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1 coronary catheter with the tip distal to the coronary lesion.
2 ation (Hosmer-Lemeshow P=0.540) for an acute coronary lesion.
3 /=0.8 was regarded to indicate a significant coronary lesion.
4 gold standard for a hemodynamic significant coronary lesion.
5 nt interventional tool for heavily calcified coronary lesions.
6 vascular ultrasound-guided stenting of 1,015 coronary lesions.
7 e best method for interrogating intermediate coronary lesions.
8 tal stents (BMS) in the treatment of de novo coronary lesions.
9 trasound analysis was performed in 46 native coronary lesions.
10 stenosis after stent implantation in de novo coronary lesions.
11 ice-independent relationships seen in native coronary lesions.
12 he preferred treatment for heavily calcified coronary lesions.
13 nlargement commonly (54%) occurs at stenotic coronary lesions.
14 es, of functionally significant intermediate coronary lesions.
15 lanned stent implantation in de-novo, native coronary lesions.
16 curate in detecting functionally significant coronary lesions.
17 FFR was </=0.80 in 54 of 144 (38%) coronary lesions.
18 the gold standard for assessing intermediate coronary lesions.
19 tual histology IVUS and FFR for intermediate coronary lesions.
20 drug-eluting stents implantation in de novo coronary lesions.
21 ve, more targeted treatment of KD to prevent coronary lesions.
22 icient mice were protected from LCWE-induced coronary lesions.
23 simple and medium complexity single de novo coronary lesions.
24 ly identified necrotic core in ex vivo human coronary lesions.
25 vascular smooth muscle cells in the advanced coronary lesions.
26 t natural history trajectories of individual coronary lesions.
27 ding treatment of patients with intermediate coronary lesions.
28 tion fraction <40%), as well as more complex coronary lesions.
29 performed in 689 patients with 1,639 native coronary lesions.
30 tage of stenosis, and the development of new coronary lesions.
31 -IV trial, 1314 patients with single de novo coronary lesions 10 to 28 mm in length, with reference-v
33 bstudy enrolled 241 patients with 263 native coronary lesions (201 PES, 62 BMS) with baseline and 13-
34 y II included fewer left anterior descending coronary lesions (46.5% vs. 32.8%, p < 0.01), more type
36 on angioplasty was performed in 1,266 native coronary lesions alone (n = 541) or after extraction ath
37 rediction model for the presence of an acute coronary lesion among patients resuscitated from an arre
38 y should be favored in patients with complex coronary lesions and anatomy and PCI in less complicated
39 ogical significance of intermediate severity coronary lesions and cases with inadequate image quality
40 ts who underwent intervention of 2780 native coronary lesions and had complete high-quality preinterv
41 ure, minimum lumen diameter (MLD), number of coronary lesions and total occlusions were not significa
42 c patients or those with ischaemia-producing coronary lesions, and reduces ischaemia to a greater ext
43 sclerosis, BMI, as well as CRP and number of coronary lesions, are independently associated with acut
47 We randomized 704 patients with bifurcation coronary lesions at 58 centers (30 from Europe and 28 fr
49 e effective in reducing restenosis in simple coronary lesions, but the evidence base for contemporary
51 hology and composition of culprit and stable coronary lesions by multidetector computed tomography (M
52 ention remodeling was assessed in 108 native coronary lesions by using intravascular ultrasound (IVUS
54 quent restenosis rates at 6 months in native coronary lesions (CAVEAT I, 50.8% for intimal resection
55 s the prediction of functionally significant coronary lesions compared with visual CTCA assessment bu
56 shed by clinical variables, they had greater coronary lesion complexity by American Heart Association
59 ional registry of patients with intermediate coronary lesions, defined as 40% to 80% stenosis by angi
63 basis that the majority of these individual coronary lesions do not in fact go on to cause clinical
65 ) with each other or against BMS for de novo coronary lesions, enrolling at least 100 patients and wi
66 accuracy for the detection of flow-limiting coronary lesions (FFR</=0.80) was compared with visual C
67 cium channel-blocking agents may prevent new coronary lesion formation, the progression of minimal le
71 ally colocalized to apoptotic VSMCs in human coronary lesions, further supporting a functional role f
