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. 2016 Sep 13;10(9-10):E300–E305. doi: 10.5489/cuaj.3655

Metabolic syndrome in patients with prostate cancer undergoing intermittent androgen-deprivation therapy

Mohammadali Mohammadzadeh Rezaei 1, Mohammadhadi Mohammadzadeh Rezaei 1, Alireza Ghoreifi 1,, Behzad Feyzzadeh Kerigh 1
PMCID: PMC5028214  PMID: 27695584

Abstract

Introduction:

The presence of metabolic syndrome in men with prostate cancer (PCa) undergoing androgen-deprivation therapy (ADT), especially intermittent type, has not been completely evaluated. The aim of this study is to evaluate metabolic syndrome in men with PCa undergoing intermittent ADT.

Methods:

In this longitudinal study, we studied the prevalence of metabolic syndrome and its components in 190 patients who were undergoing intermittent ADT. The metabolic syndrome was defined according to the Adult Treatment Panel III criteria. All metabolic parameters, including lipid profile, blood glucose, blood pressures, and waist circumferences of the patients were measured six and 12 months after treatment.

Results:

Mean age of the patients was 67.5 ± 6.74 years. The incidence of metabolic syndrome after six and 12 months was 6.8% and 14.7%, respectively. Analysis of various components of the metabolic syndrome revealed that patients had significantly higher overall prevalence of hyperglycemia, abdominal obesity, and hypertriglyceridemia in their six- and 12-month followups, but blood pressure has not been changed in the same period except for diastolic blood pressure after six months.

Conclusions:

Although there was an increased risk of metabolic syndrome in patients receiving intermittent ADT, it was lower than other studies that treated the same patients with continuous ADT. Also it seems that intermittent ADT has less metabolic complications than continuous ADT and could be used as a safe alternative in patients with advanced and metastatic PCa.

Introduction

Prostate cancer (PCa) is the most common non-cutaneous cancer diagnosed in men and the second most common cause of cancer related death, with a lifetime risk of death at 2.57%.1,2 Statistics suggest that its incidence and the death rate are rapidly increasing, despite improved detection rates. This may be due to rapid increases in the population age and changes in dietary habits.3

Radical prostatectomy and radiotherapy are the preferred treatments in men with confined PCa. However, androgen-deprivation therapy (ADT) is the main treatment of advanced and metastatic PCa. The modalities of ADT include surgery (orchiectomy) or medical therapy.4 Today, with progression in new medical drugs (gonadotropin-releasing hormone [GnRH] agonists and antagonists), most patients choose medical therapy, so the overall use of ADT has increased in the past two decades. Also because of the increasing rate of PCa diagnosis in younger men, hormonal therapy is being used for extended periods of time.5 Different studies showed that most men with PCa die of conditions other than their primary malignancy, so changes in treatment modalities and diagnosis and management of adverse effects have become more important. Therefore, different strategies for ADT, such as intermittent treatment have been described. Intermittent androgen suppression may reduce the side effects of therapy during off-treatment periods.6

The resulting hypogonadism due to ADT may leads to adverse results, such as osteoporosis, unfavourable body composition (increase in body mass index, increased fat mass, reduced lean body mass and muscle strength), sexual dysfunction, and reduced quality of life. Recent studies suggest male hypogonadism is an independent risk factor for the development of metabolic syndrome and diabetes.7 However, the presence of metabolic syndrome in men with PCa undergoing ADT, especially intermittent type, has not been completely evaluated. In this study, we evaluated metabolic syndrome in men with PCa undergoing intermittent ADT.

Methods

In this longitudinal study, we studied the patients who were undergoing intermittent ADT. All patients did not have metabolic syndrome at the start of study. Exclusion criteria were abnormal liver function tests or serum creatinine, history of any medical diseases (such as thyroid disease, hypogonadism, or glucocorticoid use), and any history of chemotherapy. Also, if prostate-specific antigen (PSA) and symptoms did not respond to a full course of ADT, the patient was considered castration-resistant and excluded from the study.

