Your search keyword '"Spencer, Lisa A."' showing total 12 results

1. Adaptive multi-interventional trial platform to improve patient care for fibrotic interstitial lung diseases

Author

Kawano-Dourado, Leticia, Kulkarni, Tejaswini, Ryerson, Christopher J, Rivera-Ortega, Pilar, Baldi, Bruno Guede, Chaudhuri, Nazia, Funke-Chambour, Manuela, Hoffmann-Vold, Anna-Maria, Johannson, Kerri A, Khor, Yet Hong, Montesi, Sydney B, Piccari, Lucilla, Prosch, Helmut, Molina-Molina, María, Sellares Torres, Jacobo, Bauer-Ventura, Iazsmin, Rajan, Sujeet, Jacob, Joseph, Richards, Duncan, Spencer, Lisa G, Wendelberger, Barbara, Jensen, Tom, Quintana, Melanie, Kreuter, Michael, Gordon, Anthony C, Martinez, Fernando J, Kaminski, Naftali, Cornelius, Victoria, Lewis, Roger, Adams, Wendy, Jenkins, Gisli, Richeldi, Luca, Richeldi, Luca (ORCID:0000-0001-8594-1448), Kawano-Dourado, Leticia, Kulkarni, Tejaswini, Ryerson, Christopher J, Rivera-Ortega, Pilar, Baldi, Bruno Guede, Chaudhuri, Nazia, Funke-Chambour, Manuela, Hoffmann-Vold, Anna-Maria, Johannson, Kerri A, Khor, Yet Hong, Montesi, Sydney B, Piccari, Lucilla, Prosch, Helmut, Molina-Molina, María, Sellares Torres, Jacobo, Bauer-Ventura, Iazsmin, Rajan, Sujeet, Jacob, Joseph, Richards, Duncan, Spencer, Lisa G, Wendelberger, Barbara, Jensen, Tom, Quintana, Melanie, Kreuter, Michael, Gordon, Anthony C, Martinez, Fernando J, Kaminski, Naftali, Cornelius, Victoria, Lewis, Roger, Adams, Wendy, Jenkins, Gisli, Richeldi, Luca, and Richeldi, Luca (ORCID:0000-0001-8594-1448)

Abstract

Background: Fibrotic interstitial lung diseases (fILDs) are a heterogeneous group of lung diseases associated with significant morbidity and mortality. Despite a large increase in the number of clinical trials in the last 10 years, current regulatory-approved management approaches are limited to two therapies that prevent the progression of fibrosis. The drug development pipeline is long and there is an urgent need to accelerate this process. This manuscript introduces the concept and design of an innovative research approach to drug development in fILD: a global Randomised Embedded Multifactorial Adaptive Platform in fILD (REMAP-ILD). Methods: Description of the REMAP-ILD concept and design: the specific terminology, design characteristics (multifactorial, adaptive features, statistical approach), target population, interventions, outcomes, mission and values, and organisational structure. Results: The target population will be adult patients with fILD, and the primary outcome will be a disease progression model incorporating forced vital capacity and mortality over 12 months. Responsive adaptive randomisation, prespecified thresholds for success and futility will be used to assess the effectiveness and safety of interventions. REMAP-ILD embraces the core values of diversity, equity, and inclusion for patients and researchers, and prioritises an open-science approach to data sharing and dissemination of results. Conclusion: By using an innovative and efficient adaptive multi-interventional trial platform design, we aim to accelerate and improve care for patients with fILD. Through worldwide collaboration, novel analytical methodology and pragmatic trial delivery, REMAP-ILD aims to overcome major limitations associated with conventional randomised controlled trial approaches to rapidly improve the care of people living with fILD.

