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2. Bronchodilator reversibility as a diagnostic test for adult asthma: Findings from the population-based tasmanian longitudinal health study.

Author

Dharmage S.C., Hamilton G.S., Thomas P.S., Abramson M.J., Haydn Walters E., Perret J.L., Tan D.J., Lodge C.J., Lowe A.J., Bui D.S., Bowatte G., Johns D.P., Dharmage S.C., Hamilton G.S., Thomas P.S., Abramson M.J., Haydn Walters E., Perret J.L., Tan D.J., Lodge C.J., Lowe A.J., Bui D.S., Bowatte G., and Johns D.P.

Abstract

Bronchodilator reversibility (BDR) is often used as a diagnostic test for adult asthma. However, there has been limited assessment of its diagnostic utility. We aimed to determine the discriminatory accuracy of common BDR cut-offs in the context of current asthma and asthma-COPD overlap (ACO) in a middle-aged community sample. The Tasmanian Longitudinal Health Study is a population-based cohort first studied in 1968 (n=8583). In 2012, participants completed respiratory questionnaires and spirometry (n=3609; mean age 53 years). Receiver operating characteristic (ROC) curves were fitted for current asthma and ACO using continuous BDR measurements. Diagnostic parameters were calculated for different categorical cut-offs. Area under the ROC curve (AUC) was highest when BDR was expressed as change in forced expiratory volume in 1 s (FEV1) as a percentage of initial FEV1, as compared with predicted FEV1. The corresponding AUC was 59% (95% CI 54-64%) for current asthma and 87% (95% CI 81-93%) for ACO. Of the categorical cut-offs examined, the European Respiratory Society/American Thoracic Society threshold (12% from baseline and 200 mL) was assessed as providing the best balance between positive and negative likelihood ratios (LR+ and LR-, respectively), with corresponding sensitivities and specificities of 9% and 97%, respectively, for current asthma (LR+ 3.26, LR- 0.93), and 47% and 97%, respectively, for ACO (LR+ 16.05, LR- 0.55). With a threshold of 12% and 200 mL from baseline, a positive BDR test provided a clinically meaningful change in the post-test probability of disease, whereas a negative test did not. BDR was more useful as a diagnostic test in those with co-existent post-bronchodilator airflow obstruction (ACO).Copyright © ERS 2021.

Published
2021

3. Early menarche is associated with lower adult lung function: A longitudinal cohort study from the first to sixth decade of life.

Author

Leynaert B., Frith P.A., Giles G.G., Thomas P.S., Gomez Real F., Campbell B., Simpson J.A., Bui D.S., Lodge C.J., Lowe A.J., Matheson M.C., Bowatte G., Burgess J.A., Hamilton G.S., Dharmage S.C., Perret J.L., Walters E.H., Abramson M.J., Jarvis D., Garcia-Aymerich J., Mishra G., Johns D.P., Leynaert B., Frith P.A., Giles G.G., Thomas P.S., Gomez Real F., Campbell B., Simpson J.A., Bui D.S., Lodge C.J., Lowe A.J., Matheson M.C., Bowatte G., Burgess J.A., Hamilton G.S., Dharmage S.C., Perret J.L., Walters E.H., Abramson M.J., Jarvis D., Garcia-Aymerich J., Mishra G., and Johns D.P.

Abstract

Background and objective: Early menarche is increasing in prevalence worldwide, prompting clinical and public health interest on its links with pulmonary function. We aimed to investigate the relationship between early menarche and lung function in middle age. Method(s): The population-based Tasmanian Longitudinal Health Study (born 1961; n = 8583), was initiated in 1968. The 5th Decade follow-up data (mean age: 45 years) included age at menarche and complex lung function testing. The 6th Decade follow-up (age: 53 years) repeated spirometry and gas transfer factor. Multiple linear regression and mediation analyses were performed to determine the association between age at menarche and adult lung function and investigate biological pathways, including the proportion mediated by adult-attained height. Result(s): Girls reporting an early menarche (<12 years) were measured to be taller with greater lung function at age 7 years compared with those reporting menarche >=12 years. By 45 years of age, they were shorter and had lower post-bronchodilator (BD) forced expiratory volume in 1 s (adjusted mean difference: -133 mL; 95% CI: -233, -33), forced vital capacity (-183 mL; 95% CI: -300, -65) and functional residual capacity (-168 mL; 95% CI: -315, -21). Magnitudes of spirometric deficits were similar at age 53 years. Forty percent of these total effects were mediated through adult-attained height. Conclusion(s): Early menarche was associated with reduced adult lung function. This is the first study to investigate post-BD outcomes and quantify the partial role of adult height in this association.Copyright © 2019 Asian Pacific Society of Respirology

