Renal Artery Stenosis

Back

Practice Essentials

Renal artery stenosis (RAS) is the major cause of renovascular hypertension and may account for 1-10% of the 50 million cases of hypertension in the United States population.[1] See the image below.



View Image

Renal artery stenosis/renovascular hypertension. Flush aortogram in a 32-year-old man with familial hypercholesterolemia and difficult-to-control hype....

Apart from its role in the pathogenesis of hypertension, renal artery stenosis is also being increasingly recognized as an important cause of chronic renal insufficiency and end-stage renal disease. In older individuals, atherosclerosis is by far the most common etiology of renal artery stenosis.[2, 3] As the renal artery lumen progressively narrows, renal blood flow decreases. Eventually,the decreased perfusion compromises renal function and structure.

Patients with renal artery stenosis may present with one or more of the following (see Presentation):

The workup in a patient with possible renal artery stenosis includes laboratory studies of renal function and imaging studies of the kidneys and renal circulation (see Workup). Treatment includes pharmacologic control of hypertension and serum cholesterol levels, with surgical or percutaneous revascularization a consideration in selected patients (see Treatment and Medication).[4, 5] Guidelines covering the diagnosis and medical and surgical therapy of renal artery stenosis have been published (see Guidelines).

For patient education information, see the Cholesterol Center, as well as Chronic Kidney Disease, High Cholesterol, Cholesterol FAQs, and Atorvastatin (Lipitor).

Pathophysiology

In patients with atherosclerosis, the initiator of endothelial injury is not clear. However, dyslipidemia, hypertension, cigarette smoking, diabetes mellitus, viral infection, immune injury, and increased homocysteine levels may contribute to endothelial injury. 

The formation of atherosclerotic lesions involves increased permeability of endothelium to plasma macromolecules (eg, low-density lipoprotein [LDL]), increased turnover of endothelial cells and smooth muscle cells, and increased numbers of intimal macrophages. When atherogenic lipoproteins exceed certain critical levels, the mechanical forces may enhance lipoprotein insudation in these regions, leading to early atheromatous lesions.

Renal blood flow is 3- to 5-fold greater than the perfusion to other organs because it drives glomerular capillary filtration. Both glomerular capillary hydrostatic pressure and renal blood flow are important determinants of the glomerular filtration rate (GFR).[6]

In patients with renal artery stenosis, the chronic ischemia produced by the obstruction of renal blood flow leads to adaptive changes in the kidney that are more pronounced in the tubular tissue. These changes include atrophy with the following:

In patients with renal artery stenosis, the GFR is dependent on angiotensin II and other modulators that maintain the autoregulation system between the afferent and efferent arteries and can fail to maintain the GFR when renal perfusion pressure drops below 70-85 mm Hg. Significant functional impairment of autoregulation, leading to a decrease in the GFR, is not likely to be observed until arterial luminal narrowing exceeds 50%.

The degree of renal artery stenosis that would justify any attempt at either surgical intervention or radiologic intervention is not known. One study found that when the pressure distal to renal artery stenosis was less than 90% of aortic pressure, renin release from the affected kidney was significantly elevated (renin being measured in the ipsilateral renal vein). This might be useful as a functional measurement of significant renovascular stenosis leading to hypertension and, thus, a marker of greater likelihood of benefit from angioplasty and stenting.[7, 8]

Etiology

Risk factors associated with ischemic renal disease (IRD) are as follows:

Epidemiology

United States

Studies suggest that ischemic nephropathy may be responsible for 5-22% of advanced renal disease in all patients older than 50 years.

Mortality/Morbidity

The consequences of renal artery stenosis are hypertension, which may be particularly difficult to control or may require multiple antihypertensive agents (with increased adverse effects), and progressive loss of renal function (ischemic nephropathy).

In addition, the discovery of atherosclerotic renal vascular disease (RVD) frequently occurs in the setting of generalized vascular disease (ie, cerebral, cardiac, peripheral), with the co-morbidity associated with disease in those vascular beds. Thus, any therapeutic intervention for renal artery stenosis should logically take into account the underlying prognosis associated with these co-morbidities.

Race-, Sex-, and Age-related Variances

RVD is less common in blacks than in whites. The incidence rate in two studies of patients with severe hypertension was 27-45% in whites versus 8-19% in blacks.[9]

Although the incidence of atherosclerotic RVD is independent of sex, Crowley et al showed that female sex (as well as older age, elevated serum creatinine level, coronary artery disease, peripheral vascular disease, hypertension, and cerebrovascular disease) is an independent predictor of RVD progression.[10]

In 1964, Holley et al reported data from 295 consecutive autopsies performed in their institution during a 10-month period.[11] The mean age at death was 61 years. The prevalence rate of renal artery stenosis was 27% of 256 cases identified as having history of hypertension, while 56% showed significant stenosis (>50% luminal narrowing). In normotensive patients, 17% had severe renal artery stenosis (> 80% luminal narrowing). In those older than 70 years, 62% had severe renal artery stenosis.

Another similar autopsy study reported similar results, with 5% of patients older than 64 years showing severe stenosis; this figure increased to 18% for patients aged 65-74 years and 42% for patients older than 75 years.

History and Physical

Patients with ischemic renal vascular disease (RVD) present with one or more of the following clinical, historical, or diagnostic scenarios:

Laboratory Studies

Obtain serum creatinine levels to assess the level of renal dysfunction. Serum levels can be used to calculate an estimated creatinine clearance based on the Cockcroft-Gault equation or the Modification of Diet in Renal Disease (MDRD) formula.[12]

Perform a 24-hour urine collection, or obtain a protein-creatinine ratio on a random void urine specimen, to more accurately assess the level of renal dysfunction and to measure the degree of proteinuria. Vascular renal disease is more often associated with minimal-to-moderate degrees of proteinuria; levels rarely reach the nephrotic range.

Perform urinalysis to ensure that red blood cells or red blood cell casts (a hallmark of glomerulonephritis) are absent.

Perform serologic tests for systemic lupus erythematosus or vasculitis if these conditions are suggested (eg, antinuclear antibodies, C3, C4, antinuclear cytoplasmic antibodies).

Studies designed to assess the renin-angiotensin system are of little diagnostic utility in patients with atherosclerotic renovascular disease (RVD).

Peripheral renin activity reflects volume status in healthy individuals. It may be elevated in patients with renovascular causes of hypertension and in those with essential hypertension. It is equally nondiscriminatory in patients with atherosclerotic RVD with ischemic nephropathy.

Imaging Studies

Ultrasonography

Renal ultrasonography scanning is performed frequently in patients with renal dysfunction. Ultrasonography scanning is an anatomic, not a functional, test. The only contribution to the entity of renal artery stenosis is a suggestion of the diagnosis when examination results indicate significant asymmetry of kidney size (ie, size discrepancy of >1.5 cm). Additionally, ultrasonography may be useful in detecting the presence of a solitary kidney, in which case, renal artery stenosis of that solitary kidney takes on more significant prognostic and therapeutic importance.

Duplex ultrasonographic scanning combines a B-mode ultrasonographic image with a pulse Doppler unit to obtain flow velocity data. The technique is noninvasive, relatively inexpensive, and can be used in patients with any level of renal function. The test is very sensitive and specific (98%); however, it is very labor intensive and technician-dependent. Thus, duplex ultrasonographic scanning may not be available in many medical centers.

Radermacher et al reported that the renal resistance index, calculated through the use of color Doppler ultrasonography, can be used to predict the outcome of invasive therapy  for renal artery stenosis.Patients with a resistance index (calculated as [1 - end-diastolic velocity divided by maximal systolic velocity] x 100) greater than 80, indicating small vessel and large vessel disease, were likely to have a poor response to angioplasty or surgery with respect to improvement in hypertension, renal function, or kidney survival.[13]

Radionuclide scanning

Use of radionuclide scanning, particularly following a single dose of captopril, is more useful in patients with normal renal function, in whom fibromuscular disease is suspected. See the image below.



