NKF
KDOQI GUIDELINES
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NKF
KDOQI GUIDELINES
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III. CLINICAL PRACTICE RECOMMENDATIONS FOR ANEMIA IN CHRONIC KIDNEY DISEASE IN CHILDREN
CPR FOR PEDIATRICS 2.1: HB RANGE
Treatment thresholds in anemia management describe the intended goal of current treatment for the individual patient. The Hb treatment range represents the intended goal of ESA and iron therapy.
2.1.1 Lower limit of Hb: (FULLY APPLICABLE TO CHILDREN)
In patients with CKD, Hb level should be 11.0 g/dL or greater. (MODERATELY STRONG RECOMMENDATION)
2.1.2 Upper limit of Hb: (FULLY APPLICABLE TO CHILDREN)
In the opinion of the Work Group, there is insufficient evidence to recommend routinely maintaining Hb levels at 13.0 g/dL or greater in ESA-treated patients.
RATIONALE
Determination of Hb targets in
pediatric patients resists definitive recommendation. QOL, so
significant to the development of the child and life of the family,
lends urgency to the consideration of higher Hb level thresholds.
However, evidence lacks both quality and quantity, rendering assessment
of both benefit and risk uncertain. Age-specific variation in normal Hb
levels introduces further uncertainty. Finally, given key metabolic,
growth, developmental, and psychological differences between children
and adults, exclusive reliance on evidence in adults is inappropriate.
The Work Group presents lower and upper targets for Hb levels in
children using values in adults for reference. However, we add 2
significant qualifications. The first is that both the lower and upper
Hb targets serve only as opinion-based CPRs, in keeping with the lack
of pediatric-specific evidence. The second is that medical decision
making to set Hb targets in individual patients should be informed by
available evidence that is uniquely pediatric. Consideration should be
given, for example, to the potential need to make adjustments for the
normal age-specific Hb distribution (Table 39 and Table 40).
In weighing the potential QOL benefits of Hb targets, the available
evidence in adults should be enriched by consideration of QOL issues
that are crucial to children, including neurocognitive development,
school attendance, exercise capacity, and family support. To assist
medical decision making, the Work Group provides the following review
of the literature.
Mortality
Observational evidence
relating Hb level to mortality is available. Children in the North
American Pediatric Renal Transplant Cooperative Study (NAPRTCS)
database from 1992 to 2001 with an Hb level less than 9.9 g/dL compared
with those with an Hb level greater than 9.9 g/dL showed an elevated
risk for mortality: adjusted RR, 1.52; 95% CI, 1.03 to 2.26; P <
0.05.306
The relationship between Hb level and mortality, when examined at other
cutoff values for Hb, appeared continuous. Patients with more severe
anemia also experienced increased risk for hospitalization (17.2% ±
1.8% versus 12.3% ± 2.1%, respectively; P < 0.01).
The Heart
A single RCT provides
evidence for the benefit of treatment of anemia with ESA compared with
placebo. In a blinded crossover trial of 11 children aged between 2.3
and 12.3 years, undergoing HD or PD, and with a baseline Hb level
between 4.3 and 8.1 g/dL, patients were assigned to either ESA therapy
(Hb > 10 g/dL) or placebo for 24 weeks.126
Seven patients completed both trial arms. ESA therapy was associated
with partial correction of an elevated cardiac index by 6 months and a
significant reduction in left ventricular mass by 12 months.
Two observational studies have examined the relationship between anemia and LVH in children with CKD.307,308 In these studies, patients with severe LVH (left ventricular mass index > 51 g/m2)
showed a statistically lower Hb level than those without LVH (Hb, 9.5 ±
1.8 versus 10.9 ± 2.3 g/dL; P = 0.027). Left ventricular compliance
also was related to Hb level in children (r = –0.65; P = 0.02). The
findings suggest that severe anemia in children with CKD stage 5 leads
to chronic increases in cardiac workload and a consequent increase in
both left ventricular end-diastolic volume and mass.
