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Contrast Awareness: Why and When Do we Worry?
Roxana Mehran, MD Professor of Medicine (Cardiology) and Health Evidence Policy Director of Interventional Cardiovascular Research and Clinical Trials The Icahn School of Medicine at Mount Sinai, New York, NY Chief Scientific Officer Cardiovascular Research Foundation, New York, NY Cardiovascular Research Technology - CRT February 23-26, 2013 Washington, DC
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Roxana Mehran, MD Consulting: AstraZeneca, Johnson and Johnson, Merck and Company, Inc., and Abbott Laboratories Grant Support: Bristol-Myers Squibb, Sanofi, The Medicines Company, Lilly and Daiichi Sankyo Honoraria: Regado Bio-Sciences
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Contrast Media During CTO: What are the Issues?
CTO procedures are one of the most complex and time consuming procedures in IC Most CTO procedures require dual injection for complete visualization of the vessel to enhance success Contrast volume in these procedures are usually twice or more than the routine PCI procedures Patients with CTO are usually more complex, with more co-morbidities which will increase the risk of contrast Induced- acute kidney injury (CI- AKI) This is the Bulleted List slide. To create this particular slide, click the NEW SLIDE button on your toolbar and choose the BULLETED LIST format. (Top row, second from left) The Sub-Heading and footnote will not appear when you insert a new slide. If you need either one, copy and paste it from the sample slide. If you choose not to use a Sub-Heading, let us know when you hand in your presentation for clean-up and we’ll adjust where the bullets begin on your master page. Also, be sure to insert the presentation title onto the BULLETED LIST MASTER as follows: Choose View / Master / Slide Master from your menu. Select the text at the bottom of the slide and type in a short version of your presentation title. Click the SLIDE VIEW button in the lower left hand part of your screen to return to the slide show. (Small white rectangle) 5
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Contrast-induced Nephropathy: In-hospital Mortality
% In-hospital Death P<0.001 In-hospital mortality is especially high in pts requiring dialysis. McCullough et al. Am J Med. 1997;
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Contrast-Induced Nephropathy: Resource Utilization
Endpoint (%) Patients P-value With CIN Without CIN Hospital length of stay (days) <0.001 ICU length of stay (days) <0.0001 Need for hemodialysis (%) 12 Iakovou I et al. J Am Coll Cardiol. 2002;39:2A.
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How to Assess Renal Function?
Abbreviated Modification of Diet in Renal Disease equations (MDRD) equation: eGFR, ml/min/1.73 m2= 186 x (Serum Creatinine [mg/dL]) x (Age-0.203x (0.742 if female) x (1.210 if African American) Cockcroft-Gault equation: (140- age) x Body Weight [kg]* Creatinine Clearance, ml/min = * Multiple by 0.8 in female Serum Creatinine mg/dL] x 72
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Contrast-Induced Nephropathy
Definition New onset or exacerbation of renal dysfunction after contrast administration in the absence of other causes: increase by > 25% or absolute of > 0.5 mg/dL from baseline serum creatinine There is a variety of definitions of RCN, the most common being an increase of serum creatinine greater than 0.5 mg/dl or increase by >25% of baseline creatinine within 24–48 hours following exposure to contrast without other identifiable causes of ARF. The time course of contrast-induced renal failure is predictable. It occurs within 24–48 hours after exposure, with a typical peak creatinine after 3–5 days and a return to baseline or near baseline in 1 to 2 weeks. Occurs 24 to 48 hrs post–contrast exposure, with creatinine peaking 5 to 7 days later and normalizing within 7 to 10 days in most cases
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Can we Prevent CIN? How to prevent CIN?
