Your search keyword '"Anna K. Coussens"' showing total 72 results

1. Influence of individuals’ determinants including vaccine type on cellular and humoral responses to SARS-CoV-2 vaccination

Author

Emma S. Chambers, Weigang Cai, Giulia Vivaldi, David A. Jolliffe, Natalia Perdek, Wenhao Li, Sian E. Faustini, Joseph M. Gibbons, Corinna Pade, Alex G. Richter, Anna K. Coussens, and Adrian R. Martineau

Subjects

Immunologic diseases. Allergy, RC581-607, Neoplasms. Tumors. Oncology. Including cancer and carcinogens, RC254-282

Abstract

Abstract Vaccine development targeting SARS-CoV-2 in 2020 was of critical importance in reducing COVID-19 severity and mortality. In the U.K. during the initial roll-out most individuals either received two doses of Pfizer COVID-19 vaccine (BNT162b2) or the adenovirus-based vaccine from Oxford/AstraZeneca (ChAdOx1-nCoV-19). There are conflicting data as to the impact of age, sex and body habitus on cellular and humoral responses to vaccination, and most studies in this area have focused on determinants of mRNA vaccine immunogenicity. Here, we studied a cohort of participants in a population-based longitudinal study (COVIDENCE UK) to determine the influence of age, sex, body mass index (BMI) and pre-vaccination anti-Spike (anti-S) antibody status on vaccine-induced humoral and cellular immune responses to two doses of BNT162b2 or ChAdOx-n-CoV-19 vaccination. Younger age and pre-vaccination anti-S seropositivity were both associated with stronger antibody responses to vaccination. BNT162b2 generated higher neutralising and anti-S antibody titres to vaccination than ChAdOx1-nCoV-19, but cellular responses to the two vaccines were no different. Irrespective of vaccine type, increasing age was also associated with decreased frequency of cytokine double-positive CD4+T cells. Increasing BMI was associated with reduced frequency of SARS-CoV-2-specific TNF+CD8% T cells for both vaccines. Together, our findings demonstrate that increasing age and BMI are associated with attenuated cellular and humoral responses to SARS-CoV-2 vaccination. Whilst both vaccines induced T cell responses, BNT162b2 induced significantly elevated humoral immune response as compared to ChAdOx-n-CoV-19.

Published

2024

2. Overlooked, dismissed, and downplayed: reversion of Mycobacterium tuberculosis immunoreactivity

Author

Katie D. Dale, Alvaro Schwalb, Anna K. Coussens, Katherine B. Gibney, Alison J. Abboud, Krista Watts, and Justin T. Denholm

Subjects

Diseases of the respiratory system, RC705-779

Abstract

Tuberculosis (TB) is caused by Mycobacterium tuberculosis (Mtb). Following infection, immune responses to Mtb antigens can be measured using the tuberculin skin test or an interferon-γ release assay. The gain of Mtb immunoreactivity, a change from a negative to a positive tuberculin skin test or interferon-γ release assay result, is called conversion and has long been used as a measure of Mtb exposure. However, the loss of immunoreactivity (reversion; a positive followed by a negative result) has often been overlooked. Instead, in clinical and epidemiological circles, Mtb immunoreactivity is commonly considered to persist lifelong and confer a lifetime of disease risk. We present a critical review, describing the evidence for reversion from cohort studies, ecological studies and studies of TB progression risk. We outline the inconsistent reasons why reversion has been dismissed from common understanding and present evidence demonstrating that, just as conversion predominantly indicates prior exposure to Mtb antigens, so its opposite, reversion, suggests the reduction or absence of exposure (endogenous or exogenous). Mtb immunoreactivity is dynamic in both individuals and populations and this is why it is useful for stratifying short-term TB progression risk. The neglect of reversion has shaped TB research and policy at all levels, influencing clinical management and skewing Mtb infection risk estimation and transmission modelling, leading to an underestimation of the contribution of re-exposure to the burden of TB, a serious oversight for an infectious disease. More than a century after it was first demonstrated, it is time to incorporate reversion into our understanding of the natural history of TB.

Published

2024

3. Vitamin D supplementation to prevent tuberculosis infection in South African schoolchildren: multicenter phase 3 double-blind randomized placebo-controlled trial (ViDiKids)

Author

Keren Middelkoop, Justine Stewart, Neil Walker, Carmen Delport, David A. Jolliffe, Anna K. Coussens, James Nuttall, Jonathan C.Y. Tang, William D. Fraser, Christopher J. Griffiths, Geeta Trilok Kumar, Suzanne Filteau, Richard L. Hooper, Robert J. Wilkinson, Linda-Gail Bekker, and Adrian R. Martineau

Subjects

Vitamin D, Tuberculosis, Randomized controlled trial, Interferon-gamma release assay, Infectious and parasitic diseases, RC109-216

Abstract

ABSTRACT: Objectives: To determine whether weekly oral supplementation with 10,000 IU vitamin D3 for 3 years reduces the risk of sensitization to M. tuberculosis in South African schoolchildren aged 6-11 years with negative QuantiFERON-tuberculosis (TB) Gold Plus (QFT-Plus) assay results at baseline. Methods: We conducted a phase 3 randomized placebo-controlled trial in 1682 children attending 23 primary schools in Cape Town. The primary outcome was a positive end-trial QFT-Plus result, analyzed using a mixed effects logistic regression model with the school of attendance included as a random effect. Results: 829 vs. 853 QFT-Plus-negative children were randomized to receive vitamin D3 vs. placebo, respectively. Mean end-study 25(OH)D concentrations in participants randomized to vitamin D vs. placebo were 104.3 vs 64.7 nmol/l, respectively (95% confidence interval for difference, 37.6 to 41.9 nmol/l). A total of 76/667 (11.4%) participants allocated to vitamin D vs. 89/687 (13.0%) participants allocated to placebo tested QFT-Plus positive at 3-year follow-up (adjusted odds ratio 0.86, 95% confidence interval 0.62-1.19, P = 0.35). Conclusion: Weekly oral supplementation with 10,000 IU vitamin D3 for 3 years elevated serum 25(OH)D concentrations among QFT-Plus-negative Cape Town schoolchildren but did not reduce their risk of QFT-Plus conversion.

Published

2023

4. Quantifying spatial dynamics of Mycobacterium tuberculosis infection of human macrophages using microfabricated patterns

Author

Anca F. Savulescu, Nashied Peton, Delia Oosthuizen, Rudranil Hazra, Robert P. Rousseau, Musa M. Mhlanga, and Anna K. Coussens

Subjects

CP: Cell biology, CP: Microbiology, Biotechnology, TP248.13-248.65, Biochemistry, QD415-436, Science

Abstract

Summary: Macrophages provide a first line of defense against invading pathogens, including the leading cause of bacterial mortality, Mycobacterium tuberculosis (Mtb). A challenge for quantitative characterization of host-pathogen processes in differentially polarized primary human monocyte-derived macrophages (MDMs) is their heterogeneous morphology. Here, we describe the use of microfabricated patterns that constrain the size and shape of cells, mimicking the physiological spatial confinement cells experience in tissues, to quantitatively characterize interactions during and after phagocytosis at the single-cell level at high resolution. Comparing pro-inflammatory (M1) and anti-inflammatory (M2) MDMs, we find interferon-γ stimulation increases the phagocytic contraction, while contraction and bacterial uptake decrease following silencing of phagocytosis regulator NHLRC2 or bacterial surface lipid removal. We identify host organelle position alterations within infected MDMs and differences in Mtb subcellular localization in line with M1 and M2 cellular polarity. Our approach can be adapted to study other host-pathogen interactions and coupled with downstream automated analytical approaches. Motivation: Mycobacterium tuberculosis (Mtb) manipulates a plethora of macrophage responses to survive within its intracellular niche. Limited knowledge exists regarding the events that occur during phagocytosis and if/how Mtb manipulates the spatial organization of its new home. The morphological heterogeneity of differentially polarized primary human monocyte-derived macrophages (hMDMs) presents a hurdle for quantitative analysis of these earliest host-pathogen interactions. This study introduces a micropatterning, image-based approach to reduce this heterogeneity, instilling uniform cell morphology and organelle positioning. This toolbox facilitates high-resolution, image-based, quantitative investigations of previously under-studied early interactions between Mtb and differentially derived hMDMs at a single-cell level.

Published

2023

5. Immune interaction between SARS-CoV-2 and Mycobacterium tuberculosis

Author

Petro Booysen, Katalin A. Wilkinson, Dylan Sheerin, Robyn Waters, Anna K. Coussens, and Robert J. Wilkinson

Subjects

COVID-19, latent TB, LTBI, Bacille Calmette Guérin, co-infection, immune response, Immunologic diseases. Allergy, RC581-607

Abstract

SARS-CoV-2 and Mycobacterium tuberculosis (Mtb) are major infectious causes of death, with meta-analyses and population-based studies finding increased mortality in co-infected patients simultaneously diagnosed with COVID-19 and tuberculosis (TB). There is a need to understand the immune interaction between SARS-CoV-2 and Mtb which impacts poor outcomes for those co-infected. We performed a PubMed and preprint search using keywords [SARS-CoV-2] AND [tuberculosis] AND [Immune response], including publications after January 2020, excluding reviews or opinions. Abstracts were evaluated by authors for inclusion of data specifically investigating the innate and/or acquired immune responses to SARS-CoV-2 and Mtb in humans and animal models, immunopathological responses in co-infection and both trials and investigations of potential protection against SARS-CoV-2 by Bacille Calmette Guérin (BCG). Of the 248 articles identified, 39 were included. Incidence of co-infection is discussed, considering in areas with a high burden of TB, where reported co-infection is likely underestimated. We evaluated evidence of the clinical association between COVID-19 and TB, discuss differences and similarities in immune responses in humans and in murine studies, and the implications of co-infection. SARS-CoV-2 and Mtb have both been shown to modulate immune responses, particularly of monocytes, macrophages, neutrophils, and T cells. Co-infection may result in impaired immunity to SARS-CoV-2, with an exacerbated inflammatory response, while T cell responses to Mtb may be modulated by SARS-CoV-2. Furthermore, there has been no proven potential COVID-19 clinical benefit of BCG despite numerous large-scale clinical trials.

Published

2023

6. Identification and control for the effects of bioinformatic globin depletion on human RNA-seq differential expression analysis

Author

Dylan Sheerin, Francisco Lakay, Hanif Esmail, Craig Kinnear, Bianca Sansom, Brigitte Glanzmann, Robert J. Wilkinson, Matthew E. Ritchie, and Anna K. Coussens

Subjects

Medicine, Science

Abstract

Abstract When profiling blood samples by RNA-sequencing (RNA-seq), RNA from haemoglobin (Hgb) can account for up to 70% of the transcriptome. Due to considerations of sequencing depth and power to detect biological variation, Hgb RNA is typically depleted prior to sequencing by hybridisation-based methods; an alternative approach is to deplete reads arising from Hgb RNA bioinformatically. In the present study, we compared the impact of these two approaches on the outcome of differential gene expression analysis performed using RNA-seq data from 58 human tuberculosis (TB) patient or contact whole blood samples–29 globin kit-depleted and 29 matched non-depleted—a subset of which were taken at TB diagnosis and at six months post-TB treatment from the same patient. Bioinformatic depletion of Hgb genes from the non-depleted samples (bioinformatic-depleted) substantially reduced library sizes (median = 57.24%) and fewer long non-coding, micro, small nuclear and small nucleolar RNAs were captured in these libraries. Profiling published TB gene signatures across all samples revealed inferior correlation between kit-depleted and bioinformatic-depleted pairs when the proportion of reads mapping to Hgb genes was higher in the non-depleted sample, particularly at the TB diagnosis time point. A set of putative “globin-fingerprint” genes were identified by directly comparing kit-depleted and bioinformatic-depleted samples at each timepoint. Two TB treatment response signatures were also shown to have decreased differential performance when comparing samples at TB diagnosis to six months post-TB treatment when profiled on the bioinformatic-depleted samples compared with their kit-depleted counterparts. These results demonstrate that failure to deplete Hgb RNA prior to sequencing has a negative impact on the sensitivity to detect disease-relevant gene expression changes even when bioinformatic removal is performed.

Published

2023

7. Effects of tuberculosis and/or HIV-1 infection on COVID-19 presentation and immune response in Africa

Author

Elsa du Bruyn, Cari Stek, Remi Daroowala, Qonita Said-Hartley, Marvin Hsiao, Georgia Schafer, Rene T. Goliath, Fatima Abrahams, Amanda Jackson, Sean Wasserman, Brian W. Allwood, Angharad G. Davis, Rachel P.-J. Lai, Anna K. Coussens, Katalin A. Wilkinson, Jantina de Vries, Nicki Tiffin, Maddalena Cerrone, Ntobeko A. B. Ntusi, HIATUS consortium, Catherine Riou, and Robert J. Wilkinson

Subjects

Science

Abstract

Here the authors describe outcomes of SARS-CoV-2 infection in an African setting of high HIV-1 and tuberculosis prevalence. They find that tuberculosis is a common co-morbidity in patients admitted to hospital with COVID-19 and that the immune response to SARS-CoV-2 is adversely affected by co-existent HIV-1 and tuberculosis.

