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2. History of tuberculosis disease is associated with genetic regulatory variation in Peruvians.

Author

Nieto-Caballero, Victor, Reijneveld, Josephine, Ruvalcaba, Angel, Innocenzi, Gabriel, Abeydeera, Nalin, Asgari, Samira, Lopez, Kattya, Iwany, Sarah, Luo, Yang, Nathan, Aparna, Fernandez-Salinas, Daniela, Chiñas, Marcos, Huang, Chuan-Chin, Zhang, Zibiao, León, Segundo, Calderon, Roger, Lecca, Leonid, Budzik, Jonathan, Murray, Megan, Van Rhijn, Ildiko, Raychaudhuri, Soumya, Moody, D, Suliman, Sara, and Gutierrez-Arcelus, Maria

Subjects
Humans, Quantitative Trait Loci, Peru, Tuberculosis, Macrophages, Mycobacterium tuberculosis, Female, Dendritic Cells, Male, Adult, Genetic Predisposition to Disease, Genetic Variation, Gene Expression Regulation, Middle Aged, Polymorphism, Single Nucleotide, Gene Expression Profiling
Abstract

A quarter of humanity is estimated to have been exposed to Mycobacterium tuberculosis (Mtb) with a 5-10% risk of developing tuberculosis (TB) disease. Variability in responses to Mtb infection could be due to host or pathogen heterogeneity. Here, we focused on host genetic variation in a Peruvian population and its associations with gene regulation in monocyte-derived macrophages and dendritic cells (DCs). We recruited former household contacts of TB patients who previously progressed to TB (cases, n = 63) or did not progress to TB (controls, n = 63). Transcriptomic profiling of monocyte-derived DCs and macrophages measured the impact of genetic variants on gene expression by identifying expression quantitative trait loci (eQTL). We identified 330 and 257 eQTL genes in DCs and macrophages (False Discovery Rate (FDR) < 0.05), respectively. Four genes in DCs showed interaction between eQTL variants and TB progression status. The top eQTL interaction for a protein-coding gene was with FAH, the gene encoding fumarylacetoacetate hydrolase, which mediates the last step in mammalian tyrosine catabolism. FAH expression was associated with genetic regulatory variation in cases but not controls. Using public transcriptomic and epigenomic data of Mtb-infected monocyte-derived dendritic cells, we found that Mtb infection results in FAH downregulation and DNA methylation changes in the locus. Overall, this study demonstrates effects of genetic variation on gene expression levels that are dependent on history of infectious disease and highlights a candidate pathogenic mechanism through pathogen-response genes. Furthermore, our results point to tyrosine metabolism and related candidate TB progression pathways for further investigation.

Published
2024

4. Dual TCR-α Expression on Mucosal-Associated Invariant T Cells as a Potential Confounder of TCR Interpretation.

Author

Suliman, Sara, Kjer-Nielsen, Lars, Iwany, Sarah K, Lopez Tamara, Kattya, Loh, Liyen, Grzelak, Ludivine, Kedzierska, Katherine, Ocampo, Tonatiuh A, Corbett, Alexandra J, McCluskey, James, Rossjohn, Jamie, León, Segundo R, Calderon, Roger, Lecca-Garcia, Leonid, Murray, Megan B, Moody, D Branch, and Van Rhijn, Ildiko

Subjects
Vaccine Related (AIDS), Prevention, Vaccine Related, Immunization, 2.1 Biological and endogenous factors, Aetiology, Histocompatibility Antigens Class I, Humans, Minor Histocompatibility Antigens, Mucosal-Associated Invariant T Cells, Mucous Membrane, Receptors, Antigen, T-Cell, Immunology
Abstract

Mucosal-associated invariant T (MAIT) cells are innate-like T cells that are highly abundant in human blood and tissues. Most MAIT cells have an invariant TCRα-chain that uses T cell receptor α-variable 1-2 (TRAV1-2) joined to TRAJ33/20/12 and recognizes metabolites from bacterial riboflavin synthesis bound to the Ag-presenting molecule MHC class I related (MR1). Our attempts to identify alternative MR1-presented Ags led to the discovery of rare MR1-restricted T cells with non-TRAV1-2 TCRs. Because altered Ag specificity likely alters affinity for the most potent known Ag, 5-(2-oxopropylideneamino)-6-d-ribitylaminouracil (5-OP-RU), we performed bulk TCRα- and TCRβ-chain sequencing and single-cell-based paired TCR sequencing on T cells that bound the MR1-5-OP-RU tetramer with differing intensities. Bulk sequencing showed that use of V genes other than TRAV1-2 was enriched among MR1-5-OP-RU tetramerlow cells. Although we initially interpreted these as diverse MR1-restricted TCRs, single-cell TCR sequencing revealed that cells expressing atypical TCRα-chains also coexpressed an invariant MAIT TCRα-chain. Transfection of each non-TRAV1-2 TCRα-chain with the TCRβ-chain from the same cell demonstrated that the non-TRAV1-2 TCR did not bind the MR1-5-OP-RU tetramer. Thus, dual TCRα-chain expression in human T cells and competition for the endogenous β-chain explains the existence of some MR1-5-OP-RU tetramerlow T cells. The discovery of simultaneous expression of canonical and noncanonical TCRs on the same T cell means that claims of roles for non-TRAV1-2 TCR in MR1 response must be validated by TCR transfer-based confirmation of Ag specificity.

Published
2022

5. Performance Evaluation of Lateral Flow Assays for Coronavirus Disease-19 Serology.

Author

Ochola, Lucy, Ogongo, Paul, Mungai, Samuel, Gitaka, Jesse, and Suliman, Sara

Subjects
Humans, Antibodies, Viral, Seroepidemiologic Studies, Pandemics, COVID-19, SARS-CoV-2, Diagnostics, LFAs, Serology, Immunization, Prevention, Infectious Diseases, Biodefense, Emerging Infectious Diseases, Lung, Vaccine Related, Infection, Good Health and Well Being, Clinical Sciences, Pathology
Abstract

The coronavirus disease of 2019 (COVID-19) pandemic, caused by infection with the severe acute respiratory syndrome coronavirus-2 (SARS-CoV-2), has undoubtedly resulted in significant morbidities, mortalities, and economic disruptions across the globe. Affordable and scalable tools to monitor the transmission dynamics of the SARS-CoV-2 virus and the longevity of induced antibodies will be paramount to monitor and control the pandemic as multiple waves continue to rage in many countries. Serologic assays detect humoral responses to the virus, to determine seroprevalence in target populations, or induction of antibodies at the individual level following either natural infection or vaccination. With multiple vaccines rolling out globally, serologic assays to detect anti-SARS-CoV-2 antibodies will be important tools to monitor the development of herd immunity. To address this need, serologic lateral flow assays (LFAs), which can be easily implemented for both population surveillance and home use, will be vital to monitor the evolution of the pandemic and inform containment measures. Such assays are particularly important for monitoring the transmission dynamics and durability of immunity generated by natural infections and vaccination, particularly in resource-limited settings. In this review, we discuss considerations for evaluating the accuracy of these LFAs, their suitability for different use cases, and implementation opportunities.