The metabolic syndrome was defined according to the Adult Treatment Panel III criteria. Patients were classified as having metabolic syndrome if three of the following five criteria were present: fasting plasma glucose level more than 110 mg/dL, serum triglyceride level more than 150 mg/dL, serum high-density lipoprotein (HDL) level less than 40 mg/dL, waist circumference more than 102 cm, and blood pressure of more than 130/85 mmHg. Participants on antihypertensive drugs and lipid-lowering medications were classified as positive for the respective criterion.

One hundred ninety patients who were candidates for ADT and responded to six injections of GnRH agonists were enrolled in this study. The patients were categorized into three groups: patients with locally advanced disease who were not suitable for radical prostatectomy; patients with metastatic disease; and patients with recurrent disease following radical prostatectomy or radiotherapy. All patients signed the informed consent. Response was defined as PSA level below 4.0 ng/L. During this induction therapy, all patients received injections of triptorelin 3.75 mg every 28 days plus flutamide 250 mg three times daily for the first two weeks. Serum PSA and testosterone, as well as clinical status, were checked every three months and if PSA rose to 10 ng/L, patients received three more injections to suppress the serum PSA to 4 ng/L or less. All metabolic parameters, including lipid profile, blood glucose, blood pressures, and waist circumferences of the patients were measured six and 12 months after treatment. All data were analyzed using SPSS version 18.0 software and p<0.05 was considered statistically significant.

Results

A total of 190 patients were evaluated in this study. The mean age of the patients was 67.5 ± 6.74 years (min 58 and max 80). Of these 190 patients, 56 patients (29.5%) had locally advanced PCa, 61 (32.1%) had metastatic disease, and 73 (38.4%) had recurrent disease after previous definitive therapy (Fig. 1). Their Gleason scores (GS) were as following: GS 6 in 12 patients (6.3%), GS 7 in 45 patients (23.7%), GS 8 in 48 patients (25.2%), GS 9 in 57 patients (30%) and GS 10 in 28 patients (14.7%) (Fig. 2).

Fig. 1.

Fig. 1.

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Patient categories.

Fig. 2.

Fig. 2.

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Gleason scores (GS) of the prostate cancers.

Analysis of various components of the metabolic syndrome revealed that patients had significantly higher overall prevalence of hyperglycemia, abdominal obesity, and hypertriglyceridemia in their six- and 12-month followups, but blood pressure had not changed in the same period except for diastolic blood pressure after six months (Table 1).

Table 1.

Components of metabolic syndrome in patients

Characteristic First of study After 6 months After 12 months p value
6 months 12 months
Fasting plasma glucose 111.92 ± 13.74 112.78 ± 16.4 114.58 ± 17.66 0.0107 <0.001
Triglyceride 104.92 ± 20.92 110.82 ± 18.58 123.57 ± 17.69 <0.001 <0.001
High-density lipoprotein 47.78 ± 9.54 50.25 ± 8.99 51.09 ± 8.18 <0.001 <0.001
Waist circumference 90.37 ± 13.3 91.04 ± 13.25 91.41 ± 13.67 <0.001 <0.001
Systolic blood pressure 126.35 ± 15.38 127.52 ± 12.80 127.23 ± 12.15 0.098 0.252
Diastolic blood pressure 82.21 ± 9.47 83.18 ± 8.41 81.31 ± 8.07 0.029 0.055
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Fasting plasma glucose of the patients was 111.92 ± 13.74, 112.78 ± 16.4, and 114.58 ± 17.66 mg/dl at the beginning of the study and at six and 12 month post-treatment, respectively. The change was not significantly different in the first six month (p=0.107), but after 12 months it was significantly higher (p<0.001). The mean amounts of triglycerides in patients at the same periods were 104.92 ± 20.92, 110.82 ± 18.58, and 123.57 ± 17.69 mg/dL, respectively, a significant increase after both six and 12 months (p<0.001). Also the mean amount of HDL cholesterol was 47.78 ± 9.54, 50.25 ± 8.99, and 51.09 ± 8.18 mg/dl), again a significant increase at six and 12 months (p<0.001).

