аЯрЁБс>ўџ PTўџџџKLMNO~џџџџџџџџџџџџџџџџџџџџџџџџџџџџџџџџџџџџџџџџџџџџџџџџџџџџџџџџџџџџџџџџџџџџџџџџџџџџџџџџџџџџџџџџџџџџџџџџџџџџџџџџџџџџџџџџџџџџџџџџџџџџџџџџџџџџџџџџџџџџџџџџџџџџџџџџџџџџџџџџџџџџџџџџџџџџџџџџџџџџџџџџџџџџџџџџџџџџџџџџџџџџџџџџџџџџџџџџџџџџџџџџџџџџџџџџџџџџџџџџџџџџџџџџџџџџџџџџџџџџџџџџџџџџџџџџџџџџџџџџџџџџџџџџџџџџџџџџџџџџџџџџџџџџџџџџџџџџџџџџџџџџџџџџџџџџџџџџџџџџџџџџџџџџџџџџџџџџџџџџџџџџџџџџџџџџџџџџџџџџџџџџџџџџџџџџџџџџџџџџџџџџџџџџџџџџьЅСР №ПvРbjbjWйWй .T5Г5ГЖиџџџџџџЗNNЈ Ј Ј Ј Ј џџџџМ М М 8є TH$ќМ Н…"D'>‚/FШ/Ш/0<1>z1Ž1 …………………$п‡В‘ŠІ6…Ј š1<1<1š1š16…Ј Ј Ш/04K…6’=’=’=š1FЈ Ш/Ј 0…’=š1…’=’=jОouШ/@џџџџPБ0S.Яџџџџр1Žжq4ќ„…<Н… r7‹n2n7‹duuо7‹Ј ьvš1š1’=š1š1š1š1š16…6…м7Жš1š1š1Н…š1š1š1š1џџџџџџџџџџџџџџџџџџџџџџџџџџџџџџџџџџџџџџџџџџџџџџџџџџџџџџџџџџџџџџџџџџџџ7‹š1š1š1š1š1š1š1š1š1N n:  Angiotensin II Receptor Antagonists: Recommendations for Use Update February 2014 VA Pharmacy Benefits Management Services, Medical Advisory Panel, and VISN Pharmacist Executives The following recommendations are based on medical evidence, clinician input, and expert opinion. The content of the document is dynamic and will be revised as new information becomes available. The purpose of this document is to assist practitioners in clinical decision-making, to standardize and improve the quality of patient care, and to promote cost-effective drug prescribing. The clinician should utilize this guidance and interpret it in the clinical context of the individual patient. Refer to the VA/DoD Angiotensin II Receptor Antagonists Drug Class Review at  HYPERLINK "http://www.pbm.va.gov" www.pbm.va.gov or  HYPERLINK "https://vaww.cmopnational.va.gov/cmop/pbm" https://vaww.cmopnational.va.gov/cmop/pbm for additional discussion and for recommendations on dosing, potential drug interactions, side effects, and precautions of the angiotensin II receptor antagonists. Recommendations for Use of an Angiotensin II Receptor Antagonist in Patients with Heart Failure with Reduced Left Ventricular Ejection Fraction Patients with heart failure (HF) with reduced left ventricular ejection fraction (HFrEF) with current or prior symptoms of HF should be maximized on therapy with agents such as an angiotensin-converting enzyme inhibitor (ACEI), beta-adrenergic blocker, diuretic, and aldosterone antagonist, as indicated. An angiotensin II receptor antagonist (ARB) is recommended in patients with HFrEF [or HF/evidence of systolic dysfunction after acute myocardial infarction (MI)] who are intolerant to an ACEI* Addition of an ARB may be considered in patients with HFrEF and persistent symptoms who are on treatment with an ACEI and beta-adrenergic blocker, where an aldosterone antagonist is not indicated or not tolerated, and if it is determined the benefit outweighs the potential risk for adverse events. Combination therapy with an ACEI and ARB in patients with HFrEF/evidence of systolic dysfunction after acute MI is not recommended due to an increased risk for adverse events without a survival benefit Recommendations for Use of an Angiotensin II Receptor Antagonist in Patients with Chronic Kidney Disease Guidelines recommend the use of either an ACEI or ARB in patients with diabetes mellitus (DM) and chronic kidney disease (CKD) with macroalbuminuria or nondiabetic CKD with macroalbuminuria, in patients where antihypertensive therapy is indicated. Use of an ACEI or ARB is suggested in patients with DM and CKD with microalbuminuria or nondiabetic CKD with microalbuminuria where antihypertensive therapy is indicated, or in normotensive patients with DM and CKD and albuminuria. Treatment with an ARB has been shown to reduce the combined endpoint of increasing serum creatinine (sCr), end-stage renal disease (ESRD), and death in patients with type 2 DM and nephropathy with hypertension (HTN) and/or on antihypertensive medications. As such, an ARB is a treatment option in this patient population. An ARB may be considered an alternative first-line treatment option in patients with type 2 DM and nephropathy (e.g., macroalbuminuria) with HTN An ARB may be considered in patients with DM and CKD with albuminuria, or nondiabetic kidney disease with albuminuria when antihypertensive therapy is indicated Combination therapy with an ACEI and ARB is not recommended due to reports of increased adverse events without evidence of long-term outcome benefit compared to monotherapy; in the rare circumstance where combination therapy is used (e.g., nephrotic syndrome), this should only be considered after evaluation of risk vs. benefit and in consultation with Nephrology  Recommendations for an Angiotensin II Receptor Antagonist in Patients with Hypertension An ARB is effective for lowering blood pressure in the treatment of hypertension. There have been mixed results with an ARB and their effect on CV morbidity and mortality in patients with HTN and/or cardiovascular (CV) disease or high CV risk [reduced CV morbidity and mortality vs. treatment with a beta-blocker or conventional treatment, no difference compared to an ACEI or dihydropyridine calcium channel blocker (CCB), and a nonsignificant reduction compared to placebo in patients with CV disease or high risk DM who were ACEI intolerant]. Taking the above into consideration along with the overall strong evidence for treatment with an ACEI, providers may prefer use of an ACEI prior to considering treatment with an ARB; however, as per recent clinical practice guidelines, use of an ARB may also be an option for the management of patients with HTN. A low cost ARB may be considered an option for the treatment of HTN Combination therapy with an ACEI and ARB for the treatment of HTN is not recommended * Intolerant to an ACEI = unable to tolerate an ACEI due to cough or other non life-threatening reason. It is unknown if an ARB can be safely used as an alternative in patients who develop kidney dysfunction, hyperkalemia, or angioedema with an ACEI, or where treatment with an ACEI is limited due to kidney dysfunction, as these adverse events have also occurred with the use of an ARB [refer to Executive Summary and Discussion for review of the literature] Executive Summary (Refer to Discussion section for review of the literature) Summary of recommendations for use of an angiotensin II receptor antagonist in patients with HF with Reduced LVEF with or without recent MI Heart Failure The ACEIs have well documented beneficial effects in the treatment and prevention of HF. The absence of data that ARBs are superior to ACEIs in patients with HFrEF precludes them as the drug of choice in HF. There is good evidence that an ARB is beneficial in reducing CV mortality and HF hospitalizations when used in patients who are intolerant to an ACEI and are therefore recommended in this setting. There are conflicting data as to whether combination of an ARB with an ACEI, with or without a beta-adrenergic blocker, is of overall benefit in the management of patients with HFrEF. One trial reported results that addition of an ARB to treatment with an ACEI (93%) and beta-adrenergic blocker (35%) reduced the primary endpoint of combined morbidity and mortality in patients with HFrEF, but showed an increase in mortality compared to placebo in the subgroup of patients who received an ARB, ACEI, and beta-adrenergic blocker. Results from another trial demonstrated a reduction in combined CV mortality and HF hospitalizations when an ARB was added to therapy with an ACEI (100%) and a beta-adrenergic blocker (55%), without an increase in mortality in the subgroup of patients receiving all three medication classes. The difference in all-cause mortality or combined CV mortality and HF hospitalizations was not statistically significant with an ARB in the subgroup of patients on an ACEI without beta-adrenergic blocker therapy; whereas, another trial demonstrated a statistically significant reduction in combined morbidity and mortality with an ARB and ACEI without a beta-adrenergic blocker, but not a difference in mortality. Data from one meta-analysis showed that all-cause mortality with the combination of an ARB and ACEI in patients with HF was not statistically significantly different compared to an ACEI alone, but was beneficial in decreasing HF hospitalizations. In another meta-analyses, addition of an aldosterone antagonist decreased mortality, CV death, HF hospitalizations, and the composite CV death or HF hospitalizations; whereas there was no difference in these outcomes when an ARB was added to standard therapy. There was an increased risk for hyperkalemia with the addition of an aldosterone antagonist, and an increase in the risk for hyperkalemia, renal failure, and hypotension when an ARB was added to standard therapy. Guidelines recommend that combination therapy with an ACEI and ARB may be considered in patients with HFrEF and persistent symptoms who are on treatment with an ACEI and beta-adrenergic blocker, where an aldosterone antagonist is not indicated or not tolerated. In addition, patients should be closely monitored if combination therapy