Your search keyword '"Odoch, Geoffrey"' showing total 19 results

1. Bacterial microbiome and host inflammatory gene expression in foreskin tissue

Author

Maust, Brandon S., Petkov, Stefan, Herrera, Carolina, Feng, Colin, Brown, Bryan P., Lebina, Limakatso, Opoka, Daniel, Ssemata, Andrew, Pillay, Natasha, Serwanga, Jennifer, Seatlholo, Portia, Namubiru, Patricia, Odoch, Geoffrey, Mugaba, Susan, Seiphetlo, Thabiso, Gray, Clive M., Kaleebu, Pontiano, Webb, Emily L., Martinson, Neil, Chiodi, Francesca, Fox, Julie, and Jaspan, Heather B.

Published

2023

2. Dose finding study for on-demand HIV pre-exposure prophylaxis for insertive sex in sub-Saharan Africa: results from the CHAPS open label randomised controlled trial

Author

Ahmed, Nadia, Alinde, Berenice, Alieu, Amara, Atujuna, Millicent, Awino, Esther, Bekker, Linda-Gail, Callebaut, Christian, Chiodi, Francesca, Chirenje, Mike, Dietrich, Janan, Dorfman, Jeffrey, Else, Laura, Fox, Julie, Gray, Clive, Hansen, Christian Holm, Herrera, Carolina, Hornschuh, Stefanie, Kakande, Ayoub, Kaleebu, Pontiano, Kelly, Charles, Khoo, Saye, Khunwane, Mamkiri, Lebina, Limaktso, Makhura, Joseph, Mangxilana, Nomvuyo, Martinson, Neil, Mugaba, Susan, Muhumuza, Richard, Kibengo, Freddie Mukasa, Mutonyi, Gertrude, Mungate, Lucia, Nabukeera, Winnie, Nagawa, Rehema, Nalubega, Phiona, Namubiru, Patricia, Nash, Stephen, Ndekezi, Denis, Nematadzira, Teacler, Nobula, Lumka, O'Hagan, Kyle, Odoch, Geoffrey, Opoka, Daniel, Penchala, Sujan Dilly, Petkov, Stefan, Pillay, Azure-Dee, Rooney, Jim, Rousseau, Elzette, Ruzagira, Eugene, Sango, Alison, Seatlholo, Ntombexolo, Seeley, Janet, Seiphetlo, Thabiso, Serwanga, Jennifer, Shattock, Robin, Ssemata, Andrew S., Stranix-Chibanda, Lynda, Tshabalala, Gugulethu, Webb, Emily, Weiss, Helen, Limakatso, Lebina, Seiphetlo, Thabiso B., Seatlholo, Portia, Gray, Clive M., and Webb, Emily L.

Published

2023

3. A randomized clinical trial of on-demand oral pre-exposure prophylaxis does not modulate lymphoid/myeloid HIV target cell density in the foreskin

Author

Rametse, Cosnet L., Webb, Emily L., Herrera, Carolina, Alinde, Berenice, Besethi, Asiphe, Motaung, Bongani, Mbangiwa, Tshepiso, Leach, Lloyd, Sebaa, Shorok, Pillay, Azure-Dee A.P., Seiphetlo, Thabiso B., Malhangu, Boitshoko, Petkov, Stefan, Else, Laura, Mugaba, Susan, Namubiru, Patricia, Odoch, Geoffrey, Opoka, Daniel, Serwanga, Jennifer, Ssemata, Andrew S., Kaleebu, Pontiano, Khoo, Saye, Lebina, Limakatso, Martinson, Neil, Chiodi, Francesca, Fox, Julie, and Gray, Clive M.

