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Original Research

GLP-1 mediates the modulating effect of thymoquinone on feeding behaviors in diabetic rats

Shu Ping Lee1 Department of Food Science, College of Agriculture, National Pingtung University of Science and Technology, Pingtung 91201, Taiwan
,
Feng Yu Kuo1 Department of Food Science, College of Agriculture, National Pingtung University of Science and Technology, Pingtung 91201, Taiwan;2 Cardiovascular Center, Veterans General Hospital, Kaohsiung City 81362, Taiwan
,
Juei-Tang Cheng3 Department of Medical Research, Chi-Mei Medical Center, Tainan City 71003, Taiwan;4 Institute of Medical Science, College of Health Science, Chang Jung Christian University, Tainan City 71101, TaiwanCorrespondence[email protected]
&
Ming Chang Wu1 Department of Food Science, College of Agriculture, National Pingtung University of Science and Technology, Pingtung 91201, TaiwanCorrespondence[email protected]
Pages 873-881 | Published online: 12 Jun 2019

Abstract

Background:

Thymoquinone (TQ) is a safe nutrient isolated from the seeds or volatile oil extract of Nigella sativa. In addition to its benefits in glucose regulation, TQ improves feeding disorders in diabetic animals. Glucagon-like peptide-1 (GLP-1) analogs improve glycemic control and ameliorate obesity or hyperphagia. Therefore, the present study aimed to investigate the role of GLP-1 in TQ-induced anorexia.

Method:

Type 2 diabetes was induced in rats by nicotinamide and streptozotocin injection. TQ was orally administered to diabetic rats at different doses for 45 days. Following TQ treatment, changes in serum glucose levels, GLP-1 concentration, body weight, food intake, and water intake were determined. To further explore the interaction between GLP-1 and TQ, the inhibitor of dipeptidyl peptidase 4, sitagliptin and the GLP-1 receptor antagonist exendin 9–39 (Ex 9–39) were separately administered to TQ- or vehicle-treated diabetic rats.

Results:

TQ treatment attenuated hyperglycemia and reduced hyperphagy and water intake in streptozotocin-induced diabetic rats in a dose-dependent manner. Moreover, TQ treatment elevated plasma GLP-1 levels compared to those in control rats. The effects of TQ were enhanced by treatment with sitagliptin and reduced by the injection of Ex 9–39 into the brain. In contrast, similar treatment with another antioxidant (either ascorbic acid or N-acetylcysteine) produced the same anorexic effect as TQ without changing the plasma GLP-1 levels in diabetic rats. Therefore, TQ attenuated hyperphagy while increasing plasma GLP-1 levels and had antioxidant-like effects.

Conclusion:

TQ increased endogenous GLP-1 levels to reduce hyperphagy in diabetic rats.

Introduction

Thymoquinone (2-isopropyl-5-methyl-1,4-benzoquinone, TQ) is a widely used ingredient isolated from the seeds and volatile oil extract of black cumin (Nigella sativa).Citation1 TQ is recognized as a safe nutrient, particularly when given orally to experimental animals.Citation2 TQ elicits many effects,Citation3 including immunomodulatory, anticancer, antidiabetic, antioxidant, anti-infertility, and anti-inflammatory activities and protects the liver, heart, and nervous system.

TQ exerts ameliorative and therapeutic effects on diabetic animal models,Citation4,Citation5 which could reduce hepatic glucose production.Citation6 In the clinic, the hypoglycemic and hypolipidemic effects of black cumin in patients suffering from diabetes and metabolic syndrome have been reported.Citation3 Additionally, TQ did not cause adverse effects on renal or hepatic function in diabetic patients.Citation7 Therefore, TQ has been recommended as a food adjunct for diabetes.Citation8 Interestingly, food intake was also reduced in diabetic animals following TQ administration.Citation9 However, no report has examined the mechanism(s) of the TQ-induced improvement of eating disorders in patients with diabetes.

