Both advancing age and HIV-1 infection are associated with an increased frequency of infection, such as those due to Streptococcus pneumoniae, and a higher rate of complications and death with these infections. Vaccines are available to prevent a number of infections common in older adults, such as pneumococcal pneumonia and blood stream infection. However, many older adults, particularly those with underlying disease, and persons living with HIV-1 infection show a decreased frequency, magnitude, quality and function of specific antibodies following pneumococcal vaccination, as well as clinical vaccine failure. Underlying these defects may be limitations in responses to infection and vaccines in both blood and at mucosal sites, where most infections, such as pneumococcal pneumonia, begin. Responses to vaccines begin quickly after immunization. We focus on the distinct events at the initiation of immune responses to a newer pneumococcal vaccine directed against the polysaccharide capsule (PCV-13). We study the initial generation of both T cell and B cell responses transiently identified in blood at 7 days after immunization that reflect the key early events occurring in the lymphoid germinal centers. T cell subsets, such as T follicular helper and regulatory cells (TFH and TFR, respectively) that promote and modulate B cell activation and differentiation, are mobilized and circulate in blood. These T cells regulate a key protein expressed in B cells, AID (activation-induced cytidine deaminase) that drives B cells to undergo antibody class switch recombination (CSR) from IgM to IgG and IgA and to undergo affinity maturation by somatic hypermutation (SHM). SHM enhances the avidity and function of these antibodies. Both TFH and AID activity may be compromised in both aging adults and those with HIV-1 infection, potentially causing additive immune compromise. We will study 80 adults, 40 with and 40 without HIV-1 infection, half of whom are 21-40 years of age, half 55-64 to distinguish the contributions of both states to the integrity of vaccine responses. The work is unique in characterizing antibody levels and quality at two relevant mucosal sites before and after vaccine - in the nasopharynx where colonization begins, in the lung where pneumonia begins, and in the blood, where invasive infections progress from initial mucosal sites, so effective mucosal defense is essential for protection. The end point of vaccination is to generate antibodies of high avidity (strength of binding) and function (opsonophagocytosis). We characterize these outcomes, the impact of aging and HIV-1 infection on acute TFH, TFR and AID activation, and their impact on the early response of antibody-secreting cells specific for the vaccine and the molecular basis of antibody quality which is determined by immunoglobulin gene mutations. By identifying the specific defects associated with aging and HIV-1 infection, we propose to direct development of improved vaccines to more effectively prevent these serious infections.

Public Health Relevance

and Relevance to the VA The VA is the largest provider of HIV-1 care in the U.S. (26,000 in 2013, up to half >55 years of age). Both HIV-1 infection and advancing age, alone and in combination, are associated with an increased risk of serious infection and impaired responses to the vaccines designed to prevent them. B cells make antibodies, but B cells can show impaired function that result in these serious infectious complications of aging and HIV-1 infection, including vaccine failure. We address two questions in this proposal. First, do HIV-1 and aging, alone and in combination, impair the ability of B cells to produce antibodies of sufficient quality to recognize and kill infecting bacteria at mucosal sites, particularly the nose and lung where these infections begin? Second, what are the specific defects in B and T helper cells and their interactions associated with aging and HIV-1 infection and antibody dysfunction that can be reversed or avoided to improve vaccine responses and protection of our veterans against disease.

Agency
National Institute of Health (NIH)
Institute
Veterans Affairs (VA)
Type
Non-HHS Research Projects (I01)
Project #
5I01CX001464-02
Application #
9421482
Study Section
Infectious Diseases B (INFB)
Project Start
2017-01-01
Project End
2020-12-31
Budget Start
2018-01-01
Budget End
2018-12-31
Support Year
2
Fiscal Year
2018
Total Cost
Indirect Cost
Name
VA Eastern Colorado Health Care System
Department
Type
DUNS #
003252830
City
Aurora
State
CO
Country
United States
Zip Code
80045
Nicholson, Lindsay K; Pratap, Harsh; Bowers, Elisabeth et al. (2018) Effective B cell activation in vitro during viremic HIV-1 infection with surrogate T cell stimulation. Immunobiology 223:839-849
Sokoya, Mofiyinfolu; Ramakrishnan, Vijay R; Frank, Daniel N et al. (2017) Expression of immunoglobulin D is increased in chronic rhinosinusitis. Ann Allergy Asthma Immunol 119:317-323.e1