Published

2023

4. Gene expression of tight junctions in foreskin is not affected by HIV pre-exposure prophylaxis.

Author

Webb, Emily L., Petkov, Stefan, Yun, Heejin, Else, Laura, Lebina, Limakatso, Serwanga, Jennifer, Pillay, Azure-Dee A. P., Seiphetlo, Thabiso B., Mugaba, Susan, Namubiru, Patricia, Odoch, Geoffrey, Opoka, Daniel, Ssemata, Andrew S., Kaleebu, Pontiano, Khoo, Saye, Martinson, Neil, Fox, Julie, Gray, Clive M., Herrera, Carolina, and Chiodi, Francesca

Subjects

MALE reproductive organs, GENE expression, PRE-exposure prophylaxis, TIGHT junctions, CIRCUMCISION

Abstract

Introduction: Tight junctions (TJs) serve as permeability filters between the internal and external cellular environment. A large number of proteins have been identified to be localized at the TJs. Due to limitations in tissue collection, TJs in the male genital tract have been understudied. Methods: We analysed the transcriptomics of 132 TJ genes in foreskin tissue of men requesting voluntary medical male circumcision (VMMC) and enrolled in the Combined HIV Adolescent Prevention Study (CHAPS) trial conducted in South Africa and Uganda (NCT03986970). The trial evaluated the dose requirements for event-driven HIV pre-exposure prophylaxis (PrEP) with emtricitabine-tenofovir (FTC-TDF) or emtricitabine-tenofovir alafenamide (FTC-TAF) during insertive sex. A total of 144 participants were randomized to either control arm or one of 8 PrEP arms (n=16/arm), receiving oral FTC-TDF or FTC-TAF over one or two days. Following in vivo oral PrEP dosing and VMMC, the expression level of three important TJ proteins (CLDN-1, OCN and ZO-1) was measured ex vivo in foreskin tissue by Western blot. The expression of cytokine genes implicated in TJ regulation was determined. Non-parametric Kruskal-Wallis tests were used to compare TJ gene expression and protein levels by type of PrEP received, and Spearman's correlation coefficients were calculated to assess whether TJ gene expression levels were related to cytokine gene levels or to PrEP drug concentrations and their active intracellularly phosphorylated metabolites. Results: A high level of expression in foreskin tissue was found for 118 (of 132) TJ genes analysed; this finding contributed to create a map of TJ components within the male genital tract. Importantly, PrEP regimens tested in the CHAPS trial did not affect the expression of TJ genes and the analysed proteins in the foreskin; thus, further supporting the safety of this prevention strategy against HIV-1 transmission during insertive sex. Additionally, we identified the level of several cytokines' genes to be correlated to TJ gene expression: among them, IL-18, IL-33 and VEGF. Discussion: TJs can limit viral entry into target cells; to affect this biological function viruses can reduce the expression of TJ proteins. Our study, on the expression and regulation of TJs in the foreskin, contribute important knowledge for PrEP safety and further design of HIV-1 prophylaxis. [ABSTRACT FROM AUTHOR]

Published

2024

5. The subdued post-boost spike-directed secondary IgG antibody response in Ugandan recipients of the Pfizer-BioNTech BNT162b2 vaccine has implications for local vaccination policies

Author

Ankunda, Violet, primary, Katende, Joseph Ssebwana, additional, Oluka, Gerald Kevin, additional, Sembera, Jackson, additional, Baine, Claire, additional, Odoch, Geoffrey, additional, Ejou, Peter, additional, Kato, Laban, additional, Kaleebu, Pontiano, additional, Serwanga, Jennifer, additional, Akoli, Christine Hermilia, additional, Namuyanja, Angela, additional, Opio, Solomon, additional, Kalyebi, Arthur Watelo, additional, Ssali, Ivan, additional, Gombe, Ben, additional, Mugaba, Susan, additional, and Nantambi, Hellen, additional

Published

2024

6. Persistent and robust antibody responses to ChAdOx1-S Oxford-AstraZeneca (ChAdOx1-S, Covishield) SARS-CoV-2 vaccine observed in Ugandans across varied baseline immune profiles.

