Abstract:Mycobacterium tuberculosis (Mtb) exposure drives antibody responses, but whether patients with active tuberculosis elicit protective antibodies, and against which antigens, is still unclear. Here we generate monoclonal antibodies from memory B cells of one patient to investigate the B cell responses during active infection. The antibodies, members of four distinct B cell clones, are directed against the Mtb phosphate transporter subunit PstS1. Antibodies p4-36 and p4-163 reduce Mycobacterium bovis-BCG and Mtb … Show more
“…Antibody titers were assessed to five Mtb antigens that vary in composition, structure, function and localization: purified protein derivative (PPD), the total protein fraction from virulent mycobacterium 13 , lipoarabinomannan (LAM), a critical cell wall glycolipid 14 , HspX, a stress-induced intracellular protein 15 , and PstS1 and Apa, cell membrane-associated glycoproteins linked to host cell invasion 16 , 17 . Of note, antibodies specific to LAM, HspX and PstS1 ameliorate TB disease in mouse passive transfer studies 18 – 20 , and antibody responses to each of the five antigens have been observed during Mtb infection in humans 20 – 22 . Fig.…”
Development of an effective tuberculosis (TB) vaccine has suffered from an incomplete understanding of the correlates of protection against Mycobacterium tuberculosis (Mtb). Intravenous (i.v.) vaccination with Bacille Calmette–Guérin (BCG) provides nearly complete protection against TB in rhesus macaques, but the antibody response it elicits remains incompletely defined. Here we show that i.v. BCG drives superior antibody responses in the plasma and the lungs of rhesus macaques compared to traditional intradermal BCG administration. While i.v. BCG broadly expands antibody titers and functions, IgM titers in the plasma and lungs of immunized macaques are among the strongest markers of reduced bacterial burden. IgM was also enriched in macaques that received protective vaccination with an attenuated strain of Mtb. Finally, an Mtb-specific IgM monoclonal antibody reduced Mtb survival in vitro. Collectively, these data highlight the potential importance of IgM responses as a marker and mediator of protection against TB.
“…Antibody titers were assessed to five Mtb antigens that vary in composition, structure, function and localization: purified protein derivative (PPD), the total protein fraction from virulent mycobacterium 13 , lipoarabinomannan (LAM), a critical cell wall glycolipid 14 , HspX, a stress-induced intracellular protein 15 , and PstS1 and Apa, cell membrane-associated glycoproteins linked to host cell invasion 16 , 17 . Of note, antibodies specific to LAM, HspX and PstS1 ameliorate TB disease in mouse passive transfer studies 18 – 20 , and antibody responses to each of the five antigens have been observed during Mtb infection in humans 20 – 22 . Fig.…”
Development of an effective tuberculosis (TB) vaccine has suffered from an incomplete understanding of the correlates of protection against Mycobacterium tuberculosis (Mtb). Intravenous (i.v.) vaccination with Bacille Calmette–Guérin (BCG) provides nearly complete protection against TB in rhesus macaques, but the antibody response it elicits remains incompletely defined. Here we show that i.v. BCG drives superior antibody responses in the plasma and the lungs of rhesus macaques compared to traditional intradermal BCG administration. While i.v. BCG broadly expands antibody titers and functions, IgM titers in the plasma and lungs of immunized macaques are among the strongest markers of reduced bacterial burden. IgM was also enriched in macaques that received protective vaccination with an attenuated strain of Mtb. Finally, an Mtb-specific IgM monoclonal antibody reduced Mtb survival in vitro. Collectively, these data highlight the potential importance of IgM responses as a marker and mediator of protection against TB.
“…In a recent clinical trial of 2655 participants, authors reported that the use of bezlotoxumab (monoclonal antibody against C. difficile toxin) for treating C. difficile infection resulted in a lower recurrence of infection (Wilcox et al, 2017 ). In another recent study, Watson et al ( 2021 ) generated a monoclonal antibody from B cells of a patient to be used against Mycobacterium tuberculosis infection in mice. Monoclonal antibodies are costlier than producing antibiotics but have many benefits and more studies in this direction will help can help transform medicine.…”
Section: Antibiotic Alternatives and Use Of Probiotics For Restoring ...mentioning
It is well established that the gut microbiota plays an important role in host health and is perturbed by several factors including antibiotics. Antibiotic‐induced changes in microbial composition can have a negative impact on host health including reduced microbial diversity, changes in functional attributes of the microbiota, formation, and selection of antibiotic‐resistant strains making hosts more susceptible to infection with pathogens such as Clostridioides difficile. Antibiotic resistance is a global crisis and the increased use of antibiotics over time warrants investigation into its effects on microbiota and health. In this review, we discuss the adverse effects of antibiotics on the gut microbiota and thus host health, and suggest alternative approaches to antibiotic use.
“…The limitation of these studies is that they only focused on epitopes singly identified from CD4 + T lymphocytes [helper T lymphocytes (Th)] or CD8 + T lymphocytes (CTLs) rather than epitopes synchronously identified from Th cells, CTL cells, and B cells. Although the traditional view is that the host clearance and killing of M. tuberculosis mainly depend on CD4 + T lymphocytes and CD8 + T lymphocytes, accumulated data show that B lymphocytes also play an irreplaceable role in fighting against M. tuberculosis (Gong et al, 2018(Gong et al, , 2021Watson et al, 2021). Therefore, peptides binding to Th cells, CTL cells, and B cells should be considered when designing new candidate biomarkers based on epitopes for distinguishing LTBI from aTB and BCG-vaccinated HCs.…”
As an ancient infectious disease, tuberculosis (TB) is still the leading cause of death from a single infectious agent worldwide. Latent TB infection (LTBI) has been recognized as the largest source of new TB cases and is one of the biggest obstacles to achieving the aim of the End TB Strategy. The latest data indicate that a considerable percentage of the population with LTBI and the lack of differential diagnosis between LTBI and active TB (aTB) may be potential reasons for the high TB morbidity and mortality in countries with high TB burdens. The tuberculin skin test (TST) has been used to diagnose TB for > 100 years, but it fails to distinguish patients with LTBI from those with aTB and people who have received Bacillus Calmette–Guérin vaccination. To overcome the limitations of TST, several new skin tests and interferon-gamma release assays have been developed, such as the Diaskintest, C-Tb skin test, EC-Test, and T-cell spot of the TB assay, QuantiFERON-TB Gold In-Tube, QuantiFERON-TB Gold-Plus, LIAISON QuantiFERON-TB Gold Plus test, and LIOFeron TB/LTBI. However, these methods cannot distinguish LTBI from aTB. To investigate the reasons why all these methods cannot distinguish LTBI from aTB, we have explained the concept and definition of LTBI and expounded on the immunological mechanism of LTBI in this review. In addition, we have outlined the research status, future directions, and challenges of LTBI differential diagnosis, including novel biomarkers derived from Mycobacterium tuberculosis and hosts, new models and algorithms, omics technologies, and microbiota.
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