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Cardiology Update
11th Update for the General Anaesthetist, June 2017
1
Daniel Bromage
NIHR Clinical Lecturer & Specialty Trainee in Cardiology
Overview
• Acute coronary syndromes & PCI
• Antiplatelet agents
• Pacemakers and peri-operative management
• Atrial fibrillation and stroke prevention
• OOHCA without ST elevation
• What’s new in heart failure?
2
ACUTE CORONARY SYNDROMES & PCI
3
Unstable angina(UA)
ST-segment elevation myocardial infarction
(STEMI)
Non-ST-segment myocardial infarction
(NSTEMI)
Collectively known as NSTE-ACS
7.5
12.1
14.8
0
5
10
15
20
Mortality for ACS
GRACE study (n = 1143)
Mortality doubles within 1 year of discharge from
hospital
In-hospital 6-months 1-year
Mo
rtality
rate
(%
)
Tang EW, et al. Am Heart J 2007;153(1):29-355
Patterns of healing
6In-stent restenosis Acute stent thrombosis?
Drug eluting stents
7Bromage DI, et al. Heart 2012;98(Suppl1):A24
Platform design
8
First-generation DES Newer-generation DES
Stent struts
Thrombus
C
Images provided by Dr N West, Papworth Hospital, Cambridge9
Stent thrombosis
• Uncommon but high mortality (10-40%)
• Mostly in the first month (60%), but even up to 5 years!
• 1.5-2% at 2 years
• Newer-generation DES have a lower risk of stent thrombosis
10Sarno G, et al. JACC. 2014;64:16-24
Risks for stent thrombosis
Procedural factors
• Under-sizing (OR 13.5)
• Dissection (OR 6)
• Poor TIMI flow post PCI (OR 5)
• Long/narrow stents
• Complex procedure/extensive disease
• Acute coronary syndrome
Patient factors
• LVEF <30% (OR 2.7)
• DM
• Renal disease
• Malignancy
Inadequate anti-platelet treatment
• Premature discontinuation of P2Y12 inhibitors (OR 36.5!)
• Resistance to clopidogrel i.e. CYP2C19 status, ?omeprazole use11
Bioresorbable vascular scaffolds
12Lancet. 2016;388:2479
ANTI-PLATELET AGENTS
13
20091998 20111991 2000’s
PrasugrelClopidogrelAspirin Ticlopidine(not available in the UK)
Dual anti-platelet therapy
1980s
TRITON-TIMI 38: Primary endpoint
Days
% o
f P
atie
nts
0
5
10
15
0 30 60 90 180 270 360 450
HR: 0.81(0.73-0.90)P<.001
Prasugrel (n=6813)
Clopidogrel (n=6795)
12.1%
9.9%
NNT=46
Wiviott SD, et al. N Engl J Med. 2007;357(20):2001-2015
CV Death/MI/Stroke at 15 months
14
TRITON-TIMI 38: Stent thrombosis
2.4
1.1
0
2
4
Prasugrel
(n=6813)
Clopidogrel
(n=6795)
% o
f P
atie
nts
P<.001
Wiviott SD, et al. N Engl J Med. 2007;357(20):2001-201515
TRITON-TIMI 38: Safety
1.8
0.9 0.9
0.1
3.0
2.4
1.41.1
0.4
4.0
0
2
4
6
TIMI MajorBleeds
LifeThreatening
Nonfatal Fatal Transfusion
Clopidogrel (n=6795)
Prasugrel (n=6813)
% E
ven
ts
*Most frequent sites of life-threatening bleeding: Gastrointestinal, intracranial, puncture, and retroperitoneal.
Wiviott SD, et al. N Engl J Med. 2007;357(20):2001-2015
P=.03
P=.01 P=.23
P=.002
P<.001
*
16
P2Y12 characteristics
Characteristics Clopidogrel1,2 Prasugrel1,3 Ticagrelor1,4
Direct acting
Reversible binding to P2Y12
receptor
Rapid onset of action
> 60% IPA (mean steady state)
More consistent response
1. Wallentin L. Eur Heart J 2009;30:1964-1977; 2. Clopidogrel. Summary of product characteristics 2010; 3. Prasugrel. Summary of product characteristics 2009; 4. Ticagrelor.
