Your search keyword '"McDonald, Donald M"' showing total 55 results

1. Controlling escape from angiogenesis inhibitors.

Author

Sennino, Barbara and McDonald, Donald M.

Subjects

*NEOVASCULARIZATION inhibitors, *VASCULAR endothelial growth factor antagonists, *HYPOXEMIA, *CANCER invasiveness, *CANCER treatment, *SINGLE nucleotide polymorphisms, *PROTEIN-tyrosine kinases

Abstract

Selective inhibition of vascular endothelial growth factor (VEGF) increases the efficacy of chemotherapy and has beneficial effects on multiple advanced cancers, but response is often limited and the disease eventually progresses. Changes in the tumour microenvironment - hypoxia among them - that result from vascular pruning, suppressed angiogenesis and other consequences of VEGF inhibition can promote escape and tumour progression. New therapeutic approaches that target pathways that are involved in the escape mechanisms add the benefits of blocking tumour progression to those of slowing tumour growth by inhibiting angiogenesis. [ABSTRACT FROM AUTHOR]

Published

2012

2. Markers for Microscopic Imaging of Lymphangiogenesis and Angiogenesis.

Author

Baluk, Peter and McDonald, Donald M.

Subjects

*NEOVASCULARIZATION, *BLOOD-vessel development, *SURGERY, *PROTEINS, *DIAGNOSIS, *GENETICS, *EMBRYOLOGY, *THERAPEUTICS, *MEDICAL care

Abstract

Imaging of lymphangiogenesis and angiogenesis requires robust and unambiguous markers of lymphatic and blood vessels. Although much progress has been made in recent years in identifying molecules specifically expressed on lymphatic and blood vessels, no perfect marker has been found that works reliably in all species, tissues, vascular beds, and in all physiological and pathologic conditions. The heterogeneity of expression of markers in both blood and lymphatic vessels reflects underlying differences in the phenotype of endothelial cells. Use of only one marker can lead to misleading interpretations, but these pitfalls can usually be avoided by use of multiple markers and three-dimensional whole-mount preparations. LYVE-1, VEGFR-3, Prox1, and podoplanin are among the most useful markers for microscopic imaging of lymphatic vessels, but, depending on histologic location, each marker can be expressed by other cell types, including vascular endothelial cells. Other markers, including CD31, junctional proteins, and receptors, such as VEGF-2, are shared by lymphatic and blood vessels. [ABSTRACT FROM AUTHOR]

Published

2008

3. Cellular actions of angiogenesis inhibitors on blood vessels.

Author

McDonald, Donald M.

Subjects

*BIBLIOGRAPHY, *NEOVASCULARIZATION inhibitors

Abstract

A list of articles related to cellular actions of angiogenesis inhibitors on blood vessels that were published in several journals is presented including "Endothelial gaps and permeability of venules in rat tracheas exposed to inflammatory stimuli," by D. M. McDonald, and "Mechanisms of adverse effects of anti-VEGF therapy for cancer," by T. Kamba and D. M. McDonald.

Published

2007

4. Imaging of Angiogenesis in Inflamed Airways and Tumors: Newly Formed Blood Vessels Are Not Alike and May Be Wildly Abnormal.

Author

McDonald, Donald M. and Baluk, Peter

Subjects

*NEOVASCULARIZATION, *TUMORS, *CYSTS (Pathology), *BLOOD vessels, *CARDIOVASCULAR system, *BLOOD circulation, *INFLAMMATION

Abstract

The article presents information on a paper which studied the imaging of angiogenesis in inflamed airways and tumors. The blood-vessels of the microvasculature have many common features which include an endothelial lining, mural cells and basement membrane enveloping both types of cells. This study used the simple microvasculature of the mouse trachea to address queries related to angiogenesis and lymphangiogenesis in chronic inflammation. Newly formed blood vessels in growing tumors are different from those in chronic airway inflammation. An increase in blood flow, plasma leakage, and leukocyte influx into inflamed tissues, the proliferation and remodeling of blood vessels facilitate clearance of allergens, toxins, organisms, and debris.

Published

2005

5. Imaging of angiogenesis: from microscope to clinic.

Author

McDonald, Donald M and Choyke, Peter L

Subjects

*NEOVASCULARIZATION, *IMAGING systems, *CLINICAL drug trials

Abstract

Advances in imaging are transforming our understanding of angiogenesis and the evaluation of drugs that stimulate or inhibit angiogenesis in preclinical models and human disease. Vascular imaging makes it possible to quantify the number and spacing of blood vessels, measure blood flow and vascular permeability, and analyze cellular and molecular abnormalities in blood vessel walls. Microscopic methods ranging from fluorescence, confocal and multiphoton microscopy to electron microscopic imaging are particularly useful for elucidating structural and functional abnormalities of angiogenic blood vessels. Magnetic resonance imaging (MRI), computed tomography (CT), positron emission tomography (PET), ultrasonography and optical imaging provide noninvasive, functionally relevant images of angiogenesis in animals and humans. An ongoing dilemma is, however, that microscopic methods provide their highest resolution on preserved tissue specimens, whereas clinical methods give images of living tissues deep within the body but at much lower resolution and specificity and generally cannot resolve vessels of the microcirculation. Future challenges include developing new imaging methods that can bridge this resolution gap and specifically identify angiogenic vessels. Another goal is to determine which microscopic techniques are the best benchmarks for interpreting clinical images. The importance of angiogenesis in cancer, chronic inflammatory diseases, age-related macular degeneration and reversal of ischemic heart and limb disease provides incentive for meeting these challenges. [ABSTRACT FROM AUTHOR]

Published

2003

6. Fixation alters the physical properties of tumor tissue that regulate nanomedicine transport.

Author

Martin, John D., Mpekris, Fotios, Chauhan, Vikash P., Martin, Margaret R., Walsh, Megan E., Stuber, Matthew D., McDonald, Donald M., Yuan, Fan, Stylianopoulos, Triantafyllos, and Jain, Rakesh K.

Subjects

*ACTIVE biological transport, *BIOLOGICAL transport, *TISSUE fixation (Histology), *HYDRAULIC conductivity, *LABORATORY mice

Abstract

To have the desired therapeutic effect, nanomedicines and macromolecular medications must move from the site of injection to the site of action, without having adverse effects. Transvascular transport is a critical step of this navigation, as exemplified by the Enhanced Permeability and Retention (EPR) effect in solid tumors, not found in normal organs. Numerous studies have concluded that passive, diffusion- and convection-based transport predominates over active, cellular mechanisms in this effect. However, recent work using a new approach reevaluated this principle by comparing tumors with or without fixation and concluded the opposite. Here, we address the controversy generated by this new approach by reporting evidence from experimental investigations and computer simulations that separate the contributions of active and passive transport. Our findings indicate that tissue fixation reduces passive transport as well as active transport, indicating the need for new methods to distinguish the relative contributions of passive and active transport. [ABSTRACT FROM AUTHOR]

Published

2024

7. Endothelial Gaps as Sites for Plasma Leakage in Inflammation.

Author

McDONALD, DONALD M, THURSTON, G A V I N, and BALUK, P E T E R

Subjects

*VASCULAR resistance, *ENDOTHELINS, *RESPIRATORY agents

Abstract

Objective: In 1961, Majno and Palade proposed that plasma leakage in acute inflammation caused by histamine, serotonin, or bradykinin results via gaps that form between endothelial cells of postcapillary venules. Now the relevance of endothelial gaps in plasma leakage is being questioned. The purpose of this review is to summarize experimental evidence from our studies showing that endothelial gaps participate in plasma leakage in inflammation. Methods: Using neurogenic inflammation as a model of plasma leakage in acute inflammation, we compared five methods to determine whether endothelial gaps form in the microvasculature of the rat trachea. 1) Endothelial cell borders and gaps were stained with silver nitrate and visualized by light, scanning, and transmission electron microscopy. 2) The luminal surface of endothelial cells was examined by scanning electron microscopy. 3) The luminal surface of endothelial cells was stained with a biotinylated lectin and avidin-biotin-peroxidase histochemistry, and then was examined by differential interference contrast microscopy. 4) Endothelial junctions were reconstructed from serial sections photographed by transmission electron microscopy. 5) Leakage was measured after perfusion of lectins or tracers through aldehyde-fixed vessels in situ. Results: The results from the five methods used in this system were consistent with the formation of gaps between endothelial cells. Endothelial gaps were rare or absent under baseline conditions, but appeared with the onset of plasma leakage and had a distribution that matched the distribution of leakage. Gaps had a complex morphology and were accompanied by fingerlike cell processes, which may anchor adjacent endothelial cells to one another and participate in gap closure. In contrast to normal vessels, vessels that were leaky in life continued to leak after aldehyde fixation, in evidence that, once formed, the leakage pathway did not require energy-dependent membrane movement or... [ABSTRACT FROM AUTHOR]

Published

1999

8. The beta2-adrenergic receptor agonist formoterol reduces microvascular leakage by inhibiting...

Author

Baluk, Peter and McDonald, Donald M.

Subjects

*ADRENERGIC beta agonists, *FORMOTEROL, *RESPIRATORY diseases

Abstract

Determines whether beta2-agonists can decrease plasma leakage by decreasing the number or size of endothelial gaps. Effect of formoterol on neurogenic plasma extravasation; Effects of formoterol on endothelial gap formation; Inflammatory stimuli; Measurement of increased vascular permeability; Silver staining; Morphometric methods.

Published

1994

9. Endothelial gaps and permeability of venules in rat tracheas exposed to inflammatory stimuli.

Author

McDonald, Donald M.

Subjects

*TRACHEITIS, *ENDOTHELIUM, *PERMEABILITY

Abstract

Determines the number of endothelial gaps in venules of the rat trachea. Relation of the number of gaps to the amount of plasma extravasation after an inflammatory stimulation; Quantification of the leukocyte attachment sites; Delineation of the tracheal vasculature; Effect of the closure of the gaps; Neurogenic stimulation.

Published

1994

10. New Antibody to Stop Tumor Angiogenesis and Lymphatic Spread by Blocking Receptor Partnering

Author

McDonald, Donald M.

