The Choice of the Iodinated Radiographic Contrast Media to Prevent Contrast-Induced Nephropathy

Andreucci, Michele; Faga, Teresa; Pisani, Antonio; Sabbatini, Massimo; Russo, Domenico; Michael, Ashour

doi:https://doi.org/10.1155/2014/691623

Advances in Nephrology

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Review Article | Open Access

Volume 2014 | Article ID 691623 | https://doi.org/10.1155/2014/691623

The Choice of the Iodinated Radiographic Contrast Media to Prevent Contrast-Induced Nephropathy

Michele Andreucci,¹Teresa Faga,¹Antonio Pisani,²Massimo Sabbatini,²Domenico Russo,²and Ashour Michael¹

Academic Editor: Jane Black

Received11 Jun 2014

Revised31 Aug 2014

Accepted08 Sept 2014

Published15 Oct 2014

Abstract

In patients with preexisting renal impairment, particularly those who are diabetic, the iodinated radiographic contrast media may cause contrast-induced nephropathy (CIN) or contrast-induced acute kidney injury (CI-AKI), that is, an acute renal failure (ARF), usually nonoliguric and asymptomatic, occurring 24 to 72 hours after their intravascular injection in the absence of an alternative aetiology. Radiographic contrast media have different osmolalities and viscosities. They have also a different nephrotoxicity. In order to prevent CIN, the least nephrotoxic contrast media should be chosen, at the lowest dosage possible. Other prevention measures should include discontinuation of potentially nephrotoxic drugs, adequate hydration with i.v. infusion of either normal saline or bicarbonate solution, and eventually use of antioxidants, such as N-acetylcysteine, and statins.

1. Introduction

Iodinated radiographic contrast media [1] are widely used in clinical practice, for both diagnostic and therapeutic procedures such as radiography, percutaneous cardiac and arterial interventions, and contrast-enhanced computed tomography (CT). The intravascular injection of CM is usually safe in healthy subjects with normal renal function. But in patients with preexisting renal impairment the CM may express their nephrotoxicity. Since the clinical need for diagnostic and therapeutic procedures using CM is increased in particular in patients with cardiovascular diseases whose renal function is frequently impaired [2], the occurrence of renal damage by CM is quite frequent.

Contrast-induced nephropathy (CIN) is defined as an acute renal failure (ARF) occurring 24 to 72 hours after the intravascular injection of radiographic contrast media in the absence of an alternative aetiology [3]. The KDIGO Group [4] “proposes that the term contrast-induced acute kidney injury (CI-AKI) be used for patients developing AKI secondary to intravascular radiocontrast media exposure” rather than CIN. But CIN is still widely used in the literature. It is also questioned whether to use the term ARF to indicate renal impairment by CM. The KDIGO Group also underlines that “the term “acute kidney injury/impairment” has been proposed to encompass the entire spectrum of the syndrome from minor changes in markers of renal function to requirement for renal replacement therapy (RRT)” [4]. However, most authors keep defining AKI as an “ARF,” sometimes “renal insufficiency,” even without the need for dialysis. It is usually a nonoliguric, asymptomatic, and transient decline in renal function. The renal function is evaluated by measuring serum creatinine (SCr) which is more accurately calculated by using the estimated glomerular filtration rate (eGFR), that is, the creatinine clearance (CrCl) calculated either by the MDRD (modification of diet in renal disease) formula [5] or by the Cockcroft-Gault formula: (140 − number of years of age) × kg body weight/72/SCr (mg/dL); in females the result is multiplied by 0.85 [6]. In addition to giving a better value of renal function, this avoids the tedious procedure of urine collection necessary to measure CrCl. The CIN is an increase of SCr by 0.5 mg/dL (or more) or by a 25% (or more) increase in SCr from baseline or a ≥25% decrease in eGFR [4]. The peak value of SCr and the lowest value of eGFR are observed on the third to fifth day; eGFR returns to baseline within 10–14 days. In some cases, CIN is a severe ARF with oliguria (<400 mL/24 hrs), requiring dialysis. In these patients the mortality is high [7].

The clinical features and the management of CIN are the same as those for ARF due to other causes [8–10].

2. Pathogenesis of CIN

The pathophysiological mechanisms responsible for CIN have not been fully elucidated [11].

