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1. Multidisciplinary team discussion: the emerging gold standard for management of cardiopulmonary complications of connective tissue disease

Author

Fairley, JL, Ross, L, Burns, A, Prior, D, Conron, M, Rouse, H, McDonald, J, MacIsaac, A, La Gerche, A, Morrisroe, K, Ferdowsi, N, Quinlivan, A, Brown, Z, Stevens, W, Nikpour, M, Fairley, JL, Ross, L, Burns, A, Prior, D, Conron, M, Rouse, H, McDonald, J, MacIsaac, A, La Gerche, A, Morrisroe, K, Ferdowsi, N, Quinlivan, A, Brown, Z, Stevens, W, and Nikpour, M

Abstract

Cardiopulmonary complications of connective tissue diseases (CTDs), particularly pulmonary arterial hypertension (PAH) and interstitial lung disease (ILD), are major determinants of morbidity and mortality. Multidisciplinary meetings may improve diagnostic accuracy and optimise treatment. We review the literature regarding multidisciplinary meetings in CTD-ILD and PAH and describe our tertiary centre experience of the role of the multidisciplinary meeting in managing CTD-PAH.

Published
2023

2. Improving outcomes in lung cancer: the value of the multidisciplinary health care team

Author

Denton E and Conron M

Subjects
Lung cancer, multidisciplinary care, mortality, tumor board, quality of life, Medicine (General), R5-920
Abstract

Eve Denton,1 Matthew Conron2 1Allergy, Immunology and Respiratory Department, Alfred Hospital, 2Department of Respiratory and Sleep Medicine, St Vincent's Hospital, Melbourne, VIC, Australia Abstract: Lung cancer is a major worldwide health burden, with high disease-related morbidity and mortality. Unlike other major cancers, there has been little improvement in lung cancer outcomes over the past few decades, and survival remains disturbingly low. Multidisciplinary care is the cornerstone of lung cancer treatment in the developed world, despite a relative lack of evidence that this model of care improves outcomes. In this article, the available literature concerning the impact of multidisciplinary care on key measures of lung cancer outcomes is reviewed. This includes the limited observational data supporting improved survival with multidisciplinary care. The impact of multidisciplinary care on other benchmark measures of quality lung cancer treatment is also examined, including staging accuracy, access to diagnostic investigations, improvements in clinical decision making, better utilization of radiotherapy and palliative care services, and improved quality of life for patients. Health service research suggests that multidisciplinary care improves care coordination, leading to a better patient experience, and reduces variation in care, a problem in lung cancer management that has been identified worldwide. Furthermore, evidence suggests that the multidisciplinary model of care overcomes barriers to treatment, promotes standardized treatment through adherence to guidelines, and allows audit of clinical services and for these reasons is more likely to provide quality care for lung cancer patients. While there is strengthening evidence suggesting that the multidisciplinary model of care contributes to improvements in lung cancer outcomes, more quality studies are needed. Keywords: lung cancer, multidisciplinary care, mortality, tumor board, quality of life

Published
2016

3. EP14.05-016 Patterns of Care for Small Cell Lung Cancer in Victoria Australia. A Prospective Population-Based Observational Study

Author

Huang, J., primary, Faisal, W., additional, Brand, M., additional, Smith, S., additional, Alexander, M., additional, Conron, M., additional, Duffy, M., additional, Briggs, L., additional, Lesage, J., additional, Philip, J., additional, John, T., additional, Samuel, E., additional, MacManus, M., additional, Mitchell, P., additional, Olesen, I., additional, Parente, P., additional, Underhill, C., additional, Zalcberg, J., additional, Harden, S., additional, and Stirling, R., additional

Published
2022
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4. The Victorian Lung Cancer Registry Pilot: Improving the Quality of Lung Cancer Care Through the Use of a Disease Quality Registry

Author

Stirling, Rob G., Evans, S. M., McLaughlin, P., Senthuren, M., Millar, J., Gooi, J., Irving, L., Mitchell, P., Haydon, A., Ruben, J., Conron, M., Leong, T., Watkins, N., and McNeil, J. J.

Subjects
Lung cancer -- Research -- Diagnosis -- Genetic aspects -- Patient outcomes -- Care and treatment, Medical care -- Quality management, Health
Abstract

Background Lung cancer remains a major disease burden in Victoria (Australia) and requires a complex and multidisciplinary approach to ensure optimal care and outcomes. To date, no uniform mechanism is available to capture standardized population-based outcomes and thereby provide benchmarking. The establishment of such a data platform is, therefore, a primary requisite to enable description of process and outcome in lung cancer care and to drive improvement in the quality of care provided to individuals with lung cancer. Materials and Methods A disease quality registry pilot has been established to capture prospective data on all adult patients with clinical or tissue diagnoses of small cell and non-small cell lung cancer. Steering and management committees provide clinical governance and supervise quality indicator selection. Quality indicators were selected following extensive literature review and evaluation of established clinical practice guidelines. A minimum dataset has been established and training and data capture by data collectors is facilitated using a web-based portal. Case ascertainment is established by regular institutional reporting of ICD-10 discharge coding. Recruitment is optimized by provision of opt-out consent. Results The collection of a standardized minimum data set optimizes capacity for harmonized population-based data capture. Data collection has commenced in a variety of settings reflecting metropolitan and rural, and public, and private health care institutions. The data set provides scope for the construction of a risk-adjusted model for outcomes. A data access policy and a mechanism for escalation policy for outcome outliers has been established. Conclusions The Victorian Lung Cancer Registry provides a unique capacity to provide and confirm quality assessment in lung cancer and to drive improvement in quality of care across multidisciplinary stakeholders., Author(s): Rob G. Stirling[sup.1] [sup.2] , S. M. Evans[sup.2] , P. McLaughlin[sup.2] , M. Senthuren[sup.2] , J. Millar[sup.3] , J. Gooi[sup.4] , L. Irving[sup.5] , P. Mitchell[sup.6] , A. Haydon[sup.7] [...]

Published
2014
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5. Lessons Learned from the Victorian Lung Cancer Registry: Opportunities for Quality Improvement in Lung Cancer Management and Outcomes

Author

Stirling, R., Brand, M., Earnest, A., Antippa, P., Ball, D., Bartlett, J., Blum, R., Briggs, L., Caldecott, M., Conron, M., Jennings, B., Langton, D., Millar, J., Mitchell, P., Olesen, I., Parente, P., Richardson, G., See, K., Torres, J., Underhill, C., Wright, G., Stenger, M., Mcneil, J., and Zalcberg, J.

Subjects
clinical quality registry, population health, quality improvement
Published
2021
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6. Thunderstorm asthma in seasonal allergic rhinitis: The TAISAR study.

Author

Douglass J.A., Lodge C., Chan S., Doherty A., Tan J.A., Jin C., Stewart A., Southcott A.M., Gillman A., Lee J., Csutoros D., Hannan L., Ruane L., Barnes S., Irving L., Harun N.-S., Lachapelle P., Spriggs K., Sutherland M., See K., McDonald C.F., Conron M., Radhakrishna N., Worsnop C., Johnston F.H., Davies J.M., Bryant V., Iles L., Ranson D., Spanos P., Vicendese D., Lowe A., Newbigin E.J., Bardin P., Dharmage S., Douglass J.A., Lodge C., Chan S., Doherty A., Tan J.A., Jin C., Stewart A., Southcott A.M., Gillman A., Lee J., Csutoros D., Hannan L., Ruane L., Barnes S., Irving L., Harun N.-S., Lachapelle P., Spriggs K., Sutherland M., See K., McDonald C.F., Conron M., Radhakrishna N., Worsnop C., Johnston F.H., Davies J.M., Bryant V., Iles L., Ranson D., Spanos P., Vicendese D., Lowe A., Newbigin E.J., Bardin P., and Dharmage S.

Abstract

Background: Asthma epidemics associated with thunderstorms have had catastrophic effects on individuals and emergency services. Seasonal allergic rhinitis (SAR) is present in the vast majority of people who develop thunderstorm asthma (TA), but there is little evidence regarding risk factors for TA among the SAR population. Objective(s): We sought to identify risk factors for a history of TA and hospital presentation in a cohort of individuals with SAR. Method(s): This multicenter study recruited adults from Melbourne, Australia, with a past diagnosis of TA and/or self-reported SAR. Clinical information, spirometry results, white blood cell count, ryegrass pollen-specific (RGP-sp) IgE concentration, and fractional exhaled nitric oxide were measured to identify risk factors for a history of TA in individuals with SAR. Result(s): From a total of 228 individuals with SAR, 35% (80 of 228) reported SAR only (the I-SAR group), 37% (84 of 228) reported TA symptoms but had not attended hospital for treatment (the O-TA group), and 28% (64 of 228) had presented to the hospital for TA (the H-TA group). All patients in the H-TA group reported a previous asthma diagnosis. Logistic regression analysis of factors associated with O-TA and H-TA indicated that lower FEV1 value and an Asthma Control Questionnaire score higher than 1.5 were associated with H-TA. Higher blood RGP-sp IgE concentration, eosinophil counts, and fractional exhaled nitric oxide level were significantly associated with both O-TA and H-TA. Receiver operating curve analysis showed an RGP-sp IgE concentration higher than 10.1 kU/L and a prebronchodilator FEV1 value of 90% or lower to be biomarkers of increased H-TA risk. Conclusion(s): Clinical tests can identify risk of a history of TA in individuals with SAR and thereby inform patient-specific treatment recommendations.Copyright © 2021

