Contrast-enhanced ultrasound imaging of the vasa vasorum of carotid artery plaque

The vasa vasorum of carotid artery plaque is a novel marker of accurately evaluating the vulnerability of carotid artery plaque, which was associated with symptomatic cerebrovascular and cardiovascular disease. The presence of ultrasound contrast agents in carotid artery plaque represents the presence of the vasa vasorum in carotid artery plaque because the ultrasoundcontrast agents are strict intravascular tracers. Therefore, contrast-enhanced ultrasound(CEUS) is a novel and safe imaging modality for evaluating the vasa vasorum in carotid artery plaque. However, there are some issues that needs to be assessed to embody fully the clinical utility of the vasa vasorum in carotid artery plaque with CEUS.

Vagina vasorum dissection during D2 lymphadenectomy for gastric carcinoma

AIM: To explore the relationship between metastasis and vagina vasorum in the progress of gastric carcinoma and to find some facts and references for gastric surgeons. METHODS: One hundred and seven specimens of left or right gastric arteries (55 left and 52 right) were gathered from 59 patients undergoing radical gastrectomy for gastric carcinoma. All the frozen specimens were cut into 3 μm-thick sections and stained with hematoxylin-eosin (HE) and immunohistochemical method separately. Cytokeratin (CK) and mesothelial cells (MC) were stained with immunohistochemical method. Cancer cells inside vagina vasorum were detected and the structure of artery wall was observed under microscope. RESULTS: Metastatic cancer cells or tubercles were found inside vagina vasorum in some stage Ⅲ or Ⅳ specimens, but not in stageⅠor Ⅱ specimens. Tumor cells in vagina vasorum were CK positive in 26 specimens of 14 tumors. Among them, stage Ⅲ was found in 4 specimens of 2 tumors, and stage Ⅳ in 22 specimens of 12 tumors. None of these specimens was positive for MC. The positive rate of CK increased with TNM staging. Compared with the lower part, tumors in the upper and middle parts of stomach were more likely to metastasize into vagina vasorum. CONCLUSION: Vagina vasorum dissection should be performed during D2 lymphadenectomy for TNM stage Ⅲ or Ⅳ gastric carcinoma.

The role of HSPB1 and ectopic F1Fo-ATPase interaction in hypoxia pulmonary hypertension vascular adventitial vasa vasorum remodeling

OBJECTIVE To investigate the role of adventitial vasa vasorum in artery remodeling during the process of pulmonary artery hypertension(PAH),we checked the small heat shock protein 27/25(HSPB1)whether involved in pathological basis of vascular remodeling.METHODS We explored the potential role of HSPB1 interacts with ectopic F1Fo-ATPase in the pulmonary vascular remodeling,investigate its effects on the endothelium cell dynamic,and further reveal its possible molecular mechanisms using hypoxic pulmonary hypertension rat model,transgenic mice and pulmonary adventitial vasa vasorum endothelial cell culture in vitro.RESULTS Our studies have shown that HSPB1 improves adventitial vasa vasorum angiogenesis and remodeling.We found that hypoxia induces-HSPB1 upregulation and HSPB1 interact with ectopic F1Fo-ATPase modulate adventitial vasa vasorum endothelial cell proliferation,migration and tube formation.And the inhibition of HSPB1can reverse the vascular inflammation and fibrosis amazingly.CONCLUSION Adventitial vasa vasorum plays an important role in vascular remodeling,and small heat shock protein 27/25 was involved in a variety of diseases during the development of PAH,which could an efficient therapeutic targets and prevention strategy for PAH clinical.

Quantification of Adventitial Vasa Vasorum Vascularization in Double-injury Restenotic Arteries

Background：Accumulating evidence indicates a potential role of adventitial vasa vasorum （VV） dysfunction in the pathophysiology of restenosis.However,characterization ofVV vascularization in restenotic arteries with primary lesions is still missing.In this study,we quantitatively evaluated the response of adventitial VV to vascular injury resulting from balloon angioplasty in diseased arteries.Methods：Primary atherosclerotic-like lesions were induced by the placement of an absorbable thread surrounding the carotid artery of New Zealand rabbits.Four weeks following double-injury induced that was induced by secondary balloon dilation,three-dimensional patterns of adventitial VV were reconstructed;the number,density,and endothelial surface of VV were quantified using micro-computed tomography.Histology and immunohistochemistry were performed in order to examine the development of intimal hyperplasia.Results：Results from our study suggest that double injured arteries have a greater number of VV,increased luminal surface,and an elevation in the intima/media ratio （I/M）,along with an accumulation ofmacrophages and smooth muscle cells in the intima,as compared to sham or single injury arteries.I/M and the number of VV were positively correlated （R^2 =0.82,P 〈 0.001）.Conclusions：Extensive adventitial VV neovascularization occurs in injured arteries after balloon angioplasty,which is associated with intimal hyperplasia.Quantitative assessment of adventitial VV response may provide insight into the basic biological process of postangioplasty restenosis.