Published
2020

4. Lifetime Risk Factors for Pre- And Post-Bronchodilator Lung Function Decline A Population-based Study.

Author

Svanes C., Marcon A., Garcia-Aymerich J., Erbas B., Jarvis D., Lodge C.J., Dharmage S.C., Bui D.S., Perret J.L., Haydn Walters E., Abramson M.J., Burgess J.A., Bui M.Q., Bowatte G., Lowe A.J., Russell M.A., Alif S.M., Thompson B.R., Hamilton G.S., Giles G.G., Thomas P.S., Morrison S., Johns D.P., Knibbs L.D., Zock J.-P., Svanes C., Marcon A., Garcia-Aymerich J., Erbas B., Jarvis D., Lodge C.J., Dharmage S.C., Bui D.S., Perret J.L., Haydn Walters E., Abramson M.J., Burgess J.A., Bui M.Q., Bowatte G., Lowe A.J., Russell M.A., Alif S.M., Thompson B.R., Hamilton G.S., Giles G.G., Thomas P.S., Morrison S., Johns D.P., Knibbs L.D., and Zock J.-P.

Abstract

Rationale: Interactions between early life and adult insults on lung function decline are not well understood, with most studies investigating prebronchodilator (pre-BD) FEV1 decline. Objective(s): To investigate relationships between adult risk factors and pre- and post-BD lung function decline and their potential effect modification by early life and genetic factors. Method(s): Multiple regression was used to examine associations between adult exposures (asthma, smoking, occupational exposures, traffic pollution, and obesity) and decline in both pre- and post-BD spirometry (forced expiratory volume in 1 s [FEV1], forced vital capacity [FVC], and FEV1/FVC) between ages 45 and 53 years in the Tasmanian Longitudinal Health Study (n = 857). Effect modification of these relationships by childhood respiratory risk factors, including low childhood lung function and GST (glutathione S-transferase) gene polymorphisms, was investigated. Result(s): Baseline asthma, smoking, occupational exposure to vapors/gases/dusts/fumes, and living close to traffic were associated with accelerated decline in both pre- and post-BD FEV1. These factors were also associated with FEV1/FVC decline. Occupational exposure to aromatic solvents was associated with pre-BD but not post-BD FEV1 decline. Maternal smoking accentuated the effect of personal smoking on pre- and post-BD FEV1 decline. Lower childhood lung function and having the GSTM1 null allele accentuated the effect of occupational exposure to vapors/gases/ dusts/fumes and personal smoking on post-BD FEV1 decline. Incident obesity was associated with accelerated decline in FEV1 and more pronounced in FVC. Conclusion(s): This study provides new evidence for accentuation of individual susceptibility to adult risk factors by low childhood lung function, GSTM1 genotype, and maternal smoking.Copyright © 2020 by the American Thoracic Society

Published
2020

7. Cohort profile: The Tasmanian Longitudinal Health STUDY (TAHS).

Author

Walters E.H., Matheson M.C., Abramson M.J., Allen K., Benke G., Burgess J.A., Dowty J.G., Erbas B., Thomas P.S., Thompson B.R., Wood-Baker R., Dharmage S.C., Feather I.H., Frith P.A., Giles G.G., Gurrin L.C., Hamilton G.S., Hopper J.L., James A.L., Jenkins M.A., Johns D.P., Lodge C.J., Lowe A.J., Markos J., Morrison S.C., Perret J.L., Southey M.C., Walters E.H., Matheson M.C., Abramson M.J., Allen K., Benke G., Burgess J.A., Dowty J.G., Erbas B., Thomas P.S., Thompson B.R., Wood-Baker R., Dharmage S.C., Feather I.H., Frith P.A., Giles G.G., Gurrin L.C., Hamilton G.S., Hopper J.L., James A.L., Jenkins M.A., Johns D.P., Lodge C.J., Lowe A.J., Markos J., Morrison S.C., Perret J.L., and Southey M.C.

