Abstract
Diabetes mellitus- (DM-) related vascular diseases attract increased attention due to their high morbidity and mortality. The incidence of obesity, atherosclerosis, coronary heart disease, hypertension, and dyslipidemia is significantly higher in DM patients, with an earlier onset and faster progression compared with non-DM patients. DM-related vascular diseases including macrovascular and microvascular complications are characterized by endothelial dysfunction. Therefore, a better understanding of the etiology and mechanisms of endothelial dysfunction is important for the diagnosis and treatment of DM. Endothelial microparticles (EMPs) are new diagnostic and therapeutic targets and biomarkers in DM-related vascular disease. Circulating EMPs containing biologically active substances act as intercellular signals under physiological and pathological conditions. They serve as biological markers of altered vascular endothelium and reflect the pathological progression and diminished endothelial function of blood vessels. Recent evidence suggests that the plasma level of EMPs is significantly higher in DM patients than in healthy population and is significantly correlated with DM-related complications. These observations have prompted speculation that EMPs play a crucial role in the pathophysiology of DM. This review summarizes the known and potential roles of EMPs in the diagnosis, staging, treatment, and clinical prognosis of DM and related vascular diseases.
1. Introduction
Diabetes mellitus (DM) is a metabolic disease characterized by chronic hyperglycemia and long-term disturbances in carbohydrate, lipid, and protein metabolism inducing chronic progressive dysfunction and failure of visual, nervous, renal, cardiac, and blood vascular systems [1]. The incidence of DM is progressively increasing in both developed and developing countries [2]. As of 2014, an estimated 387 million individuals worldwide have been diagnosed with DM and the prevalence is expected to rise to 592 million by 2035 [3]. In addition, the incidence of obesity [4], atherosclerosis [5], coronary heart disease (CAD) [6], hypertension [7, 8], and dyslipidemia [9] is significantly higher in DM patients, with an earlier onset and faster progression compared with non-DM patients [10]. All of these pathological conditions are closely related to vascular diseases in DM.
DM-induced vascular diseases including macrovascular and microvascular complications contribute to diminished quality of life and even death. Common risk factors for DM-related vascular disease include hyperglycemia, insulin resistance, dyslipidemia, inflammation, hypercoagulability, hypertension, and atherosclerosis. All of these factors contribute to endothelial dysfunction and related complications [9]. Endothelial cell injury is the main factor leading to vascular complications in DM [11]. Consequently, comprehensive analysis and improvement in endothelial cell function may inhibit the progression of DM and related complications.
Endothelial microparticles (EMPs) are novel biomarkers facilitating the evaluation of endothelial function in DM-related vascular diseases. EMPs are membrane vesicles derived from activated or apoptotic endothelial cells [12, 13]. The quantity of these membrane vesicles and their subtype profile reflect diverse pathophysiological states. Further, EMPs are garnering increased attention as putative intracellular communication vectors. As illustrated in Table 1 [14], multiple in vivo and in vitro studies demonstrated that EMPs contribute to coagulation [15, 16], disruption of angiogenesis [6, 17], and cerebral capillary damage [18], among other vascular effects [14, 19]. The plasma level of EMPs is significantly higher in DM patients than in age-matched healthy population [20]. Further, the level of plasma EMPs in DM patients with complications is considerably higher than in DM patients without complications [6, 21, 22]. These studies suggest that EMPs may serve as novel biomarkers for the diagnosis, staging, and progression of DM and related vascular complications.
Table 1.