辛伐他汀对动脉滋养管及内皮功能的影响

目的观察高脂血症对大鼠主动脉滋养血管及血管内皮生长因子(VEGF)的影响,探讨辛伐他汀逆转内皮功能障碍的机制。方法实验分3组:正常对照组、高脂血症组和高脂血症治疗组。高脂血症组持续高脂喂养,4周后其中高脂血症治疗组在高脂喂养同时喂服辛伐他汀10mg/g·d,而另一高脂血症组不予药物治疗,第20周检测3组的血脂变化,观察主动脉、滋养血管病理改变及VEGF和NO浓度。结果与正常对照组比较,高脂血症组主动脉壁内层、中层厚度、滋养层滋养血管密度均显著增高,而高脂血症组大鼠血NO水平较正常对照组明显降低,血VEGF与正常对照组相比无显著性差异;辛伐他汀治疗组动脉壁内层、中层厚度均显著小于高脂血症组,滋养血管密度显著高于高脂血症组,辛伐他汀治疗组血NO、VEGF水平明显高于高脂血症组,两者呈显著正相关。结论辛伐他汀有助于VEGF和NO浓度的升高及滋养血管的新生,可能有利于动脉内皮功能的修复。

桂芍通络对兔动脉粥样硬化早期外膜滋养血管新生及氧化应激水平的干预作用

目的观察桂芍通络对兔动脉粥样硬化早期外膜滋养血管新生及氧化应激的影响。方法 84只家兔随机分为正常组、高脂组、外膜损伤组、桂芍通络高剂量(GH)组、桂芍通络中剂量(GM)组、阿托伐他汀(ATO)组、通心络(TXL)组,每组各12只。正常组给予普通饲料,高脂组给予高脂饲料喂养建立早期高脂血症模型,外膜损伤组及各用药组实施高脂饮食复合右侧颈动脉硅胶管包裹术。GH组给予4.16 g(生药)·kg^(-1)·d^(-1)灌胃,GM组给予2.08 g(生药)·kg^(-1)·d^(-1)灌胃,ATO组给予阿托伐他汀2.5 mg·kg^(-1)·d^(-1)灌胃,TXL组给予通心络超微粉0.6 g·kg^(-1)·d^(-1)灌胃,连续给药4周后取材,生化法检测各组血脂4项水平变化;HE染色观察内中外膜病理形态学变化;检测血清超氧化物歧化酶(SOD)、丙二醛(MDA)、总抗氧化能力(T-AOC)表达水平;荧光原位杂交检测NADPH氧化酶亚单位p22phox和gp91phoxmRNA的定位与表达;Western blot检测颈动脉组织VEGF、VEGFR蛋白表达情况。结果与正常组相比,高脂组血清总胆固醇(TC)、甘油三酯(TG)及低密度脂蛋白(LDL-C)水平明显升高(P<0.01);外膜损伤组外膜新生滋养血管及VEGF、VEGFR-2蛋白表达均明显增加(P<0.01),与外膜损伤组比较,GH组、GM组、ATO组及TXL组术侧颈动脉损伤及滋养血管新生程度、颈动脉外膜NADPH氧化酶亚单位p22phox和gp91phoxmRNA均有不同程度减轻;SOD、T-AOC活力升高,MDA含量、颈动脉外膜VEGF、VEGFR蛋白表达水平降低(P<0.05或P<0.01)。结论桂芍通络具有抑制兔动脉粥样硬化早期血管外膜滋养血管新生的作用,其机制可能与提高血管本身及外膜的抗氧化能力有关。

