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246


Clinical Biomarkers of World Trade Center Airway Hyperreactivity: A 16-Year Longitudinal Study [Meeting Abstract]

Kwon, S.; Clementi, E.; Crowley, G.; Schwartz, T.; Zeig-Owens, R.; Liu, M.; Prezant, D. J.; Nolan, A.
ISI:000466771102337
ISSN: 1073-449x
CID: 3896772

Validation of Biomarkers of World Trade Center (WTC) Lung Injury: Design of a Case Cohort Control [Meeting Abstract]

Riggs, J.; Kwon, S.; Crowley, G.; Ostrofsky, D.; Talusan, A.; Mikhail, M.; Kim, J.; Zeig-Owens, R.; Schwartz, T.; Prezant, D. J.; Liu, M.; Nolan, A.
ISI:000466771102339
ISSN: 1073-449x
CID: 3896792

Metabolic Syndrome Biomarkers of World Trade Center Airway Hyperreactivity: A 16-Year Prospective Cohort Study

Kwon, Sophia; Crowley, George; Mikhail, Mena; Lam, Rachel; Clementi, Emily; Zeig-Owens, Rachel; Schwartz, Theresa M; Liu, Mengling; Prezant, David J; Nolan, Anna
Airway hyperreactivity (AHR) related to environmental exposure is a significant public health risk worldwide. Similarly, metabolic syndrome (MetSyn), a risk factor for obstructive airway disease (OAD) and systemic inflammation, is a significant contributor to global adverse health. This prospective cohort study followed N = 7486 World Trade Center (WTC)-exposed male firefighters from 11 September 2001 (9/11) until 1 August 2017 and investigated N = 539 with newly developed AHR for clinical biomarkers of MetSyn and compared them to the non-AHR group. Male firefighters with normal lung function and no AHR pre-9/11 who had blood drawn from 9 September 2001-24 July 2002 were assessed. World Trade Center-Airway Hyperreactivity (WTC-AHR) was defined as either a positive bronchodilator response (BDR) or methacholine challenge test (MCT). The electronic medical record (EMR) was queried for their MetSyn characteristics (lipid profile, body mass index (BMI), glucose), and routine clinical biomarkers (such as complete blood counts). We modeled the association of MetSyn characteristics at the first post-9/11 exam with AHR. Those with AHR were significantly more likely to be older, have higher BMIs, have high intensity exposure, and have MetSyn. Smoking history was not associated with WTC-AHR. Those present on the morning of 9/11 had 224% increased risk of developing AHR, and those who arrived in the afternoon of 9/11 had a 75.9% increased risk. Having ≥3 MetSyn parameters increased the risk of WTC-AHR by 65.4%. Co-existing MetSyn and high WTC exposure are predictive of future AHR and suggest that systemic inflammation may be a contributor.
PMID: 31035527
ISSN: 1660-4601
CID: 3830262

Receptor for advanced glycation end-products and environmental exposure related obstructive airways disease: a systematic review

Haider, Syed H; Oskuei, Assad; Crowley, George; Kwon, Sophia; Lam, Rachel; Riggs, Jessica; Mikhail, Mena; Talusan, Angela; Veerappan, Arul; Kim, James S; Caraher, Erin J; Nolan, Anna
BACKGROUND:Our group has identified the receptor for advanced glycation end-products (RAGE) as a predictor of World Trade Center particulate matter associated lung injury. The aim of this systematic review is to assess the relationship between RAGE and obstructive airways disease secondary to environmental exposure. METHODS:A comprehensive search using PubMed and Embase was performed on January 5, 2018 utilising keywords focusing on environmental exposure, obstructive airways disease and RAGE and was registered with PROSPERO (CRD42018093834). We included original human research studies in English, focusing on pulmonary end-points associated with RAGE and environmental exposure. RESULTS:A total of 213 studies were identified by the initial search. After removing the duplicates and applying inclusion and exclusion criteria, we screened the titles and abstracts of 61 studies. Finally, 19 full-text articles were included. The exposures discussed in these articles include particulate matter (n=2) and cigarette smoke (n=17). CONCLUSION/CONCLUSIONS:RAGE is a mediator of inflammation associated end-organ dysfunction such as obstructive airways disease. Soluble RAGE, a decoy receptor, may have a protective effect in some pulmonary processes. Overall, RAGE is biologically relevant in environmental exposure associated lung disease. Future investigations should focus on further understanding the role and therapeutic potential of RAGE in particulate matter exposure associated lung disease.
PMID: 30918021
ISSN: 1600-0617
CID: 3764232