The role plasma EMPs play in DM.
| Animal model | Clinical study | References | |
|---|---|---|---|
| EMPs in DM | Increased procoagulant activity (ex vivo) | [16] | |
| Faster brachial-ankle pulse-wave velocity and reduced FMD (in vivo) | [29] | ||
| CAD (in vivo) | |||
| Impaired angiogenesis (ex vivo) | [6, 17] | ||
| Progression and severity of retinopathy (in vivo) | [30] | ||
| Impaired cerebral microvascular density and impaired EPC functions (in vivo and ex vivo) | [18] |
2. Role of EMPs in DM
EMPs account for only 5% to 15% of the total MPs [19, 23]. However, they are valuable biomarkers of endothelial cell function and contribute to the pathological progression of multiple vascular diseases in DM. EMPs contain bioactive macromolecules and act as intercellular signals under pathophysiological conditions. They serve as biological markers of altered vascular endothelium and reflect the pathological progression and diminished endothelial function of blood vessels in DM-related vascular diseases.
2.1. EMP Production
Combes et al. first observed the release of EMPs measuring 0.1−1 μm in diameter, as membrane vesicles derived from human umbilical vein endothelial cells (HUVECs) in vitro following stimulation by tumor necrosis factor α (TNF-α) [24]. Subsequently, hyperglycemia, bacterial lipopolysaccharide, thrombin, C-reactive protein, active oxygen cluster, and urea were shown to induce the release of EMPs from endothelial cells [25]. Release of EMPs by apoptotic and activated endothelial cells depends on intracellular calcium elevation and disruption of the asymmetrical distribution of membrane phospholipids, which externalizes phosphatidylserine, and leads to reconstruction of the submembrane skeleton and destabilization of the plasmalemma [26]. Endothelial dysfunction in DM patients increases the plasma level of circulating EMPs resulting in vascular dysfunction [27]. MPs derived from endothelial cells under hyperglycemia induce atherogenesis, angiogenesis, and other complications [9, 28].
2.2. Characteristics of EMPs
The subtypes and mechanisms of EMPs distinguish activated endothelial cells from apoptotic endothelial cells. As shown in Table 2 [25], the surface of EMPs released from activated endothelial cells carries higher levels of CD54-intracellular adhesion molecule-1 (ICAM-1), CD62E-E-selectin (E-selectin), and CD106-vascular cell adhesion molecule-1 (VCAM-1). In addition, the EMP surface also expresses low levels of CD31-platelet cell adhesion molecule (PECAM-1), CD105-endothelin (endoglin), and CD144-vascular endothelial cell cadherin (VE-cadherin). Compared with EMPs released from activated endothelial cells, the surfaces of EMPs released from apoptotic endothelial cells express higher levels of CD31-PECAM-1, CD105-endoglin, and CD144-VE-cadherin and lower levels of CD54-ICAM-1, CD62E-E-selectin, and CD106-VCAM-1 [5].
Table 2.
Antigenic epitope in the surface of EMPs. Many studies have demonstrated that activation and apoptosis endothelial cells release EMPs, whose surface carried different antigen epitope [25].
| CD marker | Antigen | Expression | References |
|---|---|---|---|
| CD31 | PECAM-1 | Apoptosis | [20, 53, 54] |
| CD51 | Integrin av | Apoptosis | [55] |
| CD54 | ICAM-1 | Activation | [54] |
| CD62E | E-selectin | Activation | [20, 54] |
| CD105 | Endoglin | Apoptosis | [20, 54] |
| CD106 | VCAM-1 | Activation | [20, 54] |
| CD144 | VE-cadherin | Apoptosis | [20] |
| CD146 | MelCAM | Apoptosis | [12] |
CD, cluster of differentiation; EMPs, endothelial microparticles; E-selectin, endothelial-selectin; ICAM-1, intercellular adhesion molecule-1; PECAM-1, platelet endothelial cell adhesion molecule-1; VCAM-1, vascular cell adhesion molecule-1; VE-cadherin, vascular endothelial-cadherin.
