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1 ulatory support, or hospital discharge on an inotrope.
2 as been shown ex vivo to be a potent cardiac inotrope.
3 /- 63.1 vs. 215.5 +/- 68.1), and duration of inotrope.
4 cardia and intractable hypotension requiring inotropes.
5 d lower cumulative doses of vasopressors and inotropes.
6 or to that of patients who were bridged with inotropes.
7 rbidity scores, and need for vasopressors or inotropes.
8 xic antimicrobials, vasopressin, or specific inotropes.
9 ssure, peripheral edema, ascites, and use of inotropes.
10 cts that are commonly observed with positive inotropes.
11 anted, 32 received LVADs, and 50 remained on inotropes.
12 evaluates contemporary outcomes on long-term inotropes.
13 in patients who were offered LVAD but chose inotropes (15 patients), and for palliation (98 patients
15 dy, 68 patients had died, 24 were weaned off inotropes, 23 were transplanted, 32 received LVADs, and
17 ortic balloon pump usage (8.5% versus 7.5%), inotrope (39% versus 50%) and vasoconstrictor usage (66%
18 % versus 5.3%; P<0.001), require intravenous inotropes (41.4% versus 37.2%; P<0.001), and were less l
19 male patients), patients were on 2.0 +/- 0.9 inotropes, 7 (35) had an intra-aortic balloon pump, 2 we
20 tilation, 8% versus 19%; vasopressors and/or inotropes, 9% versus 16%; vasodilators, 6% versus 12%; a
22 therapy, a higher percentage were prescribed inotropes after publication (3272 [21.5%] of 15 193 pati
28 Score II, even when assessing the effect of inotrope and vasoactive treatments at 24, 48, and 72 hou
29 r and peak cTnT, ECG changes, cardiac index, inotrope and vasoconstrictor use, renal dysfunction, and
30 udes the management of neuraxial anesthesia, inotrope and vasopressor support, transthoracic echocard
31 esulted in the identification of 17 positive inotropes and 21 positive lusitropes, almost all of them
32 the DCDD group, donor age < 40 years, use of inotropes and absence of gag/cough reflexes were predict
33 or poor ejection fraction, and the need for inotropes and an intra-aortic balloon pump (OR 1.72 to 4
34 etween mortality and compliance with each of inotropes and red cell transfusions, glucocorticoids, an
35 Status 1A registrants supported with dual inotropes and right heart monitoring had a higher risk o
36 hat cooling can reduce the need for positive inotropes and that lower rather than higher temperatures
37 Twenty-one patients required intravenous inotropes and three patients required extracorporeal mem
38 probability of inadequate oxygen delivery on inotropes and vasoactive infusions (IVAI) postoperativel
39 ) over 5 to 10 mins (2C); more common use of inotropes and vasodilators for low cardiac output septic
41 eart rate of >120 beats/min, requirement for inotropes and vasopressors after surgery and on admissio
43 n 80/85 and 100 mm Hg with additional use of inotropes and vasopressors was associated with smaller m
47 et of symptoms <1 month) of whom 55 required inotropes and/or mechanical circulatory support (FM) and
49 th longer ischemic times, longer duration of inotrope, and correspond with higher glucose levels.
50 replacement therapy, use of vasopressors and inotropes, and association with cardiac index, lactate,
52 , in which intravenous fluids, vasopressors, inotropes, and blood transfusions were adjusted to reach
54 iod; administration of fluids, vasopressors, inotropes, and packed red blood cells titrated to hemody
56 than 3 L/min/m was targeted with IV fluids, inotropes, and RBC transfusion starting from cardiopulmo
58 ndothelium-dependent vasodilators and potent inotropes, and the apelin system has a reciprocal relati
60 itted to ICU in frank septic shock requiring inotropes, and with demonstrable septic myocardial depre
61 risk (P=0.012 and P=0.006 compared with non-inotrope- and inotrope-based controls, respectively), as
62 0.003) or any control therapy, including non-inotrope- and inotrope-based therapies (RR(MH), 1.54; 95
64 hat increase cardiac contractility (positive inotropes) are theoretically appealing as a heart failur
65 lume index of <30 mL/min/m2, requirement for inotropes, arterial bicarbonate of <20 mmol/L, plasma gl
66 ion fraction <30%, pre-operative intravenous inotropes, arterial vascular disease, and higher degree
71 (OR, 1.5; 95% CI, 1.1-2.0), support with >/=inotropes at HT (OR, 1.7; 95% CI, 1.2-2.5), hospitalizat
72 f worsening renal function compared with non-inotrope-based control (RR(MH), 1.52; 95% CI, 1.16 to 2.