Author

Serwanga, Jennifer, Oluka, Gerald Kevin, Baine, Claire, Ankunda, Violet, Sembera, Jackson, Kato, Laban, Katende, Joseph Ssebwana, Odoch, Geoffrey, Auma, Betty Oliver, Gombe, Ben, Musenero, Monica, and Kaleebu, Pontiano

Subjects

COVID-19 vaccines, ANTIBODY formation, IMMUNOGLOBULINS, IMMUNE response, IMMUNOGLOBULIN M, OPACITY (Optics), IMMUNOGLOBULIN G

Abstract

Understanding SARS-CoV-2 vaccine-induced antibody responses in varied antigenic and serological prior exposures can guide optimal vaccination strategies for enhanced immunogenicity. We evaluated spike (S)-directed IgG, IgM, and IgA antibody optical densities (ODs) and concentrations to the two-dose ChAdOx1-S Oxford-AstraZeneca (ChAdOx1-S, Covishield) SARS-CoV-2 vaccine in 67 Ugandans, categorised by prior infection and baseline S-IgG histories: uninfected and S-IgG-negative (n = 12); previously infected yet S-IgG-negative (n = 17); and previously infected with S-IgG-positive status (n = 38). Antibody dynamics were compared across eight timepoints from baseline till nine months. S-IgG antibodies remained consistently potent across all groups. Individuals with prior infections maintained robust S-IgG levels, underscoring the endurance of hybrid immunity. In contrast, those without prior exposure experienced an initial surge in S-IgG after the primary dose but no subsequent significant increase post-boost. However, they reached levels parallel to the previously exposed groups. S-IgM levels remained moderate, while S-IgA persisted in individuals with prior antigen exposure. ChAdOx1-S, Covishield vaccine elicited robust and sustained antibody responses in recipients, irrespective of their initial immune profiles. Hybrid immunity showed higher responses, aligning with global observations. Early post-vaccination antibody levels could predict long-term immunity, particularly in individuals without virus exposure. These findings can inform vaccine strategies and pandemic management. [ABSTRACT FROM AUTHOR]

Published

2024

7. The Distinct Absence of a Post-boost Spike-IgG Antibody Surge in Ugandan Recipients of the Pfizer-BioNTech Vaccine Has Implications for Vaccination Policies

Author

Serwanga, Jennifer, primary, Ankunda, Violet, additional, Katende, Joseph Ssebwana, additional, Sembera, Jackson, additional, Oluka, Gerald Kevin, additional, Baine, Claire, additional, Odoch, Geoffrey, additional, Ejou, Peter, additional, Kato, Laban, additional, and Kaleebu, Pontiano, additional

Published

2023

8. Dose finding study for on-demand HIV pre-exposure prophylaxis for insertive sex in sub-Saharan Africa: results from the CHAPS open label randomised controlled trial

Author

Herrera, Carolina, primary, Serwanga, Jennifer, additional, Else, Laura, additional, Limakatso, Lebina, additional, Opoka, Daniel, additional, Ssemata, Andrew S., additional, Pillay, Azure-Dee, additional, Namubiru, Patricia, additional, Seiphetlo, Thabiso B., additional, Odoch, Geoffrey, additional, Mugaba, Susan, additional, Seatlholo, Portia, additional, Alieu, Amara, additional, Penchala, Sujan Dilly, additional, Muhumuza, Richard, additional, Alinde, Berenice, additional, Petkov, Stefan, additional, O'Hagan, Kyle, additional, Callebaut, Christian, additional, Seeley, Janet, additional, Weiss, Helen, additional, Khoo, Saye, additional, Chiodi, Francesca, additional, Gray, Clive M., additional, Kaleebu, Pontiano, additional, Webb, Emily L., additional, Martinson, Neil, additional, Fox, Julie, additional, Ahmed, Nadia, additional, Atujuna, Millicent, additional, Awino, Esther, additional, Bekker, Linda-Gail, additional, Chirenje, Mike, additional, Dietrich, Janan, additional, Dorfman, Jeffrey, additional, Gray, Clive, additional, Hansen, Christian Holm, additional, Herrera, Carolina, additional, Hornschuh, Stefanie, additional, Kakande, Ayoub, additional, Kelly, Charles, additional, Khunwane, Mamkiri, additional, Lebina, Limaktso, additional, Makhura, Joseph, additional, Mangxilana, Nomvuyo, additional, Kibengo, Freddie Mukasa, additional, Mutonyi, Gertrude, additional, Mungate, Lucia, additional, Nabukeera, Winnie, additional, Nagawa, Rehema, additional, Nalubega, Phiona, additional, Nash, Stephen, additional, Ndekezi, Denis, additional, Nematadzira, Teacler, additional, Nobula, Lumka, additional, Rooney, Jim, additional, Rousseau, Elzette, additional, Ruzagira, Eugene, additional, Sango, Alison, additional, Seatlholo, Ntombexolo, additional, Seiphetlo, Thabiso, additional, Shattock, Robin, additional, Stranix-Chibanda, Lynda, additional, Tshabalala, Gugulethu, additional, and Webb, Emily, additional

