Your search keyword '"Jenkins, William S."' showing total 11 results

1. Coronary Artery and Cardiac Disease in Patients With Type 2 Myocardial Infarction: A Prospective Cohort Study.

Author

Bularga, Anda, Hung, John, Daghem, Marwa, Stewart, Stacey, Taggart, Caelan, Wereski, Ryan, Singh, Trisha, Meah, Mohammed N., Fujisawa, Takeshi, Ferry, Amy V., Chiong, Justin, Jenkins, William S., Strachan, Fiona E., Semple, Scott, van Beek, Edwin J.R., Williams, Michelle, Dey, Damini, Tuck, Chris c, Baker, Andrew H., and Newby, David E.

Published

2022

2. Effect of Denosumab or Alendronic Acid on the Progression of Aortic Stenosis: A Double-Blind Randomized Controlled Trial.

Author

Pawade, Tania A., Doris, Mhairi K., Bing, Rong, White, Audrey C., Forsyth, Laura, Evans, Emily, Graham, Catriona, Williams, Michelle C., van Beek, Edwin J. R., Fletcher, Alison, Adamson, Philip D., Andrews, Jack P. M., Cartlidge, Timothy R. G., Jenkins, William S. A., Syed, Maaz, Fujisawa, Takeshi, Lucatelli, Christophe, Fraser, William, Ralston, Stuart H., and Boon, Nicholas

Published

2021

3. Determinants and prognostic value of echocardiographic first-phase ejection fraction in aortic stenosis.

Author

Rong Bing, Haotian Gu, Chin, Calvin, Lingyun Fang, White, Audrey, Everett, Russell J., Spath, Nicholas B., Eunsoo Park, Jenkins, William S. A., Shah, Anoop S. V., Mills, Nicholas L., Flapan, Andrew D., Chambers, John B., Newby, David E., Chowienczyk, Phil, Dweck, Marc R., Bing, Rong, Gu, Haotian, Fang, Lingyun, and Park, Eunsoo

Subjects

AORTIC stenosis, AORTIC valve transplantation, MAGNETIC resonance, AORTIC coarctation, LEFT heart ventricle, ECHOCARDIOGRAPHY, RESEARCH, MYOCARDIUM, PREDICTIVE tests, RESEARCH methodology, PROGNOSIS, RETROSPECTIVE studies, FIBROSIS, MAGNETIC resonance imaging, MEDICAL cooperation, EVALUATION research, COMPARATIVE studies, RESEARCH funding, HEMODYNAMICS, STROKE volume (Cardiac output), HEART physiology, AORTIC valve

Abstract

Objective: First-phase ejection fraction (EF1) is a novel measure of early left ventricular systolic dysfunction. We investigated determinants of EF1 and its prognostic value in aortic stenosis.Methods: EF1 was measured retrospectively in participants of an echocardiography/cardiovascular magnetic resonance cohort study which recruited patients with aortic stenosis (peak aortic velocity of ≥2 m/s) between 2012 and 2014. Linear regression models were constructed to examine variables associated with EF1. Cox proportional hazards were used to determine the prognostic power of EF1 for aortic valve replacement (AVR, performed as part of clinical care in accordance with international guidelines) or death.Results: Total follow-up of the 149 participants (69.8% male, 70 (65-76) years, mean gradient 33 (21-42) mm Hg) was 238 029 person-days. Sixty-seven participants (45%) had a low baseline EF1 (<25%) despite normal ejection fraction (67% (62%-71%)). Patients with low EF1 had more severe aortic stenosis (mean gradient 39 (34-45) mm Hg vs 24 (16-35) mm Hg, p<0.001) and more myocardial fibrosis (indexed extracellular volume (iECV) (24.2 (19.6-28.7) mL/m2 vs 20.6 (16.8-24.3) mL/m2, p=0.002; late gadolinium enhancement (LGE) prevalence 52% vs 20%, p<0.001). Zva, iECV and infarct LGE were independent predictors of EF1. EF1 improved post-AVR (n=57 with post-AVR EF1 available, baseline 16 (12-24) vs follow-up 27% (22%-31%); p<0.001). Low baseline EF1 was an independent predictor of AVR/death (HR 5.6, 95% CI 3.4 to 9.4), driven by AVR.Conclusion: EF1 quantifies early, potentially reversible systolic dysfunction in aortic stenosis, is associated with global afterload and myocardial fibrosis, and is an independent predictor of AVR. [ABSTRACT FROM AUTHOR]

