Your search keyword '"Grant, Shannon P."' showing total 4 results

1. Modification of the Association Between T-Cell Immune Responses and Human Immunodeficiency Virus Type 1 Infection Risk by Vaccine-Induced Antibody Responses in the HVTN 505 Trial.

Author

Fong Y, Shen X, Ashley VC, Deal A, Seaton KE, Yu C, Grant SP, Ferrari G, deCamp AC, Bailer RT, Koup RA, Montefiori D, Haynes BF, Sarzotti-Kelsoe M, Graham BS, Carpp LN, Hammer SM, Sobieszczyk M, Karuna S, Swann E, DeJesus E, Mulligan M, Frank I, Buchbinder S, Novak RM, McElrath MJ, Kalams S, Keefer M, Frahm NA, Janes HE, Gilbert PB, and Tomaras GD

Subjects

Antibody Formation immunology, HIV Antibodies blood, HIV-1 immunology, Humans, Immunoglobulin G blood, Immunoglobulin G classification, Male, AIDS Vaccines immunology, CD8-Positive T-Lymphocytes physiology, HIV Infections prevention & control

Abstract

Background: HVTN 505 was a human immunodeficiency virus type 1 (HIV-1) preventive vaccine efficacy trial of a DNA/recombinant adenovirus serotype 5 (rAd5) vaccine regimen. We assessed antibody responses measured 1 month after final vaccination (month 7) as correlates of HIV-1 acquisition risk., Methods: Binding antibody responses were quantified in serum samples from 25 primary endpoint vaccine cases (diagnosed with HIV-1 infection between month 7 and month 24) and 125 randomly sampled frequency-matched vaccine controls (HIV-1 negative at month 24). We prespecified for a primary analysis tier 6 antibody response biomarkers that measure immunoglobulin G (IgG) and immunoglobulin A (IgA) binding to Env proteins and 2 previously assessed T-cell response biomarkers., Results: Envelope-specific IgG responses were significantly correlated with decreased HIV-1 risk. Moreover, the interaction of IgG responses and Env-specific CD8+ T-cell polyfunctionality score had a highly significant association with HIV-1 risk after adjustment for multiple comparisons., Conclusions: Vaccinees with higher levels of Env IgG have significantly decreased HIV-1 risk when CD8+ T-cell responses are low. Moreover, vaccinees with high CD8+ T-cell responses generally have low risk, and those with low CD8+ T-cell and low Env antibody responses have high risk. These findings suggest the critical importance of inducing a robust IgG Env response when the CD8+ T-cell response is low.

Published

2018

2. Sequence and vector shapes vaccine induced antibody effector functions in HIV vaccine trials.

Author

Fischinger, Stephanie, Cizmeci, Deniz, Deng, Davy, Grant, Shannon P., Frahm, Nicole, McElrath, Julie, Fuchs, Jonathan, Bart, Pierre-Alexandre, Pantaleo, Giuseppe, Keefer, Michael, O. Hahn, William, Rouphael, Nadine, Churchyard, Gavin, Moodie, Zoe, Donastorg, Yeycy, Streeck, Hendrik, and Alter, Galit

Subjects

IMMUNE response, AIDS vaccines, VACCINE trials, ADENOVIRUSES, HUMORAL immunity, MONOCYTES, KILLER cells, VIRAL antibodies

Abstract

Despite the advent of long-acting anti-retroviral therapy able to control and prevent infection, a preventative vaccine remains a global priority for the elimination of HIV. The moderately protective RV144 vaccine trial suggested functional IgG1 and IgG3 antibodies were a potential correlate of protection, but the RV144-inspired HVTN702 validation trial failed to demonstrate efficacy despite inducing targeted levels of IgG1/IgG3. Alterations in inserts, and antigens, adjuvant, and regimen also resulted in vaccine induced target quantitative levels of the immune correlates, but drove qualitative changes to the humoral immune response, pointing to the urgent need to define the influence of vaccine strategies on shaping antibody quality, not just quantity. Thus, defining how distinct prime/boost approaches tune long-lived functional antibodies represents an important goal in vaccine development. Here, we compared vaccine responses in Phase I and II studies in humans utilizing various combinations of DNA/vector, vector/vector and DNA/protein HIV vaccines. We found that adenoviral vector immunization, compared to pox-viral vectors, resulted in the most potent IgG1 and IgG3 responses, linked to highly functional antibody activity, including assisting NK cell related functions. Minimal differences were observed in the durability of the functional humoral immune response across vaccine regimens, except for antibody dependent phagocytic function, which persisted for longer periods in the DNA/rAd5 and rAd35/rAd5 regimen, likely driven by higher IgG1 levels. Collectively, these findings suggest adenoviral vectors drive superior antibody quality and durability that could inform future clinical vaccine studies. Trial registration: ClinicalTrials.gov NCT00801697, NCT00961883, NCT02207920, NCT00125970, NCT02852005). Author summary: Previous HIV-1 vaccine trials, including the RV144 efficacy trial that resulted in moderate protection from infection, showed the importance of non-neutralizing antibody responses and their contribution to protection against the virus. However, so far it is unclear how to specifically induce these potentially protective responses via vaccination and the question remains which prime/boost vaccine strategy is the most promising one. In this study, we directly compared the humoral immune response elicited by different heterologous HIV-1 prime/boost vaccine regimen utilizing different components such as DNA, pox- and adenovectors (rAd) and protein. We found that the combination of a DNA or rAd prime with a rAd boost resulted in strong IgG1 and IgG3 responses, which have been shown to be associated with reduced risk in RV144. Moreover, these regimens induced long-lived ADCP responses, an antibody driven functional response mediated by monocytes, that has been shown to be protective in non-human primate trials. In the light of the ongoing efficacy trial HVTN 705 which is utilizing an adenovirus prime, this data could give important input to analyze Fc-mediated functions and non-neutralizing antibody titers in future efficacy trials. [ABSTRACT FROM AUTHOR]

Published

2021

3. Modification of the Association Between T-Cell Immune Responses and Human Immunodeficiency Virus Type 1 Infection Risk by Vaccine-Induced Antibody Responses in the HVTN 505 Trial.

