Cinacalcet lowers parathyroid hormone levels. Whether it can prolong survival of people with chronic kidney disease (CKD) complicated by secondary hyperparathyroidism (SHPT) remains controversial, in part because a recent randomized trial excluded patients with iPTH <300 pg/ml. We examined cinacalcet’s effects at different iPTH levels. This was a prospective case-cohort and cohort study involving 8229 patients with CKD stage 5D requiring maintenance hemodialysis who had SHPT. We studied relationships between cinacalcet initiation and important clinical outcomes. To avoid confounding by treatment selection, we used marginal structural models, adjusting for time-dependent confounders. Over a mean of 33 months, cinacalcet was more effective in patients with more severe SHPT. In patients with iPTH ≥500 pg/ml, the reduction in the risk of death from any cause was about 50% (Incidence Rate Ratio [IRR] = 0.49; 95% Confidence Interval [95% CI]: 0.29–0.82). For a composite of cardiovascular hospitalization and mortality, the association was not statistically significant, but the IRR was 0.67 (95% CI: 0.43–1.06). These findings indicate that decisions about using cinacalcet should take into account the severity of SHPT.
In people with advanced chronic kidney disease (CKD), secondary hyperparathyroidism (SHPT) can cause bone-related complications. Those complications include high levels of parathyroid hormone (PTH) and mineral abnormalities such as hypercalcemia and hyperphosphatemia. Correcting these abnormalities is important because they are associated with cardiovascular disease and mortality, which occurs relatively frequently in people with CKD1,2,3. Cinacalcet is a calcimimetic drug that inhibits the secrection of PTH and can reduce the risk of mineral abnormalities4,5. By retarding the progression of vascular calcification mediated by hypercalcemia and hyperphosphatemia6, cinacalcet might prevent death and particularly death due to cardiovascular disease. However, results of previous studies of cinacalcet’s effect on cardiovascular disease and mortality were not definitive7 and may not be generalizable to many clinical settings.
In the Evaluation of Cinacalcet Therapy to Lower Cardiovascular Events (EVOLVE) study, cinacalcet’s efficacy was evaluated with a composite outcome of cardiovascular disease and all-cause death in adults with CKD stage 5D (dialysis). In that study, the difference between the cinacalcet and placebo groups was not statistically significant (hazard ratio 0.93)8. However, about 20% of the patients in the placebo group did not continue receiving placebo and instead began receiving cinacalcet. By design, the intention to treat (ITT) analysis in the randomized trial did not account for that crossover. In addition, a large percentage patients in the cinacalcet group discontinued the active drug, because of adverse effects. One consequence was that the power to detect cinacalcet’s effect in patients who were randomly assigned to receive it was probably reduced.
In addition, patients in that study might differ in important ways from patients in many clinical-practice settings. First, CKD stage 5D patients with SHPT are, on average, 7 to 8 years older than the participants in the EVOLVE study9,10. Second, to maintain intact PTH (iPTH) levels in the range of, for example, 150 to 300 pg/ml11, patients can be treated with cinacalcet even if their serum iPTH is <300 pg/ml, in which case they would not have been included in the EVOLVE study. Also, cinacalcet’s effect might depend on the serum iPTH level. Specifically, cinacalcet reduces the volume of the parathyroid glands and it reduces abnormally high levels of mineral and bone disorder (MBD) markers, but those effects are greater in patients with larger parathyroid glands and they are greater in patients with higher serum iPTH levels12,13. Therefore it is important to ask whether the effectiveness of cinacalcet against clinically important events is, similarly, greater in patients with higher serum iPTH levels. That is the question we sought to answer in the present study. The answer will allow physicians to inform their patients of the effects they can expect if they begin taking cinacalcet, including the different effects that might be expected given different severities of SHPT.
In Japan, cinacalcet has been commercially available since January 2008 and since then its use has gradually increased. With little or no prospect for enrolling patients in a randomized trial once cinacalcet was newly-authorized for clinical use, instead, just before cinacalcet became available, we started a large, prospective, observational study, the “Mineral and Bone Disorders Outcomes Study for Japanese CKD Stage 5D Patients” (MBD-5D). Using pre-specified protocols14, we analyzed data from the MBD-5D with marginal structural models (MSMs), to account for time-dependent confounding. Applying MSMs to these cinacalcet-naïve patients allowed us to better estimate the effects of cinacalcet initiation on death due to any cause and death due to cardiovascular disease in clinical practice. This is similar to ITT analysis, except that untreated patients are allowed to switch cinacalcet arms. This analytic approach of employing MSMs as a kind of ITT analyses has been used in other studies15.
