ライフサイエンスコーパス: haemodialysis

1 ior alternative to the present standard (ie, haemodialysis).

2 toneal scarring, and premature transition to haemodialysis.

3 to quantitatively evaluate the initiation of haemodialysis.

4 ccess grafts are the best option for chronic haemodialysis.

5 als of patients infected with HCV who are on haemodialysis.

6 atients with organ transplants or who needed haemodialysis.

7 no acid metabolism and insulin resistance in haemodialysis.

8 ticoagulation, as they would be for standard haemodialysis.

9 dies were performed before, during and after haemodialysis.

10 te and renal function tests before and after haemodialysis.

11 rvival of patients is now equal to that with haemodialysis.

12 favoured vascular access choice for extended haemodialysis.

13 of vascular access that allows provision of haemodialysis.

14 ss to insomnia interventions for patients on haemodialysis.

15 mortality in patients receiving maintenance haemodialysis.

16 re when compared with conventional high-flux haemodialysis.

17 on population (pmp) to 4.8 pmp (P<0.001) for haemodialysis, 1.4 pmp to 1.6 pmp for peritoneal dialysi

18 costs of KRT were: US$19 380 per person for haemodialysis, $18 959 for peritoneal dialysis, and $26

19 ncreased from 27% in 2019 to 28% in 2023 for haemodialysis, 23% to 28% for peritoneal dialysis, and 3

20 The study included 293 patients, 65% haemodialysis, 35% peritoneal dialysis.

21 ing five patients had grafts functioning for haemodialysis 6-20 months after implantation, and a tota

22 vessels seem to provide safe and functional haemodialysis access, and warrant further study in rando

23 was implanted into the arms of patients for haemodialysis access.

24 ver, options for chronic vascular access for haemodialysis - an essential part of kidney replacement

25 We analysed 12-lead ECGs from 45 haemodialysis and 12 LQT2 patients.

26 1 randomised 93 patients who were undergoing haemodialysis and being treated with non-iron-based phos

27 cluding peritoneal dialysis, continuous KRT, haemodialysis and hybrid therapy) to manage hyperammonae

28 mnia is common among patients on maintenance haemodialysis and may be exacerbated by the challenges o

29 in the provision of dialysis - particularly haemodialysis and most notably in high-income countries

30 Overall, access to haemodialysis and peritoneal dialysis improved, however,

31 have been reported in individuals undergoing haemodialysis and those with chronic kidney disease.

32 and mortality risk of patients on in-centre haemodialysis and transplant recipients.

33 ts with renal failure undergoing maintenance haemodialysis are associated with insulin resistance and

34 New means of delivering haemodialysis are therefore required.

35 ies allocated public funding to provide free haemodialysis at the point of delivery; use of this fund

36 pment cohort, whereas 504 patients who began haemodialysis between 2012 and 2013 were enrolled in the

37 rred type of vascular access for maintenance haemodialysis but it may contribute to maladaptive cardi

38 ey failure who are treated with intermittent haemodialysis, but the effects of this strategy on organ

39 More frequent haemodialysis can improve both survival and quality of l

40 ed a retrospective cohort study including 25 haemodialysis centres in Mainland China.

41 the abnormalities, which were all reduced by haemodialysis, closely resembled those in normal axons d

42 pFAK(Tyr397) were significantly decreased in haemodialysis compared to controls, whereas Rac1 and Akt

43 ic kidney disease (stage 4-5 with or without haemodialysis dependence) were randomly assigned to rece

44 Overall, 179 (76%) were haemodialysis-dependent, 122 (52%) had HCV genotype 1a i

45 , comparing online haemodiafiltration versus haemodialysis designed to measure mortality outcomes.

46 ar haemodialysis were fitted with a wearable haemodialysis device for 4-8 h.

47 This wearable haemodialysis device shows promising safety and efficacy

48 sess the safety and efficiency of a wearable haemodialysis device.

49 ma and myeloma cast nephropathy who required haemodialysis for acute kidney injury and who received a

50 percentage of patients because of dropout to haemodialysis for inherent complications of peritoneal d

51 re widely considered preferable to in-centre haemodialysis for many patients with ESKD in settings wh

52 Patients with ESRD (n = 1281) who commenced haemodialysis from 2008 to 2011 were enrolled in the dev

53 Phenylalanine kinetics were reduced in the haemodialysis group at 30 and 60 min post meal ingestion

54 ed with in 559 patients (27.0%) treated with haemodialysis (hazard ratio 0.84 [95% CI 0.74-0.95]).

