Infection with Scedosporium apiospermum and S. prolificans, Australia.Scedosporium apiospermum Sce·do·spor·i·um a·pi·os·per·mum n. The imperfect state of the fungus Pseudallescheria boydii, one of 16 species of fungi that may cause mycetoma in humans. and S. prolificans are fungi of increasing clinical importance, particularly in persons with underlying diseases. We reviewed the records of 59 patients in Australia from whom Scedosporium spp. were isolated from June 30, 1997, through December 31, 2003. S. apiospermum was isolated predominantly from the respiratory tracts of 28 of 31 patients with underlying lung diseases and resulted in 2 infections and 1 death. The annual number of S. apiospermum isolates remained constant. S. prolificans was isolated from 28 patients only after November 1999. Eight patients with acute myeloid leukemia myeloid leukemia n. See myelogenous leukemia. or hematopoietic stem cell Hematopoietic stem cell A cell that can develop into any type of specialized blood cell. Mentioned in: Umbilical Cord Blood Banking transplants had invasive infection; 4 had fungemia and 6 died from infection. S. prolificans caused locally invasive infection in 2 immunocompetent im·mu·no·com·pe·tent adj. Having the normal bodily capacity to develop an immune response following exposure to an antigen. im patients and was found in the respiratory tract of 18 patients with underlying respiratory disease but did not cause fungemia or deaths in these patients. Scedosporium spp. showed distinct clinical and epidemiologic features. ********** Scedosporium apiospermum and S. prolificans are saprophytic saprophytic pertaining to saprophyte. molds with a worldwide distribution. S. apiospermum, the anamorph of Pseudallescheria boydii Pseudallescheria boydii (syn. Petriellidium boydii, Allescheria boydi) perfect state of scedosporium apiospermum. , was described more than a century ago as a cause of Madura foot Madura foot see maduromycosis. and subsequently mycetoma Mycetoma Definition Mycetoma, or maduromycosis, is a slow-growing bacterial or fungal infection focused in one area of the body, usually the foot. and otitis externa Otitis Externa Definition Otitis externa refers to an infection of the ear canal, the tube leading from the outside opening of the ear in towards the ear drum. Description The external ear canal is a tube approximately 1 in (2. . Recently, it has been isolated from patients with chronic lung disease, particularly cystic fibrosis cystic fibrosis (sĭs`tĭk fībrō`sĭs), inherited disorder of the exocrine glands (see gland), affecting children and young people; median survival is 25 years in females and 30 years in males. (1,2), where the spectrum of infection ranges from colonization to disseminated infection. S. prolificans was first described as a human pathogen in 1984 (3). Scedosporium spp. cause a broad spectrum of diseases, including soft tissue infections (4-6), septic arthritis septic arthritis Acute inflammation of one or more joints caused by infection. Suppurative arthritis may follow certain bacterial infections; joints become swollen, hot, sore, and filled with pus, which erodes their cartilage, causing permanent damage if not promptly treated (7), 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. (8,9), ophthalmic infections (10-12), sinusitis sinusitis Inflammation of the sinuses. Acute sinusitis, usually due to infections such as the common cold, causes localized pain and tenderness, nasal obstruction and discharge, and malaise. (13), pneumonia (14,15), meningitis and brain abscesses (16,17), endocarditis endocarditis (ĕn'dōkärdī`tĭs), bacterial or fungal infection of the endocardium (inner lining of the heart) that can be either acute or subacute. (18), and disseminated infection (8,18-21). Patients at risk include those immunocompromised immunocompromised /im·mu·no·com·pro·mised/ (-kom´pro-mizd) having the immune response attenuated by administration of immunosuppressive drugs, by irradiation, by malnutrition, or by certain disease processes (e.g., cancer). because of advanced 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. infection (6,18,20), immunosuppressive therapy Immunosuppressive therapy Medical treatment in which the immune system is purposefully thwarted. Such treatment is necessary, for example, to prevent organ rejection in transplant cases. and neutropenia Neutropenia Definition Neutropenia is an abnormally low level of neutrophils in the blood. Neutrophils are white blood cells (WBCs) produced in the bone marrow that ingest bacteria. (6,18 21), or intravenous drug use intravenous drug use Intravenous drug abuse The habitual IV injection of drugs of abuse Epidemiology In the US ± 2.5 million–population ± 235 million have used IVDs Infections Pyogenic–eg, endocarditis, pneumonia, sepsis Common agents (6,20). In the final months of 1999 during construction work, an increased number of Scedosporium spp. isolates and S. prolificans were noted at Alfred Hospital, a university hospital in Prahran, Victoria, Australia, that provides statewide trauma, burn, cystic fibrosis, heart and lung transplant lung transplant Surgery Transplant of a lung allograft into a Pt with failing lungs; 90 US centers perform LT; 35 centers perform ≥ 10/yr Mean wait time 18 months Indications COPD–eg, emphysema due to α1 , and HIV services. The records of all patients from whom Scedosporium spp. were isolated from June 30, 1997, through December 31, 2003, were reviewed to describe the epidemiology, clinical features, and outcomes of these infections. Methods Data Collection Records of all patients with Scedosporium spp. cultured between June 30, 1997, and December 31, 2003, were reviewed retrospectively, and demographics, primary illness, antifungal therapy, and presence of other pathogens, and outcomes were recorded. Immunocompromised patients were defined as those with impairment of either or both natural and specific immunity specific immunity n. Immunity against a specific antigen or disease. to infection (22). Those with localized impaired host defenses caused by underlying diseases such as cystic fibrosis were classified as immunocompetent. Invasive infection was defined as a tissue biopsy specimen with hyphae hy·pha n. pl. hy·phae Any of the threadlike filaments forming the mycelium of a fungus. [New Latin, from Greek huph plus culture of the organism (23). Disseminated infection was defined as positive