Advanced search
Publication Cover
Integrated Blood Pressure Control Volume 13, 2020 - Issue
Submit an article Journal homepage
568
Views
10
CrossRef citations to date
0
Altmetric
Review

Renal Artery Stenosis in the Patient with Hypertension: Prevalence, Impact and Management

Rohini ManaktalaOchsner Clinic Foundation, Department of Cardiovascular Medicine, New Orleans, LA, USACorrespondence[email protected]
,
Jose D Tafur-SotoOchsner Clinic Foundation, Department of Cardiovascular Medicine, New Orleans, LA, USA
&
Christopher J WhiteOchsner Clinic Foundation, Department of Cardiovascular Medicine, New Orleans, LA, USAORCID Iconhttps://orcid.org/0000-0001-8618-7539
ORCID Icon
Pages 71-82 | Published online: 02 Jun 2020

Abstract

Atherosclerosis is the primary cause of renal artery stenosis. Atherosclerotic renal artery stenosis (ARAS) is associated with three clinical problems: renovascular hypertension, ischemic nephropathy and cardiac destabilization syndrome which pose huge healthcare implications. There is a significant rate of natural disease progression with worsening severity of renal artery stenosis when renal revascularization is not pursued in a timely manner. Selective sub-groups of individuals with ARAS have had good outcomes after percutaneous renal artery stenting (PTRAS). For example, individuals that underwent PTRAS and had improved renal function were reported to have a 45% survival advantage compared to those without improvement in their renal function. Advances in the imaging tools have allowed for better anatomic and physiologic measurements of ARAS. Measuring translesional hemodynamic gradients has allowed for accurate assessment of ARAS severity. Renal revascularization with PTRAS provides a survival advantage in individuals with significant hemodynamic renal artery stenosis lesions. It is important that we screen, diagnosis, intervene with invasive and medical treatments appropriately in these high-risk patients.

Introduction

Atherosclerosis is by far the most prevalent etiology of renal artery stenosis. Atherosclerotic renal artery stenosis (ARAS) contributes to the development and progression of systemic atherosclerotic disease. It stems from having a hemodynamically significant renal artery atherosclerotic lesion that causes upregulation of the renin-angiotensin-aldosterone system (RAAS) resulting in accelerated hypertension that then adversely impacts pre-existing cardiovascular disease. Additionally, ARAS can also cause three clinical problems: renovascular hypertension, ischemic nephropathy and cardiac destabilization syndrome that include, acute decompensated heart failure (ADHF), recurrent ADHF and acute coronary syndromes (ACS). The prevalence of ARAS identified by Doppler ultrasound (DUS) within a US Medicare population ranges from 0.5% to 7% of individuals.Citation1 ARAS accounts for 10–20% of individuals with end stage renal disease who are on dialysis.Citation2 Furthermore, concurrent diagnosis of coronary artery disease (CAD) among individuals with ARAS ranges from 11.3% to 39%.Citation3 There is a significant rate of natural disease progression with worsening severity of renal artery stenosis shown by previous studies reporting the progression of ARAS by 50% at 5 years.Citation4

Randomized clinical trials have not shown a benefit for renal artery stenting in the management of ARAS when used as an adjunct treatment to optimal medical therapy (OMT).Citation5Citation7 However, selective sub-groups of individuals with ARAS that include those with resistant hypertension, ischemic nephropathy and cardiac destabilization syndrome have had good outcomes after percutaneous renal artery stenting (PTRAS).Citation8 Measuring translesional hemodynamic gradients allows for accurate assessment of ARAS severity and identifies patients likely to benefit from stenting.Citation9Citation11 Advances in the imaging tools used to make anatomic and physiologic measurements of ARAS can facilitate identifying the best candidates for PTRAS. These technologies include: blood oxygenation level-dependent magnetic resonance imaging (BOLD MRI), dynamic contrast-enhanced MRI, intravascular ultrasound (IVUS) and renal frame counts. Moreover, research efforts have identified biomarkers such as brain natriuretic peptide (BNP) that may aid in patient selection.Citation12 A small series of patients with BNP greater than 80 pg/mL obtained better blood pressure control after undergoing PTRAS.Citation12

From experimental animal models, ARAS was found to cause inflammation resulting in microvascular damage via ischemia, fibrosis and apoptosis of cells.Citation13 These findings led to the development of low-energy shock wave therapy that improved microcirculation.Citation14 ARAS is known to be a progressive disease. However, studies have shown similar long-term clinical outcomes with no difference in mortality or event-free survival in ARAS individuals who initially develop impaired renal function with initiation of medications compared to those individuals without decline in renal function that are also on medical therapy.Citation15 Regarding disease progression, the 2-year cumulative incidence is 6% of ARAS individuals with greater than 60% stenosis of the renal artery who develop reduction in renal length by greater than 1 cm.Citation16,Citation17 A natural history study of individuals with high-grade ARAS, who were medically managed without renal revascularization, was performed to determine the rate of progression to renal failure and development of accelerated hypertension. This study showed that over 3-year follow-up the number of antihypertensive medications to effectively control blood pressure in this patient population increased.Citation18 Additionally, renal function declined and mortality risk rose specifically in those patients with bilateral ARAS or ARAS with a solitary functioning kidney.Citation18

Observational studies have shown that PTRAS in individuals with ARAS who also have concomitant chronic kidney disease (CKD) can improve or stabilize renal function and preserve kidney size.Citation19 Renal size assessed by pole-to-pole kidney length with ultrasound measurement is an important predictor of clinical response.Citation20 Overall, renal revascularization with PTRAS provides patient survival advantage in those with significant hemodynamic renal artery stenosis lesions and advanced CKD (stage 4 and stage 5).Citation21 It is important that we screen, diagnosis, intervene with invasive and medical treatments appropriately in these high-risk patients.

