<?xml version="1.0" encoding="UTF-8"?><!DOCTYPE article  PUBLIC "-//NLM//DTD Journal Publishing DTD v3.0 20080202//EN" "http://dtd.nlm.nih.gov/publishing/3.0/journalpublishing3.dtd"><article xmlns:mml="http://www.w3.org/1998/Math/MathML" xmlns:xlink="http://www.w3.org/1999/xlink" dtd-version="3.0" xml:lang="en" article-type="research article"><front><journal-meta><journal-id journal-id-type="publisher-id">IJCM</journal-id><journal-title-group><journal-title>International Journal of Clinical Medicine</journal-title></journal-title-group><issn pub-type="epub">2158-284X</issn><publisher><publisher-name>Scientific Research Publishing</publisher-name></publisher></journal-meta><article-meta><article-id pub-id-type="doi">10.4236/ijcm.2019.104022</article-id><article-id pub-id-type="publisher-id">IJCM-91809</article-id><article-categories><subj-group subj-group-type="heading"><subject>Articles</subject></subj-group><subj-group subj-group-type="Discipline-v2"><subject>Medicine&amp;Healthcare</subject></subj-group></article-categories><title-group><article-title>
 
 
  Discussion on the Effectiveness of Elevating HDL-C in Treating Cardiovascular Diseases of Patients with Type 2 Diabetes Mellitus
 
</article-title></title-group><contrib-group><contrib contrib-type="author" xlink:type="simple"><name name-style="western"><surname>Shasha</surname><given-names>Wang</given-names></name><xref ref-type="aff" rid="aff1"><sup>1</sup></xref><xref ref-type="corresp" rid="cor1"><sup>*</sup></xref></contrib><contrib contrib-type="author" xlink:type="simple"><name name-style="western"><surname>Liyue</surname><given-names>Wang</given-names></name><xref ref-type="aff" rid="aff2"><sup>2</sup></xref></contrib></contrib-group><aff id="aff1"><addr-line>Medical College, Wuhan University of Science and Technology, Wuhan, China</addr-line></aff><aff id="aff2"><addr-line>Puren Hospital Affiliated to Wuhan University of Science and Technology, Internal Medicine-Cardiovascular 
Department, Wuhan, China</addr-line></aff><pub-date pub-type="epub"><day>03</day><month>04</month><year>2019</year></pub-date><volume>10</volume><issue>04</issue><fpage>293</fpage><lpage>305</lpage><history><date date-type="received"><day>2,</day>	<month>March</month>	<year>2019</year></date><date date-type="rev-recd"><day>13,</day>	<month>April</month>	<year>2019</year>	</date><date date-type="accepted"><day>16,</day>	<month>April</month>	<year>2019</year></date></history><permissions><copyright-statement>&#169; Copyright  2014 by authors and Scientific Research Publishing Inc. </copyright-statement><copyright-year>2014</copyright-year><license><license-p>This work is licensed under the Creative Commons Attribution International License (CC BY). http://creativecommons.org/licenses/by/4.0/</license-p></license></permissions><abstract><p>
 
 
   
   High density lipoprotein protects cardiovascular diseases and reduces the risk of cardiovascular diseases through cholesterol reverse transport and other mechanisms. High-density lipoprotein cholesterol (HDL-C) is an independent predictor of negative events in cardiovascular diseases. Low concentration of HDL-C indicates abnormal regulation of HDL anabolism. Various proteins and receptors such as cholesteryl ester transfer protein (CETP) are involved in HDL anabolism. Type 2 Diabetes Mullitu and its related metabolic syndrome, chronic inflammation as well as oxidative stress not only affect the proteins and receptors related to HDL anabolism, but also affect their functional changes, making HDL change from anti-inflammatory, antioxidant, protecting endothelial cell function to pro-inflammatory, pro-oxidative and pro-endothelial cell apoptosis. This article will describe the relationship between HDL-C, type 2 diabetes and cardiovascular diseases from the effects of T2DM on HDL anabolism and function, and further explore the effectiveness of elevating HDL-C in treating cardiovascular diseases of patients with type 2 diabetes. 