Summary of product characteristics 2010 17
Ticagrelor
• Direct acting
• Reversibly binds toP2Y12 receptor
Ticagrelor is aCyclo-pentyl-triazolo-pyrimidine (CPTP)
Husted S, et al. Eur Heart J 2006;27:1038-1047 18
Ticagrelor is not a prodrug
No in vivobiotransformation
needed
Prasugrel
Active metabolite
Clopidogrel
Active metabolite
85%
inactive
metabolite1
Prodrug
Hydrolysis
(Esterases)
CYP-dependant
oxidation
CYP-dependant
oxidation
Intermediary metabolite
Intermediary metabolite
Ticagrelor
Figure adapted from: Schomig AS. N Eng J Med 2009;36:1108-1111.
1. Clopidogrel. Summary of product characteristics. 2010 19
Ticagrelor onset and efficacy
0
25
50
75
100
0.5 2 4 8
Ticagrelor Clopidogrel
Time post-loading dose (hours)
In
hib
itio
n o
f p
late
let
ag
gre
ga
tio
n (
%)
Patients with stable CAD, which is not a licensed population for ticagreloruse
* p < 0.0001, ticagrelor vsclopidogrel
*
* **
Adapted from: Gurbel PA, et al. Circulation 2009;120:2577-258520
Ticagrelor reduces MACE
Kaplan-Meier estimate of time to primary endpoint (composite of CV death, MI or stroke)
No. at risk
Ticagrelor 9,333 8,628 8,460 6,743 5,161
Clopidogrel 9,291 8,521 8,362 8,124 6,743 5,096 4,047
4,1478,219
Days after randomisation
0 60 120 180 240 300 360
12
11
10
9
8
7
6
5
4
3
2
1
0
13
Cu
mu
lati
ve
in
cid
en
ce
(%
)
9.8
11.7
HR 0.84 (95% CI 0.77–0.92), p=0.0003
Clopidogrel
Ticagrelor
RRR = 16%ARR = 1.9%NNT = 54
Wallentin L, et al. N Engl J Med 2009;361:1045-1057
All patients received aspirin (75-100 mg/d)
21
0.3
Major bleeding with ticagrelor
NS13
NS
NS
NS
NS
0
K-M
esti
ma
ted
ra
te (
% p
er
ye
ar)
PLATO major bleeding
1
2
3
4
5
6
7
8
9
10
12
11
TIMI major bleeding
Red cell transfusion
PLATO life-threatening/fatal bleeding
Fatal bleeding
11.611.2
7.9 7.7
8.9 8.9
5.8 5.8
0.3
TicagrelorClopidogrel
Wallentin L, et al. N Engl J Med 2009;361:1045-105722
Ticagrelor
Adenosine
Clopidogrel
Prasugrel
Dipyridamol
23
Dyspnoea with ticagrelor
• Dyspnoea in patients receiving ticagrelor is usually mild or moderate in intensity and often resolves without the need for treatment discontinuation2,3
• Dyspnoea during ticagrelor treatment does not appear to be associated with any differences in efficacy or bleeding-related clinical outcomes compared with clopidogrel2
† Most episodes of dyspnoea lasted less than a week
Dyspnoea† (%) Ticagrelor(n=9,235)
Clopidogrel(n=9,186)
p value
Any 13.8 7.8 < 0.001
With discontinuation of treatment 0.9 0.1 < 0.001
1. Wallentin L, et al. N Engl J Med 2009;361:1045-1057; 2. Storey RF, et al. Poster presented at European Society of Cardiology,
Stockholm, Sweden, 28 August–1 September 2010; 3. Ticagrelor. Summary of product characteristics. 201024
ESC guidelines - STEMI
Steg G et al. European Heart Journal 2012;33:2569-2619 25
ESC guidelines - NSTEMI
Hamm CW et al. European Heart Journal 2011;32:2999-3054 26
ESC guidelines – Stable CAD
Montalescot G et al. European Heart Journal 2013;34:2949-3003 27
Duration of DAPT
• Controversial
• Currently, 1 year after ACS, 6 months after DES, 1 month after BMS
• Several trials have examined this: ARCTIC-Interruption1, SECURITY2, DAPT3.
