Chronic Kidney Disease: A Silent Epidemic Part 1

About This Presentation

Title:

Chronic Kidney Disease: A Silent Epidemic Part 1

Description:

US Renal Data System, 2000 Atlas of ESRD in the United States. ... Inpatient Days among Elderly Medicare Pts with CKD in the United States. ... – PowerPoint PPT presentation

Number of Views:1117

Avg rating:3.0/5.0

Slides: 226

Provided by: jerryyeega

Category:

more less

Transcript and Presenter's Notes

Title: Chronic Kidney Disease: A Silent Epidemic Part 1

1
Chronic Kidney Disease A Silent Epidemic (Part
1)

Naima Ogletree, MSN, APRN, BC
Nephrology Hypertension
Henry Ford Health System

2
Objectives

Define CKD prevalence, epidemiology, and risk
factors
Discuss occurrence of complications and co-morbid
conditions of CKD
Describe treatment guidelines

3
Kidney Anatomy

Normal adult kidney is 1112 cm longWt 125170
g
Left kidney Right kidney in size,male
female located at T12 to L3
The kidney (a bean-shaped structure) is composed
of parenchyma and the collecting system.
Parenchyma consists of the renal cortex and inner
medulla. The collecting system includes the
calcyces that form the renal pelvis that drains
into the ureters
Kidneys are usually perfused by a single renal
branching artery

4
Physical Location of Human Kidney
LEFT KIDNEY
URETER
BLADDER
5
Anatomy of the Kidney
FIBROUS CAPSULE
CORTEX
PYRAMID
PAPILA
RENAL CALYX
RENAL PELVIS
RENAL ARTERY
RENAL VEIN
URETER
6
Microscopic Anatomy

There are 300,000 to 1,200,000 nephrons (basic
structure and functional unit of the kidney) in a
single kidney
Glomeruli, loop of Henle, proximal and distal
tubule compose the nephron

7
A MICROSCOPIC LOOK AT THE RENAL CORTEX
GLOMERULUS
8
Glomerulus Anatomy
9
Basic Concepts of the Kidney

Regulatory function Controls composition and
volume of the body fluids
Maintains acid-base balance by varying the
excretion of water and solutes
Endocrine function producing several hormones
- renin
- erythropoietin
- active vitamin D3
- prostaglandins, adenosine, etc

10
Basic concepts of the Kidney

Excretory function removes various nitrogenous
metabolic end products in urine. For example, the
kidneys filter blood through the glomerulus
forming an ultrafiltrate.
As the ultrafiltrate passes through the kidney,
reabsorption of essential products and secretion
of unwanted products occur.

11
DYSFunction of the Kidney

Disrupts HOMEOSTASIS.
Excretion of waste products of metabolism.
Water electrolyte and acid base balance.
Disrupts HORMONAL FUNCTION.
Erythropoietin.
Vitamin D3
Renin, prostaglandins, angiotensinogen 2, nitric
oxide , endothelin and bradykinin
Miscellaneous
Gluconeogenesis

12
CKD Background

Common disorder
Less common than HTN
More common than diabetes
Progressive disorder
Underdiagnosed
Undertreated due to lack of agreement of its
definition and staging

Kidney/Dialysis Outcomes Quality Initiative. Am J
Kidney Dis. 200240S1S246.
13
Chronic Kidney Disease (CKD)

Includes all types and levels of kidney
dysfunction
Avoid usage of CRI and CRF, which do not
indicate severity of dysfunction
CKD is not etiology-specific and causation must
always be pursued
CKD from diabetic nephropathy
CKD from hypertensive nephrosclerosis
Membranous nephropathy

Kidney/Dialysis Outcomes Quality Initiative. Am J
Kidney Dis. 200240S1S246.
14
Overview of CKD

Epidemiology of CKD
20 million adults in the United States
Millions more at risk
Aging population
Increasing prevalence of diabetes mellitus
Increasing prevalence of hypertension

15
CKD Care is Costly
TH Hostetter, National Kidney Education Program,
2003.
16
CKD Prevalence by NHANES III
7.6
5.9
5.3
0.4
0.3
J Coresh, et al. Am J Kidney Dis. 200341(1)112
17
CKD Prevalence by NHANES III

National Center for Health Statistics(19881994)
Dataset (1988-1994) 15,625 adults
Age 20 yr
Extrapolated to 177 million adults
CKD by SCr
SCr 1.5 mg/dL, 6.2 million
SCr 1.7 mg/dL, 2.5 million
SCr 2.0 mg/dL, 0.8 million
Greater SCr in older subjects, males
andnon-Hispanic blacks

HTN in 70
75 treated

CGM Jones, et al. Am J Kidney D.
199832992999. J Coresh, et al. Am J Kidney
Dis. 200341112.
18
CKD Prevalence by NHANES III
CGM Jones, et al. Am J Kidney Dis.
199832992999. J Coresh, et al. Am J Kidney
Dis. 200341112.
19
Endstage Renal Disease (ESRD)

ESRD
Medicare term permits federal reimbursement
Pt requires renal replacement therapy for
survival
Hemodialysis
Peritoneal dialysis
Kidney transplantation

Kidney/Dialysis Outcomes Quality Initiative. Am J
Kidney Dis. 200240S1S246.
20
ESRD Increasing Problem

? ESRD incidence, prevalence, cost
Pts living longer
Increased prevalence of diabetes
Prevalence in 2003, 300,000 pts
Projection for 2010, 600,000 pts
Wayne Co., MI highest prevalence of ESRD per
capita of all U.S. counties
1079 of 3093 new starts in MI, 2001
3913 of 9913 prevalent pts in MI, 2001

Data on file National Kidney Foundation of
Michigan, 2002.
21
ESRD Disease of the Elderly
148,508
125,280
55,105
26,177
5961
n361,031
United States Renal Data System (USRDS) 1997
Annual Data Report.
22
ESRD ? Risk by EthnicityRacial Differences in
ESRD in U.S. from 19901998
United States Renal Data System (USRDS) 2000
Annual Data Report WWW.USRDS.ORG.
23
ESRD Prevalence by Ethnicity
Abbrev NA, Native American AA,
African-American C, Caucasian. n 361,031
United States Renal Data System (USRDS) 1997
Annual Data Report.
24
ESRD Incidence by Ethnicity Racial Differences
in ESRD in U.S. from 19901998
United States Renal Data System (USRDS). 2000
Annual Data Report WWW.USRDS.ORG.
25
ESRD ? Incidence and Prevalence
Diabetes is the most common cause in Caucasians,
Hispanics, Asians, and overall. Among
African-Americans, hypertension is the most
common cause of ESRD.
US Renal Data System, 2000 Atlas of ESRD in the
United States.
26
ESRD Racial Distribution for Comorbidities in
Dialysis (1999)
Diabetes mellitus as a primary diagnosis or
contributing diagnosis. Diabetes mellitus that
requires insulin treatment, which is a subset of
the diabetes category.
United States Renal Data System (USRDS) 2000
Annual Data Report WWW.USRDS.ORG
27
Overall Rates of Hospitalization
Inpatient Days among Elderly Medicare Pts with
CKD in the United States.
Am J Kidney Dis. 2003 Nov42(5)972-81
28
GFR and Hospitalization
Go et al. New Engl J Med. 20043511296-1305.
29
Change in FOCUS
CKD
2
3
4
E S R D
30
CKD Becomes the Focus

Rationale for Initiative
CKD is a public health problem.
Economical, effective testing methods and
therapies exist.
Testing and therapy are inadequately applied.