In the subcohort (patients selected at ramdom from the whole cohort: see “sample sizes and study designs” section) the mean age was 61.9 years and the median dialysis vintage was 8.3 years (Table 1). At baseline (i.e. before cinacalcet was marketed), 1328 (40.5%) of the patients had iPTH values ≥300 pg/ml and the prevalences of guideline-defined hypercalcemia (corrected serum calcium level >10 mg/dl) and hyperphosphatemia (serum phosphorus level >6.0 mg/dl)16 were 25% and 32%, respectively (Table 1). Cinacalcet was prescribed at any time during follow-up to 1384 (42%) of the subcohort patients (Table 2). Baseline characteristics of the cases (patients who experienced “death due to cardiovascular disease” or “death due to any cause”; see “Sample sizes and study designs” section) outside the subcohort are shown in Table S1. When compared with patients who had never received cinacalcet, those who did receive cinacalcet were younger, less likely to have diabetic nephropathy and less likely to have cardiovascular disease (Table 2). As a group, their history of dialysis treatment was longer and they were more likely to have high levels of calcium, phosphorus and iPTH. They were more likely to have received an intravenous vitamin D receptor activator (VDRA), were less likely to have received a calcium-based phosphate binder and overall they had higher values of Kt/V, albumin and creatinine. Those in higher iPTH categories received intravenous VDRA more often and they had more severe hypercalcemia and hyperphosphatemia (Table 1). Differences in characteristics among the patients with or without cinacalcet prescription by baseline iPTH categories were similar to those in the total subcohort (Table 2).
The proportion of patients receiving cinacalcet increased monotonically from 0% at visit 0 to 42% at visit 12 (Fig. S1, intervals between visits were 3 months). At visit 12, the median (interquartile range) dose of cinacalcet in the patients who received it was 25 mg/day (25 to 50 mg/day). The estimated proportion of patients receiving cinacalcet who continued to receive it for 36 months (i.e., 12 visits) decreased from the time of the first prescription but still it was 70% in the 36th month after the first prescription (Fig. S2). When patients were stratified by baseline iPTH categories, the proportions of patients receiving cinacalcet at visit 12 differed by more than 30 percentage points: 30.9%, 49.9% and 63.2% in those with baseline iPTH levels <300 pg/ml, 300–<500 pg/ml and more than 500 pg/ml, respectively (Fig. 1). However, the estimated proportions of patients who had continuously received cinacalcet for 36 months after the first prescription differed only very slightly: 70.7%, 66.1% and 71.8% among the three baseline iPTH levels (log-rank P = 0.23) (Fig. 2).
A total of 1226 deaths occurred in the total cohort during the observation period, of which 521 (41.8% of all deaths) were due to cardiovascular disease (Table S2) and 159 (13.0% of all deaths) were of “unknown” cause and thus were not included among those due to cardiovascular causes. The crude rates of death due to any cause, death due to cardiovascular disease and cardiovascular hospitalization or death were 5.49, 2.07 and 13.2 per 100 person-years, respectively.
The iPTH level at baseline modified the effect of cinacalcet’s initiation on clinical outcomes. In higher categories of baseline iPTH, the apparent benefits of cinacalcet were larger (Table 3). In particular, in patients with baseline iPTH levels ≥500 pg/ml, cinacalcet initiation was associated with lower incidence rate ratio (IRR) for death due to any cause (adjusted IRR 0.49, 95% CI 0.29–0.82). For cardiovascular hospitalization or death due to any cause, although the association was not statistically significant, the adjusted IRR was less than 1 (IRR = 0.67; 95% CI 0.43–1.06). In contrast, in patients with baseline iPTH levels <300 pg/ml, cinacalcet initiation was not associated with any of the 3 clinical outcomes. Graded magnitudes of cinacalcet’s effects across baseline iPTH categories were consistent among all 3 clinical outcomes.
When analyses were restricted to patients with iPTH levels ≥300 pg/ml (an inclusion criterion of the EVOLVE study), cinacalcet initiation was associated with a lower incidence of cardiovascular hospitalization or death due to any cause (adjusted IRR 0.71, 95% CI 0.53–0.94) (Table 4). For death due to any cause, although the association was not statistically significant, the adjusted IRR was less than 1 (IRR = 0.75; 95% CI 0.55–1.03). Cinacalcet’s association with cardiovascular death was not statistically significant (adjusted IRR 0.90, 95% CI 0.56–1.47).
