Impaired resolution of blood transcriptomes through tuberculosis treatment with diabetes comorbidity

Clare Eckold; Cassandra L R van Doorn; Rovina Ruslami; Katharina Ronacher; Anca-Lelia Riza; Suzanne van Veen; Ji-Sook Lee; Vinod Kumar; Sarah Kerry-Barnard; Stephanus T Malherbe; Léanie Kleynhans; Kim Stanley; Simone A Joosten; Julia A Critchley; Philip C Hill; Reinout van Crevel; Cisca Wijmenga; Mariëlle C Haks; Mihai Ioana; Bachti Alisjahbana; Gerhard Walzl; Tom H M Ottenhoff; Hazel M Dockrell; Eleonora Vianello; Jacqueline M Cliff; TANDEM Consortium$

doi:10.1002/ctm2.1375

Impaired resolution of blood transcriptomes through tuberculosis treatment with diabetes comorbidity

Clin Transl Med. 2023 Sep;13(9):e1375. doi: 10.1002/ctm2.1375.

Authors

Clare Eckold¹, Cassandra L R van Doorn², Rovina Ruslami³, Katharina Ronacher^{4

5}, Anca-Lelia Riza^{6

7

8}, Suzanne van Veen², Ji-Sook Lee¹, Vinod Kumar^{6

9}, Sarah Kerry-Barnard¹⁰, Stephanus T Malherbe⁴, Léanie Kleynhans⁴, Kim Stanley⁴, Simone A Joosten², Julia A Critchley¹⁰, Philip C Hill¹¹, Reinout van Crevel^{6

12}, Cisca Wijmenga⁹, Mariëlle C Haks², Mihai Ioana^{7

8}, Bachti Alisjahbana^{13

14}, Gerhard Walzl⁴, Tom H M Ottenhoff², Hazel M Dockrell¹, Eleonora Vianello², Jacqueline M Cliff^{1

15}; TANDEM Consortium$¹

Affiliations

¹ Department of Infection Biology and TB Centre, London School of Hygiene & Tropical Medicine, London, UK.
² Department of Infectious Diseases, Leiden University Medical Center, Leiden, The Netherlands.
³ Department of Biomedical Sciences, Faculty of Medicine, Universitas Padjadjaran, Bandung, Indonesia.
⁴ DSI-NRF Centre of Excellence for Biomedical Tuberculosis Research, South African Medical Research Council Centre for Tuberculosis Research, Division of Molecular Biology and Human Genetics, Department of Biomedical Sciences, Faculty of Medicine and Health Sciences, Stellenbosch University, Cape Town, South Africa.
⁵ Mater Research Institute, Faculty of Medicine, Translational Research Institute, The University of Queensland, Brisbane, QLD, Australia.
⁶ Department of Internal Medicine and Radboud Center for Infectious Diseases, Radboud University Medical Center, Nijmegen, The Netherlands.
⁷ Human Genomics Laboratory, Department of Diagnostics and Treatment, University of Medicine and Pharmacy of Craiova, Craiova, Romania.
⁸ Regional Centre for Human Genetics - Dolj, Emergency Clinical County Hospital Craiova, Craiova, Romania.
⁹ Department of Genetics, University of Groningen, University Medical Center Groningen, Groningen, The Netherlands.
¹⁰ Population Health Research Institute, St George's, University of London, London, UK.
¹¹ Division of Health Sciences, Centre for International Health, University of Otago, Dunedin, New Zealand.
¹² Nuffield Department of Medicine, Centre for Tropical Medicine and Global Health, University of Oxford, Oxford, UK.
¹³ Internal Medicine Department, Hasan Sadikin General Hospital, Bandung, Indonesia.
¹⁴ Research Center for Care and Control of Infectious Diseases, Universitas Padjadjaran, Bandung, Indonesia.
¹⁵ Department of Life Sciences, Centre for Inflammation Research and Translational Medicine, Brunel University London, London, UK.

Abstract

Background: People with diabetes are more likely to develop tuberculosis (TB) and to have poor TB-treatment outcomes than those without. We previously showed that blood transcriptomes in people with TB-diabetes (TB-DM) co-morbidity have excessive inflammatory and reduced interferon responses at diagnosis. It is unknown whether this persists through treatment and contributes to the adverse outcomes.

Methods: Pulmonary TB patients recruited in South Africa, Indonesia and Romania were classified as having TB-DM, TB with prediabetes, TB-related hyperglycaemia or TB-only, based on glycated haemoglobin concentration at TB diagnosis and after 6 months of TB treatment. Gene expression in blood at diagnosis and intervals throughout treatment was measured by unbiased RNA-Seq and targeted Multiplex Ligation-dependent Probe Amplification. Transcriptomic data were analysed by longitudinal mixed-model regression to identify whether genes were differentially expressed between clinical groups through time. Predictive models of TB-treatment response across groups were developed and cross-tested.

Results: Gene expression differed between TB and TB-DM patients at diagnosis and was modulated by TB treatment in all clinical groups but to different extents, such that differences remained in TB-DM relative to TB-only throughout. Expression of some genes increased through TB treatment, whereas others decreased: some were persistently more highly expressed in TB-DM and others in TB-only patients. Genes involved in innate immune responses, anti-microbial immunity and inflammation were significantly upregulated in people with TB-DM throughout treatment. The overall pattern of change was similar across clinical groups irrespective of diabetes status, permitting models predictive of TB treatment to be developed.

Conclusions: Exacerbated transcriptome changes in TB-DM take longer to resolve during TB treatment, meaning they remain different from those in uncomplicated TB after treatment completion. This may indicate a prolonged inflammatory response in TB-DM, requiring prolonged treatment or host-directed therapy for complete cure. Development of transcriptome-based biomarker signatures of TB-treatment response should include people with diabetes for use across populations.

Keywords: diabetes; transcriptome; treatment; tuberculosis.

Publication types

Research Support, Non-U.S. Gov't

MeSH terms

Comorbidity
Diabetes Mellitus*
Gene Expression Profiling
Humans
Hyperglycemia*
Transcriptome / genetics

Grants and funding

MR/P017568/1/MRC_/Medical Research Council/United Kingdom