Published

2020

4. In vivo alpha-V beta-3 integrin expression in human aortic atherosclerosis.

Author

Tarkin, Jason M., Mason, Justin C., Fayad, Zahi A., Jenkins, William S, Vesey, Alex T, Vickers, Anna, Neale, Anoushka, Moles, Catriona, Connell, Martin, Joshi, Nikhil Vilas, Lucatelli, Christophe, Fletcher, Alison M, Spratt, James C, Mirsadraee, Saeed, van Beek, Edwin Jr, Rudd, James Hf, Newby, David E, and Dweck, Marc R

Subjects

CAROTID endarterectomy, NEOVASCULARIZATION, ATHEROSCLEROTIC plaque, GROWTH factors, CAROTID intima-media thickness

Abstract

Objectives: Intraplaque angiogenesis and inflammation are key promoters of atherosclerosis and are mediated by the alpha-V beta-3 (αvβ3) integrin pathway. We investigated the applicability of the αvβ3-integrin receptor-selective positron emission tomography (PET) radiotracer 18F-fluciclatide in assessing human aortic atherosclerosis.Methods: Vascular 18F-fluciclatide binding was evaluated using ex vivo analysis of carotid endarterectomy samples with autoradiography and immunohistochemistry, and in vivo kinetic modelling following radiotracer administration. Forty-six subjects with a spectrum of atherosclerotic disease categorised as stable (n=27) or unstable (n=19; recent myocardial infarction) underwent PET and CT imaging of the thorax after administration of 229 (IQR 217-237) MBq 18F-fluciclatide. Thoracic aortic 18F-fluciclatide uptake was quantified on fused PET-CT images and corrected for blood-pool activity using the maximum tissue-to-background ratio (TBRmax). Aortic atherosclerotic burden was quantified by CT wall thickness, plaque volume and calcium scoring.Results: 18F-Fluciclatide uptake co-localised with regions of increased αvβ3 integrin expression, and markers of inflammation and angiogenesis. 18F-Fluciclatide vascular uptake was confirmed in vivo using kinetic modelling, and on static imaging correlated with measures of aortic atherosclerotic burden: wall thickness (r=0.57, p=0.001), total plaque volume (r=0.56, p=0.001) and aortic CT calcium score (r=0.37, p=0.01). Patients with recent myocardial infarction had greater aortic 18F-fluciclatide uptake than those with stable disease (TBRmax 1.29 vs 1.21, p=0.02).Conclusions: In vivo expression of αvβ3 integrin in human aortic atheroma is associated with plaque burden and is increased in patients with recent myocardial infarction. Quantification of αvβ3 integrin expression with 18F-fluciclatide PET has potential to assess plaque vulnerability and disease activity in atherosclerosis. [ABSTRACT FROM AUTHOR]

Published

2019

5. End stage renal disease-induced hypercalcemia may promote aortic valve calcification via Annexin VI enrichment of valve interstitial cell derived-matrix vesicles.

Author

Cui, Lin, Rashdan, Nabil A., Zhu, Dongxing, Milne, Elspeth M., Ajuh, Paul, Milne, Gillian, Helfrich, Miep H., Lim, Kelvin, Prasad, Sai, Lerman, Daniel A., Vesey, Alex T., Dweck, Marc R., Jenkins, William S., Newby, David E., Farquharson, Colin, and Macrae, Vicky E.

Subjects

CHRONIC kidney failure, HYPERCALCEMIA, AORTIC valve, CALCIFICATION, ULTRACENTRIFUGATION, TRANSMISSION electron microscopy, LABORATORY rats, PHYSIOLOGY

Abstract

Patients with end-stage renal disease (ESRD) have elevated circulating calcium (Ca) and phosphate (Pi), and exhibit accelerated progression of calcific aortic valve disease (CAVD). We hypothesized that matrix vesicles (MVs) initiate the calcification process in CAVD. Ca induced rat valve interstitial cells (VICs) calcification at 4.5mM (16.4-fold; p < 0.05) whereas Pi treatment alone had no effect. Ca (2.7 mM) and Pi (2.5 mM) synergistically induced calcium deposition (10.8-fold; p < 0.001) in VICs. Ca treatment increased the mRNA of the osteogenic markers Msx2, Runx2, and Alpl (p < 0.01). MVs were harvested by ultracentrifugation from VICs cultured with control or calcification media (containing 2.7mM Ca and 2.5mM Pi) for 16 hr. Proteomics analysis revealed the marked enrichment of exosomal proteins, including CD9, CD63, LAMP-1, and LAMP-2 and a concomitant up-regulation of the Annexin family of calciumbinding proteins. Of particular note Annexin VI was shown to be enriched in calcifying VICderived MVs (51.9-fold; p < 0.05). Through bioinformatic analysis using Ingenuity Pathway Analysis (IPA), the up-regulation of canonical signaling pathways relevant to cardiovascular function were identified in calcifying VIC-derived MVs, including aldosterone, Rho kinase, and metal binding. Further studies using human calcified valve tissue revealed the co-localization of Annexin VI with areas of MVs in the extracellular matrix by transmission electron microscopy (TEM). Together these findings highlight a critical role for VIC-derived MVs in CAVD. Furthermore, we identify calcium as a key driver of aortic valve calcification, which may directly underpin the increased susceptibility of ESRD patients to accelerated development of CAVD. [ABSTRACT FROM AUTHOR]