Pathophysiology

Physician scientist, Goldblatt conducted foundational animal experiments investigating the effect of unilateral and bilateral renal artery stenosis on systemic blood pressure.Citation21,Citation22 Restricting blood flow to one kidney with a functioning contralateral kidney resulted in upregulation of the neurohormonal pathway of RAAS. The affected juxtaglomerular apparatus of the nephron senses the low flow state and releases renin. Renin then causes systemic vasoconstriction and affects the efferent arteriole of the unaffected kidney causing an increased glomerular filtration rate (GFR) and a pressure diuresis. Over time, the unaffected kidney develops hypertensive nephropathy, no longer able to maintain pressure diuresis, so systemic hypertension ensues. Aldosterone, which is also released from the RAAS, promotes sodium and water retention. In bilateral ARAS or a solitary kidney with significant ARAS, Goldblatt found a state of fluid retention due to decreased diuresis because of the absence of an unaffected kidney to balance the fluid retention, so volume-dependent hypertension develops.Citation23

Individuals with clinically significant ARAS also suffer from cardiovascular disease. These individuals experience proinflammatory effects on their cardiovascular system resulting in the development of: smooth muscle cell proliferation, endothelial cell dysfunction, arterial medial hypertrophy, myocardial fibrosis and plaque rupture.Citation24

Clinical Conditions

ARAS is associated with three main clinical disease processes that include: renovascular hypertension, cardiac destabilization syndromes and ischemic nephropathy. Renovascular hypertension is defined as an increase in arterial pressure caused by hemodynamically significant renal artery stenosis.Citation25 In this disease, resistant (refractory) hypertension develops which is difficult to control blood pressure despite maximally tolerated doses of three antihypertensive agents including a diuretic. In these individuals, after they undergo PTRAS they experience a significant reduction and/or normalization in their blood pressure.Citation26 A functional classification system has been developed to categorize ARAS and associated hypertension ().Citation26 Cardiac destabilization syndromes include: “flash” pulmonary edema events, ADHF and ACS.Citation27Citation30 Pickering syndrome describes a specific condition seen in individuals that have bilateral ARAS as they lack the compensatory mechanism of a functional kidney in regulating the body’s salt and fluid balance. These individuals also have hypertension and are prone to frequent “flash” pulmonary edema episodes. Ischemic nephropathy is a condition where local ischemia to the kidney causes tubulointerstitial injury and microvascular damage.Citation31 This creates a state of oxidative injury that leads to the production of cytokines and inflammation resulting in interstitial fibrosis and renal atrophy.Citation31

Table 1 Functional Classification of ARAS in Association with HypertensionCitation26

Diagnostic Modalities

The American College of Cardiology (ACC) and American Heart Association (AHA) clinical practice guidelines describe a variety of diagnostic imaging tools such as: DUS, computed tomography angiography (CTA) and magnetic resonance angiography (MRA) as screening tests to aid in the diagnosis of ARAS.Citation28 When non-invasive imaging tests are inconclusive and there is high degree of clinical suspicion for ARAS then catheter angiography is indicated.Citation32Citation35 To eliminate the inter-observer variability in the visual estimation of renal artery stenosis, a translesional pressure gradient is measured (ratio of the distal pressure to proximal pressure across the stenosis) to determine if ARAS is hemodynamically significance. A lesion is hemodynamically significant if on renal angiography the stenosis is 50–70% with a peak translesional gradient of at least 20 mmHg or a mean gradient of at least 10 mmHg.Citation34 However, angiographic ARAS lesions do not always indicate that there is renal ischemia. Newer technologies such as: BOLD MRI and dynamic contrast-enhanced MRI are used to quantify the degree of renal ischemia by measuring decreased renal tissue oxygenation with experimental-graded reduction in renal blood flow.Citation35 Although these imaging modalities are still being researched they have the potential to aid in distinguishing between viable and non-viable kidneys. compares the various imaging modalities for the detection of ARAS.Citation32Citation38 There are additional diagnostic tests that assess both the functional and physiological changes when evaluating ARAS and the interaction between the stenotic lesion and activation of RAAS. compares three physiologic diagnostic tests for ARAS.Citation39Citation41

Table 2 Imaging Modalities Utilized for Diagnosing ARASCitation32Citation38

Table 3 Physiologic Diagnostic Tests Used to Diagnose ARASCitation39Citation41

Optimal Medical Therapy

Lifestyle modifications with diet, physical activity and smoking cessation in addition to optimal medical therapy (OMT) are the initial steps for newly diagnosed ARAS. Furthermore, co-morbidities such as hypertension, hyperlipidemia and diabetes need to be well managed as they contribute to the deterioration in renal function and accelerate the disease progression in ARAS. The ACC and AHA recommend the use of an angiotensin-converting enzyme inhibitor (ACE-I) or angiotensin II receptor blocker (ARB) and calcium channel blockers for medical therapy in treatment of hypertension in the setting of ARAS.Citation42,Citation43 There is also evidence to support the use of other antihypertensive agents such as: thiazides, hydralazine, alpha-blockers and beta-blockers in addition to diuretics to effectively control blood pressure. ACE-I and ARB are 86% to 92% effective in lowering blood pressure in individuals with ARAS and should be one of the agents in their antihypertensive medication regimen.Citation43 However, individuals with ARAS and solitary functioning kidney, severe bilateral renal artery stenosis or advanced chronic kidney disease should be cautiously monitored while on ACE-I or ARB therapy as there is a slight risk for acute renal failure.Citation43 There have been no randomized-controlled studies studying the effects of various medical regimens on the management of hypertension associated with ARAS. This is due to individuals with ARAS having refractory hypertension and requiring multiple antihypertensive medications. Statin and antiplatelet therapies are also indicated in medical treatment of ARAS given that ARAS is a peripheral vascular disease.Citation44,Citation45

