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2. Serological Status of Vaccine and Hepatitis B Virus Exposure Among Children Under 5 and Aged 15–17 Years in Kampala, Uganda.

Author

Muwanda, Fahad, Kiyonga, Edward, Nambafu, Joan, Turyamubona, Agnes, Kafeero, Hussein Mukasa, Kigozi, Edgar, Babikako, Harriet Mupere, Wekiya, Enock, Mboowa, Gerald, Kateete, David Patrick, Sendagire, Hakim, Norman, Paul J., and Bagaya, Bernard Ssentalo

Subjects
CROSS-sectional method, QUALITATIVE research, RESEARCH funding, HEPATITIS viruses, HEPATITIS B vaccines, RESEARCH, SEROPREVALENCE, VACCINATION status, ADOLESCENCE, CHILDREN
Abstract

Background: Pediatric hepatitis B virus (HBV) serostatus remains variably characterized, hardly determined at times, or documented as part of national monitoring of the Extended Programs for Immunization (EPI). Methods: We cross-sectionally characterized the seroprevalence of HBV vaccine and/or infection status among 501 and 288 children <5 and 15–17 years old, respectively, in Kawempe Division, Kampala, Uganda, between May and August 2023. These children received HBV vaccination under the Uganda National Extended Program on Immunizations (UNEPI). Samples were qualitatively screened for hepatitis B surface antigen (HBsAg), hepatitis B surface antibody (HBsAb or anti-HBs), hepatitis B e antigen (HBeAg), hepatitis B e antibody (HBeAb or anti-HBe), and for hepatitis B core antibody (HBcAb or anti-HBc) using three different HBV Combo test rapid immunochromatographic diagnostic tests: Nova, Fastep, and Beright. Results: The seroprevalence of HBsAg, anti-HBs, HBeAg, anti-HBe, and anti-HBc was 1.52%, 27.75%, 0.88%, 0.63%, and 0.76%, respectively, for the combined study age groups. The HBsAg seroprevalence of 2.78% was almost 3.5-fold higher among adolescents when compared to the 0.8% observed in the under-5-year-olds. The qualitative seroprevalence of anti-HBs was 33.1% and 18.4% in the under-5 and among the 15–17-year-old study groups, respectively. Conclusions: The proportion of qualitatively detectable anti-HBs in both groups of vaccinated children is low and probably indicates reduced seroprotection. Consequently, a large proportion of children who received the hepatitis B vaccine under UNEPI may be at risk of HBV infection, especially adolescents. A booster dose of the Hepatitis B Vaccine may be required for adolescents. [ABSTRACT FROM AUTHOR]

Published
2024
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3. Impaired Mycobacterium tuberculosis-specific T-cell memory phenotypes and functional profiles among adults with type 2 diabetes mellitus in Uganda.

Author

Ssekamatte, Phillip, Nabatanzi, Rose, Sitenda, Diana, Nakibuule, Marjorie, Bagaya, Bernard Ssentalo, Kibirige, Davis, Kyazze, Andrew Peter, Kateete, David Patrick, Sande, Obondo James, van Crevel, Reinout, Cose, Stephen, and Biraro, Irene Andia

Subjects
LATENT tuberculosis, MONONUCLEAR leukocytes, TYPE 2 diabetes, LATENT infection, T cells
Abstract