After the intravascular injection, iodinated radiographic CM cause hemodynamic changes: immediate renal vasodilatation with an initial increase in renal blood flow (RBF) followed by prolonged vasoconstriction with an increase in intrarenal vascular resistance and a reduction in total RBF [12].

The extrarenal vessels show transient vasoconstriction followed by a stable decrease in vascular peripheral resistance [13, 14] (Figure 1).

The fall in total RBF will cause a decrease in the glomerular filtration rate (GFR). But the renal vasoconstriction causes particularly severe consequences in the renal medulla because of the normally poor oxygen delivery to the outer renal medulla (due to its distance from the descending vasa recta) associated with the high local O₂ consumption due to the important tubular reabsorption in S3 segments of proximal renal tubules of the outer medulla and in the medullary thick ascending limbs of Henle’s loop. Thus, the haemodynamic changes induced by CM will make medullary hypoxia quite severe (Figure 1).

After CM administration in patients with chronic renal failure, Russo et al. [15] have shown (1) an immediate GFR decline proportional to the osmolality of CM and secondary to the renal hypoperfusion that is not caused by hypovolemia and (2) an early tubular dysfunction at the level of the proximal nephron.

Furthermore, radiographic CM induce an osmotic diuresis and consequently an increase in tubular reabsorption in Henle’s loop; the resulting increase of energy need and the high O₂ consumption of the ascending limb will make the medullary hypoxia worse [8, 16] (Figure 1). The osmotic diuresis will increase the intratubular pressure and tubular obstruction thereby contributing to the fall in GFR.

Medullary hypoxia leads to the formation of reactive oxygen species (ROS) [17, 18] that may exert direct tubular and vascular endothelial injury and might further intensify renal parenchymal hypoxia by virtue of endothelial dysfunction and dysregulation of tubular transport [19, 20] (Figure 1).

The decrease in nitric oxide (NO) is believed to be due to its reaction with ROS, in particular with superoxide anions () [21, 22]. This reaction may lead to the formation of the more powerful oxidant peroxynitrite anion (ONOO⁻) [23] that may be more detrimental to the endothelial cells. Hence the reaction of the ROS with NO not only causes a reduction in the levels of the vasodilator NO, but also leads to the formation of a potent oxidant that exacerbates cell injury.

Pisani et al. [24] have recently demonstrated that a recombinant manganese superoxide dismutase administered in vivo to rats undergoing diatrizoate treatment was able to reduce renal oxidative stress, thereby preventing the reduction of GFR and the renal histologic damage that follows contrast media administration.

Iodinated radiographic contrast media also exert a direct cytotoxic effect on both endothelial and tubular cells that has been suggested to be due, at least in part, to the free iodine present in solutions of CM [21] and leads to apoptosis and cell death. The decrease in NO in the vasa recta is due not only to increased ROS production, but also to its reduced release by damaged endothelial cells (including those undergoing apoptosis) [21, 25, 26].

3. The Differences between Iodinated Radiographic CM

Radiographic CM have different osmolalities (see Table 1). The ionic high-osmolar contrast media (HOCM, e.g., diatrizoate) have an osmolality of 1500 to 1800 mOsm/kg, that is, 5–8 times the osmolality of plasma. Nonionic low-osmolar contrast media (LOCM, e.g., iohexol) have an osmolality of 600 to 850 mOsm/kg, that is, 2-3 times the osmolality of plasma. Nonionic isoosmolar contrast media (IOCM, e.g., iodixanol) have an osmolality of approximately 290 mOsm/kg, that is, the same osmolality as plasma [16, 27]. The LOCM are less nephrotoxic than HOCM. The frequency of adverse reactions to CM ranges from 5% to 12% for HOCM and from 1% to 3% for LOCM. It has been observed that the use of LOCM rather than HOCM is beneficial in the prevention of CIN in patients with preexisting chronic renal failure [28–31]. Thus, the HOCM are rarely used. The IOCM iodixanol seems less nephrotoxic than the LOCM iohexol, at least in patients with intra-arterial administration of the drug and renal insufficiency [32, 33].

4. Factors Increasing Nephrotoxicity of CM

As already mentioned, preexisting impairment of renal function, irrespective of cause, greatly favors the occurrence of CIN. The higher the baseline creatinine value or, better, the lower the eGFR, the greater the risk of CIN [8].