  
 
</p></abstract><kwd-group><kwd>HDL</kwd><kwd> Type 2 Diabetes Mellitus</kwd><kwd> Cardiovascular Diseases</kwd><kwd> Reverse Cholesterol Transport</kwd></kwd-group></article-meta></front><body><sec id="s1"><title>1. Introduction</title><p>Patients with diabetes mellitus are high-risk groups for cardiovascular and cerebrovascular diseases. The risk of cardiovascular and cerebrovascular diseases in patients with diabetes mellitus is 2 - 4 times higher than that of non-patients with diabetes mellitus. Compared with non-patients with diabetes mellitus with coronary heart disease, patients with diabetes mellitus with coronary heart disease account for 67% of coronary heart disease-related deaths. About 84% of patients with diabetes mellitus aged over 65 die from cardiovascular and cerebrovascular events [<xref ref-type="bibr" rid="scirp.91809-ref1">1</xref>]. Therefore, diabetes patients, a large group of people, have attracted extensive attention. Both type 2 diabetes mellitus and its metabolic syndrome can affect HDL [<xref ref-type="bibr" rid="scirp.91809-ref2">2</xref>]. Moreover, chronic inflammation, oxidative stress and other factors of diabetes can lead to changes in HDL serum concentration, structure and function, and even change from functional HDL with anti-inflammation, anti-oxidation, anti-apoptosis and anti-thrombosis to dysfunction HDL with pro-inflammation, pro-oxidation, pro-apoptosis and pro-thrombosis functions, thus increasing the risk of cardiovascular diseases. As a result, the effectiveness of elevating HDL-C as a therapeutic target to reduce the risk of cardiovascular diseases in patients with type 2 diabetes mellitus has been widely questioned. This article will review the effectiveness of elevating HDL-C in treating cardiovascular diseases in patients with type 2 diabetes mellitus from the aspects of the effects of type 2 diabetes mellitus on HDL anabolism and function.</p></sec><sec id="s2"><title>2. HDL</title><sec id="s2_1"><title>2.1. Structure</title><p>In plasma, HDL is the lipoprotein with the largest density and the smallest volume in human body (Density: 1.063 - 1.21 g/ml) [<xref ref-type="bibr" rid="scirp.91809-ref3">3</xref>]. The main protein component of HDL is apolipoprotein A-I(apo A-I), accounting for about 70%. Therefore, apo A-I is closely related to HDL-C concentration. Proteomics research continues to expand apolipoprotein spectrum and other related protein components in HDL [<xref ref-type="bibr" rid="scirp.91809-ref4">4</xref>]. HDL lipids are mainly free or esterified fatty acids, phospholipids and different ceramides and sphingolipids [<xref ref-type="bibr" rid="scirp.91809-ref5">5</xref>]. Unlike other apolipoproteins, HDL exists as apolipoprotein precursor particles rather than mature apolipoproteins. These particles are mostly disk-shaped and consist of phospholipid bilayers and apolipoprotein stabilized unesterified cholesterol [<xref ref-type="bibr" rid="scirp.91809-ref6">6</xref>]. There are many subgroups of HDL, which are classified by volume: HDL3c, HDL3b, HDL3a, HDL2a, HDL2b; According to density, there are HDL2 (d = 1.063 - 1.125 g/ml), HDL3 (d = 1.125 - 1.21 g/ml), etc. [<xref ref-type="bibr" rid="scirp.91809-ref7">7</xref>].</p></sec><sec id="s2_2"><title>2.2. Synthesis and Decomposition of HDL and Its Function-Related Proteins</title><p>The HDL subgroups increase or eliminate the neutral lipids, phospholipids in the components under the reaction of related proteins to undergo reconstruction or transformation, and proteins involved in HDL synthesis and decomposition and function-related include:</p><sec id="s2_2_1"><title>2.2.1. Serum Amyloid A (SAA)</title><p>SAA competitively combines with apo A-I and HDL, and can become the main protein component of HDL. HDL containing SAA mediates the decrease of cholesterol outflow activity [<xref ref-type="bibr" rid="scirp.91809-ref8">8</xref>] and is easier to be cleared by kidney. It has been reported that SAA has a certain role in the development of plaque.</p></sec><sec id="s2_2_2"><title>2.2.2. CETP</title><p>CETP mediates the exchange of cholesteryl esters in HDL with triglyceride-rich lipoproteins to promote the reverse transport of cholesterol, so that the increase of TG component in HDL increases the catabolism and leads to a decrease in HDL-C concentration.