blood cultures or infection at [greater than or equal to]2 noncontiguous sites within 7 days. Neutropenia was defined as an absolute neutrophil count Absolute neutrophil count (ANC) is a measure of the number of neutrophil granulocytes (also known as polymorphonuclear cells, PMN's, polys, granulocytes, segmented neutrophils or segs) present in the blood. Neutrophils are a type of white blood cell that fights against infection. <0.5 cells/[mm.sup.3]. Descriptive statistics descriptive statistics see statistics. and odds ratios were calculated by using STATA release 8.0 (Stata Corporation, College Station, TX, USA.) Laboratory Methods and Epidemiology Scedosporium spp. were identified after culture onto horse blood agar blood agar n. A nutrient culture medium that is enriched with whole blood and used for the growth of certain strains of bacteria. and Sabaroud dextrose dextrose: see glucose. agar (SDA SDA abbr. specific dynamic action Serotonin dopamine antagonist (SDA) The newer second-generation antipsychotic drugs, also called atypical antipsychotics. ) and incubation at 300C and 370C. Colonies were rapid-growing, gray-white, and downy down·y adj. down·i·er, down·i·est 1. Made of or covered with down. 2. a. Resembling down: downy white clouds. b. Quietly soothing; soft. Adj. , with a gray-black reverse side. Species were differentiated by microscopic morphology (24). Susceptibility testing was performed according to Clinical and Laboratory Standards Institute methods (25) and synergy studies (2-dimensional 2-agent microdilution checkerboard checkerboard the pattern of a chess or draft board; used in many circumstances to display the results of mixing a specific number of variables. The variables are listed in columns designated along the horizontal border and the same or different variables in lines along the vertical method) (26). Synergy was a summation of the fractional inhibitory concentration [less than or equal to]0.500. For comparison of temporal patterns of mold isolates, the number of persons with Scedosporium spp. during the 3 years subsequent to this review (2004--2006) and Aspergillus Aspergillus Any fungus of the genus Aspergillus of the Fungi Imperfecti (form-class Deuteromycetes). Species for which the sexual phase is known are placed in the order Eurotiales. A. niger causes black mold on some foods; A. niger, A. flavus, and A. spp. for 1999-2005 were extracted from laboratory databases. Rates of detection were expressed as per 1,000 separations and per 100,000 inpatient-patient days. Environmental Sampling From March 2001 through July 2002, environmental samples were collected from hospital public access areas within and adjacent to the construction site on 7 separate occasions. Additional sampling was conducted in ward corridors, nursing stations, patient rooms, and the patient car park. Air sampling was conducted with a portable high-volume air sampler (MAS 100; Merck, Darmstadt, Germany). The volume of air sampled at each site was 1,000 L/10 min (1 [m.sup.3]). Settle plates were placed in ward corridors and patient rooms for 60 min of exposure. Dust was collected from horizontal surfaces with sterile swabs moistened with sterile saline. Dust and soil specimens were directly placed on standard SDA and selective SDA containing amphotericin B amphotericin B (ăm'fətĕr`ĭsĭn), antibiotic that halts the growth of several disease-causing fungi. Discovered in 1956, it is produced by bacteria of the genus Streptomyces. and incubated at 27[degrees]C. Results From June 1997 through December 2003, a total of 59 isolates of Scedosporium spp. were cultured from 56 patients. S. apiospermum was isolated from 31 patients, and S. prolificans was isolated from 28 patients. Both species were isolated from 3 patients at separate times (12 days, 13 months, and 27 months apart, respectively). Demographic information, coinfections, and outcomes of the patients are shown according to the species isolated (Table 1). During the period of this review, an average of 28 allogeneic allogeneic /al·lo·ge·ne·ic/ (-je-ne´ik) 1. having cell types that are antigenically distinct. 2. in transplantation biology, denoting individuals (or tissues) that are of the same species but antigenically stem cell stem cell In living organisms, an undifferentiated cell that can produce other cells that eventually make up specialized tissues and organs. There are two major types of stem cells, embryonic and adult. , 35 lung, 27 heart, and 15 renal transplants were performed each year. S. apiospermum S. apiospermum was isolated from 32 specimens collected from 31 patients. Twenty-nine isolates were from the respiratory tract; sputum sputum /spu·tum/ (spu´tum) [L.] expectoration; matter ejected from the trachea, bronchi, and lungs through the mouth. sputum cruen´tum bloody sputum. (n = 22), bronchoalveolar lavage Bronchoalveolar lavage A way of obtaining a sample of fluid from the airways by inserting a flexible tube through the windpipe. Used to diagnose the type of lung disease. (BAL (1) (Basic Assembly Language) The assembly language for the IBM 370/3000/4000 mainframe series. (2) (Branch And Link) An instruction used to transfer control to another part of the program. BAL - Basic Assembly Language ) (n = 5), sinus (n = 1), and lung tissue (n = 1). The remaining 3 isolates were from brain tissue, a central venous catheter central venous catheter n. A catheter passed through a peripheral vein and ending in the thoracic vena cava; it is used to measure venous pressure or to infuse concentrated solutions. tip, and an ear swab, respectively. No blood cultures were positive for S. apiospermum. S. apiospermum was isolated concurrently with Aspergillus spp. from the respiratory tracts of 9 (29%) of the 31 patients. Twenty-one (68%) of the 31 patients were immunocompromised. Thirteen had undergone solid organ transplantation The transfer of organs such as the kidneys, heart, or liver from one body to another. The transplantation of human organs has become a common medical procedure. Typical organs transplanted are the kidneys, heart, liver, pancreas, cornea, skin, bones, and lungs. (11 had lung transplants and 2 had heart transplants), 4 had malignancies (3 had metastatic cancer Metastatic cancer A cancer that has spread to an organ or tissue from a primary cancer located elsewhere in the body. Mentioned in: Liver Cancer metastatic cancer and 1 had chronic lymphocytic