BA Boissonault. Niagara Health Quality Coalition,
2003. L Smith-Wheelock. National Kidney
Foundation of Michigan, 2003.
31
Timely Referral Keeps pts Out of the Red Zone
NKF CKD Stage by MDRD GFR Equation
4
5
E S R D
REFER TO KIDNEY DOCTOR

Refer in Stage 1 or 2
Uncontrolled HTN
Hematuria
Proteinuria
Structural lesion

NORMAL AGE DECLINE
60
30
15
120
90
GFR (mL / min / 1.73 m2)
Kidney/Dialysis Outcomes Initiative. Am J Kidney
Dis. 200239S1S266.
32
CKD Early CKD Treatment Preserves Kidney Function
100
75
GFR
50
25
10
4
7
9
11
Time (yr.)
TH Hostetter, National Kidney Disease Education
Program, 2003.
33
CKD ComplicationsEvolution and Acceleration by
Stage
DM, ARF CKD complications may occur earlier
34
(No Transcript)
35
CKD Three-Fold Initiative

Screen and prevent CKD in pts who are at-risk
Develop an early CKD identification process
Establish a collaborative disease management
model for internists, family practitioners, and
nephrologists

36
Detection 0f pts at Risk
BUN blood urea nitrogen GFR glomerular
filtration rate.Pereira. Personal communication.
37
CKD Screening and Prevention

Identify at-risk medical populations
Hypertension
Diabetes
Metabolic syndrome
1st degree relatives of ESRD pts
CKD history often neglected during Hx
Identify at-risk ethnic groups
Hispanics
African-Americans
American Indians (Native Americans)

United States Renal Data System (USRDS) 2000
Annual Data Report WWW.USRDS.ORG.
38
CKD High-Risk Groups

Diabetics with urine AlbCr ratios30 mg Alb/1 g
Cr
Non-diabetics with urine AlbCr ratios 300 mg
Alb/1 g Cr
Non-diabetics with MDRD GFR

Kidney/Dialysis Outcomes Initiative. Am J Kidney
Dis. 200239S1S266.
39
CKD Screening and Prevention

Screening at-risk pts
Biochemical profile
Urinalysis with microscopic exam
Urine protein (albumin) determinations
MDRD GFR estimation

40
CKD Three-Fold Initiative

Screening of pts at-risk for CKD
Development of an early CKD identification
process
Establishment of a disease management protocol
between internists and family practitioners and
nephrologists

41
CKD Evolution of GFR Estimating Methods
A Akbari, et al. Arch Intern Med.
2003163356360. S Klahr, et al. MDRD Study
Group. N Engl J Med. 1994330877884.
42
CKD MDRD GFR

Multi-variable equation
Demographics Age, Gender, Ethnicity
Biochemical Albumin, SCr, BUN
Validated in 577 pts
By iothalamate clearance
For GFRs 3090 mL/min/1.73 m2
MDRD GFR Eqn. 7 (mL/min/1.73 m2) 170 ?
SCr0.999 ? Age0.176 ? BUN0.17 ? Alb0.318 ?
0.762 (female) ? 1.18 (African-American)

Kidney/Dialysis Outcomes Quality Initiative. Am J
Kidney Dis. 200239S1S266. G Manjunath, et al.
Postgrad Med. 2001110(6)5562.
43
CKD Classification by MDRD GFR

Rationale for use
GFR direct measurement of kidney function
GFR best index of kidney function in health and
disease
GFR correlates with pathologic severity of
disease
GFR correlates functional level with risks of
CKD progression and development of CV disease

G Manjunath, et al. Postgrad Med.
2001110(6)5562.
44
CKD NKF Definition

Disorder must be 3 mo duration
MDRD GFR
GFR 90 mL/min/1.73 m2 with either
Parenchymal abnormality (cyst, scar) or
Hematuria (4 RBCs/hpf) confirmed by
microscopical examination on 2 occasions or
Proteinuria (2 occasions, 1 mo apart)
Dipstick ?2 or 100 mg/dL
ProCr ratio ?1.0 (Pro and Cr in mg/dL)
AlbCr ratio ?500 mg/g
24-h collection ?1.0 g/24-h/1.73 m2

S Klahr, et al. N Engl J Med. 1994330877. Kidney
/Dialysis Outcomes Quality Initiative. Am J
Kidney Dis. 200239S1S266.
45
CKD Normal Kidney Function

MDRD GFR 90 mL/min/1.73 m2 and all of the
following
No hematuria
No proteinuria
No parenchymal or structural abnormality (cyst,
scar, hydronephrosis)

Kidney/Dialysis Outcomes Initiative. Am J Kidney
Dis. 200239S1S266.
46
CKD Age-Related Decline in GFR

Age-related declines in GFR occur
Should not be considered disease
GFR 6089 mL/min/1.73 m2
Do not refer pt to nephrologist if GFR is stable
and all of the following
No proteinuria
No hematuria
No structural lesion(s)

Kidney/Dialysis Outcomes Initiative. Am J Kidney
Dis. 200239S1S266.
47
NKF CKD Stages 15
Kidney/Dialysis Outcomes Initiative. Am J Kidney
Dis. 200239S1S266.
48
CKD Screening and Prevention Summary

Use MDRD GFR not SCr
Spot urine AlbCr ratio
Collect specimen at 06001200 hours
24-h urine collection, no longer required
Screenees?
GFR
Not from age-related decline
Hypertension
Diabetes annual testing
FH of CKD less frequently, if normal
Hematuria
Edema of unknown cause

G Manjunath, et al. Postgrad Med.
2001110(6)5562.
49
CKD Three-Fold Initiative

Screening for and prevention of CKD in pts
at-risk for CKD
Development of an early CKD identification
process
Establishment of a collaborative disease
management model between internists and family
practitioners and nephrologists

50
CKD Under-recognized Problem

Patients unaware
Only 13 of pts with CrCl dipstick proteinuria aware of their CKD
Only 8 of pts with known CKD aware of their
CKD, despite recent physician visit
Implications
Physicians require more CKD knowledge
Late referral of pts with advanced CKD to
nephrologists, e.g., African-American men

