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GRIST 1
EXTRACORPOREAL
CARDIOPULMONARY
RESUSCITATION
(ECPR)
THE MISSOURI PERFUSION SOCIETY 23rd Annual Scientific Meeting Embassy Suites Country Club Plaza
Kansas City, Missouri June 1 & 2, 2018
Gary Grist RN CCP Emeritus
No disclosures
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OBJECTIVES
◼ Describe the mechanisms of reperfusion injury and its relationship to shock and CPR patients.
◼ Explain the strategy to revive cardiac arrest patients with the heart/lung pump who are not responsive to CPR resuscitation.
GRIST 3GRIST 3
OXYGEN TOXICITY VS. REPERFUSION INJURY
◼ AOX = antioxidants
◼ ROS = reactive oxygen species
AOX active but too much O2
AOX inactive O2 low or normal
GRIST 4
ANTIOXIDANTS
◼ Catalase, Superoxide dismutase, Glutathione peroxidase, Glutathione, Vitamin C, Vitamin E, Beta carotene, Coenzyme Q10, etc.
◼ Protect against the damaging effects of oxygen
◼ pH sensitive: > 7.20
◼ Depleted antioxidants thought to contribute to aging
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GRIST 8
GRIST 9
GRIST 10
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COMPLICATIONS OF ECMO
➢ Brain damage➢ encephalopathy➢ coma➢ seizure➢ infarct➢ hemorrhage
➢ Cardiac failure➢ arrhythmia➢ ventricular failure➢ cardiac stun➢ stone heart➢ elevated cardiac enzymes
➢ Multiple organ failure➢ renal failure➢ pulmonary infiltrates/hemorrhage➢ elevated liver enzymes➢ elevated glucose➢ gut ulcer/slough➢ coagulopathy
➢ Systemic inflamatory response➢ Failure to improve
SYMPTOMS OF REPERFUSION INJURY
➢ Brain damage➢ encephalopathy➢ coma➢ seizure➢ infarct➢ hemorrhage
➢ Cardiac failure➢ arrhythmia➢ ventricular failure➢ cardiac stun➢ stone heart➢ elevated cardiac enzymes
➢ Multiple organ failure➢ renal failure➢ pulmonary infiltrates/hemorrhage➢ elevated liver enzymes➢ elevated glucose➢ gut ulcer/slough➢ coagulopathy
➢ Systemic inflamatory response➢ Failure to improve
GRIST 12
FOUR MECHANISMS OF REPERFUSION INJURY
◼ Oxidative stress √
◼ Calcium Stress √
◼ Neutrophil-Endothelium Interaction
◼ Apoptosis
GRIST 13
OXYGEN STRESS:MYOCYTE CELL DEATH BY ISCHEMIC ANOXIA &
SUBSEQUENT REPERFUSION
Becker LB, New concepts in reactive oxygen species and cardiovascular reperfusion physiology. Cardiovascular Research 61 (2004);461-470
GRIST 14GRIST 14
CALCIUM STRESS:EXCITABLE CELLS: CARDIAC MYOCYTES AND NEURONS
◼ Intracellular [iCa+2] = __1__ Extracellular [iCa+2] 10,000
◼ Upon reperfusion, influxing calcium causes a ‘mitochondrial permeability transition pore’ (MPTP)
◼ Cardiac injury• Arrhythmia• Cardiac Stun• Stone Heart• Fibrillation feedback phenomenon
◼ Increasing Joules needed for defibrillation
◼ Central nervous system injury• Hemorrhage• Infarction
◼ ECMO w/ right neck cannulation• Left side infarcts 61%
◼ exposed to immediate reperfusion from the ECMO pump
• Right side infarcts 11%◼ protected from immediate
reperfusion by R carotid ligation• Bilateral infarcts 28%
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NEUTROPHIL-ENDOTHELIUM INTERACTION
◼ Neutrophils activated by ischemia release cytotoxic granules and ROS, damaging capillaries.
◼ Damaged capillaries become a blood flow “obstacle course”.
