Type-2 diabetes alters the basal phenotype of human macrophages and diminishes their capacity to respond, internalise, and control Mycobacterium tuberculosis

López-López, Nallely; Martinez, Ana Gabriela Ramos; García-Hernández, Mariana Haydee; Hernández-Pando, Rogelio; Castañeda-Delgado, Julio Enrique; Lugo-Villarino, Geanncarlo; Cougoule, Céline; Neyrolles, Olivier; Rivas-Santiago, Bruno; Valtierra-Alvarado, Monica Alejandra; Rubio-Caceres, Marisela; Enciso-Moreno, José Antonio; Serrano, Carmen

doi:10.1590/0074-02760170326

Cited by 43 publications

(44 citation statements)

References 26 publications

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“…T2D generates a series of changes that compromises the host response against M. tuberculosis, as recently reviewed by some authors 6,7 , including altered capacity to present antigens by macrophages 8 , activation of monocytes 9 , and chemoattraction of immune cells to lung during infection 10 . Furthermore, T2D favors more severe manifestations of TB as compared with those occurring in patients without T2D 11 , including extended lung damage especially at chronic stages of the comorbidity 12,13 .…”

Section: Introductionmentioning

confidence: 99%

BCG and BCGΔBCG1419c protect type 2 diabetic mice against tuberculosis via different participation of T and B lymphocytes, dendritic cells and pro-inflammatory cytokines

et al. 2020

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Comorbidity between Tuberculosis (TB) and type 2 diabetes (T2D) is one of the greatest contributors to the spread of Mycobacterium tuberculosis (M. tuberculosis) in low-and middle-income countries. T2D compromises key steps of immune responses against M. tuberculosis and it might affect the protection afforded by vaccine candidates against TB. We compared the protection and immune response afforded by the BCGΔBCG1419c vaccine candidate versus that of wild-type BCG in mice with T2D. Vaccination with both BCGΔBCG1419c, BCG or infection with M. tuberculosis reduced weight loss, hyperglycemia, and insulin resistance during T2D progression, suggesting that metabolic changes affecting these parameters were affected by mycobacteria. For control of acute TB, and compared with non-vaccinated controls, BCG showed a dominant T CD4 + response whereas BCGΔBCG1419c showed a dominant T CD8 + /B lymphocyte response. Moreover, BCG maintained an increased response in lung cells via IFN-γ, TNF-α, and IL-4, while BCGΔBCG1419c increased IFN-γ but reduced IL-4 production. As for chronic TB, and compared with non-vaccinated controls, both BCG strains had a predominant presence of T CD4 + lymphocytes. In counterpart, BCGΔBCG1419c led to increased presence of dendritic cells and an increased production of IL-1 β. Overall, while BCG effectively reduced pneumonia in acute infection, it failed to reduce it in chronic infection, whereas we hypothesize that increased production of IL-1 β induced by BCGΔBCG1419c contributed to reduced pneumonia and alveolitis in chronic TB. Our results show that BCG and BCGΔBCG1419c protect T2D mice against TB via different participation of T and B lymphocytes, dendritic cells, and pro-inflammatory cytokines.

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Section: Introductionmentioning

confidence: 99%

BCG and BCGΔBCG1419c protect type 2 diabetic mice against tuberculosis via different participation of T and B lymphocytes, dendritic cells and pro-inflammatory cytokines

et al. 2020

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“…Enhanced IL-10 levels in the periphery but reduced IL-10 in sputum cells from TB-DM patients at follow up, may also indicate that IL-10 producing cells fail to migrate properly from the peripheral circulation to the Mtb-infected lung. In support of this, the low IL-10 production capacity of immune cells and reduced anti-in ammatory function of IL-10 have been reported in TB-DM disease compared to TB alone [60,61]. While IL-10 could contribute to unwanted immunosuppression of Mtb-speci c immune responses [62,63], it is also necessary to control local pathological in ammation and sustain an environment that limits Mtb replication [64].…”

Section: Discussionmentioning

confidence: 91%

Slow radiological improvement and persistent low-grade inflammation after chemotherapy in tuberculosis patients with type 2 diabetes

