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Dive into the research topics where Timothy D. Henry is active.

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Featured researches published by Timothy D. Henry.


Circulation | 2000

Effect of Intracoronary Recombinant Human Vascular Endothelial Growth Factor on Myocardial Perfusion Evidence for a Dose-Dependent Effect

Robert C. Hendel; Timothy D. Henry; Krishna J. Rocha-Singh; Jeffrey M. Isner; Frank J. Giordano; Michael Simons; Robert O. Bonow

BACKGROUNDnAnimal models of therapeutic angiogenesis have stimulated development of clinical application in patients with limited options for coronary revascularization. The impact of recombinant human vascular endothelial growth factor (rhVEGF) on myocardial perfusion in humans has not been reported.nnnMETHODS AND RESULTSnFourteen patients underwent exercise (n=11), dobutamine (n=2), or dipyridamole (n=1) myocardial perfusion single photon emission CT (SPECT) before as well as 30 and 60 days after rhVEGF administration. After uniform processing and display, 2 observers blinded to the timing of the study and dose of rhVEGF reviewed the SPECT images. By a visual, semiquantitative 20-segment scoring method, summed stress scores (SSS) and summed rest scores (SRS) were generated. Although the SSS did not change from baseline to 30 days (21.6 versus 21.5; P=NS), the SRS improved after rhVEGF (13.2 versus 10.4; P<0.05). Stress and rest perfusion improved in >2 segments infrequently in patients treated with low-dose rhVEGF. However, 5 of 6 patients had improvement in >2 segments at rest and stress with the higher rhVEGF doses. Furthermore, although neither the SSS nor the SRS changed in patients treated with the low doses, the SRS decreased in the high-dose rhVEGF patients at 60 days (14.7 versus 10.7; P<0.05). Quantitative analysis was consistent with the visual findings but failed to demonstrate statistical significance.nnnCONCLUSIONSnAlthough not designed to demonstrate rhVEGF efficacy, these phase 1 data support the concept that rhVEGF improves myocardial perfusion at rest and provide evidence of a dose-dependent effect.


American Journal of Cardiology | 2003

One-year follow-up of direct myocardial gene transfer of vascular endothelial growth factor-2 using naked plasmid deoxyribonucleic acid by way of thoracotomy in no-option patients* ☆

F. David Fortuin; Peter R. Vale; Douglas W. Losordo; James F. Symes; Giacomo A. DeLaria; Jeffrey J. Tyner; Gary L. Schaer; Robert J. March; R. Jeffrey Snell; Timothy D. Henry; Joseph Van Camp; John Lopez; Wayne E. Richenbacher; Jeffrey M. Isner; Richard A. Schatz

This phase I open label, dose-escalating study shows that gene transfer of vascular endothelial growth factor-2 naked deoxyribonucleic acid by direct myocardial injection by way of thoracotomy in patients with Canadian Cardiovascular Society class 3 or 4 angina is feasible and safe. The procedure is well tolerated, with few major adverse cardiac events at 1 year, and without complications directly related to gene expression. In this prospective, nonblinded study, the procedure is associated with clinical improvement; however, there was no angiographic evidence of angiogenesis and there is a great potential for a sham or placebo effect in the study patients. A randomized phase III trial is underway that will help determine the efficacy of vascular endothelial growth factor-2 gene transfer in no-option patients.


The Lancet | 2000

Optimum percutaneous transluminal coronary angioplasty compared with routine stent strategy trial (OPUS-1): a randomised trial

W. Douglas Weaver; Mark Reisman; John J. Griffin; Christopher E Butler; Pierre P. Leimgruber; Timothy D. Henry; Christopher D'Haem; Vivian L Clark; David J. Cohen; Nancy Neil; Nathan R. Every; Jenny S. Martin

BACKGROUNDnWhether routine implantation of coronary stents is the best strategy to treat flow-limiting coronary stenoses is unclear. An alternative approach is to do balloon angioplasty and provisionally use stents only to treat suboptimum results. We did a multicentre trial to compare the outcomes of patients treated with these strategies.nnnMETHODSnWe randomly assigned 479 patients undergoing single-vessel coronary angioplasty routine stent implantation or initial balloon angioplasty and provisional stenting. We followed up patients for 6 months to determine the composite rate of death, myocardial infarction, cardiac surgery, and target-vessel revascularisation.nnnRESULTSnStents were implanted in 227 (98.7%) of the patients assigned routine stenting. 93 (37%) patients assigned balloon angioplasty had at least one stent placed because of suboptimum angioplasty results. At 6 months the composite endpoint was significantly lower in the routine stent strategy (14 events, 6.1%) than with the strategy of balloon angioplasty with provisional stenting (37 events, 14.9%, p=0.003). The cost of the initial revascularisation procedure was higher than when a routine stent strategy was used (US


