Hippo pathway activation inhibits atherosclerosis: 通過激活Hippo信號通路抑制動脈粥樣硬化的研究 / 通過激活Hippo信號通路抑制動脈粥樣硬化的研究 / CUHK electronic theses & dissertations collection / Hippo pathway activation inhibits atherosclerosis: Tong guo ji huo Hippo xin hao tong lu yi zhi dong mai zhou yang ying hua de yan jiu / Tong guo ji huo Hippo xin hao tong lu yi zhi dong mai zhou yang ying hua de yan jiu

January 2014

Hemodynamics (the patterns of blood flow along blood vessels), such as laminar shear stress (LSS) and oscillatory shear stress (OSS), plays an important role in maintaining vascular homeostasis and also the pathogenesis of atherosclerosis. LSS, occurring mainly in the straight part of the vascular tree, is protective against the formation of atherosclerotic plagues, while OSS is the predominant hemodynamic pattern experienced by the branched regions and curvatures in the vascular system, in which most of atherosclerotic plaques are developed. Recent evidence indicates that the Hippo pathway is important in transducing mechanical stimulation. However, the exact role of Hippo signaling in hemodynamics and the development of atherosclerosis is unclear. Therefore, the present study was designed to investigate how the Hippo pathway responds to hemodynamic stimulation and the impact of this pathway in the development of atherosclerosis. / The central axis of the Hippo pathway consists of a chain of kinase cascade including serine/threonine-protein kinase 1/2 (LATS1/2) and downstream YAP/TAZ effectors. Activation of the Hippo pathway leads to phosphorylation, nuclear exportation and inhibition of YAP/TAZ transcription factors. The present study is probably for the first time to demonstrate that the Hippo pathway can be activated in human umbilical vein endothelial cells (HUVECs) and human aortic endothelial cells (HAECs) subjected to LSS. Western blotting results showed that Hippo activation was most likely mediated by phosphorylation of Hippo kinase YAP. The results from the nuclear fractioning assay showed that the amount of the nuclear fraction of YAP/TAZ was reduced in HUVECs subjected to LSS. Repression of the established YAP/TAZ target genes CTGF and CYR61, and inhibition of Hippo reporter gene after LSS treatment, further supported the notion that activation of the Hippo pathway inhibits the YAP/TAZ downstream genes expression. In vivo experiments showed an increased YAP phosphorylation in the straight area of C57 mouse thoracic aortas as compared with aortic arch, which favors that LSS activates Hippo pathway under the physiological condition. To further understand whether different flow patterns have different impacts on the Hippo pathway, the effects of OSS were also studied. As expected, OSS inhibited the Hippo pathway through inducing the de-phosphorylation of YAP, and promoting the nuclear localization of YAP/TAZ. The induction of YAP/TAZ target genes (CTGF and CYR61) further confirms that OSS-induced inhibition of the Hippo pathway enhanced the YAP and TAZ transcription activity. / Since unfavorable hemodynamics is among the most important factors in the