(AKI) Acute Kidney
Injury
Daulat Tampubolon, MD
Koja Hospital
�Definition of AKI
There are more than 35 definitions of AKI
(formerly acute renal failure) in literature!
Diagnostic criteria for AKI includes an
abrupt (within 48 hours) reduction in kidney
function defined as an absolute increase in
serum creatinine of either 0.3 mg/dl or more
(>/= 26.4 umol/L) or a percentage increase
of 50% or more (1.5 fold from baseline) or a
reduction in urine output.
�Definition of Acute Kidney Injury (AKI)
based on Acute Kidney Injury
Network
Stage
Increase in Serum
Creatinine
Urine Output
1.5-2 times baseline
OR
0.3 mg/dl increase
from baseline
<0.5 ml/kg/h for >6 h
2-3 times baseline
<0.5 ml/kg/h for >12
h
3 times baseline
OR
0.5 mg/dl increase if
baseline>4mg/dl
OR
Any RRT given
<0.3 ml/kg/h for >24
h
OR
Anuria for >12 h
�RIFLE criteria for diagnosis of AKI
based on The Acute Dialysis Quality
Initiative
Increase in S
Urine output
Cr
Risk of renal injury
0.3 mg/dl increase
< 0.5 ml/kg/hr for > 6 h
Injury to the kidney
2 X baseline
< 0.5 ml/kg/hr for >12h
Failure of kidney
function
3 X baseline OR
Anuria for >12 h
> 0.5 mg/dl increase if
SCr >=4 mg/dl
Loss of kidney
function
End-stage disease
Persistent renal failure
for > 4 weeks
Persistent renal failure
for > 3 months
Am J Kidney Dis. 2005 Dec;46(6):1038-48
�Epidemiology
AKI occurs in
7% of hospitalized patients.
36 67% of critically ill patients
(depending on the definition).
5-6% of ICU patients with AKI require
RRT.
Nash K, Hafeez A, Hou S: Hospital-acquired renal insufficiency. American Journal of
Kidney Diseases 2002; 39:930-936.
Hoste E, Clermont G, Kersten A, et al.: RIFLE criteria for acute kidney injury are
associated with hospital mortality in critically ill patients: A cohort analysis. Critical Care 2006;
10:R73.
Osterman M, Chang R: Acute Kidney Injury in the Intensive Care Unit according to
RIFLE. Critical Care Medicine 2007; 35:1837-1843.
�Mortality according to RIFLE
Mortality
increases proportionately with
increasing severity of AKI (using RIFLE).
AKI requiring RRT is an independent risk factor
for in-hospital mortality.
Mortality in pts with AKI requiring RRT 50-70%.
Even small changes in serum creatinine are
associated with increased mortality.
Hoste E, Clermont G, Kersten A, et al.: RIFLE criteria for acute kidney injury are associated with hospital mortality
in critically ill patients: A cohort analysis. Critical Care 2006; 10:R73.
Chertow G, Levy E, Hammermeister K, et al.: Independent association between acute renal failure and mortality
following cardiac surgery. American Journal of Medicine 1998; 104:343-348.
Uchino S, Kellum J, Bellomo R, et al.: Acute renal failure in critically ill patients: A multinational, multicenter study.
JAMA 2005; 294:813-818.
Coca S, Peixoto A, Garg A, et al.: The prognostic importance of a small acute decrement in kidney function in
hospitalized patients: a systematic review and meta-analysis. American Journal of Kidney Diseases 2007; 50:712-720.
�Increase in Creatinine without
AKI
Inhibition of tubular creatinine
secretion
Trimethoprim, Cimetidine, Probenecid
Interference with creatinine assays in
the lab (false elevation)
acetoacetate, ascorbic acid, cefoxitin
flucytosine
�Increase in BUN without AKI
Increased production
GI Bleeding
Catabolic states (Prolonged ICU stay)
Corticosteroids
Protein loads (TPN-Albumin infusion)
�New Biomarkers in AKI
Alternatives to Serum Creatinine
Urinary Neutrophil Gelatinase-Associated
Lipocalin (NGAL)
Ann Intern Med 2008;148:810-819
Urinary Interleukin 18
Am J Kidney Dis 2004;43:405-414
Urinary Kidney Injury Molecule 1 (KIM-1)
J Am Soc Nephrol 2007;18:904-912
NGAL:
Expressed in proximal and distal nephron
Binds and transports iron-carrying molecules
Role in injury and repair
Rises very early (hours) after injury in animals, confirmed in children having CPB
IL-18:
Role in inflammation, activating macrophages and mediates ischemic renal injury
IL-18 antiserum to animals protects against ischemic AKI
Studied in several human models
KIM-1:
Epithelial transmembrane protein, ?cell-cell interaction.