◼ No reflow phenomenon caused by cellular aggregation in the damaged capillaries. Mura et al. Critical Care 2006 10:R130
http://www.benbest.com/cryonics/ischemia.html#reperfuse
Normal mouse lung Mouse lung after gastric ischemic/hypoxia reperfusion
http://www.thoracic.org/sections/clinical-information/critical-care/critical-care-research/animal-
models-of-acute-lung-injury.html
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ACCELERATED APOPTOSIS CAUSED BY REPERFUSION INJURY
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REPERFUSION INJURY POTENTIAL (RIP)Acronym for “Rest In Peace”
◼ RIP: the hidden risk of a lethal reperfusion injuryupon sudden reperfusion of ischemic tissues.
◼ Shock: inadequate blood flow = poor tissue oxygenation & CO2 removal
• Cardiogenic• Septic• Traumatic• Hypovolemic septic• Neurogenic
◼ Shock: a state of insufficient perfusion that holds the potential for reperfusion injury if normothermic oxygenation is suddenly restored.
◼ RIP markers to assess degree of shock:• Tissue anoxia = anion gap• Tissue CO2 retention = p[v-a]CO2
A cause of acute organ failure in transplants.
GRIST 18
FIRST ANION GAP IN PICU AFTER CPB: CORRELATION TO SURVIVAL
0
10
20
30
40
50
60
AG < 15mEq/L
AG 15-19mEq/L
AG 20-24mEq/L
AG =/> 25mEq/L
% Mortality
CMH survival to discharge vs. 1ST anion gap after CPB, p < 0.05
GRIST 19
VENOARTERIAL CO2 GRADIENTON ECMO VS. SURVIVAL
Lamia B, Minerva Anestesiol 2006
* CMH survival to discharge vs. average CO2 gradient on ECMO: n = 454, p < 0.05
~60% MORTALITY*
~30% MORTALITY*
~15% MORTALITY*
~100% MORTALITY*
GRIST 20
THE CO2 GRADIENT AND CORRECTED ANION GAP: MORTALITY IN CARDIAC AND RESPIRATORY
ECMO PATIENTS
0
10
20
30
40
50
60
70
80
90
100
< 15 15-19 20-24 >24
% CO2 GRADIENT MORTALITY
% AG MORTALITY
n = 360, p < 0.05
GRIST 21
244 RESPIRATORY & CARDIAC PATIENTS INSIDE THE LANE
SURVIVORS (n = 193, 95%) AND EXPIRED (n = 51, 63%)
0
5
10
15
20
25
30
35
40
0 5 10 15 20 25 30 35 40
1ST CO2 GRADIENT
1S
T C
OR
RE
CT
ED
AN
ION
GA
P
40 RESPIRATORY & CARDIAC PATIENTS OUTSIDE THE LANE
SURVIVORS (n = 10, 5%) AND EXPIRED (n = 30, 37%)
0
5
10
15
20
25
30
35
40
0 5 10 15 20 25 30 35 40
1ST CO2 GRADIENT1S
T C
OR
RE
CT
ED
AN
ION
GA
P
GRIST 21
REPERFUSION INJURY POTENTIAL (RIP) MAPPING:
BLOOD PRIMED, NORMOTHERIC ECMO PATIENTS(N = 284)
PATIENTS OUT
OF THE LANE
-
10
20
30
40
50
60
70
80
90
100
SURVIVED EXPIRED
PE
R C
EN
TA
GE
PATIENTS IN
THE LANE
-
10
20
30
40
50
60
70
80
90
100
SURVIVED EXPIRED
PE
R C
EN
TA
GE
GRIST 22GRIST 22
ECMO VS ECPRFOR ARREST PATIENTS
www.aic.cuhk.edu.hk/web8/toc.htm
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TERMINATING CPR◼ 1959
• Dr. Safar starts CPR
• 10 minute limit
◼ 1989• 30 years since CPR started
• Still a 10 minute limit
◼ 2005 AHA Guidelines for CPR• 46 years since CPR started
• No change in 10 minute limit◼ “For the newborn infant,
discontinuation of resuscitation can be justified after 10 minutes without signs of life despite continuous and adequate resuscitative efforts.”