73 Although effective coverage of challenging coronary lesions has warranted the use of overlapping dr
74 rasound imaging was used to study 212 native coronary lesions in 209 patients after percutaneous tran
75 .3 months) IVUS was used to study 251 native coronary lesions in 241 patients; 63 patients had treate
76 Thirty patients with at least 2 significant coronary lesions in different vessels were treated with
81 ta play critical roles in the development of coronary lesions in this KD mouse model, blocked by IL-1
82 liminary reports of studies involving simple coronary lesions indicate that a sirolimus-eluting stent
83 f WT and 100% of B cell(null) mice developed coronary lesions, indicating that T cells were required
87 lantation of the DREAMS 2G device in de-novo coronary lesions is feasible, with favourable safety and
88 n the era of drug-eluting stents for diffuse coronary lesions, IVUS-guided percutaneous coronary inte
89 A total of 1043 patients with focal de novo coronary lesions, <25 mm in length, in 2.5- to 4.0-mm ve
92 coronary stent deployment have more complex coronary lesion morphology and a more complicated clinic
94 ntly from the development of significant new coronary lesions, not initially severe enough to cause i
96 racoronary physiological evaluation of >/= 1 coronary lesion of intermediate severity between April 1
98 mposition and macrophage infiltration in the coronary lesions of patients with diabetes mellitus.
99 32, p = 0.005) and minimum lumen diameter of coronary lesions (OR: 1.83, 95% CI: 1.01 to 3.55, p = 0.
102 e myocardial jeopardy index, total number of coronary lesions, prior coronary revascularization, and
104 al coronary events was positively related to coronary lesion progression for all three surrogate end
105 s compared with bare metal stents in de novo coronary lesions reduces major adverse cardiac events in
110 Use of CCTA for physiological evaluation of coronary lesion-specific ischemia may facilitate evaluat
111 trial recruited patients with de novo native coronary lesions suitable for 1- or 2-vessel treatment w
112 lternative strategy that can target multiple coronary lesions suitable for treatment with any approve
115 ses were possible both of differences in the coronary lesions that developed in a normolipidemic as c
116 surgical treatment of significantly stenotic coronary lesions, the comprehensive and serial assessmen
117 inical trial involving patients with complex coronary lesions, the use of a sirolimus-eluting stent h
119 Thirty-one patients with de novo native coronary lesions treated with DCA in the Serial Ultrasou
121 trasound was used to study 25 de novo native coronary lesions treated with single MultiLink stents wi
126 Eighty-four stable patients with isolated coronary lesions underwent coronary stent deployment sta
129 nsitivity but improved specificity for right coronary lesions using attenuation/scatter correction me
130 or the detection of functionally significant coronary lesions using fractional flow reserve (FFR) as
131 gle-arm trial evaluating outcomes in de novo coronary lesions visually estimated to be 10 to 28 mm in
134 timal cutoff values to predict flow-limiting coronary lesion were 10 mm for lesion length, 1.8 mm2 fo
136 IV trial, 1,314 patients with single de novo coronary lesions were assigned to implantation of the sl
138 Before the introduction of DES, intermediate coronary lesions were commonly managed based on physiolo
140 lysis also showed that CRP and the number of coronary lesions were independent predictors of risk of
143 trial, in which 1,314 patients with de novo coronary lesions were randomized to either the paclitaxe
144 in 1,226 consecutive patients (1,259 native coronary lesions) who underwent a single vessel interven
145 g patients with stable angina and at least 1 coronary lesion with a fractional flow reserve </=0.80 w
147 termined in normal and atherosclerotic human coronary lesions with a monoclonal antibody to human PLT
149 nical interpretation of stenosis severity in coronary lesions with an independent assessment using qu
150 icient recipients had more severe aortic and coronary lesions with characteristic T cell infiltration
155 utaneous revascularization of de novo native coronary lesions with reference vessel diameters between
156 atherosclerotic lesions, we studied 20 human coronary lesions with techniques that have previously be
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