Appears to have strong relationship with severity of renal injury
�Urine analysis
Unremarkable in pre and post renal causes
Differentiates ATN vs. AIN. vs. AGN
Muddy brown casts in ATN
WBC casts in AIN
RBC casts in AGN
��Major Disease Categories
Causing AKI
Disease Category
Prerenal azotemia caused by acute renal
hypoperfusion
Incidence
Intrinsic renal azotemia caused by acute
diseases of renal parenchyma:
35-40%
-Large renal vessels dis.
-Small renal vessels and glomerular dis.
-ATN (ischemic and toxic)
-Tubulo-interestitial dis.
-Intratubular obstruccttion
Postrenal azotemia caused by acute
obstruction of the urinary tract
55-60%
*>90%*
<5%
�Prerenal Azotemia
Intravascular volume depletion
bleeding, GI loss, Renal loss, Skin loss, Third space loss
Decreased cardiac output
CHF
Renal vasoconstriction
Liver Disease, Sepsis, Hypercalcemia
Pharmacologic impairment of
autoregulation and GFR in specific
settings
ACEi in bilateral RAS, NSAIDS in any renal
hypoperfusion setting
�Intrinsic Renal Azotemia
Large Renal Vessel Disease
Thrombo-embolic disease
Renal Microvasculature and Glomerular Disease
Inflammatory: glomerulonephritis, allograft rejection
Vasospastic: malignant hypertension, scleroderma crisis, pre-eclampsia,
contrast
Hematologic: HUS-TTP, DIC
Acute Tubular Necrosis (ATN)
Ischemic
Toxic
Tubulo-interestitial Disease
Acute Interestitial Nephritis (AIN), Acute cellular allograft rejection, viral
(HIV, BK virus), infiltration (sarcoid)
Intratubular Obstruction
myoglobin, hemoglobin, myeloma light chains, uric acid, tumor lysis,
drugs (indinavir, acyclovir, foscarnet, oxalate in ethylene glycol toxicity)
�Postrenal azotemia
Stones
Blood clots
Papillary necrotic tissue
Urethral disease
anatomic: posterior valve
functional: anticholinergics, L-DOPA
Prostate disease
Bladder disease
anatomic: cancer, schistosomiasis
functional: neurogenic bladder
�Initial diagnostic tools in
AKI
History and Physical exam
Detailed review of the chart, drugs administered,
procedures done, hemodynamics during the procedures.
Urinalysis
SG, PH, protein, blood, crystals, infection
Urine microscopy
casts, cells (eosinophils)
Urine lytes
Renal imaging
US, Mag-3 scan, Retrograde Pyelogram
Markers of CKD
iPTH, size<9cm, anemia, high phosphate, low bicarb
Renal biopsy
�5 Key Steps in Evaluating Acute Kidney Injury
1)
2)
3)
4)
5)
Obtain a thorough history and physical; review the
chart in detail
Do everything you can to accurately assess volume
status
Always order a renal ultrasound
Look at the urine
Review urinary indices
�Prevention of AKI in ICU
Recognition of underlying risk factors
Diabetes
CKD
Age
HTN
Cardiac/liver dysfunction
Maintenance of renal perfusion
Avoidance of hyperglycemia
Avoidance of nephrotoxins
Dennen P, Douglas I, Anderson R,: Acute Kidney Injury in the Intensive Care Unit: An update and primer for the
Intensivist. Critical Care Medicine 2010; 38:261-275.
Antibiotics
Aminoglycosides (10-15% Incidence of Acute Tubular Necrosis)
Occurs in 10-20% patients on 7 day course
Results in non-oligurics; increased Creatinine
A single dose early in septic course is usually safe
Sulfonamides
Amphotericin B (Incidence 80-90%)
Levofloxacin
Ciprofloxacin
Rifampin
Tetracycline
Acyclovir (only nephrotoxic in intravenous form)
Pentamidine
Chemotherapy and Immunosuppressants
Cisplatin
Methotrexate
Mitomycin
Cyclosporine
Heavy Metals
Mercury Poisoning
Lead Poisoning
Arsenic Poisoning
Bismuth
Lithium related kidney disorders
Polydipsia and Nephrogenic Diabetes Insipidus
Acute Renal Failure
Dialysis indications: Creatinine >2.5 or Seizures, ALOC, Rhabdomyolysis
Chronic kidney disease with fibrosis
AntiHyperlipidemics
Statins
Gemfibrozil
Associated with Acute Renal Failure due to Rhabdomyolysis
Fenofibrate (Tricor)
�Prevention of Contrast-Induced
Nephropathy
Avoid use of intravenous contrast in high
risk patients if at all possible.