◼ 2008 Current PALS Recommendation• 49 years since CPR started
• 15-30 minute limit◼ Discontinue CPR efforts after 15
minutes for newborn in delivery room. All others, discontinue CPR efforts after 30 minutes.
www.castorcanada.com/chainofsurvival.htm
GRIST 24GRIST 24
IN-HOUSE PICU WITNESSED ARREST:DURATION OF CPR
*Morris et al. 2004 @ CHOP
GRIST 25GRIST 25
◼ How do we know that brain damage occurs after 10 minutes of cardiac arrest?• Answer: Because a few patients are revived after lengthy
CPR and have obvious brain damage.◼ Limits of resuscitation. I. Thanatophysiologic and therapeutic limits. Z
Gesamte Inn Med. 1981 May 15;36(10):305-10.
◼ Why should efforts cease after 30 minutes of CPR?• Answer: The current concept is that during CPR, poor blood
flow kills the brain cells. CNS survival after 30 minutes is unlikely.◼ AHA Circulation, 2005. 112(24 Suppl): p. IV1-203.◼ AHA Pediatrics, 2006. 117(5): p. e989-1004.
◼ New Concept: During CPR, brain cells do not die until the ROSC (or starting ECMO). Sudden tissue reperfusion with warm, oxygenated blood causes reperfusion injury that kills the brain.
• Idris AH et al. Crit Care Med 2005; 33(9):2043-8.• Becker, L.B.,Cardiovasc Res, 2004. 61(3): p. 461-70.
GRIST 26
REPERFUSION INJURY POTENTIAL MAP
0
5
10
15
20
25
30
35
40
0 5 10 15 20 25 30 35 40
1ST CO2 GRADIENT
1S
T C
OR
RE
CT
ED
AN
ION
GA
P
GRIST 26
RIP MAPPING THE CPR PATIENT
Blood gas values taken from CLINICAL APPLICATION OF BLOOD GASES, FOURTH ED. © 1989, SHAPIRO, HARRISON,
CASE & KOZLOWSKI-TEMPLIN, EDs., PP 337-338
BLOOD GAS TYPE
pH / pCO2 / pO2 / base
ABG 7.37 / 42 / 80 / -1
VBG 7.33 / 50 / 32 / -1
ABG 7.52 / 28 / 436 / -1
VBG 7.31 / 58 / 25 / -2
ABG 7.27 / 48 / 430 / -6
VBG 7.09 / 84 / 25 / -6
CPR 35 min 100% ABG 7.11 / 38 / 322 / -19
VBG 6.82 / 96 / 20 / -20
30%
CPR 5 min 100%
58
TIME FiO2 ∆ pCO2
CPR 15 min 100%
8
30
36
60 min prior
to arrest.
GRIST 27GRIST 27
ECMO VS ECPR
1. ECMO strategy:
maintain normal physiology
◼ Urgent
• Patient not coding
◼ Normothermia
◼ Blood Primed
• No hemodilution
◼ Normalized iCa+2
2. ECPR strategy:
thwart a lethal
physiology
◼ Emergent
• Patient coding
◼ Hypothermia
◼ Clear prime
• Intentional hemodilution
◼ Reduce iCa+2
GRIST 28GRIST 28
REPERFUSION STRATEGY
COMBATING RIP WITH ECPR:A TWO STEP PROCESS
1. STOP THE DYING (PREVENT REPERFUSION INJURY)
◼ Hypothermia
◼ Hemodilution
◼ Hypocalcemia
2. BRING BACK TO LIFE(REVERSE THE RIP)
◼ Normalize venous pCO2
◼ Normalize venous pH
◼ Normalize hematocrit
◼ Normalize calcium
◼ Rewarm
◼ Continue support
GRIST 29
HYPOTHERMIA PREVENTS REPERFUSION INJURY
◼ “Destructive processes following ischemia/reperfusion can be prevented or significantly mitigated by hypothermia” KH Polderman, Crit Care Med 2009 37:7(Suppl), S188
• VU University Medical Center is the university hospital affiliated with the Vrije Universiteit (literally: Free University) of Amsterdam, The Netherlands
◼ Protective effects of mild to moderate hypothermia
• Mitochondrial injury & dysfunction
• Cerebral metabolism
• Influx of calcium
• Cell membrane leakage
• Cell edema
• Intracellular acidosis
• Production of ROS
GRIST 30
◼ CPR + induced hypothermia is not a new idea
◼ 1964 Safar CPR poster
◼ Delaying hypothermia during CPR has deleterious effects
◼ Circulation, 2006. 113(23): p. 2690-6.
