About the Authors:
Xiao Zou
Affiliation: Department 1 of the Geriatric Cardiology, Chinese PLA General Hospital, Beijing, P.R. China
Haijun Wang
Affiliation: Department 1 of the Geriatric Cardiology, Chinese PLA General Hospital, Beijing, P.R. China
Lili Cai
Affiliation: Clinical Laboratory of Nanlou, Chinese PLA General Hospital, Beijing, P.R. China
Kailiang Li
Affiliation: Department 1 of the Geriatric Cardiology, Chinese PLA General Hospital, Beijing, P.R. China
Wei Zhang
Affiliation: Department 1 of the Geriatric Cardiology, Chinese PLA General Hospital, Beijing, P.R. China
Yu Ding
Affiliation: Department 1 of the Geriatric Cardiology, Chinese PLA General Hospital, Beijing, P.R. China
Quanjin Si
* E-mail: [email protected]
Affiliation: Department 1 of the Geriatric Cardiology, Chinese PLA General Hospital, Beijing, P.R. China
Introduction
Atherosclerosis is the pathological basis of coronary heart diseases [1], [2]. Rupture and its subsequent thrombosis of the vulnerable atherosclerotic plaque are responsible for the majority of acute coronary events [3]. It is clear that hyperlipidemia could cause atherosclerotic plaque formation and rupture. However, level of some patients' low density lipoprotein cholesterol (LDL-C) has been not elevated or even lower when experiencing acute coronary syndrome (ACS), and those patients were previously diagnosed dyslipidemia. Currently, it is unknown whether the fluctuation of LDL-C level is one of the factors promoting the progression and vulnerability of atherosclerotic plaques. We performed the experiment to find out the effects of lipid smoothness on the progression and vulnerability of atherosclerotic plaques in rabbits.
Materials and Methods
1 Experimental design
This study was carried out in strict accordance with the recommendations in the Guide for the Care and Use of Laboratory Animals of the National Institutes of Health. The protocol was approved by the Committee on the Ethics of Animal Experiments of the University of PLA General Hospital (Permit Number: SCXK [Beijing] 2007–0003). All surgery was performed under sodium pentobarbital anesthesia, and all efforts were made to minimize suffering.
24 male New Zealand White rabbits (2.0–2.5 kg, 12 weeks old) were randomized into three groups. Group 1 was the control group including 6 rabbits, group 2 and 3 were the study groups including 9 rabbits in each. Group 1 was given standard chow diet; group 2 was provided with cholesterol-rich diet containing 1% cholesterol and 3% lard oil during the whole study; for group 3, subjects were planned to take cholesterol-rich diet at the first phase for 12 weeks and during the second phase, low-fat (cholesterol-free diet in granular form) [4] and cholesterol-rich diet was then applied alternately every three weeks till the end of the experiment. Rabbits of group 3 were fed with cholesterol-rich diet in the last three weeks. Each rabbit was raised in a 12h light/dark cycle and temperature-controlled cage seprately, and was given 120gram-designed diet per day, with free access to water. The total experiment lasted 24 weeks.
2 Analysis of the serum lipoprotein profile
Blood samples were collected via auricular vein after a period of overnight fasting at week 0, 12th, 15th, 18th, 21th and 24th week. Samples were centrifuged (4000 rpm, 15 minutes, 4°C) to obtain blood serum and then stored in a refrigerator(−80°C). Serum total cholesterol (TC), triglyceride (TG), high-density lipoprotein cholesterol (HDL-C) levels and LDL-C levels were measured by immunoturbidimetry with Roche reagent in PLA General Hospital Clinical Laboratory. Lipoprotein smoothness index (SI) was adopted to evaluate lipoprotein fluctuation calculated as ( and s represented the mean value and standard deviation of lipoprotein profiles from 12th to 24th week respectively). With the SI value lifted, the stability of the lipoprotein level increases.