Published

2023

9. Sustained S-IgG and S-IgA antibodies to Moderna's mRNA-1273 vaccine in a Sub-Saharan African cohort suggests need for booster timing reconsiderations.

Author

Serwanga, Jennifer, Ankunda, Violet, Katende, Joseph Ssebwana, Baine, Claire, Oluka, Gerald Kevin, Odoch, Geoffrey, Nantambi, Hellen, Mugaba, Susan, Namuyanja, Angella, Ssali, Ivan, Ejou, Peter, Kato, Laban, Musenero, Monica, and Kaleebu, Pontiano

Subjects

COVID-19 vaccines, BOOSTER vaccines, VACCINE immunogenicity, IMMUNOGLOBULINS, ANTIBODY formation

Abstract

Introduction: This study sought to elucidate the long-term antibody responses to the Moderna mRNA-1273 COVID-19 vaccine within a Ugandan cohort, aiming to contribute to the sparse data on m-RNA vaccine immunogenicity in Sub-Saharan Africa. Methods: We tracked the development and persistence of the elicited antibodies in 19 participants aged 18 to 67, who received two doses of the mRNA-1273 vaccine. A validated enzyme-linked immunosorbent assay (ELISA) was used to quantify SARS-CoV-2-specific IgG, IgM, and IgA antibodies against the spike (S) and nucleoproteins (N). The study's temporal scope extended from the baseline to one year, capturing immediate and long-term immune responses. Statistical analyses were performed using the Wilcoxon test to evaluate changes in antibody levels across predetermined intervals with the Hochberg correction for multiple comparisons. Results: Our results showed a significant initial rise in spike-directed IgG (S-IgG) and spike-directed IgA (S-IgA) levels, which remained elevated for the duration of the study. The S-IgG concentrations peaked 14 days afterboosting, while spikedirected IgM (S-IgM) levels were transient, aligning with their early response role. Notably, post-booster antibody concentrations did not significantly change. Prior S-IgG status influenced the post-priming S-IgA dynamics, with baseline S-IgG positive individuals maintaining higher S-IgA responses, a difference that did not reach statistical difference post-boost. Three instances of breakthrough infections: two among participants who exhibited baseline seropositivity for SIgG, and one in a participant initially seronegative for S-IgG. Discussion: In conclusion, the mRNA-1273 vaccine elicited robust and persistent S-IgG and S-IgA antibody responses, particularly after the first dose, indicating potential for long-term immunity. Prior viral exposure enhances postvaccination S-IgA responses compared to naive individuals, which aligned with the prior-naïve, post-boost. The stable antibody levels observed post-booster dose, remaining high over an extended period, with no significant secondary rise, and no difference by baseline exposure, suggest that initial vaccination may sufficiently prime the immune system for prolonged protection in this population, allowing for potential to delay booster schedules as antibody responses remained high at the time of boosting. This finding calls for a reassessment of the booster dose scheduling in this demographic. [ABSTRACT FROM AUTHOR]

