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TamimNaber, MD 			       	9/15/2010 Journal Club
Bruce A. Cooper, M.B., B.S., Ph.D. et al, NEJM; vol. 363 no. 7; august 12, 2010 A Randomized, Controlled Trial of Early versus Late Initiation of Dialysis
Initiation of dialysis  ,[object Object]
Negative psychological impact on patients
Important socioeconomic implications
When to start - subject to much controversy ,[object Object]
to control volume overload, acid-base and electrolyte disorders
and to provide a clearance of uremic toxins enough to allow an adequate dietary protein and caloric intake
When residual renal function fails to maintain all these vital functions, we have a solid argument for starting dialysis therapy ,[object Object]
Hyperkalemia
Metabolic acidosis
Hyperphosphatemia
Hypercalcemia or hypocalcemia
Anemia
Neurological dysfunction (eg, neuropathy, encephalopathy)
Pleuritis or pericarditis
Otherwise unexplained decline in functioning or well-being
Gastrointestinal dysfunction (eg, nausea, vomiting, diarrhea, gastroduodenitis)
Weight loss or other evidence of malnutrition
Hypertension ,[object Object]
KDOQI.. Timing of Therapy When to Initiate Dialysis : K t/V urea Criterion (Opinion) patients should be advised to initiate some form of dialysis when the weekly renal Kt/V urea < 2.0. Unless:  1. Stable or increased edema-free body weight.  2. No Nutritional indications  3. Complete absence of clinical signs or symptoms attributable to uremia.  A weekly Kt/V urea of 2.0 approximates a kidney urea clearance of 7 mL/min and a kidney creatinine clearance that varies between 9 to 14 mL/min/1.73 m 2
KDOQI.. Timing of Therapy ,[object Object],[object Object]
Nephrol Dial Transplant (2005) Dialysis should be instituted whenever evidence of uremia is present, or blood pressure and hydration status cannot be controlled, or when a deterioration of the nutritional status is noticed. In any case, dialysis should be started before the GFR is <6 ml/min/1.73 m2 (creatinine clearance 8 ml/min/1.73 m2). (Evidence level C)  To ensure that dialysis is not started at a GFR of <6 ml/min/1.73 m2, initiation at the level between 8 and 10 ml/min should be considered. Diabetic patients may require an earlier start. (Evidence level C)
The CARI Guidelines – Caring for Australians with Renal Impairment, February 2005 No recommendations possible based on Level I or II evidence  Commence dialysis at first indication of malnutrition suspected to be due to uremia and unresponsive to dietary intervention or correction of other reversible causes. (Level III evidence) Look for evidence of malnutrition once a GFR of 15–20 mL/min/1.73 m2 is found, and monthly from GFR < 10 mL/min/1.73 m2. Use of absolute indications for dialysis initiation is a historical concept which is no longer valid, and their presence suggests delayed initiation. However, in some patients with co-morbid conditions, dialysis may be indicated for these reasons even when GFR is greater than 10 mL/min/1.73m2
Postulate and practice  Several series of patients taken onto RRT - (weekly Kt/V) at the start of dialysis - markedly lower than that of DOQI guidelines  Ranging between 0.68, 0.72 and 1.05 in patients reviewed in USA, Canada and UK  If DOQI guidelines are to be followed - dialysis needs to be started between 20 and 11 months earlier  Heavy additional burden  Must be justified by more convincing evidence to demonstrate unequivocal benefit from early initiation of dialysis  Prospective, controlled, randomized trials
Early initiation – Believers.. Bonomini et al, 1985 ,[object Object]
Among a subset of patients who were subsequently transplanted, there was a survival advantage for those started dialysis early (n=50) vs later (n=96), as well as less vascular calcification, bacterial infection, dyslipidemia and hospitalization! ,[object Object]
Cont’d CANUSA study.. In the CANUSA study, there was a survival advantage for higher total (residual plus dialysis) Kt/V up to 2.0, and possibly up to 2.3  This study was not designed to examine time of initiation of dialysis
Early initiation – Believers.. Tattersall et al. ( Am J Nephrol 15: 283 -2 89, 1995)  ,[object Object]
demonstrated reduced survival in patients with less residual renal function at start of dialysis, although these patients were also significantly older and had significantly more co-morbidity
Hospitalization length of stay was greater among those with residual Kt/V <1.05 at time of initiation of dialysis,[object Object]
Early initiation  ,[object Object]
early initiation of dialysis expose patients : complications of dialysis, unnecessary lifestyle restriction, potential increased cost, patient fatigue
No RCTs - Confounding influences in other studies include referral time bias, age, co-morbidity, patient compliance and starting time bias
Lead time bias,[object Object]
timely initiation - associated with a small survival benefit of 2.5 months
However, the extra time free of dialysis for “late starters ” was only 4.1 months
This study suggested that any perceived survival benefit from early start could be accounted for by lead-time,[object Object]
Early initiation does not prolong survival? ,[object Object]

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Journal club: Is Early Dialysis Better?

