Therapeutic Potential of Quercetin as an Antiatherosclerotic Agent in Atherosclerotic Cardiovascular Disease: A Review

Atherosclerotic cardiovascular disease (ASCVD) is one of the diseases with the highest morbidity and mortality globally. It causes a huge burden on families and caregivers and high costs for medicine and surgical interventions. Given expensive surgeries and failures of most conventional treatments, medical community tries to find a more cost-effective cure. Thus, attentions have been primarily focused on food or herbs. Quercetin (Qu) extracted from food, a flavonoid component, develops potentials of alternative or complementary medicine in atherosclerosis. Due to the wide range of health benefits, researchers have considered to apply Qu as a natural compound in therapy. This review is aimed to identify the antiatherosclerosis functions of Qu in treating ASCVD such as anti-inflammatory, antioxidant properties, effects on endothelium-dependent vasodilation, and blood lipid-lowering.


Introduction
Atherosclerosis (AS) is a chronic progressive inflammatory disease associated with inflammatory response, endothelial dysfunction, lipid metabolism disorders, smooth muscle cell migration and proliferation, and oxidative stress [1,2]. Atherosclerotic cardiovascular disease (ASCVD) caused by AS is one of the diseases with the highest morbidity and mortality in the world, ranking first in the total cause of death among urban and rural residents in China, with more than 40% mortality rate, whose incidence and number of cases are still rising [3]. Although the study shows that in the past 30 years, the incidence of coronary heart disease in the United States has dropped from 6.9% to 5.2%, the mortality rate due to coronary heart disease has dropped 60%, and ASCVD has been and will continue to be the leading cause of death among US residents [4]. erefore, the treatment of ASCVD is a hot topic concerned by the public. In recent years, a number of research achievements have been made in the field of atherosclerosis [5]. Various medicines, such as HMG-CoA reductase inhibitors (statins) [6], cholesteryl ester transfer protein (CETP) inhibitors (anacetrapib) [7], and cholesterol absorption inhibitors (ezetimibe) [8], have been clinically proven in the treatment of atherosclerosis.
Antimyocardial ischemia drugs, coronary angioplasty, coronary stent implantation, and surgical coronary artery bypass grafting have been widely used to treat ASCVD.
Beyond modern medical treatment, the conventional medicine featured by natural herbs with satisfactory clinical efficacy and low toxicity can be used as replacement therapies for many diseases. Relevant research has become a hot topic in modern medicine [9][10][11]. Natural products like flavonoids which have been proved to have many functions such as anticancer [12], anti-inflammatory [13], antidiabetes [14], antivirus, and antiallergy [15] are considered as important resources in the treatment of cardiovascular disease. It has been widely reported that Quercetin (Qu), as one of the important flavonoids, plays an important role in the prevention and treatment of atherosclerosis. Many biological targets of Qu have been discovered, for instance, inhibiting the formation of reactive oxygen species by blocking nicotinamide-adenine dinucleotide phosphate (NADPH) oxidase [16], preventing the formation of atherosclerotic plaques by upregulating nitric oxide synthetase [17] and stabilizing endothelial atherosclerotic plaque by downregulating matrix metalloproteinase-1 (MMP-1) [18]. Qu serves as one of the important type of flavonoids and is apparently capable of delivering anticipated antiatherosclerotic effects in ASCVD. Research interest for Qu is because of its diverse range of biological properties. For this review, we have assessed the literature which have been published in PubMed and the Web of Science related to AS or ASCVD in recent years to uncover the protective roles of Qu in antiatherosclerosis and ASCVD. e combined functions of Qu allow for the prevention of AS. is review describes the possible therapeutic benefits of Qu, along with its potential mechanisms of action, to support the clinical use of the Qu for the prevention of ASCVD via antiatherosclerosis.

