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1 (4016 with drug-eluting stents and 3201 with bare-metal stents).
2 d comparable to that in patients receiving a bare metal stent.
3 g stent and 50% for patients who preferred a bare metal stent.
4 osition) in the FP-PES compared with PES and bare metal stent.
5 tent thrombosis rates were 2.0% DCS and 2.2% bare metal stent.
6 year occurred in 7.2% DCS patients and 7.2% bare metal stent.
7 nts with diabetes mellitus (DM) treated with bare-metal stent.
8 apy for the treatment of restenosis within a bare-metal stent.
9 lymer, has shown superiority compared with a bare-metal stent.
10 ry was delayed in patients with DESs but not bare metal stents.
11 utcomes, and relative outcomes of DES versus bare metal stents.
12 panics, who had similar outcomes with DES or bare metal stents.
13 n patients with both drug-eluting stents and bare metal stents.
14 rug-eluting stents and 861 who received only bare metal stents.
15 ly reduced by RSG in SESs but not in PESs or bare metal stents.
16 rosclerosis was a common dominant finding in bare metal stents.
17 epared on both MP35N metal alloy coupons and bare metal stents.
18 complication of both drug-eluting stents and bare metal stents.
19 e put into context with the IVUS findings in bare metal stents.
20 Guard was consistent with that expected from bare metal stents.
21 metallic biolimus-eluting stents and control bare metal stents.
22 eluting compared with everolimus-eluting and bare metal stents.
23 nt compared with both everolimus-eluting and bare metal stents.
24 e commonly found in drug-eluting stents than bare-metal stents.
25 l myocardial infarction in DES compared with bare-metal stents.
26 ]; P<0.001) were higher in DES compared with bare-metal stents.
27 42; 95% CI, 0.15-1.19; P = .10) treated with bare-metal stents.
28 Drug Administration-approved drug-eluting or bare-metal stents.
29 eluting stents compared with those receiving bare-metal stents.
30 ed in drug-eluting stents in comparison with bare-metal stents.
31 ath or ST-elevation myocardial infarction to bare-metal stents.
32 drug-eluting stents, and 6461 received only bare-metal stents.
33 evascularization at 1 year, as compared with bare-metal stents.
34 n procedures as compared with treatment with bare-metal stents.
35 d ability to reduce restenosis compared with bare-metal stents.
36 months after stent implantation, similar to bare-metal stents.
37 atelet therapy longer than is necessary with bare-metal stents.
38 oups with drug-eluting stents and those with bare-metal stents.
39 arget vessel revascularization compared with bare-metal stents.
40 itaxel-eluting stents, and 2267 treated with bare-metal stents.
41 ents and paclitaxel-eluting stents than with bare-metal stents.
42 f either contemporary drug-eluting stents or bare-metal stents.
43 atients without DM or in any group receiving bare-metal stents.
44 HR 0.82, p=0.019), and in patients with only bare-metal stents (10.0 vs 12.2%, HR 0.80, p=0.003).
45 wer with paclitaxel-eluting stents than with bare-metal stents (10.0% vs. 22.9%; hazard ratio, 0.44;
48 ared with PES (10.95 mm(2) [9.64-12.46]) and bare metal stent (13.83 mm(2) [11.53-17.03]; P<0.001).