Published

2017

6. Ferumoxytol-enhanced magnetic resonance imaging assessing inflammation after myocardial infarction.

Author

Stirrat, Colin G., Alam, Shirjel R., MacGillivray, Thomas J., Gray, Calum D., Dweck, Marc R., Raftis, Jennifer, Jenkins, William S. A., Wallace, William A., Pessotto, Renzo, Lim, Kelvin H. H., Mirsadraee, Saeed, Henriksen, Peter A., Semple, Scott I. K ., Newby, David E., Jenkins, William Sa, Lim, Kelvin Hh, and Semple, Scott Ik

Subjects

MAGNETIC resonance imaging, INFLAMMATION, MYOCARDIAL infarction, INTERLEUKIN-6, TOCILIZUMAB, MYOCARDIAL infarction diagnosis, HEMATOPOIETIC agents, LONGITUDINAL method, MACROPHAGES, MYOCARDIUM, RESEARCH evaluation, RESEARCH funding, PHARMACODYNAMICS, DIAGNOSIS

Abstract

Objectives: Macrophages play a central role in the cellular inflammatory response to myocardial infarction (MI) and predict subsequent clinical outcomes. We aimed to assess temporal changes in cellular inflammation and tissue oedema in patients with acute MI using ultrasmallsuperparamagnetic particles of iron oxide (USPIO)-enhanced MRI.Methods: Thirty-one patients were recruited following acute MI and followed up for 3 months with repeated T2 and USPIO-enhanced T2*-mapping MRI. Regions of interest were categorised into infarct, peri-infarct and remote myocardial zones, and compared with control tissues.Results: Following a single dose, USPIO enhancement was detected in the myocardium until 24 hours (p<0.0001). Histology confirmed colocalisation of iron and macrophages within the infarcted, but not the non-infarcted, myocardium. Following repeated doses, USPIO uptake in the infarct zone peaked at days 2-3, and greater USPIO uptake was detected in the infarct zone compared with remote myocardium until days 10-16 (p<0.05). In contrast, T2-defined myocardial oedema peaked at days 3-9 and remained increased in the infarct zone throughout the 3-month follow-up period (p<0.01).Conclusion: Myocardial macrophage activity can be detected using USPIO-enhanced MRI in the first 2 weeks following acute MI. This observed pattern of cellular inflammation is distinct, and provides complementary information to the more prolonged myocardial oedema detectable using T2 mapping. This imaging technique holds promise as a non-invasive method of assessing and monitoring myocardial cellular inflammation with potential application to diagnosis, risk stratification and assessment of novel anti-inflammatory therapeutic interventions.Trial Registration Number: Trial registration number: 14663. Registered on UK Clinical Research Network (http://public.ukcrn.org.uk) and also ClinicalTrials.gov (https://clinicaltrials.gov/ct2/show/NCT02319278?term=DECIFER&rank=2). [ABSTRACT FROM AUTHOR]

Published

2017

7. Cardiac αVβ3 integrin expression following acute myocardial infarction in humans.

Author

Jenkins, William S. A., Vesey, Alex T., Stirrat, Colin, Connell, Martin, Lucatelli, Christophe, Neale, Anoushka, Moles, Catriona, Vickers, Anna, Fletcher, Alison, Pawade, Tania, Wilson, Ian, Rudd, James H. F., van Beek, Edwin J. R., Mirsadraee, Saeed, Dweck, Marc R., and Newby, David E.

Subjects

INTEGRINS, MYOCARDIAL infarction treatment, HEART failure, POSITRON emission tomography, GADOLINIUM, THERAPEUTICS, HEART metabolism, CONVALESCENCE, HEART physiology, LEFT heart ventricle, MAGNETIC resonance imaging, MYOCARDIAL infarction, MYOCARDIUM, PEPTIDES, POLYETHYLENE glycol, TIME, VENTRICULAR remodeling, CONTRAST media, CASE-control method, DRUG administration, DRUG dosage