Published

2024

10. Pre-pandemic SARS-CoV-2-specific IFN-γ and antibody responses were low in Ugandan samples and significantly reduced in HIV-positive specimens

Author

Nantambi, Hellen, Sembera, Jackson, Ankunda, Violet, Ssali, Ivan, Kalyebi, Arthur Watelo, Oluka, Gerald Kevin, Kato, Laban, Ubaldo, Bahemuka, Kibengo, Freddie, Katende, Joseph Ssebwana, Gombe, Ben, Baine, Claire, Odoch, Geoffrey, Mugaba, Susan, Sande, Obondo James, Kaleebu, Pontiano, and Serwanga, Jennifer

Subjects

Immunology, Immunology and Allergy

Published

2023

11. On-Demand HIV Pre-Exposure Prophylaxis Dose Finding Study for Insertive Sex in Young Men in Sub-Saharan Africa: Comparison of Emtricitabine-Tenofovir Disoproxil Fumarate and Emtricitabine-Tenofovir Alafenamide in an Open-Label Randomised Controlled Trial

Author

Herrera, Carolina, primary, Serwanga, Jennifer, additional, Else, Laura, additional, Lebina, Limakatso, additional, Opoka, Daniel, additional, Ssemata, Andrew S., additional, Pillay, Azure-Dee, additional, Namubiru, Patricia, additional, Seiphetlo, Thabiso B., additional, Odoch, Geoffrey, additional, Mugaba, Susan, additional, Seatlholo, Portia, additional, Alieu, Amara, additional, Dilly Penchala, Sujan, additional, Muhumuza, Richard, additional, Alinde, Berenice, additional, Petkov, Stefan, additional, O’Hagan, Kyle, additional, Callebaut, Christian, additional, Seeley, Janet, additional, Weiss, Helen A., additional, Khoo, Saye, additional, Chiodi, Francesca, additional, Gray, Clive M., additional, Kaleebu, Pontiano, additional, Webb, Emily, additional, Martinson, Neil A., additional, and Fox, Julie, additional

Published

2023

12. Sustained spike-specific IgG antibodies following CoronaVac (Sinovac) vaccination in sub-Saharan Africa, but increased breakthrough infections in baseline spike-naive individuals.

Author

Sembera, Jackson, Baine, Claire, Ankunda, Violet, Katende, Joseph Ssebwana, Oluka, Gerald Kevin, Akoli, Christine Hermilia, Kato, Laban, Odoch, Geoffrey, Ejou, Peter, Opio, Solomon, Musenero, Monica, Kaleebu, Pontiano, and Serwanga, Jennifer

Subjects

BREAKTHROUGH infections, COVID-19 vaccines, IMMUNOGLOBULIN G, VACCINE effectiveness, IMMUNOGLOBULINS

Abstract

Introduction: This study investigated the antibody responses to the inactivated COVID-19 vaccine, CoronaVac (Sinovac Biotech) in the African population to provide valuable insights into long-term immunity and breakthrough infections against SARS-CoV-2 in individuals with varying prior IgG seropositivity. Methods: Real-life cohorts were used to longitudinally track antibody levels against the SARS-CoV-2 spike and nucleoprotein in 60 participants over 12 months to examine the levels of multiple antibody isotypes (S-IgG, S-IgM, S-IgA, N-IgG, and N-IgM). Results: Throughout the 12 months, we observed consistently high and stable seropositivity rates for spike-IgG antibodies, spike-IgM antibodies showed a decline in frequencies over time, and spike-IgA levels remained moderate and stable. Vaccinated individuals previously positive for spike-IgG antibodies demonstrated strong and persistent seropositivity, while those initially negative experienced a gradual and delayed increase in seropositivity rates. The fold change analysis of S- and N-antibody responses demonstrated a consistently stable and comparable profile over time, indicating that vaccine-induced antibody responses remain constant and lack significant fluctuations beyond the initial boost. The study emphasized that individuals lacking previous IgG positivity showed reduced vaccine-induced spike-IgG antibodies and were more susceptible to breakthrough infections, highlighting their higher vulnerability. All cases of breakthrough infections were asymptomatic, indicating the conferred protection to the vaccinated individuals. Discussion: The findings corroborated earlier studies on the effectiveness of the CoronaVac vaccine and emphasized the significance of accounting for preexisting seropositivity in vaccine assessments. This study effectively demonstrated durable antibody responses against SARS-CoV-2 in the African population following the CoronaVac vaccination, providing crucial insights for informing vaccination strategies and safeguarding vulnerable populations. Continuous surveillance is imperative for tracking breakthrough infections and monitoring waning immunity. The insights gained offer crucial direction for public health strategies and enhance comprehension of vaccine effectiveness in sub-Saharan Africa. Further research should explore functional outcomes, cellular immune responses, and the vaccine's effectiveness against different variants to enhance our understanding and optimize vaccine strategies. [ABSTRACT FROM AUTHOR]