Pharmacology and Bioavailability of Quercetin
Quercetin (3,3′,4′,5,7 pentahydroxy flavone) is one of a group of over 4000 naturally available plant phenolic compounds whose isolation and biological recognition were first described by Rusznyak and Szent-Györgyi in 1936 [19]. Its chemical structure is an unconjugated aglycone that does not have a carbohydrate moiety and consists by a fused ring system with a benzopyran associated with an aromatic ring and phenyl substituents (the chemical structure is shown in Figure 1). Qu is the most common and widely distributed flavonol compound in our regular diet. is situation is shown in Figure 2. It can be found in almost all plant food, such as tea, onion, lettuce, broccoli, beans, fruits, and buckwheat, and it is also one of the effective components of gingko leaves, mulberry parasitic, sandalwood, and other Chinese herbs [20][21][22]. e natural flavonol exists in a glycosylated form generally with glucose as its corresponding sugar part. Glycosylation may occur at any of the five OH groups of the flavonol ring additional types of Qu are usually Qu aglycone, such as Qu 3-O-glucuronide and Qu 3′-O-sulfate [23], all kinds of Qu are consumed in the small intestine and digestive tract, the most widely recognized Qu glycoside exhibits the sugar moiety and structures speak to 60-75% of flavonoid intake [24]. With the development of research, modern research has confirmed that Qu has exhibited high antioxidative, anti-inflammatory, and antimicrobial activities [25]. Besides, recent studies have found that Qu can restrain the proliferation and metastasis of multiple cancer cell types, such as breast cancer [26], colon cancer [27], lung cancer [28], and pancreatic cancer cells [29].
Qu has a long history of cardioprotective ability, and it has been extended for clinical trials. In addition to its wellknown heart-protecting effects, Qu has also been reported to exert various other pharmacological activities such as anxiolytic [30], hypoglycemic [31], immunomodulatory [32], neuromodulation [33], and wound healing [34]. However, poor water solubility and low bioavailability of Qu have been its limitations. Qu is quickly conjugated with glucuronic acid and/or sulfate during first-pass metabolism (intestine-liver), and a portion of the metabolites is also methylated; the first investigation on the pharmacokinetics of Qu in humans suggested very poor oral bioavailability after a single oral dose (∼2%) [35]. e estimated absorption of Qu glucoside, the naturally occurring form of Qu, ranges from 3% to 17% in healthy individuals receiving 100 mg [36]. Some modified dosage forms of Qu have been developed to overcome these disadvantages, mainly including nanoparticles [37], microemulsions [38], and other drug carriers [39].

Protective Role in Endothelium Protection.
Endothelial cells are a semipermeable barrier between blood and vascular wall; it can locally regulate the blood vessels by secreting vasodilator substances such as nitric oxide (NO), prostacyclin, endothelium-derived hyperpolarizing factor, and vasoconstrictive substances such as endothelin, an endothelium-derived contractile factor [40]. ese substances can dilate blood vessels, antiproliferate, antiagglutinate, and limit blood pressure in physiological situation, while they can destroy the endothelial homeostasis in pathological states, such as local elevated tensile stress, hypercholesterolemia, total triglyceride-(TG-) rich residual   Evidence-Based Complementary and Alternative Medicine lipoproteins, circulation of vasoactive amines, and infection and immune complex [41]. Qu can relieve vascular endothelial injury through multiple approaches to play a part in antiatherosclerosis [42][43][44]. NO is an important endogenous vasodilator produced by endothelial nitric synthase (eNOS) acting on L-arginine, which can regulate vascular dilatation and endothelial function [40]. However, when the vascular endothelial cells are affected by a series of harmful factors, the release of vasomotor factors by the endothelial cells decreases, while vasoconstrictors increase, which breaks the vascular homeostasis and causes endothelial dysfunction and eventually leads to the occurrence of AS events [40]. Excessive NO can upregulate the expression of Bcl-2/Bax of mitochondrial through the intracellular Akt pathway, which inhibit the release of reactive oxygen species (ROS), cytochrome c, capase-9, and caspase-3. Qu can reverse the endothelial damage caused by excessive NO by inhibiting nitrification stress and protect endothelial cells [45]. Early studies have found that ATP can increase the shear stress generated by blood flow on vascular endothelial cells, increase the intracellular calcium concentration and the activity of eNOS, thus raise the production and release of NO, and ultimately lead to AS [46]. Qu can inhibit the promoting effect of ATP on NO production in vascular endothelial cells, reduce intracellular calcium concentration and eNOS activity, and reduce vascular endothelial injury [42]. Impaired vascular homeostasis caused by decreased bioactivity of endogenous NO is the most typical pathophysiological feature of endothelial dysfunction [41]. Stabilizing intravascular homeostasis may be an important mechanism, for Qu plays a part in protecting vascular endothelial function.
Oxidative stress is the main cause of endothelial dysfunction, which can lead to an imbalance between endothelial cell membrane stability and permeability, impair the function of endocrine and paracrine, and increase the expression of adhesion molecules and the release of endogenous reactive oxygen species (such as superoxide anion and hydrogen peroxide) [47]. In vitro studies have shown that Qu can directly act as an antioxidant, effectively scavenge oxygen free radicals, and protect vascular endothelial function [48]. Oxidative stress induced by homocysteine (HCY) can lead to endothelial damage [49]. Qu can protect the vascular endothelium from oxidative stress induced by homocysteine by inhibiting lipid peroxidation, protein oxidation, and enzymatic reaction, reducing the level of malondialdehyde (MDA) and increasing the content of glutathione (GSH) in high HCY rats [50].

