University of California San Francisco

Rong Wang - 144px
Rong
Wang
PhD

Professor of Surgery
Division of Vascular and Endovascular Surgery
Mildred V. Strouss Endowed Chair in Vascular Surgery
Director, Laboratory for Accelerated Vascular Research

Address

513 Parnassus Ave, HSW, #1618
San Francisco, CA 94143
United States

Email: [email protected]
Fax: 415-564-5698

Biography

MOLECULAR PROGRAMMING OF THE VASCULATURE IN DEVELOPMENT AND DISEASE
Proper formation and function of the vasculature are crucial for health and survival, as the vasculature supplies all cells in the body. A dysfunctional vasculature causes myriad diseases, including stroke, arterial occlusive diseases, and vascular anomalies. Our long-term goal is to identify novel drug targets and inform rational therapeutic designs to treat vascular diseases. Our strategy is to understand genes crucial for angiogenesis (new vessel formation) in the normal and diseased states, concentrating on the Notch, ephrin-B2, and TGF-beta pathways. We employ cutting-edge mouse genetics to delete or express genes in a cell lineage-specific and temporally controllable fashion in vascular cells. We combine these molecular approaches with mouse models of diseases as well as live 5D two-photon imaging (3D + blood flow over time) to uncover both the molecular mechanisms and hemodynamic signals in development and disease progression. These preclinical animal studies are coupled with patient sample validations. Our lab members come from diverse fields, including biology, bioengineering, and medicine, creating a collaborative and exciting environment. We strive to advance multiple projects across disciplines.

PROJECTS
Molecular programming of blood vessels: Building on our study of the developing dorsal aorta and cardinal vein, the first major artery-vein (AV) pair to form in the body, our lab aims to identify molecular regulators that program arteries and veins in vital organs during development and aging. We examine the interplay between genetic AV programming and flow-induced patterning. Understanding AV programming in normal angiogenesis provides important insights into how the genetic pathways can be hijacked in various disease states.

Stroke: We study two types of stroke, ischemic stroke and hemorrhagic stroke. Ischemic stroke occurs when arteries supplying the brain are blocked. Using a surgical model of ischemic stroke, we aim to identify technologies enabling better recover following arterial blockade. Hemorrhagic stroke, on the other hand, occurs when diseased blood vessels rupture. Brain arteriovenous malformations (AVMs), which are direct connections from arteries to veins, are one of the major causes of hemorrhagic stroke. We investigate AV programming in both AVM progression and regression.

Arteriovenous malformations: AVMs can occur anywhere in the body and comprise a category of hard to treat vascular anomalies. Most AVMs are sporadic, thus limiting the understanding of their etiology. In contrast, hereditary AVMs, such as those found in hereditary hemorrhagic telangiectasia (HHT) patients, offer an excellent opportunity to study how AVMs form. HHTs are caused by mutations in genes of the TGF-beta superfamily. We are interested in the molecular mechanisms underlying HHT-mediated AVMs formation.

Arterial occlusive diseases: Arterial occlusive diseases occur when the arteries in the body are blocked, causing insufficient blood flow to the tissues. Blockage of arteries in the brain causes stroke, in the heart causes myocardial infarction, and in the extremities causes peripheral arterial disease. Arteriogenesis, a process by which small dormant arteries around the blockage enlarge to form collateral circulation, holds promise to restore blood flow and rescue affected tissues. We investigate pro-arteriogenic molecular regulators to uncover potential therapeutic strategies to enhance the body’s natural defense against arterial occlusive disease.