Published

2023

13. Short-term oral pre-exposure prophylaxis against HIV-1 modulates the transcriptome of foreskin tissue in young men in Africa

Author

Petkov, Stefan, primary, Herrera, Carolina, additional, Else, Laura, additional, Lebina, Limakatso, additional, Opoka, Daniel, additional, Seiphetlo, Thabiso B., additional, Pillay, Azure-Dee AP., additional, Mugaba, Susan, additional, Namubiru, Patricia, additional, Odoch, Geoffrey, additional, Ssemata, Andrew S., additional, Serwanga, Jennifer, additional, Kaleebu, Pontiano, additional, Webb, Emily L., additional, Khoo, Saye, additional, Martinson, Neil, additional, Gray, Clive M., additional, Fox, Julie, additional, and Chiodi, Francesca, additional

Published

2022

14. Bacterial Microbiome and Host Inflammatory Gene Expression in Foreskin Tissue

Author

Maust, Brandon S., primary, Petkov, Stefan, additional, Herrera, Carolina, additional, Feng, Colin, additional, Brown, Bryan P., additional, Lebina, Limakatso, additional, Opoka, Daniel, additional, Ssemata, Andrew, additional, Pillay, Natasha, additional, Serwanga, Jennifer, additional, Seatlholo, Portia, additional, Namubiru, Patricia, additional, Odoch, Geoffrey, additional, Mugaba, Susan, additional, Seiphetlo, Thabiso, additional, Gray, Clive M., additional, Kaleebu, Pontiano, additional, Webb, Emily L., additional, Martinson, Neil, additional, Chiodi, Francesca, additional, Fox, Julie, additional, and Jaspan, Heather B., additional

Published

2022

15. Mobilization of systemic CCL4 following HIV pre-exposure prophylaxis in young men in Africa

Author

Petkov, Stefan, primary, Herrera, Carolina, additional, Else, Laura, additional, Mugaba, Susan, additional, Namubiru, Patricia, additional, Odoch, Geoffrey, additional, Opoka, Daniel, additional, Pillay, Azure-Dee A. P., additional, Seiphetlo, Thabiso B., additional, Serwanga, Jennifer, additional, Ssemata, Andrew S., additional, Kaleebu, Pontiano, additional, Webb, Emily L., additional, Khoo, Saye, additional, Lebina, Limakatso, additional, Gray, Clive M., additional, Martinson, Neil, additional, Fox, Julie, additional, and Chiodi, Francesca, additional

Published

2022

16. Seroprevalence and durability of antibody responses to AstraZeneca vaccination in Ugandans with prior mild or asymptomatic COVID-19: implications for vaccine policy .