The mean waist circumferences of the patients at the start and at six- and 12-month followups was 90.37 ± 13.3, 91.04 ± 13.25, and 91.41 ± 13.67 cm, respectively, a significant increased after six and 12 months (p<0.001).

In the same time periods, the mean systolic blood pressures of the patients were 126.35 ± 15.38, 127.52 ± 2.80, and 127.23 ± 12.15 mmHg, respectively. The changes were not significantly different (p=0.098 and 0.252 after six and 12 months, respectively). Also, the mean diastolic blood pressures of the patients were 82.21 ± 9.47, 83.18 ± 8.41, and 81.31 ± 8.07 mmHG, respectively; while the changes were significantly different after six months (p=0.029), they were not was not after 12 months (p=0.055).

After six months, 13 patients (6.8%) met the criteria of metabolic syndrome. The mean age of patients with metabolic syndrome was not statistically different that that of the other patients (70.92 ± 8.19 vs. 68.35 ± 6.61 years; p=0.185). Also, the incidence of metabolic syndrome after 12 months was 14.7% (28 patients). At this time period, the mean age of patients with metabolic syndrome was significantly higher than that of the other patients (71.21 ± 7.09 vs. 68.06 ± 6.59 years; p=0.022).

Discussion

ADT has been the cornerstone of treatment of advanced and metastatic PCa. It has progressed since 1941, when Huggins et al described the androgen dependence of PCa by showing that castration decreases its growth.8 ADT includes orchidectomy or medical therapy (GnRH agonists or antagonists), but most patients choose the latter.4 GnRH agonists were discovered in 1971 and are now the mainstay of PCa treatment; approximately 600 000 men in the U.S. alone are receiving it.9 The overall use of ADT has increased in the past two decades and most men with PCa die of conditions other than their primary malignancy, such as ADT complications. In order to increase quality of life (QoL), different strategies for ADT, with possibly fewer complications, have been described. This includes intermittent treatment.5,6 Most phase 2 studies have shown that intermittent ADT regimens decrease adverse events and improve QoL during off-therapy periods, with promising tolerability profiles. Also, early phase 3 results show a better tolerability profile and QoL with intermittent ADT than with continuous treatment. Although these early studies demonstrate the potential short-term benefits of intermittent ADT, there are still insufficient data to determine whether it has the potential to prevent or reverse the long-term complications associated with ADT.10

ADT and metabolic syndrome

One of the most challenging side effects of ADT is metabolic syndrome, which may be due to hypogonadism. Few studies have evaluated the metabolic alterations that occur as a result of ADT in men with PCa. Braga-Basaria et al found that more than half of the men receiving long-term (at least 12 months) ADT had metabolic syndrome compared with one-fifth of the men in control groups. They suggest that the high prevalence of metabolic syndrome in the ADT group may be a direct result of profound hypogonadism and independent of any influence of age, race, and disease (PCa).11 In their study, Valverde et al showed that the prevalence of metabolic syndrome in patients on ADT was 51.9% compared to 35.8% in patients without ADT.12 In a cross-section observational study, Munoz Garcia et al stated that prevalence of metabolic syndrome in men on ADT after six months of treatment is 21%, after 12–18 months treatment is 36%, and after 24 months treatment is 24%.13 Finally, in a recent meta-analysis, there was a positive association between ADT and risk of metabolic syndrome (relative risk 1.75).14 In our study, the prevalence of metabolic syndrome in patients treated with intermittent ADT was 6.8% and 14.7% after six and 12 months, respectively. Although there was an increased risk of metabolic syndrome in these patients, this increase was lower than other studies that treated the same patients with continuous ADT. It seems that the risk of metabolic syndrome in intermittent ADT is lower than with continuous treatment.