Published
2022

6. Neutrophil degranulation, NETosis and platelet degranulation pathway genes are co-induced in whole blood up to six months before tuberculosis diagnosis

Author

Meier, Stuart, Seddon, James A, Maasdorp, Elizna, Kleynhans, Léanie, du Plessis, Nelita, Loxton, Andre G, Malherbe, Stephanus T, Zak, Daniel E, Thompson, Ethan, Duffy, Fergal J, Kaufmann, Stefan HE, Ottenhoff, Tom HM, Scriba, Thomas J, Suliman, Sara, Sutherland, Jayne S, Winter, Jill, Kuivaniemi, Helena, Walzl, Gerhard, Tromp, Gerard, Consortium, GC6-74, and Consortium, Catalysis TB Biomarkers

Subjects
Biomedical and Clinical Sciences, Clinical Sciences, Lung, Infectious Diseases, Rare Diseases, Clinical Research, Tuberculosis, Genetics, Detection, screening and diagnosis, Aetiology, 4.1 Discovery and preclinical testing of markers and technologies, 2.1 Biological and endogenous factors, Infection, Good Health and Well Being, Humans, Neutrophils, Positron Emission Tomography Computed Tomography, Neutrophil Activation, Mycobacterium tuberculosis, Tuberculosis, Lymph Node, GC6-74 Consortium, Catalysis TB Biomarkers Consortium, General Science & Technology
Abstract

Mycobacterium tuberculosis (M.tb) causes tuberculosis (TB) and remains one of the leading causes of mortality due to an infectious pathogen. Host immune responses have been implicated in driving the progression from infection to severe lung disease. We analyzed longitudinal RNA sequencing (RNAseq) data from the whole blood of 74 TB progressors whose samples were grouped into four six-month intervals preceding diagnosis (the GC6-74 study). We additionally analyzed RNAseq data from an independent cohort of 90 TB patients with positron emission tomography-computed tomography (PET-CT) scan results which were used to categorize them into groups with high and low levels of lung damage (the Catalysis TB Biomarker study). These groups were compared to non-TB controls to obtain a complete whole blood transcriptional profile for individuals spanning from early stages of M.tb infection to TB diagnosis. The results revealed a steady increase in the number of genes that were differentially expressed in progressors at time points closer to diagnosis with 278 genes at 13-18 months, 742 at 7-12 months and 5,131 detected 1-6 months before diagnosis and 9,205 detected in TB patients. A total of 2,144 differentially expressed genes were detected when comparing TB patients with high and low levels of lung damage. There was a large overlap in the genes upregulated in progressors 1-6 months before diagnosis (86%) with those in TB patients. A comprehensive pathway analysis revealed a potent activation of neutrophil and platelet mediated defenses including neutrophil and platelet degranulation, and NET formation at both time points. These pathways were also enriched in TB patients with high levels of lung damage compared to those with low. These findings suggest that neutrophils and platelets play a critical role in TB pathogenesis, and provide details of the timing of specific effector mechanisms that may contribute to TB lung pathology.

Published
2022

7. Coronavirus Disease 2019 Diagnostics: Key to Africa's Recovery

Author

Naidoo, Sanushka, Gitaka, Jesse, Suliman, Sara, Baptista, Sara, Oyedemi, Blessing Mbabie, Nepolo, Emmanuel, and Enany, Shymaa

Subjects
Biochemistry and Cell Biology, Biological Sciences, Rare Diseases, Pneumonia & Influenza, Vaccine Related, Emerging Infectious Diseases, Prevention, Immunization, Lung, Infectious Diseases, Biodefense, Detection, screening and diagnosis, 4.1 Discovery and preclinical testing of markers and technologies, Infection, Good Health and Well Being, COVID-19 Testing, Humans, COVID-19, SARS-CoV-2, diagnosis, RT-PCR, Biochemistry & Molecular Biology, Biochemistry and cell biology
Abstract

With the coronavirus disease of 2019 (COVID-19) becoming a full-blown outbreak in Africa, coupled with many other challenges faced on the African continent, it is apparent that Africa continues to need diagnostics to enable case identification and recovery to this and future challenges. With the slow vaccination rates across the continent, reliable diagnostic tests will be in demand, likely for years to come. Thus, access to reliable diagnostic tools to detect the severe acute respiratory syndrome of the coronavirus-2 (SARS-CoV-2), the virus responsible for COVID-19, remain a critical pillar to monitor and contain new waves of COVID-19. Increasing the local capacity to manufacture and roll-out vaccines and decentralized COVID-19 testing are paramount for fighting the pandemic in Africa.

Published
2022

8. Multimodally profiling memory T cells from a tuberculosis cohort identifies cell state associations with demographics, environment and disease

Author

Nathan, Aparna, Beynor, Jessica I, Baglaenko, Yuriy, Suliman, Sara, Ishigaki, Kazuyoshi, Asgari, Samira, Huang, Chuan-Chin, Luo, Yang, Zhang, Zibiao, Lopez, Kattya, Lindestam Arlehamn, Cecilia S, Ernst, Joel D, Jimenez, Judith, Calderón, Roger I, Lecca, Leonid, Van Rhijn, Ildiko, Moody, D Branch, Murray, Megan B, and Raychaudhuri, Soumya

Subjects
Genetics, Prevention, Tuberculosis, Biodefense, Emerging Infectious Diseases, Rare Diseases, Vaccine Related, Infectious Diseases, Clinical Research, Lung, 2.1 Biological and endogenous factors, Aetiology, Infection, Good Health and Well Being, Adolescent, Adult, Age Factors, Aged, Aged, 80 and over, Case-Control Studies, Child, Disease Progression, Female, Follow-Up Studies, Genetic Predisposition to Disease, Genotyping Techniques, Humans, Immunologic Memory, Male, Middle Aged, Mycobacterium tuberculosis, Peru, RNA-Seq, Sex Factors, Single-Cell Analysis, Socioeconomic Factors, Th17 Cells, Tuberculosis, Pulmonary, Young Adult, Immunology
Abstract

Multimodal T cell profiling can enable more precise characterization of elusive cell states underlying disease. Here, we integrated single-cell RNA and surface protein data from 500,089 memory T cells to define 31 cell states from 259 individuals in a Peruvian tuberculosis (TB) progression cohort. At immune steady state >4 years after infection and disease resolution, we found that, after accounting for significant effects of age, sex, season and genetic ancestry on T cell composition, a polyfunctional type 17 helper T (TH17) cell-like effector state was reduced in abundance and function in individuals who previously progressed from Mycobacterium tuberculosis (M.tb) infection to active TB disease. These cells are capable of responding to M.tb peptides. Deconvoluting this state-uniquely identifiable with multimodal analysis-from public data demonstrated that its depletion may precede and persist beyond active disease. Our study demonstrates the power of integrative multimodal single-cell profiling to define cell states relevant to disease and other traits.