• Conclusions:– High risk of bleeding, stop sooner
– High risk of ischaemia/thrombus, continue
– ?personalised risk score
281. Collet JP et al. Lancet 2014;384:1577-1585; 2. Colombo A et al. JACC 2014;64:2086-2097; 3. Mauri L et al. NEJM 2014;371:2155-2166
NON-CARDIAC SURGERY POST-PCI
Ris
k o
f B
lee
din
g
Ris
k o
f T
hro
mb
osisHaemostatic
Balance
29
Discontinuation of DAPT
• 14.4% stop 1 or 2 antiplatelets for at least 5 days in the first year post PCI
• Causes of discontinuation of DAPT– Bleeding events/invasive procedures (50%)
– Medical decision (32%)
– Patient decision (18%)
• Predictors of discontinuation– Renal impairment
– Previous haemorrhage
– Peripheral vascular disease
Ferreira-Gonzalez et al. Circulation 2010 30
Eisenberg MJ et al. Circulation 2009;119:1634-1642
Discontinuation of DAPT
31
Stop or continue ...
Continuing Aspirin/DAPT
• Increased bleeding– Aspirin alone: 20%
– DAPT: 50%
• No increased mortality except in intracranial surgery
• Increased transfusion by 30%
• Background risk of MI
Withdrawing Aspirin/DAPT
• ?rebound effect
• Early stent thrombosis in up to 35%, with mortality of 20-40%, i.e. Increased peri-operative cardiac death rate 5-10x
• Poorer outcomes of peri-operative MI
MDT: Anaesthetists + Surgeons + Cardiologists + Patients32
ESC recommendation
Windecker S et al. European Heart Journal 2014;35:2541-2619 33
Timing is important: Ontario study
• N=8116, DES in 33%
• Overall event rate = 2.1% (intermediate risk)
Wijeysundera DN, et al. Circulation 2012;126(11):1355-6234
ESC recommendation
Montalescot G et al. European Heart Journal 2013;34:2949-3003 35
PACEMAKERS AND PERI-OPERATIVE MANAGEMENT
36
Cardiac devices
• What type of device is it: pacemaker or defibrillator?
• ID card?
–Device manufacturer
–Model number
–Serial number
–Implanting hospital
–Follow-up hospital
–Date of implant
–Reason for implant
37
What device is this?
38
CRT trials
TRIAL NYHA LVEF (%) QRS (msec) COMMENTS
COMPANION 1(2004)
III-IV ≤35% ≥120 ~20% reduction in all cause mortality or hospitalization from any cause
CARE-HF 2
(2005)III-IV ≤35% ≥120 RRR of death 37%
MADIT-CRT 3
(2009)I-II ≤30% ≥130 CRT-D: 34% reduction in all-cause
mortality and heart failure events vs. ICD
RAFT 4 (2010) II-III ≤30% ≥120 CRT-D: 25% reduction in all-cause mortality and hopitalisations vs. ICD
ECHO-CRT 5
(2013)III-IV ≤35% <130 +
dyssynchronyCRT does not reduce the rate of death or hospitalization for heart failure and may increase mortality
1. Bristow MR, et al. N Engl J Med 2004;350(21):2140-50; 2. Cleland JGF, et al. N Engl J Med 2005;352:1539-49; 3. Moss AJ, et al. N Engl J Med 2009;361:1329-38; 4. Tang
ASL, et al. N Engl J Med 2010;363(25):2385-95; 5. Ruschitzka F, et al. N Engl J Med 2013;369:1395-140539
Practically...
• Get device checked if possible
–Confirm in working order
–Check if pacing dependent
–Programming of device if necessary
• Monitoring
• Resuscitation/pacing equipment
• Magnet?
40
What’s new in EP?
Leadless pacemaker Subcutaneous ICD
41
What’s new in EP?