Background: Efforts to eradicate tuberculosis (TB) are threatened by diabetes mellitus (DM), which confers a 3-fold increase in the risk of TB disease. The changes in the memory phenotypes and functional profiles of Mycobacterium tuberculosis (Mtb)-specific T cells in latent TB infection (LTBI)-DM participants remain poorly characterised. We, therefore, assessed the effect of DM on T-cell phenotype and function in LTBI and DM clinical groups. Methods: We compared the memory phenotypes and function profiles of Mtb-specific CD4+ and CD8+ T cells among participants with LTBI-DM (n=21), LTBI-only (n=17) and DM-only (n=16). Peripheral blood mononuclear cells (PBMCs) were stimulated with early secretory antigenic 6 kDa (ESAT-6) and culture filtrate protein 10 (CFP-10) peptide pools or phytohemagglutinin (PHA). The memory phenotypes (CCR7/CD45RA), and functional profiles (HLA-DR, PD-1, CD107a, IFN-γ, IL-2, TNF, IL-13, IL-17A) of Mtb-specific CD4+ and CD8+ T cells were characterised by flow cytometry. Results: Naïve CD4+ T cells were significantly decreased in the LTBI-DM compared to the LTBI-only participants [0.47 (0.34-0.69) vs 0.91 (0.59-1.05); (p<0.001)]. Similarly, CD8+ HLA-DR expression was significantly decreased in LTBI-DM compared to LTBI-only participants [0.26 (0.19-0.33) vs 0.52 (0.40-0.64); (p<0.0001)], whereas CD4+ and CD8+ PD-1 expression was significantly upregulated in the LTBI-DM compared to the LTBI-only participants [0.61 (0.53-0.77) vs 0.19 (0.10-0.28); (p<0.0001) and 0.41 (0.37-0.56) vs 0.29 (0.17-0.42); (p=0.007)] respectively. CD4+ and CD8+ IFN-γ production was significantly decreased in the LTBI-DM compared to the LTBI-only participants [0.28 (0.19-0.38) vs 0.39 (0.25-0.53); (p=0.030) and 0.36 (0.27-0.49) vs 0.55 (0.41-0.88); (p=0.016)] respectively. CD4+ TNF and CD8+ IL-17A production were significantly decreased in participants with LTBI-DM compared to those with LTBI-only [0.38 (0.33-0.50) vs 0.62 (0.46-0.87); (p=0.004) and 0.29 (0.16-0.42) vs 0.47 (0.29-0.52); (0.017)] respectively. LTBI-DM participants had significantly lower dual-functional (IFN-γ+IL-2+ and IL-2+TNF+) and mono-functional (IFN-γ+ and TNF+) CD4+ responses than LTBI-only participants. LTBI-DM participants had significantly decreased dual-functional (IFN-γ+IL-2+, IFN-γ+ TNF+ and IL-2+TNF+) and mono-functional (IFN-γ+, IL-2+ and TNF+) central and effector memory CD4+ responses compared to LTBI-only participants. Conclusion: Type 2 DM impairs the memory phenotypes and functional profiles of Mtb-specific CD4+ and CD8+ T cells, potentially indicating underlying immunopathology towards increased active TB disease risk. [ABSTRACT FROM AUTHOR]

Published
2024
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4. In Utero Mother-to-Child Transmission of HIV-1 and the Associated Factors in Rwanda, Africa.

Author

Rutayisire, Gad, Ssemwanga, Emmanuel, Ntale, Roman, Grace, Uwera Marie, Gashema, Jean Pierre, Gasana, Paul, Wekia, Enock, Kiwanuka, Noah, and Bagaya, Bernard Ssentalo