Clinical Trials

Three randomized-controlled trials have been conducted to compare PTRAS with OMT to OMT alone. The Cardiovascular Outcomes in Renal Atherosclerotic Lesions (CORAL), Angioplasty and Stenting for Renal Artery Lesions (ASTRAL) and Stent Placement in Patients with Atherosclerotic Renal Artery Stenosis and Impaired Renal Function (STAR) trials did not show PTRAS to be superior to OMT in the ARAS population with mild to moderate stenosis.Citation5Citation7 The lack of benefit for PTRAS was attributed to 1) a selection of patients with mild to moderate ARAS and low-risk features and 2) the lack of hemodynamic confirmation of the severity of mild to moderate ARAS. These studies did not enroll high-risk participants who had resistant (refractory) hypertension, cardiac destabilization syndromes or ischemic nephropathy.

The CORAL trial compared OMT alone to PTRAS with OMT in individuals with ARAS. These low-risk patients had hypertension with a systolic blood pressure of 155 mm Hg or higher while receiving two or more antihypertensive medications or had CKD with GFR of less than 60 mL/min/m2 calculated from the Modification of Diet in Renal Disease (MDRD) formula and attributed their hypertension or CKD to ARAS. The mean ARAS stenosis for randomized patients was 67.3%, and hemodynamic translesional gradients were not measured in moderate ARAS (50–70% lesions).Citation7 Primary endpoints included: mortality, renal function, and occurrence of adverse cardiovascular and renal events. They did not find any statistical difference after 43 months follow-up between the two groups.Citation7 Specifically, stent treatment did not influence GFR over 3 years in participants receiving RAAS inhibitor medical therapy along with strict control of traditional risk factors for renal disease and atherosclerosis such as hypertension, hyperlipidemia and diabetes. However, there was a difference of 2.3 mmHg reduction in systolic blood pressure favoring PTRAS.Citation7

The ASTRAL trial enrolled patients with an uncertain indication for PTRAS. These patients either had refractory hypertension or unexplained impaired renal function that was suggestive of ARAS. They underwent imaging either in the form of DUS, CTA, MRA or renal angiography. Physicians were unsure if these patients would benefit from renal revascularization. So they were randomized in the trial into an OMT group and OMT plus PTRAS group. They found that there were no benefits from PTRAS in terms of improving renal function or reducing cardiovascular events and deaths.Citation5 There was a small reduction in mean systolic blood pressure by 1.6 mmHg in the revascularization group compared to the control group.Citation5 The experience and skill of the interventionalists performing PTRAS were questioned due to 9% complication rate reported in this trial.Citation5

The STAR trial also compared renal artery stenting and OMT versus OMT alone for individuals with mild to moderate ARAS. Study participants had ARAS with greater than 50% stenotic lesion, estimated creatinine clearance (eCrCl) by Cockcroft-Gault equation with less than 80 mL/min/1.73 m2 and stable blood pressure less than 140/90 mmHg8. The primary endpoint investigated was progression of renal disease defined as greater than 20% decrease in eCrCl from baseline within first two years of follow-up. There was no observed benefit with PTRAS over only medical treatment on the progression of CKD. However, it is important to take into consideration that 30% of the patients randomized to the renal revascularization group had ARAS with a lesion less than 50%.Citation6

Observational cohort studies, in patients with high-risk ARAS have shown beneficial effects such as better hypertension management with renal stenting compared to OMT alone in treatment of patients with ARAS. The Herculink Elite Renal Stent to Treat Renal Artery Stenosis (HERCULES) trial studied individuals with ARAS that had greater than or equal to 60% stenosis detected by angiogram along with uncontrolled hypertension (on average taking 3.4 antihypertensive medications) and randomized them to OMT therapy alone or with PTRAS. The study’s endpoints included: change in blood pressure, antihypertensive medication regimen and renal function comparing baseline with 9 months follow-up. Renal revascularization via PTRAS was shown to have a statistically significant reduction in systolic blood pressure and stable kidney function.Citation46

Furthermore, studies were performed investigating the treatment options for ARAS and their effect on the progression of left ventricular hypertrophy in patients with CAD and ARAS. The renal artery stenosis in coronary artery disease trial showed neither PTRAS with medical therapy or medical therapy alone led to significant change in renal function at 1-year follow-up.Citation47 However, both groups had a statistically significant reduction in left ventricular mass index.Citation47 Moreover, the Cardiac Benefits of Renal Artery Stenting (CARMEL) study showed marked improvement in left ventricular filling pressures in individuals with ARAS and heart failure after undergoing PTRAS.Citation48