View Image

Renal artery stenosis/renovascular hypertension. Left, Sonograms of the kidneys on a 57-year-old woman with difficult-to-control hypertension shows ki....

Stratigis et al reported that captopril renal scintigraphy was highly accurate in predicting the  clinical outcome of percutaneous renal revascularization with stenting in patients with atherosclerotic renal artery stenosis who have a high coronary artery disease burden. In their study of 64 consecutive patients referred after coronary angiography, scintigraphy had sensitivity and specificity of 100% for both a hypertension and renal benefit from renal revascularization in patients with atherosclerotic renal artery stenosis of ≥ 70%.[14]

Patients with possible ischemic nephropathy (ie, serum creatinine values >2 mg/dL) frequently have associated parenchymal disease or bilateral vascular disease, in which case, the results obtained with scanning are unable to distinguish between parenchymal renal disease and renal artery stenosis/ischemic nephropathy.

Spiral CT angiography

This technique involves the use of an intravenous injection of a relatively large dose of iodinated contrast material and allows 3-dimensional reconstruction images of the renal arteries.

In 1995, Olbricht et al compared renal CT angiography with arterial digital subtraction angiography for detecting renal artery narrowing of more than 50%.[15] The CT technique showed positive and negative predictive values of 91%.

Spiral CT angiography is a useful technique that avoids arterial catheterization and produces accurate images of renal artery anatomy. This technique requires iodinated contrast material and significant time to perform the computer-based reconstruction. This technique avoids arterial puncture and, thus, the risk of atheroemboli, but it can be associated with contrast associated nephropathy, particularly in patients with preexisting chronic kidney disease.

Magnetic resonance imaging

Magnetic resonance angiography (MRA) is a noninvasive technique capable of demonstrating the renal vascular anatomy and revealing physiological information about kidney function (see the image below). This technique is capable of direct visualization of renal artery lesions without iodinated contrast material and provides a measurement of the absolute blood flow rate, GFR, and renal perfusion rate. Furthermore, MRA can provide accurate serial renal size and volume measurement. The limitations of MRA are its expense and its contraindication in patients with metallic clips, pacemakers, intraocular metallic devices, or other implants.



View Image

Three-dimensional gadolinium-enhanced magnetic resonance angiograms (MRAs) show medial fibroplasia, which appears as classic string-of-beads sign. Thi....

Concern regarding the association of gadolinium use with the development of nephrogenic systemic fibrosis (NSF) in patients with moderate to severe renal insufficiency significantly limits the use of this agent and, therefore, this modality, for the recognition of anatomic renal artery stenosis. In one study, for example, Broome et al reported an odds ratio of 22.3 for the development of NSF in dialysis patients who underwent enhanced imaging with the gadolinium-based contrast agent gadodiamide (vs patients in the study who underwent unenhanced imaging).[16]

However, all of the patients in the Broome study who developed NSF received 0.2 mmol/kg of gadodiamide; no cases of NSF were found among members of the cohort who received 0.1 mmol/kg of the agent. In a subsequent study, Garovic et al found no reported cases of NSF among 335 patients who underwent contrast-enhanced MRA, using 0.1 mmol/kg gadodiamide, for suspected or known renal artery stenosis.[17]

MRA has been validated only for the stenosis situated in the proximal 3-3.5 cm of renal arteries. Distal renal artery stenosis and segmental renal artery stenosis were generally not analyzed. The sensitivity of MRA was 90% for proximal renal artery stenosis, 82% for main renal artery stenosis, and 0% for segmental stenosis. In a follow-up study, Loubeyre and colleagues examined 46 patients with clinical renal artery stenosis.[18] Using a combination of techniques, they determined a sensitivity of 100%, a specificity of 90%, a positive predictive value of 58%, and a negative predictive value of 100% for detecting stenosis of the main, but not accessory or distal, renal artery. These data were obtained with fast-scanning machines using gadolinium enhancement and a breath-holding technique.[19]

An additional study compared the accuracy of CT angiography and MRA to digital subtraction angiography and concluded that digital subtraction angiography remains the method of choice to establish a diagnosis.

However, in the above-mentioned study by Garovic et al, the diagnostic efficacy of contrast-enhanced MRA (using 0.1 mmol/kg gadodiamide) was compared with that of intra-arterial digital subtraction angiography, using a cohort of 335 patients with known or suspected renal artery stenosis. The authors concluded, based on image analyses by multiple readers, that the sensitivity and specificity of the 2 modalities were equivalent in the evaluation of renal artery stenosis.[17]

Blood oxygen level–dependent MRI

Blood oxygen level–dependent (BOLD) MRI is a noninvasive technique for evaluating kidney tissue oxygenation that requires no contrast exposure and has the potential to allow functional assessment for patients with atherosclerotic renal artery stenosis. Although a decrease in renal blood flow does not invariably lead to renal hypoxia, severe vascular occlusion can overwhelm the kidney's capacity to adapt to reduced blood flow, and BOLD MRI has demonstrated renal cortical hypoxia in patients with severe renal artery stenosis.[20]

Conventional arteriography

This technique remains the criterion standard for the confirmation and identification of renal artery occlusion in persons with IRD. Specialists can perform renal arteriography by conventional aortography, intravenous subtraction angiography, intra-arterial subtraction angiography, or carbon dioxide angiography. See the images below.



View Image

Renal artery stenosis/renovascular hypertension. Left, Flush aortogram in a 63-year-old man with hypertension shows marked stenosis of the right renal....



View Image

Conventional flush aortogram in a 47-year-old woman with difficult-to-control hypertension shows the characteristic string-of-beads sign (arrows) of t....

Conventional aortography produces excellent radiographic images of the renal artery, but it requires an arterial puncture, carries the risk of cholesterol emboli, and uses a moderate amount of contrast material with the risk of contrast-induced acute tubular necrosis (ATN). Low osmolar contrast material can limit the risk of this complication. Complication rates for renal angiography are 6-10% in most series.

Intravenous subtraction angiography is sensitive for identifying stenosis of the main renal artery but does not demonstrate accessory or branch renal arteries sufficiently. Solitary stenosis of a branch of the renal artery is a common source of renovascular hypertension in pediatric patients, among the fraction in whom the disorder does not result from syndromes such as neurofibromatosis.[21] However, intravenous subtraction angiography avoids the use of a high volume of contrast and the risk of artery puncture and arterial atherosclerotic emboli.

Intra-arterial digital subtraction angiography has a high diagnostic accuracy compared to conventional angiography and is associated with fewer complications, lower doses of contrast, and smaller catheter size.

Carbon dioxide angiography is an alternative angiographic contrast agent used in combination with digital subtraction angiography to avoid the risk of conventional nephrotoxic contrast agents in patients with severe renal insufficiency. The images obtained are similar in quality to intra-arterial digital subtraction angiography; however, the technique requires an experienced investigator and a dedicated person to inject the carbon dioxide. Discomfort and inadequate images are potential complications of the procedure.

Contrast nephrotoxicity

Patients with progressive ischemic nephropathy (ie, underlying chronic renal failure) are at risk for contrast nephrotoxicity and should be informed of this risk prior to any contrast procedure.

Contrast nephropathy typically manifests as a brief rise in the serum creatinine level 3-6 days after exposure to radiocontrast and is reported in up to 40% of patients with underlying renal failure.

Most patients with contrast nephropathy ultimately recover renal function. Porter reviewed results from nearly 300 patients with contrast nephropathy and concluded that fewer than 10% of these patients required dialysis permanently.

Selection of diagnostic tests

Once patients are identified as being at high risk for renal artery stenosis, the choice of the best test for diagnosis is controversial.

Accurate identification of patients with correctable renovascular hypertension can be difficult with use of standard noninvasive techniques (eg, sonography) because they provide only indirect evidence of the presence of renal artery lesions.