Abstract

Mother-to-child transmission (MTCT) of HIV-1 and associated mortality continue to occur at unacceptably high rates, despite the extensive rollout and implementation of Prevention of Mother-to-Child Transmission (PMTCT) Programs, including the modified versions of Option B and B+ in 2010 and 2012, respectively. Maternal HIV viral load (VL) and socio-behavioral factors sustaining MTCT in Rwanda remain largely unexplored. The study examined the effects of socio-behavioral factors on maternal VL and their contribution to in utero transmission of HIV-1 in the context of Rwanda's HIV epidemic. A prospective cohort study was conducted in 862 mother–baby pairs enrolled in 10 PMTCT clinics in Rwanda. VL was determined on plasma and Dried Blood Spots samples, whereas HIV DNA PCR was performed to determine in utero MTCT of HIV of the babies immediately at birth and then at 3 weeks, 4 weeks, 6 months, and 18 months, together with HIV antibody testing to determine other forms of MTCT of HIV. Quantitative data on socio-behavioral factors were collected through a structured questionnaire. Linear regression and univariate analysis of variances using SPSS 25.0 were used to test the hypotheses. We found 22/862 (2.55%) cases of in utero transmission and a total of 32/862 (3.7%) cases of MTCT of HIV-1 over 18 study months. Maternal VL at delivery was significantly associated with the risk of in utero transmission of HIV-1. Socio-behavioral factors associated with elevated maternal VL at delivery included alcohol, smoking, multiple sexual partners, mothers' income, being a casual laborer, and distance to health care services. We report an MTCT rate of 3.7% in our study population over the 18 months, higher than the national average of 1.5%, the majority of which occurred in utero. MTCT cases were attributable to failure to suppress maternal VL. [ABSTRACT FROM AUTHOR]

Published
2024
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5. Population attributable fraction of incident HIV infections associated with alcohol consumption in fishing communities around Lake Victoria, Uganda

Author

Kiwanuka, Noah, Ssetaala, Ali, Ssekandi, Ismail, Nalutaaya, Annet, Kitandwe, Paul Kato, Ssempiira, Julius, Bagaya, Bernard Ssentalo, Balyegisawa, Apolo, Kaleebu, Pontiano, Hahn, Judith, Lindan, Christina, and Sewankambo, Nelson Kaulukusi

Subjects
Biomedical and Clinical Sciences, Public Health, Health Sciences, Behavioral and Social Science, Clinical Research, Alcoholism, Alcohol Use and Health, HIV/AIDS, Prevention, Infectious Diseases, Substance Misuse, Infection, Stroke, Good Health and Well Being, Adolescent, Adult, Alcohol Drinking, Female, Fisheries, HIV Infections, HIV-1, Humans, Incidence, Lakes, Longitudinal Studies, Male, Middle Aged, Risk Factors, Risk-Taking, Uganda, Young Adult, General Science & Technology
Abstract

BackgroundAlthough the association between alcohol consumption and HIV risk is well documented, few studies have examined the magnitude of new HIV infections that could be prevented by controlling alcohol use. We report the population attributable fraction (PAF) of incident HIV infections due to alcohol consumption among the HIV high-risk population of fishing communities along Lake Victoria, Uganda.MethodsIn a community-based cohort study, 1607 HIV sero-negative participants aged 18-49 years were enrolled from eight fishing communities along Lake Victoria, Uganda. At follow up 12 months later, 1288 (80.1%) were seen and interviewed. At baseline and follow-up visits, participants completed interviewer-administered questionnaires on alcohol consumption, demographics, and sexual risk behavior, and were tested for HIV infection. HIV incidence and adjusted incident rate ratios (adjusted IRRs) were estimated using Poisson regression models; the crude and adjusted PAFs of incident HIV infections associated with alcohol consumption were calculated using the Greenland and Drescher method for cohort studies.ResultsAmong the 1288 participants seen at follow up, 53.5% reported drinking alcohol of whom 24.4% drank occasionally (2 days a week or less) and 29.1% drank regularly (3-7 days a week). Forty eight incident HIV infections occurred giving an incidence rate of 3.39/100 person years at-risk (pyar) (95% CI, 2.55-4.49). Compared to non-drinkers, the adjusted IRR of HIV was 3.09 (1.13-8.46) among occasional drinkers and 5.34 (2.04-13.97) among regular drinkers. The overall adjusted PAF of incident HIV infections due alcohol was 64.1 (95% CI; 23.5-83.1); ranging from 52.3 (11.9-74.2) among Muslims to 71.2 (32.6-87.7) for participants who reported ≥ 2 sexual partners in the past 12 months.ConclusionIn fishing communities along Lake Victoria, Uganda, 64% of new HIV infections can be attributed to drinking alcohol. Interventions to reduce alcohol consumption should be integrated in HIV/AIDS prevention activities for populations in whom both HIV and alcohol consumption are highly prevalent.