development of atherosclerotic plaques, I hypothesized that inhibition of the Hippo pathway is involved in the formation of atherosclerotic plaques. Adhesion molecules are a group of cell surface proteins that mediate cell-cell interaction. During the initiation phase of atherosclerosis, adhesion molecules are highly expressed on the surface of endothelial cells to enhance the attachment of monocytes to the vascular wall, leading to monocyte accumulation within the vascular wall. OSS up-regulates the expression of several adhesion molecules; however, the underlying mechanisms remain elusive. To identify the role of Hippo pathway in adhesion molecules expression, the gene expression of HUVECs with YAP/TAZ knockdown was investigated using real-time PCR. The expression of the four adhesion molecule, ICAM1, E-Selectin, MCP1 and CXCL1 were down-regulated by YAP and TAZ gene silencing. To further study the mechanism, the promoter region of the four target genes were amplified from HUVECs genomic DNA, and subcloned into PGL3 reporter plasmids. The promoter activity was tested by co-transfection of the reporter plasmids with different dosages of constructively active YAP and TAZ. The present results showed that activated YAP and TAZ dose-dependently increased the promoter activity of these four genes. CXCL1 was selected for further examination because it has been recently reported to play an important role in oxidized LDL-induced elevation of monocyte attachment to endothelial cells. Analysis of the CXCL1 promoter revealed that two TEAD1 binding sites located within the promoter region of CXCL1. The reporter gene assay results showed that TEAD1 induced the CXCL1 reporter activity, indicating that the CXCL1 promoter was regulated by YAP/TAZ/TEAD complex. The EMSA analysis further demonstrates that constitutively active YAP and TAZ induced the binding between TEAD1 and the CXCL1 promoter, suggesting a direct association between TEAD1 and CXCL1 promoter. / To further explore whether the Hippo pathway activation could regress atherosclerosis development, TAZ knockdown adenovirus was generated and administered to ApoE⁻/⁻ mice fed on Western diet. The formation and sizes of atherosclerotic plaques were visualized using oil red O staining. Monocyte infiltration was estimated using monocyte marker CD68. The expression of CXCL1 was detected using immunohistochemistry. The present results demonstrated that TAZ gene silencing significantly suppressed the expression of CXCL1 and reduced the sizes of atherosclerosis plagues as well as monocyte infiltration in the vascular wall of ApoE⁻/⁻ mice. / To further identify whether Hippo pathway could be a drug target for the treatment of atherosclerosis, several known atherosclerosis risk factors and beneficial factors were tested for their effects on Hippo pathway. Four out of nine atheroprotective factors were found to suppress the TEAD reporter activity. On the other hand, four out of six risk factors were identified to increase the TEAD reporter activity. The present results suggest that atheroprotective LSS activates while