Published
2021

7. Excess mortality and undertreatment in elderly lung cancer patients: treatment nihilism in the modern era?

Author

Pham, J, Conron, M, Wright, G, Mitchell, P, Ball, D, Philip, J, Brand, M, Zalcberg, J, Stirling, RG, Pham, J, Conron, M, Wright, G, Mitchell, P, Ball, D, Philip, J, Brand, M, Zalcberg, J, and Stirling, RG

Abstract

Treatment of elderly patients with lung cancer is significantly hindered by concerns about treatment tolerability, toxicity and limited clinical trial data in the elderly; potentially giving rise to treatment nihilism amongst clinicians. This study aims to describe survival in elderly patients with lung cancer and explore potential causes for excess mortality. Patients diagnosed with lung cancer in the Victorian Lung Cancer Registry between 2011-2018 were analysed (n=3481). Patients were age-categorised and compared using Cox-regression modelling to determine mortality risk, after adjusting for confounding. Probability of being offered cancer treatments was also determined, further stratified by disease stage. The eldest patients (≥80 years old) had significantly shorter median survival compared with younger age groups (<60 years: 2.0 years; 60-69 years: 1.5 years; 70-79 years: 1.6 years; ≥80 years: 1.0 years; p<0.001). Amongst those diagnosed with stage 1 or 2 lung cancer, there was no significant difference in adjusted-mortality between age groups. However, in those diagnosed with stage 3 or 4 disease, the eldest patients had an increased adjusted-mortality risk of 28% compared with patients younger than 60 years old (p=0.005), associated with markedly reduced probability of cancer treatment, after controlling for sex, performance status, comorbidities and histology type (OR 0.24, compared with <60 years old strata; p<0.001). Compared to younger patients, older patients with advanced-stage lung cancer have a disproportionately higher risk of mortality and lower likelihood of receiving cancer treatments, even when performance status and comorbidity are equivalent. These healthcare inequities could be indicative of widespread treatment nihilism towards elderly patients.

Published
2021

8. Outcomes following resection of non-small cell lung cancer in octogenarians.

Author

Steinfort D.P., Vazirani J., Moraes J., Barnett S., Johnson D.F., Knight S., Miller A., Wright G., Alam N.Z., Conron M., Irving L.B., Antippa P., Steinfort D.P., Vazirani J., Moraes J., Barnett S., Johnson D.F., Knight S., Miller A., Wright G., Alam N.Z., Conron M., Irving L.B., and Antippa P.

Abstract

BACKGROUND: The treatment of choice for early stage non-small cell lung cancer (NSCLC) is surgical resection. Little is known about the short- and long-term outcomes among very elderly patients. We sought to determine predictors of short- and long-term survival among octogenarians undergoing curative-intent resection for NSCLC in Victoria, Australia. METHOD(S): We retrospectively reviewed data from all patients aged >=80 years who underwent curative-intent resection for NSCLC over 12years (January 2005-December 2016) across five tertiary centres. We examined effect of age, stage of disease, extent of surgery and lung function on short- and long-term survival. RESULT(S): Two hundred patients aged >=80 years underwent curative-intent resections. Mortality at 30 and 120days was 2.9% and 5.9%, respectively. Increased early mortality was observed among those >=83years, at 30days (6.8% versus 0.8%, P = 0.044) and 120days (12.2% versus 2.3%, P = 0.0096). Early mortality was highest among patients >=83years requiring lobectomy, compared to sub-lobar resection at 120days (17% versus 3.8%, P = 0.019). Long-term survival was predicted by age and stage of disease. Among patients with Stage I disease aged <83years, lobectomy was associated with superior 5-year survival, compared to sub-lobar resection (83% versus 61%, P = 0.02). CONCLUSION(S): In carefully selected elderly patients undergoing curative-intent resection of early stage NSCLC, both short- and long-term outcomes appear consistent with younger historical cohorts. Early mortality was associated with lobectomy in those with advanced age. Older patients undergoing lobectomy appeared to be at highest risk for early mortality, while younger patients with Stage I disease undergoing at least lobectomy appear to have the best long-term survival.Copyright © 2018 Royal Australasian College of Surgeons.

Published
2020

9. OA05.06 Lessons Learned from the Victorian Lung Cancer Registry: Opportunities for Quality Improvement in Lung Cancer Management and Outcomes

Author

Stirling, R., primary, Brand, M., additional, Earnest, A., additional, Antippa, P., additional, Ball, D., additional, Bartlett, J., additional, Blum, R., additional, Briggs, L., additional, Caldecott, M., additional, Conron, M., additional, Jennings, B., additional, Langton, D., additional, Millar, J., additional, Mitchell, P., additional, Olesen, I., additional, Parente, P., additional, Richardson, G., additional, See, K., additional, Torres, J., additional, Underhill, C., additional, Wright, G., additional, Stenger, M., additional, Mcneil, J., additional, and Zalcberg, J., additional

Published
2021
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19. Predicting risk for thunderstorm asthma in patients with seasonal allergic rhinitis: The TAISAR study.

Author

Dharmage S.C., Lodge C., Stewart A.G., Newbigin E., Douglass J.A., Tan J.A., Jin C., Bardin P., Barnes S., Ruane L., Conron M., Gillman A., Hannan L.M., Harun N.S., Irving L., Johnston F.H., Lachapelle P., Lee J., Mcdonald C.F., Radhakrishna N., See K., Southcott A.M., Spriggs K., Worsnop C., Davies J.M., Dharmage S.C., Lodge C., Stewart A.G., Newbigin E., Douglass J.A., Tan J.A., Jin C., Bardin P., Barnes S., Ruane L., Conron M., Gillman A., Hannan L.M., Harun N.S., Irving L., Johnston F.H., Lachapelle P., Lee J., Mcdonald C.F., Radhakrishna N., See K., Southcott A.M., Spriggs K., Worsnop C., and Davies J.M.

Abstract

Background : Seasonal allergic rhinitis (SAR) is commonly reported by thunderstorm asthma (TA) patients and ryegrass pollen is implicated as causal. However, not all SAR patients in the community experience TA. On November 21, 2016 Melbourne (Victoria, Australia) experienced the largest recorded epidemic of thunderstorm asthma with 3300 emergency department presentations, 476 asthmarelated hospital admissions and ten fatalities. We hypothesize that the impact of such TA episodes may be mitigated by identifying susceptible individuals and providing them with preventative therapy. The aim of this study was to determine risk factors for TA in a cohort of SAR patients. Method : Adults with either a past diagnosis of TA or self- reported SAR were recruited (Melbourne Health ethics approval: 2018.270) into an ambispective cohort study conducted across six hospitals in Melbourne. Spirometry, skin prick testing to common aeroallergens, measurement of fractional exhaled nitric oxide (FeNO), blood eosinophil counts, total IgE and ryegrass- specific IgE levels were performed at study entry. Differences between cases (TA patients) and controls (self- reported SAR patients) were analysed using logistic regression. Results : Two hundred and twenty- seven patients were recruited between October and December 2018 (Melbourne spring season) of whom 106/223 (47.5%) reported SAR and 117/223 (52.5%) had a history of clinician- diagnosed TA. Preliminary data suggest that TA patients had significantly higher blood eosinophils, total IgE, ryegrass- specific IgE and FeNO levels than SAR patients ( P < 0.0001 for all variables). Each unit increase in ryegrass- specific IgE levels (1ku/L) was associated with 2.21 times increased odds of presenting to hospital with TA; Odds Ratio = 2.21; 95% CI 1.68, 2.91; P < 0.0001. Conclusion : Our findings suggest that ryegrass- specific IgE and FeNO measurements can help to identify individuals at risk of TA. Multivariate analyses are currently underway t

Published
2019

20. Recurrent lung nodules as a presentation of ventricular septal defect-related endocarditis

Author

Trytell, A, Darby, J, Conron, M, Newcomb, A, Burns, A, Trytell, A, Darby, J, Conron, M, Newcomb, A, and Burns, A

Abstract

Infective endocarditis is an uncommon microbial infection of the endocardial surface of the heart. Patients with structural heart disease, such as a ventricular septal defect, are at higher risk for infective endocarditis and clinicians must have a high index of suspicion in such patients presenting with recurrent fevers. We present a patient with a known ventricular septal defect presenting with recurrent fevers associated with migratory lung nodules following a "low-risk" dental procedure without antibiotic prophylaxis. The unusual presentation delayed the diagnosis of the migratory lung lesions as septic pulmonary emboli and consequentially the diagnosis of ventricular septal defect related infective endocarditis. The patient made an uneventful recovery following antibiotic therapy and surgical intervention.