Lipid Metabolism-Modulating Properties.
Dyslipidemia is the main risk factor of AS, including the increase of lipid level caused by total cholesterol (TC), TG, and LDL and the reduction of atherosclerotic lipid levels caused by HDL. Regulating the disorder of lipid metabolism and reducing lipid accumulation are important means to prevent and alleviate AS. In recent years, studies at home and abroad have found that Qu can regulate the metabolism of lipid substances. Some studies have shown that monosodium glutamate (MSG) induces oxidative stress and hepatotoxicity in rats [51] as well as changes the lipid profile of mice [52], and Qu can maintain normal cholesterol levels and prevent the formation of atherosclerotic plaques by treating the dyslipidemia caused by MSG [53]. Besides, Qu can regulate lipid metabolism by lowering the level of TC, TG, LDL, and VLDL in serum and tissues and increasing the content of HDL in serum and phospholipid in tissue [54]. e possible mechanisms of Qu regulating lipid metabolism is described as follows.
HMG-CoA (5-hydroxy-3-methylglutaryl-coenzyme A) reductase is the rate-limiting enzyme in cholesterol synthesis, and its catalytic substrate HMG-COA generating mevalonate is the rate-limiting step in the synthesis of cholesterol. HMG-CoA reductase activity can affect the cholesterol synthesis. It has been demonstrated that Qu can prevent the accumulation of lipid and glycoprotein components in myocardial infarcted rats by reducing the levels of cholesterol, triglycerides, and free fatty acids and decreasing the activity of plasma and liver HMG-CoA reductase [55]. Leptin is a protein hormone involved in the regulation of energy intake and expenditure by the body. Leptin is an important cytokine that plays a key role in regulating lipid metabolism, promoting inflammation, and accelerating aortic valve calcification in patients with coronary heart disease [56]. Mzhelskaya et al. found that Qu can reduce cholesterol levels and lipid levels in high fat and fructose diet rats by regulating leptin-mediated lipid reception [57]. But, the study does not directly clarify the attenuating effect of Qu on cholesterol synthesis; the possible mechanism is that Qu regulate the negative feedback mechanism between fat deposits and fat catabolism rate through leptin, thus promoting the process of lipid metabolism and glucose metabolism and reducing cholesterol intake in rats [57].
Reverse cholesterol transport (RCT) is a process of transporting cholesterol to the liver for further excretion, which can effectively remove excess cholesterol in cells. RCT of macrophages in atherosclerotic plaques is a critical mechanism of antiatherosclerosis. Liver X receptor α (LXRα) [58], scavenger receptor B-I (SR-BI) [59], and ATPbinding transporter A1 (ABCA1) play a vital role in promoting macrophages RCT and maintaining intracellular cholesterol homeostasis. Many compounds and extracts of traditional Chinese medicine can act on different targets of RCT and exert antiatherosclerosis effect [60]. Qu could promote intracellular cholesterol efflux, upregulate the expression of SR-BI, and reduce the ability of high-density lipoprotein (HDL) to selectively acquire cholesterol in a dose and time-dependent manner, indicating its protective role in atherosclerosis [61]. Peroxisome proliferator-activated receptor c (PPAR c) and LXRα are important transcriptional factors for ABCA1. Qu-induced upregulation of ABCA1 and cholesterol efflux of macrophages may be mediated by increased expression levels of the PPAR c and LXRα genes [62,63]. It was shown that Qu can induce the expression of ABCA1 in THP-1 derived foam cells, enhance the apoA-Idependent cholesterol efflux, and reduce the risk of atherosclerosis [63]. e selective uptake of HDL-C into hepatocytes and steroidogenic cells is the last step of RCT, a Evidence-Based Complementary and Alternative Medicine process that promotes HDL-C clearance in the plasma. Low clearance of plasma HDL-C aggravates the development of AS while high clearance of plasma HDL-C impedes atherogenesis. A study found that Qu promotes the selective uptake of HDL-C by enhancing SR-BI expression through stimulating the PPAR c/LXRα pathway in HepG2 cells [61]. Besides, Qu can also affect the expression of LXRα and ABCA1 through the p38-dependent pathway [64], proprotein convertase subtilisin/kexin type 9 (PCSK9) pathway [65], and cholesterol 7 alpha-hydroxylase (CYP7A1) pathway [66] to promote cholesterol efflux and reduce the risk of atherosclerosis.
Accumulation of foam cells and formation of lipid streaks are the early lesion characteristics of AS. Oxidized low-density lipoprotein (oxLDL) is thought to transform native lipoprotein into an antigenic factor that attracts monocyte-derived macrophages to the vascular wall, thereby initiating a convoluted immune response governed by inflammatory modulators [67]. Inhibiting low-density lipoprotein (LDL) oxidation of macrophages and foam cell formation are effective strategies of antiatherosclerosis. Mulberry leaf rich Qu inhibited the oxidation and lipid peroxidation of LDL and attenuated atherosclerosis [68]. An earlier study reported that Qu also targeted the oxLDL-independent pathway and lipopolysaccharide-dependent pathway of lipid droplet formation in macrophages and inhibited the reactive oxygen species production and interleukin (IL)-6 secretion, which indicated the antiatherosclerotic activity of Qu [69]. oxLDL can induce excessive production of reactive oxygen species and block the expression of lectin-like oxidized LDL receptor-1 (LOX-1) in cultured macrophages, leading to lipid accumulation. It was demonstrated in cultured macrophages that Qu could ameliorate lipid deposition and overproduction of reactive oxygen species induced by oxLDL and block the expression of LOX-1 [18].