atherogenic OSS inhibits the Hippo pathway. / The Hippo pathway could be activated by atheroprotective LSS, while it was inhibited by atherogenic OSS. Activation of the Hippo pathway inhibits the development of atherosclerosis at least in part through reducing the expression of adhesion molecules and decreasing macrophage accumulation in the vascular wall. The present new findings suggest that targeting this Hippo pathway is potentially useful for therapeutic intervention of atherosclerosis and associated vascular diseases. / 血流動力學（即血液在心血管系統中流動的模式），包括層流剪切應力（LSS）和振盪剪切應力（OSS）。血流動力學在血管穩態和動脈粥樣硬化的發展中起重要作用。LSS主要發生在血管系統的直線部分，可防止動脈粥樣硬化斑塊形成，而OSS是血管系統中分支和彎曲部分的主要血流模式，大部份粥樣硬化斑塊發生在此。最近的研究表明，Hippo通路在機械刺激傳導中起重要作用。然而，Hippo信號通路在血流動力學和動脈粥樣硬化發展中的確切作用目前尚不清楚。因此，本論文的目的是研究Hippo通路如何響應血流動力學刺激以及Hippo通路對動脈粥樣硬化的發展的影響。 / Hippo通路主要由一系列激酶鏈和下游YAP/ TAZ效應器組成，其中的激酶鏈包括絲氨酸/蘇氨酸－蛋白激酶1/2（LATS1/ 2）。激活Hippo通路可導致YAP和TAZ磷酸化，促進其出核運輸並抑制其轉錄激活的功能。本研究中，我們首次證明了在LSS條件下，人臍靜脈內皮細胞（HUVEC）和人主動脈內皮細胞（HAECs）中的Hippo通路被激活。Western雜交結果表明，Hippo通路的激活很可能是受YAP激酶的磷酸化調節。細胞核質分離結果顯示在LSS條件下，人臍靜脈內皮細胞中YAP/ TAZ的細胞核部分的量顯著減少。LSS处理后，YAP/ TAZ靶基因CTGF和CYR61的表達降低，其TEAD告基因受到抑制，这進一步證明激活Hippo通路可抑制YAP/ TAZ下游基因的表達。動物實驗結果顯示YAP磷酸化和YAP/ TAZ出核在C57小鼠的胸主動脈直的區域顯著高於彎的區域，這也表明在生理條件下，LSS可激活Hippo通路。為了進一步了解不同的血流模式是否對Hippo通路產生不同的影響，我們研究了OSS條件下的Hippo通路。正如所期，OSS通過誘導YAP的去磷酸化，促進YAP/ TAZ的核內分佈，從而抑制Hippo通路的活性。OSS誘導YAP/ TAZ靶基因（CTGF和CYR61）產生轉錄活性，證明了OSS可抑制Hippo通路。 / 不利的血流模式是動脈粥樣硬化斑塊產生的最重要因素之一，因此我們推測抑制Hippo通路或許可導致動脈粥樣硬化斑塊的形成。粘附分子是一類調節細胞間相互作用的細胞表面蛋白。在動脈粥樣硬化形成的初始階段，粘附分子會在內皮細胞的表面高表達，從而提高單核細胞附著和聚集於血管壁上。OSS上調粘附分子的表達，但機制仍不清楚。為了識別Hippo通路在粘附分子表達中的作用，本文用實時定量PCR檢測了YAP/ TAZ敲低了的人臍靜脈內皮細胞的基因表達水平。實驗結果顯示四種粘附基因，包括ICAM1，E-Selectin，MCP1和CXCL1通過YAP和TAZ的基因沉默而被下調。為了進一步研究此中機制，本文擴增了臍靜脈內皮細胞的基因組DNA中的四個靶基因啟動子區，並將其克隆到PGL3報告質粒。通過共轉染不同濃度的組成型激活的YAP和TAZ，本文測定了這四個啟動子的活性。結果顯示激活的YAP和TAZ能夠劑量依賴性上調這四個基因的啟動子活性。由於最近有報導說氧化低密度脂蛋白可誘導單核細胞附著於內皮細胞，而CXCL1在此誘導過程中具有重要作用，因此本文選擇CXCL1作進一步研究。通過分析CXCL1的啟動子，本文發現CXCL1的啟動子區域內有兩個TEAD1結合位點。報告基因檢測結果顯示TEAD1可誘導CXCL1報告活性，這表明CXCL1啟動子是通過YAP/ TAZ/ TEAD複合體來調節。EMSA分析進一步揭示了組成型激活的YAP和TAZ可誘導TEAD1和CXCL1啟動子之間的結合，表明TEAD1直接結合到CXCL1啟動子。 / 為進一步開拓Hippo通路是否是動脈粥樣硬化消退潛在的治療靶點，本文構建了TAZ敲低的腺病毒並將其轉入餵以西方飲食的ApoE⁻/⁻小鼠。通過油紅O染色來觀察動脈粥樣硬化斑塊的形態和大小。用單核細胞表面標記物CD68測定單核細胞對血管的浸潤。用免疫組化鑑定CXCL1的表達。結果表明TAZ基因沉默顯著抑制ApoE⁻/⁻小鼠血管壁CXCL1的表達，降低動脈粥樣硬化斑塊的大小及單核細胞浸潤。 / 為了進一步確定Hippo途徑是動脈粥樣硬化的藥物治療靶點，本文對幾個已知的動脈粥樣硬化的危險因子和有利因子對Hippo通路活性的影響進行了研究。出人意料的是，九個動脈粥樣硬化的保護因子中，有四個被確定為抑制TEAD報告基因活性。另一方面，六個危險因子中，有四個被鑑定為可提高TEAD報告活性。這些結果與上面的研究發現共同證明了LSS降低動脈粥樣硬化，激活Hippo通路，而OSS促進動脈粥樣硬化，抑制Hippo通路。 / 本研究確定了層流剪應力（LSS）激活Hippo通路，抑制動脈粥樣硬化；振盪剪切應力（OSS）抑制Hippo通路，導致動脈粥樣硬化。Hippo通路被激活能夠抑制動脈粥樣硬化的機制是通過降低粘附分子的表達，減少巨噬細胞在血管壁上的附著。這一新發現表明，靶向Hippo通路對介入治療動脈粥樣硬化以及相關的血管疾病具有潛在的應用意義。 / Wang, Li . / Thesis (Ph.D.)--Chinese University of Hong Kong, 2014. / Includes bibliographical references (leaves 129-138). / Abstracts also in Chinese. / Title from PDF title page (viewed on 08, November, 2016). / Wang, Li. / Detailed summary in vernacular field only. / Detailed summary in vernacular field only. / Detailed summary in vernacular field only. / Detailed summary in vernacular field only. / Detailed summary in vernacular field only. / Detailed summary in vernacular field only.