leukemia chronic lymphocytic leukemia n. Abbr. CLL Lymphocytic leukemia occurring mainly in older adults, characterized by slow onset and gradual progression of symptoms. ), 3 had advanced HIV infection, and 1 was receiving immunosuppressive therapy for rheumatoid arthritis rheumatoid arthritis Chronic, progressive autoimmune disease causing connective-tissue inflammation, mostly in synovial joints. It can occur at any age, is more common in women, and has an unpredictable course. . All 10 immunocompetent patients had chronic respiratory tract disease; cystic fibrosis (n = 5), bronchiectasis bronchiectasis Abnormal expansion of bronchi in the lungs. It usually results when preexisting lung disease causes bronchial inflammation and obstruction. Bronchial wall fibres degenerate, and bronchi become dilated or paralyzed, preventing removal of secretions, which (n = 4) and chronic mastoiditis mastoiditis Inflammation of the mastoid process, a bony projection just behind the ear, almost always due to otitis media. It may spread into small cavities in the bone, blocking their drainage. Very severe cases infect the whole middle ear cleft. (n = 1). Three patients were lost to follow-up after isolation of S. apiospermum. The remaining 28 patients were followed up for a total of 981 months. The mean duration of follow-up was 35 months (median 16 months, range 1-96 months). Two (6%) of the 31 patients had invasive infections. The first patient was a woman who received a lung transplant 5 years earlier and was previously colonized Colonized This occurs when a microorganism is found on or in a person without causing a disease. Mentioned in: Isolation with Aspergillus spp. but not S. apiospermum. She had pulmonary and cerebral lesions and was treated with amphotericin B deoxycholate and itraconazole itraconazole /it·ra·co·na·zole/ (it?rah-kon´ah-zol) a triazoleantifungal used in a variety of infections. it·ra·con·a·zole n. for presumed aspergillosis Aspergillosis Definition Aspergillosis refers to several forms of disease caused by a fungus in the genus Aspergillus. Aspergillosis fungal infections can occur in the ear canal, eyes, nose, sinus cavities, and lungs. . S. apiospermum was isolated from postmortem postmortem /post·mor·tem/ (post-mort´im) performed or occurring after death. post·mor·tem adj. Relating to or occurring during the period after death. n. See autopsy. lung and brain tissue. The second patient was a man who had advanced HIV infection with fungal sinusitis on biopsy. He was treated with voriconazole and surgery but died 3 months later from infection with cytomegalovirus cytomegalovirus (sī'təmĕg'əlōvī`rəs), member of the herpesvirus family that can cause serious complications in persons with weakened immune systems. . There were 6 deaths within 1 month of isolation of S. apiospermum. All deaths occurred in immunocompromised patients but only 1 was directly attributable to S. apiospermum. The other deaths resulted from the underlying condition. Four patients with chronic lung disease were receiving itraconazole for treatment of Aspergillus spp. infection at the time S. apiospermum was isolated. Three of these patients died of respiratory failure Respiratory Failure Definition Respiratory failure is nearly any condition that affects breathing function or the lungs themselves and can result in failure of the lungs to function properly. 7, 9, and 16 months, respectively, after isolation of S. apiospermum, and 1 was alive when last seen 96 months after fungal isolation. Seven patients received antifungal therapy after isolation of S. apiospermum from respiratory tract samples (4 received voriconazole and 3 received itraconazole). These 7 patients had HIV infection and sinusitis (n = 2), had undergone lung transplantation (n = 3) or had bronchiectasis or cystic fibrosis (n = 2). Both patients with HIV infection had sinusitis and died within 7 months of complications of HIV. Of the other 5 patients, 4 who received azole az·ole n. A class of organic compounds having a five-membered heterocyclic ring with two double bonds; pyrrole. azole therapy remained well without invasive infection at 32, 41, 48, and 88 months, respectively, of follow-up. The remaining treated patient died 15 months later; death was not attributed to fungal infection. The median duration of follow-up of those treated with azoles at the time of fungal isolation or subsequent to isolation was 16 months (range 3-96 months); S. apiospermum was not subsequently detected in these patients. The median duration of follow-up for patients receiving no treatment after fungal isolation was 19 months (range 1-84 months); S. apiospermum was isolated from 4 of these patients 1, 18, 30, and 36 months, respectively, after initial fungal isolation. S. prolificans S. prolificans was isolated from 46 specimens obtained from 28 patients. Fourteen (50%) of the 28 patients were immunocompetent. Most (12/14, [86%]) specimens from immunocompetent patients were from the respiratory tract; cystic fibrosis (n = 6), chronic airway disease (n = 3), nasal discharge and sinus aspirates with chronic sinusitis (n = 3). Patients with cystic fibrosis or airway disease were not considered to have invasive disease and none received antifungal therapy. All 3 patients with chronic sinusitis were treated with surgery, and 2 received itraconazole. One isolate was from knee cartilage of a patient with hemophilia, osteoarthritis osteoarthritis or osteoarthrosis or degenerative joint disease Most common joint disorder, afflicting over 80% of those who reach age 70. It does not involve excessive inflammation and may have no symptoms, especially at first. , and a knee replacement; the patient underwent surgery and received itraconazole. S. prolificans was also isolated from a skin-biopsy specimen from a patient with multiple-trauma 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. who was treated only with surgery. There were no cases of disseminated infection or deaths resulting from S. prolificans in these immunocompetent patients. S. prolificans was isolated from 14 immunocompromised patients. Immunodeficiency was caused by lung transplantation (n = 6), hematopoietic stem cell transplantation hematopoietic stem cell transplantation Hematology A therapy in which defective hematopoietic cells are replaced with normal BM cells after chemotherapy and/or RT Indications AML, breast CA, CML, germ cell