Subjects

*IMMUNOGLOBULINS, *NEOVASCULARIZATION, *LYMPHATICS, *CELL receptors, *CANCER periodicals, *DIMERS, *VASCULAR endothelial growth factors, *LIGANDS (Biochemistry)

Abstract

describe in this issue of Cancer Cell an antibody that inhibits homodimerization of vascular endothelial growth factor receptor-3 (VEGFR-3) and its heterodimerization with VEGFR-2, but not ligand binding. The work provides mechanistic insights into receptor dimerization and an approach to suppress both angiogenesis and lymphangiogenesis. [ABSTRACT FROM AUTHOR]

Published

2010

11. Tighter lymphatic junctions prevent obesity.

Author

McDonald, Donald M.

Subjects

*PREVENTION of obesity, *CHYLOMICRONS, *FAT, *NEUROPILINS, *VASCULAR endothelial growth factor receptors, *ENDOTHELIAL cells

Abstract

A summary is presented of the article "Lacteal junction zippering protects against diet-induced obesity" by Feng Zhang, Georgia Zarkada, Jinah Han, and others which is published in the same issue. It mentions research into how chylomicrons, which package dietary fats in the digestive tract, which enter lymphatic channels. It states the research examined the contribution of neuropilin-1, vascular endothelial growth factor receptor-1, and endothelial cell receptors in regulating fat transport.

Published

2018

12. Permeability of the Endothelial Barrier: Identifying and Reconciling Controversies.

Author

Claesson-Welsh, Lena, Dejana, Elisabetta, and McDonald, Donald M.

Subjects

*PERMEABILITY, *ADHERENS junctions, *TIGHT junctions, *G protein coupled receptors, *ENDOTHELIAL cells, *HYPERPERFUSION

Abstract

Leakage from blood vessels into tissues is governed by mechanisms that control endothelial barrier function to maintain homeostasis. Dysregulated endothelial permeability contributes to many conditions and can influence disease morbidity and treatment. Diverse approaches used to study endothelial permeability have yielded a wealth of valuable insights. Yet, ongoing questions, technical challenges, and unresolved controversies relating to the mechanisms and relative contributions of barrier regulation, transendothelial sieving, and transport of fluid, solutes, and particulates complicate interpretations in the context of vascular physiology and pathophysiology. Here, we describe recent in vivo findings and other advances in understanding endothelial barrier function with the goal of identifying and reconciling controversies over cellular and molecular processes that regulate the vascular barrier in health and disease. In the microcirculation, endothelial permeability varies from least in arterioles to greatest in venules and is regulated in an organ-specific manner to control the extravasation of fluid, solutes, and large molecules. Inflammatory factors increase vascular permeability by inducing the formation of focal endothelial gaps that can be transient in acute inflammation or sustained in chronic conditions. Gap formation requires changes in the organization of tight junctions and adherens junctions that join endothelial cells and create a barrier. Adherens junction opening requires phosphorylation, loss of homophilic interactions, and internalization of VE-cadherin accompanied by changes in the cortical cytoskeleton. Sustained hyperpermeability in pathologic conditions can lead to edema, reduced vascular perfusion, impaired drug delivery, and exaggerated disease severity. [ABSTRACT FROM AUTHOR]

Published

2021

13. Vascular targeting and antigen presentation.

Author

Pasqualini, Renata, McDonald, Donald M., and Arap, Wadih

Subjects

*ANTIGEN presenting cells, *IMMUNE response

Abstract

Focuses on vascular targeting and antigen presenting cells. Augmentation or suppression of the immune response; Advantages of targeting endothelial cells; Molecules necessary for antigen presentation.

Published

2001

14. Heterogeneity of endothelial VE-PTP downstream polarization, Tie2 activation, junctional claudin-5, and permeability in the aorta and vena cava.

Author

Baluk, Peter, Shirakura, Keisuke, Vestweber, Dietmar, and McDonald, Donald M.

Subjects

*VENAE cavae, *AORTA, *PERMEABILITY, *PROTEIN-tyrosine phosphatase, *THORACIC aorta, *BLOOD vessels, *ENDOTHELIAL cells

Abstract

Endothelial cells of mammalian blood vessels have multiple levels of heterogeneity along the vascular tree and among different organs. Further heterogeneity results from blood flow turbulence and variations in shear stress. In the aorta, vascular endothelial protein tyrosine phosphatase (VE-PTP), which dephosphorylates tyrosine kinase receptor Tie2 in the plasma membrane, undergoes downstream polarization and endocytosis in endothelial cells exposed to laminar flow and high shear stress. VE-PTP sequestration promotes Tie2 phosphorylation at tyrosine992 and endothelial barrier tightening. The present study characterized the heterogeneity of VE-PTP polarization, Tie2-pY992 and total Tie2, and claudin-5 in anatomically defined regions of endothelial cells in the mouse descending thoracic aorta, where laminar flow is variable and IgG extravasation is patchy. We discovered that VE-PTP and Tie2-pY992 had mosaic patterns, unlike the uniform distribution of total Tie2. Claudin-5 at tight junctions also had a mosaic pattern, whereas VE-cadherin at adherens junctions bordered all endothelial cells. Importantly, the amounts of Tie2-pY992 and claudin-5 in aortic endothelial cells correlated with downstream polarization of VE-PTP. VE-PTP and Tie2-pY992 also had mosaic patterns in the vena cava, but claudin-5 was nearly absent and extravasated IgG was ubiquitous. Correlation of Tie2-pY992 and claudin-5 with VE-PTP polarization supports their collective interaction in the regulation of endothelial barrier function in the aorta, yet differences between the aorta and vena cava indicate additional flow-related determinants of permeability. Together, the results highlight new levels of endothelial cell functional mosaicism in the aorta and vena cava, where blood flow dynamics are well known to be heterogeneous. [ABSTRACT FROM AUTHOR]

Published

2024

15. Uptake of Cationic Liposomes by Normal and Angiogenic Endothelial Cells In Vivo.

Author

McDonald, Donald M.

Subjects

*LIPOSOMES, *GENETIC regulation, *ENDOTHELIUM

Abstract

Examines uptake of cationic liposomes by normal and angiogenic endothelial cells. Lack of intake of cationic liposomes by the endothelial cells in various organs; Charateristics of cationic liposomes based on its access to cells outside the vasculature; Implications of the intravascular delivery of cationic liposome-DNA complexes on gene therapy.

Published

1999

16. Cellular abnormalities of blood vessels as targets in cancer

Author

Baluk, Peter, Hashizume, Hiroya, and McDonald, Donald M

Subjects

*TUMORS, *BLOOD vessels, *GENE expression, *BIOLOGICAL membranes, *PROTEINS

Abstract

Tumor blood vessels have multiple structural and functional abnormalities. They are unusually dynamic, and naturally undergo sprouting, proliferation, remodeling or regression. The vessels are irregularly shaped, tortuous, and lack the normal hierarchical arrangement of arterioles, capillaries and venules. Endothelial cells in tumors have abnormalities in gene expression, require growth factors for survival and have defective barrier function to plasma proteins. Pericytes on tumor vessels are also abnormal. Aberrant endothelial cells and pericytes generate defective basement membrane. Angiogenesis inhibitors can stop the growth of tumor vessels, prune existing vessels and normalize surviving vessels. Loss of endothelial cells is not necessarily accompanied by simultaneous loss of pericytes and surrounding basement membrane, which together can then provide a scaffold for regrowth of tumor vessels. Rapid vascular regrowth reflects the ongoing drive for angiogenesis and bizarre microenvironment in tumors that promote vascular abnormalities and thereby create therapeutic targets. [Copyright &y& Elsevier]

Published

2005

17. Shear stress-induced upregulation of connexin 43 expression in endothelial cells on upstream surfaces of rat cardiac valves.

Author

Inai, Tetsuichiro, Mancuso, Michael R., McDonald, Donald M., Kobayashi, Junichi, Nakamura, Kyoko, and Shibata, Yosaburo

Subjects

*PROTEINS, *GAP junctions (Cell biology), *CELLS, *ENDOTHELIUM, *HEART valves, *GENE expression, *LABORATORY rats

Abstract

Endothelial expression of the gap junction proteins, connexin (Cx) 37, Cx40, and Cx43, varies within the vascular network. While previous studies suggest that shear stress may upregulate Cx43, it is not well understood if shear stress affects the expression of all endothelial connexins and to what extent. Endothelial cells on the upstream and downstream surfaces of cardiac valves are subjected to considerably different intensities of shear stress. We therefore reasoned that we could determine the extent hemodynamic forces affect the ex- pression of Cx37, Cx40, and Cx43 by comparing their immunohistochemical distribution on the upstream and downstream surfaces of rat cardiac valves. We found 70- to 200-fold greater expression of Cx43 in the endothelial cells on the upstream than on the downstream surfaces. However, Cx37 was expressed almost equally in the endothelial cells on upstream and downstream surfaces, and Cx40, a major connexin in most vascular endothelial cells, was not detected on either surface. In addition to the heterogeneity in Cx43 expression, endothelial cells on the upstream surface were 35% to 65% smaller than those on the corresponding downstream surface. These results suggest that shear stress may affect endothelial cell size and Cx43 expression but not Cx37 expression. [ABSTRACT FROM AUTHOR]

Published

2004

18. Probing the structural and molecular diversity of tumor vasculature

Author

Pasqualini, Renata, Arap, Wadih, and McDonald, Donald M.

