Post on 17-Dec-2015
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Nuovi Anticoagulanti orali: dai criteri di scelta all’esperienza sul campo
RIVAROXABAN
Dr. Elisabetta TosoSOC Cardiologia
Ospedale Cardinal Massaia - Asti
2011-2012Years
1980-1990
Xabans i.v.
THE RIVAROXABAN HISTORY
1905-1980
Antistasin(FXa inhibitor)
2000
Oral Inhibitors
Rivaroxaban
FDA Approves Rivaroxaban
For NVAF, DVT and PE
ROCKET-AF
EINSTEIN-DVT
EINSTEIN-PE
2013
ATLAS TMI 51 ACS
EUROPE Approves Rivaroxaban
For ACS
Indications
Prophylaxis Treatment
NVAF15 or 20 mg od
VTE10 mg od
ACS2.5 mg bid +antiplatelets
VTE15 mg bid 21 days
20 mg od
Warfarin Warfarin (2.4%/y)(2.4%/y)
RivaroxabanRivaroxaban(2.1%/y)(2.1%/y)
14264 patientsMean age 73 y, 80% persistent AF, mean CHADS2 score 3.5
Patel et al. NEJM 2011Patel et al. NEJM 2011
ROCKET AFROCKET AF
DaysDays
Stroke or systemic embolism
ROCKET AF – all-cause mortality
Safety population – on-treatment analysis
Hazard ratio and 95% CIs
0.2 0.5 1 2 5Favours
rivaroxabanFavours warfarin
Endpoints
Rivaroxaban (N=7,061)
Warfarin (N=7,082)
Hazard ratio (95% CI)
n(% per year)
n(% per year)
All-cause mortality 208 (1.9) 250 (2.2) 0.85 (0.70,1.02)
Vascular death 170 (1.5) 193 (1.7) 0.89 (0.73, 1.10)
Non-vascular death 21 (0.2) 34 (0.3) 0.63 (0.36, 1.08)
Unknown cause 17 (0.2) 23 (0.2) 0.75 (0.40, 1.41)
Patel MR et al, NEJM 2011.Patel MR et al, NEJM 2011.
Parameter
Rivaroxaban (N=7,111)
Warfarin (N=7,125)
Hazard ratio (95% CI)n (% per year) n (% per year)
Principal safety endpoint
1,475 (14.9) 1,449 (14.5) 1.03 (0.96,1.11)
Major bleeding 395 (3.6) 386 (3.4) 1.04 (0.90,1.20)
Haemoglobin drop (≥2 g/dl)
305 (2.8) 254 (2.3) 1.22 (1.03,1.44)*
Transfusion 183 (1.6) 149 (1.3) 1.25 (1.01,1.55)*
Critical organ bleeding 91 (0.8) 133 (1.2) 0.69 (0.53,0.91)*
Intracranial haemorrhage
55 (0.5) 84 (0.7) 0.67 (0.47,0.93)*
Fatal bleeding 27 (0.2) 55 (0.5) 0.50 (0.31,0.79)*
Non-major clinically relevant bleeding
1,185 (11.8) 1,151 (11.4) 1.04 (0.96,1.13)
Safety population – on-treatment analysis; *Statistically significant
ROCKET AF – bleeding analysis
Major bleeding from gastrointestinal site (upper, lower and rectal): rivaroxaban=224 events (3.2%); warfarin=154 events (2.2%); p<0.001*
Hazard ratio and 95% CIs
0.2 0.5 1 2 5Favours
rivaroxabanFavours warfarin
Patel MR et al, NEJM 2011.Patel MR et al, NEJM 2011.
What about Rivaroxaban and..
VALVULAR HEART DISEASEHYPERTROPHIC CARDIOMYOPATHY
ELECTRICAL CARDIOVERSION
NOACs for VALVULAR HD
ESC AF Guidelines European Heart Journal 2012
Patients with prosthetic heart valves should not take dabigatran/rivaroxaban/apixaban
nor should pts with AF that is caused by a heart valve problem.
www.fda.gov
Breithardt G. et al Eur Heart Journal 2014
Valvular Heart Disease 1992 pts (14%)90% mitral regurgitation (only 3% post-rheumatic)
Stroke or SE Major Bleedings
P 0,76
• Rivaroxaban • Warfarin
P 0,01
% E
vent
s/10
0 pt
s/y
2,01
2,43
6,14
4,20
% E
vent
s/10
0 pt
s/y
• In HCM pts CHA2DS2VASC score to calculate stroke risk is not recommended
• There are no data on the use of NOACs in HCM pts
What about Rivaroxaban and..