</p></sec><sec id="s2_2_3"><title>2.2.3. Endothelial Lipase (EL)</title><p>EL is consistent with liver lipase and lipoproteinase, and tends to hydrolyze triglyceride-rich lipoproteins. Current experimental studies have shown that overexpression of adenovirus gene into EL reduces the cholesterol component and phospholipid component of HDL.</p></sec><sec id="s2_2_4"><title>2.2.4. Lecithin: Cholesterol Acytransferase (LCAT)</title><p>LCAT needs to transfer sn-2-acyl of lecithin to cholesterol under the action of apo A-I co-activation factor, so as to convert free cholesterol in HDL into cholesteryl ester. This process retains the core of HDL particles, and converts naive HDL into spherical particles, which is especially important for reverse cholesterol transport process.</p></sec><sec id="s2_2_5"><title>2.2.5. Paraoxonase (PON)</title><p>PON1 is an enzyme related to HDL which can protect LDL from oxidation as well as an important mechanism for HDL to resist atherosclerosis. The reduction of PON1 can reduce HDL antioxidant function [<xref ref-type="bibr" rid="scirp.91809-ref9">9</xref>]. Moreover, HDL-PON can decompose peroxides on the surface of cell membrane. Some researchers have found that there is a negative correlation between HDL-PON activity and HDL peroxide level, which proves that PON not only reduces LDL and membrane oxidation, but also reduces HDL oxidation.</p></sec><sec id="s2_2_6"><title>2.2.6. ATP-Binding Cassette Transporter A1 and G1 (ABCA1/ABCG1)</title><p>ABCA1 plays an important role in reverse cholesterol transport and HDL synthesis. ABCA1 promotes cholesterol efflux process (at least lipid apo A-I from cells) by consuming ATP to participate in cholesterol reverse transport process. The role of ABCG1 is to re-esterify apo A-I produced by ABCA1 pathway through energy consumption mediated lipid outflow.</p></sec></sec><sec id="s2_3"><title>2.3. HDL―Cholesterol Reverse Transport</title><p>Apo A-I, the skeleton of HDL protein, is mainly synthesized and secreted into circulation by liver and intestinal tract, and combines free phospholipids, cholesterol and triglycerides to form juvenile HDL particles [<xref ref-type="bibr" rid="scirp.91809-ref10">10</xref>]. Juvenile HDL is bound to the surface of peripheral tissues such as macrophages ABCA1 activates intracellular cholesterol ester hydrolase to produce free cholesterol, which is transported to juvenile HDL [<xref ref-type="bibr" rid="scirp.91809-ref11">11</xref>], and forms cholesterol ester after LCAT catalysis, making it easier to embed into HDL core. This process converts low-fat HDL precursor particles into lipid-rich HDL (mature HDL) [<xref ref-type="bibr" rid="scirp.91809-ref12">12</xref>]. Subsequent mature HDL is released into the circulation and reaches the liver in combination with scavenger receptor-B1 (SR-B1), making HDL lipid components more susceptible to hydrolysis by lipases such as hepatic lipase to unload their lipid components [<xref ref-type="bibr" rid="scirp.91809-ref13">13</xref>]. Subsequently, lipid-poor HDL is released into the circulation to repeat the above-mentioned cholesterol transport process [<xref ref-type="bibr" rid="scirp.91809-ref14">14</xref>], which is the reverse transport of cholesterol―HDL removes excess cholesterol from the periphery and transports it to the liver for metabolism or to steroid synthesis organs for steroid hormonessynthesis. Thus, HDL prevents lipid toxicity and reduces the formation of foam cells, thereby reducing the formation of atherosclerotic plaque and reducing the risk of cardiovascular events [<xref ref-type="bibr" rid="scirp.91809-ref15">15</xref>].</p></sec></sec><sec id="s3"><title>3. HDL, Diabetes Mellitus and Cardiovascular Diseases</title><p>Cardiovascular diseases are still the leading cause of death in many developed and developing countries [<xref ref-type="bibr" rid="scirp.91809-ref12">12</xref>]. HDL’s reverse cholesterol transport, anti-inflammatory [<xref ref-type="bibr" rid="scirp.91809-ref16">16</xref>], antioxidant and other functions play a great role in cardiovascular protection [<xref ref-type="bibr" rid="scirp.91809-ref17">17</xref>]. Type 2 diabetes mellitus and its metabolic syndrome affect HDL concentration and function in many ways.