Subjects

*BLOOD-vessel tumors, *CANCER treatment, *DIAGNOSIS

Abstract

The molecular diversity of the vasculature provides a rational basis for developing targeted diagnostics and therapeutics for cancer. Targeted imaging agents would offer better localization of primary tumors and metastases, and targeted therapies would improve efficacy and reduce side effects. The development of targeted pharmaceuticals requires the identification of specific ligand–receptor pairs, and knowledge of their cellular distribution and accessibility. Using in vivo phage display, a technique by which we can identify organ-specific and disease-specific proteins expressed on the endothelial surface, it is now possible to decipher the molecular signature of blood vessels in normal and diseased tissues. These studies have already led to the identification of peptides that target the normal vasculature of the brain, kidney, pancreas, lung and skin, as well as the abnormal vasculature of tumors, arthritis and atherosclerosis. Membrane dipeptidase in the lungs, interleukin-11 receptor in the prostate, and aminopeptidase N in tumors are examples of molecular targets on blood vessels. Corresponding confocal-microscopic imaging and ultrastructural studies are providing a more complete understanding of the cellular abnormalities of tumor blood vessels, and the distribution and accessibility of potential targets. The combined approach offers a strategy for creating a ligand–receptor map of the human vasculature, and forms a foundation for the development and application of targeted therapies in cancer and other diseases. [ABSTRACT FROM AUTHOR]

Published

2002

19. Determinants of Endothelial Cell Phenotype in Venules.

Author

THURSTON, G A V I N, BALUK, P E T E R, and McDONALD, DONALD M

Subjects

*INFLAMMATION, *NEOVASCULARIZATION, *BLOOD flow

Abstract

Inflammatory stimuli cause plasma leakage and leukocyte adhesion in venules but not in capillaries or arterioles. The specific response of venules is governed by phenotypic specialization of the venular endothelial cells. What regulates this specialized phenotype? Several recent developments have shed new light on this question and may challenge our thinking about regulation of the venular endothelial cell phenotype. In this review, we consider some of the molecular markers of venular endothelial cells, the hemodynamic and molecular factors that may regulate the phenotype of venular endothelial cells, and abnormalities in endothelial cell phenotype in disease-related angiogenesis and microvascular remodeling. The expanding list of molecular markers may help clarify the physiologic and molecular factors that regulate the phenotype of venular endothelial cells in normal development and disease. [ABSTRACT FROM AUTHOR]

Published

2000

20. Unexpected contribution of lymphatic vessels to promotion of distant metastatic tumor spread.

Author

Qiaoli Ma, Dieterich, Lothar C., Ikenberg, Kristian, Bachmann, Samia B., Mangana, Johanna, Proulx, Steven T., Amann, Valerie C., Levesque, Mitchell P., Dummer, Reinhard, Baluk, Peter, McDonald, Donald M., and Detmar, Michael

Subjects

*LYMPHATICS, *METASTASIS, *PATIENTS, *SENTINEL lymph nodes, *CANCER

Abstract

The article offers information on a study which reveals unexpected contributions of lymphatics in distant organs to the promotion of growth of metastases and their further spread to other organs, with potential clinical implications for adjuvant therapies in patients with metastatic cancer. It mentions that tumor lymphangiogenesis is accompanied by a higher incidence of sentinel lymph node metastasis and shorter overall survival in several types of cancer.

Published

2018

21. Opposing actions of angiopoietin-2 on Tie2 signaling and FOXO1 activation.

Author

Kim, Minah, Allen, Breanna, Korhonen, Emilia A., Nitschké, Maximilian, Hee Won Yang, Baluk, Peter, Saharinen, Pipsa, Alitalo, Kari, Daly, Christopher, Thurston, Gavin, McDonald, Donald M., and Yang, Hee Won

Subjects

*ANGIOPOIETIN-2, *FORKHEAD transcription factors, *GENE silencing, *VASCULAR remodeling, *BLOOD vessels, *MYCOPLASMA diseases, *GENETIC overexpression, *THERAPEUTICS

Abstract

Angiopoietin-2 (ANG2) regulates blood vessel remodeling in many pathological conditions through differential effects on Tie2 signaling. While ANG2 competes with ANG1 to inhibit Tie2, it can paradoxically also promote Tie2 phosphorylation (p-Tie2). A related paradox is that both inactivation and overactivation of Tie2 can result in vascular remodeling. Here, we reconciled these opposing actions of ANG2 by manipulating conditions that govern its actions in the vasculature. ANG2 drove vascular remodeling during Mycoplasma pulmonis infection by acting as a Tie2 antagonist, which led to p-Tie2 suppression, forkhead box O1 (FOXO1) activation, increased ANG2 expression, and vessel leakiness. These changes were exaggerated by anti-Tie2 antibody, inhibition of PI3K signaling, or ANG2 overexpression and were reduced by anti-ANG2 antibody or exogenous ANG1. In contrast, under pathogen-free conditions, ANG2 drove vascular remodeling by acting as an agonist, promoting high p-Tie2, low FOXO1 activation, and no leakage. Tie1 activation was strong under pathogen-free conditions, but infection or TNF-α led to Tie1 inactivation by ectodomain cleavage and promoted the Tie2 antagonist action of ANG2. Together, these data indicate that ANG2 activation of Tie2 supports stable enlargement of normal nonleaky vessels, but reduction of Tie1 in inflammation leads to ANG2 antagonism of Tie2 and initiates a positive feedback loop wherein FOXO1-driven ANG2 expression promotes vascular remodeling and leakage. [ABSTRACT FROM AUTHOR]

Published

2016

22. Tie1 controls angiopoietin function in vascular remodeling and inflammation.

Author

Korhonen, Emilia A., Lampinen, Anita, Giri, Hemant, Anisimov, Andrey, Kim, Minah, Allen, Breanna, Shentong Fang, D'Amico, Gabriela, Sipilä, Tuomas J., Lohela, Marja, Strandin, Tomas, Vaheri, Antti, Ylä-Herttuala, Seppo, Gou Young Koh, McDonald, Donald M., Alitalo, Kari, Saharinen, Pipsa, Fang, Shentong, and Koh, Gou Young

Subjects

*ANGIOPOIETIN-1, *VASCULAR remodeling, *INFLAMMATION, *ANGIOPOIETIN-2, *SEPSIS, *ENDOTHELIAL cells, *PHOSPHORYLATION, *PROTEIN metabolism, *ANIMALS, *ANTIGENS, *CELL receptors, *CELLULAR signal transduction, *ENDOTHELIUM, *EPITHELIAL cells, *LONGITUDINAL method, *MICE, *GENETIC mutation, *ENDOTOXEMIA, *CASE-control method, *LIPOPOLYSACCHARIDES

Abstract

The angiopoietin/Tie (ANG/Tie) receptor system controls developmental and tumor angiogenesis, inflammatory vascular remodeling, and vessel leakage. ANG1 is a Tie2 agonist that promotes vascular stabilization in inflammation and sepsis, whereas ANG2 is a context-dependent Tie2 agonist or antagonist. A limited understanding of ANG signaling mechanisms and the orphan receptor Tie1 has hindered development of ANG/Tie-targeted therapeutics. Here, we determined that both ANG1 and ANG2 binding to Tie2 increases Tie1-Tie2 interactions in a β1 integrin-dependent manner and that Tie1 regulates ANG-induced Tie2 trafficking in endothelial cells. Endothelial Tie1 was essential for the agonist activity of ANG1 and autocrine ANG2. Deletion of endothelial Tie1 in mice reduced Tie2 phosphorylation and downstream Akt activation, increased FOXO1 nuclear localization and transcriptional activation, and prevented ANG1- and ANG2-induced capillary-to-venous remodeling. However, in acute endotoxemia, the Tie1 ectodomain that is responsible for interaction with Tie2 was rapidly cleaved, ANG1 agonist activity was decreased, and autocrine ANG2 agonist activity was lost, which led to suppression of Tie2 signaling. Tie1 cleavage also occurred in patients with hantavirus infection. These results support a model in which Tie1 directly interacts with Tie2 to promote ANG-induced vascular responses under noninflammatory conditions, whereas in inflammation, Tie1 cleavage contributes to loss of ANG2 agonist activity and vascular stability. [ABSTRACT FROM AUTHOR]

Published

2016

23. Regulation of Hepatocyte Growth Factor in Mice with Pneumonia by Peptidases and Trans-Alveolar Flux.

Author

Raymond, Wilfred W., Xu, Xiang, Nimishakavi, Shilpa, Le, Catherine, McDonald, Donald M., and Caughey, George H.

Subjects

*HEPATOCYTE growth factor, *PNEUMONIA treatment, *PEPTIDASE, *LUNG injuries, *NEUTROPHILS, *EPITHELIAL cells

Abstract

Hepatocyte growth factor (HGF) promotes lung epithelial repair after injury. Because prior studies established that human neutrophil proteases inactivate HGF in vitro, we predicted that HGF levels decrease in lungs infiltrated with neutrophils and that injury is less severe in lungs lacking HGF-inactivating proteases. After establishing that mouse neutrophil elastase cleaves mouse HGF in vitro, we tested our predictions in vivo by examining lung pathology and HGF in mice infected with Mycoplasma pulmonis, which causes neutrophilic tracheobronchitis and pneumonia. Unexpectedly, pneumonia severity was similar in wild type and dipeptidylpeptidase I-deficient (Dppi-/-) mice lacking neutrophil serine protease activity. To assess how this finding related to our prediction that Dppi-activated proteases regulate HGF levels, we measured HGF in serum, bronchoalveolar lavage fluid, and lung tissue from Dppi+/+ and Dppi-/- mice. Contrary to prediction, HGF levels were higher in lavage fluid from infected mice. However, serum and tissue concentrations were not different in infected and uninfected mice, and HGF lung transcript levels did not change. Increased HGF correlated with increased albumin in lavage fluid from infected mice, and immunostaining failed to detect increased lung tissue expression of HGF in infected mice. These findings are consistent with trans-alveolar flux rather than local production as the source of increased HGF in lavage fluid. However, levels of intact HGF from infected mice, normalized for albumin concentration, were two-fold higher in Dppi-/- versus Dppi+/+ lavage fluid, suggesting regulation by Dppi-activated proteases. Consistent with the presence of active HGF, increased expression of activated receptor c-Met was observed in infected tissues. These data suggest that HGF entering alveoli from the bloodstream during pneumonia compensates for destruction by Dppi-activated inflammatory proteases to allow HGF to contribute to epithelial repair. [ABSTRACT FROM AUTHOR]

Published

2015

24. Mast Cells Present Protrusions into Blood Vessels upon Tracheal Allergen Challenge in Mice.

Author

Bose, Oishee, Baluk, Peter, Looney, Mark R., Cheng, Laurence E., McDonald, Donald M., Caughey, George H., and Krummel, Matthew F.

Subjects

*MAST cells, *BLOOD vessels, *ALLERGENS, *DENDRITIC cells, *ANTIGENS, *LABORATORY mice

Abstract

Mast cells (MC) and myeloid dendritic cells (DC) act proximally in detecting and processing antigens and immune insults. We sought to understand their comparative dynamic behavior with respect to the airway epithelium in the steady state and in response to an allergic stimulus in mouse trachea. We devised methods to label MC in living trachea and to demonstrate that MC and DC occupy distinct layers of the tracheal mucosa, with DC being closer to the lumen. DC numbers doubled after allergen challenge, but MC numbers remained stable. MC and DC migrated minimally in either steady state or allergen-challenge conditions, and their interactions with one another appeared to be stochastic and relatively infrequent. While DC, unlike MC, exhibited probing behaviors involving dendrites, these projections did not cross the epithelium into the airway lumen. MC typically were located too far from the epithelial surface to contact the tracheal lumen. However, MC had protrusions toward and into blood vessels, likely to load with IgE. Thus, DC and MC occupy distinct niches and engage in sessile surveillance in the mouse trachea. Little or no access of these cell types to the airway lumen suggests that trans-epithelial transport of proteins in the steady state would be required for them to access luminal antigens. [ABSTRACT FROM AUTHOR]

Published

2015

25. IL-7 production in murine lymphatic endothelial cells and induction in the setting of peripheral lymphopenia.

Author

Miller, Corey N., Hartigan-O’Connor, Dennis J., Lee, Myeong Sup, Laidlaw, Grace, Cornelissen, Ivo P., Matloubian, Mehrdad, Coughlin, Shaun R., McDonald, Donald M., and McCune, Joseph M.

