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19 results on '"Harawa, Visopo"'

1. Prothrombotic autoantibodies targeting platelet factor 4/polyanion are associated with pediatric cerebral malaria

Author

Vera, Iset M., Kessler, Anne, Harawa, Visopo, Ahmadu, Ajisa, Keller, Thomas E., Ray, Stephen T.J., Taylor, Terrie E., Rogerson, Stephen J., Mandala, Wilson L., Gil, Morayma Reyes, Seydel, Karl B., and Kim, Kami

Subjects
Nervous system diseases -- Risk factors -- Development and progression, Autoantibodies -- Identification and classification -- Health aspects, Malaria -- Diagnosis -- Complications and side effects, Health care industry
Abstract

BACKGROUND. Features of consumptive coagulopathy and thromboinflammation are prominent in cerebral malaria (CM). We hypothesized that thrombogenic autoantibodies contribute to a procoagulant state in CM. METHODS. Plasma from children with uncomplicated malaria (UM) (n = 124) and CM (n = 136) was analyzed by ELISA for a panel of 8 autoantibodies including anti-platelet factor 4/polyanion (anti-PF4/P), anti-phospholipid, anti-phosphatidylserine, anti-myeloperoxidase, anti-proteinase 3, anti-dsDNA, anti-[beta]-2- glycoprotein I, and anti-cardiolipin. Plasma samples from individuals with nonmalarial coma (NMC) (n = 49) and healthy controls (HCs) (n = 56) were assayed for comparison. Associations with clinical and immune biomarkers were determined using univariate and logistic regression analyses. RESULTS. Median anti-PF4/P and anti-PS IgG levels were elevated in individuals with malaria infection relative to levels in HCs (P < 0.001) and patients with NMC (PF4/P: P < 0.001). Anti-PF4/P IgG levels were elevated in children with CM (median = 0.27, IQR: 0.19-0.41) compared with those with UM (median = 0.19, IQR: 0.14-0.22, P < 0.0001). Anti-PS IgG levels did not differ between patients with UM and those with CM (P = 0.39). When patients with CM were stratified by malaria retinopathy (Ret) status, the levels of anti-PF4/P IgG correlated negatively with the peripheral platelet count in patients with [Ret.sup.+] CM (Spearman's rho [[R.sub.s]] = 0.201, P = 0.04) and associated positively with mortality (OR = 15.2, 95% CI: 1.02-275, P = 0.048). Plasma from patients with CM induced greater platelet activation in an ex vivo assay relative to plasma from patients with UM (P = 0.02), and the observed platelet activation was associated with anti-PF4/P IgG levels ([R.sub.s]= 0.293, P = 0.035). CONCLUSIONS. Thrombosis mediated by elevated anti-PF4/P autoantibodies may be one mechanism contributing to the clinical complications of CM., Introduction Immunothrombosis is a host defense mechanism where the innate and adaptive immune systems work in conjunction with the hemostatic system (platelets and endothelial cells) to control infection (1). Although [...]

Published
2024
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4. A systems serology approach to identifying key antibody correlates of protection from cerebral malaria in Malawian children.

Author

Walker, Isobel S., Dini, Saber, Aitken, Elizabeth H., Damelang, Timon, Hasang, Wina, Alemu, Agersew, Jensen, Anja T. R., Rambhatla, Janavi S., Opi, D. Herbert, Duffy, Michael F., Takashima, Eizo, Harawa, Visopo, Tsuboi, Takafumi, Simpson, Julie A., Mandala, Wilson, Taylor, Terrie E., Seydel, Karl B., Chung, Amy W., and Rogerson, Stephen J.

Subjects
CD54 antigen, CEREBRAL malaria, COMPLEMENT receptors, ERYTHROCYTE membranes, ANTIBODY formation
Abstract