Glucagon-like peptide-1 (GLP-1) is a gut hormone derived from the preproglucagon gene that is synthesized and released by intestinal L cells.Citation10 GLP-1 and GLP-1 receptor expression was decreased with chronic hyperglycemia.Citation11 Clinical study showed that GLP-1 exhibited a statistically significant decrease in type 2 diabetic compared with control subjects.Citation12 The intraperitoneal (IP) injection of GLP-1 decreased food intake in rodents.Citation13,Citation14 This finding is consistent with clinical reports that diabetic patients treated with GLP-1 or its stable receptor agonist progressively lose weight.Citation15 Additionally, activation of the GLP-1 receptor (GLP-1R) in the central nervous system (CNS) was implicated in the regulation of food intake,Citation16 mainly in the hypothalamic arcuateCitation16 and paraventricular and supraoptic nuclei.Citation17 The central administration of GLP-1-(7-36) amide inhibited food and water intake in rat.Citation18

Changes in food and water intake due to GLP-1 modulation are similar to the effects of TQ. However, whether the effects of TQ on feeding behaviors in diabetic rats are mediated by GLP-1 is unknown. Therefore, the present study aimed to clarify these effects using type 2-like diabetic rats. First, we established a new model of type 2-like diabetes as described previouslyCitation30 using the same doses of inducing agents except the change in fasting time. Then, three protocols were performed in the present study. The first experimental design aimed to confirm the effectiveness of TQ as a previous reportCitation31 in the new model. Therefore, we used the same treatment period of 45 days. Otherwise, similar to a previous reportCitation18, the results were effectively obtained in TQ-treated animals within 4 weeks, which was applied to the second experimental design. Finally, the role of the antioxidant-like effect was investigated in the third experimental design. Two antioxidants were used to treat for 45 days as that in the first experimental design. Changes in GLP-1 were then compared to clarify the role of antioxidant in the present study.

Materials and methods

TQ (purity >98%) and exendin 9–39 (Ex 9–39) were obtained from Sigma Aldrich Chemical Co. (St. Louis, MO, USA). Sitagliptin phosphate (Merck, Cramlington, Northumberland, UK), which inhibits dipeptidyl peptidase-4 (DPP-4) (Sigma Aldrich), was dissolved in normal saline.

Animals

Male Sprague-Dawley (SD) rats (a total of 120) weighing 250 to 280 g were obtained from the National Laboratory Animal Center (Taipei, Taiwan). in the animals used for all experiments were maintained under anesthesia with 2% isoflurane to minimize suffering. The experimental protocols were approved by the Institutional Animal Ethics Committee (105,051,901) of the Chi-Mei Medical Center. All experiments conformed to the Guide for the Care and Use of Laboratory Animals as well as the guidelines of the Animal Welfare Act. No mortality was observed in the experimental rats in the present study.

The generation of diabetic rats

To induce type 2-like diabetes, as described previously,Citation19 rats were given an intravenous injection of streptozotocin (STZ, Sigma-Aldrich) at 65 mg/kg (dissolved in 5 mmol/l citrate buffer, pH 4.5) 15 mins after the IP injection of 230-mg/kg nicotinamide (NA, Sigma-Aldrich) dissolved in normal saline. Prior to induction, the rats were fasted for various times, as shown in the “Results“ section. Then, the rats were given 5% dextrose instead of water on the first day of induction to avoid hypoglycemia. Fasting blood glucose levels were examined after 7 days. The rats were considered to be diabetic once they exhibited a plasma glucose level of no less than 200 mg/dL, along with polyuria and other diabetic features.

Experimental protocols

Experimental design-1

The rats were randomly divided into five groups as follows (n=6): group 1: normal control, group 2: diabetic control, group 3: diabetic rats receiving TQ 25 mg/kg, group 4: diabetic rats receiving TQ 50 mg/kg, and group 5: diabetic rats receiving TQ 100 mg/kg. Rats in the normal control group and the diabetic control group were given an equal volume of normal saline. The administration of drugs or vehicle was carried out once daily for 45 days as described previouslyCitation31 by oral gavage for the rats in all groups. The initial and final body weights of the rats in each group were recorded. Additionally, changes in daily food and water intake were measured at the end of the experiment.

Experimental design-2

In this section, the role of GLP-1 in mediating the effects of TQ was investigated. Rats were randomly assigned to 7 groups as follows (n=6): group I: normal control rats, group II: diabetic control rats (vehicle treated), group III: diabetic rats that received the oral administration of TQ (50 mg/kg/day), group IV: diabetic rats that received the oral administration of TQ (50 mg/kg/day) and the ICV injection of Ex 9–39 (50 µg in 2 µL), group V: diabetic rats that received the oral administration of vehicle and the ICV injection of Ex 9–39 (50 µg in 2 µL), group VI: diabetic rats that received the oral administration of TQ (50 mg/kg/day) and sitagliptin (5 mg/kg/day), and group VII: diabetic rats that received the oral administration of vehicle and sitagliptin (5 mg/kg/day).

