ライフサイエンスコーパス: thrombolytic agent

1 therapy and it is also used clinically as a thrombolytic agent.

2 sue plasminogen activator, is an alternative thrombolytic agent.

3 ffinity obviates continuous infusion of this thrombolytic agent.

4 cing infarct size in patients treated with a thrombolytic agent.

5 py for acute ischemic stroke is the use of a thrombolytic agent.

6 in ischemia, independent of its effect as a thrombolytic agent.

7 PA) is a highly fibrin-specific single-bolus thrombolytic agent.

8 omy without co-treatment with an intravenous thrombolytic agent.

9 swered questions remain regarding the use of thrombolytic agents.

10 inogen activator are the currently available thrombolytic agents.

11 nimizes the duration of systemic exposure to thrombolytic agents.

12 tra-arterial thrombolysis, and trials of new thrombolytic agents.

13 d antiplatelet therapies in combination with thrombolytic agents.

14 congestive heart failure, who first received thrombolytic agents.

15 tients with myocardial infarction (MI) given thrombolytic agents.

16 be observed in 10 minutes without exogenous thrombolytic agents.

17 hic potential complication of treatment with thrombolytic agents.

18 te the utility of this assay as a screen for thrombolytic agents, a 14-amino-acid PAI-1-inhibitory pe

19 myocardial infarction treated initially with thrombolytic agents-a clinical application previously un

20 medications, including medications (such as thrombolytic agents and beta-blockers) that are associat

21 The use of thrombolytic agents and captopril had no significant eff

22 intra-arterial), intra-arterial injection of thrombolytic agents and hyaluronidase, anterior chamber

23 The use of thrombolytic agents and invasive treatment plans decline

24 , including intra-arterial administration of thrombolytic agents and mechanical interventions, show p

25 outcomes of patients with OTPHV treated with thrombolytic agents and with surgery since 1996.

26 F or both), time of VT/VF occurrence, use of thrombolytic agents, and eventual outcome are unclear.

27 New devices, new thrombolytic agents, and new antithrombotic agents are c

28 rlier treatment, the use of third-generation thrombolytic agents, and the use of primary angioplasty.

29 enting; more potent and more fibrin-specific thrombolytic agents; and new antithrombotic and antiplat

30 clinical trials have investigated the use of thrombolytic agents, anticoagulants, antiplatelet drugs

31 Tissue plasminogen activator is the only thrombolytic agent approved in the United States for tre

32 Thrombolytic agents, aspirin, beta-blockers, and angiote

33 learest indication for the administration of thrombolytic agents, but patients with acute pulmonary e

34 h Gd-complexes (Gd-lip) co-encapsulated with thrombolytic agents can serve both for imaging and treat

35 In the absence of any thrombolytic agent, clots fully retracted within 2.5 h a

36 There was no benefit when intravenous thrombolytic agent co-treatment was used.

37 % of patients aged 75 to 84 years received a thrombolytic agent compared with 21.4% between 1 June 19

38 atients younger than age 55 years received a thrombolytic agent during hospitalization for acute myoc

39 ctive treatment option in conjunction with a thrombolytic agent for stroke patients.

40 teplase is being evaluated as an alternative thrombolytic agent for the treatment of acute ischemic s

41 Alteplase is currently the only approved thrombolytic agent for treatment of acute ischaemic stro

42 asminogen activator (rh-tPA) is an important thrombolytic agent for treatment of acute ischemic strok

43 and IPF2alpha-I levels in patients receiving thrombolytic agents for acute MI.

44 y be justified in severe cases, the role for thrombolytic agents for less symptomatic deep venous thr

45 rest is burgeoning in the development of new thrombolytic agents for systemic reperfusion with an imp

46 TAFIa could enhance the efficacy of existing thrombolytic agents for the treatment of acute myocardia

47 ome after myocardial infarction treated with thrombolytic agents from a large international cohort.