Mily

Sarker

Taznin

et al. 2020

Preprint

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Background: Diabetes mellitus type 2 (DM) may impede immune responses in tuberculosis (TB) and thus contribute to enhanced disease severity. In this study, we aimed to evaluate DM-mediated alterations in clinical, radiological and immunological outcomes in TB disease.Methods: Newly diagnosed pulmonary TB patients with or without DM (TB n=40; TB-DM n=40) were recruited in Dhaka, Bangladesh. Clinical symptoms, sputum smear and culture conversion as well as chest radiography were assessed. Peripheral blood and sputum samples were collected at the time of diagnosis (baseline) and after 1, 2 and 6 months of standard anti-TB treatment. Blood samples were also obtained from healthy controls (n=20). mRNA expression of inflammatory markers in blood and sputum samples were quantified using real-time PCR.Results: The majority of TB-DM patients had poor glycemic control (HbA1c>8%) and displayed elevated pulmonary pathology (P=0.039) particularly in the middle (P<0.004) and lower lung zones (P<0.02) throughout the treatment period. However, reduction of clinical symptoms and time to sputum smear and culture conversion did not differ between the groups. Transcripts levels of the pro-inflammatory cytokines IL-1β (P=0.003 at month-1 and P=0.045 at month-2) and TNF-α (P=0.005 at month-1) and the anti-inflammatory cytokine IL-10 (P=0.005 at month-2) were higher in peripheral blood after anti-TB treatment in TB-DM compared to TB patients. Conversely in sputum, TB-DM patients had reduced CD4 (P<0.009 at month-1) and IL-10 (P=0.005 at month-1 and P=0.006 at month-2) transcripts, whereas CD8 was elevated (P=0.016 at month-2). At 1- and 2-months post-treatment, sputum IL-10 transcripts were inversely correlated with fasting blood glucose and HbA1C levels in all patients. Conclusion: Insufficient up-regulation of IL-10 in the lung may fuel persistent local inflammation thereby promoting lung pathology in TB-DM patients with poorly controlled DM.

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“…Enhanced IL-10 levels in the periphery but reduced IL-10 in sputum cells from TB-DM patients at follow up, may also indicate that IL-10 producing cells fail to properly migrate from the peripheral circulation to the Mtb-infected lung. Low IL-10 production capacity of immune cells and reduced anti-inflammatory function of IL-10 have been reported in TB-DM disease compared to TB alone [53,54]. While IL-10 could contribute to unwanted immunosuppression of Mtb-specific immune responses [55,56], it is also necessary to control local pathological inflammation and sustain an environment that limits Mtb replication [57].…”

Section: Discussionmentioning

confidence: 99%

Slow radiological improvement and persistent low-grade inflammation after chemotherapy in tuberculosis patients with type 2 diabetes

Mily

Sarker

Taznin

et al. 2020

Preprint

View full text Add to dashboard Cite

Background: Diabetes mellitus type 2 (DM) may impede immune responses in tuberculosis (TB) and thus contribute to enhanced disease severity. In this study, we aimed to evaluate DM-mediated alterations in clinical, radiological and immunological outcomes of TB disease.Methods: Newly diagnosed pulmonary TB patients with or without DM (TB n=40; TB-DM n=40) were recruited in Dhaka, Bangladesh. Clinical symptoms, sputum smear and culture conversion as well as chest radiography were assessed, and peripheral blood and sputum samples were collected at the time of diagnosis (baseline) and after 1, 2 and 6 months of standard anti-TB treatment. Blood samples were also obtained from the healthy controls (n=20). mRNA expression of inflammatory markers in blood and sputum samples were quantified using real-time PCR.Results: Majority of TB-DM patients had a poor glycemic control (HbA1c>8%) and displayed elevated pulmonary pathology (P=0.039) particularly in the middle (P<0.004) and lower lung zones (P<0.02) throughout the treatment period. However, reduction of clinical symptoms, and time to sputum smear and culture conversion did not differ between the groups. Transcripts levels of pro-inflammatory cytokines IL-1β (P=0.003 at month-1 and P=0.045 at month-2) and TNF-α (P=0.005 at month-1) and the anti-inflammatory cytokine IL-10 (P=0.005 at month-2) were higher in peripheral blood after anti-TB treatment in TB-DM compared to TB patients. Instead, in sputum, TB-DM patients showed reduced CD4 (P<0.009 at month-1) and IL-10 (P=0.005 at month-1 and P=0.006 at month-2) and elevated CD8 (P=0.016 at month-2) transcripts. At 1 and 2 months post-treatment, sputum IL-10 transcripts were inversely correlated with fasting blood glucose and HbA1C levels in all patients. Conclusion: Insufficient up-regulation of IL-10 in the lung may fuel persistent local inflammation promoting lung pathology in TB-DM patients with poorly controlled DM.

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Type-2 diabetes alters the basal phenotype of human macrophages and diminishes their capacity to respond, internalise, and control Mycobacterium tuberculosis

Cited by 43 publications

References 26 publications

BCG and BCGΔBCG1419c protect type 2 diabetic mice against tuberculosis via different participation of T and B lymphocytes, dendritic cells and pro-inflammatory cytokines

BCG and BCGΔBCG1419c protect type 2 diabetic mice against tuberculosis via different participation of T and B lymphocytes, dendritic cells and pro-inflammatory cytokines

Slow radiological improvement and persistent low-grade inflammation after chemotherapy in tuberculosis patients with type 2 diabetes

Slow radiological improvement and persistent low-grade inflammation after chemotherapy in tuberculosis patients with type 2 diabetes

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