Circulation | 2005

Increased Prevalence of Coronary Artery Aneurysms Among Cocaine Users

Aaron Satran; Bradley A. Bart; Christopher R. Henry; M. Bilal Murad; Sumaiya Talukdar; Daniel Satran; Timothy D. Henry

389 vs


American Journal of Cardiology | 1998

Effects of Prior Aspirin and Anti-Ischemic Therapy on Outcome of Patients With Unstable Angina 1

Steven Borzak; Christopher P. Cannon; Phillip L. Kraft; Lori Douthat; Richard C. Becker; Sebastian T. Palmeri; Timothy D. Henry; Judith S. Hochman; Joanna Fuchs; Elliott M. Antman; Carolyn H. McCabe; Eugene Braunwald

339, p<0.001) but at 6 months, average per-patient hospital costs did not differ (


Clinica Chimica Acta | 1995

Cardiac troponin, CK-MB and myoglobin for the early detection of acute myocardial infarction and monitoring of reperfusion following thrombolytic therapy

Fred S. Apple; Ellen M. Voss; Lisa Lund; Lynne M. Preese; Charlene R. Berger; Timothy D. Henry

10,206 vs


Journal of the American College of Cardiology | 2017

OUTCOME AND CHARACTERISTICS OF SHOCKABLE VERSUS NON-SHOCKABLE CARDIAC ARREST IN ST ELEVATION MYOCARDIAL INFARCTION AT A REGIONAL TRANSFER CENTER

Benjamin Johnson; Claire Donovan; Ross Garberich; John Hibbs; David Larson; Timothy D. Henry; Scott W. Sharkey

10,490). Bootstrap replication of 6-month cost data showed continued economic benefit of the routine stent strategy.nnnINTERPRETATIONnRoutine stent implantation leads to better acute and long-term clinical outcomes at a cost similar to that of initial balloon angioplasty with provisional stenting.


Journal of the American College of Cardiology | 1995

988-3 Is there a Circadian Variation in Anticoagulation Response to Hirudin Following Acute Myocardial Infarction?

Timothy D. Henry; Richard C. Becker; Christopher P. Cannon; Carolyn H. McCabe; Joseph Loscalzo

Background—Cocaine abuse has been implicated in multiple cardiovascular complications. Coronary artery aneurysms (CAAs) and ectasia occur in 0.2% to 5.3% of patients referred for angiography and are associated with atherosclerosis, Kawasaki’s disease, and several rare disorders. After observing CAAs in multiple young cocaine users, we investigated the prevalence of CAAs among cocaine users undergoing coronary angiography. Methods and Results—Clinical and angiographic characteristics of 112 consecutive patients with a history of cocaine use and coronary angiography were compared with a control group of similar age and risk factors from an existing angiographic database over the same time period. Coronary angiograms were independently read by 3 reviewers blinded to cocaine use. Cocaine users were young (mean age, 44 years), predominantly male (80%), and cigarette smokers (95%). Control patients had higher rates of diabetes (33%) and more severe coronary artery disease (P=0.01). Previous myocardial infarction was common in both groups (45% of cocaine users, 38% of control patients). Despite the frequent history of myocardial infarction among cocaine users, 48% had nonobstructive coronary artery disease. Among cocaine users, 34 of 112 (30.4%) had CAAs compared with 6 of 79 (7.6%) in the control group (P<0.001). Cocaine use was a strong predictor of CAA by univariate and multivariate analyses. Conclusions—This is the first description of an association between cocaine use and CAA. The prevalence of CAA among cocaine users was higher than expected (30.4%), given such a young cohort. Cocaine use may predispose to the formation of CAA, which may in turn be a contributing factor to myocardial infarction.


Circulation | 2002

Pharmacological Treatment of Coronary Artery Disease With Recombinant Fibroblast Growth Factor-2: Double-Blind, Randomized, Controlled Clinical Trial

Michael Simons; Brian H. Annex; Roger J. Laham; Neal S. Kleiman; Timothy D. Henry; Harold L. Dauerman; James E. Udelson; Ernesto V. Gervino; Marilyn Pike; M.J. Whitehouse; Thomas Moon; Nicolas Chronos