Author

Serwanga, Jennifer, Baine, Claire, Mugaba, Susan, Ankunda, Violet, Auma, Betty Oliver, Oluka, Gerald Kevin, Kato, Laban, Kitabye, Isaac, Sembera, Jackson, Odoch, Geoffrey, Ejou, Peter, Nalumansi, Amina, Gombe, Ben, Musenero, Monica, and Kaleebu, Pontiano

Subjects

ANTIBODY formation, BOOSTER vaccines, VACCINATION, COVID-19 vaccines, COVID-19, HYPERCOAGULATION disorders

Abstract

Introduction: The duration and timing of immunity conferred by COVID-19 vaccination in sub-Saharan Africa are crucial for guiding pandemic policy interventions, but systematic data for this region is scarce. This study investigated the antibody response after AstraZeneca vaccination in COVID-19 convalescent Ugandans. Methods: We recruited 86 participants with a previous rt-PCR-confirmed mild or asymptomatic COVID-19 infection and measured the prevalence and levels of spike-directed IgG, IgM, and IgA antibodies at baseline, 14 and 28 days after the first dose (priming), 14 days after the second dose (boosting), and at six- and nine-months post-priming. We also measured the prevalence and levels of nucleoprotein-directed antibodies to assess breakthrough infections. Results: Within two weeks of priming, vaccination substantially increased the prevalence and concentrations of spike-directed antibodies (p < 0.0001, Wilcoxon signed rank test), with 97.0% and 66% of vaccinated individuals possessing S-IgG and S-IgA antibodies before administering the booster dose. S-IgM prevalence changed marginally after the initial vaccination and barely after the booster, consistent with an already primed immune system. However, we also observed a rise in nucleoprotein seroprevalence, indicative of breakthroughs six months after the initial vaccination. Discussion: Our results suggest that vaccination of COVID-19 convalescent individuals with the AstraZeneca vaccine induces a robust and differential spike-directed antibody response. The data highlights the value of vaccination as an effective method for inducing immunity in previously infected individuals and the importance of administering two doses to maintain protective immunity. Monitoring anti-spike IgG and IgA when assessing vaccine-induced antibody responses is suggested for this population; assessing S-IgM will underestimate the response. The AstraZeneca vaccine is a valuable tool in the fight against COVID-19. Further research is needed to determine the durability of vaccineinduced immunity and the potential need for booster doses. [ABSTRACT FROM AUTHOR]

Published

2023

17. Rapid, early, and potent Spike-directed IgG, IgM, and IgA distinguish asymptomatic from mildly symptomatic COVID-19 in Uganda, with IgG persisting for 28 months.

Author

Serwanga, Jennifer, Ankunda, Violet, Sembera, Jackson, Kato, Laban, Oluka, Gerald Kevin, Baine, Claire, Odoch, Geoffrey, Kayiwa, John, Auma, Betty Oliver, Jjuuko, Mark, Nsereko, Christopher, Cotten, Matthew, Onyachi, Nathan, Muwanga, Moses, Lutalo, Tom, Fox, Julie, Musenero, Monica, and Kaleebu, Pontiano

Subjects

IMMUNOGLOBULIN G, IMMUNOGLOBULIN A, ANTIBODY formation, COVID-19, ASYMPTOMATIC patients, HIV seroconversion