Published

2023

8. Risk surveillance and mitigation: autoantibodies as triggers and inhibitors of severe reactions to SARS-CoV-2 infection

Author

Catherine Chen, Aisah Amelia, George W. Ashdown, Ivo Mueller, Anna K. Coussens, and Emily M. Eriksson

Subjects

Autoantibodies, SARS-CoV-2, COVID-19, Autoimmunity, Therapeutics. Pharmacology, RM1-950, Biochemistry, QD415-436

Abstract

Abstract COVID-19 clinical presentation differs considerably between individuals, ranging from asymptomatic, mild/moderate and severe disease which in some cases are fatal or result in long-term effects. Identifying immune mechanisms behind severe disease development informs screening strategies to predict who are at greater risk of developing life-threatening complications. However, to date clear prognostic indicators of individual risk of severe or long COVID remain elusive. Autoantibodies recognize a range of self-antigens and upon antigen recognition and binding, important processes involved in inflammation, pathogen defence and coagulation are modified. Recent studies report a significantly higher prevalence of autoantibodies that target immunomodulatory proteins including cytokines, chemokines, complement components, and cell surface proteins in COVID-19 patients experiencing severe disease compared to those who experience mild or asymptomatic infections. Here we discuss the diverse impacts of autoantibodies on immune processes and associations with severe COVID-19 disease.

Published

2021

9. Mitigating losses: how scientific organisations can help address the impact of the COVID-19 pandemic on early-career researchers

Author

Sandra López-Vergès, Bernardo Urbani, David Fernández Rivas, Sandeep Kaur-Ghumaan, Anna K. Coussens, Felix Moronta-Barrios, Suraj Bhattarai, Leila Niamir, Velia Siciliano, Andreea Molnar, Amanda Weltman, Meghnath Dhimal, Shalini S. Arya, Karen J. Cloete, Almas Taj Awan, Stefan Kohler, Chandra Shekhar Sharma, Clarissa Rios Rojas, Yoko Shimpuku, John Ganle, Maryam M. Matin, Justine G. Nzweundji, Abdeslam Badre, and Paulina Carmona-Mora

Subjects

History of scholarship and learning. The humanities, AZ20-999, Social Sciences

Abstract

Scientific collaborations among nations to address common problems and to build international partnerships as part of science diplomacy is a well-established notion. The international flow of people and ideas has played an important role in the advancement of the ‘Sciences’ and the current pandemic scenario has drawn attention towards the genuine need for a stronger role of science diplomacy, science advice and science communication. In dealing with the COVID-19 pandemic, visible interactions across science, policy, science communication to the public and diplomacy worldwide have promptly emerged. These interactions have benefited primarily the disciplines of knowledge that are directly informing the pandemic response, while other scientific fields have been relegated. The effects of the COVID-19 pandemic on scientists of all disciplines and from all world regions are discussed here, with a focus on early-career researchers (ECRs), as a vulnerable population in the research system. Young academies and ECR-driven organisations could suggest ECR-powered solutions and actions that could have the potential to mitigate these effects on ECRs working on disciplines not related to the pandemic response. In relation with governments and other scientific organisations, they can have an impact on strengthening and creating fairer scientific systems for ECRs at the national, regional, and global level.

Published

2021

10. Vitamin D Supplementation Does Not Influence SARS-CoV-2 Vaccine Efficacy or Immunogenicity: Sub-Studies Nested within the CORONAVIT Randomised Controlled Trial

Author

David A. Jolliffe, Giulia Vivaldi, Emma S. Chambers, Weigang Cai, Wenhao Li, Sian E. Faustini, Joseph M. Gibbons, Corinna Pade, Anna K. Coussens, Alex G. Richter, Áine McKnight, and Adrian R. Martineau

Subjects

vitamin D, ChAdOx1 nCoV-19 Oxford–AstraZeneca, BNT162b2 Pfizer, breakthrough SARS-CoV-2 infection, randomised controlled trial, antibody, Nutrition. Foods and food supply, TX341-641

Abstract

Vitamin D deficiency has been reported to associate with the impaired development of antigen-specific responses following vaccination. We aimed to determine whether vitamin D supplements might boost the immunogenicity and efficacy of SARS-CoV-2 vaccination by conducting three sub-studies nested within the CORONAVIT randomised controlled trial, which investigated the effects of offering vitamin D supplements at a dose of 800 IU/day or 3200 IU/day vs. no offer on risk of acute respiratory infections in UK adults with circulating 25-hydroxyvitamin D concentrations n = 2808) investigated the effects of vitamin D supplementation on the risk of breakthrough SARS-CoV-2 infection following two doses of SARS-CoV-2 vaccine. Sub-study 2 (n = 1853) investigated the effects of vitamin D supplementation on titres of combined IgG, IgA and IgM (IgGAM) anti-Spike antibodies in eluates of dried blood spots collected after SARS-CoV-2 vaccination. Sub-study 3 (n = 100) investigated the effects of vitamin D supplementation on neutralising antibody and cellular responses in venous blood samples collected after SARS-CoV-2 vaccination. In total, 1945/2808 (69.3%) sub-study 1 participants received two doses of ChAdOx1 nCoV-19 (Oxford–AstraZeneca); the remainder received two doses of BNT162b2 (Pfizer). Mean follow-up 25(OH)D concentrations were significantly elevated in the 800 IU/day vs. no-offer group (82.5 vs. 53.6 nmol/L; mean difference 28.8 nmol/L, 95% CI 22.8–34.8) and in the 3200 IU/day vs. no offer group (105.4 vs. 53.6 nmol/L; mean difference 51.7 nmol/L, 45.1–58.4). Vitamin D supplementation did not influence the risk of breakthrough SARS-CoV-2 infection in vaccinated participants (800 IU/day vs. no offer: adjusted hazard ratio 1.28, 95% CI 0.89 to 1.84; 3200 IU/day vs. no offer: 1.17, 0.81 to 1.70). Neither did it influence IgGAM anti-Spike titres, neutralising antibody titres or IFN-γ concentrations in the supernatants of S peptide-stimulated whole blood. In conclusion, vitamin D replacement at a dose of 800 or 3200 IU/day effectively elevated 25(OH)D concentrations, but it did not influence the protective efficacy or immunogenicity of SARS-CoV-2 vaccination when given to adults who had a sub-optimal vitamin D status at baseline.

Published

2022

11. Prevalence and Determinants of Vitamin D Deficiency in 1825 Cape Town Primary Schoolchildren: A Cross-Sectional Study

Author

Keren Middelkoop, Neil Walker, Justine Stewart, Carmen Delport, David A. Jolliffe, James Nuttall, Anna K. Coussens, Celeste E. Naude, Jonathan C. Y. Tang, William D. Fraser, Robert J. Wilkinson, Linda-Gail Bekker, and Adrian R. Martineau

Subjects

vitamin D, prevalence, South Africa, children, cross-sectional, Nutrition. Foods and food supply, TX341-641

Abstract

Vitamin D deficiency (25-hydroxyvitamin D[25(OH)D] p < 0.001). However, no association between participants with hyperparathyroidism (PTH >6.9 pmol/L) and vitamin D deficiency was seen (p = 0.42). In conclusion, we report that season is the major determinant of vitamin D status among Cape Town primary schoolchildren, with prevalence of vitamin D deficiency ranging from 1.4% in January–March to 22.8% in July–September.

Published

2022

12. Correction: Mitigating losses: how scientific organisations can help address the impact of the COVID-19 pandemic on early-career researchers

Author

Sandra López-Vergès, Bernardo Urbani, David Fernández Rivas, Sandeep Kaur-Ghumaan, Anna K. Coussens, Felix Moronta-Barrios, Suraj Bhattarai, Leila Niamir, Velia Siciliano, Andreea Molnar, Amanda Weltman, Meghnath Dhimal, Shalini S. Arya, Karen J. Cloete, Almas Taj Awan, Stefan Kohler, Chandra Shekhar Sharma, Clarissa Rios Rojas, Yoko Shimpuku, John Ganle, Maryam M. Matin, Justine G. Nzweundji, Abdeslam Badre, and Paulina Carmona-Mora

Subjects

History of scholarship and learning. The humanities, AZ20-999, Social Sciences

Published

2021

13. The Wonder Years: What Can Primary School Children Teach Us About Immunity to Mycobacterium tuberculosis?

Author

James A. Seddon, Silvia S. Chiang, Hanif Esmail, and Anna K. Coussens

Subjects

tuberculosis, children, adolescence, Mycobacterium tuberculosis, vaccination, infection, Immunologic diseases. Allergy, RC581-607

Abstract

In high burden settings, the risk of infection with Mycobacterium tuberculosis increases throughout childhood due to cumulative exposure. However, the risk of progressing from tuberculosis (TB) infection to disease varies by age. Young children (

Published

2018

14. Generation of Liposomes to Study the Effect of Mycobacterium Tuberculosis Lipids on HIV-1 cis- and trans-Infections

Author

Marion Pouget, Anna K. Coussens, Alessandra Ruggiero, Anastasia Koch, Jordan Thomas, Gurdyal S. Besra, Robert J. Wilkinson, Apoorva Bhatt, Georgios Pollakis, and William A. Paxton

Subjects

HIV-1, TB, Mycobacterium tuberculosis, in vitro, DC-SIGN, liposomes, Biology (General), QH301-705.5, Chemistry, QD1-999

Abstract

Tuberculosis (TB) is the leading cause of death among HIV-1-infected individuals and Mycobacterium tuberculosis (Mtb) co-infection is an early precipitate to AIDS. We aimed to determine whether Mtb strains differentially modulate cellular susceptibility to HIV-1 infection (cis- and trans-infection), via surface receptor interaction by their cell envelope lipids. Total lipids from pathogenic (lineage 4 Mtb H37Rv, CDC1551 and lineage 2 Mtb HN878, EU127) and non-pathogenic (Mycobacterium bovis BCG and Mycobacterium smegmatis) Mycobacterium strains were integrated into liposomes mimicking the lipid distribution and antigen accessibility of the mycobacterial cell wall. The resulting liposomes were tested for modulating in vitro HIV-1 cis- and trans-infection of TZM-bl cells using single-cycle infectious virus particles. Mtb glycolipids did not affect HIV-1 direct infection however, trans-infection of both R5 and X4 tropic HIV-1 strains were impaired in the presence of glycolipids from M. bovis, Mtb H37Rv and Mtb EU127 strains when using Raji-DC-SIGN cells or immature and mature dendritic cells (DCs) to capture virus. SL1, PDIM and TDM lipids were identified to be involved in DC-SIGN recognition and impairment of HIV-1 trans-infection. These findings indicate that variant strains of Mtb have differential effect on HIV-1 trans-infection with the potential to influence HIV-1 disease course in co-infected individuals.

Published

2021

15. Neutrophils: Innate Effectors of TB Resistance?

Author

Elouise E. Kroon, Anna K. Coussens, Craig Kinnear, Marianna Orlova, Marlo Möller, Allison Seeger, Robert J. Wilkinson, Eileen G. Hoal, and Erwin Schurr

Subjects

Mycobacterium, tuberculosis, inflammation, NETs, antimicrobial, protection, Immunologic diseases. Allergy, RC581-607

Abstract

Certain individuals are able to resist Mycobacterium tuberculosis infection despite persistent and intense exposure. These persons do not exhibit adaptive immune priming as measured by tuberculin skin test (TST) and interferon-γ (IFN-γ) release assay (IGRA) responses, nor do they develop active tuberculosis (TB). Genetic investigation of individuals who are able to resist M. tuberculosis infection shows there are likely a combination of genetic variants that contribute to the phenotype. The contribution of the innate immune system and the exact cells involved in this phenotype remain incompletely elucidated. Neutrophils are prominent candidates for possible involvement as primers for microbial clearance. Significant variability is observed in neutrophil gene expression and DNA methylation. Furthermore, inter-individual variability is seen between the mycobactericidal capacities of donor neutrophils. Clearance of M. tuberculosis infection is favored by the mycobactericidal activity of neutrophils, apoptosis, effective clearance of cells by macrophages, and resolution of inflammation. In this review we will discuss the different mechanisms neutrophils utilize to clear M. tuberculosis infection. We discuss the duality between neutrophils' ability to clear infection and how increasing numbers of neutrophils contribute to active TB severity and mortality. Further investigation into the potential role of neutrophils in innate immune-mediated M. tuberculosis infection resistance is warranted since it may reveal clinically important activities for prevention as well as vaccine and treatment development.