49 for the competing risk of death was 18% with bare metal stents, 19% with DES, and 6% with coronary ar
50 n old balloon angioplasty (341% increase) to bare metal stent (218% increase) to paclitaxel-eluting s
51 Compared with 749 patients who received a bare-metal stent, 2257 patients who received a paclitaxe
52 rachytherapy, -23.4% (-36.2 to -10.8) versus bare metal stents, -24.2% (-32.2 to -16.4) versus balloo
54 1 LIMA anastomotic stenosis (3.7%), 3 after bare metal stent (30%), and 4 after drug-eluting stent p
56 ant difference in ST between drug-coated and bare-metal stents (4.4% versus 3.4%; P=0.55), but the ra
57 enosis (62%), was more prevalent in DES than bare-metal stents (68% versus 36%; P=0.02), and demonstr
60 -matched groups, mortality was similar after bare-metal stenting (9.8%) and paclitaxel-eluting stenti
61 al infarction rates compared with the use of bare metal stents among all race/ethnicity groups except
62 were lower for drug-eluting stents than for bare-metal stents among all patients with myocardial inf
63 enoses, but optimum treatment strategies for bare metal stent and drug-eluting stent in-stent resteno
64 s revealed binary restenosis rates of 27% in bare metal stents and 0% in drug-eluting stents, with me
65 atients receiving drug-eluting stents versus bare metal stents and bivalirudin alone versus heparin p
66 osis (ST) have included mostly patients with bare metal stents and early-generation drug-eluting sten
67 METHODS AND Animals receiving SESs, PESs, or bare metal stents and either RSG (3 mg/kg per day) or pl
68 e similar after excluding patients receiving bare metal stents and using an alternative MACE definiti
70 l use occurred in 54.7% of all patients with bare-metal stents and 48.7% of patients with drug-elutin
71 o receive either sirolimus-eluting stents or bare-metal stents and five double-blind trials in which
72 ys were assessed in rabbits receiving ZES or bare-metal stents and Mf or placebo by scanning electron
73 hey were treated with drug-eluting stents or bare-metal stents and whether use was standard or off-la
74 atment for CoA, including angioplasty alone, bare metal stenting, and primary covered stent therapy.
75 m outcomes for drug-eluting stents (DES) and bare metal stents, and most are relatively small randomi
77 eous revascularization with drug-eluting and bare metal stents associates with a high risk of in-sten
78 d quercetin (Q)-eluting stent with that of a bare metal stent (BMS) on neointimal hyperplasia and re-
79 outflow tract obstruction is possible with a bare metal stent (BMS), although this treatment causes p
83 , 16.3] to 7.7 [5.4, 9.9], P<0.0001), behind bare metal stents (BMS) (18.5 [13.2, 23.8] to 12.0 [6.7,
84 (PCI) with drug-eluting stents (DES) versus bare metal stents (BMS) has not been studied in the kidn
85 y of different drug-eluting stents (DES) and bare metal stents (BMS) in patients with ST-segment elev
86 luting stents (PES) and otherwise equivalent bare metal stents (BMS) in ST-segment elevation myocardi
88 ct of paclitaxel-eluting stents (PES) versus bare metal stents (BMS) on distal vessels in the serial
89 o estimate the relative impact of DES versus bare metal stents (BMS) on safety and efficacy end point
90 uting stent resolute), against each other or bare metal stents (BMS), and enrolling >/= 50 patients w
92 nary drug-eluting stents (DES) compared with bare metal stents (BMS), the relative risk of stent thro
98 ncoated balloon angioplasty for treatment of bare-metal stent (BMS) and drug-eluting stent (DES) rest
99 t therapy is safer and more effective than a bare-metal stent (BMS) for patients with high risk of bl
100 paclitaxel-eluting stent (PES) and a similar bare-metal stent (BMS) in saphenous vein graft (SVG) les
104 treated with drug-eluting balloon (DEB) plus bare-metal stent (BMS) versus BMS versus drug-eluting st
105 ive randomized comparisons of the SES to the bare-metal stent (BMS), and two were prospective non-ran
107 ith improved clinical outcomes compared with bare-metal stents (BMS) among a nationally representativ
108 tiveness of drug-eluting stents (DES) versus bare-metal stents (BMS) among patients >/=85 years of ag
109 erm efficacy and safety of DES compared with bare-metal stents (BMS) and among the DES types are less
110 long-term clinical outcomes differed between bare-metal stents (BMS) and drug-eluting stents (DES) by
112 sponses at bifurcation after implantation of bare-metal stents (BMS) and drug-eluting stents (DES).
113 s with VLST and compare the findings between bare-metal stents (BMS) and drug-eluting stents (DES).