On the other hand, invasive techniques with more accurate diagnostic potential can produce a worsening of renal function because of contrast toxicity and complications related to the procedures themselves (eg, arterial puncture, catheter-induced atheroembolism).

Gilfeather et al performed a study evaluating conventional angiography versus gadolinium-enhanced MRA in 54 patients and 107 kidneys.[22] The study showed that in 70 kidneys (65%), the average degree of stenosis reported by readers of both modalities differed by 10% or less. In 22 cases (21%), MRA overestimated the degree of stenosis by more than 10% relative to the results of conventional angiography; in 15 cases (14%), MRA underestimated the stenosis by more than 10%.

The obvious advantages of conventional angiography are its ability to determine the clinical importance of suggestive lesions and the ability to concurrently perform endovascular therapy. In addition, measurement of the pressure gradient across a stenotic lesion may be helpful in determining the clinical significance of a lesion.[23] However, specialists should weigh these advantages against the higher cost and greater morbidity of conventional angiography. The slightly inferior variability of MRA in diagnostic interpretation further supports the use of this technique as potentially the most appropriate tool for screening patients strongly suggested to have atherosclerotic RVD.

See Imaging in Renal Artery Stenosis/Renovascular Hypertension for a complete discussion of this topic.

Incidental atherosclerotic renovascular disease is often discovered in patients at the time of cardiac angiography. The impact of this finding on a patient’s outcome and, therefore, on the need to dilate and stent the renal vessel, the so-called "drive-by" percutaneous transluminal renal angioplasty with stenting (PTRAS), is the subject of intense debate.[24, 25, 26]

Medical Care

All patients with significant (>80%) bilateral stenosis or stenosis in a solitary functioning kidney are candidates for revascularization, regardless of whether they have renal insufficiency. When renal insufficiency is present, patients with unilateral stenosis are also possible candidates for revascularization. The criteria are slightly different depending on the presence or absence of renal insufficiency.

When renal function is normal or nearly normal, specialists recommend revascularization for prevention of renal insufficiency if the patient meets the following criteria:

Conversely, physicians can choose observation instead of revascularization (serial control every 6 mo with duplex scanning, accurate correction of dyslipidemia, use of drugs that block platelet aggregation) when the patient meets the following criteria:

When renal insufficiency is present and the objective is recovery of renal function together with prevention of further renal function impairment, the prerequisites for revascularization are as follows:

When either of those conditions is satisfied, the authors propose revascularization if the following apply:

Restrict conservative treatment in patients with an established diagnosis of ischemic renal disease (IRD) to those with absolute contraindications to surgery or angioplasty or to patients who are likely to succumb due to other comorbid conditions before advancing to end-stage renal disease because of IRD. Clinicians must rely on pharmacologic agents (eg, combination of calcium channel blockers to control blood pressure and optimize renal perfusion), accepting the high probability of deterioration in renal function and shortened survival.

Surgical Care

In 1962, Morris et al compiled the first report on a surgical treatment for occlusion of the renal arteries.[27] They described eight patients with renal failure who underwent revascularization. Six of these patients returned to essentially normal renal function.

Reports from retrospective studies clearly document that surgical revascularization can improve renal function in patients with ischemic nephropathy. In 1993, Rimmer and Gennari reported postoperative improvement (ie, 20% decrease in serum creatinine concentration) in more than half the patients in nine studies.[28]  A long-term study (median follow-up, 10.6 years) of open surgical renal artery reconstruction that included 31 patients with stenosis reported low mortality, fairly low morbidity, and excellent durability and recommended that open surgery remain an option for patients with complex renal artery disease.[29]

Bypass procedures include aortorenal, hepatorenal, splenorenal, and ileorenal conduits constructed with autologous saphenous veins, autologous arteries, or prosthetic material. For atherosclerotic disease, surgeons can also perform atherectomy to improve renal blood flow. In persons with nonatheromatous renal artery disease, surgeons can reconstruct the renal arteries ex vivo and then can reimplant the revascularized kidney. Reilly and coworkers reported an operative mortality rate of only 6% and immediate improvement in the serum creatinine level of 32% of surgical bypass procedures in 35 patients with solitary kidneys.[30]

In the last few years, researchers report that the results are more consistent. The largest series suggests that the glomerular filtration rate (GFR) improved postoperatively in 49-80% of patients with underlying renal failure.

Guidelines from the American Heart Association/American College of Cardiology and the European Society of Cardiology include recommendations for the use of peripheral revascularization and surgical revascularization. See Guidelines.

Revascularization

One unresolved issue is how to determine whether revascularization will salvage renal function when the renal artery is totally occluded. Features that may predict successful restoration of renal function include the following:

Specialists suggest nephrectomy as a modality of treatment in persons with unilateral renovascular disease (RVD). In one study that compared nephrectomy versus revascularization in 95 patients and 190 kidneys, and revascularization showed a greater response, better management in blood pressure, and a significant improvement in the GFR.

Angioplasty and stenting

Angioplasty is effective for treating renovascular hypertension associated with atheromatous lesions. Indicative of this is the decreased rate of referrals for surgical renovascularization of atheromatous renovascular hypertensive nephropathy by the early 1980s (from 41% to 26%). In practical terms, angioplasty can usually limit hospitalization, avoid general anesthesia, and minimize tissue trauma.

In 1987, Ziegelbaum et al compared the outcomes of angioplasty and surgical bypass.[31] The researchers studied 70 elderly patients with atheromatous disease and found that angioplasty caused major complications, including two deaths. Renal function improved (ie, >20% decrease in serum creatinine level) in 57.5% of surgery patients but in only 15.8% of angioplasty patients. After 48 months of follow-up, the unassisted patency rate was only 69% in the angioplasty group compared to 100% in the surgical group.

Erdoes et al examined the results of 58 surgical and 18 percutaneous revascularizations in nonrandomized patients.[32] These two approaches showed similar operation risk (mortality rate 4.8-5.3%); however, functional improvement (ie, blood pressure, serum creatinine level) and patency of the renal artery were dramatically better in the surgical group than in the revascularization group after nearly 4 years of follow-up.

van Jaarsveld et al reported the results of a multicenter trial designed to evaluate the relative benefit of angioplasty versus medical therapy for hypertension associated with RVD.[33] They found that both groups had similar decreases in blood pressure, although the patients who underwent angioplasty used one fewer hypertensive medication. While renal function was improved at 3 months in those undergoing angioplasty, the function at 12 months was similar. They concluded that restricting angioplasty to those with atherosclerotic renovascular hypertension persisting despite use of three or more antihypertensive medications was prudent. Note that the patients in this trial did not undergo angioplasty with stent placement. In addition, 9% of patients in the medical therapy–only group experienced total occlusion of the affected renal artery on 12-month follow-up angiography.

A randomized study by van de Ven et al that compared percutaneous transluminal angioplasty (PTA) for ostial ATH with PTA with stent (PTAS) showed that PTAS is a better technique compared to PTA to achieve vessel patency in ostial atherosclerotic renal artery stenosis.[34] The primary success rate was 57% for PTA compared with 88% for PTAS. The restenosis rate after a successful primary procedure was 48% for PTA versus 14% for PTAS. In the last few years, the use of PTAS in patients with ostial stenosis or early restenosis has led to a considerable reduction in the restenosis rate.

However, controversy still surrounds the best approach to patients with atherosclerotic renovascular disease, as reviewed by Ives et al, Textor, and Plouin.[35, 36, 37] In a study of patients with atherosclerotic renal artery stenosis, Bax et al found that renal artery stenting had no clear effect on renal function impairment in the patients and led to significant complications in some of them.[38] The multicenter trial included 140 patients with creatinine clearance of less than 80 mL/min per 1.73 m2 and renal artery stenosis of 50% or greater. All patients received medical treatment with antihypertensive agents, a statin, and aspirin. Although 64 patients were randomized to stent placement, only 46 had the procedure; in many patients, assessment of renal artery stenosis by noninvasive imaging was inaccurate and stenting was in fact not indicated.