Anti-Inflammatory Activity.
AS is a chronic inflammatory disease mediated by a network of proinflammatory cytokines. Macrophages are critical in the inflammatory response. OxLDL-activated macrophages can synthesize and secrete many growth factors and pro-inflammatory factors, such as platelet-derived growth factor, fibroblast growth factor, and tumor necrosis factor (TNF)-α, IL-1, which can promote the growth of plaque and inflammatory response [70,71]. T cells entering the intima are activated by recognizing antigens presented by macrophages and dendritic cells, producing factors with strong atherogenic effects [2], such as gamma interferon, TNF, and lymphotoxin. ere are multiple signaling pathways for Qu to inhibit the expression of inflammatory factors to stabilize atherosclerotic plaque, slow down the progression of atherosclerosis, and reduce the incidence of ASCVD.
A major signaling mechanism associated with atherosclerosis is the activation of NF-κB family of transcription factors. NF-κB is an oxidative stress-sensitive transcription factor that has been found in the early lesions of atherosclerosis [72].
e transcription of vascular cell adhesion molecule-1 (VCAM-1), intercellular adhesion molecule-1 (ICAM-1), and other adhesion molecules, such as E-selectin and P-selectin, is regulated and activated by NF-κB [73]. ese activated adhesion molecules help blood-borne cells to recruit to atherosclerotic lesions. Oral administration of Qu significantly suppressed the levels of IL-1β, TNF-α, and IL-10 in serum and attenuated atherosclerotic plaque through decreasing the transcriptional activity of the NF-κB in patients with coronary artery disease [74]. Qu also inhibited proatherogenic mediators such as ICAM-1 and VCAM-1 in oxLDL-induced smooth muscle cells [32] and downregulated expression of adhesion molecules and NF-κB in TNF-α-induced human aortic endothelial cells [75]. Another study demonstrated that Qu is effective to regulate the atherosclerotic inflammatory process by attenuating the NF-κB signaling pathway in endothelial cells and decrease the inflammatory process induced by hypercholesterolemic diet in atherosclerotic rats [32].
Phosphatidylinositol 3-kinase (PI3K) signaling is a multicell surface receptor that regulates cell proliferation, survival, and death. Akt activated by PI3K in response to growth factors or cytokines is an inactive cytoplasmic protein that is recruited to the plasma membrane. e activation of the PI3K/Akt pathway significantly promotes macrophage polarization, which stimulates or inhibits inflammatory responses [44]. Toll-like receptors (TLR) and ROS can mediate the activation of PI3K/Akt signaling pathway [76]. Qu significantly downregulated the elevated mRNA expression of TLRs and cytokine TNF-α in HCD-fed atherosclerotic rats in vivo [77]. As Qu possesses inhibition on both TLR-NF-κB signaling pathway and TLR-mediated MAPK pathway, it is evident that it could be used as a therapeutic agent to ameliorate atherosclerotic inflammation and improve ASCVD patients' symptoms [77]. Qu also displayed an inhibitory role in vitro in LPS-induced ROS production, inflammatory response, and apoptosis, which were linked with PI3K/AKT-regulated caspase-3 and NF-κB activation and reduced the atherosclerotic plaque size in high fructose feeding-induced mice [78].
Activation of p38 can activate the expression of cytokines involved in proinflammatory signaling and local recruitment of immune cells, such as E-selectin [79], VCAM-1 [79], and chemokine monocyte chemoattractant protein 1 (MCP-1) [80]. Frei Balz's team found that Qu play an anti-inflammatory role in inhibiting the activation of p38, reducing the expression of E-selectin and ICAM-1 protein in human aortic endothelial cells induced by lipopolysaccharide [81]. Qu also delayed the progression of atherosclerosis by increasing phosphorylation of p38 by activating transforming growth factor beta kinase 1 and mitogenic kinase 3/6 [64].