Published
2019

21. The Victorian Comprehensive Cancer Centre lung cancer clinical audit: collecting the UK National Lung Cancer Audit data from hospitals in Australia

Author

Mileshkin, L, Dunn, C, Cross, H, Duffy, M, Shaw, M, Antippa, P, Mitchell, P, Akhurst, T, Conron, M, Moore, M, Philip, J, Bartlett, J, Emery, J, Zambello, B, Mileshkin, L, Dunn, C, Cross, H, Duffy, M, Shaw, M, Antippa, P, Mitchell, P, Akhurst, T, Conron, M, Moore, M, Philip, J, Bartlett, J, Emery, J, and Zambello, B

Abstract

BACKGROUND: Clinical audit may improve practice in cancer service provision. The UK National Lung Cancer Audit (NLCA) collects data for all new cases of thoracic cancers. AIM: To collect similar data for our Victorian patients from six hospitals within the Victorian Comprehensive Cancer Centre and associated Western and Central Melbourne Integrated Cancer Service. METHODS: We conducted a retrospective audit of all newly diagnosed patients with lung cancer and mesothelioma in 2013 across the six Victorian Comprehensive Cancer Centre/Western and Central Melbourne Integrated Cancer Service hospitals. The objectives were to adapt the NLCA data set for use in the Australian context, to analyse the findings using descriptive statistics and to determine feasibility of implementing a routine, ongoing audit similar to that in the UK. Individual data items were adapted from the NLCA by an expert steering committee. Data were collated from the Victorian Cancer Registry, Victorian Admitted Episodes Dataset and individual hospital databases. Individual medical records were audited for missing data. RESULTS: Eight hundred and forty-five patients were diagnosed across the sites in 2013. Most were aged 65-80 (55%) and were male (62%). Most had non-small-cell lung cancer (81%) with 9% diagnosed with small cell lung cancer and 2% with mesothelioma. Data completeness varied significantly between fields. For those with higher levels of completeness, headline indicators of clinical care were comparable with NLCA data. The Victorian population seem to lack access to specialist lung cancer nurse services. CONCLUSION: Lung cancer care at participating hospitals appeared to be comparable with the UK in 2013. In future, prospective data collection should be harmonised across sites and correlated with survival outcomes. One area of concern was a lack of documented access to specialist nursing services.

Published
2019

22. The 2016 Melbourne thunderstorm asthma epidemic: Risk factors for severe attacks requiring hospital admission

Author

Hew, M, Lee, J, Susanto, NH, Prasad, S, Bardin, PG, Barnes, S, Ruane, L, Southcott, AM, Gillman, A, Young, A, Rangamuwa, K, O'Hehir, RE, McDonald, C, Sutherland, M, Conron, M, Matthews, S, Harun, N-S, Lachapelle, P, Douglass, JA, Irving, L, Langton, D, Mann, J, Erbas, B, Thien, F, Hew, M, Lee, J, Susanto, NH, Prasad, S, Bardin, PG, Barnes, S, Ruane, L, Southcott, AM, Gillman, A, Young, A, Rangamuwa, K, O'Hehir, RE, McDonald, C, Sutherland, M, Conron, M, Matthews, S, Harun, N-S, Lachapelle, P, Douglass, JA, Irving, L, Langton, D, Mann, J, Erbas, B, and Thien, F

Abstract

BACKGROUND: The world's most catastrophic and deadly thunderstorm asthma epidemic struck Melbourne, Australia, on November 21, 2016. OBJECTIVE: Among thunderstorm-affected patients presenting to emergency rooms (ERs), we investigated risk factors predicting severe attacks requiring admission to hospital. METHODS: Thunderstorm-affected patients were identified from ER records at the eight major Melbourne health services and interviewed by telephone. Risk factors for hospital admission were analyzed. RESULTS: We interviewed 1435/2248 (64%) of thunderstorm-affected patients, of whom 164 (11.4%) required hospital admission. Overall, rhinitis was present in 87%, and current asthma was present in 28%. Odds for hospital admission were higher with increasing age (odds ratio 1.010, 95% CI 1.002, 1.019) and among individuals with current asthma (adjusted odds ratio [aOR] 1.87, 95% CI 1.26, 2.78). Prior hospitalization for asthma in the previous 12 months further increased the odds for hospital admission (aOR 3.16, 95% CI 1.63, 6.12). Among patients of Asian ethnicity, the odds for hospital admission were lower than for non-Asian patients (aOR 0.59, 95% CI 0.38, 0.94), but higher if born in Australia (OR = 5.42, 95% CI 1.56, 18.83). CONCLUSIONS: In epidemic thunderstorm asthma patients who presented to the ER, higher odds for hospital admission among patients with known asthma were further amplified by recent asthma admission, highlighting the vulnerability conferred by suboptimal disease control. Odds for hospital admission were lower in Asian patients born overseas, but higher in Asian patients born locally, than in non-Asian patients; these observations suggest susceptibility to severe thunderstorm asthma may be enhanced by gene-environment interactions.

Published
2019

23. Continued loss of asthma control following epidemic thunderstorm asthma

Author

Foo, CT, Yee, ELY, Young, A, Denton, E, Hew, M, O'Hehir, R, Radhakrishna, N, Matthews, S, Conron, M, Harun, N-S, Lachapelle, P, Douglass, JA, Irving, L, Lee, J, Stevenson, W, McDonald, CF, Langton, D, Banks, C, Thien, F, Foo, CT, Yee, ELY, Young, A, Denton, E, Hew, M, O'Hehir, R, Radhakrishna, N, Matthews, S, Conron, M, Harun, N-S, Lachapelle, P, Douglass, JA, Irving, L, Lee, J, Stevenson, W, McDonald, CF, Langton, D, Banks, C, and Thien, F

Abstract

BACKGROUND: Epidemic thunderstorm asthma (ETSA) severely affected Melbourne, Australia in November 2016. There is scant literature on the natural history of individuals affected by ETSA. OBJECTIVE: A multicentre 12-month prospective observational study was conducted assessing symptomatology and behaviors of ETSA-affected individuals. METHODS: We used a structured phone questionnaire to assess asthma symptom frequency, inhaled preventer use, asthma action plan ownership and healthcare utilization over 12 months since the ETSA. Analysis of results included subgroup analyses of the "current," "past," "probable," and "no asthma" subgroups defined according to their original 2016 survey responses. RESULTS: Four hundred forty-two questionnaires were analyzed. Eighty percent of individuals reported ongoing asthma symptoms at follow-up, of which 28% were affected by asthma symptoms at least once a week. Risk of persistent asthma symptoms was significantly higher in those with prior asthma diagnosis, current asthma, and probable undiagnosed asthma (all p < 0.01). Of 442 respondents, 53% were prescribed inhaled preventers, of which 51% were adherent at least 5 days a week. Forty-two percent had a written asthma action plan and 16% had sought urgent medical attention for asthma in the preceding year. CONCLUSIONS: Following an episode of ETSA, patients experience a pivotal change in asthma trajectory with both loss of asthma control and persistence of de novo asthma. Suboptimal rates of inhaled preventer adherence and asthma action plan ownership may contribute to asthma exacerbation risk and susceptibility to future ETSA episodes. Longer-term follow-up is needed to determine the extent and severity of this apparent change.

Published
2019

29. The Melbourne epidemic thunderstorm asthma event 2016: an investigation of environmental triggers, effect on health services, and patient risk factors.

Author

Dyett J., Thien F., Beggs P.J., Csutoros D., Darvall J., Hew M., Davies J.M., Bardin P.G., Bannister T., Bellomo R., Byrne T., Casamento A., Conron M., Cross A., Crosswell A., Douglass J.A., Durie M., Ebert E., Erbas B., French C., Gelbart B., Gillman A., Harun N.-S., Huete A., Irving L., Karalapillai D., Ku D., Lachapelle P., Langton D., Looker C., MacIsaac C., McCaffrey J., McDonald C.F., McGain F., Newbigin E., O'Hehir R., Pilcher D., Prasad S., Rangamuwa K., Ruane L., Sarode V., Silver J.D., Southcott A.M., Subramaniam A., Suphioglu C., Susanto N.H., Sutherland M.F., Taori G., Taylor P., Torre P., Vetro J., Wigmore G., Young A.C., Guest C., Barnes S., Lee J., Dyett J., Thien F., Beggs P.J., Csutoros D., Darvall J., Hew M., Davies J.M., Bardin P.G., Bannister T., Bellomo R., Byrne T., Casamento A., Conron M., Cross A., Crosswell A., Douglass J.A., Durie M., Ebert E., Erbas B., French C., Gelbart B., Gillman A., Harun N.-S., Huete A., Irving L., Karalapillai D., Ku D., Lachapelle P., Langton D., Looker C., MacIsaac C., McCaffrey J., McDonald C.F., McGain F., Newbigin E., O'Hehir R., Pilcher D., Prasad S., Rangamuwa K., Ruane L., Sarode V., Silver J.D., Southcott A.M., Subramaniam A., Suphioglu C., Susanto N.H., Sutherland M.F., Taori G., Taylor P., Torre P., Vetro J., Wigmore G., Young A.C., Guest C., Barnes S., and Lee J.