GRIST 31
CPR COOLING VS. ECPR COOLING
◼ CPR COOLING
• Blood flow ~ 40%
• Cooling protects against ‘too little’ O2 deliverycausing tissue anoxia
• Depth of cooling limited to >32C due to cardiac inhibition upon ROSC
◼ ECPR COOLING
• Blood flow ~ 100%
• Cooling protects against ‘too much’ O2 deliverycausing reperfusion injury
• Depth of cooling not limited by the need for cardiac recovery
GRIST 32GRIST 32
ECPR COOLING
◼ Cool ‘perfusate’ rapidly removes CO2 from tissues
◼ CO2 is more soluble at temperatures below 37C
◼ Metabolic rate reduced by hypothermia◼ CO2 production reduced
◼ O2 need reduced
◼ Neutrophil inflammatory response reduced
◼ Apoptosis slowed
GRIST 33GRIST 33
HEMODILUTION: ECPR CLEAR PRIME
◼ Hemodilution reduces oxygen delivery to tissues.
◼ Allows high blood flow without excessive O2 delivery to facilitate CO2 removal.
◼ Counters ‘no reflow’ phenomenon by making blood ‘thinner’.
◼ http://www.thoracic.org/sections/clinical-information/critical-care/critical-care-research/animal-models-of-acute-lung-injury.html
Normal mouse lungMouse lung after gastric ischemic/hypoxia reperfusion
www.benbest.com/cryonics/ischemia.html
GRIST 34GRIST 34
HYPOCALCEMIA: ECPR CALCIUM FREE PRIME
◼ Calcium free prime reduces intracellular migration to combat cardiac & CNS damage.
◼ Calcium stress is more lethal than oxygen stress.
Wang et al. Journal of Cerebral Blood Flow & Metabolism (2002) 22, 206–214; doi:10.1097/00004647-200202000-00008
Neuronal Cell Culture:
Survival After 12 Hours Oxygen-Glucose Deprivation
Dantrolene blocks ryanodine receptor sites which prevents intracellular Ca+2 fluxes and stops the formation of the MPTP.
Dantrolene reduces neuronal cell death from hypoxic/ischemia.
Muehlschlegel S, Sims JR. Dantrolene: mechanisms of neuroprotection and possible clinical applications in the neurointensive care unit. Neurocrit Care 2009;10:103-15.
GRIST 35
DATE TIME
TOTAL
TIME
MIN.
TEMPBLOOD
GASpH pCO2 pO2 Base HCT iCa COMMENT
1st day ~ 10:30 0 37 35
PT. CODES IN CATH LAB.
TRANSPORTED TO OR DURING
CPR FOR EMERGENT
ECPS/CPB.
11:10 40 37 ABG 7.01 72 43 -15.1Corrected Anion Gap = 16
mEq/L
11:51 81 37 VBG 6.90 113 18 -11 22 1.11 ON ECPS/CPB, LIMA >LCA REPAIR
11:59 89 33 VBG 6.98 63 23 -15.9 25 0.98
12:09 99 30 VBG 7.13 44 36 -13.8 26 1.04
12:20 110 24 VBG 7.22 35 48 -12.4 25 1.02
12:39 129 26 VBG 7.33 31 64 -8.9 24 1.00
13:02 152 26 VBG 7.32 28 67 -11.5 29 0.98
13:29 179 26 VBG 7.39 26 61 -9.8 31 0.79
13:42 192 25 VBG 7.42 23 113 -9.4 31 0.88
13:54 204 25 VBG 7.49 23 115 -6.3 31 0.88
14:12 222 31 VBG 7.4 27 46 -8.1 29 1.59
14:23 233 37 VBG 7.38 36 39 -4 32 1.32
14:38 248 37 VBG 7.37 36 36 -4.1 32 1.29
15:24 294 37 OFF ECPS/CPB, ON ECMO
22:00
2nd day
3rd day
SEDATION STOPPED. PT. AWAKES NERUOLOGICALLY INTACT.