Partial antigen-specific epitopes are expressed in other cells and are not unique to endothelial cells. However, EMPs released under different pathological conditions or in response to different stimuli express different antigen-specific epitopes. Hence, the antigen-specific epitopes are used to distinguish EMPs from other MPs and accurately and specifically reflect the endothelial cell function under different pathophysiological conditions. Hyperglycemia in DM patients significantly elevates the levels of CD31+/41a− EMPs, CD31+/CD42− EMPs, CD105+ EMPs, CD106+ EMPs, and CD144+ EMPs [6, 20, 29].
The relative proportion of CD62E+/CD31+ EMPs rather than the absolute quantity distinguishes EMPs released by activated endothelial cells from those derived from apoptotic endothelial cells. A greater than 10% concentration of CD62E+/CD31+ EMPs indicates that the majority is derived from activated endothelial cells, whereas 1% or less indicates origin from apoptotic endothelial cells [20]. In DM patients, the level of CD62E+/CD31+ EMPs was less than 1%, indicating that most of them were released from apoptotic rather than activated endothelial cells [20].
2.3. Potential Pathogenic Effects of EMPs
As illustrated in Table 1 [14], multiple in vivo and in vitro studies showed that EMPs contribute to coagulation [15, 16], disruption of angiogenesis [6, 17], and cerebral capillary damage [18], in addition to other vascular effects [14, 19]. These EMPs may have pathogenic effects in vascular thrombosis and angiogenesis, which are essential for the development of DM and its complications.
Procoagulant EMPs initiate and propagate coagulation in DM both in vitro and ex vivo [30–32]. Procoagulant EMPs are significantly increased in patients with DM, even in well-controlled disease without complications and newly diagnosed type 2 diabetes mellitus (T2DM) [29, 33, 34]. In addition, patients with DM accompanied by hypertension, hyperlipidemia, stable coronary disease, angina with or without symptomatic episodes, myocardial infarction, diabetic retinopathy, and nephropathy have significantly increased levels of procoagulant MPs compared with those without DM-related complications [35]. Therefore, elevated levels of MPs may be associated with increased risk of thromboembolic complications in DM.
Taraboletti et al. demonstrated that although the low concentrations of MPs isolated from HUVECs promote angiogenesis in vitro, the high levels of EMPs suppress angiogenesis [36]. Consistent with these results, Mezentsev and colleagues reported that isolated EMPs in pathophysiological concentrations impair angiogenesis in vitro by affecting the parameters of capillary-like network [37]. Angiogenesis may be either suppressed as in the late stages of diabetic nephropathy or elevated as in diabetic retinopathy. These conditions are characterized by impaired endothelial function and increased number of circulating EMPs [35]. As discussed above, EMPs exhibit pro- and antiangiogenic features and influence angiogenic activities. The underlying mechanisms, however, are not fully understood [35].
3. Role of EMPs in the Differential Diagnosis of DM and Its Complications
The plasma levels of EMPs are significantly elevated in patients diagnosed with DM [20], hypertension [38], hypertriglyceridemia, acute coronary artery syndrome [39], and peripheral vascular diseases [19]. Therefore, assessment of the specific relationship between EMP profile and vascular endothelial injury not only deepens our understanding of the pathological progression of DM but also defines novel biomarkers for the diagnosis of DM and its complications. As illustrated in Table 3, the pathways and mechanisms of EMP production vary markedly in different disease states, suggesting that distinct EMP epitopes facilitate the identification of the disease. Compared with healthy controls, the plasma levels of CD31+/41a− EMPs, CD105+ EMPs, and CD106+ EMPs were significantly upregulated in DM patients [20]. By contrast, the plasma level of CD62E+ EMPs in DM patients was only slightly higher, without any statistical significance [20].
Table 3.