73 and P=0.006 compared with non-inotrope- and inotrope-based controls, respectively), as did nesiritid
74 control therapy, including non-inotrope- and inotrope-based therapies (RR(MH), 1.54; 95% CI, 1.19 to
75 scular problems from overuse of diuretics or inotropes because of the unusual loading conditions in T
79 but include medical therapy with intravenous inotropes, biventricular assist devices (Bi-VADs) and th
83 waitlist death or deterioration of status 1A inotrope candidates relative to status 2 candidates decr
84 to determine whether candidates listed with inotropes contribute to the excess status 1A candidates.
85 nds suggest that overtreatment with multiple inotropes contributes to the current critical excess of
86 levant concentrations of stress hormones and inotropes could directly affect the iron binding of seru
87 We report that 17 positive and 9 negative inotropes covering diverse mechanisms of action exerted
90 n of Nontransplant-Eligible Patients Who Are Inotrope Dependent) trial was a prospective, nonrandomiz
91 ntubated and on prostaglandin, 24 (89%) were inotrope dependent, and 22 (81%) had no antegrade flow f
97 sults was performed to estimate survival for inotrope-dependent and inotrope-independent patients.
98 -year-old man with progressive, debilitating inotrope-dependent heart failure due to ischemic cardiom
99 ) support on survival and quality of life in inotrope-dependent heart failure patients ineligible for
103 eligible patients, mean life expectancy with inotrope-dependent medical therapy is estimated at 9.4 m
104 options for end-stage heart failure include inotrope-dependent medical therapy, orthotopic heart tra
107 </= 2.2 l/min/m(2) without inotropes or were inotrope-dependent on optimal medical management, or lis
108 SGD 106 458 (US $79 446) per QALY gained for inotrope-dependent patients and SGD 174 798 (US $130 446
109 , United Network for Organ Sharing status I (inotrope-dependent) heart transplant (n = 3) or urgent i
111 , antibacterials, narcotics, antipsychotics, inotropes, digoxin, anesthetic agents, bronchodilators,
113 therapy algorithm for intravenous fluid and inotrope (dopexamine) infusion during and 6 hours follow
115 MACS-defined RHF was superior to postimplant inotrope duration alone in the prediction of all-cause m
117 al differences; broadly, ssTnI is a positive inotrope, especially under acidic/hypoxic conditions, wh
118 t of patient-centered outcomes in studies of inotropes for end-stage HF with reduced ejection fractio
122 13 [0-25] vs 15 [0-25]; p = 0.8) and pressor/inotrope-free days (median and interquartile range, 25 [
131 rdiogenic shock consists of vasopressors and inotropes; however, these agents can increase myocardial
132 7; P=0.003), defect size (HR=1.09; P=0.026), inotropes (HR=4.18; P=0.005), and absence of revasculari
135 Endothelin-1 (ET-1) is a potent positive inotrope in vitro, but its physiological effects on intr
137 cubation of S epidermidis with catecholamine inotropes in the presence of human plasma resulted in a
140 eceiving multiple catecholamine pressors and inotropes, including dobutamine (n=10), epinephrine (n=8
142 umber of candidates listed as status 1A with inotropes increased by 193 a year, whereas the dobutamin
143 nges and structural assumptions, whereas the inotrope-independent ICER consistently exceeded the high
144 GD 174 798 (US $130 446) per QALY gained for inotrope-independent patients (with 59% and 19% probabil
148 cal generalized linear models (0.113 for any inotrope) indicated that a noteworthy proportion of the
149 ons in operating room hemodynamic practices (inotrope infusion >60 minutes and vasopressor infusion >
150 an- and hospital-level variation existed for inotrope infusion (ICC, 6.2% [95% CI, 4.2%-8.0%] vs 17.9
151 higher for patients at hospitals with higher inotrope infusion rates (adjusted odds ratio [AOR], 1.98
153 rapy, bridging to heart transplantation with inotropes is thought to be the preferred treatment optio
158 ren were supported with multiple intravenous inotropes+/-mechanical ventilation (6) or ECMO (3) befor