tumors, lymphoma, myelodysplastic syndrome, myeloma, (HSCT HSCT Hematopoietic Stem Cell Transplant HSCT High Speed Civil Transport HSCT High School Competency Test HSCT Hypersonic Commercial Transport HSCT Hygiène Sécurité Conditions de Travail en Collectivité Territoriale HSCT Hayling Sentence Completion Task ) (n = 6), acute myeloid leukemia (AML AML - A Manufacturing Language ), and myelodysplastic syndrome (MDS MDS, n See temporomandibular pain-dysfunction syndrome. MDS 1 Maternal deprivation syndrome, see there 2 Myelodysplastic syndrome, see there ). S. prolificans was isolated from BAg of 6 lung transplant recipients. One patient was receiving itraconazole for Aspergillus spp. infection, 3 were receiving voriconazole, and 2 were receiving itraconazole and voriconazole with terbinafine, Invasive disease did not develop in any of the 4 lung transplant recipients who received antifungal treatment and none died. Two lung transplant recipients did not receive antifungal treatment. One of these patients was lost to follow-up and 1 survived >25 months without developing invasive infection, although S. prolificans was isolated again 1 year later. S. prolificans was isolated from August 2000 through September 2002 from 6 patients undergoing allogeneic HSCT and from 2 patients with hematologic malignancy. Four of the 6 HSCT recipients had positive blood cultures, and 4 recipients had skin lesions (multiple, nodular nodular marked with, or resembling, nodules. nodular dermatofibrosis see dermatofibrosis. nodular episcleritis see nodular fasciitis (below). nodular fasciitis a firm painless nodular swelling, 0. ). Findings for 8 patients in whom invasive disease developed are summarized in Table 2. Patients 1, 2, and 6 had HSCT complicated by chronic extensive refractory graft versus host disease Graft versus host disease A life-threatening complication of bone marrow transplants in which the donated marrow causes an immune reaction against the recipient's body. Mentioned in: Bone Marrow Transplantation (GVHD GVHD graft-versus-host-disease. GVHD Graft-versus-host disease, see there ). All 3 died of invasive infection despite treatment with itraconazole or voriconazole and terbinafine; 2 had positive blood cultures. Infections developed in patients 3, 4, and 5 during neutropenia after HSCT. Two of them had positive blood cultures, and both died. Patient 4 received no antifungal treatment, and patient 5 died despite replacement of prophylactic itraconazole with empiric amphotericin B. Patient 3, described elsewhere (8), survived after treatment with voriconazole, terbinafine, surgery, and neutrophil neutrophil /neu·tro·phil/ (noo´tro-fil) 1. a granular leukocyte having a nucleus with three to five lobes connected by threads of chromatin, and cytoplasm containing very fine granules; cf. heterophil. 2. recovery. Patient 7 had MDS and preceding idiopathic CD4-cell lymphocytopenia. S. prolificans was isolated from sputum, but not BAL, and this patient was not treated. One month later, S. prolificans sinusitis was diagnosed. Despite surgery and treatment with itraconazole, followed by voriconazole and terbinafine, the patient died. Patient 8, a woman, was neutropenic after remission-induction chemotherapy for AML. A swab from a Hickman catheter exit site was positive for S. prolificans. Subsequently, chest wall cellulitis, deep soft tissue infection, and multiple skin nodules Nodules A small mass of tissue in the form of a protuberance or a knot that is solid and can be detected by touch. Mentioned in: Leprosy developed. She was treated with surgery, voriconazole, and terbinafine. Her neutropenia resolved and she recovered. After isolation of S. prolificans, 5 of 28 patients were lost to follow-up. The remaining 23 were followed up for a total of 517 months. Mean length of follow-up was 22.5 months (median 9 months, range 1-68 months). Invasive infection occurred in 10 (36%) of 28 infected with S. prolificans compared with 2 (6%) of 31 infected with S. apiospermum. Deaths caused by scedosporiosis occurred in 5 (18%) of 28 infected with S. prolificans and 1 (3%) of 31 infected with S. apiospermum. All deaths occurred in immunocompromised patients; 6 (43%) of 14 infected with S. prolificans and 1 (5%) of 21 infected with S. apiospermum (odds ratio 6.0, 95% confidence interval 0.78-45.62, p = 0.05). Drug-Susceptibility Testing Drug-susceptibility testing was performed on 7 S. prolificans isolates. MICs (mg/L) were >16 for amphotericin B, >64 for fluconazole fluconazole /flu·con·a·zole/ (floo-kon´ah-zol) a triazoleantifungal used in the systemic treatment of candidiasis and cryptococcal meningitis. flu·con·a·zole n. , >8 for itraconazole, >64 for 5-fluorocytosine, and >16 for ketoconazole ketoconazole /ke·to·co·na·zole/ (ke?to-kon´ah-zol) a derivative of imidazole used as an antifungal agent. ke·to·co·na·zole n. , 2-8 for voriconazole, and 1-4 for terbinafine. Terbinafine and itraconazole were synergistic for 3 of 6 isolates tested, and terbinafine and voriconazole were synergistic for 5 of 7 isolates tested. Four S. apiospermum isolates tested had MICs of 0.5-1 mg/L for itraconazole and 0.5 mg/L for voriconazole. Epidemiology of Scedosporium spp. and Aspergillus spp. Throughout the study, S. apiospermum was isolated at a constant rate (Figure) of 3-6 isolates per year with no seasonal clustering. In contrast, S. prolificans was first detected in December 1999, and thereafter [approximately equal to]8 isolates were identified annually. Detection of S. prolificans continued in 2004 with 8 isolates but decreased to 6 in 2005 and 4 in 2006. Two clusters of infection occurred in autumn 2001 and 2003 during periods of hospital building that required deep excavation. Air, dust, and soil sampling did not detect an environmental fungal source. Aspergillus spp. were detected during 1999-2005 (mean 191 persons per year, range 153-230). Detection rates for Scedosporium spp. and Aspergillus spp. for 2003-2005 were 0.1-0.23/1,000 separations and 2-3/100,000 inpatient-patient days and 2.4-3.0/1,000 separations and 53-75/100,000 inpatient-patient days, respectively. [FIGURE OMITTED] Discussion This study describes the epidemiology of Scedosporium infection in a cohort of contemporaneous patients at a university hospital. The single-center approach, with cases identified by laboratory detection, allows capture of the full spectrum of infection from colonization to invasive