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ACE INHIBITORS : FROM VENOM
           TO DRUG
            Dr Syed Raza
       MD,MRCP(UK),CCT(UK),DIP.CARD(UK),FCCCP
              Consultant Cardiologist
Objectives

•   Overview of ACEI
•   Indications and Uses
•   Effectiveness and
•   The Evidence
Franklin D Roosevelt – 1940s
Howard Bruenn lamented in the Annals of Internal Medicine, "I have
often wondered what turn the subsequent course of history might have
taken if the modern methods for the control of hypertension had been
available’’
Originally synthesized from
compounds found in pit viper
venom(Sir John Vane -1960s)
Angiotensinogen
                    Renin

         Angiotensin I                   Bradykinin

   Non ACE          ACE     (-)   ACEi     (-)


         Angiotensin II            Inactive Metabolites



   ARB
AT1 Receptor         AT2 Receptor
ACE Inhibitor Groups
A. Sulfhydryl-containing agents:
   – Captopril , the first ACE inhibitor
B. Dicarboxylate-containing agents:
   –   Enalapril
   –   Ramipril
   –   Quinapril
   –   Perindopril
   –   Lisinopril
   –   Benazepril
C. Phosphonate-containing agents:
   – Fosinopril
   – Trandolapril
Clinical Indications for ACEI
•   Hypertension
•   CHF
•   Post MI
•   Diabetes Mellitus
•   Proteinuria
•   Vascular Disease
•   Post - transplant
Additional Benefits of ACEI

• Prevention of diabetes
• Prevention of stroke recurrence
• Prevention of atrial fibrillation
How ACEI is useful in hypertension?
• ACE inhibitors block the conversion of
  angiotensin I to angiotensin II
• Lower arteriolar and renovascular resistance
• Increase venous capacity,
• Increase cardiac output, cardiac index and
  stroke volume.
Which antihypertensive?
       NICE Diabetes Clinical Guideline 66;May 2008. NICE Full Diabetes Guideline;2008



•   First-line BP lowering therapy should be a once-daily, generic ACE
    inhibitor

•   Exceptions to this are:
     – People of African-Caribbean descent
     – Women for whom there is a possibility of
       becoming pregnant
     – For a person with continuing intolerance to an
       ACE inhibitor
Choice of antihypertensive agents

 When implementing blockade of the renin–
 angiotensin system start treatment with an ACE
 inhibitor first then move to an ARB if the ACE
 inhibitor is not tolerated.
Pharmacotherapy –BP Control
• In people without CKD aim to keep the systolic
  blood pressure below 140 mmHg (target range
  120–139 mmHg) and the diastolic blood pressure
  below 90 mmHg.

• In people with CKD and diabetes with urinary
  protein excretion 1 g/24 h or more) aim to keep
  the systolic blood pressure below 130 mmHg
  (target range 120–129 mmHg) and the diastolic
  blood pressure below 80 mmHg
Fixed Drug Combination




► To achieve recommended blood pressure
  goals, it is often necessary to combine two or
  more antihypertensive agents. Is there a
  preferred combination?
Concomitant Use of
                                    Antihypertensive Drugs
          Diuretics                                                                  Beta Blockers




        ACEIs                                                                         Calcium
        ARBs                                                                          Channel
                                                                                      Blockers
                                    α1-Receptor Blockers
                           Less effective                         Particularly effective




Adapted from Chalmers J. Clin Exp Hypertens. 1993;15:1299–1313.
The Moral of the Tale
            As long as we reach
            the objective BP
            below 140/90
            (130/80), it doesn’t
            matter how we get
            there
ALLHAT (JAMA 2002)

“The key message from ALLHAT is that what
 matters most is getting blood pressure
 controlled’’
The Heart Matters – the effect of ACEI


•   Prevents cardiac hypertrophy
•   Limits infarct size
•   Improves cardiac function
•   Improves cardiac metabolism
ACEI in Heart Failure

• ACE inhibitors are recommended to treat HF
  due to systolic dysfunction.
• The benefit of ACE inhibitors has been
  demonstrated in all severities of symptomatic
  HF and in patients with asymptomatic left
  ventricular (LV) dysfunction.
ACE in Heart Failure: the evidence
 A meta-analysis evaluated five trials