Author

Youyi Fong, Xiaoying Shen, Ashley, Vicki C., Deal, Aaron, Seaton, Kelly E., Chenchen Yu, Grant, Shannon P., Ferrari, Guido, deCamp, Allan C., Bailer, Robert T., Koup, Richard A., Montefiori, David, Haynes, Barton F., Sarzotti-Kelsoe, Marcella, Graham, Barney S., Carpp, Lindsay N., Hammer, Scott M., Sobieszczyk, Magda, Karuna, Shelly, and Swann, Edith

Subjects

ANTIBODY formation, T cells, IMMUNE response, HIV infection risk factors, ADENOVIRUSES, HIV prevention, AIDS vaccines, CLINICAL trials, COMPARATIVE studies, HIV, IMMUNOGLOBULINS, RESEARCH methodology, MEDICAL cooperation, RESEARCH, VIRAL antibodies, EVALUATION research, PHYSIOLOGY

Abstract

Background: HVTN 505 was a human immunodeficiency virus type 1 (HIV-1) preventive vaccine efficacy trial of a DNA/recombinant adenovirus serotype 5 (rAd5) vaccine regimen. We assessed antibody responses measured 1 month after final vaccination (month 7) as correlates of HIV-1 acquisition risk.Methods: Binding antibody responses were quantified in serum samples from 25 primary endpoint vaccine cases (diagnosed with HIV-1 infection between month 7 and month 24) and 125 randomly sampled frequency-matched vaccine controls (HIV-1 negative at month 24). We prespecified for a primary analysis tier 6 antibody response biomarkers that measure immunoglobulin G (IgG) and immunoglobulin A (IgA) binding to Env proteins and 2 previously assessed T-cell response biomarkers.Results: Envelope-specific IgG responses were significantly correlated with decreased HIV-1 risk. Moreover, the interaction of IgG responses and Env-specific CD8+ T-cell polyfunctionality score had a highly significant association with HIV-1 risk after adjustment for multiple comparisons.Conclusions: Vaccinees with higher levels of Env IgG have significantly decreased HIV-1 risk when CD8+ T-cell responses are low. Moreover, vaccinees with high CD8+ T-cell responses generally have low risk, and those with low CD8+ T-cell and low Env antibody responses have high risk. These findings suggest the critical importance of inducing a robust IgG Env response when the CD8+ T-cell response is low. [ABSTRACT FROM AUTHOR]

Published

2018

4. Transient Peripheral Immune Activation follows Elective Sigmoidoscopy or Circumcision in a Cohort Study of MSM at Risk of HIV Infection.

Author

Lama, Javier R., Karuna, Shelly T., Grant, Shannon P., Swann, Edith M., Ganoza, Carmela, Segura, Patricia, Montano, Silvia M., Lacherre, Martin, De Rosa, Stephen C., Buchbinder, Susan, Sanchez, Jorge, McElrath, M. Juliana, Lemos, Maria P., and null, null

Subjects

HIV prevention, SIGMOIDOSCOPY, CIRCUMCISION, AIDS vaccines, DRUG design, COHORT analysis

Abstract

Background: Rectal and genital sampling in HIV prevention trials permits assessments at the site of HIV entry. Yet the safety and acceptability of circumcision and sigmoidoscopy (and associated abstinence recommendations) are unknown in uncircumcised men who have sex with men (MSM) at high risk of HIV infection. Methods: Twenty-nine HIV-seronegative high-risk Peruvian MSM agreed to elective sigmoidoscopy biopsy collections (weeks 2 and 27) and circumcision (week 4) in a 28-week cohort study designed to mimic an HIV vaccine study mucosal collection protocol. We monitored adherence to abstinence recommendations, procedure-related complications, HIV infections, peripheral immune activation, and retention. Results: Twenty-three (79.3%) underwent a first sigmoidoscopy, 21 (72.4%) were circumcised, and 16 (55.2%) completed a second sigmoidoscopy during the study period. All who underwent procedures completed the associated follow-up safety visits. Those completing the procedures reported they were well tolerated, and complication rates were similar to those reported in the literature. Immune activation was detected during the healing period (1 week post-sigmoidoscopy, 6 weeks post-circumcision), including increases in CCR5+CD4+T cells and α4β7+CD4+T cells. Most participants adhered to post-circumcision abstinence recommendations whereas reduced adherence occurred post-sigmoidoscopy. Conclusion: Rectosigmoid mucosal and genital tissue collections were safe in high-risk MSM. Although the clinical implications of the post-procedure increase in peripheral immune activation markers are unknown, they reinforce the need to provide ongoing risk reduction counseling and support for post-procedure abstinence recommendations. Future HIV vaccine studies should also consider the effects of mucosal and tissue collections on peripheral blood endpoints in trial design and analysis. Trial Registration: ClinicalTrials.gov [ABSTRACT FROM AUTHOR]

Published

2016