Published

2018

16. Viral Apoptosis Evasion via the MAPK Pathway by Use of a Host Long Noncoding RNA

Author

Samantha Barichievy, Jerolen Naidoo, Mikaël Boullé, Janine Scholefield, Suraj P. Parihar, Anna K. Coussens, Frank Brombacher, Alex Sigal, and Musa M. Mhlanga

Subjects

lincRNA-p21, HuR, hnRNP-K, apoptosis, MAP2K1, ERK2, Microbiology, QR1-502

Abstract

An emerging realization of infectious disease is that pathogens can cause a high incidence of genetic instability within the host as a result of infection-induced DNA lesions. These often lead to classical hallmarks of cancer, one of which is the ability to evade apoptosis despite the presence of numerous genetic mutations that should be otherwise lethal. The Human Immunodeficiency Virus type 1 (HIV-1) is one such pathogen as it induces apoptosis in CD4+ T cells but is largely non-cytopathic in macrophages. As a consequence there is long-term dissemination of the pathogen specifically by these infected yet surviving host cells. Apoptosis is triggered by double-strand breaks (DSBs), such as those induced by integrating retroviruses like HIV-1, and is coordinated by the p53-regulated long noncoding RNA lincRNA-p21. As is typical for a long noncoding RNA, lincRNA-p21 mediates its activities in a complex with one of its two protein binding partners, namely HuR and hnRNP-K. In this work, we monitor the cellular response to infection to determine how HIV-1 induces DSBs in macrophages yet evades apoptosis in these cells. We show that the virus does so by securing the pro-survival MAP2K1/ERK2 cascade early upon entry, in a gp120-dependent manner, to orchestrate a complex dysregulation of lincRNA-p21. By sequestering the lincRNA-p21 partner HuR in the nucleus, HIV-1 enables lincRNA-p21 degradation. Simultaneously, the virus permits transcription of pro-survival genes by sequestering lincRNA-p21's other protein partner hnRNP-K in the cytoplasm via the MAP2K1/ERK2 pathway. Of particular note, this MAP2K1/ERK2 pro-survival cascade is switched off during T cell maturation and is thus unavailable for similar viral manipulation in mature CD4+ T cells. We show that the introduction of MAP2K1, ERK2, or HDM2 inhibitors in HIV-infected macrophages results in apoptosis, providing strong evidence that the viral-mediated apoptotic block can be released, specifically by restoring the nuclear interaction of lincRNA-p21 and its apoptosis protein partner hnRNP-K. Together, these results reveal a unique example of pathogenic control over mammalian apoptosis and DNA damage via a host long noncoding RNA, and present MAP2K1/ERK2 inhibitors as a novel therapeutic intervention strategy for HIV-1 infection in macrophages.

Published

2018

17. Socio-political prescriptions for latent tuberculosis infection are required to prevent reactivation of tuberculosis

Author

Anna K. Coussens

Subjects

Infectious and parasitic diseases, RC109-216

Published

2017

18. Anti-Inflammatory and Antimicrobial Actions of Vitamin D in Combating TB/HIV

Author

Anna K. Coussens, Adrian R. Martineau, and Robert J. Wilkinson

Subjects

Medicine, Science

Abstract

Tuberculosis (TB) disease activation is now believed to arise due to a lack of inflammatory homeostatic control at either end of the spectrum of inflammation: either due to immunosuppression (decreased antimicrobial activity) or due to immune activation (excess/aberrant inflammation). Vitamin D metabolites can increase antimicrobial activity in innate immune cells, which, in the context of HIV-1 coinfection, have insufficient T cell-mediated help to combat Mycobacterium tuberculosis (MTB) infection. Moreover, maintaining vitamin D sufficiency prior to MTB infection enhances the innate antimicrobial response to T cell-mediated interferon-γ. Conversely, vitamin D can act to inhibit expression and secretion of a broad range of inflammatory mediators and matrix degrading enzymes driving immunopathology during active TB and antiretroviral- (ARV-) mediated immune reconstitution inflammatory syndrome (IRIS). Adjunct vitamin D therapy during treatment of active TB may therefore reduce lung pathology and TB morbidity, accelerate resolution of cavitation and thereby decrease the chance of transmission, improve lung function following therapy, prevent relapse, and prevent IRIS in those initiating ARVs. Future clinical trials of vitamin D for TB prevention and treatment must be designed to detect the most appropriate primary endpoint, which in some cases should be anti-inflammatory and not antimicrobial.

Published

2014

19. Cohort Profile: A longitudinal Victorian COVID-19 cohort (COVID PROFILE)

Author

Emily M. Eriksson, Anne Hart, Maureen Forde, Siavash Foroughi, Nicholas Kiernan-Walker, Ramin Mazhari, Erin C. Lucas, Mai Margetts, Anthony Farchione, Dylan Sheerin, George Ashdown, Rachel Evans, Catherine Chen, Shazia Ruybal-Pesántez, Eamon Conway, Marilou H. Barrios, Jasper Cornish, Maria Edmonds, Lee M. Henneken, Lisa J. Ioannidis, Sam W. Z. Olechnowicz, Ryan B. Munnings, Joanna R. Groom, Diana S. Hansen, Rory Bowden, Anna K. Coussens, Jason A. Tye-Din, Vanessa L. Bryant, and Ivo Mueller

Abstract

PurposeThe COVID PROFILE cohort is a longitudinal clinical study based in Victoria Australia, which was established to understand immunity to SARS-CoV-2 in alow transmission population settingand to identify immunological markers of long-term immunity and immune-dysregulation after both infection and vaccination. Additionally, this cohort was established as a biobank resource for researchers to address other health-related immunological questions.ParticipantsWe enrolled 178 adult community members, including household contacts, who had either recovered from a SARS-CoV-2 infection or were SARS-CoV-2 naïve. Only participants ≥18 years of age and, in the case of female participants, non-pregnant women at the time of enrollment were included in the study. Detailed COVID-19 clinical data, vaccination status, medical history and demographics was collected.Findings to dateAt enrollment, we found that 87.8% of COVID-19 recovered individuals were seropositive with detectable levels of anti-SARS-CoV-2 IgG antibodies. Seronegative COVID-19 recovered individuals included asymptomatic individuals or participants that were enrolled more than 12 months after their COVID-19 diagnosis. Except for one individual who was seropositive at baseline despite a previous SARS-CoV-2 PCR negative diagnosis, all household contacts and other community members enrolled as SARS-CoV-2 PCR negative, were seronegative for all SARS-CoV-2-specific antibodies tested. The infection rate (re-infection or new infection) during 24 months of the study was 42.7%, as determined by either rapid antigen tests, PCRs or serology screens. Of the SARS-CoV-2 recovered participants, 32.6% reported ongoing symptoms at enrollment of which 47% had already experienced ongoing symptoms for more than 12 weeks.Future PlansCOVID PROFILE will be used to comprehensively understand temporal immunity to SARS-CoV-2 and COVID-19 vaccines and to understand the impact of host immunological composition on such immunity and symptom severity. Additionally, studies focusing on understanding immunity following breakthrough infections and immunological risk factors that contribute towards development of long COVID are planned.Limitations/Strengths of the studyExtensive clinical information is available and longitudinal samples (blood, saliva and oropharyngeal swabs) collected at regular intervals up to 2.5 years after initial enrolment.This low SARS-CoV-2 transmission population cohort, enables exploration of difference in both the acquisition and maintenance of naturally acquired and vaccine-induced immunity not confounded by prior, frequent and/or undetected exposures.Extensive biobank of numerous blood fractions and biospecimen enables further exploration of mucosal immunity, nasal microbiome and humoral and cellular immunity over time.The cohort may be limited in addressing research questions regarding outcomes and risk factors and their associations where low incidence is expected.

Published

2023

20. Quantifying spatial dynamics and regulators ofMycobacterium tuberculosisphagocytosis by primary human macrophages using microfabricated patterns

Author

Anca F. Savulescu, Nashied Peton, Delia Oosthuizen, Rudranil Hazra, Musa. M. Mhlanga, and Anna K. Coussens

Abstract

Macrophages provide a first line of defense against invading pathogens, including the leading cause of bacterial mortality,Mycobacterium tuberculosis(Mtb). Phagocytosing extracellular organisms mediate pathogen clearanceviaa multitude of antimicrobial mechanisms, uniquely designed against an array of pathogens. Macrophages are able to execute different programs of activation in response to pathogenic challenge with host mediators, polarizing them to a variety of differentiation states, including the pro-inflammatory M1 and anti-inflammatory M2 states. The functional polarization of a macrophage prior to infection, thus impacts the outcome of host-pathogen interaction. One of the limitations when usingin vitrodifferentiated human primary monocyte-derived macrophages (MDMs) is the heterogeneous nature of the mature population, which presents a challenge for quantitative characterization of various host-pathogen processes. Here, we describe an approach to minimize this heterogeneity, based on micropatterning of cells to reintroduce aspects of cellular homogeneity lost in a 2D tissue culture. Micropatterning consists of growing cells at the single cell level on microfabricated patterns, to constrain the size and shape of the cell, reducing cell-to-cell variation and mimicking the physiological spatial confinement that cells experience in tissues. We infected micropatterned GM-CSF- (M1) and M-CSF- (M2) derived human MDMs withMtb, which allowed us to study host-pathogen interactions at a single cell level, at high resolution and in a quantitative manner, across tens to hundreds of cells in parallel. Using our approach, we were able to quantify phagocytosis ofMtbin MDMs, finding phagocytic contraction is increased by interferon-gamma stimulation, whilst contraction and bacterial uptake is decreased following silencing of phagocytosis regulatorNHLRC2or Tween80 removal of bacterial surface lipids. We also identify alterations in host organelle position withinMtbinfected MDMs, as well as identifying differences inMtbsubcellular localization in relation to the microtubule organizing center (MTOC) and in line with the cellular polarity in M1 and M2 MDMs. Our approach described here can be adapted to study other host-pathogen interactions and co-infections in MDMs and can be coupled with downstream automated analytical approaches.

Published

2022

21. Timing ofMycobacterium tuberculosisexposure explains variation in BCG effectiveness: a systematic review and meta-analysis

Author

Anna K. Coussens, Manjula Datta, Andrew Kawai, James M. Trauer, Bridget Williams, Emma S. McBryde, and Romain Ragonnet

Subjects

Pulmonary and Respiratory Medicine, Pediatrics, medicine.medical_specialty, Tuberculosis, Context (language use), Mycobacterium tuberculosis, 03 medical and health sciences, 0302 clinical medicine, respiratory infection, Epidemiology, Humans, Medicine, 030212 general & internal medicine, Child, 030304 developmental biology, 0303 health sciences, biology, business.industry, Vaccination, Infant, Newborn, Respiratory infection, clinical epidemiology, biology.organism_classification, medicine.disease, Systematic review, Meta-analysis, BCG Vaccine, business

Abstract

RationaleThe heterogeneity in efficacy observed in studies of BCG vaccination is not fully explained by currently accepted hypotheses, such as latitudinal gradient in non-tuberculous mycobacteria exposure.MethodsWe updated previous systematic reviews of the effectiveness of BCG vaccination to 31 December 2020. We employed an identical search strategy and inclusion/exclusion criteria to these earlier reviews, but reclassified several studies, developed an alternative classification system and considered study demography, diagnostic approach and tuberculosis (TB)-related epidemiological context.Main resultsOf 21 included trials, those recruiting neonates and children aged under 5 were consistent in demonstrating considerable protection against TB for several years. Trials in high-burden settings with shorter follow-up also showed considerable protection, as did most trials in settings of declining burden with longer follow-up. However, the few trials performed in high-burden settings with longer follow-up showed no protection, sometimes with higher case rates in the vaccinated than the controls in the later follow-up period.ConclusionsThe most plausible explanatory hypothesis for these results is that BCG protects against TB that results from exposure shortly after vaccination. However, we found no evidence of protection when exposure occurs later from vaccination, which would be of greater importance in trials in high-burden settings with longer follow-up. In settings of declining burden, most exposure occurs shortly following vaccination and the sustained protection observed for many years thereafter represents continued protection against this early exposure. By contrast, in settings of continued intense transmission, initial protection subsequently declines with repeated exposure toMycobacterium tuberculosisor other pathogens.