Antiapoptosis Activity.
Apoptosis is an important factor during atherosclerotic development. Autophagy protects vascular cells in plaques against oxidative stress and apoptosis by degrading damaged organelles, which is an effective response against inflammation and oxidative stress in AS plaque cells, and thus it plays an important role in the initiation and development of AS [82]. TNF-α, IL-1β, and IL-18 are the key inflammatory factors between autophagy and inflammation. A previous study revealed that Qu stabilizes AS plaques and inhibits AS development by reducing the production of the proinflammatory cytokines TNF-α, IL-1β, and IL-18, a mechanism which involves the induction of autophagy [83]. Weakened autophagy takes place in all major cell types in AS plaques, resulting in impaired macrophage apoptosis and increased senescence of blood vessel endothelial and smooth muscle cells. mTOR, a key molecule in the process of autophagy induction, integrates multiple upstream signaling pathways and interacts with regulator proteins [84]. It also reported that Qu could downregulate the expression levels of mTOR, P53, and cyclin-dependent kinase inhibitor 1A (P21), enhance autophagy, and delay senescence [83]. Autophagy has also been termed as lipophagy, which involves the degradation of intracellular lipid droplets and contributes to cellular lipid metabolism [85]. Another study found that Qu effectively reduces oxLDL-induced RAW264.7 foam cell formation, reducing cellular lipid accumulation and delaying cell senescence through the MammalianSte20-like kinase1 (MST1) pathway [86]. MST1, a novel regulator of apoptosis, participates in multiple biological activities of cells, including autophagy, apoptosis, and oxidative stress [87,88].

