Recurrence due to Relapse or Reinfection With<i>Mycobacterium tuberculosis</i>: A Whole-Genome Sequencing Approach in a Large, Population-Based Cohort With a High HIV Infection Prevalence and Active Follow-up

Guerra-Assunção, José Afonso; Houben, Rein M. G. J.; Crampin, Amelia C.; Mzembe, Themba; Mallard, Kim; Coll, Francesc Español i; Khan, Palwasha; Banda, Louis; Chiwaya, Arthur; Pereira, Rui; McNerney, Ruth; Harris, David; Parkhill, Julian; Clark, Taane G.; Glynn, Judith R.

doi:10.1093/infdis/jiu574

Cited by 157 publications

(179 citation statements)

References 32 publications

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“…This could have biased the estimation of the effect of several demographic and clinical factors towards the null; it might also have resulted in an overestimation of relapse risk associated with HIV coinfection. Given that relapse is more likely to occur soon after treatment completion,36 we performed a sensitivity analysis examining outcomes at 12 months post-treatment completion with no substantive change in results. Last, we analysed the per-protocol analysis sets from RCTs.…”

Section: Discussionmentioning

confidence: 99%

Predicting tuberculosis relapse in patients treated with the standard 6-month regimen: an individual patient data meta-analysis

Romanowski

Balshaw

Benedetti

et al. 2018

Thorax

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BackgroundRelapse continues to place significant burden on patients and tuberculosis (TB) programmes worldwide. We aimed to determine clinical and microbiological factors associated with relapse in patients treated with the WHO standard 6-month regimen and then evaluate the accuracy of each factor at predicting an outcome of relapse.MethodsA systematic review was performed to identify randomised controlled trials reporting treatment outcomes on patients receiving the standard regimen. Authors were contacted and invited to share patient-level data (IPD). A one-step IPD meta-analysis, using random intercept logistic regression models and receiver operating characteristic curves, was performed to evaluate the predictive performance of variables of interest.ResultsIndividual patient data were obtained from 3 of the 12 identified studies. Of the 1189 patients with confirmed pulmonary TB who completed therapy, 67 (5.6%) relapsed. In multipredictor analysis, the presence of baseline cavitary disease with positive smear at 2 months was associated with an increased odds of relapse (OR 2.3(95% CI 1.3 to 4.2)) and a relapse risk of 10%. When area under the curve for each multipredictor model was compared, discrimination between low-risk and higher-risk patients was modest and similar to that of the reference model which accounted for age, sex and HIV status.ConclusionDespite its poor predictive value, our results indicate that the combined presence of cavitary disease and 2-month positive smear status may be the best currently available marker for identifying individuals at an increased risk of relapse, particularly in resource-limited setting. Further investigation is required to assess whether this combined factor can be used to indicate different treatment requirements in clinical practice.

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Section: Discussionmentioning

confidence: 99%

Predicting tuberculosis relapse in patients treated with the standard 6-month regimen: an individual patient data meta-analysis

Romanowski

Balshaw

Benedetti

et al. 2018

Thorax

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“…Clinical studies suggest that individuals with TB-cured history are susceptible to recurrent TB [19–24]. This observation implies that TB-cured persons may have underlining immune incompetence.…”

Section: Resultsmentioning

confidence: 99%

“…Particularly, no studies have been undertaken to investigate whether the population with previously tuberculosis-cured history (TB-cured) can develop reduced immune responses and immunity after PPV23 vaccination. This is not a trivial question, as multiple clinical or epidemiology studies have reported that TB-cured individuals have higher rates of re-infection TB or TB relapse in the absence or presence of HIV coinfection [19–24]. In addition, it is rational to study anti-TB and anti-pneumococcal responses in the context of PPV23 vaccination, as clinical studies have reported high co-incident rates of pneumococcus pneumonia and Mycobacterium tuberculosis (Mtb) infection irrespective of HIV infection [25–28].…”