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YES we Can!! Or at least try to…
Assess the patient’s risk status before the procedure
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Scheme to Define CIN Risk Score
Risk Factors Integer Score Hypotension 5 IABP 5 CHF 5 Risk Score Risk of CIN Risk of Dialysis ≤ 5 7.5% 0.04% 6 to 10 14.0% 0.12% 11 to 16 26.1% 1.09% ≥ 16 57.3% 12.6% Age >75 years 4 Anemia 3 Diabetes 3 Calculate Contrast media volume 1 for each 100 cc3 Serum creatinine > 1.5mg/dl 4 Recently, CIN risk score was developed and validated based on the analysis of large prospectively created database. You may see that risk of CIN may be as high as 57% and risk of dialysis maybe as high as 12% in pts with multiple risk factors. OR 2 for 40 – 60 4 for 20 – 40 6 for < 20 eGFR <60ml/min/1.73 m2 eGFR < 60ml/min/1.73 m2 = 186 x (SCr) x (Age)-0.203 X (0.742 if female) x (1.210 if African American) Mehran et al. JACC. 2004;44:
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Tips to Prevent CIN Assess the patient’s risk status before the procedure Hydrate all patients as tolerated for as long as possible but at least two- four hours before procedure- may require to bring the patient in the night before for careful/gentle hydration in those with CHF
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Optimal Hydration 0.9% NS vs 0.45% NS
3 0.9% Saline 0.45% Sodium Chloride P=.04 2 P=.93 Incidence, % P=.35 1 CN Mortality Vascular Mueller et al Arch Intern Med 2002
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Sodium Bicarbonate Hydration
p = 0.82 p = 0.97 Brar S, et al. JAMA 2009
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Create and maintain high urine output
RenalGuardTM for CI-AKI prevention is designed to: Create and maintain high urine output Prevent contrast agents from clogging tubules Limit toxin exposure in kidneys Automated matched fluid replacement in real-time to reduce side effects associated with over- or under-hydration We believe PLC’s new technology Renal Guard accomplishes this challenge – High urine flow with matched fluid replacement for C-I-N prevention. Renal Guard keeps the tubules clear and reduces exposure to contrast toxins through high urine flow. The Renal Guard therapy includes a replacement of fluid volume precisely matched to each patient, ensuring the optimal C-I-N prevention without the risk of over or under-hydration. US: Investigational device. Limited by Federal Law to investigational use. 23 23
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MYTHOS Study Consecutive CKD patients (eGFR<60ml/min/1.73m2) undergoing coronary angiography between September 1, 2008 and September 15, 2010 157 pts Elective Procedures n= 94 Urgent (<24 hrs) procedures (NSTEMI) n= 63 RenalGuard n=80 Standard i.v. hydration (1 ml/kg/hr) for 12 hrs before and after procedure n=77 Primary end point: CIN (>0.5 mg/dl or >25% sCr increase during first 72 hrs) Secondary end points: In-hospital MACE (acute pulmonary edema, cardiogenic shock, MI, need for RRT, severe arrhythmias, and death) Bartorelli A. JACC Int
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Incidence of CIN Controls % RenalGuard 25% -80% -69% 16% -60% 10% 6%
P=0.03 25% RenalGuard P=0.028 -80% -69% 16% P NS -60% 10% Added the patient numbers at the top of each column 6% 5% 4% All patients NSTEMI Elective procedures 25 25
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REMEDIAL II REnal Insufficiency Following Contrast MEDIA Administration II TriaL RenalGuard system in high risk patients for contrast induced acute kidney injury Carlo Briguori, MD, PhD Laboratoy of Interventional Cardiology Clinica Mediterranea, Naples - Italy 26
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Assessed for eligibility (n=806)
Exclusion (n=512) Not meeting inclusion/exclusion criteria (n=485 ) Refused to partecipate (n=27) Enrollement Randomized (n=294) Patients allocated in the RenalGuard group (n=147) Received allocated treatment (n=146) Did not receive the allocated treatment (n=1) Patients allocated in the Control group (n=147) Received allocated treatment (n=146) Did not receive the allocated treatment (n=1) Allocation Patients lost at follow-up (n=0) Discontinued treatment (n=2) Patients lost at follow-up (n=0) Discontinued treatement (n=0) Follow-up Analysis Patients analized (n=146) Patients excluded from analysis (n=0) Patients analized (n=146) Patients excluded from analysis (n=0) 27 27
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Primary endpoint Odds ratio = 0.47; 95% CI= 0.24-0.92 p = 0.025 20.5%
30/146 15 CI-AKI (%) 11% 10 16/146 5 Control group RenalGuard group
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A study to evaluate the safety and efficacy of the RenalGuard System when compared with standard care in the prevention of contrast induced nephropathy in the catheterization laboratory RGS001D Version 4.1 – 14 April 2011 © PLC Medical Systems, Inc.