infection. Scedosporium spp. were detected in a broad range of patients and clinical settings. However, there were distinct differences in epidemiology, clinical manifestations, antifungal susceptibility patterns, and outcomes between S. prolificans and S. apiospermum. Previous reviews have focused on invasive cases reported (10,27,28), but this approach is limited by both selection and publication bias (29) and does not describe the natural history of infection or the prevalence of these infections. Our series enables the annual incidence of cases, ratio of colonized to infected patients, and natural history of colonization to be determined for each species. We showed that invasive infections accounted for only 6% of S. apiospermum isolates and for 46% of S. prolificans isolates, and that isolation of Aspergillus spp. was 20-30 times more frequent than that of Scedosporium spp. S. apiospermum and S. prolificans are colonizers of abnormal airways caused by bronchiectasis, cystic fibrosis, chronic obstructive pulmonary disease chronic obstructive pulmonary disease n. Abbr. COPD A chronic lung disease, such as asthma or emphysema, in which breathing becomes slowed or forced. , or lung transplantation (1,2,6,18,30,31). S. apiospermum was an airway colonizer col·o·nize v. col·o·nized, col·o·niz·ing, col·o·niz·es v.tr. 1. To form or establish a colony or colonies in. 2. To migrate to and settle in; occupy as a colony. 3. in [less than or equal to]10% of patients with cystic fibrosis in France and Australia (1,2), and similar proportions of lung transplant recipients were colonized with 1 or both species at 1 center in Australia (31). However, there are few reports that S. prolificans colonized patients with lung disease (6,32). In the present study, S. prolificans was identified as an airway colonizer only after December 1999. The onset of invasive infections in HSCT and neutropenic patients occurred in August 2000. S. prolificans was first detected at the M.D. Anderson Cancer Center in Houston, Texas, after 2001 (19). Emergence of S. prolificans may be related to an environmental source that was not identified or selection pressure caused by changes in antifungal prophylaxis practices (33). This finding did not appear to be the explanation in our patients because fluconazole remains standard prophylaxis for neutropenia, and itraconazole was used in only 1 of 8 patients. Other possible explanations include use of more aggressive chemotherapy regimens in patients with acute leukemia and the advent of nonmyeloablative allografts allografts (al´  graf´ts),n.pl the transplantation of tissue between genetically nonidentical individuals of the same species. , which change characteristics of patients selected for transplants. The reason for persistence of this organism over several years after its initial appearance is also unclear but has also been observed by others (19). In patients with respiratory tract disease, both Scedosporium spp. were isolated in comparable numbers. However, the only invasive infection in this diverse group was disseminated S. apiospermum 5 years after lung transplantion. The outcome of 19 patients who had undergone lung or heart lung transplantation and were colonized with this fungus was comparable to the 17 patients in the immunocompetent group with airways disease caused by cystic fibrosis, bronchiectasis, or chronic obstructive pulmonary disease. As in other reports, other opportunistic pathogens, especially Aspergillus spp. (present in one third), were commonly cultured simultaneously (1,18,30,31). In lung transplant recipients, Scedosporium spp. in BAL was associated with advanced bronchiolitis obliterans and airway stenosis (31), which emphasizes the difficulty of interpreting the role of Scedosporium spp. in this group. Whether colonization follows airway damage, immunosuppression immunosuppression Suppression of immunity with drugs, usually to prevent rejection of an organ transplant. Its aim is to allow the recipient to accept the organ permanently with no unpleasant side effects. , or antifungal therapy to treat Aspergillus spp. colonization or is itself an ongoing cause of airway damage such as bronchiolitis obliterans is unknown. In our study group, most patients with respiratory tract colonization had not received antifungal therapy. Although antifungal treatment was used in [approximately equal to]50% of patients with S. apiospermum airway colonization, there appeared to be no survival advantage in patients treated; our study was not a randomized ran·dom·ize tr.v. ran·dom·ized, ran·dom·iz·ing, ran·dom·iz·es To make random in arrangement, especially in order to control the variables in an experiment. comparison. With S. prolificans respiratory tract colonization, too few patients were treated with antifungal drugs for valid conclusions to be made. There was no reduction in survival in 5 untreated patients with isolates of either S. apiospermum or S. prolificans. The role of Scedosporium spp. respiratory tract colonization requires further evaluation. Allogeneic HSCT and AML/MDS were the only settings in which S. prolificans was more common than S. apiospermum. There were no S. apiospermum infections in these patients, although in at 1 US cancer center, S. apiospermum infections were more common (19). This may reflect different geographic distributions of Scedosporium spp. In our study, S. prolificans caused illness with high mortality rates in HSCT and leukemia patients. In HSCT recipients, S. prolificans infections occurred equally in those with neutropenia (early after transplant) and GVHD (later after transplant). Thus, host factors unique to AML and HSCT, such as neutropenia, GVHD, associated macrophage macrophage /mac·ro·phage/ (mak´ro-faj) any of the large, mononuclear, highly phagocytic cells derived from monocytes that occur in the walls of blood vessels (adventitial cells) and in loose connective tissue (histiocytes, phagocytic dysfunction, and environmental exposure, may play a role in the propensity for invasive infection with S. prolificans in this group. As in previous reports (10,32), neutropenic patients had sepsis, positive blood cultures, and overwhelming infection (often associated with disseminated rash). In nonneutropenic patients, infection was more likely to be localized initially in lungs, joints, or sinuses. The ability of S. prolificans to grow in blood cultures in AML and HSCT