In the study, progression of renal dysfunction, as indicated by a decrease in creatinine clearance of 20% or greater, occurred in 16% of patients in the stent placement group and in 22% of patients in the medication group (hazard ratio, 0.73 [95% confidence interval [CI], 0.33-1.61]). Serious complications in the stent group included two procedure-related deaths.

The results of the 2009 ASTRAL trial included 806 patients with at least one stenotic renal artery who were randomized to revascularization (ie, interventional radiology) or medical therapy.[39] The estimated glomerular filtration rate was approximately 40 mL/min in each group. No difference was observed in the primary outcome, decline of renal function, between the two groups. Although both studies have some design flaws, they suggest that medical therapy is appropriate for the single, stenotic renal artery. Two review articles, one conducted by Simon and the other conducted by Lao et al, discuss this subject in significant detail.[40, 41]

The Cardiovascular Outcomes in Renal Atherosclerotic Lesions (CORAL) study demonstrated no added benefit from the addition of stenting to medical therapy for renal artery stenosis. In CORAL, 947 participants with atherosclerotic renal-artery stenosis and either systolic hypertension or chronic kidney disease were randomized to medical therapy plus renal artery stenting or medical therapy alone. The resulting rate of adverse cardiovascular and renal events (ie, death, myocardial infarction, stroke, hospitalization for heart failure, progressive renal insufficiency, or the need for renal replacement therapy) showed no significant differences (35.1% and 35.8%, respectively; hazard ratio with stenting, 0.94; 95% CI, 0.76 to 1.17; P = 0.58).[42]

However, a post hoc analysis of CORAL by Murphy et al found that in patients whose baseline urine albumin/creatinine ratio was at or below the median (22.5 mg/g), renal artery stenting was associated with significantly better outcome, including event-free survival, cardiovascular disease–related death, progressive renal insufficiency, and overall survival. The authors suggest that low albuminuria may identify a potentially large subgroup of renal artery stenosis patients who would benefit from stent placement plus medical therapy.[43]

A metal-analysis of revascularization versus medical therapy for the treatment of renal artery stenosis found no clear benefit from percutaneous transluminal angioplasty with or without stenting over medical management. In the final analysis, which included 540 studies and seven randomized controlled trials and 2,139 patients, angioplasty with or without stenting was not superior to medical therapy with respect to any outcome. The incidence of nonfatal myocardial infarction was 6.74% in both the stenting and medical therapy group (odds ratio 0.998, 95% CI 0.698 to 1.427, P = 0.992), and the incidence of renal events with stenting population was 19.58% versus 20.53% with medical therapy (odds ratio 0.945, 95% CI 0.755 to 1.182, P = 0.620).[44]

Revascularization may not result in restoration of renal function because of damage sustained during the period of reduced blood flow.[5] Hypoxia can result in functional loss of microcirculation (rarefaction) and recruitment of inflammatory cellular elements (as indicated by elevation of inflammatory biomarkers[45] ) that ultimately produce fibrosis.[36]

However, there is also evidence that percutaneous revascularization may benefit some patients in high-risk subgroups. In a retrospective analysis of a single-center prospective cohort study of 467 patients, Ritchie and colleagues reported that those individuals presenting with flash pulmonary edema, rapidly declining kidney function, or refractory hypertension who received revascularization had a significantly reduced risk for death and cardiovascular events compared to those who received medical management.[46]

In a single-center, case-control study that included 188 patients with RAS, Meredith and colleagues identified previous myocardial infarction, left ventricular ejection fraction (LVEF) ≤35%, and glomerular filtration rate ≤45 mL/min/1.73 m2 as risk factors. Renal artery stenting was associated with a 43% reduction in mortality in patients with one or one of those risk factors, but stenting had no effect on mortality in patients with two or three risk factors.[47]

Use of renal artery stenting has been declining in recent years, mainly because trials to date have failed to demonstrate major advantages to renal revascularization. However, in a 2013 review, Textor et al note that, “these trials have been small, conducted over short intervals, and have been ferociously criticized on methodologic grounds”.[48] These authors observe that endovascular repair is most likely to succeed when it is performed in patients with a recent deterioration in kidney function, which argues for careful identification and selection of patients for revascularization before loss of GFR becomes far advanced.

In some institutions, PTAS is the first-step approach in patients with IRD, and practitioners reserve surgery for the technical failure of percutaneous maneuvers. However, surgery remains the first choice of treatment under certain conditions, including the following:

A small, retrospective review of 20 patients who underwent a revascularization procedure (ie, surgery, PTA, PTAS) revealed a high complication rate (increased serum creatinine level in 25%, eosinophilia in 5%, atheroemboli in 15%, renal artery dissection in 5%) despite achieving improved serum creatine values in only 25%.[49] Fifty percent of patients had stable azotemia. The authors and others conclude that a prospective, randomized trial of medical management with or without PTAS is warranted for this complex clinical problem.

Renal artery fibromuscular dysplasia

PTA is the treatment of choice for renal artery fibromuscular dysplasia. A retrospective analysis by Yang et al of 76 PTA procedures in 64 patients reported that in the majority of cases (79.7%) the patient experienced immediate clinical benefit, with cure of hypertension in 35.9% and improvement in hypertension and a lower requirement for antihypertensive medications in 43.8%. In the long term (mean, 47.5 months), the survival rate was 96.9%, freedom from restenosis was 84.4%, and 76.6% of patients showed a sustained clinical benefit (cure rate 40.6%, improvement rate 35.9%).[50]

Patients with restenosis showed good response to repeat PTA. Eight patients were treated with a second procedure and two had a third procedure, resulting in improvement in hypertension in half of those patients.[50]

Consultations

The optimal approach to therapeutic interventions should be developed in consultation with an interventional radiologist and vascular surgeon to determine the relative expertise of these subspecialists at the individual medical center.

Guidelines Summary

The following organizations have released guidelines for the management of renal artery stenosis (RAS):

Diagnosis

The 2013 ACC/AHA and 2017 ESC guidelines recommend performing diagnostic studies to identify RAS in patients with any of the following[51, 52] :

The ACC/AHA guidelines define resistant hypertension as failure of blood-pressure control despite full doses of an appropriate three-drug regimen including a diuretic.[51] The ESC defines it as failure to achieve target blood pressure despite use of four drug classes, including a diuretic and a mineralocorticoid receptor antagonist in appropriate doses, in cases where another form of secondary hypertension is unlikely.[52]

The ESC also lists the combination of hypertension and abdominal bruit as a possible indication of RAS.[52]

In its 2014 SCAI Expert Consensus Statement for Renal Artery Stenting Appropriate Use, the SCAI utilized the ACC/AHA recommendations.[53]

Class I recommendations for establishing a diagnosis of RAS generally concur and include the following[51, 52] :

When the clinical index of suspicion is high and the results of noninvasive tests are inconclusive, ACC/AHA recommends catheter angiography,[51] while ESC recommends digital subtraction angiography.[52]

Both guidelines are in agreement that captopril renal scintigraphy, selective renal vein renin measurements, plasma renin activity, and the captopril test are not recommended as useful screening tests for RAS (class III).[51, 52]

SCAI recommends renal angiography as the gold standard for invasive assessment of hemodynamically significant RAS and categorizes stenosis severity as follows[53] :

Severe angiographic stenosis is considered hemodynamically significant. Moderate angiographic stenosis is considered hemodynamically significant only when the patient also has a resting mean pressure gradient >10 mm Hg or systolic hyperemic pressure gradient >20 mm Hg or renal fractional flow reserve (FFR) ≤0.8. Mild and moderate stenosis that is not hemodynamically significant should only rarely be considered for revascularization.[53]

Medical Therapy

ACC/AHA, ESC and SCAI all prefer medical therapy as the first-line treatment for RAS.[51, 52, 53] ACC/AHA and ESC recommend ACE inhibitors, ARBs, and calcium channel blockers for unilateral RAS,[51, 52] but ESC advises that patients with bilateral severe RAS or RAS in a single functional kidney require very careful monitoring when started on ACE inhibitors or ARBs.[52]