• Improvement in symptoms
• A lower total mortality.
• A lower rate of readmission for HF).
ACE Inhibitors for ‘Diastolic’ Heart
             Failure?
• Guidelines for the management of heart
  failure focus on patients with left ventricular
  systolic dysfunction.
• However, guidelines make no
  recommendation for their use in patients with
  heart failure and preserved left ventricular
  systolic function.
ACE inhibitors versus ARBs: comparison of
 practice guidelines and treatment selection


• ACC/AHA Heart Failure guidelines 2005. ACE
  inhibitors should be prescribed to all patients
  with left ventricular systolic dysfunction HF
  (class IA recommendation).
• They recommend ARBs as a "reasonable
  alternative" first-line therapy (class IIA
  recommendation).
ACE inhibitors versus ARBs: comparison of
       practice guidelines : Contd
• ACEI more cost effective
• ARB better tolerated than ACEI
• Deciding factor may be largely patient-
  specific.
Landmark trials with ACE inhibitors in HF

Trial       n      EF%        Drug         Death           Hospitalisation   Follow up   NNT
                                                                                         (death)

CONSENSUS   253    <35%       enalapril    36 vs 50        reduced           1 year      6
1987               (IV)
SOLVD-P     4228   <35        enalapril    trend to        reduced           4 years     104
1992               (I)                     reduction
SOLVD – T   2500   < 40       enalapril    12.3 vs 15.5    reduced           3 years     31
1991               (II-III)
ATLAS       3164   <35        lisinopril   no difference   reduced           4 years     -
1997               (II-IV)
• The ACE inhibitor Enalapril has also been
  shown to reduce cardiac cachexia in patients
  with chronic heart failure
• Cachexia is a poor prognostic sign in patients
  with chronic heart failure. ACE inhibitors are
  now used to reverse frailty and muscle
  wasting in elderly patients without heart
  failure.
Type 2 diabetes
Management of cardiovascular risk factors




     Lending our patients a hand
Can ACEI prevent Diabetes ?
• Several recent studies indicate that ACE
  inhibitor therapy reduces the development of
  type 2 diabetes in persons with essential
  hypertension.

• HOPE, CAPPP, SOLVD, and ALLHAT
• DREAM & ONTARGET = more recent
Path physiology
•   Exact mechanism is not known
•   ACEI reduces oxidative stress
•   Increases insulin sensitivity in the liver
•   Reduces Insulin resistance in muscles
•   Helps in the preservation of islet cells of
    pancreas
ACEI and the Kidneys

Clinical studies have shown ACE inhibitors
reduce the progress of diabetic nephropathy
independently from their blood pressure-
lowering effect.
This action of ACE inhibitors is used in the
prevention of diabetic renal failure.
ACEI and the Kidneys – Contd:
•   Decreases Proteinuria (DM and Non-DM)
•   Beneficial effect on permeability
•   Beneficial effect on size selectivity
•   Slow the Rate of GFR Decline
Intensive Multiple Risk Factor Management Patients with
                                                 Type 2 Diabetes and Microalbuminuria


                                  60        N=160; follow-up=7.8 years
Primary Composite Endpoint* (%)




                                                               Conventional Therapy

                                  40                                                        20% Absolute
                                                                                            Risk Reduction


                                  20                                                        Aggressive treatment of†:
                                                                                            – Microalbuminuria with
                                                                  Intensive Therapy†
                                                                                              ACEIs, ARBs, or combination
                                                                                            – Hypertension
                                                                                            – Hyperglycemia
                                                                                            – Dyslipidemia
                                       12     24    36    48     60      72   84       96   – Secondary prevention of CVD

                                                     Months of Follow-Up

 Primary composite endpoint: conventional therapy (44%) and intensive therapy (24%).
*
 Death from CV causes, nonfatal MI, CABG, PCI, nonfatal stroke, amputation, or surgery for peripheral atherosclerotic
  artery disease.
†
 Behavior modification and pharmacologic therapy.
 Adapted from Gaede P, et al. N Eng J Med. 2003;348:383-393.
                                      Med.
Vascular Protection
                 ACE inhibitor Trials




© Continuing Medical Implementation ®   …...bridging the care gap
HOPE (Heart Outcome Prevention
         Evaluation)
•   9297 Patients
•   Age >55
•   DM + 1 other CV factor
•   Normal EF (>40%)
•   Ramipril (10mg) vs. Placebo
HOPE (Primary endpoints)
• Death (CV) - 6.1 vs 8.1   P<0.001 RR=0.75
• MI - 9.9 vs 12.2          P<0.001 RR=0.80
• Stroke - 3.4 vs 4.9       P<0.001 RR=0.69
HOPE (secondary endpts.)
•   Death                   10.4 vs 12.2
•   Revascularization       16.0 vs 18.6
•   Cardiac arrest          0.8 vs 1.2
•   Heart Failure           7.4 vs 9.4
•   DM complications        6.2 vs 7.4