patients is well recognized (10,34), and this diagnosis, or infection with Fusarium Fusarium a genus of fungi; some species are plant pathogens and some are opportunistic infectious agents of humans and animals. Many also produce trichothecene toxins which cause poisoning of animals if the infected material, usually stored feed, is eaten. spp., should be considered when a mold is cultured from blood. In our study, S. prolificans was the only species to grow in blood culture, although others have reported S. apiospermum, albeit, less frequently (10,18,19). Although colonization with S. prolificans without progression to disease was observed in patients with respiratory disease and after lung transplantation, this was not observed in 3 patients with AML/MDS or HSCT. A nonsterile site swab or sputum culture yielding S. prolificans was soon followed by a diagnosis of invasive infection, which indicated that in these patients a culture result, even from a nonsterile site, should be viewed seriously. The clinical findings of S. prolificans in our patients suggest that this fungus is more invasive than S. apiospermum, as has been found in mice (35). In addition to disseminated infection in AML patients and HSCT recipients, S. prolificans also caused locally invasive disease in patients who were not immunocompromised, such as those with posttrauma cellulitis, septic arthritis in a damaged joint, and sinus disease. One proposed mechanism for virulence of S. prolificans is melanin melanin (mĕl`ənĭn), water-insoluble polymer of various compounds derived from the amino acid tyrosine. It is one of two pigments found in human skin and hair and adds brown to skin color; the other pigment is carotene, which contributes in the cell wall (27). Antifungal therapy is problematic with S. prolificans with high MICs for amphotericin B, echinocandins, and azoles. This finding has stimulated interest in combinations of voriconazole and terbinafine (26), voriconazole and echinocandin (36), or polyene polyene /pol·y·ene/ (pol´e-en) 1. a chemical compound with a carbon chain of four or more atoms and several conjugated double bonds. 2. any of a group of antifungal antibiotics with such a structure (e.g. and echinocandin (36). However, these infections are rare and experience is limited to case reports (8,9,36). In vitro treatment with interferon-[gamma] and granulocyte-macrophage--colony-stimulating factor has improved neutrophil function against S. prolificans hyphae (37). Surgery appears to be an important factor in survival in our cases, as well as other series (10). Although surgery and antifungal therapy were successful in 2 neutropenic patients with invasive S. prolificans infections, these patients also had concomitant neutrophil recovery that could explain their survival. Much needs to be learned about the epidemiology, transmission, pathogenesis, and environmental niche of Scedosporium spp., especially S. prolificans. A source for emergence of S. prolificans at our hospital was investigated, but none was identified. Our inability to detect the source of emergent S. prolificans was puzzling, although exposure and colonization may have occurred by the time the first case was seen. Cultures may have been obtained too late to identify environmental contamination, although changes in immunosuppression in the population at risk may also have contributed. S. prolificans appeared first as a colonizer of abnormal airways 8 months before the first invasive infection in an HSCT recipient. Shifts in the epidemiology of colonizing organisms in this patient group during hospital construction may be worthy of closer attention and surveillance. Molecular typing methods such as PCR PCR polymerase chain reaction. PCR abbr. polymerase chain reaction Polymerase chain reaction (PCR) (38) and inter-simple sequence repeat PCR fingerprinting (39) have distinguished genotypes from outbreaks and different geographic regions. Recently, S. apiospermum complex has been shown to include several individual species indistinguishable morphologically (40). These methods will be used for further investigation of our isolates as part of a larger Australian surveillance study In conclusion, S. prolificans and S. apiospermum are pathogenic fungi that demonstrate distinct clinical features dependent on the immune function of the host and the type of species isolated. They are usually found in patients with underlying disease, although occasionally after trauma. S. prolificans emerged as a major pathogen in allogeneic HSCT recipients and as a colonizer of patients with underlying lung disease. Madura foot is now rare and was not observed in this series. The high attributable mortality rate of invasive infection with both Scedosporium spp., limitations of antifungal therapy, necessity for aggressive and deforming surgery to treat infections with S. prolificans, and uncertainty over the role of airway colonization emphasize the need to better understand the epidemiology and pathogenesis of this infection. Acknowledgments We thank Glenys Harrington and Claire Franklin for investigating outbreak and environmental sampling, the clinicians and nurses at Alfred Hospital for providing patient care, and David Ellis and Rosie Handke for antifungal susceptibility testing. Dr Cooley is a medical microbiologist and director of Infectious Diseases at Royal Hobart Hospital The Royal Hobart Hospital (RHH or 'The Royal' as its often known) is the largest hospital in Tasmania, Australia. It is a public hospital managed by the Tasmanian Government. 'The Royal' is located in central Hobart. . Her research interests include diagnosis and management of infections in the immunocompromised host. References (1.) Cimon B, Carrere J, Vinatier JF, Chazalette JP, Chabasse D, Bouchara JP. Clinical significance of Scedosporium apiospermum in patients with cystic fibrosis. Eur J Clin Microbiol Infect Dis. 2000;19:53-6. (2.) Williamson EC, Speers D, Arthur IH, Harnett G, Ryan G, Inglis TJ. Molecular epidemiology of Scedosporium apiospermum infection determined by PCR amplification of ribosomal intergenic spacer sequences in patients with chronic lung disease. J Clin Microbiol. 2001;39:47-50. (3.) Salkin IF, McGinnis MR, Dykstra MJ, Rinaldi MG. Scedosporium in inflatum, an emerging pathogen. J Clin Microbiol. 