Abstract

Objective: Maladaptive repair contributes towards the development of heart failure following myocardial infarction (MI). The αvβ3 integrin receptor is a key mediator and determinant of cardiac repair. We aimed to establish whether αvβ3 integrin expression determines myocardial recovery following MI.Methods: 18F-Fluciclatide (a novel αvβ3-selective radiotracer) positron emission tomography (PET) and CT imaging and gadolinium-enhanced MRI (CMR) were performed in 21 patients 2 weeks after ST-segment elevation MI (anterior, n=16; lateral, n=4; inferior, n=1). CMR was repeated 9 months after MI. 7 stable patients with chronic total occlusion (CTO) of a major coronary vessel and nine healthy volunteers underwent a single PET/CT and CMR.Results: 18F-Fluciclatide uptake was increased at sites of acute infarction compared with remote myocardium (tissue-to-background ratio (TBRmean) 1.34±0.22 vs 0.85±0.17; p<0.001) and myocardium of healthy volunteers (TBRmean 1.34±0.22 vs 0.70±0.03; p<0.001). There was no 18F-fluciclatide uptake at sites of established prior infarction in patients with CTO, with activity similar to the myocardium of healthy volunteers (TBRmean 0.71±0.06 vs 0.70±0.03, p=0.83). 18F-Fluciclatide uptake occurred at sites of regional wall hypokinesia (wall motion index≥1 vs 0; TBRmean 0.93±0.31 vs 0.80±0.26 respectively, p<0.001) and subendocardial infarction. Importantly, although there was no correlation with infarct size (r=0.03, p=0.90) or inflammation (C reactive protein, r=-0.20, p=0.38), 18F-fluciclatide uptake was increased in segments displaying functional recovery (TBRmean 0.95±0.33 vs 0.81±0.27, p=0.002) and associated with increase in probability of regional recovery.Conclusion: 18F-Fluciclatide uptake is increased at sites of recent MI acting as a biomarker of cardiac repair and predicting regions of recovery.Trial Registration Number: NCT01813045; Post-results. [ABSTRACT FROM AUTHOR]

Published

2017

8. 18F-Fluoride and 18F-Fluorodeoxyglucose Positron Emission Tomography After Transient Ischemic Attack or Minor Ischemic Stroke.

Author

Vesey, Alex T., Jenkins, William S. A., Irkle, Agnese, Moss, Alastair, Sng, Greg, Forsythe, Rachael O., Clark, Tim, Roberts, Gemma, Fletcher, Alison, Lucatelli, Christophe, Rudd, James H. F., Davenport, Anthony P., Mills, Nicholas L., Salman, Rustam Al-Shahi, Dennis, Martin, Whiteley, William N., van Beek, Edwin J. R., Dweck, Marc R., and Newby, David E.

Published

2017

9. Optimization and Reproducibility of Aortic Valve 18F-Fluoride Positron Emission Tomography in Patients With Aortic Stenosis.

Author

Pawade, Tania A., Cartlidge, Timothy R. G., Jenkins, William S. A., Adamson, Philip D., Robson, Phillip, Lucatelli, Christophe, Van Beek, Edwin J. R., Prendergast, Bernard, Denison, Alan R., Forsyth, Laura, Rudd, James H. F., Fayad, Zahi A., Fletcher, Alison, Tuck, Sharon, Newby, David E., and Dweck, Marc R.

Published

2016

10. What can we learn about valvular heart disease from PET/CT?

Author

Jenkins, William Sa, Chin, Calvin, Rudd, James Hf, Newby, David E, Dweck, Marc R, Jenkins, William S A, and Rudd, James H F

Abstract

Valvular heart disease is a major cause of morbidity and mortality, and with an aging population, its prevalence is increasing. Here, we review the evolving use of positron emission tomography/computed tomography in valvular heart disease, with particular focus on calcific aortic stenosis and infective endocarditis. In principle, the activity of any pathological process can be studied, as long as an appropriate radiotracer can be developed. We will review some of the early data using established tracers in the above and other conditions, providing discussion as to the future research and clinical roles of these techniques. Furthermore, we will discuss the potential impact of novel tracers that are currently under development or testing in preclinical models. It is hoped that such advanced imaging might improve the diagnosis, treatment and outlook for patients with valvular heart disease. [ABSTRACT FROM AUTHOR]

Published

2013

11. Systemic Atherosclerotic Inflammation Following Acute Myocardial Infarction: Myocardial Infarction Begets Myocardial Infarction.

Author

Joshi, Nikhil V., Toor, Iqbal, Shah, Anoop S. V., Carruthers, Kathryn, Vesey, Alex T., Alam, Shirjel R., Sills, Andrew, Hoo, Teng Y., Melville, Adam J., Langlands, Sarah P., Jenkins, William S. A., Uren, Neal G., Mills, Nicholas L., Fletcher, Alison M., van Beek, Edwin J. R., Rudd, James H. F., Fox, Keith A. A., Dweck, Marc R., and Newby, David E.

Published

2015