</p><sec id="s3_1"><title>3.1. Changes in Anabolism and Catabolism</title><p>Changes in anabolism and catabolism of HDL are accompanying insulin resistance, resulting in HDL synthesis with little triglyceride and little cholesterol ester, non-enzymatic saccharification of apo A-I and other HDL related proteins, oxidative modification of HDL lipids, apolipoproteins and enzymes, etc. [<xref ref-type="bibr" rid="scirp.91809-ref18">18</xref>].</p><sec id="s3_1_1"><title>3.1.1. Proteomic Changes</title><p>Chronic inflammation in patients with type 2 diabetes mellitus increases SAA [<xref ref-type="bibr" rid="scirp.91809-ref19">19</xref>]. SAA replaces apo A-I from HDL surface, and SAA-rich HDL is more susceptible to hydrolytic metabolism. Oxidative stress in patients with diabetes mellitus is increasing, resulting in a decrease in HDL-related proteins apo A-I and PON1.</p></sec><sec id="s3_1_2"><title>3.1.2. Lipid Histological Changes</title><p>Insulin resistance and T2DM can increase the level of TG. Hypertriglyceridemia increases CETP-mediated transesterification of TG-rich lipoprotein and HDL cholesterol, which increases the content of TG-rich HDL (poor stability and loose binding with Apo-A1) in circulation and accelerates renal excretion [<xref ref-type="bibr" rid="scirp.91809-ref20">20</xref>]. Phospholipids in T2DM have changed, and the ratio of sphingomyelin/lecithin (the main determinant of HDL antioxidant function) has increased.</p></sec></sec><sec id="s3_2"><title>3.2. Functional Changes</title><p>The function of HDL depends on the shape of HDL (spherical shape is better than discoid shape [<xref ref-type="bibr" rid="scirp.91809-ref21">21</xref>]), the size and composition of HDL (fatty acid composition/triglyceride content [<xref ref-type="bibr" rid="scirp.91809-ref22">22</xref>], glycated protein, peroxide protein).</p><sec id="s3_2_1"><title>3.2.1. Impaired Reverse Cholesterol Transport Function</title><p>ABCA1 and ABCG1 are key components in cholesterol reverse transport. Their expression in macrophages up-regulates lipid loading [<xref ref-type="bibr" rid="scirp.91809-ref23">23</xref>], while ABCA1 mediates cholesterol and phospholipid efflux to apo A-I, and phospholipids and cholesterol in mature HDL are mainly derived from ABCG1-mediated lipid efflux [<xref ref-type="bibr" rid="scirp.91809-ref24">24</xref>]. Mauldin et al. [<xref ref-type="bibr" rid="scirp.91809-ref25">25</xref>] demonstrated that hyperglycemia resulted in decreased ABCG1 expression and impaired function of macrophages in a mouse model of type 2 diabetes mellitus. In vitro experiments, RAW264.7 macrophages and HepG2 hepatocytes were incubated in unsaturated fatty acid medium, and the expression of ABCA1 mRNA and protein were both down-regulated [<xref ref-type="bibr" rid="scirp.91809-ref26">26</xref>]. Significantly elevated unsaturated fatty acids in patients with diabetes mellitus have been shown to phosphorylate ABCA1 through phospholipase D2 pathway and reduce its stability, thus affecting its function [<xref ref-type="bibr" rid="scirp.91809-ref27">27</xref>] and reducing cholesterol reverse transport. The increased SAA in T2DM patients binds to HDL and increases its affinity to macrophages by 3 to 4 times, while the affinity to hepatocytes decreases. The difference in affinity may lead to HDL switching from liver to macrophage clearance, which may be closely related to HDL’s anti-atherosclerosis and anti-inflammatory properties changing to atherosclerosis promoting properties [<xref ref-type="bibr" rid="scirp.91809-ref8">8</xref>]. In addition, SAA has been shown to reduce HDL subpopulations and promote cholesterol outflow [<xref ref-type="bibr" rid="scirp.91809-ref28">28</xref>]. Advanced glycation products (AGEs) formed in patients with diabetes mellitus are increased, and AGE precursors hinder ABCA1-dependent intracellular cholesterol efflux [<xref ref-type="bibr" rid="scirp.91809-ref29">29</xref>]. In addition, AGEs [<xref ref-type="bibr" rid="scirp.91809-ref30">30</xref>] were also detected from lipoprotein isolated from diabetic subjects. The increase in apo A-I carbonyl modification associated with AGEs [<xref ref-type="bibr" rid="scirp.91809-ref30">30</xref>] may be related to abnormal HDL metabolism. A recent study shows that inflammation destroys many components of HDL cholesterol transport and efflux function [<xref ref-type="bibr" rid="scirp.91809-ref31">31</xref>]. Inflammation-induced down regulation of bile transporters ABCG5, ABCG8 and ABCB11 in the liver results in impaired cholesterol metabolism through the liver. The above-mentioned various mechanisms damage the reverse cholesterol transport process.