Abstract

Introduction: Understanding how spike (S)-, nucleoprotein (N)-, and RBDdirected antibody responses evolved in mild and asymptomatic COVID-19 in Africa and their interactions with SARS-CoV-2 might inform development of targeted treatments and vaccines. Methods: Here, we used a validated indirect in-house ELISA to characterise development and persistence of S- and N-directed IgG, IgM, and IgA antibody responses for 2430 SARS-CoV-2 rt-PCR-diagnosed Ugandan specimens from 320 mild and asymptomatic COVID-19 cases, 50 uninfected contacts, and 54 uninfected non-contacts collected weekly for one month, then monthly for 28 months. Results: During acute infection, asymptomatic patients mounted a faster and more robust spike-directed IgG, IgM, and IgA response than those with mild symptoms (Wilcoxon rank test, p-values 0.046, 0.053, and 0.057); this was more pronounced in males than females. Spike IgG antibodies peaked between 25 and 37 days (86.46; IQR 29.47-242.56 BAU/ml), were significantly higher and more durable than N- and RBD IgG antibodies and lasted for 28 months. Anti-spike seroconversion rates consistently exceeded RBD and nucleoprotein rates. Spikeand RBD-directed IgG antibodies were positively correlated until 14 months (Spearman's rank correlation test, p-values 0.0001 to 0.05), although RBD diminished faster. Significant anti-spike immunity persisted without RBD. 64% and 59% of PCR-negative, non-infected non-contacts and suspects, exhibited baseline SARS-CoV-2 N-IgM serological cross-reactivity, suggesting undetected exposure or abortive infection. N-IgG levels waned after 787 days, while N-IgM levels remained undetectable throughout. Discussion: Lower N-IgG seroconversion rates and the absence of N-IgM indicate that these markers substantially underestimate the prior exposure rates. Our findings provide insights into the development of S-directed antibody responses in mild and asymptomatic infections, with varying degrees of symptoms eliciting distinct immune responses, suggesting distinct pathogenic pathways. These longer-lasting data inform vaccine design, boosting strategies, and surveillance efforts in this and comparable settings. [ABSTRACT FROM AUTHOR]

Published

2023

18. Mobilization of systemic CCL4 following HIV preexposure prophylaxis in young men in Africa.

Author

Petkov, Stefan, Herrera, Carolina, Else, Laura, Mugaba, Susan, Namubiru, Patricia, Odoch, Geoffrey, Opoka, Daniel, Pillay, Azure-Dee A. P., Seiphetlo, Thabiso B., Serwanga, Jennifer, Ssemata, Andrew S., Kaleebu, Pontiano, Webb, Emily L., Khoo, Saye, Lebina, Limakatso, Gray, Clive M., Martinson, Neil, Fox, Julie, and Chiodi, Francesca

Subjects

YOUNG men, PRE-exposure prophylaxis, EMTRICITABINE-tenofovir, HIV, MASS spectrometry, PREVENTIVE medicine, EMTRICITABINE

Abstract

HIV-1 pre-exposure prophylaxis (PrEP) relies on inhibition of HIV-1 replication steps. To understand how PrEP modulates the immunological environment, we derived the plasma proteomic profile of men receiving emtricitabine-tenofovir (FTC-TDF) or emtricitabine-tenofovir alafenamide (FTC-TAF) during the CHAPS trial in South Africa and Uganda (NCT03986970). The CHAPS trial randomized 144 participants to one control and 8 PrEP arms, differing by drug type, number of PrEP doses and timing from final PrEP dose to sampling. Blood was collected pre- and post-PrEP. The inflammatory profile of plasma samples was analyzed using Olink (N=92 proteins) and Luminex (N=33) and associated with plasma drug concentrations using mass spectrometry. The proteins whose levels changed most significantly from pre- to post-PrEP were CCL4, CCL3 and TNF-a; CCL4 was the key discriminator between pre- and post-PrEP samples. CCL4 and CCL3 levels were significantly increased in post-PrEP samples compared to control specimens. CCL4 was significantly correlated with FTC drug levels in plasma. Production of inflammatory chemokines CCL4 and CCL3 in response to short-term PrEP indicates the mobilization of ligands which potentially block virus attachment to CCR5 HIV-1 co-receptor. The significant correlation between CCL4 and FTC levels suggests that CCL4 increase is modulated as an inflammatory response to PrEP. [ABSTRACT FROM AUTHOR]

Published

2022

19. OPTIMIZING PRE-EXPOSURE PROPHYLAXIS WITH TDF-FTC AND TAF-FTC FOR INSERTIVE SEX.

Author

Herrera, Carolina, Else, Laura J., Webb, Emily, Pillay, Azure-Dee, Seiphetlo, Thabiso B., Lebina, Limakatso, Serwanga, Jennifer, Ssemata, Andrew Sentoogo, Namubiru, Patricia, Odoch, Geoffrey, Gray, Clive M., Chiodi, Francesca, Khoo, Saye, Martinson, Neil, and Fox, Julie

Published

2023