Telemonitoring Vagal nerve stimulation
42Hindricks G et al. Lancet 2014;384:583-590
ATRIAL FIBRILLATION AND STROKE PREVENTION
43
AF and stroke
• AF is associated with a 5-fold higher stroke risk overall1
• Without prevention, approximately 1 in 20 patients will have a stroke each year3
• Responsible for nearly a third of all strokes,5 and the leading cause of embolic stroke6
1. Savelieva I et al. Ann Med 2007;39:371–91; 2. ACC/AHA/HRS focused update guidelines: Fuster V et al. Circulation 2011;123:e269–357; 3. Atrial Fibrillation Investigators. Arch Intern
Med 1994;154:1449–57; 4. Carlson M. Medscape Cardiol 2004;8; available at http://www.medscape.org/viewarticle/487849; accessed Feb 2010; 5. Hannon N et al. Cerebrovasc Dis
2010;29:43–9; 6. Emmerich J et al. Eur Heart J 2005;7(Suppl C):C28–3344
Strokes in AF are worse!
• Compared with other causes, stroke in AF:
–Is usually more severe1
–Is more likely to be disabling:2
–Has double the post-stroke mortality rate3
1. Savelieva I et al. Ann Med 2007;39:371–91; 2. Dulli DA et al. Neuroepidemiology 2003;22:118–23; 3. Benjamin EJ et al. Circulation 1998;98:946–52 45
Source of thromboembolism in AF
The left atrial appendage is the source of thromboemboli in ~80% of AF patients with stroke
46
47http://www.nice.org.uk/nicemedia/live/14573/68045/68045.pdf
DAPT vs. warfarin
RR = 1.72 AR ↑= 1.0%
48
Stroke prevention: CHA2DS2-VASc
• CCF 1
• Hypertension 1
• Vascular disease 1
• Diabetes 1
• Stroke or TIA 2
• Female gender 1
• Age ≥ 65 1 or
• Age ≥ 75 2
0: No anticoagulation
≥1 (Men) or ≥2 (Women): Anticoagulate
49Lip GY et al. Chest 2010;137(2):263-72, http://www.nice.org.uk/nicemedia/live/14573/68045/68045.pdf
Bleeding risk
• HAS-BLED• Hypertension 1• Abnormal renal or liver function 2• Stroke 1• Bleeding history 1• Labile INR 1• Age > 65 1• Drugs or alcohol 2
• 3+: High risk for bleeding with warfarin
50Pisters R. Chest. 2010 Nov;138(5):1093-100
Warfarin therapeutic window
Relationship between clinical events and INR intensity
ICH=intracranial hemorrhage
INR=international normalized ratio
1. Hylek EM et al. Ann Intern Med 1994;120:897-902; 2. Hylek EM et al. N Engl J Med 1996;335:540-54651
Time in therapeutic range (TTR)
0 500 1000 1500 2000
Survival to stroke (days)
0.6
0.7
0.8
0.9
1.0
Cu
mu
lati
ve s
urv
ival
71–100%
Warfarin group
61–70%51–60%41–50%31–40%<30%Non warfarin
Morgan CL et al. Thrombosis Research 2009;124:37–41 52
Alternatives to warfarin (NOACs)
Factor Xa inhibitors:ApixabanRivaroxabanEdoxaban
Direct Thrombin inhibitor:Dabigatran
53
NOACs vs. warfarin
SSE* vs. Warfarin(ITT population)
ARR HR
D150 0.60 0.65 (0.52-0.81)
D110 0.17 0.90 (0.74-1.10)
Rivaroxaban 0.30 0.88 (0.75-1.03)
Apixaban 0.33 0.79 (0.66-0.95)
Haemorrhagic stroke vs. Warfarin
ARR HR
D150 0.28 0.26 (0.14-0.49)
D110 0.26 0.31 (0.17-0.56)
Rivaroxaban 0.18 0.59 (0.37-0.93)
Apixaban 0.23 0.51 (0.35-0.75)
Connolly et al, N Eng J Med 2009; 361 and Vol. 363 No.19; Patel et al, N Eng J Med 2011; 365; Granger et al, N Eng J Med 2011; 365
*SSE (Stroke, Systemic Embolism)