Am J Kidney Dis. 20024011731178.
51
CKD Under-recognized Problem

Only 10 of Medicare beneficiaries with diabetes
receive annual urine albumin tests
Less than 1/3 of hospitalized CKD pts with
proteinuria are prescribed an ACEI at discharge

Medicare data on file WM McClellan, et al. Am J
Kidney Dis. 199729368.
52
CKD Survey of PCPs
53
CKD Delayed Referral to Nephrologist
A Stack. Am J Kidney Dis. 200341310318.
54
CKD Reasons for Delayed Referral to Nephrologist

CKD is under-recognized
Failure to screen pts at-risk
Fear of loss of control over pt
PCPs unaware of incremental benefits of earlier
referral
Fewer ER visits (pulmonary edema)
Significant healthcare cost savings
Lack of education regarding CKD management

R Sesso, AG Belasco. Nephron Dial Transplant.
1998112417. DW Eadington. Nephron Dial
Transplant. 1996112124-2126. RJ Schmidt, et al.
Am J Kidney Dis. 199632278283. P Jungers, et
al. Kidney Int. 199341S170S173.
55
CKD Consequences of Delayed Referral
A Stack. Am J Kidney Dis. 200341310318. Late
referral means Nephrology consultation and dialysis. AVF,
arteriovenous fistula AVG, arteriovenous graft.
56
CKD Delayed Referral Results in Higher Medical
Costs in Early ESRD
Source BA Boissonault for the Niagara Health
Quality Coalition, 2003.
57
Advanced CKD Substantially Impairs Quality of Life
Klang et al. Quality of Life Research.
19965109-116.
58
Ultimate GoalDelay CKD Progression

Diagnose / treat comorbid conditions
Evaluate / treat CVD
Iatrogenic risks _at_ CKD Stage 3
protect against further insults (e.g., ARF)

59
CKD ARF Prevention

Rationale for Intervention
ARF often preventable
ARF produces residual kidney damage, i.e., CKD
CKD pts at higher risk for ARF

PA McCullough, et al. Am J Med.
1997103368375 L Gruberg, et al. J Am Coll
Cardiol 20003615421548
60
CKD Increased Risk for ARF

ECF volume depletion fosters ARF
High-risk groups
DM, types 1 and 2
Non-DM CKD Stage 35 (i.e., GFR
Liver failure
Heart failure
CV operations
Radiocontrast procedures

E Nikolsky, et al. Rev Cardiovasc Med
20034(Suppl 1)S7S14. Data extrapolated from
multiple studies
61
Avoid Iatrogenic Injury

AVOID NEPHROTOXINS
NSAIDs, AGs, Amphotericin B
Radiocontrast
Stop diuretics 34 d before procedure
ECF volume expansion(preferably with HCO3 ?)
N-Acetylcysteine (SCr dependent)

M Tepel, et al. NEJM, 343180184, 2000 C Caputo,
et al. AJKD Dis 39A14, 2002 (abstract)
62
Acute Renal Failure NSAID-Induced Afferent
Arteriolar Constriction
NORMAL PGC
Paff
Peff
?PGC
? RAA
Paff
NSAID
Peff
VA Valentini, et al. Arch Intern Med.
199115123672372. RAA, afferent arteriolar
resistance.
63
NSAIDS

NSAIDs (COX-1/-2 inhibitors) lower GFR, retain
sodium and may cause hyperkalemia
People with an activated Renin-Angiotensin-Aldoste
rone system are especially at risk for
NSAID-induced ARF
Advanced age
Hypertension
Diabetes
Dehydration
Concomitant diuretic use

64
CKD Radiocontrast-induced Nephropathy

Common complication in CKD and other high risk
groups
Significant morbidity and / or mortality
Event-free survival is ? by contrast nephropathy
In-hospital mortality ? by contrast nephropathy
Preventable, modifiable

R Solomon, et al. N Engl J Med 19943314161423.
NE Lepor. Rev Cardiovasc Med 20034(Suppl
1)S15S20.
65
(No Transcript)
66
CKD Radiocontrast-induced Nephropathy

High-risk groups
CKD of any cause
Advanced age
Diabetes
Nephrotoxin co-administration
NSAID (not aspirin)
Diuretics
ACEI, ARB
Aminoglycosides
Cyclosporine, tacrolimus
cis-platinol

R Solomon, et al. New England Journal of
Medicine. 1994331141620.
67
CKD Radiocontrast-induced Nephropathy Prevention

Nephrotoxins
Stop diuretics, ACEIs/ARBs, NSAIDs
Avoid aminoglycosides, amphotericin B
Prophylaxis
Normal saline to expand ECF volume, unless edema
is present
N-acetylcysteine
Preferred contrast media
Non-ionic, low osmolar contrast
Iso-osmolar agents, if available

R Solomon, et al. N Engl J Med 19943314161423 N
E Lepor. Rev Cardiovasc Med 20034(Suppl
1)S15S20
68
Recommendations for Common Interventions Used to
Prevent Contrast-medium-induced Nephropathy
69
CKD Preventing Progression

Attain glycemic control in DM
Attain BP target
Block RAAS
Treat anemia of CKD
Treat associated CVD and dyslipidemia
Prevent renal osteodystrophy (ROD)
Prevent ARF and avoid nephrotoxins
Optimize nutrition

ME Rosenberg. Chronic Kidney Disease Progression
in NephSAP. Ed. RJ Glassock. 20032(3)85111.
70
Chronic Kidney Disease (CKD)

Generic
Any kidney disorder
Does not replace specific disorders
CKD, secondary to ________
Stratified into Stages by GFR
Complications stratification
Morbidity stratification
Guides intensity of therapy

71
CKD Guidelines for Treatment

National Kidney Foundations Kidney Disease
Outcomes Quality Initiative (NKF KDOQI)
Based heavily on Evidenced Based Medicine
Offers opinions that guide treatment

72
(No Transcript)
73
NKF Guidelines address domains of CKD care
74
NKF Guidelines address domains of CKD care
Periodic eGFR
75
Decrease CV Disease Risk Factors
76
CKD CVD Prevention Strategies Level of
Evidence
Large RCTs that involve CV risk prevention
strategies in CKD have not been performed.
77
Major Cause of Death in CKDCardiovascular Disease
Shulman et al. Hypertension. 199813(supple
1)I-80I-93.
78
CKD CVD Risks

CVD risk ? 1.42.05X ifSCr 1.41.5 mg/dL
CVD risk ? 1.53.5X with microalbuminuria
First-year CVD mortality of CKD (3.5) increases
5-fold (17) with addition of diabetes
Annual CVD ?10100X in ESRD

Multiple Sources J Flack, et al., 1993. AS
Levey, et al., 1998. Jensen, et al., 2000.
Ruilope, et al., 2001. JFE Mann, et al. 2001. AS
Collins, et al., 2002.
79
Cardiovascular Health Study Even Mildly
Elevated SCr Increases CV Disease (CVD) Risk.
Kidney/Dialysis Outcomes Initiative Clinical
Practice Guidelines for Managing Dyslipidemias in
Chronic Kidney Disease. Am J Kidney Dis.
200341(Suppl 3)S1S91.
80
CKD CVD Comorbidities (1999)
Diabetes mellitus as a primary or contributing
diagnosis. Diabetes mellitus that requires
insulin treatment, which is a subset of the
diabetes category.
81
CV Mortality in General Population (GP)
Dialysis pts by Ethnicity
MJ Sarnak, AS Levey. Semin Dial. 1999126976.
82
Cardiovascular Health Study Even Mildly
Elevated SCr Increases CV Disease (CVD) Risk.