Published
2021

9. RISK6, a 6-gene transcriptomic signature of TB disease risk, diagnosis and treatment response

Author

Penn-Nicholson, Adam, Mbandi, Stanley Kimbung, Thompson, Ethan, Mendelsohn, Simon C, Suliman, Sara, Chegou, Novel N, Malherbe, Stephanus T, Darboe, Fatoumatta, Erasmus, Mzwandile, Hanekom, Willem A, Bilek, Nicole, Fisher, Michelle, Kaufmann, Stefan HE, Winter, Jill, Murphy, Melissa, Wood, Robin, Morrow, Carl, Van Rhijn, Ildiko, Moody, Branch, Murray, Megan, Andrade, Bruno B, Sterling, Timothy R, Sutherland, Jayne, Naidoo, Kogieleum, Padayatchi, Nesri, Walzl, Gerhard, Hatherill, Mark, Zak, Daniel, and Scriba, Thomas J

Subjects
Biomedical and Clinical Sciences, Clinical Sciences, Clinical Research, Prevention, Infectious Diseases, HIV/AIDS, Lung, Tuberculosis, Rare Diseases, 4.1 Discovery and preclinical testing of markers and technologies, Detection, screening and diagnosis, 4.2 Evaluation of markers and technologies, Infection, Good Health and Well Being, Adolescent, Area Under Curve, Biomarkers, Cohort Studies, Female, HIV Infections, Humans, Male, Mycobacterium tuberculosis, Point-of-Care Systems, Positron-Emission Tomography, Prognosis, RNA, Bacterial, ROC Curve, Real-Time Polymerase Chain Reaction, Sensitivity and Specificity, Adolescent Cohort Study team, GC6-74 Consortium, SATVI Clinical and Laboratory Team, ScreenTB Consortium, AE-TBC Consortium, RePORT Brazil Team, Peruvian Household Contacts Cohort Team, CAPRISA IMPRESS team
Abstract

Improved tuberculosis diagnostics and tools for monitoring treatment response are urgently needed. We developed a robust and simple, PCR-based host-blood transcriptomic signature, RISK6, for multiple applications: identifying individuals at risk of incident disease, as a screening test for subclinical or clinical tuberculosis, and for monitoring tuberculosis treatment. RISK6 utility was validated by blind prediction using quantitative real-time (qRT) PCR in seven independent cohorts. Prognostic performance significantly exceeded that of previous signatures discovered in the same cohort. Performance for diagnosing subclinical and clinical disease in HIV-uninfected and HIV-infected persons, assessed by area under the receiver-operating characteristic curve, exceeded 85%. As a screening test for tuberculosis, the sensitivity at 90% specificity met or approached the benchmarks set out in World Health Organization target product profiles for non-sputum-based tests. RISK6 scores correlated with lung immunopathology activity, measured by positron emission tomography, and tracked treatment response, demonstrating utility as treatment response biomarker, while predicting treatment failure prior to treatment initiation. Performance of the test in capillary blood samples collected by finger-prick was noninferior to venous blood collected in PAXgene tubes. These results support incorporation of RISK6 into rapid, capillary blood-based point-of-care PCR devices for prospective assessment in field studies.

Published
2020

11. The Coronavirus Standards Working Group’s roadmap for improved population testing

Author

Mercer, Tim, Almond, Neil, Crone, Michael A., Chain, Patrick S. G., Deshpande, Alina, Eveleigh, Deepa, Freemont, Paul, Fuchs, Sebastien, Garlick, Russell, Huggett, Jim, Kammel, Martin, Li, Po-E, Milavec, Mojca, Marlowe, Elizabeth M., O’Sullivan, Denise M., Page, Mark, Pestano, Gary A., Suliman, Sara, Simen, Birgitte, Sninsky, John J., Sopchak, Lynne, Tato, Cristina M., Vallone, Peter M., Vandesompele, Jo, White, Thomas J., Zeichhardt, Heinz, and Salit, Marc

Published
2022
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12. A TCR β-Chain Motif Biases toward Recognition of Human CD1 Proteins.

Author

Reinink, Peter, Shahine, Adam, Gras, Stephanie, Cheng, Tan-Yun, Farquhar, Rachel, Lopez, Kattya, Suliman, Sara A, Reijneveld, Josephine F, Le Nours, Jérôme, Tan, Li Lynn, León, Segundo R, Jimenez, Judith, Calderon, Roger, Lecca, Leonid, Murray, Megan B, Rossjohn, Jamie, Moody, D Branch, and Van Rhijn, Ildiko

Subjects
Biochemistry and Cell Biology, Biomedical and Clinical Sciences, Biological Sciences, Immunology, Biotechnology, Clinical Research, Underpinning research, 1.1 Normal biological development and functioning, Amino Acid Motifs, Antigen Presentation, Antigens, CD1d, Binding Sites, Conserved Sequence, Epitopes, T-Lymphocyte, Gene Rearrangement, High-Throughput Nucleotide Sequencing, Humans, Immunophenotyping, Lipids, Models, Molecular, Mutation, Protein Binding, Protein Conformation, Protein Multimerization, Receptors, Antigen, T-Cell, alpha-beta, Structure-Activity Relationship, T-Lymphocytes, Biochemistry and cell biology
Abstract

High-throughput TCR sequencing allows interrogation of the human TCR repertoire, potentially connecting TCR sequences to antigenic targets. Unlike the highly polymorphic MHC proteins, monomorphic Ag-presenting molecules such as MR1, CD1d, and CD1b present Ags to T cells with species-wide TCR motifs. CD1b tetramer studies and a survey of the 27 published CD1b-restricted TCRs demonstrated a TCR motif in humans defined by the TCR β-chain variable gene 4-1 (TRBV4-1) region. Unexpectedly, TRBV4-1 was involved in recognition of CD1b regardless of the chemical class of the carried lipid. Crystal structures of two CD1b-specific TRBV4-1+ TCRs show that germline-encoded residues in CDR1 and CDR3 regions of TRBV4-1-encoded sequences interact with each other and consolidate the surface of the TCR. Mutational studies identified a key positively charged residue in TRBV4-1 and a key negatively charged residue in CD1b that is shared with CD1c, which is also recognized by TRBV4-1 TCRs. These data show that one TCR V region can mediate a mechanism of recognition of two related monomorphic Ag-presenting molecules that does not rely on a defined lipid Ag.

Published
2019

13. MR1-Independent Activation of Human Mucosal-Associated Invariant T Cells by Mycobacteria

Author

Suliman, Sara, Murphy, Melissa, Musvosvi, Munyaradzi, Gela, Anele, Meermeier, Erin W, Geldenhuys, Hennie, Hopley, Christiaan, Toefy, Asma, Bilek, Nicole, Veldsman, Ashley, Hanekom, Willem A, Johnson, John L, Boom, W Henry, Obermoser, Gerlinde, Huang, Huang, Hatherill, Mark, Lewinsohn, David M, Nemes, Elisa, and Scriba, Thomas J

Subjects
Biomedical and Clinical Sciences, Immunology, Rare Diseases, Vaccine Related, Immunization, HIV/AIDS, Prevention, Infectious Diseases, Clinical Research, Tuberculosis, Tuberculosis Vaccine, Aetiology, 2.1 Biological and endogenous factors, Infection, Good Health and Well Being, Adolescent, Child, Cohort Studies, Cytokines, Histocompatibility Antigens Class I, Humans, Minor Histocompatibility Antigens, Mucosal-Associated Invariant T Cells, Mycobacterium tuberculosis, Receptors, Antigen, T-Cell, Biochemistry and cell biology
Abstract