There are two randomized trials that have yet to publish their results. The Nephropathy Ischemic Therapy (NITER) trial randomized ARAS individuals into two arms: OMT alone versus OMT and PTRAS. The patients selected had stable chronic kidney disease (GFR >30 mL/min/m2), hypertension and hemodynamically significant renal luminal lesion greater than 70% diagnosed by DUS and confirmed by MRA.Citation49 The clinical endpoints include: initiation of dialysis, reduction of GFR by greater than 20% and death. The other trial is the Medical and Endovascular Treatment of Atherosclerotic Renal Artery Stenosis (METRAS), which had a similar intervention arm and enrolled similar participants from the ARAS population. Their main clinical endpoint is the GFR value in the ischemic kidney determined by renal scintigraphy. Additional endpoints include: reduction in blood pressure reading, improvement in quality of life and prevention of cardiovascular events.Citation50

Overall, published randomized control trials did not show differences in cumulative endpoint outcomes such as: blood pressure reduction, cardiovascular and cerebrovascular events, and change in renal function (decline, stabilization, improvement) or death compared to the observational trials. This is likely due to several factors. First of all, there was selection bias starting with the low-risk patients enrolled in the randomized trials. For example, participants in the ASTRAL trial had stable underlying chronic kidney disease, baseline eCrCl of 40 mL/min/1.73 m2 and it is not surprising to see that were no significant changes in renal function in either groups. Moreover, these patients did not have resistant hypertension and the inclusion criteria for blood pressure management varied considerably with blood pressure readings and number of medications used. Also, individuals with severe ARAS may not always have clinical manifestations. This was seen in the patient population of the ASTRAL trial who were asymptomatic and majority had ARAS incidentally diagnosed. That is why there is no justification for PTRAS of incidentally discovered ARAS. Additional factors that limited the application of these randomized control trials findings include: small sample size and short time interval with follow-up. Since these were intention to treat designed trials, the increased cross-over rate from the conservative therapy arm also influenced the overall results. See for summary of the top three clinical trials regarding PTRAS among the ARAS patient population.

Table 4 Comparison of Randomized Control Trials for OMT versus OMT and PTRAS in ARAS

Renal Revascularization

Renal revascularization using PTRAS in select groups of individuals with severe ARAS has proven to be beneficial. Severe ARAS is defined as a luminal stenosis of >70%, or if the stenosis is between 50% and 70% a trans-stenotic peak pressure gradient greater than 20 mmHg or mean pressure gradient greater than 10 mmHg is required.Citation26,Citation27 Clinical guidelines support stenting ARAS in individuals with an established indication for renal revascularization. Revascularization in patients with severe ARAS is indicated in the following individuals: (i) cardiac destabilization syndromes: flash pulmonary edema with severe hypertension, (ii) resistant (refractory) hypertension and (iii) rapidly progressive ischemic nephropathy, chronic kidney disease with GFR less than 45 cc/min/m2 and global renal ischemia.Citation26,Citation51 Observational studies have shown that after renal revascularization, ARAS individuals have improvement in their New York Heart Association (NYHA) functional class and fewer hospitalizations for ADHF.Citation29,Citation52 These individuals also have better controlled blood pressure. Renal revascularization in addition to coronary intervention for individuals with cardiac destabilization syndromes results in significant improvement in their left ventricular filling pressure.Citation29,Citation30

PTRAS with drug-eluting stents (DES) were studied in The Palmaz Genesis Peripheral Stainless Steel Balloon Expandable Stent in Renal Artery Treatment (GREAT) trial that compared sirolimus DES to bare-metal stents (BMS).Citation53 They observed no procedural complications, stent implantation failure/displacement or need for additional stent implantation in patients with ARAS who underwent PTRAS. The binary restenosis rate was 6.7% for DES versus 14.6% for the BMS (p=0.30).Citation53 With regard to the long-term procedural success of PTRAS, it is important to look at the long-term patency rates. Stent restenosis is 10–20% after 5 years of follow-up.Citation54,Citation55 Factors that promote long-term stent patency include short stent length and good implantation technique.

The reported rate of procedural complications with PTRAS in the first 30 days is low in experienced operator hands ().Citation56 The CORAL trial reported renal artery dissection in 2.2%, branch-vessel occlusion in 1.2% and distal embolization in 1.2%.Citation6 Other complications associated with PTRAS include: stent misplacement, access-vessel damage, stent embolization, renal artery thrombosis or occlusion and death.Citation6 Alternative access sites (such as: radial and brachial artery) to femoral artery access are preferred due to most individuals with ARAS having concurrent peripheral artery disease and the associated risk with femoral vascular complications.Citation57 A “no-touch” technique has been adopted for PTRAS where a second 0.035-inch J wire is placed within the guide catheter that is sitting within the renal artery to minimize contact between the guide catheter and atherosclerotic plaque.Citation58 This ultimately prevents cholesterol embolization.Citation58

Table 5 Procedural Complications Seen with PTRASCitation56

Percutaneous renal artery interventions are also associated with the risk of distal embolization. Preventative measures include the use of embolic protection device (EPDs). The Renal Artery Stenting With or Without Distal Protection Device and Use of a Platelet Aggregator Inhibitor (RESIST) were a prospective-randomized study that evaluated the safety and efficacy of PTRAS along with glycoprotein IIb/IIIa inhibitor (abciximab) and EPD on renal function. Platelets secrete soluble CD40 ligand (sCD40L) which promotes platelet activation. GP IIb/IIIa inhibits platelet activation. In this study, participants were randomized to one of the four groups: (1) EPD only, (2) no EPD and no abciximab, (3) abciximab only and (4) EPD and abciximab. Of those study participants who received EPD with renal revascularization, 26% of them had captured emboli in their filter.Citation59 Participants that were randomized to the EPD and abciximab showed significant decrease in sCD40L after PTRAS. Findings revealed that individuals that received abciximab and EPD during their renal artery stenting had stable or improved renal function compared to the controls.Citation59

