Renal transplantation has been performed for the treatment of patients with chronic renal failure since 1954. Nevertheless, renal transplantation can give rise to urologic, vascular, and even clinical complications due to the use of immunosuppressive drugs.

Vascular complications are infrequent in kidney transplantations; however, they are one of the major causes of morbidity and mortality, occasionally resulting in renal graft dysfunction, graft removal, or death.1,2 Among the vascular complications are renal graft artery stenosis, arteriovenous fistula, and renal vein thrombosis. Renal graft artery stenosis is the most common and occurs in 1% to 15% of transplanted patients.3−5 According to the United States Renal Data System registry, 41,867 renal transplantations were performed in the period from 2000 to 2005, of which 823 developed renal graft artery stenosis, corresponding to a rate of 8.3 cases per 1,000 patient-years.6 According to data from the Brazilian Transplantation Registry, 19,101 procedures were performed in that same period, but no data are available regarding the incidence of renal graft artery stenosis.7 In the present institution, Lopes et al.8 reported a renal graft artery stenosis rate of approximately 1.6%.

Although no specific study has confirmed the association between vascular complications and graft position, the most often used technique is graft implantation in the common iliac or external artery, using termino-lateral anastomosis due to its speed and simplicity. The main causes of renal graft artery stenosis are inappropriate suture due to technical failure, intimal lesion during graft perfusion or when performing the implant, and excessive length of the renal artery causing torsion or tension at the suture site.1,4−9 Atherosclerosis and fibrosis at the anastomosis site are also causes of renal artery stenosis, and generally occur at a later stage after transplantation.9

In general, clinical findings that suggest renal graft artery stenosis are severe arterial hypertension refractory to drug treatment, and audible murmur at the site of the graft associated with unexplained progressive graft dysfunction. The presence of hypertension in renal transplantation recipients is a clinical finding in 50% to 60% of cases in the long-term.9,10 In the study by Mendes et al.,9 in all cases of haemodynamically significant renal graft artery stenosis (defined as stenosis>60%), there was progressive loss of graft function and difficult-to-control hypertension (with the use of three or more antihypertensive drugs).

Colour Doppler ultrasonography is an excellent diagnostic method for initial assessment of renal graft artery stenosis, with a sensitivity of 94% and a specificity of 87% when compared to conventional angiography.10 Computed tomography angiography (CTA) has a sensitivity and a specificity of 100% and 96%, respectively; its disadvantages are the use of ionising radiation and iodinated contrast.11 Magnetic resonance angiography (MRA) using gadolinium has been shown to be a good method for the detection of renal artery stenosis. Korst et al.12 found a sensitivity and a specificity of 100% and 85%, respectively. It is an excellent technique for patients with impaired renal function and allergy to iodinated contrast medium, in whom digital angiography cannot be performed.13

In general, all patients submitted to renal transplantation at this institution who have high clinical suspicion of graft stenosis undergo Doppler ultrasound assessment, and when the results are altered (peak systolic velocity>180cm/s), a renal angiography is indicated. Angiography, an examination considered to be the gold standard for the definitive diagnosis of renal artery stenosis, is used to confirm the injury indicated by Doppler ultrasonography and/or CTA, and guides the therapeutic approach. However, angiography is based on findings of visual estimation or by quantitative renal angiography (QRA), thereby determining the severity of a stenosis while quantifying t. Stenoses are considered severe when there is>60% of vessel lumen obstruction.7,11

Once the diagnosis is attained, treatment options include percutaneous treatment using a conventional percutaneous intervention with a balloon or, preferably, stenting (percutaneous renal intervention [PRI]) and revascularisation surgery. The PRI results in resolution or improvement in 76% of cases, with the discontinuation of at least two antihypertensive medications, and in some patients already on dialysis, it is possible to achieve graft function recovery.7 Success rates are high, and restenosis with stenting is below 10%, mainly due to the high luminal diameter of the vessel and the immunosuppressive therapy used after transplantation.7,9

In contrast, some patients submitted to renal graft angiography have moderate stenosis (> 30% and<60%), in addition to cases in which the visual estimation/ QRA cannot define the actual severity of the stenosis. This usually occurs in stenosis with ostial location or even as a result of the limitations of luminography. In this scenario, the idea of using a method that would help in the functional stratification of renal graft artery stenosis has been proposed. Developed and validated for the functional stratification of coronary stenosis, the fractional flow reserve for native renal artery stenosis has been studied by Leesar et al.14 and Kapoor et al.15 These studies evaluated the severity of stenosis based on the maximum and mean translesional systolic pressure gradients, and based on the association between maximum systolic pressure in the aorta and pressure distal to the stenosis (Pd/Pa), measured by the pressure wire during maximum hyperaemia induced by 30mg papaverine infused as an intrarenal bolus. To predict the severity of native renal artery stenosis, accuracy, sensitivity and specificity of 84%, 82%, and 84% were determined, respectively, for maximum systolic gradient>21mmHg, and 79%, 82%, and 88%, respectively, for a Pd/Pa ratio<0.9.

