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Page 1: HEARTLINE 2013  Genova 15/11/2013

HEARTLINE 2013 Genova 15/11/2013

Dr Felice Achilli

Le cellule staminali ripareranno il cuore del Paziente infartuato?

Lo studio STEMAMI OUTCOME

Page 2: HEARTLINE 2013  Genova 15/11/2013

20 years ago ….Ejection Fraction in GISSI 1

(Volpi et al, Circulation 1993)

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10 years ago ….not only EF!

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Zhang Y, et al. Am Heart J 2008;156:1124-32.

Cardiac Remodeling Post AMI

ESV, end systolic volume; Ts-SD: Standard deviation of time to peak myocardial contraction Te-SD: Standard deviation of time to peak early relaxation

Characteristic Normal LV Gp Remodeled Gpearly Post MI (n = 31) (n=16) P value

Q waves 24/31 13/16 NS

Anterior wall 11/31 14/16 .007

Peak CK (u/L) 1910 ± 1046 4098 ± 2081 .006

ESV mL 40.6 ± 8.5 47.6 ± 8.4 .006

Ts-SD 33.7 ± 7.5 50.9 ± 10.8 <.0005

Te-SD 36.2 ± 20.2 45.2 ± 23.2 .048

EF% 53.1 ± 11.7 40.8 ± 7.6 <.0005

Infarct size 10.7 ± 5.9 26.4 ± 10.2 <.0005

Transmurality % 73.6 ± 17.3 85.7 ± 19.6 .039

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Data from BLITZ 4Mortality rates vs "ischemic time" and AMI location

4,2

7,26,9

2,9

5,75,1

3,5

4,4

1,9

0

1

2

3

4

5

6

7

8

<3h >3h tot

30d M

orta

lity R

ates

(%) Anterio

Non Anterior

All

< 3 h > 3 h ALL

r

Today…..

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Tomorrow….: “Reverse Remodeling” or….

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Myocardial Recovery!

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“CARDIOMYOCITE RENEW”

(MI) results in the loss of 1 billion functional cardiomyocytes, which are replaced with a fibrous scar, frequently leading to heart failure. Experimental data demonstrate that the mitotic renewal in the human myocardium exists but at a very low rate: 1% annually at the age of 25 and 0.45% at the age of 75. With this turnover rate, most cardiomyocytes will never be exchanged during a normal life span. Although the renewal rate may increase somewhat after injury, the heart itself is not able to effect large-scale cardiac regeneration.

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Dimmler S., 2012 (with permission)

Cell Therapy of Cardiovascular Disease: start of CT

Bone Marrow derived Cells

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CELL SOURCES TARGETED for CARDIAC REGENERATION

Evolution of the cell types used:

1) Myoblasts

2) Bone Marrow Derived Cells:

• Hematopoetic stem cells

• Mesenchymal stem cells

• Endothelial progenitor cells

• Side population cells

FOURTH GENERATION :

Cardiac Progenitors Cells (CPC)

MORE THAN 2000 PATIENTS

TREATED IN 10 YEARS!

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European Heart Journal (2012) Zimmet et Al.

CELL THERAPHY AND ACUTE CORONARY DISEASES

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J.Tongers,D.W. Losordo, U.Landmesser EHJ 2011 Review (modif)

“EXOGENOUS CELL THERAPY” FOR CARDIAC REPAIR

C. Direct Endomyocardial cell injection

Chronic ICM

Acute MI

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FGF familyEPO

FLT-3 ligand

VEGF family(PIGF)

Angiopoietin-1

HGF/IGF-1/GH

Growth

Factors

G-CSF/GM-CSF

SDF

“ENDOGENOUS CELL THERAPY” FOR CARDIAC REPAIR

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Sanganalmat SK, et al., Basic Res Cardiol 2011

CLINICAL BENEFIT

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CELLS THERAPY IN AMI: SAFETY

Zimmet et Al. EHJ 2012

NO DIFFERENCE ABOUT : IN STENT RESTENOSIS

THROMBOSIS

Re-AMI

DEATH

HOSPITALIZATION

ARRYTHMIA

SURGICAL REVASCULARIZATION

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META-ANALYSIS OF BMSC IN AMI PTS

Follow-up 6mFollow-up 18m

Zimmet et Al. EHJ 2012

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Postgrad Med J 2011; 87:558

Changes in LVEF in Clinical Trial that have changed clinical practice

based on effect on clinical outcome

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Mc Alister et al JAMA 2007

CRT for Patients With LV Dysfunction: A Systematic Review

4420 PtsBasal mean LVEF range, 21%-30%

QRS duration (mean range, 155-209 milliseconds)NYHA 3 or 4 despite optimal pharmacotherapy.