Significance of different antigenic epitope of EMPs in diabetic patients.
| Antigen epitope | Disease | References | |
|---|---|---|---|
| CD31+/41a− | DM | CD31+/41a− EMPs: 22238 to 157 × 104/μL [DM versus control], P = 0.0006 | [20] |
|
| |||
| CD31+/CD42− | DM | (1) CD31+/CD42− EMPs in DM patients were significantly higher than those in healthy controls (P < 0.001) | [29] |
| (2) Age was positively correlated with CD31+/CD42− EMPs (rs = 0.322, P = 0.010) | [29] | ||
| (3) The systolic blood pressure was positively correlated with CD31+/CD42− EMPs (rs = 0.329, P = 0.008) | [29] | ||
| (4) HbA1c level was positively correlated with CD31+/CD42− EMPs (rs = 0.337, P = 0.008) | [29] | ||
| (5) Fasting blood glucose level was positively correlated with CD31+/CD42− EMPs (rs = 0.275, P = 0.029) | [29] | ||
| (6) CD31+/CD42− EMPs were independently correlated with FMD and baPWV; FMD was negatively correlated with CD31+/CD42− EMPs (rs = −0.441, P = 0.008); the level of baPWV was correlated with CD31+/CD42− EMPs (rs = 0.497, P < 0.001) | [29] | ||
| DM macrovascular complications | (7) The CD31+/CD42b− EMPs levels were higher in DM patients with macroangiopathy than in DM patients with microangiopathy and no complications | [40] | |
|
| |||
| CD31+ | T2DM | (1) Compared with metformin, pioglitazone treatment improved the imbalance between endothelial damage and repair capacity and led to more favourable changes in coronary risk factors in patients with newly diagnosed T2DM | [34] |
| (2) The univariate analysis showed that the decrease in circulating EMPs was significantly correlated with increase in adiponectin (rs = −0.391, P = 0.01) and with decrease in CRP concentrations (rs = 0.416, P= 0.01), which remained significant in multivariate analysis (rs = −0.321, 95% CI 0.245 to 0.402, for adiponectin, and rs = 0.265, 95% CI 0.299 to 0.406, for CRP) | [34] | ||
| (3) Levels of EMPs expressing CD31 were significantly different among study groups (P < 0.01). DM patients were found to have the highest levels of CD31+ EMPs, while non-DM men without ED were those with the lowest levels; non-DM men with ED had CD31+ EMPs levels that were intermediate (P< 0.05 for both comparisons, DM versus non-DM men with ED, and non-DM men with ED versus non-DM men without ED) | [46] | ||
| (4) Among T2DM patients, an increased level of CD31+/annexin V+ MPs was significantly associated with asymptomatic atherosclerosis | [56] | ||
|
| |||
| CD51+ | DM | (1) CD51+ EMPs in DM patients were significantly higher than those in healthy controls (P < 0.001) | [29] |
| (2) Age was positively correlated with CD51+ EMPs (rs = 0.367, P = 0.003) | [29] | ||
| (3) The systolic blood pressure was positively correlated with CD51+ EMPs (rs = 0.311, P = 0.013) | [29] | ||
| (4) HbA1c level was positively correlated with CD51+ EMPs (rs = 0.266, P = 0.038) | [29] | ||
| (5) CD51+ EMPs were independently correlated with FMD and baPWV; FMD was negatively correlated with CD51+ EMPs (rs = −0.405, P = 0.016); the level of baPWV was correlated with CD51+ EMPs (rs = 0.428, P = 0.001) | [29] | ||
|
| |||
| CD51+/CD41− | DM | CD51+/CD41− EMPs levels correlated with albuminuria and microvascular complications (e.g., diabetic nephropathy) | [16] |
|
| |||
| CD62E | DM | (1) Plasma CD62E+ EMPs levels were significantly higher when the patient is suffering from erectile dysfunction with or without DM | [46] |
| T2DM | (2) Among T2DM patients, decreased CD62E+ EMPs were significantly associated with asymptomatic atherosclerosis | [26] | |
|
| |||
| CD105+ | DM | (1) CD105+ EMPs: 2200 to 390 × 103/μL [DM versus control], P = 0.002 | [20] |
| DM | (2) CD105+ EMPs may play a critical role in the development and progression of diabetic retinopathy | [57] | |
|
| |||
| CD106+ | DM | CD106+ EMPs: 4939 to 740 × 103/μL [DM versus control], P = 0.001 | [20] |