In the sensitivity analyses of effect modifications in the total cohort and primary effects in patients with iPTH levels ≥300 pg/ml, the directions of associations between cinacalcet initiation and IRs of the 3 clinical outcomes and the precisions of those estimates, were similar to the results of the main analyses (Tables S3, S4).
In this large prospective study of CKD stage 5D patients with SHPT receiving hemodialysis, cinacalcet initiation was more effective in patients who had higher levels of iPTH at baseline, on two important clinical outcomes: death due to any cause and a composite of cardiovascular hospitalization and mortality. Specifically, in patients with baseline iPTH levels ≥300 pg/ml cinacalcet initiation was associated with lower incidences of cardiovascular hospitalization or death due to any cause.
Several strengths of the present study warrant mention. First, the effects estimated by MSMs can be interpreted as average differences between two rates: the rate of outcomes that would be expected if all patients initiated cinacalcet and the rate that would be expected if none received it. By starting the study before cinacalcet was marketed, we acquired information regarding cinacalcet use from the time that it was first prescribed. Enrolling only new cinacalcet users who had pretreatment baseline measurements prevents survivorship bias. Analyzing those data together with variables likely to affect cinacalcet prescription (e.g., PTH, calcium and VDRA), we adjusted for the effects of those time-dependent confounders. With MSMs, we adjusted for those confounders without removing their intermediate effect caused by previous cinacalcet use. Probably because of these advantages of MSMs, their use is becoming common in nephrology research17,18,19. Second, the results indicating iPTH-dependence of cinacalcet’s effects came from circumstances found in regular clinical practice. This point is important because SHPT treatment varies between dialysis facilities and dialysis patients vary widely regarding comorbid conditions and severity of SHPT. Third, regarding generalizability, we note that in age, vintage and comorbidities the patients in this study were similar to a randomly-selected sample of dialysis patients in Japan20.
Cinacalcet initiation was more effective in patients with more severe iPTH levels. The EVOLVE study found no statistically significant effect of cinacalcet on cardiovascular outcomes (hazard ratio 0.93, 95% CI 0.85–1.02), which appears to conflict with the results of the present study restricted to patients with baseline iPTH levels ≥300 pg/ml. However, interpretation of that hazard ratio is complicated by imbalance in prognostic factors at baseline, by discontinuation of active cinacalcet therapy among two thirds of patients in the cinacalcet group and by 20% crossover from the placebo group21. In the present study, the analyses were designed to simulate ITT analyses except that untreated patients were allowed to switch to the cinacalcet arm and their results might be less diluted by non-adherence to cinacalcet than were the results of the EVOLVE study, partly because the estimated proportion of patients receiving cinacalcet continuously was high during the 3 years after the first prescription. Consistent with this observation, compliance regarding drug continuation and dialysis treatment are better in Japan than in other countries22,23. In addition, we could also examine effects of cinacalcet’s initiation in patients with baseline iPTH levels <300 pg/ml, who would have been excluded from the EVOLVE study. Among them, cinacalcet was associated with none of the 3 clinical outcomes. Further study is warranted to determine whether patients with iPTH <300 pg/ml can benefit from cinacalcet. These findings may be strengthened by three facts: First, SHPT is treated to lower target values in Japan than in the US16. Second, in 41.2% of the dialysis facilities in this MBD-5D study (a representative random sample of dialysis facilities in Japan) cinacalcet can be started at iPTH levels of 150–300 pg/ml24. Third, the very high iPTH levels seen in African-Americans25 are less common in Japan.
Although the cohort size was large and the follow-up of 3 years offered a good time range to report on meaningful outcomes, the effects of cinacalcet’s initiation on cardiovascular death were not statistically significant, even in patients with high levels of serum iPTH. A number of explanations are possible. In particular, we note that 13% of deaths were of unknown cause. If any of those deaths were actually of cardiovascular cause, then they were misclassified, which might have led to results being not statistically significant. In addition, only 4.6% of deaths were attributed to sudden death in our study. The EVOLVE post-hoc study suggested that cinacalcet could benefit the cardiovascular system by attenuating nonatherosclerotic cardiovascular events like sudden death, which accounted for 24.5% of deaths in the EVOLVE trial26. Also, the ITT-like analysis cannot account for dilution of effects caused by discontinuation of cinacalcet. In addition, when we calculated the sample size we overestimated both the size of the effect of a drug such as cinacalcet and the numbers of clinical outcomes14. It is clear in retrospect that our study was underpowered, as both the event rate and the effect size were overestimated in the sample-size computations. Discontinuation of cincalcet by some patients also contributed to underpowering. This could explain the failure to differentiate cinacalcet’s effects on some clinical outcomes from the null.
