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Clinical and Immune Impact of Mycobacterium bovis BCG Vaccination Scarring
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ABSTRACT
The World Health Organization recommends
Mycobacterium bovis
BCG vaccination in areas of high tuberculosis prevalence. BCG's clinical and immune effects, not necessarily
Mycobacterium tuberculosis
specific, are unclear. BCG vaccine scarring often is used as a surrogate marker of vaccination or of effective vaccination. We evaluated BCG scarring status in relation to clinical findings and outcome in 700 hospitalized Malawians, of whom 32 had
M. tuberculosis
bloodstream infections (BSI) (10 of whom had cellular immune studies done) and of whom 48 were infants <6 months old and therefore recently vaccinated (19 of whom had immune studies). In the patients ≥6 months old, scarring was not related to the presence of pulmonary symptoms (35 versus 30%), chronic cough or fever, mortality, or
M. tuberculosis
BSI. In
M. tuberculosis
BSI patients, scarring was unrelated to mortality, vital signs, or clinical symptoms but those with scarring had higher proportions of memory and activated T cells and more type 2-skewed cytokine profiles. Infants with either BCG scarring (
n
= 10) or BCG lesional inflammation (
n
= 5) had no symptoms of sepsis, but 18 of 33 infants without BCG vaccination lesions did. Those with BCG lesions had localized infections more often than did those without BCG lesions. These infants also had lower median percentages of lymphocytes spontaneously making interleukin-4 (IL-4) or tumor necrosis factor alpha (TNF-α) and lower ratios of T cells spontaneously making IL-4 to T cells making IL-6. Thus, we found that, in older patients, BCG vaccine scarring was not associated with
M. tuberculosis
-specific or nonspecific clinical protection. Those with
M. tuberculosis
BSI and scarring had immune findings suggesting previous
M. tuberculosis
antigen exposure and induction of a type 2 cytokine pattern with acute reexposure. It is unlikely that this type 2 pattern would be protective against mycobacteria, which require a type 1 response for effective containment. In infants <6 months old, recent BCG vaccination was associated with a non-
M. tuberculosis
-specific, anti-inflammatory cytokine profile. That the vaccinated infants had a greater frequency of localized infections and lesser frequency of sepsis symptoms suggests that this postvaccination cytokine pattern may provide some non-
M. tuberculosis
-specific clinical benefits.
American Society for Microbiology
Title: Clinical and Immune Impact of
Mycobacterium bovis
BCG Vaccination Scarring
Description:
ABSTRACT
The World Health Organization recommends
Mycobacterium bovis
BCG vaccination in areas of high tuberculosis prevalence.
BCG's clinical and immune effects, not necessarily
Mycobacterium tuberculosis
specific, are unclear.
BCG vaccine scarring often is used as a surrogate marker of vaccination or of effective vaccination.
We evaluated BCG scarring status in relation to clinical findings and outcome in 700 hospitalized Malawians, of whom 32 had
M.
tuberculosis
bloodstream infections (BSI) (10 of whom had cellular immune studies done) and of whom 48 were infants <6 months old and therefore recently vaccinated (19 of whom had immune studies).
In the patients ≥6 months old, scarring was not related to the presence of pulmonary symptoms (35 versus 30%), chronic cough or fever, mortality, or
M.
tuberculosis
BSI.
In
M.
tuberculosis
BSI patients, scarring was unrelated to mortality, vital signs, or clinical symptoms but those with scarring had higher proportions of memory and activated T cells and more type 2-skewed cytokine profiles.
Infants with either BCG scarring (
n
= 10) or BCG lesional inflammation (
n
= 5) had no symptoms of sepsis, but 18 of 33 infants without BCG vaccination lesions did.
Those with BCG lesions had localized infections more often than did those without BCG lesions.
These infants also had lower median percentages of lymphocytes spontaneously making interleukin-4 (IL-4) or tumor necrosis factor alpha (TNF-α) and lower ratios of T cells spontaneously making IL-4 to T cells making IL-6.
Thus, we found that, in older patients, BCG vaccine scarring was not associated with
M.
tuberculosis
-specific or nonspecific clinical protection.
Those with
M.
tuberculosis
BSI and scarring had immune findings suggesting previous
M.
tuberculosis
antigen exposure and induction of a type 2 cytokine pattern with acute reexposure.
It is unlikely that this type 2 pattern would be protective against mycobacteria, which require a type 1 response for effective containment.
In infants <6 months old, recent BCG vaccination was associated with a non-
M.
tuberculosis
-specific, anti-inflammatory cytokine profile.
That the vaccinated infants had a greater frequency of localized infections and lesser frequency of sepsis symptoms suggests that this postvaccination cytokine pattern may provide some non-
M.
tuberculosis
-specific clinical benefits.
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