    * all statistically significant
Study rationale and design
EUROPA
   Randomised 12,218 patients with stable coronary
    artery disease (CAD) and a broad range of risk for
    cardiovascular complications
   Showed the benefit of long-term (mean 4.2 years)
    ACE-inhibition (perindopril 8 mg/day)
Study end points
Primary endpoint
     Non Fatal MI, Cardiac arrest and CV mortality


Secondary endpoints


     Heart failure
     Revascularisation (PCI/CABG)
     Stroke
Primary endpoint
                % CV death, MI or cardiac arrest
14

12          RRR: 20%                             Placebo
            p = 0.0003
10
                                                Perindopril
8

6

4

2

0
     0      1         2        3    4      5   Years

 Placebo annual event rate: 2.4%
Primary endpoint
            CV death, MI or cardiac arrest
                RRR: 20% [95% CI : 9 - 29]
No events
      700
                                             9.9%
      600
                      8.0%                   603
      500

      400              488
      300

      200

      100

        0
                    Perindopril          Placebo
                      (6 110)                (6 108)
The Prevention of Events with
   Angiotensin Converting Enzyme
       Inhibition (PEACE) Trial
    A double-blind, placebo-controlled, randomized trial
 Sponsored by the National Heart, Lung, and Blood Institute
Hypothesis

To test whether ACE inhibitor therapy,
 when added to modern conventional
 therapy, reduces CV mortality, MI, or
 coronary revascularization in low-risk,
  stable CAD patients with normal or
      mildly reduced LV function.
Inclusion Criteria

• Age ≥ 50 years
• Coronary artery disease
  – MI, or
  – CABG or PCI, or
  – Coronary angiogram with obstruction of ≥50%
    luminal diameter in at least one native vessel
• LVEF > 40%
• Tolerated 2 week run-in of 2 mg/day
  trandolapril
Change in Systolic Blood
                                              Pressure
                          0
Pressure Change (mm Hg)




                          -1                                  ∆=-1.4
                          -2
                          -3
                          -4
                          -5
                                                              ∆=-4.4, p<0.001
                          -6
                                   0       1        2         3         4         5   6
                               Baseline=       Time Since Randomization (Years)
                               133±17
                                                    Placebo       Trandolapril
Change in Diastolic
                                             Blood Pressure
                           0
Pressure Change (mm Hg)




                          -1
                          -2                                   ∆=-2.3
                          -3
                          -4
                          -5
                                                               ∆=-3.6, p<0.001
                          -6
                          -7
                                   0        1        2         3         4         5   6

                               Baseline=        Time Since Randomization (Years)
                               78±10
                                                     Placebo       Trandolapril
PEACE Trial: All Death
      All-Cause Death

             p = 0.13              • A slight reduction in all-
                                   cause death seen in the
10                                 Trandolapril arm was not
                                   statistically significant
                        8.1
8    7.2


6

4

2

0
     Trandolapril        Placebo

                                               Presented at AHA 2004
PEACE Trial: Primary Endpoint
            The individual components of the primary endpoint were also
                  equivalent in the Trandolapril and placebo groups


    16                                                          p=0.65

                                                                12.4         12.0
    12                                        p=0.24
                            p=1.00
     8    p=0.67                                     7.1
                                              6.5
%




                            5.3      5.3

          3.5    3.7
     4



     0

         Cardio death      Nonfatal MI          CABG                   PCI
                         Trandolapril           Placebo

                                                               Presented at AHA 2004
IMAGINE
Trial design: IMAGINE was a double-blinded, randomized, placebo-controlled trial
designed to test the effects of early ACE inhibitor initiation (quinapril 10 or 20 mg/day within
7 to 10 days) after CABG in patients with preserved LV function, and no clear indication for
ACE inhibitor therapy.