As possible explanations for the finding that cinacalcet was more effective in patients with higher iPTH levels, we note that the magnitudes of the reductions in iPTH and phosphorus are greater in patients with higher levels of iPTH at baseline13. In addition, although median cinacalcet dose prescribed in our study population was 25 mg/day (interquartile range 25–50 mg/day), our previous study showed that initiating cinacalcet resulted in better iPTH control, with an absolute difference of 25%27. That previous study also showed that initiating cinacalcet and reducing VDRA dosage resulted in 9% and 12% increases in the number s of patients who were within the guideline-specified calcium and phosphorus ranges. Initiating cinacalcet alone while maintaining the VDRA dosage resulted in an 8% increase in the number of patients who were within the guideline-specified calcium range27.Thus patients with higher levels of MBD markers might particularly benefit from the reduction of MBD markers by initiation of cinacalcet with subsequent VDRA adjustment.
Several limitations of this study should be mentioned. First, we might not have measured all of the important influences on cinacalcet prescription. However, several sensitivity analyses with more covariates than the primary analyses gave results similar to those of the primary analyses, which indicates that the main findings are unlikely to have been influenced by residual confounding. Although cinacalcet users were younger, much more likely to have longer vintage, less comorbidity and glomerulonephritis as the primary renal disease, those covariates were included in the MSMs. A major implication of our study is that differences in iPTH levels are causally related to differences in cinacalcet’s effectiveness with regard to important clinical outcomes. Imbalances in measured and unmeasured factors are unlikely to explain the variation in cinacalcet’s effectiveness related to iPTH levels.
The second limitation is that although several iPTH assay methods were available in Japan, information on the specific assay used for iPTH in each center could not be obtained. Third, multiple inferences were made but no adjustment was considered for the overall type-I error rate. Fourth, although the proportion of patients receiving cinacalcet continuously was described, we could not track actual cinacalcet use over time. However, compliance regarding drug continuation is better in Japan than in other countries22,23 and in Japanese dialysis practice the patient’s adherence is regularly determined every two weeks or every month, we believe it unlikely that the lack of tracking of cinacalcet prescriptions lead to misclassification. Fifth, we could not measure other MBD-related serum biomarkers such as bone specific alkaline phosphatase. Sixth, because patients could begin to receive cinacalcet at any time, the period between baseline iPTH measurement and cinacalcet initiation varied from 3–36 months, whereas in a randomized trial the baseline variables would be measured immediately prior to treatment initiation. However, our MSMs controlled for the variation in iPTH levels between baseline and cinacalcet initiation.
In conclusion, in this large unselected group of CKD stage 5D patients in Japan who had SHPT and received hemodialysis, cinacalcet was more beneficial in patients with higher iPTH levels on death from any cause and on a composite of cardiovascular hospitalization and mortality. These findings can inform the decisions of physicians and dialysis patients as they consider whether or not to use cinacalcet, given the severity of a patient’s SHPT.
The MBD-5D was a 3-year prospective case-cohort and cohort study. Because this study was an observational study using anonymized data collected during routine practice, informed consent was not mandatory according to the ethical guidelines for epidemiological research in Japan28. The study protocol and the waiver of informed consent were approved by a central ethics committee at Kobe University’s School of Medicine (No. 754). The study was conducted in accordance with the Declaration of Helsinki and the ethical guidelines for epidemiological research in Japan28.
The target population was CKD-5D patients with SHPT who received maintenance hemodialysis. Eligible patients were i) those receiving hemodialysis at one of the participating facilities as of 1 January 2008 and ii) either those with iPTH concentration ≥180 pg/mL or those who were receiving an intravenous Vitamin D receptor activator (VDRA) (calcitriol or maxacalcitol) or an oral active VDRA (falecalcitriol, the only oral VDRA approved in Japan for SHPT treatment). Patients who had been receiving dialysis for less than 3 months were excluded. From 86 facilities across Japan, 8229 patients were registered in the study cohort. Data were collected until January 2011.