Background: Plasmodium falciparum erythrocyte membrane protein 1 (PfEMP1) proteins are expressed on the surface of infected erythrocytes, mediating parasite sequestration in the vasculature. PfEMP1 is a major target of protective antibodies, but the features of the antibody response are poorly defined. Methods: In Malawian children with cerebral or uncomplicated malaria, we characterized the antibody response to 39 recombinant PfEMP1 Duffy binding like (DBL) domains or cysteine-rich interdomain regions (CIDRs) in detail, including measures of antibody classes, subclasses, and engagement with Fcγ receptors and complement. Using elastic net regularized logistic regression, we identified a combination of seven antibody targets and Fc features that best distinguished between children with cerebral and uncomplicated malaria. To confirm the role of the selected targets and Fc features, we measured antibody-dependent neutrophil and THP-1 cell phagocytosis of intercellular adhesion molecule-1 (ICAM-1) and endothelial protein C (EPCR) co-binding infected erythrocytes. Results: The selected features distinguished between children with cerebral and uncomplicated malaria with 87% accuracy (median, 80–96% interquartile range) and included antibody to well-characterized DBLβ3 domains and a less well-characterized CIDRγ12 domain. The abilities of antibodies to engage C1q and FcγRIIIb, rather than levels of IgG, correlated with protection. In line with a role of FcγRIIIb binding antibodies to DBLβ3 domains, antibody-dependent neutrophil phagocytosis of ICAM-1 and EPCR co-binding IE was higher in uncomplicated malaria (15% median, 8–38% interquartile range) compared to cerebral malaria (7%, 30–15%, p < 0.001). Conclusions: Antibodies associated with protection from cerebral malaria target a subset of PfEMP1 domains. The Fc features of protective antibody response include engagement of FcγRIIIb and C1q, and ability to induce antibody-dependent neutrophil phagocytosis of infected erythrocytes. Identifying the targets and Fc features of protective immunity could facilitate the development of PfEMP1-based therapeutics for cerebral malaria. [ABSTRACT FROM AUTHOR]

Published
2024
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5. Pro-thrombotic autoantibodies targeting Platelet Factor 4/polyanion are associated with pediatric cerebral malaria

Author

Vera, Iset M., primary, Kessler, Anne, additional, Harawa, Visopo, additional, Ahmadu, Ajisa, additional, Keller, Thomas E., additional, Ray, Stephen T.J., additional, Taylor, Terrie E., additional, Rogerson, Stephen J., additional, Mandala, Wilson L., additional, Reyes Gil, Morayma, additional, Seydel, Karl B., additional, and Kim, Kami, additional

Published
2024
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7. Additional file 2 of The ability of Interleukin–10 to negate haemozoin-related pro-inflammatory effects has the potential to restore impaired macrophage function associated with malaria infection

Author

Tembo, Dumizulu, Harawa, Visopo, Tran, Tam C., Afran, Louise, Molyneux, Malcolm E., Taylor, Terrie E., Seydel, Karl B., Nyirenda, Tonney, Russell, David G., and Mandala, Wilson

Abstract

Additional file 2: Table S1. Clinical characteristic of children with cerebral malaria versus the healthy controls in the second paediatric cohort recruited between 2013 and 2016.

Published
2023
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8. Additional file 1 of The ability of Interleukin–10 to negate haemozoin-related pro-inflammatory effects has the potential to restore impaired macrophage function associated with malaria infection

Author

Tembo, Dumizulu, Harawa, Visopo, Tran, Tam C., Afran, Louise, Molyneux, Malcolm E., Taylor, Terrie E., Seydel, Karl B., Nyirenda, Tonney, Russell, David G., and Mandala, Wilson

Abstract

Additional file 1: Figure S1. Gating strategy for cytokine producing monocytes: Whole blood samples were stimulated with LPS, labelled with CD14 APC, lysed with 2.0ml of 1 x FACS lysing solution and fixed with BFA before the labelling with Isotype Control (PE) and various cytokine antibodies (PE). Flow cytometer dot plots illustrating the side scatter plot versus CD14 (A) with R1 gate for CD14+ cells (monocytes), the Isotype Control plot for setting the gates (B), IL-6 producing monocytes (CD14+IL-6+ cells) (C) and TNF-α producing monocytes (CD14+TNF-α+ cells) (D).Figure. S2 Gating strategy for monocytes expressing HLA-DR and CD86: Whole blood samples were stimulated with LPS, labelled with CD14 APC, HLA-DR-FITC and CD86-FITC and incubated for 20 minutes. The samples were then lysed with 2.0ml of 1 x FACS lysing solution and washed with PBS before acquisition on Flow Cytometer. The dot plots (A) illustrate the side scatter plot versus CD14 (A) with R1 gate for CD14+ cells (monocytes), geometric mean florescence intensity (GMFI) of HLA-DR (B) and CD86 (C) expression on monocytes from children presenting with different malaria clinical types Figure. S3 Gating strategy for cytokine producing T cells: Whole blood samples were stimulated with PMA+ION, labelled with CD3 PerCP, lysed with 2.0ml of 1 x FACS lysing solution and fixed with BFA before the labelling with Isotype Control (PE) and various cytokine antibodies (PE). The Flow cytometer dot plots illustrate the side scatter plot versus CD3-PerCP (A) with R1 gate for CD3+ lymphocytes (Total T cells), the Isotype Control plot for setting the gates (B), INF-γproducing cells (CD3+IFN-γ+ cells) (C) and TNF producing T cells (CD3+TNF+ cells) (D).