with two or more agents that act at the renin-angiotensin-aldosterone system is initiated. Heart Failure with Acute Myocardial Infarction Results of outcome trials are not available to provide enough evidence in favor of recommending an ARB over an ACEI in patients with acute MI and HF/evidence of systolic dysfunction. An ARB should be used in this patient population who are ACEI intolerant. The combination of an ARB with an ACEI did not demonstrate a statistically significant improvement in all-cause mortality or CV endpoints compared to an ARB alone and resulted in an increase in adverse events; therefore combination therapy with an ACEI and ARB is not recommended in this patient population. Summary of recommendations for use of an angiotensin II receptor antagonist in patients with CKD Type 2 Diabetic Nephropathy There is good evidence that treatment with an ARB in patients with type 2 DM with nephropathy (with HTN or on additional antihypertensive medications) reduced the composite endpoints of doubling sCr, ESRD, or death. The ACEIs have been shown to decrease surrogate endpoints in this patient population, with results from one comparison trial in patients with early nephropathy demonstrating an ARB to be noninferior to treatment with an ACEI. Chronic Kidney Disease with or without Diabetes There is good evidence that in patients with type 1 DM nephropathy, an ACEI decreases the rate of decline in kidney function and reduces the combined risk of death, dialysis, or transplantation; and in patients with type 1 or 2 DM and microalbuminuria or nondiabetic kidney disease, an ACEI slows the progression of kidney disease. Treatment with an ARB has also been shown to prevent the decline in kidney function in patients with type 2 DM and microalbuminuria. In general, guidelines suggest the use of either an ACEI or ARB in patients with DM and CKD with albuminuria or nondiabetic kidney disease with microalbuminuria (Level 2D) or macroalbuminuria (Level 1B Recommendation). Combination therapy with an ACEI and ARB is not recommended due to reports of increased adverse events without evidence of long-term outcome benefit compared to monotherapy; in the rare circumstance where combination therapy is used (e.g., nephrotic syndrome), this should only be considered after evaluation of the risk vs. benefit and in consultation with a nephrologist. Although combination therapy has been shown to further reduce proteinuria compared to monotherapy; combination therapy with an ACEI and ARB increased the secondary endpoint of risk for dialysis, doubling sCr, and death, and also increased the risk for hypotension and hyperkalemia, when compared to an ACEI alone in patients with vascular disease or high risk DM. In patients with diabetic nephropathy, combination with an ACEI and ARB was associated with an increased risk for acute kidney injury and hyperkalemia, without a significant improvement in kidney outcomes or mortality, compared to monotherapy. Summary of recommendations for use of an angiotensin II receptor antagonist in patients with Hypertension According to clinical guideline recommendations used by VA (pending update), thiazide-type diuretics are recommended as initial therapy for most patients with uncomplicated HTN; another class of antihypertensive agents reported to have benefits in reducing morbidity or mortality should be considered in patients who have a contraindication to or are inadequately controlled on a thiazide-type diuretic. These agents may be used together or in combination with other selected agents to achieve goal blood pressure. Several clinical practice guideline updates have recently been published which include varying recommendations for an ACEI or ARB depending on the patient’s age, race, or concomitant DM or CKD. A low cost ARB may be considered a treatment option in patients with HTN. Combination therapy with an ACEI and ARB for the treatment of HTN is not recommended. Additional considerations in patients with ACEI intolerance ACEI Induced Cough Use of an ARB may be considered in patients who have a specific indication for an ACEI (e.g., systolic HF, evidence of HF with recent MI, DM and CKD with proteinuria or nonDM CKD with proteinuria) where an ARB has either been reported to be similar to an ACEI or demonstrated a reduction in long-term outcomes of morbidity and mortality in a similar patient population and where the patient is unable to tolerate an ACEI due to cough. Patients being treated with an ACEI for the management of HTN who develop cough associated with an ACEI may experience improvement if switched to fosinopril; or consideration of treatment with an ARB may be appropriate. Angioedema An ARB should be used with caution in patients who have previously experienced angioedema on an ACEI, taking into consideration risk vs. benefit of therapy. Hyperkalemia It is unclear if treatment with an ARB is an appropriate alternative in patients who develop hyperkalemia with an ACEI since they may experience the same adverse effect with an ARB. An alternative class of antihypertensive agent is recommended or the addition of a diuretic may be considered to offset the hyperkalemia. If use of a diuretic is contraindicated or is not effective, an ARB may be considered instead of an ACEI, under close monitoring, in patients with moderate kidney dysfunction who develop hyperkalemia on an ACEI and who have an indication for an ACEI. Kidney Failure It is unknown if an ARB can be used as an alternative in patients where treatment with an ACEI is limited due to kidney dysfunction or in a patient who develops kidney dysfunction as a result of treatment with an ACEI. As with the ACEIs, similar precautions are recommended for the ARBs in patients with renal artery stenosis. Discussion Heart Failure Discussion: According to the American College of Cardiology Foundation and American Heart Association (ACCF/AHA) guidelines1 and the VA PBM-MAP The Pharmacologic Management of Chronic Heart Failure (refer to document located under Clinical Guidance/VA National Clinical Practice Guidelines at  HYPERLINK "http://www.pbm.va.gov" www.pbm.va.gov or  HYPERLINK "http://vaww.pbm.va.gov" http://vaww.pbm.va.gov), an ARB is recommended in patients with HFrEF (i.e., clinical diagnosis of HF and LVEF < 40%) on standard therapy who are unable to tolerate therapy with an ACEI. Combination therapy with an ARB and an ACEI may be considered to decrease HF hospitalizations;1-4 however, there are conflicting data as to the effect of this combination on all-cause mortality.2-4 In addition, patients with New York Heart Association (NYHA) class II to IV HF from reduced left ventricular ejection fraction (LVEF) < 35%, who are on standard therapy for HFrEF should be considered as a candidate for an aldosterone antagonist (provided the patient does not have significant kidney impairment [sCr > 2.5 mg/dL or creatinine clearance < 30 mL/min] and has normal potassium levels), as treatment with an aldosterone antagonist was shown to improve symptoms, decrease hospitalizations for worsening HF, and decrease mortality in this patient population.5,6 Guidelines recommend that combination therapy with an ACEI and ARB may be considered in patients with HFrEF and persistent symptoms who are on treatment with an ACEI and beta-adrenergic blocker, where an aldosterone antagonist is not indicated or not tolerated.7,8 In earlier trials such as Evaluation of Losartan in Elderly Study (ELITE ),9 the ARB losartan (titrated to 50mg once daily) was compared to an ACEI, captopril (titrated to 50mg three times daily), in 722 patients with NYHA class II to IV HF and LVEF < 40%, for 48 weeks. The secondary endpoint of composite death and/or hospitalization for HF occurred in 9.4% of patients on losartan and 13.2% on captopril (32% risk reduction, P=0.075). These results were primarily due to a 46% decrease in all-cause mortality in patients on losartan compared to patients on captopril (P=0.035), largely due to a reduction in sudden cardiac death. The two treatment groups did not differ in the frequency of hospital admissions for HF. NYHA functional class improved significantly and similarly compared to baseline for both groups. The favorable mortality rate in the losartan group was not hypothesized a priori. Therefore, replication of the results was attempted in ELITE II. ELITE II10 enrolled 3,152 HF patients (mean LVEF 31%) to evaluate the effects of losartan 50mg once daily compared to captopril 50mg three times daily (diuretics: 78%; beta-adrenergic blockers: 22%; and digoxin 50%) on overall mortality and cardiac events (sudden cardiac death or resuscitated cardiac arrest) after a mean follow-up of approximately 2 years. There was no significant difference in the primary endpoint of all-cause mortality between the treatment groups. Patients taking captopril experienced a lower incidence of events compared to losartan (event rate 15.9% vs. 17.2%, respectively), but the difference was not statistically significant (P=0.16). There was no difference between the groups in sudden death, HF mortality, MI, stroke, or noncardiovascular deaths. Several researchers speculated that the dose of losartan may have been suboptimal in the trials.11 It was for this reason that the Heart Failure endpoint Evaluation with the Angiotensin II Antagonist Losartan (HEAAL) study12 was undertaken to determine the effect of losartan 50 mg compared with losartan 150 mg on all-cause mortality and HF hospitalizations in 3846 patients with HF and LVEF < 40%, who were intolerant to an ACEI (86% reported intolerance due to cough). Seventy-two percent of patients received concomitant treatment with beta-adrenergic blockers. After a median of 4.7 years of follow-up, treatment with losartan 150 mg (mean 129+39 mg) resulted in a 10% decrease in the risk for death or HF hospitalization compared to patients randomized to losartan 50 mg (mean 46+11 mg) [losartan 150 mg 828 (43.0%) vs. losartan 50 mg 889 (46.3%); HR 0.90 95% CI 0.82-0.99; P=0.027). The secondary endpoint of all-cause mortality did not differ between treatment groups; although, there was a significant reduction in HF hospitalizations in patients treated with the higher dose of losartan (HR 0.87 95% CI 0.76-0.98; P=0.025). Hyperkalemia, hypotension, kidney impairment, and angioedema all occurred more frequently in the losartan 150 mg treatment group compared to the 50 mg dose, with no difference in discontinuations due to these adverse events. Losartan is not currently FDA approved for use in HF with reduced LVEF; the target dose studied in the HEAAL trial is higher than the maximum recommended dose used for other indications. The Valsartan Heart Failure Treatment (Val-HeFT)3 trial included 5,010 patients with NYHA class II (62%), III (36%), or IV (2%) HF (baseline LVEF 27%) on standard therapy (diuretics: 85%; ACEI: 93%; beta-adrenergic blockers: 35%; and digoxin 67%). Patients were randomized to therapy with either valsartan (40mg twice daily, titrated to a target of 160mg twice daily; 84% achieved target dose; mean 254mg per day) or placebo. Mean follow-up was 1.9 years. The two primary endpoints were mortality and the combined endpoint of mortality and morbidity (i.e., cardiac arrest with resuscitation, HF hospitalization, or intravenous inotropic agents or vasodilators for over 4 hours). Overall mortality was similar in the two groups. There was a 13% relative risk reduction in the combined primary endpoint in patients on valsartan compared to placebo. However, death from any cause (as first event) was higher in patients on valsartan compared to patients receiving placebo (14.2% vs. 12.6%, respectively). According to a subgroup analysis, there was an increased risk of mortality (P=0.009) and a trend toward an increased risk of combined morbidity and mortality (P=0.10) in patients receiving valsartan in conjunction with an ACEI and beta-adrenergic blocker. In the subgroup of patients who were on an ACEI without a beta-adrenergic blocker, there was a statistically significant reduction in the combined endpoint of morbidity and mortality (P=0.002) but the difference in all-cause mortality was not statistically significant. Patients who were not on an ACEI or beta-adrenergic blocker experienced a significant reduction in mortality (P=0.012). Patients on valsartan but not on an ACEI (with or without a beta-adrenergic blocker) had a lower risk of death (RR 0.67 95% CI 0.42-1.06) and a lower risk of the combined endpoint (RR 0.56 95% CI 0.39-0.81).3 Another publication of the subanalysis of the 366 patients in Val-HeFT who were not on an ACEI reported a 33% decrease in all-cause mortality (P=0.017) and a 53% decrease in combined morbidity and mortality (P<0.001) in those treated with an ARB compared to placebo.13 FDA approval for valsartan is for treatment of NYHA class II-IV HF and that valsartan significantly reduced hospitalizations for HF. The product information also includes a statement that there is no evidence that valsartan provides added benefits when it is used with an adequate dose of an ACEI. The Candesartan in Heart failure Assessment of Reduction in Mortality and morbidity (CHARM)-Added trial2 randomized 2548 patients with LVEF < 40% (mean LVEF 28%; NYHA class: II 24%; III 73%; IV 3%) to candesartan (61% achieved target dose at 6 months; mean dose 24mg per day) in addition to standard therapy for HF (diuretics: 90%; ACEIs: 100%; beta-adrenergic blockers: 55%; digoxin: 58%; spironolactone: 17%) for 3.4 years. The combined primary endpoint of CV mortality or HF hospitalization was significantly reduced by 15% compared to placebo. The difference in all-cause mortality was not statistically significant. In the subgroup of patients on therapy with candesartan in combination with an ACEI and beta-adrenergic blocker, there was a significant risk reduction in the primary endpoint of CV death or HF hospitalization compared to patients on placebo. The difference in all-cause mortality was not statistically significant. These results differ from the subgroup analysis of patients enrolled in Val-HeFT as described above. The CHARM-Alternative trial14 randomized 2028 patients with LVEF < 40% (mean LVEF 30%; NYHA class: II 48%; III 48%; IV 4%), on standard therapy for HFrEF (diuretics: 85%; beta-adrenergic blockers: 55%; digoxin: 45%; spironolactone: 25%) with a history of ACEI intolerance, to candesartan 4mg once daily titrated to a target dose of 32mg once daily (59% achieved target dose at 6 months; mean dose 23mg per day) or placebo for 2.8 years. Cough was reported in 70% of patients as the reason for ACEI intolerance. The combined primary endpoint of CV mortality or HF hospitalization was reduced by 23% in patients on candesartan compared to placebo. There was not a statistically significant reduction in all-cause mortality. Candesartan received FDA approval for the treatment of NYHA class II-IV HF and LVEF < 40% to reduce the risk of death from cardiovascular causes and to reduce HF hospitalizations. Candesartan is also approved for use in combination with an ACEI. The CHARM-Preserved trial15 enrolled 3023 patients with HF and LVEF > 40% (HFpEF). The reduction in the primary endpoint of CV mortality or HF hospitalizations did not reach statistical significance (P=0.118). The CHARM Overall program16 combined the results of the three CHARM trials above and reported results of treatment with candesartan or placebo over 3 years in 7599 patients with symptomatic HF (NYHA class: II 45%; III 52%; IV 3%) on standard therapy (diuretics: 83%; ACEI: 0-100% depending on the protocol; beta-adrenergic blockers: 55%; digoxin: 43%; spironolactone: 17%). The primary outcome of all-cause mortality was reduced with candesartan (63% achieved target dose at 6 months; mean dose 24mg per day), although the result did not achieve statistical significance. The secondary endpoint of combined CV death or HF hospitalization was significantly reduced by 16% compared to placebo. When data of patients with low LVEF (< 40%) from the CHARM program (i.e., from CHARM Added and CHARM Alternative) were evaluated (N=4576), there was a reduction in the primary endpoint of CV death or HF hospitalization (with a reduction when each endpoint was analyzed separately), as well as a reduction in all-cause mortality (HR 0.88 95% CI 0.79-0.98; P=0.018) with candesartan compared to the placebo group.17 Results of CHARM-Alternative14 and HEAAL12 confirm the recommendation from Val-HeFT3 to use an ARB in patients who are intolerant of an ACEI. The results of CHARM-Added2 support the recommendation that the combination of an ARB with an ACEI and beta-adrenergic blocker may reduce cardiovascular death and HF hospitalizations. The effect of combination therapy with an ARB, ACEI, and beta-adrenergic blocker on all-cause mortality requires further study. A meta-analysis of 38,080 patients reported that use of an ARB in patients with HF reduced all-cause mortality [OR (odds ratio) 0.83 95% CI 0.69-1.00] compared to placebo, although this was influenced largely by data from CHARM-Alternative, and the reduction was not statistically significant when results from this trial were excluded from the analysis. There was a statistically significant reduction in HF hospitalizations (OR 0.64 95% CI 0.53-0.78) with an ARB compared to placebo. When data with an ARB was compared to results with an ACEI, there was not a statistically significant difference in all-cause mortality or HF hospitalizations. The analysis also compared data with an ARB in combination with an ACEI vs. an ACEI alone and reported that there was not a statistically significant difference in all-cause mortality between the two treatment groups, but there was a statistically significant reduction in HF hospitalizations (OR 0.77 95% CI 0.69-0.87).18 Similar results were found in another meta-analysis of 27,495 patients, with no difference in all-cause mortality between treatment with an ARB compared to an ACEI (HR 1.06 95% CI 0.56-1.62), no difference in