|
| |||
| CD144+ | DM | (1) CD144+ EMPs: 0.541 (0.423–0.652) × 106/mL | [6] |
| DM with CAD | (2) Identified a subpopulation of T2DM patients at risk of developing CAD; CD144+ EMPs: 0.706 (0.577–1.067) × 106/mL | ||
| DM without MetS | (3) CD144+ EMPs: 139.07 (81.6–271.5) × 103/mL | [17, 58] | |
| DM with MetS | (4) CD144+ EMPs: 251.80 (121.2–499.3) × 103/mL; associated with oxidative stress and MetS and negatively correlated with HDLC levels | ||
| DM with ACS | (5) CD144+EMPs: 442.27 (154.2–826.9) × 103/mL | [6] | |
|
| |||
| CD146 | DM with MetS | Associated with the development of MetS | [59] |
3.1. DM-Induced Macrovascular and Microvascular Complications
Endothelial dysfunction is a crucial pathogenic mechanism in the progression of DM-related macrovascular and microvascular complications. In fact, EMPs facilitate the differentiation of macrovascular from microvascular complications in clinical practice. The plasma levels of CD31+/CD42b− EMPs and CD31+/AV+ EMPs were significantly higher in DM patients with macrovascular complications compared with patients showing microvascular complications. The study found that CD31+/AV+ EMPs, duration of DM, and BMI were independent variables predictive of macrovascular complications. Independent variables predictive of microvascular complications included HbA1c and duration of DM. Therefore, altered plasma EMP levels are independent risk factors for T2DM complicated by macrovascular complications. Furthermore, EMP levels show higher prognostic accuracy compared with conventional vascular risk factors and blood glucose levels [40].
3.2. DM Complicated with Cardiovascular Diseases
Diabetes is a major risk factor for cardiovascular diseases, which in turn aggravate the incidence and progression of DM. Studies reported that 75% of DM cases are complicated with hypertension [38]. The plasma levels of EMPs were significantly higher in T2DM patients complicated with hypertension compared with those without hypertension [8]. The study found that systolic blood pressure, diastolic blood pressure, and mean arterial pressure were all positively correlated with plasma EMP levels. After controlling for lipid levels and factors related to blood glucose, we found that the EMP level was still positively correlated with systolic blood pressure and mean arterial pressure. Therefore, EMP concentration is a potential risk factor for cardiovascular injury in DM patients, which in turn is closely associated with the incidence of hypertension and arterial wall stiffness [38].
Compared with healthy populations, the prevalence of hypertension and other cardiovascular diseases is significantly higher in DM patients and increases the risk of atherosclerosis [5]. However, not all patients with atherosclerosis manifest clinical symptoms, which may contribute to progression and catastrophic cardiovascular events. The plasma level of CD62+ EMPs was significantly lower in T2DM patients complicated with asymptomatic atherosclerosis compared with T2DM patients without atherosclerosis. Multivariate analysis revealed that CD62E+ EMPs act as potential prognostic indicators for T2DM complicated with asymptomatic atherosclerosis, providing an early biomarker for treatment. Compared with healthy population, patients with T2DM also exhibited significantly elevated plasma levels of CD144+ EMPs. The CD144+ EMP level is a stronger risk factor for T2DM complicated with CAD, compared with other conventional risk factors. In addition, the level of plasma CD144+ EMPs represents a biomarker for the diagnosis of T2DM complicated with CAD without typical angina. Therefore, plasma CD144+ EMPs not only contribute to endothelial dysfunction but also serve as a risk factor for the differential diagnosis and treatment of T2DM complicated with CAD [6].