Abstract

Background: A multidisciplinary collaboration investigated the world's largest, most catastrophic epidemic thunderstorm asthma event that took place in Melbourne, Australia, on Nov 21, 2016, to inform mechanisms and preventive strategies. Method(s): Meteorological and airborne pollen data, satellite-derived vegetation index, ambulance callouts, emergency department presentations, and data on hospital admissions for Nov 21, 2016, as well as leading up to and following the event were collected between Nov 21, 2016, and March 31, 2017, and analysed. We contacted patients who presented during the epidemic thunderstorm asthma event at eight metropolitan health services (each including up to three hospitals) via telephone questionnaire to determine patient characteristics, and investigated outcomes of intensive care unit (ICU) admissions. Finding(s): Grass pollen concentrations on Nov 21, 2016, were extremely high (>100 grains/m3). At 1800 AEDT, a gust front crossed Melbourne, plunging temperatures 10degreeC, raising humidity above 70%, and concentrating particulate matter. Within 30 h, there were 3365 (672%) excess respiratory-related presentations to emergency departments, and 476 (992%) excess asthma-related admissions to hospital, especially individuals of Indian or Sri Lankan birth (10% vs 1%, p<0.0001) and south-east Asian birth (8% vs 1%, p<0.0001) compared with previous 3 years. Questionnaire data from 1435 (64%) of 2248 emergency department presentations showed a mean age of 32.0 years (SD 18.6), 56% of whom were male. Only 28% had current doctor-diagnosed asthma. 39% of the presentations were of Asian or Indian ethnicity (25% of the Melbourne population were of this ethnicity according to the 2016 census, relative risk [RR] 1.93, 95% CI 1.74-2.15, p <0.0001). Of ten individuals who died, six were Asian or Indian (RR 4.54, 95% CI 1.28-16.09; p=0.01). 35 individuals were admitted to an intensive care unit, all had asthma, 12 took inhaled preventers, and five died.

Published
2018

30. Outcomes following resection of non-small cell lung cancer in octogenarians

Author

Vazirani, J, Moraes, J, Barnett, S, Johnson, DF, Knight, S, Miller, A, Wright, G, Alam, NZ, Conron, M, Irving, LB, Antippa, P, Steinfort, DP, Vazirani, J, Moraes, J, Barnett, S, Johnson, DF, Knight, S, Miller, A, Wright, G, Alam, NZ, Conron, M, Irving, LB, Antippa, P, and Steinfort, DP

Abstract

BACKGROUND: The treatment of choice for early stage non-small cell lung cancer (NSCLC) is surgical resection. Little is known about the short- and long-term outcomes among very elderly patients. We sought to determine predictors of short- and long-term survival among octogenarians undergoing curative-intent resection for NSCLC in Victoria, Australia. METHODS: We retrospectively reviewed data from all patients aged ≥80 years who underwent curative-intent resection for NSCLC over 12 years (January 2005-December 2016) across five tertiary centres. We examined effect of age, stage of disease, extent of surgery and lung function on short- and long-term survival. RESULTS: Two hundred patients aged ≥80 years underwent curative-intent resections. Mortality at 30 and 120 days was 2.9% and 5.9%, respectively. Increased early mortality was observed among those ≥83 years, at 30 days (6.8% versus 0.8%, P = 0.044) and 120 days (12.2% versus 2.3%, P = 0.0096). Early mortality was highest among patients ≥83 years requiring lobectomy, compared to sub-lobar resection at 120 days (17% versus 3.8%, P = 0.019). Long-term survival was predicted by age and stage of disease. Among patients with Stage I disease aged <83 years, lobectomy was associated with superior 5-year survival, compared to sub-lobar resection (83% versus 61%, P = 0.02). CONCLUSION: In carefully selected elderly patients undergoing curative-intent resection of early stage NSCLC, both short- and long-term outcomes appear consistent with younger historical cohorts. Early mortality was associated with lobectomy in those with advanced age. Older patients undergoing lobectomy appeared to be at highest risk for early mortality, while younger patients with Stage I disease undergoing at least lobectomy appear to have the best long-term survival.

Published
2018

31. The Melbourne epidemic thunderstorm asthma event 2016: an investigation of environmental triggers, effect on health services, and patient risk factors.

Author

Thien, F, Beggs, PJ, Csutoros, D, Darvall, J, Hew, M, Davies, JM, Bardin, PG, Bannister, T, Barnes, S, Bellomo, R, Byrne, T, Casamento, A, Conron, M, Cross, A, Crosswell, A, Douglass, JA, Durie, M, Dyett, J, Ebert, E, Erbas, B, French, C, Gelbart, B, Gillman, A, Harun, N-S, Huete, A, Irving, L, Karalapillai, D, Ku, D, Lachapelle, P, Langton, D, Lee, J, Looker, C, MacIsaac, C, McCaffrey, J, McDonald, CF, McGain, F, Newbigin, E, O'Hehir, R, Pilcher, D, Prasad, S, Rangamuwa, K, Ruane, L, Sarode, V, Silver, JD, Southcott, AM, Subramaniam, A, Suphioglu, C, Susanto, NH, Sutherland, MF, Taori, G, Taylor, P, Torre, P, Vetro, J, Wigmore, G, Young, AC, Guest, C, Thien, F, Beggs, PJ, Csutoros, D, Darvall, J, Hew, M, Davies, JM, Bardin, PG, Bannister, T, Barnes, S, Bellomo, R, Byrne, T, Casamento, A, Conron, M, Cross, A, Crosswell, A, Douglass, JA, Durie, M, Dyett, J, Ebert, E, Erbas, B, French, C, Gelbart, B, Gillman, A, Harun, N-S, Huete, A, Irving, L, Karalapillai, D, Ku, D, Lachapelle, P, Langton, D, Lee, J, Looker, C, MacIsaac, C, McCaffrey, J, McDonald, CF, McGain, F, Newbigin, E, O'Hehir, R, Pilcher, D, Prasad, S, Rangamuwa, K, Ruane, L, Sarode, V, Silver, JD, Southcott, AM, Subramaniam, A, Suphioglu, C, Susanto, NH, Sutherland, MF, Taori, G, Taylor, P, Torre, P, Vetro, J, Wigmore, G, Young, AC, and Guest, C

Abstract

BACKGROUND: A multidisciplinary collaboration investigated the world's largest, most catastrophic epidemic thunderstorm asthma event that took place in Melbourne, Australia, on Nov 21, 2016, to inform mechanisms and preventive strategies. METHODS: Meteorological and airborne pollen data, satellite-derived vegetation index, ambulance callouts, emergency department presentations, and data on hospital admissions for Nov 21, 2016, as well as leading up to and following the event were collected between Nov 21, 2016, and March 31, 2017, and analysed. We contacted patients who presented during the epidemic thunderstorm asthma event at eight metropolitan health services (each including up to three hospitals) via telephone questionnaire to determine patient characteristics, and investigated outcomes of intensive care unit (ICU) admissions. FINDINGS: Grass pollen concentrations on Nov 21, 2016, were extremely high (>100 grains/m3). At 1800 AEDT, a gust front crossed Melbourne, plunging temperatures 10°C, raising humidity above 70%, and concentrating particulate matter. Within 30 h, there were 3365 (672%) excess respiratory-related presentations to emergency departments, and 476 (992%) excess asthma-related admissions to hospital, especially individuals of Indian or Sri Lankan birth (10% vs 1%, p<0·0001) and south-east Asian birth (8% vs 1%, p<0·0001) compared with previous 3 years. Questionnaire data from 1435 (64%) of 2248 emergency department presentations showed a mean age of 32·0 years (SD 18·6), 56% of whom were male. Only 28% had current doctor-diagnosed asthma. 39% of the presentations were of Asian or Indian ethnicity (25% of the Melbourne population were of this ethnicity according to the 2016 census, relative risk [RR] 1·93, 95% CI 1·74-2·15, p <0·0001). Of ten individuals who died, six were Asian or Indian (RR 4·54, 95% CI 1·28-16·09; p=0·01). 35 individuals were admitted to an intensive care unit, all had asthma, 12 took inhaled preventers, and five died. INTERPRE

Published
2018

32. Impact of sex on prognostic host factors in surgical patients with lung cancer

Author

Wainer, Z, Wright, GM, Gough, K, Daniels, MG, Choong, P, Conron, M, Russell, PA, Alam, NZ, Ball, D, Solomon, B, Wainer, Z, Wright, GM, Gough, K, Daniels, MG, Choong, P, Conron, M, Russell, PA, Alam, NZ, Ball, D, and Solomon, B

Abstract

BACKGROUND: Lung cancer has markedly poorer survival in men. Recognized important prognostic factors are divided into host, tumour and environmental factors. Traditional staging systems that use only tumour factors to predict prognosis are of limited accuracy. By examining sex-based patterns of disease-specific survival in non-small cell lung cancer patients, we determined the effect of sex on the prognostic value of additional host factors. METHODS: Two cohorts of patients treated surgically with curative intent between 2000 and 2009 were utilized. The primary cohort was from Melbourne, Australia, with an independent validation set from the American Surveillance, Epidemiology and End Results (SEER) database. Univariate and multivariate analyses of validated host-related prognostic factors were performed in both cohorts to investigate the differences in survival between men and women. RESULTS: The Melbourne cohort had 605 patients (61% men) and SEER cohort comprised 55 681 patients (51% men). Disease-specific 5-year survival showed men had statistically significant poorer survival in both cohorts (P < 0.001); Melbourne men at 53.2% compared with women at 68.3%, and SEER 53.3% men and 62.0% women were alive at 5 years. Being male was independently prognostic for disease-specific mortality in the Melbourne cohort after adjustment for ethnicity, smoking history, performance status, age, pathological stage and histology (hazard ratio = 1.54, 95% confidence interval: 1.10-2.16, P = 0.012). CONCLUSIONS: Sex differences in non-small cell lung cancer are important irrespective of age, ethnicity, smoking, performance status and tumour, node and metastasis stage. Epidemiological findings such as these should be translated into research and clinical paradigms to determine the factors that influence the survival disadvantage experienced by men.