曲张大隐静脉管壁滋养血管分布与定量研究

目的探讨在不同病期、不同部位血管壁中滋养血管变化与大隐静脉曲张(GSVV)病期的关系。方法 19例GSVV患者,其中曲张静脉伴皮肤营养改变9例(皮肤改变组),单纯曲张静脉10例(曲张组)。分别取其曲张大隐静脉主干上、中、下三段管壁标本,另设9例正常静脉作对照(对照组);行苏木素-伊红染色,观察管壁中的滋养血管分布和密度情况。结果皮肤改变组、曲张组外膜和中膜外层见滋养血管明显增多。滋养血管密度测定:皮肤改变组、曲张组管壁中滋养血管密度明显高于对照组,差异有统计学意义(P<0.05);三组内上、中、下三段各段间滋养血管密度差异均无统计学意义(P>0.05)。结论曲张大隐静脉主干管壁中滋养血管分布和密度与病期和部位不存在量的变化关系。曲张静脉管壁外膜和中膜滋养血管增多,推断可能与静脉高压、缺氧导致血管壁重塑有关。

四妙勇安汤调控滋养血管网重建稳定ApoE^(-/-)小鼠动脉粥样硬化易损斑块的实验研究

观察四妙勇安汤干预AS易损斑块的效应,并以滋养血管(Vasa Vasorum,VV)新生为切入点,进一步探讨其起效的机制和靶点。方法:将雄性Apo E-/-小鼠随机分模型组、辛伐他汀组、四妙勇安汤组,采用添加1.1%L-蛋氨酸的高脂饲料喂养8周,建立AS易损斑块模型,并以C57BL/6小鼠作为对照。连续给药8周后,采用HE染色观察斑块的病理形态;采用免疫组化法观察斑块内与主动脉外膜VV密度以及斑块内巨噬细胞的聚集情况;检测血清TC、TG、LDL-C、HDL-C等血脂变化;采用Western blot技术检测HIF-1α-Apelin/APJ信号通路的关键节点蛋白。四妙勇安汤能够显著改善小鼠主动脉斑块病理形态,减小斑块面积及斑块与管腔面积比,增加最小纤维帽厚度以稳定斑块,且四妙勇安汤对纤维帽厚度的改善明显优于辛伐他汀;可有效抑制斑块内与血管外膜VV新生,降低斑块内巨噬细胞含量。四妙勇安汤可有效降低小鼠血清TC、TG、LDL-C水平,但对血清HDL-C水平无明显的改善作用。四妙勇安汤可降低HIF-1α蛋白表达水平,且其作用优于辛伐他汀;下调主动脉Apelin蛋白、APJ蛋白表达水平;显著降低Phospho-MEK1/2(Ser217/221)、Phospho-p44/42 MAPK(Erk1/2)(Thr202/Tyr204)、Phospho-p70 S6 Kinase(Thr421/Ser424)蛋白表达水平。结论:四妙勇安汤可通过调节HIF-1α-Apelin/APJ信号通路,抑制VV新生,从而稳定AS易损斑块。

血管滋养血管及血管内皮生长因子与动脉粥样硬化斑块研究进展

血管滋养血管其主要功能是运送营养物质和氧至动静脉血管壁,同时清除血管壁细胞及通过动静脉血管内皮扩散转运所产生的"废物"。尽管血管滋养血管特性的改变与动脉粥样硬化斑块进展之间的关系已得到很好的证实,但血管滋养血管的作用,特别是疾病过程中如动脉粥样硬化,以何种方式存在及消失,是该疾病的成因或仅仅起作用,目前仍未完全明了。然而,即使其增值作用较小,其新生的微血管由于内皮损害而作为单核细胞移行至早期疾病位点的通路,成为疾病进展的根源之一。鉴于血管滋养血管以上两种功能特点,现就血管滋养血管及血管内皮生长因子与动脉粥样硬化斑块形成之间的关系作相关综述。

调控滋养血管新生稳定动脉粥样硬化斑块的中西医治疗进展

动脉粥样硬化(Atherosclerosis,AS)病变的主要临床危险在于斑块的不稳定性、易损性。斑块内新生滋养血管(Vasa Vasorum,VV)具有结构缺陷,其脆性大、渗漏性高,容易破裂出血,促进炎症反应,也为血细胞及血液可溶性成分进入斑块提供通道,促进AS斑块的形成,并且与斑块内出血、斑块破裂及临床心脑血管事件的发生密切相关。深入研究VV的功能及关键信号途径在AS中的作用,有望从根本上阻止稳定斑块发展为易损斑块,或者阻止不稳定斑块破裂及其并发症的发生。本文将新生VV在AS形成中的作用与机制以及相关治疗作一综述,以期为稳定AS易损斑块提供理论依据。