Intravascular ultrasound (IVUS) is commonly utilized with PTRAS to aid in stent sizing and confirming apposition of the stent to the arterial wall. IVUS can reveal detailed information on the plaque morphology and accurately measure vessel diameter so operators of PTRAS can predict in advance which lesions are at risk for complications after interventions.Citation60 In a large case series study conducted at a single center site, the role of IVUS with PTRAS was evaluated. ARAS cases where IVUS was performed in conjunction with PTRAS and achieved good angiographic result required only additional therapeutic interventions in 23.5% of the cases.Citation60 This could be explained by 14.4% of the stents having incomplete stent apposition/expansion, 5.2% of renal arteries having dissections and 3.9% of the stents not covering the ostia.Citation60 Additional stenting was needed in 4.5% of the arteries that were treated. It is found that restenosis most often occurs in renal arteries with a diameter of less than 4.5 mm10. IVUS allows for successful placement of these stents while minimizing the risk of vessel wall rupture.Citation8 Overall, IVUS is used to achieve optimal stenting results by safely delivering the appropriate size stent with hopes of reducing future occurrence of developing renal artery restenosis.Citation60

Follow-Up

Patients should be followed clinically in terms of blood pressure control with laboratory results to monitor renal function, and surveillance DUS imaging is recommended to evaluate stent patency. DUS is the recommended imaging technique to screen for in-stent restenosis (ISR). DUS surveillance monitoring for renal stent patency should take into account that a stented artery is less compliant than a native artery and that peak systolic velocity (PSV) and systolic renal to aortic ratio (RAR) obtained by DUS are higher for any given degree of arterial narrowing within the stent; therefore, obtaining a post-procedure DUS is reasonable to establish a new baseline PSV.Citation61 ISR based on DUS is defined as greater than 70% stenosis and peak systolic velocity (PSV) greater than 395 cm/s.Citation61 Patients should have routine 30-day, 3-month, 6-month, 12-month and annual clinical, laboratory, and DUS follow-up for surveillance of ISR.Citation61

Guidelines and Appropriate Use Criteria (AUC)

The ACC/AHA guidelines for treating ARAS stem from the peripheral artery disease guidelines created in 2006.Citation27,Citation28 These recommendations are based on expert opinion, and observational studies. In 2018 Society for Cardiovascular Angiography and Interventions (SCAI) produced an appropriate use criteria (AUC) statement for renal artery stenting. They reported stenting as an appropriate treatment in specific groups of individuals with ARAS with severe stenosis.Citation28 See for summary of AUC for treatment of ARAS.Citation27,Citation28

Table 6 American College of Cardiology Appropriate Use Criteria for Treatment of ARAS

Conclusion

The clinical outcome of individuals with ARAS depends on both the degree of underlying renal parenchymal damage and atherosclerotic burden. In randomized control trials, the recruited patients had low-risk ARAS with <70% stenosis and underlying normal to mildly reduced renal function.Citation62 The selection of low-risk participants impacted the results of the trials. The subanalysis of the trials showed that participants with ARAS of 80% or greater along with acute presentation of ADHF, unstable angina, rapid deterioration of renal function and severe uncontrolled hypertension significantly benefited from renal revascularization in addition to OMT.Citation62

It may be worthwhile determining which ARAS patients have hibernating renal parenchyma along with functionally significant stenosis that can truly benefit from renal revascularization. Long-term outcomes of individuals with ARAS can be improved potentially from interventions such as, stem cell therapies that can inhibit oxidative injury and inflammation to the renal parenchyma and cardiovascular system.Citation63 These adjunct therapies could change the natural disease progression and improve their morbidity and mortality rate in individuals with ARAS. However, further investigative studies will need to prove that these therapies provide a renoprotective benefit.

Disclosure

There are no relationships with industry. The authors report no conflicts of interest in this work.