VALVULAR HEART DISEASEHYPERTROPHIC CARDIOMYOPATHY
ELECTRICAL CARDIOVERSION
Electrical Cardioversion on warfarin
664 pts1841 pts 521 pts 275 pts 1946 pts
0.7%
0.5%
0.4%0.3%
0
13/ 5247 pts0.24%
Sintomatic cerebrovascular complications
Electrical Cardioversion on NOACs
647 pts 672 pts
0.8%
265 pts
0.30%
0
Sintomatic cerebrovascular complications
Flaker G. et al JACC 2014Nagarakanti R et al Circulation 2011
265 pts
1.6%
Piccinini et al JACC 2013
9/1708 pts0,52%
CHADS 2.1-2.2
CHADS 2.1
CHADS 3.5
Cappato R. et al. Eur Heart Journal 2014
X-VERT Trial1504 patients, 141 Centres across 16 countries
GermanyFrance
Netherlands
UK
South Africa
Canada Belgium
China
Denmark
Finland
SpainPortugal
USA
Singapore
Greece
Italy:•Botto GL •Calò L•Cappato R •Capucci A•Gaita F•Grimaldi M•Gulizia MM•Themistoclakis S
30-day follow-up
OAC
Randomized, open-label, parallel-group, active-controlled multicentre study
Early#
Delayed
Cardioversionstrategy
1–5 daysR
Rivaroxaban 20 mg od*
VKA2:1
2:1
≥21 days(max. 56 days)
Rivaroxaban 20 mg od*
VKA
R
Inclusion criteria:Age ≥18 years, non-valvular AF lasting >48 h or unknown duration, scheduled for cardioversion
Ezekowitz MD et al. Am Heart J 2014;167:646–652;
*15 mg if CrCl 30–49 ml/min; VKA with INR 2.0–3.0; #protocol recommended only if adequate anticoagulation or immediate TEE
42 days
42 days
Rivaroxaban 20 mg od*
VKA
Rivaroxaban 20 mg od*
VKA
End
of
stud
y tr
eatm
ent
Car
dio
vers
ion
Car
dio
vers
ion
Total(N=1504)
Rivaroxaban(n=1002)
VKA(n=502)
Age, mean SD, years 64.9 ±10 64.9±10 64.7±10
Male, % 72.7 72.6 73.1
Persistent 53.9 55.9 50.0
Hypertension, % 66.2 65.0 68.7
Renal function/CrCI, % ≥80 ml/min
60.2 61.5 57.6
Prior OAC use for ≥6 weeks, % 42.8 42.3 43.8
Previous stroke/TIA or SE, % 7.7 6.7 9.8
CHADS2 score, mean SD 1.4±1.1 1.3±1.1 1.4±1.1
CHA2DS2-VASc score, mean SD 2.3±1.6 2.3±1.6 2.3±1.6Cappato R et al. Eur Heart J 2014
X-VeRT: clinical characteristics
X-VeRT: Stroke or TIA
768/872 early CV performed
567 pts
0.7%
277 pts
1,08%
399/632 delayed CV performed
321 pts
0.2%
78 pts
0,9%
Cappato R et al. Eur Heart J 2014
p<0.001
1 patient with inadequate
anticoagulation
95 patients with inadequate
anticoagulation
Patients cardioverted as scheduled
X-VeRT: time to cardioversion
Cappato R et al. Eur Heart J 2014
Rivaroxaban: 841/1002 pts (84%)Warfarin: 385/502 pts (77%)
Pati
ents
(%
)
Delayed cardioversion
Rivaroxaban: 321/417 pts (77%)Warfarin: 78/215 pts (36.3%)
Median time to cardioversion
Day
s
0
20
40
60
80
100
Early Delayed
p=0.628
p<0.001
RivaroxabanVKA
22 days
30 days
X-VeRT: time to cardioversion
Cappato R et al. Eur Heart J 2014
The time between randomization and CV was similar or shorter in Rivaroxaban vs Warfarin Early median 1 (1-2 ) vs 1 (1-3)
Delayed 22 (21-26) vs 30 (23-42)
Thrombosis Research Global Forum 2014, Berlin 6-8 November
Thanks for your attention!