</p></sec><sec id="s3_2_2"><title>3.2.2. Impaired Antioxidant Function</title><p>Chronic inflammation induces the secretion of myeloperoxidase (MPO), and MPO activity increases in HDL in patients with type 2 diabetes mellitus [<xref ref-type="bibr" rid="scirp.91809-ref32">32</xref>]. MPO has been proved to selectively catalyzenitrosation, chlorination, oxidation of Apo-A1, and oxidized apo A-I selectively inhibit ABCA1-dependent cholesterol outflow process [<xref ref-type="bibr" rid="scirp.91809-ref33">33</xref>]. Apo A-I has a pro-inflammatory effect after oxidation by MPO. Oxidative modification of HDL apolipoproteins and enzymes in patients with diabetes [<xref ref-type="bibr" rid="scirp.91809-ref22">22</xref>] and increased sphingomyelin/phosphatidylcholine ratios lead to an increase in the surface hardness of HDL (a key antioxidant factor [<xref ref-type="bibr" rid="scirp.91809-ref34">34</xref>] ), which reduces their antioxidant activity. The content of very low density lipoprotein increases in type 2 diabetes mellitus, which is proved to be an effective LCAT activity inhibitor [<xref ref-type="bibr" rid="scirp.91809-ref35">35</xref>]. In addition to its importance in reverse cholesterol transport, LCAT can hydrolyze platelet activating factor (PAF) [<xref ref-type="bibr" rid="scirp.91809-ref36">36</xref>] [<xref ref-type="bibr" rid="scirp.91809-ref37">37</xref>] and phosphatidylcholine produced during lipoprotein oxidation, eliminating its pro-inflammatory function and cytotoxicity. In addition to its antioxidant properties, LCAT has an effect on the concentration of PON1 and PAF acetylhydrolase [<xref ref-type="bibr" rid="scirp.91809-ref38">38</xref>]. This indicates that LCAT plays an important role in the reverse cholesterol transport and HDL antioxidant function.</p><p>The anti-atherosclerosis effect of HDL is closely related to the regulation of LDL and cell membrane oxidation by PON1. Increased oxidative stress in T2DM reduces the concentration of PON1 [<xref ref-type="bibr" rid="scirp.91809-ref39">39</xref>], which is 40% of that in non-patients with diabetes mellitus [<xref ref-type="bibr" rid="scirp.91809-ref40">40</xref>]. PON1 inhibits the production of monocyte chemotactic protein 1 (MCP1) mediated by oxLDL through endothelial cells [<xref ref-type="bibr" rid="scirp.91809-ref41">41</xref>]. MCP1 induces monocytes to recruit subcutaneously, which lays a foundation for the occurrence of atherosclerosis. The protective effect of PON1 transfected cells and PON1 transgenic mice on macrophage oxidative stress [<xref ref-type="bibr" rid="scirp.91809-ref42">42</xref>] reduces the formation of atherosclerotic lesions [<xref ref-type="bibr" rid="scirp.91809-ref43">43</xref>], and PON1 deficiency is found to be related to macrophage oxidative stress and increased atherosclerosis [<xref ref-type="bibr" rid="scirp.91809-ref44">44</xref>]. The more peroxide components in HDL, the lower HDL-PON activity [<xref ref-type="bibr" rid="scirp.91809-ref45">45</xref>]. In short, the decrease of PON activity and HDL anti-membrane and LDL oxidation protection in patients with diabetes mellitus accelerates atherosclerosis in patients with diabetes mellitus.