References

  • Kalra P, Guo H, Kausz A, et al. Atherosclerotic renovascular disease in United States patients aged 67 years or older: risk factors, revascularization and prognosis. Kidney Int. 2005;68(1):293–301. doi:10.1111/j.1523-1755.2005.00406.x15954920
  • Scoble J. The epidemiology and clinical manifestations of atherosclerotic renal disease In: Renal Vascular Disease. London, UK: WB Saunders Co, Ltd; 1996:303–314.
  • Payami B, Jafarizade M, Mousavi S, Sattari S, Nokhostin F. Prevalence and predictors of atherosclerotic renal artery stenosis in the hypertensive patients undergoing simultaneous coronary and renal angiography: a cross-sectional study. J Renal Inj Prev. 2016;5(1):34–38. doi:10.15171/jrip.2016.0827069966
  • Schreiber M, Pohl M, Novick A. The natural history of atherosclerotic and fibrous renal artery disease. Urol Clin North Am. 1984;11(3):383–392.6464247
  • Wheatley K, Ives N, Gray R, et al. Revascularization versus Medical Therapy for Renal-Artery Stenosis. N Engl J Med. 2009;361:1953–1962.19907042
  • Bax L, Mali W, Buskens E, et al. The benefit of stent placement and blood pressure and lipid-lowering for the prevention of progression of renal dysfunction caused by atherosclerotic ostial stenosis of the renal artery. the star-study: rationale and study design. J Nephrol. 2003;16(6):807–812.14736007
  • Cooper C, Murphy T, Cutlip D, et al. Stenting and medical therapy for atherosclerotic renal-artery stenosis. N Engl J Med. 2014;370(1):13–22. doi:10.1056/NEJMoa131075324245566
  • Lederman R, Mendelsohn F, Santos R, Phillips H, Stack R, Crowley J. Primary renal artery stenting: characteristics and outcomes after 363 procedures. Am Heart J. 2001;142(2):314–323. doi:10.1067/mhj.2001.11695811479472
  • Mitchell J, Subramanian R, White C, et al. Predicting Blood pressure improvement in hypertensive patients after renal artery stent placement: renal fractional flow reserve. Catheter Cardiovasc Interv. 2007;69(5):685–689. doi:10.1002/ccd.2109517351955
  • Leesar M, Varma J, Shapira A, et al. Prediction of hypertension improvement after stenting of renal artery stenosis: comparative accuracy of translesional pressure gradients, intravascular ultrasound, and angiography. J Am Coll Cardiol. 2009;53(25):2363–2371. doi:10.1016/j.jacc.2009.03.03119539148
  • Mangiacapra F, Trana C, Sarno G, et al. Translesional pressure gradients to predict blood pressure response after renal artery stenting in patients with renovascular hypertension. Circ Cardiovasc Interv. 2010;3(6):537–542. doi:10.1161/CIRCINTERVENTIONS.110.95770421078879
  • Silva J, Chan A, White C, et al. Elevated brain natriuretic peptide predicts blood pressure response after stent revascularization in patients with renal artery stenosis. Circulation. 2005;111(3):328–333. doi:10.1161/01.CIR.0000153271.77341.9F15655135
  • Sun D, Eirin A, Ebrahimi B, Textor S, Lerman A, Lerman L. Early atherosclerosis aggravates renal microvascular loss and fibrosis in swine renal artery stenosis. J Am Soc Hypertens. 2016;10(4):325–335. doi:10.1016/j.jash.2016.01.01926879682
  • Zhang X, Krier J, Carrascal C, et al. Low- energy shockwave therapy improves ischemic kidney microcirculation. JASN. 2016;27(12):3715–3724. doi:10.1681/ASN.201506070427297945
  • Cooper E, Xie Y, Nguyen H, et al. Early rapid decline in kidney function in medically managed patients with atherosclerotic renal artery stenosis. J Am Heart Assoc. 2019;8(11). doi:10.1161/JAHA.119.012366
  • Zierler R, Bergelin R, Isaacson J, Strandness D. Natural history of atherosclerotic renal artery stenosis: a prospective study with duplex ultrasonography. J Vasc Surg. 1994;19(2):250–257. doi:10.1016/S0741-5214(94)70100-88114186
  • Caps M, Zierler R, Polissar N, et al. Risk of atrophy in kidneys with atherosclerotic renal artery stenosis. Kidney Int. 1998;53(3):735–742. doi:10.1046/j.1523-1755.1998.00805.x9507221
  • Chabova V, Schirger A, Stanson A, McKusick M, Textor S. Outcomes of atherosclerotic renal artery stenosis managed without revascularization. Mayo Clin Proc. 2000;75(5):437–444. doi:10.1016/S0025-6196(11)64210-910807070
  • Watson P, Hadjipetrou P, Cox S, Piemonte T, Eisenhauer A. Effect of renal artery stenting on renal function and size in patients with atherosclerotic renovascular disease. Circulation. 2000;102(14):1671–1677. doi:10.1161/01.CIR.102.14.167111015346
  • Kalra P, Chrysochou C, Green D, et al. The benefit of renal artery stenting in patients with atheromatous renovascular disease and advanced chronic kidney disease. Catheter Cardiovasc Interv. 2010;75(1):1–10. doi:10.1002/ccd.2229019937777
  • Goldblatt H, Lynch J, Hanzal R, Summerville W. Studies on experimental hypertension: i. the production of persistent elevation of systolic blood pressure by means of renal ischemia. J Exp Med. 1934;59(3):347–379. doi:10.1084/jem.59.3.34719870251
  • Cohen J, Townsend R. Use of renin-angiotensin system blockade in patients with renal artery stenosis. CJASN. 2014;9(7):1149–1152. doi:10.2215/CJN.0424041424903389
  • Hocher B, George I, Rebstock J, et al. Endothelin system- dependent cardiac remodeling in renovascular hypertension. Hypertension. 1999;33(3):816–822. doi:10.1161/01.HYP.33.3.81610082493