Published
2019

8. Childhood predictors of lung function trajectories and future COPD risk: a prospective cohort study from the first to the sixth decade of life.

Author

Dharmage S.C., Hopper J., Giles G.G., Abramson M.J., Walters E.H., Matheson M.C., Bui D.S., Lodge C.J., Burgess J.A., Lowe A.J., Perret J., Bui M.Q., Bowatte G., Gurrin L., Johns D.P., Thompson B.R., Hamilton G.S., Frith P.A., James A.L., Thomas P.S., Jarvis D., Svanes C., Russell M., Morrison S.C., Feather I., Allen K.J., Wood-Baker R., Dharmage S.C., Hopper J., Giles G.G., Abramson M.J., Walters E.H., Matheson M.C., Bui D.S., Lodge C.J., Burgess J.A., Lowe A.J., Perret J., Bui M.Q., Bowatte G., Gurrin L., Johns D.P., Thompson B.R., Hamilton G.S., Frith P.A., James A.L., Thomas P.S., Jarvis D., Svanes C., Russell M., Morrison S.C., Feather I., Allen K.J., and Wood-Baker R.

Abstract

Background: Lifetime lung function is related to quality of life and longevity. Over the lifespan, individuals follow different lung function trajectories. Identification of these trajectories, their determinants, and outcomes is important, but no study has done this beyond the fourth decade. Method(s): We used six waves of the Tasmanian Longitudinal Health Study (TAHS) to model lung function trajectories measured at 7, 13, 18, 45, 50, and 53 years. We analysed pre-bronchodilator FEV1 z-scores at the six timepoints using group-based trajectory modelling to identify distinct subgroups of individuals whose measurements followed a similar pattern over time. We related the trajectories identified to childhood factors and risk of chronic obstructive pulmonary disease (COPD) using logistic regression, and estimated population-attributable fractions of COPD. Finding(s): Of the 8583 participants in the original cohort, 2438 had at least two waves of lung function data at age 7 years and 53 years and comprised the study population. We identified six trajectories: early below average, accelerated decline (97 [4%] participants); persistently low (136 [6%] participants); early low, accelerated growth, normal decline (196 [8%] participants); persistently high (293 [12%] participants); below average (772 [32%] participants); and average (944 [39%] participants). The three trajectories early below average, accelerated decline; persistently low; and below average had increased risk of COPD at age 53 years compared with the average group (early below average, accelerated decline: odds ratio 35.0, 95% CI 19.5-64.0; persistently low: 9.5, 4.5-20.6; and below average: 3.7, 1.9-6.9). Early-life predictors of the three trajectories included childhood asthma, bronchitis, pneumonia, allergic rhinitis, eczema, parental asthma, and maternal smoking. Personal smoking and active adult asthma increased the impact of maternal smoking and childhood asthma, respectively, on the early below average

Published
2018

9. The dose-response association between nitrogen dioxide exposure and serum interleukin-6 concentrations.

Author

Abramson M.J., Markos J., Tang M.L.K., Walters E.H., Dharmage S.C., Matheson M.C., Perret J.L., Bowatte G., Lodge C.J., Knibbs L.D., Gurrin L.C., Kandane-Rathnayake R., Johns D.P., Lowe A.J., Burgess J.A., Thompson B.R., Thomas P.S., Wood-Baker R., Morrison S., Giles G.G., Marks G., Abramson M.J., Markos J., Tang M.L.K., Walters E.H., Dharmage S.C., Matheson M.C., Perret J.L., Bowatte G., Lodge C.J., Knibbs L.D., Gurrin L.C., Kandane-Rathnayake R., Johns D.P., Lowe A.J., Burgess J.A., Thompson B.R., Thomas P.S., Wood-Baker R., Morrison S., Giles G.G., and Marks G.