CRT improved LVEF 3.0%;

(95% CI: 0.9%-5.1%),

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TARGET ?

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• Smalls and monocentric studies

• No randomization

• Heterogeneous populations

• No blinded study

• Similar surrogate end-points but measured with

different methods (ECHO / MRI / SPECT )

PHASE 2 TRIALS IN CELL THERAPY: LIMITS

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PHASE III CT aiming for approval of Cell Therapy

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Cell Therapy with CARDIAC stem cells

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Meta-analysis of G-CSF Trials in AMI Pts

Effect on EF at 6m of follow-up

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Hill J et al., Circulation, 2006Hill J et al., Circulation, 2006Abdel-Latif A, Am Heart J 2008 Abdel-Latif A, Am Heart J 2008

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Achilli F. et Al. Heart 2013 (submitted)

STEM-AMI Trial 3 YEARS FOLLOW-UP

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STEM-AMI Trial: 3 YEARS FOLLOW-UP

European Heart Journal (2012) Zimmet et Al.

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Time has come for hard clinical endpoints:

GISSI Outliers STEM-AMI OUTCOME TRIAL

Large Phase III, open, randomized, multicenter nationwide Trial.

1502 patients; 65 centres involved.

Anterior STEMI with low ejection fraction post PCI (<45%).

Symptoms-to-baloon time >3 h and <24 h

G-CSF (n=751) vs. saline (n=751) within 12 h from reperfusion.

Primary endpoint: Death, Recurrence of MI, Rehospitalisation for heart failure

(accrural=2y; follow-up=3 y).

E.C. APPROVAL

MAY,8, 2013!

FIRST PATIENT NOV,8,2013

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SWISS-AMI Trial

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TIME Trial

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EPO & G-CSF: dual protective mechanism after AMI

ADAPTED FROM: NAGAI T, AM J PHYSIOL HEART CIRC PHYSIOL 2012

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Which growth factor for AMI?

Growth Factor Safety in humans

Preclinical studies(large animal models)

Preliminary data in patients

Dual mode of action

G-CSF (swine,

primates)

EPO (1 study on

swine)

GM-CSF (concerns

after MI: worsens outcome?)

- (chronic HF)

-

FLT-3 - - - (combined with G-CSF)

SDF - - - (combined with G-CSF)

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Large EPO clinical trials on STEMI TRIAL POPULATION DESIGN ENDPOINTS

Voors et al.Eur Heart J, 2010

HEBE IIII

STEMI after successfull PCIN=529 (1:1)

- Phase II, prospective, randomized, open-label. placebo-controlled.

- Single bolus EPO

- powered to detect differences in EF

Infarct size/EF = negative (MR)

Event-free survival = positive (at 6 weeks)

Najjar SS et al.JAMA, 2011

REVEAL

STEMI after successfull PCIN=222 (1:1)

Phase II prospective, randomized, placebo-controlled.

- Single bolus EPO (i.v.)

- powered to detect differences in infarct size

Infarct size = negative (MR)

Event-free survival = higher rates of CV events in EPO group(at 12 weeks)

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Which determinants of success after AMI for the “dream growth factor”?

Extent of BMCs mobilization and homing

Characteristics of mobilized cells

Timing of therapy

Mobilization-independent effects

Patients characteristics

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Timing?

Martin_Rendon E et al., Eur Heart J 2008Bartunek J et al. Nat Clin Pract Cardiovasc Med 2006

Exp

ressio

n (

fold

in

cre

ase

esti

mate

) Adhesion

Migration

ROS

Inflammatory cytokines

Matrix SupportCollagen

Mobilization

0

1

2

3

4

5

6

BL

Day 3

Day 7

Day 14

Day 21-28

Optimal timingOptimal timingOptimal timingOptimal timing

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Timing?

Kuhlmann MT, et al. JEM 2006.