The TQ treatment course in each group lasted 4 weeks.Citation20 The rats in group III received the ICV injection of Ex 9–39 to block GLP-1 receptors in the brainCitation21 30 mins before TQ administration during the final week of treatment. The rats in group VI were orally treated with 5 mg/kg/day sitagliptin to inhibit the GLP-1 metabolic enzyme (DPP-4)Citation22 1 hr before the oral administration of TQ daily for the last 2 weeks of treatment. The initial and final body weights of the rats in each group were recorded. Similarly, the daily food and water intake were measured before the end of the experiment.

Intracerebroventricular (ICV) injection

To understand the interaction between TQ consumption and GLP-1 receptor signaling in the CNS, the ICV infusion of Ex 9–39 was performed to block CNS GLP-1 activity.Citation23 The rats were anesthetized with a mixture of isoflurane in oxygen (2%) and placed in a Kopf stereotaxic instrument equipped with blunt ear bars. The stereotactic coordinates were 2.2 mm posterior to the bregma at a 7.5-mm depth from the dura mater and in the midline following the guide.Citation24 The recovery period was at least 1 week; only rats that had regained more than 90% of their presurgery body weight were used in subsequent experiments.

The infusion cannula (22-gauge) attached to PE-10 tubing was inserted into the guide cannula and extended 0.5 mm beyond the guide. A 10.0 μL Hamilton syringe was used to manually deliver saline or the tested agent over a 2-min period following our previous method.Citation25 The infusion cannula was kept in place for an additional 1 min following infusion.

Collection of blood and the estimation of biochemical parameters

Blood samples (200 μL) from fasting rats were collected from the tail vein under isoflurane anesthesiaCitation23 at the end of the feeding protocol. Then, the plasma was immediately separated by centrifuging at 13,000 rpm for 10 mins at 4°C. All samples were stored at −80°C until their analysis. The glucose levels were evaluated using a reagent from a glucose kit (Biosystems SA, Barcelona, Spain). Plasma insulin levels were determined using a rat insulin ELISA kit (Mercodia, Uppsala, Sweden). Insulin resistance was calculated using the homeostasis model assessment (HOMA-IR) method. HOMA-IR was then calculated as fasting glucose (mmol/L) × fasting insulin (μU/mL)/22.5.Citation26 The GLP-1 levels were estimated using a commercial ELISA kit (Millipore).

Measurement of body weight and food and water intake

At the beginning and end of the study, the rats in each group were weighed using an electronic balance. Food intake and water intake were measured daily. Food intake was determined by measuring the difference between the preweighed food and the weight of the remaining food in the hopper and spilled food after 24 hrs. Water intake was measured by recording the quantity of water remaining in the feeding bottle.

Administration of antioxidants to examine their effects on feeding behaviors in diabetic rats

In an attempt to exclude the effects of antioxidants on the amelioration of diabetic like phenotypes, we administered two antioxidants, ascorbic acid (vitamin C)Citation27 and N-acetylcysteine (NAC),Citation28 to diabetic rats. The diabetic rats received ascorbic acid (1 g/kg)Citation29 or NAC (0.5 g/kg) orally every day for 45 days, which was similar to the TQ treatment period. Then, feeding behaviors and plasma glucose or GLP-1 levels were determined as described above.

Statistical analysis

The results are indicated as the means ± SDs of the indicated sample number (n) in each group. To investigate the effect of fasting time on glucose levels and insulin levels during induction of diabetes in rats and the changes in the body weight before and after TQ treatment with different dosage for 45 days, we conducted a two-way ANOVA, followed by Tukey’s post hoc comparison. The rest of the results were compared using one-way ANOVA with Tukey’s post-hoc test. The statistical analysis software SPSS 21 was used. A P-value of 0.05 indicated significance.

Results

Effect of fasting time on the blood sugar response in diabetic rats

In the present study, we compared the plasma glucose levels of diabetic rats that had fasted for various times. Hyperglycemia was more marked in diabetic rats with short fasting times than in diabetic rats with long fasting times (). Similarly, the insulin concentration was also significantly different after 8–10 hrs of fasting (). Therefore, diabetic rats that had fasted approximately 8–10 hrs were used as the model in the present study.