</p></sec><sec id="s3_2_3"><title>3.2.3. Impaired Endothelial Protective Function</title><p>Some studies have found that the protective effect of HDL on vascular endothelium is obviously impaired in patients with T2DM [<xref ref-type="bibr" rid="scirp.91809-ref32">32</xref>]. Pers&#233;gol et al. [<xref ref-type="bibr" rid="scirp.91809-ref46">46</xref>] proved that HDL lipid peroxidation and myeloperoxidase (MPO) activity increased in patients with T2DM, and the ability of resisting oxidized low density lipoprotein to inhibit endothelium-dependent vasodilation was impaired. Increased MPO can increases endothelial dysfunction [<xref ref-type="bibr" rid="scirp.91809-ref47">47</xref>] [<xref ref-type="bibr" rid="scirp.91809-ref48">48</xref>] and coronary heart disease risk [<xref ref-type="bibr" rid="scirp.91809-ref49">49</xref>]. In vitro studies have shown that HDL isolated from healthy individuals incubates endothelial cells and found that HDL could induce the expression of endothelial NO synthase (eNOS). However, the loss of HDL vasodilation function in patients with T2DM is due to the reduction of NO production and endothelium-dependent relaxation function. Moreover, in patients with diabetes and coronary heart disease, HDL’s function of inhibiting expression of endothelial intercellular adhesion molecule-1 (VCAM-1) is absent, thus macrophages are more likely to adhere to activated vascular endothelial cells [<xref ref-type="bibr" rid="scirp.91809-ref47">47</xref>], and endothelium is more likely to be damaged. Recent studies have shown that HDL endothelial protective function mainly increases the number of serum endothelial progenitor cells (EPCs) [<xref ref-type="bibr" rid="scirp.91809-ref50">50</xref>] and accelerates endothelial cell neogenesis. Some studies have found that HDL loss from T2DM patients with coronary heart disease inhibits endothelial cell apoptosis because it cannot activate anti-apoptotic proteins and stimulate the pro-apoptotic pathway. In vitro, cardiomyocytes are incubated with high glucose, and HDL supplementation can offset the apoptosis-promoting effect of some high glucose on cardiomyocytes. In healthy control group and patients with diabetes mellitus, low HDL is an independent risk factor for endothelial dysfunction [<xref ref-type="bibr" rid="scirp.91809-ref51">51</xref>].</p></sec></sec></sec><sec id="s4"><title>4. Diabetes Mellitus and Coronary Heart Disease</title><p>Numerous epidemiological studies have shown that diabetes is one of the independent risk factors for cardiovascular diseases. Endothelial dysfunction plays an important role in the pathogenesis of microangiopathy in patients with diabetes mellitus [<xref ref-type="bibr" rid="scirp.91809-ref52">52</xref>], and is the main cause of diabetes morbidity and mortality. At the early stage of atherosclerosis formation, endothelial dysfunction already exists, while there is no obvious morphological change in vascular wall at this time. Endothelial dysfunction is common in patients with diabetes mellitus. eNOS expression is down-regulated, NO synthesis is reduced, and endothelium-dependent vasodilation is abnormal [<xref ref-type="bibr" rid="scirp.91809-ref53">53</xref>]. Diabetes-related hyperglycemia and increase of angiotensin II (Ang II) can increase reactive oxygen species (ROS) in circulation. Oxidative stress causes endothelial dysfunction [<xref ref-type="bibr" rid="scirp.91809-ref54">54</xref>], partly due to NO degradation. NO has important antithrombotic, anti-apoptosis and anti-inflammatory functions. This makes people wonder whether other functions such as anti-inflammatory function and anti-apoptosis function are also changed after vascular endothelial relaxation dysfunction. A large number of studies have shown that activation of angiotensin II type 1 receptor (AT1R) increases vascular endothelial oxidation products and initiates apoptosis process, which promotes the occurrence and development of vascular endothelial dysfunction [<xref ref-type="bibr" rid="scirp.91809-ref54">54</xref>]. The expression level of AT1R determines its biological activity. Currently, several known agonists include glucose, angiotensin II, insulin, reactive oxygen species and others including diabetes itself [<xref ref-type="bibr" rid="scirp.91809-ref53">53</xref>]. The understanding of up-regulation of AT1R expression and angiotensin II mediated signaling in patients with diabetes mellitus comes from the discovery that endothelial function is repaired after patients with diabetes mellitus use AT1R antagonist [<xref ref-type="bibr" rid="scirp.91809-ref55">55</xref>]. Some