  • Herrmann S, Textor S. Current concepts in the treatment of renovascular hypertension. Am J Hypertens. 2018;31(2):139–149. doi:10.1093/ajh/hpx15428985335
  • Van der Niepen P, Rossignol P, Lengele J, et al. Renal artery stenosis in patients with resistant hypertension: stent it or not? Curr Hypertens Rep. 2017;19(5). doi:10.1007/s11906-017-0703-8
  • Rocha-Singh K, Eisenhauer A, Textor S, et al. Atherosclerotic peripheral vascular disease symposium ii: interventional for renal artery disease. Circulation. 2008;118(25):2873–2878. doi:10.1161/CIRCULATIONAHA.108.19117819106410
  • Klein A, Jaff M, Gray B, et al. SCAI appropriate use criteria for peripheral arterial interventions: an update. Catheter Cardiovasc Interv. 2017;90(4):E90–E110. doi:10.1002/ccd.2714128489285
  • Hirsch A, Haskal Z, Hertzer N, et al. ACC/AHA 2005 practice guidelines for the management of patients with peripheral arterial disease (lower extremity, renal, mesenteric, and abdominal aortic): a collaborative report from the american association for vascular surgery/society for vascular surgery, society for cardiovascular angiography and interventions, society for vascular medicine and biology, society of interventional radiology, and the acc/aha task force on practice guidelines. Circulation. 2006;113(11):e463–e654. doi:10.1161/CIRCULATIONAHA.106.17452616549646
  • Messerli F, Bangalore S, Makani H, et al. Flash pulmonary edema and bilateral renal artery stenosis: the Pickering syndrome. Eur Heart J. 2011;32(18):2231–2235. doi:10.1093/eurheartj/ehr05621406441
  • Khosla S, White C, Collins T, Jenkins J, Shaw D, Ramee S. Effects of renal artery stent implantation in patients with renovascular hypertension presenting with unstable angina or congestive heart failure. Am J Cardiol. 1997;80(3):363–366. doi:10.1016/S0002-9149(97)00368-89264441
  • Garcia-Donaire J, Alcazar J. Ischemic nephropathy: detection and therapeutic intervention. Kidney Int. 2005;68(99):S131–S136. doi:10.1111/j.1523-1755.2005.09924.x
  • Schaberle W, Leyerer L, Schierling W, et al. Ultrasound diagnostics of renal artery stenosis. Gefasschirurgie. 2016;21(S1):4–13. doi:10.1007/s00772-015-0060-327034579
  • Rountas C, Vlychou M, Liakopoulos V, et al. Imaging modalities for renal artery stenosis in suspected renovascular hypertension: prospective intraindividual comparison of color doppler US, CT angiography, GD-enhanced MR angiography, and digital substraction angiography. Ren Fail. 2007;29(3):295–302. doi:10.1080/0886022060116630517497443
  • McLaughlin K, Jardine A, Moss J. Renal artery stenosis. BMJ. 2000;320(7242):1124–1127. doi:10.1136/bmj.320.7242.112410775226
  • Lim S, Chrysochou C, Buckley D, Kalra P, Sourbron S. Prediction and assessment of responses to renal artery revascularization with dynamic contrast-enhanced magnetic resonance imaging: a pilot study. Am J Physiol Renal Physiol. 2013;305(5):F672–F678. doi:10.1152/ajprenal.00007.201323804449
  • Ebrahimi B, Textor S, Lerman L. Renal Relevant radiology: renal functional magnetic resonance imaging. Clin J Am Soc Nephrol. 2014;9(2):395–405. doi:10.2215/CJN.0290031324370767
  • Waksman R, Kitabata H, Prati F, Albertucci M, Mintz G. Intravascular ultrasound versus optical coherence tomography guidance. J Am Coll Cardiol. 2013;67(17):S32–S40. doi:10.1016/j.jacc.2013.08.709
  • Naghi J, Palakodeti S, Ang L, Reeves R, Patel M, Mahmud E. Renal Frame Count: A Measure Of Renal Flow That Predicts Success Of Renal Artery Stenting In Hypertensive Patients. Catheter Cardiovasc Interv. 2015;86(2):304–309. doi:10.1002/ccd.2594626198066
  • Kotiliar C, Inserra F, Forcada P. Are plasma renin activity and aldosterone levels useful as a screening test to differentiate between unilateral and bilateral renal artery stenosis in hypertensive patients? J Hypertens. 2010;28(3):594–601. doi:10.1097/HJH.0b013e32833487d420104188
  • Stratigis S, Stylianou K, Kyriazis P, et al. Renal artery stenting for atherosclerotic renal artery stenosis identified in patients with coronary artery disease: does captopril renal scintigraphy predict outcomes? J Clin Hypertens. 2018;20(2):373–381. doi:10.1111/jch.13160
  • Taylor A, Fletcher J, Nally J, et al. Procedure guideline for diagnosis of renovascular hypertension. society of nuclear medicine. J Nucl Med. 1998;39(7):1297–1302.9669414
  • Badila E, Tintea E. How to manage renovascular hypertension. An article from the e-journal of the ESC council for cardiology practice. ESC. 2014;13:8–9.
  • Muneer K, Nair A. Angiotensin-converting enzyme inhibitors and receptor blockers in heart failure and chronic kidney disease- Demystifying controversies. Indian Heart J. 2017;69(3):371–374. doi:10.1016/j.ihj.2016.08.00728648436
  • Silva V, Martin L, Franco R, et al. Pleiotropic effects of statins may improve outcomes in atherosclerotic renovascular disease. Am J Hypertens. 2008;21(10):1163–1168. doi:10.1038/ajh.2008.24918670414
  • Berger J, Krantz M, Kittelson J, Hiatt W. Aspirin for the prevention of cardiovascular events in patients with peripheral artery disease. a meta-analysis of randomized trials. JAMA. 2009;301(18):1909–1919. doi:10.1001/jama.2009.62319436018
