Invasive Pulmonary Aspergillosis Clinical Trial
Official title:
Early Molecular Detection for the Improved Diagnosis of Invasive Pulmonary Aspergillosis and Invasive Pulmonary Zygomycosis
Background:
- Fungal infections of the lung (pneumonia) can be caused by molds, such as Aspergillus
and Zygomycetes, but these causes are often difficult for a doctor to diagnose. Early
and accurate diagnosis of these infections can help doctors to select the correct
medicines for proper treatment.
- A number of methods are used to diagnose fungal pneumonia. Ones that are commonly used
in clinical practice include radiographic imaging (chest X-rays and computed tomography
(CT) scans), blood tests, and cultures taken from fluid from the lungs (broncho-alveolar
lavage (BAL) fluid). Other new methods may improve the diagnosis of fungal pneumonias.
These methods include tests that can detect DNA from the fungal germ in blood and BAL
fluid of some patients with these infections.
Objectives:
- To help develop better and more accurate methods of diagnosing fungal lung infections.
- To detect fungal DNA and chemicals in the bloodstream and BAL fluid of immunocompromised
patients with pneumonia.
Eligibility:
- Immunocompromised patients who are currently enrolled in another NIH protocol and who have
a CT scan that shows a possible fungal infection of the lung.
Design:
- Researchers will review patients' existing medical records and CT scans, and current
pneumonia treatment plans.
- Patients will provide blood and BAL samples for the duration of their treatment for
pneumonia, as required by researchers. Additional CT scans will not be performed, except
as part of existing treatment plans.
Background:
Invasive fungal infections are an important cause of infectious disease, morbidity and
mortality in immunocompromised patients with cancer, hematopoietic stem cell transplantation,
aplastic anemia, autoimmune diseases, and primary immune deficiencies.
Foremost among the more lethal of these infections are invasive pulmonary aspergillosis and
zygomycosis. Early detection of these infections allows timely initiation of specific
antifungal therapy, which may be life saving. However, early diagnosis of respiratory fungal
infections is difficult, often leading to delay in therapy and inaccurate treatment.
The Immunocompromised Host Section has developed a series of sensitive and highly specific
PCR assays for the detection of these life-threatening infections. We also have characterized
the expression of cell wall derived biomarkers, (1-3)-Beta-D-glucan and galactomannan in
vitro and in vivo. Laboratory animal studies indicate that these assays may complement
current diagnostic modalities and allow for more accurate and earlier detection of invasive
pulmonary fungal infections in immunocompromised patients.
Objectives:
The primary objective of this study is to improve the early diagnosis of invasive pulmonary
aspergillosis and invasive pulmonary zygomycosis in immunocompromised patients through the
addition of molecular biomarker detection methodology to the standard diagnostic systems used
in clinical microbiology laboratories.
The secondary objectives are:
A. To compare the diagnostic yield and analytical performance of the PCR, galactomannan and
(1-3)-Beta-D-glucan to standard diagnostic systems.
B. To evaluate the effect of different independent variables on expression of the
aforementioned assays
C. To characterize the variables that may contribute to therapeutic outcome (global response;
survival)
D. To characterize the use of these biomarkers in the context of EORTC/MSG definitions
E. To identify genetic markers which may predispose patients to invasive fungal pulmonary
infections.
Eligibility:
Immunocompromised patients currently enrolled in any NIH IRB approved Clinical Center
protocol for the evaluation and/or treatment of his/her primary disease, or patients
receiving treatment at the Children's National Medical Center (CNMC) who develop a pulmonary
infiltrate radiologically compatible with invasive pulmonary aspergillosis or invasive
pulmonary zygomycosis, by EORTC/MSG criteria.
Design:
This is a multi-center, prospective diagnostic interventional study.
Patients referred to the Clinical Center for evaluation and treatment in primary research
protocols will be eligible for enrollment in this protocol at the Clinical Center. Patients
meeting eligibility criteria may also be enrolled from the CNMC.
Patients who have compatible radiologic signs and are at risk for development of invasive
pulmonary aspergillosis and invasive pulmonary zygomycosis will have specimens of
bronchoalveolar lavage (BAL) fluid supernatant and /or tissue from lung biopsy when
available, obtained for the measurement of diagnostic PCR for Aspergillus and Zygomycete
identification, proteomics, cytokines and for the presence of galactomannan and
(1-3)-Beta-D-glucan. The BAL will be performed only if clinically indicated as part of the
patient's routine care of pneumonic infiltrates.