114 fter percutaneous coronary intervention with bare-metal stents (BMS) and first-generation and second-
115 on drug-eluting stents (n-DES) compared with bare-metal stents (BMS) and old-generation drug-eluting
116 ion with paclitaxel-eluting stents (PES) and bare-metal stents (BMS) and to formally evaluate the inc
117 e-polymer (DP)-drug-eluting stents (DES) and bare-metal stents (BMS) by means of a network meta-analy
118 DES) platforms, previous generation DES, and bare-metal stents (BMS) for percutaneous coronary interv
121 differences in outcome after implantation of bare-metal stents (BMS) have been described, there are n
122 ompared everolimus-eluting stents (EES) with bare-metal stents (BMS) in an all-comer population with
125 t their long-term safety relative to that of bare-metal stents (BMS) in general use remains uncertain
126 nts has equal risks but higher efficacy than bare-metal stents (BMS) in long femoropopliteal artery d
127 er drug-eluting stents (DES) are superior to bare-metal stents (BMS) in octogenarian patients with an
128 y of drug-eluting stents (DES) compared with bare-metal stents (BMS) in older patients with chronic k
129 vessel revascularization in comparison with bare-metal stents (BMS) in patients with chronic kidney
131 imus-eluting stents (SES) in comparison with bare-metal stents (BMS) in treatment of focal infrapopli
135 ous coronary intervention (PCI) using either bare-metal stents (BMS) or drug-eluting stents (DES).
136 th a unique drug fast-release profile versus bare-metal stents (BMS) under similar durations of dual-
137 ortality among drug-eluting stents (DES) and bare-metal stents (BMS) while adjusting for many confoun
138 luminal balloon coronary angioplasty (PTCA), bare-metal stents (BMS), and drug-eluting stents (DES) s
139 d improved efficacy and safety compared with bare-metal stents (BMS), and international guidelines re
140 duce repeat revascularizations compared with bare-metal stents (BMS), but their effects on death and
141 d for repeat revascularization compared with bare-metal stents (BMS), data suggest the window of thro
142 ed with higher rate of late ST compared with bare-metal stents (BMS), especially in patients with ST-
143 ry intervention to SVG in patients receiving bare-metal stents (BMS), first-generation DES, and newer
144 r 1 and between 1 and 5 years after PCI with bare-metal stents (BMS), first-generation drug-eluting s
145 slates into superior outcomes, compared with bare-metal stents (BMS), for the full spectrum of patien
146 data on the restenosis benefit of DES versus bare-metal stents (BMS), the incremental risk of stent t
147 of ST with drug-eluting stents (DES) versus bare-metal stents (BMS), the timing of the event, clinic
148 stents (DES) reduce restenosis compared with bare-metal stents (BMS), virtually all of these studies
155 erent types of drug-eluting stents (DES) and bare-metal stents (BMS); however, most prior trials in t
156 and neointimal proliferation of a therapy of bare metal stents (BMSs) postdilated with the paclitaxel
157 ng biolimus from a biodegradable polymer and bare-metal stents (BMSs) in the COMFORTABLE trial (Compa
158 ive safety of drug-eluting stents (DESs) and bare-metal stents (BMSs) with respect to stent thrombosi
159 dom from myocardial infarction compared with bare metal stents, but increase the risk of stent thromb
160 uting stents reduce restenosis compared with bare metal stents, but there is growing concern that dru
161 ificantly different in patients treated with bare metal stents compared with drug-eluting stents (1.4
162 ent-graft implantation and/or placement of a bare metal stent, complications, and follow-up images we
163 g stents reduce restenosis rates relative to bare-metal stents, concerns have been raised that drug-e
164 used to characterize NA in 65 (51 DES and 14 bare-metal stents) consecutive symptomatic patients with
165 (n=12) and PES (n=12) was compared against a bare metal stent control (n=12; Innova, Boston Scientifi
167 abetes mellitus, stent type (drug-eluting or bare metal stent), CYP2C19 genetic status, loading dose
171 when only bare-metal stents were available (bare-metal stent era cohort) and 28,086 similar patients
172 ty era), group 2 (early stent era), group 3 (bare-metal stent era), and group 4 (drug-eluting stent e
174 Studies from the balloon angioplasty and bare metal stent eras have demonstrated that coronary ar
176 us coronary intervention (PCI) often receive bare-metal stents followed by 1 month of dual antiplatel
177 rovides better clinical outcomes compared to bare-metal stenting for ULMCA disease, there is a paucit
178 een shown to be cost-effective compared with bare-metal stents for select clinical trial patients, wh
180 % confidence interval 0.22 to 0.95]) and the bare-metal stent group (0.64 [95% confidence interval 0.