Outcomes and exposures
We examined three clinical outcomes: (1) death due to any cause, (2) death due to cardiovascular disease and (3) single cardiovascular hospitalization or death due to any cause, whichever came first (Table S5). We examined the effects of “cinacalcet initiation” as the primary exposure. Specifically, before cinacalcet initiation all patients in the study were considered to be in the non-initiation arm. Once cinacalcet was initiated, all patients to whom it was prescribed were considered to be in the cinacalcet arm until the end of follow-up. As this was an observational study, the decision to prescribe or not prescribe cinacalcet was made by each physician. Prescription information was extracted from medical records and was handled as a time-dependent variable. Misclassification due to primary non-adherence (not filling a prescription) is unlikely in this study, because patients in Japan usually go to a pharmacy soon after receiving a physician’s prescription, that is, about every two weeks or every month. In regular dialysis practice in Japan, at the time of each patient’s visit to a hemodialysis facility, a staff nurse verifys that the previously given prescription has been filled and the medication has been taken regularly.
Sample sizes and study designs
As the MBD-5D study was designed to answer more than one research question (associations between mineral abnormalities and outcomes and associations between cinacalcet and outcomes), the sample size was not determined for specific treatments14. However, sample size was determined as follows: for death due to cardiovascular disease, (1) the expected rate was 2.5 deaths per 100 person-years during the 3-year follow up period, (2) the effect size of a drug was 20% to 25% of the relative risk, (3) the proportion of patients to whom the drug was prescribed was one-third. With those values, 6000–7500 patients would be required for 80% power with a two-sided alpha of 0.05. We did not have the financial resources needed to hire clinical research coordinators to collect data repeatedly from all of the patients (the “whole cohort”, n = 8229) and therefore we conducted a case-cohort study. Patients were randomly sampled from the whole cohort to yield a “subcohort”. Although data were prospectively and repeatedly collected only from patients in the subcohort, drug’s effect could be estimated by analyzing data from the whole cohort14,29. (Figure 3) Specifically, the case-cohort analysis included records of all patients in whom an outcome event occurred as well as all records of subcohort patients in whom an outcome event did not occur. The former received a weight of 1.0 and the latter received a weight determined by the inverse of the sampling fraction, to account for the fact that non-cases outside the subcohort were not observed29. The case-cohort design was used for “death due to cardiovascular disease” and for “death due to any cause” (cases) (Fig. 3). To examine whether a drug was associated with reduced cardiovascular hospitalization or death due to any cause in the subcohort, the sampling fraction used was 0.4 (i.e. the subcohort n = 3276) based on the following assumptions: (1) the expected rate of cardiovascular hospitalization or death due to any cause was assumed to be 13.0 events per 100 person-years during the 3-year follow-up period, (2) the effect size of a drug was assumed to be 20% to 25% of the relative risk and (3) the proportion of patients to whom the drug was prescribed was one-third. With those values, 3000 patients would be required for 80% power with a two-sided alpha of 0.0514. A cohort design was used for cardiovascular hospitalization or death due to any cause. Details of the participants in each part of the study are given in Figure S3. As reported previously, the randomly-selected subcohort and the whole cohort were similar in terms of age, gender and iPTH at baseline10.
Covariates used in the primary analyses included baseline (time of entry into cohort) patient characteristics (age, gender, vintage, primary renal disease, cardiovascular disease, lung disease, liver disease, malignancy and history of parathyroidectomy), MBD-related serum markers (calcium, phosphorus and iPTH), prescriptions for MBD-related drugs (VDRAs and phosphate binders) and other potential confounders (dialysate calcium concentration, Kt/V, albumin, BMI and hemoglobin).
Data were collected from 86 dialysis facilities by trained staff. Data on demographics and comorbidities were collected at the time of enrollment (visit 0). Data on MBD markers and treatments were collected at the time of enrollment (visit 0) and every 3 months for 3 years (visits 1–12). Data were collected every 6 months for the other time-dependent variables, prospectively for the subcohort patients and retrospectively for cases outside the subcohort. The laboratory data used were those measured closest to the end of each visit. Serum iPTH levels (reference 10–65 pg/ml) were measured in 73 facilities. Serum whole PTH levels measured by a third-generation PTH assay (immunoradiometric assay; reference 9–39 pg/ml) were used in 13 facilities and converted to iPTH levels: iPTH = whole PTH × 1.716. Serum calcium levels were corrected for albumin concentration using the modified Payne method, which is commonly used in Japanese dialysis settings16.
Crude mortality rate and cardiovascular mortality rate were estimated using all cases and the subcohort patients. Crude incidence rates (IRs) for cardiovascular hospitalization and death due to any cause were estimated from the subcohort data. The crude rates were calculated for those 3 clinical outcomes, stratified by the status of cinacalcet use.