Atherosclerosis--Pathogenesis

Hemodynamics

Atherosclerosis--physiopathology

Hemodynamics

Hemodynamic analysis of blood flows in carotid bifurcations

Yu, Xiaohong,

January 2007

Thesis (Ph. D.)--University of Hong Kong, 2007. / Title proper from title frame. Also available in printed format.

Comparison and application of rheological constitutive functions for whole human blood

Easthope, Peter Lyall

January 1979

This work develops an empirical method for investigation of the flow properties of blood and applies it to a clinically oriented problem. The development focuses on the characterization of the flow properties of a blood sample. According to the theory of continuum mechanics the steady state flow properties of a material are characterized completely by its constitutive (Burchfield, 1972) function which relates the shear stress measured in a rheometer to the shear rate and hematocrit of the sample. Eleven functions derived from various sources were examined for their ability to fit flow data from thirty—one normal individuals, eleven of whom were using oral contraceptives. (The remainder were not using any drugs). A shear rate range of 0.0312 to 124 s⁻¹ was used at hematocrits from 0.29 to 0.55. A non-linear curve fitting procedure allowed an ordering of the functions to be established with respect to their goodness of fit. The function first employed by Walburn and Schneck (1976), T = X₁ exp (X₂ H+X₄ /H²)D[sup 1-X₃] where T = shear stress, D = shear rate, H = hematocrit and X₁ to X₄ are adjustable parameters, was found to be the most successful. This constitutive function was then used to examine data obtained from a population of normal women at various times during the menstrual cycle, as a hemorheological cycle had been reported to occur over this period. The concentrations of several plasma proteins were also determined and plotted over time. No evident cycle of hemorheological properties or protein concentrations was found. / Medicine, Faculty of / Pathology and Laboratory Medicine, Department of / Graduate

Hemodynamics

Blood Flow Velocity

Hemodynamics

Blood flow

Hemodynamics and atherogenesis at the human carotid bifurcation

Ku, David N.

05 1900

No description available.

Hemodynamics

Blood flow

Atherosclerosis

Regulation of endothelial cell VCAM-1 gene expression and transcription by fluid flow

Varner, Signe E.

12 1900

No description available.