death between combination with an ARB and ACEI compared to an ACEI alone (HR 0.98 95% CI 0.84-1.15), and a 17% reduction in HF hospitalizations with combination therapy compared to an ACEI alone (RR 0.83 95% CI 0.71-0.97).19 According to a more recent meta-analysis of 33 randomized controlled trials evaluating the long-term efficacy and safety with dual blockade of the renin-angiotensin aldosterone system compared to monotherapy with an ACEI, ARB or direct renin inhibitor, there was no significant difference in all-cause or CV mortality between treatment groups. In the trials that reported HF hospitalizations, there was a reduction in HF hospitalizations (RR 0.82 95% CI 0.74 to 0.92; P=0.0003) in patients receiving combination therapy compared to those in the monotherapy treatment group. Heart failure hospitalizations were also reduced when the groups were analyzed according to patients with HF (RR 0.77 95% CI 0.68 to 0.99; P<0.001); although, the difference was not significant in the subgroup of patients without HF. There was no significant difference in all-cause or CV mortality with dual therapy vs. monotherapy in the subgroup of patients with HF. According to the safety analysis, there was an increase in the risk for hyperkalemia (RR 1.55 95% CI 1.32 to 1.82; P<0.001), hypotension (RR 1.66 95% CI 1.38 to 1.98; P<0.001), and renal failure (RR 1.41 95% CI 1.09 to 1.84; P=0.01) with combination compared to monotherapy in the overall patient population, that was also significantly increased in the subgroup of patients with HF.4 In a meta-analysis evaluating the addition of an ARB, direct renin inhibitor, or aldosterone antagonist in patients receiving standard therapy for HF that included an ACEI, addition of an aldosterone antagonist decreased the rate of death (RR 0.79 95% credibility interval [CrI] 0.66 to 0.98), CV death (RR 0.78 95% CrI 0.65 to 0.93), HF hospitalizations (RR 0.74 95% CrI 0.55 to 0.94), and the composite CV death or HF hospitalizations (RR 0.73 95% CrI 0.55 to 0.90). There was no difference in these outcomes when either an ARB or direct renin inhibitor was added to standard therapy. Regarding safety, addition of an aldosterone antagonist increased the risk for hyperkalemia by 110%; whereas the addition of an ARB increased the risk of hyperkalemia by 138%, renal failure by 126%, and hypotension by 63%, and addition of a direct renin inhibitor increased the risk for hypotension by 98%.7 Table 1. Results of CHARM, Val-HeFT, and HEAAL Trials in Patients with HFa CHARM-OverallOutcomesCandesartan (N=3803)Placebo (N=3796)Unadjusted HR (95% CI)P valueARRcNNTc (3.1 years)All-cause mortalityb886 (23%)945 (25%)0.91 (0.83-1.00)0.055--CV mortality or HF hospitalization1150 (30.2%)1310 (34.5%)0.84 (0.77-0.91)<0.00014.3%23CV mortality693 (18.2%)796 (20.3%)0.88 (0.79-0.97)0.0122.8%36HF hospitalization757/3801 (19.9%)918 (24.2%)0.79 (0.72-0.87)<0.00014.3%23CHARM-AlternativeOutcomesCandesartan (N=1013)Placebo (N=1015)Unadjusted HR (95% CI)P valueARRcNNTc (2.8 years)All-cause mortality265 (26.2%)296 (29.2%)0.87 (0.74-1.03)0.11--CV mortality or HF hospitalizationb334 (33.0%)406 (40.0%)0.77 (0.67-0.89)<0.00017%14CV mortality219 (21.6%)252 (24.8%)0.85 (0.71-1.02)0.072--HF hospitalization207 (20.4%)286 (28.2%)0.68 (0.57-0.81)<0.0017.7%13CHARM-AddedOutcomesCandesartan (N=1276)Placebo (N=1272)Unadjusted HR (95% CI)P valueARRcNNTc (3.4 years)All-cause mortality377 (30.0%)412 (32.0%)0.89 (0.77-1.02)0.086--CV mortality or HF hospitalizationb483 (37.9%)538 (42.3%)0.85 (0.75-0.96)0.0114.4%23CV mortality302 (23.7%)347 (27.3%)0.84 (0.72-0.98)0.0293.6%28HF hospitalization309 (24.2%)356 (28.0%)0.83 (0.71-0.96)0.0143.8%27Val-HeFTOutcomesValsartan (N=2511)Placebo (N=2499)RR (97.5% CI)P valueARRcNNTc (1.9 years)All-cause mortality b495 (19.7%)484 (19.4%)1.02 (0.88-1.18)d0.80--All-cause mortality and morbidity b723 (28.8%)801(32.1%)0.87 (0.77-0.97)0.0093.3%31HF hospitalization348 (13.8%)454 (18.2%)0.76<0.0014.4%23HEAALOutcomesLosartan 150 mg (N=1927)Losartan 50 mg (N=1919)HR (95% CI)P valueARRcNNTc (4.7 years)All-cause mortality635 (33.0%)665 (34.7%)0.94 (CI 0.84-1.04)0.24Death or HF hospitalizationb828 (43.0%)889 (46.3%)0.90 (CI 0.82-0.99)0.0273.4% 30HF hospitalizations450 (23.4%)503 (26.2%)0.87 (CI 0.76-0.98)0.0252.9%35a CV=cardiovascular; HF=heart failure as defined by study entry criteria; HR=hazard ratio; RR=relative risk b Primary endpoint c Calculated value (ARR=absolute risk reduction; NNT=number needed to treat) d 98% Confidence Interval Heart Failure with Acute Myocardial Infarction Discussion: The recommendation to use an ARB in patients with an acute MI and HF/evidence of systolic dysfunction who are intolerant to an ACEI is based on the following data. The Valsartan in Acute Myocardial Infarction Trial (VALIANT)20 evaluated the effects of the ARB valsartan (target dose of 160 mg twice daily), the ACEI captopril (target dose of 50 mg three times daily) and the combination of valsartan and captopril (target dose of 80 mg twice daily and 50 mg three times daily, respectively) over a 2 year period on all-cause mortality in 14,808 high-risk (i.e., signs and symptoms of acute HF, or left ventricular systolic dysfunction) patients within 0.5 to 10 days of an acute MI. The study reported a similar mortality rate with valsartan as with captopril. The combination of captopril plus valsartan resulted in an increased incidence of adverse events (leading to a dose reduction or permanent discontinuation of study treatment), without improving survival. Similar results were seen for the composite secondary endpoint of fatal and nonfatal cardiovascular events (Refer to Table 2). In addition, approximately 70% of patients enrolled were receiving concomitant therapy with a beta-adrenergic blocker and according to subgroup analysis there was not an increase in mortality in patients receiving an ARB and ACEI in addition to a beta-adrenergic blocker. The trial was designed to assess equivalency of an ARB compared to an ACEI and according to the results valsartan can be considered as effective as captopril in reducing all-cause mortality and fatal and non-fatal cardiovascular events in this patient population. Valsartan is FDA approved to reduce CV mortality in patients with left ventricular failure or left ventricular dysfunction following MI. According to results of Optimal Trial in Myocardial Infarction with the Angiotensin II Antagonist Losartan (OPTIMAAL),21 a trial with losartan (target dose 50mg once daily) compared to captopril (target dose 50mg three times daily) in 5477 high-risk (i.e., signs and symptoms of HF or Q-wave MI) patients with acute MI, the primary endpoint of all-cause mortality was higher (18.2%) in patients on losartan compared to 16.4% of patients on captopril, with a trend toward statistical significance (RR 1.13 95% CI 0.99-1.28; P=0.069) after a mean follow-up of 2.7 years. There was not a statistically significant difference between treatment groups in the secondary endpoints. Due to the study design, superiority or non-inferiority of losartan relative to captopril was not shown. As with ELITE II, the target dose of losartan was thought to be suboptimal in this study.11 A meta-analysis reported that there was not a difference in all-cause mortality or HF hospitalizations with an ARB compared with an ACEI in patients with high-risk acute MI. This conclusion was based on results of VALIANT and OPTIMAAL, although the data were not pooled due to heterogeneity.18 Table 2. Results of VALIANT in Patients with HF and Acute MIa VALIANTOutcomes Valsartan (N=4909)Captopril (N=4909)Valsartan + Captopril (N=4885)HR (vs. captopril) (97.5% CI)P valueAll-cause mortalityb979 (19.9%)958 (19.5%)941 (19.3%)1.00 (0.90-1.11) 0.98 (0.89-1.09) (combination)0.98 0.73Combined CV death, recurrent MI, HF hospitalization 1529 (31.1%)1567 (31.9%)1518 (31.1%)0.95 (0.88-1.03) 0.97 (0.89-1.05) (combination)0.20 0.37a CV=cardiovascular; HR=hazard ratio; MI=myocardial infarction b Primary endpoint Chronic Kidney Disease Discussion: The American Diabetes Association (ADA) recommends treatment with an ACEI or ARB in patients with DM and microalbuminuria [Level of Evidence C] or macroalbuminuria [Level of Evidence A] to slow the progression of CKD, with addition of other drug classes (e.g., diuretics, CCBs, beta-adrenergic blockers) as needed for additional blood pressure reduction.22 The Kidney Disease Improving Global Outcomes (KDIGO) guideline on the management of blood pressure in CKD recommends treatment with an ACEI or ARB in patients with DM and albuminuria, due to their benefit in reducing proteinuria in patients with microalbuminuria [Level 2D Suggestion] and based on slowing the progression of CKD in patients with type 1 or 2 DM; with strong evidence for use of an ACEI in patients with type 1 DM and macroalbuminuria and for an ARB in type 2 DM and macroalbuminuria [Level 1B Recommendation].23 These statements to use an ACEI or ARB are consistent with the KDIGO recommendations in patients with nondiabetic CKD with microalbuminuria and macroalbuminuria, respectively, requiring blood pressure lowering23,24 and with the National Kidney Foundation (NKF) Kidney Disease Outcomes Quality Initiative (KDOQI) guidelines on DM in CKD in normotensive patients with DM and albuminuria [Level 2C Suggestion].25 Use of an ACEI or ARB is not recommended in patients with normoalbuminuria (albumin excretion < 30mg/24hr) and DM who are normotensive.25-27 In general, several guidelines on the management of patients with CKD23,25,28 do not promote use of combination with an ACEI and ARB.  