球囊扩张压力、时间及周期对动脉再狭窄与外膜滋养血管增生的影响

目的探讨不同压力、时间、周期球囊扩张后动脉外膜滋养血管增生与动脉再狭窄关系。方法前瞻性选取2015年1月至2017年7月收治的下肢动脉硬化闭塞症患者80例,术前CT血管造影(CTA)提示股浅动脉狭窄超65%。根据球囊扩张压力、时间、周期不同分为4组:Ⅰ组(n=20)6 atm,2 min×1次;Ⅱ组(n=20)10 atm,2 min×1次;III组(n=20)6 atm,4 min×1次;Ⅳ组(n=20)6 atm,2 min×2次,间隔5 min。于术前、术后3 d、术后3个月行踝肱指数测定(ABI)、多普勒超声及超声造影检查,评估不同球囊扩张压力、时间及周期对ABI、动脉狭窄程度、血流动力学改善程度影响,并评估与滋养血管关系。结果不同压力、时间及周期球囊扩张术后3 d均能明显改善患者ABI指数、狭窄程度及血流动力学,差异有统计学意义(P<0.05);但术后3个月ABI指数、狭窄程度及血流动力学均较术后3 d明显降低(P<0.05),而组间比较无显著差异(P>0.05)。且与术前、术后动脉外膜滋养血管增生情况相一致。结论球囊扩张可导致动脉内膜显著增厚,动脉外膜VV显著增生,并且当球囊扩张压力超过一定程度,增生的强度与球囊扩张的压力、时间和周期无显著相关性。

新生滋养血管在动脉粥样硬化形成中的作用及临床意义

动脉粥样硬化（As）病变的主要临床危险性在于斑块的不稳定性、易损性。斑块内新生滋养血管（VV）具有结构缺陷,其脆性大、渗漏性高,容易破裂出血,促进炎症反应,也为血细胞及血液可溶性成分进入斑块提供通道,促进As斑块的形成,并且与斑块内出血、斑块破裂及临床心脑血管事件的发生密切相关。深入研究新生滋养血管的功能及关键信号途径在As中的作用,有望从根本上阻止稳定斑块发展为易损斑块,或者阻止不稳定斑块破裂及其并发症的发生。

Egr-1的特异性脱氧核酶对大鼠颈总动脉损伤后内膜增生的影响

目的探讨早期生长反应因子1(Egr-1)的特异性脱氧核酶对大鼠颈总动脉损伤后新生内膜形成的影响。方法对Wistar大鼠行颈总动脉损伤后,在转染试剂Fugene6介导下经血管腔内转染Egr1的特异性脱氧核酶(ED5),以假手术组、单纯损伤组及空白转染试剂组(Fugene6组)作为对照,于术后3、7、14和21d4个时间点取材,检测内膜增生程度及增殖细胞核抗原(PCNA)、转化生长因子-β(TGF-β)和Egr-1的表达变化。结果单纯损伤组及Fugene6组7d时可见内膜增生,14d、21d时内膜增厚更明显,PCNA及TGF-β于损伤后3天明显表达,7d时在新生内膜及中膜中表达达到高峰,14d后逐渐下降,而Egr-1呈持续高表达。经ED5作用后,内膜增生减轻,动脉中PCNA、TGF-β及Egr-1表达明显降低,与单纯损伤组和FuGene6组比较差异有显著性。结论结果提示ED5可能是通过特异性抑制其相应基因的表达来阻遏动脉损伤后的内膜增生。

小腿皮神经营养血管皮瓣的术后护理

目的 探讨以皮神经营养血管为成活基础的新型皮神经营养血管皮瓣的术后护理特点。方法 1998年～ 2 0 0 0年3月 ,采用小腿皮神经营养血管皮瓣修复小腿中下段及足跟与足踝部深度创面 2 1例 2 2处 ,强化和改进术后护理 :体位的选择 ;观察皮瓣方法的改进 ;血运障碍的处理 ;预防血管痉挛 ,保持血管通畅 ;废用性功能障碍的预防。结果 2 1例 2 2处皮瓣全部成活良好 ,伤口一期愈合 ,术后外形与功能恢复满意。结论 皮神经营养血管皮瓣为深度创面的修复提供了新的手段 ,术后护理是皮瓣成活的重要环节 ,临床护理必须抓住上述特点 ,落实健康指导与护理措施。