ADT and diabetes

There are some studies that have evaluated the components of metabolic syndrome in patients treated with ADT. In the meta-analysis mentioned above, diabetes was the only component present in more than three of nine studies, and also showed an increased risk following ADT (relative risk 1.36).14 Keating et al, in an observational study on 37 443 population-based men who were diagnosed with local or regional PCa, showed that treatment with GnRH agonists was associated with statistically significantly increased risk of incident diabetes (adjusted hazard ratio 1.44). They showed 159.4 events of diabetes per 1000 person-years in patients on ADT compared to 87.5 events for no ADT patients.15 In their study, Lage et al showed that the estimated relative risk of incident diabetes associated with the receipt of ADT was 1.36.16 Basaria et al also showed that men on ADT had significantly higher levels of fasting serum glucose compared with men not on ADT. In their study, 44% of ADT patients had glucose levels in the diabetic range and the duration of ADT was directly related to the severity of these metabolic abnormalities.17 Alibhai et al, in an age-matched cohort study, showed that men on ADT who were followed for an average of 6.47 years had an increased risk of diabetes compared with men who did not receive ADT.18 A recent study on Chinese patients who were given ADT showed a higher risk of diabetes mellitus (hazard ratio 4.39).19 In the Barga-Basiria study, hyperglycemia and abdominal obesity were the major determinants of the higher prevalence of metabolic syndrome in this group, leading to the conclusion that hyperinsulinemia in these patients was associated with increase in fat mass.11 On the other hand, some short-term studies have shown different results. Smith et al, in a short-term prospective study of 22 men with PCa undergoing ADT, showed a significant increase in insulin levels after three months of treatment compared with baseline; however, there was no significant change in plasma glucose levels.20 In their study, Dockery et al showed that ADT for three months resulted in a 63% increase in fasting insulin levels without any changes in fasting glucose.21 A study done by Nishiyama et al evaluated 49 men with PCa undergoing ADT for six months showed a mild increase in fasting blood glucose (from 103–106 mg/dl), but the levels remained below the diabetes range.22 In a recent study, Davis et al retrospectively reviewed the charts of 100 consecutive men with intermediate or high-risk localized PCa referred to the British Columbia Cancer Agency for ADT; baseline diabetes or impaired glucose tolerance was 24%, but in study cohort, they had a similar prevalence (odds ratio 0.93; p =0.8).23 According to the various studies mentioned above, the effect of ADT on plasma glucose is different in short- and long-term followup. These studies suggest an increased level of insulin develops within a few months of starting ADT and prevents the development of hyperglycemia. The etiology of this hyperinsulinemia is not clearly defined. There is some evidence that testosterone can modulate hepatic and lipoprotein lipases in visceral adipose tissue, which consequently affects insulin clearance.24 However, it seems that in the long-term, male hypogonadism is associated with a decrease in lean body mass (LBM) and an increase in fat mass, which results in elevated levels of adiponektines, which in turn, are responsible for causing insulin resistance.25 In our study, the change of fasting blood glucose was not significantly different in the first six months, but after 12 months it was significantly higher. Our results showed that in short-term treatment with intermittent ADT there is no difference in fasting blood glucose, which is in agreement with other short-term studies. However, in long-term followup, there is significant hyperglycemia.

ADT and hyperlipidemia

In their study, Davis et al stated that baseline dyslipidemia was present in 51% patients receiving ADT.23 In a study by Bo et al, after three months, ADT group had increased levels of low-density lipoprotein (LDL) compared to the control groups. After 12 months, ADT group had increased levels of waist circumference, total cholesterol, HDL, and LDL compared to the other two groups.26 Dockery et al, in their study, showed that continuous ADT for three months resulted in increased levels of cholesterol and HDL, but no significant change occurred in LDL or triglyceride levels.21 In their study, Eri et al evaluated the impact of the luteinizing hormone-releasing hormone (LHRH) agonist leuprolide on 26 patients with benign prostatic hyperplasia (BPH) and showed that the mean total cholesterol level increased by 10.6%, HDL cholesterol by 8.2%, and triglycerides by 26.9%, but LDL levels were unchanged.27 Smith et al in their study on 26 men treated with leuprolide for 12 months showed the same increase in HDL levels.28 In our study, the mean amount of trigycerides in patients significantly increased after both six and 12 months. Also, the mean amounts of HDL cholesterol and the mean waist circumferences significantly increased after the same periods. Hyperinsulinemia might have been expected to cause a decrease in HDL levels, therefore, some other non-investigated factors may be involved in the complex relationship between androgens and metabolic factors. Maybe an increase in adiponektin levels due to an increase in fat mass in these patients contributed to high levels of cholesterol (especially HDL).