The ACC/AHA also recommends beta-blockers for treatment of hypertension associated with RAS.[51] The ESC considers the use of antiplatelet agents to be part of best medical therapy.[52]

Revascularization

The ACC/AHA guidelines recommend percutaneous revascularization in patients with hemodynamically significant RAS and any of the following[51] :

In addition, percutaneous revascularization is reasonable for patients with progressive chronic kidney disease (CKD) and bilateral RAS or a RAS to a single functioning kidney and can be considered for unilateral RAS with chronic renal insufficiency.[51] The ESC also recommends revascularization in patients with symptomatic fibromuscular dysplasia who have signs of organ ischemia.[52]

ACC/AHA and ESC recommend renal stent placement for ostial atherosclerotic RAS (class I).[51]

ACC/AHA  gives a class I recommendation for balloon angioplasty with bailout stent placement if necessary for fibromuscular dysplasia lesions;[51] whereas ESC recommends considering balloon angioplasty with or without stenting for patients with RAS and recurrent congestive heart failure or sudden pulmonary edema and preserved systolic left ventricular function (class IIb).{ref55)

Based on an expert panel review of scientific data, the SCAI concluded that patients with the following are most likely to benefit from renal artery stenting[53] :

The SCAI concluded that patients with any of the following are typically not good candidates for renal artery stenting[53] :

ACC/AHA gives class I recommendations to surgical revascularization for the following indications:[51]

ESC gives a class IIb recommendation to consider surgical revascularization in patients undergoing repair of the aorta or with complex anatomy of renal arteries or after failure of endovascular treatment.[52]

Medication Summary

The general approach to therapy of ischemic nephropathy involves control of hypertension, preferably with angiotensin-converting enzyme (ACE) inhibitors or angiotensin receptor blockers (ARBs). Unfortunately, these two classes of drugs may lead to increased serum creatinine levels and hyperkalemia, limiting their utility. In this case, calcium channel blockers are likely the most useful and best-tolerated agents.

Initiate strict control of serum cholesterol, which usually requires the use of statins, as with all conditions associated with atherosclerosis. A study by Bianchi et al suggested that statins, in addition to ACE inhibitors and ARBs, may reduce proteinuria and slow the progression of kidney disease.[54]

Captopril (Capoten)

Clinical Context:  Parent compound of this class of medications. Sulfhydryl group associated with proteinuria and neutropenia when used at high doses. Prevents conversion of angiotensin I to angiotensin II, a potent vasoconstrictor, resulting in lower aldosterone secretion.

Enalapril (Vasotec)

Clinical Context:  One example of this class of compounds. Similar precautions to captopril with respect to potential increase in potassium and creatinine. Major adverse effect is dry cough. Newer and, occasionally, better tolerated than parent compound. Many variations that allow for once-daily dosing and better tissue ACE inhibition.

Class Summary

These agents decrease aldosterone secretion.

Losartan (Cozaar)

Clinical Context:  Initial compound in class to gain approval. Useful for treatment of hypertension and heart failure in patients who are intolerant of ACE inhibitors. Many alternative compounds exist with few significant clinical differences. Nonpeptide angiotensin II receptor antagonist that blocks the vasoconstricting and aldosterone-secreting effects of angiotensin II. May induce a more complete inhibition of the renin-angiotensin system than ACE inhibitors, does not affect the response to bradykinin, and is less likely to be associated with cough and angioedema. For patients unable to tolerate ACE inhibitors.

Class Summary

Useful for hypertension and heart failure in patients who are intolerant of ACE inhibitors. Many alternative compounds exist with few significant clinical differences.

Atorvastatin (Lipitor)

Clinical Context:  One of many compounds with comparable efficacy and adverse effect profiles. Inhibits HMG-CoA reductase, which, in turn, inhibits cholesterol synthesis and increases cholesterol metabolism.

Class Summary

Adjunct to diet to reduce total and LDL cholesterol in patients with hypercholesterolemia. Also lower triglycerides.

Further Outpatient Care

In view of the natural history of RVD, patients require serial determinations of serum creatinine levels. Adequate blood pressure control is required, with monitoring of serum potassium levels as necessary. Duplex ultrasound, if available, allows regular follow-up of radiologic progression.

Prognosis

Researchers have studied the natural history of atherosclerotic renal artery stenosis by obtaining images from sequential abdominal aortographs or duplex ultrasound scans in patients with documented renal artery lesions who have been treated medically. Most studies show that progressive arterial obstruction occurs in 42-53% of patients with atherosclerotic renal artery stenosis, often within the first 2 years of radiographic follow-up. The incidence rate of progression to complete renal artery occlusion in these studies ranges from 9-16%; this often occurs in patients with a high-degree stenosis. In a study of 85 patients at the Cleveland Clinic who were followed for 3-172 months, patients with mild-to-moderate stenosis remained unchanged upon follow-up, and 39% of patients with greater than 75% lesions progressed to total occlusion.[55]