Figure 1 Effect of fasting time on glucose levels and insulin levels during the induction of diabetes in rats. After starvation for different time durations, the rats received an intraperitoneal injection of nicotinamide (230 mg/kg) 15 mins before the intravenous administration of STZ (65 mg/kg) (black column, Nicotinamide + STZ [NICO+STZ]). (A) Plasma glucose levels. (B) Plasma insulin levels. Values are expressed as means ± SDs (n=6). *P<0.05 compared with the control group (white column). #P<0.05 compared with the vehicle-treated diabetic group.

Abbreviations: STZ, streptozocin; Con, control.
Figure 1 Effect of fasting time on glucose levels and insulin levels during the induction of diabetes in rats. After starvation for different time durations, the rats received an intraperitoneal injection of nicotinamide (230 mg/kg) 15 mins before the intravenous administration of STZ (65 mg/kg) (black column, Nicotinamide + STZ [NICO+STZ]). (A) Plasma glucose levels. (B) Plasma insulin levels. Values are expressed as means ± SDs (n=6). *P<0.05 compared with the control group (white column). #P<0.05 compared with the vehicle-treated diabetic group.

Effects of TQ on feeding behaviors and body weights of diabetic rats

The increased plasma glucose levels in diabetic rats were reversed by TQ treatment in a dose-dependent manner (). In the diabetic group, insulin sensitivity was markedly reduced, as revealed by increased HOMA-IR. TQ treatment decreased the HOMA-IR score compared with vehicle group (). The body weights at the beginning were similar in all groups. The body weights of diabetic rats in the control group were markedly reduced during the study period compared to those of rats in the normal control group. However, TQ treatment did not affect the body weights of diabetic rats (). Moreover, food and water intake were markedly increased in the diabetic rats compared to those in the normal control group. TQ decreased food () and water intake () in STZ-induced diabetic rats in a dose-dependent manner.

Figure 2 Chronic effects of thymoquinone (TQ) in normal and diabetic rats. (A) Plasma glucose levels in normal (white column) and diabetic (black column) rats. (B) Changes in HOMA-IR before (white column) and after (black column) treatment with different doses of TQ for 45 days. (C) Changes in body weight before (white column) and after (black column) treatment with different doses of TQ for 45 days. (D) Changes in food intake in normal (white column) and diabetic (black column) rats. (E) Changes in water intake in normal (white column) and diabetic (black column) rats. Values are expressed as means ± SDs (n=6). *P<0.05 compared with the control group. #P<0.05 compared with the vehicle-treated diabetic group.

Abbreviation: HOMA-IR, homeostatic model assessment of insulin resistance.
Figure 2 Chronic effects of thymoquinone (TQ) in normal and diabetic rats. (A) Plasma glucose levels in normal (white column) and diabetic (black column) rats. (B) Changes in HOMA-IR before (white column) and after (black column) treatment with different doses of TQ for 45 days. (C) Changes in body weight before (white column) and after (black column) treatment with different doses of TQ for 45 days. (D) Changes in food intake in normal (white column) and diabetic (black column) rats. (E) Changes in water intake in normal (white column) and diabetic (black column) rats. Values are expressed as means ± SDs (n=6). *P<0.05 compared with the control group. #P<0.05 compared with the vehicle-treated diabetic group.

Mediation of GLP-1 in TQ-induced hypophagia in diabetic rats

The ability of TQ to lower blood glucose levels was attenuated by the administration of Ex 9–39 in diabetic rats (P<0.05; ). Additionally, the pretreatment of diabetic rats with Ex 9–39 reduced the TQ-induced increase in plasma GLP-1 levels (P<0.05; ). The sitagliptin+TQ group showed a greater decrease in blood glucose and a marked increase in plasma GLP-1 levels compared to those in the TQ- or sitagliptin-treated groups ( and ). In addition, TQ ameliorated polydipsia and polyphagia in diabetic rats; these effects were inhibited by Ex 9–39 treatment. In the presence of sitagliptin,Citation22 the effects of TQ on food intake and water intake were increased ( and ). In particular, the blood glucose level, GLP-1 concentration, food intake, and water intake of diabetic rats administered Ex 9–39 were no different than those of rats in the vehicle-treated group.

