EORTC/BAMSG Consensus Revised definitions draft VI
Now Available for Public Comment
On this page you can review the revised EORTC/MSG definitions, which were presented at ICAAC 2005.
You can view and download a Word document of the proposed revised definitions by clicking here.
In addition, you can also view and download the PowerPoint presentations made at the ICAAC 2005 symposium
"Defining Invasive Fungal Infections: New Directions" during which the revised definitions were discussed by clicking here.
EORTC/MSG Consensus Revised definitions draft VI
Participants in the Consensus Group
Ben
De Pauw (Chair)
Tom
Walsh(Chair)
J
Peter Donnelly(Secretary)
Sibel
Ascioglu
Jack
Bennett
Jacques
Bille
David
Denning
Bill
Dismukes
Jack
Edwards
Raoul
Herbrecht
William
Hope
Carol
Kauffman
Chris
Kibbler
Bart-Jan
Kullberg
Olivier
Lorthalary
Johan
Maertens
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Kieren
Marr
Georg
Maschmeyer
Patricia
Munoz
Frank
Odds
Pete
Pappas
Tom
Patterson
John
Perfect
Angela
Restrepo
Markus
Ruhnke
Brahm
Segal
Jack
Sobel
Tania
C Sorrell
David
Stevens
Claudio
Viscoli
John
Wingard
Theoklis
Zaoutis
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Proven invasive fungal diseases
Deep tissue disease
Moulds
Histopathologic, cytopathologic,
or direct microscopic examination
of a needle aspiration or biopsy specimen showing hyphal forms with evidence of
associated tissue damage (either microscopically or as an infiltrate or lesion
by imaging)
OR
Recovery of a mould by culture
from a sample obtained by a sterile procedure from a normally sterile and
clinically or radiologically abnormal site consistent with an infectious
disease process, excluding BAL, cranial sinus cavity, and urine.
Yeasts
Histopathologic or
cytopathologic examination2 of a needle aspiration or biopsy
specimen from a normally sterile site excluding mucous membranes showing yeast
cells (Candida species may also show pseudohyphae or true hyphae)
OR
Recovery of a yeast by culture
from a sample obtained by a sterile procedure (including a freshly (<24h)
placed drain) from a normally sterile and clinically or radiologically abnormal
site consistent with an infectious disease process,
Fungemia
Moulds
Blood culture that yields a
mould e.g. Fusarium spp. in the context of a compatible infectious
disease process.
Yeasts
Blood
culture that yields yeast (e.g. Candida species) or yeast-like fungi
(e.g. Trichosporon spp.)
Endemic fungal disease
Disseminated and/or pulmonary
disease
Must be proven by recovery in
culture from a specimen obtained from the affected site, in host with a
temporally related illness consistent with a fungal infectious disease process;
OR
if culture is sterile or not
obtained, histopathologic or direct microscopic demonstration of appropriate
morphological forms is considered adequate for dimorphic fungi having truly
distinctive appearance.
OR
Positive blood culture
In the case of histoplasmosis a
diagnosis of disseminated disease may be established by a positive Histoplasma
antigen test
on CSF, urine or serum by EIA, or the presence of characteristic intracellular
yeast forms in a peripheral blood smear or in bone marrow.
Or in the case of
coccidioidomycosis a diagnosis of disseminated disease may be established by
demonstration of coccidioidal antibody9 in CSF, or a 2-dilution rise
measured in two consecutive blood samples tested concurrently in the setting of
a temporally related infectious disease process.
Cryptococcosis
Probable invasive fungal disease
Defined by at least
a) one host criterion
AND
b) one clinical criterion
AND
c) one microbiological criterion
Possible
invasive fungal disease
Defined by at least
a) one host criterion
AND
b) one clinical criterion
BUT
c) no microbiological criterion
Host factors
Host factors
are not synonymous with risk factors and are characteristics by which
individuals predisposed to invasive fungal diseases can be recognized. They are
intended primarily to apply to patients treated for malignant disease and to
recipients of allogeneic hematopoietic stem cell and solid organ transplant.