Published
2017

6. Alcohol Consumption Modifies Susceptibility to HIV-1 Entry in Cervical Mucosa-Derived CD4+ T cells of Women Resident in a Fishing Community of Lake Victoria, Uganda

Author

Bagaya, Bernard Ssentalo, primary, Driciru, Emmanuella, additional, Fahad, Muwanda, additional, Nantongo, Mary, additional, Namuleme, Marion, additional, Kitandwe, Paul Kato, additional, Ssekayita, Enoch Muyanja, additional, Galiwango, Ronald, additional, Mirembe, Violet, additional, Muwenda, Barbarah Kawoozo, additional, Muwanga, Moses, additional, Kayongo, Alex, additional, and Lutwama, Fredrick, additional

Published
2023
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7. Proportion of Ugandans with pre-pandemic SARS-CoV-2 cross-reactive CD4+ and CD8+ T-cell responses: A pilot study

Author

Namuniina, Annemarie, primary, Muyanja, Enoch S., additional, Biribawa, Victoria M., additional, Okech, Brenda A., additional, Ssemaganda, Aloysious, additional, Price, Matt A., additional, Hills, Nancy, additional, Nanteza, Ann, additional, Bagaya, Bernard Ssentalo, additional, Weiskopf, Daniela, additional, Riou, Catherine, additional, Reynolds, Steven J., additional, Galiwango, Ronald M., additional, and Redd, Andrew D., additional

Published
2023
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9. High proportion of Ugandans with pre-pandemic SARS-CoV-2 cross-reactive CD4+ and CD8+ T-cell responses

Author

Namuniina, Annemarie, primary, Muyanja, Enoch S, additional, Biribawa, Victoria M, additional, Okech, Brenda A, additional, Ssemaganda, Aloysious, additional, Price, Matt A, additional, Hills, Nancy, additional, Nanteza, Ann, additional, Bagaya, Bernard Ssentalo, additional, Weiskopf, Daniela, additional, Riou, Catherine, additional, Reynolds, Steven J, additional, Galwango, Ronald M, additional, and Redd, Andrew D, additional

Published
2023
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11. Antimicrobial susceptibility surveillance and antimicrobial resistance in Neisseria gonorrhoeae in Africa from 2001 to 2020: A mini-review.

Author

Kakooza, Francis, Kiggundu, Reuben, Mboowa, Gerald, Kateete, Patrick David, Nsangi, Olga Tendo, Kabahita, Jupiter Marina, Bagaya, Bernard Ssentalo, Golparian, Daniel, and Unemo, Magnus

Abstract

Antimicrobial resistance (AMR) in Neisseria gonorrhoeae (NG), compromising gonorrhea treatment, is a global public health concern. Improved, quality-assured NG AMR monitoring at the global level is essential. This mini-review examined NG AMR susceptibility surveillance and AMR data from the African continent from 2001 to 2020. Eligible peer-reviewed publications (n = 30) containing NG AMR data for antimicrobials currently recommended for gonorrhea treatment were included. Overall, very limited NG surveillance and AMR data was available. Furthermore, the NG AMR surveillance studies varied greatly regarding surveillance protocols (e.g., populations and samples tested, sample size, antimicrobials examined), methodologies (e.g., antimicrobial susceptibility testing method [agar dilution, minimum inhibitory concentration (MIC) gradient strip test, disc diffusion test] and interpretative criteria), and quality assurance (internal quality controls, external quality assessments [EQA], and verification of AMR detected). Moreover, most studies examined a suboptimal number of NG isolates, i.e., less than the WHO Global Gonococcal Antimicrobial Surveillance Program (GASP) and WHO Enhanced GASP (EGASP) recommendations of ≥100 isolates per setting and year. The notable inter-study variability and frequently small sample sizes make appropriate inter-study and inter-country comparisons of AMR data difficult. In conclusion, it is imperative to establish an enhanced, standardized and qualityassured NG AMR surveillance, ideally including patient metadata and genome sequencing as in WHO EGASP, in Africa, the region with the highest gonorrhea incidence globally. This will enable the monitoring of AMR trends, detection of emerging AMR, and timely refinements of national and international gonorrhea treatment guidelines. To achieve this aim, national and international leadership, political and financial commitments are imperative. [ABSTRACT FROM AUTHOR]