Rationale for Intervention
CV mortality is higher in CKD than general
population
50 of ESRD pts die from CVD
Death before CKD Stage 5/ESRD is common
CVD inherent in CKD
CV risk CKD 30 y.o. 75 y.o. non-CKD
CKD is CHD/diabetic equivalent
CKD is pro-inflammatory

Kidney/Dialysis Outcomes Initiative Clinical
Practice Guidelines for Managing Dyslipidemias in
Chronic Kidney Disease. Am J Kidney Dis.
200341(Suppl 3)S1S91.
83
Decrease CV Risk Factors

Strict BP control
Tight glycemic control
Use anti-RAAS drugs
Lipid control
Correct anemia

84
Hypertension CKD
85
Guideline Hypertension

1.1 Antihypertensive therapy should be used in
CKD to
1.1.a. Lower blood pressure (A)
1.1.b. Reduce the risk of CVD, in pts with or
without hypertension (B)
1.1.c. Slow progression of kidney disease, in pts
with or without hypertension (A)
1.2 Modifications to antihypertensive therapy
should be considered based on the level of
proteinuria during treatment (C)
1.3 Antihypertensive therapy should be
coordinated with other therapies for CKD as part
of a multi-intervention strategy (A).
1.4 If there is a discrepancy between the
treatment recommended to slow progression of CKD
and to reduce the risk of CVD, individual
decision-making should be based on risk
stratification (C).

86
BP Control is Suboptimal
SBP NHLBI. JNC 7 Express. The Seventh Report of the
Joint National Committee on Prevention,
Detection, Evaluation and Treatment of High Blood
Pressure. 2003.
87
JNC 7 Reclassification of BP Based on Risk
JNC VIBP (mm Hg)
JNC 7BP (mm Hg)
Optimal
Normal
Normal
120-129/80-84
Prehypertension
120-139/80-89
Borderline
130-139/85-89
Hypertension
Stage 1
140-159/90-99
Stage 1
140-159/90-99
Stage 2
160-179/100-109
Stage 2
160/100
Stage 3
180/110
Source for JNC VI Arch Intern Med.
19971572413-2446. Adapted from Chobanian AV, et
al. Hypertension. 2003421206-1252.
88
HTN Treatment by JNC 7
HTN w/ No Compelling Indications
C(KD)ompelling Indications
Stage 1 HTN (SBP 140-159 or DBP 9099
mmHg) Thiazidediuretic for most Consider ACEI,
ARB, ß-blocker, CCB or combination
Stage 2 HTN (SBP 160 or DBP 100 mmHg) 2-drug
combofor most Usually thiazide ACEI, ARB,
ß-blocker, or CCB
Drug(s) for compelling indications Other BP drugs
(thiazide ACEI, ARB, ß-blocker, CCB)as needed
Chobanian AV, et al. The JNC 7 Report. JAMA.
20032892560-2572. Compelling indications CHF,
post-MI, high risk of CAD, DM, CKD, stroke,
migraine
89
BP Targets in Diabetic and Nondiabetics with
Kidney Disease
Am J Kidney Dis, May (Suppl.), 2004
90
HTN Treatment in CKDDiabetic or Nondiabetic
91
Hypertension in CKD

Rationale for Intervention
Elevated BP worsens CKD
GFR declines faster with HTN
Rapid decline rate is 4 ml/min/1.73 m2/yr
Target BP
1 g/d

92
BP Control Prevents CKD Progression
MAP (mm Hg)
95
98
101
107
104
110
113
116
119
r0.69 PGFR Decline(mL/min/y)
Untreated HTN
130/85
140/90
GFR, glomerular filtration rate HTN,
hypertension MAP, mean arterial
pressure. Adapted from Bakris GL et al. Am J
Kidney Dis. 200036646-661.
93
Hypertension CKDOptimal BP Control

No edema
Limit daily sodium intake
6 gm NaCl (102 mEq)
2400 mg sodium (104 mEq)
Diuretics
GFR 40 ml/min/1.73 m2, HCTZ
GFR
RAAS blockade
ACEI
ARB

94
Benefits of BP TherapyGeneral Population
CAD coronary artery disease, PAD peripheral
artery disease CHF congestive heart
failure. Adapted from Kannel WB. JAMA.
19962751571-1576.
95
Hypertension and CKDMultiple Drugs Required
UKPDS (Type 2 DM
MDRD (Nondiabetic Kidney Disease
HOT (DM Subgroup Analysis
AASK (African Americans, No DM
RENAAL (Type 2 DM Nephropathy
IDNT (?135/85 mm Hg)
Type 2 DM Nephropathy
4
3
2
1
Number of BP Medications
MAP mean arterial pressure.
Bakris G, et al. AJKD. 200036646-661 Brenner
BM, et al. NEJM. 2001345861-869. Lewis EJ, et
al. NEJM. 2001345851-860.
96
(No Transcript)
97
Glycemic Control
98
T2DN Global Perspective

Diabetes (DM) affects more than 170 million
people worldwide
Number will rise to 370 million by 2030
About 1/3 of affected will eventually develop
progressive renal deterioration
Microalbuminuria (MA) develops in25 of pts per
year

98
99
Epidemiology of Diabetes

19 million persons
0.5 million type 1 DM
Remainder, type 2
Over-representation in ESRD population worldwide
Over-representation in U.S. ESRD population
Incidence increasing with rate of obesity

100
(No Transcript)
101
Global Estimates and Projectionsfor Incidence of
Diabetes Mellitus
Type I Diabetes
Type II Diabetes
250
200
150
In Millions
100
50
0
1997
2010
Year
A Amos, et al. Diabetes Medicine. 199714Suppl
5S1-85.
102
NEW ESRD Incidence from DM
Centers for Disease Control Diabetes
Surveillance, 1997.
103
Predictions Regarding T2DM

Year 2000 and beyond
One of three newborns will develop type II
diabetes as an adult
One of two newborns, Hispanic or African
American, will develop type II diabetes as an
adult
Year 2050
U.S. 45?50 million will develop T2DM
Implications for CKD and RRT uncertain