Published
2017

34. Improving outcomes in lung cancer: the value of the multidisciplinary health care team.

Author

Denton, E, Conron, M, Denton, E, and Conron, M

Abstract

Lung cancer is a major worldwide health burden, with high disease-related morbidity and mortality. Unlike other major cancers, there has been little improvement in lung cancer outcomes over the past few decades, and survival remains disturbingly low. Multidisciplinary care is the cornerstone of lung cancer treatment in the developed world, despite a relative lack of evidence that this model of care improves outcomes. In this article, the available literature concerning the impact of multidisciplinary care on key measures of lung cancer outcomes is reviewed. This includes the limited observational data supporting improved survival with multidisciplinary care. The impact of multidisciplinary care on other benchmark measures of quality lung cancer treatment is also examined, including staging accuracy, access to diagnostic investigations, improvements in clinical decision making, better utilization of radiotherapy and palliative care services, and improved quality of life for patients. Health service research suggests that multidisciplinary care improves care coordination, leading to a better patient experience, and reduces variation in care, a problem in lung cancer management that has been identified worldwide. Furthermore, evidence suggests that the multidisciplinary model of care overcomes barriers to treatment, promotes standardized treatment through adherence to guidelines, and allows audit of clinical services and for these reasons is more likely to provide quality care for lung cancer patients. While there is strengthening evidence suggesting that the multidisciplinary model of care contributes to improvements in lung cancer outcomes, more quality studies are needed.

Published
2016

35. Reconciling Healthcare Professional and Patient Perspectives in the Development of Disease Activity and Response Criteria in Connective Tissue Disease Related Interstitial Lung Diseases

Author

Saketkoo, La, Mittoo, S, Frankel, S, Lesage, D, Sarver, C, Phillips, K, Strand, V, Matteson, El, OMERACT Baughman RP, Brown, Kk, Christmann, Rb, Dellaripa, P, Denton, Cp, Distler, O, Fischer, A, Flaherty, K, Huscher, D, Khanna, D, Kowal Bielecka, O, Merkel, Pa, Oddis, Cv, Pittrow, D, Sandorfi, N, Seibold, Jr, Swigris, J, Wells, A, Antoniou, K, Castelino, Fv, Christopher Stine, L, Collard, Hr, Cottin, V, Danoff, S, Hedlund, R, Highland, Kb, Hummers, L, Lynch, Da, Kim, Ds, Ryu, Jh, Miller, Fw, Nichols, K, Proudman, Sm, Richeldi, L, Shah, Aa, van den Assum, P, Aggarwal, R, Ainslie, G, Alkassab, F, Allanore, Y, Anderson, Me, Andonopoulos, Ap, Antin Ozerkis, D, Arrobas, A, Ascherman, Dp, Assassi, S, Baron, M, Bathon, Jm, Baughman, Rp, Behr, J, Beretta, L, Bingham, Co, Binnie, M, Birring, Ss, Boin, F, Bongartz, T, Bourdin, A, Bouros, D, Brasington, R, Bresser, P, Buch, Mh, Burge, Ps, Carmona, L, Carreira, Pe, Carvalho, Cr, Catoggio, Lj, Chan, Km, Chapman, J, Chatterjee, S, Chua, F, Chung, L, Conron, M, Corte, T, Cosgrove, G, Costabel, U, Cox, G, Crestani, B, Crofford, Lj, Csuka, Me, Curbelo, P, Czirják, L, Daniil, Z, D'Arsigny, Cl, Davis, Gs, de Andrade JA, Dellaripa, Pf, De Vuyst, P, Dempsey, Oj, Derk, Ct, Distler, J, Dixon, Wg, Downey, G, Doyle, Mk, Drent, M, Durairaj, L, Emery, P, Espinoza, Lr, Farge, D, Fathi, M, Fell, Cd, Fessler, Bj, Fitzgerald, Je, Flaherty, Kr, Foeldvari, I, Fox, Ga, Frech, Tm, Freitas, S, Furst, De, Gabrielli, A, García Vicuña, R, Georgiev, Ob, Gerbino, A, Gillisen, A, Gladman, Dd, Glassberg, M, Gochuico, Br, Gogali, A, Goh, Ns, Goldberg, A, Goldberg, Hj, Gourley, Mf, Griffing, L, Grutters, Jc, Gunnarsson, R, Hachulla, E, Hall, Fc, Harari, S, Herrick, Al, Herzog, El, Hesselstrand, R, Highland, K, Hirani, N, Hodgson, U, Hollingsworth, Hm, Homer, Rj, Hoyles, Rk, Hsu, Vm, Hubbard, Rb, Hunzelmann, N, Isasi, Me, Isasi, Es, Jacobsen, S, Jimenez, Sa, Johnson, Sr, Jones, Ch, Kahaleh, B, Kairalla, Ra, Kalluri, M, Kalra, S, Kaner, Rj, Kinder, Bw, Kiter, G, Klingsberg, Rc, Kokosi, M, Kolb, Mr, Kowal Bielecka OM, Kur Zalewska, J, Kuwana, M, Lake, Fr, Lally, Ev, Lasky, Ja, Laurindo, Im, Able, L, Lee, P, Leonard, Ct, Lien, Dc, Limper, Ah, Liossis, Sn, Lohr, Km, Loyd, Je, Lundberg, Ie, Mageto, Yn, Maher, Tm, Mahmud, Th, Manganas, H, Marie, I, Marras, Tk, Martinez, Ja, Martinez, Fj, Mathieu, A, Matucci Cerinic, M, Mayes, Md, Mckown, Km, Medsger, Ta, Meehan, Rt, Mendes, Ac, Meyer, Kc, Millar, Ab, Moğulkoc, N, Molitor, Ja, Morais, A, Mouthon, L, Müller, V, Müller Quernheim, J, Nadashkevich, O, Nador, R, Nash, P, Nathan, Sd, Navarro, C, Neves, S, Noth, I, Nunes, H, Olson, Al, Opitz, Cf, Padilla, M, Pappas, D, Parfrey, H, Pego Reigosa JM, Pereira, Ca, Perez, R, Pope, Je, Porter, Jc, Renzoni, Ea, Riemekasten, G, Riley, Dj, Rischmueller, M, Rodriguez Reyna TS, Rojas Serrano, J, Roman, J, Rosen, Gd, Rossman, M, Rothfield, N, Sahn, Sa, Sanduzzi, A, Scholand, Mb, Selman, M, Senécal, Jl, Seo, P, Shah, A, Silver, Rm, Solomon, Jj, Steen, V, Stevens, W, Strange, C, Sussman, R, Sutton, Ed, Sweiss, Nj, Tornling, G, Tzelepis, Ge, Undurraga, A, Vacca, A, Vancheri, Carlo, Varga, J, Veale, Dj, Volkov, S, Walker, Ua, Wells, Au, Wencel, M, Wesselius, Lj, Wickremasinghe, M, Wilcox, P, Wilsher, Ml, Wollheim, Fa, Wuyts, Wa, Yung, G, Zanon, P, Zappala, Cj, Groshong, Sd, Leslie, Ko, Myers, Jl, Padera, Rf, Desai, Sr, Goldin, J, Kazerooni, Ea, Klein, Js, and Keen, Kj

Subjects
Male, medicine.medical_specialty, Delphi Technique, Consensus Development Conferences as Topic, Health Personnel, Immunology, Context (language use), Disease, Severity of Illness Index, Article, Idiopathic pulmonary fibrosis, Rheumatology, medicine, Immunology and Allergy, Humans, Disease management (health), Intensive care medicine, Connective Tissue Diseases, Randomized Controlled Trials as Topic, business.industry, Interstitial lung disease, Disease Management, respiratory system, Focus Groups, medicine.disease, Comorbidity, Connective tissue disease, respiratory tract diseases, Clinical trial, Treatment Outcome, Patient Satisfaction, Physical therapy, Quality of Life, ÍNDICE DE GRAVIDADE DA DOENÇA, Interdisciplinary Communication, business, Lung Diseases, Interstitial
Abstract

Interstitial lung diseases (ILD), including those related to connective tissue disease (CTD), and idiopathic pulmonary fibrosis (IPF) carry high morbidity and mortality. Great efforts are under way to develop and investigate meaningful treatments in the context of clinical trials. However, efforts have been challenged by a lack of validated outcome measures and by inconsistent use of measures in clinical trials. Lack of consensus has fragmented effective use of strategies in CTD-ILD and IPF, with a history of resultant difficulties in obtaining agency approval of treatment interventions. Until recently, the patient perspective to determine domains and outcome measures in CTD-ILD and IPF had never been applied. Efforts described here demonstrate unequivocally the value and influence of patient involvement on core set development. Regarding CTD-ILD, this is the first OMERACT working group to directly address a manifestation/comorbidity of a rheumatic disease (ILD) as well as a disease not considered rheumatic (IPF). The OMERACT 11 proceedings of the CTD-ILD Working Group describe the forward and lateral process to include both the medical and patient perspectives in the urgently needed identification of a core set of preliminary domains and outcome measures in CTD-ILD and IPF.