Published

2021

22. Tuberculosis prevalence: beyond the tip of the iceberg

Author

Rein M G J Houben, Hanif Esmail, Frank Cobelens, Caroline M L Williams, Anna K Coussens, Global Health, AII - Infectious diseases, APH - Methodology, APH - Quality of Care, and APH - Global Health

Subjects

Pulmonary and Respiratory Medicine, Humans, Tuberculosis

Published

2022

23. Mind the gap - Managing tuberculosis across the disease spectrum

Author

Hanif Esmail, Liana Macpherson, Anna K. Coussens, and Rein M.G.J. Houben

Subjects

Antitubercular Agents, Humans, Tuberculosis, General Medicine, Tuberculosis, Pulmonary, General Biochemistry, Genetics and Molecular Biology

Abstract

We currently have a binomial approach to managing tuberculosis. Those with active disease, ideally confirmed microbiologically, are treated with a standard 6-month, multi-drug regimen and those with latent infection and no evidence of disease with shorter, one or two drug regimens. Clinicians frequently encounter patients that fall between these two management pathways with some but not all features of disease and this will occur more often with the increasing emphasis on chest X-ray-based systematic screening. The view of tuberculosis as a spectrum of disease states is being increasingly recognised and is leading to new diagnostic approaches for early disease. However, the 6-month regimen for treating disease was driven by the duration required to treat the most extensive forms of pulmonary TB and shorter durations appear sufficient for less extensive disease. It is time undertake clinical trials to better define the optimal treatment for tuberculosis across the disease spectrum.

Published

2022

24. Mitigating losses: how scientific organisations can help address the impact of the COVID-19 pandemic on early-career researchers

Author

Felix Moronta-Barrios, Suraj Bhattarai, Justine G. Nzweundji, Clarissa Rios Rojas, Meghnath Dhimal, Amanda Weltman, Andreea Molnar, Sandra López-Vergès, Bernardo Urbani, Leila Niamir, Abdeslam Badre, Yoko Shimpuku, Velia Siciliano, Shalini S. Arya, Almas Taj Awan, Chandra Shekhar Sharma, David Fernández Rivas, Maryam Moghaddam Matin, Paulina Carmona-Mora, Sandeep Kaur-Ghumaan, Karen J. Cloete, Anna K. Coussens, John Kuumuori Ganle, Stefan Kohler, Kaur-Ghumaan, Sandeep [0000-0002-0688-3428], Coussens, Anna K [0000-0002-7086-2621], Moronta-Barrios, Felix [0000-0002-9433-8576], Bhattarai, Suraj [0000-0001-6843-6677], Niamir, Leila [0000-0002-0285-5542], Kohler, Stefan [0000-0003-1365-7506], Rios Rojas, Clarissa [0000-0001-6544-4663], Matin, Maryam M [0000-0002-7949-7712], Badre, Abdeslam [0000-0002-8582-2892], Carmona-Mora, Paulina [0000-0001-8560-1232], Apollo - University of Cambridge Repository, Mesoscale Chemical Systems, TechMed Centre, and MESA+ Institute

Subjects

2019-20 coronavirus outbreak, Coronavirus disease 2019 (COVID-19), Research system, media_common.quotation_subject, Social Sciences, Science, Technology And Society, Health Humanities, Political science, AZ20-999, Pandemic, Vulnerable population, Science communication, Early career, General Psychology, Diplomacy, media_common, business.industry, General Arts and Humanities, Comment, General Social Sciences, Public relations, General Business, Management and Accounting, History of scholarship and learning. The humanities, business, General Economics, Econometrics and Finance

Abstract

Scientific collaborations among nations to address common problems and to build international partnerships as part of science diplomacy is a well-established notion. The international flow of people and ideas has played an important role in the advancement of the 'Sciences' and the current pandemic scenario has drawn attention towards the genuine need for a stronger role of science diplomacy, science advice and science communication. In dealing with the COVID-19 pandemic, visible interactions across science, policy, science communication to the public and diplomacy worldwide have promptly emerged. These interactions have benefited primarily the disciplines of knowledge that are directly informing the pandemic response, while other scientific fields have been relegated. The effects of the COVID-19 pandemic on scientists of all disciplines and from all world regions are discussed here, with a focus on early-career researchers (ECRs), as a vulnerable population in the research system. Young academies and ECR-driven organisations could suggest ECR-powered solutions and actions that could have the potential to mitigate these effects on ECRs working on disciplines not related to the pandemic response. In relation with governments and other scientific organisations, they can have an impact on strengthening and creating fairer scientific systems for ECRs at the national, regional, and global level.

Published

2021

25. Communicable and non-communicable co-morbidities and the presentation of COVID-19 in an African setting of high HIV-1 and tuberculosis prevalence

Author

Elsa du Bruyn, Cari Stek, Remi Daroowala, Qonita Said-Hartley, Marvin Hsiao, Rene T. Goliath, Fatima Abrahams, Amanda Jackson, Sean Wasserman, Brian W Allwood, Angharad G. Davis, Rachel P-J. Lai, Anna K. Coussens, Katalin A. Wilkinson, Jantina de Vries, Nicki Tiffin, Maddalena Cerrone, Ntobeko A. B. Ntusi, Catherine Riou, Robert J. Wilkinson, Saalikha Aziz, Nonzwakazi Bangani, John Black, Marise Bremer, Wendy Burgers, Zandile Ciko, Hanif Esmail, Siamon Gordon, Yolande X. R. Harley, Francisco Lakay, Fernando-Oneissi Martinez-Estrada, Graeme Meintjes, Marc Mendelson, Tari Papavarnavas, Alize Proust, Sheena Ruzive, Georgia Schafer, Keboile Serole, Claire Whitaker, and Kennedy Zvinairo

Subjects

medicine.medical_specialty, Tuberculosis, Exacerbation, business.industry, Type 2 Diabetes Mellitus, Type 2 diabetes, Disease, medicine.disease, Obesity, Internal medicine, Pandemic, Medicine, Observational study, business

Abstract

ObjectivesTo describe the presentation and outcome of SARS-CoV2 infection in an African setting of high non-communicable co-morbidity and also HIV-1 and tuberculosis prevalence.DesignCase control analysis with cases stratified by HIV-1 and tuberculosis status.SettingA single-centre observational case-control study of adults admitted to a South African hospital with proven SARS-CoV-2 infection or alternative diagnosis.Participants104 adults with RT-PCR-proven SARS-CoV2 infection of which 55 (52.9%) were male and 31 (29.8%) HIV-1 co-infected. 40 adults (35.7% male, 30.9% HIV-1 co-infected) admitted during the same period with no RT-PCR or serological evidence of SARS-CoV2 infection and assigned alternative diagnoses. Additional in vitro data from prior studies of 72 healthy controls and 118 HIV-1 uninfected and infected persons participants enrolled to a prior study with either immune evidence of tuberculosis sensitization but no symptoms or microbiologically confirmed pulmonary tuberculosis.ResultsTwo or more co-morbidities were present in 57.7% of 104 RT-PCR proven COVID-19 presentations, the commonest being hypertension (48%), type 2 diabetes mellitus (39%), obesity (31%) but also HIV-1 (30%) and active tuberculosis (14%). Amongst patients dually infected by tuberculosis and SARS-CoV-2, clinical features could be dominated by either SARS-CoV-2 or tuberculosis: lymphopenia was exacerbated, and some markers of inflammation (D-dimer and ferritin) elevated in singly SARS-CoV-2 infected patients were even further elevated (p < 0.05). HIV-1 and SARS-CoV2 co-infection resulted in lower absolute number and proportion of CD4 lymphocytes, with those in the lowest peripheral CD4 percentage strata exhibiting absent or lower antibody responses against SARS-CoV2. Death occurred in 30/104 (29%) of all COVID-19 patients and in 6/15 (40%) of patients with coincident SARS-CoV-2 and tuberculosis.ConclusionsIn this South African setting, HIV-1 and tuberculosis are common co-morbidities in patients presenting with COVID-19. In environments in which tuberculosis is common, SARS-CoV-2 and tuberculosis may co-exist with clinical presentation being typical of either disease. Clinical suspicion of exacerbation of co-existent tuberculosis accompanying SARS-CoV-2 should be high.What is already known on this topic?It has been quite widely thought that Africa has been spared the worst effects of the COVID-19 pandemic. There are very few reported case series and no case-control studies comparing COVID-19 patients admitted to hospital to those admitted for other reasons. However several studies have indicated both HIV-1 and tuberculosis co-infection that are endemic in Africa constitute risk factors for poor outcome. In addition Africa is subject to demographic transition and the prevalence of non-communicable co-morbidities such as type 2 diabetes, hypertension and cardiovascular disease is rising rapidly. No study from Africa has described the clinical impact on the presentation of COVID-19 infection.What this study addsTwo or more co-morbidities were present in over half COVID-19 presentations, including HIV-1 (30%) and active tuberculosis (14%). Patients dually infected by tuberculosis and SARS-CoV-2, presented as either SARS-CoV-2 or tuberculosis. HIV-1 and SARS-CoV2 co-infection resulted in lower absolute number and proportion of CD4 lymphocytes, and those with low CD4 counts had absent or lower antibody responses against SARS-CoV2. Death occurred 29% of all COVID-19 patients and in 40% of patients with coincident SARS-CoV-2 and tuberculosis. Thus in environments in which tuberculosis is common, SARS-CoV-2 and tuberculosis may co-exist with clinical presentation being typical of either disease and clinical suspicion of exacerbation of co-existent tuberculosis accompanying SARS-CoV-2 should be high.

Published

2021

26. Generation of Liposomes to Study the Effect of Mycobacterium Tuberculosis Lipids on HIV-1 cis- and trans-Infections

Author

William A. Paxton, Georgios Pollakis, Anna K. Coussens, Alessandra Ruggiero, Apoorva Bhatt, Robert J. Wilkinson, Anastasia Koch, Jordan Thomas, Gurdyal S. Besra, Marion Pouget, Department of Medicine, Faculty of Health Sciences, and Wellcome Trust

Subjects

0301 basic medicine, Chemistry, Multidisciplinary, lcsh:Chemistry, M. smegmatis, Cell Wall, PDIM, BCG, H37Rv, lcsh:QH301-705.5, Spectroscopy, Mycobacterium bovis, biology, Coinfection, Mycobacterium smegmatis, in vitro, General Medicine, 3. Good health, Computer Science Applications, DC-SIGN, Chemistry, TB, Physical Sciences, Life Sciences & Biomedicine, CDC1551, liposomes, Biochemistry & Molecular Biology, 0699 Other Biological Sciences, 030106 microbiology, Mycobacterium Infections, Nontuberculous, Receptors, Cell Surface, Catalysis, Virus, Article, Microbiology, Inorganic Chemistry, Mycobacterium tuberculosis, TDM, 03 medical and health sciences, Glycolipid, Antigen, trans-infection, 0399 Other Chemical Sciences, Humans, Tuberculosis, Lectins, C-Type, Physical and Theoretical Chemistry, Molecular Biology, 0604 Genetics, Science & Technology, Chemical Physics, AIDS-Related Opportunistic Infections, HN878, Organic Chemistry, Virus Internalization, SL1, biology.organism_classification, HEK293 Cells, smegmatis, 030104 developmental biology, lcsh:Biology (General), lcsh:QD1-999, biology.protein, HIV-1, Glycolipids, EU127, Cell Adhesion Molecules, Mycobacterium

Abstract

Tuberculosis (TB) is the leading cause of death among HIV-1-infected individuals and Mycobacterium tuberculosis (Mtb) co-infection is an early precipitate to AIDS. We aimed to determine whether Mtb strains differentially modulate cellular susceptibility to HIV-1 infection (cis- and trans-infection), via surface receptor interaction by their cell envelope lipids. Total lipids from pathogenic (lineage 4 Mtb H37Rv, CDC1551 and lineage 2 Mtb HN878, EU127) and non-pathogenic (Mycobacterium bovis BCG and Mycobacterium smegmatis) Mycobacterium strains were integrated into liposomes mimicking the lipid distribution and antigen accessibility of the mycobacterial cell wall. The resulting liposomes were tested for modulating in vitro HIV-1 cis- and trans-infection of TZM-bl cells using single-cycle infectious virus particles. Mtb glycolipids did not affect HIV-1 direct infection however, trans-infection of both R5 and X4 tropic HIV-1 strains were impaired in the presence of glycolipids from M. bovis, Mtb H37Rv and Mtb EU127 strains when using Raji-DC-SIGN cells or immature and mature dendritic cells (DCs) to capture virus. SL1, PDIM and TDM lipids were identified to be involved in DC-SIGN recognition and impairment of HIV-1 trans-infection. These findings indicate that variant strains of Mtb have differential effect on HIV-1 trans-infection with the potential to influence HIV-1 disease course in co-infected individuals.

