TY - JOUR KW - Serology KW - Multidrug therapy KW - leprosy KW - diagnosis KW - Cellular immunity AU - Freitas A AU - Oliveira RM AU - Hungria EM AU - Paula Vaz Cardoso L AU - Sousa ALOM AU - Costa MB AU - Reed S AU - Duthie M AU - Stefani MMA AB -
This study evaluated the impact of leprosy multidrug therapy (MDT) on cell-mediated immunity (CMI) and antibody responses at diagnosis in untreated paucibacillary (PB) (n=15) and multibacillary (MB) patients (n=15) using a panel of Mycobacterium leprae recombinant antigens (rMLs) (CMI: 46f, ML0276, ML2055, leprosy IDRI diagnostic 1 [LID-1], and ML2629, as negative control; serology: LID-1, 46f, 92f, and 33f, as negative control, and phenolic glycolipid I [PGL-I]) and at 2 time points after MDT (PB: 8-20months; MB: 4-22months). At diagnosis, PB patients produced interferon gamma (IFNγ), and MB patients exhibited low/absent response. Shortly after MDT, IFNγ production in PB patients declined except for LID-1; MB patients produced IFNγ to LID-1. Almost 2years after MDT, IFNγ levels declined in PB and MB patients. Most untreated PB patients were seronegative to PGL-I and rML, remaining so after MDT. Most untreated MB patients were seropositive to all antigens, and IgG to rMLs declined after MDT. Reduction in antigen-specific CMI in PB and in antibody response in MB patients may help monitor MDT effectiveness.
BT - Diagnostic microbiology and infectious disease C1 -http://www.ncbi.nlm.nih.gov/pubmed/26233487?dopt=Abstract
DO - 10.1016/j.diagmicrobio.2015.06.021 J2 - Diagn. Microbiol. Infect. Dis. LA - eng N2 -This study evaluated the impact of leprosy multidrug therapy (MDT) on cell-mediated immunity (CMI) and antibody responses at diagnosis in untreated paucibacillary (PB) (n=15) and multibacillary (MB) patients (n=15) using a panel of Mycobacterium leprae recombinant antigens (rMLs) (CMI: 46f, ML0276, ML2055, leprosy IDRI diagnostic 1 [LID-1], and ML2629, as negative control; serology: LID-1, 46f, 92f, and 33f, as negative control, and phenolic glycolipid I [PGL-I]) and at 2 time points after MDT (PB: 8-20months; MB: 4-22months). At diagnosis, PB patients produced interferon gamma (IFNγ), and MB patients exhibited low/absent response. Shortly after MDT, IFNγ production in PB patients declined except for LID-1; MB patients produced IFNγ to LID-1. Almost 2years after MDT, IFNγ levels declined in PB and MB patients. Most untreated PB patients were seronegative to PGL-I and rML, remaining so after MDT. Most untreated MB patients were seropositive to all antigens, and IgG to rMLs declined after MDT. Reduction in antigen-specific CMI in PB and in antibody response in MB patients may help monitor MDT effectiveness.
PY - 2015 T2 - Diagnostic microbiology and infectious disease TI - Alterations to antigen-specific immune responses before and after multidrug therapy of leprosy. UR - http://www.researchgate.net/profile/Ludimila_Cardoso/publication/280613429_Alterations_To_Antigen-Specific_Immune_Responses_Before_And_After_Multidrug_Therapy_Of_Leprosy/links/55c0ac5e08aed621de13d472.pdf SN - 1879-0070 ER -