Published
2023
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12. Enterococcus and Eggerthella species are enriched in the gut microbiomes of COVID-19 cases in Uganda

Author

Agudelo, Carolina, Kateete, David Patrick, Nasinghe, Emmanuel, Kamulegeya, Rogers, Lubega, Christopher, Mbabazi, Monica, Baker, Noah, Lin, Kathryn Y., Liu, Chang C., Kasambula, Arthur Shem, Kigozi, Edgar, Komakech, Kevin, Mukisa, John, Mulumba, Kassim, Mwachan, Patricia, Nakalanda, Brenda Sharon, Nalubega, Gloria Patricia, Nsubuga, Julius, Sitenda, Diana, Ssenfuka, Henry, Cirolia, Giana T., Gustafson, Jeshua T., Wang, Ruohong, Nsubuga, Moses Luutu, Yiga, Fahim, Stanley, Sarah A., Bagaya, Bernard Ssentalo, Elliott, Alison, Joloba, Moses, and Wolf, Ashley R.

Published
2025
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13. Whole-genome sequencing of SARS-CoV-2 in Uganda: implementation of the low-cost ARTIC protocol in resource-limited settings

Author

Mboowa, Gerald, primary, Mwesigwa, Savannah, additional, Kateete, David, additional, Wayengera, Misaki, additional, Nasinghe, Emmanuel, additional, Katagirya, Eric, additional, Katabazi, Ashaba Fred, additional, Kigozi, Edgar, additional, Kirimunda, Samuel, additional, Kamulegeya, Rogers, additional, Kabahita, Jupiter Marina, additional, Luutu, Moses Nsubuga, additional, Nabisubi, Patricia, additional, Kanyerezi, Stephen, additional, Bagaya, Bernard Ssentalo, additional, and Joloba, Moses L, additional

Published
2021
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14. Effectiveness of thermal screening in detection of COVID-19 among truck drivers at Mutukula Land Point of Entry, Uganda

Author

Nsawotebba, Andrew, primary, Ibanda, Ivan, additional, Ssewanyana, Isaac, additional, Ogwok, Patrick, additional, Ocen, Francis, additional, Okiira, Christopher, additional, Kagirita, Atek, additional, Mujuni, Dennis, additional, Tugumisirize, Didas, additional, Kabugo, Joel, additional, Nyombi, Abdunoor, additional, Majwala, Robert Kaos, additional, Bagaya, Bernard Ssentalo, additional, Kalyesubula-Kibuuka, Simeon, additional, Ssengooba, Willy, additional, and Nabadda, Susan, additional

Published
2021
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15. Operationalization of COVID-19 Rapid Diagnosis Using Xpert® Xpress SARS CoV-2 Assay in Resource-Limited Settings: Early Implementation Lessons From Uganda

Author

Nsawotebba, Andrew, primary, Ibanda, Ivan, additional, Ssewanyana, Isaac, additional, Bagaya, Bernard Ssentalo, additional, Nyombi, Abdunoor, additional, Kagirita, Atek, additional, Mujuni, Dennis, additional, Tugumisirize, Didas, additional, Majwala, Robert Kaos, additional, Ocen, Francis, additional, Kabugo, Joel, additional, Adam, Isa, additional, Wekiya, Enock, additional, Munduku, Benoni, additional, Linda, Lillian, additional, Otita, Morgan, additional, Kalyesubula-Kibuuka, Simon, additional, Okiira, Christopher, additional, Kigozi, Edgar, additional, Ogwok, Patrick, additional, Joloba, Moses Lutakoome, additional, Nabadda, Susan, additional, and Ssengooba, Willy, additional