Subjects

*INTERLEUKIN-7, *LYMPHOPENIA, *LABORATORY mice, *T cells, *ENDOTHELIAL cells, *GREEN fluorescent protein, *LYMPHOCYTES

Abstract

IL-7 is a required factor for T-cell homeostasis. Because of low expression levels and poor reagent availability, the cellular sources of IL-7 have proven challenging to characterize. In this study, we describe a reporter mouse in which enhanced GFP is expressed from the endogenous Il7 locus. We show that IL-7 is produced by lymphatic endothelial cells (LECs) distributed throughout the systemic lymphatic vasculature as well as by fibroblastic reticular cells, and that phosphorylation of STAT5 in lymphocytes is higher in lymphatics than in blood. Furthermore, in nodes depleted of lymphocytes, Il7 transcription is increased in stromal but not in myeloid subsets. These data support recent findings that lymphocyte homeostasis is influenced by access to secondary lymphoid organs and point to LECs as an important in vivo source of IL-7, bathing trafficking immune cells under both resting and lymphopenic conditions. [ABSTRACT FROM PUBLISHER]

Published

2013

26. Inhibition of c-Met Reduces Lymphatic Metastasis in RIP-Tag2 Transgenic Mice.

Author

Sennino, Barbara, Ishiguro-Oonuma, Toshina, Schriver, Brian J., Christensen, James G., and McDonald, Donald M.

Subjects

*LYMPHATIC metastasis, *MET receptor, *VASCULAR endothelial growth factors, *CELLULAR signal transduction, *TRANSGENIC mice, *PROTEIN-tyrosine kinase inhibitors

Abstract

Inhibition of VEGF signaling can promote lymph node metastasis in preclinical models, but the mechanism is not fully understood, and successful methods of prevention have not been found. Signaling of hepatocyte growth factor (HGF) and its receptor c-Met can promote the growth of lymphatics and metastasis of some tumors. We sought to explore the contributions of c-Met signaling to lymph node metastasis after inhibition of VEGF signaling. In particular, we examined whether c-Met is upregulated in lymphatics in or near pancreatic neuroendocrine tumors in RIP-Tag2 transgenic mice and whether lymph node metastasis can be reduced by concurrent inhibition of VEGF and c-Met signaling. Inhibition of VEGF signaling by anti-VEGF antibody or sunitinib in mice from the age of 14 to 17 weeks was accompanied by more intratumoral lymphatics, more tumor cells inside lymphatics, and more lymph node metastases. Under these conditions, lymphatic endothelial cells, like tumor cells, had strong immunoreactivity for c-Met and phospho-c-Met. c-Met blockade by the selective inhibitor, PF-04217903, significantly reduced metastasis to local lymph nodes. Together, these results indicate that inhibition of VEGF signaling in RIP-Tag2 mice upregulates c-Met expression in lymphatic endothelial cells, increases the number of intratumoral lymphatics and number of tumor cells within lymphatics, and promotes metastasis to local lymph nodes. Prevention of lymph node metastasis by PF-04217903 in this setting implicates c- Met signaling in tumor cell spread to lymph nodes. [ABSTRACT FROM AUTHOR]

Published

2013

27. Therapeutic angiogenesis due to balanced single-vector delivery of VEGF and PDGF-BB.

Author

Banfi, Andrea, von Degenfeld, Georges, Gianni-Barrera, Roberto, Reginato, Silvia, Merchant, Milton J., McDonald, Donald M., and Blau, Helen M.

Subjects

*NEOVASCULARIZATION, *VASCULAR endothelial growth factors, *GENE therapy, *PLATELET-derived growth factor, *ISCHEMIA

Abstract

Therapeutic angiogenesis by delivery of vascular growth factors is an attractive strategy for treating debilitating occlusive vascular diseases, yet clinical trials have thus far failed to show efficacy. As a result, limb amputation remains a common outcome for muscle ischemia due to severe atherosclerotic disease, with an overall incidence of 100 per million people in the United States per year. A challenge has been that the angiogenic master regulator vascular endothelial growth factor (VEGF) induces dysfunctional vessels, if expressed outside of a narrow dosage window. We tested the hypothesis that codelivery of platelet-derived growth factor-BB (PDGF-BB), which recruits pericytes, could induce normal angiogenesis in skeletal muscle irrespective of VEGF levels. Coexpression of VEGF and PDGF-BB encoded by separate vectors in different cells or in the same cells only partially corrected aberrant angiogenesis. In marked contrast, coexpression of both factors in every cell at a fixed relative level via a single bicistronic vector led to robust, uniformly normal angiogenesis, even when VEGF expression was high and heterogeneous. Notably, in an ischemic hindlimb model, single-vector expression led to efficient growth of collateral arteries, revascularization, increased blood flow, and reduced tissue damage. Furthermore, these results were confirmed in a clinically applicable gene therapy approach by adenoviral-mediated delivery of the bicistronic vector. We conclude that coordinated expression of VEGF and PDGF-BB via a single vector constitutes a novel strategy for harnessing the potency of VEGF to induce safe and efficacious angiogenesis. [ABSTRACT FROM AUTHOR]

Published

2012

28. Permeability to macromolecular contrast media quantified by dynamic MRI correlates with tumor tissue assays of vascular endothelial growth factor (VEGF)

Author

Cyran, Clemens C., Sennino, Barbara, Fu, Yanjun, Rogut, Victor, Shames, David M., Chaopathomkul, Bundit, Wendland, Michael F., McDonald, Donald M., Brasch, Robert C., and Raatschen, Hans-Juergen

Subjects

*CONTRAST media, *MOLECULAR diagnosis, *MAGNETIC resonance imaging, *VASCULAR endothelial growth factors, *TISSUES, *PERMEABILITY (Biology), *ALBUMINS

Abstract

Abstract: Purpose: To correlate dynamic MRI assays of macromolecular endothelial permeability with microscopic area–density measurements of vascular endothelial growth factor (VEGF) in tumors. Methods and material: This study compared tumor xenografts from two different human cancer cell lines, MDA-MB-231 tumors (n =5), and MDA-MB-435 (n =8), reported to express respectively higher and lower levels of VEGF. Dynamic MRI was enhanced by a prototype macromolecular contrast medium (MMCM), albumin-(Gd-DTPA)35. Quantitative estimates of tumor microvascular permeability (K PS; μl/min×100cm3), obtained using a two-compartment kinetic model, were correlated with immunohistochemical measurements of VEGF in each tumor. Results: Mean K PS was 2.4 times greater in MDA-MB-231 tumors (K PS =58±30.9μl/min×100cm3) than in MDA-MB-435 tumors (K PS =24±8.4μl/min×100cm3) (p <0.05). Correspondingly, the area–density of VEGF in MDA-MB-231 tumors was 2.6 times greater (27.3±2.2%, p <0.05) than in MDA-MB-435 cancers (10.5±0.5%, p <0.05). Considering all tumors without regard to cell type, a significant positive correlation (r =0.67, p <0.05) was observed between MRI-estimated endothelial permeability and VEGF immunoreactivity. Conclusion: Correlation of MRI assays of endothelial permeability to a MMCM and VEGF immunoreactivity of tumors support the hypothesis that VEGF is a major contributor to increased macromolecular permeability in cancers. When applied clinically, the MMCM-enhanced MRI approach could help to optimize the appropriate application of VEGF-inhibiting therapy on an individual patient basis. [Copyright &y& Elsevier]

Published

2012

29. VEGF and c-Met Blockade Amplify Angiogenesis Inhibition in Pancreatic Islet Cancer.

Author

Weon-Kyoo You, Sennino, Barbara, Williamson, Casey W., Falcón, Beverly, Hashizume, Hiroya, Li-Chin Yao, Aftab, Dana T., and McDonald, Donald M.

Subjects

*NEOVASCULARIZATION, *CANCER invasiveness, *METASTASIS, *ISLANDS of Langerhans, *PANCREATIC cancer, *PROTEIN-tyrosine kinases, *CANCER

Abstract

Angiogenesis inhibitors that block VEGF receptor (VEGFR) signaling slow the growth of many types of tumors, but eventually the disease progresses. Multiple strategies are being explored to improve efficacy by concurrent inhibition of other functionally relevant receptor tyrosine kinases (RTK). XL880 (foretinib, GSK1363089) and XL184 (cabozantinib) are small-molecule inhibitors that potently block multiple RTKs, including VEGFR and the receptor of hepatocyte growth factor c-Met, which can drive tumor invasion and metastasis. This study compared the cellular effects of XL880 and XL184 with those of an RTK inhibitor (XL999) that blocks VEGFR but not c-Met. Treatment of RIP-Tag2 mice with XL999 resulted in 43% reduction in vascularity of spontaneous pancreatic islet tumors over 7 days, but treatment with XL880 or XL184 eliminated approximately 80% of the tumor vasculature, reduced pericytes and empty basement membrane sleeves, caused widespread intratumoral hypoxia and tumor cell apoptosis, and slowed regrowth of the tumor vasculature after drug withdrawal. Importantly, XL880 and XL184 also decreased invasiveness of primary tumors and reduced metastasis. Overall, these findings indicate that inhibition of c-Met and functionally related kinases amplifies the effects of VEGFR blockade and leads to rapid, robust, and progressive regression of tumor vasculature, increased intratumoral hypoxia and apoptosis, and reduced tumor invasiveness and metastasis. Cancer Res; 71(14); 4758-68. © 2011 AACR. [ABSTRACT FROM AUTHOR]

Published

2011

30. TNF-alpha drives remodeling of blood vessels and lymphatics in sustained airway inflammation in mice.

Author

Baluk, Peter, Yao, Li-Chin, Feng, Jennifer, Romano, Talia, Jung, Sonia S, Schreiter, Jessica L, Yan, Li, Shealy, David J, and McDonald, Donald M

