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Transcript 
CARDIOVASCULAR EFFECTS OF
ANTHRACYCLINE-LIKE
CHEMOTHERAPY AGENTS
JOHN N. HAMATY FACC, FACOI
ANTHRACYCLINE AGENTS
• 1) DOXORUBICIN-Adriamycin
• 2) Daunorubicin-Cerubidine
• 3) Idarubicin-Idamycin
• 4) Epirubicin-Ellence
2 MAIN CATAGORYS
• ACUTE/SUBACUTE
• LATE/CHRONIC
-CAN ARRISE AT ANY TIME FROM
INITIATION OF THERAPY TO WEEKS
AFTER TREATMENT TERMINATION
TYPICALLY MANIFESTED AS CLINICAL
HEART FAILURE OR SUBCLINICAL DECLINE
IN MYOCARADIAL FUNCTION.
USUALLY OCCURS WITHIN ONE YEAR
OFTER TREATMENT TERMINATION OR
EVEN LATER, AFTER ONE YEAR OF
TREATMENT END
ACUTE/SUBACUTE TOXICITY
•
•
•
•
•
•
ECG ABNORMALITIES
ARRHYMIAS(SVT/VT)
HEART BLOCK
LV DYSFUNCTION
INCREASE BNP
PERICARDITIS-MYOCARDITIS SYNDROME
ACUTE TOXICITY
•
•
•
•
•
RELATIVELY UNCOMMON
DOXORUBICIN 3.2%
MOST ARE NOT LIFE-THREATENING
RESOLVE WITHIN 1 WEEK
MONITORING IS NOT RECOMMENDED OR
REQUIRED IF NORMAL LV FUNCTION BY
HISTORY, PHYSICAL EXAM OR TESTING
SUBACUTE TOXICITY
• MORE COMMON
• CHOP IS HIGHER RISK
• VARIES BETWEEN 11-21%
• Relationship between acute and developing
subacute toxicity is not clear.
CHRONIC CARDIOTOXICITY
• CARDIOMYOPAHTY IS DOSE-LIMITING SIDE
EFFECT OF ANTHRACYCLINES.
• USE OF ANTHRACYCLINES WAS ASSOCIATED
WITH SIGNIFICANTLY INCREASED RISK OF
BOTH CLINICAL AND SUBCLINICAL
CARDIOTOXICITY.
• CARDIAC RELATED DEATHS(RARE) WAS ALSO
SIGNIFICANTLY HIGHER
CLINICAL MANIFESTATIONS
• CHRONIC ANTHRACYCLINE RELATED
CARDIOTOXICITY TYPICALLY PRESNETS EARLY,
WITHIN 1 YR OFTER TERMINATION OF
CHEMO.
• PEAK TIMING OF SYMPTOMS OF CHF IS
ABOUT 3 MONTHS AFTER LAST
ANTHRACYCLINE DOSE.
• MORTALITY IS HIGH(60%) BUT DECREASING
DUE TO NEWER TREATMENTS.
CLINICAL MANIFISTATIONS
• HEART FAILURE CAN OCCUR MORE THAN A
DECADE AFTER LAST DOSE.
