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The Department is proud to announce the following new grants to support our industry-leading research:

Development of Long-acting Vascular Endothelial Growth Factor (VEGF) as a therapeutic for Wound Healing
The Science and Technology Ventures Office of Columbia has provided Dr. Joyce Lustbader with funding to support this work. This technology increases the longevity of Vascular Endothelial Growth Factor (VEGF) from minutes to almost ten hours. VEGF is the most potent known stimulator of angiogenesis, and has wide ranging potential for many applications, including, but not limited to, wound healing and closure. VEGF-LA is a distinct, chemically modified version of VEGF, engineered with site-specific glycosylation. VEGF-LA represents a novel approach that can supplement existing wound healing strategies. Wound healing is a mature competitive space, and while recruitment of growth factors is an active strategy in commercial development, current technologies have not fully addressed the benefits of improved angiogenesis. One factor limiting innovation has been the cost associated with the effective use of growth factors, given the low half life of these molecules in vivo. The dramatic increase in half-life associated with VEGF-LA could provide a cost-effective way of administering potent pro-angiogenic therapy. The technology could provide valuable new characteristics to wound healing products ranging from sterile dressings, antimicrobial products, or pharmaceutical treatments (e.g. for diabetic ulcer).

Gonadotropin Inhibitors: A Structural Biology Approach to Immunocontraception
It is well established that the gonadotropins hCG and FSH are critical factors required for maintenance of gonadal function. Interference of hormone activity by specific antibodies disrupts reproductive processes in male and female. This is the premise for the development of male and female contraceptive vaccines. A prerequisite for successful development for these vaccines is the thorough understanding of the structures of both hormones and their specific receptors so that new and novel strategies for producing specific antigens for immunocontraception can be developed. In addition, with better understanding of the gonadotropin and their receptors it will be possible to design molecules that will interfere in the actions of gonadotropins leading to disruption of reproductive function. The principal objective of the proposal is to investigate the structure-function relationship of gonadotropins to prepare new contraceptive vaccines. Dr. Joyce Lustbader is this project which is being funded by the Joint Indo-US Program on Contraception and Reproductive Health Research (CRHR).

17Alpha-Estradiol: A Study of Its Functional Adaptation on the Brain
Dr. Dominique Toran-Allerand has been funded by the National Science Foundation to study the role of 17alpha-estradiol in the brain. Functional adaptation of the brain throughout life involves its ability to reorganize itself, following injury or disease, through the formation of new neural connections by interactions with environmental stimuli. Such stimuli include changing levels of circulating sex hormones, such as the estrogen 17beta-estradiol, and androgens, such as testosterone, that can be converted by the enzyme aromatase to 17beta-estradiol. It is generally accepted that 17beta-estradiol is the estrogen active in the brain, while its little studied isomer, 17alpha-estradiol, a chemical compound with the same molecular formula but different functional groups, is largely ignored and generally considered biologically inactive. This NSF proposal considers that this concept is inaccurate and addresses the role of 17alpha-estradiol in the brain, about which little is known. We propose that 17alpha-estradiol, which, unlike 17beta-estradiol, is not made in the ovaries but synthesized primarily in the brain, may be the more important estrogen for such neural functions as neurogenesis [new neuron formation] in the adult hippocampus, a brain region implicated in learning, memory and mood regulation. We have recently found that the content of 17alpha-estradiol is significantly higher than that of 17beta-estradiol in the brains of adult mice of both sexes, as determined by mass spectrometry, a technique used to determine the structure of a molecule or compound by fragmenting it into its component parts. Complicating matters are our findings that sesame oil, in which estrogens are frequently dissolved before use, may itself have properties that also induce cell division and are antidepressant. This proposal consists of a series of correlative experiments, using hippocampal neurons in culture and intact mice with either very low or elevated brain levels of 17alpha-estradiol, to compare the effects of 17alpha-estradiol, 17beta-estradiol, sesame oil and the antidepressant desipramine, on (i) neurogenesis, (ii) as antidepressants, and (iii) on the synthesis of the growth factor BDNF (brain-derived neurotrophic factor), a growth factor with antidepressant properties.