48 nting, glycoprotein IIb/IIIa inhibitors plus thrombolytic agents, glycoprotein IIb/IIIa inhibitors pl

49 al, an appropriate dose of this single-bolus thrombolytic agent has been identified for phase III tes

50 te ST segment elevation MI, new single-bolus thrombolytic agents have been unable to break the "throm

51 Although current thrombolytic agents have proven their clinical benefit,

52 uture directions for a safer use of tPA as a thrombolytic agent in the setting of acute ischemic stro

53 Patients meeting ECG criteria were given thrombolytic agents in 49% of cases, but age, comorbidit

54 must be excluded prior to administration of thrombolytic agents in acute stroke.

55 All thrombolytic agents in current clinical usage are plasmi

56 as well as local intra-arterial delivery of thrombolytic agents in patients with acute stroke, are t

57 helped avoid the risks from angiography and thrombolytic agents in some or spurred the judicious use

58 ubbles not only enhance the effectiveness of thrombolytic agents in the presence of ultrasound but ma

59 py may be a non-invasive safe alternative to thrombolytic agents in treating thrombotic CVC occlusion

60 nergistic effect on thrombus disruption with thrombolytic agents in vitro.

61 Thrombolytic agents (including tissue plasminogen activa

62 Thrombolytic agents, including tenecteplase, are general

63 placement and to allow administration of the thrombolytic agent into the core of the haematoma via a

64 Further study of this new thrombolytic agent is ongoing.

65 Streptokinase (SK), a widely used thrombolytic agent, is an efficient activator of human P

66 TNK-tPA, a fibrin specific second generation thrombolytic agent, is effective in reducing ischemic vo

67 Newer thrombolytic agents may have advantages, but are less we

68 Our findings indicate that thrombolytic agents may have therapeutic value in the tr

69 The effect of a thrombolytic agent on biochemical bond degradation was m

70 theterization was performed more often after thrombolytic agents (OR 1.85, 95% CI 0.97 to 3.54), but

71 s older age and therapy with anticoagulants, thrombolytic agents, or captopril affect long-term rates

72 minogen activator (TPA) with a direct-acting thrombolytic agent, plasmin, in an animal model of fibri

73 The use of thrombolytic agents (plasminogen activators) in the earl

74 VWF) that blocks VWF binding to GPIb, of the thrombolytic agent recombinant tissue plasminogen activa

75 In addition, both thrombolytic agents reduced cerebral lesion volume (dete

76 In contrast, Microlyse, a novel thrombolytic agent, requires von Willebrand factor (VWF)

77 Finally, we show that the thrombolytic agent streptokinase has therapeutic value f

78 f important virulence factors, including the thrombolytic agent streptokinase, the protease inhibitor

79 ich regulates the expression of pili and the thrombolytic agent streptokinase.

80 urokinase-type plasminogen activator or the thrombolytic agent streptokinase.

81 as in clots that have been treated with the thrombolytic agents streptokinase and alteplase.

82 lacing of the thrombus with a fibrin-binding thrombolytic agent such as alteplase is an alternative t

83 parin, oral anticoagulants, antibiotics, and thrombolytic agents such as urokinase and tissue plasmin

84 rial and requires a more effective and safer thrombolytic agent than those currently available.

85 plase has emerged as a potential alternative thrombolytic agent that might be preferred over alteplas

86 yocardial infarction less commonly receive a thrombolytic agent, use of thrombolytic therapy in this

87 oup analyses to assess the effect of type of thrombolytic agent used and the strategy of emergent hos

88 up, and were independent of both the type of thrombolytic agent used, and whether or not the patient

89 association between age and treatment with a thrombolytic agent was determined by crude and multivari

90 We demonstrated that long-term exposure to a thrombolytic agent was essential to achieve high thrombo

91 Use of a thrombolytic agent was inversely related to patient age:

92 However, the interaction with thrombolytic agents was not specifically assessed.

93 ocardial infarction, the odds of receiving a thrombolytic agent were significantly reduced for patien

94 ngiotensin-converting enzyme inhibitors, and thrombolytic agents were used in 72%, 39%, 32%, and 15%

95 olysis, but the relative benefits of various thrombolytic agents with earlier administration are unce

96 Over the past two decades, new thrombolytic agents with sufficient pharmacologic potenc