Published

2024

2. Adaptive multi-interventional trial platform to improve patient care for fibrotic interstitial lung diseases

Author

Kawano-Dourado, Leticia; https://orcid.org/0000-0003-0784-1331, Kulkarni, Tejaswini; https://orcid.org/0000-0002-4251-4988, Ryerson, Christopher J, Rivera-Ortega, Pilar, Baldi, Bruno Guedes; https://orcid.org/0000-0002-9609-5117, Chaudhuri, Nazia, Funke-Chambour, Manuela, Hoffmann-Vold, Anna-Maria; https://orcid.org/0000-0001-6467-7422, Johannson, Kerri A; https://orcid.org/0000-0003-1205-5511, Khor, Yet Hong; https://orcid.org/0000-0002-5434-9342, Montesi, Sydney B, Piccari, Lucilla; https://orcid.org/0000-0002-2241-7523, Prosch, Helmut, Molina-Molina, María, Sellares Torres, Jacobo; https://orcid.org/0000-0001-6047-1670, Bauer-Ventura, Iazsmin, Rajan, Sujeet, Jacob, Joseph; https://orcid.org/0000-0002-8054-2293, Richards, Duncan; https://orcid.org/0000-0002-8093-7084, Spencer, Lisa G, Wendelberger, Barbara, Jensen, Tom, Quintana, Melanie, Kreuter, Michael, Gordon, Anthony C; https://orcid.org/0000-0002-0419-547X, Martinez, Fernando J, Kaminski, Naftali; https://orcid.org/0000-0001-5917-4601, Cornelius, Victoria, Lewis, Roger, Adams, Wendy, Jenkins, Gisli, Kawano-Dourado, Leticia; https://orcid.org/0000-0003-0784-1331, Kulkarni, Tejaswini; https://orcid.org/0000-0002-4251-4988, Ryerson, Christopher J, Rivera-Ortega, Pilar, Baldi, Bruno Guedes; https://orcid.org/0000-0002-9609-5117, Chaudhuri, Nazia, Funke-Chambour, Manuela, Hoffmann-Vold, Anna-Maria; https://orcid.org/0000-0001-6467-7422, Johannson, Kerri A; https://orcid.org/0000-0003-1205-5511, Khor, Yet Hong; https://orcid.org/0000-0002-5434-9342, Montesi, Sydney B, Piccari, Lucilla; https://orcid.org/0000-0002-2241-7523, Prosch, Helmut, Molina-Molina, María, Sellares Torres, Jacobo; https://orcid.org/0000-0001-6047-1670, Bauer-Ventura, Iazsmin, Rajan, Sujeet, Jacob, Joseph; https://orcid.org/0000-0002-8054-2293, Richards, Duncan; https://orcid.org/0000-0002-8093-7084, Spencer, Lisa G, Wendelberger, Barbara, Jensen, Tom, Quintana, Melanie, Kreuter, Michael, Gordon, Anthony C; https://orcid.org/0000-0002-0419-547X, Martinez, Fernando J, Kaminski, Naftali; https://orcid.org/0000-0001-5917-4601, Cornelius, Victoria, Lewis, Roger, Adams, Wendy, and Jenkins, Gisli

Abstract

BACKGROUND Fibrotic interstitial lung diseases (fILDs) are a heterogeneous group of lung diseases associated with significant morbidity and mortality. Despite a large increase in the number of clinical trials in the last 10 years, current regulatory-approved management approaches are limited to two therapies that prevent the progression of fibrosis. The drug development pipeline is long and there is an urgent need to accelerate this process. This manuscript introduces the concept and design of an innovative research approach to drug development in fILD: a global Randomised Embedded Multifactorial Adaptive Platform in fILD (REMAP-ILD). METHODS Description of the REMAP-ILD concept and design: the specific terminology, design characteristics (multifactorial, adaptive features, statistical approach), target population, interventions, outcomes, mission and values, and organisational structure. RESULTS The target population will be adult patients with fILD, and the primary outcome will be a disease progression model incorporating forced vital capacity and mortality over 12 months. Responsive adaptive randomisation, prespecified thresholds for success and futility will be used to assess the effectiveness and safety of interventions. REMAP-ILD embraces the core values of diversity, equity, and inclusion for patients and researchers, and prioritises an open-science approach to data sharing and dissemination of results. CONCLUSION By using an innovative and efficient adaptive multi-interventional trial platform design, we aim to accelerate and improve care for patients with fILD. Through worldwide collaboration, novel analytical methodology and pragmatic trial delivery, REMAP-ILD aims to overcome major limitations associated with conventional randomised controlled trial approaches to rapidly improve the care of people living with fILD.

