HYPERTENSION in ADPKD Sabine Karam M.D.. Introduction  ADPKD is the most common life-threatening single-gene disease  It affects over 12 million people.

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Presentation transcript:

HYPERTENSION in ADPKD Sabine Karam M.D.

Introduction  ADPKD is the most common life-threatening single-gene disease  It affects over 12 million people worldwide  Fourth leading cause of end-stage renal disease (ESRD) in the US  Hypertension identified as a factor associated with progression to ESRD

HYPERTENSION in ADPKD  Occurs in 50-75% of patients prior to the onset of marked renal insufficiency  Early high incidence correlated with renal structural abnormalities  Most important potentially treatable variable  Important risk factor for cardiovascular death, the most frequent cause of mortality in ADPKD patients JASN Jan;12(1):

Mean renal volume is significantly higher in Hypertensive (HBP) vs Normotensive (NBP) ADPKD patients Kidney International, Vol. 38 (1990), pp. 1177— subjects Creat<1.5 mg/dL Renal Volume by Ultrasound

The Progression of Renal Disease in Hypertensive and Normotensive ADPKD Patients Kidney International, Vol. 41(1992), pp. 1311—1319 P<0.001

Does the choice of the agent matter?

Mean PRA and plasma aldosterone concentration in 14 patients with HTN and ADPKD vs 9 patients with essential hypertension before and after 50 mg of captopril NEJM.1990;323:1091-6

Pathogenetic role of RAAS in ADPKD. Robert W. Schrier JASN 2009;20:

The annual loss of creatinine clearance adjusted for initial creatinine clearances was significantly larger in the diuretic group than the ACEI group Am J Nephrol 2001;21:98–103 Diuretic group: n=14 ACEI group: n=19 Follow up 5 years

No significant differences in the decline of GFR (ANOVA; P > 0.05) during the 3 years of follow-up of a cohort of 35 patients randomized to Enalapril or Atenolol Marjan A. van Dijk et al. Nephrol. Dial. Transplant. 2003;18:

Mean GFR (ml/min) as calculated according to Cockcroft and Gault at baseline, 12, 24 months, and at the end of the study in the two treatment groups. **P < 0.01 for GFR at baseline compared with GFR at the end of the study in both groups. Raoul Zeltner et al. Nephrol. Dial. Transplant. 2008;23: Metoprolol=23 Ramipril=23 Follow up 3 years

LVMI (g/m2) according to BP control at baseline and after the 3 years follow-up (end). *P < 0.01 for LVMI in the standard vs the rigorous BP control group at 3 years of follow-up. **P < 0.01 for LVMI at baseline compared with LVMI at the end of the study in the standard BP control group. Raoul Zeltner et al. Nephrol. Dial. Transplant. 2008;23:

Figure 1 American Journal of Kidney Diseases , DOI: ( /j.ajkd )

Is there an Ideal Target?

HYPERTENSION IN CKD TREATMENT GUIDELINES JNCVIIIESH/ESCKDIGO 2012 Lifestyle Modifications Na+<2.4g/day BMI Exercise 30x5 EtOH≤1-2(f-m) Na+<2.4g/day BMI Exercise 30x5 EtOH≤1-2(f-m) Na+<2g/day BMI Exercise 30x5 EtOH≤1-2(f-m) BP Goals <140/90 SBP<140 SBP<130 if overt proteinuria <140/90 mmHg <130/80 mmHg If UAE>30mg/day Preferred ACEI or ARB Yes Yes if UAE>30mg/day

MDRD Study: Mean changes in GFR versus time in patients randomized to a usual (dashed line) or a low blood pressure (solid line) group JASN.1995; 5: participants Follow up=2.2 years Usual” MAP goal =107 mm Hg for age ≤60 yr =113 mm Hg if older than 60 yr Low MAP goal =92 mm Hg for age≤ 60 yr and 98 mm Hg if older than 60 yr.

Effect of rigorous versus standard BP control on left ventricular mass index (LVMI) over 7 yr. Robert Schrier et al. JASN 2002;13:

Effect of rigorous versus standard BP control on 24-h creatinine clearance over 7 yr. Robert Schrier et al. JASN 2002;13:

HALT-PKD TRIAL: Goals and Design InterventionBP Target (mmHg) Primary Outcome Study A (CKD1-2) N=558 1.ACE+ARB 2.ACE 3.ACE+ARB 4.ACE / /60-75 Change in renal volume by MRI Study B (CKD 3) N=470 1.ACE+ARB 2.ACE /70-80 Doubling in serum creatinine ESRD/Death Goals: 1)ACEI+ARB> ACEI alone (CKD 1-3) 2)Low>standard BP target (CKD1-2)

HALT-PKD TRIAL: Protocol for addition of antihypertensive agents StepTreatmentControl 1-4 Combination ACE-ARB:ACE Lisinopril 5 mg Lisinopril 10 mg Lisinopril 20 mg Lisinopril 40 mg Combination ACE-ARB:ARB Telmisartan 40 mg Telmisartan 80 mg ACE-I Lisinopril 5 mg Lisinopril 10 mg Lisinopril 20 mg Lisinopril 40 mg Placebo 5 Hydrochlorothiazide 12.5 mg 6-8 Metoprolol 50 mg BID Metoprolol 100 mg BID Metoprolol 200 mg BID Metoprolol 50 mg BID Metoprolol 100 mg BID Metoprolol 200 mg BID 9 onwards Non dihydropyridine calcium channel blocker (diltiazem), clonidine, minoxidil, hydralazine at discretion of investigator

Total Kidney Volume and Estimated Glomerular Filtration Rate (eGFR) during Follow-up and Subgroup Analyses, According to Blood-Pressure Group. Schrier RW et al. N Engl J Med 2014;371:

Changes in Total Kidney Volume and eGFR during Follow-up, and Subgroup Analyses, According to Treatment Group. Schrier RW et al. N Engl J Med 2014;371:

Blood-Pressure Levels and Medication Steps between the two groups Torres VE et al. N Engl J Med 2014;371: Lisinopril–placebo higher systolic blood pressure (difference, 1.23 mm Hg; 95% confidence interval [CI], 0.24 to 2.21; P = 0.02)

Urinary Aldosterone and Albumin Excretion in both groups Torres VE et al. N Engl J Med 2014;371: P=0.08

Effect of Lisinopril–Telmisartan, as Compared with Lisinopril–Placebo, on the Time to Primary-Outcome Events and on the Estimated Glomerular Filtration Rate (eGFR). Torres VE et al. N Engl J Med 2014;371:

Effect of Lisinopril–Telmisartan, as Compared with Lisinopril–Placebo, on the Time to Primary-Outcome Events and on the Estimated Glomerular Filtration Rate (eGFR). Torres VE et al. N Engl J Med 2014;371:

Effect of Lisinopril–Telmisartan, as Compared with Lisinopril–Placebo, on the Time to Primary-Outcome Events and on the Estimated Glomerular Filtration Rate (eGFR). Torres VE et al. N Engl J Med 2014;371:

Treatment of hypertension in the adult ADPKD population  BP target 140/90mmHg  Agents that interfere with the renin-angiotensin- aldosterone system (RAAS) are first-line BP- lowering agents  Sodium-restricted diet  Calcium channel blockers and diuretics may be preferred over beta-blockers for cardiovascular protection

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