  • Jaff M, Bates M, Sullivan T, et al. Significant reduction in systolic blood pressure following renal artery stenting in patients with uncontrolled hypertension: results from the HERCULES trial. Catheter Cardiovasc Interv. 2012;80(3):343–350. doi:10.1002/ccd.2444922511402
  • Marcantoni C, Zanoli L, Rastelli S, et al. Stenting of renal artery stenosis in coronary artery disease (ras-cad) study: a prospective, randomized trial. J Nephrol. 2009;22(1):13–16.19229814
  • Kawarada O, Kume T, Nakamura S, et al. Cardiac function response to stenting in atherosclerotic renal artery disease with and without heart failure: results from the Carmel study. ESC Heart Fail. 2019;6(2):319–327. doi:10.1002/ehf2.1239130614643
  • Scarpioni R, Michieletti E, Cristinelli L, et al. Atherosclerotic renovascular disease: medical therapy versus medical therapy plus renal artery stenting in preventing renal failure progression: the rationale and study design of a prospective, multicenter and randomized trial (NITER). J Nephrol. 2005;18(4):423–428.16245247
  • Rossi G, Seccia T, Miotto D, et al. The medical and endovascular treatment of atherosclerotic renal artery stenosis (METRAS) study: rationale and study design. J Hum Hypertens. 2012;26(8):507–516. doi:10.1038/jhh.2011.6221716318
  • Bailey S, Beckman J, Dao T, et al. ACC/AHA/SCAI/SIR/SVM 2018 appropriate use criteria for peripheral artery intervention: a report of the american college of cardiology appropriate use criteria task force, american heart association, society for cardiovascular angiography and interventions, society of interventional radiology, and society for vascular medicine. J Am Coll Cardiol. 2019;73(2):214–237. doi:10.1016/j.jacc.2018.10.00230573393
  • Gray B, Olin J, Childs M, Sullivan T, Bacharach M. Clinical benefit of renal artery angioplasty with stenting for the control of recurrent and refractory congestive heart failure. Vasc Med. 2002;7(4):275–279. doi:10.1191/1358863x02vm456oa12710843
  • Sapoval M, Zahringer M, Pattynama P, et al. Low-profile stent system for treatment of atherosclerotic renal artery stenosis: the GREAT trial. J Vasc Interv Radiol. 2005;16(9):1195–1202. doi:10.1097/01.RVI.0000171765.67665.D316151060
  • Blum U, Krumme B, Flugel P, et al. Treatment of ostial renal-artery stenoses with vascular endoprostheses after unsuccessful balloon angioplasty. N Engl J Med. 1997;336(7):459–465. doi:10.1056/NEJM1997021333607029017938
  • Henry M, Amor M, Henry I, et al. Stents in the treatment of renal artery stenosis: long-term follow-up. J Endovasc Surg. 1999;6(1):42–51. doi:10.1583/1074-6218(1999)006<0042:SITTOR>2.0.CO;210088889
  • Ruzsa Z, Toth K, Jambrik Z, et al. Transradial access for renal artery intervention. Interv Med Appl Sci. 2014;6(3):97–103. doi:10.1556/IMAS.6.2014.3.125243074
  • Feldman R, Wargovich T, Bittl J. No-touch technique for reducing aortic wall trauma during renal artery stenting. Catheter Cardiovasc Interv. 1999;46(2):245–248. doi:10.1002/(SICI)1522-726X(199902)46:2<245::AID-CCD27>3.0.CO;2-V10348553
  • Haller S, Adlakha S, Reed G, et al. Platelet activation in patients with atherosclerotic renal artery stenosis undergoing stent revascularization. Clinical Journal of the American Society of Nephrology. 2011;6(9):2185–2191. doi:10.2215/CJN.0314041121817131
  • Campbell J, Stone P, Bates M. Technical discussion of diagnostic angiography and intervention of atherosclerotic renal artery stenosis. Semin Vasc Surg. 2013;26(4):150–160. doi:10.1053/j.semvascsurg.2014.06.00225220320
  • Mohler E, Gornik H, Gerhard-Herman M, et al. ACCF/ACR/AIUM/ASE/ASN/ICAVL/SCAI/SCCT/SIR/SVM/SVS 2012 appropriate use criteria for peripheral vascular ultrasound and physiological testing part i: arterial ultrasound and physiological testing: a report of the american college of cardiology foundation appropriate use criteria task force, american college of radiology, american institute of ultrasound in medicine, american society of echocardiography, american society of nephrology, intersocietal commission for the accreditation of vascular laboratories, society for cardiovascular angiography and interventions, society of cardiovascular computed tomography, society for interventional radiology, society for vascular medicine, and society for vascular surgery. J Am Coll Cardiol. 2012;60(3):242–276. doi:10.1016/j.jacc.2012.02.00922694840
  • Chi Y, White C, Thornton S, Milani R. Ultrasound velocity criteria for renal in-stent restenosis. J Vasc Surg. 2009;50(1):119–123. doi:10.1016/j.jvs.2008.12.06619233590
  • Ritchie J, Kalra P. ASTRAL and beyond: who is appropriate to consider for renal artery revascularization? Vasc Dis Manage. 2011;8:E12–E20.
  • Eirin A, Textor S, Lerman L. Novel therapeutic strategies for renovascular disease. Curr Opin Nephrol Hypertens. 2019;28(4):383–389. doi:10.1097/MNH.000000000000051331045658
Download PDF

Related research

People also read lists articles that other readers of this article have read.

Recommended articles lists articles that we recommend and is powered by our AI driven recommendation engine.

Cited by lists all citing articles based on Crossref citations.
Articles with the Crossref icon will open in a new tab.