Subjects

*BLOOD-vessel physiology, *LYMPHATIC physiology, *RESPIRATORY organ anatomy, *BLOOD vessels, *LYMPHATICS, *ANIMALS, *ANTIGENS, *CELL receptors, *CELLULAR signal transduction, *GLYCOPROTEINS, *INFLAMMATION, *MICE, *MYCOPLASMA, *MYCOPLASMA diseases, *RESPIRATORY organs, *TUMOR necrosis factors, *FETAL development, *GENE expression profiling, *ANATOMY

Abstract

Inflammation is associated with blood vessel and lymphatic vessel proliferation and remodeling. The microvasculature of the mouse trachea provides an ideal opportunity to study this process, as Mycoplasma pulmonis infection of mouse airways induces widespread and sustained vessel remodeling, including enlargement of capillaries into venules and lymphangiogenesis. Although the mediators responsible for these vascular changes in mice have not been identified, VEGF-A is known not to be involved. Here, we sought to determine whether TNF-alpha drives the changes in blood vessels and lymphatics in M. pulmonis-infected mice. The endothelial cells, but not pericytes, of blood vessels, but not lymphatics, were immunoreactive for TNF receptor 1 (TNF-R1) and lymphotoxin B receptors. Most TNF-R2 immunoreactivity was on leukocytes. Infection resulted in a large and sustained increase in TNF-alpha expression, as measured by real-time quantitative RT-PCR, and smaller increases in lymphotoxins and TNF receptors that preceded vessel remodeling. Substantially less vessel remodeling and lymphangiogenesis occurred when TNF-alpha signaling was inhibited by a blocking antibody or was silenced in Tnfr1-/- mice. When administered after infection was established, the TNF-alpha-specific antibody slowed but did not reverse blood vessel remodeling and lymphangiogenesis. The action of TNF-alpha on blood vessels is probably mediated through direct effects on endothelial cells, but its effects on lymphangiogenesis may require inflammatory mediators from recruited leukocytes. We conclude that TNF-alpha is a strong candidate for a mediator that drives blood vessel remodeling and lymphangiogenesis in inflammation. [ABSTRACT FROM AUTHOR]

Published

2009

31. TNF-α drives remodeling of blood vessels and lymphatics in sustained airway inflammation in mice.

Author

Baluk, Peter, Li-Chin Yao, Feng, Jennifer, Romano, Talia, Jung, Sonia S., Schreiter, Jessica L., Li Van, Shealy, David J., and McDonald, Donald M.

Subjects

*IMMUNOLOGY of inflammation, *MICROCIRCULATION disorders, *TUMOR necrosis factors, *BLOOD vessels, *LYMPHATICS, *MICE as carriers of disease

Abstract

Inflammation is associated with blood vessel and lymphatic vessel proliferation and remodeling. The microvasculature of the mouse trachea provides an ideal opportunity to study this process, as Mycoplasmapulmonis infection of mouse airways induces widespread and sustained vessel remodeling, including enlargement of capillaries into venules and lymphangiogenesis. Although the mediators responsible for these vascular changes in mice have not been identified, VEGF-A is known not to be involved. Here, we sought to determine whether TNF-α drives the changes in blood vessels and lymphatics in M. pulmonis-infected mice. The endothelial cells, but not pericytes, ofblood vessels, but not lymphatics, were immunoreactive for TNF receptor 1 (TNF-R1) and lymphotoxin B receptors. Most TNF-R2 inimunoreactivity was on leukocytes. Infection resulted in a large and sustained increase in TNF-α expression, as measured by real-time quantitative RT-PCR, and smaller increases in lymphotoxins and TNF receptors that preceded vessel remodeling. Substantially less vessel remodeling and lymphangiogenesis occurred when TNF-a signaling was inhibited by a blocking antibody or was silenced in Tnfr1-/- mice. When administered after infection was established, the TNF-α-specific antibody slowed but did not reverse blood vessel remodeling and lymphangiogenesis. The action ofTNF-α on blood vessels is probably mediated through direct effects on endothelial cells, but its effects on lymphangiogenesis may require inflammatory mediators from recruited leukocytes. We conclude that TNF-α is a strong candidate for a mediator that drives blood vessel remodeling and lymphangiogenesis in inflanimation. [ABSTRACT FROM AUTHOR]

Published

2009

32. Magnetic resonance imaging for monitoring the effects of thalidomide on experimental human breast cancers.

Author

Cyran CC, Sennino B, Chaopathomkul B, Fu Y, Rogut VS, Shames DM, Wendland MF, McDonald DM, Brasch RC, Cyran, Clemens C, Sennino, Barbara, Chaopathomkul, Bundit, Fu, Yanjun, Rogut, Victor S, Shames, David M, Wendland, Michael F, McDonald, Donald M, and Brasch, Robert C

Abstract

Thalidomide, which inhibits angiogenesis in certain tumor types, reduced extravasation of a macromolecular contrast medium (MMCM) in a human breast cancer model as assayed by MMCM-enhanced dynamic magnetic resonance imaging (MRI) and fluorescence microscopy in the same tumors. After a 1-week, three-dose course of thalidomide, the mean MRI-assayed endothelial transfer coefficient, K(PS), decreased significantly (p < 0.05) from 19.4 +/- 9.1 to 6.3 +/- 9.1 microl/min.100 cm(3). Correspondingly, microscopic measurements of extravasated MMCM, expressed as fractional area of streptavidin staining, were significantly (p < 0.05) lower in thalidomide-treated tumors (18.6 +/- 11.9%) than in control saline-treated tumors (50.2 +/- 2.3%). On a tumor-by-tumor basis, post-treatment K(PS) values correlated significantly (r(2) = 0.55, p < 0.05) with microscopic measures of MMCM extravasation. However, no significant differences were observed between saline- and thalidomide-treated tumors with respect to rate of growth, vascular richness, or amount of VEGF-containing cells. Because of its sensitivity to the detection of changes in vascular leakage in tumors, this MMCM-enhanced MRI assay could prove useful for monitoring the effects of thalidomide on an individual patient basis. The significant correlation between MRI and fluorescence microscopic measures of MMCM extravasation supports the utility of the non-invasive MRI approach for assessing the action of thalidomide on tumor blood vessels. [ABSTRACT FROM AUTHOR]

Published

2009

33. Lymphatic endothelial cell identity is reversible and its maintenance requires Prox1 activity.

Author

Johnson, Nicole C., Dillard, Miriam E., Baluk, Peter, McDonald, Donald M., Harvey, Natasha L., Frase, Sharon L., and Oliver, Guillermo

Subjects

*GENOTYPE-environment interaction, *GENES, *GENETICS, *GROWTH factors, *CYTOKINES, *PHENOTYPES

Abstract

The activity of the homeobox gene Prox1 is necessary and sufficient for venous blood endothelial cells (BECs) to acquire a lymphatic endothelial cell (LEC) fate. We determined that the differentiated LEC phenotype is a plastic, reprogrammable condition that depends on constant Prox1 activity for its maintenance. We show that conditional down-regulation of Prox1 during embryonic, postnatal, or adult stages is sufficient to reprogram LECs into BECs. Consequently, the identity of the mutant lymphatic vessels is also partially reprogrammed as they acquire some features typical of the blood vasculature. siRNA-mediated down-regulation of Prox1 in LECs in culture demonstrates that reprogramming of LECs into BECs is a Prox1-dependent, cell-autonomous process. We propose that Prox1 acts as a binary switch that suppresses BEC identity and promotes and maintains LEC identity; switching off Prox1 activity is sufficient to initiate a reprogramming cascade leading to the dedifferentiation of LECs into BECs. Therefore, LECs are one of the few differentiated cell types that require constant expression of a certain gene to maintain their phenotypic identity. [ABSTRACT FROM AUTHOR]

Published

2008

34. Organization and signaling of endothelial cell-to-cell junctions in various regions of the blood and lymphatic vascular trees.

Author

Dejana, Elisabetta, Orsenigo, Fabrizio, Molendini, Cinzia, Baluk, Peter, and McDonald, Donald M.

Subjects

*CELL junctions, *ENDOTHELIUM, *BLOOD vessels, *CELL growth, *GROWTH factors

Abstract

Adhesive intercellular junctions between endothelial cells are formed by tight junctions and adherens junctions. In addition to promoting cell-to-cell adhesion, these structures regulate paracellular permeability, contact inhibition of endothelial cell growth, cell survival, and maintenance of cell polarity. Furthermore, adherens junctions are required for the correct organization of new vessels during embryo development or during tissue proliferation in the adult. Extensive research on cultured epithelial and endothelial cells has resulted in the identification of many molecular components of tight junctions and adherens junctions. Such studies have revealed the complexity of these structures, which are formed by membrane-associated adhesion proteins and a network of several intracellular signaling partners. This review focuses on the structural organization of junctional structures and their functional interactions in the endothelium of blood vessels and lymphatics. We emphasize the way that these structures regulate endothelial cell homeostasis by transferring specific intracellular signals and by modulating activation and signaling of growth factor receptors. [ABSTRACT FROM AUTHOR]

Published

2008

35. Soluble receptor-mediated selective inhibition of VEGFR and PDGFRß signaling during physiologic and tumor angiogenesis.

Author

Kuhnert, Frank, Tam, Betty V. V., Sennino, Barbara, Gray, John T., Yuan, Jenny, Jocson, Angeline, Nayak, Nihar R, Mulligan, Richard C., McDonald, Donald M., and Kuo, Calvin J.