In this RCT,
exercise capacity improved with ESA treatment (mean achieved Hb, 11.2
g/dL; range, 9.5 to 14.2 g/dL) compared with placebo control.126
Measures of capacity significantly affected included a 2-minute walking
test (n = 7) and a formal treadmill testing using the Bruce protocol,
full (n = 3) or modified (n = 3). Distance walked, in meters,
approached but did not reach statistical significance in the ESA arm of
the crossover, P = 0.06; similar results were seen from both the
regular or modified treadmill data, P = 0.07.
In a
nonrandomized interventional trial, 18 children with CKD stage 5 (15
patients, on HD or PD) and a Hb level less than 9.9 g/dL were
administered IV or SC ESA until Hb level was greater than 9.9 g/dL;
baseline Hb level of 6.5 ± 0.8 g/dL changed to a final level of 10.0 ±
0.6 g/dL; P = 0.001.309
Exercise time (treadmill with a modified Bruce protocol) increased
significantly (before ESA, 10.3 ± 1.9 minutes; after ESA, 11.2 ± 1.9
minutes; P = 0.01), and resting oxygen consumption decreased from 7.8 ±
1.8 to 6.9 ± 1.4 mL/min/kg; P = 0.01 with the higher Hb level. However,
there was no change in stroke volume, blood pressure, or any cardiac
indices after the first month at the higher Hb level.
Similarly, a small cohort (n = 7) of HD patients showed an improvement
in aerobic work capacity and effort tolerance, as evidenced by
statistically significant changes in the workload reached, peak oxygen
uptake, and average ventilatory anaerobic threshold after treatment of
anemia with ESA (baseline Hb, 6.3 ± 0.9 g/dL versus final Hb, 11.2 ±
1.2 g/dL).310
Finally, 10 children undergoing PD were evaluated before and 18 months
after limited correction of anemia with ESA (baseline Hb, 5.9 ± 0.9
g/dL versus final Hb, 8.7 ± 1.5 g/dL). Patients showed a significant
slowing of heart rate, P < 0.01, but no improvement for other
cardiac parameters.311
QOL and Neurocognitive Effects
The relationship between QOL and anemia has been examined in children with CKD.126,312,313 In 2 trials,312,313
QOL instruments were not validated in patients with CKD and were
completed by parents. Only 1 study blinded parent-responders to use of
ESA or placebo, although 5 of 7 parents in that study correctly
identified use of ESA during the appropriate treatment.126
In 116 children enrolled in a multicenter trial, sleep, activity (in
school, at home, or in social situations), alertness, feelings, and a
summary score composed of all subscores were assessed at baseline and
every 6 months during ESA treatment to attain a target Hb level of 9.6
to 11.2 g/dL compared with baseline pretreatment Hb level of 6.7 g/dL
(range, 3.4 to 9.5 g/dL).313
Scores at 1 year after ESA increased after treatment for all aspects
examined, but only the 10% increase in the summary score achieved
significance (P < 0.05).
In the previously described randomized crossover trial,126
a 25-question modified parental questionnaire used a visual analog
scale to assess 5 domains: sleep, school performance, diet,
psychosocial, and a physical performance/health construct. Only
physical performance and general health showed a significant treatment
effect (again, baseline Hb, 4.3 to 8.1 g/dL versus final Hb, 11.2 g/dL;
range, 9.5 to 14.2 g/dL).
