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Reducing the Burden of Cardiovascular Calcification in Patients with Chronic Kidney Disease

Department of Medicine, University of Texas Health Sciences Center at San Antonio, San Antonio, Texas

Address correspondence to: Dr. Wajeh Y. Qunibi, Department of Medicine, University of Texas Health Sciences Center at San Antonio, 7703 Floyd Curl Drive, San Antonio, TX 78229-3900. Phone: 210-422-2692; Fax: 210-358-4710; E-mail: qunibi{at}uthscsa.edu

	Abstract

Top Abstract Introduction Clinical Consequences of CVC Interventions Designed to Reduce... Curbing Effects of Factors... Augmenting Effects of Factors... Other Interventions Genetic Susceptibility or... Can Cardiovascular Calcification... References

 
Patients with chronic kidney disease (CKD) have a higher burden of atherosclerotic coronary artery disease compared with age- and gender-matched individuals with normal renal function. Cardiovascular calcification (CVC), a marker of atherosclerosis, is also more prevalent in these patients and is associated with serious clinical consequences. The pathogenesis of CVC is complex and includes factors that promote calcification and others that inhibit calcification. Thus, multiple therapeutic interventions should be used simultaneously to reduce the burden of calcification in patients with CKD. Thus far, interventional attempts have focused on curtailing the effects of factors that promote calcification such as management of known traditional factors for atherosclerotic coronary artery disease and on adopting specific approaches to normalize mineral metabolism, deliver adequate dialysis, and control serum cholesterol level. By contrast, interventions that may bolster the effects of inhibitors of calcification have not yet been studied well but are beginning to attract attention. Ideally, the goal of interventions is not only to slow or halt progression of calcification but also to reverse pre-existing calcification. Whether this goal is achievable is not currently known. This review examines the potential of various therapeutic interventions in reducing the CVC burden in patients with CKD. Moreover, the review is intended to stimulate more research in this area because the efficacy of these interventions has not been examined in controlled clinical trials.

	Introduction

Top Abstract Introduction Clinical Consequences of CVC Interventions Designed to Reduce... Curbing Effects of Factors... Augmenting Effects of Factors... Other Interventions Genetic Susceptibility or... Can Cardiovascular Calcification... References

 
Coronary artery calcification (CAC), which is absent in normal vessels, represents an integral part of the atherosclerotic plaque (1). Detection and quantification of arterial calcification now can be easily achieved by the use of newer imaging techniques such as electron-beam computed tomography (EBCT) and multislice computed tomography (2,3). In the general population, coronary artery calcium (CAC) score as measured by EBCT was found to be an independent predictor of subsequent cardiac events in both symptomatic and asymptomatic individuals (3,4).

The pathogenesis of CVC is complex and includes factors that promote calcification and others that inhibit calcification (Tables 1 and 2). Several studies have clearly established that the prevalence and the extent of CVC are increased in patients with ESRD (5–8). The mechanisms that are responsible for CVC in patients with ESRD are still being debated and have been reviewed previously in detail (9). Briefly, cross-sectional studies in dialysis patients have shown a correlation between CAC and a number of uremia-related factors such as dialysis vintage, hyperphosphatemia, high calcium (Ca) x phosphorus (P) product, vitamin D therapy, and the prescribed daily dose of Ca-based phosphate binders (CBPB) (5–9).

	Clinical Consequences of CVC

Top Abstract Introduction Clinical Consequences of CVC Interventions Designed to Reduce... Curbing Effects of Factors... Augmenting Effects of Factors... Other Interventions Genetic Susceptibility or... Can Cardiovascular Calcification... References

	Interventions Designed to Reduce CVC in Patients with CKD

Top Abstract Introduction Clinical Consequences of CVC Interventions Designed to Reduce... Curbing Effects of Factors... Augmenting Effects of Factors... Other Interventions Genetic Susceptibility or... Can Cardiovascular Calcification... References

 
Theoretically, for any intervention to reduce CVC, it should curtail the influence of factors that promote calcification and/or augment the effects of factors that inhibit calcification. Unfortunately, such interventions have not been investigated in controlled clinical trials. Therefore, the potential beneficial role of some of these interventions on CVC must be considered speculative at this time. Hopefully, future interventional clinical studies will be designed to examine more carefully the role of these factors in reducing the burden of CVC in calcification-prone CKD patients (Table 3).