181 n the Taxus group and 0.76% +/- 0.23% in the bare-metal stent group at 3 years (hazard ratio 1.51 [95
182 the sirolimus-stent group versus 0.6% in the bare-metal-stent group (P=0.20) and 1.3% in the paclitax
183 the sirolimus-stent group versus 0.6% in the bare-metal-stent group (P=0.20; 95% confidence interval
184 he paclitaxel-stent group versus 0.8% in the bare-metal-stent group (P=0.24; 95% CI, -0.3 to 1.4).
186 he paclitaxel-stent group versus 1.4% in the bare-metal-stent group (P=0.52; 95% CI, -0.7 to 1.4).
187 the sirolimus-stent group versus 1.7% in the bare-metal-stent group (P=0.70; 95% CI, -1.5 to 1.0) and
188 ent group and in 154 patients (12.9%) in the bare-metal-stent group (risk difference, -3.6 percentage
189 tent group and in 113 patients (9.8%) in the bare-metal-stent group (risk difference, -4.8 percentage
190 the sirolimus-stent group versus 0.4% in the bare-metal-stent group and 0.9% in the paclitaxel-stent
193 drug-eluting stent showed similar safety as bare-metal stent >12 months and between 6 and 12 months
194 itaxel-eluting stents and those treated with bare-metal stents had similar 12-month rates of death (3
195 tients receiving drug-eluting stents (versus bare-metal stents) had a lower 30-month mortality (IPW H
196 stents, as compared with those who received bare-metal stents, had significantly lower 12-month rate
198 rials of approved drug-eluting stents versus bare metal stents have shown additional cases of late st
199 -stent restenosis in the cohort treated with bare-metal stents (hazard ratio [HR] = 2.03 [95% confide
200 ble polymer and 49 patients (8.7%) receiving bare-metal stents (hazard ratio [HR], 0.49; 95% CI, 0.30
201 ting stents and 19.8% in the group receiving bare-metal stents (hazard ratio, 0.76; 95% CI, 0.69 to 0
202 ting stents and 17.1% in the group receiving bare-metal stents (hazard ratio, 0.98; 95% confidence in
203 dence interval [CI], 0.61, 0.82; P<0.01) and bare metal stents (HR, 0.85; 95% CI, 0.76, 0.96; P=0.01)
204 (HR, 0.70; 95% CI, 0.64, 0.84) compared with bare metal stents (HR, 0.88; 95% CI, 0.79, 0.98; interac
205 ould be postponed for at least 4 weeks after bare metal stent implantation and 6-12 months after drug
206 xel-eluting stent implantation compared with bare metal stent implantation was modified by angiograph
207 surgery be delayed until 30 to 45 days after bare-metal stent implantation and 1 year after drug-elut
208 for elective surgery is 46 to 180 days after bare-metal stent implantation or >180 days after drug-el
209 r drug-eluting stent placement compared with bare-metal stent implantation remain unsettled, with con
210 llowed by provisional self-expanding nitinol bare-metal stent implantation with a strategy of systema
211 ly approved therapy for restenosis following bare-metal stent implantation, drug-eluting stents are n
213 imus A9 Drug Coated Stent Versus the Gazelle Bare Metal Stent in Patients With High Risk of Bleeding
215 s Eluted From an Erodible Stent Coating With Bare Metal Stents in Acute ST-Elevation Myocardial Infar
216 lled in the DIVA (Drug-Eluting Stents Versus Bare Metal Stents in Saphenous Vein Graft Angioplasty; N
217 relative risks of drug-eluting stents versus bare metal stents in specific high-risk groups require f
219 g drug-eluting stent performance relative to bare metal stents in the setting of acute myocardial inf
220 ed the drug-coated stent with a very similar bare-metal stent in patients with a high risk of bleedin
223 ents with drug-eluting stents and those with bare-metal stents in randomized clinical trials, althoug
224 ving drug-eluting stents and those receiving bare-metal stents in the composite outcome of death from
225 ing stents may have clinical advantages over bare-metal stents in the extremely proliferative environ
226 acy of drug-eluting stents, as compared with bare-metal stents, in patients with ST-segment elevation
230 were reported between drug-eluting stent and bare-metal stent ISR groups in terms of device-oriented
231 treatment of complex drug-eluting stent and bare-metal stent ISR lesions might be associated with ac