studies have found that endothelial progenitor cells (EPCs) are also targeted to repair damaged sites after vascular wall integrity is destroyed, in addition to repairing adjacent mature endothelial cells [<xref ref-type="bibr" rid="scirp.91809-ref56">56</xref>]. EPC is not only reduced in number but also impaired in function in patients with diabetes mellitus [<xref ref-type="bibr" rid="scirp.91809-ref57">57</xref>], which may be related to endothelial dysfunction [<xref ref-type="bibr" rid="scirp.91809-ref58">58</xref>]. Primary myocardial injury in patients with diabetic heart disease occurs before hypertension and coronary artery disease. Ventricular dysfunction in diabetic heart disease is mainly due to myocardial cell apoptosis, interstitial inflammatory reaction, myocardial cell hypertrophy, glycogen accumulation in myocardium, changes in myocardial extracellular matrix (interstitial and perivascular fibrosis), myocardial microvascular lesions, intracellular Ca<sup>2+</sup> abnormalities and endothelial cell dysfunction [<xref ref-type="bibr" rid="scirp.91809-ref59">59</xref>]. Some animal studies have found that cell apoptosis increases in diabetic animals induced by streptozotocin (STZ) [<xref ref-type="bibr" rid="scirp.91809-ref60">60</xref>], as well as in patients with diabetes mellitus [<xref ref-type="bibr" rid="scirp.91809-ref61">61</xref>]. Apoptosis is mainly due to increased oxidative stress caused by hyperglycemia. Hyperglycaemia not only increases the production of reactive oxygen species, but also inhibits the production of antioxidant enzymes [<xref ref-type="bibr" rid="scirp.91809-ref62">62</xref>]. In addition to inducing lipid peroxidation, ROS can also change cell proteins and initiate various stress signal pathways, such as Erk, JNK and p38 MAPK. Activation of cardiac p38 MAPK is of pathological importance in diabetic heart disease, which indicates that inhibition of p38 MAPK can improve STZ-induced left ventricular dysfunction in diabetic mice [<xref ref-type="bibr" rid="scirp.91809-ref63">63</xref>]. It has been confirmed in transgenic and knockout animal models that antioxidant enzymes superoxide dismutase (SOD), SOD-1, SOD-2, and extracellular (ec)-SOD convert O<sub>2</sub>-anions into oxygen molecules and hydrogen peroxide [<xref ref-type="bibr" rid="scirp.91809-ref64">64</xref>], and SOD-2 is the same in patients with diabetes mellitus [<xref ref-type="bibr" rid="scirp.91809-ref65">65</xref>]. In the heart, overexpression of ec-SOD reduces macrophage infiltration and fibrosis, and improves left ventricular dysfunction [<xref ref-type="bibr" rid="scirp.91809-ref64">64</xref>], while up-regulation of SOD-2 expression can prevent apoptosis induction and protect mitochondrial respiratory function [<xref ref-type="bibr" rid="scirp.91809-ref66">66</xref>].</p></sec><sec id="s5"><title>5. Conclusion</title><p>To sum up, HDL has long been considered as a protective component of cardiovascular diseases, and HDL-C concentration is a good predictor of cardiovascular disease risk factors. Type 2 diabetes mellitus affects HDL metabolism and thus reduces HDL-C concentration, but increasing HDL-C concentration with drugs has not been able to reduce the risk of cardiovascular events as scheduled. Not only that, T2DM changes HDL in size, shape and composition, thus changing its function and even transforming it from cardiovascular protective effects such as anti-inflammation, anti-apoptosis and antithrombotic to cardiovascular disease events such as pro-inflammation, pro-apoptosis and thrombosis. Therefore, we should not only pay attention to HDL-C concentration, but also pay attention to its morphology, composition and functional changes in the treatment of type 2 diabetes patients with cardiovascular diseases, which provides a new research direction for cardiovascular disease risk prediction and treatment targeting of patients with T2DM.</p></sec><sec id="s6"><title>Conflicts of Interest</title><p>The authors declare no conflicts of interest regarding the publication of this paper.</p></sec><sec id="s7"><title>Cite this paper</title><p>Wang, S.S. and Wang, L.Y. 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