Both aspirin and beta-adrenergic blocking drugs have been shown to reduce the risk of death or acute myocardial infarction (AMI) in patients with unstable angina, but their effect during chronic use on the presentation of acute coronary syndromes is less well defined. Calcium antagonists and oral nitrates are also widely prescribed for patients with coronary disease, but their effect on presentation of acute myocardial ischemia is unknown. We retrospectively examined the effects of prior aspirin and anti-ischemic medical therapy on clinical events in 410 patients hospitalized for unstable angina. Ischemic pain occurred at rest for a duration of 5 to 60 minutes. During hospitalization, 97% of patients received aspirin and all received the direct thrombin inhibitor bivalirudin for at least 72 hours. Despite being older and more likely to have risk factors for coronary disease and poor outcome, patients receiving aspirin before admission were less likely to present with non-Q-wave AMI (5% vs 14% in patients not on aspirin, p = 0.004). Prior beta blocker, calcium antagonist, or nitrate administration did not appear to modify presentation as unstable angina or non-Q-wave AMI. In a multivariate model, the combined incidence of death, AMI not present at enrollment, or recurrent angina was best predicted by age (adjusted odds ratio [95% confidence interval] 2.38 [1.14 to 3.98]) and presence of electrocardiographic changes with pain on presentation (adjusted odds ratio 2.83 [1.50 to 5.35]) but was not related to prior or in-hospital medical therapy. Thus, aspirin but not anti-ischemic therapy before hospitalization of patients with unstable angina was associated with a decreased incidence of non-Q-wave AMI on admission.Abstract Both aspirin and β-adrenergic blocking drugs have been shown to reduce the risk of death or acute myocardial infarction (AMI) in patients with unstable angina, but their effect during chronic use on the presentation of acute coronary syndromes is less well defined. Calcium antagonists and oral nitrates are also widely prescribed for patients with coronary disease, but their effect on presentation of acute myocardial ischemia is unknown. We retrospectively examined the effects of prior aspirin and anti-ischemic medical therapy on clinical events in 410 patients hospitalized for unstable angina. Ischemic pain occurred at rest for a duration of 5 to 60 minutes. During hospitalization, 97% of patients received aspirin and all received the direct thrombin inhibitor bivalirudin for at least 72 hours. Despite being older and more likely to have risk factors for coronary disease and poor outcome, patients receiving aspirin before admission were less likely to present with non–Q-wave AMI (5% vs 14% in patients not on aspirin, p = 0.004). Prior β blocker, calcium antagonist, or nitrate administration did not appear to modify presentation as unstable angina or non–Q-wave AMI. In a multivariate model, the combined incidence of death, AMI not present at enrollment, or recurrent angina was best predicted by age (adjusted odds ratio [95% confidence interval] 2.38 [1.14 to 3.98]) and presence of electrocardiographic changes with pain on presentation (adjusted odds ratio 2.83 [1.50 to 5.35]) but was not related to prior or in-hospital medical therapy. Thus, aspirin but not anti-ischemic therapy before hospitalization of patients with unstable angina was associated with a decreased incidence of non–Q-wave AMI on admission.


American Heart Journal | 2001

Intracoronary administration of recombinant human vascular endothelial growth factor to patients with coronary artery disease

Timothy D. Henry; Krishna J. Rocha-Singh; Jeffrey M. Isner; Frank J. Giordano; Michael Simons; Douglas W. Losordo; Robert C. Hendel; G. Robert O. Bonow; Stephen Eppler; Thomas F. Zioncheck; Eric Holmgren; Edward R. McCluskey

It is important to establish as soon as possible whether patients who present with chest pain are having an acute myocardial infarction (AMI). Ideally, sensitive and specific serum myocardial markers could provide the basis for early detection as well as determine the status of reperfusion following thrombolytic therapy. The present study examined the utility of cardiac troponin I (cTnI), CK-MB, and myoglobin for the sensitive and specific detection of AMI in 98 consecutive patients presenting to the emergency department (ED) with chest pain. In addition, cardiac troponin T (cTnT), CK-MB, and myoglobin samples were measured over a 90 min time period following thrombolytic therapy in nine separate AMI patients to assess reperfusion. In the ED study, CK-MB, myoglobin, and cTnI were equally sensitive (100%) for the detection of AMI in patients who presented 7.4-14 h after onset of chest pain. However, cTnI was the most specific serum marker (specificity 91.9% compared to CK-MB 85.6%, myoglobin 61.4%). Five of the six non-related AMI patients who had an elevated cTnI had clinically documented myocardial involvement. In the reperfusion study, cTnT, CK-MB and myoglobin, relative increases were greater in reperfused compared to non-reperfused patients. Within the reperfused group, the relative increase of cTnT was greater than CK-MB and myoglobin at 90 min following thrombolytic therapy. These findings show the clinical utility of cardiac-specific troponins as markers for the early detection of AMI and monitoring of reperfusion following thrombolytic therapy.

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Carolyn H. McCabe

Hennepin County Medical Center

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Christopher P. Cannon

Hennepin County Medical Center

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