3 Measurement of serum high-sensitivity C-reactive protein (hs-CRP), interleukin-18(IL-18), endothelin-1(ET-1), oxidized low density lipoprotein (OX-LDL) and nitric oxide (NO)
The serum hs-CRP, IL-18, ET-1, OX-LDL and NO levels were measured with rabbit ELISA kits (Santa Cruz Biotechnology, Inc) as previously described in literature [5]–[7].
4 Ultrasonography of the abdominal aorta
The abdominal aorta was detected by ultrasound with 8–14MHz transducer (Siemens, SEQUOIA512 type ultrasonic instrument) in 0 week, 12th week and 24th week.
5 Pathology analysis
All rabbits were sacrificed, and their aortic trees were isolated and dissected carefully. Both the quantity of gross lesions and the histological changes were analyzed.
For the histological analysis, tissues were stained with Oil Red O and analyzed after fully fixed in 10% formalin as previously described in study [8]. The positively stained areas with Oil Red O were quantified with the Image Pro-PlusV2.0 image analysis software program. Aortic arches were cut into 10 sections, as described [9], for histological analysis. All of the sections were embedded in paraffin and cut into 5 µm-thick serial cross-sectional slices. The gross atherosclerotic lesions were evaluated as previously described in paper [9]. All the aortic sections were stained with hematoxylin-eosin (H&E) for microscopic quantification of the lesion areas. The H&E staining slices were observed with microscope to study the ultrastructure of the atherosclerotic plaque in different groups.
Serial paraffin sections of the thoracic aorta were immunohistochemically stained with antibodies against MMP-9 (matrix metalloproteinase-9) and LOX-1 (lectin-like oxidized low density lipoprotein receptor-1). For the preparations, the sections were washed 3 times with PBS for 5 minutes per wash. Endogenous peroxidases were blocked by incubation for 10 minutes in 0.3% hydrogen peroxide. The sections were washed 3 times with PBS for 5 minutes each. To reduce the background staining, the sections were then incubated in 10% normal goat serum for 60 minutes. The sections were incubated in the primary antibody at 4°C over night, and they were then washed 3 times for 5 minutes with PBS. The secondary antibody (antimurine IgG, Beijing Zhong Shan Biotechnology CO., China) was applied to the sections for 60 minutes. The sections were washed 3 times with PBS for 10 minutes each and were detected with an AEC kit (AEC kit, Beijing Zhong Shan Biotechnology CO., China).
All of the sections (H&E and immunostained) that were used for microscopic quantification were captured under a Motic Olympus BX60 digital camera-applied (Motic Moticcam 2306, Canada) light microscope and were measured using the image pro-plusV2.0 analysis software program (Media Cybernetics Inc., USA). Measurements of plaque thickness and fibrous cap thickness were performed with a length-measurement computer system in which pixels were transformed to micrometers based on a scale set for each image (the image pro-plusV2.0 analysis software) [10].
6 Statistical analysis
All data were performed as the mean [SD] unless indicated. Data from each two groups were compared by Student's t-test, while three groups were compared by one-way ANOVA. The enumeration data were expressed as frequency and compared with chi-square test. Statistical significance was defined as P<0.05. Statistical analysis was performed using the statistical software SPSS ver. 13.0.
Results
1 The general conditions of animals after 24 weeks
At the end of the experiment, one rabbit of group 1 died for unclear reason, one in group 2 and two in group 3 died due to diarrhea. 20 rabbits survived at the end of the experiment. The animals' body weights in all three groups increased, and the animals at 24th week were significantly heavier than 12th week. But there was no statistical significance between groups, see Table 1.
[Figure omitted. See PDF.]
Table 1. Body weight in the three groups (mean [SD]).
https://doi.org/10.1371/journal.pone.0093686.t001
2 Serum lipids profile
Rabbits in group 2 and group 3 all presented severe hypercholesterolemia (Figure 1). Serum HDL-C level decreased dramatically in cholesterol-rich diet fed groups as shown in Figure 1, while TG level did not change compared with the rabbits in group 1 (Figure 1). At 12th week, TC and LDL-C levels in group 2 and 3 were all higher than baseline, also higher than in group 1, and HDL-C level was significantly lower than group 1. TC and LDL-C levels in group 3 were lower than group 2 at 24th week.