Tuberculosis (TB) is the leading cause of mortality from a single infectious agent, Mycobacterium tuberculosis Relevant immune targets of the partially efficacious TB vaccine bacille Calmette-Guérin (BCG) remain poorly defined. Mucosal-associated invariant T (MAIT) cells are MHC-related protein 1 (MR1)-restricted T cells, which are reactive against M. tuberculosis, and underexplored as potential TB vaccine targets. We sought to determine whether BCG vaccination activated mycobacteria-specific MAIT cell responses in humans. We analyzed whole blood samples from M. tuberculosis-infected South African adults who were revaccinated with BCG after a six-month course of isoniazid preventative therapy. In vitro BCG stimulation potently induced IFN-γ expression by phenotypic (CD8+CD26+CD161+) MAIT cells, which constituted the majority (75%) of BCG-reactive IFN-γ-producing CD8+ T cells. BCG revaccination transiently expanded peripheral blood frequencies of BCG-reactive IFN-γ+ MAIT cells, which returned to baseline frequencies a year following vaccination. In another cohort of healthy adults who received BCG at birth, 53% of mycobacteria-reactive-activated CD8 T cells expressed CDR3α TCRs, previously reported as MAIT TCRs, expressing the canonical TRAV1-2-TRAJ33 MAIT TCRα rearrangement. CD26 and CD161 coexpression correlated with TRAV1-2+CD161+ phenotype more accurately in CD8+ than CD4-CD8- MAIT cells. Interestingly, BCG-induced IFN-γ expression by MAIT cells in vitro was mediated by the innate cytokines IL-12 and IL-18 more than MR1-induced TCR signaling, suggesting TCR-independent activation. Collectively, the data suggest that activation of blood MAIT cells by innate inflammatory cytokines is a major mechanism of responsiveness to vaccination with whole cell vaccines against TB or in vitro stimulation with mycobacteria (Clinical trial registration: NCT01119521).

Published
2019

14. Early progression to active tuberculosis is a highly heritable trait driven by 3q23 in Peruvians

Author

Luo, Yang, Suliman, Sara, Asgari, Samira, Amariuta, Tiffany, Baglaenko, Yuriy, Martínez-Bonet, Marta, Ishigaki, Kazuyoshi, Gutierrez-Arcelus, Maria, Calderon, Roger, Lecca, Leonid, León, Segundo R, Jimenez, Judith, Yataco, Rosa, Contreras, Carmen, Galea, Jerome T, Becerra, Mercedes, Nejentsev, Sergey, Nigrovic, Peter A, Moody, D Branch, Murray, Megan B, and Raychaudhuri, Soumya

Subjects
Biological Sciences, Genetics, Prevention, Orphan Drug, Lung, Infectious Diseases, Rare Diseases, Tuberculosis, Vaccine Related, Human Genome, Aetiology, 2.1 Biological and endogenous factors, Infection, Good Health and Well Being, Adult, Disease Progression, Female, Gene Expression, Genetic Loci, Genome-Wide Association Study, Genotype, Humans, Male, Monocytes, Mycobacterium tuberculosis, Peru, Sodium-Potassium-Exchanging ATPase
Abstract

Of the 1.8 billion people worldwide infected with Mycobacterium tuberculosis, 5-15% will develop active tuberculosis (TB). Approximately half will progress to active TB within the first 18 months after infection, presumably because they fail to mount an effective initial immune response. Here, in a genome-wide genetic study of early TB progression, we genotype 4002 active TB cases and their household contacts in Peru. We quantify genetic heritability ([Formula: see text]) of early TB progression to be 21.2% (standard error 0.08). This suggests TB progression has a strong genetic basis, and is comparable to traits with well-established genetic bases. We identify a novel association between early TB progression and variants located in a putative enhancer region on chromosome 3q23 (rs73226617, OR = 1.18; P = 3.93 × 10-8). With in silico and in vitro analyses we identify rs73226617 or rs148722713 as the likely functional variant and ATP1B3 as a potential causal target gene with monocyte specific function.

Published
2019

15. Discovery and validation of a prognostic proteomic signature for tuberculosis progression: A prospective cohort study

Author

Penn-Nicholson, Adam, Hraha, Thomas, Thompson, Ethan G, Sterling, David, Mbandi, Stanley Kimbung, Wall, Kirsten M, Fisher, Michelle, Suliman, Sara, Shankar, Smitha, Hanekom, Willem A, Janjic, Nebojsa, Hatherill, Mark, Kaufmann, Stefan HE, Sutherland, Jayne, Walzl, Gerhard, De Groote, Mary Ann, Ochsner, Urs, Zak, Daniel E, and Scriba, Thomas J

Subjects
Biomedical and Clinical Sciences, Clinical Sciences, Infectious Diseases, Rare Diseases, HIV/AIDS, Tuberculosis, Clinical Research, Prevention, Detection, screening and diagnosis, 4.1 Discovery and preclinical testing of markers and technologies, 4.2 Evaluation of markers and technologies, Infection, Good Health and Well Being, Adolescent, Biomarkers, Child, Cohort Studies, Diagnostic Tests, Routine, Disease Progression, Female, Humans, Longitudinal Studies, Male, Point-of-Care Testing, Prognosis, Prospective Studies, Proteome, Proteomics, ACS and GC6–74 cohort study groups, Medical and Health Sciences, General & Internal Medicine, Biomedical and clinical sciences, Health sciences
Abstract

BackgroundA nonsputum blood test capable of predicting progression of healthy individuals to active tuberculosis (TB) before clinical symptoms manifest would allow targeted treatment to curb transmission. We aimed to develop a proteomic biomarker of risk of TB progression for ultimate translation into a point-of-care diagnostic.Methods and findingsProteomic TB risk signatures were discovered in a longitudinal cohort of 6,363 Mycobacterium tuberculosis-infected, HIV-negative South African adolescents aged 12-18 years (68% female) who participated in the Adolescent Cohort Study (ACS) between July 6, 2005 and April 23, 2007, through either active (every 6 months) or passive follow-up over 2 years. Forty-six individuals developed microbiologically confirmed TB disease within 2 years of follow-up and were selected as progressors; 106 nonprogressors, who remained healthy, were matched to progressors. Over 3,000 human proteins were quantified in plasma with a highly multiplexed proteomic assay (SOMAscan). Three hundred sixty-one proteins of differential abundance between progressors and nonprogressors were identified. A 5-protein signature, TB Risk Model 5 (TRM5), was discovered in the ACS training set and verified by blind prediction in the ACS test set. Poor performance on samples 13-24 months before TB diagnosis motivated discovery of a second 3-protein signature, 3-protein pair-ratio (3PR) developed using an orthogonal strategy on the full ACS subcohort. Prognostic performance of both signatures was validated in an independent cohort of 1,948 HIV-negative household TB contacts from The Gambia (aged 15-60 years, 66% female), longitudinally followed up for 2 years between March 5, 2007 and October 21, 2010, sampled at baseline, month 6, and month 18. Amongst these contacts, 34 individuals progressed to microbiologically confirmed TB disease and were included as progressors, and 115 nonprogressors were included as controls. Prognostic performance of the TRM5 signature in the ACS training set was excellent within 6 months of TB diagnosis (area under the receiver operating characteristic curve [AUC] 0.96 [95% confidence interval, 0.93-0.99]) and 6-12 months (AUC 0.76 [0.65-0.87]) before TB diagnosis. TRM5 validated with an AUC of 0.66 (0.56-0.75) within 1 year of TB diagnosis in the Gambian validation cohort. The 3PR signature yielded an AUC of 0.89 (0.84-0.95) within 6 months of TB diagnosis and 0.72 (0.64-0.81) 7-12 months before TB diagnosis in the entire South African discovery cohort and validated with an AUC of 0.65 (0.55-0.75) within 1 year of TB diagnosis in the Gambian validation cohort. Signature validation may have been limited by a systematic shift in signal magnitudes generated by differences between the validation assay when compared to the discovery assay. Further validation, especially in cohorts from non-African countries, is necessary to determine how generalizable signature performance is.ConclusionsBoth proteomic TB risk signatures predicted progression to incident TB within a year of diagnosis. To our knowledge, these are the first validated prognostic proteomic signatures. Neither meet the minimum criteria as defined in the WHO Target Product Profile for a progression test. More work is required to develop such a test for practical identification of individuals for investigation of incipient, subclinical, or active TB disease for appropriate treatment and care.