  • 1. TamimNaber, MD 9/15/2010 Journal Club
  • 2. Bruce A. Cooper, M.B., B.S., Ph.D. et al, NEJM; vol. 363 no. 7; august 12, 2010 A Randomized, Controlled Trial of Early versus Late Initiation of Dialysis
  • 3.
  • 6.
  • 7. to control volume overload, acid-base and electrolyte disorders
  • 8. and to provide a clearance of uremic toxins enough to allow an adequate dietary protein and caloric intake
  • 9.
  • 15. Neurological dysfunction (eg, neuropathy, encephalopathy)
  • 17. Otherwise unexplained decline in functioning or well-being
  • 18. Gastrointestinal dysfunction (eg, nausea, vomiting, diarrhea, gastroduodenitis)
  • 19. Weight loss or other evidence of malnutrition
  • 20.
  • 21. KDOQI.. Timing of Therapy When to Initiate Dialysis : K t/V urea Criterion (Opinion) patients should be advised to initiate some form of dialysis when the weekly renal Kt/V urea < 2.0. Unless: 1. Stable or increased edema-free body weight. 2. No Nutritional indications 3. Complete absence of clinical signs or symptoms attributable to uremia. A weekly Kt/V urea of 2.0 approximates a kidney urea clearance of 7 mL/min and a kidney creatinine clearance that varies between 9 to 14 mL/min/1.73 m 2
  • 22.
  • 23. Nephrol Dial Transplant (2005) Dialysis should be instituted whenever evidence of uremia is present, or blood pressure and hydration status cannot be controlled, or when a deterioration of the nutritional status is noticed. In any case, dialysis should be started before the GFR is <6 ml/min/1.73 m2 (creatinine clearance 8 ml/min/1.73 m2). (Evidence level C) To ensure that dialysis is not started at a GFR of <6 ml/min/1.73 m2, initiation at the level between 8 and 10 ml/min should be considered. Diabetic patients may require an earlier start. (Evidence level C)
  • 24. The CARI Guidelines – Caring for Australians with Renal Impairment, February 2005 No recommendations possible based on Level I or II evidence Commence dialysis at first indication of malnutrition suspected to be due to uremia and unresponsive to dietary intervention or correction of other reversible causes. (Level III evidence) Look for evidence of malnutrition once a GFR of 15–20 mL/min/1.73 m2 is found, and monthly from GFR < 10 mL/min/1.73 m2. Use of absolute indications for dialysis initiation is a historical concept which is no longer valid, and their presence suggests delayed initiation. However, in some patients with co-morbid conditions, dialysis may be indicated for these reasons even when GFR is greater than 10 mL/min/1.73m2
  • 25. Postulate and practice Several series of patients taken onto RRT - (weekly Kt/V) at the start of dialysis - markedly lower than that of DOQI guidelines Ranging between 0.68, 0.72 and 1.05 in patients reviewed in USA, Canada and UK If DOQI guidelines are to be followed - dialysis needs to be started between 20 and 11 months earlier Heavy additional burden Must be justified by more convincing evidence to demonstrate unequivocal benefit from early initiation of dialysis Prospective, controlled, randomized trials
  • 26.
  • 27.
  • 28. Cont’d CANUSA study.. In the CANUSA study, there was a survival advantage for higher total (residual plus dialysis) Kt/V up to 2.0, and possibly up to 2.3 This study was not designed to examine time of initiation of dialysis
  • 29.
  • 30. demonstrated reduced survival in patients with less residual renal function at start of dialysis, although these patients were also significantly older and had significantly more co-morbidity
  • 31.
  • 32.
  • 33. early initiation of dialysis expose patients : complications of dialysis, unnecessary lifestyle restriction, potential increased cost, patient fatigue
  • 34. No RCTs - Confounding influences in other studies include referral time bias, age, co-morbidity, patient compliance and starting time bias
  • 35.
  • 36. timely initiation - associated with a small survival benefit of 2.5 months
  • 37. However, the extra time free of dialysis for “late starters ” was only 4.1 months
  • 38.
  • 39.
  • 40. Post-hoc analysis of the MDRD study, comparing early (predicted MDRD GFR>7.5 ml/min; N = 1,444) with late (predicted GFR <7.5 ml/min); N = 1,476), higher MDRD GFR at initiation was associated with an increased risk of death in multivariate Cox model (hazard ratio 1.27 for each 5 ml/min increase)
  • 41. “ reflect an erroneous GFR estimation by MDRD formula”
  • 42.