Marginal structural models
Marginal structural models (MSMs) were used to estimate cinacalcet’s effects on clinical outcomes15,30,31. MSMs appropriately account for effects of potential time-dependent confounders such as iPTH and calcium, which are also a potential source of confounding by indication30. They are affected by previous cinacalcet use and they are also predictors of future cinacalcet use and of clinical outcomes32. In addition, MSMs allow us to compare two IRs: the IR that would be expected if all study patients were treated and the IR that would be expected if none of the study patients were treated. IRR of clinical outcomes were estimated for cinacalcet initiation in comparison with non-initiation.
For each 3-month period ending at visit t, the incidence of each clinical outcome was modeled as a function of whether cinacalcet had been initiated at or before the previous 3-month period (visit t-1). Weights were calculated from the inverse of the probability of the cinacalcet-prescription history a patient actually had during each 3-month period of follow-up until cinacalcet initiation. These probabilities were predicted from a pooled logistic regression model. In that model, the dependent variable was cinacalcet prescription at a given visit t-1. The independent variables were time-dependent confounders at visit t-2 (calcium, phosphorus, iPTH, VDRA, phosphate binder, several product terms of these MBD biomarkers and treatments, dialysate calcium, Kt/V, albumin, BMI, hemoglobin), baseline covariates (age, gender, vintage, primary renal disease, cardiovascular disease, lung disease, liver disease, malignancy, history of parathyroidectomy) and visit number. Similarly, censoring weighting was calculated to account for loss to follow-up (n = 143), switch to peritoneal dialysis (n = 2) or renal transplantation (n = 5).
Weighted Poisson regression with robust variance was used to estimate the IRRs. Any data missing at baseline were replaced by their mean or median values, or by predicted values from linear regression models. Missing data were imputed by carrying the last observation forward. We used these simple imputation methods for two reasons: First, there were very few missing values of MBD-related markers of interest (<0.2% at baseline and about 2% during the follow-up, except for 6% in iPTH). Second, for laboratory values, the last-observation-forward technique makes sense in that physicians would likely use a similar method to make prescription decisions.
To estimate modification of effect of cinacalcet intiation by iPTH at baseline, we used three categories of baseline iPTH: <300 pg/ml, 300–<500 pg/ml and 500 ≥ pg/ml. The cut-off value of 300 pg/ml was based on the upper limit of the targeted range in the KDOQI guideline and on the inclusion criteria in the EVOLVE study8,11. The cut-off value of 500 pg/ml was based on the reference for parathyroid intervention therapy recommended in the Japanese guidelines, as patients with iPTH ≥500 pg/ml are considered to have a higher likelihood of having nodular hyperplasia in the parathyroid glands14. These three categories were entered into the weighted Poisson regression model with interaction terms with cinacalcet initiation32.
To estimate cinacalcet’s effects in patients similar to those in the EVOLVE study, further analyses were done using data only from those patients with an iPTH level ≥300 pg/ml (the “restricted” analyses).
Sensitivity analysis of effect modification was done, with baseline iPTH categories included in models estimating treatment weights or with more covariates (covariates in the primary analysis, plus dementia, other central nervous disease, baseline creatinine and total cholesterol, time-varying values of total iron, ferritin and CRP and specific cardiovascular conditions: coronary artery disease, atrial fibrillation, arrhythmia, congestive heart failure, cerebrovascular disease, peripheral vascular disease, aortic disease, pacemaker, or other cardiovascular conditions. About 20% of the data on total iron, ferritin and CRP were missing, so the function aRegImpute in R was used to make an imputed dataset33.). Sensitivity analyses were also done with or without more covariates for the patients restricted to those with baseline iPTH levels ≥300 pg/ml (an inclusion criterion of the EVOLVE study).
P values < 0.05 were taken as indicators of statistical significance. Using SAS 9.2 (SAS Institute, Cary, NC), N.K. and Y.O. analyzed the data first. Then A.E.R. used his original SAS coding and obtained the same results.
How to cite this article: Akizawa, T. et al. PTH-dependence of the effectiveness of cinacalcet in hemodialysis patients with secondary hyperparathyroidism. Sci. Rep. 6, 19612; doi: 10.1038/srep19612 (2016).
Go, A. S., Chertow, G. M., Fan, D., McCulloch, C. E. & Hsu, C. Y. Chronic kidney disease and the risks of death, cardiovascular events and hospitalization. N Engl J Med 351, 1296–1305 (2004).