Published
2021
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16. Prevalence and correlates of HIV infection among adolescents and young people living in fishing populations along Lake Victoria Fishing Communities in Uganda

Author

Nanyonjo, Gertrude, primary, Asiki, Gershim, additional, Ssetaala, Ali, additional, Nakaweesa, Teddy, additional, Wambuzi, Mathias, additional, Nanvubya, Annet, additional, Mpendo, Juliet, additional, Okech, Brenda, additional, Kitandwe, Paul Kato, additional, Nielsen, Leslie, additional, Nalutaaya, Annet, additional, Welsh, Sabrina, additional, Bagaya, Bernard Ssentalo, additional, Chinyenze, Kundai, additional, Fast, Pat, additional, Price, Matt, additional, and Kiwanuka, Noah, additional

Published
2020
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17. Field Performance of PIMA Point-of-Care Machine for CD4 Enumeration Under a Mobile HIV Counseling and Testing Program in Remote Fishing Communities of Lake Victoria, Uganda

Author

Namuniina, Annemarie, primary, Lutwama, Fredrick, additional, Biribawa, Victoria Menya, additional, Kizza, David, additional, Kabuubi, Brian Roy, additional, Kitandwe, Paul Kato, additional, Mpendo, Juliet, additional, Nanvubya, Annet, additional, Ssempiira, Julius, additional, Nalutaaya, Annet, additional, Ssetaala, Ali, additional, Welsh, Sabrina, additional, Price, Matt A., additional, Kiwanuka, Noah, additional, and Bagaya, Bernard Ssentalo, additional

Published
2019
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18. HIV-1 INTERSUBTYPE RECOMBINATION WITHIN GP120 IMPOSES SEVERE FUNCTIONAL RESTRICTION ON RESULTANT ENVELOPES

Author

BAGAYA, BERNARD SSENTALO

Subjects
Microbiology, Molecular Biology, Immunology, Virology, HIV Intersubtype recombination bottlenecks, functional genomes and restriction
Abstract