  • 43. Patients in the general dialysis population who initiated dialysis therapy at a GFR >10 mL/min/1.73 m2 had a 42% increased risk for death compared with patients with a GFR < 5 mL/min/1.73 m2 at initiation of dialysis therapy after adjusting for all covariates
  • 44.
  • 45. A Randomized, Controlled Trial of Early versus Late Initiation of DialysisNEJM; vol. 363 no. 7; august 12, 2010 Bruce A. Cooper, M.B., B.S., Ph.D., Pauline Branley, B.Med., Ph.D., LilianaBulfone, B.Pharm., M.B.A., John F. Collins, M.B., Ch.B., Jonathan C. Craig, M.B., Ch.B., Ph.D., Margaret B. Fraenkel, B.M., B.S., Ph.D., Anthony Harris, M.A., M.Sc., David W. Johnson, M.B., B.S., Ph.D., Joan Kesselhut, Jing Jing Li, B.Pharm., B.Com., Grant Luxton, M.B., B.S., Andrew Pilmore, B.Sc., David J. Tiller, M.B., B.S., David C. Harris, M.B., B.S., M.D., and Carol A. Pollock, M.B., B.S., Ph.D., for the IDEAL Study*
  • 46.
  • 47. Funded by the National Health and Medical Research Council of Australia and others
  • 48. Conducted in accordance of Helsinski, the Good Clinical Practice guidelines of the International Conference on Harmonization, and local regulatory requirements.
  • 49. Approved by the ethic committee at each participating center.
  • 51. Patients recruited at 32 center in Australia and New Zealand “urban and rural locations, general and university hospitals”/all provided written informed consent
  • 52. Blinded statistical personnel, and an independent end-point committee unaware of the treatment assignments.
  • 53. Owing to the nature of the intervention, it wasn’t possible to conceal the treatment assignments from the patients, nurses, or investigators
  • 54.
  • 55. 1ry outcome: Death from any cause
  • 56.
  • 58. Plan to receive live donor kidney transplant within the next 12 months
  • 59. Recently diagnosed Cancer likely to affect survival
  • 60. Unable to provide written informed ConsentMethods
  • 61. GFR Estimate? Cockroft-Gault equation For comparison, they also calculated the estimated GFR at baseline and at the start of dialysis with the use of the Modification of Diet in Renal Disease (MDRD) equation
  • 62.
  • 63. Planned method of dialysis “PD vs HD” specified before randomization by the choice of the patient and treating physician
  • 64. Continue to receive Medical care and commence dialysis when GFR 5-7
  • 65.
  • 66. 244 in New Zealand, 584 in Australia
  • 67. 404 – Early start / 424 – Late start
  • 68. Median duration of follow up was 3.64 years, (range, 0.03 to 9.15) in the early-start group and 3.57 years (range, 0.02 to 8.78) in the late-start group.
  • 69.
  • 71. GFR that had not fallen to the assigned range for initiation of dialysis (6 patients in the early-start group and 8 in the late-start group)
  • 72. Death (10 patients in the early-start group and 22 in the late-start group).
  • 73.
  • 74.
  • 75. GFR was 12.0 ml per minute in the early-start group, as compared with 9.8 ml per minute in the late-start group
  • 76. In the early-start group, 75 (18.6%) started dialysis with an estimated GFR of less than 10.0 ml per minute
  • 77. In the late-start group, 322 (75.9%) started dialysis with an estimated GFR of more than 7.0 ml per minute.
  • 78.
  • 79. The causes of the deaths are summarized in (Table 2)
  • 80. There was no significant difference in survival between patients in the late-start group and patients in the early-start group (hazard ratio for death in the early-start group, 1.04; 95% CI, 0.83 to 1.30; P = 0.75) (Fig. 2B)
  • 81.
  • 82.
  • 83. with careful clinical management of CKD, dialysis can be delayed for some patients until the GFR drops below 7.0 ml/m, or until more traditional clinical indicators for the initiation of dialysis are present
  • 84. all the previous studies were nonrandomized and were subject to potential confounding factors that do not apply to the IDEAL trial!
  • 85. Dialysis should not be started on the basis of an estimate of GFR alone
  • 86. the most important parameters to be considered being; uremic, adequate control of blood pressure, and quality of nutritional status
  • 87.
  • 88. What about us?When would you initiate dialysis on ESRD patient? N = 19 Favors early start RRT= 5 (26%) Attendings N= 12 (17% favors early start) Fellows N= 7 (43% favors early start)