Published
2019

17. Novel PIK3R1 gene mutation associated with SHORT syndrome: a case report of a 15-year-old female.

Author

Osman, Amani, Morsi, Amr, El-Refee, Sherif, and Suliman, Sara

Abstract

To present the clinical journey and management of a 15-year-old female with SHORT syndrome, highlighting the diagnostic challenges and the novel genetic mutation identified. A 15-year-old Filipino female was initially seen in a dermatology clinic at 9 years old for axillary skin darkening, indicative of acanthosis nigricans. Early evaluations revealed elevated blood glucose levels, resulting in a pediatric diabetes diagnosis without the usual hyperglycemic symptoms. Her medical history was notable for premature birth, intrauterine growth restriction, a cardiac murmur from patent ductus arteriosus and a bicuspid aortic valve, delayed teething, and distinct dysmorphic features. Genetic testing identified a novel PIK3R1 gene mutation. Treatment with metformin significantly improved her glycemic control and lipid profiles. The patient also displayed delayed puberty and polycystic ovary syndrome-like symptoms, but growth hormone deficiency was excluded. Endocrine evaluation for her short stature and lipodystrophy confirmed the presence of the PIK3R1 mutation. This case highlights the importance of thorough endocrine and genetic evaluations in patients with complex clinical presentations like SHORT syndrome. The identification of a novel PIK3R1 gene mutation expands the understanding of the genetic basis of this syndrome and underscores the need for individualized treatment approaches. [ABSTRACT FROM AUTHOR]

Published
2024
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18. The Impact of the Clinical Pharmacist-Led Diabetes Education on the Knowledge and Attitude of Individuals with Type II Diabetes Mellitus: An Interventional Study.

Author

Badi, Safaa, Suliman, Sara Zainelabdein, Almahdi, Rayan, Aldomah, Mohammed A., Elkheir, Habab Khalid, Ibrahim, Mohamed Izham Mohamed, and Ahmed, Mohamed H.

Subjects
TYPE 2 diabetes, GLYCEMIC control, PHARMACISTS' attitudes, CLINICAL trials, DIABETES
Abstract

Background: Diabetes mellitus is a complex condition to manage. Patients with a greater understanding and knowledge of their condition might achieve better glycemic control than others. This study aimed to evaluate the impact of clinical pharmacist-led diabetes education on the knowledge and attitude of individuals with type II diabetes mellitus (T2DM). Methods: This study was a quasi-experimental study which was conducted at a diabetes clinic in Khartoum, Sudan. The study population was adult individuals with T2DM who attended the diabetes clinic. The estimated sample size was 182 participants. The participants were selected randomly by a simple random sampling method. The knowledge and attitudes of the participants were assessed at baseline and at the end of the study after 12 months. The intervention was carried out through educational materials about diabetes and medications for its treatment. Results: The majority of the participants were females. The mean age was 54.5 (±10) years. Most participants had a family history of diabetes (69.2%). The mean knowledge score after the intervention was increased by 1.4 (±0.1) from baseline, p value (<0.001), while the mean attitude score was increased by 1.7 (±0.2) from baseline, p value (<0.001). At baseline, 14.8% of the participants had a high level of knowledge and 18.7% had a negative attitude, while after intervention for 12 months, 28.5% of them had a high level of knowledge and 16.8% had a negative attitude (p values < 0.001, 0.032, respectively). Conclusions: The knowledge of and attitudes towards diabetes differed significantly as a result of the educational program provided by the clinical pharmacist. [ABSTRACT FROM AUTHOR]

Published
2024
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19. Effects of BCG vaccination on donor unrestricted T cells in two prospective cohort studies

Author

Gela, Anele, Murphy, Melissa, Rodo, Miguel, Hadley, Kate, Hanekom, Willem A., Boom, W.Henry, Johnson, John L., Hoft, Daniel F., Joosten, Simone A., Ottenhoff, Tom H.M., Suliman, Sara, Moody, D.Branch, Lewinsohn, David M., Hatherill, Mark, Seshadri, Chetan, Nemes, Elisa, Scriba, Thomas J., Briel, Libby, Veldtsman, Hellen, Khomba, Nondumiso, Pienaar, Bernadette, Africa, Hadn, and Steyn, Marcia

Published
2022
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20. Four-Gene Pan-African Blood Signature Predicts Progression to Tuberculosis

Author

Suliman, Sara, Thompson, Ethan G, Sutherland, Jayne, Weiner, January, Ota, Martin OC, Shankar, Smitha, Penn-Nicholson, Adam, Thiel, Bonnie, Erasmus, Mzwandile, Maertzdorf, Jeroen, Duffy, Fergal J, Hill, Philip C, Hughes, E Jane, Stanley, Kim, Downing, Katrina, Fisher, Michelle L, Valvo, Joe, Parida, Shreemanta K, van der Spuy, Gian, Tromp, Gerard, Adetifa, Ifedayo MO, Donkor, Simon, Howe, Rawleigh, Mayanja-Kizza, Harriet, Boom, W Henry, Dockrell, Hazel M, Ottenhoff, Tom HM, Hatherill, Mark, Aderem, Alan, Hanekom, Willem A, Scriba, Thomas J, Kaufmann, Stefan HE, Zak, Daniel E, Walzl, Gerhard, Black, Gillian F, Kriel, Magdalena, Du Plessis, Nelita, Nene, Nonhlanhla, Roberts, Teri, Kleynhans, Leanie, Gutschmidt, Andrea, Smith, Bronwyn, Loxton, Andre G, Chegou, Novel N, Tromp, Gerhardus, Tabb, David, Klein, Michel R, Haks, Marielle C, Franken, Kees LMC, Geluk, Annemieke, van Meijgaarden, Krista E, Joosten, Simone A, Joloba, Moses, Zalwango, Sarah, Nsereko, Mary, Okwera, Brenda, Kisingo, Hussein, Golinski, Robert, Jacobson, Marc, Dockrell, Hazel, Smith, Steven, Gorak-Stolinska, Patricia, Hur, Yun-Gyoung, Lalor, Maeve, Lee, Ji-Sook, Crampin, Amelia C, French, Neil, Ngwira, Bagrey, Ben-Smith, Anne, Watkins, Kate, Ambrose, Lyn, Simukonda, Felanji, Mvula, Hazzie, Chilongo, Femia, Saul, Jacky, Branson, Keith, Mahomed, Hassan, Bilek, Nicole, Xasa, Onke, Veldsman, Ashley, Fisher, Michelle, and Mulenga, Humphrey

Subjects
HIV/AIDS, Rare Diseases, Infectious Diseases, Tuberculosis, Clinical Research, Emerging Infectious Diseases, Prevention, Genetics, 2.1 Biological and endogenous factors, 4.2 Evaluation of markers and technologies, 4.1 Discovery and preclinical testing of markers and technologies, Aetiology, Detection, screening and diagnosis, Infection, Good Health and Well Being, GC6-74 cohort study team, The ACS cohort study team, biomarkers, gene expression, tuberculosis, Medical and Health Sciences, Respiratory System
Abstract