Tentori, F. et al. Mortality risk for dialysis patients with different levels of serum calcium, phosphorus and PTH: The Dialysis Outcomes and Practice Patterns Study (DOPPS). Am J Kidney Dis 52, 519–530 (2008).
Fukagawa, M. et al. Abnormal mineral metabolism and mortality in hemodialysis patients with secondary hyperparathyroidism: Evidence from marginal structural models used to adjust for time-dependent confounding. Am J Kidney Dis 63, 979–987 (2014).
Akizawa, T. et al. Decreases in PTH in japanese hemodialysis patients with secondary hyperparathyroidism: Associations with changing practice patterns. Clin J Am Soc Nephrol 6, 2280–2288 (2011).
Block, G. A. et al. Cinacalcet for secondary hyperparathyroidism in patients receiving hemodialysis. N Engl J Med 350, 1516–1525 (2004).
Raggi, P. et al. The ADVANCE study: A randomized study to evaluate the effects of cinacalcet plus low-dose vitamin D on vascular calcification in patients on hemodialysis. Nephrol Dial Transplant 26, 1327–1339 (2011).
Carney, E. F. Chronic kidney disease: No significant effect of cinacalcet on cardiovascular outcomes in patients undergoing dialysis- EVOLVE results. Nat Rev Nephrol 9, 4 (2013).
Chertow, G. M. et al. Effect of cinacalcet on cardiovascular disease in patients undergoing dialysis. N Engl J Med 367, 2482–2494 (2012).
Block, G. A. et al. Cinacalcet hydrochloride treatment significantly improves all-cause and cardiovascular survival in a large cohort of hemodialysis patients. Kidney Int 78, 578–589 (2010).
Fukagawa, M. et al. Mineral metabolism management in hemodialysis patients with secondary hyperparathyroidism in Japan: Baseline data from the MBD-5D. Am J Nephrol 33, 427–437 (2011).
National Kidney Foundation. KDOQI clinical practice guidelines for bone metabolism and disease in chronic kidney disease. Am J Kidney Dis 42, Supplement 3, 1–201 (2003).
Komaba, H. et al. Cinacalcet effectively reduces parathyroid hormone secretion and gland volume regardless of pretreatment gland size in patients with secondary hyperparathyroidism. Clin J Am Soc Nephrol 5, 2305–2314 (2010).
Cooper, K., Quarles, D., Kubo, Y., Tomlin, H. & Goodman, W. Relationship between reductions in parathyroid hormone and serum phosphorus during the management of secondary hyperparathyroidism with calcimimetics in hemodialysis patients. Nephron Clin Pract 121, c124–c130 (2012).
Fukuhara, S. et al. Mineral and bone disorders outcomes study for Japanese chronic kidney disease stage 5D patients: Rationale and study design. Ther Apher Dial 15, 169–175 (2011).
Hernán, M. Á., Brumback, B. & Robins, J. M. Marginal structural models to estimate the causal effect of zidovudine on the survival of HIV-positive men. Epidemiology 11, 561–570 (2000).
Clinical practice guideline for the management of secondary hyperparathyroidism in chronic dialysis patients. Ther Apher Dial 12, 514–525 (2008).
Weinhandl, E. D., Rao, M., Gilbertson, D. T., Collins, A. J. & Pereira, B. J. G. Protective effect of intravenous levocarnitine on subsequent-month hospitalization among prevalent hemodialysis patients, 1998 to 2003. Am J Kidney Dis 50, 803–812 (2007).
Brunelli, S. M. et al. History-adjusted marginal structural analysis of the association between hemoglobin variability and mortality among chronic hemodialysis patients. Clin J Am Soc Nephrol 3, 777–782 (2008).
Brunelli, S. M., Chertow, G. M., Ankers, E. D., Lowrie, E. G. & Thadhani, R. Shorter dialysis times are associated with higher mortality among incident hemodialysis patients. Kidney Int 77, 630–636 (2010).
Akizawa, T. et al. Japanese haemodialysis anaemia management practices and outcomes (1999–2006): Results from the DOPPS. Nephrol Dial Transplant 23, 3643–3653 (2008).
Perkovic, V. & Neal, B. Trials in kidney disease–time to EVOLVE. N Engl J Med 367, 2541–2542 (2012).
Bleyer, A. J. et al. An international study of patient compliance with hemodialysis. JAMA 281, 1211–1213 (1999).
Hirth, R. A., Greer, S. L., Albert, J. M., Young, E. W. & Piette, J. D. Out-of-pocket spending and medication adherence among dialysis patients in twelve countries. Health Aff (Millwood) 27, 89–102 (2008).
