ライフサイエンスコーパス: conduction defect

1 nce interval, 2.14-5.81 for intraventricular conduction defect).

2 a-TcD) are believed to represent interatrial conduction defect.

3 VES and CAP2 murine knockouts caused cardiac conduction defects.

4 ults in adult late-onset cardiomyopathy with conduction defects.

5 ith unknown ingestions or those with cardiac conduction defects.

6 cardiac hypertrophy and cardiomyopathy with conduction defects.

7 alvular defects were present in 42%; 75% had conduction defects.

8 tients with congenital atrioventricular (AV) conduction defects.

9 weeks after birth, most likely from cardiac conduction defects.

10 m the immunized group had varying degrees of conduction defects.

11 ystrophy and myotonia, cataracts and cardiac conduction defects.

12 an equal number of GUSTO-I patients without conduction defects.

13 (13% versus 7%, P:=0.013), and postoperative conduction defects (21.6% versus 12.4%, P:=0.001).

14 associated with 63% prevention of the nerve conduction defect and complete prevention of structural

15 -L-carnitine resulted in 76% recovery of the conduction defect and corrected neuropathologic changes

16 ltage and are influenced by intraventricular conduction defects and acute myocardial infarction.

17 neonatal lupus, comprising atrioventricular conduction defects and cardiomyopathy, occur in fetuses

18 that PKC inhibition ameliorated the cardiac conduction defects and contraction abnormalities found i

19 ve neuropathy in Lewis rats characterized by conduction defects and demyelination in spinal nerves.

20 resulted in progressive and profound cardiac conduction defects and heart failure.

21 een found in patients with DCM with familial conduction defects and muscular dystrophy, but the clini

22 relevant role in myotonic dystrophy cardiac conduction defects and pathology.

23 ults in adult late-onset cardiomyopathy with conduction defects and up-regulation of mXinbeta.

24 LBBB, intraventricular conduction defect, and RBBB combined with left anterior

25 tricular preexcitation, atrial fibrillation, conduction defects, and cardiac hypertrophy.

26 hmias, atrial fibrillation, atrioventricular conduction defects, and death by 4 months of age.

27 nsorimotor and autonomic neuropathy, cardiac conduction defects, and infiltrative cardiomyopathy.

28 ment depression, T-wave changes, ventricular conduction defects, and left ventricular hypertrophy bas

29 ever, since few patients had baseline severe conduction defects before paclitaxel treatment, the safe

30 Hop-/- adult mice display conduction defects below the atrioventricular node (AVN)

31 e deficient in Etv1 exhibited marked cardiac conduction defects coupled with developmental abnormalit

32 level leads to cardiac dysfunction, such as conduction defect, DCM, and heart failure, remains uncle

33 kyphoscoliosis, muscle pathology and cardiac conduction defects develop.

34 Cx46 mutant revealed the presence of cardiac conduction defects frequently associated with human hear

35 Heterogeneous Cx43 expression resulted in conduction defects, however, as well as markedly depress

36 c pathway for progressive cardiomyopathy and conduction defects in congenital heart disease.

37 ription factor Nkx2-5 cause atrioventricular conduction defects in humans by unknown mechanisms.

38 ntractility and ameliorated intraventricular conduction defects in LmnaH222P/H222P mice, which was as

39 ted in diverse congenital heart diseases and conduction defects in mouse models and humans.

40 Postnatal conduction defects in Nkx2-5 mutation may result at leas

41 represent the first direct demonstration of conduction defects in the specialized conduction system

42 c heart, which may contribute in part to the conduction defects in the transgenic mice.

43 ransgenic heart, which may contribute to the conduction defects in the transgenic mice.

44 ilar mouse model, which reported only subtle conduction defects in their nervous system.

45 Conduction defects in these tissues produce a disproport

46 Transgene expression resulted in cardiac conduction defects, increased expression of the cardiac-

47 is associated with total and sudden deaths, conduction defects, left ventricular dysfunction, and su

48 ions that cause isolated progressive cardiac conduction defect (Lenegre syndrome), long-QT syndrome (

49 alterations of muscle excitability, cardiac conduction defects, mental retardation, and cognitive de

50 associated with the presence at baseline of conduction defects on the ECG and left ventricular systo

51 tem, but its absence does not cause baseline conduction defects or arrhythmias in the adult mouse.

52 1), supraventricular arrhythmia (p = 0.003), conduction defects (p = 0.01), and "mildly" DCM (p = 0.0

53 -type BBBs (LBBB, RBBB, and intraventricular conduction defect, respectively).

54 +/- mice develop first-degree heart block, a conduction defect strikingly similar to that observed in

55 The range and frequency of conduction defects suggest that additional factors promo

56 d by a chronotropic incompetence and cardiac conduction defects, thus increasing the susceptibility t

57 kx2-5 lead to progressive cardiomyopathy and conduction defects via unknown mechanisms.

58 In the prevention study, the conduction defect was 73% prevented and structural abnor

59 Conduction defect was accompanied by reduction in ventri

60 story of sudden death or progressive cardiac conduction defect was found in 1.4% and 11.1%, respectiv

61 omen with no BBB, LBBB, and intraventricular conduction defect were strong predictors of incident HF

62 These conduction defects were accompanied by overt mislocaliza

63 Conduction defects were correlated with dephosphorylatio

64 DMPK-/- mice develop cardiac conduction defects which include first-, second-, and th

65 rface and ambulatory ECGs documented cardiac conduction defects, which were further confirmed by elec

66 rstitial and focal replacement fibrosis, and conduction defects with altered connexin 43 distribution

67 excitable cells and tissues can repair large conduction defects within primary 2- and 3-dimensional c