Alteration of the Gut Microbiota and Reduction of Atherogenic Lipid Metabolites.
Recent studies of pathogenesis have highlighted the significant roles of the intestinal microbiota and chronic inflammation in both the onset and development of AS [89][90][91]. e occurrence of AS is strongly associated with inflammatory response caused by the disorder of the intestinal immune system [92]. AS patients have metabolic characteristics, for the community composition of their intestinal flora is different [93]. Inhibiting the inflammatory response and regulating the lipid metabolism of intestinal microorganisms can be used as strategies to delay the development of AS. Short-chain fatty acids (SCFAs) are metabolites of systemic inflammation and are associated with the expansion and rupture of AS plaques [94]; Qu can increase the concentration of SCFAs in the intestinal tract and inhibit the progression of AS [95]. A microbiome with high abundances of Firmicutes and Actinobacteria can result in atherosclerotic area [96,97]; oral administration Qu reduced the levels of atherogenic lipid metabolites by modulating the abundances of Firmicutes and Actinobacteria [98].

Elimination of Etiology, Reduction of Complications, and Effective Prevention and Treatment of AS.
In hemodynamically activated arterial regions, free radical-induced lipoprotein oxidation, enzymatic changes in the intima, production of active lipids, and increased enzymatic activity of MDA and ROS can increase the inflammatory response of arterial intima, thus causing atherosclerotic lesions [99]. Obesity and hypercholesterolemia increase the production of oxygen free radicals and cause oxidative stress [100]; Parvin et al. [101] found that Qu can reduce the blood lipid in obese rats, reduce the expression of oxidative stress factors, improve the vascular remodeling, and prevent the formation of atherosclerotic plaque through antioxidant activity.
In addition to the activities mentioned above, Qu also exerts antithrombotic activity both in vitro and in vivo [102,103]. Isorhamnetin and tamarixetin inhibit platelet function and thrombus formation through effects on early activation processes including calcium mobilization, granule secretion, and integrin activation [104]. According to the recommendations of the ASCVD Global Guidelines, antiplatelet and antithrombotic treatment is a critical approach for the treatment of acute coronary artery syndrome and secondary prevention of  Evidence-Based Complementary and Alternative Medicine coronary heart disease [105,106]. Aspirin is one of the most widely used antiplatelet agents worldwide. Its use is associated with adverse events such as gastric bleeding, and whilst studies showed that decreasing aspirin doses reduces adverse event numbers without a reduction in antiplatelet efficacy, even lowdose aspirin treatment is associated with an increased bleeding risk [107]. As such, the pharmacological implications of the effects of the methylated metabolites of Qu with respect to the antiplatelet effects of aspirin are worthy of consideration. Apart from these actions, one more recent study showed that Qu processes an antiapoptotic effect in ischemic myocardial damage [108]. Altogether, these studies demonstrated that Qu may be a promising drug for the treatment and prevention of atherosclerosis in ASCVD. Wistar rats Decrease serum LDL, TC, MDA, and ROS to improve the vascular structure and prevent from the plaque formation [101] Anti-inflammation ApoE −/− mice Decrease serum TNF-α and IL-6 levels and increase levels [110] ApoE −/− mice Inhibit phenotypic and functional maturation of DCs [111] Balb/c mice Mediate HDL function and lipid-glucose state in the circulation by improving biological activity (quality) and the activity of bound to PON1 [112] Antiapoptosis Nude mice Activate ERK and the ERK signaling pathway to promote autophagy [113] ApoE −/− mice Enhance autophagy and downregulate mTOR, P53 and P21 protein expression levels to alleviate AS lesions and reduce lipid accumulation and increase ratio of LC3 II/I [83] Regulate lipid metabolism and reduce the atherosclerotic plaque area ApoE −/− mice Increase ABCA1 and LXRα expression and downregulate PCSK9 protein expression [110] Wistar rats Elevate activity of hepatic CYP7A1, LXRα, and ABCG1 to promote cholesterol-to-bile acid conversion and cholesterol efflux [114] C57BL/6J mice Upregulate LDLR and CYP7A1 gene expression to facilitate the removal of cholesterol via fecal excretion [115] Wistar rats Promote conversion of cholesterol to bile acids and cholesterol efflux by increasing hepatic CYP7A1 activity and hepatic LXRα, ABCG1, and LDLR protein expressions [116] ApoE −/− mice Elevate cholesterol accepting ability of HDL and increase ABCA1/G1 expression levels of proteins related to RCT [117] Sprague-Dawley rats Influence gene and protein expression of SREBP1c and HMGR to lower lipid [118] Sprague-Dawley rats Upregulate hepatic gene expression CYP7A1, LXRα, ABCA1, and ABCG1 to promote cholesterol efflux [119] Zucker rats Lower the level of HDL cholesterol and increase phosphorus level by increasing the ratio of ASAT/ALAT activity induced by leptin [56] ApoE −/− mice Regulate expressions of ABCA1, LXRα, and PCSK9 [26] ApoE −/− mice Downregulate PCSK9 and CD36 protein expression and upregulate PPAR c, LXRα, and ABCA1 protein expression levels in both the aortic and liver tissues [65] Alter the gut microbiota ApoE −/− mice Regulate primary bile acid biosynthesis [95] C57BL/6J mice Improve composition and functionality of gut microbiome and production of short chain fatty acids [120] Wistar rats Stimulate bacterial enzymatic activity and increase enzymatic activity of the intestinal microbiota [121] Ldlr −/− mice Reduce MDA, cholesterol, and LPC 18 : 1 and increase IL-6 and coprostanol levels [98] Humans Anti-inflammation