Rationale: Contacts of patients with tuberculosis (TB) constitute an important target population for preventive measures because they are at high risk of infection with Mycobacterium tuberculosis and progression to disease.Objectives: We investigated biosignatures with predictive ability for incident TB.Methods: In a case-control study nested within the Grand Challenges 6-74 longitudinal HIV-negative African cohort of exposed household contacts, we employed RNA sequencing, PCR, and the pair ratio algorithm in a training/test set approach. Overall, 79 progressors who developed TB between 3 and 24 months after diagnosis of index case and 328 matched nonprogressors who remained healthy during 24 months of follow-up were investigated.Measurements and Main Results: A four-transcript signature derived from samples in a South African and Gambian training set predicted progression up to two years before onset of disease in blinded test set samples from South Africa, the Gambia, and Ethiopia with little population-associated variability, and it was also validated in an external cohort of South African adolescents with latent M. tuberculosis infection. By contrast, published diagnostic or prognostic TB signatures were predicted in samples from some but not all three countries, indicating site-specific variability. Post hoc meta-analysis identified a single gene pair, C1QC/TRAV27 (complement C1q C-chain / T-cell receptor-α variable gene 27) that would consistently predict TB progression in household contacts from multiple African sites but not in infected adolescents without known recent exposure events.Conclusions: Collectively, we developed a simple whole blood-based PCR test to predict TB in recently exposed household contacts from diverse African populations. This test has potential for implementation in national TB contact investigation programs.

Published
2018

21. Evaluation of the Access Bio CareStart rapid SARS-CoV-2 antigen test in asymptomatic individuals tested at a community mass-testing program in Western Massachusetts

Author

Suliman, Sara, Matias, Wilfredo R., Fulcher, Isabel R., Molano, Francisco J., Collins, Shannon, Uceta, Elizabeth, Zhu, Jack, Paxton, Ryan M., Gonsalves, Sean F., Harden, Maegan V., Fisher, Marissa, Meldrim, Jim, Gabriel, Stacey, Franke, Molly F., Hung, Deborah T., Smole, Sandra C., Madoff, Lawrence C., and Ivers, Louise C.

Published
2022
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25. Sequential inflammatory processes define human progression from M. tuberculosis infection to tuberculosis disease

Author

Scriba, Thomas J, Penn-Nicholson, Adam, Shankar, Smitha, Hraha, Tom, Thompson, Ethan G, Sterling, David, Nemes, Elisa, Darboe, Fatoumatta, Suliman, Sara, Amon, Lynn M, Mahomed, Hassan, Erasmus, Mzwandile, Whatney, Wendy, Johnson, John L, Boom, W Henry, Hatherill, Mark, Valvo, Joe, De Groote, Mary Ann, Ochsner, Urs A, Aderem, Alan, Hanekom, Willem A, and Zak, Daniel E

Subjects
Biomedical and Clinical Sciences, Immunology, Genetics, Tuberculosis Vaccine, Tuberculosis, Emerging Infectious Diseases, Lung, Vaccine Related, Immunization, Clinical Research, Infectious Diseases, Prevention, Rare Diseases, Biotechnology, Aetiology, 2.1 Biological and endogenous factors, Inflammatory and immune system, Infection, Good Health and Well Being, Adolescent, Child, Disease Progression, Humans, Inflammation, Mycobacterium tuberculosis, T-Lymphocytes, Vaccines, other members of the ACS cohort study team, Microbiology, Medical Microbiology, Virology, Medical microbiology
Abstract

Our understanding of mechanisms underlying progression from Mycobacterium tuberculosis infection to pulmonary tuberculosis disease in humans remains limited. To define such mechanisms, we followed M. tuberculosis-infected adolescents longitudinally. Blood samples from forty-four adolescents who ultimately developed tuberculosis disease (“progressors”) were compared with those from 106 matched controls, who remained healthy during two years of follow up. We performed longitudinal whole blood transcriptomic analyses by RNA sequencing and plasma proteome analyses using multiplexed slow off-rate modified DNA aptamers. Tuberculosis progression was associated with sequential modulation of immunological processes. Type I/II interferon signalling and complement cascade were elevated 18 months before tuberculosis disease diagnosis, while changes in myeloid inflammation, lymphoid, monocyte and neutrophil gene modules occurred more proximally to tuberculosis disease. Analysis of gene expression in purified T cells also revealed early suppression of Th17 responses in progressors, relative to M. tuberculosis-infected controls. This was confirmed in an independent adult cohort who received BCG re-vaccination; transcript expression of interferon response genes in blood prior to BCG administration was associated with suppression of IL-17 expression by BCG-specific CD4 T cells 3 weeks post-vaccination. Our findings provide a timeline to the different immunological stages of disease progression which comprise sequential inflammatory dynamics and immune alterations that precede disease manifestations and diagnosis of tuberculosis disease. These findings have important implications for developing diagnostics, vaccination and host-directed therapies for tuberculosis.Trial registrationClincialtrials.gov, NCT01119521.

Published
2017

26. CD1: From Molecules to Diseases

Author

Moody, D Branch and Suliman, Sara

Subjects
Biochemistry and Cell Biology, Biomedical and Clinical Sciences, Biological Sciences, Immunology, Clinical Research, Underpinning research, 1.1 Normal biological development and functioning, Generic health relevance, CD1, T cell receptor, TCR, antigen display, Clinical Sciences, Oncology and Carcinogenesis
Abstract

The human cluster of differentiation (CD)1 system for antigen display is comprised of four types of antigen-presenting molecules, each with a distinct functional niche: CD1a, CD1b, CD1c, and CD1d. Whereas CD1 proteins were thought solely to influence T-cell responses through display of amphipathic lipids, recent studies emphasize the role of direct contacts between the T-cell receptor and CD1 itself. Moving from molecules to diseases, new research approaches emphasize human CD1-transgenic mouse models and the study of human polyclonal T cells in vivo or ex vivo in disease states. Whereas the high genetic diversity of major histocompatibility complex (MHC)-encoded antigen-presenting molecules provides a major hurdle for designing antigens that activate T cells in all humans, the simple population genetics of the CD1 system offers the prospect of discovering or designing broadly acting immunomodulatory agents.

Published
2017

27. History of tuberculosis disease is associated with genetic regulatory variation in Peruvians

Author

Nieto-Caballero, Victor E., Reijneveld, Josephine F., Ruvalcaba, Angel, Innocenzi, Gabriel, Abeydeera, Nalin, Asgari, Samira, Lopez, Kattya, Iwany, Sarah K., Luo, Yang, Nathan, Aparna, Fernandez-Salinas, Daniela, Chiñas, Marcos, Huang, Chuan Chin, Zhang, Zibiao, León, Segundo R., Calderon, Roger I., Lecca, Leonid, Budzik, Jonathan M., Murray, Megan, Van Rhijn, Ildiko, Raychaudhuri, Soumya, Moody, D. Branch, Suliman, Sara, Gutierrez-Arcelus, Maria, Nieto-Caballero, Victor E., Reijneveld, Josephine F., Ruvalcaba, Angel, Innocenzi, Gabriel, Abeydeera, Nalin, Asgari, Samira, Lopez, Kattya, Iwany, Sarah K., Luo, Yang, Nathan, Aparna, Fernandez-Salinas, Daniela, Chiñas, Marcos, Huang, Chuan Chin, Zhang, Zibiao, León, Segundo R., Calderon, Roger I., Lecca, Leonid, Budzik, Jonathan M., Murray, Megan, Van Rhijn, Ildiko, Raychaudhuri, Soumya, Moody, D. Branch, Suliman, Sara, and Gutierrez-Arcelus, Maria