Dr. KM Venkat Narayan
104
it appears that there is an emerging pediatric
epidemic of type 2 diabetes. If this epidemic
cannot be averted, its full public health effect
will be felt as affected children become adults
and the long-term complications of diabetes
develop.
New Engl J Med 2002346(11)
105
ESRD Etiology by 1 Diagnosis
Other 10
DM 50
GN 13
HTN 27
United States Renal Data System (USRDS) 2000
Annual Data Report WWW.USRDS.ORG.
106
First-year mortality rates, by CKD diabetic
status
General Medicare patients age 67 older rates
adjusted for age, gender, race, determined
for the first year after the cohort-defining
period. Reference population 19992000 cohort.
107
Natural History of Diabetic Nephropathy
108
Glomerulus Site of Hyperfiltration in Diabetes
and Obesity
109
(No Transcript)
110
Diabetic Glomerulosclerosis
111
Glycemic Control Retards Progression of CKD
50 Reduction
Based on Diabetic Control and Complications
Trial data
Adapted with permission from Skyler JS.
Endocrinol Metab Clin North Am. 199625243
112
HbA1c Delay DN

OHKUBO TRIAL (1995)
Hypothesis Development of nephropathy is
decreased by intensive insulin therapy
Primary and secondary prevention study
6-mo F/U intervals for 6 yr

Glycemic Control
113
HbA1c Delay DN
Glycemic Control
114
HbA1c Delay DN

REQUIREMENTS
HbA1C 6.5
FBS 110 mg/dl
2-h PPG 180 mg/dl

Glycemic Control
115
HbA1c Delay DN

EUGLYCEMIA
Partially reverses glomerular hypertrophy and
hyperfiltration
Type 1 DM delays onset of microalbuminuria
Kidney-Pancreas transplant pancreatic
transplant prevents recurrent nephropathy in
allograft kidney

Fioretto, et al. New Engl J Med 3396975, 1998
116
HbA1c Delay DN
DCCT Research Group. New Engl J Med 329977, 1993
117
(No Transcript)
118
Decline of GFR in DN
119
Questions?
120
Chronic Kidney Disease A Silent Epidemic (Part
2)

Naima Ogletree, MSN, APRN, BC
Nephrology Hypertension
Henry Ford Health System

121
Proteinuria Reduction
122
CKD Albuminuria
G Remuzzi, et al. New Engl J Med. 2002
34611451150.
123
ProteinuriaDual Significance

Proteinuria results from injury to glomerular
circulation
Increased proteinuria is associated with
progressive CKD
In diabetes and hypertension, proteinuria
signifies injury to the systemic circulation
Proteinuria is associated with increased CV risk

124
RAAS, Albuminuria and AtherosclerosisSteno
Hypothesis
American Journal of Kidney Diseases, Vol 47, No 6
(June), 2006 pp 927-946
125
CKD Anti-Proteinuric Therapy

Rationale for Intervention
Microalbuminuria independent CVD risk factor
In-hospital mortality ? 3-fold by proteinuria
(100 mg pro/g Cr)
Proteinuria correlates with CKD progression
Proteinuria may worsen CKD

Adapted from multiple studies. HOPE subanalysis
JFE Mann, et al. J Am Soc Nephrol. 2003
14641647. MARVAL Circulation.
2002106672-678. RENAAL N Engl J Med.
2001345861869. IDNT N Engl J Med.
2001345851860.
126
Albuminuria Decreases SurvivalGraded Effect
Gall MA, et al. Diabetes 1995441303-1309
127
UPC _at_ 6 Mo Predicts Kidney CVD Events RENAAL
Substudy (losartan, no ACEI)
RENAAL Study Group, 2002
128
BP, Proteinuria and CKD

Reduction of protein and albuminuria
Intermediate goals in slowing CKD
Complementary
Aggressive BP control is primary consideration of
anti-proteinuria
Multi-drug regimens required

129
Renin-Angiotensin System Blockade

Moderate to high doses of ACEIs / ARBs have been
associated with beneficial effects on kidney
disease progression in controlled trials
Where tested, ACEIs / ARBs have generally similar
effects on BP, urine protein excretion, and
slowing CKD progression

Greatest efficacy in proteinuric disorders
130
How RAAS Blockade is Beneficial
Adapted from Hall JE et al. J Am Soc Nephrol.
199910S258-S265. A Chagnac, et al. Glomerular
hemodynamics in severe obesity. Am J Physiol
2000278F817-F822.
131
ACEIs / ARBs

Clinicians often avoid / withdraw ACEIs / ARBs in
CKD fearing hyperkalemia or ? SCr
Tolerate
up to 30 increases of SCr
K of 5.55.8 mEq/L
Kidney dietitian, not Kayexelate

FF Hou, et al. NEJM, 2006.
132
Alternative to RAAS Blockers

Non-dihydropyridine CCBs for those who cannot
tolerate anti-RAAS agents, especially with
proteinuria
Diltiazem
Verapamil

133
CKD Anti-Proteinuric Therapy

RAAS blockade
ARBs preferred in type 2 diabetic nephropathy
ACEIs preferred in type 1 diabetic nephropathy
Quantitate proteinuria q1-2 mo
Proteinuria reduction maximized by Week 8 of tx
Perform spot urine tests to assess efficacy

From HOPE JFE Mann, et al. J Am Soc Nephrol
2003 14641647.MARVAL. Author. Circulation
2002106672-678. RENAAL. BM Brenner, et al. N
Engl J Med 2001345861869. IDNT. EJ Lewis, et
al. N Engl J Med345851860.
134
RENAAL Combined CCB and ARB Reduce Progression
to Diabetic Nephropathy
NORMAL PGC
Paff
Peff
?RAA
?REA
NORMAL PGC
Paff
Peff
ACEI (type 1 DM) ARB (type 2 DM)
CCB
Adapted from RENAAL Study. BM Brenner, et al. N
Engl J Med. 2001345861869. RAA, afferent
arteriolar resistance. REA, efferent arteriolar
resistance.
135
IRMA 2 ARB Prevents Transition from Micro- to
Macroalbuminuria
H-H Parving, et al. New Engl J Med.
2001345870878.
136
IRMA 2 ARB Prevents Transition from Micro- to
Macroalbuminuria
H-H Parving, et al. New Engl J Med.
2001345870878.
137
IRMA 2 ARB Normalizes Albumin Excretion Rate
P H-H Parving, et al. New Engl J Med. 2001870878.
138
Effect of AngII Receptor Blockade in Type 2
Diabetic Nephropathy
BM Brenner, et al. N Engl J Med 2001345861869.
139
Irbesartan Diabetic Nephropathy Trial
EJ Lewis, et al. N Engl J Med. 2001345851860.
140
Reduction in Endpoints in Non-Insulin Dependent
DM with the Angiotensin II Antagonist Losartan
BM Brenner, et al. N Engl J Med 2001345861869.
141
Diabetes and RAAS BlockadeType 2 DM