Published
2014

36. Connective tissue disease related interstitial lung diseases and idiopathic pulmonary fibrosis: Provisional core sets of domains and instruments for use in clinical trials

Author

Saketkoo, La, Mittoo, S, Huscher, D, Khanna, D, Dellaripa, Pf, Distler, O, Flaherty, Kr, Frankel, S, Oddis, Cv, Denton, Cp, Fischer, A, Kowal Bielecka OM, Lesage, D, Merkel, Pa, Phillips, K, Pittrow, D, Swigris, J, Antoniou, K, Baughman, Rp, Castelino, Fv, Christmann, Rb, Christopher Stine, L, Collard, Hr, Cottin, V, Danoff, S, Highland, Kb, Hummers, L, Shah, Aa, Kim, Ds, Lynch, Da, Miller, Fw, Proudman, Sm, Richeldi, L, Ryu, Jh, Sandorfi, N, Sarver, C, Wells, Au, Strand, V, Matteson, El, Brown, Kk, Seibold, Jr, Aggarwal, R, Ainslie, G, Alkassab, F, Allanore, Y, Descartes, P, Anderson, Me, Andonopoulos, Ap, Antin Ozerkis, D, Arrobas, A, Ascherman, Dp, Assassi, S, Baron, M, Bathon, Jm, Behr, J, Beretta, L, Bingham, Co, Binnie, M, Birring, Ss, Boin, F, Bongartz, T, Bourdin, A, Bouros, D, Brasington, R, Bresser, P, Buch, Mh, Burge, Ps, Carmona, L, Carreira, Pe, Carvalho, Cr, Catoggio, Lj, Chan, Km, Chapman, J, Chatterjee, S, Chua, F, Chung, L, Conron, M, Corte, T, Cosgrove, G, Costabel, U, Cox, G, Crestani, B, Crofford, Lj, Csuka, Me, Curbelo, P, László, C, Daniil, Z, D'Arsigny, Cl, Davis, Gs, de Andrade JA, De Vuyst, P, Dempsey, Oj, Derk, Ct, Distler, J, Dixon, Wg, Downey, G, Doyle, Mk, Drent, M, Durairaj, L, Emery, P, Espinoza, Lr, Farge, D, Fathi, M, Fell, Cd, Fessler, Bj, Fitzgerald, Je, Fox, Ga, Foeldvari, I, Frech, Tm, Freitas, S, Furst, De, Gabrielli, A, García Vicuña, R, Georgiev, Ob, Gerbino, A, Gillisen, A, Gladman, Dd, Glassberg, M, Gochuico, Br, Gogali, A, Goh, Ns, Goldberg, A, Goldberg, Hj, Gourley, Mf, Griffing, L, Grutters, Jc, Gunnarsson, R, Hachulla, E, Hall, Fc, Harari, S, Herrick, Al, Herzog, El, Hesselstrand, R, Hirani, N, Hodgson, U, Hollingsworth, Hm, Homer, Rj, Hoyles, Rk, Hsu, Vm, Hubbard, Rb, Hunzelmann, N, Isasi, Me, Isasi, Es, Jacobsen, S, Jimenez, Sa, Johnson, Sr, Jones, Ch, Kahaleh, B, Kairalla, Ra, Kalluri, M, Kalra, S, Kaner, Rj, Kinder, Bw, Klingsberg, Rc, Kokosi, M, Kolb, Mr, Kur Zalewska, J, Kuwana, M, Lake, Fr, Lally, Ev, Lasky, Ja, Laurindo, Im, Able, L, Lee, P, Leonard, Ct, Lien, Dc, Limper, Ah, Liossis, Sn, Lohr, Km, Loyd, Je, Lundberg, Ie, Mageto, Yn, Maher, Tm, Mahmud, Th, Manganas, H, Marie, I, Marras, Tk, Antônio Baddini Martinez, J, Martinez, Fj, Mathieu, A, Matucci Cerinic, M, Mayes, Md, Mckown, Km, Medsger, Ta, Meehan, Rt, Cristina, Ma, Meyer, Kc, Millar, Ab, Moğulkoc, N, Molitor, Ja, Morais, A, Luc Mouthon, P, Müller, V, Müller Quernheim, J, Nadashkevich, O, Nador, R, Nash, P, Nathan, Sd, Navarro, C, Neves, S, Noth, I, Nunes, H, Olson, Al, Opitz, Cf, Padilla, M, Pappas, D, Parfrey, H, Pego Reigosa JM, Pereira, Ca, Perez, R, Pope, Je, Porter, Jc, Renzoni, Ea, Riemekasten, G, Riley, Dj, Rischmueller, M, Rodriguez Reyna TS, Rojas, Serrano, Roman, J, Rosen, Gd, Rossman, M, Rothfield, N, Sahn, Sa, Sanduzzi, A, Scholand, Mb, Selman, M, Senécal, Jl, Seo, P, Silver, Rm, Solomon, Jj, Steen, V, Stevens, W, Strange, C, Sussman, R, Sutton, Ed, Sweiss, Nj, Tornling, G, Tzelepis, Ge, Undurraga, A, Vacca, A, Vancheri, Carlo, Varga, J, Veale, Dj, Volkov, S, Walker, Ua, Wencel, M, Wesselius, Lj, Wickremasinghe, M, Wilcox, P, Wilsher, Ml, Wollheim, Fa, Wuyts, Wa, Yung, G, Zanon, P, Zappala, Cj, Groshong, Sd, Leslie, Ko, Myers, Jl, Padera, Rf, Desai, Sr, Goldin, J, Kazerooni, Ea, Klein, Js, Cenac, Sl, Grewal, Hk, Christensen, Am, Ferguson, S, Tran, M, Keen, K. J., Costabel, Ulrich (Beitragende*r), Raynauds & Scleroderma Association, Arthritis Research UK, The Scleroderma Society, and British Lung Foundation

Subjects
Lung Diseases, Connective tissue disease associated lung disease, CTD-ILD Special Interest Group, International Cooperation, Respiratory System, Medizin, Rheumatoid lung disease, Idiopathic pulmonary fibrosis, Quality of life, QUALITY-OF-LIFE, CYCLOPHOSPHAMIDE, SCLERODERMA LUNG, Registries, Connective Tissue Diseases, Societies, Medical, Randomized Controlled Trials as Topic, Interstitial lung disease, respiratory system, Connective tissue disease, Interstitial Fibrosis, medicine.anatomical_structure, Life Sciences & Biomedicine, Pulmonary and Respiratory Medicine, medicine.medical_specialty, Consensus, Clinical Sciences, END-POINT, Interstitial Lung Disease, Systemic disease and lungs, Medical, medicine, Humans, ENSAIO CLÍNICO CONTROLADO RANDOMIZADO, VALIDITY, Intensive care medicine, Lung, Science & Technology, COUGH, business.industry, Clinical study design, MORTALITY, SYSTEMIC-SCLEROSIS, 1103 Clinical Sciences, Congresses as Topic, medicine.disease, GEORGES RESPIRATORY QUESTIONNAIRE, respiratory tract diseases, Clinical trial, IPF, Physical therapy, Interstitial, Societies, business, Lung Diseases, Interstitial
Abstract

Rationale: Clinical trial design in interstitial lung diseases (ILDs) has been hampered by lack of consensus on appropriate outcome measures for reliably assessing treatment response. In the setting of connective tissue diseases (CTDs), some measures of ILD disease activity and severity may be confounded by non-pulmonary comorbidities. Methods: The Connective Tissue Disease associated Interstitial Lung Disease (CTD-ILD) working group of Outcome Measures in Rheumatology-a non-profit international organisation dedicated to consensus methodology in identification of outcome measures-conducted a series of investigations which included a Delphi process including >248 ILD medical experts as well as patient focus groups culminating in a nominal group panel of ILD experts and patients. The goal was to define and develop a consensus on the status of outcome measure candidates for use in randomised controlled trials in CTD-ILD and idiopathic pulmonary fibrosis (IPF). Results: A core set comprising specific measures in the domains of lung physiology, lung imaging, survival, dyspnoea, cough and health-related quality of life is proposed as appropriate for consideration for use in a hypothetical 1-year multicentre clinical trial for either CTD-ILD or IPF. As many widely used instruments were found to lack full validation, an agenda for future research is proposed. Conclusion: Identification of consensus preliminary domains and instruments to measure them was attained and is a major advance anticipated to facilitate multicentre RCTs in the field.