Pro-vs anti-stenotic capacities of type-Ⅰ vs type-Ⅱ human induced pluripotent-derived endothelial cells

AIM:To verify in vivo relevance of the categorization of human vascular endothelial cells(VECs)into type-I(proproliferative)and type-II(anti-proliferative).METHODS:Endothelial layers of murine femoral arteries were removed by wire injury(WI)operation,a common technique to induce arteriostenosis.Type-I and type-II VECs produced from human induced pluripotent stem cells(iPSCs),whose characters were previously determined by their effects on the proliferation of vascular smooth muscle cells in in vitro co-culture experiments,were mixed with Matrigel?Matrix.The mixtures were injected into subcutaneous spaces around WI-operated femoral arteries for the transplanted human iPSC-derived VECs(iPSdECs)to take a route to the luminal surface via vasa vasorum,a nutrient microvessel for larger arteries.Histologies of the femoral arteries were examined over time.The presence of human iPSdECs was checked by immunostaining studies using an antibody that specifically recognizes human VECs.Degrees of stenosis of the femoral arteries were calculated after three weeks.To determine the optimal experimental condition,xenotransplantation experiments were performed under various conditions using immunocompromised mice as well as immunocompetent mice with or without administration of immunosuppressants.RESULTS:Because immunocompromised mice showed unexpected resistance to WI-induced arteriostenosis,we performed xenotransplantation experiments using immunocompetent mice along with immunosuppressant administrations.After one week,luminal surfaces of the WI-operated arteries were completely covered by human iPSdECs,showing the efficacy of our novel transplantation technique.After three weeks,type-IiPSdECs-transplanted arteries underwent total stenosis,while type-II-iPSdECs-transplanted arteries remained intact.However,untransplanted arteries of immunosuppressant-treated mice also remained intact by unknown reasons.We found that transplanted human VECs had already been replaced by murine endothelial cells by this time,indicating that a transient existence of human type-II-iPSdECs on arterial luminal surfaces can sufficiently prevent the development of stenosis.Thus,we re-performed xenotransplantation experiments using immunocompetent mice without administrating immunosuppressants and found that arteriostenosis was accelerated or prevented by transplantation of type-I or type-II iPSdECs,respectively.Similar results were obtained from the experiments using human embryonic stem cell-derived VECs at early passages(i.e.,type-II)and late passages(i.e.,type-I).CONCLUSION:Pro-and anti-stenosis capacities of type-I and type-II human iPSdECs were verified,respectively,promising a therapeutic application of allogenic iPSdECs.

四肢带皮神经营养血管蒂岛状皮瓣的临床应用

目的 探讨四肢各类型皮神经营养血管蒂岛状皮瓣修复组织缺损的临床效果。方法 临床分别应用了5种皮神经营养血管蒂岛状皮瓣修复皮肤、软组织缺损8例的实践。皮瓣最大面积15cm×10cm。最小面积3.5cm×2.5cm。结果 8例皮瓣均成活良好,创面Ⅰ期愈合,经6～12月随访,效果满意。结论 四肢带皮神经营养血管蒂岛状皮瓣血供可靠,不牺牲主要血管。

动态增强磁共振成像对瑞舒伐他汀治疗颈动脉粥样硬化斑块的早期疗效评价

目的动态增强MRI(dynamic contrast enhanced-MRI,DCE-MRI)评价瑞舒伐他汀对颈动脉粥样硬化斑块的疗效。方法 2009年3月~2010年8月解放军总医院门诊MRI证实有明确颈动脉粥样硬化斑块(含脂质核),从未使用过他汀类药物治疗的无症状患者32例,因图像不符合动态模型分析要求而剔除者5例,因层面匹配欠佳而剔除者2例,最终完成入选患者25例。所有患者进行瑞舒伐他汀(5~20mg/d)强化治疗2年,并于筛查时以及治疗3、12、24个月均行颈动脉DCE-MRI检查。测量并分析调脂治疗过程中颈动脉外膜灌流参数血浆容积百分比(Vp值)和血管外膜传输常数(Ktrans值)的变化。结果治疗3、12、24个月Vp值明显低于基线水平,差异有统计学意义(0.09±0.05、0.07±0.04、0.06±0.05 vs 0.12±0.06,P<0.05)。治疗3个月,Vp值降低了25.0%,下降幅度较大;治疗24个月内,Vp值呈现逐渐下降趋势(P<0.05)。与基线水平比较,治疗24个月的Ktrans值轻度降低,差异无统计学意义(P>0.05)。结论 DCE-MRI能够早期评价他汀类药物调脂治疗颈动脉粥样硬化斑块的疗效。