Published
2023
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13. Plasma cell-free DNA predicts pediatric cerebral malaria severity

Author

Vera, Iset Medina, primary, Kessler, Anne, additional, Ting, Li-Min, additional, Harawa, Visopo, additional, Keller, Thomas, additional, Allen, Dylan, additional, Njie, Madi, additional, Moss, McKenze, additional, Soko, Monica, additional, Ahmadu, Ajisa, additional, Kadwala, Innocent, additional, Ray, Stephen, additional, Nyirenda, Tonney S., additional, Mandala, Wilson L., additional, Taylor, Terrie E, additional, Rogerson, Stephen J., additional, Seydel, Karl B., additional, and Kim, Kami, additional

Published
2020
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15. Linking EPCR-Binding PfEMP1 to Brain Swelling in Pediatric Cerebral Malaria

Author

Kessler, Anne, primary, Dankwa, Selasi, additional, Bernabeu, Maria, additional, Harawa, Visopo, additional, Danziger, Samuel A., additional, Duffy, Fergal, additional, Kampondeni, Sam D., additional, Potchen, Michael J., additional, Dambrauskas, Nicholas, additional, Vigdorovich, Vladimir, additional, Oliver, Brian G., additional, Hochman, Sarah E., additional, Mowrey, Wenzhu B., additional, MacCormick, Ian J.C., additional, Mandala, Wilson L., additional, Rogerson, Stephen J., additional, Sather, D. Noah, additional, Aitchison, John D., additional, Taylor, Terrie E., additional, Seydel, Karl B., additional, Smith, Joseph D., additional, and Kim, Kami, additional

Published
2017
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17. Impaired CD4 T Cell Memory Response to Streptococcus pneumoniae Precedes CD4 T Cell Depletion in HIVInfected Malawian Adults.

Author

Glennie, Sarah J., Sepako, Enoch, Mzinza, David, Harawa, Visopo, Miles, David J. C., Jambo, Kondwani C., Gordon, Stephen B., Williams, Neil A., and Heyderman, Robert S.

Subjects
T cells, CELL physiology, HIV-positive persons, STREPTOCOCCUS pneumoniae, MALAWIANS, IMMUNOREGULATION, DISEASE susceptibility
Abstract

Objective: Invasive pneumococcal disease (IPD) is a leading cause of morbidity and mortality in HIV-infected African adults. CD4 T cell depletion may partially explain this high disease burden but those with relatively preserved T cell numbers are still at increased risk of IPD. This study evaluated the extent of pneumococcal-specific T cell memory dysfunction in asymptomatic HIV infection early on in the evolution of the disease. Methods: Peripheral blood mononuclear cells were isolated from asymptomatic HIV-infected and HIV-uninfected Malawian adults and stained to characterize the underlying degree of CD4 T cell immune activation, senescence and regulation. Pneumococcal-specific T cell proliferation, IFN-c, IL-17 production and CD154 expression was assessed using flow cytometry and ELISpot. Results: We find that in asymptomatic HIV-infected Malawian adults, there is considerable immune disruption with an increase in activated and senescent CD4+CD38+PD-1+ and CD4+CD25highFoxp3+ Treg cells. In the context of high pneumococcal exposure and therefore immune stimulation, show a failure in pneumococcal-specific memory T cell proliferation, skewing of T cell cytokine production with preservation of interleukin-17 but decreased interferon-gamma responses, and failure of activated T cells to express the co-stimulatory molecule CD154. Conclusion: Asymptomatic HIV-infected Malawian adults show early signs of pneumococcal- specific immune dysregulation with a shift in the balance of CD4 memory, T helper 17 cells and Treg. Together these data offer a mechanistic understanding of how antigen-specific T cell dysfunction occurs prior to T cell depletion and may explain the early susceptibility to IPD in those with relatively preserved CD4 T cell numbers. [ABSTRACT FROM AUTHOR]

Published
2011
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18. Convalescent <italic>Plasmodium falciparum</italic>-specific seroreactivity does not correlate with paediatric malaria severity or Plasmodium antigen exposure.