Diabetes mellitus is another predisposing factor for the development of CIN, particularly when associated with renal insufficiency [34]. At any given degree of baseline GFR, diabetes doubles the risk of developing CIN compared with non-diabetic patients. The incidence of CIN in diabetic patients varies from 5.7 to 29.4% [35]. Coupling chronic kidney disease and diabetes dramatically increases the risk for CIN compared with that observed for chronic kidney disease alone [36].

The concomitant use of nephrotoxic drugs, such as aminoglycosides, cyclosporin A, amphotericin, cisplatin, and nonsteroidal anti-inflammatory drugs, is undoubtedly another factor favoring the onset of CIN [8].

Most authors believe that patients with chronic renal disease under treatment with angiotensin-converting enzyme inhibitors (ACEIs) or angiotensin II receptor blockers (ARBs) are at higher risk for developing CIN [37–42] particularly in the elderly [43]. According to KDIGO (kidney disease improving global outcome) guidelines for Acute Kidney Injury Work Group, there is insufficient evidence to recommend discontinuation of these medications prior to contrast administration [4].

Dehydration and/or volume contraction and reduction of “effective” circulating blood volume are major individual risk factors for CIN [8].

Use of large doses of contrast media and their multiple injections within 72 hrs increases the risk of CIN [44–49].

Advance age (>65 years), anemia, congestive heart failure, sepsis, and renal transplant all predispose to CIN [8].

5. The Effect of the Route of Administration on Nephrotoxicity of CM

CIN occurs more frequently after intra-arterial than after i.v. contrast medium administration [32, 50], probably because of the higher acute intrarenal concentration, particularly if the arterial injection is suprarenal [51–57]. The closer to the renal arteries the injection of contrast medium occurs, the higher the risk of CIN appears to be [57].

The meta-analysis by Dong et al. [32] obtained from 18 randomized controlled trials including 3,129 patients showed that the IOCM iodixanol significantly decreased the risk of CIN as compared with a pool of LOCM (iopromide, iopamidol, iohexol, ioversol, ioxaglate, and iomeprol) when contrast media were given intra-arterially (11 trials). In contrast, it was not associated with a reduction in CIN compared with the LOCM (iopromide, iopamidol, iomeprol, and iohexol) pooled together following i.v. application (7 trials). Probably the different nephrotoxicity between the intra-arterial and the i.v. administration of contrast media is accounted for by the different reactions to oxidative stress between arteries and veins [32].

6. Viscosity of CM

Contrast media share common iodine-related cytotoxic features but differ considerably with regard to osmolality and viscosity (Table 1). According to some authors [58–60], in fact, in addition to their osmolality the viscosity of CM is also very important.

Fluid viscosity is a measure of the fluid’s resistance to flow due to friction between neighboring parcels that are moved at different velocities. Radiographic CM are tri-iodinated benzene derivatives. Their radioopacity relies on iodine. Thus, solutions with high iodine concentration (usually with 250–400 mg I/mL) are required. This is obtained by high molar concentrations of benzene derivatives that are responsible for the osmolality and viscosity of the solution. The osmolality of the CM solution increases linearly with the molar concentration, while the viscosity increases exponentially [58].

The low osmolality achieved with the IOCM occurred at the price of considerably increased viscosity at comparable iodine concentration and X-ray attenuation; nonionic dimeric IOCM have about twice the viscosity of nonionic monomeric LOCM [60–62].

The CM are freely filtered by the glomeruli so that their concentration in primary urine equals that of the blood plasma entering the kidney. They are not reabsorbed by tubules. Most of the water and salt filtered by the glomeruli, however, is reabsorbed along the renal tubules, particularly the proximal tubules. Thus, the concentration of CM increases considerably within the tubular lumen. According to Seeliger et al. [58–60] the high viscosity of CM may contribute to their nephrotoxicity. The increase of CM concentration will cause a progressive increase in tubular fluid osmolality and, due to the exponential concentration-viscosity relationship, an overproportional increase in tubular fluid viscosity [16, 58]. Since the fluid flow rate through a tube increases with the pressure gradient and decreases with the flow resistance and since the resistance increases proportionally to fluid viscosity, the increased viscosity caused by the contrast medium concentrated within the tubule increases the intratubular pressure [58]. This hypothesis has been validated by the studies of Ueda et al. [63, 64] who measured the intratubular pressure in proximal and distal convoluted renal tubules by micropuncture techniques. These authors, in fact, with micropuncture studies in rats found that the IOCM, iotrolan, increased tubular pressure much more and decreased single nephron GFR much more as compared with the HOCM and LOCM studied. Thus, the high intratubular pressure will have four consequences: (a) it hinders the glomerular filtration, thereby reducing tubular flow rate; (b) the reduction of tubular flow prolongs the contact time of cytotoxic CM with the tubular epithelium, consequently making the injury to the epithelial tubular cells more severe; (c) the high intratubular pressure contributes to medullary hypoperfusion and hypoxia: in presence of a tough renal capsule, in fact, the circular distension of the tubules will lead to compression of medullary vasa recta; (d) the reduced blood flow rate in the latter will increase the contact time of cytotoxic CM with the vascular endothelium contributing to its damage [16, 58]. In conclusion, the CM viscosity would contribute to the overall nephrotoxicity of CM.