Published
2014
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39. EGFR gene copy number alterations are not a useful screening tool for predicting EGFR mutation status in lung adenocarcinoma

Author

Russell, PA, Yu, Y, Do, H, Clay, TD, Moore, MM, Wright, GM, Conron, M, Wainer, Z, Dobrovic, A, McLachlan, S-A, Russell, PA, Yu, Y, Do, H, Clay, TD, Moore, MM, Wright, GM, Conron, M, Wainer, Z, Dobrovic, A, and McLachlan, S-A

Abstract

We investigated if gene copy number (GCN) alterations of the epidermal growth factor receptor (EGFR), as detected by silver enhanced in situ hybridisation (SISH), could be used to select patients for EGFR mutation testing. Resected lung adenocarcinoma specimens with adequate tumour were identified. EGFR SISH was performed using the Ventana Benchmark Ultra platform. EGFR GCN was classified according to the Colorado Classification System. EGFR mutations were scanned by high resolution melting and confirmed by Sanger sequencing. Thirty-four of 96 tumours were EGFR SISH positive (35%), and 31 of 96 tumours harboured one or more EGFR mutations (32%). Of 31 EGFR-mutant tumours, 18 were EGFR SISH positive (58%). There was a statistically significant relationship between the presence of an EGFR mutation and EGFR GCN (p = 0.003). Thirteen of 31 EGFR-mutant tumours were EGFR SISH negative (42%), and 16 of 65 EGFR-wild type tumours were EGFR SISH positive (24%). The sensitivity, specificity, positive predictive value and negative predictive value were 58%, 75%, 52.9% and 79%, respectively. Despite a significant relationship between EGFR GCN alterations and EGFR mutations, our results indicate that EGFR GCN as detected by SISH is not a suitable way to select patients for EGFR mutation testing.

Published
2014

40. The Clinical Relevance of Pathologic Subtypes in Metastatic Lung Adenocarcinoma

Author

Clay, TD, Do, H, Sundararajan, V, Moore, MM, Conron, M, Wright, GM, McLachlan, S-A, Dobrovic, A, Russell, PA, Clay, TD, Do, H, Sundararajan, V, Moore, MM, Conron, M, Wright, GM, McLachlan, S-A, Dobrovic, A, and Russell, PA

Abstract

INTRODUCTION: The International Association for the Study of Lung Cancer/American Thoracic Society/European Respiratory Society classification of lung adenocarcinoma recommends identification of pathologic patterns in metastatic samples where possible. We investigated the clinical relevance of these patterns. METHODS: Patients with a surgical biopsy of lung adenocarcinoma from a metastatic site were included. Slides were reviewed by an anatomical pathologist identifying the histologic patterns of solid with mucin, acinar, micropapillary, papillary, and assigning a major adenocarcinoma subtype according to the International Association for the Study of Lung Cancer/American Thoracic Society/European Respiratory Society classification. EGFR and KRAS mutation testing were performed on formalin-fixed, paraffin-embedded blocks. Mutations were detected by high resolution melting assay with high resolution melting-positive samples confirmed by Sanger sequencing. RESULTS: One-hundred patients were included. The major histologic subtype prevalence was as follows: solid (50), acinar (29), micropapillary (20), and papillary (1). Of 100 patients, 45 received no systemic therapy with no overall survival differences seen by histologic subtype and 55 received systemic therapy (chemoradiotherapy with curative intent or palliative chemotherapy). Worse survival was seen in the major solid histologic subtype compared with major acinar (hazard ratio 0.32 [95% confidence interval 0.15-0.68], p = 0.003) and micropapillary subtypes (hazard ratio 0.34 [95% confidence interval, 0.17-0.69], p = 0.003). The major solid histologic subtype was less likely to harbor EGFR mutations (p = 0.006) and was less frequent in never smokers (p = 0.010) compared with other histologic subtypes. CONCLUSION: The major solid histologic subtype of lung adenocarcinoma at metastatic sites is associated with shorter overall survival on systemic anticancer therapy. Furthermore, the major solid histologic subtype is

Published
2014

41. The Victorian Lung Cancer Registry Pilot: Improving the Quality of Lung Cancer Care Through the Use of a Disease Quality Registry

Author

Stirling, RG, Evans, SM, McLaughlin, P, Senthuren, M, Millar, J, Gooi, J, Irving, L, Mitchell, P, Haydon, A, Ruben, J, Conron, M, Leong, T, Watkins, N, McNeil, JJ, Stirling, RG, Evans, SM, McLaughlin, P, Senthuren, M, Millar, J, Gooi, J, Irving, L, Mitchell, P, Haydon, A, Ruben, J, Conron, M, Leong, T, Watkins, N, and McNeil, JJ

Abstract

BACKGROUND: Lung cancer remains a major disease burden in Victoria (Australia) and requires a complex and multidisciplinary approach to ensure optimal care and outcomes. To date, no uniform mechanism is available to capture standardized population-based outcomes and thereby provide benchmarking. The establishment of such a data platform is, therefore, a primary requisite to enable description of process and outcome in lung cancer care and to drive improvement in the quality of care provided to individuals with lung cancer. MATERIALS AND METHODS: A disease quality registry pilot has been established to capture prospective data on all adult patients with clinical or tissue diagnoses of small cell and non-small cell lung cancer. Steering and management committees provide clinical governance and supervise quality indicator selection. Quality indicators were selected following extensive literature review and evaluation of established clinical practice guidelines. A minimum dataset has been established and training and data capture by data collectors is facilitated using a web-based portal. Case ascertainment is established by regular institutional reporting of ICD-10 discharge coding. Recruitment is optimized by provision of opt-out consent. RESULTS: The collection of a standardized minimum data set optimizes capacity for harmonized population-based data capture. Data collection has commenced in a variety of settings reflecting metropolitan and rural, and public, and private health care institutions. The data set provides scope for the construction of a risk-adjusted model for outcomes. A data access policy and a mechanism for escalation policy for outcome outliers has been established. CONCLUSIONS: The Victorian Lung Cancer Registry provides a unique capacity to provide and confirm quality assessment in lung cancer and to drive improvement in quality of care across multidisciplinary stakeholders.

Published
2014

42. Evaluation of relationship of cancer stem cell markers and risk of recurrence in early stage non small cell lung cancer.

Author

Russell P., Ganju V., Conron M., Wainer Z., Blake E., Alamgeer M., Brown T., Kumar B., Wright G.M., Russell P., Ganju V., Conron M., Wainer Z., Blake E., Alamgeer M., Brown T., Kumar B., and Wright G.M.

Abstract

Background: Current cancer treatment failure is due to a small population of slow-growing and drug resistant cells known as cancer stem cells (CSCs). Unlimited self-renewal and exclusive tumerogenicity are hypothesized to be the properties of stem cells responsible for relapse. In Vitro studies have proved that NSCLC cells expressing certain markers (CD44, CD 133 and ALDH 1) have stem cell properties. We aimed to investigate the expression of three cancer stem cell markers (CD44, CD133, ALDH 1) in NSCLC and evaluated their prognostic values for postoperative relapse and correlation with histological subtypes. Method(s): Tumours were obtained from 102 patients with stage 1 NSCLC (both Adenocarcinoma and SCC) who underwent surgical resection (1999-2008). Sequentially sampled paraffin sections were immunoprobed with antibodies for CD44standard, CD133 and ALDH 1 followed by reaction with DAB-conjugated secondary antibodies. All slides were scored by an independent pathologist in a blinded manner. Statistical analysis was conducted where correlations between CSC biomarker expression, histological subtypes and cancer recurrence rates was performed. Cumulative risks for developing recurrence of lung cancer after curative treatment of primary tumours was calculated using the Kaplan-Meier method and was compared between the groups using the log-rank test. Result(s): 102 pts with age range of 42-84 (median 68) underwent radical surgery and were pathologically staged as WHO stage1A (64) or 1B (38). Median follow up was 60 months (10-108) where follow up data was unavailable for 2 patients. Within the patient population 39% had relapsed; 31% had distant and 8% locoregional relapses where within these relaspses, 17/63 (23%) were Stage 1A and 22/37(59%) stage 1B. Analysis demonstrated a higher expression of CD44 in Squamous Cell Carcinoma (SCC) than Adenocarcinoma (ACA). Within the 102 stained sections, 53% in SCC vs. 24% in ACA were positive for CD44 (p=0.005) with 61% of positi

Published
2013

43. The prognostic significance of aldehyde dehydrogenase 1A1 (ALDH1A1) and CD133 expression in early stage non-small cell lung cancer.

Author

Watkins D.N., Prodanovic Z., Kumar B., Wainer Z., Brown T., Schneider-Kolsky M., Conron M., Wright G., Alamgeer M., Ganju V., Szczepny A., Russell P.A., Watkins D.N., Prodanovic Z., Kumar B., Wainer Z., Brown T., Schneider-Kolsky M., Conron M., Wright G., Alamgeer M., Ganju V., Szczepny A., and Russell P.A.

Abstract

Background Expression of aldehyde dehydrogenase 1A1 (ALDH1A1) and CD133 has been functionally associated with a stem cell phenotype in normal and malignant cells. The prevalence of such cells in solid tumours should therefore correlate with recurrence and/ or metastasis following definitive surgical resection. The aim of this study was to evaluate the prognostic significance of ALDH1A1 and CD133 in surgically resected, early stage non-small cell lung cancer (NSCLC). Methods A retrospective analysis of ALDH1A1 and CD133 expression in 205 patients with pathologic stage I NSCLC was performed using immunohistochemistry. The association between the expression of both markers and survival was determined. Results We identified 62 relapses and 58 cancer-related deaths in 144 stage 1A and 61 stage 1B patients, analysed at a median of 5-years follow-up. Overexpression of ALDH1A1 and CD133, detected in 68.7% and 50.7% of primary tumours, respectively, was an independent prognostic indicator for overall survival by multivariable Cox proportional hazard model (p=0.017 and 0.039, respectively). Overexpression of ALDH1A1, but not of CD133, predicted poor recurrence-free survival (p=0.025). When categorised into three groups according to expression of ALDH1A1/CD133, patients with overexpression of both ALDH1A1 and CD133 belonged to the group with the shortest recurrence-free and overall survival (p=0.015 and 0.017, respectively). Conclusions Expression of ALDH1A1 and CD133, and coexpression of ALDH1A1 and CD133, is strongly associated with poor survival in early-stage NSCLC following surgical resection. These data are consistent with the hypothesis that expression of stem cell markers correlates with recurrence as an indirect measure of selfrenewal capacity.