55 High cutoff haemodialysis (HCO-HD) can remove large quantities of fr

56 LV mass, can be observed following long-term haemodialysis (HD) and has been attributed to regression

57 valent among adults treated with maintenance haemodialysis (HD) and has profound negative effects.

58 femoral arteries caused by fluid loss during haemodialysis (HD) and to determine the direction and am

59 Patients commencing on haemodialysis (HD) have an increased risk of cardiovascu

60 End-stage renal disease patients on haemodialysis (HD) have been largely excluded from SARS-

61 ients, because their removal by conventional haemodialysis (HD) is severely limited by their low free

62 e associated with morbidity and mortality in haemodialysis (HD) patients.

63 ey disease (CKD) patients, especially in the haemodialysis (HD) population.

64 MVs were isolated from the blood of 20 haemodialysis (HD), 17 peritoneal dialysis (PD) patients

65 elative to treatment with standard high-flux haemodialysis (HF-HD).

66 erview of incidence, modality use (in-centre haemodialysis, home dialysis, or transplantation), and m

67 Children did not have access to haemodialysis in 12 (19%) of 62 countries, peritoneal di

68 was then constructed using factors affecting haemodialysis initiation as input variables and 3-year s

69 ntribute to hyperphosphatemia in maintenance haemodialysis (MHD) patients.

70 teristics of patients undergoing maintenance haemodialysis (MHD).

71 e effects of haemodiafiltration and standard haemodialysis on all-cause and cause-specific mortality.

72 Compared with haemodialysis, online haemodiafiltration reduces all-cau

73 Patients on haemodialysis or peritoneal dialysis are likely to be at

74 The study included incident haemodialysis or peritoneal dialysis patients.

75 imates were stratified by dialysis modality (haemodialysis or peritoneal dialysis) and for the subpop

76 fferences were found in mortality by sex for haemodialysis or peritoneal dialysis.

77 SKD worldwide who are treated with in-centre haemodialysis, overall survival is poor, but longer in s

78 The Proactive IV Iron Therapy in Haemodialysis Patients (PIVOTAL) trial randomized 2141 p

79 ment, and can maintain anaemia management in haemodialysis patients when given intravenously at 4-wee

80 perform longitudinal blood sampling of ESKD haemodialysis patients with COVID-19, collecting samples

81 e the effects of FC on anaemia management in haemodialysis patients with hyperphosphataemia.

82 integrin-cytoskeleton linkage are reduced in haemodialysis patients, suggesting for the first time th

83 flux without affecting insulin resistance in haemodialysis patients.

84 y response and can be safely administered in haemodialysis patients.

85 ameters related to anaemia and CKD-MBD among haemodialysis patients.

86 hropoietin resistance in the long term among haemodialysis patients.

87 ee times per week for haemoglobin control in haemodialysis patients.

88 flux without affecting insulin resistance in haemodialysis patients.

89 Compared with haemodialysis, PD has numerous potential advantages, inc

90 Commendable haemodialysis practice includes exceptionally high use o

91 nal cohort study to highlight differences in haemodialysis practices that affect survival and the exp

92 Haemodialysis presents an additional high-risk exposure

93 Haemodialysis provides various options for vascular acce

94 brils extracted from patients suffering from haemodialysis-related amyloidosis and those formed by se

95 Creation of AVF for haemodialysis resulted in a significant increase of LV m

96 In persons on haemodialysis, SAF is an independent risk factor for car

97 ps for patient-led cognitive training during haemodialysis sessions.

98 y failure who were treated with intermittent haemodialysis suggest that fast UF(NET) rates are also a

99 This paper charts the development of haemodialysis, the cornerstone of renal replacement ther

100 Nine patients were studied during routine haemodialysis therapy.

101 d-stage renal disease who had been receiving haemodialysis through an access graft that had a high pr

102 hysiological values from patients undergoing haemodialysis treatment in the Renal Unit of the Churchi

103 e UK to allow patients to have more frequent haemodialysis treatments in hospital and satellite haemo

104 ght in February, 1996, all 126 patients in a haemodialysis unit in Caruaru, north-east Brazil, develo

105 ialysis treatments in hospital and satellite haemodialysis units.

106 Chronic haemodialysis was available in 162 (98%) of 165 countrie

107 y phase (0-3 months) and effectiveness after haemodialysis was started.

108 ients and toxicological studies of serum and haemodialysis water filters.

109 13.8] years) who were established on regular haemodialysis were fitted with a wearable haemodialysis

110 made from polysulfone hollow fibre for human haemodialysis, which has an inner diameter of 200 mum an

111 d improve the well-being of people receiving haemodialysis without necessitating significant clinical