These host factors are also applicable to those receiving corticosteroids and
other T-cell suppressants as well as those with primary immune deficiencies
1) Recent
history of neutropenia (< 0.5 x 109/L {<500 neutrophils/mm3}
for >10 days) temporally related to the onset of fungal disease or ongoing
neutropenia
2) Receipt of
an allogeneic stem cell transplant
3) Prolonged
use of corticosteroids (excluding patients with ABPA) at an average minimum
dose of 0.3 mg/kg/day prednisone equivalent for > 3 weeks
4) Treatment
with other recognized T-cell immune suppressants such as ciclosporin, TNF-a blockers, specific monoclonal antibodies
alemtuzumab, nucleoside analogues during the past 90 days
5) Inherited
severe immunodeficiency (e.g., chronic granulomatous disease, severe combined
immunodeficiency)
Clinical criteria
Must be consistent with the
microbiological findings, if any, temporally related to current episode and
other potential causes must have been eliminated
Lower
respiratory tract fungal disease
A) the presence of one of the
following "specific" imaging signs on CT:-
- Well defined nodule(s) with or without a halo sign
- Wedge-shaped infiltrate
- Air crescent sign
- Cavity
B) the presence of a new non-specific focal infiltrate
PLUS at least one of the
following:-
Pleural rub
Pleural pain
Hemoptysis
Tracheobronchitis
Tracheobronchial
ulceration, nodule, pseudomembrane, plaque or eschar seen on bronchoscopy
Sinonasal infection
Imaging showing sinusitis
PLUS
at least one of the following:-
Acute localized Pain (including pain radiating to eye)
Nasal ulcer, black eschar
extension from the
paranasal sinus across bony barriers, including into the orbit
Endophthalmitis
as determined by ophthalmologic examination
CNS infection
at least one of the following:-
Focal lesions on imaging
Meningeal enhancement on MRI or CT
Chronic disseminated candidiasis
Small, peripheral, target like
abscesses (new nodular filling defects, bull's-eye
lesions) in liver and/or spleen
Microbiological Criteria
Cytology, direct microscopy or culture:
- sputum, BAL and bronchial brush samples demonstrating the presence of
fungal elements either by recovery by culture of a mould (e.g. Aspergillus spp.,
Fusarium spp., Zygomycetes, Scedosporium spp.) or detection
by cytology or direct microscopy of hyphal forms
- sinus aspirate: recovery by culture of moulds from or detection of
hyphal forms by cytology or direct microscopy.
- Skin ulcers, draining soft tissue lesions or fissure for which both
microscopy and culture are required
Detection of antigen, cell wall constituents or nucleic acid
- Galactomannan antigen EIA (Platelia).
a)
a single plasma or serum sample positive for galactomannan
b)
a single BAL, pleural fluid or CSF sample positive for
galactomannan
6. Glucan Assay is primarily
applicable for aspergillosis and candidiasis and does not detect Cryptococcus
species nor the Zygomycetes (Rhizopus spp., Mucor spp. Absidia
spp.)
a single
serum sample positive for beta-D-glucan
7. Polymerase Chain Reaction to detect nucleic acid
Until a PCR system is
developed that has been externally validated, a positive PCR result for blood,
tissue, or BAL fluid for the specific fungus studied will not be considered
microbiological evidence of invasive fungal disease.
Append identification at genus or species level from
culture, if available.
tissue and cells submitted for histopathology or
cytopathology should be stained by Grocott-Gomorri methenamine silver stain or
by periodic acid Schiff stains to facilitate inspection of fungal structures.
Where possible, wet mounts of specimens from foci related to invasive fungal infectious
disease should be stained with a fluorescent marker (e.g., calcofluor or
Blancophor)
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