Published
2013

44. The prognostic significance of aldehyde dehydrogenase 1A1 (ALDH1A1) and CD133 expression in early stage non-small cell lung cancer

Author

Alamgeer, M, Ganju, V, Szczepny, A, Russell, PA, Prodanovic, Z, Kumar, B, Wainer, Z, Brown, T, Schneider-Kolsky, M, Conron, M, Wright, G, Watkins, DN, Alamgeer, M, Ganju, V, Szczepny, A, Russell, PA, Prodanovic, Z, Kumar, B, Wainer, Z, Brown, T, Schneider-Kolsky, M, Conron, M, Wright, G, and Watkins, DN

Abstract

BACKGROUND: Expression of aldehyde dehydrogenase 1A1 (ALDH1A1) and CD133 has been functionally associated with a stem cell phenotype in normal and malignant cells. The prevalence of such cells in solid tumours should therefore correlate with recurrence and/or metastasis following definitive surgical resection. The aim of this study was to evaluate the prognostic significance of ALDH1A1 and CD133 in surgically resected, early stage non-small cell lung cancer (NSCLC). METHODS: A retrospective analysis of ALDH1A1 and CD133 expression in 205 patients with pathologic stage I NSCLC was performed using immunohistochemistry. The association between the expression of both markers and survival was determined. RESULTS: We identified 62 relapses and 58 cancer-related deaths in 144 stage 1A and 61 stage 1B patients, analysed at a median of 5-years follow-up. Overexpression of ALDH1A1 and CD133, detected in 68.7% and 50.7% of primary tumours, respectively, was an independent prognostic indicator for overall survival by multivariable Cox proportional hazard model (p=0.017 and 0.039, respectively). Overexpression of ALDH1A1, but not of CD133, predicted poor recurrence-free survival (p=0.025). When categorised into three groups according to expression of ALDH1A1/CD133, patients with overexpression of both ALDH1A1 and CD133 belonged to the group with the shortest recurrence-free and overall survival (p=0.015 and 0.017, respectively). CONCLUSIONS: Expression of ALDH1A1 and CD133, and coexpression of ALDH1A1 and CD133, is strongly associated with poor survival in early-stage NSCLC following surgical resection. These data are consistent with the hypothesis that expression of stem cell markers correlates with recurrence as an indirect measure of self-renewal capacity.

Published
2013

45. Validity of the Assessment of Quality of Life (AQoL) utility instrument in patients with operable and inoperable lung cancer.

Author

McLachlan S.-A., Campbell D.A., Manser R.L., Wright G., Byrnes G., Hart D., Conron M., Carter R., McLachlan S.-A., Campbell D.A., Manser R.L., Wright G., Byrnes G., Hart D., Conron M., and Carter R.

Abstract

There have been few longitudinal studies of quality of life in patients with all stages of lung cancer, particularly those that have included measures of utility. The purpose of this study was to examine the psychometric properties of the Assessment of Quality of Life instrument (AQoL) in patients with lung cancer. The AQoL is a health-related quality of life questionnaire and provides a descriptive system for a multi-attribute utility instrument (MAU), so that scores can be used in cost-utility evaluations. In the present study the reliability (internal consistency) of the AQoL was examined and the concurrent validity was assessed using the Medical Outcomes 36-item Short Form Health Survey (SF-36) as the comparator instrument. The sensitivity to different health states of the AQoL and the responsiveness to change over time was also examined. A prospective, non-experimental cohort study was undertaken. Ninety-two participants with all stages of lung cancer were recruited from a tertiary multi-disciplinary lung cancer clinic. Ninety participants had non-small cell lung cancer (NSCLC) and two had limited stage small cell lung cancer. The AQOL and SF-36 surveys were administered concurrently at baseline. In patients with NSCLC the surveys were then repeated 3 and 6 months later. Correlations between the baseline AQoL summary scales and SF-36 summary scales support the divergent and convergent validity of the AQoL. Reliability was also found to be sufficient (Cronbach's Alpha = 0.76). In addition, in patients with inoperable NSCLC, baseline AQoL scores were found to be predictive of survival at 6 months in Cox proportional hazards multivariate analysis. However, the physical components summary score of the SF-36 was more sensitive to differences in health states between patients with different stages of NSCLC at 6 months of follow-up and more responsive to change over time in both operable and inoperable patients with NSCLC than the AQoL. The findings support the constr

Published
2012

46. Fibrosing alveolitis in systemic sclerosis: The need for early screening and treatment.

Author

Sahhar J., Conron M., Littlejohn G., Sahhar J., Conron M., and Littlejohn G.

Abstract

Abnormalities in lung function occur in 70% of patients with systemic sclerosis (SSc). Fibrosing alveolitis in SSc (FASSc) is more commonly seen in the diffuse cutaneous form of SSc, particularly in the presence of antitopoisomerase antibodies (Scl70), and with the decreasing incidence of scleroderma renal crisis it is now the major cause of mortality in this patient population. Screening of patients recently diagnosed with SSc by pulmonary function tests and the performance of high resolution computed tomography when physiological abnormalities are identified has resulted in the identification of significant numbers of patients with early, asymptomatic FASSc. Whether these patients should be further investigated with a surgical lung biopsy or receive immunosuppression is unclear, because it cannot yet be reliably predicted who will develop progressive disease and the evidence to support the efficacy of treatment is not strong. The objective of the present article was to review the evidence to support the use of immunosuppressive therapy in FASSc and, based on these data, to propose an algorithm for the investigation and management of this difficult clinical problem.

Published
2012

47. Integrated mutation, copy number and expression profiling in resectable non-small cell lung cancer

Author

Newnham, GM, Conron, M, McLachlan, S, Dobrovic, A, Do, H, Li, J, Opeskin, K, Thompson, N, Wright, GM, Thomas, DM, Newnham, GM, Conron, M, McLachlan, S, Dobrovic, A, Do, H, Li, J, Opeskin, K, Thompson, N, Wright, GM, and Thomas, DM

Abstract

BACKGROUND: The aim of this study was to identify critical genes involved in non-small cell lung cancer (NSCLC) pathogenesis that may lead to a more complete understanding of this disease and identify novel molecular targets for use in the development of more effective therapies. METHODS: Both transcriptional and genomic profiling were performed on 69 resected NSCLC specimens and results correlated with mutational analyses and clinical data to identify genetic alterations associated with groups of interest. RESULTS: Combined analyses identified specific patterns of genetic alteration associated with adenocarcinoma vs. squamous differentiation; KRAS mutation; TP53 mutation, metastatic potential and disease recurrence and survival. Amplification of 3q was associated with mutations in TP53 in adenocarcinoma. A prognostic signature for disease recurrence, reflecting KRAS pathway activation, was validated in an independent test set. CONCLUSIONS: These results may provide the first steps in identifying new predictive biomarkers and targets for novel therapies, thus improving outcomes for patients with this deadly disease.

Published
2011

49. High resolution melting analysis for the rapid and sensitive detection of mutations in clinical samples:: KRAS codon 12 and 13 mutations in non-small cell lung cancer

Author

Krypuy, M, Newnham, GM, Thomas, DM, Conron, M, Dobrovic, A, Krypuy, M, Newnham, GM, Thomas, DM, Conron, M, and Dobrovic, A

Abstract

BACKGROUND: The development of targeted therapies has created a pressing clinical need for the rapid and robust molecular characterisation of cancers. We describe here the application of high-resolution melting analysis (HRM) to screen for KRAS mutations in clinical cancer samples. In non-small cell lung cancer, KRAS mutations have been shown to identify a group of patients that do not respond to EGFR targeted therapies and the identification of these mutations is thus clinically important. METHODS: We developed a high-resolution melting (HRM) assay to detect somatic mutations in exon 2, notably codons 12 and 13 of the KRAS gene using the intercalating dye SYTO 9. We tested 3 different cell lines with known KRAS mutations and then examined the sensitivity of mutation detection with the cell lines using 189 bp and 92 bp amplicons spanning codons 12 and 13. We then screened for KRAS mutations in 30 non-small cell lung cancer biopsies that had been previously sequenced for mutations in EGFR exons 18-21. RESULTS: Known KRAS mutations in cell lines (A549, HCT116 and RPMI8226) were readily detectable using HRM. The shorter 92 bp amplicon was more sensitive in detecting mutations than the 189 bp amplicon and was able to reliably detect as little as 5-6% of each cell line DNA diluted in normal DNA. Nine of the 30 non-small cell lung cancer biopsies had KRAS mutations detected by HRM analysis. The results were confirmed by standard sequencing. Mutations in KRAS and EGFR were mutually exclusive. CONCLUSION: HRM is a sensitive in-tube methodology to screen for mutations in clinical samples. HRM will enable high-throughput screening of gene mutations to allow appropriate therapeutic choices for patients and accelerate research aimed at identifying novel mutations in human cancer.

Published
2006

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