Use pre-procedure volume expansion using
isotonic saline (?bicarbonate).
NAC
Avoid concomitant use of nephrotoxic
medications if possible.
Use low volume low- or iso-osmolar contrast
Dennen P, Douglas I, Anderson R,: Acute Kidney Injury in the Intensive Care Unit: An update and primer for the
Intensivist. Critical Care Medicine 2010; 38:261-275.
�Prevention of AKI in hepatic
dysfunction
Intravenous
albumin significantly reduces the
incidence of AKI and mortality in patients with
cirrhosis.
Albumin decreases the incidence of AKI after
large volume paracentesis.
Albumin and terlipressin decrease mortality in
HRS.
Sort P, Navasa M, Arroyo V, et al.: Effect of intravenous albumin on renal impairment and mortality in patients with
cirrhosis and spontaneous bacterial peritonitis. New England Journal of Medicine 1999; 341:403-409.
Gines P, Tito L, Arroyo V, et al.: Randomised comparative study of therapeutic paracentesis with and without
intravenous albumin in cirrhosis. Gastroenterology 1988; 94:1493-1502.
Gluud L, Kjaer M, Christensen E: Terlipressin for hepatorenal syndrome. Cochrane Database Systematic Reviews
2006; CD005162.
�Management of AKI in ICU
Treatment
is largely supportive in nature
Maintain renal perfusion
Correct metabolic derangements
Provide adequate nutrition
? Role of diuretics
Renal Replacement therapy remains the
cornerstone of management of minority of
patients with severe AKI
�Maintaining renal
perfusion
Human kidney has a compromised ability to
autoregulate in AKI.
Maintaining haemodynamic stability and
avoiding volume depletion are a priority in
AKI.
Kelleher S, Robinette J, Conger J: Sympathetic nervous system in the loss of autoregulation in
acute renal failure. American Journal of Physiology 1984; 246: F379-386.
�Maintaining renal
perfusion
The individual BP target depends on age,
co-morbidities (HTN) and the current acute
illness.
A generally accepted target remains MAP
65.
Bourgoin A, Leone M, Delmas A, et al.: Increasing mean arterial pressure in patients with septic shock: Effects on
oxygen variables and renal function. Critical Care Medicine 2005; 33:780-786
�Volume resuscitation which
fluid?
no statistical difference between volume
resuscitation with saline or albumin in
survival rates or need for RRT.
Finfer S, Bellomo R, Boyce N, et al.: A comparison of albumin and saline for fluid resuscitation in the intensive
care unit. New England Journal of Medicine 2004; 350: 2247-2256.
�Volume resuscitation how
much fluid?
Fluid
conservative therapy decreased
ventilator days and didnt increase the need
for RRT in ARDS patients.
Association between positive fluid balance
and increased mortality in AKI patients.
Wiedeman H, Wheeler A, Bernard G, et al.: Comparison of two fluid management strategies in acute lung
injury. New England Journal of Medicine 2006; 354:2564-2575.
Payen D, de Pont A, Sakr Y, et al.; A positive fluid balance is associated with worse outcome in patients with
acute renal failure. Critical Care 2008; 12: R74
�Which
inotrope/vasopressor?
There is no evidence that from a renal
protection standpoint, there is a
vasopressor agent of choice to improve
kidney outcome.
Dennen P, Douglas I, Anderson R,: Acute Kidney Injury in the Intensive Care Unit: An update and primer for the
Intensivist. Critical Care Medicine 2010; 38:261-275.
�Renal vasodilators?
renal
dose dopamine (<5 g/kg of body weight/min)
increases RBF and, to a lesser extent, GFR.
Dopamine is unable to prevent or alter the course of
ischaemic
or
nephrotoxic
AKI].
Furthermore,
dopamine, even at low doses, can induce tachyarrhythmias,
myocardial
ischaemia,
and
extravasation out of the vein can cause severe
necrosis .Thus, the routine administration of
dopamine to patients for the prevention of AKI or
incipient AKI is no longer justified.