3.3. Diabetic Nephropathy
Diabetic nephropathy is a leading cause of renal failure and almost 30% of T2DM patients suffer from diabetic nephropathy [41]. The plasma level of EMPs was elevated in T2DM patients complicated with diabetic nephropathy compared with T2DM patients without renal complications. Further, the plasma level of EMPs was significantly decreased by sarpogrelate hydrochloride, a blocker of serotonin-induced platelet aggregation [42]. Therefore, plasma EMPs may be potential biomarkers for DM-induced vascular complications, especially diabetic nephropathy.
3.4. DM-Induced Retinopathy
Diabetic retinopathy remains the primary cause of blindness in adults [43]. The incidence of DM-induced retinopathy is strongly associated with the activation or apoptosis of retinal nerve and vascular endothelial cells [44]. Changes in plasma and intravitreous MPs have been widely investigated in DM patients with retinal nerve degeneration to detect apoptosis of retinal neurons. A few retina-derived EMPs (PNA+ or ILB4+ MPs) are absent from the plasma of patients with DM-induced retinopathy. In contrast, the intravitreous level of CD144+ EMPs was elevated in DM patients complicated with retinopathy compared with DM patients without retinopathy. Further, platelet-derived MPs account for a larger proportion of the total MPs in DM retinopathy patients, whereas EMPs represent a lower percentage. However, the CD144+ EMPs represent the largest MP subtype in the vitreous body of DM patients complicated with retinopathy, and CD144+ EMP concentration differs significantly from the plasma levels. Bevacizumab therapy significantly reduces intravitreous CD144+ EMP levels in DM patients with retinopathy, a finding that may be used to gauge treatment response and disease progression [45].
3.5. DM Complicated with Erectile Dysfunction
The incidence of ED is three times higher in DM patients compared with age-matched healthy adults. The plasma levels of CD62E+ EMPs were significantly higher in both DM and non-DM patients diagnosed with ED than in control non-DM population without ED, while CD62E+ EMP levels did not differ between ED patients with and without DM. Thus, elevated CD62E+ EMPs appear to be specific for ED independent of DM. In contrast, the CD31+ EMP level was considerably higher in DM patients complicated with ED than in non-DM patients with ED, although the level in the latter population was still significantly higher than in adults without DM or ED. A high level of CD62E+ and CD31+ EMPs reflects endothelial cell activation, and a low level suggests apoptosis. The proportion is low (20%) in DM patients complicated with ED, suggesting that DM complicated with ED enhances endothelial cell apoptosis [21, 46].
3.6. DM and Metabolic Syndrome
Despite similarities, the EMP profile is different between DM and metabolic syndrome. Compared with non-DM metabolic syndrome, the plasma percentage of combined CD62E+ and CD31+ EMPs was significantly downregulated in T2DM, suggesting that a majority of plasma EMPs are released from apoptotic endothelial cells rather than activated endothelial cells in T2DM patients. Statistical analysis revealed that T2DM, hs-CRP, OPG, and adiponectin are independent factors influencing the decrease in plasma CD62E+ plus CD31+ EMPs in T2DM, suggesting a role in accelerated endothelial cell apoptosis [22].
4. Changes in MicroRNA Levels within Plasma EMPs of DM Patients
The mechanisms controlling the formation, release, and content of MPs are critical issues. Protein, lipid, and RNA levels within EMPs mediate intercellular signaling under physiological and pathological conditions. Studies have shown that endothelial cells possess significantly different miRNA patterns and seem to selectively pack their EMPs with distinct miRNAs in different pathological states [47, 48]. MiRNAs have been implicated in the epigenetic regulation of key metabolic homeostasis including glucose-induced insulin secretion, lipid metabolism, adipose cell differentiation, and inflammatory and antiangiogenic pathways in T2DM and related complications [49]. Nine miRNAs including miR-126, miR-222, miR-let7d, miR-21, miR-30, miR-92a, miR-139, miR-199a, and miR-26a regulate vascular homeostasis. The miR-126 and miR-26a were significantly reduced in DM patients compared with non-DM patients. Patients with low miR-26a and miR-126 levels were at a higher risk for concomitant CAD. Endothelial cells are the major cell sources of MPs containing miR-126 and miR-26a, respectively. Finally, consistent with our clinical results, in vitro studies suggest that hyperglycemia reduces the assembly of miR-126 and miR-26a into EMPs [28, 49]. These findings suggest that miRNA is selectively incorporated into EMPs under certain pathophysiological conditions. Increasing evidence suggests the potential role of EMP-associated miRNA signatures in body fluids or peripheral blood as biomarkers that predict metabolic diseases [35].