Videos

Education

Institution Degree Dept or School End Date
University of California Diversity, Equity, and Inclusion Champion Training 2019
University of California, San Francisco Coro-UCSF Collaborative Faculty Leadership Training 2008
University of California, San Francisco Postdoctoral Fellowship Cancer Biology 1999
University of North Carolina, Chapel Hill Ph.D. Biology (Angiogenesis) 1993
Graduate School of Chinese Science and Technology University, Institute of Genetics, Academia Sinica M.S. Candidate Mammalian Genetics 1988
Sichuan University B.S. Biology 1984

In the News

Gene is Likely Cause of Stroke-Inducing Vascular Malformations
September, 02, 2008 | Wang Lab

Grants and Funding

  • Molecular Pathogenesis of Hereditary Hemorrhagic Telangiectasia | NIH | 2020-02-01 - 2025-01-31 | Role: Principal Investigator
  • Molecular Pathogenesis of Hereditary Hemorrhagic Telangiectasia | NINDS | 2020-02-01 - 2025-01-31 | Role: Principal Investigator
  • Identifying Molecular Regulators of Hereditary Hemorrhagic Telangiectasia In a Novel Mouse Model | American Heart Association | 2019-07-01 - 2022-06-30 | Role: Principal Investigator
  • Molecular Pathogenesis and Therapy for Critical Lim Ischemia | Tobacco Related Disease Research Program | 2018-07-01 - 2021-06-30 | Role: Principal Investigator
  • RBPJ and EphrinB2 as Molecular Targets to Treat Brain Arteriovenous Malformation in Notch4-Induced Mouse Models | Department of the Army | 2016-09-30 - 2020-09-30 | Role: Principal Investigator
  • Molecular Pathogenesis of Brain Arteriovenous Malformation | NIH | 2010-08-01 - 2020-03-31 | Role: Principal Investigator
  • Notch Signaling in Arterial-Venous Specification | NIH | 2003-12-01 - 2017-02-28 | Role: Principal Investigator

Research Interests

  • Angiogenesis Inhibitors
  • Neovascularization
  • Physiologic, Ischemia
  • Developmental Biology
  • Gene Expression Regulation
  • Embryonic Development
  • Developmental Growth
  • Arteriovenous Malformations
  • Carcinoma, Hepatocellular
  • Arteriogenesis
  • Notch Pathway
  • EphrinB2
  • Vascular Development
  • Collateral Vessel Formation
  • Vascular Physiology
  • Stem Cells