Published

2024

3. Morphine for treatment of cough in idiopathic pulmonary fibrosis (PACIFY COUGH):a prospective, multicentre, randomised, double-blind, placebo-controlled, two-way crossover trial

Author

Wu, Zhe, Spencer, Lisa G., Banya, Winston, Westoby, John, Tudor, Veronica A., Rivera-Ortega, Pilar, Chaudhuri, Nazia, Jakupovic, Ira, Patel, Brijesh, Thillai, Muhunthan, West, Alex, Wijsenbeek, Marlies, Maher, Toby M., Smith, Jacky A., Molyneaux, Philip L., Wu, Zhe, Spencer, Lisa G., Banya, Winston, Westoby, John, Tudor, Veronica A., Rivera-Ortega, Pilar, Chaudhuri, Nazia, Jakupovic, Ira, Patel, Brijesh, Thillai, Muhunthan, West, Alex, Wijsenbeek, Marlies, Maher, Toby M., Smith, Jacky A., and Molyneaux, Philip L.

Abstract

Background: Idiopathic pulmonary fibrosis is a progressive fibrotic lung disease, with most patients reporting cough. Currently, there are no proven treatments. We examined the use of low dose controlled-release morphine compared with placebo as an antitussive therapy in individuals with idiopathic pulmonary fibrosis. Methods: The PACIFY COUGH study is a phase 2, multicentre, randomised, double-blind, placebo-controlled, two-way crossover trial done in three specialist centres in the UK. Eligible patients aged 40–90 years had a diagnosis of idiopathic pulmonary fibrosis within 5 years, self-reported cough (lasting >8 weeks), and a cough visual analogue scale (VAS) score of 30 mm or higher. Patients were randomly assigned (1:1) to placebo twice daily or controlled-release morphine 5 mg orally twice daily for 14 days followed by crossover after a 7-day washout period. Patients were randomised sequentially to a sequence group defining the order in which morphine and placebo were to be given, according to a computer-generated schedule. Patients, investigators, study nurses, and pharmacy personnel were masked to treatment allocation. The primary endpoint was percentage change in objective awake cough frequency (coughs per h) from baseline as assessed by objective digital cough monitoring at day 14 of treatment in the intention-to-treat population, which included all randomised participants. Safety data were summarised for all patients who took at least one study drug and did not withdraw consent. This study was registered at ClinicalTrials.gov, NCT04429516, and has been completed. Findings: Between Dec 17, 2020, and March 21, 2023, 47 participants were assessed for eligibility and 44 were enrolled and randomly allocated to treatment. Mean age was 71 (SD 7·4) years, and 31 (70%) of 44 participants were male and 13 (30%) were female. Lung function was moderately impaired; mean forced vital capacity (FVC) was 2·7 L (SD 0·76), mean predicted FVC was 82% (17·3), and mea

Published

2024

4. PAciFy Cough—a multicentre, double-blind, placebo-controlled, crossover trial of morphine sulphate for the treatment of pulmonary Fibrosis Cough

Author

Wu, Zhe, Banya, Winston, Chaudhuri, Nazia, Jakupovic, Ira, Maher, Toby M., Patel, Brijesh, Spencer, Lisa G., Thillai, Muhunthan, West, Alex, Westoby, John, Wijsenbeek, Marlies, Smith, Jaclyn, Molyneaux, Philip L., Wu, Zhe, Banya, Winston, Chaudhuri, Nazia, Jakupovic, Ira, Maher, Toby M., Patel, Brijesh, Spencer, Lisa G., Thillai, Muhunthan, West, Alex, Westoby, John, Wijsenbeek, Marlies, Smith, Jaclyn, and Molyneaux, Philip L.