Subjects

*NEOVASCULARIZATION, *TUMORS, *DRUG antagonism, *THERAPEUTICS, *MESSENGER RNA

Abstract

The simultaneous targeting of both endothelial cells and pericytes via inhibition of VEGF receptor (VEGFR) and PDGFβ receptor (PDGFRβ) signaling, respectively, has been proposed to enhance the efficacy of antiangiogenic tumor therapy. Clinical and preclinical modeling of combined VEGFR and PDGFRβ signaling inhibition, however, has used small molecule kinase inhibitors with inherently broad substrate specificities, precluding detailed examination of this hypothesis. Here, adenoviral expression of a soluble VEGFR2/Flk1 ectodomain (Ad Flk1-Fc) in combination with a soluble ectodomain of PDGFRβ (Ad sPDGFRβ) allowed highly selective inhibition of these pathways. The activity of Ad SPDGFRβ was validated in vitro against PDGF-BB and in vivo with near-complete blockade of pericyte recruitment in the angiogenic corpus luteum, resulting in prominent hemorrhage, thus demonstrating an essential function for PDGF signaling during ovarian angiogenesis. Combination therapy with Ad PDGFRβ and submaximal doses of Ad Flk1-Fc produced modest additive antitumor effects; however, no additivity was observed with maximal VEGF inhibition in numerous s.c. models. Notably. VEGF inhibition via Ad Flk1-Fc was sufficient to strongly suppress tumor endothelial and pericyte content as well as intratumoral PDGF-B mRNA. obscuring additive Ad SPDGFRβ effects on pericytes or tumor volume. These studies using highly specific soluble receptors suggest that additivity between VEGFR and PDGFRβ inhibition depends on the strength of VEGF blockade and appears minimal under conditions of maximal VEGF antagonism. [ABSTRACT FROM AUTHOR]

Published

2008

36. Cell labeling with the positive MR contrast agent Gadofluorine M.

Author

Henning, Tobias D., Saborowski, Olaf, Golovko, Daniel, Boddington, Sophie, Bauer, Jan S., Yanjun Fu, Meier, Reinhard, Pietsch, Hubertus, Sennino, Barbara, McDonald, Donald M., Daldrup-Link, Heik E., Fu, Yanjun, and Daldrup-Link, Heike E

Subjects

*MONOCYTES, *FLUORESCENCE microscopy, *MACROPHAGES, *PSYCHOANALYSIS, *RADIOSCOPIC diagnosis, *MEDICAL radiography, *RADIOGRAPHY, *CELL culture, *COMPARATIVE studies, *MAGNETIC resonance imaging, *RESEARCH methodology, *MEDICAL cooperation, *MICROSCOPY, *ORGANOMETALLIC compounds, *RESEARCH, *RESEARCH funding, *SPECTROPHOTOMETRY, *STAINS & staining (Microscopy), *EVALUATION research, *CONTRAST media

Abstract

The purpose of this study was to label human monocytes with Gadofluorine M by simple incubation for subsequent cell depiction at 1.5 and 3 T. Gadofluorine M displays a high r(1) relaxivity and is spontaneously phagocytosed by macrophages. Human monocytes were incubated with Gadofluorine M-Cy at varying concentrations and incubation times and underwent MR imaging at 1.5 and 3 T at increasing time intervals after the labeling procedure. R1-relaxation rates and r1 relaxivities of the labeled cells and non-labeled controls were determined. Cellular contrast agent uptake was examined by fluorescence microscopy and quantified by ICP-AES. Efficient cell labeling was achieved after incubation of the cells with 25 mM Gd Gadofluorine M for 12 h, resulting in a maximal uptake of 0.3 fmol Gd/cell without impairment of cell viability. Fluorescence microscopy confirmed internalization of the fluorescent contrast agent by monocytes. The r1 relaxivity of the labeled cells was 137 mM(-1)s(-1) at 1.5 T and 80.46 mM(-1)s(-1) at 3 T. Imaging studies showed stable labeling for at least 7 days. Human monocytes can be effectively labeled for MR imaging with Gadofluorine M. Potential in vivo cell-tracking applications include targeting of inflammatory processes with Gadofluorine-labeled leukocytes or monitoring of stem cell therapies for the treatment of arthritis. [ABSTRACT FROM AUTHOR]

Published

2007

37. Rapid vascular regrowth in tumors after reversal of VEGF inhibition.

Author

Mancuso, Michael R., Davis, Rachel, Norberg, Scott M., O'Brien, Shaun, Sennino, Barbara, Nakahara, Tsutomu, Yao, Virginia J., Inai, Tetsuichiro, Brooks, Peter, Freimark, Bruce, Shalinsky, David R., Hu-Lowe, Dana D., and McDonald, Donald M.

Subjects

*VASCULAR endothelial growth factors, *NEOVASCULARIZATION, *BLOOD-vessel development, *CANCER treatment, *LUNG cancer, *TUMOR growth

Abstract

Inhibitors of VEGF signaling can block angiogenesis and reduce tumor vascularity, but little is known about the reversibility of these changes after treatment ends. In the present study, regrowth of blood vessels in spontaneous RIP-Tag2 tumors and implanted Lewis lung carcinomas in mice was assessed after inhibition of VEGF receptor signaling by AG-013736 or AG-028262 for 7 days. Both agents caused loss of 50%–60% of tumor vasculature. Empty sleeves of basement membrane were left behind. Pericytes also survived but had less α—SMA immunoreactivity. One day after drug withdrawal, endothelial sprouts grew into empty sleeves of basement membrane. Vessel patency and connection to the bloodstream followed close behind. By 7 days, tumors were fully revascularized, and the pericyte phenotype returned to baseline. Importantly, the regrown vasculature regressed as much during a second treatment as it did in the first. Inhibition of MMPs or targeting of type IV collagen cryptic sites by antibody HUIV26 did not eliminate the sleeves or slow revascularization. These results suggest that empty sleeves of basement membrane and accompanying pericytes provide a scaffold for rapid revascularization of tumors after removal of anti-VEGF therapy and highlight their importance as potential targets in cancer therapy. [ABSTRACT FROM AUTHOR]

Published

2006

38. Rapid vascular regrowth in tumors after reversal of VEGF inhibition.

Author

Mancuso, Michael R., Davis, Rachel, Norberg, Scott M., O'Brien, Shaun, Sennino, Barbara, Nakahara, Tsutomu, Yao, Virginia J., Inai, Tetsuichiro, Brooks, Peter, Freimark, Bruce, Shalinsky, David R., Hu-Lowe, Dana D., and McDonald, Donald M.

Subjects

*VASCULAR endothelial growth factors, *TUMOR growth, *NEOVASCULARIZATION inhibitors, *REGENERATION (Biology), *BLOOD vessels, *CANCER treatment, *CELL receptors, *BASAL lamina

Abstract

Inhibitors of VEGF signaling can block angiogenesis and reduce tumor vascularity, but little is known about the reversibility of these changes after treatment ends. In the present study, regrowth of blood vessels in spontaneous RIP-Tag2 tumors and implanted Lewis lung carcinomas in mice was assessed after inhibition of VEGF receptor signaling by AG-013736 or AG-028262 for 7 days. Both agents caused loss of 50%-60% of tumor vasculature. Empty sleeves of basement membrane were left behind. Pericytes also survived but had less alpha-SMA immunoreactivity. One day after drug withdrawal, endothelial sprouts grew into empty sleeves of basement membrane. Vessel patency and connection to the bloodstream followed close behind. By 7 days, tumors were fully revascularized, and the pericyte phenotype returned to baseline. Importantly, the regrown vasculature regressed as much during a second treatment as it did in the first. Inhibition of MMPs or targeting of type IV collagen cryptic sites by antibody HUIV26 did not eliminate the sleeves or slow revascularization. These results suggest that empty sleeves of basement membrane and accompanying pericytes provide a scaffold for rapid revascularization of tumors after removal of anti-VEGF therapy and highlight their importance as potential targets in cancer therapy. [ABSTRACT FROM AUTHOR]

Published

2006

39. Essential role of nitric oxide in VEGF-induced, asthma-like angiogenic, inflammatory, mucus, and physiologic responses in the lung.

Author

Bhandari, Vineet, Choo-Wing, Rayman, Chapoval, Svetlana P., Lee, Chun G., Tang, C., Kim, V. K., Ma, Bing, Baluk, Peter, Lin, Michelle I., McDonald, Donald M., Homer, Robert J., Sessa, William C., and Elias, Jack A.

Subjects

*VASCULAR endothelial growth factors, *NITRIC oxide, *ASTHMA, *NEOVASCULARIZATION, *LABORATORY mice, *HYPERPLASIA

Abstract

VEGF, nitric oxide (NO), inflammation, and vascular- and extravascular remodeling coexist in asthma and other disorders. In these responses, VEGF regulates angiogenesis. VEGF also induces inflammation and remodeling. The mechanisms of the latter responses have not been defined, however. We hypothesized that VEGF-induces extravascular tissue responses via NO-dependent mechanisms. To evaluate this hypothesis, we compared the effects of transgenic VEGF165 in lungs from normal mice, mice treated with pan-NO synthase (NOS) or endothelial NOS (eNOS) inhibitors, and mice with null mutations of inducible NOS (iNOS) or eNOS. These studies demonstrate that VEGF selectively stimulates eNOS and iNOS. They also demonstrate that VEGF induces pulmonary alterations via NO-dependent and -independent mechanisms with angiogenesis, edema, mucus metaplasia, airway hyperresponsive- ness, lymphocyte accumulation, dendritic cell hyperplasia and S-nitrosoglutathione reductase stimulation being NO-dependent and dendritic cell activation being NO-independent. Furthermore, they demonstrate that eNOS and iNOS both contribute to these responses. NO/NOS-based interventions may be therapeutic in VEGF-driven inflammation and remodeling. [ABSTRACT FROM AUTHOR]

Published

2006

40. Cellular changes in normal blood capillaries undergoing regression after inhibition of VEGF signaling.

Author

Baffert, Fabienne, Tom Le, Sennino, Barbara, Thurston, Gavin, Kuo, Calvin J., Hu-Lowe, Dana, and McDonald, Donald M.

Subjects

*VASCULAR endothelial growth factors, *GROWTH factors, *CYTOKINES, *HUMAN growth hormone, *VASCULAR endothelium, *BLOOD vessels

Abstract

The vasculature of the embryo requires vascular endothelial growth factor (VEOF) during development, but most adult blood vessels lose VEGF dependence. However, some capillaries in the respiratory tract and selected other organs of adult mice regress after VEGF inhibition. The present study sought to identify the sequence of events and the fate of endothelial cells, pericytes, and vascular basement membrane during capillary regression in mouse tracheas after VEGF signaling was blocked with a VEGF-receptor tyrosine kinase inhibitor AG-013736 or soluble receptor construct (VEGF Trap or soluble adenoviral VEGFR-1). Within I day, patency was lost and fibrin accumulated in some tracheal capillaries. Apoptotic endothelial cells marked by activated caspase-3 were present in capillaries without blood flow. VEGF inhibition was accompanied by a 19% decrease in tracheal capillaries over 7 days and 30% over 21 days. During this period, desmin/NG2- immunoreactive pericytes moved away from regressing capillaries onto surviving vessels. Empty sleeves of basement membrane, left behind by regressing endothelial cells, persisted for about 2 wk and served as a scaffold for vascular regrowth after treatment ended. The amount of regrowth was limited by the number of surviving basement membrane sleeves. These findings demonstrate that, after inhibition of VEGF signaling, some normal capillaries regress in a systematic sequence of events initiated by a cessation of blood flow and followed by apoptosis of endothelial cells, migration of pericytes away from regressing vessels, and formation of empty basement membrane sleeves that can facilitate capillary regrowth. [ABSTRACT FROM AUTHOR]

Published

2006

41. VEGF-dependent plasticity of fenestrated capillaries in the normal adult microvasculature.

Author

Kamba, Tomomi, Tam, Betty Y. Y., Hashizume, Hiroya, Haskell, Amy, Sennino, Barbara, Mancuso, Michael R., Norberg, Scott M., O'Brien, Shaun M., Davis, Rachel B., Gowen, Lori C., Anderson, Keith D., Thurston, Gavin, Joho, Shuji, Springer, Matthew L., Kuo, Calvin J., and McDonald, Donald M.