Yokoyama, K., Fukuhara, S., Fukagawa, M., Akizawa, T. & Kurokawa, K. Results of the survey on practice patterns including MBD management at dialysis facilities: As part of the MBD-5D. J Jpn Soc Dial Ther 44, 557–566 (Japanese) (2011).
Gupta, A., Kallenbach, L. R., Zasuwa, G. & Divine, G. W. Race is a major determinant of secondary hyperparathyroidism in uremic patients. J Am Soc Nephrol 11, 330–334 (2000).
Wheeler, D. C. et al. Effects of cinacalcet on atherosclerotic and nonatherosclerotic cardiovascular events in patients receiving hemodialysis: The EValuation Of cinacalcet HCl therapy to Lower cardiovascular Events (EVOLVE) trial. J Am Heart Assoc 3, e001363 (2014).
Fukagawa, M. et al. Prescription patterns and mineral metabolism abnormalities in the cinacalcet era: Results from the mbd-5d study. Clin J Am Soc Nephrol 7, 1473–1480 (2012).
Ministry of education, culture, sports, science and technology (MEXT) and ministry of health, labour and welfare (MHLW) of Japan. Ethical guidelines for epidemiological research, (2002) Available at: http://www.mhlw.go.jp/stf/seisakunitsuite/bunya/hokabunya/kenkyujigyou/i-kenkyu/dl/02-02.pdf. (Accessed: Nov 17, 2014).
Barlow, W. E., Ichikawa, L., Rosner, D. & Izumi, S. Analysis of case-cohort designs. J Clin Epidemiol 52, 1165–1172 (1999).
Bradbury, B. D. et al. Evolving statistical methods to facilitate evaluation of the causal association between erythropoiesis-stimulating agent dose and mortality in nonexperimental research: Strengths and limitations. Am J Kidney Dis 54, 554–560 (2009).
Hernán, M. Á., Brumback, B. & Robins, J. M. Marginal structural models to estimate the joint causal effect of nonrandomized treatments. J Am Stat Assoc 96, 440–448 (2001).
Robins, J. M., Hernán, M. Á. & Brumback, B. Marginal structural models and causal inference in epidemiology. Epidemiology 11, 550–560 (2000).
Harrell, F. E. In Regression modeling strategies: With applications to linear models, logistic regression and survival analysis. (Springer-Verlag 2001).
Preliminary results of the present study were presented at the 49th Meeting of the European Renal Association-European Dialysis and Transplant Association, May 2012. We would like to thank Joseph Green, DMSc (Graduate School of Medicine, The University of Tokyo) for editorial advice. We would like to thank Ayumi Shintani, PhD, MPH (Osaka University Graduate School of Medicine) for valuable comments on our statistical analyses. The MBD-5D is supported by research grants from Kyowa Hakko Kirin (manufacturer of intravenous calcitriol, cinacalcet hydrochloride and sevelamer hydrochloride), without restrictions on publications.
T.A. has acted as a consultant for Kyowa Hakko Kirin, has received grants (research support) from Kyowa Hakko Kirin and is a member of a speakers’ bureau of Kyowa Hakko Kirin. S. Fukuhara has acted as a scientific advisor for Kyowa Hakko Kirin and has received grants (research support) from Kyowa Hakko Kirin. M.F. has acted as a consultant for Kyowa Hakko Kirin, has received honoraria from Kyowa Hakko Kirin and has received grants (research support) from Kyowa Hakko Kirin. A.E.R. has received research funding from Amgen for other projects unrelated to the MBD-5D; He has also received unrelated research funding from the UNC Center for Pharmacoepidemiology, which receives support from the pharmaceutical industry and from Merck. M.A.B. receives investigator-initiated research funding from the National Institutes of Health (R01 AG042845, R21 HD080214, R01 AG023178) and through contracts with the Agency for Healthcare Research and Quality’s DEcIDE program and the Patient Centered Outcomes Research Institute. He has also received investigator-initiated research support from Amgen and has sat on advisory boards for Amgen, Merck and Pfizer (honoraria received by institution). He has received consulting fees from RxAnte, Inc. and World Health Information Science Consultants, LLC. The other authors report having nothing to disclose.
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Akizawa, T., Kurita, N., Mizobuchi, M. et al. PTH-dependence of the effectiveness of cinacalcet in hemodialysis patients with secondary hyperparathyroidism. Sci Rep 6, 19612 (2016). https://doi.org/10.1038/srep19612
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