5. Plasma EMPs Are Altered in Response to Therapy
Plasma EMP levels are altered following treatment with insulin, sulfonylurea, biguanide, or thiazolidinedione. As illustrated in Table 4, pioglitazone effectively reduced the plasma level of CD31+ EMPs compared with metformin and significantly improved the risk factors for CAD in T2DM patients. In addition, a decrease in the plasma CD31+ EMPs level was strongly correlated with an increase in adiponectin level and decline in C-reactive protein expression in univariate analysis and further correlated with the level of adiponectin and C-reactive protein in multivariate analysis [34].
Table 4.
The effects of drugs on plasma levels of EMPs in patients with DM.
| Pharmacological effects | Drugs | Patient or cells | The effects of drugs on EMPs | References |
|---|---|---|---|---|
| Antihypertensive | Nifedipine | T2DM with hypertension | Decrease | [50] |
| Losartan | T2DM with hypertension | Decrease | [51] | |
|
| ||||
| Antiatherosclerosis | Simvastatin | HUVEC | Increase | [60] |
| Simvastatin + losartan | T2DM with hyperlipidemia and hypertension | Decrease | [51] | |
| Eicosapentaenoic acid | T2DM with hyperlipidemia | Decrease | [52] | |
| Vitamin C | T2DM with acute myocardial infarction | Decrease | [33] | |
|
| ||||
| Antihyperglycemic | Pioglitazone | T2DM | Decrease | [34] |
The levels of plasma EMPs are significantly higher in hypertensive patients with DM than in normotensive and non-DM controls. Although the levels in total cholesterol, triglycerides, hemoglobin A1c, fasting glucose, and body weight did not demonstrate any differences after CR nifedipine administration, the plasma EMPs decreased significantly in hypertensive patients with DM after 3 months of nifedipine CR (controlled release nifedipine: 20 mg/day) treatment [50]. In addition, losartan also significantly decreased the level of plasma EMPs in T2DM patients with hypertension at a dose of 50 mg/d for 24 weeks. Simvastatin significantly decreased the level of plasma EMPs in T2DM patients with hypertension and hyperlipidemia at a dose of 10 mg/d for 24 weeks [51].
The study found that the level of plasma EMPs was decreased significantly in DM patients with hyperlipidemia and high angiopoietin-2 (Ang-2) level (Ang-2 ≥ 3.6 ng/mL) after 6 months of eicosapentaenoic acid (EPA) treatment. Compared with the control group, the level of plasma EMPs in patients with low Ang-2 level (<3.6 ng/mL) after 6 months of EPA treatment and in patients with high Ang-2 level after 3 months of EPA treatment showed no significant difference [52]. In summary, altered plasma EMP levels correspond to changes in pathophysiology following treatment, which suggests that EMPs are potential biomarkers in DM therapy.
6. Conclusion
Despite unclear mechanisms and carrier information of EMPs in DM patients, there is no doubt that EMPs act as biomarkers of endothelial cell function during the pathological progression of DM and related vascular diseases. Furthermore, EMPs are promising diagnostic markers of disease progression, treatment, and clinical prognosis of DM and associated vascular illnesses.
Competing Interests
The authors declare that they have no competing interests.
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