Published

2021

27. Immunopathogenic Overlap and Shared Therapeutic Targets for Covid-19 and Tuberculosis Predicted from Transcriptomic Meta-Analysis

Author

Johnson We, Sheerin D, Abhimanyu, Xiaobin Wang, and Anna K. Coussens

Subjects

Oncology, medicine.medical_specialty, Tuberculosis, Coronavirus disease 2019 (COVID-19), business.industry, Disease, Medical research, medicine.disease, Transcriptome, Meta-analysis, Active tb, Internal medicine, Biomarker (medicine), Medicine, business

Abstract

Current and previous tuberculosis (TB) increase the risk for severe and fatal COVID-19. To identify mechanisms of immunopathogenic interaction which may increase severity of COVID-19 and determine the impact of co-infection on subsequent TB progression, we performed a systematic review and patient-level meta-analysis of COVID-19 transcriptomic signatures, spanning mild-critical disease, from whole blood, PBMCs and BALF. Thirty-five eligible signatures were profiled on 1181 RNA-seq samples from 853 individuals, across the spectrum of TB infection. Twenty COVID-19 gene-signatures had significantly higher “COVID-19 risk scores” in active and progressive TB compared with non-progressing latent infection and uninfected controls (p

Published

2021

28. Lifetime burden of disease due to incident tuberculosis: a global reappraisal including post-tuberculosis sequelae

Author

Anthony D. Harries, Matthew Quaife, Anthony Byrne, Florian M. Marx, Joshua A. Salomon, Sedona Sweeney, Nicolas A Menzies, Ted Cohen, Brian W. Allwood, Debora Pedrazzoli, Rein M G J Houben, Robert S. Wallis, Sanne van Kampen, Anna K. Coussens, and Jamilah Meghji

Subjects

Burden of disease, Male, wc_20, Tuberculosis, media_common.quotation_subject, Disease, Global Health, wf_205_1, Neglect, Global Burden of Disease, Cost of Illness, Pulmonary tuberculosis, Risk Factors, Environmental health, Case fatality rate, wf_250, Medicine, Humans, Disabled Persons, Survivors, Tuberculosis, Pulmonary, Disease burden, media_common, business.industry, General Medicine, Articles, medicine.disease, Socioeconomic Factors, Cohort, Female, wf_200, Quality-Adjusted Life Years, Public aspects of medicine, RA1-1270, business

Abstract

Summary Background Many individuals who survive tuberculosis disease face ongoing disability and elevated mortality risks. However, the impact of post-tuberculosis sequelae is generally omitted from policy analyses and disease burden estimates. We therefore estimated the global burden of tuberculosis, inclusive of post-tuberculosis morbidity and mortality. Methods We constructed a hypothetical cohort of individuals developing tuberculosis in 2019, including pulmonary and extrapulmonary disease. We simulated lifetime health outcomes for this cohort, stratified by country, age, sex, HIV status, and treatment status. We used disability-adjusted life-years (DALYs) to summarise fatal and non-fatal health losses attributable to tuberculosis, during the disease episode and afterwards. We estimated post-tuberculosis mortality and morbidity based on the decreased lung function caused by pulmonary tuberculosis disease. Findings Globally, we estimated 122 (95% uncertainty interval [UI] 98–151) million DALYs due to incident tuberculosis disease in 2019, with 58 (38–83) million DALYs attributed to post-tuberculosis sequelae, representing 47% (95% UI 37–57) of the total burden estimate. The increase in burden from post-tuberculosis varied substantially across countries and regions, driven largely by differences in estimated case fatality for the disease episode. We estimated 12·1 DALYs (95% UI 10·0–14·9) per incident tuberculosis case, of which 6·3 DALYs (5·6–7·0) were from the disease episode and 5·8 DALYs (3·8–8·3) were from post-tuberculosis. Per-case post-tuberculosis burden estimates were greater for younger individuals, and in countries with high incidence rates. The burden of post-tuberculosis was spread over the remaining lifetime of tuberculosis survivors, with almost a third of total DALYs (28%, 95% UI 23–34) accruing 15 or more years after incident tuberculosis. Interpretation Post-tuberculosis sequelae add substantially to the overall disease burden caused by tuberculosis. This hitherto unquantified burden has been omitted from most previous policy analyses. Future policy analyses and burden estimates should take better account of post-tuberculosis, to avoid the potential misallocation of funding, political attention, and research effort resulting from continued neglect of this issue. Funding National Institutes of Health.

Published

2021

29. The Lifetime Burden of Disease Due to Incident Tuberculosis: A Global Re-Appraisal Including Post-TB Sequelae

Author

Florian M. Marx, Jamilah Meghji, Anthony Byrne, Debora Pedrazzoli, Anthony D. Harries, Sanne van Kampen, Ted Cohen, Robert S. Wallis, Anna K. Coussens, Nicholas A Menzies, Joshua A. Salomon, Brian W. Allwood, Sedona Sweeney, Rein M G J Houben, and Matthew Quaife

Subjects

Burden of disease, History, Tuberculosis, Polymers and Plastics, business.industry, media_common.quotation_subject, Disease, medicine.disease, Industrial and Manufacturing Engineering, Neglect, Environmental health, Case fatality rate, Cohort, Medicine, Hiv status, Business and International Management, business, Disease burden, media_common

Abstract

Background : Many individuals who survive TB disease face ongoing disability and elevated mortality risks. However, the impact of post-TB sequelae is generally omitted from policy analyses and disease burden estimates. We therefore estimated the global burden of TB, inclusive of post-TB morbidity and mortality. Methods : Lifetime health outcomes were simulated for the cohort developing TB disease globally in 2019, stratified by country, age, sex, HIV status, and treatment status. We used disability-adjusted life-years (DALYs) to summarize fatal and nonfatal health losses attributable to TB, during the disease episode and afterwards. We estimated post-TB mortality and morbidity based on the decreased lung function caused by pulmonary TB disease. Findings : Globally, we estimated 122 (95% uncertainty interval: 98, 151) million DALYs due to incident TB disease in 2019, with 58 (38, 83) million DALYs attributed to post-TB sequelae, representing 47% (37, 57) of the total burden estimate. The increase in burden from post-TB varied substantially across countries and regions, driven largely by differences in estimated case fatality for the disease episode. We estimated 12.1 (10.0, 14.9) DALYs per incident TB case, of which 6.3 (5.6, 7.0) DALYs were from the disease episode and 5.8 (3.8, 8.3) from post-TB. Per-case post-TB burden estimates were greater for younger individuals, and in countries with high incidence rates. The burden of post-TB was spread over the remaining lifetime of TB survivors, with almost one-third (28% (23, 34)) of total DALYs accruing 15 or more years after incident TB. Interpretation : Post-TB sequelae produce a substantial fraction of the disease burden caused by TB. This hitherto unquantified burden has been omitted from most prior policy analyses. Future policy analyses and burden estimates should take better account of post-TB, to avoid the potential misallocation of funding, political attention, and research effort resulting from continued neglect of this issue. Funding: NAM and TC acknowledge funding from the NIH (R01AI146555). MQ acknowledges funding from the Bill and Melinda Gates Foundation (INV-001754). AKC acknowledges funding from WEHI philanthropy. JM acknowledges funding from the Medical Research Council MR/S02042X/1). RSW acknowledges funding from Horizon 2020 and EDCTP. RMGJH acknowledges funding from the European Research Council (757699). Declaration of Interest: The authors declare no conflicts of interest.

Published

2021

30. Systematic evaluation of transcriptomic disease risk and diagnostic biomarker overlap between COVID-19 and tuberculosis: a patient-level meta-analysis

Author

Johnson We, Anna K. Coussens, Xiaobin Wang, Abhimanyu, and Sheerin D

Subjects

Oncology, medicine.medical_specialty, Tuberculosis, Coronavirus disease 2019 (COVID-19), business.industry, Respiratory disease, medicine.disease, medicine.disease_cause, Article, Transcriptome, Syndemic, Meta-analysis, Internal medicine, Medicine, Platelet activation, business, Coronavirus

Abstract

BackgroundThe novel coronavirus, SARS-CoV-2, has increased the burden on healthcare systems already strained by a high incidence of tuberculosis (TB) as co-infection and dual presentation are occurring in syndemic settings. We aimed to understand the interaction between these diseases by profiling COVID-19 gene expression signatures on RNA-sequencing data from TB-infected individuals.MethodsWe performed a systematic review and patient-level meta-analysis by querying PubMed and pre-print servers to derive eligible COVID-19 gene expression signatures from human whole blood (WB), PBMCs or BALF studies. A WB influenza dataset served as a control respiratory disease signature. Three large TB RNA-seq datasets, comprising multiple cohorts from the UK and Africa and consisting of TB patients across the disease spectrum, were chosen to profile these signatures. Putative “COVID-19 risk scores” were generated for each sample in the TB datasets using the TBSignatureProfiler package. Risk was stratified by time to TB diagnosis in progressors and contacts of pulmonary and extra-pulmonary TB. An integrative analysis between TB and COVID-19 single-cell RNA-seq data was performed and a population-level meta-analysis was conducted to identify shared gene ontologies between the diseases and their relative enrichment in COVID-19 disease severity states.Results35 COVID-19 gene signatures from nine eligible studies comprising 98 samples were profiled on TB RNA-seq data from 1181 samples from 853 individuals. 25 signatures had significantly higher COVID-19 risk in active TB (ATB) compared with latent TB infection (p FCN1- andSPP1-expressing macrophages enriched in BALF during severe COVID-19 were identified in circulation during ATB. Shared perturbed ontologies included antigen presentation, epigenetic regulation, platelet activation, and ROS/RNS production were enriched with increasing COVID-19 severity. Finally, we demonstrate that the overlapping transcriptional responses may complicate development of blood-based diagnostic signatures of co-infection.InterpretationOur results identify shared dysregulation of immune responses in COVID-19 and TB as a dual risk posed by co-infection to COVID-19 severity and TB disease progression. These individuals should be followed up for TB in the months subsequent to SARS-CoV-2 diagnosis.

Published

2020

31. The Mtb-HIV syndemic interaction: why treating M. tuberculosis infection may be crucial for HIV-1 eradication

Author

Robert J. Wilkinson, Melissa-Rose Abrahams, Anna K. Coussens, Robyn Waters, Collin R. Diedrich, and Mthawelanga Ndengane

Subjects

0301 basic medicine, viral reservoir, CD4(+) T-CELLS, Tuberculosis, PULMONARY TUBERCULOSIS, 030106 microbiology, HIV-1 cure, Human immunodeficiency virus (HIV), Review, SET-POINT, medicine.disease_cause, Virus, immune activation, LONG TERMINAL REPEAT, LATENT TUBERCULOSIS, Mycobacterium tuberculosis, 03 medical and health sciences, Syndemic, Acquired immunodeficiency syndrome (AIDS), 1108 Medical Microbiology, Virology, Medicine, Tuberculosis Disease, granuloma, latency, TUMOR-NECROSIS-FACTOR, Science & Technology, biology, business.industry, Transmission (medicine), transmission, virus diseases, FACTOR-ALPHA, respiratory system, medicine.disease, biology.organism_classification, bacterial infections and mycoses, viral expansion, AIDS, 030104 developmental biology, VIRAL LOAD, tuberculosis, HUMAN-IMMUNODEFICIENCY-VIRUS, MYCOBACTERIUM-TUBERCULOSIS, business, Life Sciences & Biomedicine, 0605 Microbiology

Abstract

Accelerated tuberculosis and AIDS progression seen in HIV-1 and Mycobacterium tuberculosis (Mtb)-coinfected individuals indicates the important interaction between these syndemic pathogens. The immunological interaction between HIV-1 and Mtb has been largely defined by how the virus exacerbates tuberculosis disease pathogenesis. Understanding of the mechanisms by which pre-existing or subsequent Mtb infection may favor the replication, persistence and progression of HIV, is less characterized. We present a rationale for the critical consideration of ‘latent’ Mtb infection in HIV-1 prevention and cure strategies. In support of this position, we review evidence of the effect of Mtb infection on HIV-1 acquisition, replication and persistence. We propose that ‘latent’ Mtb infection may have considerable impact on HIV-1 pathogenesis and the continuing HIV-1 epidemic in sub-Saharan Africa., Graphical abstract The proposed impact of Mycobacterium tuberculosis (Mtb) coinfection (solid lines) on the life-course progression of HIV-1 infection (dotted lines). In addition to enhancing the speed of AIDS progression and tuberculosis development in those HIV-1 infected, Mtb infection increases myeloid and T-cell immune activation and the susceptibility of cells to HIV-1 infection and HIV-1 replication in infected and bystander cells. Following antiretroviral therapy initiation, a larger pool of reservoir cells harboring HIV-1 and higher immune activation status has the potential to result in more frequent blips in viremia above the level of clinical detection (thin line).