More specifically, the KDIGO guideline on CKD states there is insufficient evidence for use of combination of an ACEI and ARB to prevent the progression of CKD (not graded).28 This recommendation is based on discussion in the KDIGO guideline on blood pressure and CKD.23 The KDOQI guideline in patients with DM and CKD states that combination with an ACEI and ARB cannot be recommended at this time,25 despite the potential benefit on further reduction in proteinuria with combination compared to monotherapy,29 referencing one trial of patients with vascular disease or high risk DM where there was no outcome benefit but an increase in hypotension, hyperkalemia and renal impairment with combination ACEI and ARB therapy compared to an ACEI alone.30 In addition, this trial showed an increase in the secondary endpoint of risk for dialysis, doubling sCr, and death with combination therapy when compared to an ACEI alone.31 Recommendations from the above clinical practice guidelines are included in the following table: GuidelinePatient Population*RecommendationLevel of Evidence (Grading System)KDIGO (2012) HTN, DM, CKD w/macroalbuminuriaACEI or ARB1B (GRADE)HTN, DM, CKD w/microalbuminuriaACEI or ARB2D (GRADE)HTN, nonDM CKD w/macroalbuminuriaACEI or ARB1B (GRADE)HTN, nonDM CKD w/microalbuminuriaACEI or ARB2D (GRADE)KDOQI (2012)nonHTN, DM, CKD w/macroalbuminuria or microalbuminuriaACEI or ARB2C (GRADE)ADA (2013)DM and CKD with macroalbuminuriaACEI or ARBA (ADA)DM and CKD with microalbuminuriaACEI or ARBC (ADA)*macroalbuminuria (e.g., urinary albumin excretion > 300 mg/24hr); microalbuminuria (e.g., urinary albumin excretion 30 to 300 mg/24hr) The ACEIs have been reported to be beneficial in patients with type 1 DM with macroalbuminuria to reduce the combined risk of death, dialysis, or transplantation,32 and in type 1 DM with microalbuminuria to decrease the progression of kidney disease.33-35 The long-term effects of the ARBs have not been adequately studied in patients with type 1 DM. Treatment with an ACEI in trials of patients with type 2 DM that also included a percentage of patients with microalbuminuria, have demonstrated a reduction in CV endpoints.36-40 Both the ACEIs and the ARBs have resulted in a decrease in the progression of kidney disease in patients with type 2 DM and microalbuminuria.41-43 As per results from the Irbesartan Type 2 Diabetic Nephropathy (IDNT)44 and Reduction of Endpoints in Patients with NIDDM with the Angiotensin II Antagonist Losartan (RENAAL)45 trials in patients with type 2 DM and macroalbuminuria, there are clinical trial data to support use of an ARB in this patient population.44,45 An ACEI has been shown to decrease surrogate endpoints in patients with type 2 DM and macroalbuminuria, but not long-term outcomes, as the ACEIs have not been as extensively studied in this patient population.46 The recommendation to use an ARB in patients with type 2 DM and nephropathy is based on the results of two long-term outcome trials in this patient population. Both IDNT44 and RENAAL45 evaluated the effect of an ARB on the primary endpoint of composite all-cause mortality, doubling of sCr, and ESRD. In IDNT, 1715 patients with HTN, type 2 DM and nephropathy were randomized to irbesartan 300mg once daily, amlodipine 10mg once daily, or placebo for a mean follow-up of 2.6 years.44 In RENAAL, 1513 patients with type 2 DM and nephropathy (with over 90% % on antihypertensive medications) were randomized to losartan 50-100mg once daily (71% received a dosage of 100 mg once daily) or placebo for a mean follow-up of 3.4 years.45 Both trials demonstrated a reduction in the primary endpoint with an ARB compared to placebo44,45 and, in IDNT, this endpoint was also significantly reduced compared to amlodipine.44 The secondary endpoints evaluating cardiac events were not statistically significantly different with an ARB compared to placebo.44,45 Refer to Table 3. Table 3. Results of IDNT and RENAAL Trials in Patients with HTN and Type 2 Diabetic Nephropathya IDNTOutcomesIrbesartan (N=579)Placebo (N=569)Unadjusted RR (95% CI)P valueARRcNNTc (2.6 years)Composite all-cause mortality, ESRD, doubling sCr b189 (32.6%)222 (39%)0.80 (0.66-0.97)0.026.4%16Doubling sCr98 (16.9%)135 (23.7%)0.67 (0.52-0.87)0.0036.8%15ESRD82 (14.2%)101 (17.8%)0.77 (0.57-1.03)0.07--All-cause mortality87 (15.1%)93 (16.3%)0.92 (0.69-1.23)0.57--RENAALOutcomesLosartan (N=751)Placebo (N=762)Adjusted RR (95% CI)P valueARRcNNTc (3.4 years)Composite all-cause mortality, ESRD, doubling sCr b327 (43.5%)359 (47.1%)0.84 (0.72-0.98)0.023.6%-dDoubling sCr162 (21.6%)198 (26.0%)0.75 (0.61-0.92)0.006 4.4%23ESRD147 (19.6%)194 (25.5%)0.72 (0.58-0.89)0.0025.9%17All-cause mortality158 (21.0%)155 (20.3%)1.02 (0.81-1.27)0.88--a ESRD=end-stage renal disease; RR=relative risk; sCr=serum creatinine b Primary endpoint c Calculated value (ARR=absolute risk reduction; NNT=number needed to treat) d NNT not calculable based on crude rates of events There have also been studies comparing an ACEI to ARB, or evaluating the combination of two agents that block the renin-angiotensin-aldosterone system, on surrogate endpoints of kidney function. When an ARB has been compared to an ACEI in trials including patients with type 1 or 2 DM, and microalbuminuria or macroalbuminuria, there has been a similar reduction in surrogate endpoints of kidney function between the two treatment groups.47-51 The Candesartan and Lisinopril Microalbuminuria (CALM) study compared the effects of candesartan 16mg, lisinopril 20mg, or the combination on urinary albumin excretion (UAE) and blood pressure in 197 patients with HTN, type 2 DM, and microalbuminuria for 24 weeks. There was a statistically significant reduction in blood pressure in all treatment groups, with the greatest reduction in patients on combination therapy. Urinary albumin:creatinine ratio was reduced with candesartan (24%, 0% to 43%; P=0.05), lisinopril (39%, 20% to 54%; P<0.001), and combination therapy (50%, 36% to 61%; P<0.001). Combination therapy decreased the urinary albumin:creatinine ratio 34% compared to patients on candesartan alone (P=0.04). The difference between combination therapy and lisinopril was not statistically significant.52 There have also been short-term trials in patients with type 1 or 2 DM and nephropathy, with a greater reduction in albuminuria seen with the combination of an ARB and an ACEI, or an ARB and a direct renin inhibitor (aliskiren), compared to monotherapy.53-57 This benefit has also been seen with the combination of an ACEI and nondihydropyridine CCB compared to treatment with either agent alone in a long-term trial of patients with type 2 DM and nephropathy.58 As mentioned previously, updated guidelines now caution against the use of combination of an ACEI and ARB in patients with DM and CKD.25 There has been added concern about combination therapy with agents that block the renin-angiotensin-aldosterone system, especially when used for the potential benefit on kidney outcomes. A VA Cooperative Study, Combination Angiotensin Receptor Blocker and Angiotensin-Converting Enzyme Inhibitor for Treatment of Diabetic Nephropathy (VA NEPHRON-D), was terminated early based on a greater number of observed acute kidney injury events (HR 1.7 95% CI 1.3 to 2.2; P<0.001) and hyperkalemia (HR 2.8 95% CI 1.8 to 4.3; P<0.001) in the combination ARB (losartan) and ACEI (lisinopril) therapy group compared to patients receiving an ARB plus placebo. There was no significant difference in the primary endpoint of first occurrence of a decline in estimated glomerular filtration rate (eGFR), ESRD, or death between treatment groups (HR 0.88 95% CI 0.70 to 1.12; P=0.30).59 Further discussion and recommendations in VA are available at  HYPERLINK "http://www.pbm.va.gov/vamedsafe/nationalpbmbulletin/DualRenin-AngiotensinAldosteroneSystemBlockadeandImpairedRenalFu.pdf" http://www.pbm.va.gov/vamedsafe/nationalpbmbulletin/DualRenin-AngiotensinAldosteroneSystemBlockadeandImpairedRenalFu.pdf (National PBM Bulletin Dual Renin-Angiotensin-Aldosterone System Blockade in Diabetic Nephropathy and Increased Adverse Events, February 12, 2013). The Ongoing Telmisartan Alone and in Combination with Ramipril Global Endpoint Trial (ONTARGET) trial30 looked at patients with vascular disease (coronary, peripheral, or cerebrovascular) or high-risk DM (with end-organ damage) and found no significant difference in the primary composite