Blood will be obtained from patients meeting the eligibility requirements, regardless of
whether they have had a BAL or lung tissue biopsy, to be submitted for the measurement of
diagnostic PCR for Aspergillus and Zygomycete identification, proteomics, cytokines, presence
of galactomannan and (1-3)-Beta-D-glucan and host genomics.
Digital copies of computer tomography (CT) images, that are part of routine care will
utilized to reconstruct multi-dimensional volumetric images and correlate clinical and
laboratory outcomes with the extent of lung volume involvement.
Background:
Invasive fungal infections are an important cause of infectious disease, morbidity and
mortality in immunocompromised patients with cancer, hematopoietic stem cell transplantation,
aplastic anemia, autoimmune diseases, and primary immune deficiencies.
Foremost among the more lethal of these infections are invasive pulmonary aspergillosis and
zygomycosis. Early detection of these infections allows timely initiation of specific
antifungal therapy, which may be life saving. However, early diagnosis of respiratory fungal
infections is difficult, often leading to delay in therapy and inaccurate treatment.
The Immunocompromised Host Section has developed a series of sensitive and highly specific
PCR assays for the detection of these life-threatening infections. We also have characterized
the expression of cell wall derived biomarkers, (1-3)-Beta-D-glucan and galactomannan in
vitro and in vivo. Laboratory animal studies indicate that these assays may complement
current diagnostic modalities and allow for more accurate and earlier detection of invasive
pulmonary fungal infections in immunocompromised patients.
Objectives:
The primary objective of this study is to improve the early diagnosis of invasive pulmonary
aspergillosis and invasive pulmonary zygomycosis in immunocompromised patients through the
addition of molecular biomarker detection methodology to the standard diagnostic systems used
in clinical microbiology laboratories.
The secondary objectives are:
A. To compare the diagnostic yield and analytical performance of the PCR, galactomannan and
(1-3)-Beta-D-glucan to standard diagnostic systems.
B. To evaluate the effect of different independent variables on expression of the
aforementioned assays
C. To characterize the variables that may contribute to therapeutic outcome (global response;
survival)
D. To characterize the use of these biomarkers in the context of EORTC/MSG definitions
E. To identify genetic markers which may predispose patients to invasive fungal pulmonary
infections.
Eligibility:
Immunocompromised patients currently enrolled in any NIH IRB approved Clinical Center
protocol for the evaluation and/or treatment of his/her primary disease, or patients
receiving treatment at the Children's National Medical Center (CNMC) who develop a pulmonary
infiltrate radiologically compatible with invasive pulmonary aspergillosis or invasive
pulmonary zygomycosis, by EORTS/MSG criteria.
Design:
This is a multi-center, prospective diagnostic interventional study.
Patients referred to the Clinical Center for evaluation and treatment in primary research
protocols will be eligible for enrollment in this protocol at the Clinical Center. Patients
meeting eligibility criteria may also be enrolled from the CNMC.
Patients who have compatible radiologic signs and are at risk for development of invasive
pulmonary aspergillosis and invasive pulmonary zygomycosis will have specimens of
bronchoalveolar lavage (BAL) fluid supernatant and /or tissue from lung biopsy when
available, obtained for the measurement of diagnostic PCR for Aspergillus and Zygomycete
identification, proteomics, cytokines and for the presence of galactomannan and
(1-3)-Beta-D-glucan. The BAL will be performed only if clinically indicated as part of the
patient's routine care of pneumonic infiltrates.
Blood will be obtained from patients meeting the eligibility requirements, regardless of
whether they have had a BAL or lung tissue biopsy, to be submitted for the measurement of
diagnostic PCR for Aspergillus and Zygomycete identification, proteomics, cytokines, presence
of galactomannan and (1-3)-Beta-D-glucan and host genomics.
Digital copies of computer tomography (CT) images, that are part of routine care will be
utilized to reconstruct multi-dimensional volumetric images and correlate clinical and
laboratory outcomes with the extent of lung volume involvement.
;
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