TRANSPORTED ON ECMO TO ARKANSAS/TEXAS FOR HEART & KIDNEY TX. SURVIVES NEURLOGICALLY
INTACT.
11 Y/O UNDERGOING ABLATION IN CATH LAB. LMCA OCCLUSION.
HIGHEST LACTIC ACID = 13 mmol/L
GRIST 36
TIME
TOTAL
TIME
MIN
TEMP pH pCO2 pO2 BASE HCT iCaANION
GAP
LACTIC
ACIDCOMMENT
0845 0
DESATURATED, NO
END TIDAL CO2, CPR
STARTED
0850 5 37 ABG 6.95 90 11 -15 22 1.25 CPR
0855 10 37 ABG 6.89 90 17 -18 40 1.24 CPR
0912 27 37 ABG 6.93 67 63 -19 38 1.22 CPR
0929 44 37 ABG 6.72 131 14 -21 35 1.12 CPR
0930 45STARTED ON ECPR
PUMP, COOLING
0934 49 25 VBG 6.77 106 57 -18 16 0.74 ON ECPR PUMP
0957 72 32 VBG 7.16 32 38 -16 19 0.98 ON ECPR PUMP
1033 108 32 VBG 7.02 52 59 -17 28 1.09 ON ECPR PUMP
1120 155TRANSFER TO ECMO
PUMP
1215 210 32 ABG 7.45 23 58 -6 ON ECMO PUMP
1215 210 32 VBG 7.42 29 34 -4 39 1.34 19 10 ON ECMO PUMP
S/P NW1 POD 15, FUNDOPLICATION, EMERGENT ECPR, WT = 3.8 KG
1 MIN OF CPR IN A SHUNTED PATIENT = 2 MIN OF CPR IN A PATIENT WITH NORMAL CARDIAC ANATOMY
SUCCESSFULLY WEANED FROM ECMO AFTER 122 HOURS, LARGE IVH BUT NO INFARCTIONS
GRIST 37
TIMECOUNT
DOWNTEMP pH pCO2 pO2 BASE
CO2
GRADHCT iCa
ANION
GAP
LACTIC
ACIDCOMMENT
1432 -380 37 OFF CPB
ABG 7.38 45 <33 0.7
VBG 7.35 52 <33 2
ABG 7.35 48 <33 -0.2
VBG 7.29 61 <33 0.4
ABG 7.36 37 <33 -4.2
VBG 7.27 56 <33 -2.2
ABG 7.31 21 38 -14.7
VBG 7.01 74 <33 -14.4
2016 -36 37 MINI CODE
2052 0 37 CODE CALLED, CPR STARTED
2125 33 28 VBG 7.05 46 71 -17 STARTED ON ECPR PUMP, COOLING
2141 49 30 VBG 7.14 55 61 -9.7 ON ECPR PUMP
2214 82 32 VBG 7.2 36 43 -13.4 ON ECPR PUMP
ABG 7.2 30 84 -14.8
VBG 7.24 30 54 -14.7
2334 TRANSFER TO ECMO PUMP
ABG 7.22 35 98 -14.9 ON ECMO PUMP
VBG 7.23 36 44 -15.6 ON ECMO PUMP
ABG 7.38 36 221 -3.6 ON ECMO PUMP
VBG 7.39 40 40 -0.8 ON ECMO PUMP
6 HRS S/P NW1, EMERGENT ECPR, WT = 2.6 KG
SUCCESSFULLY WEANED FROM ECMO AFTER 135 HOURS
~ 1 HR POSTOP3.7131.4150371650
191750 37
-242
32
16 21.1
1 1.0439
32
1.44 14.219
195
4625 32
0005
1030
~ 2 HR POSTOP
53
1442 35
~ 4 HR POSTOP1940 37
-182
-72
13
1.42 14-370 LAST BLOOD GASES IN OR737
ON ECPR PUMP02230 100
GRIST 38
Lancet 2008;372(9638):554-561
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THE END
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