What is renal artery stenosis (RAS)?What are the signs and symptoms of renal artery stenosis (RAS)?What is involved in the workup and management of renal artery stenosis (RAS)?What is the pathophysiology of renal artery stenosis (RAS)?Which factors affect the glomerular filtration rate (GFR) in the pathophysiology of renal artery stenosis (RAS)?What is the effect of chronic ischemia in the pathophysiology of renal artery stenosis (RAS)?What is the role of glomerular filtration rate (GFR) in the pathophysiology of renal artery stenosis (RAS)?What degree of renal artery stenosis justifies an attempt at either surgical or radiologic intervention?What are the risk factors for renal artery stenosis (RAS)?What is the prevalence of renal artery stenosis (RAS) in the US?What are the morbidities of renal artery stenosis (RAS)?What are the racial predilections for renal artery stenosis (RAS)?How does the prevalence of renal artery stenosis (RAS) vary by sex?How does the prevalence of renal artery stenosis (RAS) vary by age?Which clinical history is characteristic of renal artery stenosis (RAS)?Which physical findings suggest renal artery stenosis (RAS)?Which physical findings are characteristic of renal vascular disease (RVD) in renal artery stenosis (RAS)?What are the differential diagnoses for Renal Artery Stenosis?What is the role of serum creatinine testing in the workup of renal artery stenosis (RAS)?What is the role of 24-hour urine collection in the workup of renal artery stenosis (RAS)?What is the role of urinalysis in the workup of renal artery stenosis (RAS)?What is the role of serologic tests in the workup of renal artery stenosis (RAS)?What is the role of renin-angiotensin system assessment in the workup of renal artery stenosis (RAS)?What is the role of peripheral renin activity in the diagnosis of renal artery stenosis (RAS)?What is the role of blood oxygen level–dependent (BOLD) MRI in the workup of renal artery stenosis (RAS)?What is the role of ultrasonography in the workup of renal artery stenosis (RAS)?What is the role of radionuclide scanning in the workup of renal artery stenosis (RAS)?What is the role of spiral angiography in the workup of renal artery stenosis (RAS)?What is the role of magnetic resonance angiography (MRA) in the workup of renal artery stenosis (RAS)?What are concerns regarding gadolinium use in imaging studies for the diagnosis of renal artery stenosis (RAS)?What is the efficacy of magnetic resonance angiography (MRA) in the workup of renal artery stenosis (RAS)?What is the role of conventional angiography in the workup of renal artery stenosis (RAS)?What are the advantages of conventional aortography in the workup of renal artery stenosis (RAS)?What is the role of IV subtraction angiography in the workup of renal artery stenosis (RAS)?What are the advantages of intra-arterial digital subtraction angiography in the workup of renal artery stenosis (RAS)?What is the role of carbon dioxide angiography in the workup of renal artery stenosis (RAS)?What causes contrast nephrotoxicity in the workup of renal artery stenosis (RAS)?How are diagnostic tests selected for renal artery stenosis (RAS)?How does conventional angiography compare to gadolinium-enhanced magnetic resonance angiography (MRA) for the diagnosis of renal artery stenosis (RAS)?What is the significance of an incidental finding of atherosclerotic renovascular disease during the evaluation of renal artery stenosis (RAS)?What is the role of revascularization in the treatment of renal artery stenosis (RAS)?What are the criteria for observation instead of revascularization in treatment of renal artery stenosis (RAS)?What are the prerequisites for revascularization in the treatment of renal artery stenosis (RAS)?What are the indications for conservative treatment of renal artery stenosis (RAS)?What is the efficacy of surgical revascularization for renal artery stenosis (RAS)?What is the role of bypass procedures in the treatment of renal artery stenosis (RAS)?Which features predict successful restoration of renal function after revascularization in renal artery stenosis (RAS)?What is the efficacy of angioplasty in the treatment of renal artery stenosis (RAS)?What are the outcomes of angioplasty and surgical bypass for the treatment of renal artery stenosis (RAS)?How does angioplasty compare to percutaneous revascularization for the treatments for renal artery stenosis (RAS)?What are the benefits of angioplasty for the management of hypertension in renal artery stenosis (RAS)?What is the efficacy of percutaneous transluminal angioplasty with stent (PTAS) for the treatment of renal artery stenosis (RAS)?What is the best approach to treatment of atherosclerotic renal artery stenosis (RAS)?What are the benefits of the addition of stenting to medical therapy for renal artery stenosis?What is the evidence for the use of revascularization in the treatment of renal artery stenosis?What are risk factors for mortality in the treatment of renal artery stenosis (RAS)?What is the role of renal artery stenting in the treatment of renal artery stenosis (RAS)?When is surgery indicated as first-line treatment for renal artery stenosis (RAS)?What are the complication rates associated with percutaneous transluminal angioplasty with stent (PTAS) for the treatment of renal artery stenosis (RAS)?What is the treatment of choice for renal artery fibromuscular dysplasia?Which specialist consultations are beneficial in the treatment of renal artery stenosis (RAS)?What are the treatment guidelines for renal artery fibromuscular dysplasia?Which organizations have released treatment guidelines for renal artery stenosis (RAS)?What are guidelines for the workup of renal artery stenosis (RAS)?What are the class I recommendations for establishing a diagnosis of renal artery stenosis (RAS)?What are the SCAI guidelines for use of renal angiography in renal artery stenosis (RAS)?What are guidelines for first-line treatments of renal artery stenosis (RAS)?What are ACC/AHA guidelines for percutaneous revascularization in renal artery stenosis (RAS)?What are the treatment guidelines for ostial atherosclerotic renal artery stenosis (RAS)?According to SCAI guidelines, which patients with renal artery stenosis (RAS) are most likely to benefit from renal artery stenting?What are the ACC/AHA guidelines for surgical revascularization for renal artery stenosis (RAS)?Which medications are used for the treatment of renal artery stenosis (RAS)?Which medications in the drug class HMG-CoA reductase inhibitors are used in the treatment of Renal Artery Stenosis?Which medications in the drug class Angiotensin II receptor antagonists are used in the treatment of Renal Artery Stenosis?Which medications in the drug class Angiotensin-converting enzyme inhibitors are used in the treatment of Renal Artery Stenosis?What is included in long-term monitoring of patients with renal artery stenosis (RAS)?What is the prognosis of renal artery stenosis (RAS)?

Author

Bruce S Spinowitz, MD, FACP, Clinical Professor of Medicine, Weill Medical College of Cornell University; School of Medicine; Associate Chairman, Associate Director and Attending Physician, Department of Medicine, Division of Nephrology, New York Hospital Medical Center Queens; Associate, Nephrology Associates, PC

Disclosure: Received grant/research funds from AMAG Pharmaceuticals for independent contractor; Received grant/research funds from Amgen for independent contractor; Received grant/research funds from Vifor for independent contractor; Received grant/research funds from Hospira for independent contractor; Received grant/research funds from Relypsa for independent contractor; Received grant/research funds from Akebia for independent contractor; Received grant/research funds from ZS Pharma for none.

Coauthor(s)

Joanna Rodriguez, MD,

Disclosure: Nothing to disclose.

Specialty Editors

Francisco Talavera, PharmD, PhD, Adjunct Assistant Professor, University of Nebraska Medical Center College of Pharmacy; Editor-in-Chief, Medscape Drug Reference

Disclosure: Received salary from Medscape for employment. for: Medscape.

Eleanor Lederer, MD, FASN, Professor of Medicine, Chief, Nephrology Division, Director, Nephrology Training Program, Director, Metabolic Stone Clinic, Kidney Disease Program, University of Louisville School of Medicine; Consulting Staff, Louisville Veterans Affairs Hospital

Disclosure: Serve(d) as a director, officer, partner, employee, advisor, consultant or trustee for: American Society of Nephrology<br/>Received income in an amount equal to or greater than $250 from: Healthcare Quality Strategies, Inc<br/>Received grant/research funds from Dept of Veterans Affairs for research; Received salary from American Society of Nephrology for asn council position; Received salary from University of Louisville for employment; Received salary from University of Louisville Physicians for employment; Received contract payment from American Physician Institute for Advanced Professional Studies, LLC for independent contractor; Received contract payment from Healthcare Quality Strategies, Inc for independent cont.

Chief Editor

Vecihi Batuman, MD, FASN, Huberwald Professor of Medicine, Section of Nephrology-Hypertension, Tulane University School of Medicine; Chief, Renal Section, Southeast Louisiana Veterans Health Care System

Disclosure: Nothing to disclose.

Acknowledgements

Donald A Feinfeld, MD, FACP, FASN Consulting Staff, Division of Nephrology and Hypertension, Beth Israel Medical Center

Disclosure: Nothing to disclose.