Hemodynamics

Atherosclerosis

Vascular endothelium

The Relationship between Retinal Vascular Reactivity and Arteriolar Diameter

Tayyari, Faryan

07 December 2006

ABSTRACT Purpose: The primary aim of the study (i.e. Chapter 3) was to compare the magnitude of retinal vascular reactivity in arterioles of varying diameter in healthy, young subjects. The secondary aims were to determine: a) if there are any order effects in terms of provoking vasoconstriction or vasodilation first; and b) the repeatability of the vascular reactivity measurements. An additional aim (i.e. Chapter 4) was to determine the effect of healthy aging on the relationship between retinal vascular reactivity and vessel diameter. Method: The sample comprised 10 healthy, young subjects (mean age 26.5 years, SD 4.04) and 7 healthy, older subjects (mean age 55.43 years, SD 5.41). Each subject from the young age group attended for three sessions. The first session was used to determine eligibility and select hemodynamic measurement sites. At sessions 2 and 3, O2 and CO2 were sequentially administered to the subjects using a face mask and sequential re-breathing circuit (to maintain standardized hyperoxia and hypercapnia). The order of vasoconstriction and vasodilation was varied across sessions 2 and 3. The design of the protocol was simplified for the subjects from the older age group. Each subject from the older group attended for one visit. O2 and CO2 were administered to the subjects using a face mask and sequential re-breathing circuit. The order of gas provocation was varied among the subjects (i.e. hyperoxia or hypercapnia first). For both groups, measurements of vessel diameter, centerline blood velocity and derived blood flow were acquired at each condition (i.e. baseline, during stabilized vasoconstriction, vasodilation, and recovery) at two discrete measurement sites along the supero-temporal arteriole. Results: The results of the repeated measures ANOVA showed a significant difference between the narrow and wide measurement sites for the younger group for flow (p??? 0.0003) and a significant influence of inspired gas provocation on flow for both protocols (p<0.0001). In addition, the interaction of measurement site and inspired gas provocation was significant (p<0.0001). The magnitude of retinal vascular reactivity showed a significantly greater blood flow response for the wide measurement site (p<0.0001). O2 provocation resulted in vasoconstriction that was still present up to 10 minutes after cessation of the stimulus (order effect of O2; p???0.046). No such order effect was apparent for CO2 provocation (order effect of CO2; p=0.352). The group mean blood flow Coefficient of Repeatability (COR) for the narrow measurement site was 0.74 ??l/min (relative to group mean flow of 4.85 ??l/min ?? SD 1.31) and for the wide measurement site was 1.49 ??l/min (relative to group mean flow of 11.29 ??l/min ?? SD 3.55). There was no difference between the young and the older age groups in retinal vascular reactivity for both the narrow (two-tailed Student t-test, p=0.8692) and wide (two-tailed Student t-test, p=0.2795) measurement sites. Conclusion: This study demonstrated that the magnitude of retinal vascular reactivity was greater for arteriolar measurement sites with wider baseline vessel diameters. In addition, it demonstrated that hyperoxic provocation resulted in a persistent vasoconstriction up to 10 minutes after cessation of the stimulus. The study demonstrated that the repeatability of retinal blood flow measurements in absolute terms is lower for smaller diameter vessels. Finally, this study also suggests that age does not affect the relationship between retinal vascular reactivity and vessel diameter.

Retina

Vascular Reactivity

hemodynamics

An Advanced Protocol-Driven Transition from Parenteral Prostanoids to Inhaled Trepostinil in Pulmonary Arterial Hypertension

Oudiz, Ronald, Agarwal, Manyoo, Rischard, Franz, De Marco, Teresa

12 1900

Patients with pulmonary arterial hypertension (PAH) often require parenteral prostanoids to improve symptoms and signs of PAH. Complications of parenteral prostanoids-such as catheter-related infections and intolerable adverse effects-may develop, prompting transition to inhaled prostanoids. We report a prospective, protocol-driven transition from parenteral prostanoids to inhaled prostanoids with monitoring of exercise gas exchange and acute hemodynamics. Three PAH centers recruited patients transitioning from parenteral prostanoids to inhaled trepostinil. Rigid inclusion criteria were used, including parenteral prostanoid dose < 30 ng/kg/min, New York Heart Association functional class (FC) < 3, and pulmonary vascular resistance (PVR) < 6 Wood units. Of the 9 patients meeting initial inclusion criteria, 3 were excluded. In the remaining patients, the parenteral prostanoid was reduced and the inhaled prostanoid was increased over 24-36 hours with continuous hemodynamic monitoring. Exercise capacity and FC were measured at baseline and weeks 1, 4, and 12. All patients were successfully weaned from parenteral prostanoids. An acute PVR decrease was seen with most inhaled prostanoid doses, but PVR varied throughout the transition. Patients tolerated inhaled prostanoids for 9-12 breaths 4 times a day with no treatment-limiting adverse events. At week 12, FC was unchanged, and all patients continued to receive inhaled prostanoids without serious adverse events or additional PAH therapy. In 5 of 6 patients, 6-minute walk distance and peak VO2 were within 10% of baseline. Using a strict transition protocol and rigid patient selection criteria, the parenteral prostanoid to inhaled prostanoid transition appeared safe and well tolerated and did not result in clinical deterioration over 12 weeks. Hemodynamic variability noted acutely during transition in our study did not adversely affect successful transition.

