to the full [beta]-hemolysis and large colony size typical of S. aureus, intermediate susceptibility to vancomycin was lost, and daptomycin susceptibility was regained. Pulsed-field gel electrophoresis with Sinai digestion was performed on the 2 blood isolates from November and February and the lumbar isolate from April. All 3 isolates shared an identical pattern with the USA300-0114 control strain (Figure). Sequencing of the protein A gene polymorphic region (spa typing) (1) of the lumbar isolate obtained the sequence YHGFMBQBLO, typical for clonal cluster 8. PCR PCR polymerase chain reaction. PCR abbr. polymerase chain reaction Polymerase chain reaction (PCR) was positive for the presence of mecA, ACME (arginine arginine (är`jənĭn), organic compound, one of the 20 amino acids commonly found in animal proteins. Only the l-stereoisomer participates in the biosynthesis of proteins. catabolic Catabolic A metabolic process in which energy is released through the conversion of complex molecules into simpler ones. Mentioned in: Anabolic Steroid Use catabolic see catabolism. mobile element, a signature gene cluster of USA300), and Panton-Valentine leukocidin genes and negative for the presence of the vanA gene, when primers and sequences previously described were used (2-4). [FIGURE OMITTED] The community MRSA clone USA300, first identified in 2001, has emerged as a notable cause of colonization and disease in San Francisco (5). This clone has been remarkable for its rapid spread and propensity to cause severe infection, particularly skin and soft tissue and pulmonary infection. Recent sequencing of its genome demonstrated possible contributors to its virulence, most notably Panton-Valentine leukocidin and ACME (2). The USA300-0114 subclone has been the predominant one during the community MRSA epidemic in San Francisco (6) and is becoming widely prevalent in communities throughout the United States (7). Surveys of clinical MRSA isolates throughout the city of San Francisco
The first report of clinical VISA infection was from Japan in 1997 (8). Molecular typing of this and subsequent VISA isolates showed these to be derived from prevalent hospital-acquired clones primarily belonging to clonal cluster 5 (9). The accessory gene regulator (agr) group II genotype present in clonal cluster 5 strains has been speculated to predispose pre·dis·pose v. To make susceptible, as to a disease. to emergence of the VISA phenotype. USA300 is an agr group III clone (6). The occurrence of the vancomycin-intermediate phenotype in USA300 suggests that development of this phenotype may simply reflect the prevalence of clones in a particular population, rather than a causal relationship to agr. The mechanism of reduced vancomycin susceptibility in VISA is thought to be mediated by an increase in the number of false targets because of a thickened cell wall (10), perhaps aided by altered expression of penicillin-binding proteins 2 and 4 (11). VISA and hVISA, strains of S. aureus that contain subpopulations of daughter cells displaying intermediate sensitivity to vancomycin but for which the MICs for vancomycin fall within the susceptible range, can be difficult to detect in the microbiology laboratory because the phenotypes are unstable and can be lost on subsequent passages (12); this situation was demonstrated in our case. Reduced susceptibility to daptomycin in vancomycin-intermediate isolates has been described previously, perhaps because of reduced diffusion of the molecule through the thickened cell wall, although this has not been proven (13). The clinical importance of the reduced daptomycin susceptibility seen in vancomycin-intermediate isolates, however, is unclear at this time. Our patient experienced clinical