[Figure omitted. See PDF.]
Figure 1. The fluctuations of serum lipids level in the three groups.
https://doi.org/10.1371/journal.pone.0093686.g001
The lipids level in group 3 was of significant fluctuation as given cholesterol-rich and low-fat diet alternately. Significant fluctuations were not found in the other two groups (Figure 1).
3 Serum lipid smoothness
SI values of each group were calculated at the end of the experiment. As shown in table 2, the SI values in group 2 and 3 were both lower than group 1, and were significant lower in group 3 compared with group 2.
[Figure omitted. See PDF.]
Table 2. SI values in the three groups (mean [SD]).
https://doi.org/10.1371/journal.pone.0093686.t002
4 Changes of serum hs-CRP, IL-18, ET-1, OX-LDL and NO
Hs-CRP, IL-18, ET-1, OX-LDL and NO levels were investigated to evaluate the inflammatory state of the atherosclerotic plaques for all rabbits in three groups. As shown in table 3, hs-CRP, IL-18, OX-LDL and ET-1levels in group 2 and 3 were significantly higher than in group 1 at 12th week, While NO level was significantly lower compared with group 1. The hs-CRP, IL-18, OX-LDL and ET-1 levels kept increasing in group 2 and 3 at 24th week, and they were significantly higher in group 3 than those in group 2. The NO level continued to decline in group 2 and 3 at 24th week, and it was even lower in group 3.
[Figure omitted. See PDF.]
Table 3. Serum hs-CRP, IL-18, ET-1, OX-LDL and NO levels in the three groups (mean [SD]).
https://doi.org/10.1371/journal.pone.0093686.t003
5 Changes of the aortic ultrasound
The arterial intima-media thickness (IMT) was severely thickening and multiple plaques were clearly observed in the arterial wall after giving cholesterol-rich diet feeding for 12 weeks. There were no significant differences in IMT between three groups at baseline but it was increased considerably both in group 2 and 3compared with baseline and group 1 at 12th week. IMT thickened greatly at 24th week than 12th week in both group 2 and 3, but changes of IMT in group 3 were more obvious than group 2 at 24th week, see Table 4. Aortic ultrasound showed that the plaque sizes of the same location in group 3 were (0.80×4.90) mm and (1.40×9.90)mm, in group 2 were (0.74×3.46)mm and (0.75×4.34)mm at 12th week and 24th week respectively.(See in Figure 2.)
[Figure omitted. See PDF.]
Figure 2. The vascular ultrasound of group 2 and group 3 in different weeks.
Legend: (A) and (C): group 2 at week 12 and week 24; (B) and (D): group 3 at week 12 and week 24.
https://doi.org/10.1371/journal.pone.0093686.g002
[Figure omitted. See PDF.]
Table 4. The IMT of the three groups in different weeks (mean [SD], mm).
https://doi.org/10.1371/journal.pone.0093686.t004
6 The gross appearance of the aorta
The percentage of plaque area of intima shown as red stained with Oil Red O in group 3 was significantly higher than that in group 2, see Figure 3 and Table 5. Grossly, the intima in group 1 was smooth and was not colored by Oil Red O. Fatty lipid-like material could be observed easily. There were severe atherosclerotic lesions in the vascular intima especially in the aortic arch and the plaques had distinct borders with no surface rupture in group 2. While in group 3, more serious lesions appeared especially in the descending aorta compared with group 2. Diffuse plaques could be seen in the intima and were confluent to big patches. Moreover, the plaque borders were not clear and the surface was not smooth.
[Figure omitted. See PDF.]
Figure 3. The intima with Oil Red O staining of atherosclerosis in the three groups.
https://doi.org/10.1371/journal.pone.0093686.g003
[Figure omitted. See PDF.]