Regarding renal graft artery stenosis, there have been no studies that used fractional flow reserve for the functional analysis of these stenoses. Thus, the usefulness of this method in the functional evaluation of these patients and the possibility of predicting the therapeutic effectiveness of the PRI has not yet been explored.

METHODSFractional flow reserve: definitions and principles

Renal fractional flow reserve is defined as the ratio between the maximum blood flow to the renal parenchyma in the presence of a determined stenosis (or stenoses) and this same flow if there were no stenoses. This ratio represents the fraction of normal maximum renal flow that can be achieved in the presence of stenosis. The fractional flow reserve can be readily determined by dividing the mean pressure distal to the renal lesion by the mean pressure in the aorta during maximal vasodilation induced by administering an intra-arterial bolus dose of 30mg papaverine in the renal graft. A fractional flow reserve of 0.6 indicates that the maximum amount of blood (and oxygen) that irrigates that particular area of renal tissue is only 60% of what it would be if the culprit artery was completely normal. If, after a PRI, the fractional flow reserve in that case increases to 0.90, it means the maximum achievable flow into the parenchymal area supplied by that artery (and hence, the oxygen supply) increased by 50% and is now 90% of the attainable value if the artery was completely normal.Figures 1 and 2 show, schematically, how to determine the fractional flow reserve and how the flow measurement can be inferred by dividing pressures.

Figure 1.

Definition of renal fractional flow reserve. If there is no stenosis (gray lines), the perfusion pressure determines the maximum normal flow rate (100%) of the renal parenchyma (Pa=Pd). In case of stenosis (black lines), responsible for a gradient of 30mmHg during maximum hyperaemia, the distal perfusion pressure will decrease to 70mmHg. As the ratio between renal flow and pressure is linear during hyperaemia (chart), renal flow will reach only 70% of its normal value. Pa, perfusion pressure, Pd, distal pressure.

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Figure 2.

Renal fractional flow reserve is calculated by dividing the distal pressure in the renal artery by the pressure in the aorta during maximum hyperaemia. FFR, fractional flow reserve, QStenosis, flow in renal graft artery with stenosis; QNormal, flow in the renal graft artery in the absence of stenosis; Pd, distal pressure; PV, venous pressure; PA, pressure in the aorta; RMIO, renal resistance.

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Protocol descriptionStudy goals

• 1.

  To describe and standardise the study protocol of fractional flow reserve in patients with severe stenosis of the renal graft artery who are selected for PRI, observing whether the cutoff used for native renal artery stenosis (maximum systolic gradient>21mm or Pd/Pa<0.9) is reproducible for renal graft artery stenosis.

• 2.

  To compare the results obtained through direct measurements of pressure gradients (pre- and poststenosis) at rest and after hyperaemic stimulation performed with a conventional 4F catheter, as well as the pressure measured by the pressure wire.

• 3.

  To evaluate the association between fractional flow reserve values before and after the procedure and procedural success through ultra-sensitive markers of renal function.

Study population

A total of ten 15 to 65 year-old patients will be initially assessed, after an informed consent is signed. The patients will have been referred to the Interventional Cardiology Service of the Hospital São Paulo (Escola Paulista de Medicina, Universidade Federal de São Paulo (UNIFESP/EPM), São Paulo, SP, Brazil), with a clinical picture of renal graft artery stenosis, associated with Doppler ultrasound and/or CTA suggestive of renal graft artery stenosis to undergo renal angiography and, when the presence of this stenosis is confirmed, will have an indication for PRI (renal graft artery stenosis≥60% at visual estimation). The project was approved by the research ethics committee, protocol No. 51,518 – Plataforma Brasil – Brazilian Ministry of Health.Figure 3 summarises the study design. Patients will be admitted 12 hours before the procedure, and intravenous hydration will be carried out with 0.9% saline solution at 1mL/kg/hour, 12 hours before and after the test. Low-osmolarity contrast will be used to minimise the risk of contrast-induced nephropathy. Dual antiplatelet therapy will be administered (with 300mg acetylsalicylic acid and 300mg clopidogrel, 12 hours prior to the procedure). A dose of 100mg acetylsalicylic acid will be maintained indefinitely, as well as 75mg clopidogrel for 30 days.