                                                  CONCLUSION
            CV death or cardiac arrest
                                                  •In patients at low risk of CV
                      (p = 0.57)
                                                   events after CABG, routine
                                                   early initiation of ACE
      0.6
    0.6         0.5
                                   0.4
                                                   inhibitor therapy does not
      0.4
    0.4                                            appear to improve clinical
%
      0.2
    0.2                                            outcome up to 3 years after
                                                   CABG
                                                  Conclusions
      00


             Quinapril              Placeb
            (n = 1,280)                o
                                     (n =
                                    1,273)
THANK YOU

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Ace inhibitor

  • 1. ACE INHIBITORS : FROM VENOM TO DRUG Dr Syed Raza MD,MRCP(UK),CCT(UK),DIP.CARD(UK),FCCCP Consultant Cardiologist
  • 2. Objectives • Overview of ACEI • Indications and Uses • Effectiveness and • The Evidence
  • 3. Franklin D Roosevelt – 1940s Howard Bruenn lamented in the Annals of Internal Medicine, "I have often wondered what turn the subsequent course of history might have taken if the modern methods for the control of hypertension had been available’’
  • 4. Originally synthesized from compounds found in pit viper venom(Sir John Vane -1960s)
  • 5. Angiotensinogen Renin Angiotensin I Bradykinin Non ACE ACE (-) ACEi (-) Angiotensin II Inactive Metabolites ARB AT1 Receptor AT2 Receptor
  • 6. ACE Inhibitor Groups A. Sulfhydryl-containing agents: – Captopril , the first ACE inhibitor B. Dicarboxylate-containing agents: – Enalapril – Ramipril – Quinapril – Perindopril – Lisinopril – Benazepril C. Phosphonate-containing agents: – Fosinopril – Trandolapril
  • 7. Clinical Indications for ACEI • Hypertension • CHF • Post MI • Diabetes Mellitus • Proteinuria • Vascular Disease • Post - transplant
  • 8. Additional Benefits of ACEI • Prevention of diabetes • Prevention of stroke recurrence • Prevention of atrial fibrillation
  • 9. How ACEI is useful in hypertension? • ACE inhibitors block the conversion of angiotensin I to angiotensin II • Lower arteriolar and renovascular resistance • Increase venous capacity, • Increase cardiac output, cardiac index and stroke volume.
  • 10. Which antihypertensive? NICE Diabetes Clinical Guideline 66;May 2008. NICE Full Diabetes Guideline;2008 • First-line BP lowering therapy should be a once-daily, generic ACE inhibitor • Exceptions to this are: – People of African-Caribbean descent – Women for whom there is a possibility of becoming pregnant – For a person with continuing intolerance to an ACE inhibitor
  • 11. Choice of antihypertensive agents When implementing blockade of the renin– angiotensin system start treatment with an ACE inhibitor first then move to an ARB if the ACE inhibitor is not tolerated.
  • 12. Pharmacotherapy –BP Control • In people without CKD aim to keep the systolic blood pressure below 140 mmHg (target range 120–139 mmHg) and the diastolic blood pressure below 90 mmHg. • In people with CKD and diabetes with urinary protein excretion 1 g/24 h or more) aim to keep the systolic blood pressure below 130 mmHg (target range 120–129 mmHg) and the diastolic blood pressure below 80 mmHg
  • 13. Fixed Drug Combination ► To achieve recommended blood pressure goals, it is often necessary to combine two or more antihypertensive agents. Is there a preferred combination?
  • 14. Concomitant Use of Antihypertensive Drugs Diuretics Beta Blockers ACEIs Calcium ARBs Channel Blockers α1-Receptor Blockers Less effective Particularly effective Adapted from Chalmers J. Clin Exp Hypertens. 1993;15:1299–1313.
  • 15. The Moral of the Tale As long as we reach the objective BP below 140/90 (130/80), it doesn’t matter how we get there
  • 16. ALLHAT (JAMA 2002) “The key message from ALLHAT is that what matters most is getting blood pressure controlled’’