References

  1. Bokhari MR, Bokhari SRA. Renal Artery Stenosis. Radiology. 2018 Jan. 181320. [View Abstract]
  2. Chrysochou C, Kalra PA. Current Management of Atherosclerotic Renovascular Disease - What Have We Learned from ASTRAL?. Nephron Clin Pract. 2010 Feb 20. 115(1):c73-c81. [View Abstract]
  3. Plouin PF, Bax L. Diagnosis and treatment of renal artery stenosis. Nat Rev Nephrol. 2010 Mar. 6(3):151-9. [View Abstract]
  4. Tafur JD, White CJ. Renal Artery Stenosis: When to Revascularize in 2017. Curr Probl Cardiol. 2017 Apr. 42 (4):110-135. [View Abstract]
  5. Textor SC. Renal Arterial Disease and Hypertension. Med Clin North Am. 2017 Jan. 101 (1):65-79. [View Abstract]
  6. Iida M, Maeda H, Yamamoto M, et al. Association of renal artery stenosis with aortic jet velocity in hypertensive patients with aortic valve sclerosis. Am J Hypertens. 2010 Feb. 23(2):197-201. [View Abstract]
  7. De Bruyne B, Manoharan G, Pijls NH, et al. Assessment of renal artery stenosis severity by pressure gradient measurements. J Am Coll Cardiol. 2006 Nov 7. 48(9):1851-5. [View Abstract]
  8. Simon JF. Stenting atherosclerotic renal arteries: time to be less aggressive. Cleve Clin J Med. 2010 Mar. 77(3):178-89. [View Abstract]
  9. Jazrawi A, Darda S, Burke P, et al. Is race a risk factor for the development of renal artery stenosis?. Cardiol Res Pract. 2009. 2009:817987. [View Abstract]
  10. Crowley JJ, Santos RM, Peter RH, et al. Progression of renal artery stenosis in patients undergoing cardiac catheterization. Am Heart J. 1998 Nov. 136(5):913-8. [View Abstract]
  11. Holley KE, Hunt JC, Brown AL Jr, et al. Renal artery stenosis. A clinical-pathologic study in normotensive and hypertensive patients. Am J Med. 1964 Jul. 37:14-22.
  12. Levey AS, Bosch JP, Lewis JB, et al. A more accurate method to estimate glomerular filtration rate from serum creatinine: a new prediction equation. Modification of Diet in Renal Disease Study Group. Ann Intern Med. 1999 Mar 16. 130(6):461-70. [View Abstract]
  13. Radermacher J, Chavan A, Bleck J, et al. Use of Doppler ultrasonography to predict the outcome of therapy for renal-artery stenosis. N Engl J Med. 2001 Feb 8. 344(6):410-7. [View Abstract]
  14. Stratigis S, Stylianou K, Kyriazis PP, Dermitzaki EK, Lygerou D, Syngelaki 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 (Greenwich). 2018 Feb. 20 (2):373-381. [View Abstract]
  15. Olbricht CJ, Paul K, Prokop M, et al. Minimally invasive diagnosis of renal artery stenosis by spiral computed tomography angiography. Kidney Int. 1995 Oct. 48(4):1332-7. [View Abstract]
  16. Broome DR, Girguis MS, Baron PW, et al. Gadodiamide-associated nephrogenic systemic fibrosis: why radiologists should be concerned. AJR Am J Roentgenol. 2007 Feb. 188(2):586-92. [View Abstract]
  17. Garovic VD, Achauer MA, Kittner T, et al. Comparison of gadodiamide-enhanced MR angiography to intraarterial digital subtraction angiography for evaluation of renal artery stenosis: results of a phase III multicenter trial. J Magn Reson Imaging. 2010 Feb. 31(2):390-7. [View Abstract]
  18. Loubeyre P, Trolliet P, Cahen R, et al. MR angiography of renal artery stenosis: value of the combination of three-dimensional time-of-flight and three-dimensional phase-contrast MR angiography sequences. AJR Am J Roentgenol. 1996 Aug. 167(2):489-94. [View Abstract]
  19. Vasbinder GB, Nelemans PJ, Kessels AG, et al. Accuracy of computed tomographic angiography and magnetic resonance angiography for diagnosing renal artery stenosis. Ann Intern Med. 2004 Nov 2. 141(9):674-82; discussion 682. [View Abstract]
  20. Gloviczki ML, Saad A, Textor SC. Blood oxygen level-dependent (BOLD) MRI analysis in atherosclerotic renal artery stenosis. Curr Opin Nephrol Hypertens. 2013 Sep. 22 (5):519-24. [View Abstract]
  21. Andersson Z, Thisted E, Andersen UB. Renal Branch Artery Stenosis: a Diagnostic Challenge? A Case Report with Review of the Literature. Urology. 2016 Jun 28. 96 (1):205-9. [View Abstract]
  22. Gilfeather M, Yoon HC, Siegelman ES, et al. Renal artery stenosis: evaluation with conventional angiography versus gadolinium-enhanced MR angiography. Radiology. 1999 Feb. 210(2):367-72. [View Abstract]
  23. Gross CM, Kramer J, Weingartner O, et al. Determination of renal arterial stenosis severity: comparison of pressure gradient and vessel diameter. Radiology. 2001 Sep. 220(3):751-6.
  24. Cooper CJ, Murphy TP. Is renal artery stenting the correct treatment of renal artery stenosis? The case for renal artery stenting for treatment of renal artery stenosis. Circulation. 2007 Jan 16. 115(2):263-9; discussion 270. [View Abstract]
  25. Dworkin LD, Jamerson KA. Is renal artery stenting the correct treatment of renal artery stenosis? Case against angioplasty and stenting of atherosclerotic renal artery stenosis. Circulation. 2007 Jan 16. 115(2):271-6; discussion 276. [View Abstract]
  26. Levin A, Linas S, Luft FC, et al. Controversies in renal artery stenosis: a review by the American Society of Nephrology Advisory Group on Hypertension. Am J Nephrol. 2007. 27(2):212-20. [View Abstract]
  27. Morris GC, DeBakey ME, Cooley DA. Surgical Treatment of renal failure of renovascular origin. JAMA. 1962. 182:609-12.
  28. Rimmer JM, Gennari FJ. Atherosclerotic renovascular disease and progressive renal failure. Ann Intern Med. 1993 May 1. 118(9):712-9. [View Abstract]
  29. Steuer J, Bergqvist D, Björck M. Surgical Renovascular Reconstruction for Renal Artery Stenosis and Aneurysm: Long-Term Durability and Survival. Eur J Vasc Endovasc Surg. 2018 Oct 18. [View Abstract]
  30. Reilly JM, Rubin BG, Thompson RW, et al. Revascularization of the solitary kidney: a challenging problem in a high risk population. Surgery. 1996 Oct. 120(4):732-6; discussion 736-7. [View Abstract]
  31. Ziegelbaum M, Novick AC, Hayes J, et al. Management of renal arterial disease in the elderly patient. Surg Gynecol Obstet. 1987 Aug. 165(2):130-4. [View Abstract]
  32. Erdoes LS, Berman SS, Hunter GC, et al. Comparative analysis of percutaneous transluminal angioplasty and operation for renal revascularization. Am J Kidney Dis. 1996 Apr. 27(4):496-503. [View Abstract]
  33. van Jaarsveld BC, Krijnen P, Pieterman H, et al. The effect of balloon angioplasty on hypertension in atherosclerotic renal-artery stenosis. Dutch Renal Artery Stenosis Intervention Cooperative Study Group. N Engl J Med. 2000 Apr 6. 342(14):1007-14. [View Abstract]
  34. van de Ven PJ, Kaatee R, Beutler JJ, et al. Arterial stenting and balloon angioplasty in ostial atherosclerotic renovascular disease: a randomised trial. Lancet. 1999 Jan 23. 353(9149):282-6. [View Abstract]
  35. Ives NJ, Wheatley K, Stowe RL, et al. Continuing uncertainty about the value of percutaneous revascularization in atherosclerotic renovascular disease: a meta-analysis of randomized trials. Nephrol Dial Transplant. 2003 Feb. 18(2):298-304. [View Abstract]
  36. Textor SC, Lerman LO. Paradigm Shifts in Atherosclerotic Renovascular Disease: Where Are We Now?. J Am Soc Nephrol. 2015 Sep. 26 (9):2074-80. [View Abstract]
  37. Plouin PF. Stable patients with atherosclerotic renal artery stenosis should be treated first with medical management. Am J Kidney Dis. 2003 Nov. 42(5):851-7. [View Abstract]
  38. Bax L, Woittiez AJ, Kouwenberg HJ, et al. Stent placement in patients with atherosclerotic renal artery stenosis and impaired renal function: a randomized trial. Ann Intern Med. 2009 Jun 16. 150(12):840-8, W150-1. [View Abstract]
  39. Wheatley K, Ives N, Gray R, et al. Revascularization versus medical therapy for renal-artery stenosis. N Engl J Med. 2009 Nov 12. 361(20):1953-62. [View Abstract]
  40. Simon JF. Stenting atherosclerotic renal arteries: time to be less aggressive. Cleve Clin J Med. 2010 Mar. 77(3):178-89. [View Abstract]
  41. Safian RD, Textor SC. Renal-artery stenosis. N Engl J Med. 2001 Feb 8. 344(6):431-42. [View Abstract]
  42. Cooper CJ, Murphy TP, Cutlip DE, Jamerson K, Henrich W, Reid DM, et al. Stenting and medical therapy for atherosclerotic renal-artery stenosis. N Engl J Med. 2014 Jan 2. 370(1):13-22. [View Abstract]
  43. Murphy TP, Cooper CJ, Pencina KM, D'Agostino R, Massaro J, Cutlip DE, et al. Relationship of Albuminuria and Renal Artery Stent Outcomes: Results From the CORAL Randomized Clinical Trial (Cardiovascular Outcomes With Renal Artery Lesions). Hypertension. 2016 Nov. 68 (5):1145-1152. [View Abstract]
  44. Riaz IB, Husnain M, Riaz H, Asawaeer M, Bilal J, Pandit A, et al. Meta-analysis of revascularization versus medical therapy for atherosclerotic renal artery stenosis. Am J Cardiol. 2014 Oct 1. 114(7):1116-23. [View Abstract]
  45. Wang W, Saad A, Herrmann SM, Eirin Massat A, McKusick MA, Misra S, et al. Changes in inflammatory biomarkers after renal revascularization in atherosclerotic renal artery stenosis. Nephrol Dial Transplant. 2016 Jan 29. [View Abstract]
  46. Ritchie J, Green D, Chrysochou C, Chalmers N, Foley RN, Kalra PA. High-risk clinical presentations in atherosclerotic renovascular disease: prognosis and response to renal artery revascularization. Am J Kidney Dis. 2014 Feb. 63(2):186-97. [View Abstract]
  47. Meredith D, Bazemore TC, Shah A, Dilley J, Stouffer GA. Identification of Factors Associated With Improved Survival After Renal Artery Stenting. Am J Cardiol. 2017 Feb 15. 119 (4):664-668. [View Abstract]
  48. Textor SC, Misra S, Oderich GS. Percutaneous revascularization for ischemic nephropathy: the past, present, and future. Kidney Int. 2013 Jan. 83(1):28-40. [View Abstract]
  49. Dejani H, Eisen TD, Finkelstein FO. Revascularization of renal artery stenosis in patients with renal insufficiency. Am J Kidney Dis. 2000 Oct. 36(4):752-8. [View Abstract]
  50. Yang YK, Zhang Y, Meng X, Yang KQ, Jiang XJ, Wu HY, et al. Clinical characteristics and treatment of renal artery fibromuscular dysplasia with percutaneous transluminal angioplasty: a long-term follow-up study. Clin Res Cardiol. 2016 Jun 6. [View Abstract]
  51. [Guideline] Anderson JL, Halperin JL, Albert NM, Bozkurt B, Brindis RG, Curtis LH, et al. Management of patients with peripheral artery disease (compilation of 2005 and 2011 ACCF/AHA guideline recommendations): a report of the American College of Cardiology Foundation/American Heart Association Task Force on Practice Guidelines. Circulation. 2013 Apr 2. 127 (13):1425-43. [View Abstract]
  52. [Guideline] Aboyans V, et al; ESC Scientific Document Group. 2017 ESC Guidelines on the Diagnosis and Treatment of Peripheral Arterial Diseases, in collaboration with the European Society for Vascular Surgery (ESVS): Document covering atherosclerotic disease of extracranial carotid and vertebral, mesenteric, renal, upper and lower extremity arteriesEndorsed by: the European Stroke Organization (ESO)The Task Force for the Diagnosis and Treatment of Peripheral Arterial Diseases of the European Society of Cardiology (ESC) and of the European Society for V... Eur Heart J. 2017 Aug 26. 32 (22):2851-906. [View Abstract]
  53. [Guideline] Parikh SA, Shishehbor MH, Gray BH, White CJ, Jaff MR. SCAI expert consensus statement for renal artery stenting appropriate use. Catheter Cardiovasc Interv. 2014 Dec 1. 84 (7):1163-71. [View Abstract]
  54. Bianchi S, Bigazzi R, Caiazza A, et al. A controlled, prospective study of the effects of atorvastatin on proteinuria and progression of kidney disease. Am J Kidney Dis. 2003 Mar. 41(3):565-70. [View Abstract]
  55. Schreiber MJ, Pohl MA, Novick AC. The natural history of atherosclerotic and fibrous renal artery disease. Urol Clin North Am. 1984 Aug. 11(3):383-92. [View Abstract]
  56. Textor SC. Ischemic nephropathy: where are we now?. J Am Soc Nephrol. 2004 Aug. 15(8):1974-82. [View Abstract]
  57. Lao D, Parasher PS, Cho KC, Yeghiazarians Y. Atherosclerotic renal artery stenosis--diagnosis and treatment. Mayo Clin Proc. 2011 Jul. 86(7):649-57. [View Abstract]