Brenner et al. (losartan, RENAAL) (N1513)
Lewis et al. (irbesartan, IDNT) (N1715)
ARBs reduced proteinuria (35)
reduce rate of GFR decline
later onset of ESRD compared to placebo
Mean delay of ESRD by 2.3 yr

142
Lipid Control
143
Guideline Lipids in CKD 14

1.1. All adults and adolescents with CKD should
be evaluated for dyslipidemias. (B)
1.2. For adults and adolescents with CKD, the
assessment of dyslipidemias should include a
complete fasting lipid profile with total
cholesterol, LDL, HDL, and triglycerides. (B)
1.3. For adults and adolescents with Stage 5 CKD,
dyslipidemias should be evaluated upon
presentation (when the pt is stable), at 23 MO
after a change in treatment or other conditions
known to cause dyslipidemias and at least
annually thereafter. (B)

144
Dyslipidemia CKDTreatment Protocol
Lifestyle Modification Always
145
Dyslipidemia CKDTreatment Protocol
Lifestyle Modification Always
146
Treatment of Dyslipidemia Therapeutic Targets

CKD pts are considered the highest CV risk
population
Primary Target LDL-C reduction to
Secondary Target TG reduction to non-HDL-C reduction to
Constant reinforcement of therapeutic lifestyle
changes

147
CKD Dyslipidemia Treatment

Smoking cessation
Aspirin use
Wt loss
Aerobic Exercise
Statins
Fibric Acid Derivatives
LDL Goal 40mg/dL, TG 150mg/dL, Non-HDL-C

K/DOQI Clinical Practice Guidelines for Managing
Dyslipidemias in Chronic Kidney Disease. Am J
Kidney Dis 200341(Suppl 3)S1S91.
148
CKD Lipid Therapy

Rationale for Intervention
CKD progresses faster in dyslipidemia
Physicians Health Study (19821996)
N4,483 initially healthy males
14-Yr followup
Baseline SCr
HDL 40 mg/dL 50 ? risk of reduced GFR
Non-HDL-C 196 mg/dL 100 ? risk of reduced GFR

T Kurth, et al. J Am Soc Nephrol
20031420842091.
149
CKD Lipid Targets
Kidney/Dialysis Outcomes Initiative Clinical
Practice Guidelines for Managing Dyslipidemias in
Chronic Kidney Disease. Am J Kidney Dis
200341(Suppl 3)S1S91.
150
CKD Dyslipidemia Therapy

HMG-CoA synthetase inhibitors
Fibric acid derivatives
Use with caution
Gemfibrozil preferred
Cholesterol absorption inhibitor
Ezitimibe (Zetia) statin-sparing
No controlled trials in CKD

Kidney/Dialysis Outcomes Quality Initiative
Clinical Practice Guidelines for Managing
Dyslipidemias in Chronic Kidney Disease. Am J
Kidney Dis. 200341(Suppl 3)S1S91.
151
Lipid TargetsTotal Cholesterol 200

LDL-C
TG
Non-HDL-C

http//www.kidney.org/PROFESSIONALS/kdoqi/guidelin
es_lipids/ii.htmguide3
152
Anemia of CKD
153
(No Transcript)
154
CKD Anemia Induces LVH
Excerpt H Hampl, L Henning and E Riedel.
Dialysis Times 20039(5)16 A Mohanran and AS
Kliger presentations at NKF Meeting 2003
155
(No Transcript)
156
NKF KDOQI Guideline CPR 2.1 Hb range

Moderately strong recommendation
2.1.1 Lower limit of Hb
In pts with CKD, the Hb should be 11 g/dL
2.1.2 Upper limit of Hb
In the opinion of the Work Group, there is
insufficient evidence to recommend routinely
maintaining Hb levels 13 g/dL in ESA treated
pts.

157
CKD Anemia Therapy

Rationale for Intervention
Anemia worsens with CKD progression
Tx regresses LVH/LVMI
Tx prevents CHF and hospitalization
Tx slows CKD progression?
QOL improved by ? Hb
Cognition
Sexual function
Exercise tolerance

Excerpt H Hampl, et al. Dialysis Times
20039(5)16. Presentations A Mohanran and AS
Kliger. National Kidney Foundation Annual
Meeting, 2003.
158
CKD Anemia ? as GFR ?
Adapted from Radtke, et al. Blood.
197954877884 (original study used Hct).
159
RBC Production Response in CKD
6X
5X
Normal
4X
RBC Production (mL/Day)
3X
CKD
2X
1X
0
0.1
1.0
10
102
103
104
EPO Concentration (mU/mL)
160
EPO Response Blunted as CKD Progresses
Hemoglobin (g/dL)
EPO level (mU/mL)
15
14
13
12
11
10
9
8
7
6
59
29
18
18
34
18
N
5
100-70
70-40
40-25
25-15
15-10
Percent of Normal Kidney Function
Radtke HW. et al Blood 197954877 Erslev AJ. N
Engl J Med 19913241339
161
Anemia A Risk Multiplier
Source Medicare sample (5), followup from 1996
to 1997 of enrollees aged 65 y.o., adjusted for
age, gender and race.
162
QoL Improves with Higher Hb

Cognitive function
Energy/activity
Sleep and eating behavior
Satisfaction with health
Well-being
Satisfaction

Exercise capacity
Functional ability
Health Status
Sex Life
Psychological effect
Happiness

163
How Can We Reach Hb Target?

Efficient erythropoesis requires both iron and
erythropoetin.
Use of maintenance iron improves patients
response to EPO therapy, replaces continuous iron
losses, and maintains patients target Hb/HCT
ranges.
IV iron improves iron and hematologic parameters
with health benefits that outweigh the potential
adverse effects.
Besarab, A.
Clin J Am Soc Nephrol 1S1-S3, 2006

164
IV Iron May Have an Independent Erythropoietic
Effect in HD
39 new HD pts (no EPO therapy) with baseline
iron deficiency by bone marrow aspiration.
P 199879299305.
165
More Rapid Hgb Response With EPO IV Iron
Defined as 0.5-g/dL increase in Hgb. Panesar et
al. Am J Kidney Dis. 200240924-931.
166
Available Oral Iron Preparations
167
Currently Available Erythropoietic Agents

First generation erythropoietic agents
Epoetin alfa (Amgen Epogen , JJ Procrit)
Epoetin beta (Roche)
Epoetin omega (South America)
Epoetin delta (in clinical trials, humanized
using immortalized
Second generation epoetin
Darbepoetin alfa (Amgen, Aranesp)
Other erythropoietic agents in clinical trials
PEG-epoetin beta (CERA Roche)
Hematide (totally synthetic peptide)
Fibrogen product. HIF1-alpha inhibitor

168
CKD Anemia Therapy

Begin tx at Hb
Steps (by Nephrology CKD Clinic)
Replete iron stores
Oral iron salts
Iron dextran (INFeD?) or Iron gluconate
(Ferrlecit?) or Iron sucrose (Venofer?)
Use erythropoietic agent
Epoetin-a (Procrit?) or
Darbepoetin (Aranesp?)