Abstract

A quarter of humanity is estimated to have been exposed to Mycobacterium tuberculosis (Mtb) with a 5-10% risk of developing tuberculosis (TB) disease. Variability in responses to Mtb infection could be due to host or pathogen heterogeneity. Here, we focused on host genetic variation in a Peruvian population and its associations with gene regulation in monocyte- derived macrophages and dendritic cells (DCs). We recruited former household contacts of TB patients who previously progressed to TB (cases, n = 63) or did not progress to TB (controls, n = 63). Transcriptomic profiling of monocyte-derived DCs and macrophages measured the impact of genetic variants on gene expression by identifying expression quantitative trait loci (eQTL). We identified 330 and 257 eQTL genes in DCs and macrophages (False Discovery Rate (FDR) < 0.05), respectively. Four genes in DCs showed interaction between eQTL variants and TB progression status. The top eQTL interaction for a proteincoding gene was with FAH, the gene encoding fumarylacetoacetate hydrolase, which mediates the last step in mammalian tyrosine catabolism. FAH expression was associated with genetic regulatory variation in cases but not controls. Using public transcriptomic and epigenomic data of Mtb-infected monocyte-derived dendritic cells, we found that Mtb infection results in FAH downregulation and DNA methylation changes in the locus. Overall, this study demonstrates effects of genetic variation on gene expression levels that are dependent on history of infectious disease and highlights a candidate pathogenic mechanism through pathogen-response genes. Furthermore, our results point to tyrosine metabolism and related candidate TB progression pathways for further investigation.

Published
2024

28. The Impact of Clinical Pharmacist Diabetes Education on Medication Adherence in Patients with Type 2 Diabetes Mellitus: An Interventional Study from Khartoum, Sudan

Author

Badi, Safaa, primary, Suliman, Sara Zainelabdein, additional, Almahdi, Rayan, additional, Aldomah, Mohammed A., additional, Marzouq, Mohamed ELsir, additional, Ibrahim, Eiman Eltayeb M., additional, Ahmed, Musaab, additional, Ahmed, Mohamed H., additional, Elkheir, Habab Khalid, additional, and Ibrahim, Mohamed Izham Mohamed, additional

Published
2024
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31. Genetic and physiological investigations of monogenic disorders resulting in severe insulin resistance and aberrant adipose tissue distribution

Author

Suliman, Sara, Karpe, Fredrik, and Gloyn, Anna

Subjects
616.462, Insulin resistance, Adipose tissues, Obesity, Gene expression
Abstract

Background: Regional adiposity and in particular central adiposity is associated with a hazardous metabolic profile, insulin resistance (IR), hypertension and increased cardiovascular mortality whilst gluteo-femoral fat (peripheral fat) is protective. Extreme phenotypes, especially those due to monogenic disorders, are experiments of nature, which have been pivotal in identifying genes involved in disease. The hypothesis tested in this thesis was that investigating individuals with monogenic causes of regional adiposity and IR would identify genes and physiological processes contributing to their phenotype. Methods: Two families with balanced translocations, sixty-nine patients with partial lipodystrophy and eight individuals with lipoma were investigated. Genetic investigations included mapping of balanced translocations using fluorescent in-situ hybridisation, DNA and cDNA sequencing and gene expression studies. In vivo investigations of adipose tissue included microdialysis and measurement of adipose tissue blood flow. Results: Genetic and physiological factors contributing to regional adipose tissue deposition and IR were identified in (1) individuals with lipodystrophy where mutations were identified in eleven families including one novel PPARG mutation V450M. Also a skinfold ratio was developed for the clinical diagnosis of partial lipodystrophy (2) a family with a balanced I translocation, IR and growth retardation, digenic disruption of INSR and CHN2 was identified, which accounted for the clinical phenotype (3) a family with a balanced translocation, central adiposity and peas associated with disruption of KIBRA (4) lipoma tissue relative to adjacent healthy subcutaneous tissue, where differential gene expression profiles were identified, we also demonstrated reduced metabolic flexibility and reduced lipolysis in lipoma relative to healthy adipose tissue despite no change in adipose tissue blood flow. Conclusion: Investigating individuals with extreme phenotypes and monogenic causes of regional adiposity and IR identified key genetic and physiological factors.

Published
2011

32. T cell autoreactivity directed toward CD1c itself rather than toward carried self lipids

Author

Wun, Kwok S., Reijneveld, Josephine F., Cheng, Tan-Yun, Ladell, Kristin, Uldrich, Adam P., Le Nours, Jérôme, Miners, Kelly L., McLaren, James E., Grant, Emma J., Haigh, Oscar L., Watkins, Thomas S., Suliman, Sara, Iwany, Sarah, Jimenez, Judith, Calderon, Roger, Tamara, Kattya L., Leon, Segundo R., Murray, Megan B., Mayfield, Jacob A., Altman, John D., Purcell, Anthony W., Miles, John J., Godfrey, Dale I., Gras, Stephanie, Price, David A., Van Rhijn, Ildiko, Moody, D. Branch, and Rossjohn, Jamie

Published
2018
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33. History of tuberculosis disease is associated with genetic regulatory variation in Peruvians

Author

Suliman, Sara, primary, Nieto-Caballero, Victor E., additional, Asgari, Samira, additional, Lopez, Kattya, additional, Iwany, Sarah K., additional, Luo, Yang, additional, Nathan, Aparna, additional, Fernandez-Salinas, Daniela, additional, Chiñas, Marcos, additional, Huang, Chuan-Chin, additional, Zhang, Zibiao, additional, León, Segundo R, additional, Calderon, Roger I, additional, Lecca, Leonid, additional, Murray, Megan, additional, Van Rhijn, Ildiko, additional, Raychaudhuri, Soumya, additional, Moody, D. Branch, additional, and Gutierrez-Arcelus, Maria, additional

Published
2023
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38. A blood RNA signature for tuberculosis disease risk: a prospective cohort study

Author

Zak, Daniel E, Penn-Nicholson, Adam, Scriba, Thomas J, Thompson, Ethan, Suliman, Sara, Amon, Lynn M, Mahomed, Hassan, Erasmus, Mzwandile, Whatney, Wendy, Hussey, Gregory D, Abrahams, Deborah, Kafaar, Fazlin, Hawkridge, Tony, Verver, Suzanne, Hughes, E Jane, Ota, Martin, Sutherland, Jayne, Howe, Rawleigh, Dockrell, Hazel M, Boom, W Henry, Thiel, Bonnie, Ottenhoff, Tom H M, Mayanja-Kizza, Harriet, Crampin, Amelia C, Downing, Katrina, Hatherill, Mark, Valvo, Joe, Shankar, Smitha, Parida, Shreemanta K, Kaufmann, Stefan H E, Walzl, Gerhard, Aderem, Alan, and Hanekom, Willem A

Published
2016
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39. Newborn BCG vaccination induces robust infant IFNγ-expressing NK cell responses to mycobacteria

Author

Murphy, Melissa, primary, Suliman, Sara, additional, Briel, Libby, additional, Veldtsman, Helen, additional, Khomba, Nondumiso, additional, Africa, Hadn, additional, Steyn, Marcia, additional, Snyders, Candice I., additional, van Rensburg, Ilana C., additional, Walzl, Gerhard, additional, Chegou, Novel N., additional, Hatherill, Mark, additional, Hanekom, Willem A., additional, Scriba, Thomas J., additional, and Nemes, Elisa, additional

Published
2023
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42. First-in-human trial of the post-exposure tuberculosis vaccine H56:IC31 in Mycobacterium tuberculosis infected and non-infected healthy adults

Author

Luabeya, Angelique Kany Kany, Kagina, Benjamin M.N., Tameris, Michele D., Geldenhuys, Hennie, Hoff, Soren T., Shi, Zhongkai, Kromann, Ingrid, Hatherill, Mark, Mahomed, Hassan, Hanekom, Willem A., Andersen, Peter, Scriba, Thomas J., Schoeman, Elisma, Krohn, Colleen, Day, Cheryl L., Africa, Hadn, Makhethe, Lebohang, Smit, Erica, Brown, Yolande, Suliman, Sara, Hughes, E. Jane, Bang, Peter, Snowden, Margaret A., McClain, Bruce, and Hussey, Gregory D.