Abstract

Systemic inflammation is an integral part of chronic obstructive pulmonary disease (COPD), and air pollution is associated with cardiorespiratory mortality, yet the interrelationships are not fully defined. We examined associations between nitrogen dioxide (NO2) exposure (as a marker of traffic-related air pollution) and pro-inflammatory cytokines, and investigated effect modification and mediation by post-bronchodilator airflow obstruction (post-BD-AO) and cardiovascular risk. Data from middle-aged participants in the Tasmanian Longitudinal Health Study (TAHS, n = 1389) were analyzed by multivariable logistic regression, using serum interleukin (IL)-6, IL-8 and tumor necrosis factor-alpha (TNF-alpha) as the outcome. Mean annual NO2 exposure was estimated at residential addresses using a validated satellite-based land-use regression model. Post-BD-AO was defined by post-BD forced expiratory ratio (FEV1/FVC) < lower limit of normal, and cardiovascular risk by a history of either cerebrovascular or ischaemic heart disease. We found a positive association with increasing serum IL-6 concentration (geometric mean 1.20 (95% CI: 1.1 to 1.3, p = 0.001) per quartile increase in NO2). This was predominantly a direct relationship, with little evidence for either effect modification or mediation via post-BD-AO, or for the small subgroup who reported cardiovascular events. However, there was some evidence consistent with serum IL-6 being on the causal pathway between NO2 and cardiovascular risk. These findings raise the possibility that the interplay between air pollution and systemic inflammation may differ between post-BD airflow obstruction and cardiovascular diseases.Copyright © 2017 by the authors.Licensee MDPI, Basel, Switzerland.

Published
2017

10. Lung function trajectories over the life span, their associated childhood factors and consequences: A population based longitudinal cohort.

Author

Johns D.P., Hamilton G.S., Frith P.A., Walters E.H., Dharmage S.C., Matheson M.C., Bui D.S., Burgess J.A., Lodge C.L., Bui M.Q., Lowe A., Perret J., Bowatte G., Abramson M.J., Thompson B.R., Allen K.J., James A.L., Thomas P.S., Johns D.P., Hamilton G.S., Frith P.A., Walters E.H., Dharmage S.C., Matheson M.C., Bui D.S., Burgess J.A., Lodge C.L., Bui M.Q., Lowe A., Perret J., Bowatte G., Abramson M.J., Thompson B.R., Allen K.J., James A.L., and Thomas P.S.

Abstract

Introduction/Aim: Individuals with different patterns of lung function growth and decline may have different risks for developing COPD. We investigated trajectories of lung function from childhood to middle age and their associated childhood factors. Method(s): Using 2142 subjects from the Tasmanian Longitudinal Health Study, pre-bronchodilator FEV1, measured at 7, 13, 18, 45, 50 and 53 years, was modelled with Group Based Trajectory Modelling. Logistic regression was used to investigate the relationship between childhood factors and trajectory groups. Result(s): The best fit model showed six distinct trajectories (Figure 1). Based on initial lung function at 7 years, lung function growth and decline rates, the trajectories were labelled as "early low, reduced growth, accelerated decline" (7.4%; n = 159), "early normal/high, normal growth, accelerated decline" (5%; n = 107), "early low, normal growth, normal decline" (28.7%; n = 615), "early low, accelerated growth, normal decline" (4.2%, n = 90), "persistently high" (14%; n = 300) and "normal" (40.7%; n = 871). The first three trajectories had increased risk of COPD (post-bronchodilator FEV1/ FVC < LLN) at age 53 years compared with the "normal" group. Childhood asthma, bronchitis, pneumonia/pleurisy, maternal asthma and maternal smoking were positively associated with these three trajectories while negative associations were observed for breast feeding and childhood overweight (Figure presented). Conclusion(s): This is the first study to develop lung function trajectories from childhood to middle age in a general population. We identified three trajectories for increased risk of COPD: (1) only accelerated lung decline in adulthood, (2) low initial lung function in childhood with normal growth and normal decline, and (3) low initial lung function in childhood with reduced growth and accelerated decline. Important modifiable childhood risk factors for these three trajectories included exposure to maternal smoking in

Published
2017

16. Effect of breathing circuit resistance on the measurement of ventilatory function

Author

Johns, D.P., Ingram, C.M., Khov, S., Rochford, P.D., and Walters, E.H.