Abstract

Background: Idiopathic pulmonary fibrosis (IPF) is a progressive disease that leads to lung scarring. Cough is reported by 85% of patients with IPF and can be a distressing symptom with a significant impact on patients’ quality of life. There are no proven effective therapies for IPF-related cough. Whilst morphine is frequently used as a palliative agent for breathlessness in IPF, its effects on cough have never been tested. PAciFy Cough is a multicenter, double-blind, placebo-controlled, crossover trial of morphine sulphate for the treatment of cough in IPF. Methods: We will recruit 44 subjects with IPF prospectively from three interstitial lung disease units in the UK, namely the Royal Brompton Hospital, Manchester University NHS Foundation Trust (MFT) and Aintree University Hospital NHS Foundation Trust. Patients will be randomised (1:1) to either placebo twice daily or morphine sulphate 5 mg twice daily for 14 days. They will then crossover after a 7-day washout period. The primary endpoint is the percent change in daytime cough frequency (coughs per hour) from baseline as assessed by objective cough monitoring at day 14 of treatment. Discussion: This multicentre, randomised trial will assess the effect of opioids on cough counts and cough associated quality of life in IPF subjects. If proven to be an effective intervention, it represents a readily available treatment for patients. Trial registration: The study was approved by the UK Medicines and Healthcare Regulatory Agency (Ref: CTA 21268/0224/001-0001 – EUDRACT 2019-003571-19 – Protocol Number RBH2019/001) on 08 April 2020, in compliance with the European Clinical Trials Directive and the Medicines for Human Use (Clinical Trials) Regulations 2004 and its subsequent amendments. The study was provided with ethical approval by the London Brent Research Ethics Committee (Ref: 20/LO/0368) on 21 May 2020 and is registered with clinicaltrials.gov (NCT04429516) on 12 June 2020, available at https://clinicaltrials

Published

2022

5. Treatment of May–Thurner’s Syndrome and Associated Complications: A Multicenter Experience

Author

Sigua-Arce,Priscilla, Mando,Ramy, Spencer,Lisa, Halalau,Alexandra, Sigua-Arce,Priscilla, Mando,Ramy, Spencer,Lisa, and Halalau,Alexandra

Abstract

Priscilla Sigua-Arce,1 Ramy Mando,1 Lisa Spencer,2 Alexandra Halalau1,2 1Department of Internal Medicine, Beaumont Health System, Royal Oak, MI, USA; 2Oakland University William Beaumont School of Medicine, Rochester Hills, MI, USACorrespondence: Alexandra Halalau Email Alexandra.halalau@beaumont.eduObjective: To assess the treatment options and associated complications in patients with May–Thurner’s syndrome (MTS).Methods: We retrospectively reviewed the charts of patients diagnosed with MTS. Thorough review was completed and data relevant to methods of diagnosis, treatment, complications, hospital readmission, and mortality were extracted from patient charts. The patients were followed for two years after diagnosis.Results: Of the 47 patients identified as having “MTS”, 32 (70%) were diagnosed formally with either magnetic resonance venography, computed tomography venography, or ultrasound. Two patients were excluded for insufficient availability of follow-up records. Mean age of the population included (N = 30) was 50.24 ± 15.33 years and 83% (N = 25) had female gender. The majority (40%) of patients were treated with anticoagulation, thrombolysis, and stent placement, and 13.3% received a combination of anticoagulation, antiplatelet agent, thrombolysis, and stent placement. Overall, we found 28 patients (93%) who underwent endovascular stenting. However, 39.3% (11/28) had stent-related complications that included stent thrombosis, stenosis, and migration. One patient underwent open heart surgery for stent retrieval. Duration of anticoagulation therapy ranged from 6 months to lifelong. Two patients (6.7%) suffered major bleeds requiring transfusion. Fourteen patients (46.6%) developed post-thrombotic syndrome. Seven (23.3%) patients required MTS-related readmission within 30 days. No mortality was noted at two-year follow-up.Conclusion: Although our study only included 30 patients, it was evident to us that there is no consensus in the management of MTS.

Published

2021

6. Heterogeneity of Intestinal Tissue Eosinophils: Potential Considerations for Next-Generation Eosinophil-Targeting Strategies

Author

Masterson, Joanne C., Menard-Katcher, Calies, Larsen, Leigha D., Furuta, Glenn T., Spencer, Lisa A., Masterson, Joanne C., Menard-Katcher, Calies, Larsen, Leigha D., Furuta, Glenn T., and Spencer, Lisa A.

Abstract

Eosinophils are implicated in the pathophysiology of a spectrum of eosinophil-associated diseases, including gastrointestinal eosinophilic diseases (EGIDs). Biologics that target the IL-5 pathway and are intended to ablate eosinophils have proved beneficial in severe eosinophilic asthma and may offer promise in treating some endotypes of EGIDs. However, destructive effector functions of eosinophils are only one side of the coin; eosinophils also play important roles in immune and tissue homeostasis. A growing body of data suggest tissue eosinophils represent a plastic and heterogeneous population of functional sub-phenotypes, shaped by environmental (systemic and local) pressures, which may differentially impact disease outcomes. This may be particularly relevant to the GI tract, wherein the highest density of eosinophils reside in the steady state, resident immune cells are exposed to an especially broad range of external and internal environmental pressures, and greater eosinophil longevity may uniquely enrich for co-expression of eosinophil sub-phenotypes. Here we review the growing evidence for functional sub-phenotypes of intestinal tissue eosinophils, with emphasis on the multifactorial pressures that shape and diversify eosinophil identity and potential targets to inform next-generation eosinophil-targeting strategies designed to restrain inflammatory eosinophil functions while sustaining homeostatic roles.

