Your search keyword '"Gupta, Shaili"' showing total 2 results

1. Serum Neutralizing Antibody Titers 12 Months After Coronavirus Disease 2019 Messenger RNA Vaccination: Correlation to Clinical Variables in an Adult, US Population.

Author

Zhao, Min, Slotkin, Rebecca, Sheth, Amar H, Pischel, Lauren, Kyriakides, Tassos C, Emu, Brinda, McNamara, Cynthia, Shi, Qiaosu, Delgobbo, Jaden, Xu, Jin, Marhoffer, Elizabeth, Mercer-Falkoff, Aleagia, Holleck, Jürgen, Ardito, David, Sutton, Richard E, and Gupta, Shaili

Subjects

EVALUATION of medical care, IMMUNOGLOBULINS, COVID-19, IMMUNIZATION, COVID-19 vaccines, MULTIPLE regression analysis, TIME, MESSENGER RNA, QUALITY of life, IMMUNITY, DESCRIPTIVE statistics, RESEARCH funding, VIRAL antibodies, COMORBIDITY

Abstract

Background We studied whether comorbid conditions affect strength and duration of immune responses after severe acute respiratory syndrome coronavirus 2 (SARS-CoV-2) messenger RNA vaccination in a US-based, adult population. Methods Sera (before and after BNT162b2 vaccination) were tested serially up to 12 months after 2 doses of vaccine for SARS-CoV-2-anti-Spike neutralizing capacity by pseudotyping assay in 124 individuals; neutralizing titers were correlated to clinical variables with multivariate regression. Postbooster (third dose) effect was measured at 1 and 3 months in 72 and 88 subjects, respectively. Results After completion of primary vaccine series, neutralizing antibody half maximal inhibitory concentration (IC50) values were high at 1 month (14-fold increase from prevaccination), declined at 6 months (3.3-fold increase), and increased at 1 month postbooster (41.5-fold increase). Three months postbooster, IC50 decreased in coronavirus disease (COVID)-naïve individuals (18-fold increase) and increased in prior COVID 2019 (COVID-19+) individuals (132-fold increase). Age >65 years (β = −0.94, P =.001) and malignancy (β = −0.88, P =.002) reduced strength of response at 1 month. Both neutralization strength and durability at 6 months, respectively, were negatively affected by end-stage renal disease ([β = −1.10, P =.004]; [β = −0.66, P =.014]), diabetes mellitus ([β = −0.57, P =.032]; [β = −0.44, P =.028]), and systemic steroid use ([β = −0.066, P =.032]; [β = −0.55, P =.037]). Postbooster IC50 was robust against WA-1 and B.1.617.2. Postbooster neutralization increased with prior COVID-19 (β = 2.9, P <.0001), and malignancy reduced neutralization response (β = −0.68, P =.03), regardless of infection status. Conclusions Multiple clinical factors affect the strength and duration of neutralization response after primary series vaccination, but not the postbooster dose strength. Malignancy was associated with lower booster-dose response regardless of prior COVID infection, suggesting a need for clinically guided vaccine regimens. [ABSTRACT FROM AUTHOR]

Published

2023

2. Long-term quantitative assessment of anti-SARS-CoV-2 spike protein immunogenicity (QUASI) after COVID-19 vaccination in older people living with HIV (PWH).

Author

Tuan, Jessica J., Zapata, Heidi, Barakat, Lydia, Andrews, Laurie, Behnegar, Anousheh, Kim, Yee Won, Kayani, Jehanzeb, Mutic, Suzana, Ryall, Linda, Turcotte, Barbara, Critch-Gilfillan, Terese, Zhao, Min, Salahuddin, Syim, Gupta, Shaili, Sutton, Richard, Friedland, Gerald, Emu, Brinda, and Ogbuagu, Onyema

Subjects

HIV-positive persons, OLDER people, COVID-19 vaccines, IMMUNE response, WILCOXON signed-rank test

Abstract

Background: The durability of immune responses to COVID-19 vaccines among older people living with HIV (PWH) is clinically important.Methods: We aimed to assess vaccine-induced humoral immunity and durability in older PWH (≥ 55 years, n = 26) over 6 months (post-initial BNT162b2 series). A secondary and exploratory objective was to assess T-cell response and BNT162b2 booster reactogenicity, respectively. Our Visit 1 (3 weeks post-initial BNT162b2 dose) SARS-CoV-2 humoral immunity results are previously reported; these subjects were recruited for Visit 2 [2 weeks (+ 1 week window) post-second vaccination] and Visit 3 [6 months (± 2 week window) post-initial vaccination] in a single-center longitudinal observational study. Twelve participants had paired Visit 2/3 SARS-CoV-2 Anti-Spike IgG data. At Visit 3, SARS-CoV-2 Anti-Spike IgG testing occurred, and 5 subjects underwent T-cell immune response evaluation. Thereafter, subjects were offered BNT162b2 booster (concurrent day outside our study) per US FDA/CDC guidance; reactogenicity was assessed. The primary study outcome was presence of detectable Visit 3 SARS-CoV-2 Anti-Spike-1-RBD IgG levels. Secondary and exploratory outcomes were T-cell immune response and BNT162b2 booster reactogenicity, respectively. Wilcoxon signed-rank tests analyzed median SARS-CoV-2 Anti-Spike IgG 6-month trends.Results: At Visit 3, 26 subjects underwent primary analysis with demographics noted: Median age 61 years; male n = 16 (62%), female n = 10 (38%); Black n = 13 (50%), White n = 13 (50%). Most subjects (n = 20, 77%) had suppressed HIV viremia on antiretroviral therapy, majority (n = 24, 92%) with CD4 > 200 cells/µL. At Visit 3, 26/26 (100%) had detectable Anti-Spike-1-RBD (≥ 0.8 U/mL). Among 12 subjects presenting to Visit 2/3, median SARS-CoV-2 Anti-Spike 1-RBD was 2087 U/mL at Visit 2, falling to 581.5 U/mL at Visit 3 (p = 0.0923), with a median 3.305-fold decrease over 6 months. Among subjects (n = 5) with 6-month T-cell responses measured, all had detectable cytokine-secreting anti-spike CD4 responses; 3 had detectable CD4 + Activation induced marker (AIM) + cells. Two had detectable cytokine-secreting CD8 responses, but all had positive CD8 + AIM + cells.Conclusions: Among older PWH, SARS-CoV-2 Anti-Spike IgG and virus-specific T-cell responses are present 6 months post-primary BNT162b2 vaccination, and although waning, suggest retention of some degree of long-term protective immunity. [ABSTRACT FROM AUTHOR]

Published

2022