	Curbing Effects of Factors that Promote Vascular Calcification

Top Abstract Introduction Clinical Consequences of CVC Interventions Designed to Reduce... Curbing Effects of Factors... Augmenting Effects of Factors... Other Interventions Genetic Susceptibility or... Can Cardiovascular Calcification... References

Because dietary restriction of P and intermittent dialysis are not usually effective in controlling serum P, most dialysis patients require dietary phosphate binders (18). CBPB such as Ca acetate and Ca carbonate have replaced aluminum hydroxide as the most widely prescribed phosphate binders. Although cost-effective, recent concern over the possible role of Ca loading from these binders in progression of CVC has led to more frequent use of the considerably more expensive noncalcium, nonaluminum phosphate binder sevelamer hydrochloride (Renagel) (7–10). This concern became more widespread after the publication of the Treat to Goal Study, which showed a 25% increase in the coronary Ca scores among the patients who were treated with Ca salts compared with a 6% increment in the sevelamer group and a similar difference in aortic artery calcification scores. However, the mechanism of the beneficial effect of sevelamer on progression of calcification is unknown. One possible mechanism is reduced Ca loading during treatment with sevelamer. However, reduced cardiovascular calcification may also result from dramatic reductions in total and LDL cholesterol, which occur during treatment with this bile acid sequestrant. Moreover, results of the Calcium Acetate Renagel Evaluation (CARE), a randomized, double-blind trial, demonstrated that Ca acetate is significantly more effective than sevelamer in controlling serum P and Ca x P product to the recommended goal levels (19). Thus, it is conceivable that Ca acetate might in fact reduce the risk for CVC and mortality in dialysis patients as a result of better control of both serum P and Ca x P product. Clearly, more studies on the role of Ca loading from CBPB in progression of CVC are needed before prematurely abandoning these cost-effective binders.

Control of Hyperlipidemia
Hyperlipidemia, particularly increased LDL, has been implicated in progression of CAC (20–23). In addition, the beneficial effect of lowering LDL cholesterol levels on progression of calcification in the general population has been reported by several groups (21–23). Callister et al. (22) demonstrated that treatment with 3-hydroxy-3-methylglutaryl CoA reductase inhibitors can reduce the volume of calcified plaque in the coronary arteries (Figure 1). At the follow-up EBCT scans, a net reduction in the Ca-volume score of 7% was observed only in treated patients whose final LDL cholesterol levels were <120 mg/dl (P < 0.01). Moreover, in the only prospective study on the effect of lipid-lowering therapy on the progression of CAC, Achenbach et al. (23) found that treatment with the cholesterol-synthesis enzyme inhibitor cerivastatin significantly reduced coronary artery Ca progression in patients with LDL cholesterol levels >130 mg/dl (Figure 2). The median annual relative increase in coronary Ca was 25% during the untreated period versus 8.8% during the treatment period (P < 0.0001).

View larger version (16K): [in this window] [in a new window] [as a PowerPoint slide]   Figure 1. Reduction of LDL cholesterol to <120 mg/dl resulted in halting progression of coronary artery calcification (CAC). , Initial values; , final values for coronary artery Ca volume scores. As can be seen, patients in group 1 who were not treated with 3-hydroxy-3-methylglutaryl CoA (HMG-CoA) reductase inhibitor had significant progression of CAC. Similarly, patients in group 2 who were also treated but their average LDL cholesterol levels remained >120 mg/dl had significant progression of calcification. Patients in group 3 who were treated with HMG-CoA reductase inhibitor and their average LDL cholesterol levels were successfully reduced to <120 mg/dl had no progression of calcification. Reprinted from reference (29), with permission.

View larger version (48K): [in this window] [in a new window] [as a PowerPoint slide]   Figure 2. (A) Reduction of progression of CAC during treatment with a cholesterol-synthesis enzyme inhibitor cerivastatin. The figure shows the annualized relative change of the calcium volume score during the untreated period (electron-beam tomography [EBT] 1 to EBT 2) and during the treatment period (EBT 2 to EBT 3) for all 66 patients. Despite interindividual variation, the median annualized relative change (bold line) was significantly lowered by cerivastatin (25 versus 8.8%; P < 0.0001). (B) Annualized relative change of the calcium volume score in 32 patients who achieved an LDL cholesterol level <100 mg/dl during treatment with cerivastatin. In these patients, the median annualized change (bold line) decreased from 27% to –3.4% (P = 0.0001). Reprinted from reference (64), with permission.