Published

2020

32. Post-tuberculosis mortality and morbidity: valuing the hidden epidemic

Author

Ted Cohen, Sedona Sweeney, Brian W. Allwood, Rein M G J Houben, Anthony D. Harries, Florian M. Marx, Matthew Quaife, Anna K. Coussens, Robert S. Wallis, Sanne van Kampen, and Nicolas A Menzies

Subjects

Pulmonary and Respiratory Medicine, Lung Diseases, medicine.medical_specialty, Tuberculosis, business.industry, MEDLINE, medicine.disease, 03 medical and health sciences, Pulmonary Disease, Chronic Obstructive, 0302 clinical medicine, 030228 respiratory system, Cause of Death, medicine, Humans, 030212 general & internal medicine, Morbidity, Mortality, Intensive care medicine, business, Epidemics

Published

2020

33. Natural Resistance to and Host-Directed Prevention of Tuberculosis

Author

Thomas Richard Hawn, Robert Wilkinson, and Anna K. Coussens

Subjects

Natural resistance, Tuberculosis, Host (biology), medicine, Biology, medicine.disease, Virology

Published

2020

34. Plasma Biomarkers to Detect Prevalent or Predict Progressive Tuberculosis Associated With Human Immunodeficiency Virus–1

Author

Cara Pienaar, Molebogeng X Rangaka, Maia Lesosky, Katalin A. Wilkinson, Anna K. Coussens, Gary Maartens, Robert J. Wilkinson, Shaheed Mathee, Rene Goliath, Judith Mwansa-Kambafwile, and Wellcome Trust

Subjects

Adult, Male, 0301 basic medicine, Microbiology (medical), medicine.medical_specialty, Tuberculosis, 030106 microbiology, HIV Infections, Disease, Microbiology, QuantiFERON, law.invention, Plasma, 03 medical and health sciences, 0302 clinical medicine, Randomized controlled trial, law, Clinical Decision Rules, Internal medicine, Humans, Medicine, Blood test, predictive, 030212 general & internal medicine, Articles and Commentaries, 11 Medical and Health Sciences, medicine.diagnostic_test, Diagnostic Tests, Routine, business.industry, Isoniazid, Area under the curve, 06 Biological Sciences, medicine.disease, 3. Good health, Infectious Diseases, tuberculosis, HIV-1, biomarker, Biomarker (medicine), Female, business, Biomarkers, medicine.drug

Abstract

Background The risk of individuals infected with human immunodeficiency virus (HIV)-1 developing tuberculosis (TB) is high, while both prognostic and diagnostic tools remain insensitive. The potential for plasma biomarkers to predict which HIV-1–infected individuals are likely to progress to active disease is unknown. Methods Thirteen analytes were measured from QuantiFERON Gold in-tube (QFT) plasma samples in 421 HIV-1–infected persons recruited within the screening and enrollment phases of a randomized, controlled trial of isoniazid preventive therapy. Blood for QFT was obtained pre-randomization. Individuals were classified into prevalent TB, incident TB, and control groups. Comparisons between groups, supervised learning methods, and weighted correlation network analyses were applied utilizing the unstimulated and background-corrected plasma analyte concentrations. Results Unstimulated samples showed higher analyte concentrations in the prevalent and incident TB groups compared to the control group. The largest differences were seen for C-X-C motif chemokine 10 (CXCL10), interleukin-2 (IL-2), IL-1α, transforming growth factor-α (TGF-α). A predictive model analysis using unstimulated analytes discriminated best between the control and prevalent TB groups (area under the curve [AUC] = 0.9), reasonably well between the incident and prevalent TB groups (AUC > 0.8), and poorly between the control and incident TB groups. Unstimulated IL-2 and IFN-γ were ranked at or near the top for all comparisons, except the comparison between the control vs incident TB groups. Models using background-adjusted values performed poorly. Conclusions Single plasma biomarkers are unlikely to distinguish between disease states in HIV-1 co-infected individuals, and combinations of biomarkers are required. The ability to detect prevalent TB is potentially important, as no blood test hitherto has been suggested as having the utility to detect prevalent TB amongst HIV-1 co-infected persons., In prevalent tuberculosis (TB), incident TB, and control samples, we evaluated 13 plasma biomarkers to identify individuals infected with human immunodeficiency virus–1 who were susceptible to active TB: biomarkers differentiated prevalent TB from control samples, but not incident TB.

Published

2018

35. The role of UV radiation and vitamin D in the seasonality and outcomes of infectious disease

Author

Abhimanyu and Anna K. Coussens

Subjects

0301 basic medicine, Vitamin, Ultraviolet Rays, Disease, Biology, Communicable Diseases, 03 medical and health sciences, chemistry.chemical_compound, 0302 clinical medicine, Immune system, Immunity, Vitamin D and neurology, Animals, Humans, Antimicrobial peptide production, Vitamin D, Physical and Theoretical Chemistry, Innate immune system, integumentary system, fungi, Immunity, Innate, 030104 developmental biology, chemistry, Infectious disease (medical specialty), Immunology, Seasons, 030215 immunology

Abstract

The seasonality of infectious disease outbreaks suggests that environmental conditions have a significant effect on disease risk. One of the major environmental factors that can affect this is solar radiation, primarily acting through ultraviolet radiation (UVR), and its subsequent control of vitamin D production. Here we show how UVR and vitamin D, which are modified by latitude and season, can affect host and pathogen fitness and relate them to the outcomes of bacterial, viral and vector-borne infections. We conducted a thorough comparison of the molecular and cellular mechanisms of action of UVR and vitamin D on pathogen fitness and host immunity and related these to the effects observed in animal models and clinical trials to understand their independent and complementary effects on infectious disease outcome. UVR and vitamin D share common pathways of innate immune activation primarily via antimicrobial peptide production, and adaptive immune suppression. Whilst UVR can induce vitamin D-independent effects in the skin, such as the generation of photoproducts activating interferon signaling, vitamin D has a larger systemic effect due to its autocrine and paracrine modulation of cellular responses in a range of tissues. However, the seasonal patterns in infectious disease prevalence are not solely driven by variation in UVR and vitamin D levels across latitudes. Vector-borne pathogens show a strong seasonality of infection correlated to climatic conditions favoring their replication. Conversely, pathogens, such as influenza A virus, Mycobacterium tuberculosis and human immunodeficiency virus type 1, have strong evidence to support their interaction with vitamin D. Thus, UVR has both vitamin D-dependent and independent effects on infectious diseases; these effects vary depending on the pathogen of interest and the effects can be complementary or antagonistic.

Published

2017

36. Relationship Between HIV Coinfection, Interleukin 10 Production, and Mycobacterium tuberculosis in Human Lymph Node Granulomas

Author

Collin R, Diedrich, Jennifer, O'Hern, Maximiliano G, Gutierrez, Nafiesa, Allie, Patricia, Papier, Graeme, Meintjes, Anna K, Coussens, Helen, Wainwright, and Robert J, Wilkinson

Subjects

Adult, CD4-Positive T-Lymphocytes, Male, antiretroviral therapy, HIV Infections, CD8-Positive T-Lymphocytes, mycobacterium, histology, Interferon-gamma, Young Adult, Major Articles and Brief Reports, Humans, granuloma, Aged, Coinfection, HIV, Mycobacterium tuberculosis, Middle Aged, lymph node, Interleukin-10, CD4 Lymphocyte Count, tuberculosis, IL-10, HIV-1, HIV/AIDS, Female, Lymph Nodes

Abstract

Background. Human immunodeficiency virus type 1 (HIV)–infected persons are more susceptible to tuberculosis than HIV–uninfected persons. Low peripheral CD4+ T-cell count is not the sole cause of higher susceptibility, because HIV–infected persons with a high peripheral CD4+ T-cell count and those prescribed successful antiretroviral therapy (ART) remain more prone to active tuberculosis than HIV–uninfected persons. We hypothesized that the increase in susceptibility is caused by the ability of HIV to manipulate Mycobacterium tuberculosis–associated granulomas. Methods. We examined 71 excised cervical lymph nodes (LNs) from persons with HIV and M. tuberculosis coinfection, those with HIV monoinfection, and those with M. tuberculosis monoinfection with a spectrum of peripheral CD4+ T-cell counts and ART statuses. We quantified differences in M. tuberculosis levels, HIV p24 levels, cellular response, and cytokine presence within granulomas. Results. HIV increased M. tuberculosis numbers and reduced CD4+ T-cell counts within granulomas. Peripheral CD4+ T-cell depletion correlated with granulomas that contained fewer CD4+ and CD8+ T cells, less interferon γ, more neutrophils, more interleukin 10 (IL-10), and increased M. tuberculosis numbers. M. tuberculosis numbers correlated positively with IL-10 and interferon α levels and fewer CD4+ and CD8+ T cells. ART reduced IL-10 production. Conclusions. Peripheral CD4+ T-cell depletion correlated with increased M. tuberculosis presence, increased IL-10 production, and other phenotypic changes within granulomas, demonstrating the HIV infection progressively changes these granulomas.

Published

2016

37. Recent progress in understanding immune activation in the pathogenesis in HIV-tuberculosis co-infection

Author

Elsa Du Bruyn, Anna K. Coussens, Robert J. Wilkinson, Hanif Esmail, Nashied Peton, and Patrick Howlett

Subjects

0301 basic medicine, CD4-Positive T-Lymphocytes, Tuberculosis, Immunology, Human immunodeficiency virus (HIV), HIV Infections, medicine.disease_cause, Immune complex formation, Pathogenesis, 03 medical and health sciences, Interferon, Virology, medicine, Animals, Humans, Risk factor, Cause of death, Oncology (nursing), business.industry, Coinfection, Hematology, Mycobacterium tuberculosis, medicine.disease, 030104 developmental biology, Infectious Diseases, Oncology, HIV-1, business, medicine.drug, Co infection

Abstract

Tuberculosis is the leading infectious cause of death worldwide, and HIV-1 the best recognized risk factor for active TB. This review focuses on immune complex formation; the interplay of type I and II interferon signaling; and T-cell activation in HIV-TB pathogenesis.Circulating immune complexes and complement, and Fcγ signaling in whole blood act as early markers of TB disease in HIV-1-infected persons. HIV-1 is associated with a type I interferon response in whole blood, reducing the specificity of TB biomarkers dependent on type I and II interferon genes. Type I and type II interferons are implicated in both protection and TB disease, a protective outcome may depend on modulating these pathways. Whilst M. tuberculosis-specific CD4 T cells are preferentially depleted during HIV-1 infection, activation markers on M. tuberculosis-specific CD4 T cells, in particular HLA-DR, reflect immune activation and have promise as biomarkers of M. tuberculosis disease activity in individuals with HIV-1.TB pathogenesis in HIV-1 involves a complex interaction of underlying activation of both the innate and adaptive immune systems. Further research is required to understand whether biomarkers of activation could be used to predict or quantify TB disease in the context of HIV-1 infection.

Published

2018

38. Complement pathway gene activation and rising circulating immune complexes characterize early disease in HIV-associated tuberculosis

Author

Clifton E. Barry, Katalin A. Wilkinson, Anne O'Garra, Stuart Horswell, Christine M. Graham, Hanif Esmail, Rachel P. J. Lai, Maia Lesosky, Robert J. Wilkinson, Anna K. Coussens, and Wellcome Trust

Subjects

0301 basic medicine, incipient disease, Transcription, Genetic, immune complex, PATHOGENESIS, HIV Infections, Disease, Antigen-Antibody Complex, Comorbidity, Positron Emission Tomography Computed Tomography, Cluster Analysis, complement, Subclinical infection, Oligonucleotide Array Sequence Analysis, Multidisciplinary, biology, Coinfection, SIGNATURE, Immune complex, Multidisciplinary Sciences, PNAS Plus, Disease Progression, Science & Technology - Other Topics, Antibody, medicine.symptom, Signal Transduction, Transcriptional Activation, Tuberculosis, POST PRIMARY TUBERCULOSIS, Asymptomatic, Antibodies, 03 medical and health sciences, Classical complement pathway, Fluorodeoxyglucose F18, MYCOBACTERIAL ANTIGENS, medicine, Humans, Science & Technology, business.industry, HIV, Complement System Proteins, medicine.disease, Complement system, 030104 developmental biology, Immunology, CELLS, biology.protein, Interferons, business, Transcriptome

Abstract

The transition between latent and active tuberculosis (TB) occurs before symptom onset. Better understanding of the early events in subclinical disease will facilitate the development of diagnostics and interventions that improve TB control. This is particularly relevant in the context of HIV-1 coinfection where progression of TB is more likely. In a recent study using [ 18 F]-fluoro-2-deoxy- d -glucose positron emission/computed tomography (FDG-PET/CT) on 35 asymptomatic, HIV-1–infected adults, we identified 10 participants with radiographic evidence of subclinical disease, significantly more likely to progress than the 25 participants without. To gain insight into the biological events in early disease, we performed blood-based whole genome transcriptomic analysis on these participants and 15 active patients with TB. We found transcripts representing the classical complement pathway and Fcγ receptor 1 overabundant from subclinical stages of disease. Levels of circulating immune (antibody/antigen) complexes also increased in subclinical disease and were highly correlated with C1q transcript abundance. To validate our findings, we analyzed transcriptomic data from a publicly available dataset where samples were available in the 2 y before TB disease presentation. Transcripts representing the classical complement pathway and Fcγ receptor 1 were also differentially expressed in the 12 mo before disease presentation. Our results indicate that levels of antibody/antigen complexes increase early in disease, associated with increased gene expression of C1q and Fcγ receptors that bind them. Understanding the role this plays in disease progression may facilitate development of interventions that prevent this, leading to a more favorable outcome and may also be important to diagnostic development.