Lauschke A, Teichgraber U, Frei U, et al.: Low-dose dopamine worsens renal perfusion in patients with acute renal failure. Kidney
2006; 69:1669-1674.
Argalious M, Motta P, Khandwala F, et al.: Renal dose dopamine is associated with the risk of new onset atrial fibrillation after cardiac
surgery. Critical Care Medicine 2005; 33:1327-1332.
�Role of ANP analogues in AKI?
61 patients in 2 cardiothoracic ICU with post-op
AKI assigned to receive recombinent ANP
(50ng/kg/min) or placebo
The need for RRT before day 21 after
development of AKI was significantly lower in ANP
group (21% vs 47%)
The need for RRT or death after day 21 was
significantly lower in ANP group (28% vs 57%)
Crit Care Med. 2004 Jun;32(6):1310-5
�Is there a role for Fenoldopam in
prevention or treatment of AKI in ICU
setting?
Dopamine-1 receptor agonist, lack of Dopamine-2, and
alpha-1 receptor effect, make it a potentially safer drug
than Dopamine!
Reduces in hospital mortality and the need for RRT in AKI
Reverses renal hypoperfusion more effectively than
renal dose Dopamine
So far so good specially in cardiothoracic ICU patients,
awaiting more powered trials in other groups!
J Cardiothorac Vasc Anesth. 2008 Feb;22(1):23-6.
J Cardiothorac Vasc Anesth. 2007 Dec;21(6):847-50
Am J Kidney Dis. 2007 Jan;40(1):56-68
Crit Care Med. 2006 Mar;34(3):707-14
�Is there a role for diuretics in the
treatment of AKI in ICU setting?
Loop diuretics may convert an oliguric into a nonoliguric form of AKI that may allow easier fluid
and/or nutritional support of the patient. Volume
overload in AKI patients is common and diuretics
may provide symptomatic benefit in that
situation. However, loop diuretics are neither
associated with improved survival, nor with better
recovery of renal function in AKI.
JAMA. 2002 Nov 27;288(20):2547-53
Crit Care Resusc. 2007 Mar;9(1):60-8
�NAC
The most recent trials seem to confirm a
potential positive preventive effect of Nacetylcysteine (NAC), particularly in
contrast-induced nephropathy (CIN), NAC
alone should never take the place of IV
hydration in patients at risk for CIN; fluids
likely have a more substantiated benefit. (150
mg/kg in 500 mL saline (0.9%)] over 30 min immediately before contrast
exposure and followed by 50 mg/kg in 500 mL saline (0.9%) over the
subsequent 4 h )
�EPO
Erythropoietin (EPO) has tissue-protective
effects and prevents tissue damage during
ischaemia and inflammation, and currently
trials are performed with EPO in the
prevention of AKI post-cardiac surgery, CIN
and post-kidney transplantation.
�Case 1
26 yo F is involved in a MVA, with multiple
fractures, blunt chest and abdominal trauma. She
was briefly hypotensive on arrival to ED, received
6L NS and normalized BP. Non contrast CT
showed small retroperitoneal hematoma. On
day#2 her SCr is 0.9 mg/dl, lipase is elevated and
tense abdominal distension is noted. US showed
massive ascites. UOP drops to <20 cc/hr despite
of 10 L total IV intake. On day#3, SCr is 2.1mg/dl,
CVP is 17, UNa is 10 meq/L, with a bland
sediment.
What is the cause of her AKI?
What bedside diagnostic test and therapeutic
intervention is indicated?
Bladder pressure was 29 mmHg
UOP and SCr improved with emergent
paracenthesis.
Dx: Abdominal Compartment Syndrome
causing decreased renal perfusion from
increased renal vein pressure.
�Case 2
59 yo M, s/p liver transplant in 2001 and acute on chronic
rejection, now decompensated ESLD, is admitted with
worsening ascites, hepatic encephalopathy and GI bleed
(which is now controlled). The only medications he has
been receiving are Lactulose and omeprazole. He has been
hemodynamically stable with average BP~100/70
mmHg.He had a 3.5 L paracenthesis on day 2. His SCr has
been slowly rising from 1.2 to 4.7 mg/dl within the 2nd to
4th day of admission and his UOP has dropped to 150
cc/day. His daily FeNa is <1% despite of 2 L fluid challenge.
His Urine sediment is blend. His renal US is normal.
What is the cause of his AKI?
� Patient
required HD.
He
had a second liver transplant
and came off HD after the
surgery with stable SCr of 1.4
mg/dl.