7. Cytotoxic Effects of CM In Vitro

Heinrich et al. [65] compared the cytotoxic effects of dimeric and monomeric iodinated CM on renal tubular cells in vitro. Cell viability was assessed by using the 3-(4,5-dimethyl-2-thiazolyl)-2,5-diphenyl-2H-tetrazolium bromide (MTT) uptake assay. The conversion of MTT, a tetrazolium salt, into formazan depends on the activity of a group of mitochondrial dehydrogenases and, thus, is an indicator of cell metabolic activity [65]. Results of this study indicated that HOCM have a greater potential for cytotoxic effects on proximal renal tubular cells in vitro than LOCM or IOCM do. At equal iodine concentrations (300 mg I/mL), the HOCM ioxithalamate showed stronger cytotoxic effects than other contrast media did: MTT conversion for the HOCM ioxithalamate was 4% versus that for the LOCM ioversol of 32%, that for the LOCM iomeprol-300 of 34%, that for the IOCM iodixanol of 40%, and that for the IOCM iotrolan of 41% of undamaged control cells at 75 mg of iodine per milliliter (); there was no significant difference between monomeric LOCM and dimeric IOCM (). Thus, there is no difference in the cytotoxicity of LOCM iomeprol and IOCM iodixanol at equal iodine concentrations in renal proximal tubular cells in vitro [33].

Michael et al. [66] and Andreucci et al. [67–70] have investigated the signaling pathways in renal tubular cell lines (including primary human renal tubular cells) that may be affected by exposure of renal tubular cells to CM. The incubation of human renal tubular proximal cells with the HOCM sodium diatrizoate, the LOCM iopromide, and the LOCM iomeprol caused a marked dephosphorylation of the kinase Akt on Ser473 within 5 min of incubation. This observation is remarkable given the suggestion that CM give rise to ROS [66] and treatment of renal cells with powerful oxidants or subjecting renal cells to conditions that favour ROS formation cause an increase in Akt phosphorylation in renal tubular cells [71–73]. All of these CM also caused a decrease in cell viability [68–70], which was substantially alleviated by transfecting the cells with a constitutively active form of Akt [68]. Further downstream targets of Akt, including the Forkhead family of transcription factors FKHR and FKHRL1, were also dephosphorylated by the three CM at Thr24 and Thr32, respectively. The p70S6 kinase was also dephosphorylated at Thr389 and Ser371 by these CM [68].

The HOCM sodium diatrizoate and the LOCM iomeprol at a concentration of 75 mg I/mL for 2 h have been shown, by the same authors, to cause an increase in phosphorylation of p38 mitogen-activated protein kinase (MAPK) (p38) and c-Jun N-terminal kinases (JNKs) and NF-κB (at Ser276), with sodium diatrizoate having a more drastic effect. Although cell viability was reduced significantly by both CM, in cells pretreated with the LOCM iomeprol the cell viability recovered over a 22 h time period after removal of the CM. However, viability of diatrizoate-treated cells rose at 5 h but then fell at 22 h after removal of the RCM. The decrease in cell viability in diatrizoate-treated cells corresponded with an increase in phosphorylation of JNKs, p38, and NF-κB and a decrease in phosphorylation of Akt, signal transducer and activator of transcription (STAT)3, and forkhead box O3a, as well as poly (ADP-ribose) polymerase (PARP) and caspase-3 cleavage. The recovery in viability of the LOCM iomeprol-treated cells corresponded most notably with an increase in STAT3 phosphorylation and induction of Pim-1 kinase. There was also an increase in interleukin-8 release by diatrizoate-treated cells indicating the possibility of proinflammatory effects of this CM [69].