endpoint of death from CV causes, MI, stroke, or hospitalization for HF when comparing the combination of an ARB (telmisartan) and an ACEI (ramipril) to ACEI monotherapy. However, combination therapy with an ARB and ACEI increased the risk of renal impairment compared to the ACEI alone treatment group (RR 1.33 95% CI 1.22-1.44; P<0.001).30 As part of ONTARGET, the pre-specified kidney endpoint (composite of dialysis, doubling serum creatinine, and death) did not differ in patients treated with an ARB alone (13.4%) compared to patients on an ACEI alone (13.5%), but increased in patients receiving the combination (14.5%) compared to treatment with an ACEI alone (HR 1.09 95% CI 1.01-1.18; P=0.037).31 Another trial of combination with two agents that block the renin-angiotensin-aldosterone system, the Aliskiren Trial in Type 2 Diabetes Using Cardiorenal Endpoints (ALTITUDE), evaluated patients with type 2 DM and CKD, CV disease, or both. There was no difference between treatment groups in the primary composite outcome (time to CV death or a first occurrence of cardiac arrest with resuscitation; nonfatal MI; nonfatal stroke; unplanned hospitalization for HF; ESRD, death attributable to kidney failure, or the need for renal-replacement therapy with no dialysis or transplantation available or initiated; or doubling of the baseline sCr level). However, there was a significant increase in discontinuations due to an adverse event (13.2% vs. 10.2%), rates of hyperkalemia (39.1% vs. 29.0%) and hypotension (12.1% vs. 8.3%) with combination with aliskiren compared to either an ACEI or ARB alone, respectively.60 As a result of this trial, the manufacturer has recommended that aliskiren be discontinued in patients with DM who are also taking an ACEI or ARB. A meta-analysis of data with the ACEIs and the ARBs in patients with diabetic nephropathy showed a significant reduction in all-cause mortality with the ACEIs vs. placebo (RR 0.79 95% CI 0.63-0.99; P=0.04); a difference that was not statistically significant when the ARBs were compared to placebo (RR 0.99 95% CI 0.85-1.17; P=0.95). The reduction in doubling of sCr and ESRD were not significant (P=0.08 and P=0.07, respectively) with the ACEIs compared to placebo or no treatment. With the ARBs, the reduction in doubling of sCr (P=0.004), ESRD (P=0.001), microalbuminuria to macroalbuminuria (P=0.001), and regression from microalbuminuria to normoalbuminuria (P=0.02) were significant compared to placebo or no treatment. The reduction in progression from microalbuminuria to macroalbuminuria (P=0.0007), and regression from microalbuminuria to normoalbuminuria (P=0.0001) were statistically significant with the ACEIs vs. placebo or no treatment. In the three trials comparing an ACEI to an ARB, there was not a statistically significant difference in kidney outcomes (i.e., progression from microalbuminuria to macroalbuminuria; regression from microalbuminuria to normoalbuminuria). The meta-analysis concluded that ACEIs should be used as first-line treatment in patients with diabetic nephropathy due their survival benefit, that which has yet to be demonstrated with the ARBs.61 A systematic review and meta-analysis of 127 trials evaluating an ARB or ACEI on kidney outcomes reported a nonsignificant reduction with an ACEI or ARB on doubling sCr and a significant decrease in ESRD when compared with other antihypertensive treatment groups, with no difference in the degree of change in blood pressure. When comparing an ACEI or ARB to placebo, there was a benefit in reducing ESRD and doubling sCr that was associated with a reduction in blood pressure.62 A systematic review and meta-analysis of 21 trials including 654 patients with proteinuria evaluated the antiproteinuric effect of combination with an ARB and an ACEI and reported a further reduction in proteinuria with the addition of an ARB compared to an ACEI alone. This was accompanied by a slight increase in potassium (0.11 mEq/L) that was statistically significant. The effect on long-term outcomes was not evaluated.63 Another meta-analysis evaluated the effect of an ARB alone or in combination with an ACEI on proteinuria in 6181 patients from 49 trials and reported that an ARB reduced proteinuria compared to placebo, with the combination providing further reduction in proteinuria compared to either agent as monotherapy. The effect of an ARB or the combination of an ARB with an ACEI on long-term outcomes was also not evaluated in this meta-analysis.29 Finally, as noted in the meta-analysis discussed in the section on HF, dual blockade of the renin-angiotensin-aldosterone system with an ACEI, ARB, or direct renin inhibitor, compared to monotherapy showed no significant difference in all-cause or CV mortality with combination therapy compared to monotherapy; however, there was a significant increase in the risk for hyperkalemia, hypotension, and renal failure with combination compared to monotherapy.4 Hypertension Discussion: According to the Seventh Report of the Joint National Committee on Prevention, Detection, Evaluation and Treatment of High Blood Pressure (JNC 7) guidelines64 a thiazide-type diuretic is recommended as initial therapy for most patients with uncomplicated HTN. Other classes (ACEIs, ARBs, beta-adrenergic blockers, CCBs) that have demonstrated positive outcomes in randomized controlled trials may be considered as alternative or supplemental therapy for uncomplicated HTN or for treatment of patients with compelling indications. Regarding compelling indications, the JNC 7 guidelines state that diuretics, ACEIs, beta-adrenergic blockers, CCBs, and ARBs have all demonstrated benefit in reducing CVD and stroke in patients with DM and HTN; ACEIs, beta-adrenergic blockers, ARBs, and aldosterone antagonists are recommended in patients with HF; and ACEIs and ARBs have demonstrated benefit on the progression of DM and nondiabetic kidney disease.64 The VA/DoD Clinical Practice Guideline for the Management of Hypertension in Primary Care (refer to  HYPERLINK "http://www.oqp.med.va.gov/cpg/HTN04/HTN_base.htm" http://www.oqp.med.va.gov/cpg/HTN04/HTN_base.htm) concur with the recommendations of JNC 7; in addition, these guidelines recommend that an ARB may be considered in patients with uncomplicated HTN who are intolerant to an ACEI. The VA/DoD Hypertension Guidelines recommend a preference for a thiazide-type diuretic or an ACEI as initial therapy in patients with HTN and DM; a beta-adrenergic blocker, CCB, or ARB may be considered as additional or alternative therapy. The VA/DoD Clinical Practice Guideline for the Management of Hypertension in Primary Care is in the process of being updated. More recently, guidelines have been published based on an evidence review by panel members appointed to the eighth Joint National Committee (JNC 8). These guidelines recommend initiation of a thiazide-type diuretic, ACEI, ARB, or CCB in nonblack patients of all ages, with or without DM; and a thiazide-type diuretic or CCB in black patients. An ACEI or ARB is recommended in patients with HTN and concomitant CKD.65 The evidence review was conducted by the JNC 8 panel that was originally appointed by the National Heart Lung and Blood Institute (NHLBI); however, NHLBI recently announced that it would no longer be developing guidelines and instead appointed the American Heart Association (AHA) and American College of Cardiology (ACC), which are planning to issue their own guidelines. Another clinical practice guideline recently published by the American Society of Hypertension (ASH) and International Society of Hypertension (ISH) recommends initial therapy with a thiazide diuretic or CCB in black patients of any age or nonblack patients > 60 years of age; and an ACEI or ARB in non-black patients < 60 years of age. An ACEI or ARB is recommended in patients with HTN and concomitant DM, CKD, or stroke, and in addition to a beta-adrenergic blocker in patients with clinical coronary artery disease.66 The European Society of Hypertension (ESH)/European Society of Cardiology (ESC) 2013 HTN guidelines consider a diuretic (including thiazides, chlorthalidone and indapamide), ACEI, ARB, beta-adrenergic blocker, or CCB as appropriate for initiation and management of hypertension, either as monotherapy or in certain combinations.67 In addition, an ARB may be considered preferable (as are the other medications listed) in the following conditions: LVH: ACEI, CCB, ARB; microalbuminuria: ACEI, ARB; kidney dysfunction: ACEI, ARB; previous stroke: any agent that lowers BP; previous MI: beta-adrenergic blocker, ACEI, ARB; HF: diuretics, beta-adrenergic blocker, ACEI, ARB, aldosterone antagonist; prevention of atrial fibrillation: consider ARB, ACEI, beta-blocker, aldosterone antagonist; kidney failure/proteinuria: ACEI, ARB; metabolic syndrome: ACEI, ARB, CCB; DM: ACEI, ARB.67,68 The National Institute for Health and Clinical Excellence (NICE) 2011 HTN guideline, based on clinical and economic evidence and quality for the National