Published

2021

7. New developments in patients with eosinophilic gastrointestinal diseases presented at the CEGIR/TIGERS Symposium at the 2018 American Academy of Allergy, Asthma & Immunology Meeting.

Author

Spergel, Jonathan M, Spergel, Jonathan M, Aceves, Seema S, Kliewer, Kara, Gonsalves, Nirmala, Chehade, Mirna, Wechsler, Joshua B, Groetch, Marion, Friedlander, Joshua, Dellon, Evan S, Book, Wendy, Hirano, Ikuo, Muir, Amanda B, Cianferoni, Antonella, Spencer, Lisa, Liacouras, Chris A, Cheng, Edaire, Kottyan, Leah, Wen, Ting, Platts-Mills, Thomas, Rothenberg, Marc E, Spergel, Jonathan M, Spergel, Jonathan M, Aceves, Seema S, Kliewer, Kara, Gonsalves, Nirmala, Chehade, Mirna, Wechsler, Joshua B, Groetch, Marion, Friedlander, Joshua, Dellon, Evan S, Book, Wendy, Hirano, Ikuo, Muir, Amanda B, Cianferoni, Antonella, Spencer, Lisa, Liacouras, Chris A, Cheng, Edaire, Kottyan, Leah, Wen, Ting, Platts-Mills, Thomas, and Rothenberg, Marc E

Abstract

The Consortium of Eosinophilic Gastrointestinal Diseases and the International Gastrointestinal Eosinophil Researchers organized a day-long symposium at the recent 2018 Annual Meeting of the American Academy of Allergy, Asthma & Immunology, which was coupled for the first time with the World Allergy Organization meeting to create an international platform. The symposium featured experts in many facets of eosinophilic gastrointestinal diseases, including allergy, immunology, gastroenterology, pathology, and nutrition, and was a well-attended event. The basic science, genetics, cellular immunology, and clinical features of the diseases, with a focus on epithelial, eosinophil, and mast cell responses, as well as current and emerging treatment options, were reviewed. Here we briefly review some of the highlights of the material presented at the meeting.

Published

2018

8. New developments in patients with eosinophilic gastrointestinal diseases presented at the CEGIR/TIGERS Symposium at the 2018 American Academy of Allergy, Asthma & Immunology Meeting.

Author

Kliewer, Kara, Kliewer, Kara, Gonsalves, Nirmala, Chehade, Mirna, Wechsler, Joshua, Groetch, Marion, Friedlander, Joshua, Dellon, Evan, Book, Wendy, Hirano, Ikuo, Muir, Amanda, Cianferoni, Antonella, Spencer, Lisa, Liacouras, Chris, Cheng, Edaire, Kottyan, Leah, Wen, Ting, Platts-Mills, Thomas, Rothenberg, Marc, Spergel, Jonathan, Aceves, Seema, Kliewer, Kara, Kliewer, Kara, Gonsalves, Nirmala, Chehade, Mirna, Wechsler, Joshua, Groetch, Marion, Friedlander, Joshua, Dellon, Evan, Book, Wendy, Hirano, Ikuo, Muir, Amanda, Cianferoni, Antonella, Spencer, Lisa, Liacouras, Chris, Cheng, Edaire, Kottyan, Leah, Wen, Ting, Platts-Mills, Thomas, Rothenberg, Marc, Spergel, Jonathan, and Aceves, Seema

Abstract

The Consortium of Eosinophilic Gastrointestinal Diseases and the International Gastrointestinal Eosinophil Researchers organized a day-long symposium at the recent 2018 Annual Meeting of the American Academy of Allergy, Asthma & Immunology, which was coupled for the first time with the World Allergy Organization meeting to create an international platform. The symposium featured experts in many facets of eosinophilic gastrointestinal diseases, including allergy, immunology, gastroenterology, pathology, and nutrition, and was a well-attended event. The basic science, genetics, cellular immunology, and clinical features of the diseases, with a focus on epithelial, eosinophil, and mast cell responses, as well as current and emerging treatment options, were reviewed. Here we briefly review some of the highlights of the material presented at the meeting.

