Latent Tuberculosis Clinical Trial
Official title:
Correlation of the Precursor Frequency of CD4 + Effector Memory T Cells With Induration Measured in the Tuberculin Skin Test (TST)
This study will examine how the immune system responds to infection with Mycobacterium
tuberculosis bacteria (bacteria that cause tuberculosis) in order to better understand how
the germ produces infection and how the immune response might work to control the infection.
Only about one in 10 people infected by M. tuberculosis become sick, sometimes years or even
decades after exposure. It is not known why some people become sick and most do not, but the
immune system of people who never develop disease may be better able to control the bacteria.
This study will evaluate the latent form of M. tuberculosis infection to further the
understanding of the immune mechanisms - particularly the role of certain white blood cells -
involved in the disease process.
Healthy volunteers 18 years of age and older may be eligible for this study. Candidates are
screened with a medical history, family history of medical conditions, sexual history,
history of drug use, physical examination and blood tests, including a test for HIV. People
in Mali, West Africa, and in local health clinics in the United States may participate.
At the start of the study, participants have blood tests and a tuberculin skin test (PPD
test), which indicates whether a person has been exposed to tuberculosis bacteria. For the
PPD, a tiny amount of liquid containing dead tuberculosis antigen is put under the skin of
the forearm with a needle. The antigen cannot cause infection or disease.
After 3 days, participants have another blood test and the site of the tuberculin test is
examined for swelling that would indicate a positive result. Participants with a positive PPD
have a chest x-ray to check for tuberculosis disease. Those whose x-ray is also positive are
withdrawn from the study and referred to their doctor for evaluation and treatment. Those
whose x-ray is negative return to the clinic within 3 weeks of the tuberculin test to give
another blood sample.
Participants whose PPD is negative have a second tuberculin test 10 to 21 days later and
return 3 days after the test to determine if it is still negative or if it is positive. (Some
people who are negative after the first test may test positive after the second procedure.)
Those whose test is still negative end their participation in the study at that time.
Participants whose second PPD is positive have a chest x-ray as described above, and those
with a negative chest x-ray return in 3 weeks to donate one last blood sample.
The purpose of the present study is to evaluate the latent form of this infection, the
prevalence of which worldwide exceeds that of active disease. Our hypothesis is that in
latent tuberculosis antigen specific effector memory CD4+ T cells are responsible for the
generation of clinically measurable delayed type hypersensitivity and that central memory
CD4+T cells are not directly involved in this process. We base this idea on the assumption
that latent tuberculosis is a state of antigen persistence and that effector memory T cells
should be maintained as long as antigen/infection is present.
We propose to conduct this study in Mali, West Africa and local clinics in the U.S.
Tuberculosis affects 593/100,000(2) individuals in Mali and most have been exposed to the
disease. Additionally it would be important to evaluate the same parameters locally as latent
infection is one of the major factors for reactivation tuberculosis in this country. Patients
would be enrolled in 4 major groups: HIV-/TST- (Group A), HIV-/TST+ (Group B), HIV+/TST+(G
roup C) and HIV+/TST- (Group D).
To evaluate this hypothesis we plan to enroll between 100 - 300 patients over the course of 2
years from both countries. Blood samples before and at predetermined time points after the
application of Purified Protein Derivative (PPD) will be obtained to determine the fraction
of CD4+ T cells which produce interferon gamma in response to stimulation with PPD with a
16hr antigen stimulation assay. Appropriate staining will be done to ascertain the phenotype
as well as cytokine production (Interferon gamma,( IFN gamma), Interleukin 2 (IL2) and Tumour
Necrosis Factor ( TNF)). Additionally lymphocyte proliferation will be studied using
5-(and-6)-carboxyflouorescein diacetate succinimidyl ester (CFSE.)
In conducting this study we hope to further the understanding of the immune mechanisms
involved, particularly mechanisms of T cell memory, which would provide insights into TB and
HIV pathogenesis. We also believe that understanding these mechanisms could lead towards
establishment of surrogates for immunity in TB vaccine studies, which could enhance vaccine
trial design. It might also help in understanding better the immunological dynamics of
tuberculosis co-infection in individuals with HIV infection.
Tuberculosis (TB) is a major global health concern. One third of the world's population is
infected with Mycobacterium tuberculosis. Two to 3 million people die every year of the
disease with 8-10 million new cases per year. It is projected that there will be 90 million
new cases and 30 million deaths over the next decade. For a disease, which we know to have
existed since 2400 BC, our understanding of its pathogenesis is incomplete, especially in
relation to the human immune response and the role of lymphocytes in particular.
The purpose of the present study is to evaluate the latent form of this infection, the
prevalence of which worldwide exceeds that of active disease. Our hypothesis is that in
latent tuberculosis antigen specific effector memory CD4+ T cells are responsible for the
generation of clinically measurable delayed type hypersensitivity and that central memory
CD4+T cells are not directly involved in this process. We base this idea on the assumption
that latent tuberculosis is a state of antigen persistence and that effector memory T cells
should be maintained as long as antigen/infection is present.
We propose to conduct this study in Mali, West Africa and local clinics in the U.S.
Tuberculosis affects 593/100,000(2) individuals in Mali and most have been exposed to the
disease. Additionally it would be important to evaluate the same parameters locally as latent
infection is one of the major factors for reactivation tuberculosis in this country. Patients
would be enrolled in 4 major groups: HIV-/TST- (Group A), HIV-/TST+ (Group B), HIV+/TST+
(Group C) and HIV+/TST- (Group D).
To evaluate this hypothesis we plan to enroll between 100 - 300 patients over the course of 2
years from both countries. Blood samples before and at predetermined time points after the
application of Purified Protein Derivative (PPD) will be obtained to determine the fraction
of CD4+ T cells which produce interferon gamma in response to stimulation with PPD with a
16hr antigen stimulation assay. Appropriate staining will be done to ascertain the phenotype
as well as cytokine production (Interferon gamma, ( IFN gamma), Interleukin 2 (IL2) and
Tumour Necrosis Factor (TNF)). Additionally lymphocyte proliferation will be studied using
5-(and-6)-carboxyflouorescein diacetate succinimidyl ester (CFSE.)
In conducting this study we hope to further the understanding of the immune mechanisms
involved, particularly mechanisms of T cell memory, which would provide insights into TB and
HIV pathogenesis. We also believe that understanding these mechanisms could lead towards
establishment of surrogates for immunity in TB vaccine studies, which could enhance vaccine
trial design. It might also help in understanding better the immunological dynamics of
tuberculosis co-infection in individuals with HIV infection.
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