Table 5. The characteristics of atherosclerotic plaque in the three groups (mean [SD]).
https://doi.org/10.1371/journal.pone.0093686.t005
7 The histological changes of the aorta
The aorta intima was smooth with only one layer of endothelial cells without foam cells and lipid accumulation in group 1 under microscopic examination; see Figure 4(A). In group 2, the IMT was obvious thickening and the endothelial cells were shedding. There were obvious atherosclerosis lesions formation with numerous foam cells and cholesterol crystal. Cell necrosis and calcium deposition in some areas also could be seen, see Figure 4(B1–B2). In group 3, atherosclerotic plaques were larger with thinner fibrous caps and bigger lipid cores compared with group 2, see Figure 4(C1). There were amount of inflammatory cells and new vessels in the intima and near the surface of the lesions, and the fiber cap was found discontinuous, as shown in the representative images (Figure 4(C2–C4)). The microscopic lesion thickness of the sections of aortic arch was further calculated. It showed that the lesion thickness in group 3 was significantly thicker than that in group 2 (P<0.05). In addition, the fibrous cap thickness was thinner than that in group 2 (P<0.01), see Table 5.
[Figure omitted. See PDF.]
Figure 4. The H&E staining of atherosclerosis in the three groups.
Legend: Magnifications: ×200(A–C2), ×400(C3). A: Normal aorta intima in group 1. B1–B2: Atherosclerotic plaque in group 2. The endothelial cells shed, numerous foam cells and cholesterol crystal (B1); cell necrosis and calcium deposition (B2). C1–C3: Atherosclerotic plaque in group 3. plaques with thin fibrous caps and big lipid cores (C1), the discontinuous fiber cap (C2), inflammatory cells (C3).
https://doi.org/10.1371/journal.pone.0093686.g004
8 MMP-9 and LOX-1 expressions in aorta
The immuohistochemical staining of atherosclerosis was performed to detect the expressions of MMP-9 and LOX-1. Compared to group 2, numbers of both MMP-9 and LOX-1-expressing cells were significantly increased in atherosclerotic plaque in group 3(Figure 5). Furthermore, the quantity of MMP-9 and LOX-1 IOD in group 3 were significantly higher than those in group 2, see table 6.
[Figure omitted. See PDF.]
Figure 5. The immuohistochemical staining of atherosclerosis in the 3 groups.
Legend: Magnifications: ×400. MMP-9: matrix metalloproteinase-9; LOX-1: lectin-like oxidized low density lipoprotein receptor-1. Representative pictures of MMP-9 and LOX-1 expressions immuohistochemical staining in the aortic atherosclerotic plaque of the three groups.
https://doi.org/10.1371/journal.pone.0093686.g005
[Figure omitted. See PDF.]
Table 6. The IOD of MMP-9 and LOX-1 in the three groups (mean [SD]).
https://doi.org/10.1371/journal.pone.0093686.t006
Discussion
An abundance of experimental, clinical, and epidemiologic data has shown that hypercholesterolemia was a major causative factor in atherogenesis [11]. Hypercholesterolemia is strongly believed to contribute to atheroma development in human beings and in animal models, and cholesterol exposure directly determined the atherosclerotic progress in the rabbit model [12]. The clear mechanism of ACS is rupture and its subsequent thrombosis of the atherosclerotic plaque following plaque erosion of the unstable atherosclerotic plaques [3]. Plaque rupture is a mechanical event mainly determined by the fibrous cap thickness and the lipid core size. Biological factors such as inflammatory infiltration may contribute to weakening and fracture of the fibrous cap [13]. The vulnerable plaques mainly compose of an atrophic fibrous cap, a lipid-rich necrotic core, and accumulation of inflammatory cells [14]. The main factors involved in the conversion of a stable plaque into an unstable and rupture-prone lesion are hypercholesterolemia [15], vascular endothelial dysfunction [16], as well as the inflammatory response [17], [18]. It is known that a high level of LDL-C is the culprit of atherosclerotic plaque, and its oxidative modified form, ox-LDL, plays an important biological role in the formation of arterial plaque in the early and late phases [19]. In this study, we demonstrated a persistent hyperlipidemia could promote the progression of the atherosclerotic plaques (as in group 2). With previous evidence showed that some ACS patients with hyperlipidemia had a lower level of LDL-C in clinical practice, our study bring to light that lipids fluctuation could also accelerate the atherosclerotic plaque formation and its subsequent vulnerability.