Published

2018

9. Effect of ambulatory oxygen on quality of life for patients with fibrotic lung disease (AmbOx): a prospective, open-label, mixed-method, crossover randomised controlled trial

Author

Visca, Dina, Mori, Letizia, Tsipouri, Vicky, Fleming, Sharon, Firouzi, Ashi, Bonini, Matteo, Pavitt, Matthew J, Alfieri, Veronica, Canu, Sara, Bonifazi, Martina, Boccabella, Cristina, De Lauretis, Angelo, Stock, Carmel J W, Saunders, Peter, Montgomery, Andrew, Hogben, Charlotte, Stockford, Anna, Pittet, Margaux, Brown, Jo, Chua, Felix, George, Peter M, Molyneaux, Philip L, Margaritopoulos, Georgios A, Kokosi, Maria, Kouranos, Vasileio, Russell, Anne Marie, Birring, Surinder S, Chetta, Alfredo, Maher, Toby M, Cullinan, Paul, Hopkinson, Nicholas S, Banya, Winston, Whitty, Jennifer A, Adamali, Huzaifa, Spencer, Lisa G, Farquhar, Morag, Sestini, Piersante, Wells, Athol U, Renzoni, Elisabetta A, Bonini, Matteo (ORCID:0000-0002-3042-0765), Visca, Dina, Mori, Letizia, Tsipouri, Vicky, Fleming, Sharon, Firouzi, Ashi, Bonini, Matteo, Pavitt, Matthew J, Alfieri, Veronica, Canu, Sara, Bonifazi, Martina, Boccabella, Cristina, De Lauretis, Angelo, Stock, Carmel J W, Saunders, Peter, Montgomery, Andrew, Hogben, Charlotte, Stockford, Anna, Pittet, Margaux, Brown, Jo, Chua, Felix, George, Peter M, Molyneaux, Philip L, Margaritopoulos, Georgios A, Kokosi, Maria, Kouranos, Vasileio, Russell, Anne Marie, Birring, Surinder S, Chetta, Alfredo, Maher, Toby M, Cullinan, Paul, Hopkinson, Nicholas S, Banya, Winston, Whitty, Jennifer A, Adamali, Huzaifa, Spencer, Lisa G, Farquhar, Morag, Sestini, Piersante, Wells, Athol U, Renzoni, Elisabetta A, and Bonini, Matteo (ORCID:0000-0002-3042-0765)

Abstract

Background: In fibrotic interstitial lung diseases, exertional breathlessness is strongly linked to health-related quality of life (HRQOL). Breathlessness is often associated with oxygen desaturation, but few data about the use of ambulatory oxygen in patients with fibrotic interstitial lung disease are available. We aimed to assess the effects of ambulatory oxygen on HRQOL in patients with interstitial lung disease with isolated exertional hypoxia. Methods: AmbOx was a prospective, open-label, mixed-method, crossover randomised controlled clinical trial done at three centres for interstitial lung disease in the UK. Eligible patients were aged 18 years or older, had fibrotic interstitial lung disease, were not hypoxic at rest but had a fall in transcutaneous arterial oxygen saturation to 88% or less on a screening visit 6-min walk test (6MWT), and had self-reported stable respiratory symptoms in the previous 2 weeks. Participants were randomly assigned (1:1) to either oxygen treatment or no oxygen treatment for 2 weeks, followed by crossover for another 2 weeks. Randomisation was by a computer-generated sequence of treatments randomly permuted in blocks of constant size (fixed size of ten). The primary outcome, which was assessed by intention to treat, was the change in total score on the King's Brief Interstitial Lung Disease questionnaire (K-BILD) after 2 weeks on oxygen compared with 2 weeks of no treatment. General linear models with treatment sequence as a fixed effect were used for analysis. Patient views were explored through semi-structured topic-guided interviews in a subgroup of participants. This study was registered with ClinicalTrials.gov, number NCT02286063, and is closed to new participants with all follow-up completed. Findings: Between Sept 10, 2014, and Oct 5, 2016, 84 patients were randomly assigned, 41 randomised to ambulatory oxygen first and 43 to no oxygen. 76 participants completed the trial. Compared with no oxygen, ambulatory oxygen was ass