Dx:
Hepatorenal Syndrome
(HRS)
�Hepatorenal Syndrome
Major diagnostic criteria:
No improvement with at least 1.5 L fluid challenge
SCr >1.5 mg/dl or GFR< 40 cc/min
Absence of proteinuria (<500 mg/d)
Other causes are rouled out (obstruction, ATN, etc.)
Minor diagnostic criteria:
Urine volume < 400 cc/day
UNa < 10 meq/L
SNa < 130 meq/L
Urine RBC < 50/hpf
�Case 3
45 yo M with CHF and Bipolar Disorder on
Lithium for 10 years, admitted for
abdominal pain after a heavy meal, which
turned out to be due to acute
cholecyctitis. He was kept NPO on D5
1/2NS 50 cc/hr. Next morning he felt well
but thirsty and hungry, BP=120/80,
I/O=1200/4500. His SCr rose from 1.2 to
1.9 mg/dl. SNa 149 meq/L. UNa 10 meq/L.
UOsm 190 mOsm/Kg.
What is the cause of his AKI?
Patients IVF was changed to NS, replacing
80% of UOP per hour. SCr and SNa
improved to baseline in 2 days.
Dx: Prerenal azotemia secondary to
renal free water loss in DI.
�Case 4
54 yo F with CAD, on statin, started a new
exercise program with intense weight
training. She was brought to ED with neck
pain, and LE weakness. VS stable, normal
UOP, with dry mucosa. LE muscle strength
2/5 bilaterally. BUN 40 mg/dl, creatinine=8
mg/dl. FeNa 1.5%. Renal US normal. UA:
1.010, 3+ blood, few RBCs, few granular
casts.
What would be the next test to order?
What may be the cause of her AKI?
�Her CPK=57,700
She was treated with IV NaHCO3 to
alkalinize urine to PH>6.5 .
Her UOP remained normal but she
required HD for uremia.
Dx: ATN due to Rhabdomyolysis
�Case 5
72 yo M with DM, and prostate cancer metastatic to the
bone, s/p radiotherapy, on hormonal therapy. He is
admitted with weakness, progressive weight loss, and
persistent nausea. His med list also includes Diclofenac
sodium daily for hip pain. BP=150/90, 350cc of urine
collection immediately after foley placement, and
normal exam. BUN=107 mg/dl, creatinine=9.8 mg/dl
(2.0 almost for 6 months), which remained unchanged
with hydration. Uric acid=8.2 mg/dl. UA: 1.010, 1+
protein, 1+ blood, few RBCs, no cast, no WBC. US
showed 10-11 cm kidneys, no hydronephrosis.
What seems to be the cause for his AKI?
�Patient was initiated on HD for uremia and
remained HD dependent for his
symptomatic uremia.
Patient and his family were concerned
about his renal recovery (outcome), so a
renal Bx was done showing severe chronic
interstitial nephritis, with fibrosis and
glomerulosclerosis.
Dx: ESRD due to chronic tubulointerstitial disease secondary to
NSAIDs
�Case 6
38 yo M with post ERCP pancreatitis, is admitted to ICU,
intubated for hypoxic respiratory distress, is anuric, febrile,
and hypotensive, requiring massive volume resuscitation,
on two vasopressors. He has received 11 L of NS and other
IV meds within the last 8 hours and currently his CVP~12,
has coarse crackles, and 2+ edema. His Creatinine rose
from 1.2 to 3.5 the morning after the above event, FeNa >
1%, UNa 45 meq/L, UA: 1.010, no protein, no blood,
moderate epithelial cells, many muddy brown granular cell
casts, moderate epithelial cell casts. US showed normal
sized kidneys with no hydronephrosis.
What is the cause of his AKI?
He was started on CVVH (continuous
venovenous hemofiltration )for volume
control. Has had a long hospital stay
complicated with polymicrobial bacteremia
and VAP (Ventilator-associated
pneumonia).
Dx: ATN secondary to renal ischemia
and sepsis
�Natural Clinical Course of ATN
Initiation Phase (hours to days)
Continuous ischemic or toxic insult
Evolving renal injury
ATN is potentially preventable at this time
Maintenance Phase (typically 1-2 wks)
Maybe prolonged to 1-12 months
Established renal injury
GFR < 10 cc/min, The lowest UOP
Recovery Phase
Gradual increase in UOP toward post-ATN diuresis
Gradual fall in SCr (may lag behind the onset of
diuresis by several days)
�Thank you!