  • 17. The Heart Matters – the effect of ACEI • Prevents cardiac hypertrophy • Limits infarct size • Improves cardiac function • Improves cardiac metabolism
  • 18. ACEI in Heart Failure • ACE inhibitors are recommended to treat HF due to systolic dysfunction. • The benefit of ACE inhibitors has been demonstrated in all severities of symptomatic HF and in patients with asymptomatic left ventricular (LV) dysfunction.
  • 19. ACE in Heart Failure: the evidence A meta-analysis evaluated five trials • Improvement in symptoms • A lower total mortality. • A lower rate of readmission for HF).
  • 20.
  • 21. ACE Inhibitors for ‘Diastolic’ Heart Failure? • Guidelines for the management of heart failure focus on patients with left ventricular systolic dysfunction. • However, guidelines make no recommendation for their use in patients with heart failure and preserved left ventricular systolic function.
  • 22. ACE inhibitors versus ARBs: comparison of practice guidelines and treatment selection • ACC/AHA Heart Failure guidelines 2005. ACE inhibitors should be prescribed to all patients with left ventricular systolic dysfunction HF (class IA recommendation). • They recommend ARBs as a "reasonable alternative" first-line therapy (class IIA recommendation).
  • 23. ACE inhibitors versus ARBs: comparison of practice guidelines : Contd • ACEI more cost effective • ARB better tolerated than ACEI • Deciding factor may be largely patient- specific.
  • 24. Landmark trials with ACE inhibitors in HF Trial n EF% Drug Death Hospitalisation Follow up NNT (death) CONSENSUS 253 <35% enalapril 36 vs 50 reduced 1 year 6 1987 (IV) SOLVD-P 4228 <35 enalapril trend to reduced 4 years 104 1992 (I) reduction SOLVD – T 2500 < 40 enalapril 12.3 vs 15.5 reduced 3 years 31 1991 (II-III) ATLAS 3164 <35 lisinopril no difference reduced 4 years - 1997 (II-IV)
  • 25. • The ACE inhibitor Enalapril has also been shown to reduce cardiac cachexia in patients with chronic heart failure • Cachexia is a poor prognostic sign in patients with chronic heart failure. ACE inhibitors are now used to reverse frailty and muscle wasting in elderly patients without heart failure.
  • 26. Type 2 diabetes Management of cardiovascular risk factors Lending our patients a hand
  • 27. Can ACEI prevent Diabetes ? • Several recent studies indicate that ACE inhibitor therapy reduces the development of type 2 diabetes in persons with essential hypertension. • HOPE, CAPPP, SOLVD, and ALLHAT • DREAM & ONTARGET = more recent
  • 28. Path physiology • Exact mechanism is not known • ACEI reduces oxidative stress • Increases insulin sensitivity in the liver • Reduces Insulin resistance in muscles • Helps in the preservation of islet cells of pancreas
  • 29. ACEI and the Kidneys Clinical studies have shown ACE inhibitors reduce the progress of diabetic nephropathy independently from their blood pressure- lowering effect. This action of ACE inhibitors is used in the prevention of diabetic renal failure.
  • 30. ACEI and the Kidneys – Contd: • Decreases Proteinuria (DM and Non-DM) • Beneficial effect on permeability • Beneficial effect on size selectivity • Slow the Rate of GFR Decline
  • 31. Intensive Multiple Risk Factor Management Patients with Type 2 Diabetes and Microalbuminuria 60 N=160; follow-up=7.8 years Primary Composite Endpoint* (%) Conventional Therapy 40 20% Absolute Risk Reduction 20 Aggressive treatment of†: – Microalbuminuria with Intensive Therapy† ACEIs, ARBs, or combination – Hypertension – Hyperglycemia – Dyslipidemia 12 24 36 48 60 72 84 96 – Secondary prevention of CVD Months of Follow-Up Primary composite endpoint: conventional therapy (44%) and intensive therapy (24%). * Death from CV causes, nonfatal MI, CABG, PCI, nonfatal stroke, amputation, or surgery for peripheral atherosclerotic artery disease. † Behavior modification and pharmacologic therapy. Adapted from Gaede P, et al. N Eng J Med. 2003;348:383-393. Med.
  • 32. Vascular Protection ACE inhibitor Trials © Continuing Medical Implementation ® …...bridging the care gap