Published

2018

10. Revisiting the NIH Taskforce on the Research needs of Eosinophil-Associated Diseases (RE-TREAD)

Author

Khoury, Paneez, Akuthota, Praveen, Ackerman, Steven S.J., Arron, Joseph J.R., Bochner, Bruce B.S., Collins, Margaret M.H., Kahn, Jean-Emmanuel, Fulkerson, Patricia P.C., Gleich, Gerald G.J., Gopal-Srivastava, Rashmi, Jacobsen, Elizabeth E.A., Leiferman, Kristin, Francesca, Levi Schaffer, Mathur, Sameer S.K., Minnicozzi, Michael, Prussin, Calman, Rothenberg, Marc, Roufosse, Florence, Sable, Kathleen, Simon, Dagmar, Simon, Hans-Uwe, Spencer, Lisa L.A., Steinfeld, Jonathan, Wardlaw, Andrew, Wechsler, Michael M.E., Weller, Peter, Klion, Amy, Khoury, Paneez, Akuthota, Praveen, Ackerman, Steven S.J., Arron, Joseph J.R., Bochner, Bruce B.S., Collins, Margaret M.H., Kahn, Jean-Emmanuel, Fulkerson, Patricia P.C., Gleich, Gerald G.J., Gopal-Srivastava, Rashmi, Jacobsen, Elizabeth E.A., Leiferman, Kristin, Francesca, Levi Schaffer, Mathur, Sameer S.K., Minnicozzi, Michael, Prussin, Calman, Rothenberg, Marc, Roufosse, Florence, Sable, Kathleen, Simon, Dagmar, Simon, Hans-Uwe, Spencer, Lisa L.A., Steinfeld, Jonathan, Wardlaw, Andrew, Wechsler, Michael M.E., Weller, Peter, and Klion, Amy

Abstract

Eosinophil-associated diseases (EADs) are rare, heterogeneous disorders characterized by the presence of eosinophils in tissues and/or peripheral blood resulting in immunopathology. The heterogeneity of tissue involvement, lack of sufficient animal models, technical challenges in working with eosinophils, and lack of standardized histopathologic approaches have hampered progress in basic research. Additionally, clinical trials and drug development for rare EADs are limited by the lack of primary and surrogate endpoints, biomarkers, and validated patient-reported outcomes. Researchers with expertise in eosinophil biology and eosinophil-related diseases reviewed the state of current eosinophil research, resources, progress, and unmet needs in the field since the 2012 meeting of the NIH Taskforce on the Research of Eosinophil-Associated Diseases (TREAD). RE-TREAD focused on gaps in basic science, translational, and clinical research on eosinophils and eosinophil-related pathogenesis. Improved recapitulation of human eosinophil biology and pathogenesis in murine models was felt to be of importance. Characterization of eosinophil phenotypes, the role of eosinophil subsets in tissues, identification of biomarkers of eosinophil activation and tissue load, and a better understanding of the role of eosinophils in human disease were prioritized. Finally, an unmet need for tools for use in clinical trials was emphasized. Histopathologic scoring, patient- and clinician-reported outcomes, and appropriate coding were deemed of paramount importance for research collaborations, drug development, and approval by regulatory agencies. Further exploration of the eosinophil genome, epigenome, and proteome was also encouraged. Although progress has been made since 2012, unmet needs in eosinophil research remain a priority., SCOPUS: re.j, info:eu-repo/semantics/published

Published

2018

11. Simulation of Synthetic Aperture Radar II: Simulating SAR (Synthetic Aperture Radar) Using the Advanced Visual Technology System

Author

GENERAL ELECTRIC CO DAYTONA BEACH FL SIMULATION AND CONTROL SYSTEMS DEPT, Ferguson, Robert L., Ellis, John, French, Steven R., Ball, Jeanne, Spencer, Lisa, Bell, Herbert H., Crane, Peter M., GENERAL ELECTRIC CO DAYTONA BEACH FL SIMULATION AND CONTROL SYSTEMS DEPT, Ferguson, Robert L., Ellis, John, French, Steven R., Ball, Jeanne, Spencer, Lisa, Bell, Herbert H., and Crane, Peter M.