In this study, the rabbit lipids fluctuation model was successfully established by feeding low-fat diet and cholesterol-rich diet every three weeks alternately after the atherosclerotic plaques formation. Lipids SI values were adopted to evaluate the stability of lipid levels for the first time. The results revealed that SI values of LDL-C in group 3 were the lowest but the progression of the atherosclerotic plaques was the fastest between groups, and the smaller the SI values were, the faster of the plaques formation.
Literatures showed that pathological angiogenesis could be seen in atherosclerotic plaques, which might be linked to plaque's progression and subsequent occlusive thrombosis [20]. Pathological angiogenesis provided a pathway infiltrating inflammatory cells into plaques, while plaques infiltrated diffusely by inflammatory cells were always prone to plaque rupture [21], [22]. Some literatures also mentioned that this type of plaque, a thin-capped fibroatheroma with increased inflammatory cell content, was considered to be most vulnerable to disruption [23]. Accordingly, present result showed that the arterial IMT was significantly higher, the plaque area was bigger and the atherosclerotic lesions formation was quicker under ultrasonography in group 3. Moreover, the atherosclerotic lesions of vascular intima in histological examination were significantly larger with a large number of infiltrations of inflammatory cells around plaques. Neovascularization were also found in the intima near the surface of the lesions. The fiber cap thickness was thinner and some fiber cap was even discontinuous. These findings indicated that lipids fluctuation was of impact on the progression and vulnerability of atherosclerotic plaques.
Unstable carotid atherosclerotic plaques are characterized by cap rupture, leading to thromboembolism and stroke. MMPs have been implicated in the progression of atherosclerosis and plaque rupture, and MMP-9 was strongly correlated with plaque instability [24]. The OX-LDL receptor LOX-1, mainly expressed at the shoulder of plaques, plays a crucial role in atherosclerosis. It can activate the inflammatory activity and also induce expression and activation of MMPs [25]. The pathological effects of LOX-1 not only initiate atherosclerotic lesion formation, but also contribute to the vulnerability of a plaque [26]. In this study, expressions of MMP-9 and LOX-1 in group 3 were dramatically higher than in group 2 and group 1. Combining the ultrasonographic and histological changes of atherosclerosis, we suggested that lipids fluctuation might increase the expressions of MMP-9 and LOX-1, accordingly accelerate the progression of atherosclerosis and lead to the formation of unstable plaques.
Previous studies revealed that the development of plaques was closely correlated to the inflammatory process involving the arterial wall [27]. Many literatures supported that inflammation played a pivotal role in all phases of atherosclerosis, from the fatty streak lesion formation to the acute coronary event due to vulnerable plaque rupture [28]. Vascular inflammation contributes to the pathogenesis of atherosclerosis and later in the disease process, it is a major determinant for the acute coronary syndromes. Hs-CRP, a simple downstream marker of inflammation, has been proved to closely connect the atherosclerotic plaque progression [29], [30]. Some studies also showed that thin cap fibroatheromas were commonly seen in those patients with elevated high levels of hs-CRP [13]. Elevated baseline concentrations of hs-CRP are associated with the risk of atherosclerotic events in general population and show a predictive value even in terms of secondary prevention. IL-18 is a pleiotropic proinflammatory cytokine and plays a central role in the inflammatory cascade [31]. It was identified as an interferon-γ–inducing factor, stimulating interferon-γ production in T lymphocytes and natural killer cells, which are ascribed a key role in atherosclerotic plaque growth and vulnerability [32]. This study showed that hs-CRP and IL-18 levels in group 3 were significantly higher than those in the other two groups and therefore, inflammation might play an important role in the accelerating process of atherosclerotic plaques due to lipid fluctuation.