Control of Secondary Hyperparathyroidism: Vitamin D versus Calcimimetic Agents
The current treatment of secondary hyperparathyroidism (SHPT) in dialysis patients includes suppression of parathyroid hormone secretion with supraphysiologic doses of vitamin D or its analogues. Unfortunately, vitamin D may predispose to vascular calcification. Rats that were treated with high-dose vitamin D developed calcification in the aorta, carotid, hepatic, mesenteric, renal, and femoral arteries (26). Clinical studies have also reported an association between vascular calcification and use of vitamin D therapy in hyperphosphatemic patients with renal failure (27,28). Vascular smooth muscle cells (VSMC) have been shown to express vitamin D receptors (29). Although vitamin D inhibits VSMC proliferation by enhancing Ca flux into cells, it induces VSMC to exhibit an osteoblastic phenotype (29). Vitamin D has also been shown to increase calcification in VSMC in vitro (30). Moreover, vitamin D therapy enhances the intestinal absorption of Ca and P and, therefore, often results in hypercalcemia, worsening hyperphosphatemia, and increased Ca x P product. Thus, although effective in reducing the severity of SHPT, vitamin D may increase the risk for CVC.

The new calcimimetic agents offer several advantages over vitamin D with respect to CVC. They prevent or treat SHPT without increasing serum Ca, P, or Ca x PO₄ product (31). Moreover, they have no adverse effects on vascular calcification. Although no clinical studies have demonstrated such a beneficial effect, preliminary in vitro and in vivo studies indicated that, compared with vitamin D, calcimimetic agents do not enhance aortic calcification (32–34). These effects, if confirmed in clinical studies, may result in the preferential use of calcimimetic agents to slow or halt progression of CVC in patients with CKD.

Treatment of Hypertension with Ca Channel Blockers
Several clinical trials in the general population have suggested a therapeutic or prophylactic effect of Ca channel blockers (CCB) on the progression of the atherosclerotic process (35–37). In the PREVENT study, the CCB amlodipine was found to reduce intimal medial thickness in type 2 diabetes (37). More recently, Motro and Shamesh (38) compared the effect of nifedipine and diuretics on progression of CAC in 201 hypertensive patients over a 3-yr period. They showed that CAC score increased by 40% in patients who were treated with nifedipine versus 78% on diuretics (P = 0.02). The effect was more pronounced in patients who had higher CAC scores at baseline. No similar studies have been reported in patients with CKD. Clearly, the effect of CCB on progression of CVC deserves further study, particularly in patients with CKD.

Role of Renal Transplantation
Cardiovascular mortality is clearly lower in renal transplant recipients than in dialysis patients (39,40). Moreover, the prevalence of CVC is also lower in renal transplant recipients than in dialysis patients (41). A preliminary study by Moe et al. (42) showed that CAC can be slowed or arrested after renal transplantation (Figure 3). A study by Stompor et al. (43) also showed no progression of CAC in renal transplant recipients compared with peritoneal dialysis patients. There are a number of potential mechanisms by which renal transplantation reduces the burden of CVC: First, renal transplantation restores renal function and therefore eliminates the role of uremic toxins in promoting CVC. Second, because baseline CAC scores in renal transplant recipients are dependent on the duration of dialysis (44), transplantation may reduce the burden of calcification by shortening the duration of dialysis. Third, renal transplantation may improve some disorders of mineral metabolism. Indeed, hypophosphatemia, rather than hyperphosphatemia, may develop in renal transplant recipients with normal graft function. Further studies designed to examine the role of renal transplantation in ameliorating CVC are clearly needed.

View larger version (26K): [in this window] [in a new window] [as a PowerPoint slide]   Figure 3. Change in coronary artery calcium score over time. The changes in CAC in transplant recipients (A) and hemodialysis patients (B) are plotted for individual patients who had calcification at baseline. Reprinted from reference (53), with permission.

	Augmenting Effects of Factors that Inhibit Vascular Calcification

Top Abstract Introduction Clinical Consequences of CVC Interventions Designed to Reduce... Curbing Effects of Factors... Augmenting Effects of Factors... Other Interventions Genetic Susceptibility or... Can Cardiovascular Calcification... References

Several animal knockout models have shown that the Ca-regulatory factors matrix Gla protein (MGP), osteoprotegerin (OPG), and fetuin-A (2-Heremans-Schmid glycoprotein-Ahsg) may be protective from vascular calcification (46–49). Mice deficient in MGP or OPG develop spontaneous vascular calcification (48). Similarly, mice deficient in fetuin-A also develop severe ectopic calcification when fed a mineral- and vitamin D–rich diet or when fed a normal diet when combined with a DBA/2 genetic background (49). Unfortunately, the therapeutic potential of these inhibitors of calcification has not been explored in clinical trials. However, because MGP requires vitamin K for -carboxylation, acquired vitamin K deficiency, as with the use of warfarin, may predispose to vascular calcification (50). It is interesting that calciphylaxis, or calcific uremic arteriolopathy, has been reported with increasing frequency in patients who are treated with warfarin therapy (11). Thus, it is possible that by avoiding the use of warfarin in patients with CKD, the risk for CVC may be reduced by not interfering in the production of MGP.