Author

Kessler, Anne, Campo, Joseph J., Harawa, Visopo, Mandala, Wilson L., Rogerson, Stephen J., Mowrey, Wenzhu B., Seydel, Karl B., and Kim, Kami

Subjects
PLASMODIUM falciparum, MALARIA, CONVALESCENCE, SEROPREVALENCE, ANTIGENS
Abstract

Background: Antibody immunity is thought to be essential to prevent severe Plasmodium falciparum infection, but the exact correlates of protection are unknown. Over time, children in endemic areas acquire non-sterile immunity to malaria that correlates with development of antibodies to merozoite invasion proteins and parasite proteins expressed on the surface of infected erythrocytes. Results: A 1000 feature P. falciparum 3D7 protein microarray was used to compare P. falciparum-specific seroreactivity during acute infection and 30 days after infection in 23 children with uncomplicated malaria (UM) and 25 children with retinopathy-positive cerebral malaria (CM). All children had broad P. falciparum antibody reactivity during acute disease. IgM reactivity decreased and IgG reactivity increased in convalescence. Antibody reactivity to CIDR domains of "virulent" PfEMP1 proteins was low with robust reactivity to the highly conserved, intracellular ATS domain of PfEMP1 in both groups. Although children with UM and CM differed markedly in parasite burden and PfEMP1 exposure during acute disease, neither acute nor convalescent PfEMP1 seroreactivity differed between groups. Greater seroprevalence to a conserved Group A-associated ICAM binding extracellular domain was observed relative to linked extracellular CIDRα1 domains in both case groups. Pooled immune IgG from Malawian adults revealed greater reactivity to PfEMP1 than observed in children. Conclusions: Children with uncomplicated and cerebral malaria have similar breadth and magnitude of P. falciparum antibody reactivity. The utility of protein microarrays to measure serological recognition of polymorphic PfEMP1 antigens needs to be studied further, but the study findings support the hypothesis that conserved domains of PfEMP1 are more prominent targets of cross reactive antibodies than variable domains in children with symptomatic malaria. Protein microarrays represent an additional tool to identify cross-reactive Plasmodium antigens including PfEMP1 domains that can be investigated as strain-transcendent vaccine candidates. [ABSTRACT FROM AUTHOR]

Published
2018
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19. Hybrid Mentorship of Medical Laboratories to Achieve ISO 15189:2012 Accreditation in Malawi: The University of Maryland Malawi Experience.

Author

Moyo H, Osawe S, Nyangulu C, Ndhlovu P, Harawa V, Divala O, Msukwa M, Croxton T, Blanco N, Mwandama D, Mkandawire M, Kampira E, Kaba M, Maida A, Auld AF, Kim L, Mwenda R, Kress H, Kandulu J, Sumani T, Bitilinyu J, Kalua T, and Abimiku A

Abstract

Introduction: As part of a laboratory strengthening program in Malawi to achieve and maintain International Organization for Standardization (ISO) 15189 accreditation, we intended to mentor selected HIV molecular laboratories to achieve this accreditation. Due to the COVID-19 pandemic, mentorship pivoted to a hybrid model using an Internet-based approach and on-site mentorships. We describe the implementation of this strategy, successes, and challenges., Methods: We conducted weekly, 1-hour virtual mentorship sessions for the 5 initial laboratories (cohort 1) selected based on their Stepwise Laboratory Quality Improvement Process Towards Accreditation (SLIPTA) performance score of 3 or more stars. Laboratories presented updates and supporting documents electronically, and trainings were conducted virtually. In September 2020, when travel restrictions were relaxed, we initiated hybrid mentorships and audits for cohort 1 laboratories. The same hybrid approach was used to mentor 4 additional laboratories in cohort 2. We performed descriptive analysis, and the Wilcoxon signed-rank test was used to compare the training pre-and post-test scores., Results: Between March 2020 and May 2023, the team completed a total of 54 virtual mentorship sessions and 20 on-site visits across 9 laboratories. Overall, the team conducted 8 training sessions for 35 laboratory quality officers. Median score improvement (pre-test vs. post-test scores) was observed across individual trainings and across cohorts ( P <.01). At the end of cohort 1, 4 of 5 (80%) laboratories were accredited. One laboratory that did not reach accreditation joined cohort 2. At the end of the mentoring period, all 5 cohort 2 laboratories were accredited., Conclusions: We demonstrated that using a hybrid mentorship model for accreditation was a successful strategy during the COVID-19 pandemic. For the first time in Malawi, this strategy resulted in accrediting 9 of the 10 HIV molecular laboratories in 3 years at a reduced cost. Continuous mentorship is key in the maintenance of accreditation., (© Moyo et al.)

Published
2024
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