Published

2018

39. The effect of antiretroviral treatment on selected genes in whole blood from HIV-infected adults sensitised by Mycobacterium tuberculosis

Author

Nishtha Jhilmeet, Katalin A. Wilkinson, Thomas J. Scriba, Rene Goliath, David M. Lowe, Anna K. Coussens, Robert J. Wilkinson, Catherine Riou, and Wellcome Trust

Subjects

CD4(+) T-CELLS, Bacterial Diseases, RNA viruses, CD4-Positive T-Lymphocytes, Male, 0301 basic medicine, Gene Expression, HIV Infections, Pathology and Laboratory Medicine, THERAPY, Memory T cells, 0302 clinical medicine, Immunodeficiency Viruses, Antiretroviral Therapy, Highly Active, Cellular types, Whole blood, Multidisciplinary, biology, Coinfection, Immune cells, Viral Load, 3. Good health, Multidisciplinary Sciences, Actinobacteria, Infectious Diseases, Treatment Outcome, medicine.anatomical_structure, Medical Microbiology, Viral Pathogens, Viruses, Science & Technology - Other Topics, White blood cells, Medicine, Female, Pathogens, Viral load, Research Article, EXPRESSION, Cell biology, Blood cells, Tuberculosis, General Science & Technology, T cell, Science, Immunology, T cells, Viral diseases, Microbiology, Mycobacterium tuberculosis, 03 medical and health sciences, Immune system, MD Multidisciplinary, Retroviruses, Genetics, medicine, Humans, T Helper Cells, Microbial Pathogens, Medicine and health sciences, Science & Technology, Bacteria, business.industry, Gene Expression Profiling, Lentivirus, Organisms, Biology and Life Sciences, HIV, Tropical Diseases, biology.organism_classification, medicine.disease, CD4 Lymphocyte Count, Gene expression profiling, 030104 developmental biology, Animal cells, Gene Expression Regulation, HIV-1, Immunization, business, Interferon-gamma Release Tests, RESPONSES, 030215 immunology

Abstract

HIV-1 co-infection is a leading cause of susceptibility to tuberculosis (TB), with the risk of TB being increased at all stages of HIV-1 infection. Antiretroviral treatment (ART) is the most effective way to reduce the risk of TB in HIV-1 co-infected people. Studying protective, ART-induced, immune restoration in HIV-1 infected individuals sensitised by Mycobacterium tuberculosis (Mtb) can thus help identify mechanisms of protection against TB. In order to understand ART-mediated prevention of TB in HIV-1 infected adults, we investigated the expression of 30 genes in whole blood from HIV-1 infected patients during the first 6 months of ART-induced immune reconstitution. The 30 selected genes were previously described to be differentially expressed between sorted Mtb specific central and effector memory CD4 T cells. HIV-1 infected persons sensitised by Mtb were recruited in Khayelitsha, South Africa, when initiating ART. RNA was extracted from whole blood at initiation and 1, 3 and 6 months of ART. qRT-PCR was used to determine gene expression and three reference ‘housekeeping’ genes were used to calculate the fold change in the expression of each gene relative to day 0 of ART. Results were assessed longitudinally. We observed a decrease in the expression of a number of genes at 6 months of ART, reflecting a decrease in immune activation. However, following correction for multiple comparisons and increasing CD4 counts, only the decrease in CD27 gene expression remained statistically significant. While not statistically significant, a number of genes also showed increased expression at various timepoints, illustrating the broad regeneration of the T cell pool in HIV-1 infected adults on ART. Our findings generate hypotheses underlying ART- induced protective immune reconstitution and may pave the way for future studies to evaluate ART mediated prevention of TB in HIV-1 infected persons.

Published

2018

40. Human Immunology of Tuberculosis

Author

Thomas J. Scriba, Anna K. Coussens, and Helen A. Fletcher

Subjects

0301 basic medicine, 03 medical and health sciences, 030104 developmental biology, 0302 clinical medicine, 030215 immunology

Published

2017

41. Socio-political prescriptions for latent tuberculosis infection are required to prevent reactivation of tuberculosis

Author

Tolu Oni, Paul H. Mason, and Anna K. Coussens

Subjects

Microbiology (medical), Tuberculosis, Latent tuberculosis, business.industry, General Medicine, Mycobacterium tuberculosis, medicine.disease, lcsh:Infectious and parasitic diseases, 03 medical and health sciences, Politics, 0302 clinical medicine, Infectious Diseases, 030228 respiratory system, Latent Tuberculosis, Environmental health, medicine, Humans, lcsh:RC109-216, 030212 general & internal medicine, Medical prescription, business

Published

2017

42. Regulation of CYP27B1 and CYP24A1 hydroxylases limits cell-autonomous activation of vitamin D in dendritic cells

Author

Mahdad Noursadeghi, Bernard Khoo, Rhiannon Kundu, Anna K. Coussens, and Benjamin M. Chain

Subjects

Vitamin, medicine.medical_specialty, Calcitriol, Immunology, Vitamin D3 24-Hydroxylase, Biology, Cell biology, Paracrine signalling, chemistry.chemical_compound, Endocrinology, CYP24A1, Downregulation and upregulation, chemistry, Internal medicine, medicine, Vitamin D and neurology, Immunology and Allergy, Autocrine signalling, medicine.drug

Abstract

The active vitamin D metabolite 1α,25-dihydroxyvitamin D (1,25[OH]2D) potently inhibits DC priming of T-cell activation, suggesting that it mediates a homeostatic role in this context. Therefore, careful regulation of 1,25[OH]2D levels is necessary to avoid inappropriate inhibition of T-cell activation. Cell-autonomous control of vitamin D activity can be modulated by the action of the vitamin D-activating and -inactivating hydroxylases, CYP27B1, and CYP24A1, respectively. We show that in comparison to macrophages, human monocyte-derived DCs exhibit significantly less activation of 25-dihydroxyvitamin D to 1,25[OH]2D, and that DCs predominantly express a truncated CYP27B1 transcript that may contribute to the deficiency in activation of vitamin D. Furthermore, in response to stimulation with 1,25[OH]2D, upregulation of the inactivating enzyme CYP24A1 curtailed the functional effects of vitamin D in DCs, but not macrophages. Production of 1,25[OH]2D by macrophages was adequate to induce expression of vitamin D-responsive genes by DCs, inhibit DC maturation in response to innate immune stimulation and DC-dependent T-cell responses. Our data suggest that in comparison to macrophages, differential regulation of hydroxylases limits autocrine vitamin D activity in DCs, and that paracrine activation of vitamin D exerts a more potent mechanism for homeostatic control of DC function.

Published

2014

43. Human Immunology of Tuberculosis

Author

Helen A. Fletcher, Thomas J. Scriba, and Anna K. Coussens

Subjects

0301 basic medicine, Microbiology (medical), Tuberculosis, Physiology, Disease, Adaptive Immunity, Mycobacterium tuberculosis, 03 medical and health sciences, 0302 clinical medicine, Immune system, Immunity, Genetics, medicine, Animals, Humans, 030212 general & internal medicine, Immunoassay, Innate immune system, General Immunology and Microbiology, Ecology, biology, Diagnostic Tests, Routine, Transmission (medicine), Cell Biology, biology.organism_classification, Acquired immune system, medicine.disease, Virology, Immunity, Innate, Disease Models, Animal, 030104 developmental biology, Infectious Diseases, Immunology, Disease Susceptibility

Abstract

Immunology is a central theme when it comes to tuberculosis (TB). The outcome of human infection with Mycobacterium tuberculosis is dependent on the ability of the immune response to clear or contain the infection. In cases where this fails, the bacterium replicates, disseminates within the host, and elicits a pathologic inflammatory response, and disease ensues. Clinical presentation of TB disease is remarkably heterogeneous, and the disease phenotype is largely dependent on host immune status. Onward transmission of M. tuberculosis to new susceptible hosts is thought to depend on an excessive inflammatory response causing a breakdown of the lung matrix and formation of lung cavities. But this varies in cases of underlying immunological dysfunction: for example, HIV-1 infection is associated with less cavitation, while diabetes mellitus comorbidity is associated with increased cavitation and risk of transmission. In compliance with the central theme of immunology in tuberculosis, we rely on detection of an adaptive immune response, in the form of interferon-gamma release assays or tuberculin skin tests, to diagnose infection with M. tuberculosis . Here we review the immunology of TB in the human host, focusing on cellular and humoral adaptive immunity as well as key features of innate immune responses and the underlying immunological dysfunction which associates with human TB risk factors. Our review is restricted to human immunology, and we highlight distinctions from the immunological dogma originating from animal models of TB, which pervade the field.

Published

2016

44. Characterization of progressive HIV-associated tuberculosis using 2-deoxy-2-[(18)F]fluoro-D-glucose positron emission and computed tomography

Author

Maia Lesosky, Qonita Said-Hartley, Anna K. Coussens, Douglas B. Young, Coenraad F.N. Koegelenberg, Tolu Oni, Katalin A. Wilkinson, Hanif Esmail, James M. Warwick, Rachel P. J. Lai, Robert J. Wilkinson, JoAnne L. Flynn, Clifton E. Barry, Anne O'Garra, Christine M. Graham, Gerhard Walzl, and Wellcome Trust

Subjects

Male, 0301 basic medicine, Pathology, Radiography, Human immunodeficiency virus (HIV), HIV Infections, Computed tomography, Research & Experimental Medicine, medicine.disease_cause, DISEASE, South Africa, Positron Emission Tomography Computed Tomography, INFECTION, Positron emission, 11 Medical and Health Sciences, Subclinical infection, medicine.diagnostic_test, Latent tuberculosis, Coinfection, General Medicine, PREVALENCE, 3. Good health, Medicine, Research & Experimental, Disease Progression, Female, Radiography, Thoracic, medicine.symptom, Life Sciences & Biomedicine, Adult, Biochemistry & Molecular Biology, FUTURE-PROSPECTS, medicine.medical_specialty, Tuberculosis, STRATEGIES, PULMONARY TUBERCULOSIS, Immunology, Asymptomatic, General Biochemistry, Genetics and Molecular Biology, Article, 03 medical and health sciences, Fluorodeoxyglucose F18, Latent Tuberculosis, medicine, Humans, Tuberculosis, Pulmonary, Science & Technology, business.industry, Sputum, Cell Biology, ADULTS, Mycobacterium tuberculosis, ACTIVE TUBERCULOSIS, medicine.disease, 030104 developmental biology, Radiopharmaceuticals, business, LUNG, Interferon-gamma Release Tests

Abstract

Tuberculosis is classically divided into states of latent infection and active disease. Using combined positron emission and computed tomography in 35 asymptomatic, antiretroviral-therapy-naive, HIV-1-infected adults with latent tuberculosis, we identified ten individuals with pulmonary abnormalities suggestive of subclinical, active disease who were substantially more likely to progress to clinical disease. Our findings challenge the conventional two-state paradigm and may aid future identification of biomarkers that are predictive of progression.

Published

2016

45. Vitamin D Status and Its Consequences for Health in South Africa

Author

Caradee Y. Wright, Mary Norval, Robyn M. Lucas, Liza Bornman, Robert J. Wilkinson, Anna K. Coussens, and Wellcome Trust

Subjects

0301 basic medicine, 25(OH)D levels, Ultraviolet Rays, Health, Toxicology and Mutagenesis, Library science, lcsh:Medicine, HIV Infections, Comorbidity, Review, Environment, Toxicology, 03 medical and health sciences, South Africa, sun exposure, 0302 clinical medicine, Age Distribution, MD Multidisciplinary, Medicine, Humans, vitamin D receptor, Genetic Predisposition to Disease, 030212 general & internal medicine, Sex Distribution, Vitamin D, Life Style, National health, Life style, business.industry, lcsh:R, Public Health, Environmental and Occupational Health, Medical research, Vitamin D Deficiency, 3. Good health, Diet, 030104 developmental biology, tuberculosis, Dietary Supplements, Sunlight, HIV-1, Receptors, Calcitriol, Age distribution, Sun exposure, business

Abstract

In this review, reports were retrieved in which vitamin D status, as assessed by serum 25-hydroxyvitamin D [25(OH)D] levels, was measured in South African population groups with varied skin colours and ethnicities. Healthy children and adults were generally vitamin D-sufficient [25(OH)D level >50 nmol/L] but the majority of those aged above 65 years were deficient. A major role for exposure to solar ultraviolet radiation (UVR) in determining 25(OH)D levels was apparent, with the dietary contribution being minor. Limited data exist regarding the impact of recent changes in lifestyles on vitamin D status, such as urbanisation. With regard to disease susceptibility, 11 of 22 relevant publications indicated association between low 25(OH)D levels and disease, with deficiency most notably found in individuals with tuberculosis and HIV-1. Information on the relationship between vitamin D receptor variants and ethnicity, disease or treatment response in the South African population groups demonstrated complex interactions between genetics, epigenetics and the environment. Whether vitamin D plays an important role in protection against the range of diseases that currently constitute a large burden on the health services in South Africa requires further investigation. Only then can accurate advice be given about personal sun exposure or dietary vitamin D supplementation.