1988;26:498-503. (4.) Schaenman JM, Digiulio DB, Mirels LF, McClenny NM, Berry GJ, Fothergill AW, et al. Scedosporium apiospermum soft tissue infection successfully treated with voriconazole: potential pitfalls in the transition from intravenous to oral therapy. J Clin Microbiol. 2005;43:973-7. (5.) Karaarslan A, Arikan S, Karaarslan F, Cetin ES. Skin infection caused by Scedosporium apiospermum. Mycoses. 2003 ;46:524-6. (6.) Wood GM, McCormack JG, Muir DB, Ellis DH, Ridley MF, Pritchard R, et al. Clinical features of human infection with Scedosporium inflatum. Clin Infect Dis. 1992;14:1027-33. (7.) Tirado-Miranda R, Solera-Santos J, Brasero JC, Haro-Estarriol M, Cascales-Sanchez P, Igualada JB. Septic arthritis due to Scedosporium apiospermum: case report and review. J Infect. 2001;43:210-2. (8.) Howden BP, Slavin MA, Schwarer AP, Mijch AM. Successful control of disseminated Scedosporium prolificans infection with a combination of voriconazole and terbinafine. Eur J Clin Microbiol Infect Dis. 2003;22:111-3. (9.) Steinbach WJ, Schell WA, Miller JL, Perfect JR. Scedosporium prolificans osteomyelitis in an immunocompetent child treated with voriconazole and caspofungin, as well as locally applied polyhexamethylene biguanide Biguanides (ATC A10 BA) form a class of oral antihyperglycemic drugs used for diabetes mellitus or prediabetes treatment. Examples Examples of biguanides:
(10.) Husain S, Munoz P, Forrest G, Alexander BD, Somani J, Brennan K, et al. Infections due to Scedosporium apiospermum and Scedosporium prolificans in transplant recipients: clinical characteristics and impact of antifungal agent therapy on outcome. Clin Infect Dis. 2005 ;40:89-99. (11.) Vagefi MR, Kim ET, Alvarado RG, Duncan JL, Howes EL, Crawford JB. Bilateral endogenous Scedosporium prolificans endophthalmitis after lung transplantation. Am J Ophthalmol. 2005;139:370-3. (12.) Leck A, Matheson M, Tuft S, Waheed K, Lagonowski H. Scedosporium apiospermum keratomycosis with secondary endophthalmitis. Eye. 2003;17:841-3. (13.) Eckburg PB, Zolopa AR, Montoya JG. Invasive fungal sinusitis due to Scedosporium apiospermum in a patient with AIDS. Clin Infect Dis. 1999;29:212-3. (14.) Al Refai M, Duhamel C, Le Rochais JP, Icard P. Lung scedosporiosis: a differential diagnosis of aspergillosis. Eur J Cardiothorac Surg. 2002;21:938-9. (15.) Jabado N, Casanova JL, Haddad E, Dulieu F, Fournet JC, Dupont B, et al. Invasive pulmonary infection due to Scedosporium apiospermum in two children with chronic granulomatous disease Chronic Granulomatous Disease Definition Chronic granulomatous disease (CGD) is an inherited disorder in which white blood cells lose their ability to destroy certain bacteria and fungi. . Clin Infect Dis. 1998;27:1437-41. (16.) Danaher PJ, Walter EA. Successful treatment of chronic meningitis caused by Scedosporium apiospermum with oral voriconazole. Mayo Clin Proc. 2004;79:707-8. (17.) Nesky MA, McDougal EC, Peacock JE Jr. Pseudallescheria boydii brain abscess successfully treated with voriconazole and surgical drainage: case report and literature review of central nervous system pseudallescheriasis. Clin Infect Dis. 2000;31:673-7. (18.) Guarro J, Kantarcioglu AS, Horre R, Rodriguez-Tudela JL, Cuenca Estrella M, Berenguer J, et al. Scedosporium apiospermum: changing clinical spectrum of a therapy-refractory opportunist. Med Mycol. 2006;44:295-327. (19.) Lamaris GA, Chamilos G, Lewis RE, Safdar A, Raad II, Kontoyiannis DP. Scedosporium infection in a tertiary care cancer center: a review of 25 cases from 1989-2006. Clin Infect Dis. 2006;43:1580-4. (20.) Berenguer J, Rodriguez-Tudela JL, Richard C, Alvarez M, Sanz MA, Gaztehlurrutia L, et al. Deep infections caused by Scedosporium prolificans. A report on 16 cases in Spain and a review of the literature. Scedosporium prolificans Spanish Study Group. Medicine (Baltimore). 1997;76:256-65. (21.) Idigoras P, Perez-Trallero E, Pineiro L, Larruskain J, Lopez-Lopategui MC, Rodriguez N, et al. Disseminated infection and colonization by Scedosporium prolificans: a review of 18 cases, 1990-1999. Clin Infect Dis. 2001;32:E158-65. (22.) Rubin RH, Young LW, editors. Clinical approach to infection in the compromised host. 4th ed. New York: Kluwer Academic/Plenum Publishers; 2002. (23.) Ascioglu S, Rex JH, de Pauw B, Bennett JE, Bille J, Crokaert F, et al. Defining opportunistic invasive fungal infections in immunocompromised patients with cancer and hematopoietic stem cell transplants: an international consensus. Clin Infect Dis. 2002;34:7-14. (24.) Dixon DM, Polak-Wyss A. The medically important dematiaceous fungi and their identification. Mycoses. 1991 ;34:1-18. (25.) Clinical and Laboratory Standards Institute (CLSI CLSI Clinical and Laboratory Standards Institute (Wayne, PA) CLSI Cisco Link Services Interface ). Reference method for broth dilution. Antifungal susceptibility testing of filamentous filamentous /fil·a·men·tous/ (fil?ah-men´tus) composed of long, threadlike structures. filamentous composed of long, threadlike structures. fungi; CLSI document 38-A. Wayne (PA): the Institute; 2002. (26.) Meletiadis J, Mouton mouton lamb pelt made to resemble seal or beaver. JW, Meis JF, Verweij PE. In vitro drag interaction modeling of combinations of azoles with terbinafine against clinical Scedosporium prolificans isolates. Antimicrob Agents Chemother. 2003;47:106-17. (27.) Revankar SG, Patterson JE, Sutton DA, Pullen R, Rinaldi MG. Disseminated phaeohyphomycosis: review of an emerging mycosis mycosis: see fungal infection. . Clin Infect Dis. 2002;34:467-76. (28.) Maertens J, Lagrou K, Deweerdt H, Sunnont I, Verhoef GE, Verhaegen J, et al. Disseminated infection by Scedosporium prolificans: an emerging fatality among haematology patients. Case report and review. Ann Hematol. 2000;79:340-4. (29.) Easterbrook PJ, Berlin JA, Gopalan R, Matthews DR. Publication bias in clinical research. Lancet. 1991 ;337:867-72. (30.) Travis LB, Roberts GD, Wilson WR. Clinical significance of Pseudallescheria boydii: a review of l0 years' experience. Mayo Clin Proc. 1985;60:531-7. (31.) Tamm M, Malouf M, Glanville A. Pulmonary Puhnonary Scedosporium infection following lung transplantation. Transpl Infect Dis. 2001;3:189-94. (32.) del Palacio A, Garau M, Amor E, Martinez-Alonso I, Calvo T, Carrillo-Munoz A, et al. Case reports. Transient colonization with Scedosporium prolificans. Report of four cases in Madrid. Mycoses. 