News Release

Antibody function may help keep tuberculosis infection under control

The different antibody signatures of latent and active TB could improve diagnosis, lead to more effective vaccines

Peer-Reviewed Publication

Massachusetts General Hospital

A study led by investigators from the Ragon Institute of MGH, MIT and Harvard finds evidence that antibody protection may help control infection with the bacteria that causes tuberculosis (TB). In their study receiving online publication in Cell, the research team describes finding consistent differences in both the structure and function of antibodies targeting the TB bacteria between individuals with active TB disease and those with latent TB, which neither produces symptoms nor can be transmitted. The findings may lead to better ways of distinguishing between active and latent disease and to a more effective vaccine against a disease that kills more than 1.5 million people each year.

"Ending tuberculosis by 2030 is one of the targets of the World Health Organization's newly adopted Sustainable Developmental Goals," says Lenette Lu, MD, PhD, of the Ragon Institute and the Massachusetts General Hospital (MGH) Department of Medicine, a co-lead author of the Cell report. "A more effective vaccine against TB could substantially contribute towards that goal, impacting the nearly one in three people worldwide who are infected and addressing the leading killer of individuals infected with HIV."

The only currently available preventive against infection with the TB bacteria - the BCG vaccine - has been available since the 1920s; but its effectiveness against pulmonary TB, the most common form of the disease, has always been uncertain. BCG is believed to work by stimulating cellular immunity, which is carried out by specialized immune cells including T cells and the macrophages that are directly infected by TB bacteria. Previous investigations into a possible role for antibodies in the immune response to TB have had conflicting results, but the Ragon team - led by Galit Alter, PhD, of MGH Department of Medicine and Sarah Fortune, MD, of the Harvard T.H. Chan School of Public Health - used a novel approach.

In addition to binding to their target pathogens and marking them for destruction by the immune system, antibodies also directly stimulate pathogen-killing cells of the innate immune system by binding to a cell-surface protein called the Fc receptor. The Ragon team profiled TB-specific antibodies from 22 individuals with latent TB and 20 with active TB for 70 different features associated with Fc-mediated antibody function. They first identified nine characteristics that differentiated between antibodies of the two groups of participants, and further investigation identified the biomarker that best distinguished between them.

A key regulator of Fc-mediated immune function is the addition to antibodies of compounds called glycans, made up of sugar molecules; and distinct differences in glycosylation patterns were found to clearly distinguish latent TB antibodies from active TB antibodies. To confirm these results in the initial group of participants, who were from South Africa, the team conducted a similar analysis of antibodies from 20 individuals from Texas and Mexico - half with latent and half with active TB - and had the same results. Further experiments revealed that application of latent TB antibodies to TB-infected human macrophages not only increased the activation of several antimicrobial processes but also reduced the survival of the TB bacteria.

Co-lead author Amy Chung, PhD, now at the Peter Doherty Institute for Infection and Immunity in Melbourne, Australia - a joint venture between The University of Melbourne and The Royal Melbourne Hospital - explains, "This is a completely new area of immune research in tuberculosis, since these antibodies don't just recognize the infection, they also recruit immune cells to target it. People with latent infection have inactive disease for a reason, and if antibodies are playing a role in controlling the infection, the mechanism they use could be harnessed for future vaccine development."

Alter, an associate professor of Medicine at Harvard Medical School, adds, "The diagnostic potential of these findings should not be overlooked. The detection of Fc-related modifications of TB-specific antibodies could be easily translated into a rapid, inexpensive point-of-care diagnostic that could have enormous public health impact, particularly in those parts of the globe where TB is endemic."

"These findings - which could lead to major advances in the fight against one of humanity's oldest diseases - would have been impossible without visionary philanthropists like Terry and Susan Ragon, whose major gift created the Ragon Institute in 2009, and Mark and Lisa Schwartz, whose long-term support provided seed funding for Dr. Alter's work," says Peter Slavin, MD, president of Massachusetts General Hospital, where the Ragon Institute is administratively based.

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Tracy Rosebrock, PhD, of the Harvard Chan School is also a co-lead author of the Cell paper. The study was supported by National Institutes of Health grants R01 AI080289 and AI102660 and T32 AI007387, DARPA grant BAA-11-65, the Harvard Center for AIDS research, the Bill and Melinda Gates Foundation, National Health and Medical Research Council (Australia) grant APP1036470, and support from the Pozen Family Foundation, the Doris Duke Medical Research Foundation, and the Burroughs Wellcome Foundation, along with Ragon Institute funding.

The Ragon Institute of MGH, MIT and Harvard was established in 2009 with a gift from the Philip T. and Susan M. Ragon Foundation, creating a collaborative scientific mission among these institutions to harness the immune system to combat and cure human diseases. The primary initial focus of the institute is to contribute to the development of an effective AIDS vaccine. The Ragon Institute draws scientists and engineers from diverse backgrounds and areas of expertise across the Harvard and MIT communities and throughout the world, in order to apply the full arsenal of scientific knowledge to understanding mechanisms of immune control and immune failure and to apply these advances to directly benefit patients.


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