failure of vancomycin therapy despite high serum drug levels, which speaks to the difficulty with which highly invasive S. aureus infections are successfully treated with vancomycin, particularly in patients receiving hemodialysis. While most VISA isolates reported in the United States have been isolated from patients receiving hemodialysis, chronic renal disease and hemodialysis have not been definitively identified as risk factors for infections caused by VISA or hVISA (14). The frequency of nasal colonization with hVISA was low in hemodialysis patients monitored from 1999 to 2002 in the San Francisco Bay Area “Bay Area” redirects here. For other uses, see Bay Area (disambiguation). The San Francisco Bay Area, colloquially known as the Bay Area or The Bay (15). However, as the prevalence of USA300 increases and prompts further use of vancomycin, intermediate vancomycin susceptibility in USA300 may become more common among both community and hospital isolates. Dr Graber is a senior infectious diseases fellow at the University of California, San Francisco . His research interests include the molecular and clinical epidemiology of S. aureus infection and its interaction with HIV HIV (Human Immunodeficiency Virus), either of two closely related retroviruses that invade T-helper lymphocytes and are responsible for AIDS. There are two types of HIV: HIV-1 and HIV-2. HIV-1 is responsible for the vast majority of AIDS in the United States. disease. References (1.) Shopsin B, Gomez M, Montgomery SO, Smith DH, Waddington M, Dodge BE, et al. Evaluation of protein A gene polymorphic region DNA sequencing for typing of Staphylococcus aureus strains. J Clin Microbiol. 1999;37:356-63. (2.) Diep BA, Gill SR, Chang RF, Phan TH, Chen JH, Davidson MG, et al. Complete genome sequence of USA300, an epidemic clone of community-acquired methicillin-resistant Staphylococcus aureus. Lancet. 2006;367:731-9. (3.) Lina G, Piemont Y, Godail-Gamot F, Bes M, Peter MO, Gauduchon V, et al. Involvement of Panton-Valentine leukocidin--producing Staphylococcus aureus in primary skin infections and pneumonia. Clin Infect Dis. 1999;29:1128-32. (4.) Weigel LM, Clewell DB, Gill SR, Clark NC, McDougal LK, Flannagan SE, et al. Genetic analysis of a high-level vancomycin resistant isolate of Staphylococcus aureus. Science. 2003;302: 1569-71. (5.) Carleton HA, Diep BA, Charlebois ED, Sensabaugh GF, Perdreau-Remington F. Community-adapted methicillin-resistant Staphylococcus aureus (MRSA): population dynamics of an expanding community reservoir of MRSA. J Infect Dis. 2004; 190:1730-8. (6.) Diep BA, Carleton HA, Chang RF, Sensabaugh GF, Perdreau-Remington F. Roles of 34 virulence genes in the evolution of hospital-and community-associated strains of methicillin-resistant Staphylococcus aureus. J Infect Dis. 2006; 193:1495-503. (7.) Tenover FC, McDougal LK, Goering RV, Killgore G, Projan SJ, Patel JB, et al. Characterization of a strain of community-associated methicillin-resistant Staphylococcus aureus widely disseminated in the United States. J Clin Microbiol. 2006;44:108-18. (8.) Hiramatsu K, Hanaki H, Ino T, Yabuta K, Oguri T, Tenover FC. Methicillin-resistant Staphylococcus aureus clinical strain with reduced vancomycin susceptibility. J Antimicrob Chemother. 1997;40:135-6. (9.) McDougal LK, Steward CD, Killgore GE, Chaitram JM, McAllister SK, Tenover FC. Pulsed-field gel electrophoresis typing of oxacillin-resistant Staphylococcus aureus isolates from the United States: establishing a national database. J Clin Microbiol. 2003;41:5113-20. (10.) Cui L, Iwamoto A, Lian J-Q, Neoh H-M, Maruyama T, Horikawa Y, et al. Novel mechanism of antibiotic resistance originating in vancomycin-intermediate Staphylococcus aureus. Antimicrob Agents Chemother. 