Abstract

The Advanced Visual Technology System (AVTS) computer image generator was modified to produce highly accurate simulations of synthetic aperture radar (SAR) reflectively and elevation effects that can be precisely correlated with corresponding visual and infrared imagery. The resulting SAR snapshot is a plan view of the selected patch area with the field-of-view corresponding to a selected scale of 0.65, 1.3, or 2.6 nm. The image generator is interrupted for only one frame time, during which the entire processing power of the AVTS, up to 4,000 polygons, is brought to bear on the SAR snapshot. Once the SAR patch is computed, the AVTS continues with visual and infrared processing. A post- processor then adds feature and terrain shadows, horizontal and vertical incidence effects, resolution fall-off in azimuth and range, and speckle.

Published

1989

12. Investigating the role of CCN2 in a bleomycin model of Idiopathic Pulmonary Fibrosis

Author

Horwell, A. L., Bou-Gharios, George, Spencer, Lisa, and Moots, robert

Subjects

617.4

Abstract

Idiopathic Pulmonary Fibrosis (IPF) is a chronic, progressive and ultimately lethal disease of the lung characterised by excessive synthesis and deposition of extracellular matrix (ECM). The 5-year survival rate for IPF is lower than that of breast, prostate and skin cancer, with the average mortality rate currently standing at 3 years post diagnosis. Incidence and mortality appear to be on the rise, and prevalence is expected to increase in an aging population. Recently several new drugs have been approved (Pirfenidone, Nintedanib and Pamrevlumab). However, the pathobiology of IPF still remains elusive and there is an ever more pressing need to elucidate the molecular processes behind this disease to identify potential therapeutic targets. It is widely believed that at the cellular level, the key mediators of fibrosis are the fibroblast cell and their profibrotic phenotype, the myofibroblast. In normal homeostasis the myofibroblast is activated to synthesise new ECM during wound healing. In IPF there is believed to be a dysregulation in this process leading to persistent activation of myofibroblasts after the healing response is complete. Transforming growth factor - β (TGF-β) is known to be one of the master regulators of wound healing has been shown to be capable of activating myofibroblasts. However, research has looked downstream in the TGF - β signalling pathway to another protein - connective tissue growth factor (CCN2). CCN2 is considered a key downstream mediator of the profibrotic effects of TGF- β and has been shown to induce a fibrotic response independently of TGF-β both in vitro and in animal models of IPF. A clinical trial of a monoclonal antibody to CCN2 (Pamrevlumab) has demonstrated the ability to reverse the fibrosis in various murine models of fibrosis and is showing promising efficacy in human trials. The mechanism of action of CCN2 in fibrosis is still yet to be fully understood. The aim of this thesis was to utilise the murine bleomycin model of IPF to further investigate the role of CCN2 in fibrosis. Two new double transgenic mouse lines were generated, containing a CCN2 floxed transcript and a tamoxifen-inducible cre recombinase (CreERT2). Two different CreERT2 were used to facilitate loss of function of CCN2 in fibroblast cells specifically (Col1α2-CreERT2), or in all cells (ROSA-CreERT2). A dosing regimen for initiating recombination in vivo was established, and the phenotype in the lungs characterised for both new mouse lines. A third double transgenic mouse line was generated to examine the expression pattern of the Col1α2-CreERT2 during adulthood and embryonic development using a dual fluorescent reporter construct (mT/mG). A protocol was established for the induction of fibrosis in these mice using bleomycin, and a novel imaging protocol using an ex vivo μCT scanner was developed to enable full imaging of unfixed lungs prior to genetic and histological analysis. In summary, the studies reported in this thesis presented novel findings on the role of CCN2 in the pathogenesis of fibrosis. Two novel transgenic mouse lines were established for the genetic manipulation of CCN2 in vivo. These were used in conjunction with the bleomycin model, which was established for the first time at the University of Liverpool. The results from these experiments unveiled unexpected results and raised further questions as to the role CCN2 plays in homeostatic regulation of ECM production by demonstrating a potent anti-fibrotic effect of CCN2. A third transgenic mouse line was used to characterise the expression profile of a fibroblast specific CreERT2 developed by the Bou-Gharios lab group and found that the fibroblast specificity was prevalent in a wider population of fibroblasts than described previously.

Published

2018