Health Service in the UK, recommends a CCB first-line if > 55 years of age or black, or a thiazide diuretic if a CCB is not appropriate (e.g., if it is not tolerated or the patient has edema) or the patient has evidence of HF or is at high risk for HF; and an ACEI or low-cost ARB (if an ACEI is used initially and not tolerated, an ARB can be considered; an ACEI and ARB should not be combined) first-line if < 55 years of age. It is recommended that Step 2 therapy should include treatment with a CCB in combination with an ACEI or ARB. If a CCB is not appropriate, as previously stated, a thiazide diuretic should be included. It is recommended that Step 3 therapy include combination with a CCB, ACEI or ARB, and thiazide diuretic.69 The Canadian Hypertension Education Program 2013 recommends a thiazide diuretic as initial therapy in uncomplicated HTN; a beta-blocker (in patients < 60 years of age); an ACEI (not in black patients); a long-acting CCB; or an ARB. Additional therapy should be selected from the choices for initial therapy; however, combination therapy with an ACEI and ARB is not recommended.70 A systematic review of benefits and harms of first-line antihypertensive therapies concluded that first-line therapy with a thiazide diuretic reduced morbidity and mortality (e.g., mortality, stroke, CHD, CV events), with the ACEIs reducing mortality, stroke, CHD, CV events, and the CCBs decreasing stroke and CV events; with the stronger evidence to support treatment with a thiazide diuretic. No randomized controlled trials with an ARB compared to placebo or no treatment were found.71 In a meta-analysis of first-line therapies for HTN that included comparison trials, an ARB was not significantly more effective for any of the treatment outcomes (total or CV mortality, CV events, stroke, HF, or CHD) compared to a low-dose thiazide diuretic.72 Another meta-analysis found no difference in all-cause mortality with an ARB vs. active controls.73 A meta-analysis reported a significant reduction in the risk of stroke with an ARB; however, there was a nonsignificant increase in MI with an ARB compared to controls.74 An evaluation of the literature that included 147,020 patients from 37 randomized clinical trials found no increased risk of MI with the ARBs compared to the control group (placebo or active treatment). There was also no difference in all-cause mortality, CV death, or angina. The ARBs were found to reduce stroke, HF, and new-onset DM compared to controls.75 In a meta-analysis of 20 trials including 158,998 patients treated with a renin-angiotensin-aldosterone system blocker or control treatment, a renin-angiotensin-aldosterone system blocker was associated with a decreased risk of all-cause mortality and CV mortality compared to the control group. When treatment with a renin-angiotensin-aldosterone system blocker was analyzed separately, there was a decrease in the risk for all-cause mortality with an ACEI compared to the control group. There was no difference in all-cause mortality between an ARB and control treatment. There was a significant difference in the treatment effect between an ACEI and ARB, suggesting that the difference in all-cause mortality with a renin-angiotensin-aldosterone system blocker was due to the ACEI.76 It is noted that data from the KYOTO HEART Study (publication retracted by the European Heart Journal due to critical problems with some of the data) were included as part of the meta-analyses in these two publications.75,76 According to a comparative effectiveness review, there was no difference in blood pressure control, mortality, or CV events between an ACEI and ARB; with clarification that there was not enough evidence to determine a difference in mortality or CV events due to the inclusion of trials with patients with low event rates and a short-treatment duration. There were higher rates of cough in patients treated with an ACEI (8.7%; vs. 2.2% with an ARB), and more patients withdrew from treatment with an ACEI (5%; vs. 3% with an ARB).77 According to randomized controlled trials in patients with HTN, treatment with an ARB reduced hospitalization for stroke and hospitalization for MI (candesartan) compared to conventional treatment,78 reduced nonfatal stroke (candesartan) vs. open-label antihypertensive therapy,79 and decreased combined death, CV and cerebrovascular events (eprosartan) compared to a dihydropyridine CCB.80 In patients at high CV risk or CV disease, treatment with an ARB has been shown to reduce the composite death, MI, stroke (losartan) compared to a beta-blocker;81 there was no difference in CV morbidity and mortality (telmisartan) compared to an ACEI,30 or with telmisartan compared to placebo in patients intolerant to an ACEI,82 or with valsartan83 or candesartan84 compared to a dihydropyridine CCB; no significant difference in reducing major adverse CV events (candesartan) compared to conventional therapy;85 and no significant reduction in the rate of CV events with valsartan compared to placebo, although there was a decrease in development of DM in patients with impaired glucose intolerance.86 Although the reduction in CV events appear largely driven from the reduction in stroke, there was no difference in recurrent stroke when treatment with an ARB (telmisartan) was compared to placebo.87 In two trials of Japanese men, there was no difference in the composite CV outcomes between treatment with an ARB-based regimen (valsartan) compared to a dihydropyridine CCB-based regimen in patients with HTN and type 2 DM or glucose intolerance;88 and no difference in the composite outcome of mortality, CV events, and renal events in patient with HTN treated with an ARB (valsartan) compared to a dihydropyridine CCB.89 In summary, an ARB is effective for lowering blood pressure in the treatment of hypertension. There have been mixed results with an ARB in patients with HTN and/or CV disease or high CV risk; an ARB has been shown to reduce CV morbidity and mortality in patients with high CV risk when compared to treatment with a beta-blocker or conventional treatment, with no difference compared to an ACEI or dihydropyridine CCB (per controlled clinical trials including patients in the U.S.), and a nonsignificant reduction compared to placebo in patients with CV disease or high risk DM who were ACEI intolerant. According to a recent meta-analysis, treatment with an ARB does not increase the risk for MI compared to controls; however, the reduction seen in all-cause mortality with a renin-angiotensin-aldosterone system blocker appears to be driven by the benefit seen from treatment with an ACEI, and not an ARB. Taking the above into consideration along with the overall strong evidence for treatment with an ACEI, providers may prefer use of an ACEI prior to considering treatment with an ARB; however, as per recent clinical practice guidelines, use of an ARB may also be an option for use in the management of patients with HTN. ACEI Induced Cough Discussion: The incidence of cough with an ACEI is estimated to be anywhere from 0.5 to 39%.90 The cough associated with an ACEI has been described as dry, nonproductive, persistent, beginning with a tickling sensation, and often worse at night. The onset is usually within the first week of ACEI therapy and continues throughout treatment, resolving within a few days to 4 weeks after the ACEI is discontinued. The cough is not usually dose-dependent, although in some instances it may be eliminated with a reduction in dose. Since therapy with an ACEI has proven valuable, it is important to consider alternative diagnoses (e.g., asthma, chronic obstructive pulmonary disease, allergic rhinitis, upper respiratory tract infection, HF, gastroesophageal reflux disease) before a diagnosis of ACEI-induced cough is made. If congestion is present, which is often noted in patients with HF, adjustment of the diuretic dose may relieve symptoms due to congestion, allowing the ACEI to be continued. In SOLVD (evaluating patients with HF), cough was reported in 37% of patients treated with enalapril compared to 31% of patients randomized to placebo.91 In V-HeFT II, 37% of HF patients on enalapril complained of cough compared to 29% receiving hydralazine and isosorbide dinitrate.92 Patients who experienced cough with an ACEI were found to have a significant decrease in frequency, severity, index, and characteristics of the cough when switched to fosinopril.93-96 However, one open-label comparison study found the incidence of cough with fosinopril (12%) to be higher compared to other select ACEIs (6.6% of patients each on enalapril, lisinopril, ramipril).97 The incidence of cough associated with the ARBs is reported to be similar to placebo (1.6-3.4%).90 In a systematic review of head-to-head comparison trials of an ACEI and ARB, cough was reported in 0 to 23% (mean 10%) of patients treated with an ACEI and 0 to 13% (mean 3%) of patients receiving an ARB.98 In another comparative-effectiveness review, cough was reported