160 dverse clinical outcomes, including need for inotropes, mechanical ventilation, meningitis, and death
161 dged to heart transplantation with either IV inotropes (n = 38) or an implantable LVAD (n = 66; Heart
163 mortality or HF hospitalization were need of inotropes, New York Heart Association class or natriuret
164 val 1.04 to 1.17; p = .005), and infusion of inotropes (odds ratio 4.7; 95% confidence interval 1.3 t
166 =6.5 [CI, 1.39-50.15]), and increased use of inotropes on ECMO (OR=3.77 [CI, 1.39-11.07]), whereas LV
167 brane oxygenation cardiac arrest, the use of inotropes on extracorporeal membrane oxygenation, and po
169 tratified by bridging modality: no bridging, inotropes only, intra-aortic balloon pump (IABP), tempor
170 ardiovascular effects of a novel intravenous inotrope, OPC-18790, the observed benefits on contractil
172 age, greater FiO2 and PEEP requirements and inotrope or anticoagulant use were associated with incre
174 transplantation with either intravenous (IV) inotropes or an implantable left ventricular assist devi
175 t failure needing intravenous treatment with inotropes or diuretics was the most common adverse event
176 stry form; and/or (ii) pre-procedural use of inotropes or mechanical circulatory support devices and/
178 Under these circumstances, treatment with inotropes or renal vasodilators may be more appropriate
180 greater risk of patient-important bleeding: inotropes or vasopressors (HR, 2.05 [95% CI = 1.35, 3.12
184 5%, cardiac index </= 2.2 l/min/m(2) without inotropes or were inotrope-dependent on optimal medical
188 tropes for palliation or those who preferred inotropes over LVAD had median survival of 9.0 months (i
190 acidosis (P:=0.03), need for bicarbonate or inotropes (P:=0.008 and 0.04), and ventricular dysfuncti
191 PaO2/FIO2 less than 300, use of vasopressors/inotropes, pancreatitis, hepatic failure/cirrhosis with
193 creatinine concentration >3.0 mg/dL, use of inotropes, presence of myocardial stun, and requirement
194 led Doppler-derived risk groups, intravenous inotrope requirement and blood urea nitrogen as signific
195 ICU admission and predicts ICU mortality and inotrope requirement as well as or better than APACHE II
197 of shock, intensive care unit admission and inotrope requirement, and increased inflammatory markers
198 was associated with reductions in procedural inotrope requirement, intensive care unit and hospital l
199 adjusting for age, sex, listing status, and inotrope requirement, waitlist mortality risk was lower
200 enal dysfunction (44% > 44% > 35% > 29%) and inotrope requirements (52% > 25% > 36% > 29%) were lower
201 unit stay (p = 0.175), survival (p = 0.877), inotrope requirements (p = 0.495), need for extracorpore
202 patients with the TAH have no postoperative inotrope requirements, arrhythmias or inflow/outflow can
203 nical ventilation and biochemical variables, inotrope requirements, extracorporeal membrane oxygenati
208 erapy (odds ratio, 4.89; 3.83-6.28), and for inotrope(s) and/or vasopressor(s) (odds ratio, 3.64; 2.8
210 al replacement therapy was needed in 23% and inotropes(s) and/or vasopressor(s) in 77% of studied pat
211 vity assay of serum troponin T at 72 hours), inotrope score (calculated from the maximum dose of the
212 FIO2, oxygenation index, and 24-hour maximal inotrope score (p</=0.02), although end-tidal alveolar d
213 s 27%), more severe haemodynamic impairment (inotrope score 279 mug/kg per min vs 145 mug/kg per min,
214 ee patients (75%) had a change in Vasoactive-Inotrope Score after the fluid bolus, of whom 60% receiv
215 Organ Dysfunction 2 score, day 0 vasopressor-inotrope score and fluid balance, and PaO2/FIO2 6 hours
217 or less) and severe haemodynamic compromise (inotrope score at least 75 mug/kg per min or lactic acid
218 aO2/FIO2, oxygenation index, 24-hour maximal inotrope score, and Pediatric Risk of Mortality III (all
219 nation of oxygenation index, 24-hour maximal inotrope score, and Pediatric Risk of Mortality III.
220 nation of oxygenation index, 24-hour maximal inotrope score, and Pediatric Risk of Mortality III.