Subjects

*VASCULAR endothelial growth factors, *GROWTH factors, *VASCULAR endothelium, *BLOOD vessels, *TUMORS, *PATHOLOGY

Abstract

Unlike during development, blood vessels in the adult are generally thought not to require VEOF for normal function. However, VEGF is a survival factor for many tumor vessels, and there are clues that some normal blood vessels may also depend on VEGF. In this study, we sought to identify which, if any, vascular beds in adult mice depend on VEGF for survival. Mice were treated with a small-molecule VEGF receptor (VEGFR) tyrosine kinase inhibitor or soluble VEOFRs for 1–3 wk. Blood vessels were assessed using immunohistochemistry or scanning or transmission electron microscopy. In a study of 17 normal organs after VEGF inhibition, we found significant capillary regression in pancreatic islets, thyroid, adrenal cortex, pituitary, choroid plexus, small-intestinal villi, and epididymal adipose tissue. The amount of regression was dose dependent and varied from organ to organ, with a maximum of 68% in thyroid, but was less in normal organs than in tumors in RIP-Tag2-transgenic mice or in Lewis lung carcinoma. VEOF-dependent capillaries were fenestrated, expressed high levels of both VEOFR-2 and VEGFR-3, and had normal pericyte coverage. Surviving capillaries in affected organs had fewer fenestrations and less VEGFR expression. All mice appeared healthy, but distinct physiological changes, including more efficient blood glucose handling, accompanied some regimens of VEGF inhibition. Strikingly, most capillaries in the thyroid grew back within 2 wk after cessation of treatment for 1 wk. Our findings of VEGF dependency of normal fenestrated capillaries and rapid regrowth after regression demonstrate the plasticity of the adult microvasculature. [ABSTRACT FROM AUTHOR]

Published

2006

42. Angiopoietin-1 decreases plasma leakage by reducing number and size of endothelial gaps in venules.

Author

Baffert, Fabienne, Le, Tom, Thurston, Gavin, and McDonald, Donald M.

Subjects

*AIRWAY (Anatomy), *CELLULAR mechanics, *BRADYKININ, *KININS, *CONFOCAL microscopy

Abstract

Angiopoietin-1 (Ang-1) is essential for remodeling of the primitive vascular plexus and recruitment of mural cells during embryonic development. In the adult vasculature, Ang-1 can reduce plasma leakage in inflammation, but the mechanism of this action is not well understood. In the present study, we determined the magnitude and cellular mechanism of the antileak effect of Ang-1 in the airways of mice. Intravenous injection of bradykinin resulted in leakage of fluorescent microspheres (diameter 25-1,000 nm) from tracheal venules. The leakage peaked in 3-4 mm and resolved by 10 mm. High-resolution confocal microscopy revealed the presence of focal gaps at intercellular junctions of leaky venules. Genetically engineered Ang- 1*, delivered systemically by adenoviral transduction of the liver, reduced leakage of 500-nm microspheres after bradykinin by 69%. The reduction in leakage coincided with a decrease in number and size of endothelial gaps. The proportion of venular surface occupied by endothelial gaps decreased 61%. Microsphere leakage correlated strongly with gap number and size (r² = 0.89). Together the results suggest that Ang-1 reduces leakage from inflamed venules by restricting the number and size of gaps that form at endotheliaI cell junctions through effects on intracellular signaling, cytoskeleton, and junction-related molecules. [ABSTRACT FROM AUTHOR]

Published

2006

43. Angiopoietin 1 causes vessel enlargement, without angiogenic sprouting, during a critical developmental period.

Author

Thurston, Gavin, Quan Wang, Baffert, Fabienne, Rudge, John, Papadopoulos, Nicholas, Jean-Guillaume, Danielle, Wiegand, Stanley, Yancopoulos, George D., and McDonald, Donald M.

Subjects

*NEOVASCULARIZATION, *BLOOD vessels, *CELLS, *VASCULAR endothelial growth factors, *CELL proliferation

Abstract

Early in development, endothelial cells proliferate, coalesce, and sprout to form a primitive plexus of undifferentiated microvessels. Subsequently, this plexus remodels into a hierarchical network of different-sized vessels. Although the processes of proliferation and sprouting are well studied and are dependent on the angiogenic growth factor VEGF, the factors involved in subsequent vessel remodeling are poorly understood. Here, we show that angiopoietin 1 can induce circumferential vessel enlargement, specifically on the venous side of the circulation. This action is due to the ability of angiopoietin 1 to promote endothelial cell proliferation in the absence of angiogenic sprouting; vessel growth without sprouting has not been ascribed to other vascular growth factors, nor has specificity for a particular segment of the vasculature. Moreover, angiopoietin 1 potently mediates widespread vessel enlargement only during a brief postnatal period, in particular, prior to the fourth postnatal week, corresponding to stages in which VEGF inhibition causes widespread vessel regression. These findings show that angiopoietin 1 has a potentially unique role among the vascular growth factors by acting to enlarge blood vessels without inducing sprouting, and also define a critical window of vascular plasticity in neonatal development. Finding the key molecular factors that regulate this plasticity may prove crucial to the further development of pro- and anti-angiogenic therapies. [ABSTRACT FROM AUTHOR]

Published

2005

44. Pathogenesis of persistent lymphatic vessel hyperplasia in chronic airway inflammation.

Author

Baluk, Peter, Tammela, Tuomas, Ator, Erin, Lyubynska, Natalya, Achen, Marc G., Hicklin, Daniel J., Jeltsch, Michael, Petrova, Tatiana V., Pytowski, Bronislaw, Stacker, Steven A., Ylä-Herttuala, Seppo, Jackson, David G., Alitalo, Kari, McDonald, Donald M., and Ylä-Herttuala, Seppo

Subjects

*INFLAMMATION, *CELLULAR pathology, *ANTIASTHMATIC agents, *CILIA & ciliary motion, *CYTOKINES, *CONNECTIVE tissue cells, *HYPERPLASIA, *ANIMAL experimentation, *BRONCHI, *CELLULAR signal transduction, *CHRONIC diseases, *COMPARATIVE studies, *DENDRITIC cells, *GENES, *LYMPH nodes, *LYMPHATICS, *MACROPHAGES, *RESEARCH methodology, *MEDICAL cooperation, *MICE, *MYCOPLASMA, *MYCOPLASMA diseases, *NEUTROPHILS, *PULMONARY edema, *RESEARCH, *RESPIRATORY mucosa, *RESPIRATORY obstructions, *VIRUSES, *EVALUATION research, *ENDOTHELIAL growth factors, *PATHOLOGIC neovascularization, *METABOLISM

Abstract

Edema occurs in asthma and other inflammatory diseases when the rate of plasma leakage from blood vessels exceeds the drainage through lymphatic vessels and other routes. It is unclear to what extent lymphatic vessels grow to compensate for increased leakage during inflammation and what drives the lymphangiogenesis that does occur. We addressed these issues in mouse models of (a) chronic respiratory tract infection with Mycoplasma pulmonis and (b) adenoviral transduction of airway epithelium with VEGF family growth factors. Blood vessel remodeling and lymphangiogenesis were both robust in infected airways. Inhibition of VEGFR-3 signaling completely prevented the growth of lymphatic vessels but not blood vessels. Lack of lymphatic growth exaggerated mucosal edema and reduced the hypertrophy of draining lymph nodes. Airway dendritic cells, macrophages, neutrophils, and epithelial cells expressed the VEGFR-3 ligands VEGF-C or VEGF-D. Adenoviral delivery of either VEGF-C or VEGF-D evoked lymphangiogenesis without angiogenesis, whereas adenoviral VEGF had the opposite effect. After antibiotic treatment of the infection, inflammation and remodeling of blood vessels quickly subsided, but lymphatic vessels persisted. Together, these findings suggest that when lymphangiogenesis is impaired, airway inflammation may lead to bronchial lymphedema and exaggerated airflow obstruction. Correction of defective lymphangiogenesis may benefit the treatment of asthma and other inflammatory airway diseases. [ABSTRACT FROM AUTHOR]

Published

2005

45. Vascular endothelial growth factor (VEGF) induces remodeling and enhances TH2-mediated sensitization and inflammation in the lung.

Author

Chun Geun Lee, Link, Holger, Baluk, Peter, Homer, Robert J., Chapoval, Svetlana, Bhandari, Vineet, Min Jong Kang, Cohn, Lauren, Yoon Keun Kim, McDonald, Donald M., and Elias, Jack A.

Subjects

*VASCULAR endothelial growth factors, *ASTHMA, *TRANSGENIC mice, *EDEMA, *METAPLASIA, *DENDRITIC cells

Abstract

Exaggerated levels of VEGF (vascular endothelial growth factor) are present in persons with asthma, but the role(s) of VEGF in normal and asthmatic lungs has not been defined. We generated lung-targeted VEGF165 transgenic mice and evaluated the role of VEGF in T-helper type 2 cell (TH2)-mediated inflammation. In these mice, VEGF induced, through IL-13-dependent and-independent pathways, an asthma-like phenotype with inflammation, parenchymal and vascular remodeling, edema, mucus metaplasia, myocyte hyperplasia and airway hyper-responsiveness. VEGF also enhanced respiratory antigen sensitization and TH2 inflammation and increased the number of activated DC2 dendritic cells. In antigen-induced inflammation, VEGF was produced by epithelial cells and preferentially by TH2 versus TH1 cells. In this setting, it had a critical role in TH2 inflammation, cytokine production and physiologic dysregulation. Thus, VEGF is a mediator of vascular and extravascular remodeling and inflammation that enhances antigen sensitization and is crucial in adaptive TH2 inflammation. VEGF regulation may be therapeutic in asthma and other TH2 disorders. [ABSTRACT FROM AUTHOR]

Published

2004

46. Matrix metalloproteinase-2 and -9 expression increases in Mycoplasma-infected airways but is not required for microvascular remodeling.