ADT and hypertension

The role of androgens in cardiovascular disease (CVD) in men has long been debated. Previous studies mainly evaluated the relationship between ADT and CVD, but few of them focused on the changes in blood pressure and arterial compliance. Some epidemiologic studies have shown that low testosterone levels in men are independently associated with hypertension. A recent study in patients with PCa undergoing short-term ADT showed a significant decrease in systemic arterial compliance.21 On the other hand, Smith et al showed no significant change in blood pressure after 12 months treatment with leuprolide.28 Davis et al showed that hypertension was more prevalent in ADT patients than in an age- and sex-matched population sample (odds ratio 1.74; p=0.006).23

Previous studies have shown that approximately half of men with PCa die of non-cancer-related causes, and the most common etiology is CVD.11 Keating et al showed an association between ADT and CVD (adjusted hazard ratio 1.16), myocardial infarction (hazard ratio 1.11), and sudden cardiac death or life-threatening ventricular arrhythmia (hazard ratio 1.16).29 Another study by Tsai et al also showed that men receiving ADT were 2.6 times more likely to die of CV events than non-ADT controls. They found that men who received ADT had a 20% higher risk of serious CV morbidity than similar men who did not.30 Although these studies showed a relationship between ADT and increased risk of CVD, some other studies have not confirmed this association. Alibhai et al, in a cohort study of nearly 20 000 ADT users who were observed for a mean of 6.47 years, showed an increased risk of diabetes, but there was no such association with incidence of acute myocardial infarction.18 An analysis from the Radiation Therapy Oncology Group showed similar results. The study found that long-term ADT does not increase CV mortality in men with locally advanced PCa.31 A recent, large study assessing the impact of ADT on CVD mortality in men undergoing curative-intent external beam radiation therapy confirmed these findings. Among these men, the cumulative CV mortality at seven years was 2.6% for men not undergoing ADT, 2.1% for men with six months ADT, and 1.4% for men undergoing ADT for six months.32 Punnen et al also analyzed a total of 7248 men to assess the relationship between ADT and CV mortality and found that there was no significant difference in CV mortality among men who did vs. those who did not receive ADT.33

Although the relationship between ADT and CVD is controversial, many authors have shown that the profound hypogonadism in patients undergoing ADT may be responsible for high CV mortality. Low testosterone levels are a risk factor for metabolic syndrome and metabolic syndrome is also a known cause of increased CV mortality. Men with metabolic syndrome are three times more likely to die of coronary heart disease and other CVD.11 Still, some have voiced concerned that unmeasured factors maybe confounding the relationship between ADT use and CV mortality.33 In our study, the changes in mean systolic blood pressures of the patients were not significantly different after six and 12 months. On the other hand, the changes in mean diastolic blood pressures of the patients were significantly different after six months, but not after 12 months. According to CV changes, it would appear intermittent ADT is safer than continuous ADT. Long-term studies are needed to document the effect of intermittent ADT on morbidity and mortality due to CVD.

To our knowledge, this study is the first study that evaluates the metabolic syndrome in patients receiving intermittent type of ADT. The major limitation of our study is that it was an observational study, so we recommend a long-term, prospective study with a larger sample size.

Conclusion

Our study showed that although there was an increased risk of metabolic syndrome in patients receiving intermittent ADT, this increase was lower than other studies that treated the same patients with continuous ADT. We concluded that the risk of metabolic syndrome in intermittent ADT is lower than that with continuous treatment. Further, patients on ADT had significantly higher overall prevalence of hyperglycemia, abdominal obesity, and hypertriglyceridemia, but blood pressure did not change in the 12-month follow up (except for diastolic blood pressure after six months). We therefore further concluded that intermittent ADT has less metabolic complications than continuous ADT and could be used as a safe alternative in patients with advanced and metastatic PCa.

Footnotes

Competing interests: The authors report no competing personal or financial interests.

This paper has been peer-reviewed.

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