NO and ET-1 level disorder are also key point to promote atherosclerosis progression. In our study, NO level was significant lower while ET-1 level was higher in group 3 than the other groups. Therefore, the endothelium dysfunction of group 3 exacerbated and accelerated the plaque progression. It indicated that the accelerated progression and vulnerability of arterial atherosclerotic plaques caused by instability of lipid levels was mainly linked to activation and worsening of arterial endothelium dysfunction and inflammatory reactions.
In conclusion, marked serum lipids fluctuation is considered to be associated with the atherosclerotic plaque progression and vulnerability in cholesterol-rich diet induced hypercholesterolemia in rabbits. It could exacerbate the arterial endothelium dysfunction and inflammatory reactions, accelerate the progression and impair the stability of atherosclerotic plaques. Our findings might shed light on further exploration of risk factors affecting the atherosclerotic plaque progression and vulnerability in human beings.
In our study, the establishment of rabbit lipid fluctuation model and the idea of observation of the relationship between atherosclerosis progression and lipids fluctuation are novel. There must be some limitations in this study: 1) the sample size of rabbits is not big enough; 2) whether the current animal results can represent the clinical patients or not; 3) the specific mechanisms of lipids fluctuation affecting atherosclerotic plaques. We will continue focusing on the following research in the future.
Acknowledgments
The authors are grateful for the Department of statistics and the department of biochemistry of Chinese PLA General Hospital for assistance. The authors would like to express heartfelt acknowledgement to Professor Li Fan, from Geriatric Cardiology of Chinese PLA General Hospital, for her major assistance in the revision work.
Author Contributions
Conceived and designed the experiments: XZ QS. Performed the experiments: XZ HW LC KL WZ YD. Analyzed the data: XZ HW. Contributed reagents/materials/analysis tools: XZ LC. Wrote the paper: XZ QS.
Citation: Zou X, Wang H, Cai L, Li K, Zhang W, Ding Y, et al. (2014) Effects of Serum Lipid Smoothness on the Progression and Vulnerability of Atherosclerotic Plaques in Rabbits. PLoS ONE 9(7): e93686. https://doi.org/10.1371/journal.pone.0093686
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Abstract
Objective
We aimed to explore the effects of lipid smoothness on the progression and vulnerability of atherosclerotic plaques.
Approach
24 rabbits were divided into three groups randomly. Group 1 was given standard chow diet; group 2 was fed with cholesterol-rich diet; for group 3, subjects were planned to take cholesterol-rich diet at the first phase for 12 weeks and during the second phase, low-fat and cholesterol-rich diet was then applied alternately every three weeks till the end of the experiment. Lipid profiles, inflammatory factors, endothelium functions, pathological and histological changes were examined. Expressions of matrix metalloproteinase-9 and lectin-like oxidized LDL receptor-1 were measured by immunohistochemical staining.
Results
According to data collected during the whole experiment, lipid smoothness index of group 3 was the lowest. Compared with group 2, statistics of the group 3 indicated that: the development of plaques progressed faster; the plaque area and plaque thickness (53.53[22.6]% vs 33.90[24.91]% , 800.38[98.25]µm vs 675.00[109.67]µm) were higher while the fibrous cap thickness (103.50[45.66]µm vs 295.83[97.90]µm) was lower; hs-CRP (0.53[0.07]mg/dL vs 0.45[0.06]mg/dL), interleukin-18 (186.01[8.41]ng/L vs 158.08[2.37]ng/L), OX-LDL (177.15[5.93]µg/L vs 139.57[2.35] µg/L) and endothelin-1 (164.66[9.54]ng/L vs 131.52[4.39]ng/L) were higher while nitric-oxide (22.41[1.69]µmol/L vs 27.23[1.36]µmol/L) was lower; expressions of matrix metalloproteinase-9 (IOD: 37375.87[5634.52] vs 20956.57[4616.93]) and lectin-like oxidized LDL receptor-1 (IOD: 45213.04[16653.81] vs 21921.68[6142.32]) were higher.
Conclusions
Lipids fluctuation could accelerate the progression and vulnerability of atherosclerotic plaques through worsening arterial endothelium dysfunction and inflammatory reactions.
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