Renal artery stenosis/renovascular hypertension. Flush aortogram in a 32-year-old man with familial hypercholesterolemia and difficult-to-control hypertension. Radiograph shows a complete occlusion of the right renal artery and marked stenosis of the left renal artery (arrow).

Renal artery stenosis/renovascular hypertension. Left, Sonograms of the kidneys on a 57-year-old woman with difficult-to-control hypertension shows kidneys of uneven sizes: The left kidney is 96 mm, and the right kidney is 63 mm. Top right, Isotopic renogram (obtained with technetium mercaptoacetyltriglycine [MAG3]) after captopril shows a markedly depressed renal function in the right kidney. Bottom right, Analogous images show negligible activity in the right kidney. Note that this pattern is more typical for DTPA than MAG3 (as DTPA depends on the glomerular filtration rate for uptake which is decreased after captopril in renovascular hypertension [RVHT]). In severe cases of RVHT, MAG3 uptake can be decreased, as in this case. However, typically, uptake is preserved with decreased cortical excretion.

Three-dimensional gadolinium-enhanced magnetic resonance angiograms (MRAs) show medial fibroplasia, which appears as classic string-of-beads sign. This sign is due to multiple stenoses with intervening outpouchings that form a chain. In this case, the lesions involve the main right renal artery and the right accessory renal artery in a 37-year-old man with difficult-to-control hypertension.

Renal artery stenosis/renovascular hypertension. Left, Flush aortogram in a 63-year-old man with hypertension shows marked stenosis of the right renal artery and complete occlusion of the left renal artery. Note the extensive atheroma in the aorta and iliac arteries. Right, nephrogram-phase image shows a significantly smaller left kidney with a faint nephrogram. Some blood supply to the left kidney is retained via collaterals (see image on the left).

Conventional flush aortogram in a 47-year-old woman with difficult-to-control hypertension shows the characteristic string-of-beads sign (arrows) of the right renal artery due to medial fibroplasia.

Renal artery stenosis/renovascular hypertension. Left, Sonograms of the kidneys on a 57-year-old woman with difficult-to-control hypertension shows kidneys of uneven sizes: The left kidney is 96 mm, and the right kidney is 63 mm. Top right, Isotopic renogram (obtained with technetium mercaptoacetyltriglycine [MAG3]) after captopril shows a markedly depressed renal function in the right kidney. Bottom right, Analogous images show negligible activity in the right kidney. Note that this pattern is more typical for DTPA than MAG3 (as DTPA depends on the glomerular filtration rate for uptake which is decreased after captopril in renovascular hypertension [RVHT]). In severe cases of RVHT, MAG3 uptake can be decreased, as in this case. However, typically, uptake is preserved with decreased cortical excretion.

Renal artery stenosis/renovascular hypertension. Left, Flush aortogram in a 63-year-old man with hypertension shows marked stenosis of the right renal artery and complete occlusion of the left renal artery. Note the extensive atheroma in the aorta and iliac arteries. Right, nephrogram-phase image shows a significantly smaller left kidney with a faint nephrogram. Some blood supply to the left kidney is retained via collaterals (see image on the left).

Renal artery stenosis/renovascular hypertension. Flush aortogram in a 32-year-old man with familial hypercholesterolemia and difficult-to-control hypertension. Radiograph shows a complete occlusion of the right renal artery and marked stenosis of the left renal artery (arrow).

Three-dimensional gadolinium-enhanced magnetic resonance angiograms (MRAs) show medial fibroplasia, which appears as classic string-of-beads sign. This sign is due to multiple stenoses with intervening outpouchings that form a chain. In this case, the lesions involve the main right renal artery and the right accessory renal artery in a 37-year-old man with difficult-to-control hypertension.

Conventional flush aortogram in a 47-year-old woman with difficult-to-control hypertension shows the characteristic string-of-beads sign (arrows) of the right renal artery due to medial fibroplasia.