222 ore-1, Pediatric Logistic Organ Dysfunction, inotrope score, duration of ventilation and pediatric IC
223 l length of stay, primary graft dysfunction, inotrope score, mechanical circulatory support use, cere
224 t ventricular (RV) adrenergic remodeling for inotrope selection and the therapeutic benefit of interr
225 100 versus 107 mm Hg in those not receiving inotropes, serum sodium was 134 versus 137 mEq/L, and le
226 d Circulatory Support class, use of multiple inotropes, severe right ventricular dysfunction on echoc
230 d that clinically relevant concentrations of inotropes, such as amrinone and dopamine, which increase
232 .25]; RD, -0.09 [95% CI, -0.22 to 0.05]), or inotrope support (RR, 0.77 [95% CI, 0.51 to 1.17]; RD, -
233 d as the need for post-operative intravenous inotrope support for >14 days, inhaled nitric oxide for
234 rt, mechanical ventilation with vasopressors/inotrope support, mechanical ventilation without hemodyn
237 This underscores an unmet need for positive inotropes that improve heart function without any advers
238 neutrophils were pretreated with or without inotropes, then stimulated with n-formyl methyl leucine
239 exception requests and fewer candidates with inotrope therapy than expected, thus leading to signific
240 90 mm Hg, and red blood cell transfusions or inotropes to attain a central venous oxygen saturation o
241 ive iron showed the ability of catecholamine inotropes to facilitate acquisition of iron by S epiderm
242 s in 2006, transplant programs used multiple inotropes to list candidates at status 1A more frequentl
243 ability of catecholamine stress hormones and inotropes to stimulate the growth of infectious bacteria
248 trograde cardioplegia had significantly less inotrope use (71% versus 84%, P:=0.002), right ventricul
249 ), a medical diagnosis (hazard ratio, 1.43), inotrope use (hazard ratio, 3.47), and treatment limitat
250 % CI, 1.2-8.2), and had a longer duration of inotrope use (median, 5.5 [IQR, 4-8] vs 4.0 [IQR, 3-6] d
251 1 to 5.70; P<0.001), intraoperative multiple inotrope use (OR, 2.75; CI, 1.75 to 4.31; P<0.001), intr
253 47; P=0.0001) and a significant reduction in inotrope use 6 to 12 hours postoperatively (odds ratio,
254 t to characterize institutional variation in inotrope use among patients hospitalized with heart fail
256 te hospital-level risk-standardized rates of inotrope use and risk-standardized in-hospital mortality
257 y of atrial fibrillation, those who required inotrope use during or after surgery, and those having v
258 , including mean arterial blood pressure and inotrope use during the 48 h after hypoxia-ischaemia.
259 Hospitals with higher risk-standardized inotrope use had modestly longer risk-standardized lengt
262 icated that 21% of the observed variation in inotrope use was potentially attributable to random hosp
264 ed risk-standardized hospital-level rates of inotrope use within 209 hospitals participating in Get W
267 lmonary bypass, anesthesia, ventilation, and inotrope use; and complication and reintervention rates.
269 CS was defined as the coding of: 1) CS; 2) inotrope use; or 3) mechanical circulatory support befor
273 ies (n = 149, 51.0%) including chemotherapy, inotropes, vasoactive agents, and sedatives were the mos
276 ho have metabolic acidosis, a bicarbonate or inotrope/vasopressor requirement, cardiopulmonary resusc
277 emography, clinical classification, outcome, inotrope/vasopressor requirement, clinical assessment of
281 ients with cardiogenic shock unresponsive to inotropes/vasopressors and intraaortic balloon pumps (IA
283 or illness severity, mechanical ventilation, inotropes/vasopressors, renal replacement therapy, and s
292 operative ejection fraction and the need for inotropes when coming off bypass did not exhibit statist
293 f 200 advanced heart failure patients not on inotropes who met indications for LVAD implantation, com
295 Thus, NO(-) is a redox-sensitive positive inotrope with selective venodilator action, whose cardia
296 insufficiency, and 40% were on at least two inotropes with a mean cardiac index of 1.8 L/min/m2.
298 e pressure >/=24 mm Hg and dependent on >/=2 inotropes with or without intra-aortic balloon pump) wer
300 iogram (80%) and/or the need for intravenous inotropes within 7 days of hospital admission (69%).