Similarly, OPG knockout mice develop osteoporosis and severe vascular calcification (48). This observation indicates that OPG is an important inhibitor of calcification of blood vessel walls. Paradoxically, serum OPG levels are associated with the extent of vascular calcification in hemodialysis patients (46,51). This may be a compensatory, protective response to the progression of vascular calcification or due to the effect of OPG on decreasing bone turnover, thus impairing the ability of bone to buffer Ca load (46). It is interesting that a study by Price et al. (52) showed that subcutaneous doses of OPG that inhibited bone resorption in rats were effective in inhibiting arterial calcification induced by warfarin or vitamin D.

Finally, fetuin-A has also been shown to be a potent systemic inhibitor of calcification, accounting for approximately 50% of the precipitation inhibitory capacity of serum (49,53). Hemodialysis patients have lower levels of fetuin-A compared with control subjects with normal renal function (53). The effect of restoring fetuin-A levels in dialysis patients on progression of CVC has not been reported but potentially could represent an attractive therapeutic modality.

Inhibitors of Bone Resorption
Clinical and experimental studies have consistently established an association between arterial calcification and bone resorption (54–56). Consequently, it can be hypothesized that treatment strategies that reduce bone resorption and increase bone mineralization may simultaneously decrease the risk for vascular calcification. Indeed, several preliminary studies have shown a beneficial effect of bisphosphonates and other inhibitors of bone resorption on vascular calcification (54,57).

Etidronate was shown previously to inhibit vitamin D–induced arterial calcification in rats (58,59). Other bisphosphonates, such as ibandronate and alendronate, also inhibited arterial and cardiac valve calcification after 2 and 4 wk in a warfarin-induced ectopic calcification model (50,54). The effect of intermittent etidronate therapy on progression of vascular calcification was recently reported in 35 hemodialysis patients (Figure 4) (59). In that study, three courses of etidronate, 200 mg/d for 14 d every 3 mo, significantly suppressed CAC progression with no change in bone mineral density. This effect was associated with a decrease in both C-reactive protein and serum OPG levels.

View larger version (52K): [in this window] [in a new window] [as a PowerPoint slide]   Figure 4. Axial cross-section obtained by spiral computed tomography in a 73-yr-old patient at baseline (A) and after cyclic intermittent etidronate therapy (B). Reprinted from reference (59), with permission.

	Other Interventions

Top Abstract Introduction Clinical Consequences of CVC Interventions Designed to Reduce... Curbing Effects of Factors... Augmenting Effects of Factors... Other Interventions Genetic Susceptibility or... Can Cardiovascular Calcification... References

	Genetic Susceptibility or Immunity

Top Abstract Introduction Clinical Consequences of CVC Interventions Designed to Reduce... Curbing Effects of Factors... Augmenting Effects of Factors... Other Interventions Genetic Susceptibility or... Can Cardiovascular Calcification... References

 
Limited evidence suggests that CAC has strong genetic determinants (62). Possibly, some genes are procalcification genes, whereas others are anticalcification (protective) genes. Little is known about these CAC susceptibility genes, and it is vitally important to identify and characterize these genes by identifying the chromosomal regions that harbor them. The identification of susceptibility genes for CAC should increase the knowledge about CVD risk for a given patient and help to identify those for whom intensive preventive or therapeutic measures may be most beneficial.

	Can Cardiovascular Calcification Be Reversed?

Top Abstract Introduction Clinical Consequences of CVC Interventions Designed to Reduce... Curbing Effects of Factors... Augmenting Effects of Factors... Other Interventions Genetic Susceptibility or... Can Cardiovascular Calcification... References

 
So far, the goal of most interventional studies has been to slow or halt progression of CVC. However, whether calcification can realistically be reversed, particularly in patients with CKD, is not known at the present time. It is interesting that several studies have indicated that reversal of calcification may indeed be possible. Callister et al. (29) reported regression of Ca volume score in 63% of 65 patients with LDL levels <120 mg/dl. In another study of 102 symptomatic patients with CAC, Schmermund et al. (20) reported that standard therapy for coronary artery disease resulted in regression of calcification in 15% of patients with suspected or known coronary artery disease on follow-up EBCT scans. Although it is possible that regression of calcification may be due to interscan variability, these authors speculated that reduction of calcification may be the result of shrinkage and increased density of the calcified lesions. Given that CAC may be predictive of cardiovascular events and death from CVD, interventions designed to induce regression of calcification may help to reduce the risk for death in patients with CKD and coronary artery disease.

	References

Top Abstract Introduction Clinical Consequences of CVC Interventions Designed to Reduce... Curbing Effects of Factors... Augmenting Effects of Factors... Other Interventions Genetic Susceptibility or... Can Cardiovascular Calcification... References

 

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