J Yee, A Besarab. Am J Kidney Dis
20024011111121
169
CKD Anemia Therapy

Targets
Hb 11 g/dL (Hct 33)
TSAT 20 Ferritin 100 ng/mL
EPO level
Does not predict marrow response
Two-thirds of levels in normal range
Do not obtain EPO levels
R/O blood loss and/or iron deficiency

A Besarab, J Yee. J Am Soc Nephrol
19991020292043 AR Nissenson. Am J Kidney Dis
20013813901397
170
Chronic Kidney DiseaseMineral and Bone Disorder
171
Position Statement from KDIGO(Kidney Disease
Improving Global Outcomes)

Definition of CKD-MBD
A systemic disorder of mineral and bone
metabolism due to CKD manifested by either one or
a combination of the following
Abnormalities of calcium, phosphorus, PTH, or
vitamin D metabolism
Abnormalities in bone turnover, mineralization,
volume, linear growth, or strength
Vascular or other soft tissue calcification

Definition, evaluation, and classification of
renal osteodystrophy. KI, April 2006
172
Position Statement from KDIGO(Kidney Disease
Improving Global Outcomes)
Definition of Renal Osteodystrophy Renal
osteodystrophy is an alteration of bone
morphology in pts with CKD. It is one measure of
the skeletal component of the systemic disorder
of CKD-MBD that is quantifiable by
histomorphometry of bone biopsy.
Definition, evaluation, and classification of
renal osteodystrophy. KI, April 2006
173
CKD Metabolic Bone Disease

Consequence of ? renal mass
? Vitamin D3
? P
? Ca2
Metabolic acidosis
Increased protein catabolism
Increased bone lysis / loss

Draft Kidney/Dialysis Outcomes Initiative
Clinical Practice Guidelines for Bone Metabolism
and Disease. National Kidney Foundation Task
Force, 2003
174
CKD Metabolic Bone Disease

Definition any / all metabolic bone disorders
associated with CKD
2 hyperparathyroidism
Osteoporosis
Osteomalacia
Adynamic bone disease
Mixtures of above

KA Hruska, SL Teitelbaum. New Engl J Med.
1995333(3)166-174. DJ Sherrard, et al. Kidney
Int. 199343(2)436442.
175
CKD Metabolic Bone Disease

Rationale for Intervention
Multiple aberrations of Ca/P/PTH and bone
metabolism accompany GFR decline.
Hyperphosphatemia is an independent CV risk
factor in ESRD (presumed in non-ESRD CKD).
ESRD pts develop CV calcification (by EBCT) from
? Ca P product.

WG Goodman, et al. New Engl J Med.
2000342(20)14781483.
176
CKD Pathophysiology of 2 HPT
177
Progression of PTH Gland Hyperplasia in CKD
VDR vitamin D receptor CaR Ca-Sensing
receptor. Adapted from Murayama A et al.
Endocrinology. 19991402224-2231. Satomura K et
al. Kidney Int. 198834712716
178
CKD Renal Osteodystrophy Ca / P / PTH Axis
KG Koenig, et al. Kidney Int. 199141161165.
179
CKD ROD PTH Target
150
300
K/DOQI PTHTarget (pg/mL)
100
500
Low bone turnover Adynamic bone disease
High bone turnover Bone pain Cardiovascular
disease Cognitive impairment
180
CKD ROD Ca Target
9.5
8.4
K/DOQI Target Ca(mg/dL)
10.2
7.5
Stimulus for PTH secretion Stimulus for PT
gland enlargement Inadequate skeletal
mineralization
Vascular/soft tissue calcification
Hypertension
181
CKD ROD P Target
Malnutrition Inadequate bone mineralization
Vascular/soft tissue calcification
Cardiovascular disease Higher mortality risk
182
CKD Renal Osteodystrophy

Targets
Ca 8.49.5 mg/dL
P 2.75.5 mg/dL
Ca P
HCO3 2226 mEq/dL
PTH

Draft Kidney/Dialysis Outcomes Initiative
Clinical Practice Guidelines for Bone Metabolism
and Disease. National Kidney Foundation Task
Force, 2003
183
CKD Renal Osteodystrophy ? P ? Relative Risk
of Mortality
GA Block, et al. Am J Kidney Dis 199831607617.
184
Mortality Risk in ESRDby Serum P and Ca Levels
RR relative risk Not adjusted for active
vitamin D intake Block et al. J Am Soc Nephrol.
2004152208-2218.
185
Prevalence of Calcitriol Deficiency and Anemia in
pts With CKD by eGFR

Design
N 80 CDK
Anemia defined as Hb ESA
Calcitriol deficiency defined as calcitriol pg/mL
Results
Prevalence of calcitriol deficiency was greater
than prevalence of anemia at all stages of CKD

Gutierrez et al. J Am Soc Nephrol
2005162205-2215.
186
SHPT Occurs Early in CKD
N150
Martinez et al. NDT 19961122-28.
187
CKD-Mineral Bone DisorderCa/P/PTH Progression
in CKD
P 100 and CrCl 50-59,
N 157
Martinez I, et al. Am J Kidney Dis.
199729496-502.
188
Recommendations for Early Monitoring of PTH, Ca,
and P Metabolism in CKD
GFR in mL/min/1.73 m2 KDOQI Guidelines for Bone
Metabolism and Disease. Am J Kidney Dis.
200342(4 suppl 3)S1-S201.
189
Vitamin D in CKD Stages 3 and 4

Stages 3 and 4 Measure serum 25(OH) D in pts
with ? PTH.If normal, repeat q12 mo.

Normal 25(OH)D ?30 ng/mL Insufficiency

NKF. Am J Kidney Dis. 200342(4 suppl 3)S1-S201.
190
CKD Metabolic Bone Disease Tx

Vascular calcification at any site
Avoid Ca-containing P-binders
Use sevelamer (not confined to ESRD)
Ca 10.2 mg/dL, stop calcitriol
Switch to non-Ca-containing P-binders (sevelamer)
Limit elemental Ca in Ca-based binders to 1500
mg/d or sum of total dietary Ca plus elemental Ca
to 2000 mg/d
P 5.5 mg/dL
Switch to non-Ca-containing P-binders (sevelamer)
Restrict P to 0.81.0 g/d if P 5.5 mg/dL
Restrict P to 0.81.0 g/d if PTH 50 pg/mL

Draft Kidney/Dialysis Outcomes Initiative
Clinical Practice Guidelines for Bone Metabolism
and Disease. National Kidney Foundation Task
Force, 2003
191
High-Turnover Bone Disease Can Result in
Soft-Tissue Calcification
192
Low-Turnover Bone Disease Can Result in
Soft-Tissue Calcification
193
CKD Renal Osteodystrophy Tx