2006;50:428-38. (11.) Finan JE, Archer G, Pucci M, Climo M. Role of penicillin-binding protein 4 in expression of vancomycin resistance among clinical isolates of oxacillin-resistant Staphylococcus aureus. Antimicrob Agents Chemother. 2001;45:3070-5. (12.) Boyle-Vavra S, Berke SK, Lee JC, Daum RS. Reversion of the glycopeptide resistance phenotype in Staphylococcus aureus clinical isolates. Antimicrob Agents Chemother. 2000;44:272-7. (13.) Patel JB, Jevitt LA, Hageman J, McDonald LC, Tenover FC. An association between reduced susceptibility to daptomycin and reduced susceptibility to vancomycin in Staphylococcus aureus. Clin Infect Dis. 2006;42:1652. (14.) Fridkin SK, Hageman J, McDougal LK, Mohammed J, Jarvis WR, Perl TM, et al. Epidemiological and microbiological characterization of infections caused by Staphylococcus aureus with reduced susceptibility to vancomycin, United States, 1997-2001. Clin Infect Dis. 2003;36:429-39. (15.) Eguia JM, Liu C, Moore M, Wrone EM, Pont J, Gerberding JL, et al. Low colonization prevalence of Staphylococcus aureus with reduced vancomycin susceptibility among patients undergoing hemodialysis in the San Francisco Bay area. Clin Infect Dis. 2005;40:1617-24. Address for correspondence: Christopher J. Graber, University of California The University of California has a combined student body of more than 191,000 students, over 1,340,000 living alumni, and a combined systemwide and campus endowment of just over $7.3 billion (8th largest in the United States). , Division of Infectious Diseases, San Francisco General Hospital, 1001 Potrero Ave, Bldg 30, Box 0868, San Francisco, CA 94110, USA; email: christopher.graber@ucsf.edu Christopher J. Graber, * Margaret K. Wong, * Heather A. Carleton, * Francoise Perdreau-Remington, * Barbara L. Hailer hail·er n. 1. One that greets, acclaims, or catches someone's attention. 2. A bullhorn. , * and Henry F. Chambers * * San Francisco General Hospital, University of California, San Francisco, California, USA
Table. Antimicrobial susceptibility profiles of blood isolate from
November 2005, blood isolate from February 2006, and lumbar isolate
from April 2006 *
MIC ([micro]g/mL) and CLSI interpretation
Antimicrobial drug November February
Nafcillin >2 R 16 R
Clindamycin 21 [less than or equal to]
0.25 S
Erythromycin 41 >8 R
Trimethoprim- [less than or equal to] [less than or equal to]
sulfamethoxazole 0.5/9.5 S 0.25/5 S
Tetracycline [less than or equal to] [less than or equal to]
1 S 0.5 S ([dagger])
Rifampin [less than or equal to] [less than or equal to]
1 S 0.25 S
Ciprofloxacin >2 R >4 R
Levofloxacin >4 R ND
Gentamicin [less than or equal to] [less than or equal to]
1 S 0.5 S
Vancomycin [less than or equal to] 2 S
2 S
Daptomycin ND 1 S
Linezolid ND 2 S
Tigecycline ND 0.125 S
MIC ([micro]g/mL) and
CLSI interpretation
Antimicrobial drug April
Nafcillin >2 R
Clindamycin [less than or equal to]
0.25 S
Erythromycin >4 R
Trimethoprim- [less than or equal to]
sulfamethoxazole 0.5/9.5 S
Tetracycline [less than or equal to]
1 S
Rifampin [less than or equal to]
1 S
Ciprofloxacin >2 R
Levofloxacin >4 R
Gentamicin 2 S
Vancomycin 8 I
4-6 I ([dagger])
Daptomycin 2 ([section])
Linezolid 2 S
Tigecycline 0.125 S
* CLSI, Clinical and Laboratory Standards Institute; R, resistant;
I, intermediately resistant; S, susceptible, ND, not done.
([dagger]) Susceptibility to doxycycline performed instead of to
tetracycline.
([double dagger]) Confirmatory susceptibility by E-test and growth
on vancomycin (6 [micro]g/mL) agar screen plates.
([section]) Interpreted as nonsusceptible by the Centers for Disease
Control and Prevention. Formal CLSI breakpoints for daptomycin
resistance have not been established.
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