2001;44:321-5. (33.) Imhof A, Balajee SA, Fredricks DN, Englund JA, Marr KA. Breakthrough fungal infections in stem cell transplant recipients receiving voriconazole. Clin Infect Dis. 2004;39:743-6. (34.) Lionakis MS, Bodey GP, Tarrand JJ, Raad II, Kontoyiannis DP. The significance of blood cultures positive for emerging saprophytic moulds in cancer patients. Clin Microbiol Infect. 2004;10:922-5. (35.) Ortoneda M, Pastor FJ, Mayayo E, Guarro J. Comparison of the virulence of Scedosporium prolificans strains from different origins in a murine murine /mu·rine/ (mur´en) pertaining to, derived from, or characteristic of mice or rats. mu·rine adj. model. J Med Microbiol. 2002;51:924-8. (36.) Nivoix Y, Zamfir A, Lutun P, Kara F, Remy V, Lioure B, et al. Combination of caspofungin and an azole or an amphotericin B formulation in invasive fungal infections. J Infect. 2006;52:67-74. (37.) Gil-Lamaignere C, Winn RM, Simitsopoulou M, Maloukou A, Walsh TJ, Roilides E. Interferon gamma and granulocyte-macrophage colony-stimulating factor granulocyte-macrophage colony-stimulating factor n. A naturally occurring protein that stimulates the production of granulocytes and macrophages by stem cells and is used as a drug by some immunosuppressed individuals. augment the antifungal activity of human polymorphonuclear leukocytes against Scedosporium spp.: comparison with Aspergillus spp. Med Mycol. 2005;43:253-60. (38.) Guerrero A, Torres P, Duran MT, Ruiz-Diez B, Rosales M, Rodriguez-Tudela JL. Airborne outbreak of nosocomial nosocomial /noso·co·mi·al/ (nos?o-ko´me-il) pertaining to or originating in a hospital. nos·o·co·mi·al adj. 1. Of or relating to a hospital. 2. Scedosporium prolificans infection. Lancet. 2001 ;357:1267-8. (39.) Sole M, Cano J, Rodriguez-Tudela JL, Ponton J, Sutton DA, Perrie R, et al. Molecular typing of clinical and environmental isolates of Scedosporittm prolificans by inter-simple-sequence-repeat polymerase chain reaction polymerase chain reaction (pŏl`ĭmərās') (PCR), laboratory process in which a particular DNA segment from a mixture of DNA chains is rapidly replicated, producing a large, readily analyzed sample of a piece of DNA; the process is . Med Mycol. 2003;41:293-300. (40.) Gilgado F, Cano J, Gene J, Guarro J. Molecular phylogeny of the Pseudallescheria boydii species complex. Proposal of two new species. J Clin Microbiol. 2005;43:4930-42. Address for correspondence: Monica Slavin, Department of Infectious Diseases, Peter MacCallum Cancer Centre, St Andrew's Pl, East Melbourne, Victoria East Melbourne is an inner city suburb of Melbourne, Victoria, Australia. East Melbourne is a small area of inner Melbourne located between Richmond and the Melbourne Central Business District. , Australia; email: monica.slavin@petermac.org Louise Cooley, *([dagger]), Denis Denis, king of Portugal: see Diniz. Spelman,* Karin Thursky,([double dagger])and Monica Slavin *([double dagger]) * Alfred Hospital, Prahran, Victoria, Australia; ([dagger]) Royal Hobart Hospital, Hobart, Tasmania, Australia; and ([double dagger]) Royal Melbourne Hospital The Royal Melbourne Hospital (RMH) in Parkville is one of Australia’s leading public hospitals. It is a major teaching hospital for tertiary health care with a reputation in clinical research. , Parkville, Victoria, Australia
Table 1. Characteristics and outcomes of patients infected
with Scedosporium spp., Australia, 1997-2003
Characteristic S. apiospermum S. prolificans
No. patients 31 28
Patient demographics
Mean age (range), y 40 42
Sex (M:F) 19:12 16:12
Immunocompromised (%) 21 (68) 14 (50)
Stem cell transplant 0 6
Hematologic malignancy 0 2
Lung and/or heart transplant 13 6
HIV infection, cancer, immuno- 8 0
suppression
Immunocompetent (%) 10 (32) 14 (50)
Cystic fibrosis 5 6
Airways disease * 4 3
Sinusitis 1 3
Other condition [dagger] 0 2
Specimen type
Respiratory tract (%) 27 (68) 20 (71)
Tissue 3 6
Blood 0 4
Other [double dagger] 2 1
Additional microorganisms iden- 16 (42) 14 (50)
tified (%)
Molds [section] 9 10
Bacterial [paragraph] 9 8
Outcome at 1 mo
Invasive infection (%) # 2 (6) 10 (36)
Died at 1 mo (%) ** 6 (19) 5 (18)
Died of scedosporiosis 1 (3) 5 (18)
(%) [dagger] [dagger]
Attributable mortality rate of 1/2 (50) 5/10 (50)
invasive disease (%) [double
dagger] [double dagger]
* Bronchiectasis, asthma, and chronic obstructive pulmonary disease.
[dagger] Osteoarthritis and trauma.
[double dagger] Ear swab, central catheter tip, and synovial fluid.
[section] Aspergillus spp, Rhizopus orrhyzae, and Paecilomyces sp.
[paragraph] Bacteria not found in normal flora included Pseudomonas
aeruginosa, Stenotrophomonas maltophilia, Staphylococcus aureus,
Nocardia sp., and Mycobacterium avium complex.
# Odds ratio (OR) 6.64, 95% confidence interval (CI) 1.62-27.12,
p = 0.001.
** OR 1.11, 95% CI 0.40-3.04, p = 0.84.
[dagger] [dagger] OR 5.53, 95% CI 0.68-44.54, p = 0.06.
[double dagger] [double dagger] OR 1.0, 95% CI 0.21-4.56, p = 1.0.
Table 2. Characteristics of 8 patients with invasive disease
and Scedospoeium prolificans infections, Australia, 1997-2003 *
Patient Primary Transplant Neutropenia
no. disease type within 30 d
1 ALL Allogeneic Yes
HSCT
2 AML Allogeneic No
HSCT
3 MM Allogeneic Yes
HSCT
4 NHL Allogeneic Yes
HSCT
5 AML Allogeneic Yes
HSCT
6 MM Allogeneic Yes
HSCT
7 MDS NA No
8 AML NA Yes
Patient GVHD Date of Days post
no. first transplant
isolate
1 Chronic Aug >400
extensive 2000
2 Chronic Apr >500
extensive 2001
3 No Nov 28
2000
4 No Dec 10
2000
5 No Mar 10
2003
6 Chronic Nov 120
extensive 2002
7 NA Nov NA
2003
8 NA May NA
2002
Patient Initial Site of Outcome
no. symptom isolates following
diagnosis
1 Knee Blood, Died d 21
effusion synovium,
cartilage,
prostate
2 Pulmonary Blood, Died d 5
infiltrate sputum,
BAL, lung
3 Ethmoid Ethmoid Alive d 500
sinus sinus,
infiltrate vertebral
disc,
mycotic
aneurysm
4 Neutropenic Blood Died before
sepsis diagnosis
5 Neutropenic Blood, Died d 1
sepsis sputum,
BAL, lung,
skin
6 Pneumonia Sputum Died d 1
7 Maxillary Sputum, Died d 14
sinus maxillary
infiltrate sinus,
pericardium,
myocardium,
kidney,
skin,lung
8 Catheter- Chest wall, Alive d 500
related Hickman
sepsis catheter
* GVHD, graft versus host disease; ALL, acute lymphoblastic
leukemia; HSCT, hematopoietic stem cell transplantation;K AML,
acute myeloid leukemia; BAL, bronchoalveolar lavage; MM,
multiple myeloma; NHL, non-Hodgkin iy,,Nhoma; MDS,
myelodysplastic syndrome; NA, not applicable because patients
did not undergo stem cell transplantation.
|
|
||||||||||||||||||
Printer friendly
Cite/link
Email
Feedback
Reader Opinion