Figure 3.

Overview of the study protocol. RGAS, renal graft artery stenosis; Echo, echocardiography; CTA, computed tomography angiography; FFR, fractional flow reserve; PRI, percutaneous renal intervention; Ur, urea; Cr, creatinine; NGAL, neutrophil gelatinase-associated lipocalin; IL-18, interleukin-18; KIM-1, kidney injury molecule-1.

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The angiograms of all patients selected for the study will be analysed by an experienced interventional physician. Then, artery lesions considered to be severe (visual estimates showing stenosis≥60%), and thus with an indication for PRI, will be submitted to the protocol for the analysis of the mean systolic translesional pressure gradients and fractional flow reserve pre- and post-treatment under hyperaemia with papaverine.

Materials

6F or 7F therapeutic guide-catheters without lateral holes will be used for selective catheterisation of the artery to be approached. The measurement of the translesional pressure gradient will be mandatorily performed with 4F guide catheters, as larger-calibre catheters interfere with the assessment of stenosis during their retreat to perform the gradient measurement. The guidewire to be used for measurement of fractional flow reserve uses a specific sensor located 3cm from its tip, has a diameter of 0.014 inch (0.36mm), and has a soft tip, similar in calibre to the guide wires routinely used in PRI procedures. PressureWire Certus Hydrophilic ® guidewires (Radi Medical Systems AB Inc., Uppsala, Sweden) will also be used. The guide wire is connected to a monitor, which, by converting the pressure signal to an electrical signal, presents the results directly on the screen, allowing the data to be viewed and saved in a few seconds.

The angiograms will be performed with Philips Allure FD10 equipment (flat panel), which has software with appropriate settings for acquisition and processing of images in rotational angiography of the abdomen.

Hyperaemia

It is essential to induce maximal vasodilation in the two compartments of renal circulation, in the vessel itself and in the microcirculation, to calculate the renal fractional flow reserve. Administration of 30mg papaverine by an intra-arterial route in bolus is the available option. The drug’s action lasts up to 50 seconds; it has no side effects and can be used in catheter withdrawal manoeuvres. The systolic and mean translesional gradients are calculated simultaneously during the analysis of the renal fractional flow reserve.

Systematisation for the initial angiographies, angiographic definition of lesion severity, measurement of renal fractional flow reserve, and PRI with a stent and new measurement of fractional flow reserve.

A total of ten patients who have a clinical picture of renal artery graft stenosis and angiography showing graft stenosis≥60% and are admitted to undergo PRI will be selected. For the evaluation of graft dysfunction, serum measurements of urea and creatinine will be performed 12 hours before and 12 and 72 hours after the procedure. Measurement of urinary neutrophil gelatinase-associated lipocalin (NGAL), interleukin-18 (IL-18), kidney injury molecule-1 (KIM-1), and serum cystatin C will be performed at the beginning and 6 hours, 12 hours, 24 hours, and 48 hours after the procedure.

The following steps will be performed during the procedure:

• 1.

  Local anaesthesia of the arterial puncture site with 2% lidocaine (10 – 15mL).

• 2.

  Insertion of a 6F or 7F arterial sheath.

• 3.

  Introduction of a 4F Judkins right (JR) catheter after the stenosis and maximum hyperaemia induced with 30mg papaverine in bolus followed by evaluation of translesional gradients.

• 4.

  Selective catheterisation of the renal graft artery with an RDC guide catheter or a JR 4 of PRI, 6F, or 7F without lateral holes.

• 5.

  Administration of 100 UI/kg IV heparin.

• 6.

  Calibration of guide-catheter and pressure wire.

• 7.

  Connection of the pressure wire to the analyser, equating the pressures of the guide-catheter and wire pressure when the sensor of the latter is close to the tip of the guide-catheter.

• 8.

  Placement of the pressure wire in the distal bed of the renal graft artery to be analysed.

• 9.

  Evaluation of graft stenosis by measuring the fractional flow reserve during maximum hyperaemia induced by an intra-arterial injection of 30mg papaverine in bolus in the renal graft.

• 10.

  Performing PRI with stent implantation.

• 11.

  New gradient assessment through maximum hyperaemia with papaverine using the pressure wire and a 4F catheter.