Ca-based P-binders
Ca acetate (Calphron, PhosLo)
667 mg (elemental Ca) 1 capsule tid with meals
Ca carbonate (Tums)
500 mg (elemental Ca) 1 tab tid with meals
Ca-based P-binders in CKD Stages 3 and 4
permitted
Avoid concurrent Ca-based P-binder and iron salt
ingestion
Avoid concurrent Ca-based P-binder and
levothyroxine ingestion

Draft Kidney/Dialysis Outcomes Initiative
Clinical Practice Guidelines for Bone Metabolism
and Disease. National Kidney Foundation Task
Force, 2003
194
CKD Renal Osteodystrophy Tx

Non-Ca-based binders
Avoid aluminum-based gels
Sevelamer hydrochloride (Renagel)
Use in CKD Stages 3 and 4
800 mg capsules 12 tid with meals
Only FDA-approved for ESRD
Alone or with Ca-based P-binders

Draft Kidney/Dialysis Outcomes Initiative
Clinical Practice Guidelines for Bone Metabolism
and Disease. National Kidney Foundation Task
Force, 2003
195
CKD Metabolic Acidosis

The serum bicarbonate reflects the degree or
severity of systemic acidosis. This parameter
should be at 22 meq/L or greater, to offset
acidosis-driven bone lysis.
Bicarbonate therapy
NaHCO3 dose 0.51.0 mEq/kg bw/d
3.87 mEq per 325 mg tablet
7.73 mEq per 650 mg tablet
Usual CKD dose 1300 mg TID

FC Husted, et al. J Clin Invest.
197556(2)414419.
196
Acidosis Aggravates Renal Osteodystrophy
197
Acidosis Treatment

May occur earlier in diabetic CKD, compared to
non-diabetic CKD
Type IV RTA
Treatment same in diabetic and non-diabetic CKD
HCO3 22 mEq/L
NaHCO3 tablets (0.51.0 mEq/kg/day)

Verify acidemia with ABG
198
Nutritional Assessment
199
Nutrition Assessment

Dietician (RD) integral part of CKD
management.Consultation at any CKD stage.
Utilize RD within 2 wk of initial consultation
for dietary assessment and recommendations.
RD will educate pts on food preparation
techniques ? increasing compliance with dietary
restrictions.

200
Rationale for RD consult

Malnutrition evolves during the progression of
CKD
Hypoalbuminemia and vitamin deficiencies are
common
Diet high in biological value must be maintained,
while restricting Na, P, K

201
Food Sources

Na usually all processed foods (hot dogs,
bologna, soups) are high in Na. Be wary of foods
that are labeled low in sodium. The RD will
need to determine how low is low.
K chief sources are fruits and vegetables and
anything that grows below or sits in the ground.
Highly colored fruits (i.e., watermelon), deep
green vegetables, even dried fruits.
P04 all high P foods are also in high K foods,
unless phosphoric acid is added. Found in dairy
products (except butter). Foods prepared with
skim milk (i.e., cake mix, biscuits), nuts, dried
peas, baked beans, legumes and colas.

202
Intervention

Caloric restriction
25 cal/kg of SBW to lose wt
30 cal/kg of SBW to maintain wt
3540 cal/kg of SBW to gain wt
Fluid restriction
implement only if Nacompliant with low Na diet.
may be temporary

203
CKD Nutrition

Rationale for Intervention
amino acid loads induce glomerular
hyperfiltration
protein restriction in small studies retards CKD
progression, but not in largest RCT, MDRD study
obesity (BMI 38 kg/m2) associated with
glomerular hyperfiltration

S Klahr, et al. N Engl J Med 1994330877884. EL
Knight, et al. Ann Intern Med 2003138460467.
204
CKD Nutrition ? Protein Intake Associated with
? Kidney Function

Nurses Health Study (n1135 females) 11-year
followup
Median protein intake, 92.3 g/d
Each 10-g ? in non-dairy protein intake ? CCr by
1.21 mL/min
Highest quintile ? CCr by 4.77 mL/min

S Klahr, et al. for th MDRD Study Group. N Engl J
Med. 1994330877884 EL Knight, et al. Ann
Intern Med 2003138460467.
205
CKD Nutrition Therapy

Consult Renal Dietitian at CKD Stage 3
Protein restrict _at_ GFR
High biologic protein 0.60.75 g/kg bw
Initiate dialysis if
GFR protein intake
6 wt loss or

Kidney/Dialysis Quality Outcomes Initiative
Clinical Practice Guidelines for Managing
Dyslipidemias in Chronic Kidney Disease. Am J
Kidney Dis 200341(Suppl 3)S1S91.
206
Dietary P Restriction to Control SHPT in CKD

Commentary
In summary, the available data and the OPINION
of the Work Group support the proposal that
dietary phosphate restriction should be initiated
when blood PTH levels begin to rise (Stage 2)
and/or when serum phosphorus levels are elevated
at any stage of CKD. p S65
KDOQI Guideline 4. Restriction of Dietary
Phosphorus in pts with CKD
4.1 Dietary phosphorus should be restricted
to8001000 mg/day when the serum phosphorus
levels are elevated (4.6 mg/dL) at CKD Stages 3
and 4 (OPINION p S63)

NKF. Am J Kidney Dis. 200342(4 suppl 3)S1-S201.
207
Vaccinations
208
Vaccinations

CKD pts immunocompromised
Despite immunodeficiency, CKD pt immunized less
frequently against flu and S pneumoniae than
general medical pts

209
Vaccinations Recommendations

Annual influenza A/B
23-valent polysaccharide pneumoccocal (Pneumovax,
PPV23) Q6 years
HBV vax give at any CKD stage. Immunization
series should be completed by stage 4 since
late stage 5 vax induces lower Ab titers

210
Influenza Vax rates Below National Target
(Healthy People 2000)
Gilbertson et al, Kidney Int 2003 63738-743
MMWR 2001, 50532-37
211
Odds of Hospitalization Death are Reduced In
Vaccinated HD pts
_________________ __________________________
Hospitalization Death
Gilbertson et al, Kidney Int 2003 63738-743
212
Evaluate Progression of CKD
213
Strategies to Improve Vascular Access Education
NKF-K/DOQI Guidelines

Education when SCr 3 mg/dl
Vascular access is necessary to access blood
circulation. Refers to fistulas, grafts, and
catheters.

214
Vascular Access

Preserve arm veins suitable for placement of
vascular access, regardless of arm dominance.
Arm veins, especially cephalic veins of the
non-dominant arm, should not be used for
venipuncture or iv catheters.

215
Vascular Access

Dorsum of the hand should be used for iv lines.
When venipuncture of the arm veins is necessary,
sites should be rotated.
Avoid subclavian vein cannulation increases
risk of central vein stenosis

216
DIALYSIS Arteriovenous Fistula