Figure 3 The chronic effects of thymoquinone (TQ) were modified by Ex 9–39 (GLP-1 receptor antagonist) or sitagliptin (DPP-4 inhibitor) treatment. Diabetic rats were orally administered TQ (50 mg/kg/day). (A) Plasma glucose levels. (B) Plasma GLP-1 levels. (C) Food and (D) water intake in diabetic rats (black column). Values are expressed as the mean ± SD (n=6). *P<0.05 compared with the control group (white column). #P<0.05 compared with the vehicle-treated diabetic group.

Abbreviations: GLP-1, glucagon-like peptide-1; DPP-4, dipeptidyl peptidase-4.
Figure 3 The chronic effects of thymoquinone (TQ) were modified by Ex 9–39 (GLP-1 receptor antagonist) or sitagliptin (DPP-4 inhibitor) treatment. Diabetic rats were orally administered TQ (50 mg/kg/day). (A) Plasma glucose levels. (B) Plasma GLP-1 levels. (C) Food and (D) water intake in diabetic rats (black column). Values are expressed as the mean ± SD (n=6). *P<0.05 compared with the control group (white column). #P<0.05 compared with the vehicle-treated diabetic group.

Effects of antioxidants on feeding disorders in diabetic rats

TQ exerts antioxidant-like effects.Citation20 Similar to the effects of TQ, hyperglycemia was attenuated in diabetic rats that received NAC or ascorbic acid (). However, plasma GLP-1 levels were not modified by NAC or ascorbic acid (). Furthermore, changes in food intake () and water intake () were increased after the administration of these antioxidants in diabetic rats. Therefore, the role of endogenous GLP-1 in antioxidant-induced anorexic effects appears unlikely.

Figure 4 Effects of antioxidant treatment in rats. The diabetic rats (black column) received ascorbic acid (1 g/kg) or NAC (0.5 g/kg) orally every day for 45 days. (A) Plasma glucose levels. (B) Plasma GLP-1 levels. (C) Food and (D) water intake of the rats. Values are expressed as mean ± SD (n=6). *P<0.05 compared with the control group (white column). #P<0.05 compared with the vehicle-treated diabetic group.

Abbreviation: NAC, N-acetylcysteine.
Figure 4 Effects of antioxidant treatment in rats. The diabetic rats (black column) received ascorbic acid (1 g/kg) or NAC (0.5 g/kg) orally every day for 45 days. (A) Plasma glucose levels. (B) Plasma GLP-1 levels. (C) Food and (D) water intake of the rats. Values are expressed as mean ± SD (n=6). *P<0.05 compared with the control group (white column). #P<0.05 compared with the vehicle-treated diabetic group.

Discussion

TQ is the active principal ingredient in black cumin and has been recommended as a food adjunct for the management of diabetes.Citation8 The present study found that TQ ameliorated feeding disorders in diabetic rats through endogenous GLP-1 activity.

Regarding the T2DM, many animal models have been developed and the model induced by nicotinamide with streptozotocin (NA-STZ) has widely been used.Citation30Citation32 NA-STZ rats are induced easily and quickly with a marked change in insulin, while hyperglycemia and hypoinsulinemia disorders meet the criteria for T2DM.Citation33,Citation34 But, the original NA-STZ model showed a hyperglycemia less than 198 mg/dL in rats.Citation30 Therefore, researcher(s) changed the dose of NA or STZ during the induction of model for a higher plasma glucose in animals.Citation35 In the present study, we demonstrated an alternative method without the change in NA or STZ dose as original report.Citation30 To compare the effects of fasting period, we arranged for the rats to undergo fasting for various time periods during the induction of diabetes using the NA- or STZ-induced diabetic model,Citation30,Citation36 which was generated exactly as described in the original report.Citation30 Fasting is usually used to minimize competition between STZ and glucose for low-affinity glucose transporter 2 on β cells.Citation37 The starvation period may also potentiate NA to protect β-cells against the cytotoxicity of STZ.Citation35 Our results indicated that a short fasting time elevated the plasma glucose level in NA-STZ rats, reaching a level (>260 mg/dl) near that of the model induced by low doses of STZ alone.Citation19 Therefore, we used this model in the present study. However, the degree of IR was not conducted, although the changes in HOMA-IR were significant. HOMA-IR is widely applied in clinical practice, but it remains questionable in animal research.Citation19 Therefore, the degree of IR in this model should be investigated in the future.