A generic health QOL
questionnaire has been administered in a cross-sectional fashion to the
parents of children with CKD stages 1 to 5 and transplant recipients.312
This instrument, which has shown internal consistency and concurrent
validity and has been used in a single-center trial of children on HD
therapy,314
measures 12 aspects of health-related QOL in the domains of physical
functioning; limitations in schoolwork and activities with friends,
general health, bodily pain and discomfort, limitations in family
activities; emotional/time impact on the parent; impact of emotional or
behavior problems on school work and other daily activities;
self-esteem; mental health; behavior; family cohesion; and change in
health. When evaluated as a continuous variable, Hct was linked
directly to measures of improved health, as seen in the single-item
general health (r = 0.36; P = 0.003), general health (r = 0.29; P =
0.004), and physical functioning (r = 0.35; P = 0.0004) domains.312
Further analysis of the same data, adjusting for eGFR, age, sex, race,
dialysis modality, and transplantation or chronic renal insufficiency
and dividing the patients into groups with Hb level greater than or
less than 10.8 g/dL (defined by the investigators as anemic), showed an
association between anemia and 4 domains: Parental Impact-Time, Family
Activities, Role–Physical, and Physical Functioning. Further
multivariate analysis done after division of the group into Hb
tertiles, less than 9.9 g/dL, 9.9 to 10.8 g/dL, and greater than 10.8
g/dL, showed a strong dose-response relationship between Hb level and
health-related QOL as measured by this instrument. It should be noted
that differences between the mid and upper tertile of Hb levels did not
reach significance, whereas those between the lowest and upper tertile
in the areas of Physical Functioning (P = 0.02), Role–Emotional (P =
0.05), Role–Physical (P = 0.02), Parental Impact–Time (P = 0.004),
Family Activities (P = 0.003), and Physical Summary score (P = 0.01)
did. (Note: these results have been converted from Hct to Hb values.)
The neurocognitive effects of anemia also have been examined. In
healthy children aged 6 to 11 years, impairment in cognition is
associated with iron deficiency and an Hb level less than 11.8 g/dL.315
Furthermore, in a multicenter single-arm interventional trial
evaluating 22 children with CKD aged 4 months through 16 years,
treatment of anemia was associated with a significant increase in IQ,
determined by using the Weschler intelligence test, although the
relative increase in Hb levels was small (Hb baseline, 9.2 ± 1.6 versus
final, 9.7 ± 1.7 g/dL; P = 0.007).316
Nutrition and Growth
No reliable
studies have been published that examine the relationship between
treatment of anemia and nutrition in children. The literature consists
largely of subjective reports by the child or family or short small
trials that fail to achieve significant treatment effects.
Treatment of anemia apparently fails to reverse growth retardation in children with CKD undergoing HD or PD.317-318
In a US phase III, randomized, double-blinded, placebo-controlled trial
of ESA therapy in children, 81 children on HD or PD therapy showed a
substantial increase in Hb levels with treatment (baseline, 6.3 to 6.6
g/dL to final, 9.3 g/dL), and no effect was seen for any measured
nutrition or growth parameter, including midarm circumference, triceps
skin-fold thickness, weight gain, or the SD scores for growth velocity
or height.317
Hypertension
The development or
worsening of hypertension during treatment with ESAs in children is of
significant concern. In a study of children aged 4 months to 21 years,
assignment to either high-dose (epoetin, 450 IU/kg/wk) or low-dose (150
IU/kg/wk) ESA treatment was associated with a significant increase in
diastolic blood pressure by week 12 compared with baseline (88 ± 6.7
versus 68 ± 17 mm Hg; paired t-test, P = 0.01).319
The investigators reported a nonsignificant trend between increasing Hb
levels and increasing systolic and diastolic blood pressures despite
stable or lower ESA dose.
Thrombotic Events
No thrombotic
events, including vascular access thrombosis, were reported in either
arm of the mentioned high-dose versus low-dose ESA trial.319
However, the small number of patients, relatively short length of
follow-up, and relatively few patients with HD preclude any reliable
conclusions about safety. No other larger prospective trials of
pediatric patients treated with ESAs to various Hb targets are
available to further address the issue of clotting or access
thrombosis, although it has been reported to occur intermittently in
children.318,320-323
ESA Therapy and Loss of Renal Function
In patients with ND-CKD assigned to high-dose compared with low-dose
ESA treatment, no significant difference in creatinine levels was seen;
in the same trial, between-group comparison showed no change in Kt/V
among patients with HD-CKD.319
| © 2006 National Kidney Foundation, Inc. |