• GREATEST CONCERN WHERE
ANTHRACYCLINES ARE USED FOR CURATIVE
OR ADJUVANT REGIMEN
• IN CHILDREN, LATE TOXICITY IS LV
DYSFUNCTION, CARDIOMYOPATHY(57%)
CLINICAL MANIFISTATIONS
• LATE HEART FAILURE IS INCREASED IN ELDERLY
WOMEN TREATED WITH ADJUVANT CHEMO
CONTAINING ANTHRACYCLINES COMPARED
TO NOT TREATED WITH THEM
• REGARDLESS OF TIMING, CHRONIC
CARDIOMYOPATHY BEGINS WITH
ASYMPTOMATIC DIASTOLIC OR SYSTOLIC
DYSFUNCTION, PROGRESSING THE CHF
CLINICAL MANIFISTATIONS
• ALTHOUGH TREATABLE, CUMULATIVE
CARDIOTOXICITY IS A RESULT OF PERMANENT
LOSS OF CARADIOMYOCYTES AND GENERALLY
NOT REVERSIBLE
MECHANISMS
• ALTHOUGH ANTHRACYCLINE RELATED
CARDIOTOXICITY IS WELL KNOWN THE
MECHANISM IS NOT
• OVEREXPRESSION OF FREE RADICAL
SCAVENGERS
• INHIBITION OF FORMATION OF
PEROXYNITRATE
RISK FACTORS
• STRONGEST PREDICTOR IS CUMULATIVE DOSE
• HOWEVER, AGE AT TIME OF DRUG EXPOSURE,
CONCOMITANT ADMINISTRATION OF OTHER
CARDIOTOXIC AGENTS(PACLITAXEL AND
TRASTUZUMAB) OR CHEST RADIATION OR
PREEXISTING CV DISEASE ALSO INCREASE RISK
• LONG TERM SURVIVAL IS A RISK!-PROVEN THAT
DETERIORATION OF CARDIAC FUNCTION OCCURS UP
TO 30 YEARS
CUMULATIVE DOSE
• IN ONE STUDY 88% OF PTS TREATED WITH ANTHRACYCLINES
DEVELOPED SYMPTOMATIC HEART FAILURE
• 0.14% RECEIVED< 400 MG/M2
• 7% RECEIVED 550 MG/M2
• 18% BEYOND 700 MG/M2
• DOXORUBICIN RELATED CARDIOTOXICITY IS UNDERESTIMATED. 26%
PTS RECEIVING 550MG/M2 DEVELOPED CHF
CUMULATIVE DOSING
• THEREFORE IT IS GENERALLY ACCEPTED
CUMULATIVE DOXORUBICIN DOSES BE
LIMITED TO 450-500 MG/M2
ALTHOUGH LIMITING THE LIFETIME
CUMULATIVE DOSE OF ANTHRACYCLINES IS
IMPORTANT TO PREVENTION, SURVEILLANCE OF
MYOCARDIAL FUNCTION DURING AND AFTER
THERAPY, WITH EARLY DETECTION OF ADVERSE
CARDIAC EFFECTS REMAINS THE PRINCIPAL
METHOD OF PREVENTING ANTHRACYCLINE
CARDIOTOXICITY.
PRE-TREATMENT
• Beta-blockers- carvedilol may be benefit. 50
pts. treated with anthracycline. Half got
carvedilol. Echo after 6 months showed no
change in LVEF after chemo. Pts. assigned to
placebo had 17% reduction in EF.
• High risk pts. needing anthracycline chemo
may be considered for beta blocker therapy.
ACE INHIBITORS
• NO DEFINITIVE DATA TO SUGGEST
PRETREATMENT WITH ACE INHIBITORS
CHANGES OUTCOMES.
NONINVASIVE MONITORING OF LVEF
• NO GUIDELINES FOR PRE ASSESSMENT OR
EVALUATION PRIOR TO CHEMO TREATMENT
• RISK ASSESS-IF HIGH, CONSIDER LV
EVALUATION OR CARDIOLOGY CONSULT
• MONITORING OF CARDIAC FUNCTIN IS HIGHLY
RECOMMENDED BEFORE, DURING AND AFTER
ALTHOUGH NO CLEAR GUIDELINES ON
FREQUENCY OR OPTIMAL METHOD OF LVEF
ASSESSMENT ARE GIVEN
LVEF ASSESSMENT
•
•
•
•
•
ECHO-METHOD OF CHOICE
EASY
NO RADIATION
REPRODUCABLE
RNA-EARLY GOLD STANDARD BUT NOW HAS
BEEN REPLACED WITH ECHO
CARDIAC MRI
• SELECT PTS
• USED WHEN ECHO HAS POOR WINDOWS
ECHOCARDIOGRAPHY
•
•
•
•
ANY CLINICAL SUSPISION OF CHANGE
REALLY ONLY EFFECTIVE IN ACUTE TOXICITY
DOESN’T HELP WIT LATENT PERIOD CHANGE
STRESS AND STRAIN RATES MAY BE FUTURE
• JASE-VOLUME 25-NUMBER 11-NOV 2012 PG 1141
– NO CONSENSUS FOR MONITORING BUT DIASTOLIC
FUNCTION, STRAIN AND TISSUE DOPPLER SHOW
PROMISSING FUTURE
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