232 Results of 94 patients treated with EES for bare-metal stent ISR were compared with those of 155 pat
236 s (1077 ISR lesions) distributed as follows: bare metal stent (n=388), first-generation DES (n=425),
238 reatment with paclitaxel DEB and provisional bare-metal stenting (n = 90) or PES implantation (n = 92
239 litaxel-coated balloon angioplasty (N=3543), bare-metal stenting (N= 2045) versus paclitaxel-eluting
240 therosclerosis (n =10) or implanted coronary bare-metal stents (n = 10, 3.5-mm diameter, day 7 post-i
242 ing the benefits of drug-eluting stents over bare-metal stents observed in randomized clinical trials
243 rary drug-eluting stents versus contemporary bare-metal stents on rates of death, myocardial infarcti
244 2.31%, HR 0.36, p<0.0001), and in those with bare-metal stents only (1.27 vs 2.41%, HR 0.52, p=0.0009
247 s (such as conventional balloon angioplasty, bare-metal stents, or drug-eluting stents) for the treat
248 were 4.4% with both drug-eluting stents and bare metal stents (P=0.98) and 4.3% versus 4.6% in patie
249 -eluting stents versus none in patients with bare-metal stents (P=0.025) and nine episodes in patient
252 Stent) and RIBS V (Restenosis Intra-Stent of Bare Metal Stents: Paclitaxel-Eluting Balloon vs Everoli
254 eriod, there was no change in the percent of bare-metal stent patients reporting clopidogrel use at 6
256 404 days (P < .001) and decreased following bare metal stent placement from 402 to 309 days (P < .00
258 0% to 13% after angioplasty, 0% to 5% after bare metal stent placement, and <1% after covered stent
261 se mortality included balloon angioplasty or bare-metal stent placement compared with drug-eluting st
262 Between 1992 and 2010, 27 patients underwent bare-metal stent placement in the ventricular septum or
263 raphy, fractional flow reserve measurements, bare-metal stents, postprocedural medications, and radia
264 safety of drug-eluting stents compared with bare-metal stents remains controversial in patients with
268 ns of balloon angioplasty or with the use of bare-metal stents, results in greater relief from angina
269 ty rates were 14.5% for DES versus 23.0% for bare metal stents (risk difference, -8.5%; P<0.001), an
271 paclitaxel-eluting stents, as compared with bare-metal stents, significantly reduced angiographic ev
273 limitations of plain balloon angioplasty and bare-metal stents, some limitations apply, most notably
274 1 to receive a paclitaxel-eluting stent or a bare metal stent (stent randomisation; stratified by pha
275 e Initial Double-Blind Drug-Eluting Stent vs Bare-Metal Stent Study, NCT00233805; The Study of the BX
277 effects of drug-eluting stents compared with bare-metal stents, the evidence seems to suggest that th
281 usted differences in outcomes for DES versus bare metal stents using a 2-stage least squares instrume
283 erval was 45 to 180 days, the event rate for bare-metal stents was 2.6%, approaching that of intermed
284 ceived a balanced mixture of drug-eluting or bare-metal stents was not significantly more effective t
285 using human coronary artery sections with a bare metal stent, we demonstrate the expression of Fn-ED
286 receive either paclitaxel-eluting stents or bare-metal stents; we then analyzed the major clinical e
289 IIa inhibitor and use of drug-eluting versus bare metal stents were not significant predictors of rei
290 om October 2002 through March 2003 when only bare-metal stents were available (bare-metal stent era c
291 revascularization) with drug-eluting versus bare-metal stents were compared using inverse probabilit
292 ving drug-eluting stents and those receiving bare-metal stents were determined from vital-statistics
293 covered stents, and 11.2% balloon expandable bare metal stents) were placed in 692 renal arteries, 15
296 g-eluting stents as compared with those with bare-metal stents, whereas the risk of repeat revascular
297 entional cardiologists have quickly replaced bare metal stents with intravascular drug-eluting stents
298 ee umirolimus-coated stent was superior to a bare-metal stent with respect to the primary safety and
299 e patients randomized to drug-eluting versus bare-metal stents with successful stenting documented by