Validation of Predictive Metabolic Syndrome Biomarkers of World Trade Center Lung Injury: a 16-Year Longitudinal Study

Kwon, Sophia; Crowley, George; Caraher, Erin J; Haider, Syed Hissam; Lam, Rachel; Veerappan, Arul; Yang, Lei; Liu, Mengling; Zeig-Owens, Rachel; Schwartz, Theresa; Prezant, David J; Nolan, Anna
BACKGROUND:Metabolic Syndrome (MetSyn) predicted future development of World Trade Center lung injury(WTC-LI) in a subgroup of never smoking, male firefighters. An intra-cohort validation of MetSyn as predictors of WTC-LI is examined in the WTC-exposed cohort that has been longitudinally followed for 16 years. METHODS:<LLN. RESULTS:Cases were more likely to smoke, be highly exposed, and have MetSyn. There was a significant exposure dose response; the most highly-exposed individuals had 30.1%-increased risk of developing WTC-LI; having MetSyn increased risk of WTC-LI by 55.7%; smoking increased risk by 15.2%. There was significant interaction between smoking and exposure. CONCLUSIONS:We validated the utility of MetSyn to predict future WTC-LI in a larger population of exposed individuals. MetSyn defined by dyslipidemia, insulin resistance, and cardiovascular disease suggests that systemic inflammation can contribute to future lung function loss.
PMID: 30836056
ISSN: 1931-3543
CID: 3722962

Metabolic Syndrome and Air Pollution: A Narrative Review of Their Cardiopulmonary Effects

Clementi, Emily A; Talusan, Angela; Vaidyanathan, Sandhya; Veerappan, Arul; Mikhail, Mena; Ostrofsky, Dean; Crowley, George; Kim, James S; Kwon, Sophia; Nolan, Anna
Particulate matter (PM) exposure and metabolic syndrome (MetSyn) are both significant global health burdens. PM exposure has been implicated in the pathogenesis of MetSyn and cardiopulmonary diseases. Individuals with pre-existing MetSyn may be more susceptible to the detrimental effects of PM exposure. Our aim was to provide a narrative review of MetSyn/PM-induced systemic inflammation in cardiopulmonary disease, with a focus on prior studies of the World Trade Center (WTC)-exposed Fire Department of New York (FDNY). We included studies (1) published within the last 16-years; (2) described the epidemiology of MetSyn, obstructive airway disease (OAD), and vascular disease in PM-exposed individuals; (3) detailed the known mechanisms of PM-induced inflammation, MetSyn and cardiopulmonary disease; and (4) focused on the effects of PM exposure in WTC-exposed FDNY firefighters. Several investigations support that inhalation of PM elicits pulmonary and systemic inflammation resulting in MetSyn and cardiopulmonary disease. Furthermore, individuals with these preexisting conditions are more sensitive to PM exposure-related inflammation, which can exacerbate their conditions and increase their risk for hospitalization and chronic disease. Mechanistic research is required to elucidate biologically plausible therapeutic targets of MetSyn- and PM-induced cardiopulmonary disease.
PMID: 30704059
ISSN: 2305-6304
CID: 3626852

Metabolomics of World Trade Center-Lung Injury: a machine learning approach (vol 5, e000274, 2018) [Correction]