The same group has recently compared the changes of intracellular signaling pathways affected by the LOCM iomeprol and the IOCM iodixanol. Both CM caused a dramatic decrease in phosphorylation of the kinase Akt at Ser473 and Thr308 in human proximal renal tubular cells, with iomeprol having a greater effect and causing a greater decrease in cell viability. Iodixanol caused a greater decrease in the phosphorylation of the extracellular-signal regulated kinases (ERKs) 1 and 2 and mammalian target of rapamycin (mTOR), but both CM caused a similar decrease in the phosphorylation of phospho-p70S6 kinase (at Ser371) [70].

8. Protection by Adequate Hydration

Under normal physiological circumstances the entity of tubular reabsorption of water and salt depends on the subject’s hydration and volume status. In subjects who are dehydrated and/or hypovolaemic, physiological mechanisms for water and/or volume preservation are activated, that is, the renin-angiotensin system and vasopressin. This leads to increase of tubular reabsorption of water and salt from the tubular fluid, thereby making the urine more concentrated. This tubular fluid overreabsorption during volume depletion (hypovolemia) does occur already in the proximal tubules. Thus, when CM are injected in dehydrated/hypovolaemic patients, the water and salt overreabsorption will further increase the tubular concentration of CM and, due to the concentration-viscosity relationship, overproportionally increase the tubular fluid and urine viscosity. This is why dehydration (for instance in the elderly due to impaired sensation of thirst [74]) and/or volume contraction (salt depletion following abnormal gastrointestinal, renal or dermal fluid losses associated with insufficient salt intake and reduction of “effective” circulating blood volume [75]) are major individual risk factors for CIN. Thus, it is a very crucial point to recommend prehydration and correction of volume depletion in all patients before undergoing the diagnostic and therapeutic procedures requiring intravascular injection of CM [7, 58]. The “effective” circulating blood volume may be defined as the relative fullness of the arterial tree as determined by cardiac output, peripheral vascular resistance, and total blood volume [9]. A reduction of “effective” circulating blood volume may be due to congestive heart failure, compromised left ventricle systolic performance, prolonged hypotension, or liver cirrhosis or nephrotic syndrome [16].

9. The Different Nephrotoxicity of Different CM

McCullough et al. [76] had performed a meta-analysis of the renal safety of IOCM iodixanol compared with LOCM, including 16 double-blind, randomized, controlled trials with data from 2,727 patients. They found that the use of the IOCM iodixanol was associated with smaller rises in SCr and lower rates of CIN than LOCM, especially in patients with chronic kidney disease and/or diabetes mellitus.

Most of the recent studies and meta-analyses, however, have found no significant difference in the rates of CIN between IOCM and LOCM [8, 32, 33, 50, 77–79].

Thus, the meta-analysis of Heinrich et al. [33] that included 25 randomized controlled trials with data from 2,850 patients compared the nephrotoxicity of IOCM iodixanol (1701 patients) with that of LOCM (iohexol, iopamidol, iopromide, iomeprol, ioversol, and iobitridol) (1569 patients). They found that iodixanol did not significantly reduce the risk of CIN after i.v. administration of the CM (8 trials) as compared with LOCM pooled together. However, in patients with intra-arterial administration (17 trials) and renal insufficiency, they found that the risk of CIN was greater for the LOCM iohexol (494 patients) than for IOCM iodixanol, whereas no significant difference between iodixanol and other LOCM could be found.

Reed et al. [78] conducted another meta-analysis (16 trials including 2,763 subjects) also comparing the nephrotoxicity of the IOCM iodixanol to LOCM. They found no significant difference in the incidence of CIN between the iodixanol group and the LOCM group. They admitted that the relative renal safety of LOCM compared with iodixanol may vary depending on the particular type of LOCM.