Abstract

Background The American Thoracic Society (ATS) has set the acceptable resistance for spirometers at less than 1.5 cm H 2O/l/s over the flow range 0-14 l/s and for monitoring devices at less than 2.5 cm H 2O/l/s (0-14 l/s). The aims of this study were to determine the resistance characteristics of commonly used spirometers and monitoring devices and the effect of resistance on ventilatory function. Methods The resistance of five spirometers (Vitalograph wedge bellows, Morgan rolling seal, Stead Wells water sealed, Fleisch pneumotachograph, Lilly pneumotachograph) and three monitoring devices (Spiro 1, Ferraris, mini-Wright) was measured from the back pressure developed over a range of known flows (1.6-13.1 l/s). Peak expiratory flow (PEF), forced expiratory flow in one second (FEV 1), forced vital capacity (FVC), and mid forced expiratory flow (FEF 25-75%) were measured on six subjects with normal lung function and 13 subjects with respiratory disorders using a pneumotachograph. Ventilatory function was then repeated with four different sized resistors (approximately 1-11 cmH 2O/l/s) inserted between the mouthpiece and pneumotachograph. Results All five diagnostic spirometers and two of the three monitoring devices passed the ATS upper limit for resistance. PEF, FEV 1 and FVC showed significant (p&lt;0.05) inverse correlations with added resistance with no significant difference between the normal and patient groups. At a resistance of 1.5 cm H 2O/l/s the mean percentage falls (95% confidence interval) were: PEF 6.9% (5.4 to 8.3); FEV 1 1.9% (1.0 to 2.8), and FVC 1.5% (0.8 to 2.3). Conclusions The ATS resistance specification for diagnostic spirometers appears to be appropriate. However, the specification for monitoring devices may be too conservative. PEF was found to be the most sensitive index to added resistance.

Published
1998

17. Bronchial hyperresponsiveness in lung transplant recipients: lack of correlation with airway inflammation

Author

Liakakos, P., Snell, G.I., Ward, C., Johns, D.P., Bamford, T.L., Williams, T.J., and Walters, E.H.

Abstract

BackgroundBronchial hyperresponsiveness (BHR) to methacholine has been reported to occur in most lung transplant recipients. BHR to physical stimuli such as exercise and non-isotonic aerosols has not been as extensively studied in this subject population. This report aims to assess the presence and degree of BHR to methacholine and hypertonic saline in stable lung transplant recipients and to relate it to the presence of airway inflammation.MethodsTen patients undergoing bilateral sequential lung transplantation and six heart-lung transplant recipients, all with stable lung function, were recruited 66-1167 days following transplantation. Subjects underwent a methacholine challenge and bronchoscopy for sampling of bronchoalveolar lavage fluid, transbronchial and endobronchial biopsy tissues. Hypertonic saline challenge was performed six days later.ResultsNine of the 16 transplant recipients had positive methacholine challenges (geometric mean PD200.18 mg, interquartile range 0.058-0.509) and three of these subjects also had positive hypertonic saline challenges (PD15=2.3, 33.0, and 51.5 ml). No clear relationship was found between BHR to either methacholine or hypertonic saline and levels of mast cells, eosinophils or lymphocytes in samples of biopsy tissue or lavage fluid.ConclusionsMost of the lung transplant recipients studied were responsive to methacholine and unresponsive to hypertonic saline. BHR was not clearly related to airway inflammation, suggesting an alternative mechanism for BHR following lung transplantation from that usually assumed in asthma.

Published
1997

18. Occupational exposures to solvents and metals are associated with fixed airflow obstruction

Author

Alif, S.M., Dharmage, S.C., Benke, G., Dennekamp, M., Burgess, J.L., Perret, Lodge, C.J., Morrison, S., Johns, D.P., Giles, G.G., Gurrin, L.C., Thomas, P.S., Hopper, J.L., Wood-Baker, R., Thompson, B.R., Feather, I.H., Vermeulen, R., Kromhout, H., Walters, E.H., Abramson, M.J., Matheson, M.C., Alif, S.M., Dharmage, S.C., Benke, G., Dennekamp, M., Burgess, J.L., Perret, Lodge, C.J., Morrison, S., Johns, D.P., Giles, G.G., Gurrin, L.C., Thomas, P.S., Hopper, J.L., Wood-Baker, R., Thompson, B.R., Feather, I.H., Vermeulen, R., Kromhout, H., Walters, E.H., Abramson, M.J., and Matheson, M.C.

Abstract

peer-reviewed, Our study is the first to investigate the associations between exposures to solvents and metals using lifetime work history calendars and fixed airflow obstruction (AO). We have shown that increasing cumulative exposure-unit years to chlorinated solvents is associated with fixed AO. We found that women were at increased risk of fixed AO with increasing cumulative exposed-unit-years to chlorinated solvents but not men.

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