从滋养血管成熟化探讨稳定动脉粥样硬化易损斑块的作用

动脉粥样硬化(As)疾病在各种易损因素的影响下,最终导致斑块的形成、破裂。在这一过程中斑块内新生血管的数量、通透性成为关键因素,因此,对于新生血管的调节成为近几年As疾病的治疗策略。然而,仅仅通过抑制新生血管的进展具有一定局限性,怎样促进斑块内滋养血管成熟化将成为稳定As易损斑块新的治疗途径。本文综述了滋养血管成熟化相关生长因子及信号通路,以期为As易损斑块新的治疗奠定理论基础。

通心络联合阿托伐他汀、阿司匹林对家兔动脉粥样硬化早期血管外膜滋养血管新生的干预作用

目的观察通心络联合阿托伐他汀、阿司匹林对家兔动脉粥样硬化早期颈动脉外膜滋养血管新生的影响。方法72只健康♀♂各半新西兰白兔随机分为对照组、模型组、通心络(TXL)组、阿托伐他汀(ATO)组、阿司匹林(ASP)组、金三角(ATS)[1]组,各12只。对照组给予普通饲料、模型组及各用药组家兔均实施单侧颈动脉硅胶管包裹术复合高脂饲料喂养,TXL组给予通心络超微粉混悬液0.3 g·kg-1·d-1灌胃,ATO组给予阿托伐他汀2.5 mg·kg-1·d-1灌胃,ASP组给予阿司匹林12 mg·kg-1·d-1灌胃,ATS组给予通心络超微粉混悬液0.3 g·kg-1·d-1加阿托伐他汀2.5 mg·kg-1·d-1加阿司匹林12 mg·kg-1·d-1灌胃,连续给药4周后取材,HE染色观察颈动脉内中膜的变化;免疫组化法检测颈动脉外膜CD34表达情况;微球检测颈动脉微血管血流量的变化;RT-PCR和Western blot检测颈动脉组织中VEGF、VEGFR-2基因和蛋白表达情况。结果与对照组比较,模型组VEGF、VEGFR-2基因和蛋白表达以及微血管血流量明显增强(P<0.01)。与模型组比较,各用药组VEGF、VEGFR-2基因和蛋白表达以及微血管血流量明显减弱(P<0.01,P<0.05)。与其他用药组比较,ATS组VEGF、VEGFR-2基因和蛋白表达以及微血管血流量明显减弱(P<0.01,P<0.05)。与ASP组比较,TXL组、ATO组VEGFR-2蛋白表达均明显降低(P<0.05),ATO组微血管血流量减少明显(P<0.05)。TXL组与ATO组两组间比较差异无显著性(P>0.05)。VEGF、VEGFR-2基因和VEGF蛋白表达组间比较无统计学意义(P>0.05)。各用药组颈动脉外膜CD34表达减少。结论 "ATS"方案有助于减少动脉粥样硬化早期颈动脉VEGF、VEGFR-2表达,抑制血管外膜滋养血管新生,减少促炎物质进入血管中膜、内膜,延缓动脉粥样硬化进程。

超声造影在动脉粥样硬化诊断中的研究进展

动脉粥样硬化(As)是大、中动脉血管内膜脂质沉积和炎症反应不断循环往复的病变结果。其中,外膜滋养血管的增殖、斑块内炎症细胞的聚集、各种炎症因子的高表达及血管新生化程度是引起斑块易损、破裂的主要原因,而破裂后形成的血栓是引起急性心脑血管事件的关键。目前,超声造影被认为是评价血管外膜滋养血管和斑块内新生血管分布密度的金标准。近年来超声造影剂的快速研发及分子成像技术的飞速发展,打破了造影剂脉管显像的局限性,为血池外靶组织在分子水平进行超声成像提供了可能,未来应进一步探索超声造影技术在As诊断方面的应用。