in 2.2% of patients who received an ARB compared to 8.7% of patients on an ACEI.77 In a large comparison study of valsartan 160 mg daily and lisinopril 20 mg daily in patients with HTN, dry cough was reported in 1.0% of patients on valsartan and in 7.2% of patients treated with lisinopril (P<0.001).99 The TRANSCEND trial enrolled patients who were intolerant to an ACEI, with cough as the reported reason for ACEI intolerance in 88.2% (i.e., 5225 patients) enrolled in the trial. Cough was subsequently reported as the reason for discontinuation in 15 (0.51%) of patients treated with telmisartan compared to 18 (0.61%) patients in the placebo group.82 In patients with HF in the ELITE Study, 3.8% of patients on an ACEI withdrew from the study due to complaints of cough compared to 0% of patients treated with an ARB.9 In the CHARM-Alternative trial, over 70% of patients with HF randomized to candesartan experienced previous intolerance to an ACEI due to cough. In this trial, cough was the reason for discontinuation in 0.2% of patients on candesartan compared to 0.4% patients on placebo.14 A number of trials evaluating an ARB in patients with previous ACEI induced cough showed that patients treated with an ARB complained of cough similar to that seen with placebo (15.6%-36.7% ARB, 9.7%-31.4% placebo), but statistically significantly less than seen when an ACEI was included (60-97%).100-107 In a meta-analysis of randomized controlled trials evaluating an ARB in patients with previous ACEI intolerance, the incidence of cough was reported in 67% of patients on an ACEI compared to 24% in patients receiving an ARB (RR 0.37 95% CI 0.28 to 0.48), with the incidence of cough being similar between an ARB and placebo.108 There is a slight chance that patients who are unable to tolerate treatment with an ACEI due to cough may develop a cough with an ARB.107,108 Angioedema Discussion: The incidence of angioedema in patients taking an ACEI is approximately 0.1-1.2%. The exact mechanism is unknown; in ACEIs, it is thought to be related to bradykinin accumulation. In an evaluation of veteran patients initiating treatment with an ACEI, 0.2% were reported to have experienced angioedema, with rates being four times higher in black patients and 50% higher in women.109 Angioedema has also been reported with the ARBs but to a much lesser degree than ACEIs.108,110-112 In the CHARM-Alternative trial with candesartan in patients with HF and a history of ACEI intolerance, 3 of 1013 patients randomized to candesartan experienced angioedema. One of these patients required discontinuation of the drug (0.1%). All 3 cases occurred out of the 39 patients who previously experienced angioedema or anaphylaxis on an ACEI (7.7%). None of the 1015 patients who received placebo experienced angioedema.14 In a large trial of 5926 patients at high CV risk intolerant to an ACEI, 75 (1.3%) of patients were intolerant due to angioedema or anaphylaxis. Of the 2954 patients randomized to telmisartan, angioedema was reported as the reason for discontinuation in 2 patients (0.07%) compared to 3 patients (0.10%) on placebo (P=0.660).87 A systematic review of 61 trials comparing an ARB with an ACEI reported angioedema (in 3 of the studies) in only those patients who were treated with an ACEI.98 There have been a number of published case reports of angioedema in patients treated with an ARB.90,113-132 In several of these cases, the patients previously experienced angioedema with an ACEI. A systematic review found the risk for angioedema to be 9.4% (95% CI 2 to 17%) of patients on an ARB who previously experienced angioedema on an ACEI; and 3.5% (95% CI 0 to 9.2%) of patients with previously confirmed angioedema on an ACEI.133 Another review estimated the risk of cross-reactivity of angioedema with an ARB in patients who previously experienced this adverse event with an ACEI to be from less than 7% up to 17%.134 Therefore, an ARB should be used with caution in patients who have previously experienced angioedema.113,121,122,124,133,134 Hyperkalemia Discussion: The ARBs, like the ACEIs, decrease release of aldosterone from the adrenal cortex, which can lead to decreased potassium excretion. It is unclear at this time if treatment with an ARB would be an appropriate alternative in patients who develop hyperkalemia on an ACEI. In SOLVD, hyperkalemia with potassium levels greater than 5.5 mmol/L was reported in 6.4% of patients on enalapril compared to 2.5% of patients on placebo.91 In the ELITE Study, an increase in serum potassium of > 0.5 mmol/L above baseline was observed in 22.7% patients receiving captopril compared to 18.8% of patients on losartan.9 In the CHARM-Overall programme, hyperkalemia resulted in discontinuation of study drug in 2.2% of patients on candesartan compared to 0.6% patients on placebo (P<0.0001). In the overall analysis, 41% of patients received concomitant treatment with an ACEI and approximately 17% were on spironolactone.16 A meta-analysis of data in patients with previous intolerance to an ACEI (majority due to cough) from CHARM-Alternative that included patients with HF, and TRANSCEND that studied patients with high CV risk, showed an increased risk for hyperkalemia with an ARB compared to placebo (RR 3.37 95% CI 1.60 to 7.11).108 In ONTARGET that included patients with vascular disease or high-risk DM, a similar percent of patients experienced an increase in potassium > 5.5 mmol/L in the ARB treatment group (3.36%) compared to patients receiving treatment with an ACEI (3.30%).30 The VAL-K Study Group reported that the change in serum potassium was not significantly different in patients with mild kidney impairment on lisinopril compared to valsartan; in patients with moderate kidney dysfunction (with a glomerular filtration rate < 60mL/min/1.73 m2), there was a significant increase of 0.28 mEq/L (P=0.04) above baseline (4.6 mEq/L) with lisinopril. The increase of 0.12 mEq/L seen with valsartan in this subgroup was not significant (P=0.1).135 Kidney Failure Discussion: In patients whose kidney function may depend upon the activity of the renin-angiotensin-aldosterone system, treatment with the ARBs and ACEIs has been associated with acute kidney failure. These drugs are capable of reducing intraglomerular filtration pressure by causing dilation of the efferent renal arterioles. As with the ACEIs, similar precautions are recommended for the ARBs in patients with renal artery stenosis. In ELITE, where the primary endpoint was the effect of treatment on sCr (> 0.3mg/dL increase), there was no difference between treatment with an ACEI vs. an ARB in the rise in serum creatinine during continued treatment.9 In the renal outcome component of ONTARGET that included patients with vascular disease or high-risk DM, a similar percent of patients experienced the secondary renal outcome of dialysis or doubling serum creatinine in patients receiving an ARB compared to patients receiving treatment with an ACEI (2.21% vs. 2.03%, respectively; HR 1.09 95% CI 0.89 to 1.34).31 A meta-analysis of data in patients with previous intolerance to an ACEI (majority due to cough) from CHARM-Alternative that included patients with HF, and TRANSCEND that studied patients with high CV risk, showed an increased risk for relapse of renal dysfunction with an ARB compared to placebo (RR 1.83 95% CI 1.01 to 3.34).108 It is unknown if an ARB can be used as an alternative in patients where treatment with an ACEI is limited due to kidney dysfunction or in a patient who develops kidney dysfunction as a result of treatment with an ACEI.136 References 1Yancy CW, Jessup M, Bozkurt B, Butler J, Casey DE Jr, Drazner MH, Fonarow GC, Geraci SA, Horwich T, Januzzi JL, Johnson MR, Kasper EK, Levy WC, Masoudi FA, McBride PE, McMurray JJV, Mitchell JE, Peterson PN, Riegel B, Sam F, Stevenson LW, Tang WHW, Tsai EJ, Wilkoff BL. 2013 ACCF/AHA guideline for the management of heart failure: a report of the American College of Cardiology Foundation/American Heart Association Task Force on Practice Guidelines. 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laіytЖUЯ‡|“|Ÿ|А|Ж|И|К|їїїїїї!$$IfК|Л|Ю|+ !$$$Ifa$гkdš$$If–lжжž”џЈ Hœд !(€tџџџџџџџџ€ џџџџџџџџ€ џџџџџџџџ€Tџџџџџџџџ€8џџџџџџџџ€8џџџџџџџџ€џџџџџџџџж0џџџџџџіііжџџџџџџџжџџџџџџџџџџџџџџџџџџџџџџџџџџџџжџџџџџџџжџџџџџџџџџџџџџџџџџџџџџџџџџџџџ4ж laіytЖUЯЮ|к|ц|ї|ў|}}їїїїїї!$$If}}}+#!$$Ifгkd`$$If–lжжž”џЈ Hœд !(€tџџџџџџџџ€ џџџџџџџџ€ џџџџџџџџ€Tџџџџџџџџ€8џџџџџџџџ€8џџџџџџџџ€џџџџџџџџж0џџџџџџіііжџџџџџџџжџџџџџџџџџџџџџџџџџџџџџџџџџџџџжџџџџџџџжџџџџџџџџџџџџџџџџџџџџџџџџџџџџ4ж laіytЖUЯ}}})}2}:}C}Q}Z}b}g}l}x}Žƒ{{{{{{{{{{!$$If !$$$Ifa$qkd& $$If–lжж”џ(€€(џџџџџџџџ жж џйййж0џџџџџџіііжџжџџџџжџжџџџџ4ж laіpж џйййytЖUЯ x}y}}) !$$$Ifa$еkdг $$If–lж”жž”џЈ Hœд !(€tџџџџџџџџ€ џџџџџџџџ€ џџџџџџџџ€Tџџџџџџџџ€8џџџџџџџџ€8џџџџџџџџ€џџџџџџџџж0џџџџџџіііжџџџџџџџжџџџџџџџџџџџџџџџџџџџџџџџџџџџџжџџџџџџџжџџџџџџџџџџџџџџџџџџџџџџџџџџџџ4ж laіytЖUЯ}™}Ѕ}Ж}М}О}Р}љёёёёё!$$If!$IfР}С}б}х}) !$$$Ifa$еkd $$If–lж”жž”џЈ Hœд 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