Publications

MOST RECENT PUBLICATIONS FROM A TOTAL OF 43
  1. Site-specific protein conjugates incorporating Para-Azido-L-Phenylalanine for cellular and in vivo imaging.
    Lightle HE, Kafley P, Lewis TR, Wang RE| | PubMed
  2. Meeting Proceedings from ICBS 2022 - Uncovering Solutions for Diseases.
    Syphers JL, Xue L, Yi X, Wang RE, Haubrich BA| | PubMed
  3. Nitric oxide synthase and reduced arterial tone contribute to arteriovenous malformation.
    Huang L, Cheng F, Zhang X, Zielonka J, Nystoriak MA, Xiang W, Raygor K, Wang S, Lakshmanan A, Jiang W, Yuan S, Hou KS, Zhang J, Wang X, Syed AU, Juric M, Takahashi T, Navedo MF, Wang RA| | PubMed
  4. Monitoring of cell-cell communication and contact history in mammals.
    Zhang S, Zhao H, Liu Z, Liu K, Zhu H, Pu W, He L, Wang RA, Zhou B| | PubMed
  5. Endothelial Rbpj deletion normalizes Notch4-induced brain arteriovenous malformation in mice.
    Nielsen CM, Zhang X, Raygor K, Wang S, Bollen AW, Wang RA| | PubMed
  6. Mechanical Stretch Increases Expression of CXCL1 in Liver Sinusoidal Endothelial Cells to Recruit Neutrophils, Generate Sinusoidal Microthombi, and Promote Portal Hypertension.
    Hilscher MB, Sehrawat T, Arab JP, Zeng Z, Gao J, Liu M, Kostallari E, Gao Y, Simonetto DA, Yaqoob U, Cao S, Revzin A, Beyder A, Wang RA, Kamath PS, Kubes P, Shah VH| | PubMed
  7. Abnormal arterial-venous fusions and fate specification in mouse embryos lacking blood flow.
    Hwa JJ, Beckouche N, Huang L, Kram Y, Lindskog H, Wang RA| | PubMed
  8. Endothelial notch signaling is essential to prevent hepatic vascular malformations in mice.
    Cuervo H, Nielsen CM, Simonetto DA, Ferrell L, Shah VH, Wang RA| | PubMed
  9. Mouse Models of Cerebral Arteriovenous Malformation.
    Nielsen CM, Huang L, Murphy PA, Lawton MT, Wang RA| | PubMed
  10. Constitutively active Notch4 receptor elicits brain arteriovenous malformations through enlargement of capillary-like vessels.
    Murphy PA, Kim TN, Huang L, Nielsen CM, Lawton MT, Adams RH, Schaffer CB, Wang RA| | PubMed
  11. Endothelial ephrin-B2 is essential for arterial vasodilation in mice.
    Lin Y, Jiang W, Ng J, Jina A, Wang RA| | PubMed
  12. Deletion of Rbpj from postnatal endothelium leads to abnormal arteriovenous shunting in mice.
    Nielsen CM, Cuervo H, Ding VW, Kong Y, Huang EJ, Wang RA| | PubMed
  13. Molecular identification of venous progenitors in the dorsal aorta reveals an aortic origin for the cardinal vein in mammals.
    Lindskog H, Kim YH, Jelin EB, Kong Y, Guevara-Gallardo S, Kim TN, Wang RA| | PubMed
  14. Notch4 is required for tumor onset and perfusion.
    Costa MJ, Wu X, Cuervo H, Srinivasan R, Bechis SK, Cheang E, Marjanovic O, Gridley T, Cvetic CA, Wang RA| | PubMed
  15. Line-scanning particle image velocimetry: an optical approach for quantifying a wide range of blood flow speeds in live animals.
    Kim TN, Goodwill PW, Chen Y, Conolly SM, Schaffer CB, Liepmann D, Wang RA| | PubMed
  16. Notch4 normalization reduces blood vessel size in arteriovenous malformations.
    Murphy PA, Kim TN, Lu G, Bollen AW, Schaffer CB, Wang RA| | PubMed
  17. Inefficient skeletal muscle repair in inhibitor of differentiation knockout mice suggests a crucial role for BMP signaling during adult muscle regeneration.
    Clever JL, Sakai Y, Wang RA, Schneider DB| | PubMed
  18. Constitutively active endothelial Notch4 causes lung arteriovenous shunts in mice.
    Miniati D, Jelin EB, Ng J, Wu J, Carlson TR, Wu X, Looney MR, Wang RA| | PubMed
  19. Arterial-venous segregation by selective cell sprouting: an alternative mode of blood vessel formation.
    Herbert SP, Huisken J, Kim TN, Feldman ME, Houseman BT, Wang RA, Shokat KM, Stainier DY| | PubMed
  20. Endothelial Notch signaling is upregulated in human brain arteriovenous malformations and a mouse model of the disease.
    Murphy PA, Lu G, Shiah S, Bollen AW, Wang RA| | PubMed
  21. Cellular and molecular mechanism regulating blood flow recovery in acute versus gradual femoral artery occlusion are distinct in the mouse.