hemodynamics

pulmonary circulation

exercise

Blood flow responses to mild-intensity exercise in ectopic versus orthotopic prostate tumors: dependence upon host-tissue hemodynamics and vascular reactivity

Garcia, Emmanuel

January 1900

Master of Science / Department of Kinesiology / Bradley J. Behnke / Given the critical role of tumor O₂ delivery on patient prognosis and the rise in preclinical exercise-oncology studies, we investigated tumor and host-tissue blood flow at rest and during exercise as well as vascular reactivity using a rat prostate cancer model grown in two transplantation sites. Methods. In male COP/CrCrl rats, blood flow (via radiolabeled microspheres) to prostate tumors (R3327-MatLyLu cells injected in the left flank (ectopic) or ventral prostate (orthotopic)) and host-tissue was measured at rest and during a bout of mild-intensity exercise. Alpha-adrenergic vasoconstriction to norepinephrine (NE: 10⁻⁹ to 10⁻⁴ M) was determined in arterioles perforating the tumors and host-tissue. To determine host-tissue exercise hyperemia in healthy tissue, a sham-operated group was included. Results. Blood flow was lower at rest and during exercise in ectopic tumors and host-tissue (subcutaneous adipose) versus the orthotopic tumor and host-tissue (prostate). During exercise, blood flow to the ectopic tumor significantly decreased by 25 ± 5%, whereas flow to the orthotopic tumor increased by 181 ± 30%. Maximal vasoconstriction to NE was not different between arterioles from either tumor location. However, there was a significantly higher peak vasoconstriction to NE in subcutaneous adipose arterioles (92 ± 7%) versus prostate arterioles (55 ± 7%). Establishment of the tumor did not alter host-tissue blood flow from either location at rest or during exercise. Conclusion. These data demonstrate blood flow in tumors is dependent on host-tissue hemodynamics and that the location of the tumor may critically affect how exercise impacts the tumor microenvironment and treatment outcomes.

Kinesiology

Oncology

Tumor

Hemodynamics

Hemodynamic Model of the Cardiovascular System during Valsalva Maneuver and Orthostatic Changes

Moberg, Niklas

January 2011

The goal of the Master's Thesis was to extend an existing cardiovascular model to include the mechanics of the lung, thus allowing to simulate breathing maneuvers such as the Valsalva maneuver and the Forced Vital Capacity maneuver. This included a remodeling of the pulmonary capillaries and of the existing interactions of the model with the intrathoracic pressure. The existing description of the vascular compartments was found to be insufficient to describe the hemodynamic response to orthostatic changes and was extended to include a compartment representing the upper body. Stress relaxation was included into all the larger vascular compartments. The results showed an improved accuracy of the extended model when subjected to large intrathoracic pressure changes and during orthostatic stress. The internal responses of the newly modeled pulmonary capillaries were studied and verified against literature with satisfying results.

Hemodynamics

model

Valsalva

cardiovascular

In Vitro flow visualization and pressure measurement studies in the pulmonary artery

Philpot, Elizabeth Rebecca Fanning

08 1900

No description available.

Hemodynamics

Fluid dynamics