Author

Baluk, Peter, Raymond, Wilfred W., Ator, Erin, Coussens, Lisa M., McDonald, Donald M., and Caughey, George H.

Subjects

*METALLOPROTEINASES, *EXTRACELLULAR matrix proteins, *MYCOPLASMA, *AIRWAY (Anatomy), *LUNG physiology, *MICROCIRCULATION

Abstract

Murine Mycoplasma pulmonis infection induces chronic lung and airway inflammation accompanied by profound and persistent microvascular remodeling in tracheobronchial mucosa. Because matrix metalloproteinase (MMP)-2 and -9 are important for angiogenesis associated with placental and long bone development and skin cancer, we hypothesized that they contribute to microvascular remodeling in airways infected with M. pulmonis. To test this hypothesis, we compared microvascular changes in airways after M. pulmonis infection of wild-type FVB/N mice with those of MMP9-/- and MMP-2-/- /MMP-9-/- double-null mice and mice treated with the broad-spectrum MMP inhibitor AG3340 (Prinomastat). Using zymography and immunohistochemistry, we find that MMP-2 and MMP-9 rise strikingly in lungs and airways of infected wild-type FVB/N and C57BL/6 mice, with no zymographic activity or immunoreactivity in MMP-2-/-/MMP-9-/- animals. However, microvascular remodeling as assessed by Lycopersicon esculentum lectin staining of whole-mounted tracheae is as severe in infected MMP-9-/-, MMP-2-/-/MMP-9-/- and AG3340-treated mice as in wild-type mice. Furthermore, all groups of infected mice develop similar inflammatory infiltrates and exhibit similar overall disease severity as indicated by decrease in body weight and increase in lung weight. Uninfected wild-type tracheae show negligible MMP-2 immunoreactivity, with scant MMP-9 immunoreactivity in and around growing cartilage. By contrast, MMP-2 appears in epithelial cells of infected, wild-type tracheae, and MMP-9 localizes to a large population of infiltrating leukocytes. We conclude that despite major increases in expression, MMP-2 and MMP-9 are not essential for microvascular remodeling in M. pulmonis-induced chronic airway inflammation. [ABSTRACT FROM AUTHOR]

Published

2004

47. Microenvironmental VEGF concentration, not total dose, determines a threshold between normal and aberrant angiogenesis.

Author

Ozawa, Clare R., Banfi, Andrea, Glazer, Nicole L., Thurston, Gavin, Springer, Matthew L., Kraft, Peggy E., McDonald, Donald M., and Blau, Helen M.

Subjects

*VASCULAR endothelial growth factors, *NEOVASCULARIZATION, *BLOOD-vessel development, *MYOBLASTS, *VASCULAR diseases, *GROWTH factors

Abstract

Use of long-term constitutive expression of VEGF for therapeutic angiogenesis may be limited by the growth of abnormal blood vessels and hemangiomas. We investigated the relationship between VEGF dosage and the morphology and function of newly formed blood vessels by implanting retrovirally transduced myoblasts that constitutively express VEGF164 into muscles of adult mice. Reducing VEGF dosage by decreasing the total number of VEGF myoblasts implanted did not prevent vascular abnormalities. However, when clonal populations of myoblasts homogeneously expressing different levels of VEGF were implanted, a threshold between normal and aberrant angiogenesis was found. Clonal myoblasts that expressed low to medium levels of VEGF induced growth of stable, pericyte-coated capillaries of uniform size that were not leaky and became VEGF independent, as shown by treatment with the potent VEGF blocker VEGF-TrapR1R2. In contrast, clones that expressed high levels of VEGF induced hemangiomas. Remarkably, when different clonal populations were mixed, even a small proportion of cells with high production of VEGF was sufficient to cause hemangioma growth. These results show for the first time to our knowledge that the key determinant of whether VEGF-induced angiogenesis is normal or aberrant is the microenvironmental amount of growth factor secreted, rather than the overall dose. Long-term continuous delivery of VEGF, when maintained below a threshold microenvironmental level, can lead to normal angiogenesis without other exogenous growth factors. [ABSTRACT FROM AUTHOR]

Published

2004

48. Microenvironmental VEGF concentration, not total dose, determines a threshold between normal and aberrant angiogenesis.

Author

Ozawa, Clare R, Banfi, Andrea, Glazer, Nicole L, Thurston, Gavin, Springer, Matthew L, Kraft, Peggy E, McDonald, Donald M, and Blau, Helen M

Subjects

*EAR anatomy, *ANIMAL experimentation, *BLOOD vessels, *CELL culture, *CELL transplantation, *COMPARATIVE studies, *RESEARCH methodology, *MEDICAL cooperation, *MICE, *NEOVASCULARIZATION, *RESEARCH, *PHENOTYPES, *STEM cells, *EVALUATION research, *VASCULAR endothelial growth factors, *PATHOLOGIC neovascularization, *ANATOMY, *PHYSIOLOGY

Abstract

Use of long-term constitutive expression of VEGF for therapeutic angiogenesis may be limited by the growth of abnormal blood vessels and hemangiomas. We investigated the relationship between VEGF dosage and the morphology and function of newly formed blood vessels by implanting retrovirally transduced myoblasts that constitutively express VEGF164 into muscles of adult mice. Reducing VEGF dosage by decreasing the total number of VEGF myoblasts implanted did not prevent vascular abnormalities. However, when clonal populations of myoblasts homogeneously expressing different levels of VEGF were implanted, a threshold between normal and aberrant angiogenesis was found. Clonal myoblasts that expressed low to medium levels of VEGF induced growth of stable, pericyte-coated capillaries of uniform size that were not leaky and became VEGF independent, as shown by treatment with the potent VEGF blocker VEGF-TrapR1R2. In contrast, clones that expressed high levels of VEGF induced hemangiomas. Remarkably, when different clonal populations were mixed, even a small proportion of cells with high production of VEGF was sufficient to cause hemangioma growth. These results show for the first time to our knowledge that the key determinant of whether VEGF-induced angiogenesis is normal or aberrant is the microenvironmental amount of growth factor secreted, rather than the overall dose. Long-term continuous delivery of VEGF, when maintained below a threshold microenvironmental level, can lead to normal angiogenesis without other exogenous growth factors. [ABSTRACT FROM AUTHOR]

Published

2004

49. Expression of genes involved in vascular development and angiogenesis in endothelial cells of adult lung.

Author

Favre, Cecile J., Mancuso, Michael, Maas, Kevin, McLean, John W., Baluk, Peter, and McDonald, Donald M.

Subjects

*GENE expression, *ENDOTHELIUM, *CAPILLARIES

Abstract

Profiling gene expression in endothelial cells advances the understanding of normal vascular physiology and disease processes involving angiogenesis. However, endothelial cell purification has been challenging because of the difficulty of isolating cells and their low abundance. Here we examine gene expression in endothelial cells freshly isolated from lung capillaries after in vivo labeling with fluorescent cationic liposomes and purification by fluorescence-activated cell sorting (FACS). Of the 39,000 genes and expressed sequence tags evaluated on custom oligonucleotide arrays, 555 were enriched in endothelial cell fraction. These included familiar endothelial cell-associated genes such as VEGF, VEGF receptor (VEGFR)-1, VEGFR-2, angiopoietin-2, Tie1, Tie2, Edg1 receptor, VE-cadherin, claudin 5, connexin37, CD31, and CD34. Also enriched were genes in semaphorin/neuropilin (Sema3c and Nrp1), ephrin/Eph (ephrin A1, B1, B2, and EphB4), delta/notch (Hey1, Jagged 2, Notch 1, Notch 4, Numb, and Siah1b), and Wingless (Frizzled-4 and Tle1) signaling pathways involved in vascular development and angiogenesis. Expression of representative genes in alveolar capillary endothelial cells was verified by immunohistochemistry. Such expression reflects features that endothelial cells of normal lung capillaries have in common with embryonic and growing blood vessels. About half of the enriched genes, including exostosin 2, lipocalin 7, phospholipid scramblase 2, pleckstrin 2, protocadherin 1, Ryk, scube 1, serpinh1, SNFrelated kinase, and several tetraspanins, had little or no previous association with endothelial cells. This approach can readily be used to profile genes expressed in blood vessels in tumors, chronic inflammation, and other sites in which endothelial cells avidly take up cationic liposomes. [ABSTRACT FROM AUTHOR]

Published

2003

50. Mechanisms of increased immunogenicity for DNA-based vaccines adsorbed onto cationic microparticles

Author

Denis-Mize, Kimberly S., Dupuis, Marc, Singh, Manmohan, Woo, Carolyn, Ugozzoli, Mildred, O’Hagan, Derek T., Donnelly III, John J., Ott, Gary, and McDonald, Donald M.

Subjects

*VACCINES, *IMMUNE response, *PLASMIDS, *LYMPHOCYTES, *IMMUNIZATION

Abstract

Investigation into the mechanism of action of vaccine adjuvants provides opportunities to define basic immune principles underlying the induction of strong immune responses and insights useful for the rational development of subunit vaccines. A novel HIV vaccine composed of plasmid DNA-encoding p55 gag formulated with poly-lactide-co-glycolide microparticles (PLG) and cetyl trimethyl ammonium bromide (CTAB) elicits both serum antibody titers and cytotoxic lymphocyte activity in mice at doses two orders of magnitude lower than those required for comparable response to plasmid DNA in saline. Using this model, we demonstrated the increase in potency requires the DNA to be complexed to the PLG–CTAB microparticles. Furthermore, the PLG–CTAB–DNA formulation increased the persistence of DNA at the injection site, recruited mononuclear phagocytes to the site of injection, and activated a population of antigen presenting cells. Intramuscular immunization with the PLG–CTAB–DNA complex induced antigen expression at both the injection site and the draining lymph node. These findings demonstrate that the PLG–CTAB–DNA formulation exhibits multiple mechanisms of immunopotentiation. [Copyright &y& Elsevier]

Published

2003