    Yang Y, Tang G, Yan J, Park B, Hoffman A, Tie G, Wang R, Messina LM| | PubMed
  22. Artery and vein size is balanced by Notch and ephrin B2/EphB4 during angiogenesis.
    Kim YH, Hu H, Guevara-Gallardo S, Lam MT, Fong SY, Wang RA| | PubMed
  23. Endothelial Notch4 signaling induces hallmarks of brain arteriovenous malformations in mice.
    Murphy PA, Lam MT, Wu X, Kim TN, Vartanian SM, Bollen AW, Carlson TR, Wang RA| | PubMed
  24. Placental rescue reveals a sole requirement for c-Myc in embryonic erythroblast survival and hematopoietic stem cell function.
    Dubois NC, Adolphe C, Ehninger A, Wang RA, Robertson EJ, Trumpp A| | PubMed
  25. c-myc in the hematopoietic lineage is crucial for its angiogenic function in the mouse embryo.
    He C, Hu H, Braren R, Fong SY, Trumpp A, Carlson TR, Wang RA| | PubMed
  26. Cell-autonomous requirement for beta1 integrin in endothelial cell adhesion, migration and survival during angiogenesis in mice.
    Carlson TR, Hu H, Braren R, Kim YH, Wang RA| | PubMed
  27. Distinct pathways of genomic progression to benign and malignant tumors of the liver.
    Tward AD, Jones KD, Yant S, Cheung ST, Fan ST, Chen X, Kay MA, Wang R, Bishop JM| | PubMed
  28. Endothelial FAK is essential for vascular network stability, cell survival, and lamellipodial formation.
    Braren R, Hu H, Kim YH, Beggs HE, Reichardt LF, Wang R| | PubMed
  29. Optimization of adenovirus-mediated endothelial nitric oxide synthase delivery in rat hindlimb ischemia.
    Yan J, Tang GL, Wang R, Messina LM| | PubMed
  30. Vascular development of the brain requires beta8 integrin expression in the neuroepithelium.
    Proctor JM, Zang K, Wang D, Wang R, Reichardt LF| | PubMed
  31. Endothelial expression of constitutively active Notch4 elicits reversible arteriovenous malformations in adult mice.
    Carlson TR, Yan Y, Wu X, Lam MT, Tang GL, Beverly LJ, Messina LM, Capobianco AJ, Werb Z, Wang R| | PubMed
  32. VEGF is crucial for the hepatic vascular development required for lipoprotein uptake.
    Carpenter B, Lin Y, Stoll S, Raffai RL, McCuskey R, Wang R| | PubMed
  33. The effect of gradual or acute arterial occlusion on skeletal muscle blood flow, arteriogenesis, and inflammation in rat hindlimb ischemia.
    Tang GL, Chang DS, Sarkar R, Wang R, Messina LM| | PubMed
  34. Genomic progression in mouse models for liver tumors.
    Tward AD, Jones KD, Yant S, Kay MA, Wang R, Bishop JM| | PubMed
  35. CCR2-/- knockout mice revascularize normally in response to severe hindlimb ischemia.
    Tang G, Charo DN, Wang R, Charo IF, Messina L| | PubMed
  36. Adeno-associated viral vector-mediated gene transfer of VEGF normalizes skeletal muscle oxygen tension and induces arteriogenesis in ischemic rat hindlimb.
    Chang DS, Su H, Tang GL, Brevetti LS, Sarkar R, Wang R, Kan YW, Messina LM| | PubMed
  37. Activation of the Met receptor by cell attachment induces and sustains hepatocellular carcinomas in transgenic mice.
    Wang R, Ferrell LD, Faouzi S, Maher JJ, Bishop JM| | PubMed
  38. European surveillance of infections and risk factors in cancer patients.
    Buchheidt D, Hiddemann W, Schiel X, Kremery V, Karthaus M, Donnelly JP, Wilhelm M, Maschmeyer G, Link H, Adam D, Helmerking M| | PubMed
  39. Cellular adherence elicits ligand-independent activation of the Met cell-surface receptor.
    Wang R, Kobayashi R, Bishop JM| | PubMed
  40. Developmental analysis of bone tumors in polyomavirus transgenic mice.
    Wang R, Siegal GP, Scott DL, Bautch VL| | PubMed
  41. Embryonic stem cell-derived cystic embryoid bodies form vascular channels: an in vitro model of blood vessel development.
    Wang R, Clark R, Bautch VL| | PubMed
  42. Isolation and characterization of an established endothelial cell line from transgenic mouse hemangiomas.
    Dubois NA, Kolpack LC, Wang R, Azizkhan RG, Bautch VL| | PubMed
  43. The polyomavirus early region gene in transgenic mice causes vascular and bone tumors.
    Wang R, Bautch VL| | PubMed