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STUDY PROCEDURES RENALGUARD RANDOMIZATION CONTROL
Baseline Blood (prior to therapy) Foley Cath RG Match Hydration Hydration Bolus (NS mls) NAC per protocol Lasix Dose (0.3 mg/Kg) Visipaque or Isovue Additional Lasix ( if needed) RG Matched Hydration (for 4 hrs post last administration of contrast) Blood Draw/urine post procedure (2- 4 post last contrast) Urine output monitoring ( from hour 4 to hour 6) NAC per site protocol 3 ml/Kg/hr Bicarb hydration (x 60 min prior to cath) 1 ml/Kg/hr Bicarb 1 ml/Kg/hr saline hydration (for 6 hours post cath) Patient monitoring RANDOMIZATION CONTROL RENALGUARD Approx 90 min prior Approx 60 min prior During Cath Post Catheterization © PLC Medical Systems, Inc, Company Confidential
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Tips to Prevent CIN Assess the patient’s risk status before the procedure Hydrate all patients as tolerated for as long as possible but at least two- four hours before procedure- may require to bring the patient in the night before for careful/gentle hydration in those with CHF Choose low-osmolar contrast media and monitor the volume
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CARE Design 482 patients enrolled between July 2005 and June 2006 in 25 clinical site in North America DESIGN: Prospective, randomized, double-blind, parallel-group, multi-center clinical evaluation ipamidol-370 and iodixanol-320 OBJECTIVE: To compare the incidence of CIN between iopamidol-370 and iodixanol-320 PRIMARY ENDPOINT: Increase in SCr ≥ 0.5 mg/dL from baseline to 45 to 120 hours after administration 14 patients withdrew consent 468 assigned to a treatment arm 230 patients assigned to Iopamidol-370 236 patients assigned to Iodixanol-320 26 excluded 26 excluded 204 evaluable patient 210 evaluable patient Solomon RJ et al. Circulation. 2007;115,3189.
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CARE p = 0.39 p = 0.44 p = 0.15
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Tips to Prevent CIN Assess the patient’s risk status before the procedure Hydrate all patients as tolerated for as long as possible but at least two- four hours before procedure- may require to bring the patient in the night before for careful/gentle hydration in those with CHF Choose low-osmolar contrast media and monitor the volume!!
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Columbia University CTO Experience N=390
(ml) Contrast Volume Min. 43 – Max.1120 ml P=0.68
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Tips to Prevent CIN Assess the patient’s risk status before the procedure Hydrate all patients as tolerated for as long as possible but at least two- four hours before procedure- may require to bring the patient in the night before for careful/gentle hydration in those with CHF Choose low-osmolar contrast media and monitor the volume!! Follow the patient post procedure with repeat creat ( 24 hours, hrs with PMD) and continue hydration for 12 hours
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Conclusions (1) CTO procedures are usually in the most complex patients and are the most time consuming and require the largest volume of contrast media than most coronary procedures. CI- AKI remains a frequent source of acute renal failure and is associated with increased morbidity and mortality, and higher resource utilization Several factors predispose patients to CIN Preventive measures pre procedure, as well as careful post procedure management should be routine in all patients This is the Bulleted List slide. To create this particular slide, click the NEW SLIDE button on your toolbar and choose the BULLETED LIST format. (Top row, second from left) The Sub-Heading and footnote will not appear when you insert a new slide. If you need either one, copy and paste it from the sample slide. If you choose not to use a Sub-Heading, let us know when you hand in your presentation for clean-up and we’ll adjust where the bullets begin on your master page. Also, be sure to insert the presentation title onto the BULLETED LIST MASTER as follows: Choose View / Master / Slide Master from your menu. Select the text at the bottom of the slide and type in a short version of your presentation title. Click the SLIDE VIEW button in the lower left hand part of your screen to return to the slide show. (Small white rectangle)
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Conclusions (2) Limit contrast agent volume
Hydration pre-PCI (12 hours recommended) D/C nephrotoxic drugs (NSAIDS, antibiotics, etc) NO ROLE for n-acetylcysteine !! No Role for IV Fenoldopam Sodium bicarbonate may be useful, but need more definitive data Limit contrast agent volume Low-osmolar agents are better than high-osmolar Within non-ionic contrast, the data are contradictory This is the Bulleted List slide. To create this particular slide, click the NEW SLIDE button on your toolbar and choose the BULLETED LIST format. (Top row, second from left) The Sub-Heading and footnote will not appear when you insert a new slide. If you need either one, copy and paste it from the sample slide. If you choose not to use a Sub-Heading, let us know when you hand in your presentation for clean-up and we’ll adjust where the bullets begin on your master page. Also, be sure to insert the presentation title onto the BULLETED LIST MASTER as follows: Choose View / Master / Slide Master from your menu. Select the text at the bottom of the slide and type in a short version of your presentation title. Click the SLIDE VIEW button in the lower left hand part of your screen to return to the slide show. (Small white rectangle)
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