Published

2016

46. Corticosteroid Therapy, Vitamin D Status, and Inflammatory Cytokine Profile in the HIV-Tuberculosis Immune Reconstitution Inflammatory Syndrome

Author

Adrian R. Martineau, Robert J. Wilkinson, Katalin A. Wilkinson, Graeme Meintjes, Anali Conesa-Botella, Rodrigo Moreno-Reyes, Anna K. Coussens, Robert Colebunders, Charlotte Schutz, Helen van der Plas, Rene Goliath, and Meera R. Mehta

Subjects

Microbiology (medical), Adult, Male, medicine.drug_class, medicine.medical_treatment, HIV Infections, Invited Articles, vitamin D deficiency, Proinflammatory cytokine, 03 medical and health sciences, 0302 clinical medicine, Immune reconstitution inflammatory syndrome, Adrenal Cortex Hormones, Immune Reconstitution Inflammatory Syndrome, medicine, Vitamin D and neurology, Humans, Immunologic Factors, Tuberculosis, 030212 general & internal medicine, Prospective Studies, Interleukin 6, Biology, 030304 developmental biology, 0303 health sciences, biology, business.industry, Interleukin, medicine.disease, Vitamin D Deficiency, 3. Good health, Infectious Diseases, Cytokine, Immunology, biology.protein, Corticosteroid, HIV/AIDS, Cytokines, Female, Human medicine, business

Abstract

Vitamin D deficiency is common in human immunodeficiency virus–tuberculosis coinfected patients in Cape Town. Those who develop tuberculosis-immune reconstitution inflammatory syndrome have a further reduction in circulating 25-hydroxyvitamin D levels 2 weeks into combined antiretroviral therapy with a concomitant increase in inflammatory cytokines and chemokines., Background. Tuberculosis-immune reconstitution inflammatory syndrome (TB-IRIS) in patients coinfected with human immunodeficiency virus (HIV) and tuberculosis starting antiretroviral therapy (ART) is associated with hypercytokinemia. As adjunctive corticosteroid therapy and vitamin D have immunomodulatory properties, we investigated the relationship between cytokine/chemokine profiles, corticosteroid use, and vitamin D deficiency in TB-IRIS patients. Methods. Plasma from 39 TB-IRIS and 42 non-IRIS patients was collected during a prospective study of HIV-associated tuberculosis patients starting ART. In total, 26% of patients received corticosteroid (CTC) therapy pre-ART for severe tuberculosis. Concentrations of total 25-hydroxyvitamin D (25(OH)D) and 14 cytokines/chemokines were determined at ART initiation and 2 weeks later. Results. Patients prescribed concurrent CTC had lower interferon γ (IFN-γ), IP-10, tumor necrosis factor (TNF), interleukin (IL)-6, IL-8, IL-10, IL-12p40, and IL-18 pre-ART (P ≤ .02). TB-IRIS presented at 12 days (median) of ART, irrespective of CTC use. In patients who developed TB-IRIS (not on CTC) IL-6, IL-8, IL-12p40, IL-18, IP-10, and TNF increased during 2 weeks (P ≤ .04) of ART. Vitamin D deficiency (total 25(OH)D

Published

2012

47. Immunomodulatory Actions of Vitamin D Metabolites and their Potential Relevance to Human Lung Disease

Author

Anna K. Coussens

Subjects

Pulmonary and Respiratory Medicine, medicine.anatomical_structure, Vitamin D+Metabolites, business.industry, Immunology, Medicine, Relevance (information retrieval), Disease, Pharmacology, business, Human lung

Published

2011

48. Identification of genes differentially expressed by prematurely fused human sutures using a novel in vivo – in vitro approach

Author

Ian P. Hughes, Anna K. Coussens, C. Phillip Morris, Barry C. Powell, Angela van Daal, C. R. Wilkinson, and Peter J. Anderson

Subjects

Male, Cancer Research, Cellular differentiation, Morphogenesis, In Vitro Techniques, Biology, Craniosynostosis, Craniosynostoses, Tissue culture, Osteogenesis, In vivo, medicine, Humans, Craniosynostosis, Microarray, Differentiation, Osteoblast, De-differentiate, Molecular Biology, Cells, Cultured, Adaptor Proteins, Signal Transducing, Oligonucleotide Array Sequence Analysis, Osteoblasts, Gene Expression Profiling, Gene Expression Regulation, Developmental, Infant, Cell Differentiation, Cranial Sutures, Cell Biology, Acrocephalosyndactylia, Cell Dedifferentiation, medicine.disease, Molecular biology, In vitro, Culture Media, Repressor Proteins, Gene expression profiling, RNA, Messenger, Stored, Fibroblast Growth Factor 2, 060103 Cell Development Proliferation and Death, 060405 Gene Expression (incl. Microarray and other genome-wide approaches), Developmental Biology, Explant culture

Abstract

Craniosynostosis is the premature fusion of calvarial sutures. It results from abnormal differentiation or proliferation of cells within the osteogenic fronts of growing calvarial bones. To date, research has focused on animal models and in vitro organ and tissue culture to determine the molecular mechanisms controlling calvarial suture morphogenesis. Here, we test a new, in vivo–in vitro approach based on the hypothesis that calvarial suture cells passaged in minimal medium exhibit a stable gene expression profile similar to undifferentiated osteoblastic cells that can provide a benchmark for comparison with in vivo expression of differentiated tissue. We show that tissue-specific expression is lost after the first passage and, using cDNA microarrays, compare expression between fused suture tissue from craniosynostosis patients and in vitro de-differentiated explant cells. A large number of differentially expressed genes were identified, including novel genes WIF1, LEF1, SATB2, RARRES1, DEFA1, DMP1, PTPRZ1, and PTPRC, as well as those commonly associated with human suture morphogenesis, e.g., FGF2, MSX2, and BMP2. Two differentially expressed genes, WIF1 and FGF2, were further examined in an in vivo–in vivo comparison between unfused and prematurely fused tissue. The same pattern of differential expression was observed in each case, further validating the ability of our in vivo–in vitro approach to identify genes involved in in vivo human calvarial tissue differentiation.

Published

2008

49. High-dose vitamin D3 reduces deficiency caused by low UVB exposure and limits HIV-1 replication in urban Southern Africans

Author

Rene Goliath, Anna K. Coussens, Celeste E Naude, Robert J. Wilkinson, George Chaplin, and Nina G. Jablonski

Subjects

Adult, Vitamin, Urban Population, Ultraviolet Rays, Anemia, Population, HIV Infections, Virus Replication, Polymorphism, Single Nucleotide, Africa, Southern, vitamin D deficiency, Young Adult, chemistry.chemical_compound, HIV Seroprevalence, Immunity, Vitamin D and neurology, medicine, Humans, Longitudinal Studies, Young adult, education, Cholecalciferol, education.field_of_study, Multidisciplinary, Dose-Response Relationship, Drug, Biological Sciences, Vitamin D Deficiency, medicine.disease, 3. Good health, Geography, chemistry, Immunology, HIV-1, Seasons

Abstract

Cape Town, South Africa, has a seasonal pattern of UVB radiation and a predominantly dark-skinned urban population who suffer high HIV-1 prevalence. This coexistent environmental and phenotypic scenario puts residents at risk for vitamin D deficiency, which may potentiate HIV-1 disease progression. We conducted a longitudinal study in two ethnically distinct groups of healthy young adults in Cape Town, supplemented with vitamin D3 in winter, to determine whether vitamin D status modifies the response to HIV-1 infection and to identify the major determinants of vitamin D status (UVB exposure, diet, pigmentation, and genetics). Vitamin D deficiency was observed in the majority of subjects in winter and in a proportion of individuals in summer, was highly correlated with UVB exposure, and was associated with greater HIV-1 replication in peripheral blood cells. High-dosage oral vitamin D3 supplementation attenuated HIV-1 replication, increased circulating leukocytes, and reversed winter-associated anemia. Vitamin D3 therefore presents as a low-cost supplementation to improve HIV-associated immunity.

Published

2015

50. Phenylbutyrate Is Bacteriostatic against Mycobacterium tuberculosis and Regulates the Macrophage Response to Infection, Synergistically with 25-Hydroxy-Vitamin D?

Author

Adrian R. Martineau, Robert J. Wilkinson, Anna K. Coussens, Institute of Infectious Disease and Molecular Medicine, and Faculty of Health Sciences

Subjects

MAPK signaling cascades, medicine.medical_treatment, Receptor expression, Immunology, Inflammation, Microbiology, Phenylbutyrate, Cathelicidin, 03 medical and health sciences, 0302 clinical medicine, CYP24A1, Virology, parasitic diseases, Genetics, medicine, Humans, Tuberculosis, CXCL10, Vitamin D, Molecular Biology, Secretion, Calcifediol, Cell Proliferation, 030304 developmental biology, 0303 health sciences, Reverse Transcriptase Polymerase Chain Reaction, Chemistry, Antimicrobials, Macrophages, Drug Synergism, Inflammasome, Mycobacterium tuberculosis, Flow Cytometry, Phenylbutyrates, Anti-Bacterial Agents, 3. Good health, Gene regulation, Chemokine secretion, Parasitology, Gene expression, medicine.symptom, Research Article, 030215 immunology, medicine.drug

Abstract

Adjunctive vitamin D treatment for pulmonary tuberculosis enhances resolution of inflammation but has modest effects on bacterial clearance. Sodium 4-phenylbutyrate (PBA) is in clinical use for a range of conditions and has been shown to synergise with vitamin D metabolites to upregulate cathelicidin antimicrobial peptide (CAMP) expression. We investigated whether clinically attainable plasma concentrations of PBA (0.4-4mM) directly affect Mycobacterium tuberculosis (Mtb) growth and human macrophage and PBMC response to infection. We also tested the ability of PBA to enhance the immunomodulatory actions of the vitamin D metabolite 25(OH)D3 during infection and synergistically inhibit intracellular Mtb growth. PBA inhibited Mtb growth in broth with an MIC99 of 1mM, which was reduced to 0.25mM by lowering pH. During human macrophage infection, PBA treatment restricted Mtb uptake, phagocytic receptor expression and intracellular growth in a dose-dependent manner. PBA independently regulated CCL chemokine secretion and induced expression of the antimicrobial LTF (lactoferrin), the anti-inflammatory PROC (protein C) and multiple genes within the NLRP3 inflammasome pathway. PBA co-treatment with 25(OH)D3 synergistically modulated expression of numerous vitamin D-response genes, including CAMP, CYP24A1, CXCL10 and IL-37. This synergistic effect was dependent on MAPK signalling, while the effect of PBA on LTF, PROC and NLRP3 was MAPK-independent. During PBA and 25(OH)D3 co-treatment of human macrophages, in the absence of exogenous proteinase 3 (PR3) to activate cathelicidin, Mtb growth restriction was dominated by the effect of PBA, while the addition of PR3 enhanced growth restriction by 25(OH)D3 and PBA co-treatment. This suggests that PBA augments vitamin D–mediated cathelicidin-dependent Mtb growth restriction by human macrophages and independently induces antimicrobial and anti-inflammatory action. Therefore through both host-directed and bacterial-directed mechanisms PBA and vitamin D may prove an effective combinatorial adjunct therapy for tuberculosis to both resolve immunopathology and enhance bacterial clearance., Author Summary Tuberculosis (TB) is the world’s leading bacterial cause of death. Effective treatment currently requires a minimum of 4 drugs taken for at least 6 months. While these drugs kill the TB causing bacteria (Mtb), they do not directly resolve the inmmunopathology associated with morbidity. Immunomodulatory agents that not only enhance an individual’s ability to kill Mtb but also help heal lung pathology could be used as adjuncts to current therapies to improve treatment outcome. Phenylbutyrate (PBA) has been in clinical use for more than 30 years to treat a range of conditions. It has also been shown to synergise with vitamin D to induce cellular production of the anti-Mtb peptide, cathelicidin. We investigated whether PBA and vitamin D synergistically kill Mtb in human macrophages and whether PBA has any independent effect on macrophages and Mtb. At concentrations that are achieved in plasma clinically, PBA inhibited Mtb growth. PBA also inhibited growth of Mtb in human macrophages via a cell-dependent mechanism, inducing the inflammasome pathway and antimicrobial lactoferrin. PBA also synergistically enhanced macrophage response to vitamin D and co-treatment further inhibited Mtb growth, when synergistically-induced cathelicidin was activated. PBA and vitamin D may therefore prove an effective combinatorial adjunct therapy for tuberculosis.

Published

2015