NOACs vs. warfarin
IntracranialBleeding
ARR HR
D150 0.44 0.41 (0.28-0.06)
D110 0.53 0.30 (0.19-0.45)
Rivaroxaban 0.20 0.67 (0.47-0.93)
Apixaban 0.47 0.42 (0.30-0.58)
Connolly et al, N Eng J Med 2009; 361 and Vol. 363 No.19
Patel et al, N Eng J Med 2011; 365 Granger et al, N Eng J Med 2011; 365
Major Bleeding ARR HR
D150 0.25 0.93 (0.81-1.07)
D110 0.70 0.80 (0.70-0.93)
Rivaroxaban -0.20 1.04 (0.90-1.20)
Apixaban 0.96 0.69 (0.60-0.80)
NOACs
Pros
• No frequent blood tests
• Beneficial in all bleeding risks
• All reduce ICH
Cons
• Caution in patients with elevated bleeding risk and prior to invasive therapy
• Renal and liver impairment
• Drug interactions
• Can’t monitor
• Cost
• NOT licensed in valvular AF or prosthetic valves
56
Practical issues
• Dabigatran prolongs TT but not aPTT• Rivaroxaban and apixaban prolong aPTT (slightly) but
not TT• PT/INR is not helpful• Need to stop at least 5 doses before major surgery• If major bleeding:
– Maintained diuresis– Supportive treatment with blood/platelet
transfusion– Consider PCC (e.g. FEIBA, Beriplex)– Consider haemodialysis (remove 40-60% in 4 hrs)
57
OOHCA WITHOUT ST ELEVATION
58
Meta-analysis
NO RANDOMISED STUDIES!
Larsen JM and Ravkilde Jl. Resuscitation 2012;83:1427-143359
Consensus document
Noc M, et al. Eurointervention 2014;10:31-3760
Advice…
• VF: ischaemia?
• LBBB: ischaemia?
• ACS treatment
• Echo if unsure
61
WHAT’S NEW IN HEART FAILURE?
62
The headlines: PARADIGM
63McMurray JJV, et al. NEJM 2014;371(11):2993-1004
The headlines: SERVE-HF
64Cowie MR, et al. NEJM 2015;373(12):1095-105
The headlines: CONFIRM-HF
65Ponikowski P, et al. EHJ 2015;36(11):657-68
The headlines: EMPA-REG OUTCOME
66Zinman B, et al. NEJM 2015;373(22):2117-28
2016 ESC Guidelines
• Recommendations on the diagnostic criteria for HF with reduced EF (HFrEF), HF with mid-range EF (HFmrEF) and HF with preserved EF (HFpEF)
• A new algorithm for the diagnosis of HF in the non-acute setting based on the evaluation of HF probability
• Recommendations aimed at prevention or delay of the development of overt HF or the prevention of death before the onset of symptoms
• Indications for the use of the new compound sacubitril/valsartan, the first in the class of angiotensin receptor neprilysin inhibitors (ARNIs)
• Modified indications for cardiac resynchronization therapy (CRT)• The concept of an early initiation of appropriate therapy going• A new algorithm for a combined diagnosis and treatment
approach of acute HF
67
Cardioprotection
No ‘Conditioning’
Heart Ischaemia Reperfusion‘Conditioned’
Ischaemic
Postconditioning
2003
< 1min
Ischaemic
Preconditioning
1986
0 to 3 hrs
Remote
Ischaemic
Conditioning
Pharmacological
conditioning
68
ERICCA
69Hausenloy D, et al. NEJM 2015;373(15):1408-17
Thank you
Summary
• Acute coronary syndromes & PCI
• Antiplatelet agents
• Pacemakers and peri-operative management
• Atrial fibrillation and stroke prevention
• OOHCA without ST elevation
• What’s new in heart failure – LCZ696, IV iron, SGLT-2 inhibitors
71
• EMPA-REG
• SERVE-HF
72