Healthy nonsmokers
Inhibit production of IL-1β, TNF-α, IL-6, and IL-8 in Lipopolysaccharide-stimulated [122] CVD patients Decrease transcriptional activity of NF-kB [74] Endothelial protection CVD individuals Enhance NO bioavailability, possibly by stimulating eNOS activity [123] 6 Evidence-Based Complementary and Alternative Medicine Taken as in vitro and ex vitro together, the possible pathway of Qu on anti-atherosclerotic function is shown in Figure 3.

HaVSMCs
Decrease relative expression levels of members of the mitochondrial apoptotic pathway, including P53, puma and Noxa, caspase-3, and caspase-8 [133] EA.hy926 cells Regulate Akt/GSK3β signaling pathway by increasing the expression of p-Akt and p-GSK3β [134] Lowering lipid Human HepG2 cell line Promote selective uptake of HDL-C by enhancing SR-BI expression through stimulating the PPAR c/LXRα pathway. [61] THP-1 macrophages Increase ABCA1 expression and cholesterol efflux through LXRα pathway to promote RCT [62] Evidence-Based Complementary and Alternative Medicine

Conclusion
In the treatment of ASCVD, Qu can reduce the formation of AS plaque through anti-inflammatory, antioxidation, regulation of lipid metabolism disorders, and other pharmacological effects, therefore reducing the incidence of ASCVD and improving the prognosis of ASCVD patients. In spite of medicine, surgery and intervention operation can improve the cardiac function; it still causes a considerable burden on families and caregivers and results in huge financial costs. Moreover, the high cost of surgery treatments and the failure of most conventional treatments have led the medical community to pursue cost-effective prevention and treatment. For ASCVD patients who are intolerant to surgery and cannot afford the high economic cost of treatment, it is a good choice to increase the Qu-rich low-fat diet in diet. Qu is rich in sources and has a wide range of pharmacological effects such as antitumor, antivirus, antiallergy, and antibacterial effects, which possess a broad prospect in application.
Although the new formulation of Qu has been developed and is partially used in clinics, due to its low bioavailability and low absorption rate, there are still many problems to be solved. Researchers need to further explore the pharmacological mechanism of Qu in human body so as to apply it to the prevention and treatment of clinical diseases better. It is also important to increase the water solubility and oral bioavailability of Qu in the future research. In the further study of phytochemistry, the research field of medicinal activity of Qu should be highlighted for its multiple biological characteristics.

Conflicts of Interest
e authors declare that they have no conflicts of interest regarding the publication of this paper.

Authors' Contributions
Jingui Xue and Qian Deng contributed to the topic conception, manuscript revision, and decision to submit for publication. Xin Chen, Xiaoxue Li, and YanTing Fang participated in the collection of documentation.