The study PREDICT (patients with renal impairment and diabetes undergoing CT) compared the incidence of CIN after administration of either LOCM iopamidol 370 (n. 125) or IOCM iodixanol 320 (n. 123) in patients with diabetes and chronic renal insufficiency (eGFR = 20–59 mL/min/1.73 m²) undergoing CT. CIN (increase in the serum creatinine of ≥25% from the baseline level) occurred in 7 patients (5.6%) receiving iopamidol 370 and in 6 patients (4.9%) receiving iodixanol 320 (). The authors concluded that there is no difference in the incidence of CIN between iopamidol and iodixanol in patients with diabetes and chronic renal insufficiency [50].

Barrett et al. [80] compared the effects on renal function of equi-iodine i.v. doses (40 gI) of either LOCM iopamidol 370 (n. 77) or IOCM iodixanol 320 (n. 76) in 153 patients with chronic kidney disease (SCr, ≥1.5 mg/dL, and/or CrCl, ≥60 mL/min) undergoing contrast-enhanced multidetector CT using a multicenter, double-blind, randomized, parallel-group design. An increase of ≥0.5 mg/dL in SCr was observed in none of the patients receiving iopamidol-370 and in two of the patients receiving iodixanol-320 (). An increase of ≥25% in SCr occurred in three of the patients receiving iopamidol-370 and in three of the patients receiving iodixanol-320 (). The authors concluded that the incidence of CIN was similarly low in risk patients after i.v. administration of iopamidol-370 (LOCM) or iodixanol-320 (IOCM).

Solomon et al. [77] have performed the CARE (Cardiac Angiography in Renally Impaired Patients) trial, a randomized double-blind trial of CIN in patients with chronic kidney disease, enrolling 414 patients with an eGFR of 20 to 59 mL/min/1.73 m² who underwent cardiac catheterization by using either LOCM iopamidol or IOCM iodixanol. SCr increase ≥0.5 mg/dL occurred in 4.4% (9 of 204 patients) after iopamidol and 6.7% (14 of 210 patients) after iodixanol (), whereas SCr increase ≥25% was 9.8% and 12.4%, respectively (). Thus, the incidence of CIN was not different between the two study groups. In patients with diabetes (), there was also no statistically significant difference in the incidence of CIN between iopamidol and iodixanol (10.3% versus 15.2%, resp.; ). The authors concluded that the incidence of CIN is not statistically different after the intra-arterial administration of iopamidol or iodixanol to high-risk patients, with or without diabetes mellitus.

10. The Choice of the CM

As described above, no significant difference in nephrotoxicity has been found between the IOCM iodixanol and all the LOCM, probably with the only exception being iohexol [81, 82]. Once it has been decided which CM is to be used, it is very important to take into consideration the dosage of the CM, to limit its nephrotoxicity. The lowest dosage possible of the radiographic contrast agent should be used [16].

High doses of contrast agents are required in percutaneous coronary interventions (PCI). Some formulas have been suggested to calculate the dosage that is least dangerous for renal function [8].(1)Cigarroa’s formula is 5 mL of contrast per kg b.w./SCr (mg/dL) with maximum acceptable dose of 300 mL for diagnostic coronary arteriography [83].(2)Laskey’s formula is volume of contrast to eGFR ratio with a cutoff point of the ratio at 3.7 for PCI. It has been demonstrated that a ratio >3.7 is associated with a decrease in CrCl [84]. More recently Gurm et al. [85] have suggested a cutoff point at 2.0: below a ratio of 2.0 CIN would be a rare complication of PCI, but it would increase dramatically at a ratio of 3.0.(3)A new formula seems to be superior and takes into consideration the ratio of grams of iodine to the eGFR; it has been suggested that a ratio of 1.42, or even better a ratio of 1.0, would prevent CIN [86].