Section: Introductionmentioning

confidence: 99%

23-valent pneumococcal polysaccharide vaccine elicits hierarchical antibody and cellular responses in healthy and tuberculosis-cured elderly, and HIV-1-infected subjects

Huang

Qian

Pan

et al. 2018

Clinical Immunology

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The PPV23 immunizes healthy elderly and other high-risk populations against pneumococcal disease. Immune mechanisms whereby these populations differently mount antibody(Ab) and cellular responses to PPV23 vaccination remain unknown. Here, healthy elderly, those elderly with prior tuberculosis-cured history (TB-cured), and HIV-infected humans were vaccinated with PPV23, and assessed for opsonophagocytic Ab responses and potential cellular mechanisms. PPV23 vaccination elicited hierarchical responses of opsonophagocytic Ab. PPV23-elicited Ab titers were highest in healthy elderly, significantly lower in TB-cured elderly and lowest in HIV-infected subjects. Mechanistically, high PPV23-elicited Ab titers in healthy elderly were associated with increases in CD19 + CD69+ cells and CD19 + CD138 + plasma cells. Surprisingly, TB-cured elderly failed to show PPV23-induced increases in these cells. While HIV-infected subjects showed a depressed CD19 + CD69+ cellular response, PPV23 vaccination uncovered HIV-related over-reactive increases in CD19 + CD138 + cells. For the first time, we demonstrate that PPV23-elicted opsonophagocytic Ab titers correlate with different cellular responses in healthy, TB-cured and HIV statuses.

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“…If reactivation were simply the result of a secondary infection acquired by proximity with an infectious host, there was no reason to believe that persisters were anything more than dying M. tuberculosis , incapable of causing disease. However, population-based epidemiologic studies, combined with molecular strain typing methods, showed that disease relapse in countries with low burden was largely due to the same strain causing the initial episode of disease, suggestive of reactivation (15–18), while relapse in high burden areas was associated with different strains, suggestive of re-infection (19, 20). Work by Vandiviere, comparing bacilli recovered from resected lesions of patients receiving chemotherapy that were either in communication with (open) or closed off (closed) from the airways, showed that bacteria recovered from closed lesions were uniformly drug susceptible, while those from open lesions were drug resistant despite similar levels of drug penetration (21).…”

Section: Modelsmentioning

confidence: 99%

Metabolic Perspectives on Persistence

Hartman¹,

Wang²,

Jansen³

et al. 2017

Microbiol Spectr

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SUMMARY Accumulating evidence has left little doubt about the importance of persistence or metabolism in the biology and chemotherapy of tuberculosis. However, knowledge of the intersection between these two factors has begun to emerge only recently. Here, we provide a focused review of metabolic characteristics associated with M. tuberculosis persistence. We focus on metabolism because it is the biochemical foundation of all physiologic processes and a distinguishing hallmark of M. tuberculosis’s physiology and pathogenicity. In addition, it serves as the chemical interface between host and pathogen. However, existing knowledge derives largely from physiologic contexts in which replication is the primary biochemical objective. The goal of this review is to reframe existing knowledge of M. tuberculosis metabolism in the context of persistence where quiescence is often a key distinguishing characteristic. Such a perspective may help guide ongoing efforts to develop more efficient cures and inform on novel strategies to break the cycle of transmission sustaining the pandemic.

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Recurrence due to Relapse or Reinfection WithMycobacterium tuberculosis: A Whole-Genome Sequencing Approach in a Large, Population-Based Cohort With a High HIV Infection Prevalence and Active Follow-up

Cited by 157 publications

References 32 publications

Predicting tuberculosis relapse in patients treated with the standard 6-month regimen: an individual patient data meta-analysis

Predicting tuberculosis relapse in patients treated with the standard 6-month regimen: an individual patient data meta-analysis

23-valent pneumococcal polysaccharide vaccine elicits hierarchical antibody and cellular responses in healthy and tuberculosis-cured elderly, and HIV-1-infected subjects

Metabolic Perspectives on Persistence

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