Published
2015
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43. COVID-19 vaccinology landscape in Africa

Author

Baptista, Sara, primary, Naidoo, Sanushka, additional, Suliman, Sara, additional, Nepolo, Emmanuel, additional, Kanoi, Bernard N., additional, Gitaka, Jesse, additional, Blessing, Oyedemi Mbaebie, additional, and Enany, Shymaa, additional

Published
2022
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44. An Assessment of a Rapid SARS-CoV-2 Antigen Test in Bangladesh

Author

Kawser, Zannat, primary, Hossain, Mohabbat, additional, Suliman, Sara, additional, Lockman, Shahin, additional, Gitaka, Jesse, additional, Bandawe, Gama, additional, Rahmat, Redwan, additional, Hasan, Imrul, additional, Siddik, Abu Bakar, additional, Afrad, Mokibul Hassan, additional, Rahman, Mohammed Ziaur, additional, Miller, Glenn, additional, Walt, David R., additional, Ivers, Louise C., additional, LaRocque, Regina C., additional, Harris, Jason B., additional, and Qadri, Firdausi, additional

Published
2022
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47. Metabolite changes in blood predict the onset of tuberculosis

Author

Weiner, 3rd, January, Maertzdorf, Jeroen, Sutherland, Jayne S., Duffy, Fergal J., Thompson, Ethan, Suliman, Sara, McEwen, Gayle, Thiel, Bonnie, Parida, Shreemanta K., Zyla, Joanna, Hanekom, Willem A., Mohney, Robert P., Boom, W. Henry, Mayanja-Kizza, Harriet, Howe, Rawleigh, Dockrell, Hazel M., Ottenhoff, Tom H. M., Scriba, Thomas J., Zak, Daniel E., Walzl, Gerhard, Kaufmann, Stefan H. E., and The GC6-74 consortium

Published
2018
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48. Dual TCR-a Expression on Mucosal-Associated Invariant T Cells as a Potential Confounder of TCR Interpretation

Author

Suliman, Sara, Kjer-Nielsen, Lars, Iwany, Sarah K, Lopez Tamara, Kattya, Loh, Liyen, Grzelak, Ludivine, Kedzierska, Katherine, Ocampo, Tonatiuh A, Corbett, Alexandra J, McCluskey, James, Rossjohn, Jamie, León, Segundo R, Calderon, Roger, Lecca-Garcia, Leonid, Murray, Megan B, Moody, D Branch, Van Rhijn, Ildiko, Suliman, Sara, Kjer-Nielsen, Lars, Iwany, Sarah K, Lopez Tamara, Kattya, Loh, Liyen, Grzelak, Ludivine, Kedzierska, Katherine, Ocampo, Tonatiuh A, Corbett, Alexandra J, McCluskey, James, Rossjohn, Jamie, León, Segundo R, Calderon, Roger, Lecca-Garcia, Leonid, Murray, Megan B, Moody, D Branch, and Van Rhijn, Ildiko

Abstract

Mucosal-associated invariant T (MAIT) cells are innate-like T cells that are highly abundant in human blood and tissues. Most MAIT cells have an invariant TCRa-chain that uses T cell receptor a-variable 1-2 (TRAV1-2) joined to TRAJ33/20/12 and recognizes metabolites from bacterial riboflavin synthesis bound to the Ag-presenting molecule MHC class I related (MR1). Our attempts to identify alternative MR1-presented Ags led to the discovery of rare MR1-restricted T cells with non-TRAV1-2 TCRs. Because altered Ag specificity likely alters affinity for the most potent known Ag, 5-(2-oxopropylideneamino)-6-D-ribitylaminouracil (5-OP-RU), we performed bulk TCRa- and TCRb-chain sequencing and single-cell-based paired TCR sequencing on T cells that bound the MR1-5-OP-RU tetramer with differing intensities. Bulk sequencing showed that use of V genes other than TRAV1-2 was enriched among MR1-5-OP-RU tetramerlow cells. Although we initially interpreted these as diverse MR1-restricted TCRs, single-cell TCR sequencing revealed that cells expressing atypical TCRa-chains also coexpressed an invariant MAIT TCRa-chain. Transfection of each non-TRAV1-2 TCRa-chain with the TCRb-chain from the same cell demonstrated that the non-TRAV1-2 TCR did not bind the MR1-5-OP-RU tetramer. Thus, dual TCRa-chain expression in human T cells and competition for the endogenous b-chain explains the existence of some MR1-5-OP-RU tetramerlow T cells. The discovery of simultaneous expression of canonical and noncanonical TCRs on the same T cell means that claims of roles for non-TRAV1-2 TCR in MR1 response must be validated by TCR transfer-based confirmation of Ag specificity. The Journal of Immunology, 2022, 208: 1-7.

Published
2022

49. Dual TCR-a Expression on Mucosal-Associated Invariant T Cells as a Potential Confounder of TCR Interpretation

Author

Immunologie, dI&I RA-I&I I&I, Suliman, Sara, Kjer-Nielsen, Lars, Iwany, Sarah K, Lopez Tamara, Kattya, Loh, Liyen, Grzelak, Ludivine, Kedzierska, Katherine, Ocampo, Tonatiuh A, Corbett, Alexandra J, McCluskey, James, Rossjohn, Jamie, León, Segundo R, Calderon, Roger, Lecca-Garcia, Leonid, Murray, Megan B, Moody, D Branch, Van Rhijn, Ildiko, Immunologie, dI&I RA-I&I I&I, Suliman, Sara, Kjer-Nielsen, Lars, Iwany, Sarah K, Lopez Tamara, Kattya, Loh, Liyen, Grzelak, Ludivine, Kedzierska, Katherine, Ocampo, Tonatiuh A, Corbett, Alexandra J, McCluskey, James, Rossjohn, Jamie, León, Segundo R, Calderon, Roger, Lecca-Garcia, Leonid, Murray, Megan B, Moody, D Branch, and Van Rhijn, Ildiko

Published
2022

50. Systematic Approach to Address Early Pandemic's Diagnostic Unmet Needs

Author

Cabrera, Catherine, primary, Pilobello, Kanoelani, additional, Dalvin, Steven, additional, Bobrow, Johanna, additional, Shah, Darshi, additional, Garg, Lori Freed, additional, Chalise, Sujata, additional, Doyle, Patrick, additional, Miller, Glenn A., additional, Walt, David R., additional, Suliman, Sara, additional, and Jolly, Pawan, additional

Published
2022
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