HIV-1 Intersubtype Recombination Within gp120 Imposes Severe Functional Restrictions on Resultant EnvelopesAbstractbyBERNARD SSENTALO BAGAYARecombination is an integral part of HIV-1 replication and brings numerous advantages to HIV-1 including; modification of HIV-1 fitness, development of drug resistance, repair and rescue of lethally mutated genomes, immune escape, and exacerbates HIV-1 genetic diversity. Recombination therefore may be indispensable for HIV-1’s continued survival. Despite bringing benefits, recombination also imposes functional constraints on resultant genomes through disruption of epistatically linked sites, making it an Achilles heel for the virus. Understanding the mechanisms underlying recombination will generate knowledge useful in treatment and control of HIV-1, however challenges in obtaining recombinant HIV-1 for study still remain.In this study we have developed novel systems to generate HIV-1 Env and pol genes in vitro. The recombination systems comprise of two plasmids each; pRECnfl_5’LTR_HIVEnvA and pREC_3’LTR¿pol_HIVEnvD, and pREC_5’LTR_gag.polA and pRECnfl_3’LTR¿p7_HIV plasmids for the Env and pol recombination system respectively. Co-transfection of both Env and pol recombination system plasmid pairs into HEK293T cells results in packaging of both homodiploid and heterodiploid virions. At de novo infection of U87.CD4.CCR5 cells, only heterodiploid RNAs can complement each other to complete reverse transcription, however they mustrecombine within Env or pol gene respectively in order to produce replication-competent virus, otherwise a “dead” genome incapable of further replication is produced.Using subtype A and D Env pairs; EnvA91/EnvD109 and EnvA115/EnvD109 in the Env recombination system, we confirmed by clonal sequencing of 81 Envs that 100% recombinants are generated by the system. All 81 recombinants clustered in 12 unique breakpoints, mostly in the rev2 exon in gp41 with no gp120 breakpoints. However the dual infection method with the same virus pairs A91/D109 and A115/D109 generated both gp120 (28 [33%]) and gp41 (58 [67%]) breakpoints. To further understand the source of the discrepancy between the two methods, we analyzed breakpoint distribution in 329 database-derived recombinant Envs of two subtypes, revealing presence of 45% (150) gp120 breakpoints albeit with 98 (65%) of them clustering in a C1 domain. To rule out defects of the Env recombination system in generating gp120 recombinants, we performed 454 deep sequencing of provirus. The results showed a gp120 breakpoint composition of 50%, 34%, 32% and 38% within A91/D109, A115/D109, A91/V3.Ad8 and A115/V3.Ad8 HIV-1 Env pairs respectively, meaning that the recombination system was not defective. To determine whether the gp120 recombinants were functionally restricted and therefore screened out by the recombination system design strategy, we performed a comprehensive functional analysis on the 22 unique breakpoint gp120 recombinants generated by dual infection method with same HIV-1 isolate pairs of A91/D109 and A115/D109. We found that all gp120 recombinants were incapable of mediating membrane fusion or supporting virus replication. Mechanistic studies showed that discordance in gp120 C1/C5-gp41 interaction domains was responsible for the loss of function in some, but not all recombinant Envs. These findings indicated that mostgp120 intersubtype recombinants were functionally restricted, probably mostly by the incompatibilities at the gp120-gp41 interaction interface. More studies need to be done to elucidate other mechanisms posing bottleneck for recombinant Env function. The labile nature of gp120/gp41 interface is an Achilles heel for intersubtype recombination that could be exploited in development of therapies against HIV-1.

Published
2015

19. High proportion of Ugandans with pre-pandemic SARS-CoV-2 cross-reactive CD4+ and CD8+ T-cell responses.

Author

Namuniina A, Muyanja ES, Biribawa VM, Okech BA, Ssemaganda A, Price MA, Hills N, Nanteza A, Bagaya BS, Weiskopf D, Riou C, Reynolds SJ, Galwango RM, and Redd AD

Abstract

The estimated mortality rate of the SARS-CoV-2 pandemic varied greatly around the world with multiple countries in East, Central, and West Africa having significantly lower rates of COVID-19 related fatalities than many resource-rich nations with significantly earlier wide-spread access to life-saving vaccines. One possible reason for this lower mortality could be the presence of pre-existing cross-reactive immunological responses in these areas of the world. To explore this hypothesis, stored peripheral blood mononuclear cells (PBMC) from Ugandans collected from 2015-2017 prior to the COVID-19 pandemic (n=29) and from hospitalized Ugandan COVID-19 patients (n=3) were examined using flow-cytometry for the presence of pre-existing SARS-CoV-2 cross-reactive CD4+ and CD8+ T-cell populations using four T-cell epitope mega pools. Of pre-pandemic participants, 89.7% (26/29) had either CD4+ or CD8+, or both, SARS-CoV-2 specific T-cell responses. Specifically, CD4+ T-cell reactivity (72.4%) and CD8+ T-cell reactivity (65.5%) were relatively similar, and 13 participants (44.8%) had both types of cross-reactive types of T-cells present. There were no significant differences in response by sex in the population. The rates of cross-reactive T-cell populations in these Ugandans is higher than previous estimates from resource-rich countries like the United States (20-50% reactivity). It is unclear what role, if any, this cross-reactivity played in decreasing COVID-19 related mortality in Uganda and other African countries, but does suggest that a better understanding of global pre-existing immunological cross-reactivity could be an informative data of epidemiological intelligence moving forward.

Published
2023
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