Obviously, all other prevention measures should be made in order to prevent the onset of CIN as follows [8, 87]. (A) Monitoring of the eGFR before and once daily for 5 days after the radiographic procedure and consider that patients with coronary artery disease may have initial and silent renal dysfunction [2]. (B) Discontinuation of potentially nephrotoxic drugs (aminoglycosides, vancomycin, amphotericin B, metformin, and nonsteroidal anti-inflammatory drugs). (C) Adequate hydration, in the opinion of some authors, by giving 500 mL of water or soft drinks orally before and 2,500 mL for 24 hours after contrast administration in order to secure urine output of at least 1 mL/min in a nondehydrated patient [88]). It is undoubtedly better to give i.v. infusion of saline or a bicarbonate solution since the water alone will dilute the tubular fluid only in the collecting ducts, thereby giving no protection at all. Thus, Trivedi et al. [89] randomized 53 patients on the day before scheduled elective cardiac catheterization to group 1 (n. 27) that received normal saline for 24 h (at a rate of 1 mL/kg per h) beginning 12 h before scheduled catheterization and group 2 (n. 26) that was allowed unrestricted oral fluids; an increase in SCr by at least 0.5 mg/dL within 48 h of contrast exposure was considered to represent clinically significant ARF; the incidence of CIN was significantly lower in group 1 (one out of 27) as compared to group 2 (nine out of 26; ) demonstrating that oral supplement of water has no protective effect as normal saline does. Thus, an i.v. infusion of 0.9% saline at a rate of 1 mL/kg b.w. per hour, beginning 6–12 hours before the procedure and continuing for up to 12–24 hours after, is suggested, if urine output is appropriate and cardiovascular condition allows it [48, 90]. Some authors suggest using sodium bicarbonate hydration that has been shown to be superior to sodium chloride in many clinical studies and meta-analysis [91–101]. For coronary angiography or intervention 154 mEq/L infusion of sodium bicarbonate as a bolus of 3 mL/kg b.w./hour for 1 hour before the administration of IRCA, followed by 1 mL/kg/hour for 6 hours during and after the procedure, has been used [102]. The alkalinization of tubular fluid by bicarbonate would reduce the production and increase the neutralization of oxygen-free radicals, thereby protecting the kidney from injury by CM. The adequate hydration is undoubtedly the most important preventive measure against CI-AKI. (D) Use of antioxidants, such as N-acetylcysteine in high-risk patients (oral dose of 600 mg twice daily the day before and the day of procedure [48] or an i.v. dose of 150 mg/kg over half an hour before the procedure or 50 mg/kg administered over 4 hours [103]). (E) Use of statins, which have been demonstrated to be protective also under other circumstances of kidney injury [104–109], for example, short-term pretreatment with atorvastatin: 80 mg 12 hours before intervention with another 40 mg preprocedure, followed by long-term treatment of 40 mg/day [110]. More recently, only in patients with low or medium risk, Quintavalle et al. have shown that a single high loading dose of atorvastatin (80 mg) administered within 24 hours before the CM exposure is effective for the reduction of the rate of CIN [111]. (F) Use of furosemide to reduce salt reabsorption in the thick ascending limb of Henle’s loops, thereby reducing oxygen consumption and medullary hypoxia; but several studies have demonstrated no protection against CIN of this diuretic or even deleterious effects mainly related to the salt depletion caused by furosemide [112–114]. To overcome the problem of hypovolemia caused by furosemide, a perfect combination of hydration plus furosemide has been suggested: this is obtained by delivering i.v. fluid in an amount exactly matched to the volume of urine produced by the patient under the effect of furosemide; this procedure was accomplished by a special device, called “RenalGuard,” with excellent results [101, 115]. (G) Use of hemodialysis or hemofiltration to remove CM immediately after the radiographic procedure; but so far this measure has not diminished the rate of CIN [116, 117].

Abbreviations

CM:	Contrast media
AKI:	Acute kidney injury
ARF:	Acute renal failure
eGFR:	Estimated glomerular filtration rate
GFR:	Glomerular filtration rate
CIN:	Contrast-induced nephropathy
SCr:	Serum creatinine
CrCl:	Creatinine clearance
RBF:	Renal blood flow
CT:	Computed tomography
MDRD:	Modification of diet in renal disease
NO:	Nitric oxide
ROS:	Reactive oxygen species
LOCM:	Low-osmolar contrast media
HOCM:	High-osmolar contrast media
IOCM:	Isoosmolar contrast media
MTT:	3-(4,5-Dimethyl-2-thiazolyl)-2,5-diphenyl-2H-tetrazolium bromide
PCI:	Percutaneous coronary interventions.

Conflict of Interests

The authors declare that there is no conflict of interests regarding the publication of this paper.

Acknowledgment

Dr. Ashour Michael is currently recipient of an “Assegno di Ricerca” (Research check) at the “Magna Graecia” University, Catanzaro, Italy.

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Copyright © 2014 Michele Andreucci et al. This is an open access article distributed under the Creative Commons Attribution License, which permits unrestricted use, distribution, and reproduction in any medium, provided the original work is properly cited.

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