  • 33. HOPE (Heart Outcome Prevention Evaluation) • 9297 Patients • Age >55 • DM + 1 other CV factor • Normal EF (>40%) • Ramipril (10mg) vs. Placebo
  • 34. HOPE (Primary endpoints) • Death (CV) - 6.1 vs 8.1 P<0.001 RR=0.75 • MI - 9.9 vs 12.2 P<0.001 RR=0.80 • Stroke - 3.4 vs 4.9 P<0.001 RR=0.69
  • 35. HOPE (secondary endpts.) • Death 10.4 vs 12.2 • Revascularization 16.0 vs 18.6 • Cardiac arrest 0.8 vs 1.2 • Heart Failure 7.4 vs 9.4 • DM complications 6.2 vs 7.4 * all statistically significant
  • 37. EUROPA  Randomised 12,218 patients with stable coronary artery disease (CAD) and a broad range of risk for cardiovascular complications  Showed the benefit of long-term (mean 4.2 years) ACE-inhibition (perindopril 8 mg/day)
  • 38. Study end points Primary endpoint  Non Fatal MI, Cardiac arrest and CV mortality Secondary endpoints  Heart failure  Revascularisation (PCI/CABG)  Stroke
  • 39. Primary endpoint % CV death, MI or cardiac arrest 14 12 RRR: 20% Placebo p = 0.0003 10 Perindopril 8 6 4 2 0 0 1 2 3 4 5 Years Placebo annual event rate: 2.4%
  • 40. Primary endpoint CV death, MI or cardiac arrest RRR: 20% [95% CI : 9 - 29] No events 700 9.9% 600 8.0% 603 500 400 488 300 200 100 0 Perindopril Placebo (6 110) (6 108)
  • 41.
  • 42. The Prevention of Events with Angiotensin Converting Enzyme Inhibition (PEACE) Trial  A double-blind, placebo-controlled, randomized trial  Sponsored by the National Heart, Lung, and Blood Institute
  • 43. Hypothesis To test whether ACE inhibitor therapy, when added to modern conventional therapy, reduces CV mortality, MI, or coronary revascularization in low-risk, stable CAD patients with normal or mildly reduced LV function.
  • 44. Inclusion Criteria • Age ≥ 50 years • Coronary artery disease – MI, or – CABG or PCI, or – Coronary angiogram with obstruction of ≥50% luminal diameter in at least one native vessel • LVEF > 40% • Tolerated 2 week run-in of 2 mg/day trandolapril
  • 45. Change in Systolic Blood Pressure 0 Pressure Change (mm Hg) -1 ∆=-1.4 -2 -3 -4 -5 ∆=-4.4, p<0.001 -6 0 1 2 3 4 5 6 Baseline= Time Since Randomization (Years) 133±17 Placebo Trandolapril
  • 46. Change in Diastolic Blood Pressure 0 Pressure Change (mm Hg) -1 -2 ∆=-2.3 -3 -4 -5 ∆=-3.6, p<0.001 -6 -7 0 1 2 3 4 5 6 Baseline= Time Since Randomization (Years) 78±10 Placebo Trandolapril
  • 47. PEACE Trial: All Death All-Cause Death p = 0.13 • A slight reduction in all- cause death seen in the 10 Trandolapril arm was not statistically significant 8.1 8 7.2 6 4 2 0 Trandolapril Placebo Presented at AHA 2004
  • 48. PEACE Trial: Primary Endpoint The individual components of the primary endpoint were also equivalent in the Trandolapril and placebo groups 16 p=0.65 12.4 12.0 12 p=0.24 p=1.00 8 p=0.67 7.1 6.5 % 5.3 5.3 3.5 3.7 4 0 Cardio death Nonfatal MI CABG PCI Trandolapril Placebo Presented at AHA 2004
  • 49. IMAGINE Trial design: IMAGINE was a double-blinded, randomized, placebo-controlled trial designed to test the effects of early ACE inhibitor initiation (quinapril 10 or 20 mg/day within 7 to 10 days) after CABG in patients with preserved LV function, and no clear indication for ACE inhibitor therapy. CONCLUSION CV death or cardiac arrest •In patients at low risk of CV (p = 0.57) events after CABG, routine early initiation of ACE 0.6 0.6 0.5 0.4 inhibitor therapy does not 0.4 0.4 appear to improve clinical % 0.2 0.2 outcome up to 3 years after CABG Conclusions 00 Quinapril Placeb (n = 1,280) o (n = 1,273)

Notas do Editor

  1. Diabetes - Risk Management &amp; New Drugs 15/06/12 National Prescribing Centre
  2. Concomitant Use of Antihypertensive Drugs Antihypertensive drugs typically are very complimentary; however, there are some combinations which tend to be more favorable and are shown in this slide by the yellow lines. Although drug combinations shown by the pink line can be used, they tend to be less complimentary and frequently do not result in an additive reductions in BP. Reference: Chalmers J. The Place of Combination Therapy in the Treatment of Hypertension in 1993. Clin Exp Hypertens. 1993;15:1299-1313.
  3. Diabetes - Risk Management &amp; New Drugs 15/06/12 National Prescribing Centre
  4. 10/24/97 1 J:\\artem\\F151097\\Europa