Notch as a Diagnostic Marker and Therapeutic Target in Human Breast Cancer
In the United States, breast cancer is the second most common cancer and contributes to 40,000 deaths a year. Early detection is key to improving survival as more than 90% of women will live longer than 10 years after the diagnosis if tumors are 10 millimeters or smaller in size. Current diagnostic tool include mammography and biopsy, but the former technique is nonspecific (cannot distinguish between malignant and non-malignant tumors) and is not infallible, as a certain proportion (11%) of tumors are not detected. Thus, all women would benefit by the development of a more specific and sensitive method of screening. Fortunately, progress has been made in our understanding of the biochemical and molecular mechanisms of breast cancer that permit us to better delineate cellular and local microenvironment changes that occur during the initial phase of tumor growth. Unfortunately, technologies capable of exploiting this knowledge for the early detection and treatment of this devastating disease have been poor at best. The goal of this proposal is to develop enhanced diagnostic methods and to explore a potential novel therapy for the treatment of breast cancer by exploiting the molecular signatures that best define this disease state.

To accomplish these goals, we will utilize molecular markers that help identify patients with breast cancer in the early stages of their disease and/or a cancer that needs aggressive treatment. Our focus is on the cell surface proteins Notch and its ligands, which are highly expressed in human breast cancer and the vasculature that supplies it. Moreover, this cell signaling system is known to promote breast cancer growth and as well as the formation of tumor blood vessels. We will focus specifically on the Notch receptor, Notch1 and the Notch ligands known as Jagged-1 and Delta-4 (Delta-like 4). There are several compelling reasons to develop diagnostic tools to detect this class of cell surface proteins. First, Delta-4 is over-expressed on the vasculature supplying human breast cancer in contrast to non-tumor vessels, thus making it an excellent candidate marker for diagnosis by imaging. Second, Jagged-1 and Notch1 are highly produced in breast cancer patients with poor prognosis. In fact, preliminary data suggests that breast cancer undergoing metastasis expresses high levels of the activated form of Notch1. Thus, it would of great benefit to be able to detect elevated expression of these proteins in such individuals, as they may need a more aggressive course of therapy. Moreover, preliminary in vivo observations also suggest that blockade of the Notch signaling pathway by use of a decoy receptor significantly retards tumor growth.

The first aims of this proposal are to develop new diagnostic strategies for assessing serum levels as well as tissue and tumor vessel expression of Notch and its ligands. We propose to generate antibodies that specifically recognize these proteins to ultimately develop an ELISA based detection system for Jagged-1 and Notch1 in blood that can be used in clinics. In addition, such antibodies will be used to target nanoparticles to tumor vessels that can be detected by commercially available imaging modalities such as ultrasound and MRI. Xenografts of human breast cancer cell lines that over-express Jagged-1 be will be grown in mice. Serum will be collected and analyzed for the extracellular domains of Jagged-1 that may be shed into the blood stream from breast tumors. We will also incorporate antibodies directed against Notch ligands, such as Delta-4, into a nanoparticle based detection system and evaluate their ability to preferentially localize on blood vessels supplying breast cancer tumors using state-of-the-art imaging technology, confocal intravital microscopy. This imaging system permits for direct observation of nanoparticle localization on the vessel wall in real time in a living animal. Information gleaned from such experiments include the 1) selectively of nanoparticle binding to Delta-like 4, and 2) the rate of accumulation and duration of binding, events critical for determining optimal viewing time and signal strength for future clinical imaging modalities. These combined studies may lead to a series of non-invasive assays that can be applied in the clinic in a timely fashion. FDA approval is currently being sought for the in vivo use of the nanoparticle imaging system and alliances with industry have already been formed, which will also expedite clinical development.

Ultimately, the successful treatment of breast cancer will depend on a pipeline of novel and safe inhibitors of tumor growth and angiogenesis. This proposal will also explore novel therapeutics that target the Notch signaling pathway. To date, no published work has described specific inhibitors of ligand-dependent Notch. We will make neutralizing antibodies to its ligands Jagged-1 and Delta-4 and compare their utility and efficacy to an inhibitor we have already developed, Notch1 decoy, that shows promise in retarding tumor growth in vivo. Exploring multiple inhibitory paradigms (decoys versus neutralizing antibodies) is merited if one is to define the most efficacious and least toxic reagent to pursue in the clinic. Thus, we present a new, and hopefully, powerful series of approaches to address the need for novel Notch inhibitors for the treatment of breast cancer.

This work is being funded by the Department of Defense with Dr. Jan Kitajewski as the Principal Investigator.