Chronic treatment with TQ attenuated hyperglycemia and ameliorated feeding disorders in a dose-dependent manner in NA-STZ rats. It confirmed the results of a previous reportCitation38 involving the 45-day oral intake. Additionally, it was also similar to a previous report.Citation39,Citation40 Rats in the diabetic group showed a significant increase in HOMA-IR,Citation38 and treatment with TQ in NA-STZ diabetic rats decreased the HOMA-IR. However, the decreased body weights observed in diabetic rats were not reversed by TQ. Diabetes is traditionally diagnosed by a severe loss in body weight, which appears primarily due to the unavailability of carbohydrates as an energy sourceCitation41 or the resultant dehydration of the plasma fluid compartment.Citation42 Recent research has indicated that TQ improved islet revascularization and alleviated metabolic and hepatorenal disturbances in STZ-induced diabetic rats.Citation43 In addition, TQ treatment also had a beneficial effect on glucose tolerance and insulin sensitivity in a diet-induced obesity mouse model of type 2 diabetes.Citation5

Ex 9–39 specifically blocks the GLP-1 receptor (GLP-1R), and it may inhibit the function of GLP-1 in the hypothalamus.Citation44 The direct injection of Ex 9–39 into the brain changed eating behaviors in satiated rats.Citation45 The injection of Ex 9–39 blocks the cerebral GLP-1RCitation23 and was used to investigate the effects of TQ. After diabetic rats were administered Ex 9–39, the positive effects of TQ on both food intake and water intake were markedly reduced. Moreover, the effects of TQ on feeding disorders were enhanced in diabetic rats that received sitagliptin to inhibit DPP-4, a GLP-1-inactivating enzyme.Citation46 The effective dose of sitagliptin administered was in accordance with previous reports.Citation22,Citation47 Additionally, the plasma GLP-1 level was markedly increased in diabetic rats that received sitagliptin compared to that in control rats. Therefore, the effects of TQ were mediated via endogenous GLP-1.

It was recently demonstrated that TQ exerts antioxidant-like effects.Citation24 The antioxidant effect of TQ in cells might interact with the mitochondrial respiratory chain.Citation48 TQ prevented diabetic induced cardiomyopathy via decrease of the cardiac malondialdehyde levels and significantly increased cardiac total superoxide dismutase.Citation49 To determine the role of these potential antioxidant effects in the anorexic response to TQ, we compared the effects of two antioxidants in diabetic rats. Consistent with previous reports, the effects of the established antioxidants ascorbic acidCitation27 and NACCitation28 were compared. Consistent with a previous report,Citation43 the two antioxidants attenuated hyperglycemia and improved hyperphagia and water intake behaviors in diabetic rats. These effects were the same as those of TQ, with the exception that plasma GLP-1 levels were not influenced by NAC or ascorbic acid treatment. Antioxidants may ameliorate glucose homeostasis to improve disorders in diabetic rats.Citation50 Therefore, the mediation of the anorexic effects of TQ treatment via endogenous GLP-1 is not entirely due to its antioxidant-like effects. Taken together, our results suggest that GLP-1 is released by TQ in the peripheral tissues and that it may reach the feeding center of the brain. The finding that the central administration of exogenous GLP-1 induced a marked reduction in food and water intake is consistent with previous findings in rats.Citation18 Therefore, TQ likely ameliorates feeding disorders via endogenous GLP-1, at least in part.

Conclusion

In summary, we demonstrate that TQ treatment increased endogenous GLP-1 levels to ameliorate commonly observed feeding disorders in type 2-like diabetic rats. TQ is suitable for further development for the clinical treatment of obesity.

Author contributions

All authors contributed to data analysis, drafting or revising the article, gave final approval of the version to be published, and agreed to be accountable for all aspects of the work.

Acknowledgments

We thank Dr. Y Li and YC Chen for their helpful assistance in the preparation of the manuscript and collection of references and in the assistance of experiments, respectively. The present study was supported by a grant from the Chi-Mei Medical Foundation (CMFHT10503), Tainan City, Taiwan.

Disclosure

The authors report no conflicts of interest in this work.

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