Crowley, George; Kwon, Sophia; Haider, Syed Hissam; Caraher, Erin J.; Lam, Rachel; St-Jules, David E.; Liu, Mengling; Prezant, David J.; Nolan, Anna
ISI:000457714400003
ISSN: 2052-4439
CID: 5518992

Zika Virus-Associated Guillain-Barré Syndrome in a Returning US Traveler

Beattie, Jason; Parajuli, Sunita; Sanger, Matthew; Lee, Gregory; Pleninger, Perrin; Crowley, George; Kwon, Sophia; Murthy, Vivek; Manko, Jeffrey A; Caplan, Arthur; Dufort, Elizabeth; Pastula, Daniel M; Nolan, Anna
Zika virus (ZIKV) infection has been associated with Guillain-Barré Syndrome (GBS). Roughly 60% of people in countries such as the U.S. live in areas at risk for seasonal spread of ZIKV. ZIKV belongs to a class of diseases that is not typically seen in hospital settings across the U.S. and Europe. We describe the case presentation, management, and treatment of ZIKV infection complicated by GBS. A 64-year-old woman with recent travel to the Dominican Republic presented with rash followed by an acute, ascending polyneuropathy consistent with GBS. She was confirmed to have an acute ZIKV infection by detection of ZIKV nucleic acid by reverse transcription-polymerase chain reaction. She met Brighton Collaboration criteria level 1 evidence for GBS. She received two courses of intravenous immunoglobulin and slowly improved, though still had weakness at discharge. More research is needed to identify the pathophysiology behind ZIKV-associated GBS and its optimal treatment. Prevention is fundamental to limiting infection and spread of ZIKV.
PMCID:6433380
PMID: 30923438
ISSN: 1056-9103
CID: 3777472

Non-Cardiac Chest Pain: A Review of Environmental Exposure-Associated Comorbidities and Biomarkers

Mikhail, Mena; Crowley, George; Haider, Syed Hissam; Veerappan, Arul; Lam, Rachel; Talusan, Angela; Clementi, Emily; Ostrofsky, Dean; Kwon, Sophia; Nolan, Anna
The prevalence of non-cardiac chest pain (NCCP) ranges from 13-33%. A majority of those presenting with a chief complaint of chest pain are found to have a diagnosis of NCCP. Aerodigestive diseases are a cause of NCCP, and billions of dollars are spent annually on the treatment of NCCP. Furthermore, NCCP can cause significant psychological stress. NCCP is commonly diagnosed when patients have chest pain despite a normal cardiac evaluation. The leading cause of NCCP is gastro-oesophageal reflux disease (GORD). GORD should be suspected in patients who report a history of acid regurgitation, cough, dysphagia, and bloating. Another common cause of NCCP is obstructive airway disease (OAD). A thorough history and review of the symptoms should be performed for those with suspected NCCP, especially because of the contributing end organs. It is known that environmental exposures can commonly cause GORD and OAD; however, NCCP has not been fully explored in the context of environmental exposure. Patients with a history of exposure to particulate matter can develop environmental-exposure-associated GORD and coexisting OAD. This narrative review aims to provide a practical overview of NCCP, its causes, their relation to environmental exposure, and associated biomarkers. The authors used a PubMed search that spanned 2003-2018 to accomplish this. Additionally, this review provides a broad overview of biomarkers of GORD-associated NCCP and OAD-associated NCCP due to environmental exposure.
PMCID:6375490
PMID: 30774967
ISSN: 2054-6203
CID: 3663812

Pioglitazone Pre-Treatment by Gavage Attenuates Particulate Matter Induced Lung Disease [Meeting Abstract]

Caraher, E.; Haider, S.; Kwon, S.; Crowley, G.; Chen, L.; Nolan, A.
ISI:000449980300358
ISSN: 1073-449x
CID: 3513132